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蛋白磷酸酶2A(PPP2R1B)的β亚基中甘氨酸90位点向天冬氨酸的改变与乳腺癌相关,并导致蛋白质功能缺陷。

The glycine 90 to aspartate alteration in the Abeta subunit of PP2A (PPP2R1B) associates with breast cancer and causes a deficit in protein function.

作者信息

Esplin Edward D, Ramos Purita, Martinez Bobbie, Tomlinson Gail E, Mumby Marc C, Evans Glen A

机构信息

Department of Pharmacology, University of Texas Southwestern Medical Center, Dallas, 75390-9041, USA.

出版信息

Genes Chromosomes Cancer. 2006 Feb;45(2):182-90. doi: 10.1002/gcc.20284.

Abstract

Mutations of the PPP2R1B gene, which encodes the Abeta scaffolding subunit of serine/threonine protein phosphatase 2A (PP2A), have been identified in several types of cancer including lung and breast carcinoma. One of these mutations results in an alteration of glycine 90 to aspartic acid (G90D), which has been found in both tumor and genomic DNA, raising the possibility that it is associated with an increased risk for cancer. A novel microarray-based technology was used to screen for this single-nucleotide polymorphism in 387 cancer patients and 329 control individuals. These data were used for case-control and family-based comparisons in order to study the association of this polymorphism with susceptibility to lung carcinoma, breast carcinoma, and acute lymphoblastic leukemia. The frequency of the G90D polymorphism in breast cancer patients was significantly higher in cases (3%) than in controls (0.3%). The wild-type Abeta subunit interacted with the B56gamma (PPP2R5C), PR72 (PPP2R3A), and PR48 subunits of PP2A but did not interact with the B55alpha (PPP2R2A), B56alpha (PPP2R5A), or B56beta (PPP2R5B) regulatory subunits in an in vitro binding assay. The G90D alteration inhibited the interaction of Abeta with the B56gamma subunit but had no effect on binding to the PR72 subunit. These results provide evidence that the G90D alteration of the Abeta subunit of PP2A is associated with a low frequency of breast carcinoma and that the role of this alteration in transformation is likely to involve decreased interaction with the B56gamma regulatory subunit.

摘要

PPP2R1B基因编码丝氨酸/苏氨酸蛋白磷酸酶2A(PP2A)的Aβ支架亚基,该基因的突变已在包括肺癌和乳腺癌在内的多种癌症中被发现。其中一种突变导致甘氨酸90变为天冬氨酸(G90D),在肿瘤和基因组DNA中均已发现,这增加了其与癌症风险增加相关的可能性。一种基于微阵列的新技术被用于在387名癌症患者和329名对照个体中筛查这种单核苷酸多态性。这些数据用于病例对照和基于家系的比较,以研究这种多态性与肺癌、乳腺癌和急性淋巴细胞白血病易感性的关联。乳腺癌患者中G90D多态性的频率在病例组(3%)中显著高于对照组(0.3%)。在体外结合试验中,野生型Aβ亚基与PP2A的B56γ(PPP2R5C)、PR72(PPP2R3A)和PR48亚基相互作用,但不与B55α(PPP2R2A)、B56α(PPP2R5A)或B56β(PPP2R5B)调节亚基相互作用。G90D改变抑制了Aβ与B56γ亚基的相互作用,但对与PR72亚基的结合没有影响。这些结果提供了证据,表明PP2A的Aβ亚基的G90D改变与乳腺癌的低发生率相关,并且这种改变在转化中的作用可能涉及与B56γ调节亚基的相互作用减少。

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