PPM1D 的遗传变异和突变控制着对 DNA 损伤的反应。
Genetic variants and mutations of PPM1D control the response to DNA damage.
机构信息
Department of Pediatrics, Rutgers Cancer Institute of New Jersey, Rutgers University, New Brunswick, NJ, USA.
出版信息
Cell Cycle. 2013 Aug 15;12(16):2656-64. doi: 10.4161/cc.25694. Epub 2013 Jul 18.
Abstract
The Wip1 phosphatase is an oncogene that is overexpressed in a variety of primary human cancers. We were interested in identifying genetic variants that could change Wip1 activity. We identified 3 missense SNPs of the human Wip1 phosphatase, L120F, P322Q, and I496V confer a dominant-negative phenotype. On the other hand, in primary human cancers, PPM1D mutations commonly result in a gain-of-function phenotype, leading us to identify a hot-spot truncating mutation at position 525. Surprisingly, we also found a significant number of loss-of-function mutations of PPM1D in primary human cancers, both in the phosphatase domain and in the C terminus. Thus, PPM1D has evolved to generate genetic variants with lower activity, potentially providing a better fitness for the organism through suppression of multiple diseases. In cancer, however, the situation is more complex, and the presence of both activating and inhibiting mutations requires further investigation to understand their contribution to tumorigenesis.
摘要
Wip1 磷酸酶是一种癌基因,在多种原发性人类癌症中过表达。我们有兴趣确定能够改变 Wip1 活性的遗传变异。我们鉴定了人 Wip1 磷酸酶的 3 个错义 SNP,L120F、P322Q 和 I496V,它们赋予显性负表型。另一方面,在原发性人类癌症中,PPM1D 突变通常导致获得性功能表型,这导致我们在位置 525 鉴定出一个热点截断突变。令人惊讶的是,我们还在原发性人类癌症中发现了大量 PPM1D 的失活功能突变,既有在磷酸酶结构域内的,也有在 C 末端的。因此,PPM1D 已经进化出具有较低活性的遗传变异,可能通过抑制多种疾病为生物体提供更好的适应性。然而,在癌症中,情况更加复杂,激活和抑制突变的存在需要进一步研究,以了解它们对肿瘤发生的贡献。
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