Schönwasser D C, Marais R M, Marshall C J, Parker P J
Imperial Cancer Research Fund, London, United Kingdom.
Mol Cell Biol. 1998 Feb;18(2):790-8. doi: 10.1128/MCB.18.2.790.
Phorbol ester treatment of quiescent Swiss 3T3 cells leads to cell proliferation, a response thought to be mediated by protein kinase C (PKC), the major cellular receptor for this class of agents. We demonstrate here that this proliferation is dependent on the activation of the extracellular signal-regulated kinase/mitogen-activated protein kinase (ERK/MAPK) cascade. It is shown that dominant-negative PKC-alpha inhibits stimulation of the ERK/MAPK pathway by phorbol esters in Cos-7 cells, demonstrating a role for PKC in this activation. To assess the potential specificity of PKC isotypes mediating this process, constitutively active mutants of six PKC isotypes (alpha, beta, delta, epsilon, eta, and zeta) were employed. Transient transfection of these PKC mutants into Cos-7 cells showed that members of all three groups of PKC (conventional, novel, and atypical) are able to activate p42 MAPK as well as its immediate upstream activator, the MAPK/ERK kinase MEK-1. At the level of Raf, the kinase that phosphorylates MEK-1, the activation cascade diverges; while conventional and novel PKCs (isotypes alpha and eta) are potent activators of c-Raf1, atypical PKC-zeta cannot increase c-Raf1 activity, stimulating MEK by an independent mechanism. Stimulation of c-Raf1 by PKC-alpha and PKC-eta was abrogated for RafCAAX, which is a membrane-localized, partially active form of c-Raf1. We further established that activation of Raf is independent of phosphorylation at serine residues 259 and 499. In addition to activation, we describe a novel Raf desensitization induced by PKC-alpha, which acts to prevent further Raf stimulation by growth factors. The results thus demonstrate a necessary role for PKC and p42 MAPK activation in 12-O-tetradecanoylphorbol-13-acetate induced mitogenesis and provide evidence for multiple PKC controls acting on this MAPK cascade.
佛波酯处理静止的瑞士3T3细胞可导致细胞增殖,这种反应被认为是由蛋白激酶C(PKC)介导的,PKC是这类药物的主要细胞受体。我们在此证明,这种增殖依赖于细胞外信号调节激酶/丝裂原活化蛋白激酶(ERK/MAPK)级联反应的激活。结果表明,显性负性PKC-α可抑制佛波酯对Cos-7细胞中ERK/MAPK途径的刺激,证明PKC在这种激活中起作用。为了评估介导这一过程的PKC同工型的潜在特异性,我们使用了六种PKC同工型(α、β、δ、ε、η和ζ)的组成型活性突变体。将这些PKC突变体瞬时转染到Cos-7细胞中表明,所有三组PKC(传统型、新型和非典型型)的成员都能够激活p42 MAPK及其直接上游激活剂MAPK/ERK激酶MEK-1。在Raf水平上,即磷酸化MEK-1的激酶,激活级联发生分歧;虽然传统型和新型PKC(同工型α和η)是c-Raf1的有效激活剂,但非典型PKC-ζ不能增加c-Raf1的活性,而是通过独立机制刺激MEK。PKC-α和PKC-η对c-Raf1的刺激被RafCAAX消除,RafCAAX是c-Raf1的一种膜定位的、部分活性形式。我们进一步确定,Raf的激活独立于丝氨酸残基259和499处的磷酸化。除了激活作用外,我们还描述了一种由PKC-α诱导的新型Raf脱敏作用,它可防止生长因子对Raf的进一步刺激。因此,这些结果证明了PKC和p42 MAPK激活在12-O-十四烷酰佛波醇-13-乙酸酯诱导的有丝分裂中的必要作用,并为作用于该MAPK级联反应的多种PKC调控提供了证据。
