Lawlor M A, Rotwein P
Molecular Medicine Division, Oregon Health Sciences University, Portland, Oregon 97201-3098, USA.
J Cell Biol. 2000 Dec 11;151(6):1131-40. doi: 10.1083/jcb.151.6.1131.
Peptide growth factors control diverse cellular functions by regulating distinct signal transduction pathways. In cultured myoblasts, insulin-like growth factors (IGFs) stimulate differentiation and promote hypertrophy. IGFs also maintain muscle cell viability. We previously described C2 skeletal muscle lines lacking expression of IGF-II. These cells did not differentiate, but underwent progressive apoptotic death when incubated in differentiation medium. Viability could be sustained and differentiation enabled by IGF analogues that activated the IGF-I receptor; survival was dependent on stimulation of phosphatidylinositol 3-kinase (PI3-kinase). We now find that IGF action promotes myoblast survival through two distinguishable PI3-kinase-regulated pathways that culminate in expression of the cyclin-dependent kinase inhibitor, p21. Incubation with IGF-I or transfection with active PI3-kinase led to rapid induction of MyoD and p21, and forced expression of either protein maintained viability in the absence of growth factors. Ectopic expression of MyoD induced p21, and inhibition of p21 blocked MyoD-mediated survival, thus defining one PI3-kinase-dependent pathway as leading first to MyoD, and then to p21 and survival. Unexpectedly, loss of MyoD expression did not impede IGF-mediated survival, revealing a second pathway involving activation by PI3-kinase of Akt, and subsequent induction of p21. Since inhibition of p21 caused death even in the presence of IGF-I, these results establish a central role for p21 as a survival factor for muscle cells. Our observations also define a MyoD-independent pathway for regulating p21 in muscle, and demonstrate that distinct mechanisms help ensure appropriate expression of this key protein during differentiation.
肽生长因子通过调节不同的信号转导途径来控制多种细胞功能。在培养的成肌细胞中,胰岛素样生长因子(IGFs)刺激分化并促进肥大。IGFs还维持肌肉细胞的活力。我们之前描述了缺乏IGF-II表达的C2骨骼肌细胞系。这些细胞不会分化,但在分化培养基中孵育时会经历渐进性凋亡死亡。能够激活IGF-I受体的IGF类似物可以维持细胞活力并使其分化;细胞存活依赖于磷脂酰肌醇3-激酶(PI3-激酶)的刺激。我们现在发现,IGF的作用通过两条可区分的PI3-激酶调节途径促进成肌细胞存活,这两条途径最终导致细胞周期蛋白依赖性激酶抑制剂p21的表达。用IGF-I孵育或用活性PI3-激酶转染导致MyoD和p21的快速诱导,并且在没有生长因子的情况下,这两种蛋白的强制表达均可维持细胞活力。MyoD的异位表达诱导p21,而抑制p21则阻断MyoD介导的细胞存活,从而将一条PI3-激酶依赖性途径定义为首先导致MyoD,然后导致p21和细胞存活。出乎意料的是,MyoD表达的缺失并不妨碍IGF介导的细胞存活,这揭示了另一条途径,该途径涉及PI3-激酶对Akt的激活以及随后p21的诱导。由于即使在存在IGF-I的情况下抑制p21也会导致细胞死亡,因此这些结果确立了p21作为肌肉细胞存活因子的核心作用。我们的观察结果还定义了一条在肌肉中调节p21的不依赖MyoD的途径,并证明了不同的机制有助于确保在分化过程中该关键蛋白的适当表达。