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<record><TEI><teiHeader><fileDesc><titleStmt><title xml:lang="en">Targeting zoonotic viruses: Structure-based inhibition of the 3C-like protease from bat coronavirus HKU4—The likely reservoir host to the human coronavirus that causes Middle East Respiratory Syndrome (MERS)</title><author><name sortKey="St John, Sarah E" sort="St John, Sarah E" uniqKey="St John S" first="Sarah E." last="St. John">Sarah E. St. John</name><affiliation><nlm:aff id="af005">Department of Biological Sciences, Purdue University, West Lafayette, IN, USA</nlm:aff></affiliation><affiliation><nlm:aff id="af010">Department of Chemistry, Purdue University, West Lafayette, IN, USA</nlm:aff></affiliation><affiliation><nlm:aff id="af015">Centers for Cancer Research & Drug Discovery, Purdue University, West Lafayette, IN, USA</nlm:aff></affiliation></author><author><name sortKey="Tomar, Sakshi" sort="Tomar, Sakshi" uniqKey="Tomar S" first="Sakshi" last="Tomar">Sakshi Tomar</name><affiliation><nlm:aff id="af005">Department of Biological Sciences, Purdue University, West Lafayette, IN, USA</nlm:aff></affiliation><affiliation><nlm:aff id="af015">Centers for Cancer Research & Drug Discovery, Purdue University, West Lafayette, IN, USA</nlm:aff></affiliation></author><author><name sortKey="Stauffer, Shaun R" sort="Stauffer, Shaun R" uniqKey="Stauffer S" first="Shaun R." last="Stauffer">Shaun R. Stauffer</name><affiliation><nlm:aff id="af020">Department of Pharmacology, Vanderbilt University Medical Center, Nashville, TN, USA</nlm:aff></affiliation><affiliation><nlm:aff id="af025">Department of Chemistry, Vanderbilt University Medical Center, Nashville, TN, USA</nlm:aff></affiliation></author><author><name sortKey="Mesecar, Andrew D" sort="Mesecar, Andrew D" uniqKey="Mesecar A" first="Andrew D." last="Mesecar">Andrew D. Mesecar</name><affiliation><nlm:aff id="af005">Department of Biological Sciences, Purdue University, West Lafayette, IN, USA</nlm:aff></affiliation><affiliation><nlm:aff id="af010">Department of Chemistry, Purdue University, West Lafayette, IN, USA</nlm:aff></affiliation><affiliation><nlm:aff id="af015">Centers for Cancer Research & Drug Discovery, Purdue University, West Lafayette, IN, USA</nlm:aff></affiliation></author></titleStmt><publicationStmt><idno type="wicri:source">PMC</idno><idno type="pmid">26190463</idno><idno type="pmc">5433438</idno><idno type="url">http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5433438</idno><idno type="RBID">PMC:5433438</idno><idno type="doi">10.1016/j.bmc.2015.06.039</idno><date when="2015">2015</date><idno type="wicri:Area/Pmc/Corpus">000B35</idno><idno type="wicri:explorRef" wicri:stream="Pmc" wicri:step="Corpus" wicri:corpus="PMC">000B35</idno></publicationStmt><sourceDesc><biblStruct><analytic><title xml:lang="en" level="a" type="main">Targeting zoonotic viruses: Structure-based inhibition of the 3C-like protease from bat coronavirus HKU4—The likely reservoir host to the human coronavirus that causes Middle East Respiratory Syndrome (MERS)</title><author><name sortKey="St John, Sarah E" sort="St John, Sarah E" uniqKey="St John S" first="Sarah E." last="St. John">Sarah E. St. John</name><affiliation><nlm:aff id="af005">Department of Biological Sciences, Purdue University, West Lafayette, IN, USA</nlm:aff></affiliation><affiliation><nlm:aff id="af010">Department of Chemistry, Purdue University, West Lafayette, IN, USA</nlm:aff></affiliation><affiliation><nlm:aff id="af015">Centers for Cancer Research & Drug Discovery, Purdue University, West Lafayette, IN, USA</nlm:aff></affiliation></author><author><name sortKey="Tomar, Sakshi" sort="Tomar, Sakshi" uniqKey="Tomar S" first="Sakshi" last="Tomar">Sakshi Tomar</name><affiliation><nlm:aff id="af005">Department of Biological Sciences, Purdue University, West Lafayette, IN, USA</nlm:aff></affiliation><affiliation><nlm:aff id="af015">Centers for Cancer Research & Drug Discovery, Purdue University, West Lafayette, IN, USA</nlm:aff></affiliation></author><author><name sortKey="Stauffer, Shaun R" sort="Stauffer, Shaun R" uniqKey="Stauffer S" first="Shaun R." last="Stauffer">Shaun R. Stauffer</name><affiliation><nlm:aff id="af020">Department of Pharmacology, Vanderbilt University Medical Center, Nashville, TN, USA</nlm:aff></affiliation><affiliation><nlm:aff id="af025">Department of Chemistry, Vanderbilt University Medical Center, Nashville, TN, USA</nlm:aff></affiliation></author><author><name sortKey="Mesecar, Andrew D" sort="Mesecar, Andrew D" uniqKey="Mesecar A" first="Andrew D." last="Mesecar">Andrew D. Mesecar</name><affiliation><nlm:aff id="af005">Department of Biological Sciences, Purdue University, West Lafayette, IN, USA</nlm:aff></affiliation><affiliation><nlm:aff id="af010">Department of Chemistry, Purdue University, West Lafayette, IN, USA</nlm:aff></affiliation><affiliation><nlm:aff id="af015">Centers for Cancer Research & Drug Discovery, Purdue University, West Lafayette, IN, USA</nlm:aff></affiliation></author></analytic><series><title level="j">Bioorganic & Medicinal Chemistry</title><idno type="ISSN">0968-0896</idno><idno type="eISSN">1464-3391</idno><imprint><date when="2015">2015</date></imprint></series></biblStruct></sourceDesc></fileDesc><profileDesc><textClass></textClass></profileDesc></teiHeader><front><div type="abstract" xml:lang="en"><title>Graphical abstract</title><fig id="f0045" position="anchor"><graphic xlink:href="fx1"></graphic></fig></div></front><back><div1 type="bibliography"><listBibl><biblStruct><analytic><author><name sortKey="Mcintosh, K" uniqKey="Mcintosh K">K. 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<front><journal-meta><journal-id journal-id-type="nlm-ta">Bioorg Med Chem</journal-id><journal-id journal-id-type="iso-abbrev">Bioorg. Med. Chem</journal-id><journal-title-group><journal-title>Bioorganic & Medicinal Chemistry</journal-title></journal-title-group><issn pub-type="ppub">0968-0896</issn><issn pub-type="epub">1464-3391</issn><publisher><publisher-name>Elsevier Ltd.</publisher-name></publisher></journal-meta><article-meta><article-id pub-id-type="pmid">26190463</article-id><article-id pub-id-type="pmc">5433438</article-id><article-id pub-id-type="publisher-id">S0968-0896(15)00533-7</article-id><article-id pub-id-type="doi">10.1016/j.bmc.2015.06.039</article-id><article-categories><subj-group subj-group-type="heading"><subject>Article</subject></subj-group></article-categories><title-group><article-title>Targeting zoonotic viruses: Structure-based inhibition of the 3C-like protease from bat coronavirus HKU4—The likely reservoir host to the human coronavirus that causes Middle East Respiratory Syndrome (MERS)</article-title></title-group><contrib-group><contrib contrib-type="author" id="au005"><name><surname>St. John</surname><given-names>Sarah E.</given-names></name><xref rid="af005" ref-type="aff">a</xref><xref rid="af010" ref-type="aff">b</xref><xref rid="af015" ref-type="aff">c</xref></contrib><contrib contrib-type="author" id="au010"><name><surname>Tomar</surname><given-names>Sakshi</given-names></name><xref rid="af005" ref-type="aff">a</xref><xref rid="af015" ref-type="aff">c</xref></contrib><contrib contrib-type="author" id="au015"><name><surname>Stauffer</surname><given-names>Shaun R.</given-names></name><xref rid="af020" ref-type="aff">d</xref><xref rid="af025" ref-type="aff">e</xref></contrib><contrib contrib-type="author" id="au020"><name><surname>Mesecar</surname><given-names>Andrew D.</given-names></name><email>amesecar@purdue.edu</email><xref rid="af005" ref-type="aff">a</xref><xref rid="af010" ref-type="aff">b</xref><xref rid="af015" ref-type="aff">c</xref><xref rid="cor1" ref-type="corresp">⁎</xref></contrib></contrib-group><aff id="af005"><label>a</label>Department of Biological Sciences, Purdue University, West Lafayette, IN, USA</aff><aff id="af010"><label>b</label>Department of Chemistry, Purdue University, West Lafayette, IN, USA</aff><aff id="af015"><label>c</label>Centers for Cancer Research & Drug Discovery, Purdue University, West Lafayette, IN, USA</aff><aff id="af020"><label>d</label>Department of Pharmacology, Vanderbilt University Medical Center, Nashville, TN, USA</aff><aff id="af025"><label>e</label>Department of Chemistry, Vanderbilt University Medical Center, Nashville, TN, USA</aff><author-notes><corresp id="cor1"><label>⁎</label>Corresponding author at present address: Departments of Biological Sciences and Chemistry, Purdue University, 915 West State Street, West Lafayette, IN 47907, USA. Tel.: +1 765 494 1924. <email>amesecar@purdue.edu</email></corresp></author-notes><pub-date pub-type="pmc-release"><day>19</day><month>6</month><year>2015</year></pub-date><pmc-comment> PMC Release delay is 0 months and 0 days and was based on .</pmc-comment>
<pub-date pub-type="ppub"><day>1</day><month>9</month><year>2015</year></pub-date><pub-date pub-type="epub"><day>19</day><month>6</month><year>2015</year></pub-date><volume>23</volume><issue>17</issue><fpage>6036</fpage><lpage>6048</lpage><history><date date-type="received"><day>16</day><month>4</month><year>2015</year></date><date date-type="rev-recd"><day>2</day><month>6</month><year>2015</year></date><date date-type="accepted"><day>10</day><month>6</month><year>2015</year></date></history><permissions><copyright-statement>Copyright © 2015 Elsevier Ltd. All rights reserved.</copyright-statement><copyright-year>2015</copyright-year><copyright-holder>Elsevier Ltd</copyright-holder><license><license-p>Since January 2020 Elsevier has created a COVID-19 resource centre with free information in English and Mandarin on the novel coronavirus COVID-19. The COVID-19 resource centre is hosted on Elsevier Connect, the company's public news and information website. Elsevier hereby grants permission to make all its COVID-19-related research that is available on the COVID-19 resource centre - including this research content - immediately available in PubMed Central and other publicly funded repositories, such as the WHO COVID database with rights for unrestricted research re-use and analyses in any form or by any means with acknowledgement of the original source. These permissions are granted for free by Elsevier for as long as the COVID-19 resource centre remains active.</license-p></license></permissions><abstract abstract-type="graphical" id="ab005"><title>Graphical abstract</title><fig id="f0045" position="anchor"><graphic xlink:href="fx1"></graphic></fig></abstract><abstract id="ab010"><p>The bat coronavirus HKU4 belongs to the same 2c lineage as that of the deadly Middle East Respiratory Syndrome coronavirus (MERS-CoV) and shows high sequence similarity, therefore potentiating a threat to the human population through a zoonotic shift or ‘spill over’ event. To date, there are no effective vaccines or antiviral treatments available that are capable of limiting the pathogenesis of any human coronaviral infection. An attractive target for the development of anti-coronaviral therapeutics is the 3C-like protease (3CL<sup>pro</sup>), which is essential for the progression of the coronaviral life cycle. Herein, we report the screening results of a small, 230-member peptidomimetic library against HKU4-CoV 3CL<sup>pro</sup> and the identification of 43 peptidomimetic compounds showing good to excellent inhibitory potency of HKU4-CoV 3CL<sup>pro</sup> with IC<sub>50</sub> values ranging from low micromolar to sub-micromolar. We established structure–activity relationships (SARs) describing the important ligand-based features required for potent HKU4-CoV 3CL<sup>pro</sup> inhibition and identified a seemingly favored peptidic backbone for HKU4-CoV 3CL<sup>pro</sup> inhibition. To investigate this, a molecular sub-structural analysis of the most potent HKU4-CoV 3CL<sup>pro</sup> inhibitor was accomplished by the synthesis and testing of the lead peptidomimetic inhibitor’s sub-structural components, confirming the activity of the favored backbone (<bold>22A</bold>) identified via SAR analysis. In order to elucidate the structural reasons for such potent HKU4-CoV 3CL<sup>pro</sup> inhibition by the peptidomimetics having the <bold>22A</bold> backbone, we determined the X-ray structures of HKU4-CoV 3CL<sup>pro</sup> in complex with three peptidomimetic inhibitors. Sequence alignment of HKU4-CoV 3CL<sup>pro</sup>, and two other lineage C <italic>Betacoronaviruses</italic> 3CL<sup>pro</sup>’s, HKU5-CoV and MERS-CoV 3CL<sup>pro</sup>, show that the active site residues of HKU4-CoV 3CL<sup>pro</sup> that participate in inhibitor binding are conserved in HKU5-CoV and MERS-CoV 3CL<sup>pro</sup>. Furthermore, we assayed our most potent HKU4-CoV 3CL<sup>pro</sup> inhibitor for inhibition of HKU5-CoV 3CL<sup>pro</sup> and found it to have sub-micromolar inhibitory activity (IC<sub>50</sub> = 0.54 ± 0.03 μM). The X-ray structures and SAR analysis reveal critical insights into the structure and inhibition of HKU4-CoV 3CL<sup>pro</sup>, providing fundamental knowledge that may be exploited in the development of anti-coronaviral therapeutics for coronaviruses emerging from zoonotic reservoirs.</p></abstract><kwd-group id="kg005"><title>Keywords</title><kwd>Coronavirus</kwd><kwd>3C-like protease</kwd><kwd>MERS</kwd><kwd>HKU4</kwd><kwd>HKU5</kwd><kwd>SARS</kwd><kwd>Peptidomimetic compounds</kwd><kwd>Broad-spectrum inhibitors</kwd><kwd>Protease inhibitors</kwd><kwd>Zoonotic reservoir</kwd></kwd-group></article-meta></front><body><sec id="s0005"><label>1</label><title>Introduction</title><p id="p0005">Zoonotic viruses, including coronaviruses, Ebola virus, HIV, influenza A viruses, hantaviruses and henipaviruses, are ubiquitous and can emerge as significant human pathogens capable of global epidemics and pandemics. Most often, we spend our time and resources in targeting only the human pathogens using small molecule inhibitors with the ultimate goal of developing therapeutic compounds to treat the associated diseases. A missed opportunity, however, is targeting the zoonotic host using small molecule inhibitors with the goal of utilizing the acquired chemical and structural knowledge to inform us of the evolutionary path of the virus on a biological basis. So, we believe that by using small molecule compounds as probes of the structural evolution of viral enzyme drug targets, from the zoonotic reservoirs to the human pathogens, we can gain new insights and predict a priori the structural scaffolds of small molecule compounds that can serve as lead templates for therapeutic development against emerging human pathogenic viruses such as coronaviruses.</p><p id="p0010">Coronaviruses (CoVs) are enveloped, single-stranded, positive-sense RNA viruses that infect and cause disease in a variety of species including bats, birds, cats, dogs, pigs, mice, horses, whales, and humans.<xref rid="b0005" ref-type="bibr">1</xref>, <xref rid="b0010" ref-type="bibr">2</xref>, <xref rid="b0015" ref-type="bibr">3</xref> Coronaviral infections may range from mild to severe and can result in respiratory, enteric, hepatic, or neurological diseases in their carriers. The first two human CoV strains (HCoV-229E and HCoV-OC43) were identified in the mid-1960s, and it was not until the 21st century that a new human coronavirus (Severe Acute Respiratory Syndrome or SARS-CoV) was identified.<xref rid="b0020" ref-type="bibr">4</xref>, <xref rid="b0025" ref-type="bibr">5</xref> Currently, there are at least six known human CoVs including: HCoV-229E, HCoV-NL63, HCoV-OC43, HCoV-HKU1, SARS-CoV, and most recently, the Middle East Respiratory Syndrome coronavirus (MERS-CoV).<xref rid="b0030" ref-type="bibr"><sup>6</sup></xref> MERS-CoV, formerly known as HCoV-EMC, was identified in November 2012, when it was isolated from the sputum a 60-year-old Saudi Arabian man presenting acute pneumonia and renal failure.<xref rid="b0035" ref-type="bibr"><sup>7</sup></xref> Since the time of its identification, the virus has grown to be a threat to public health worldwide having a case-fatality rate of about 30%.<xref rid="b0040" ref-type="bibr"><sup>8</sup></xref> To date, there are no vaccines or antiviral agents capable of preventing or treating any human coronaviral infection.</p><p id="p0015">MERS-CoV belongs to lineage C in the genus <italic>Betacoronavirus</italic> of the <italic>Coronaviridae</italic> family in the <italic>Nidovirales</italic> order.<xref rid="b0045" ref-type="bibr"><sup>9</sup></xref> Also of this lineage are the species <italic>Tylonycteris</italic> bat coronavirus HKU4 (HKU4-CoV) and <italic>Pipistrellus</italic> bat coronavirus HKU5 (HKU5-CoV), where the overall amino acid sequence identities of MERS-CoV to HKU4-CoV and HKU5-CoV across the conserved domains are approximately 75% and 76.7%, respectively.<xref rid="b0030" ref-type="bibr">6</xref>, <xref rid="b0050" ref-type="bibr">10</xref>, <xref rid="b0055" ref-type="bibr">11</xref> Though the exact origin of MERS-CoV is currently debated, a bat origin is strongly suspected as MERS-CoV is so closely related to HKU4- and HKU5-CoV and because MERS-CoV genomic RNA has been found in bats and dromedary camels in Qatar.<xref rid="b0060" ref-type="bibr">12</xref>, <xref rid="b0065" ref-type="bibr">13</xref> Though HKU4-CoV and HKU5-CoV have been found only in bats, studies have shown that their accessory proteins are capable of inhibiting human antiviral signaling pathways in vitro.<xref rid="b0070" ref-type="bibr">14</xref>, <xref rid="b0075" ref-type="bibr">15</xref> This, and the close similarity of MERS-CoV to HKU4-CoV and HKU5-CoV, suggests that a zoonotic shift from bats or camels to humans may have occurred.<xref rid="b0075" ref-type="bibr"><sup>15</sup></xref> A recent investigation into the interactions between the human CD26 receptor and the receptor binding domains (RBDs) in the MERS-CoV, HKU4-CoV and HKU5-CoV envelope-embedded spike protein revealed that MERS-CoV and HKU4-CoV both engage this receptor for viral entry whereas HKU5-CoV does not.<xref rid="b0080" ref-type="bibr"><sup>16</sup></xref> These observations suggest that an evolutionary pathway from bat HKU4-CoV to human MERS-CoV exists and that investigating the molecular basis of this zoonotic shift from a structural and chemical-biology perspective may allow us to predict and target the these viruses with small molecule therapeutics.</p><p id="p0020">Coronaviral genomes are polycistronic, encoding for two large polyproteins, pp1a and pp1ab.<xref rid="b0085" ref-type="bibr">17</xref>, <xref rid="b0090" ref-type="bibr">18</xref>, <xref rid="b0095" ref-type="bibr">19</xref>, <xref rid="b0100" ref-type="bibr">20</xref> Initiation of coronavirus replication in cells occurs by the translation of two overlapping, open reading frames (ORF1a and ORF1b) to produce pp1a and, following a −1 ribosomal frameshift mechanism, pp1ab. These polyproteins are then proteolytically processed at 14 cleavage sites by two essential viral cysteine proteases, the papain-like protease (PL<sup>pro</sup>, or nsp3) and the 3C-like protease (3CL<sup>pro</sup>, also known as the main protease, M<sup>pro</sup>, or nsp5). Cleavage by both proteases results in the production of 16 nonstructural proteins (nsps), where PL<sup>pro</sup> is responsible for cleavage at 3 sites and 3CL<sup>pro</sup> is responsible for cleavage at 11 sites (<xref rid="f0005" ref-type="fig">Fig. 1</xref>). The function of 3CL<sup>pro</sup> is vital for the coronaviral life cycle, making it an attractive target for the development of antiviral drugs.<xref rid="b0105" ref-type="bibr">21</xref>, <xref rid="b0110" ref-type="bibr">22</xref><fig id="f0005"><label>Figure 1</label><caption><p>Genome and proteome organization of HKU4-, HKU5-, and MERS-CoV non-structural proteins highlighting the PLpro and 3CL-pro cleavage sites.</p></caption><graphic xlink:href="gr1"></graphic></fig></p><p id="p0025">The present work was undertaken to investigate the kinetic and structural properties of HKU4-CoV 3CL<sup>pro</sup> and to utilize this knowledge to discover and develop potent inhibitors of HKU4-CoV 3CL<sup>pro</sup>. Targeting the immediate zoonotic reservoirs of coronaviruses with small molecule inhibitors can help inform structure-based design strategies aimed at creating molecular scaffolds that may also target the emerging human CoVs and ultimately aid in the development of therapeutics against coronaviral infection. Toward this goal, we first expressed, purified, and characterized the kinetic properties of HKU4-CoV 3CL<sup>pro</sup>. We then determined the inhibition of HKU4-CoV 3CLpro by a small library of 230 peptidomimetic compounds, which resulted in the identification of 43 HKU4-CoV 3CLpro inhibitors, two of which showed sub-micromolar potency. With a potent lead inhibitor compound in hand, we investigated the contributions of its individual sub-structural components to inhibitory potency and identified a favored peptidic backbone for HKU4-CoV 3CL<sup>pro</sup> inhibition. Finally, we determined the X-ray crystal structures of the three most potent inhibitors containing this favored backbone in complex with HKU4-CoV 3CL<sup>pro</sup> and elucidated the structural reasons behind such potent HKU4-CoV 3CL<sup>pro</sup> inhibition.</p></sec><sec id="s0010"><label>2</label><title>Results and discussion</title><sec id="s0015"><label>2.1</label><title>Screen of peptidomimetic library for HKU4-CoV 3CL<sup>pro</sup> inhibition</title><p id="p0030">A library of 230 previously reported, peptidomimetic-type compounds<xref rid="b0115" ref-type="bibr">23</xref>, <xref rid="b0120" ref-type="bibr">24</xref> was screened for inhibition of HKU4-CoV 3CL<sup>pro</sup> at a single concentration of 100 μM, and IC<sub>50</sub> values were determined for compounds that showed greater than 50% inhibition of HKU4-CoV 3CL<sup>pro</sup> at that concentration. This screen resulted in the identification of 43 peptidomimetic compounds with inhibitory concentrations ranging from micromolar to sub-micromolar (vide infra). The peptidomimetic inhibitors can be grouped into two classes, inhibitors with a single amide bond in the inhibitor backbone (Class A) and inhibitors with a dipeptide-like backbone (Class B). The results of this screen are displayed in <xref rid="t0005" ref-type="table">Table 1a</xref>(Class A) and <xref rid="t0010" ref-type="table">Table 1b</xref>(Class B), where only the compounds that showed greater than 50% inhibition of HKU4-CoV 3CL<sup>pro</sup> at 100 μM are shown (see <xref rid="s0085" ref-type="sec">Supporting information S1 and S2</xref> for comprehensive list of compounds tested). The compounds are listed in the tables in rank order by IC<sub>50</sub> values starting with the lowest IC<sub>50</sub> value. Of the 25 Class A inhibitors that were tested for inhibition of HKU4-CoV 3CL<sup>pro</sup>, 19 were found to inhibit HKU4-CoV 3CL<sup>pro</sup> above 50% at a concentration of 100 μM, and subsequently, IC<sub>50</sub> values were determined. Remarkably, the two most potent inhibitors, <bold>1A</bold> and <bold>2A</bold>, proved to be sub-micromolar inhibitors of HKU4-CoV 3CL<sup>pro</sup>, having IC<sub>50</sub>’s of 0.33 ± 0.02 and 0.41 ± 0.04 μM, respectively. Upon examination of the 19 Class A inhibitors, an immediate trend is apparent where there is an overwhelming preference for a 3-thiophene at the R<sub>1</sub> position and a 1-methylbenzotriazole at the R<sub>3</sub> position of the peptidomimetic backbone. This is observed in every Class A inhibitor found to produce inhibition of HKU4-CoV 3CL<sup>pro</sup> over 50% at 100 μM, with the exception of the least active analog in this series, <bold>19A</bold>. <bold>19A</bold> only differs from the more active compound <bold>6A</bold> in that <bold>19A</bold> has a triazole in place of a benzotriazole; however, this difference is significant enough to decrease inhibitory potency ten-fold between the analogs, from 1.6 ± 0.1 μM for <bold>6A</bold> to 16.0 ± 4.0 μM for <bold>19A</bold>. Interestingly, <bold>19A</bold> maintains a triazole ring in the R<sub>3</sub> position, indicating that the position of the nitrogen atoms in this heterocycle is essential for good HKU4-CoV 3CL<sup>pro</sup> inhibition. Other R<sub>3</sub> heterocycles incorporated in the less active members of Class A include 4-substituted methyltriazoles, 4-imidazoles, and 2-furans, underscoring the importance of the methylbenzotriazole at the R<sub>3</sub> position and pointing to the potential significance of a precisely oriented hydrogen bond acceptor (see <xref rid="s0085" ref-type="sec">Supporting information S1</xref> for a comprehensive list).<table-wrap position="float" id="t0005"><label>Table 1a</label><caption><p>Class A peptidomimetic inhibitors<fig id="f0035"><graphic xlink:href="fx2"></graphic></fig></p></caption><table frame="hsides" rules="groups"><thead><tr><th>Compd</th><th>R<sub>1</sub></th><th>R<sub>2</sub></th><th>R<sub>3</sub></th><th>IC<sub>50</sub> (μM)</th></tr></thead><tbody><tr><td><bold>1A</bold></td><td><inline-graphic xlink:href="fx3.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx4.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx5.gif"></inline-graphic></td><td align="char">0.33 ± 0.02</td></tr><tr><td><bold>2A</bold></td><td><inline-graphic xlink:href="fx6.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx7.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx8.gif"></inline-graphic></td><td align="char">0.41 ± 0.04</td></tr><tr><td><bold>3A</bold></td><td><inline-graphic xlink:href="fx9.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx10.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx11.gif"></inline-graphic></td><td align="char">1.2 ± 0.2</td></tr><tr><td><bold>4A</bold></td><td><inline-graphic xlink:href="fx12.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx13.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx14.gif"></inline-graphic></td><td align="char">1.2 ± 0.06</td></tr><tr><td><bold>5A</bold></td><td><inline-graphic xlink:href="fx15.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx16.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx17.gif"></inline-graphic></td><td align="char">1.5 ± 0.1</td></tr><tr><td><bold>6A</bold></td><td><inline-graphic xlink:href="fx18.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx19.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx20.gif"></inline-graphic></td><td align="char">1.6 ± 0.09</td></tr><tr><td><bold>7A</bold></td><td><inline-graphic xlink:href="fx21.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx22.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx23.gif"></inline-graphic></td><td align="char">1.7 ± 0.2</td></tr><tr><td><bold>8A</bold></td><td><inline-graphic xlink:href="fx24.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx25.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx26.gif"></inline-graphic></td><td align="char">1.9 ± 0.09</td></tr><tr><td><bold>9A</bold></td><td><inline-graphic xlink:href="fx27.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx28.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx29.gif"></inline-graphic></td><td align="char">2.0 ± 0.2</td></tr><tr><td><bold>10A</bold></td><td><inline-graphic xlink:href="fx30.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx31.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx32.gif"></inline-graphic></td><td align="char">2.2 ± 0.2</td></tr><tr><td><bold>11A</bold></td><td><inline-graphic xlink:href="fx33.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx34.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx35.gif"></inline-graphic></td><td align="char">2.4 ± 0.3</td></tr><tr><td><bold>12A</bold></td><td><inline-graphic xlink:href="fx36.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx37.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx38.gif"></inline-graphic></td><td align="char">2.8 ± 0.4</td></tr><tr><td><bold>13A</bold></td><td><inline-graphic xlink:href="fx39.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx40.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx41.gif"></inline-graphic></td><td align="char">3.1 ± 0.3</td></tr><tr><td><bold>14A</bold></td><td><inline-graphic xlink:href="fx42.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx43.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx44.gif"></inline-graphic></td><td align="char">3.1 ± 0.3</td></tr><tr><td><bold>15A</bold></td><td><inline-graphic xlink:href="fx45.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx46.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx47.gif"></inline-graphic></td><td align="char">3.7 ± 0.4</td></tr><tr><td><bold>16A</bold></td><td><inline-graphic xlink:href="fx48.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx49.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx50.gif"></inline-graphic></td><td align="char">4.8 ± 0.4</td></tr><tr><td><bold>17A</bold></td><td><inline-graphic xlink:href="fx51.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx52.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx53.gif"></inline-graphic></td><td align="char">5.3 ± 0.6</td></tr><tr><td><bold>18A</bold></td><td><inline-graphic xlink:href="fx54.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx55.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx56.gif"></inline-graphic></td><td align="char">8.8 ± 0.8</td></tr><tr><td><bold>19A</bold></td><td><inline-graphic xlink:href="fx57.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx58.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx59.gif"></inline-graphic></td><td align="char">16.0 ± 4.0</td></tr></tbody></table></table-wrap><table-wrap position="float" id="t0010"><label>Table 1b</label><caption><p>Class B peptidomimetic inhibitors<fig id="f0040"><graphic xlink:href="fx60"></graphic></fig></p></caption><table frame="hsides" rules="groups"><thead><tr><th>Compd</th><th>R<sub>1</sub></th><th>R<sub>2</sub></th><th>R<sub>3</sub></th><th>R<sub>4</sub></th><th>IC<sub>50</sub> (μM)</th></tr></thead><tbody><tr><td><bold>1B</bold></td><td><inline-graphic xlink:href="fx61.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx62.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx63.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx64.gif"></inline-graphic></td><td align="char">1.3 ± 0.3</td></tr><tr><td><bold>2B</bold></td><td><inline-graphic xlink:href="fx65.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx66.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx67.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx68.gif"></inline-graphic></td><td align="char">1.5 ± 0.3</td></tr><tr><td><bold>3B</bold></td><td><inline-graphic xlink:href="fx69.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx70.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx71.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx72.gif"></inline-graphic></td><td align="char">1.8 ± 0.5</td></tr><tr><td><bold>4B</bold></td><td><inline-graphic xlink:href="fx73.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx74.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx75.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx76.gif"></inline-graphic></td><td align="char">2.2 ± 0.6</td></tr><tr><td><bold>5B</bold></td><td><inline-graphic xlink:href="fx77.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx78.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx79.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx80.gif"></inline-graphic></td><td align="char">2.2 ± 0.4</td></tr><tr><td><bold>6B</bold></td><td><inline-graphic xlink:href="fx81.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx82.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx83.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx84.gif"></inline-graphic></td><td align="char">2.7 ± 0.4</td></tr><tr><td><bold>7B</bold></td><td><inline-graphic xlink:href="fx85.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx86.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx87.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx88.gif"></inline-graphic></td><td align="char">3.4 ± 0.4</td></tr><tr><td><bold>8B</bold></td><td><inline-graphic xlink:href="fx89.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx90.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx91.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx92.gif"></inline-graphic></td><td align="char">3.9 ± 0.7</td></tr><tr><td><bold>9B</bold></td><td><inline-graphic xlink:href="fx93.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx94.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx95.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx96.gif"></inline-graphic></td><td align="char">4.2 ± 0.2</td></tr><tr><td><bold>10B</bold></td><td><inline-graphic xlink:href="fx97.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx98.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx99.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx100.gif"></inline-graphic></td><td align="char">6.9 ± 0.7</td></tr><tr><td><bold>11B</bold></td><td><inline-graphic xlink:href="fx101.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx102.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx103.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx104.gif"></inline-graphic></td><td align="char">7.0 ± 1.2</td></tr><tr><td><bold>12B</bold></td><td><inline-graphic xlink:href="fx105.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx106.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx107.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx108.gif"></inline-graphic></td><td align="char">8.6 ± 0.9</td></tr><tr><td><bold>13B</bold></td><td><inline-graphic xlink:href="fx109.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx110.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx111.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx112.gif"></inline-graphic></td><td align="char">9.3 ± 0.5</td></tr><tr><td><bold>14B</bold></td><td><inline-graphic xlink:href="fx113.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx114.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx115.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx116.gif"></inline-graphic></td><td align="char">9.5 ± 2.0</td></tr><tr><td><bold>15B</bold></td><td><inline-graphic xlink:href="fx117.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx118.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx119.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx120.gif"></inline-graphic></td><td align="char">11.1 ± 0.6</td></tr><tr><td><bold>16B</bold></td><td><inline-graphic xlink:href="fx121.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx122.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx123.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx124.gif"></inline-graphic></td><td align="char">14.7 ± 1.1</td></tr><tr><td><bold>17B</bold></td><td><inline-graphic xlink:href="fx125.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx126.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx127.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx128.gif"></inline-graphic></td><td align="char">15.4 ± 2.1</td></tr><tr><td><bold>18B</bold></td><td><inline-graphic xlink:href="fx129.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx130.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx131.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx132.gif"></inline-graphic></td><td align="char">17.2 ± 2.8</td></tr><tr><td><bold>19B</bold></td><td><inline-graphic xlink:href="fx133.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx134.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx135.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx136.gif"></inline-graphic></td><td align="char">18.3 ± 4.7</td></tr><tr><td><bold>20B</bold></td><td><inline-graphic xlink:href="fx137.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx138.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx139.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx140.gif"></inline-graphic></td><td align="char">18.7 ± 2.6</td></tr><tr><td><bold>21B</bold></td><td><inline-graphic xlink:href="fx141.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx142.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx143.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx144.gif"></inline-graphic></td><td align="char">22.0 ± 7.4</td></tr><tr><td><bold>22B</bold></td><td><inline-graphic xlink:href="fx145.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx146.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx147.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx148.gif"></inline-graphic></td><td align="char">35.6 ± 5.2</td></tr><tr><td><bold>23B</bold></td><td><inline-graphic xlink:href="fx149.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx150.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx151.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx152.gif"></inline-graphic></td><td align="char">52.3 ± 21.2</td></tr><tr><td><bold>24B</bold></td><td><inline-graphic xlink:href="fx153.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx154.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx155.gif"></inline-graphic></td><td><inline-graphic xlink:href="fx156.gif"></inline-graphic></td><td align="char">55.6 ± 14.3</td></tr></tbody></table></table-wrap></p><p id="p0035">Of the 19 Class A peptidomimetics found to be good inhibitors of HKU4-CoV 3CL<sup>pro</sup>, 13 have amide substituents at R<sub>2</sub>, four have aromatics (<bold>5A</bold>, <bold>7A</bold>, <bold>9A</bold>, and <bold>11A</bold>), and two have amines (<bold>16A</bold> and <bold>17A</bold>). Among the inhibitors with amide substituents at R<sub>2</sub>, a trend can be observed where cyclic carboxamides are preferred (<bold>1A</bold>, <bold>2A</bold>, <bold>3A</bold>, <bold>4A</bold>, and <bold>8A</bold>) to alkyl carboxamides, with the aromatic carboxamides being the most active (<bold>1A</bold> and <bold>2A</bold>). A preference for larger cyclic carboxamides is also observed, where 4, 5 or 6 membered cycles (<bold>1A</bold>, <bold>2A</bold>, <bold>3A</bold>, and <bold>4A</bold>) are preferred over the smaller cyclopropylcarboxamide (<bold>8A</bold>).</p><p id="p0040">Among the six Class A inhibitors with aromatic groups substituted at the R<sub>2</sub> position (<bold>5A</bold>, <bold>7A</bold>, <bold>9A</bold>, <bold>11A</bold>, <bold>20A</bold>, <bold>21A</bold>), only the four compounds <bold>5A</bold>, <bold>7A</bold>, <bold>9A</bold> and <bold>11A</bold> were found to inhibit HKU4-CoV 3CL<sup>pro</sup> above 50% at 100 μM and they each contain aromatic nitrogen heterocycles. The position of the nitrogen is of moderate significance, as a <italic>p</italic>-substituted pyridine at R<sub>2</sub> is 2-fold more active than the <italic>m</italic>-substituted pyridine (<bold>5A</bold> vs <bold>11A</bold>, <xref rid="t0005" ref-type="table">Table 1</xref>a). Bulky substituents on R<sub>2</sub> aromatic heterocycles, such as in <bold>20A</bold>, decrease inhibition of HKU4-CoV 3CL<sup>pro</sup>, indicating a steric requirement within the R<sub>2</sub> binding pocket (<xref rid="t0005" ref-type="table">Table 1</xref>a and <xref rid="s0085" ref-type="sec">S1</xref>). Interestingly, <bold>20A</bold> is one of only two Class A compound having a 3-thiophene at the R<sub>1</sub> position and a 1-methylbenzotriazole at the R<sub>3</sub> position that is not a good inhibitor of HKU4-CoV 3CLpro at 100 μM. Addition of a methoxy substituent to the R<sub>2</sub> heterocycle is tolerated (<bold>7A</bold> and <bold>9A</bold>, <xref rid="t0005" ref-type="table">Table 1</xref>a), but does not increase or decrease inhibition significantly, indicating that the addition of another hydrogen-bond acceptor does not further engage the R<sub>2</sub> binding pocket and that smaller aromatic substituents can be tolerated.</p><p id="p0045">The two Class A peptidomimetics that have R<sub>2</sub> amines, <bold>16A</bold> and <bold>17A</bold>, have similar IC<sub>50</sub> values (4.8 ± 0.4 and 5.3 ± 0.6 μM, respectively); however, they have vastly different steric requirements (methyl vs benzyl). As opposed to the R<sub>2</sub> amides and aromatics, this may indicate that when an amine substituent is present at the R<sub>2</sub> position, it dictates an alternative binding orientation within the R<sub>2</sub> binding space that does not lead to such strict steric requirements. Alternatively, the relatively hydrophobic benzyl group of <bold>17A</bold> may decrease inhibitor solubility and consequent inhibitor availability, therefore resulting in lower% maximum inhibition and IC<sub>50</sub> value than would otherwise be observed. This may also be the case for <bold>21A</bold>, where the R<sub>2</sub> aromatic ring lacks the nitrogen found in the more active inhibitors <bold>5A</bold> and <bold>11A</bold> (<xref rid="t0005" ref-type="table">Table 1</xref>a and <xref rid="s0085" ref-type="sec">S1</xref>).</p><p id="p0050">A comparison of <bold>17A</bold> to the second most active inhibitor in Class A, <bold>2A</bold>, which is only different from <bold>17A</bold> by the presence of a carbonyl, shows that the carbonyl of <bold>2A</bold> is crucial for sub-micromolar inhibitory potency (0.41 ± 0.04 μM for <bold>2A</bold> vs. 5.3 ± 0.6 μM for <bold>17A</bold>). This observed 10-fold increase in IC<sub>50</sub> may be a consequence of the loss of a stabilizing hydrogen-bond interaction between the amide –NH group or carbonyl oxygen of the inhibitor and the HKU4-CoV 3CL<sup>pro</sup> binding site. The change in hybridization between an amine and an amide also results in a change in the molecular geometry of the R<sub>2</sub> substituent, which may alter hydrogen-bonding properties and introduce additional effects that may be important factors in dictating good enzymatic inhibition. The X-ray structure of HKU4-CoV 3CL<sup>pro</sup> in complex with <bold>2A</bold>, discussed below, shows that the amide –NH group of the carboxamide group of <bold>2A</bold> forms an important interaction with the backbone carbonyl of His41.</p><p id="p0055">Of the 205 Class B inhibitors that were tested for inhibition of HKU4-CoV 3CL<sup>pro</sup>, 24 were found to inhibit HKU4-CoV 3CL<sup>pro</sup> above 50% at a concentration of 100 μM, and subsequently, IC<sub>50</sub> values were determined (<xref rid="t0005" ref-type="table">Table 1</xref>b). Interestingly, we found fewer good inhibitors and no sub-micromolar inhibitors of HKU4-CoV 3CL<sup>pro</sup> among this larger, more substituted dipeptide-like class of compounds (∼76% of compounds in Class A (19 of 25 compounds tested) were good inhibitors of HKU4-CoV 3CL<sup>pro</sup> while only ∼12% of compounds in Class B (24 of 205 compounds tested) were found to be good inhibitors). This result could be a consequence of the increased steric bulk perturbing the preferred binding orientation of the Class B compounds in the HKU4-CoV 3CL<sup>pro</sup> binding site. A comparison of similar Class A and Class B inhibitors more clearly elucidates this trend, where the addition of the sterically bulky R<sub>4</sub><italic>t</italic>-Bu amide in the Class B compounds decreases HKU4-CoV 3CL<sup>pro</sup> inhibition in each instance (S3) (see <xref rid="s0085" ref-type="sec">Table S3 in the Supporting information</xref>). For example, the most active Class A inhibitor, <bold>1A</bold>, having and IC<sub>50</sub> of 0.33 ± 0.02 μM and 93% inhibition at 100 μM, is almost completely inactivated by the addition of the <italic>t</italic>-Bu amide as seen in the Class B compound <bold>25B</bold>, with only 26% inhibition at 100 μM. Within the Class B inhibitors, there is a preference for the 3-thiophene at the R<sub>1</sub> position and a 1-methylbenzotriazole at the R<sub>3</sub> position of the peptidomimetic backbone, though it is not as strong as that observed in within Class A (25% of compounds in Class B vs. 95% of compounds in Class A). Among the series where R<sub>1</sub> = 3-thiophene and R<sub>3</sub> = 1-methylbenzotriazole (compounds <bold>3B</bold>, <bold>6B</bold>, <bold>9B</bold>, <bold>16B</bold>, <bold>18B</bold>, and <bold>21B</bold>) small carboxamide groups at the R<sub>2</sub> position are favored as observed by the comparison of <bold>3B</bold> to <bold>28B</bold> and <bold>6B</bold> to <bold>27B</bold> (see <xref rid="s0085" ref-type="sec">Table S2 in the Supporting information</xref>). Possibly, Class B inhibitors with small R<sub>2</sub> amides allow for a shift in the position of the inhibitor in the HKU4-CoV 3CL<sup>pro</sup> binding site to accommodate the bulky <italic>t</italic>-Bu amide at the R<sub>4</sub> position. Again, an R<sub>2</sub> amide is preferred to an amine for good inhibition of HKU4-CoV 3CL<sup>pro</sup> (IC<sub>50</sub> = 1.8 ± 0.5 μM for <bold>3B</bold> versus 22.0 ± 7.4 μM for <bold>21B</bold>). Replacement of the benzotriazole within this series with a benzimidazole has dissimilar effects; for example, comparing <bold>19B</bold> (<xref rid="t0010" ref-type="table">Table 1</xref>b) to <bold>28B</bold> (S2 and S3) where the benzimidazole of <bold>19B</bold> has been replaced with a benzotriazole, inhibition decreases from 68% to 34% at 100 μM, respectively. In contrast, comparison of <bold>23B</bold> to <bold>18B</bold> shows that substitution of benzimidazole for benzotriazole increases inhibition from 56% to 76% at 100 μM (<xref rid="t0005" ref-type="table">Table 1</xref>b). Interestingly, only Class B compounds having a <italic>para</italic>-substituted phenyl ring with an R<sub>2</sub> substituent were found to be good inhibitors of HKU4-CoV 3CL<sup>pro</sup>; compounds with other, non-phenyl rings including cyclopropyl, cyclohexyl, adamantane, and bicycloheptane were not found to be active inhibitors.</p></sec><sec id="s0020"><label>2.2</label><title>1A-RFL Sub-structural activity analysis via component synthesis</title><p id="p0060">In an attempt to delineate the structural relationships that contribute to the enhanced activity of our most active inhibitor, <bold>1A</bold>, we synthesized the sub-structural components of <bold>1A</bold> and determined their individual inhibitory activities against HKU4-CoV 3CL<sup>pro</sup> (<xref rid="f0030" ref-type="fig">Scheme 1</xref>). The straightforward synthesis of these sub-structural <bold>1A</bold> components, <bold>22A</bold>, <bold>23A</bold>, and <bold>24A</bold>, was accomplished from the commercially available starting materials, benzotriazole and <italic>p</italic>-phenylenediamine. The synthesis of <bold>22A</bold> was achieved in two steps. First, alkylation of benzotriazole by reaction with chloroacetic acid and sodium hydroxide yielded the benzotriazoleacetic acid <bold>22</bold> in 50% yield.<xref rid="b0125" ref-type="bibr"><sup>25</sup></xref> Subsequent coupling of <bold>22</bold> with the commercially available thiophenylmethanamine using EDC produced the desired <bold>1A</bold> component <bold>22A</bold> in 25% yield (<xref rid="f0030" ref-type="fig">Scheme 1</xref>, top). The synthesis of <bold>23A</bold> and <bold>24A</bold> was accomplished linearly by first coupling <italic>p</italic>-phenylenediamine with the commercially available thiophenecarboxylic acid using HATU, which resulted in the desired <bold>1A</bold> component <bold>23A</bold> in 58% yield. Reductive amination of <bold>23A</bold> and commercially available thiophenecarbaldehyde using sodium triacetoxyborohydride produced the desired <bold>1A</bold> sub-structural component <bold>24A</bold> in 81% yield. Finally, <bold>1A</bold> was resynthesized according to the literature procedure by coupling <bold>24A</bold> with <bold>22</bold> using EDC as a coupling reagent.<xref rid="b0120" ref-type="bibr"><sup>24</sup></xref><fig id="f0030"><label>Scheme 1</label><caption><p>Synthesis of sub-structural components of <bold>1A</bold>.</p></caption><graphic xlink:href="gr6"></graphic></fig></p><p id="p0065">The sub-structural components <bold>22A</bold>, <bold>23A</bold>, and <bold>24A</bold> were then individually tested for inhibition of HKU4-CoV 3CL<sup>pro</sup> at a concentration of 100 μM. The <bold>22A</bold> component, representing the R<sub>1</sub> and R<sub>3</sub> substituents of the Class A peptidomimetic backbone, showed 28% inhibition of HKU4-CoV 3CL<sup>pro</sup> at 100 μM and had an IC<sub>50</sub> of 68 μM, supporting our hypothesis that this backbone has some inhibitory capacity even in the absence of the R<sub>2</sub> component. The <bold>23A</bold> sub-structural component, representing the R<sub>2</sub> substituent of the Class A peptidomimetic backbone, was found to have no inhibitory activity against HKU4-CoV 3CL<sup>pro</sup> at 100 μM, supporting R<sub>1</sub> and R<sub>3</sub> as essential substituents. Additionally, the <bold>24A</bold> sub-structural component, representing the R<sub>1</sub> and R<sub>2</sub> substituents of the Class A peptidomimetic backbone, showed no inhibition of HKU4-CoV 3CL<sup>pro</sup> at 100 μM, indicating the crucial nature of the 1-methylbenzotriazole at the R<sub>3</sub> position of the Class A backbone and supporting our previous observation of the need for a precisely oriented hydrogen bond acceptor at this position within the Class A peptidomimetics (vide supra). This finding establishes <bold>22A</bold> as a minimum component necessary for inhibition of HKU4-CoV 3CL<sup>pro</sup> and suggests it may be used as a scaffold for future fragment based design of HKU4-CoV 3CL<sup>pro</sup> inhibitors. Interestingly, the work of Wong and coworkers showed that a series of benzotriazole esters, which act as potent, covalent inhibitors of SARS-3CL<sup>pro</sup>, are also able to inhibit SARS-3CL<sup>pro</sup> upon replacement of the ester oxygen with carbon, albeit weakly.<xref rid="b0130" ref-type="bibr"><sup>26</sup></xref> Taken together, these findings may indicate an inhibitory preference for benzotriazoles among coronaviral 3C-like proteases.</p></sec><sec id="s0025"><label>2.3</label><title>X-ray crystallographic analysis of HKU4-CoV 3CL<sup>pro</sup> in complex with <bold>1A</bold>, <bold>2A</bold>, and <bold>3B</bold></title><p id="p0070">In order to more fully elucidate the structural factors underlying the structure–activity relationships (SARs) observed in the kinetic data, we determined the X-ray crystal structures of HKU4-CoV 3CL<sup>pro</sup> in complex with three of the most potent inhibitors, <bold>1A</bold>, <bold>2A</bold>, <bold>3B</bold> and the favored backbone <bold>22A</bold>. These complexes were chosen to determine the potential structural explanations behind our observations that Class A and B inhibitor backbones, containing a 3-thiophene and 1-methylbenzotriazole, are favored for HKU4-CoV 3CL<sup>pro</sup> inhibition. We also sought to determine the structural reasons behind the preference for inhibition by Class A compounds over Class B compounds.</p><p id="p0075">Co-crystallization of <bold>1A</bold>, <bold>2A</bold>, <bold>3B</bold>, and <bold>22A</bold> with HKU4-CoV 3CL<sup>pro</sup> produced high-quality crystals suitable for X-ray data collection and structure determination. Complete X-ray data sets were collected on these four HKU4-CoV 3CL<sup>pro</sup>-inhibitor complexes to resolutions between 1.8 Å and 2.3 Å. A summary of the data collection and refinement statistics are provided in S4.</p><p id="p0080">The X-ray crystal structures confirm that both the Class A (<bold>1A</bold> and <bold>2A</bold>) and B (<bold>3B</bold>) peptidomimetics bind in the active site pocket of HKU4-Co 3CL<sup>pro</sup>, which is lined primarily with polar residues and is solvent exposed (<xref rid="f0010" ref-type="fig">Fig. 2</xref>). In each of the HKU4-CoV 3CL<sup>pro</sup>-inhibitor complexes, the carbonyl carbon of the central inhibitor backbone, that is, preceding the R<sub>3</sub> group, is located between 4.5 and 4.8 Å from the sulfur atom of the catalytic cysteine (Cys148, <xref rid="f0010" ref-type="fig">Fig. 2</xref>A, C and E). Both <bold>1A</bold> and <bold>2A</bold>, which have a 3-thiophene at the R<sub>1</sub> position and a 1-methylbenzotriazole at the R<sub>3</sub> position of the peptidomimetic backbone, position these moieties in identical chemical space (<xref rid="f0010" ref-type="fig">Fig. 2</xref>A and C). The Class B inhibitor, <bold>3B</bold>, which has a 3-thiophene at the R<sub>1</sub> position and a 1-methylbenzotriazole at the R<sub>3</sub> position, also positions the 3-thiophene and 1-methylbenzotriazole functionalities in the same chemical space utilized by the Class A inhibitors (<xref rid="f0010" ref-type="fig">Fig. 2</xref>E). The 3-thiophene in the R<sub>1</sub> position of all three inhibitors occupies the S<sub>2</sub>–S<sub>4</sub> sub-sites of the HKU4-CoV 3CL<sup>pro</sup> active site, the anilido and R<sub>2</sub>-functionality reside in the S<sub>2</sub>–S<sub>1</sub>′ sub-sites, and the R<sub>3</sub> benzotriazole occupies the S<sub>1</sub>-subsite, acting as the P<sub>1</sub> group of the substrate.<fig id="f0010"><label>Figure 2</label><caption><p>X-ray crystal structures of <bold>1A</bold>, <bold>2A</bold> and <bold>3B</bold> in complex with HKU4-CoV 3CL<sup>pro</sup>. Inhibitors are colored according to atom type and shown in ball and stick representation. Wall-eye stereo-view is shown in panels A, C, and E. Water molecules are shown as red spheres. Hydrogen bonds are shown as gray dashes with distances between heteroatoms labeled (Å). Interatomic distances (Å) are displayed using a gray arrow. Electron density omit maps (<italic>F<sub>o</sub></italic> − <italic>F<sub>c</sub></italic>) are shown in grey mesh and are contoured to +3.0<italic>σ</italic> around the inhibitor only. The binding orientation of each inhibitor is the same in the active site of each monomer of the dimer in the asymmetric unit of HKU4-CoV 3CL<sup>pro</sup>, therefore only one active site is shown for clarity. (A) HKU4-CoV 3CL<sup>pro</sup> (pale yellow) in complex with <bold>1A</bold> (sky blue), PDB <ext-link ext-link-type="uri" xlink:href="pdb:4YOI" id="ir0010">4YOI</ext-link>, (B) <bold>1A</bold> electron density omit map, (C) HKU4-CoV 3CL<sup>pro</sup> (wheat) in complex with <bold>2A</bold> (pale cyan), PDB <ext-link ext-link-type="uri" xlink:href="pdb:4YOJ" id="ir0015">4YOJ</ext-link>, (D) <bold>2A</bold> electron density omit map, (E) HKU4-CoV 3CL<sup>pro</sup> (light orange) in complex with <bold>3B</bold> (slate), PDB <ext-link ext-link-type="uri" xlink:href="pdb:4YOG" id="ir0020">4YOG</ext-link>, (F) <bold>3B</bold> electron density omit map contoured at +3.0<italic>σ</italic> (blue) and +2.0<italic>σ</italic> (grey).</p></caption><graphic xlink:href="gr2"></graphic></fig></p><p id="p0085">The X-ray structures reveal the structural determinants for the inhibitory preference for Class A and B compounds with backbones containing a 3-thiophene and 1-methylbenzotriazole. This backbone allows the inhibitor to anchor into the HKU4-CoV 3CL<sup>pro</sup> active site via the formation of three key hydrogen bonds. First, there is a direct hydrogen bond that exists between the 3-nitrogen atom of benzotriazole and the <italic>tele</italic>-nitrogen of His166 in each enzyme-inhibitor complex, securing the location and position of the benzotriazole in the active site. A second hydrogen bond between the carbonyl oxygen of the inhibitor backbone and the backbone nitrogen of Glu169 in each structure further anchors the inhibitor in the HKU4-CoV 3CL<sup>pro</sup> active site. Finally, the thiophene ring is positioned within the HKU4-CoV 3CL<sup>pro</sup> active site allowing the formation of a relatively uncommon hydrogen bond to the hydroxyl hydrogen of Tyr54.<xref rid="b0135" ref-type="bibr">27</xref>, <xref rid="b0140" ref-type="bibr">28</xref>, <xref rid="b0145" ref-type="bibr">29</xref>, <xref rid="b0150" ref-type="bibr">30</xref></p><p id="p0090">In each of the HKU4-CoV 3CL<sup>pro</sup>-inhibitor complexes, the R<sub>2</sub>-substituted aryl ring of both Class A and B inhibitors is positioned in the HKU4-CoV 3CL<sup>pro</sup> active site to take advantage of an edge-to-face pi-interaction with the catalytic histidine, His41 (<xref rid="f0010" ref-type="fig">Fig. 2</xref>A, C and E). This interaction may be important for good inhibition of HKU4-CoV 3CL<sup>pro</sup> for two reasons. First, comparing <bold>1A</bold> and <bold>2A</bold> to <bold>22A</bold>, where the R<sub>2</sub>-substituted aromatic ring of <bold>1A</bold> and <bold>2A</bold> is absent, a greater than 200-fold increase in IC<sub>50</sub> is observed for <bold>22A</bold>. Second, Class B compounds having non-aromatic substituents instead of an R<sub>2</sub>-substituted aryl ring were not found to be good inhibitors of HKU4-CoV 3CL<sup>pro</sup> (vide supra). These data indicate that for low micromolar to sub-micromolar inhibition of HKU4-CoV 3CL<sup>pro</sup>, an R<sub>2</sub>-substituted aryl ring may be required. Furthermore, there is a conserved active site water molecule present in the X-ray crystal structure of each HKU4-CoV 3CL<sup>pro</sup>-inhibitor complex that mediates a hydrogen-bond between the backbone carbonyl oxygen of His41 and the amide R<sub>2</sub> nitrogen of the inhibitor (<xref rid="f0010" ref-type="fig">Fig. 2</xref>A, C and E). This finding illuminates the observed preference for an amide substituent at the R<sub>2</sub> position in both Class A and B inhibitors.</p><p id="p0095">Our attempt to solve the X-ray crystal structure of <bold>22A</bold> in complex with HKU4-CoV 3CL<sup>pro</sup> did not result in the structure of the HKU4-CoV 3CL<sup>pro</sup>-inhibitor complex, but instead resulted in the X-ray structure of the unliganded, or free, HKU4-CoV 3CL<sup>pro</sup> enzyme, which was found to crystallize in a different space group than the HKU4-CoV 3CL<sup>pro</sup>-inhibitor complexes (<xref rid="f0015" ref-type="fig">Fig. 3</xref>A). The unbound, or free, HKU4-CoV 3CL<sup>pro</sup> enzyme was found to have noteworthy changes in the active site architecture in comparison to the X-ray crystal structures of the HKU4-CoV 3CL<sup>pro</sup>-inhibitor complexes. In the absence of an inhibitor, what appears to be a metal ion binds to the HKU4-CoV 3CL<sup>pro</sup> active site by coordinating to the catalytic cysteine (Cys148), which is rotated 180° from the inhibitor bound structures, resulting in a 3.2 Å positional change in the location of the sulfur atom with a distance of 2.2 Å between the sulfur of Cys148 and the metal atom. The metal is presumed to be a zinc cation, as it is present in water and likely to bind to a sulfur atom (also seen in PDB ID 2YNA), though it could also be iron. The <italic>tele</italic>-nitrogen of His41 is shifted 2.6 Å from its position in the HKU4-CoV 3CL<sup>pro</sup>-<bold>1A-RFL</bold> complex X-ray crystal structure, allowing for the coordination of the Zn<sup>2+</sup> atom, which is located 2.4 Å away (<xref rid="f0015" ref-type="fig">Fig. 3</xref>A). Additionally, the positions of the Met25, Cys44, Ala46, Tyr54, and Gln192 residues all noticeably shift upon superposition of the free and inhibitor-bound forms of HKU4-CoV 3CL<sup>pro</sup>.<fig id="f0015"><label>Figure 3</label><caption><p>(A) Superposition of unbound HKU4-CoV 3CL<sup>pro</sup> (gray, PDB <ext-link ext-link-type="uri" xlink:href="pdb:4YO9" id="ir0025">4YO9</ext-link>) and HKU4-CoV 3CL<sup>pro</sup> co-crystallized with inhibitor <bold>1A</bold> (where HKU4-CoV 3CL<sup>pro</sup> is shown in ribbon representation in light yellow and <bold>1A</bold> is shown in sky blue and colored by element, PDB <ext-link ext-link-type="uri" xlink:href="pdb:4YOI" id="ir0030">4YOI</ext-link>). The Zn atom in the unbound HKU4-CoV 3CL<sup>pro</sup> is represented as a gray sphere. (B) Superposition of HKU4-CoV 3CL<sup>pro</sup> co-crystallized with <bold>1A</bold> (where HKU4-CoV 3CL<sup>pro</sup> is shown in ribbon representation in light yellow and <bold>1A</bold> is shown in sky blue and colored by element, PDB <ext-link ext-link-type="uri" xlink:href="pdb:4YOI" id="ir0035">4YOI</ext-link>) and HKU4-CoV 3CL<sup>pro</sup> co-crystallized with <bold>2A</bold> (where HKU4-CoV 3CL<sup>pro</sup> is shown as cartoon in wheat and <bold>2A</bold> is shown in pale cyan and colored by element, PDB <ext-link ext-link-type="uri" xlink:href="pdb:4YOJ" id="ir0040">4YOJ</ext-link>). (C) Superposition of HKU4-CoV 3CL<sup>pro</sup> co-crystallized with <bold>1A</bold> (where HKU4-CoV 3CL<sup>pro</sup> is shown in ribbon representation in light yellow and <bold>1A</bold> is shown in sky blue and colored by element, PDB <ext-link ext-link-type="uri" xlink:href="pdb:4YOI" id="ir0045">4YOI</ext-link>) and HKU4-CoV 3CL<sup>pro</sup> co-crystallized with <bold>3B</bold> (where HKU4-CoV 3CL<sup>pro</sup> is shown as cartoon in light orange and <bold>3B</bold> is shown in slate and colored by element, PDB <ext-link ext-link-type="uri" xlink:href="pdb:4YOG" id="ir0050">4YOG</ext-link>). Wall-eye stereo-view is shown in each panel.</p></caption><graphic xlink:href="gr3"></graphic></fig></p><p id="p0100">Comparing the most potent Class B inhibitor having the 1-methylbenzotriazole and 3-thiophene backbone, <bold>3B</bold>, to the top HKU4-CoV 3CL<sup>pro</sup> inhibitor identified, <bold>1A</bold>, elucidates the observed preference for Class A inhibitors over Class B inhibitors (<xref rid="f0015" ref-type="fig">Fig. 3</xref>C). The (<italic>R</italic>)-enantiomer of the Class B compound, <bold>3B</bold>, was found in the HKU4-CoV 3CL<sup>pro</sup> active site, with the backbone of the inhibitor oriented similarly to the backbones of the Class A inhibitors <bold>1A</bold> and <bold>2A</bold>, utilizing the same hydrogen bonds; however, the (<italic>R</italic>)-R<sub>4</sub><italic>t</italic>-Bu amide substituent of <bold>3B</bold>, which is absent in the Class A inhibitors, marginally rotates the thiophene away from Tyr54, increasing the distance to the hydrogen-bond donor Tyr54 from 3.9 to 4.5 Å compared to <bold>1A</bold>, and moving the thiophene out of hydrogen-bonding distance to Tyr54 (distance measured to heteroatoms). The R<sub>4</sub><italic>t</italic>-Bu amide of <bold>3B</bold> extends out toward the solvent exposed side of the active site, inducing a structural rearrangement of HKU4-CoV 3CL<sup>pro</sup> where Gln192, which encloses <bold>1A</bold> and <bold>2A</bold> in the active site, is moved 2.7 Å to accommodate the steric bulk of the R<sub>4</sub> substituent of <bold>3B</bold>. The combination of these factors may be attributed for the observed 5-fold increase in IC<sub>50</sub> when comparing <bold>1A</bold> and <bold>2A</bold> to <bold>3B</bold> and likely account for the reduced inhibitory activity of Class B compounds relative to Class A compounds.</p><p id="p0105">The Class B peptidomimetic compounds were synthesized and tested for HKU4-CoV 3CL<sup>pro</sup> inhibition as racemates, which may lead to significant differences in IC<sub>50</sub> values. An example of this can be seen by the comparison of (<italic>R</italic>)-<bold>13B</bold> to racemic- and (<italic>S</italic>)-<bold>13B</bold> (<xref rid="f0020" ref-type="fig">Fig. 4</xref>). The enantiopure (<italic>R</italic>)-<bold>13B</bold> has an IC<sub>50</sub> of 9.3 ± 0.5 μM while the <bold>13B</bold> racemate has an IC<sub>50</sub> of 11.1 ± 0.6 μM and (<italic>S</italic>)-<bold>13B</bold> has a 50% reduction in inhibition relative to the racemate, with only 44% inhibition of HKU4-CL<sup>pro</sup> at 100 μM. Interestingly, (<italic>R</italic>)-<bold>3B</bold> was found in the active site of HKU4-CoV 3CL<sup>pro</sup> in the X-ray crystal structure (<xref rid="f0010" ref-type="fig">Fig. 2</xref>E and F), suggesting a preference for (<italic>R</italic>)-stereochemistry in the inhibitor for good inhibition of HKU4-CoV 3CL<sup>pro</sup>, despite the nature of the R<sub>1</sub> and R<sub>3</sub> heterocyclic groups.<fig id="f0020"><label>Figure 4</label><caption><p>Effect of <bold>13B</bold> stereocenter configuration on HKU4-CoV 3CL<sup>pro</sup> inhibition. Where% inhibition is determined at 100 μM inhibition concentration, n/t = not tested.</p></caption><graphic xlink:href="gr4"></graphic></fig></p><p id="p0110">The X-ray structures of HKU4-CoV 3CL<sup>pro</sup> in complex with inhibitors provide vital insights into the types of compounds that can be developed as therapeutics against lineage C <italic>Betacoronaviruses.</italic> A sequence alignment of HKU4-CoV, HKU5-CoV, and MERS-CoV 3CL<sup>pro</sup>, all of which are lineage C <italic>Betacoronaviruses</italic>, show that HKU4-CoV and HKU5-CoV are 81.0% and 82.7% identical to MERS-CoV 3CL<sup>pro</sup>, and HKU4-CoV is 83.7% identical to HKU5-CoV 3CL<sup>pro</sup> (<xref rid="f0025" ref-type="fig">Fig. 5</xref>).<xref rid="b0155" ref-type="bibr">31</xref>, <xref rid="b0160" ref-type="bibr">32</xref>, <xref rid="b0165" ref-type="bibr">33</xref> Moreover, the pertinent HKU4-CoV 3CL<sup>pro</sup> active site residues (Met25, His41, Cys44, Ala46, Tyr54, Cys148, His166, Glu169, and Gln192, <xref rid="f0015" ref-type="fig">Figure 3</xref>, <xref rid="f0020" ref-type="fig">Figure 4</xref>) identified in the X-ray crystal structures that line the active site and interact with the peptidomimetic inhibitors are all conserved in HKU5-CoV and MERS-CoV 3CL<sup>pro</sup>. These data indicate that the active site architectures among HKU4-CoV, HKU5-CoV, and MERS-CoV 3CL<sup>pro</sup> may be similar enough to design broad-spectrum antiviral therapeutics against lineage C <italic>Betacoronaviruses</italic> and have implications for the structure and inhibition of lineage C <italic>Betacoronaviruses</italic> yet to emerge. To test this hypothesis, we tested whether our lead HKU4-CoV 3CL<sup>pro</sup> inhibitor, compound <bold>1A</bold>, would also have inhibition of HKU5-CoV 3CL<sup>pro</sup>. We found that compound <bold>1A</bold> is a good inhibitor of HKU5-CoV 3CL<sup>pro</sup>, having 91% inhibition at 100 μM and a sub-micromolar IC<sub>50</sub> value of 0.54 ± 0.03 μM which is comparable to the IC<sub>50</sub> value of 0.33 ± 0.02 μM against HKU4-3CL<sup>pro</sup>. Based on these data, we predict compound <bold>1A</bold> will show inhibition of MERS-CoV 3CL<sup>pro</sup> as well.<fig id="f0025"><label>Figure 5</label><caption><p>Sequence alignment of HKU4-CoV, HKU5-CoV, and MERS-CoV 3CL<sup>pro</sup> where the top row indicates the secondary structure of HKU4-3CLpro at a particular residue position, conserved residues among all three 3CL<sup>pro</sup>’s are shaded in red, and residues that have similar steric or electronic properties are shown in red text with no shading. Non-conserved residues are displayed in black text. The pertinent active site residues that border and interact with the peptidomimetic inhibitors (Met25, His41, Cys44, Ala46, Tyr54, Cys148, His166, Glu169, and Gln192) are indicated by blue arrows.</p></caption><graphic xlink:href="gr5"></graphic></fig></p></sec></sec><sec id="s0030"><label>3</label><title>Conclusions</title><p id="p0115">In conclusion, 43 of the 230 peptidomimetics were found to inhibit HKU4-CoV 3CL<sup>pro</sup>, 19 of which belonged to the Class A peptidomimetic series and 24 of which belonged to the Class B peptidomimetic series. Overall, the Class A peptidomimetics were found to be better inhibitors relative to the Class B compounds, and two of the Class A compounds were determined to have sub-micromolar inhibitory potency against HKU4-CoV 3CL<sup>pro</sup>, <bold>1A</bold> and <bold>2A</bold>. Analysis of the inhibition data from the 230 peptidomimetics resulted in the identification of a favored inhibitor backbone consisting of 3-thiophene and 1-methylbenzotriazole functionalities. To evaluate the relative contribution of the favored inhibitor backbone to the total HKU4-CoV 3CL<sup>pro</sup> inhibition observed for the molecule, we synthesized the sub-structural components of the lead inhibitor, <bold>1A</bold>, and tested them for inhibition of HKU4-CoV 3CL<sup>pro</sup>. The simple compound, <bold>22A</bold>, which represents the R<sub>1</sub> and R<sub>3</sub> inhibitor functionalities and consists of the 3-thiophene and 1-methylbenzotriazole of the favored backbone, was found to inhibit HKU4-CoV 3CL<sup>pro</sup> even in the absence of the anilido and R<sub>2</sub> components of the inhibitor. We then determined the X-ray crystal structures of the three most potent inhibitors containing this favored backbone, <bold>1A</bold>, <bold>2A</bold>, <bold>3B,</bold> in complex with HKU4-CoV 3CL<sup>pro</sup>. These X-ray crystal structures prove that the three Class A and B inhibitors bind in the HKU4-CoV 3CL<sup>pro</sup> active site, utilizing the same set of three hydrogen-bonding interactions between the favored backbone and the HKU4-CoV 3CL<sup>pro</sup> active site residues, serving to anchor compounds with this backbone into the active site of the enzyme. Our attempt to solve the X-ray structure of the privileged backbone compound, <bold>22A</bold>, in complex with HKU4-CoV 3CL<sup>pro</sup> resulted in the structure of unbound HKU4-CoV 3CL<sup>pro</sup>, which is presumably as a consequence of weak inhibition by <bold>22A</bold> (28% at 100 μM). Superposition of the unbound and inhibitor-bound forms of HKU4-CoV 3CL<sup>pro</sup> revealed several subtle, but important changes in the active site architecture upon inhibitor binding. Furthermore, sequence alignment of HKU4-CoV, HKU5-CoV, and MERS-CoV 3CL<sup>pro</sup> show that the residues involved in inhibitor binding are conserved, indicating that identification of broad spectrum 3CL<sup>pro</sup> inhibitors of lineage C <italic>Betacoronaviruses</italic> is possible. In support of this, we found our most active HKU4-CoV 3CL<sup>pro</sup> inhibitor to have inhibition of HKU5-CoV 3CL<sup>pro</sup> in the sub-micromolar range (IC<sub>50</sub> = 0.54 ± 0.03 μM). These findings, and the structural details underlying the potent inhibition of HKU4-CoV 3CL<sup>pro</sup> by compounds containing 3-thiophene and 1-methylbenzotriazole backbones, can be used in the future to design compounds with the ability to more fully exploit the HKU4-CoV 3CL<sup>pro</sup> active site, leading ultimately to the development of more highly potent and selective inhibitors against human pathogens such as SARS and MERS.</p></sec><sec id="s0035"><label>4</label><title>Experimental</title><sec id="s0040"><label>4.1</label><title>Expression and purification of HKU4-CoV 3CL<sup>pro</sup></title><p id="p0120">The gene encoding the 3CL<sup>pro</sup> of HKU4-CoV (residues 3292-3597 in the <italic>Tylonycteris</italic> bat-CoV polyprotein)<xref rid="b0045" ref-type="bibr"><sup>9</sup></xref> was codon optimized for expression in <italic>Escherichia coli</italic> and cloned into pET-11a expression vector with an N-terminal (His)<sub>6</sub>-tag followed by nsp4-/5 auto-cleavage site by BioBasic Inc. This construct results in the expression of HKU4-CoV 3CL<sup>pro</sup> without an N-terminal or C-terminal extension. E<italic>. coli</italic> BL21(DE3) cells, transformed with pET11a-HKU4 3CL<sup>pro</sup> plasmid were grown in Super LB media (3 g potassium phosphate monobasic, 6 g sodium phosphate dibasic, 20 g tryptone, 5 g yeast extracts, 5 g sodium in 1 L water, pH 7.2 adjusted with 1 M NaOH) in the presence of 1 mL 100 mg/mL carbenicillin, 25 mL 8% lactose, 10 mL 60% glycerol, and 5 mL of 10% glucose per 1 L of expression culture for 24 h at 25 °C. The cells were harvested by centrifugation (8400<italic>g</italic> for 20 min) to yield 15.5 g/L of cells. The cell pellet was then re-suspended in 5 mL of Buffer A/1 g cell pellet (50 mM Tris pH 7.5, 0.2 M ammonium sulfate, 0.05 mM EDTA, 5 mM BME) containing 1 mg/mL lysozyme. After the cells were homogenized, they were lysed via sonication for 10 min with 10 s pulses at 50% amplitude using a Branson Digital Sonifier. The cell lysate was clarified by pelleting the cell debris via centrifugation (28,960<italic>g</italic>, 4 °C, 20 min) and loaded onto a 30 mL Phenyl Sepharose 6 Fast Flow HiSub column equilibrated with Buffer A. Protein was eluted with a gradient to 100% Buffer B (20 mM Tris pH 7.5, 0.05 mM EDTA, 5 mM BME) over five column volumes (150 mL) collecting 5 mL fractions. Fractions containing HKU4 3CL<sup>pro</sup> were pooled and loaded onto a 60 mL DEAE Sepharose Fast Flow column equilibrated with Buffer B. Protein was eluted with a gradient to 50% Buffer C (50 mM Tris pH 7.5, 1 M sodium chloride, 0.05 mM EDTA, 5 mM BME, 10% glycerol) over five column volumes (300 mL) collecting 5 mL fractions. Fractions containing pure HKU4-CoV 3CL<sup>pro</sup> were pooled, dialyzed into storage buffer (25 mM HEPES, pH 7.5, 2.5 mM DTT, 10% glycerol), and concentrated. The protein was then aliquoted into 1.5 mL push-cap Eppendorf tubes, flash frozen in liquid nitrogen, and stored at -80 °C in a freezer until further use.</p></sec><sec id="s0045"><label>4.2</label><title>IC<sub>50</sub> Determination of inhibitors against HKU4-CoV 3CL<sup>pro</sup> at 25 °C and 37 °C</title><p id="p0125">Each of the 230 dipeptide-like inhibitors were first screened for inhibition of HKU4 3CL<sup>pro</sup> at a concentration of 100 μM in duplicate assays containing the following assay buffer (50 mM HEPES, 0.1 mg/mL BSA, 0.01% TritonX-100, 1 mM DTT). The assays were carried out in Costar 3694 EIA/RIA 96-Well Half Area, Flat Bottom, Black Polystyrene plates from Corning Incorporated. 1 μL of 100× inhibitor stock in DMSO was added to 79 μL of enzyme in assay buffer and the enzyme-inhibitor mixture was incubated for 10 min. The reaction was initiated by the addition of 20 μL of 10 μM UIVT3 substrate, a custom synthesized Förster resonance energy transfer substrate peptide with the following sequence: HilyteFluor<sup>TM</sup>488-ESARLQSGLRKAK-QXL520<sup>TM</sup>-NH<sub>2</sub>, producing final concentrations of 100 nM and 100 μM for the 3CL<sup>pro</sup> enzyme and UIVT3 substrate, respectively. The fluorescence intensity of the reaction was then measured over time as relative fluorescence units (RFU<sub>t</sub>) for a period of 10 min, using an excitation wavelength of 485 and bandwidth of 20 nM and monitoring emission at 528 and bandwidth of 20 nM using a BioTek Synergy H1 multimode microplate reader.</p><p id="p0130">The inhibition of HKU4-CoV 3CL<sup>pro</sup> by inhibitor compounds was monitored by following the change in RFUs over time, using the initial slope of the progress curve to determine the initial rate (<italic>V<sub>i</sub></italic>). The percent inhibition of the 3CL<sup>pro</sup> enzymes was determined using the following equation:<disp-formula id="e0005"><mml:math id="M1" altimg="si1.gif" overflow="scroll"><mml:mo>%</mml:mo><mml:mspace width="0.35em"></mml:mspace><mml:mtext>Inhibition</mml:mtext><mml:mo>=</mml:mo><mml:mrow><mml:mfenced open="[" close="]"><mml:mrow><mml:mn>1</mml:mn><mml:mo>-</mml:mo><mml:mfrac><mml:mrow><mml:mtext>Inhibited</mml:mtext><mml:mspace width="0.35em"></mml:mspace><mml:mn>3</mml:mn><mml:mtext>CLpro</mml:mtext><mml:mspace width="0.35em"></mml:mspace><mml:mtext>RFU</mml:mtext><mml:mo>/</mml:mo><mml:mtext>s</mml:mtext><mml:mo>-</mml:mo><mml:mtext>Background RFU</mml:mtext><mml:mo>/</mml:mo><mml:mtext>s</mml:mtext></mml:mrow><mml:mrow><mml:mtext>Uninhibited</mml:mtext><mml:mspace width="0.35em"></mml:mspace><mml:mn>3</mml:mn><mml:mtext>CLpro</mml:mtext><mml:mspace width="0.35em"></mml:mspace><mml:mtext>RFU</mml:mtext><mml:mo>/</mml:mo><mml:mtext>s</mml:mtext><mml:mo>-</mml:mo><mml:mtext>Background RFU</mml:mtext><mml:mo>/</mml:mo><mml:mtext>s</mml:mtext></mml:mrow></mml:mfrac></mml:mrow></mml:mfenced></mml:mrow><mml:mo>∗</mml:mo><mml:mn>100</mml:mn></mml:math></disp-formula></p><p id="p0135">Full IC<sub>50</sub> data were acquired for the compounds that showed greater than 50% inhibition of HKU4-CoV 3CL<sup>pro</sup> at 100 μM of inhibitor compound. The IC<sub>50</sub> values were determined at ambient temperature from 100 μL assays performed in triplicate in the following buffer: 50 mM HEPES, 0.1 mg/mL BSA, 0.01% TritonX-100, 1 mM DTT. Kinetic assays were carried out in Costar 3694 EIA/RIA 96-Well Half Area, Flat Bottom, Black Polystyrene plates from Corning Incorporated. Each inhibitor was tested at concentrations of 0.313, 0.652, 1.25, 2.5, 5.0, 10.0, 20.0, 40.0, 60.0, 80.0, 100.0, and 120.0 μM; 1 μL of 100× inhibitor stock in DMSO was added to 79 μL of enzyme in assay buffer and the enzyme-inhibitor mixture was incubated for 10 min. The reaction was initiated by the addition of 20 μL of 10 μM UIVT3 substrate, producing final concentrations of 100 nM and 2 μM for the 3CL<sup>pro</sup> enzyme and UIVT3 substrate, respectively. The fluorescence intensity of the reaction was then measured over time as RFU<sub>t</sub> for a period of 20 min, using an excitation wavelength of 485 and bandwidth of 20 nM and monitoring emission at 528 and bandwidth of 20 nM using a BioTek Synergy H1 multimode microplate reader.</p><p id="p0140">The percent inhibition of the 3CL<sup>pro</sup> enzymes was then plotted as a function of inhibitor concentration. The SigmaPlot Enzyme Kinetics Wizard was used to fit the triplicate percent inhibition data and associated standard error to a non-linear Michaelis-Menten type regression model and determine the IC<sub>50</sub> for each enzyme using the following equation:<disp-formula id="e0010"><mml:math id="M2" altimg="si2.gif" overflow="scroll"><mml:mo>%</mml:mo><mml:mspace width="0.35em"></mml:mspace><mml:mtext>Inhibition</mml:mtext><mml:mo>=</mml:mo><mml:mfrac><mml:mrow><mml:mo>%</mml:mo><mml:msub><mml:mrow><mml:mi>I</mml:mi></mml:mrow><mml:mrow><mml:mtext>max</mml:mtext></mml:mrow></mml:msub><mml:mo>∗</mml:mo><mml:mo stretchy="false">[</mml:mo><mml:mtext>Inhibitor</mml:mtext><mml:mo stretchy="false">]</mml:mo></mml:mrow><mml:mrow><mml:msub><mml:mrow><mml:mtext>IC</mml:mtext></mml:mrow><mml:mrow><mml:mn>50</mml:mn></mml:mrow></mml:msub><mml:mo>+</mml:mo><mml:mo stretchy="false">[</mml:mo><mml:mtext>Inhibitor</mml:mtext><mml:mo stretchy="false">]</mml:mo></mml:mrow></mml:mfrac></mml:math></disp-formula>where %<italic>I</italic><sub>max</sub> is the percent maximum inhibition of 3CL<sup>pro</sup> and the error in IC<sub>50</sub> values was determined as the error in the fitted parameter.</p></sec><sec id="s0050"><label>4.3</label><title>Crystallization and X-ray structure determination of HKU4 3C-like protease in complex with inhibitors</title><p id="p0145">The HKU4 3CL<sup>pro</sup>-inhibitor complexes were co-crystallized from four different crystallization solutions. Briefly, the hanging-drop, vapor-diffusion method was used for crystallization by setting up drops and adding 1 μL of purified HKU4-CoV 3CL<sup>pro</sup> (2.5 mg/mL, 75 μM), that had been incubated for three hours with a 3 molar excess of the appropriate inhibitor, and 1 μL of reservoir solution. For <bold>1A</bold>: 15% PEG-3350, 2% tacsimate, 5% isopropanol, 0.1 M imidazole pH 6; for <bold>3B</bold>: 20% PEG-3350, 0.2 M ammonium acetate, 0.1 M Bis-Tris pH 5.5; for <bold>2A</bold>: 18% PEG-3350, 5% tacsimate, 0.2 M ammonium sulfate, 0.1 M Bis-Tris pH5.5; for <bold>22A</bold>: 10% PEG-3350, 2% tacsimate, 5% isopropanol, 0.1 M imidazole pH 6.5. Protein crystals appeared between 14 h and 7 days after setting up crystallization plates. Crystals were harvested with a nylon loop, which was then swiped through the same mother-liquor solution supplemented with 15% MPD. The crystals were cooled by plunging into liquid nitrogen and stored in shipping dewars containing liquid nitrogen until X-ray data collection at an available synchrotron could be performed.</p><p id="p0150">All diffraction data were collected at 100 K at the Life Sciences Collaborative Access Team (LS-CAT) at the Advanced Photon Source (APS) at Argonne National Laboratories. Crystals were transferred from shipping dewars into automated dewars and then and mounted robotically on a goniostat while under a stream of N<sub>2</sub>. X-ray data sets of HKU4 3CL<sup>pro</sup>-inhibitor complexes were collected on a Rayonix 225 HE detector at a wavelength of 0.98 Å. X-ray data were processed and scaled using the program HLK2000, crystals of HKU4-CoV 3CL<sup>pro</sup> complexes with the inhibitors <bold>1A</bold>, <bold>2A</bold>, and <bold>3B</bold> belonged to the space group P2<sub>1</sub>2<sub>1</sub>2<sub>1,</sub> and HKU4-CoV 3CL<sup>pro</sup> crystallized as a dimer in the asymmetric unit. Co-crystallization of HKU4-CoV 3CL<sup>pro</sup> with <bold>22A</bold> did not result in an HKU4-CoV 3CL<sup>pro</sup>:inhibitor co-complex, but instead yielded the apo form of HKU4-CoV 3CL<sup>pro</sup>, which crystallized in a different space group, P3<sub>1</sub>21 with one dimer per asymmetric unit.</p><p id="p0155">The initial phases for HKU4-CoV 3CL<sup>pro</sup> in complex with <bold>1A</bold>, <bold>2A</bold>, and <bold>3B</bold> were determined by molecular replacement using Phaser-MR (simple interface) in the Phenix suite and the protein database PDB file 2YNA.<xref rid="b0170" ref-type="bibr"><sup>34</sup></xref> The inhibitors were built and optimized from their SMILES strings using eLBOW and fit into the density using LigandFit in the Phenix suite and the program COOT. Structures were refined using Phenix. Water molecules were added manually to the 2<italic>F<sub>o</sub></italic>−<italic>F<sub>c</sub></italic> density peaks that were greater than 3.0<italic>σ</italic> and iterative rounds of refinement were carried out until <italic>R<sub>work</sub></italic> and <italic>R<sub>free</sub></italic> reached their lowest values. The electron density maps presented in the figures were calculated using Phenix and COOT and the figures generated using the program PyMol.</p></sec><sec id="s0055"><label>4.4</label><title>General chemistry methods</title><p id="p0160">All reagents and chemicals were purchased from SigmaAldrich or Acros Organics and used without further purification. Anhydrous solvents were purchased or purified by passage through a solvent column composed of activated alumina and a supported copper redox catalyst. Analytical thin-layer chromatography was performed using Sorbent Technologies Glass-Backed Silica Gel HL TLC plates w/UV254. Flash chromatography was performed with Sorbent Technologies 200–400 mesh silica gel. Nuclear magnetic resonance (NMR) data was acquired using either a Varian Inova300, Bruker ARX400, or Bruker AV-III-800 spectrometers at 300, 400, or 800 MHz for <sup>1</sup>H or 75, 100, or 200 MHz for <sup>13</sup>C. All compounds were purified by flash chromatography to >90% purity by <sup>1</sup>H NMR.</p><sec id="s0060"><label>4.4.1</label><title>2-(1<italic>H</italic>-Benzo[<italic>d</italic>][1,2,3]triazol-1-yl)-<italic>N</italic>-(thiophen-3-ylmethyl)acetamide (<bold>22A</bold>)</title><p id="p0165">To 2-(1<italic>H</italic>-benzo[<italic>d</italic>][1,2,3]triazol-1-yl)acetic acid (1.5 equiv) in anhydrous dichloromethane (0.2 M) at 0 °C under nitrogen atmosphere was added EDC (3.0 equiv) and HOBT (3.0 equiv). The mixture was allowed to stir for five minutes before the addition of DIEA (13.0 equiv). The mixture was allowed to stir for an additional 20 min before the addition of thiophen-3-ylmethanamine (1.0 equiv). The reaction mixture was allowed to warm to ambient temperature and stirred under nitrogen atmosphere for 16 h. The reaction was quenched by addition of saturated potassium bicarbonate and the aqueous layer was extracted with ethyl acetate (3×). The combined organic layers were washed with water (1×) and brine (1×), dried over sodium sulfate, and concentrated. The crude residue was recrystallized from hot ethanol to provide the product as a beautiful white, crystalline solid in 30% yield. <sup>1</sup>H NMR (800 MHz, CD<sub>3</sub>OD) <italic>δ</italic> (ppm): 8.03 (1H, d, <italic>J</italic> = 8.37), 7.72 (1H, d, <italic>J</italic> = 8.37), 7.59 (1H, dd, <italic>J</italic> = 8.37, 0.96), 7.48 (1H, dd, <italic>J</italic> = 8.37, 0.96), 7.40 (1H, dd, <italic>J</italic> = 4.94, 2.97), 7.29 (1H, m), 7.08 (1H, dd, <italic>J</italic> = 4.93, 1.30), 5.51 (2H, s), 4.46 (2H, s). <sup>13</sup>C NMR (200 MHz, CD<sub>3</sub>OD) <italic>δ</italic> (ppm): 166.47, 145.30, 138.67, 133.83, 127.63, 126.92, 125.81, 124.28, 121.90, 118.60, 110.11, 49.87, 38.19. ESI-MS(+): 273 [M+1], 295 [M+23].</p></sec><sec id="s0065"><label>4.4.2</label><title><italic>N</italic>-(4-Aminophenyl)thiophene-2-carboxamide (<bold>23A</bold>)</title><p id="p0170">Thiophene-2-carboxylic acid (1.0 equiv) and HATU (1.4 equiv) were added to anhydrous dichloromethane (0.2 M) at room temperature followed by drop-wise addition of DIEA (3.0 equiv) under nitrogen atmosphere. The mixture was allowed to stir at ambient temperature for 5 min before benzene-1,4-diamine was added in one portion. The reaction mixture was allowed to stir for 14 h before it was quenched with saturated potassium bicarbonate. The aqueous layer was extracted with ethyl acetate (3×) and the combined organic extracts were washed with water (1×) and brine (1×), dried over sodium sulfate, and concentrated. The crude yellow residue was purified by flash chromatography using a gradient of 20% to 70% ethyl acetate in hexanes to give the final product in 50% yield. This reaction was performed from mg to g scale with no detrimental effect on yield. <sup>1</sup>H NMR (800 MHz, CD<sub>3</sub>OD) <italic>δ</italic> (ppm): 7.84 (1H, d, <italic>J</italic> = 3.74), 7.67 (1H, dd, <italic>J</italic> = 4.97, 1.08), 7.37 (2H, d, <italic>J</italic> = 8.56), 7.15 (1H, dd, <italic>J</italic> = 4.97, 3.74). <sup>13</sup>C NMR (200 MHz, CD<sub>3</sub>OD) <italic>δ</italic> (ppm): 161.26, 144.66, 139.63, 130.56, 128.71, 128.31, 127.49, 122.85. ESI-MS(+): 219 [M+1], 241 [M+23].</p></sec><sec id="s0070"><label>4.4.3</label><title><italic>N</italic>-(4-((Thiophen-3-ylmethyl)amino)phenyl)thiophene-2-carboxamide (<bold>24A</bold>)</title><p id="p0175"><bold>23A</bold> (1.0 equiv) and thiophene-3-carbaldehyde (1.0 equiv) were dissolved in anhydrous 1,2-DCE (0.2 M) at ambient temperature under nitrogen atmosphere. Sodium triacetoxyborohydride (1.6 equiv) and acetic acid (1.0 equiv) were then added in one portion. The reaction mixture was allowed to stir for 30 min before the reaction was quenched with 1 N sodium hydroxide. The aqueous layer was extracted with ethyl acetate (3×) and the combined organic extracts were washed with water (1×) and brine (1×), dried over sodium sulfate, and concentrated. The crude yellow residue was purified by flash chromatography using a gradient of 20–70% ethyl acetate in hexanes to give the final product in 50–80% yield. <sup>1</sup>H NMR (800 MHz, CD<sub>3</sub>OD) <italic>δ</italic> (ppm): 7.85 (1H, m), 7.69 (1H, m), 7.36 (3H, m), 7.26 (1H, m), 7.17 (1H, d, <italic>J</italic> = 5.15), 7.12 (1H, d, <italic>J</italic> = 5.15), 6.70 (2H, m), 4.34–4.35 (2H, rotomeric peaks). <sup>13</sup>C NMR (200 MHz, CD<sub>3</sub>OD) <italic>δ</italic> (ppm): 172.76, 146.24, 141.08, 130.47, 128.20, 127.65, 127.43, 126.82, 125.27, 122.87, 120.85, 112.81, 43.08). ESI-MS(+): 315 [M+1], 337 [M+23].</p></sec></sec></sec><sec id="s0075"><title>Author contributions</title><p id="p0180">Sarah E. St. John (SSJ) expressed, purified, and characterized HKU4-3CL<sup>pro</sup>. SSJ designed and performed all of the experiments and synthesis detailed herein and was responsible for crystallizing unbound and bound HKU4-3CL<sup>pro</sup>:inhibitor complexes and solving their X-ray structures. SSJ wrote the research article and made all figures/schemes/tables. Sakshi Tomar (ST) designed the HKU4- and HKU5-3CL<sup>pro</sup> expression plasmids, and over expressed and purified the HKU5-3CL<sup>pro</sup> enzyme and tested for inhibition by <bold>1A</bold>. The original compound library (S1 and S2) was synthesized in the laboratory of Shaun R. Stauffer (SRS), who also edited this article. Andrew D. 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D</source><volume>66</volume><year>2010</year><fpage>213</fpage><pub-id pub-id-type="pmid">20124702</pub-id></element-citation></ref></ref-list><sec id="s0085" sec-type="supplementary-material"><title>Supplementary data</title><p id="p0190"><supplementary-material content-type="local-data" id="m0005"><caption><title>Supplementary data</title><p>Supporting information.</p></caption><media xlink:href="mmc1.pdf"></media></supplementary-material></p></sec><ack id="ak005"><title>Acknowledgements</title><p>This work was supported in part by Grants (AI085089 and AI26603) to A.D.M. from the <funding-source id="gp005">National Institutes of Health</funding-source> via the <funding-source id="gp010">National Institute of Allergy and Infectious Diseases</funding-source>. A.D.M. also wishes to also acknowledge partial support from the <funding-source id="gp015">Walther Cancer Foundation</funding-source>. Sakshi Tomar is supported by a Grant from the <funding-source id="gp020">Purdue University Research Foundation</funding-source>. Crystallization and DNA sequencing were partially supported by the <funding-source id="gp025">Purdue Center</funding-source> for Cancer Research Macromolecular Crystallography and DNA Sequencing Shared Resources which are partially supported by an <funding-source id="gp030">NIH</funding-source> Grant (P30 CA023168). The authors would also like to acknowledge the scientists at the Vanderbilt Specialized Chemistry Center for synthesis of the initial compound library used in this work, which was supported in part by the <funding-source id="gp035">MLPCN</funding-source> (1U54 MH084659 and MH084512). Finally, the authors would like to acknowledge the LS-CAT beamline staff for their help in acquiring X-ray data. Use of the Advanced Photon Source, an Office of Science User Facility operated for the U.S. Department of Energy (DOE) Office of Science by Argonne National Laboratory, was supported by the <funding-source id="gp040">U.S. DOE</funding-source> under Contract No. DE-AC02-06CH11357. Use of the LS-CAT Sector 21 was supported by the <funding-source id="gp045">Michigan Economic Development Corporation</funding-source> and the <funding-source id="gp050">Michigan Technology Tri-Corridor</funding-source> (Grant 085P1000817).</p></ack><fn-group><fn id="s0080" fn-type="supplementary-material"><p id="p0185">Supplementary data associated with this article can be found, in the online version, at <ext-link ext-link-type="doi" xlink:href="10.1016/j.bmc.2015.06.039" id="ir0005">http://dx.doi.org/10.1016/j.bmc.2015.06.039</ext-link>.</p></fn></fn-group></back></pmc></record>Pour manipuler ce document sous Unix (Dilib)
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