Src家族激酶活性是kit介导的丝裂原活化蛋白(MAP)激酶激活所必需的,然而,功能性视网膜母细胞瘤蛋白的缺失使得MAP激酶激活对于小细胞肺癌细胞的生长是不必要的。

C Bondzi, J Litz, P Dent, G W Krystal
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引用次数: 0

摘要

小细胞肺癌(SCLC)的特征是多种遗传改变,包括视网膜母细胞瘤蛋白(Rb)失活,干细胞因子(SCF)和Kit共表达诱导的几个自分泌环的建立,以及Src家族激酶的异位表达和激活。先前的研究表明,在SCF刺激SCLC细胞后,Lck与Kit相关并被Kit激活。在本研究中,我们已经证明了PP1, Src激酶的药理学抑制剂,阻断了scf介导的丝裂原活化蛋白(MAP)激酶的激活,但它也抑制Kit的激活。然而,MAP激酶激活比Kit激活对PP1的影响更敏感。过表达Lck降低了MAP激酶对PP1激活的敏感性,但没有改变Kit激活的敏感性,这表明Lck在scf介导的MAP激酶激活中起作用。诱导表达显性负Lck以剂量依赖的方式抑制MAP激酶激活,这证实了Src家族激酶活性是scf诱导的MAP激酶激活所必需的。然而,尽管MAP激酶受到抑制,表达显性负Lck的细胞的生长不受影响。PD 98059对MAP激酶通路的抑制也不影响生长,但对MAP/细胞外信号调节激酶激酶抑制剂的敏感性可以通过表达野生型Rb部分恢复。因此,只有在Rb表达缺失的情况下,MAP激酶激活对于SCLC的生长似乎是必不可少的。这些数据表明,SCF/Kit自分泌环,通过激活Lck和随后的MAP激酶,以及Rb的突变失活,导致SCLC发病过程中G1-S期检查点调节的丧失。此外,数据表明,在已建立的SCLC细胞系中,Kit启动的增殖信号转导是由经典的MAP激酶途径以外的途径介导的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Src family kinase activity is required for Kit-mediated mitogen-activated protein (MAP) kinase activation, however loss of functional retinoblastoma protein makes MAP kinase activation unnecessary for growth of small cell lung cancer cells.

Small cell lung cancer (SCLC) is characterized by multiple genetic alterations that include inactivation of the retinoblastoma protein (Rb), the establishment of several autocrine loops including that induced by coexpression of stem cell factor (SCF) and Kit, and the ectopic expression and activation of Src family kinases. Previous studies have shown that Lck associates with, and becomes activated by, Kit after SCF stimulation of SCLC cells. In the present study, we have demonstrated that PP1, a pharmacological inhibitor of Src kinases, blocked SCF-mediated activation of mitogen-activated protein (MAP) kinase, but it also inhibited Kit activation. However, MAP kinase activation was more sensitive than Kit activation to the effects of PP1. Overexpression of Lck reduced the sensitivity of MAP kinase activation to PP1 without altering the sensitivity of Kit activation, which suggested a role for Lck in SCF-mediated MAP kinase activation. Inducible expression of a dominant negative Lck inhibited MAP kinase activation in a dose-dependent manner, which confirmed that Src family kinase activity is required for SCF-induced MAP kinase activation. The growth of cells that expressed dominant negative Lck was unaffected, however, despite the inhibition of MAP kinase. Growth was also unaffected by the inhibition of the MAP kinase pathway using PD 98059, but sensitivity to the MAP/extracellular signal-regulated kinase kinase inhibitor could be partially restored by expression of wild-type Rb. Therefore, MAP kinase activation seems to be dispensable for the growth of SCLC only in the absence of Rb expression. These data suggest that the SCF/Kit autocrine loop, through activation of Lck and subsequently MAP kinase, and the mutational inactivation of Rb contribute to the loss of G1-S phase checkpoint regulation during the pathogenesis of SCLC. Furthermore, the data demonstrate that, in established SCLC cell lines, proliferative signal transduction initiated by Kit is mediated by pathways other than the classic MAP kinase pathway.

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