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Artificial antigen-presenting cells expressing HLA class II molecules as an effective tool for amplifying human specific memory CD4 + T cells

Identifieur interne : 000060 ( France/Analysis ); précédent : 000059; suivant : 000061

Artificial antigen-presenting cells expressing HLA class II molecules as an effective tool for amplifying human specific memory CD4 + T cells

Auteurs : Anthony Garnier [France] ; Mohamad Hamieh [France] ; Aurélie Drouet [France] ; Jérôme Leprince [France] ; Denis Vivien [France] ; Thierry Frebourg [France] ; Brigitte Le Mauff [France] ; Jean-Baptiste Latouche [France] ; Olivier Toutirais [France]

Source :

RBID : Hal:hal-02379907

Abstract

Owing to their multiple immune functions, CD4(+) T cells are of major interest for immunotherapy in chronic viral infections and cancer, as well as for severe autoimmune diseases and transplantation. Therefore, standardized methods allowing rapid generation of a large number of CD4(+) T cells for adoptive immunotherapy are still awaited. We constructed stable artificial antigen-presenting cells (AAPCs) derived from mouse fibroblasts. They were genetically modified to express human leukocyte antigen (HLA)-DR molecules and the human accessory molecules B7.1, Intercellular adhesion molecule-1 (ICAM-1) and lymphocyte function-associated antigen-3 (LFA-3). AAPCs expressing HLA-DR1, HLA-DR15 or HLA-DR51 molecules and loaded with peptides derived from influenza hemagglutinin (HA), myelin basic protein (MBP) or factor VIII, respectively, activated specific CD4(+) T-cell clones more effectively than Epstein-Barr virus (EBV)-transformed B cells. We also showed that AAPCs were able to take up and process whole Ag proteins, and present epitopes to specific T cells. In primary cultures, AAPCs loaded with HA peptide allowed generation of specific Th1 lymphocytes from healthy donors as demonstrated by tetramer and intracellular cytokine staining. Although AAPCs were less effective than autologous peripheral blood mononuclear cells (PBMCs) to stimulate CD4(+) T cells in primary culture, AAPCs were more potent to reactivate and expand memory Th1 cells in a strictly Ag-dependent manner. As the availability of autologous APCs is limited, the AAPC system represents a stable and reliable tool to achieve clinically relevant numbers of CD4(+) T cells for adoptive immunotherapy. For fundamental research in immunology, AAPCs are also useful to decipher mechanisms involved in the development of human CD4 T-cell responses.


Url:
DOI: 10.1038/icb.2016.25


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<name sortKey="Toutirais, Olivier" sort="Toutirais, Olivier" uniqKey="Toutirais O" first="Olivier" last="Toutirais">Olivier Toutirais</name>
<affiliation wicri:level="1">
<hal:affiliation type="institution" xml:id="struct-323838" status="VALID">
<orgName>Etablissement français du sang - Normandie</orgName>
<orgName type="acronym">EFS</orgName>
<desc>
<address>
<addrLine>Chu hopital charles nicolle1 rue de germont76000 Rouen</addrLine>
<country key="FR"></country>
</address>
</desc>
</hal:affiliation>
<country>France</country>
</affiliation>
</author>
</analytic>
<idno type="DOI">10.1038/icb.2016.25</idno>
<series>
<title level="j">Immunology and Cell Biology</title>
<idno type="ISSN">0818-9641</idno>
<imprint>
<date type="datePub">2016-08</date>
</imprint>
</series>
</biblStruct>
</sourceDesc>
</fileDesc>
<profileDesc>
<textClass></textClass>
</profileDesc>
</teiHeader>
<front>
<div type="abstract" xml:lang="en">
<p>Owing to their multiple immune functions, CD4(+) T cells are of major interest for immunotherapy in chronic viral infections and cancer, as well as for severe autoimmune diseases and transplantation. Therefore, standardized methods allowing rapid generation of a large number of CD4(+) T cells for adoptive immunotherapy are still awaited. We constructed stable artificial antigen-presenting cells (AAPCs) derived from mouse fibroblasts. They were genetically modified to express human leukocyte antigen (HLA)-DR molecules and the human accessory molecules B7.1, Intercellular adhesion molecule-1 (ICAM-1) and lymphocyte function-associated antigen-3 (LFA-3). AAPCs expressing HLA-DR1, HLA-DR15 or HLA-DR51 molecules and loaded with peptides derived from influenza hemagglutinin (HA), myelin basic protein (MBP) or factor VIII, respectively, activated specific CD4(+) T-cell clones more effectively than Epstein-Barr virus (EBV)-transformed B cells. We also showed that AAPCs were able to take up and process whole Ag proteins, and present epitopes to specific T cells. In primary cultures, AAPCs loaded with HA peptide allowed generation of specific Th1 lymphocytes from healthy donors as demonstrated by tetramer and intracellular cytokine staining. Although AAPCs were less effective than autologous peripheral blood mononuclear cells (PBMCs) to stimulate CD4(+) T cells in primary culture, AAPCs were more potent to reactivate and expand memory Th1 cells in a strictly Ag-dependent manner. As the availability of autologous APCs is limited, the AAPC system represents a stable and reliable tool to achieve clinically relevant numbers of CD4(+) T cells for adoptive immunotherapy. For fundamental research in immunology, AAPCs are also useful to decipher mechanisms involved in the development of human CD4 T-cell responses.</p>
</div>
</front>
</TEI>
<affiliations>
<list>
<country>
<li>France</li>
</country>
</list>
<tree>
<country name="France">
<noRegion>
<name sortKey="Garnier, Anthony" sort="Garnier, Anthony" uniqKey="Garnier A" first="Anthony" last="Garnier">Anthony Garnier</name>
</noRegion>
<name sortKey="Drouet, Aurelie" sort="Drouet, Aurelie" uniqKey="Drouet A" first="Aurélie" last="Drouet">Aurélie Drouet</name>
<name sortKey="Frebourg, Thierry" sort="Frebourg, Thierry" uniqKey="Frebourg T" first="Thierry" last="Frebourg">Thierry Frebourg</name>
<name sortKey="Hamieh, Mohamad" sort="Hamieh, Mohamad" uniqKey="Hamieh M" first="Mohamad" last="Hamieh">Mohamad Hamieh</name>
<name sortKey="Latouche, Jean Baptiste" sort="Latouche, Jean Baptiste" uniqKey="Latouche J" first="Jean-Baptiste" last="Latouche">Jean-Baptiste Latouche</name>
<name sortKey="Le Mauff, Brigitte" sort="Le Mauff, Brigitte" uniqKey="Le Mauff B" first="Brigitte" last="Le Mauff">Brigitte Le Mauff</name>
<name sortKey="Leprince, Jerome" sort="Leprince, Jerome" uniqKey="Leprince J" first="Jérôme" last="Leprince">Jérôme Leprince</name>
<name sortKey="Toutirais, Olivier" sort="Toutirais, Olivier" uniqKey="Toutirais O" first="Olivier" last="Toutirais">Olivier Toutirais</name>
<name sortKey="Vivien, Denis" sort="Vivien, Denis" uniqKey="Vivien D" first="Denis" last="Vivien">Denis Vivien</name>
</country>
</tree>
</affiliations>
</record>

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