Comparative and kinetic analysis of viral shedding and immunological responses in MERS patients representing a broad spectrum of disease severity
Identifieur interne : 000434 ( Pmc/Corpus ); précédent : 000433; suivant : 000435Comparative and kinetic analysis of viral shedding and immunological responses in MERS patients representing a broad spectrum of disease severity
Auteurs : Chan-Ki Min ; Shinhye Cheon ; Na-Young Ha ; Kyung Mok Sohn ; Yuri Kim ; Abdimadiyeva Aigerim ; Hyun Mu Shin ; Ji-Yeob Choi ; Kyung-Soo Inn ; Jin-Hwan Kim ; Jae Young Moon ; Myung-Sik Choi ; Nam-Hyuk Cho ; Yeon-Sook KimSource :
- Scientific Reports [ 2045-2322 ] ; 2016.
Abstract
Despite the ongoing spread of MERS, there is limited knowledge of the factors affecting its severity and outcomes. We analyzed clinical data and specimens from fourteen MERS patients treated in a hospital who collectively represent a wide spectrum of disease severity, ranging from mild febrile illness to fatal pneumonia, and classified the patients into four groups based on severity and mortality. Comparative and kinetic analyses revealed that high viral loads, weak antibody responses, and lymphopenia accompanying thrombocytopenia were associated with disease mortality, whereas persistent and gradual increases in lymphocyte responses might be required for effective immunity against MERS-CoV infection. Leukocytosis, primarily due to increased neutrophils and monocytes, was generally observed in more severe and fatal cases. The blood levels of cytokines such as IL-10, IL-15, TGF-β, and EGF were either positively or negatively correlated with disease mortality. Robust induction of various chemokines with differential kinetics was more prominent in patients that recovered from pneumonia than in patients with mild febrile illness or deceased patients. The correlation of the virological and immunological responses with disease severity and mortality, as well as their responses to current antiviral therapy, may have prognostic significance during the early phase of MERS.
The online version of this article (doi:10.1038/srep25359) contains supplementary material, which is available to authorized users.
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DOI: 10.1038/srep25359
PubMed: 27146253
PubMed Central: 4857172
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PMC:4857172Le document en format XML
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institution-id-type="GRID">grid.31501.36</institution-id><institution-id institution-id-type="ISNI">0000 0004 0470 5905</institution-id><institution>Cancer Research Institute, Seoul National University College of Medicine,</institution></institution-wrap>Seoul Republic of Korea</nlm:aff></affiliation></author><author><name sortKey="Inn, Kyung Soo" sort="Inn, Kyung Soo" uniqKey="Inn K" first="Kyung-Soo" last="Inn">Kyung-Soo Inn</name><affiliation><nlm:aff id="Aff5"><institution-wrap><institution-id institution-id-type="GRID">grid.289247.2</institution-id><institution-id institution-id-type="ISNI">0000 0001 2171 7818</institution-id><institution>Department of Pharmaceutical Science,</institution><institution>College of Pharmacy, Kyung Hee University,</institution></institution-wrap>Seoul Republic of Korea</nlm:aff></affiliation></author><author><name sortKey="Kim, Jin Hwan" sort="Kim, Jin Hwan" uniqKey="Kim J" first="Jin-Hwan" last="Kim">Jin-Hwan Kim</name><affiliation><nlm:aff 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xml:lang="en" level="a" type="main">Comparative and kinetic analysis of viral shedding and immunological responses in MERS patients representing a broad spectrum of disease severity</title><author><name sortKey="Min, Chan Ki" sort="Min, Chan Ki" uniqKey="Min C" first="Chan-Ki" last="Min">Chan-Ki Min</name><affiliation><nlm:aff id="Aff1"><institution-wrap><institution-id institution-id-type="GRID">grid.31501.36</institution-id><institution-id institution-id-type="ISNI">0000 0004 0470 5905</institution-id><institution>Department of Microbiology and Immunology,</institution><institution>Seoul National University College of Medicine,</institution></institution-wrap>Seoul Republic of Korea</nlm:aff></affiliation><affiliation><nlm:aff id="Aff2"><institution-wrap><institution-id institution-id-type="GRID">grid.31501.36</institution-id><institution-id institution-id-type="ISNI">0000 0004 0470 5905</institution-id><institution>Department of Biomedical Sciences,</institution><institution>Seoul National University College of Medicine,</institution></institution-wrap>Seoul Republic of Korea</nlm:aff></affiliation></author><author><name sortKey="Cheon, Shinhye" sort="Cheon, Shinhye" uniqKey="Cheon S" first="Shinhye" last="Cheon">Shinhye Cheon</name><affiliation><nlm:aff id="Aff3"><institution-wrap><institution-id institution-id-type="GRID">grid.254230.2</institution-id><institution-id institution-id-type="ISNI">0000 0001 0722 6377</institution-id><institution>Division of Infectious Diseases, Department of Internal Medicine,</institution><institution>Chungnam National University School of Medicine,</institution></institution-wrap>Daejeon, Republic of Korea</nlm:aff></affiliation></author><author><name sortKey="Ha, Na Young" sort="Ha, Na Young" uniqKey="Ha N" first="Na-Young" last="Ha">Na-Young Ha</name><affiliation><nlm:aff id="Aff1"><institution-wrap><institution-id institution-id-type="GRID">grid.31501.36</institution-id><institution-id institution-id-type="ISNI">0000 0004 0470 5905</institution-id><institution>Department of Microbiology and Immunology,</institution><institution>Seoul National University College of Medicine,</institution></institution-wrap>Seoul Republic of Korea</nlm:aff></affiliation><affiliation><nlm:aff id="Aff2"><institution-wrap><institution-id institution-id-type="GRID">grid.31501.36</institution-id><institution-id institution-id-type="ISNI">0000 0004 0470 5905</institution-id><institution>Department of Biomedical Sciences,</institution><institution>Seoul National University College of Medicine,</institution></institution-wrap>Seoul Republic of Korea</nlm:aff></affiliation></author><author><name sortKey="Sohn, Kyung Mok" sort="Sohn, Kyung Mok" uniqKey="Sohn K" first="Kyung Mok" last="Sohn">Kyung Mok Sohn</name><affiliation><nlm:aff id="Aff3"><institution-wrap><institution-id institution-id-type="GRID">grid.254230.2</institution-id><institution-id institution-id-type="ISNI">0000 0001 0722 6377</institution-id><institution>Division of Infectious Diseases, Department of Internal Medicine,</institution><institution>Chungnam National University School of Medicine,</institution></institution-wrap>Daejeon, Republic of Korea</nlm:aff></affiliation></author><author><name sortKey="Kim, Yuri" sort="Kim, Yuri" uniqKey="Kim Y" first="Yuri" last="Kim">Yuri Kim</name><affiliation><nlm:aff id="Aff1"><institution-wrap><institution-id institution-id-type="GRID">grid.31501.36</institution-id><institution-id institution-id-type="ISNI">0000 0004 0470 5905</institution-id><institution>Department of Microbiology and Immunology,</institution><institution>Seoul National University College of Medicine,</institution></institution-wrap>Seoul Republic of Korea</nlm:aff></affiliation><affiliation><nlm:aff id="Aff2"><institution-wrap><institution-id institution-id-type="GRID">grid.31501.36</institution-id><institution-id institution-id-type="ISNI">0000 0004 0470 5905</institution-id><institution>Department of Biomedical Sciences,</institution><institution>Seoul National University College of Medicine,</institution></institution-wrap>Seoul Republic of Korea</nlm:aff></affiliation></author><author><name sortKey="Aigerim, Abdimadiyeva" sort="Aigerim, Abdimadiyeva" uniqKey="Aigerim A" first="Abdimadiyeva" last="Aigerim">Abdimadiyeva Aigerim</name><affiliation><nlm:aff id="Aff1"><institution-wrap><institution-id institution-id-type="GRID">grid.31501.36</institution-id><institution-id institution-id-type="ISNI">0000 0004 0470 5905</institution-id><institution>Department of Microbiology and Immunology,</institution><institution>Seoul National University College of Medicine,</institution></institution-wrap>Seoul Republic of Korea</nlm:aff></affiliation><affiliation><nlm:aff id="Aff2"><institution-wrap><institution-id institution-id-type="GRID">grid.31501.36</institution-id><institution-id institution-id-type="ISNI">0000 0004 0470 5905</institution-id><institution>Department of Biomedical Sciences,</institution><institution>Seoul National University College of Medicine,</institution></institution-wrap>Seoul Republic of Korea</nlm:aff></affiliation></author><author><name sortKey="Shin, Hyun Mu" sort="Shin, Hyun Mu" uniqKey="Shin H" first="Hyun Mu" last="Shin">Hyun Mu Shin</name><affiliation><nlm:aff id="Aff1"><institution-wrap><institution-id institution-id-type="GRID">grid.31501.36</institution-id><institution-id institution-id-type="ISNI">0000 0004 0470 5905</institution-id><institution>Department of Microbiology and Immunology,</institution><institution>Seoul National University College of Medicine,</institution></institution-wrap>Seoul Republic of Korea</nlm:aff></affiliation><affiliation><nlm:aff id="Aff2"><institution-wrap><institution-id institution-id-type="GRID">grid.31501.36</institution-id><institution-id institution-id-type="ISNI">0000 0004 0470 5905</institution-id><institution>Department of Biomedical Sciences,</institution><institution>Seoul National University College of Medicine,</institution></institution-wrap>Seoul Republic of Korea</nlm:aff></affiliation></author><author><name sortKey="Choi, Ji Yeob" sort="Choi, Ji Yeob" uniqKey="Choi J" first="Ji-Yeob" last="Choi">Ji-Yeob Choi</name><affiliation><nlm:aff id="Aff2"><institution-wrap><institution-id institution-id-type="GRID">grid.31501.36</institution-id><institution-id institution-id-type="ISNI">0000 0004 0470 5905</institution-id><institution>Department of Biomedical Sciences,</institution><institution>Seoul National University College of Medicine,</institution></institution-wrap>Seoul Republic of Korea</nlm:aff></affiliation><affiliation><nlm:aff id="Aff4"><institution-wrap><institution-id institution-id-type="GRID">grid.31501.36</institution-id><institution-id institution-id-type="ISNI">0000 0004 0470 5905</institution-id><institution>Cancer Research Institute, Seoul National University College of Medicine,</institution></institution-wrap>Seoul Republic of Korea</nlm:aff></affiliation></author><author><name sortKey="Inn, Kyung Soo" sort="Inn, Kyung Soo" uniqKey="Inn K" first="Kyung-Soo" last="Inn">Kyung-Soo Inn</name><affiliation><nlm:aff id="Aff5"><institution-wrap><institution-id institution-id-type="GRID">grid.289247.2</institution-id><institution-id institution-id-type="ISNI">0000 0001 2171 7818</institution-id><institution>Department of Pharmaceutical Science,</institution><institution>College of Pharmacy, Kyung Hee University,</institution></institution-wrap>Seoul Republic of Korea</nlm:aff></affiliation></author><author><name sortKey="Kim, Jin Hwan" sort="Kim, Jin Hwan" uniqKey="Kim J" first="Jin-Hwan" last="Kim">Jin-Hwan Kim</name><affiliation><nlm:aff id="Aff6"><institution-wrap><institution-id institution-id-type="GRID">grid.254230.2</institution-id><institution-id institution-id-type="ISNI">0000 0001 0722 6377</institution-id><institution>Department of Radiology,</institution><institution>Chungnam National University School of Medicine,</institution></institution-wrap>Daejeon, Republic of Korea</nlm:aff></affiliation></author><author><name sortKey="Moon, Jae Young" sort="Moon, Jae Young" uniqKey="Moon J" first="Jae Young" last="Moon">Jae Young Moon</name><affiliation><nlm:aff id="Aff7"><institution-wrap><institution-id institution-id-type="GRID">grid.254230.2</institution-id><institution-id institution-id-type="ISNI">0000 0001 0722 6377</institution-id><institution>Division of Pulmonology and Critical Care Medicine, Department of Internal Medicine,</institution><institution>Chungnam National University School of Medicine,</institution></institution-wrap>Daejeon, Republic of Korea</nlm:aff></affiliation></author><author><name sortKey="Choi, Myung Sik" sort="Choi, Myung Sik" uniqKey="Choi M" first="Myung-Sik" last="Choi">Myung-Sik Choi</name><affiliation><nlm:aff id="Aff1"><institution-wrap><institution-id institution-id-type="GRID">grid.31501.36</institution-id><institution-id institution-id-type="ISNI">0000 0004 0470 5905</institution-id><institution>Department of Microbiology and Immunology,</institution><institution>Seoul National University College of Medicine,</institution></institution-wrap>Seoul Republic of Korea</nlm:aff></affiliation></author><author><name sortKey="Cho, Nam Hyuk" sort="Cho, Nam Hyuk" uniqKey="Cho N" first="Nam-Hyuk" last="Cho">Nam-Hyuk Cho</name><affiliation><nlm:aff id="Aff1"><institution-wrap><institution-id institution-id-type="GRID">grid.31501.36</institution-id><institution-id institution-id-type="ISNI">0000 0004 0470 5905</institution-id><institution>Department of Microbiology and Immunology,</institution><institution>Seoul National University College of Medicine,</institution></institution-wrap>Seoul Republic of Korea</nlm:aff></affiliation><affiliation><nlm:aff id="Aff2"><institution-wrap><institution-id institution-id-type="GRID">grid.31501.36</institution-id><institution-id institution-id-type="ISNI">0000 0004 0470 5905</institution-id><institution>Department of Biomedical Sciences,</institution><institution>Seoul National University College of Medicine,</institution></institution-wrap>Seoul Republic of Korea</nlm:aff></affiliation><affiliation><nlm:aff id="Aff8"><institution-wrap><institution-id institution-id-type="GRID">grid.31501.36</institution-id><institution-id institution-id-type="ISNI">0000 0004 0470 5905</institution-id><institution>Institute of Endemic Disease, Seoul National University Medical Research Center and Bundang Hospital,</institution></institution-wrap>Seoul Republic of Korea</nlm:aff></affiliation></author><author><name sortKey="Kim, Yeon Sook" sort="Kim, Yeon Sook" uniqKey="Kim Y" first="Yeon-Sook" last="Kim">Yeon-Sook Kim</name><affiliation><nlm:aff id="Aff3"><institution-wrap><institution-id institution-id-type="GRID">grid.254230.2</institution-id><institution-id institution-id-type="ISNI">0000 0001 0722 6377</institution-id><institution>Division of Infectious Diseases, Department of Internal Medicine,</institution><institution>Chungnam National University School of Medicine,</institution></institution-wrap>Daejeon, Republic of Korea</nlm:aff></affiliation></author></analytic><series><title level="j">Scientific Reports</title><idno type="eISSN">2045-2322</idno><imprint><date when="2016">2016</date></imprint></series></biblStruct></sourceDesc></fileDesc><profileDesc><textClass></textClass></profileDesc></teiHeader><front><div type="abstract" xml:lang="en"><p id="Par1">Despite the ongoing spread of MERS, there is limited knowledge of the factors affecting its severity and outcomes. We analyzed clinical data and specimens from fourteen MERS patients treated in a hospital who collectively represent a wide spectrum of disease severity, ranging from mild febrile illness to fatal pneumonia, and classified the patients into four groups based on severity and mortality. Comparative and kinetic analyses revealed that high viral loads, weak antibody responses, and lymphopenia accompanying thrombocytopenia were associated with disease mortality, whereas persistent and gradual increases in lymphocyte responses might be required for effective immunity against MERS-CoV infection. Leukocytosis, primarily due to increased neutrophils and monocytes, was generally observed in more severe and fatal cases. The blood levels of cytokines such as IL-10, IL-15, TGF-β, and EGF were either positively or negatively correlated with disease mortality. Robust induction of various chemokines with differential kinetics was more prominent in patients that recovered from pneumonia than in patients with mild febrile illness or deceased patients. The correlation of the virological and immunological responses with disease severity and mortality, as well as their responses to current antiviral therapy, may have prognostic significance during the early phase of MERS.</p><sec><title>Supplementary information</title><p>The online version of this article (doi:10.1038/srep25359) contains supplementary material, which is available to authorized users.</p></sec></div></front><back><div1 type="bibliography"><listBibl><biblStruct><analytic><author><name sortKey="Chan, Jf" uniqKey="Chan J">JF Chan</name></author></analytic></biblStruct><biblStruct></biblStruct><biblStruct><analytic><author><name sortKey="Azhar, Ei" uniqKey="Azhar E">EI Azhar</name></author></analytic></biblStruct><biblStruct><analytic><author><name sortKey="Drosten, C" uniqKey="Drosten C">C Drosten</name></author></analytic></biblStruct><biblStruct><analytic><author><name sortKey="Oboho, Ik" uniqKey="Oboho I">IK 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<front><journal-meta><journal-id journal-id-type="nlm-ta">Sci Rep</journal-id><journal-id journal-id-type="iso-abbrev">Sci Rep</journal-id><journal-title-group><journal-title>Scientific Reports</journal-title></journal-title-group><issn pub-type="epub">2045-2322</issn><publisher><publisher-name>Nature Publishing Group UK</publisher-name><publisher-loc>London</publisher-loc></publisher></journal-meta><article-meta><article-id pub-id-type="pmid">27146253</article-id><article-id pub-id-type="pmc">4857172</article-id><article-id pub-id-type="publisher-id">BFsrep25359</article-id><article-id pub-id-type="doi">10.1038/srep25359</article-id><article-categories><subj-group subj-group-type="heading"><subject>Article</subject></subj-group></article-categories><title-group><article-title>Comparative and kinetic analysis of viral shedding and immunological responses in MERS patients representing a broad spectrum of disease severity</article-title></title-group><contrib-group><contrib contrib-type="author" equal-contrib="yes"><name><surname>Min</surname><given-names>Chan-Ki</given-names></name><xref ref-type="aff" rid="Aff1">1</xref><xref ref-type="aff" rid="Aff2">2</xref></contrib><contrib contrib-type="author" equal-contrib="yes"><name><surname>Cheon</surname><given-names>Shinhye</given-names></name><xref ref-type="aff" rid="Aff3">3</xref></contrib><contrib contrib-type="author" equal-contrib="yes"><name><surname>Ha</surname><given-names>Na-Young</given-names></name><xref ref-type="aff" rid="Aff1">1</xref><xref ref-type="aff" rid="Aff2">2</xref></contrib><contrib contrib-type="author" equal-contrib="yes"><name><surname>Sohn</surname><given-names>Kyung Mok</given-names></name><xref ref-type="aff" rid="Aff3">3</xref></contrib><contrib contrib-type="author"><name><surname>Kim</surname><given-names>Yuri</given-names></name><xref ref-type="aff" rid="Aff1">1</xref><xref ref-type="aff" rid="Aff2">2</xref></contrib><contrib contrib-type="author"><name><surname>Aigerim</surname><given-names>Abdimadiyeva</given-names></name><xref ref-type="aff" rid="Aff1">1</xref><xref ref-type="aff" rid="Aff2">2</xref></contrib><contrib contrib-type="author"><name><surname>Shin</surname><given-names>Hyun Mu</given-names></name><xref ref-type="aff" rid="Aff1">1</xref><xref ref-type="aff" rid="Aff2">2</xref></contrib><contrib contrib-type="author"><name><surname>Choi</surname><given-names>Ji-Yeob</given-names></name><xref ref-type="aff" rid="Aff2">2</xref><xref ref-type="aff" rid="Aff4">4</xref></contrib><contrib contrib-type="author"><name><surname>Inn</surname><given-names>Kyung-Soo</given-names></name><xref ref-type="aff" rid="Aff5">5</xref></contrib><contrib contrib-type="author"><name><surname>Kim</surname><given-names>Jin-Hwan</given-names></name><xref ref-type="aff" rid="Aff6">6</xref></contrib><contrib contrib-type="author"><name><surname>Moon</surname><given-names>Jae Young</given-names></name><xref ref-type="aff" rid="Aff7">7</xref></contrib><contrib contrib-type="author"><name><surname>Choi</surname><given-names>Myung-Sik</given-names></name><xref ref-type="aff" rid="Aff1">1</xref></contrib><contrib contrib-type="author" corresp="yes"><name><surname>Cho</surname><given-names>Nam-Hyuk</given-names></name><address><email>chonh@snu.ac.kr</email></address><xref ref-type="aff" rid="Aff1">1</xref><xref ref-type="aff" rid="Aff2">2</xref><xref ref-type="aff" rid="Aff8">8</xref></contrib><contrib contrib-type="author" corresp="yes"><name><surname>Kim</surname><given-names>Yeon-Sook</given-names></name><address><email>alice@cnuh.co.kr</email></address><xref ref-type="aff" rid="Aff3">3</xref></contrib><aff id="Aff1"><label>1</label><institution-wrap><institution-id institution-id-type="GRID">grid.31501.36</institution-id><institution-id institution-id-type="ISNI">0000 0004 0470 5905</institution-id><institution>Department of Microbiology and Immunology,</institution><institution>Seoul National University College of Medicine,</institution></institution-wrap>Seoul Republic of Korea</aff><aff id="Aff2"><label>2</label><institution-wrap><institution-id institution-id-type="GRID">grid.31501.36</institution-id><institution-id institution-id-type="ISNI">0000 0004 0470 5905</institution-id><institution>Department of Biomedical Sciences,</institution><institution>Seoul National University College of Medicine,</institution></institution-wrap>Seoul Republic of Korea</aff><aff id="Aff3"><label>3</label><institution-wrap><institution-id institution-id-type="GRID">grid.254230.2</institution-id><institution-id institution-id-type="ISNI">0000 0001 0722 6377</institution-id><institution>Division of Infectious Diseases, Department of Internal Medicine,</institution><institution>Chungnam National University School of Medicine,</institution></institution-wrap>Daejeon, Republic of Korea</aff><aff id="Aff4"><label>4</label><institution-wrap><institution-id institution-id-type="GRID">grid.31501.36</institution-id><institution-id institution-id-type="ISNI">0000 0004 0470 5905</institution-id><institution>Cancer Research Institute, Seoul National University College of Medicine,</institution></institution-wrap>Seoul Republic of Korea</aff><aff id="Aff5"><label>5</label><institution-wrap><institution-id institution-id-type="GRID">grid.289247.2</institution-id><institution-id institution-id-type="ISNI">0000 0001 2171 7818</institution-id><institution>Department of Pharmaceutical Science,</institution><institution>College of Pharmacy, Kyung Hee University,</institution></institution-wrap>Seoul Republic of Korea</aff><aff id="Aff6"><label>6</label><institution-wrap><institution-id institution-id-type="GRID">grid.254230.2</institution-id><institution-id institution-id-type="ISNI">0000 0001 0722 6377</institution-id><institution>Department of Radiology,</institution><institution>Chungnam National University School of Medicine,</institution></institution-wrap>Daejeon, Republic of Korea</aff><aff id="Aff7"><label>7</label><institution-wrap><institution-id institution-id-type="GRID">grid.254230.2</institution-id><institution-id institution-id-type="ISNI">0000 0001 0722 6377</institution-id><institution>Division of Pulmonology and Critical Care Medicine, Department of Internal Medicine,</institution><institution>Chungnam National University School of Medicine,</institution></institution-wrap>Daejeon, Republic of Korea</aff><aff id="Aff8"><label>8</label><institution-wrap><institution-id institution-id-type="GRID">grid.31501.36</institution-id><institution-id institution-id-type="ISNI">0000 0004 0470 5905</institution-id><institution>Institute of Endemic Disease, Seoul National University Medical Research Center and Bundang Hospital,</institution></institution-wrap>Seoul Republic of Korea</aff></contrib-group><pub-date pub-type="epub"><day>5</day><month>5</month><year>2016</year></pub-date><pub-date pub-type="pmc-release"><day>5</day><month>5</month><year>2016</year></pub-date><pub-date pub-type="collection"><year>2016</year></pub-date><volume>6</volume><elocation-id>25359</elocation-id><history><date date-type="received"><day>2</day><month>3</month><year>2016</year></date><date date-type="accepted"><day>15</day><month>4</month><year>2016</year></date></history><permissions><copyright-statement>© The Author(s) 2016</copyright-statement><license license-type="OpenAccess"><license-p>This work is licensed under a Creative Commons Attribution 4.0 International License. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in the credit line; if the material is not included under the Creative Commons license, users will need to obtain permission from the license holder to reproduce the material. To view a copy of this license, visit <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 id="Abs1"><p id="Par1">Despite the ongoing spread of MERS, there is limited knowledge of the factors affecting its severity and outcomes. We analyzed clinical data and specimens from fourteen MERS patients treated in a hospital who collectively represent a wide spectrum of disease severity, ranging from mild febrile illness to fatal pneumonia, and classified the patients into four groups based on severity and mortality. Comparative and kinetic analyses revealed that high viral loads, weak antibody responses, and lymphopenia accompanying thrombocytopenia were associated with disease mortality, whereas persistent and gradual increases in lymphocyte responses might be required for effective immunity against MERS-CoV infection. Leukocytosis, primarily due to increased neutrophils and monocytes, was generally observed in more severe and fatal cases. The blood levels of cytokines such as IL-10, IL-15, TGF-β, and EGF were either positively or negatively correlated with disease mortality. Robust induction of various chemokines with differential kinetics was more prominent in patients that recovered from pneumonia than in patients with mild febrile illness or deceased patients. The correlation of the virological and immunological responses with disease severity and mortality, as well as their responses to current antiviral therapy, may have prognostic significance during the early phase of MERS.</p><sec><title>Supplementary information</title><p>The online version of this article (doi:10.1038/srep25359) contains supplementary material, which is available to authorized users.</p></sec></abstract><kwd-group kwd-group-type="npg-subject"><title>Subject terms</title><kwd>SARS virus</kwd><kwd>Viral host response</kwd></kwd-group><custom-meta-group><custom-meta><meta-name>issue-copyright-statement</meta-name><meta-value>© The Author(s) 2016</meta-value></custom-meta></custom-meta-group></article-meta></front><body><sec id="Sec1"><title>Introduction</title><p id="Par2">The Middle East respiratory syndrome coronavirus (MERS-CoV) is an emerging zoonotic pathogen that causes acute and severe respiratory illness with a high mortality rate<sup><xref ref-type="bibr" rid="CR1">1</xref></sup>. Since 2012, more than 1,600 patients have been reported and the mortality rate approaches 35%<sup><xref ref-type="bibr" rid="CR2">2</xref></sup>. Primary transmission of MERS-CoV might be mediated by close contact between humans and infected animal reservoirs such as camels<sup><xref ref-type="bibr" rid="CR3">3</xref>,<xref ref-type="bibr" rid="CR4">4</xref></sup>. However, in Middle Eastern countries, most MERS cases are associated with human-to-human spread starting in healthcare settings that then spark sporadic outbreaks<sup><xref ref-type="bibr" rid="CR5">5</xref></sup>. An unexpected large outbreak in South Korea (186 confirmed cases with 38 deaths), initiated by an infected traveler from the Arabian peninsula, was also attributed to nosocomial infections<sup><xref ref-type="bibr" rid="CR6">6</xref></sup> and highlights our limited knowledge of this emerging infectious disease<sup><xref ref-type="bibr" rid="CR7">7</xref></sup>.</p><p id="Par3">The major symptoms of MERS cases are acute viral pneumonia often associated with extrapulmonary manifestations such as enteric illness<sup><xref ref-type="bibr" rid="CR5">5</xref></sup>. Patients infected with MERS-CoV present with a wide range of clinical severity varying from asymptomatic to severe pneumonia with respiratory failure<sup><xref ref-type="bibr" rid="CR5">5</xref></sup>. Mortality mainly results from acute respiratory distress syndrome (ARDS)<sup><xref ref-type="bibr" rid="CR4">4</xref>,<xref ref-type="bibr" rid="CR5">5</xref>,<xref ref-type="bibr" rid="CR8">8</xref></sup>. Currently, the pathogenesis of the pulmonary and extrapulmonary manifestations of MERS remains poorly defined and knowledge of factors affecting disease severity is limited, although underlying illness, older age, and high viral loads are associated with poorer outcomes<sup><xref ref-type="bibr" rid="CR5">5</xref>,<xref ref-type="bibr" rid="CR8">8</xref>,<xref ref-type="bibr" rid="CR9">9</xref>,<xref ref-type="bibr" rid="CR10">10</xref></sup>.</p><p id="Par4">Since the outbreak of MERS in South Korea was initiated by an infected person, the clinical courses and epidemiological features, including exposure periods, are well documented for most cases<sup><xref ref-type="bibr" rid="CR6">6</xref>,<xref ref-type="bibr" rid="CR11">11</xref></sup>. Most patients that developed respiratory illness received a combined antiviral therapy composed of pegylated interferon (IFN)-α, ribavirin, and lopinavir/ritonavir, a treatment with unknown efficacy<sup><xref ref-type="bibr" rid="CR12">12</xref>,<xref ref-type="bibr" rid="CR13">13</xref></sup>. We sought to identify the factors dictating disease severity and the outcomes of patients treated with antiviral regimens. Here, we retrospectively analyzed clinical data from fourteen hospitalized MERS patients who collectively represent a wide spectrum of disease severity, ranging from mild febrile illness to fatal pneumonia. In addition, we investigated virological and immunological features of the patients using clinical samples acquired during various stages of MERS progression. Comparative and kinetic analyses may provide valuable insight into the critical factors affecting disease progression and severity as well as the underlying mechanisms contributing to MERS pathogenesis.</p></sec><sec id="Sec2"><title>Results</title><sec id="Sec3"><title>Clinical characteristics of MERS-CoV patientss</title><p id="Par5">We reviewed all available clinical and laboratory data of fourteen patients treated in a hospital during the MERS outbreak. The patients were classified into four groups based on the severity and mortality (<xref rid="Tab1" ref-type="table">Table 1</xref>, <xref rid="MOESM197" ref-type="media">Supplementary Fig. S1</xref>, and <xref rid="MOESM197" ref-type="media">Supplementary Table S1</xref>). Group I patients includes two patients who only developed fever and recovered without developing pneumonia. They recovered without any treatment. Group II includes three patients (P03–P05) who developed mild pneumonia without hypoxemia (<xref rid="Tab1" ref-type="table">Table 1</xref> and <xref rid="MOESM197" ref-type="media">Supplementary Table S1</xref>). P04 and P05 showed elevated C-reactive protein (CRP, >3 mg/dl) and P05 had elevated levels of aspartate aminotransferase (AST), alanine aminotransferase (ALT), and lactate dehydrogenase (LDH) (<xref rid="MOESM197" ref-type="media">Supplementary Table S1</xref>). Four patients (P06–P09) recovered from more prolonged and severe pneumonia, and are classified as group III. Severe pneumonia was defined as pneumonia severity index (PSI) ≥ 60 at initial presentation (<xref rid="Tab1" ref-type="table">Table 1</xref>). All patients in this group exhibited elevated liver enzymes and proteinuria during the acute phase. Among them, P09 had pneumonia, rapidly progressing to respiratory failure, and required mechanical ventilation (MV) and extracorporeal membrane oxygenation (ECMO). She also received convalescent plasma therapy twice on days 10 and 16 after symptom onset (<xref rid="MOESM197" ref-type="media">Supplementary Fig. 1</xref>). Group IV includes five fatal cases (P10–P14). All group IV patients suffered from severe pneumonia and ARDS requiring high flow nasal cannula and/or mechanical ventilation. The deceased patients were older than 60, except for P11, and had underlying illnesses, except for P10. P11 had decompensated liver cirrhosis and poorly controlled blood glucose levels before MERS-CoV infection. P12 was diagnosed with active pulmonary tuberculosis about one week before he encountered a MERS-CoV infected patient. He developed pneumonia two days after the onset of fever and progressed to ARDS within a week. P13 and P14 had comorbidities including chronic pulmonary obstructive disease (COPD) and asthma. They were infected with MERS-CoV while being treated for an acute exacerbation of their pulmonary diseases. They died within 2 weeks after symptom onset despite mechanical ventilation.<table-wrap id="Tab1"><label>Table 1</label><caption><p>Clinical characteristics of MERS patients included in this study.</p></caption><table frame="hsides" rules="groups"><thead><tr><th align="center" colspan="2">Group</th><th align="center">Patient’s ID.</th><th align="center">Age</th><th align="center">Sex</th><th align="center">Underlying diseases <sup>*</sup></th><th align="center">Incubation period (days)</th><th align="center">Fever onset to pneumonia (days)</th><th align="center">Severity of Pneumonia (PSI) <sup>**</sup></th><th align="center">Anti-viral therapy (days) <sup>***</sup></th><th align="center">Defervescence after the therapy (days) <sup>****</sup></th><th align="center">O<sub>2</sub> therapy (days) <sup>*****</sup></th></tr></thead><tbody><tr><td valign="middle" rowspan="9">Recovered</td><td valign="middle" rowspan="2">G I</td><td align="center">P01</td><td>65</td><td>F</td><td>–</td><td>18</td><td>–</td><td>–</td><td>–</td><td>–</td><td>–</td></tr><tr><td align="center">P02</td><td>66</td><td>F</td><td>–</td><td>12</td><td>–</td><td>–</td><td>–</td><td>–</td><td>–</td></tr><tr><td valign="middle" rowspan="3">G II</td><td align="center">P03</td><td>39</td><td>F</td><td>–</td><td>8</td><td>3</td><td>29</td><td>12</td><td>3</td><td>–</td></tr><tr><td align="center">P04</td><td>55</td><td>F</td><td>–</td><td>10</td><td>4</td><td>45</td><td>14</td><td>5</td><td>–</td></tr><tr><td align="center">P05</td><td>57</td><td>F</td><td>–</td><td>9</td><td>4</td><td>47</td><td>14</td><td>9</td><td>–</td></tr><tr><td valign="middle" rowspan="4">G III</td><td align="center">P06</td><td>60</td><td>M</td><td>–</td><td>5</td><td>4</td><td>60</td><td>19</td><td>19</td><td>–</td></tr><tr><td align="center">P07</td><td>63</td><td>F</td><td>–</td><td>6</td><td>5</td><td>63</td><td>14</td><td>10</td><td>NP (1)</td></tr><tr><td align="center">P08</td><td>41</td><td>M</td><td>FAP</td><td>4</td><td>2</td><td>71</td><td>7</td><td>2</td><td>NP (1)</td></tr><tr><td align="center">P09</td><td>61</td><td>F</td><td>–</td><td>14</td><td>6</td><td>71</td><td>14</td><td>10</td><td>MV/ECMO (14/7)</td></tr><tr><td valign="middle" rowspan="5">Deceased</td><td valign="middle" rowspan="5">G IV</td><td align="center">P10</td><td>82</td><td>F</td><td>–</td><td>5</td><td>7</td><td>102</td><td>11</td><td>N.D.</td><td>HFNC (3)</td></tr><tr><td align="center">P11</td><td>49</td><td>M</td><td>Cirrhosis, DM</td><td>4</td><td>7</td><td>119</td><td>10</td><td>N.D.</td><td>HFNC (2)</td></tr><tr><td align="center">P12</td><td>69</td><td>M</td><td>TB</td><td>3</td><td>5</td><td>119</td><td>11</td><td>N.D.</td><td>MV (5)</td></tr><tr><td align="center">P13</td><td>74</td><td>M</td><td>COPD</td><td>2</td><td>2</td><td>144</td><td>11</td><td>N.D.</td><td>MV (7)</td></tr><tr><td align="center">P14</td><td>78</td><td>M</td><td>COPD, Asthma, DM</td><td>2</td><td>3</td><td>148</td><td>10</td><td>4</td><td>MV (4)</td></tr></tbody></table><table-wrap-foot><p><sup>*</sup>FAP: Familial adenomatous polyposis, DM: Diabetes mellitus, COPD: Chronic obstructive pulmonary disease, TB: Tuberculosis.</p><p><sup>**</sup>PSI: Pneumonia severity index at initial presentation.</p><p><sup>***</sup>Anti–viral therapy: combined therapy composed of pegylated interferon (IFN)-alpha 2a, ribavirin, and lopinavir/ritonavir (see details in <xref rid="MOESM197" ref-type="media">Supplementary Table S2</xref>).</p><p><sup>****</sup>N.D.: No defervescence.</p><p><sup>*****</sup>NP: nasal prong, HFNC: high flow nasal cannula, MV: mechanical ventilation, ECMO: extracorporeal membrane oxygenation.</p></table-wrap-foot></table-wrap></p><p id="Par6">All the patients with pneumonia were treated with anti-viral drugs (<xref rid="MOESM197" ref-type="media">Supplementary Table S2</xref>) and examined daily by chest X-rays until the resolution of pneumonia. Representative radiologic findings of MERS patents with pneumonia are shown in <xref rid="Fig1" ref-type="fig">Fig. 1</xref>. Patients with pneumonia almost always showed ground-glass opacity or airspace consolidation involving either or both sides of lower lung fields. Chest computed tomography (CT) was performed on P08 and his chest CT scans revealed lobar consolidation in right lower lobe and segmental infiltration in the left upper lobe. Patients in group II showed more rapid clearing of pneumonic infiltrates compared to patients in group III.<fig id="Fig1"><label>Figure 1</label><caption><title>Representative chest images of the MERS patients.</title><p>Chest images of the MERS patients suffered from mild (P05) or severe pneumonia (P08 and P13) were presented. P05 and P08 were recovered from the pneumonia whereas P13 died due to ARDS. Images were taken at the indicated days after symptom onset. Paired chest radiographs and computed tomography (CT) scans were performed on the same day in P08. Initial chest radiographs shows patchy consolidation along with ground-glass opacities involving unilateral or both lung zones. Follow-up frontal chest radiographs and CT scan (P08) obtained in acute phase show progression in density and extent in all three patients. Chest radiographs taken in convalescent stage show improvement in survived patients (P05 and P08) whereas that of P13 shows progression with bilateral extensive consolidation in both lung zones.</p></caption><graphic xlink:href="41598_2016_Article_BFsrep25359_Fig1_HTML" id="d29e1064"></graphic></fig></p></sec><sec id="Sec4"><title>Kinetics of viral shedding from respiratory secretions and plasma</title><p id="Par7">Since the lower respiratory samples had higher viral loads and showed more sustained viral release than upper respiratory secretions<sup><xref ref-type="bibr" rid="CR14">14</xref>,<xref ref-type="bibr" rid="CR15">15</xref></sup>, we primarily measured viral loads in lower respiratory secretions such as sputa and tracheal aspirates (<xref rid="Fig2" ref-type="fig">Fig. 2</xref>). Patient P01 secreted 1.5–1.7 × 10<sup>6</sup> virus copies/ml in the sputa during the first week and P02 shed a similar level (3.1–6.7 × 10<sup>6</sup> copies/ml) of virions up to ten days after fever onset. No viremia was observed in P01, but a transient viremia (8.9 × 10<sup>3</sup> copies/ml) occurred in P02 on day 5. In group II patients with mild pneumonia, viral shedding (1.6 × 10<sup>6</sup> to 6.5 × 10<sup>8</sup> copies/ml, average = 3.5 × 10<sup>7</sup> copies/ml) was detected in sputa up to ten days after symptom onset. Viremia (average = 2.2 × 10<sup>4</sup> copies/ml) was observed in P03 and P05 until ten and thirteen days, respectively, whereas P04 had no viremia. Since P05 complained of severe headache and nausea from day 12 to 13<sup><xref ref-type="bibr" rid="CR16">16</xref>,<xref ref-type="bibr" rid="CR17">17</xref></sup>, cerebrospinal fluid (CSF) was collected and examined for inflammatory signs and viremia, but we detected no evidence of CNS infection. Viral shedding from group II patients stopped after initiation of antiviral therapy. In group III patients who suffered from more severe pneumonia, viral secretion in the lower respiratory tract was more sustained, continuing for up to 18 to 27 days following the onset of symptoms. In addition, viremia was detected in serum samples for up to 34 days as in the case of P08. Viral shedding ceased during antiviral therapy in two patients (P07 and P09), whereas viremia continued in all patients. Initial viral loads in respiratory secretions during the second week ranged from 3.9 × 10<sup>4</sup> to 2.4 × 10<sup>9</sup> copies/ml. However, the average viral load in plasma was around 1.1 × 10<sup>4</sup> copies/ml, similar to group II patients. In the case of P09 who received convalescent-phase plasma twice, viral loads in respiratory secretions increased slightly and the level of viremia remained virtually unchanged until day 18. Viral loads in lower respiratory secretions from the fatal cases (group IV) were relatively higher (5.0 × 10<sup>8</sup> to 1.4 × 10<sup>9</sup> copies/ml, average = 6.3 × 10<sup>8</sup> copies/ml) than survivors. Viremia (average = 3.2 × 10<sup>4</sup> copies/ml) was also sustained during antiviral therapy in group IV cases.<fig id="Fig2"><label>Figure 2</label><caption><title>Kinetic viral loads in respiratory secretions and blood of MERS patients.</title><p>Changes of average viral loads in respiratory and plasma samples are presented. The patients were classified into group I ~ IV (G I ~ IV) based on disease severity and mortality as described in the text. Gray boxes indicate the average periods of antiviral therapy administered to the patients of each group. P09 in group III received convalescent plasma therapy twice on days 10 and 16 after symptom onset.</p></caption><graphic xlink:href="41598_2016_Article_BFsrep25359_Fig2_HTML" id="d29e1142"></graphic></fig></p></sec><sec id="Sec5"><title>Kinetic responses of serum IgG and secretory IgA in respiratory samples</title><p id="Par8">Antibody responses against spike (S1) antigen were measured by ELISA and compared among the four groups. Gradual increases of S1-specific serum IgG were observed in all the recovered patients regardless of disease severity, whereas serum IgG responses were generally static until the second week in the lethal patients (<xref rid="Fig3" ref-type="fig">Fig. 3</xref>). P09 who had a long incubation period (~14 days) showed decreased antibody responses after passive plasma therapy even though she showed the highest IgG response among the patients at day 7. The effect of antiviral therapy on IgG responses is not clear.<fig id="Fig3"><label>Figure 3</label><caption><title>Kinetic responses of serum IgG and respiratory IgA antibody in MERS patients.</title><p>Serum IgG and secretory IgA specific to spike (S1) antigen in respiratory samples were measured by ELISA. Definition of units and normalized OD (nOD) of antibody response are described in the Methods section. Gray boxes indicate the average periods of antiviral therapy administered to the patients of each group. P09 in group III received convalescent plasma therapy twice on days 10 and 16 after symptom onset.</p></caption><graphic xlink:href="41598_2016_Article_BFsrep25359_Fig3_HTML" id="d29e1161"></graphic></fig></p><p id="Par9">We also examined S1-specific secretory IgA responses in respiratory secretions (<xref rid="Fig3" ref-type="fig">Fig. 3</xref> and <xref rid="MOESM197" ref-type="media">Supplementary Fig. S2</xref>). The level of antigen-specific secretory IgA, as measured by relative OD or titers, generally increased up to two to three weeks after symptom onset and then reached steady state or declined in all the recovered patients. Notably, secretory IgA titers of group III patients were relatively higher than mild cases during the second and third week. Among the deceased patients, three patients (P10, 12, and 14) developed detectable secretory IgA during the second or third week, whereas P13 failed to produce the specific IgA until day 10.</p><p id="Par10">The levels of S1-specific antibody responses were compared against viral loads in plasma and respiratory secretions (<xref rid="Fig4" ref-type="fig">Fig. 4</xref>). The level of serum IgG was inversely correlated with viral loads in both plasma and respiratory secretions although these did not reach statistical significance. Respiratory viral loads were also negatively correlated with secretory IgA levels without statistical significance. Secretory IgA did not show any negative correlation with viral loads in plasma. The consistently high viral loads in the clinical samples even in the presence of specific antibodies suggest that the early antibody responses induced in systemic and mucosal immune systems may not provide sufficient protective immunity against MERS-CoV replication. Nevertheless, since we measured viral nucleic acid levels rather than infectious viral titers in the clinical samples, we cannot exclude the possibility that viral infectivity is lower due to opsonization by antiviral antibodies.<fig id="Fig4"><label>Figure 4</label><caption><title>Correlation of antibody responses and viral loads.</title><p>The level of antibody and viral loads in the same sample were plotted. Statistical analysis was performed by linear regression assay as described in Materials and Methods.</p></caption><graphic xlink:href="41598_2016_Article_BFsrep25359_Fig4_HTML" id="d29e1185"></graphic></fig></p></sec><sec id="Sec6"><title>Kinetic responses of white blood cells and platelets</title><p id="Par11">Hematological changes during the course of MERS were examined in all the patients (<xref rid="Fig5" ref-type="fig">Fig. 5</xref>, <xref rid="MOESM197" ref-type="media">Supplementary Table S3</xref>). In group I patients, there were no significant abnormalities observed in leukocytes counts and absolute counts remained within the normal range. We did note a gradual increase of lymphocytes and platelets up to 2 week after symptom onset. The gradual rise in lymphocyte and platelet counts was also observed in group II patients up to 2 ~ 3 weeks after symptom onset. P03 also showed a transient rise in neutrophil counts during the second week. Transient or persistent leukocytosis, primarily due to increased neutrophils, was observed in P06, P08, and P09 among group III patients. Monocyte counts also rose rapidly in P08 and P09 during the second and third week, but returned to basal levels thereafter. Thus, all the recovered patients exhibited a gradual increase in lymphocyte counts, suggesting that lymphocyte responses may be correlated with disease resolution. Among the five lethal cases, neutrophilia (>8,000 cell/μl) was observed in P12 and P13. Early increases of lymphocyte counts occurred in all the group IV patients except P14, however, they suffered from lymphopenia (<1,500 cells/μl) and thrombocytopenia (<140 × 10<sup>3</sup>/μl) during antiviral therapy. Slight increases in monocyte counts were detected in P11, P12, and P13 during treatment.<fig id="Fig5"><label>Figure 5</label><caption><title>Kinetic responses of leukocyte subsets and platelets in MERS patients.</title><p>The changes in absolute counts (×10<sup>3</sup> cells/μL) of the indicated subset of leukocytes and platelets are presented. Gray boxes indicate the average periods of antiviral therapy administered to the patients of each group.</p></caption><graphic xlink:href="41598_2016_Article_BFsrep25359_Fig5_HTML" id="d29e1213"></graphic></fig></p></sec><sec id="Sec7"><title>Kinetic responses of cytokines and chemokines</title><p id="Par12">Prominent and differential changes in the white blood cells prompted us to measure the cytokines and chemokines in the patients’ plasma. We measured 39 cytokines, chemokines, and growth factors at different time points (<xref rid="MOESM197" ref-type="media">Supplementary Table S4</xref>). IFN-α was substantially elevated in most of the patients and peaked during the second week after symptom onset (<xref rid="MOESM197" ref-type="media">Fig. S3</xref>). Since all group II ~ IV patients received pegylated IFN-α, the elevation of the cytokines may be primarily attributed to a response to therapy. G-CSF and GM-CSF, which stimulate the bone marrow to produce granulocytes and monocytes, were also upregulated in the patients (<xref rid="Fig6" ref-type="fig">Fig. 6</xref>. and <xref rid="MOESM197" ref-type="media">Supplementary Fig. S4</xref>). Moreover, G-CSF rapidly increased but patients who died had relatively poor GM-CSF responses during antiviral treatment. We also measured several pro- or anti- inflammatory cytokines such as IL-1, TNF-α, IL-6, IL-10, and TGF-β in the patients’ plasma (<xref rid="MOESM197" ref-type="media">Supplementary Table S4</xref> and <xref rid="Fig6" ref-type="fig">Fig. 6</xref>). Most of the patients with pneumonia had relative elevations of these cytokines during the second and third week. Some cytokines, such as IL-6 and IL-10, were generally higher in severe (group III) and fatal cases (group IV) than in mild cases (group I and II) (<xref rid="Fig6" ref-type="fig">Fig. 6</xref>). It is also interesting to note that TGF-β responses were prominent only in group I and group III patients but barely detected in group II and group IV patients (<xref rid="Fig6" ref-type="fig">Fig. 6</xref>). Robust induction of diverse chemokines including Fractalkine, MCP-1 (CCL2), IP-10 (CXCL10), MDC (CCL22), RANTES (CCL5), IL-8 (CXCL8), MIP-1 (CCL3), Eotaxin (CCL11), and GRO (CXCL1) were observed in most of the patients although the their levels and expression kinetics were quite variable (<xref rid="MOESM197" ref-type="media">Supplementary Table S4</xref> and <xref rid="Fig7" ref-type="fig">Fig. 7</xref>). Transient upregulation of IL-8 and MCP-3 (CCL7) was more prominent in group II and III patients than group I and IV patients. IP-10 was significantly higher in pneumonia patients (group II ~IV) than group I patients. Production of IP-10 generally waned during treatment periods in patients that recovered from pneumonia (group II and III). Expression of MIP-1β was also highly induced in group II and III patients but with differential kinetics. In group II, MIP-1β was elevated during treatment periods but increased in three group III patients (P06, P07, and P08) after antiviral therapy (<xref rid="Fig7" ref-type="fig">Fig. 7</xref>). This chemokine was barely induced in the lethal patients (group IV) except P14. Induction of GRO also showed similar kinetics as MIP-1β (<xref rid="Fig7" ref-type="fig">Fig. 7</xref>). Robust induction of MCP-1, MDC, IP-10, and Fractalkine, which recruit monocytes and/or T cells to inflamed tissues, may contribute to inflammatory responses and/or viral clearance in the lungs. In addition, chemokines such as IL-8, MIP-1, and GRO, may help recruit neutrophils and induce the infiltration of immune cells into infected lung tissues during viral pneumonia. The induction of RANTES and Eotaxin, which recruit eosinophils and/or basophils, was detected in all the patients, suggesting a potential role of these innate immune cells in lung inflammation in MERS patients (<xref rid="MOESM197" ref-type="media">Supplementary Table S4</xref> and <xref rid="Fig7" ref-type="fig">Fig. 7</xref>).<fig id="Fig6"><label>Figure 6</label><caption><title>Kinetic responses of cytokines in MERS patients.</title><p>Among the 39 cytokines and chemokines analyzed, kinetic changes of five representative cytokines that showed differences in the level and/or kinetics among the patients of different groups, are presented. Gray boxes indicate the average periods of antiviral therapy administered to the patients of each group. The concentrations of the cytokines are presented in pg/ml except TGF-β (ng/ml). *: data point is out of y-axis range.</p></caption><graphic xlink:href="41598_2016_Article_BFsrep25359_Fig6_HTML" id="d29e1273"></graphic></fig><fig id="Fig7"><label>Figure 7</label><caption><title>Kinetic responses of chemokines in MERS patients.</title><p>Among the 39 cytokines and chemokines analyzed, kinetic changes of five representative chemokines that showed differences in the level and/or kinetics among the patients of different groups, are presented. Gray boxes indicate the average periods of antiviral therapy administered to the patients of each group. The concentrations of IL-8, GRO, and IP-10 are presented in ng/ml and those of RANTES and MIP-1β in pg/ml.</p></caption><graphic xlink:href="41598_2016_Article_BFsrep25359_Fig7_HTML" id="d29e1284"></graphic></fig></p><p id="Par13">Cytokines (IL-2, IL-4, IL-5, IL-7, IL-9, IL-12, IL-15, IL-17 A, and IFN-γ) regulating T cell homeostasis and functional responses were detected only in some patients and none of the cytokines seem to be correlated with disease severity or mortality (<xref rid="MOESM197" ref-type="media">Supplementary Table S4</xref> and <xref rid="MOESM197" ref-type="media">Supplementary Fig. S3</xref>). IFN-γ, a key cytokine involved in the activation of Th1 cells, was consistently observed in most patients during the first and second weeks after symptom onset. Interestingly, two cytokines, IL-7 and IL-15, regulating T cell homeostasis <sup><xref ref-type="bibr" rid="CR18">18</xref></sup>, were substantially increased in most patients. In particular, IL-15 responses were significantly higher in pneumonia patients (except P12) than group I patients (<xref rid="MOESM197" ref-type="media">Supplementary Fig. S4</xref>).</p><p id="Par14">Soluble CD40 ligand (sCD40L) was also increased in the patients’ plasma (<xref rid="Fig6" ref-type="fig">Fig. 6</xref>). Since sCD40L has a cytokine-like activity in inflammatory responses and is primarily produced by activated platelets<sup><xref ref-type="bibr" rid="CR19">19</xref></sup>, the level of this serum protein may reflect platelet activity during MERS progression. Indeed, the kinetic responses of sCD40L remained suppressed among group IV patients who suffered from thrombocytopenia (<xref rid="Fig5" ref-type="fig">Fig. 5</xref>).</p><p id="Par15">Several growth factors such as EGF, FGF-2, VEGF, and TGF-α were also significantly elevated in the plasma of MERS patients (<xref rid="MOESM197" ref-type="media">Supplementary Table S4</xref> and <xref rid="MOESM197" ref-type="media">Supplementary Fig. S3</xref>). It is interesting to note that the level of EGF was significantly higher in the recovered patients compared to fatal cases, whereas the level of TGF-α was generally higher in the patients that suffered from severe pneumonia compared to mild cases. Previously, it was shown that EGF has a protective effect on gastrointestinal insults by porcine epidemic diarrhea virus (PEDV), a member of Coronavirus family, potentially via promoting the recovery of damaged mucosal epithelium<sup><xref ref-type="bibr" rid="CR20">20</xref></sup>.</p></sec><sec id="Sec8"><title>Statistical analysis of virological and immunological factors associated with mortality</title><p id="Par16">The hazard ratios (HR) of mortality according to the levels of various virological and immunological factors are shown in <xref rid="MOESM197" ref-type="media">Supplementary Table S5</xref>. Overall, patients with higher antibody responses (especially respiratory IgA) and lymphocyte responses, as well as lower leukocyte and neutrophil counts, had significantly lower hazard ratios for mortality after MERS-CoV infection although the hazards ratio of white blood cell counts is very limited (IgA (nOD), HR = 0.082, 95% CI = 0.007–1.002; leukocytes counts, HR = 1.0005, 95% CI = 1.0001–1.0008; neutrophil counts, HR = 1.0005, 95% CI = 1.0001–1.0009; lymphocytes counts, HR = 0.9954, 95% CI = 0.9909–0.9999). Regarding cytokines, chemokines, and growth factors, patients with higher levels of IL-10 and IL-15 as well as lower levels of TGF-β, RANTES, and EFG had higher hazard ratios for mortality, which were marginally significant after adjusting for age (IL-10, HR = 1.013, 95% CI = 1.002–1.024; IL-15, HR = 1.146, 95% CI = 1.022–1.287; TGF-β, HR = 0.876, 95% CI = 0.770–0.998; RANTES, HR = 0.900, 95% CI = 0.780–1.015; EGF, HR = 0.9633, 95% CI = 0.9303–0.9974).</p><p id="Par17">In addition to virological and immunological factors, patients’ gender and comorbidities seem to be associated with mortality and morbidity. Although the association of gender on mortality was not statistically significant (<italic>p</italic> = 0.071) potentially due to limited patient numbers, it is worth nothing that two-thirds of patients in the severe disease groups (group III and IV) were men and all the patients in the mild disease groups (group I and II) were women. The presence of chronic underlying illness before MERS-CoV exposure, as well as age (<italic>p</italic> = 0.002 tested by Log-rank test), was significantly associated with mortality. These findings are consistent with other case series as reviewed previously<sup><xref ref-type="bibr" rid="CR1">1</xref></sup>.</p></sec></sec><sec id="Sec9"><title>Discussion</title><p id="Par18">The rapid and wide spread of MERS-CoV infection in South Korea during the outbreak had a disastrous impact on the whole country and highlights our limited knowledge on MERS. However, most Korean MERS cases reported had well documented transmission routes and exposed periods, enabling us to finely characterize disease progression in infected patients. In this study, we systemically analyzed clinical, virological, and immunological responses in a group of patients that collectively represent a broad spectrum of MERS severity, from mild febrile to fatal. Although the number of patients included in this study is limited, our data help more clearly delineate MERS progression in humans, and also provide scientific basis for better preventive measures. In addition, the observed responses of multiple factors and their association with disease severity during therapeutic periods might help us develop proper strategies to improve the efficacy of current MERS treatments.</p><p id="Par19">The fourteen patients could be readily classified into four clinical groups based on disease severity and mortality. Group I patients (14.2%, 2/14) produced MERS-CoV (1.5 ~ 6.7 × 10<sup>6</sup> copies/ml) in sputa up to 10 days after fever onset. Considering their long incubation periods (12 and 18 days) viral shedding may precede the onset of fever. Therefore, early diagnosis and quarantine of persons who have had contact with MERS patients may be required to prevent MERS-CoV spread, even if they are asymptomatic or have mild symptoms. Since secretory IgA specific to spike antigen increased in the respiratory tract for up to 10 days after symptom onset, MERS-CoV specific mucosal antibody responses may be a potential diagnostic biomarker in mild cases early in the disease course.</p><p id="Par20">Among the patients that developed pneumonia but completely recovered from MERS (50.0%, 7/14), effective viral clearance was achieved with antiviral therapy only in group II patients (21.4%, 3/14), whereas sustained viral secretion was observed, especially in blood, in group III patients (28.6%, 4/14) even following antiviral therapy. Considering that viral shedding was poorly controlled in the fatal cases (35.7%, 5/14), it is possible that only a limited proportion of MERS patients responded to the current antiviral regimen <sup><xref ref-type="bibr" rid="CR12">12</xref></sup>. The MERS-CoV receptor, dipeptidylpeptidase 4 (DPP4), is expressed in greater abundance in the lung parenchyma (alveolar type I and II cells, macrophages and vascular endothelia) than in the upper airways and conducting airway epithelia<sup><xref ref-type="bibr" rid="CR21">21</xref></sup>. In addition, DPP4 expression is inducible and may increase in some chronic disease conditions<sup><xref ref-type="bibr" rid="CR21">21</xref></sup>. We speculate that the higher respiratory tract virus shedding observed in the more severe and fatal cases may reflect both the normal distribution of DPP4 and increases in receptor abundance associated with chronic disease states.</p><p id="Par21">Most of the patients developed virus-specific serum IgG and secretory IgA in the respiratory tract except one fatal case (P13) who failed to develop secretory IgA. Consistent with a recent report<sup><xref ref-type="bibr" rid="CR14">14</xref></sup>, the antibody responses in the blood as well as in the respiratory tract of survivors were more sustained and elevated than in fatal cases. Although we did not measure the neutralizing activity of the antibody responses, it was reported that the specific ELISA values are generally correlated with neutralizing antibody titers<sup><xref ref-type="bibr" rid="CR14">14</xref>,<xref ref-type="bibr" rid="CR22">22</xref></sup>. Nevertheless, viral shedding was detected in the presence of specific antibody responses, suggesting a weak protective effect against viral replication during primary MERS-CoV infection<sup><xref ref-type="bibr" rid="CR14">14</xref></sup>. The patient who received convalescent-phase plasma (P09), showed no significant changes in blood and respiratory tract viral loads during the subsequent several days following treatment (<xref rid="Fig2" ref-type="fig">Fig. 2</xref>). Rather, serum IgG responses rapidly dropped after plasma therapy (<xref rid="Fig3" ref-type="fig">Fig. 3</xref>). Although we could not explain these unexpected responses, they are consistent with a report that a Korean patient given plasma therapy showed more delayed antibody responses in the days following treatment compared to other patients<sup><xref ref-type="bibr" rid="CR22">22</xref></sup>. Although a more systematic study of patients receiving plasma therapy is needed, our findings suggest that passive antibody transfer may have limited efficacy. A previous report on plasma therapy in SARS patients showed that benefit was achieved only in a subset of patients when administered within 14 days after the onset of illness<sup><xref ref-type="bibr" rid="CR23">23</xref></sup>.</p><p id="Par22">One of the most prominent factors associated with MERS disease severity and outcome was the hematological changes in leukocyte populations (<xref rid="Fig5" ref-type="fig">Fig. 5</xref>). Gradual and persistent increases of lymphocyte counts during MERS progression was observed in all the survivors, whereas all the deceased patients showed rapid drops of lymphocyte counts during the second week, resulting in lymphopenia. In contrast, lymphocyte counts rapidly increased up to 10 days after symptom onset in group I patients and one group II patient (P04), strongly suggesting that adaptive immune responses play a protective role. In most patients that recovered from pneumonia (groups II and III), the kinetics of lymphocyte responses were rather delayed but generally correlated with resolution of viral pneumonia. Elevation of chemokines, including MCP-1, IP-10, Fractalkine, and RANTES, which can recruit T lymphocytes, may contribute to cell-mediated antiviral responses in inflamed tissues. Among these, RANTES was rapidly elevated during the first week in group I patients and rather delayed but robustly induced in group II and III patients (<xref rid="Fig7" ref-type="fig">Fig. 7</xref>). The chemokine was also increased in group IV patients but generally weaker than in recovered patients. Increased levels of IFN-γ (<xref rid="MOESM197" ref-type="media">Supplementary Fig. S3</xref>) during the first and second week also support anti-viral T cell responses in the inflamed tissues<sup><xref ref-type="bibr" rid="CR24">24</xref></sup>. Recently, it was shown that cytokines and chemokines are actively expressed in MERS-CoV-infected dendritic cells and macrophages<sup><xref ref-type="bibr" rid="CR25">25</xref>,<xref ref-type="bibr" rid="CR26">26</xref></sup>. Nevertheless, other cytokines associated with the functional activation of specific subsets of T cells were barely detected in our study. Instead, elevations of IL-7 and IL-15 with differential kinetics were noted. An association between elevations of IL-7 and IL-15 and inflammatory pulmonary diseases has been previously reported in humans<sup><xref ref-type="bibr" rid="CR27">27</xref>,<xref ref-type="bibr" rid="CR28">28</xref></sup>, as well as in MERS-CoV infected animals<sup><xref ref-type="bibr" rid="CR29">29</xref></sup>. In addition, leukocytosis characterized by increased neutrophils and monocytes was primarily observed in several group III and IV patients, suggesting that innate immune cell responses rather than anti-viral responses might be responsible for MERS pathogenesis in the lung. Elevations in G-CSF during the second and third week, especially in fatal cases, may account for the observed leukocytosis. Although most of the chemokines involved in the recruitment of neutrophils and monocytes were highly elevated in group II and III patients who suffered from pneumonia, the overall chemokine responses, except MCP-1 and IP-10, were relatively reduced in the fatal cases. In addition, a specific correlation between chemokine levels and disease mortality was not observed. Among the inflammatory cytokines examined, TNF-α and IL-6 levels during the acute phase were generally, but not absolutely, associated with disease severity and mortality<sup><xref ref-type="bibr" rid="CR1">1</xref></sup>, whereas the anti-inflammatory cytokines, IL-10 and TGF-β were significantly correlated with disease mortality (<xref rid="MOESM197" ref-type="media">Supplementary Table S5</xref>). Previously, it was shown that ARDS caused by SARS-CoV infection is associated with the induction of inflammatory cytokines and chemokines such as IL-1, IL-6, IL-8, IP-10, and TNF-α, many of which were highly expressed in the lungs of SARS patients<sup><xref ref-type="bibr" rid="CR30">30</xref></sup>. Interestingly, TGF-β responses were elevated in group I and III patients. Considering that TGF-β is involved in the antibody class switching to IgA<sup><xref ref-type="bibr" rid="CR31">31</xref></sup>, wound healing and scar formation via fibrosis, as well as suppression of adaptive immune responses during lung inflammation<sup><xref ref-type="bibr" rid="CR32">32</xref></sup>, the differential expression of the cytokine in MERS patients might be linked to disease severity and/or protection against the viral infection. Nevertheless, since pre-existing comorbidities, especially in group IV, likely contribute to the observed variation in cytokines and chemokines during MERS progression, we may need to be more careful in interpreting our results and the association of chemokines and cytokines with disease severity and mortality.</p><p id="Par23">In conclusion, we analyzed diverse virological and immunological factors which may affect the severity, progression, and outcome of MERS in a well-defined clinical setting. High viral loads, weak antibody responses, and lymphopenia accompanied by thrombocytopenia were associated with disease mortality, whereas persistent lymphocyte responses might be required for effective immunity against MERS-CoV infection. Leukocytosis primarily due to an increase in neutrophils and monocytes was generally observed in more severe and fatal cases. The blood levels of cytokines such as IL-10, IL-15, TGF-β, and EGF were correlated with disease severity. Robust induction of various chemokines such as IL-8, IP-10, MIP-1, GRO, and RANTES with differential kinetics were more prominent in patients that recovered from pneumonia than in patients with mild febrile illness or deceased patients. Although the number of patients in this study was limited, the correlations between virus shedding and immunological responses with disease severity and mortality, as well as responses to current antiviral therapy, may indicate prognostic significance during the acute phase after symptom onset. Further studies on the functional relationship of these factors with effective immunity and pathogenesis in MERS need to be conducted.</p></sec><sec id="Sec10"><title>Methods</title><sec id="Sec11"><title>Study approval</title><p id="Par24">Clinical data and specimens obtained from the MERS patients were used in this study after ethnical approval granted by the institutional review boards of Chungnam National University Hospital and Seoul National University Hospital. This study was performed in accordance with the ethical standards laid down in the 1964 declaration of Helsinki and all subsequent revisions. All surviving patients provided written, informed consent to participate. In fatal cases, we obtained an exemption of patients’ consent from the institutional review boards for the retrospective analysis of clinical samples.</p></sec><sec id="Sec12"><title>Patients and study design</title><p id="Par25">MERS-CoV infection was confirmed in fourteen patients treated at Chungnam National University Hospital between June 7th and August 5th, 2015 by positive real-time RT-PCR assay targeting the <italic>upE</italic> and <italic>orf1a</italic> sequences at a Korean Center for Disease Control laboratory. We reviewed clinical information and daily findings from history and physical examination, pulse oximetry, and haematological, biochemical, radiological investigations. Clinical specimens collected for viral diagnosis included respiratory secretions, blood, cerebrospinal fluids, and ascitic fluids of MERS patients. These were used for quantification of specific antibodies, subsets of cytokines, and viral loads. Pneumonia severity index (PSI) was used to estimate the severity of pneumonia in each patient as described previously<sup><xref ref-type="bibr" rid="CR33">33</xref></sup>. We classified the patients into four groups based on disease severity and mortality, and performed comparative analysis.</p></sec><sec id="Sec13"><title>Quantitation of viral loads</title><p id="Par26">Total RNA was extracted from respiratory samples, including sputa and tracheal aspirates, and plasma using TRIzol LS reagent (Thermo Fisher Scientific) according to the manufacturer’s instruction. The RNA samples were then used for titration of viral genomes using a quantitative real-time RT-PCR kit (Cosmogenetech Co. and Kogenebiotech) amplifying <italic>orf1a</italic>, <italic>orf1b</italic>, or <italic>upE</italic> sequences<sup><xref ref-type="bibr" rid="CR34">34</xref></sup>. Viral copy numbers were estimated by comparing Ct values of each sample with dilutions of positive control viral cDNAs according to the manufacturer’s instruction (Cosmogenetech Co). In our hands, the detection limit of viral copy numbers was ~10<sup>4</sup> copies/ml when <italic>orf1a</italic> and <italic>orf1b</italic> were targeted and ~10<sup>3</sup> copies/ml when <italic>upE</italic> was used as the target. If triplicate results showed consistently positive reactions, the copy number data were used for kinetic analysis even if they were below detection limit. Otherwise, the data were regarded as negative.</p></sec><sec id="Sec14"><title>Quantitation of specific antibody responses</title><p id="Par27">Specific antibody responses to the MERS-CoV spike protein S1 domain were measured by ELISA, using a recombinant MERS-CoV spike protein S1 domain control<sup><xref ref-type="bibr" rid="CR35">35</xref></sup>, according to the manufacturer’s instruction (Anti-MERS-CoV S1 ELISA kit, Alpha Diagnostic International). Specific IgG responses were determined as unit/ml by comparing the net O.D. value of each plasma sample with calibration standards assayed together in each experimental set (Alpha Diagnostic International). Secretory IgA responses were also semi-quantitated and titrated using serial dilutions of the respiratory samples using the same ELISA kit, with substituting an anti-human IgA-horseradish peroxidase conjugate (SouthernBiotech) as the secondary antibody<sup><xref ref-type="bibr" rid="CR36">36</xref></sup>. Since lower respiratory tract samples such as sputa were difficult to analyze directly, they were processed before performing ELISA as described previously<sup><xref ref-type="bibr" rid="CR37">37</xref></sup>. Due to limited samples, antibody responses were measured at 3 ~7 days interval and all the data obtained were included for kinetic analysis.</p></sec><sec id="Sec15"><title>Quantitation of cytokines and chemokines</title><p id="Par28">Thirty eight cytokines, chemokines, and growth factors were measured in plasma samples using MILLIPLEX MAP 38-plex cytokine assay kit (Millipore) as specified by the manufacturer’s instructions. These included sCD40L, VEGF, TNF-β, TNF-α, TGF-α, MIP-1β, MIP-1α, MDC (CCL22), MCP-3, MCP-1, IP-10, IL-17, IL-15, IL-13, IL-12 (p70), IL-12 (p40), IL-10, IL-9, IL-8, IL-7, IL-6, IL-5, IL-4, IL-3, IL-2, IL-1ra, IL-1β, IL-1α, IFN-γ, IFN-α2, GRO, GM-CSF, G-CSF, Fractalkine, Flt-3 L, FGF-2, Eotaxin, and EGF. RANTES was measured independently using a quantitative ELISA kit (BioLegend). All the samples were measured in duplicate and the mean values were used for analysis.</p></sec><sec id="Sec16"><title>Statistics</title><p id="Par29">All the data from each patient were arranged from date of exposure to an infected patient to the date of death (event, n = 5) or to the date that recovered patients were discharged from the hospital (censored case, n = 9) (<xref rid="MOESM197" ref-type="media">Supplementary Fig. S1</xref>). We performed time-varying analyses of each data value obtained from the patients’ samples. There were total 67 to 103 individual observations, depending on the number of measurements of virological and immunological factors, during 461 observation period. Cox-proportional hazards regression models with the virological and immunological factors entered as time varying covariates were used to calculate crude hazard ratios (HRs) with 95% confidence intervals (CIs) of the factors per 1 unit of mortality. All the factors were treated as continuous variables. Age-adjusted hazard ratios were calculated for every factor. In this study, a <italic>p</italic>-value less than 0.05 (two-tailed) was considered statistically significant. All statistical analyses were performed by Stata (version 12.1; Stata Co.). Statistical analyses of the correlation of antibody responses and viral loads was performed by linear regression assay embedded in GraphPad Prism software (Ver. 5.0).</p></sec></sec><sec id="Sec17"><title>Additional Information</title><p id="Par30"><bold>How to cite this article</bold>: Min, C.-K. <italic>et al</italic>. Comparative and kinetic analysis of viral shedding and immunological responses in MERS patients representing a broad spectrum of disease severity. <italic>Sci. Rep</italic>. <bold>6</bold>, 25359; doi: 10.1038/srep25359 (2016).</p></sec><sec sec-type="supplementary-material"><title>Supplementary information</title><sec id="Sec18"><p><supplementary-material content-type="local-data" id="MOESM197"><media xlink:href="41598_2016_BFsrep25359_MOESM197_ESM.pdf"><caption><p>Supplementary Information (PDF 2202 kb)</p></caption></media></supplementary-material></p></sec></sec></body><back><fn-group><fn><p>Chan-Ki Min, Shinhye Cheon, Na-Young Ha and Kyung Mok Sohn: These authors contributed equally to this work.</p></fn></fn-group><ack><title>Acknowledgements</title><p>We acknowledge Dr. Paul B. McCray, Jr. for editing and comments on the manuscript. This study was supported by grants of the Korea Health Technology R&D Project through the Korea Health Industry Development Institute (KHIDI), funded by the Ministry of Health & Welfare, Republic of Korea (HI15C3034 and HI15C3227).</p></ack><notes notes-type="author-contribution"><title>Author Contributions</title><p>N.-H.C. and Y.-S.K. conceived and designed the experiments. C.-K.M., S.C., N.-Y.H., K.M.S., Y.K., A.A. H.M.S., J.-Y.C., K.-S.I., J.-W.K., J.Y.M. and M.-S.C. analyzed clinical data, performed the experiments and statistical analysis. N.-H.C. and Y.-S.K. analyzed the data and wrote the paper. 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