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Sequence homology between HLA-bound cytomegalovirus and human peptides: A potential trigger for alloreactivity

Identifieur interne : 001B32 ( Ncbi/Merge ); précédent : 001B31; suivant : 001B33

Sequence homology between HLA-bound cytomegalovirus and human peptides: A potential trigger for alloreactivity

Auteurs : Charles E. Hall [États-Unis] ; Vishal N. Koparde [États-Unis] ; Maximilian Jameson-Lee [États-Unis] ; Abdelrhman G. Elnasseh [États-Unis] ; Allison F. Scalora [États-Unis] ; David J. Kobulnicky [États-Unis] ; Myrna G. Serrano [États-Unis] ; Catherine H. Roberts [États-Unis] ; Gregory A. Buck [États-Unis] ; Michael C. Neale [États-Unis] ; Daniel E. Nixon [États-Unis] ; Amir A. Toor [États-Unis]

Source :

RBID : PMC:5553991

Descripteurs français

English descriptors

Abstract

Human cytomegalovirus (hCMV) reactivation may often coincide with the development of graft-versus-host-disease (GVHD) in stem cell transplantation (SCT). Seventy seven SCT donor-recipient pairs (DRP) (HLA matched unrelated donor (MUD), n = 50; matched related donor (MRD), n = 27) underwent whole exome sequencing to identify single nucleotide polymorphisms (SNPs) generating alloreactive peptide libraries for each DRP (9-mer peptide-HLA complexes); Human CMV CROSS (Cross-Reactive Open Source Sequence) database was compiled from NCBI; HLA class I binding affinity for each DRPs HLA was calculated by NetMHCpan 2.8 and hCMV- derived 9-mers algorithmically compared to the alloreactive peptide-HLA complex libraries. Short consecutive (≥6) amino acid (AA) sequence homology matching hCMV to recipient peptides was considered for HLA-bound-peptide (IC50<500nM) cross reactivity. Of the 70,686 hCMV 9-mers contained within the hCMV CROSS database, an average of 29,658 matched the MRD DRP alloreactive peptides and 52,910 matched MUD DRP peptides (p<0.001). In silico analysis revealed multiple high affinity, immunogenic CMV-Human peptide matches (IC50<500 nM) expressed in GVHD-affected tissue-specific manner. hCMV+GVHD was found in 18 patients, 13 developing hCMV viremia before GVHD onset. Analysis of patients with GVHD identified potential cross reactive peptide expression within affected organs. We propose that hCMV peptide sequence homology with human alloreactive peptides may contribute to the pathophysiology of GVHD.


Url:
DOI: 10.1371/journal.pone.0178763
PubMed: 28800601
PubMed Central: 5553991

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PMC:5553991

Le document en format XML

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<term>Clone Cells</term>
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<term>Cytomegalovirus (metabolism)</term>
<term>Graft vs Host Disease (immunology)</term>
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<term>Antigènes HLA ()</term>
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<term>Mimétisme moléculaire</term>
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<front>
<div type="abstract" xml:lang="en">
<p>Human cytomegalovirus (hCMV) reactivation may often coincide with the development of graft-versus-host-disease (GVHD) in stem cell transplantation (SCT). Seventy seven SCT donor-recipient pairs (DRP) (HLA matched unrelated donor (MUD), n = 50; matched related donor (MRD), n = 27) underwent whole exome sequencing to identify single nucleotide polymorphisms (SNPs) generating alloreactive peptide libraries for each DRP (9-mer peptide-HLA complexes); Human CMV CROSS (Cross-Reactive Open Source Sequence) database was compiled from NCBI; HLA class I binding affinity for each DRPs HLA was calculated by NetMHCpan 2.8 and hCMV- derived 9-mers algorithmically compared to the alloreactive peptide-HLA complex libraries. Short consecutive (≥6) amino acid (AA) sequence homology matching hCMV to recipient peptides was considered for HLA-bound-peptide (IC50<500nM) cross reactivity. Of the 70,686 hCMV 9-mers contained within the hCMV CROSS database, an average of 29,658 matched the MRD DRP alloreactive peptides and 52,910 matched MUD DRP peptides (p<0.001).
<italic>In silico</italic>
analysis revealed multiple high affinity, immunogenic CMV-Human peptide matches (IC50<500 nM) expressed in GVHD-affected tissue-specific manner. hCMV+GVHD was found in 18 patients, 13 developing hCMV viremia before GVHD onset. Analysis of patients with GVHD identified potential cross reactive peptide expression within affected organs. We propose that hCMV peptide sequence homology with human alloreactive peptides may contribute to the pathophysiology of GVHD.</p>
</div>
</front>
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<title xml:lang="en" level="a" type="main">Sequence homology between HLA-bound cytomegalovirus and human peptides: A potential trigger for alloreactivity</title>
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<name sortKey="Hall, Charles E" sort="Hall, Charles E" uniqKey="Hall C" first="Charles E." last="Hall">Charles E. Hall</name>
<affiliation wicri:level="2">
<nlm:aff id="aff001">
<addr-line>Bone Marrow Transplant Program, Massey Cancer Center, Virginia Commonwealth University, Richmond, Virginia, United States of America</addr-line>
</nlm:aff>
<country xml:lang="fr">États-Unis</country>
<wicri:regionArea>Bone Marrow Transplant Program, Massey Cancer Center, Virginia Commonwealth University, Richmond, Virginia</wicri:regionArea>
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<region type="state">Virginie</region>
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</affiliation>
</author>
<author>
<name sortKey="Koparde, Vishal N" sort="Koparde, Vishal N" uniqKey="Koparde V" first="Vishal N." last="Koparde">Vishal N. Koparde</name>
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<nlm:aff id="aff002">
<addr-line>Center for the Study of Biological Complexity, Virginia Commonwealth University, Richmond, Virginia, United States of America</addr-line>
</nlm:aff>
<country xml:lang="fr">États-Unis</country>
<wicri:regionArea>Center for the Study of Biological Complexity, Virginia Commonwealth University, Richmond, Virginia</wicri:regionArea>
<placeName>
<region type="state">Virginie</region>
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<name sortKey="Jameson Lee, Maximilian" sort="Jameson Lee, Maximilian" uniqKey="Jameson Lee M" first="Maximilian" last="Jameson-Lee">Maximilian Jameson-Lee</name>
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<nlm:aff id="aff001">
<addr-line>Bone Marrow Transplant Program, Massey Cancer Center, Virginia Commonwealth University, Richmond, Virginia, United States of America</addr-line>
</nlm:aff>
<country xml:lang="fr">États-Unis</country>
<wicri:regionArea>Bone Marrow Transplant Program, Massey Cancer Center, Virginia Commonwealth University, Richmond, Virginia</wicri:regionArea>
<placeName>
<region type="state">Virginie</region>
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</affiliation>
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<name sortKey="Elnasseh, Abdelrhman G" sort="Elnasseh, Abdelrhman G" uniqKey="Elnasseh A" first="Abdelrhman G." last="Elnasseh">Abdelrhman G. Elnasseh</name>
<affiliation wicri:level="2">
<nlm:aff id="aff001">
<addr-line>Bone Marrow Transplant Program, Massey Cancer Center, Virginia Commonwealth University, Richmond, Virginia, United States of America</addr-line>
</nlm:aff>
<country xml:lang="fr">États-Unis</country>
<wicri:regionArea>Bone Marrow Transplant Program, Massey Cancer Center, Virginia Commonwealth University, Richmond, Virginia</wicri:regionArea>
<placeName>
<region type="state">Virginie</region>
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</affiliation>
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<author>
<name sortKey="Scalora, Allison F" sort="Scalora, Allison F" uniqKey="Scalora A" first="Allison F." last="Scalora">Allison F. Scalora</name>
<affiliation wicri:level="2">
<nlm:aff id="aff001">
<addr-line>Bone Marrow Transplant Program, Massey Cancer Center, Virginia Commonwealth University, Richmond, Virginia, United States of America</addr-line>
</nlm:aff>
<country xml:lang="fr">États-Unis</country>
<wicri:regionArea>Bone Marrow Transplant Program, Massey Cancer Center, Virginia Commonwealth University, Richmond, Virginia</wicri:regionArea>
<placeName>
<region type="state">Virginie</region>
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</affiliation>
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<affiliation wicri:level="2">
<nlm:aff id="aff001">
<addr-line>Bone Marrow Transplant Program, Massey Cancer Center, Virginia Commonwealth University, Richmond, Virginia, United States of America</addr-line>
</nlm:aff>
<country xml:lang="fr">États-Unis</country>
<wicri:regionArea>Bone Marrow Transplant Program, Massey Cancer Center, Virginia Commonwealth University, Richmond, Virginia</wicri:regionArea>
<placeName>
<region type="state">Virginie</region>
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</affiliation>
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<affiliation wicri:level="2">
<nlm:aff id="aff002">
<addr-line>Center for the Study of Biological Complexity, Virginia Commonwealth University, Richmond, Virginia, United States of America</addr-line>
</nlm:aff>
<country xml:lang="fr">États-Unis</country>
<wicri:regionArea>Center for the Study of Biological Complexity, Virginia Commonwealth University, Richmond, Virginia</wicri:regionArea>
<placeName>
<region type="state">Virginie</region>
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<affiliation wicri:level="2">
<nlm:aff id="aff001">
<addr-line>Bone Marrow Transplant Program, Massey Cancer Center, Virginia Commonwealth University, Richmond, Virginia, United States of America</addr-line>
</nlm:aff>
<country xml:lang="fr">États-Unis</country>
<wicri:regionArea>Bone Marrow Transplant Program, Massey Cancer Center, Virginia Commonwealth University, Richmond, Virginia</wicri:regionArea>
<placeName>
<region type="state">Virginie</region>
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<nlm:aff id="aff002">
<addr-line>Center for the Study of Biological Complexity, Virginia Commonwealth University, Richmond, Virginia, United States of America</addr-line>
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<country xml:lang="fr">États-Unis</country>
<wicri:regionArea>Center for the Study of Biological Complexity, Virginia Commonwealth University, Richmond, Virginia</wicri:regionArea>
<placeName>
<region type="state">Virginie</region>
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<affiliation wicri:level="2">
<nlm:aff id="aff003">
<addr-line>Department of Microbiology and Immunology, Virginia Commonwealth University, Richmond, Virginia, United States of America</addr-line>
</nlm:aff>
<country xml:lang="fr">États-Unis</country>
<wicri:regionArea>Department of Microbiology and Immunology, Virginia Commonwealth University, Richmond, Virginia</wicri:regionArea>
<placeName>
<region type="state">Virginie</region>
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<author>
<name sortKey="Neale, Michael C" sort="Neale, Michael C" uniqKey="Neale M" first="Michael C." last="Neale">Michael C. Neale</name>
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<nlm:aff id="aff004">
<addr-line>Departments of Psychiatry and Human & Molecular Genetics, Virginia Commonwealth University, Richmond, Virginia, United States of America</addr-line>
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<country xml:lang="fr">États-Unis</country>
<wicri:regionArea>Departments of Psychiatry and Human & Molecular Genetics, Virginia Commonwealth University, Richmond, Virginia</wicri:regionArea>
<placeName>
<region type="state">Virginie</region>
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<name sortKey="Nixon, Daniel E" sort="Nixon, Daniel E" uniqKey="Nixon D" first="Daniel E." last="Nixon">Daniel E. Nixon</name>
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<addr-line>Division of Infectious Diseases, Virginia Commonwealth University, Richmond, Virginia, United States of America</addr-line>
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<country xml:lang="fr">États-Unis</country>
<wicri:regionArea>Division of Infectious Diseases, Virginia Commonwealth University, Richmond, Virginia</wicri:regionArea>
<placeName>
<region type="state">Virginie</region>
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<author>
<name sortKey="Toor, Amir A" sort="Toor, Amir A" uniqKey="Toor A" first="Amir A." last="Toor">Amir A. Toor</name>
<affiliation wicri:level="2">
<nlm:aff id="aff001">
<addr-line>Bone Marrow Transplant Program, Massey Cancer Center, Virginia Commonwealth University, Richmond, Virginia, United States of America</addr-line>
</nlm:aff>
<country xml:lang="fr">États-Unis</country>
<wicri:regionArea>Bone Marrow Transplant Program, Massey Cancer Center, Virginia Commonwealth University, Richmond, Virginia</wicri:regionArea>
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<series>
<title level="j">PLoS ONE</title>
<idno type="eISSN">1932-6203</idno>
<imprint>
<date when="2017">2017</date>
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</teiHeader>
<front>
<div type="abstract" xml:lang="en">
<p>Human cytomegalovirus (hCMV) reactivation may often coincide with the development of graft-versus-host-disease (GVHD) in stem cell transplantation (SCT). Seventy seven SCT donor-recipient pairs (DRP) (HLA matched unrelated donor (MUD), n = 50; matched related donor (MRD), n = 27) underwent whole exome sequencing to identify single nucleotide polymorphisms (SNPs) generating alloreactive peptide libraries for each DRP (9-mer peptide-HLA complexes); Human CMV CROSS (Cross-Reactive Open Source Sequence) database was compiled from NCBI; HLA class I binding affinity for each DRPs HLA was calculated by NetMHCpan 2.8 and hCMV- derived 9-mers algorithmically compared to the alloreactive peptide-HLA complex libraries. Short consecutive (≥6) amino acid (AA) sequence homology matching hCMV to recipient peptides was considered for HLA-bound-peptide (IC50<500nM) cross reactivity. Of the 70,686 hCMV 9-mers contained within the hCMV CROSS database, an average of 29,658 matched the MRD DRP alloreactive peptides and 52,910 matched MUD DRP peptides (p<0.001).
<italic>In silico</italic>
analysis revealed multiple high affinity, immunogenic CMV-Human peptide matches (IC50<500 nM) expressed in GVHD-affected tissue-specific manner. hCMV+GVHD was found in 18 patients, 13 developing hCMV viremia before GVHD onset. Analysis of patients with GVHD identified potential cross reactive peptide expression within affected organs. We propose that hCMV peptide sequence homology with human alloreactive peptides may contribute to the pathophysiology of GVHD.</p>
</div>
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<name sortKey="Hall, Charles E" sort="Hall, Charles E" uniqKey="Hall C" first="Charles E" last="Hall">Charles E. Hall</name>
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<nlm:affiliation>Bone Marrow Transplant Program, Massey Cancer Center, Virginia Commonwealth University, Richmond, Virginia, United States of America.</nlm:affiliation>
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<name sortKey="Koparde, Vishal N" sort="Koparde, Vishal N" uniqKey="Koparde V" first="Vishal N" last="Koparde">Vishal N. Koparde</name>
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<name sortKey="Jameson Lee, Maximilian" sort="Jameson Lee, Maximilian" uniqKey="Jameson Lee M" first="Maximilian" last="Jameson-Lee">Maximilian Jameson-Lee</name>
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<name sortKey="Elnasseh, Abdelrhman G" sort="Elnasseh, Abdelrhman G" uniqKey="Elnasseh A" first="Abdelrhman G" last="Elnasseh">Abdelrhman G. Elnasseh</name>
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<country xml:lang="fr">États-Unis</country>
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<name sortKey="Kobulnicky, David J" sort="Kobulnicky, David J" uniqKey="Kobulnicky D" first="David J" last="Kobulnicky">David J. Kobulnicky</name>
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<country xml:lang="fr">États-Unis</country>
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<country xml:lang="fr">États-Unis</country>
<wicri:regionArea>Bone Marrow Transplant Program, Massey Cancer Center, Virginia Commonwealth University, Richmond, Virginia</wicri:regionArea>
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<region type="state">Virginie</region>
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<title level="j">PloS one</title>
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<term>Clone Cells</term>
<term>Computational Biology</term>
<term>Cross Reactions (immunology)</term>
<term>Cytomegalovirus (metabolism)</term>
<term>Graft vs Host Disease (immunology)</term>
<term>Graft vs Host Disease (virology)</term>
<term>HLA Antigens (chemistry)</term>
<term>Humans</term>
<term>Molecular Mimicry</term>
<term>Peptides (chemistry)</term>
<term>Proteome (metabolism)</term>
<term>Sequence Homology, Amino Acid</term>
<term>T-Lymphocytes (cytology)</term>
<term>Viral Proteins (metabolism)</term>
</keywords>
<keywords scheme="KwdFr" xml:lang="fr">
<term>Antigènes HLA ()</term>
<term>Biologie informatique</term>
<term>Clones cellulaires</term>
<term>Cytomegalovirus (métabolisme)</term>
<term>Humains</term>
<term>Lymphocytes T (cytologie)</term>
<term>Maladie du greffon contre l'hôte (immunologie)</term>
<term>Maladie du greffon contre l'hôte (virologie)</term>
<term>Mimétisme moléculaire</term>
<term>Peptides ()</term>
<term>Protéines virales (métabolisme)</term>
<term>Protéome (métabolisme)</term>
<term>Réactions croisées (immunologie)</term>
<term>Similitude de séquences d'acides aminés</term>
</keywords>
<keywords scheme="MESH" type="chemical" qualifier="chemistry" xml:lang="en">
<term>HLA Antigens</term>
<term>Peptides</term>
</keywords>
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<term>Lymphocytes T</term>
</keywords>
<keywords scheme="MESH" qualifier="cytology" xml:lang="en">
<term>T-Lymphocytes</term>
</keywords>
<keywords scheme="MESH" qualifier="immunologie" xml:lang="fr">
<term>Maladie du greffon contre l'hôte</term>
<term>Réactions croisées</term>
</keywords>
<keywords scheme="MESH" qualifier="immunology" xml:lang="en">
<term>Cross Reactions</term>
<term>Graft vs Host Disease</term>
</keywords>
<keywords scheme="MESH" qualifier="metabolism" xml:lang="en">
<term>Cytomegalovirus</term>
<term>Proteome</term>
<term>Viral Proteins</term>
</keywords>
<keywords scheme="MESH" qualifier="métabolisme" xml:lang="fr">
<term>Cytomegalovirus</term>
<term>Protéines virales</term>
<term>Protéome</term>
</keywords>
<keywords scheme="MESH" qualifier="virologie" xml:lang="fr">
<term>Maladie du greffon contre l'hôte</term>
</keywords>
<keywords scheme="MESH" qualifier="virology" xml:lang="en">
<term>Graft vs Host Disease</term>
</keywords>
<keywords scheme="MESH" xml:lang="en">
<term>Clone Cells</term>
<term>Computational Biology</term>
<term>Humans</term>
<term>Molecular Mimicry</term>
<term>Sequence Homology, Amino Acid</term>
</keywords>
<keywords scheme="MESH" xml:lang="fr">
<term>Antigènes HLA</term>
<term>Biologie informatique</term>
<term>Clones cellulaires</term>
<term>Humains</term>
<term>Mimétisme moléculaire</term>
<term>Peptides</term>
<term>Similitude de séquences d'acides aminés</term>
</keywords>
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<front>
<div type="abstract" xml:lang="en">Human cytomegalovirus (hCMV) reactivation may often coincide with the development of graft-versus-host-disease (GVHD) in stem cell transplantation (SCT). Seventy seven SCT donor-recipient pairs (DRP) (HLA matched unrelated donor (MUD), n = 50; matched related donor (MRD), n = 27) underwent whole exome sequencing to identify single nucleotide polymorphisms (SNPs) generating alloreactive peptide libraries for each DRP (9-mer peptide-HLA complexes); Human CMV CROSS (Cross-Reactive Open Source Sequence) database was compiled from NCBI; HLA class I binding affinity for each DRPs HLA was calculated by NetMHCpan 2.8 and hCMV- derived 9-mers algorithmically compared to the alloreactive peptide-HLA complex libraries. Short consecutive (≥6) amino acid (AA) sequence homology matching hCMV to recipient peptides was considered for HLA-bound-peptide (IC50<500nM) cross reactivity. Of the 70,686 hCMV 9-mers contained within the hCMV CROSS database, an average of 29,658 matched the MRD DRP alloreactive peptides and 52,910 matched MUD DRP peptides (p<0.001). In silico analysis revealed multiple high affinity, immunogenic CMV-Human peptide matches (IC50<500 nM) expressed in GVHD-affected tissue-specific manner. hCMV+GVHD was found in 18 patients, 13 developing hCMV viremia before GVHD onset. Analysis of patients with GVHD identified potential cross reactive peptide expression within affected organs. We propose that hCMV peptide sequence homology with human alloreactive peptides may contribute to the pathophysiology of GVHD.</div>
</front>
</TEI>
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