B 淋巴细胞中 TNFR 相关因子 2 缺乏导致小鼠慢性淋巴细胞白血病/小淋巴细胞淋巴瘤。
TNFR-associated factor 2 deficiency in B lymphocytes predisposes to chronic lymphocytic leukemia/small lymphocytic lymphoma in mice.
机构信息
Universidad Autónoma de Madrid, Madrid, Spain.
出版信息
J Immunol. 2012 Jul 15;189(2):1053-61. doi: 10.4049/jimmunol.1200814. Epub 2012 Jun 18.
We have previously shown that transgenic (tg) mice expressing in B lymphocytes both BCL-2 and a TNFR-associated factor 2 (TRAF2) mutant lacking the really interesting new gene and zinc finger domains (TRAF2DN) develop small lymphocytic lymphoma and chronic lymphocytic leukemia with high incidence (Zapata et al. 2004. Proc. Nat. Acad. Sci. USA 101: 16600-16605). Further analysis of the expression of TRAF2 and TRAF2DN in purified B cells demonstrated that expression of both endogenous TRAF2 and tg TRAF2DN was negligible in Traf2DN-tg B cells compared with wild-type mice. This was the result of proteasome-dependent degradation, and rendered TRAF2DN B cells as bona fide TRAF2-deficient B cells. Similar to B cells with targeted Traf2 deletion, Traf2DN-tg mice show expanded marginal zone B cell population and have constitutive p100 NF-κB2 processing. Also, TRAF3, X-linked inhibitor of apoptosis, and Bcl-X(L) expression levels were increased, whereas cellular inhibitors of apoptosis 1 and 2 levels were drastically reduced compared with those found in wild-type B cells. Moreover, consistent with previous results, we also show that TRAF2 was required for efficient JNK and ERK activation in response to CD40 engagement. However, TRAF2 was deleterious for BCR-mediated activation of these kinases. In contrast, TRAF2 deficiency had no effect on CD40-mediated p38 MAPK activation but significantly reduced BCR-mediated p38 activation. Finally, we further confirm that TRAF2 was required for CD40-mediated proliferation, but its absence relieved B cells of the need for B cell activating factor for survival. Altogether, our results suggest that TRAF2 deficiency cooperates with BCL-2 in promoting chronic lymphocytic leukemia/small lymphocytic lymphoma in mice, possibly by specifically enforcing marginal zone B cell accumulation, increasing X-linked inhibitor of apoptosis expression, and rendering B cells independent of B cell activating factor for survival.
我们之前已经表明,在 B 淋巴细胞中同时表达 BCL-2 和缺乏真正有趣的新基因和锌指结构域的 TNFR 相关因子 2(TRAF2)突变体(TRAF2DN)的转基因(tg)小鼠会发展出小淋巴细胞淋巴瘤和慢性淋巴细胞白血病,发病率很高(Zapata 等人,2004 年。Proc。Nat。Acad。Sci。USA 101:16600-16605)。进一步分析纯化 B 细胞中 TRAF2 和 TRAF2DN 的表达表明,与野生型小鼠相比,Traf2DN-tg B 细胞中内源性 TRAF2 和 tg TRAF2DN 的表达可忽略不计。这是蛋白酶体依赖性降解的结果,使 TRAF2DN B 细胞成为真正的 TRAF2 缺陷 B 细胞。与靶向 Traf2 缺失的 B 细胞类似,Traf2DN-tg 小鼠显示出扩展的边缘区 B 细胞群体,并具有组成性的 p100 NF-κB2 加工。此外,TRAF3、X 连锁凋亡抑制剂和 Bcl-X(L)的表达水平增加,而细胞凋亡抑制剂 1 和 2 的水平与野生型 B 细胞相比则大幅降低。此外,与之前的结果一致,我们还表明 TRAF2 是 CD40 结合后 JNK 和 ERK 激活所必需的。然而,TRAF2 对 BCR 介导的这些激酶的激活是有害的。相反,TRAF2 缺乏对 CD40 介导的 p38 MAPK 激活没有影响,但显著降低了 BCR 介导的 p38 激活。最后,我们进一步证实 TRAF2 是 CD40 介导的增殖所必需的,但它的缺失使 B 细胞免于对 B 细胞激活因子的生存需要。总之,我们的结果表明,TRAF2 缺乏与 BCL-2 一起促进了小鼠慢性淋巴细胞白血病/小淋巴细胞淋巴瘤的发生,可能通过特异性地促进边缘区 B 细胞的积累、增加 X 连锁凋亡抑制剂的表达,并使 B 细胞在生存上不再依赖于 B 细胞激活因子。
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