TY - JOUR
T1 - CMV-specific T cells generated from naïve T cells recognize atypical epitopes and may be protective in vivo
AU - Hanley, Patrick J.
AU - Melenhorst, Jan J.
AU - Nikiforow, Sarah
AU - Scheinberg, Phillip
AU - Blaney, James W.
AU - Demmler-Harrison, Gail
AU - Cruz, C. Russell
AU - Lam, Sharon
AU - Krance, Robert A.
AU - Leung, Kathryn S.
AU - Martinez, Caridad A.
AU - Liu, Hao
AU - Douek, Daniel C.
AU - Heslop, Helen E.
AU - Rooney, Cliona M.
AU - Shpall, Elizabeth J.
AU - Barrett, A. John
AU - Bollard, Catherine M.
N1 - Publisher Copyright:
Copyright © 2015, American Association for the Advancement of Science.
PY - 2015/4/29
Y1 - 2015/4/29
N2 - Adoptive transfer of cytomegalovirus (CMV)-specific T cells derived from adult seropositive donors can effectively restore antiviral immunity after transplantation. However, CMV-seronegative donors lack CMV-specific memory T cells, which restricts the availability of virus-specific T cells for immunoprophylaxis. We demonstrate the feasibility of deriving CMV-specific T cells from naïve cells for T cell therapy. Naïve T cells primed to recognize CMV were restricted to different, atypical epitopes than T cells derived from CMV-seropositive individuals; however, these two cell populations had similar avidities. CMV-seropositive individuals also had T cells recognizing these atypical epitopes, but these cells had a lower avidity than those derived from the seronegative subjects, which suggests that high-avidity T cells to these epitopes may be lost over time. Indeed, recipients of cord blood (CB) grafts who did not develop CMV were found by clonotypic analysis to have T cells recognizing atypical CMVpp65 epitopes. Therefore, we examined unmanipulated CB units and found that T cells with T cell receptors restricted by atypical epitopes were the most common, which may explain why these T cells expanded. When infused to recipients, naïve donor-derived virus-specific T cells that recognized atypical epitopes were associated with prolonged periods of CMV-free survival and complete remission. These data suggest that naïve-derived T cells from seronegative patients may be an additional source of cells for CMV immunoprophylaxis.
AB - Adoptive transfer of cytomegalovirus (CMV)-specific T cells derived from adult seropositive donors can effectively restore antiviral immunity after transplantation. However, CMV-seronegative donors lack CMV-specific memory T cells, which restricts the availability of virus-specific T cells for immunoprophylaxis. We demonstrate the feasibility of deriving CMV-specific T cells from naïve cells for T cell therapy. Naïve T cells primed to recognize CMV were restricted to different, atypical epitopes than T cells derived from CMV-seropositive individuals; however, these two cell populations had similar avidities. CMV-seropositive individuals also had T cells recognizing these atypical epitopes, but these cells had a lower avidity than those derived from the seronegative subjects, which suggests that high-avidity T cells to these epitopes may be lost over time. Indeed, recipients of cord blood (CB) grafts who did not develop CMV were found by clonotypic analysis to have T cells recognizing atypical CMVpp65 epitopes. Therefore, we examined unmanipulated CB units and found that T cells with T cell receptors restricted by atypical epitopes were the most common, which may explain why these T cells expanded. When infused to recipients, naïve donor-derived virus-specific T cells that recognized atypical epitopes were associated with prolonged periods of CMV-free survival and complete remission. These data suggest that naïve-derived T cells from seronegative patients may be an additional source of cells for CMV immunoprophylaxis.
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U2 - 10.1126/scitranslmed.aaa2546
DO - 10.1126/scitranslmed.aaa2546
M3 - Article
C2 - 25925682
AN - SCOPUS:84929493070
SN - 1946-6234
VL - 7
JO - Science translational medicine
JF - Science translational medicine
IS - 285
M1 - 285ra63
ER -