Kee Barbara L, Bain Gretchen, Murre Cornelis
Department of Biology, University of California San Diego, La Jolla, CA 92093, USA.
EMBO J. 2002 Jan 15;21(1-2):103-13. doi: 10.1093/emboj/21.1.103.
Mice that lack the transcription factors encoded by the E2A gene or the receptor for interleukin 7 (IL-7R) have severe overlapping defects in lymphocyte development. Here, we show that E2A proteins are required for the survival of early T-lineage cells; however, they function through a pathway that is distinct from the survival pathway initiated by IL-7R signaling. While E2A proteins are required to suppress caspase 3 activation, ectopic expression of the anti-apoptotic protein Bcl-2 is not sufficient to overcome the lymphopoietic defects observed in the absence of E2A. Remarkably, mice that lack both IL-7Ralpha and E47 display a synergistic decrease in the number of T-cell, NK-cell and multipotent progenitors in the thymus, indicating that these distinct survival pathways converge to promote the development of multipotent lymphoid progenitors.
缺乏由E2A基因编码的转录因子或白细胞介素7受体(IL - 7R)的小鼠在淋巴细胞发育中存在严重的重叠缺陷。在此,我们表明E2A蛋白是早期T细胞系细胞存活所必需的;然而,它们通过一条与IL - 7R信号启动的存活途径不同的途径发挥作用。虽然E2A蛋白是抑制半胱天冬酶3激活所必需的,但抗凋亡蛋白Bcl - 2的异位表达不足以克服在没有E2A的情况下观察到的淋巴细胞生成缺陷。值得注意的是,同时缺乏IL - 7Rα和E47的小鼠胸腺中T细胞、NK细胞和多能祖细胞的数量出现协同减少,这表明这些不同的存活途径汇聚以促进多能淋巴祖细胞的发育。