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Improved Expansion and In Vivo Function of Patient T Cells by a Serum-free Medium
Author(s) -
Andrew Medvec,
Christopher Ecker,
Hong Kong,
Emily A. Winters,
Joshua Glover,
Angel VarelaRohena,
James L. Riley
Publication year - 2017
Publication title -
molecular therapy — methods and clinical development
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.285
H-Index - 32
ISSN - 2329-0501
DOI - 10.1016/j.omtm.2017.11.001
Subject(s) - in vivo , cell culture , immunology , multiple myeloma , in vitro , cancer research , t cell , function (biology) , microbiology and biotechnology , biology , medicine , immune system , biochemistry , genetics
Improvements to T cell culture systems that promote long-term engraftment and function of adoptively transferred T cells will likely result in superior clinical benefit to more individuals. To this end, we recently developed a chemically defined cell culture medium that robustly expands all T cell subsets in the absence of human serum. Using a humanized mouse model, we observed that T cells expanded in the absence of human serum provided durable control of tumors, whereas T cells expanded in medium supplemented with human serum only mediated transient control of tumor growth. Importantly, our new medium effectively expanded more differentiated T cells from multiple myeloma patients in the absence of serum. These patient-derived T cells were also able to provide durable control of B cell tumors in vivo , and this long-term control of cancer was lost when T cells were expanded in the presence of serum. Thus, engineered T cells expanded in an optimized medium in the absence of serum may have improved therapeutic potential.

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