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癌相关变异表达和 CIZ1 与细胞周期蛋白 A1 在分化的雄性生殖细胞中的相互作用。

Cancer-associated variant expression and interaction of CIZ1 with cyclin A1 in differentiating male germ cells.

机构信息

Leeds Institute of Genetics, Health and Therapeutics (LIGHT), University of Leeds, Leeds, UK.

出版信息

J Cell Sci. 2012 May 15;125(Pt 10):2466-77. doi: 10.1242/jcs.101097. Epub 2012 Feb 24.

DOI:10.1242/jcs.101097
PMID:22366453
Abstract

CIZ1 is a nuclear-matrix-associated DNA replication factor unique to higher eukaryotes, for which alternatively spliced isoforms have been associated with a range of disorders. In vitro, the CIZ1 N-terminus interacts with cyclin E and cyclin A at distinct sites, enabling functional cooperation with cyclin-A-Cdk2 to promote replication initiation. C-terminal sequences anchor CIZ1 to fixed sites on the nuclear matrix, imposing spatial constraint on cyclin-dependent kinase activity. Here we demonstrate that CIZ1 is predominantly expressed as a predicted full-length product throughout mouse development, consistent with a ubiquitous role in cell and tissue renewal. CIZ1 is expressed in proliferating stem cells of the testis, but is notably downregulated following commitment to differentiation. Significantly, CIZ1 is re-expressed at high levels in non-proliferative spermatocytes before meiotic division. Sequence analysis identifies at least seven alternatively spliced variants, including a dominant cancer-associated form and a set of novel isoforms. Furthermore, we show that in these post-replicative cells, CIZ1 interacts with germ-cell-specific cyclin A1, which has been implicated in the repair of DNA double-strand breaks. Consistent with this role, antibody depletion of CIZ1 reduces the capacity for testis extract to repair digested plasmid DNA in vitro. Together, the data imply post-replicative roles for CIZ1 in germ cell differentiation that might include meiotic recombination - a process intrinsic to genome stability and diversification.

摘要

CIZ1 是一种与高等真核生物独特相关的核基质相关 DNA 复制因子,其不同剪接异构体与多种疾病相关。在体外,CIZ1 的 N 端与细胞周期蛋白 E 和细胞周期蛋白 A 在不同的位点相互作用,使与细胞周期蛋白-A-Cdk2 的功能合作能够促进复制起始。C 端序列将 CIZ1 锚定在核基质的固定位点上,对细胞周期蛋白依赖性激酶活性施加空间限制。在这里,我们证明 CIZ1 在整个小鼠发育过程中主要表达为预测的全长产物,这与它在细胞和组织更新中的普遍作用一致。CIZ1 在睾丸的增殖干细胞中表达,但在向分化方向分化后明显下调。值得注意的是,在减数分裂之前,CIZ1 在非增殖性精母细胞中高水平重新表达。序列分析确定了至少七种不同的剪接变体,包括一种显性癌症相关形式和一组新的异构体。此外,我们还表明,在这些复制后细胞中,CIZ1 与生殖细胞特异性细胞周期蛋白 A1 相互作用,后者与 DNA 双链断裂的修复有关。与这一作用一致,CIZ1 抗体耗尽会降低睾丸提取物在体外修复消化质粒 DNA 的能力。综上所述,数据表明 CIZ1 在生殖细胞分化中的复制后作用,可能包括减数分裂重组,这是基因组稳定性和多样化的内在过程。

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