Novel Crizotinib–GnRH Conjugates Revealed the Significance of Lysosomal Trapping in GnRH-Based Drug Delivery Systems
Identifieur interne : 000B93 ( Ncbi/Merge ); précédent : 000B92; suivant : 000B94Novel Crizotinib–GnRH Conjugates Revealed the Significance of Lysosomal Trapping in GnRH-Based Drug Delivery Systems
Auteurs : J Zsef Murányi ; Attila Varga ; Pál Gyulavári ; Kinga Pénzes ; Csilla E. Németh ; Mikl S Csala ; Lilla Peth [Hongrie] ; Antal Csámpai ; Gábor Halmos ; István Peták ; István Vályi-NagySource :
- International Journal of Molecular Sciences [ 1422-0067 ] ; 2019.
Abstract
Several promising anti-cancer drug–GnRH (gonadotropin-releasing hormone) conjugates have been developed in the last two decades, although none of them have been approved for clinical use yet. Crizotinib is an effective multi-target kinase inhibitor, approved against anaplastic lymphoma kinase (ALK)- or ROS proto-oncogene 1 (ROS-1)-positive non-small cell lung carcinoma (NSCLC); however, its application is accompanied by serious side effects. In order to deliver crizotinib selectively into the tumor cells, we synthesized novel crizotinib analogues and conjugated them to a [
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DOI: 10.3390/ijms20225590
PubMed: 31717403
PubMed Central: 6888004
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<record><TEI><teiHeader><fileDesc><titleStmt><title xml:lang="en">Novel Crizotinib–GnRH Conjugates Revealed the Significance of Lysosomal Trapping in GnRH-Based Drug Delivery Systems</title><author><name sortKey="Muranyi, J Zsef" sort="Muranyi, J Zsef" uniqKey="Muranyi J" first="J Zsef" last="Murányi">J Zsef Murányi</name><affiliation><nlm:aff id="af1-ijms-20-05590">MTA-SE Pathobiochemistry Research Group, Tűzoltó St. 37-47, H1094 Budapest, Hungary;<email>varga.attila@med.semmelweis-univ.hu</email> (A.V.);<email>gyulavari.pal@med.semmelweis-univ.hu</email> (P.G.);<email>penzes.kinga@med.semmelweis-univ.hu</email> (K.P.)</nlm:aff></affiliation><affiliation><nlm:aff id="af2-ijms-20-05590">Department of Medical Chemistry, Molecular Biology and Pathobiochemistry, Semmelweis University, H1094 Budapest, Hungary;<email>nemeth.csilla@med.semmelweis-univ.hu</email> (C.E.N.);<email>csala.miklos@med.semmelweis-univ.hu</email> (M.C.)</nlm:aff></affiliation></author><author><name sortKey="Varga, Attila" sort="Varga, Attila" uniqKey="Varga A" first="Attila" last="Varga">Attila Varga</name><affiliation><nlm:aff id="af1-ijms-20-05590">MTA-SE Pathobiochemistry Research Group, Tűzoltó St. 37-47, H1094 Budapest, Hungary;<email>varga.attila@med.semmelweis-univ.hu</email> (A.V.);<email>gyulavari.pal@med.semmelweis-univ.hu</email> (P.G.);<email>penzes.kinga@med.semmelweis-univ.hu</email> (K.P.)</nlm:aff></affiliation></author><author><name sortKey="Gyulavari, Pal" sort="Gyulavari, Pal" uniqKey="Gyulavari P" first="Pál" last="Gyulavári">Pál Gyulavári</name><affiliation><nlm:aff id="af1-ijms-20-05590">MTA-SE Pathobiochemistry Research Group, Tűzoltó St. 37-47, H1094 Budapest, Hungary;<email>varga.attila@med.semmelweis-univ.hu</email> (A.V.);<email>gyulavari.pal@med.semmelweis-univ.hu</email> (P.G.);<email>penzes.kinga@med.semmelweis-univ.hu</email> (K.P.)</nlm:aff></affiliation></author><author><name sortKey="Penzes, Kinga" sort="Penzes, Kinga" uniqKey="Penzes K" first="Kinga" last="Pénzes">Kinga Pénzes</name><affiliation><nlm:aff id="af1-ijms-20-05590">MTA-SE Pathobiochemistry Research Group, Tűzoltó St. 37-47, H1094 Budapest, Hungary;<email>varga.attila@med.semmelweis-univ.hu</email> (A.V.);<email>gyulavari.pal@med.semmelweis-univ.hu</email> (P.G.);<email>penzes.kinga@med.semmelweis-univ.hu</email> (K.P.)</nlm:aff></affiliation></author><author><name sortKey="Nemeth, Csilla E" sort="Nemeth, Csilla E" uniqKey="Nemeth C" first="Csilla E." last="Németh">Csilla E. Németh</name><affiliation><nlm:aff id="af2-ijms-20-05590">Department of Medical Chemistry, Molecular Biology and Pathobiochemistry, Semmelweis University, H1094 Budapest, Hungary;<email>nemeth.csilla@med.semmelweis-univ.hu</email> (C.E.N.);<email>csala.miklos@med.semmelweis-univ.hu</email> (M.C.)</nlm:aff></affiliation></author><author><name sortKey="Csala, Mikl S" sort="Csala, Mikl S" uniqKey="Csala M" first="Mikl S" last="Csala">Mikl S Csala</name><affiliation><nlm:aff id="af2-ijms-20-05590">Department of Medical Chemistry, Molecular Biology and Pathobiochemistry, Semmelweis University, H1094 Budapest, Hungary;<email>nemeth.csilla@med.semmelweis-univ.hu</email> (C.E.N.);<email>csala.miklos@med.semmelweis-univ.hu</email> (M.C.)</nlm:aff></affiliation></author><author><name sortKey="Peth, Lilla" sort="Peth, Lilla" uniqKey="Peth L" first="Lilla" last="Peth">Lilla Peth</name><affiliation wicri:level="1"><nlm:aff id="af3-ijms-20-05590">MTA-ELTE Research Group of Peptide Chemistry, Eötvös Loránd University, H1117 Budapest, Hungary</nlm:aff><country xml:lang="fr">Hongrie</country><wicri:regionArea>MTA-ELTE Research Group of Peptide Chemistry, Eötvös Loránd University, H1117 Budapest</wicri:regionArea><wicri:noRegion>H1117 Budapest</wicri:noRegion></affiliation></author><author><name sortKey="Csampai, Antal" sort="Csampai, Antal" uniqKey="Csampai A" first="Antal" last="Csámpai">Antal Csámpai</name><affiliation><nlm:aff id="af4-ijms-20-05590">Institute of Chemistry, Eötvös Loránd University, H1117 Budapest, Hungary;<email>csampai@chem.elte.hu</email></nlm:aff></affiliation></author><author><name sortKey="Halmos, Gabor" sort="Halmos, Gabor" uniqKey="Halmos G" first="Gábor" last="Halmos">Gábor Halmos</name><affiliation><nlm:aff id="af5-ijms-20-05590">Department of Biopharmacy, Faculty of Pharmacy, University of Debrecen, H4032 Debrecen, Hungary;<email>halmos.gabor@pharm.unideb.hu</email></nlm:aff></affiliation></author><author><name sortKey="Petak, Istvan" sort="Petak, Istvan" uniqKey="Petak I" first="István" last="Peták">István Peták</name><affiliation><nlm:aff id="af6-ijms-20-05590">Oncompass Medicine Hungary Ltd., H1024 Budapest, Hungary;<email>istvan.petak@oncompassmedicine.com</email></nlm:aff></affiliation></author><author><name sortKey="Valyi Nagy, Istvan" sort="Valyi Nagy, Istvan" uniqKey="Valyi Nagy I" first="István" last="Vályi-Nagy">István Vályi-Nagy</name><affiliation><nlm:aff id="af7-ijms-20-05590">Central Hospital of Southern Pest National Institute of Hematology and Infectious Diseases, H1097 Budapest, Hungary;<email>drvnistvan@gmail.com</email></nlm:aff></affiliation></author></titleStmt><publicationStmt><idno type="wicri:source">PMC</idno><idno type="pmid">31717403</idno><idno type="pmc">6888004</idno><idno type="url">http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6888004</idno><idno type="RBID">PMC:6888004</idno><idno type="doi">10.3390/ijms20225590</idno><date when="2019">2019</date><idno type="wicri:Area/Pmc/Corpus">000617</idno><idno type="wicri:explorRef" wicri:stream="Pmc" wicri:step="Corpus" wicri:corpus="PMC">000617</idno><idno type="wicri:Area/Pmc/Curation">000617</idno><idno type="wicri:explorRef" wicri:stream="Pmc" wicri:step="Curation">000617</idno><idno type="wicri:Area/Pmc/Checkpoint">000534</idno><idno type="wicri:explorRef" wicri:stream="Pmc" wicri:step="Checkpoint">000534</idno><idno type="wicri:Area/Ncbi/Merge">000B93</idno></publicationStmt><sourceDesc><biblStruct><analytic><title xml:lang="en" level="a" type="main">Novel Crizotinib–GnRH Conjugates Revealed the Significance of Lysosomal Trapping in GnRH-Based Drug Delivery Systems</title><author><name sortKey="Muranyi, J Zsef" sort="Muranyi, J Zsef" uniqKey="Muranyi J" first="J Zsef" last="Murányi">J Zsef Murányi</name><affiliation><nlm:aff id="af1-ijms-20-05590">MTA-SE Pathobiochemistry Research Group, Tűzoltó St. 37-47, H1094 Budapest, Hungary;<email>varga.attila@med.semmelweis-univ.hu</email> (A.V.);<email>gyulavari.pal@med.semmelweis-univ.hu</email> (P.G.);<email>penzes.kinga@med.semmelweis-univ.hu</email> (K.P.)</nlm:aff></affiliation><affiliation><nlm:aff id="af2-ijms-20-05590">Department of Medical Chemistry, Molecular Biology and Pathobiochemistry, Semmelweis University, H1094 Budapest, Hungary;<email>nemeth.csilla@med.semmelweis-univ.hu</email> (C.E.N.);<email>csala.miklos@med.semmelweis-univ.hu</email> (M.C.)</nlm:aff></affiliation></author><author><name sortKey="Varga, Attila" sort="Varga, Attila" uniqKey="Varga A" first="Attila" last="Varga">Attila Varga</name><affiliation><nlm:aff id="af1-ijms-20-05590">MTA-SE Pathobiochemistry Research Group, Tűzoltó St. 37-47, H1094 Budapest, Hungary;<email>varga.attila@med.semmelweis-univ.hu</email> (A.V.);<email>gyulavari.pal@med.semmelweis-univ.hu</email> (P.G.);<email>penzes.kinga@med.semmelweis-univ.hu</email> (K.P.)</nlm:aff></affiliation></author><author><name sortKey="Gyulavari, Pal" sort="Gyulavari, Pal" uniqKey="Gyulavari P" first="Pál" last="Gyulavári">Pál Gyulavári</name><affiliation><nlm:aff id="af1-ijms-20-05590">MTA-SE Pathobiochemistry Research Group, Tűzoltó St. 37-47, H1094 Budapest, Hungary;<email>varga.attila@med.semmelweis-univ.hu</email> (A.V.);<email>gyulavari.pal@med.semmelweis-univ.hu</email> (P.G.);<email>penzes.kinga@med.semmelweis-univ.hu</email> (K.P.)</nlm:aff></affiliation></author><author><name sortKey="Penzes, Kinga" sort="Penzes, Kinga" uniqKey="Penzes K" first="Kinga" last="Pénzes">Kinga Pénzes</name><affiliation><nlm:aff id="af1-ijms-20-05590">MTA-SE Pathobiochemistry Research Group, Tűzoltó St. 37-47, H1094 Budapest, Hungary;<email>varga.attila@med.semmelweis-univ.hu</email> (A.V.);<email>gyulavari.pal@med.semmelweis-univ.hu</email> (P.G.);<email>penzes.kinga@med.semmelweis-univ.hu</email> (K.P.)</nlm:aff></affiliation></author><author><name sortKey="Nemeth, Csilla E" sort="Nemeth, Csilla E" uniqKey="Nemeth C" first="Csilla E." last="Németh">Csilla E. Németh</name><affiliation><nlm:aff id="af2-ijms-20-05590">Department of Medical Chemistry, Molecular Biology and Pathobiochemistry, Semmelweis University, H1094 Budapest, Hungary;<email>nemeth.csilla@med.semmelweis-univ.hu</email> (C.E.N.);<email>csala.miklos@med.semmelweis-univ.hu</email> (M.C.)</nlm:aff></affiliation></author><author><name sortKey="Csala, Mikl S" sort="Csala, Mikl S" uniqKey="Csala M" first="Mikl S" last="Csala">Mikl S Csala</name><affiliation><nlm:aff id="af2-ijms-20-05590">Department of Medical Chemistry, Molecular Biology and Pathobiochemistry, Semmelweis University, H1094 Budapest, Hungary;<email>nemeth.csilla@med.semmelweis-univ.hu</email> (C.E.N.);<email>csala.miklos@med.semmelweis-univ.hu</email> (M.C.)</nlm:aff></affiliation></author><author><name sortKey="Peth, Lilla" sort="Peth, Lilla" uniqKey="Peth L" first="Lilla" last="Peth">Lilla Peth</name><affiliation wicri:level="1"><nlm:aff id="af3-ijms-20-05590">MTA-ELTE Research Group of Peptide Chemistry, Eötvös Loránd University, H1117 Budapest, Hungary</nlm:aff><country xml:lang="fr">Hongrie</country><wicri:regionArea>MTA-ELTE Research Group of Peptide Chemistry, Eötvös Loránd University, H1117 Budapest</wicri:regionArea><wicri:noRegion>H1117 Budapest</wicri:noRegion></affiliation></author><author><name sortKey="Csampai, Antal" sort="Csampai, Antal" uniqKey="Csampai A" first="Antal" last="Csámpai">Antal Csámpai</name><affiliation><nlm:aff id="af4-ijms-20-05590">Institute of Chemistry, Eötvös Loránd University, H1117 Budapest, Hungary;<email>csampai@chem.elte.hu</email></nlm:aff></affiliation></author><author><name sortKey="Halmos, Gabor" sort="Halmos, Gabor" uniqKey="Halmos G" first="Gábor" last="Halmos">Gábor Halmos</name><affiliation><nlm:aff id="af5-ijms-20-05590">Department of Biopharmacy, Faculty of Pharmacy, University of Debrecen, H4032 Debrecen, Hungary;<email>halmos.gabor@pharm.unideb.hu</email></nlm:aff></affiliation></author><author><name sortKey="Petak, Istvan" sort="Petak, Istvan" uniqKey="Petak I" first="István" last="Peták">István Peták</name><affiliation><nlm:aff id="af6-ijms-20-05590">Oncompass Medicine Hungary Ltd., H1024 Budapest, Hungary;<email>istvan.petak@oncompassmedicine.com</email></nlm:aff></affiliation></author><author><name sortKey="Valyi Nagy, Istvan" sort="Valyi Nagy, Istvan" uniqKey="Valyi Nagy I" first="István" last="Vályi-Nagy">István Vályi-Nagy</name><affiliation><nlm:aff id="af7-ijms-20-05590">Central Hospital of Southern Pest National Institute of Hematology and Infectious Diseases, H1097 Budapest, Hungary;<email>drvnistvan@gmail.com</email></nlm:aff></affiliation></author></analytic><series><title level="j">International Journal of Molecular Sciences</title><idno type="eISSN">1422-0067</idno><imprint><date when="2019">2019</date></imprint></series></biblStruct></sourceDesc></fileDesc><profileDesc><textClass></textClass></profileDesc></teiHeader><front><div type="abstract" xml:lang="en"><p>Several promising anti-cancer drug–GnRH (gonadotropin-releasing hormone) conjugates have been developed in the last two decades, although none of them have been approved for clinical use yet. Crizotinib is an effective multi-target kinase inhibitor, approved against anaplastic lymphoma kinase (ALK)- or ROS proto-oncogene 1 (ROS-1)-positive non-small cell lung carcinoma (NSCLC); however, its application is accompanied by serious side effects. In order to deliver crizotinib selectively into the tumor cells, we synthesized novel crizotinib analogues and conjugated them to a [<sc>d</sc>-Lys<sup>6</sup>]–GnRH-I targeting peptide. Our most prominent crizotinib–GnRH conjugates, the amide-bond-containing [<sc>d</sc>-Lys<sup>6</sup>(crizotinib*)]–GnRH-I and the ester-bond-containing [<sc>d</sc>-Lys<sup>6</sup>(MJ55*)]–GnRH-I, were able to bind to GnRH-receptor (GnRHR) and exert a potent c-Met kinase inhibitory effect. The efficacy of compounds was tested on the <italic>MET</italic>-amplified and GnRHR-expressing EBC-1 NSCLC cells. In vitro pharmacological profiling led to the conclusion that that crizotinib–GnRH conjugates are transported directly into lysosomes, where the membrane permeability of crizotinib is diminished. As a consequence of GnRHR-mediated endocytosis, GnRH-conjugated crizotinib bypasses its molecular targets—the ATP-binding site of RTKs— and is sequestered in the lysosomes. These results explained the lower efficacy of crizotinib–GnRH conjugates in EBC-1 cells, and led to the conclusion that drug escape from the lysosomes is a major challenge in the development of clinically relevant anti-cancer drug–GnRH conjugates. </p></div></front><back><div1 type="bibliography"><listBibl><biblStruct><analytic><author><name sortKey="Maggi, R" uniqKey="Maggi R">R. Maggi</name></author><author><name sortKey="Cariboni, A M" uniqKey="Cariboni A">A.M. Cariboni</name></author><author><name sortKey="Marelli, M M" uniqKey="Marelli M">M.M. 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<front><journal-meta><journal-id journal-id-type="nlm-ta">Int J Mol Sci</journal-id><journal-id journal-id-type="iso-abbrev">Int J Mol Sci</journal-id><journal-id journal-id-type="publisher-id">ijms</journal-id><journal-title-group><journal-title>International Journal of Molecular Sciences</journal-title></journal-title-group><issn pub-type="epub">1422-0067</issn><publisher><publisher-name>MDPI</publisher-name></publisher></journal-meta><article-meta><article-id pub-id-type="pmid">31717403</article-id><article-id pub-id-type="pmc">6888004</article-id><article-id pub-id-type="doi">10.3390/ijms20225590</article-id><article-id pub-id-type="publisher-id">ijms-20-05590</article-id><article-categories><subj-group subj-group-type="heading"><subject>Article</subject></subj-group></article-categories><title-group><article-title>Novel Crizotinib–GnRH Conjugates Revealed the Significance of Lysosomal Trapping in GnRH-Based Drug Delivery Systems</article-title></title-group><contrib-group><contrib contrib-type="author"><contrib-id contrib-id-type="orcid" authenticated="true">https://orcid.org/0000-0001-5672-6482</contrib-id><name><surname>Murányi</surname><given-names>József</given-names></name><xref ref-type="aff" rid="af1-ijms-20-05590">1</xref><xref ref-type="aff" rid="af2-ijms-20-05590">2</xref><xref rid="c1-ijms-20-05590" ref-type="corresp">*</xref></contrib><contrib contrib-type="author"><name><surname>Varga</surname><given-names>Attila</given-names></name><xref ref-type="aff" rid="af1-ijms-20-05590">1</xref></contrib><contrib contrib-type="author"><name><surname>Gyulavári</surname><given-names>Pál</given-names></name><xref ref-type="aff" rid="af1-ijms-20-05590">1</xref></contrib><contrib contrib-type="author"><name><surname>Pénzes</surname><given-names>Kinga</given-names></name><xref ref-type="aff" rid="af1-ijms-20-05590">1</xref></contrib><contrib contrib-type="author"><name><surname>Németh</surname><given-names>Csilla E.</given-names></name><xref ref-type="aff" rid="af2-ijms-20-05590">2</xref></contrib><contrib contrib-type="author"><contrib-id contrib-id-type="orcid" authenticated="true">https://orcid.org/0000-0002-3829-4361</contrib-id><name><surname>Csala</surname><given-names>Miklós</given-names></name><xref ref-type="aff" rid="af2-ijms-20-05590">2</xref></contrib><contrib contrib-type="author"><contrib-id contrib-id-type="orcid" authenticated="true">https://orcid.org/0000-0002-0298-3341</contrib-id><name><surname>Pethő</surname><given-names>Lilla</given-names></name><xref ref-type="aff" rid="af3-ijms-20-05590">3</xref></contrib><contrib contrib-type="author"><name><surname>Csámpai</surname><given-names>Antal</given-names></name><xref ref-type="aff" rid="af4-ijms-20-05590">4</xref></contrib><contrib contrib-type="author"><name><surname>Halmos</surname><given-names>Gábor</given-names></name><xref ref-type="aff" rid="af5-ijms-20-05590">5</xref></contrib><contrib contrib-type="author"><name><surname>Peták</surname><given-names>István</given-names></name><xref ref-type="aff" rid="af6-ijms-20-05590">6</xref></contrib><contrib contrib-type="author"><name><surname>Vályi-Nagy</surname><given-names>István</given-names></name><xref ref-type="aff" rid="af7-ijms-20-05590">7</xref></contrib></contrib-group><aff id="af1-ijms-20-05590"><label>1</label>MTA-SE Pathobiochemistry Research Group, Tűzoltó St. 37-47, H1094 Budapest, Hungary;<email>varga.attila@med.semmelweis-univ.hu</email> (A.V.);<email>gyulavari.pal@med.semmelweis-univ.hu</email> (P.G.);<email>penzes.kinga@med.semmelweis-univ.hu</email> (K.P.)</aff><aff id="af2-ijms-20-05590"><label>2</label>Department of Medical Chemistry, Molecular Biology and Pathobiochemistry, Semmelweis University, H1094 Budapest, Hungary;<email>nemeth.csilla@med.semmelweis-univ.hu</email> (C.E.N.);<email>csala.miklos@med.semmelweis-univ.hu</email> (M.C.)</aff><aff id="af3-ijms-20-05590"><label>3</label>MTA-ELTE Research Group of Peptide Chemistry, Eötvös Loránd University, H1117 Budapest, Hungary</aff><aff id="af4-ijms-20-05590"><label>4</label>Institute of Chemistry, Eötvös Loránd University, H1117 Budapest, Hungary;<email>csampai@chem.elte.hu</email></aff><aff id="af5-ijms-20-05590"><label>5</label>Department of Biopharmacy, Faculty of Pharmacy, University of Debrecen, H4032 Debrecen, Hungary;<email>halmos.gabor@pharm.unideb.hu</email></aff><aff id="af6-ijms-20-05590"><label>6</label>Oncompass Medicine Hungary Ltd., H1024 Budapest, Hungary;<email>istvan.petak@oncompassmedicine.com</email></aff><aff id="af7-ijms-20-05590"><label>7</label>Central Hospital of Southern Pest National Institute of Hematology and Infectious Diseases, H1097 Budapest, Hungary;<email>drvnistvan@gmail.com</email></aff><author-notes><corresp id="c1-ijms-20-05590"><label>*</label>Correspondence: <email>muranyi.jozsef@med.semmelweis-univ.hu</email></corresp></author-notes><pub-date pub-type="epub"><day>08</day><month>11</month><year>2019</year></pub-date><pub-date pub-type="collection"><month>11</month><year>2019</year></pub-date><volume>20</volume><issue>22</issue><elocation-id>5590</elocation-id><history><date date-type="received"><day>30</day><month>9</month><year>2019</year></date><date date-type="accepted"><day>06</day><month>11</month><year>2019</year></date></history><permissions><copyright-statement>© 2019 by the authors.</copyright-statement><copyright-year>2019</copyright-year><license license-type="open-access"><license-p>Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (<ext-link ext-link-type="uri" xlink:href="http://creativecommons.org/licenses/by/4.0/">http://creativecommons.org/licenses/by/4.0/</ext-link>).</license-p></license></permissions><abstract><p>Several promising anti-cancer drug–GnRH (gonadotropin-releasing hormone) conjugates have been developed in the last two decades, although none of them have been approved for clinical use yet. Crizotinib is an effective multi-target kinase inhibitor, approved against anaplastic lymphoma kinase (ALK)- or ROS proto-oncogene 1 (ROS-1)-positive non-small cell lung carcinoma (NSCLC); however, its application is accompanied by serious side effects. In order to deliver crizotinib selectively into the tumor cells, we synthesized novel crizotinib analogues and conjugated them to a [<sc>d</sc>-Lys<sup>6</sup>]–GnRH-I targeting peptide. Our most prominent crizotinib–GnRH conjugates, the amide-bond-containing [<sc>d</sc>-Lys<sup>6</sup>(crizotinib*)]–GnRH-I and the ester-bond-containing [<sc>d</sc>-Lys<sup>6</sup>(MJ55*)]–GnRH-I, were able to bind to GnRH-receptor (GnRHR) and exert a potent c-Met kinase inhibitory effect. The efficacy of compounds was tested on the <italic>MET</italic>-amplified and GnRHR-expressing EBC-1 NSCLC cells. In vitro pharmacological profiling led to the conclusion that that crizotinib–GnRH conjugates are transported directly into lysosomes, where the membrane permeability of crizotinib is diminished. As a consequence of GnRHR-mediated endocytosis, GnRH-conjugated crizotinib bypasses its molecular targets—the ATP-binding site of RTKs— and is sequestered in the lysosomes. These results explained the lower efficacy of crizotinib–GnRH conjugates in EBC-1 cells, and led to the conclusion that drug escape from the lysosomes is a major challenge in the development of clinically relevant anti-cancer drug–GnRH conjugates. </p></abstract><kwd-group><kwd>targeted drug delivery 1</kwd><kwd>GnRH 2</kwd><kwd>GnRHR 3</kwd><kwd>lysosome 3</kwd><kwd>permeability 4</kwd><kwd>crizotinib 5</kwd><kwd>conjugate 6</kwd><kwd>NSCLC 7</kwd><kwd>c-Met 8</kwd><kwd>endocytosis 9</kwd><kwd>galectin 10</kwd></kwd-group></article-meta></front><floats-group><fig id="ijms-20-05590-f001" orientation="portrait" position="float"><label>Figure 1</label><caption><p>The nitrogen atom of piperidine in crizotinib was selected for conjugation (marked by red arrow). (<bold>A</bold>) Structure of (R)-crizotinib; (<bold>B</bold>) X-ray structure of crizotinib bound to the kinase domain of c-Met (2WGJ). The hydrophobicity of the ATP-binding pocket is colored from red (hydrophilic) to green (hydrophobic). Hydrogen bonds are marked with blue dashed lines.</p></caption><graphic xlink:href="ijms-20-05590-g001"></graphic></fig><fig id="ijms-20-05590-f002" orientation="portrait" position="float"><label>Figure 2</label><caption><p>Synthesis of crizotinib*, [<sc>d</sc>-Lys<sup>6</sup>(crizotinib*)]–GnRH-I, MJ55*, and [<sc>d</sc>-Lys<sup>6</sup>(MJ55*)]–GnRH-I. (<bold>a</bold>) 2 M Cs<sub>2</sub>CO<sub>3</sub> in H<sub>2</sub>O, Pd(dppf)Cl<sub>2</sub>*, dimethyl sulfoxide, 70 °C, 3 h; (<bold>b</bold>) trifluoroacetic acid/water (9:1 ratio) 25 °C, 2 h; (<bold>c</bold>) glutaric anhydride, triethylamine, CH<sub>2</sub>Cl<sub>2</sub>, 25 °C, 2 h; (<bold>d</bold>) COMU**, 4-methylmorpholine, <italic>N,N</italic>-dimethylformamide, 25 °C, 2 h; (<bold>e</bold>) trifluoroacetic acid /phenol/water/triisopropyl silane (88:5:5:2 ratio) 25 °C, 2 h; (<bold>f</bold>) K<sub>2</sub>CO<sub>3</sub>, bromoethanol, tetrahydrofuran, reflux, 24 h. *Pd(dppf)Cl<sub>2</sub>—[1,1′-Bis(diphenylphosphino)ferrocene]dichloropalladium(II). **COMU—(1-Cyano-2-ethoxy-2-oxoethylidenaminooxy)dimethylamino-morpholino-carbenium hexafluorophosphate.</p></caption><graphic xlink:href="ijms-20-05590-g002"></graphic></fig><fig id="ijms-20-05590-f003" orientation="portrait" position="float"><label>Figure 3</label><caption><p>GnRHR expression and cellular uptake of [<sc>d</sc>-Lys<sup>6</sup>(FITC)]–GnRH-I on EBC-1 cells. (<bold>A</bold>) Expression of GnRHR in EBC-1 cells, confirmed by western blot; (<bold>B</bold>) EBC-1 cells contain a high level of GnRHR (total GnRHR) and a high proportion of these receptors are located in the plasma membrane (membrane GnRHR). Nuclei: blue (DRAQ5), GnRHR: red (Alexa Fluor 594); (<bold>C</bold>) Time- and concentration-dependent dynamic uptake of [<sc>d</sc>-Lys<sup>6</sup>(FITC)]–GnRH-I was confirmed by flow cytometry. Results are presented as mean relative fluorescent intensity ± SD (<italic>N</italic> = 3); (<bold>D</bold>) Intracellular localization of [<sc>d</sc>-Lys<sup>6</sup>(FITC)]–GnRH-I (green; 10 µM, 24 h) in EBC-1 cells was confirmed by confocal microscopy (nuclei: blue).</p></caption><graphic xlink:href="ijms-20-05590-g003"></graphic></fig><fig id="ijms-20-05590-f004" orientation="portrait" position="float"><label>Figure 4</label><caption><p>Biological evaluation of compounds. (<bold>A</bold>) Viability inhibition effect on EBC-1 NSCLC cells; (<bold>B</bold>) viability inhibition effect on human primary skin fibroblast cells; (<bold>C</bold>) in vitro inhibition effect on the recombinant c-Met kinase; (<bold>D</bold>) stability in cell culture medium at 37 °C; All values are the mean ± SD of at least three independent experiments.</p></caption><graphic xlink:href="ijms-20-05590-g004"></graphic></fig><fig id="ijms-20-05590-f005" orientation="portrait" position="float"><label>Figure 5</label><caption><p>The c-Met inbibitory effect of the compounds in EBC-1 cells. Cells were treated with [<sc>d</sc>-Lys<sup>6</sup>]–GnRH-I, crizotinib*, MJ55*, [<sc>d</sc>-Lys<sup>6</sup>(crizotinib*)]–GnRH-I, and [<sc>d</sc>-Lys<sup>6</sup>(MJ55*)]–GnRH-I for 6 h, and c-Met phosphorylation was analyzed by western blot. Untreated cells and the [<sc>d</sc>-Lys<sup>6</sup>]–GnRH-I-treated cells were used as negative controls. α-tubulin was used as the loading control (<italic>N</italic> = 3).</p></caption><graphic xlink:href="ijms-20-05590-g005"></graphic></fig><fig id="ijms-20-05590-f006" orientation="portrait" position="float"><label>Figure 6</label><caption><p>Colocalization of [<sc>d</sc>-Lys<sup>6</sup>(FITC)]–GnRH-I and the lysosomes in EBC-1 cells. The green fluorescent signal of [<sc>d</sc>-Lys<sup>6</sup>(FITC)]–GnRH-I (10 µM, 24 h) showed strong colocalization with the red fluorescent signal of lysosome marker Lysoview 633.</p></caption><graphic xlink:href="ijms-20-05590-g006"></graphic></fig><fig id="ijms-20-05590-f007" orientation="portrait" position="float"><label>Figure 7</label><caption><p>The pH-dependent artificial membrane permeability assay revealed the lysosomotropic character of crizotinib* and MJ55*. (<bold>A</bold>) Permeability of crizotinib* and MJ55*. Caffeine was used as control; (<bold>B</bold>) the pKa value of the pyridinium cation is ~5.6 in crizotinib [<xref rid="B20-ijms-20-05590" ref-type="bibr">20</xref>] and MJ55*. The pKa value of the piperidinium cation is 9.4 in crizotinib* [<xref rid="B20-ijms-20-05590" ref-type="bibr">20</xref>] and 8.5 in MJ55* (predicted by ChemDraw Prime 15.1). The pKa value of the caffeine cation is 0.7 (<uri xlink:href="https://pubchem.ncbi.nlm.nih.gov/compound/caffeine">https://pubchem.ncbi.nlm.nih.gov/compound/caffeine</uri>).</p></caption><graphic xlink:href="ijms-20-05590-g007"></graphic></fig><fig id="ijms-20-05590-f008" orientation="portrait" position="float"><label>Figure 8</label><caption><p>Galectin puncta assay for crizotinib* and [<sc>d</sc>-Lys<sup>6</sup>(crizotinib*)]–GnRH-I in EBC-1 cells. Galectin-3 and galectin-1 puncta formation indicate lysosomal membrane damage. Galectin-3: green (Alexa Fluor 488); galectin-1: red (Alexa Fluor 594); nuclei: blue (DRAQ5).</p></caption><graphic xlink:href="ijms-20-05590-g008"></graphic></fig><fig id="ijms-20-05590-f009" orientation="portrait" position="float"><label>Figure 9</label><caption><p>Intracellular trafficking of crizotinib* and [<sc>d</sc>-Lys<sup>6</sup>(crizotinib*)]–GnRH-I. (<bold>A</bold>) Crizotinib is able to reach the ATP-binding site of c-Met by passive diffusion and to effectively inhibit the c-Met-mediated oncogenic signaling, while <bold>only</bold> a proportion of the drug accumulates in the lysosomes. (<bold>B</bold>) The GnRHR-mediated endocytosis leads to the lysosomal sequestration of GnRHR-targeted crizotinib* at the nanomolar concentration range; meanwhile, crizotinib* bypasses c-Met. (<bold>C</bold>) One possible explanation for the c-Met inhibition and the cell viability inhibition effect of [<sc>d</sc>-Lys<sup>6</sup>(crizotinib*)]–GnRH-I at the micromolar concentration range is that during the GnRHR internalization, non–GnRHR-bound conjugates might loaded into the vesicles as “passive passengers”. High lysosomal accumulation of these passive passengers might destabilize the membrane of the lysosomes, leading to drug leakage and cell death.</p></caption><graphic xlink:href="ijms-20-05590-g009"></graphic></fig><table-wrap id="ijms-20-05590-t001" orientation="portrait" position="float"><object-id pub-id-type="pii">ijms-20-05590-t001_Table 1</object-id><label>Table 1</label><caption><p>Inhibition of [<sup>125</sup>I]-[<sc>d</sc>-Trp<sup>6</sup>]–GnRH-I binding to the membranes of human pituitary and human prostate cancer cells by GnRH derivatives.</p></caption><table frame="hsides" rules="groups"><thead><tr><th rowspan="2" align="center" valign="middle" style="border-top:solid thin;border-bottom:solid thin" colspan="1">Compound</th><th colspan="2" align="center" valign="middle" style="border-top:solid thin;border-bottom:solid thin" rowspan="1">IC<sub>50</sub> Values (nM) <sup>1</sup></th></tr><tr><th align="center" valign="middle" style="border-bottom:solid thin" rowspan="1" colspan="1">Human Pituitary</th><th align="center" valign="middle" style="border-bottom:solid thin" rowspan="1" colspan="1">Human Prostate Cancer</th></tr></thead><tbody><tr><td align="center" valign="middle" rowspan="1" colspan="1">[<sc>d</sc>-Lys<sup>6</sup>]GnRH-I (vehicle)</td><td align="center" valign="middle" rowspan="1" colspan="1">6.44 ± 1.0</td><td align="center" valign="middle" rowspan="1" colspan="1">4.31 ± 0.8</td></tr><tr><td align="center" valign="middle" rowspan="1" colspan="1">[<sc>d</sc>-Lys<sup>6</sup>(FITC)]–GnRH-I</td><td align="center" valign="middle" rowspan="1" colspan="1">27.2 ± 2.8</td><td align="center" valign="middle" rowspan="1" colspan="1">18.3 ± 2.9</td></tr><tr><td align="center" valign="middle" rowspan="1" colspan="1">[<sc>d</sc>-Lys<sup>6</sup>(crizotinib*)]–GnRH-I </td><td align="center" valign="middle" rowspan="1" colspan="1">34.6 ± 4.2</td><td align="center" valign="middle" rowspan="1" colspan="1">39.5 ± 1.7</td></tr><tr><td align="center" valign="middle" style="border-bottom:solid thin" rowspan="1" colspan="1">[<sc>d</sc>-Lys<sup>6</sup>(MJ55*)]–GnRH-I </td><td align="center" valign="middle" style="border-bottom:solid thin" rowspan="1" colspan="1">21.7 ± 1.4</td><td align="center" valign="middle" style="border-bottom:solid thin" rowspan="1" colspan="1">29.7 ± 3.1</td></tr></tbody></table><table-wrap-foot><fn><p><sup>1</sup> IC<sub>50</sub> values were calculated via computerized curve-fitting program from displacement experiments, as described previously [<xref rid="B19-ijms-20-05590" ref-type="bibr">19</xref>]. IC<sub>50</sub> is defined as the dose causing 50% inhibition of specific binding of [<sup>125</sup>I]-[<sc>d</sc>-Trp<sup>6</sup>]–GnRH-I to the membranes. Values are mean ± standard deviation (SD) of two to three independent experiments.</p></fn></table-wrap-foot></table-wrap></floats-group></pmc><affiliations><list><country><li>Hongrie</li></country></list><tree><noCountry><name sortKey="Csala, Mikl S" sort="Csala, Mikl S" uniqKey="Csala M" first="Mikl S" last="Csala">Mikl S Csala</name><name sortKey="Csampai, Antal" sort="Csampai, Antal" uniqKey="Csampai A" first="Antal" last="Csámpai">Antal Csámpai</name><name sortKey="Gyulavari, Pal" sort="Gyulavari, Pal" uniqKey="Gyulavari P" first="Pál" last="Gyulavári">Pál Gyulavári</name><name sortKey="Halmos, Gabor" sort="Halmos, Gabor" uniqKey="Halmos G" first="Gábor" last="Halmos">Gábor Halmos</name><name sortKey="Muranyi, J Zsef" sort="Muranyi, J Zsef" uniqKey="Muranyi J" first="J Zsef" last="Murányi">J Zsef Murányi</name><name sortKey="Nemeth, Csilla E" sort="Nemeth, Csilla E" uniqKey="Nemeth C" first="Csilla E." last="Németh">Csilla E. Németh</name><name sortKey="Penzes, Kinga" sort="Penzes, Kinga" uniqKey="Penzes K" first="Kinga" last="Pénzes">Kinga Pénzes</name><name sortKey="Petak, Istvan" sort="Petak, Istvan" uniqKey="Petak I" first="István" last="Peták">István Peták</name><name sortKey="Valyi Nagy, Istvan" sort="Valyi Nagy, Istvan" uniqKey="Valyi Nagy I" first="István" last="Vályi-Nagy">István Vályi-Nagy</name><name sortKey="Varga, Attila" sort="Varga, Attila" uniqKey="Varga A" first="Attila" last="Varga">Attila Varga</name></noCountry><country name="Hongrie"><noRegion><name sortKey="Peth, Lilla" sort="Peth, Lilla" uniqKey="Peth L" first="Lilla" last="Peth">Lilla Peth</name></noRegion></country></tree></affiliations></record>Pour manipuler ce document sous Unix (Dilib)
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