Importance of Cellular Microenvironment and Circulatory Dynamics in B Cell Immunotherapy

Qian Gong(Gene Therapy Laboratory), Qinglin Ou(Gene Therapy Laboratory), Shiming Ye(Gene Therapy Laboratory), Wyne P. Lee(Gene Therapy Laboratory), Jennine Cornelius(Gene Therapy Laboratory), Lauri Diehl(Gene Therapy Laboratory), Wei Lin(Gene Therapy Laboratory), Zhilan Hu(Gene Therapy Laboratory), Yanmei Lu(Genesys (United States)), Yongmei Chen(Recombinant Antibody Technology (United Kingdom)), Yan Wu(Gene Therapy Laboratory), Y. Gloria Meng(Genesys (United States)), Peter Gribling(Gene Therapy Laboratory), Zhonghua Lin(Gene Therapy Laboratory), Kathy Nguyen(Gene Therapy Laboratory), Thanhvien Tran(Gene Therapy Laboratory), Yifan Zhang(Gene Therapy Laboratory), Hugh Rosen(Scripps Research Institute), Flavius Martin(Gene Therapy Laboratory), Andrew C. Chan(Gene Therapy Laboratory)
The Journal of Immunology
January 1, 2005
Cited by 540Open Access
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Abstract

B cell immunotherapy has emerged as a mainstay in the treatment of lymphomas and autoimmune diseases. Although the microenvironment has recently been demonstrated to play critical roles in B cell homeostasis, its contribution to immunotherapy is unknown. To analyze the in vivo factors that regulate mechanisms involved in B cell immunotherapy, we used a murine model for human CD20 (hCD20) expression in which treatment of hCD20(+) mice with anti-hCD20 mAbs mimics B cell depletion observed in humans. We demonstrate in this study that factors derived from the microenvironment, including signals from the B cell-activating factor belonging to the TNF family/BLyS survival factor, integrin-regulated homeostasis, and circulatory dynamics of B cells define distinct in vivo mechanism(s) and sensitivities of cells in anti-hCD20 mAb-directed therapies. These findings provide new insights into the mechanisms of immunotherapy and define new opportunities in the treatment of cancers and autoimmune diseases.


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