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有证据表明,ras癌基因编码的p21蛋白通过激活蛋白激酶C诱导卵母细胞成熟。

Evidence that the ras oncogene-encoded p21 protein induces oocyte maturation via activation of protein kinase C.

作者信息

Chung D L, Brandt-Rauf P W, Weinstein I B, Nishimura S, Yamaizumi Z, Murphy R B, Pincus M R

机构信息

Department of Chemistry, New York University, NY 10003.

出版信息

Proc Natl Acad Sci U S A. 1992 Mar 1;89(5):1993-6. doi: 10.1073/pnas.89.5.1993.

Abstract

The ras oncogene-encoded p21 protein is known to induce cell maturation of Xenopus laevis oocytes and malignant transformation of NIH 3T3 mouse fibroblasts. The pathways involved in oocytes and NIH 3T3 cells appear to be similar to one another. For example, in both cases, the ras p21-induced cellular events involve increased intracellular levels of the second messengers diacylglycerol and inositol phosphates, the former of which activates protein kinase C (PKC). To investigate the pathway of ras-induced oocyte maturation, we have explored the relationship between p21 protein and PKC. We show that the maturation signal from oncogenic p21 microinjected into Xenopus oocytes is completely blocked by the relatively specific PKC inhibitor CGP 41251, a staurosporine analogue that selectively inhibits PKC, but not by an inactive analogue of staurosporine, CGP 42700. Microinjection of purified PKC or of phorbol ester induces maturation of oocytes. PKC-induced maturation is inhibited by CGP 41251 but not by CGP 42700. Maturation induced by microinjected PKC is also not inhibited by two specific anti-p21 agents, the inactivating anti-p21 monoclonal antibody Y13-259 and the amino acid derivative azatyrosine. Both of these agents block p21-induced cell maturation. These results suggest that ras effects depend upon the action of PKC, whose activation is an event that occurs downstream of p21 in the maturation signal pathway.

摘要

已知由原癌基因ras编码的p21蛋白可诱导非洲爪蟾卵母细胞的细胞成熟以及NIH 3T3小鼠成纤维细胞的恶性转化。卵母细胞和NIH 3T3细胞中涉及的信号通路似乎彼此相似。例如,在这两种情况下,ras p21诱导的细胞事件都涉及细胞内第二信使二酰基甘油和肌醇磷酸水平的升高,前者可激活蛋白激酶C(PKC)。为了研究ras诱导的卵母细胞成熟途径,我们探讨了p21蛋白与PKC之间的关系。我们发现,注入非洲爪蟾卵母细胞的致癌p21产生的成熟信号被相对特异性的PKC抑制剂CGP 41251(一种选择性抑制PKC的星形孢菌素类似物)完全阻断,但未被星形孢菌素的无活性类似物CGP 42700阻断。显微注射纯化的PKC或佛波酯可诱导卵母细胞成熟。PKC诱导的成熟被CGP 41251抑制,但未被CGP 42700抑制。显微注射PKC诱导的成熟也未被两种特异性抗p21剂(失活的抗p21单克隆抗体Y13 - 259和氨基酸衍生物氮杂酪氨酸)抑制。这两种试剂均可阻断p21诱导的细胞成熟。这些结果表明,ras的作用取决于PKC的作用,PKC的激活是成熟信号通路中发生在p21下游的一个事件。

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