Zhoujie Ding, Maree Hagan, Feng Yan, Nick W Y Schroer, Jack Polmear, Kim L Good-Jacobson, Alexandra R Dvorscek, Catherine Pitt, Kristy O'Donnell, Stephen L Nutt, Dimitra Zotos, Craig McKenzie, Danika L Hill, Marcus J Robinson, Isaak Quast, Frank Koentgen, David M Tarlinton
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引用次数: 0
摘要
增殖标记物 Ki67 在细胞周期中具有维持有丝分裂染色体形态和异染色质组织的关键功能,这表明它在需要严格控制细胞周期的发育过程中具有潜在作用。在这里,我们发现尽管生殖力和器官形成正常,但种系缺乏 Ki67 会导致外周 B 淋巴细胞和 T 淋巴细胞出现实质性缺陷。这并不是由于细胞增殖受损,而是由于早期淋巴造血在特定阶段发生了抗原受体基因重排。我们发现,Ki67 是正常的全染色质可及性所必需的,它涉及 B 细胞淋巴细胞形成过程中检查点阶段关键基因的调控区域。与此相一致,在 Ki67 缺失的情况下,Rag1 的 mRNA 表达减少,基因重排的效率降低。编码有效重排的免疫球蛋白重链和轻链的转基因补充了 Ki67 的缺乏,完全恢复了早期 B 细胞的发育。总之,这些结果确定了 Ki67 在淋巴细胞形成过程中对体细胞抗原受体基因重排的独特贡献。
Ki67 deficiency impedes chromatin accessibility and BCR gene rearrangement.
The proliferation marker Ki67 has been attributed critical functions in maintaining mitotic chromosome morphology and heterochromatin organization during the cell cycle, indicating a potential role in developmental processes requiring rigid cell-cycle control. Here, we discovered that despite normal fecundity and organogenesis, germline deficiency in Ki67 resulted in substantial defects specifically in peripheral B and T lymphocytes. This was not due to impaired cell proliferation but rather to early lymphopoiesis at specific stages where antigen-receptor gene rearrangements occurred. We identified that Ki67 was required for normal global chromatin accessibility involving regulatory regions of genes critical for checkpoint stages in B cell lymphopoiesis. In line with this, mRNA expression of Rag1 was diminished and gene rearrangement was less efficient in the absence of Ki67. Transgenes encoding productively rearranged immunoglobulin heavy and light chains complemented Ki67 deficiency, completely rescuing early B cell development. Collectively, these results identify a unique contribution from Ki67 to somatic antigen-receptor gene rearrangement during lymphopoiesis.
期刊介绍:
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