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Generation of rejuvenated antigen-specific T cells by reprogramming to pluripotency and redifferentiation.
by:
Toshinobu Nishimura ,
Shin Kaneko ,
Ai Kawana-Tachikawa ,
Yoko Tajima ,
Haruo Goto ,
Dayong Zhu ,
Kaori Nakayama-Hosoya ,
Shoichi Iriguchi ,
Yasushi Uemura ,
Takafumi Shimizu ,
Naoya Takayama ,
Daisuke Yamada ,
Ken Nishimura ,
Manami Ohtaka ,
Nobukazu Watanabe ,
Satoshi Takahashi ,
Aikichi Iwamoto ,
Haruhiko Koseki ,
Mahito Nakanishi ,
Koji Eto ,
Hiromitsu Nakauchi
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Abstract
Adoptive immunotherapy with functional T cells is potentially an effective therapeutic strategy for combating many types of cancer and viral infection. However, exhaustion of antigen-specific T cells represents a major challenge to this type of approach. In an effort to overcome this problem, we reprogrammed clonally expanded antigen-specific CD8(+) T cells from an HIV-1-infected patient to pluripotency. The T cell-derived induced pluripotent stem cells were then redifferentiated into CD8(+) T cells that had a high proliferative capacity and elongated telomeres. These "rejuvenated" cells possessed antigen-specific killing activity and exhibited T cell receptor gene-rearrangement patterns identical to those of the original T cell clone from the patient. We also found that this method can be effective for generating specific T cells for other pathology-associated antigens. Thus, this type of approach may have broad applications in the field of adoptive immunotherapy. Copyright © 2013 Elsevier Inc. All rights reserved.
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