Experimental animal modeling for immuno-oncology

被引:40
作者
Li, Qi-Xiang [1 ,2 ]
Feuer, Gerold [3 ]
Ouyang, Xuesong [1 ]
An, Xiaoyu [1 ,2 ]
机构
[1] Crown Biosci Inc, 3375 Scott Blvd,Suite 108, Santa Clara, CA 95054 USA
[2] Peking Univ, State Key Lab Nat & Biomimet Drugs, Beijing 100191, Peoples R China
[3] HuMurine Technol Inc, 2700 Stockton Blvd,Rm 1403, Sacramento, CA 95817 USA
关键词
Xenograft; Syngeneic; Homograft; GEMM; Murine and human immunity; Humanization; PATIENT-DERIVED XENOGRAFTS; CD8(+) T-CELLS; CANCER-IMMUNOTHERAPY; ANTITUMOR IMMUNITY; SUPPRESSOR-CELLS; TUMOR XENOGRAFTS; PD-L1; EXPRESSION; HUMANIZED MICE; MOUSE MODELS; ANTI-PD-L1; ANTIBODY;
D O I
10.1016/j.pharmthera.2017.02.002
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Immuno-oncology (I/O) research has intensified significantly in recent years due to the breakthrough development and the regulatory approval of several immune checkpoint inhibitors, leading to the rapid expansion of the new discovery of novel I/O therapies, new checkpoint inhibitors and beyond. However, many I/O questions remain unanswered, including why only certain subsets of patients respond to these treatments, who the responders would be, and how to expand patient response (the conversion of non-responders or maximizing response in partial responders). All of these require relevant I/O experimental systems, particularly relevant preclinical animal models. Compared to other oncology drug discovery, e.g. cytotoxic and targeted drugs, a lack of relevant animal models is a major obstacle in I/O drug discovery, and an urgent and unmet need. Despite the obvious importance, and the fact that much I/O research has been performed using many different animal models, there are few comprehensive and introductory reviews on this topic. This article attempts to review the efforts in development of a variety of such models, as well as their applications and limitations for readers new to the field, particularly those in the pharmaceutical industry. (C) 2017 Published by Elsevier Inc.
引用
收藏
页码:34 / 46
页数:13
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