Expansion of KRAS hotspot mutations reactive T cells from human pancreatic tumors using autologous T cells as the antigen-presenting cells

被引:3
作者
Wang, Sizhen [1 ]
Zhang, Xiaohui [2 ]
Zou, Xuemei [2 ]
Wen, Maorong [2 ]
Gan, Chi [2 ]
Jiang, Xiaochun [2 ]
Li, Min [1 ]
Shen, Rongxi [1 ]
Zhu, Daojun [1 ]
Yao, Anlong [1 ]
Fang, Yu [1 ]
Fox, Bernard A. [3 ]
Hu, Hong-Ming [2 ,3 ]
Yu, Guangjie [2 ]
Wang, Xinbo [1 ]
机构
[1] Nanjing Univ, Jinling Hosp, Res Inst Gen Surg, Med Sch, 305 Zhong Shan East Rd, Nanjing 210002, Peoples R China
[2] ImmuXell Biotech Ltd, 299 Kangwei Rd, Shanghai 201315, Peoples R China
[3] Ubivac Inc, 18183 SW Boones Ferry Rd, Portland, OR 97224 USA
关键词
TRANSFER THERAPY; NK CELLS; IMMUNOTHERAPY; LYMPHOCYTES; VALIDATION; RECEPTOR; CANCER; RAS;
D O I
10.1007/s00262-022-03335-w
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Adoptive cell therapy (ACT) with expanded tumor-infiltrating lymphocytes (TIL) or TCR gene-modified T cells (TCR-T) that recognize mutant KRAS neo-antigens can mediate tumor regression in patients with advanced pancreatic ductal adenocarcinoma (PDAC) (Tran et al in N Engl J Med, 375:2255-2262, 2016; Leidner et al in N Engl J Med, 386:2112-2119, 2022). The mutant KRAS-targeted ACT holds great potential to achieve durable clinical responses for PDAC, which has had no meaningful improvement over 40 years. However, the wide application of mutant KRAS-centric ACT is currently limited by the rarity of TIL that recognize the mutant KRAS. In addition, PDAC is generally recognized as a poorly immunogenic tumor, and TILs in PDAC are less abundant than in immunogenic tumors such as melanoma. To increase the success rate of TIL production, we adopted a well-utilized K562-based artificial APC (aAPC) that expresses 4-1BBL as the costimulatory molecules to enhance the TIL production from PDCA. However, stimulation with K562-based aAPC led to a rapid loss of specificity to mutant KRAS. To selectively expand neo-antigen-specific T cells, particularly mKRAS, from the TILs, we used tandem mini gene-modified autologous T cells (TMG-T) as the novel aAPC. Using this modified IVS protocol, we successfully generated TIL cultures specifically reactive to mKRAS (G12V). We believe that autologous TMG-T cells provide a reliable source of autologous APC to expand a rare population of neoantigen-specific T cells in TILs.
引用
收藏
页码:1301 / 1313
页数:13
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