Tyr 磷酸酶介导的 P-ERK 抑制可抑制 EIA + v-raf 转化细胞的衰老,矛盾的是,这些细胞以 MEK 依赖的方式受到凋亡保护。
Tyr phosphatase-mediated P-ERK inhibition suppresses senescence in EIA + v-raf transformed cells, which, paradoxically, are apoptosis-protected in a MEK-dependent manner.
机构信息
Dipartimento di Scienze e Tecnologie Biologiche ed Ambientali, Facoltà di Scienze Matematiche Fisiche e Naturali, Università degli Studi del Salento, Lecce, Italy.
出版信息
Neoplasia. 2011 Feb;13(2):120-30. doi: 10.1593/neo.101152.
Activation of the Ras-Raf-extracellular signal-regulated kinase (ERK) pathway causes not only proliferation and suppression of apoptosis but also the antioncogenic response of senescence. How these contrasting effects are reconciled to achieve cell transformation and cancer formation is poorly understood. In a system of two-step carcinogenesis (dedifferentiated PC EIA, transformed PC EIA-polyoma-middle T [PC EIA + Py] and PC EIA-v-raf [PC EIA + raf] cells], v-raf cooperated with EIA by virtue of a strong prosurvival effect, not elicited by Py-middle T, evident toward serum-deprivation-and H(2)O(2)-induced apoptosis. Apoptosis was detected by DNA fragmentation and annexin V staining. The prosurvival function of v-raf was, in part, mitogen-activated protein kinase/ERK kinase (MEK)-dependent, as shown by pharmacological MEK inhibition. The MEK-dependent antiapoptotic effect of v-raf was exerted despite a lower level of P-ERK1/2 in EIA + raf cells with respect to EIA + Py/EIA cells, which was dependent on a high tyrosine phosphatase activity, as shown by orthovanadate blockade. An ERK1/2 tyrosine phosphatase was likely involved. The high tyrosine phosphatase activity was instrumental to the complete suppression of senescence, detected by β-galactosidase activity, because tyrosine phosphatase blockade induced senescence in EIA + raf but not in EIA + Py cells. High tyrosine phosphatase activity and evasion from senescence were confirmed in an anaplastic thyroid cancer cell line. Therefore, besides EIA, EIA + raf cells suppress senescence through a new mechanism, namely, phosphatase-mediated P-ERK1/2 inhibition, but, paradoxically, retain the oncogenic effects of the Raf-ERK pathway. We propose that the survival effect of Raf is not a function of absolute P-ERK1/2 levels at a given time but is rather dynamically dependent on greater variations after an apoptotic stimulus.
Ras-Raf-细胞外信号调节激酶(ERK)通路的激活不仅导致增殖和抑制细胞凋亡,还导致肿瘤抑制反应的衰老。这些相反的作用如何协调以实现细胞转化和癌症形成,目前还了解甚少。在两步致癌(去分化 PC EIA、转化 PC EIA-多瘤中 T [PC EIA + Py] 和 PC EIA-v-raf [PC EIA + raf] 细胞)系统中,v-raf 通过强大的生存促进作用与 EIA 合作,而这种作用不是由 Py-中 T 引起的,在血清剥夺和 H(2)O(2)诱导的细胞凋亡中明显。通过 DNA 片段化和膜联蛋白 V 染色检测细胞凋亡。v-raf 的促生存作用部分依赖于丝裂原激活蛋白激酶/ERK 激酶(MEK),如通过药理学 MEK 抑制所示。v-raf 的 MEK 依赖性抗凋亡作用尽管在 EIA + raf 细胞中 P-ERK1/2 的水平低于 EIA + Py/EIA 细胞,但由于高酪氨酸磷酸酶活性,这种作用得以发挥,如通过正钒酸盐阻断所示。可能涉及一种 ERK1/2 酪氨酸磷酸酶。高酪氨酸磷酸酶活性对于通过β-半乳糖苷酶活性检测到的衰老的完全抑制是必不可少的,因为酪氨酸磷酸酶阻断诱导 EIA + raf 但不诱导 EIA + Py 细胞衰老。在间变性甲状腺癌细胞系中证实了高酪氨酸磷酸酶活性和逃避衰老。因此,除了 EIA,EIA + raf 细胞还通过一种新的机制抑制衰老,即通过磷酸酶介导的 P-ERK1/2 抑制,但矛盾的是,保留了 Raf-ERK 通路的致癌作用。我们提出,Raf 的生存作用不是给定时间内绝对 P-ERK1/2 水平的功能,而是动态地依赖于凋亡刺激后的更大变化。
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