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首页> 外文期刊>The Journal of biological chemistry >Disruption of Serine/Threonine Protein Phosphatase 5 (PP5:PPP5c) in Mice Reveals a Novel Role for PP5 in the Regulation of Ultraviolet Light-induced Phosphorylation of Serine/Threonine Protein Kinase Chk1 (CHEK1)
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Disruption of Serine/Threonine Protein Phosphatase 5 (PP5:PPP5c) in Mice Reveals a Novel Role for PP5 in the Regulation of Ultraviolet Light-induced Phosphorylation of Serine/Threonine Protein Kinase Chk1 (CHEK1)

机译:小鼠中丝氨酸/苏氨酸蛋白磷酸酶5(PP5:PPP5C)的破坏显示了PP5在调节紫外线磷酸溶解的丝氨酸/苏氨酸蛋白激酶激酶CHK1(CHEK1)中的新作用

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PP5 is a ubiquitously expressed Ser/Thr protein phosphatase. High levels of PP5 have been observed in human cancers, and constitutive PP5 overexpression aids tumor progression in mouse models of tumor development. However, PP5 is highly conserved among species, and the roles of PP5 in normal tissues are not clear. Here, to help evaluate the biological actions of PP5, a Cre/loxP-conditional mouse line was generated. In marked contrast to the early embryonic lethality associated with the genetic disruption of other PPP family phosphatases (e.g. PP2A and PP4), intercrosses with mouse lines that ubiquitously express Cre recombinase starting early in development (e.g. MeuCre40 and ACTB-Cre) produced viable and fertile PP5-deficient mice. Phenotypic differences caused by the total disruption of PP5 were minor, suggesting that small molecule inhibitors of PP5 will not have widespread systemic toxicity. Examination of roles for PP5 in fibroblasts generated from PP5-deficient embryos (PP5?/? mouse embryonic fibroblasts) confirmed some known roles and identified new actions for PP5. PP5?/? mouse embryonic fibroblasts demonstrated increased sensitivity to UV light, hydroxyurea, and camptothecin, which are known activators of ATR (ataxia-telangiectasia and Rad3-related) kinase. Further study revealed a previously unrecognized role for PP5 downstream of ATR activation in a UV light-induced response. The genetic disruption of PP5 is associated with enhanced and prolonged phosphorylation of a single serine (Ser-345) on Chk1, increased phosphorylation of the p53 tumor suppressor protein (p53) at serine 18, and increased p53 protein levels. A comparable role for PP5 in the regulation of Chk1 phosphorylation was also observed in human cells.
机译:PP5是普遍地表达的Ser / Thr蛋白磷酸酶。在人类癌症中观察到高水平的PP5,并且组成型PP5过表达助剂涉及肿瘤发育小鼠模型中的肿瘤进展。然而,PP5在物种之间受到高度保守,并且PP5在正常组织中的作用尚不清楚。这里,为了帮助评估PP5的生物学作用,产生CRE / LOXP条件鼠标线。与与其他PPP家族磷酸酶(例如PP2A和PP4)相关的早期胚胎致致对性的对比,与小鼠线的间断,以普遍存在的开发早期(例如MEUCRE40和ACTB-CRE)产生可行和肥沃的CRE重组酶PP5缺乏小鼠。由PP5的总破坏引起的表型差异是轻微的,表明PP5的小分子抑制剂不会具有广泛的全身毒性。检查从PP5缺陷胚胎产生的成纤维细胞中PP5的角色(PP5?/?小鼠胚胎成纤维细胞)证实了一些已知的角色并确定了PP5的新作用。 pp5?/?小鼠胚胎成纤维细胞显示对紫外线,羟基脲和喜树碱的敏感性增加,这些敏感性是ATR(共济失调 - 毛细管扩张和RAD3相关)激酶的已知活化剂。进一步的研究表明,在UV光诱导的反应中,在ATR激活下游的PP5中预先发现的作用。 PP5的遗传破坏与CHK1上的单个丝氨酸(Ser-345)的增强和延长的磷酸化相关,在丝氨酸18下增加P53肿瘤抑制蛋白(P53)的磷酸化,并增加P53蛋白质水平。在人体细胞中也观察到在CHK1磷酸化调节中PP5的比较作用。

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