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在SV40转化细胞处于预分化生长停滞状态的有丝分裂过程中,选择性诱导c-jun和jun-B,而不诱导c-fos或c-myc。

Selective induction of c-jun and jun-B but not c-fos or c-myc during mitogenesis in SV40-transformed cells at the predifferentiation growth arrest state.

作者信息

Wang H, Wang J Y, Johnson L R, Scott R E

机构信息

Department of Pathology, University of Tennessee Medical Center, Memphis.

出版信息

Cell Growth Differ. 1991 Dec;2(12):645-52.

PMID:1667087
Abstract

Insulin has recently been reported to function as a complete mitogen for SV40 large T antigen-transformed 3T3 T-cells, designated CSV3-1, but not for nontransformed 3T3 T-cells (H. Wang and R. E. Scott, J. Cell. Physiol., 147: 102-110, 1991). It is now reported that sodium orthovanadate mimics this effect of insulin. For example, when exposed to 1-5 microM vanadate, most predifferentiation growth-arrested CSV3-1 cells undergo DNA synthesis within 24 h, but neither vanadate nor insulin induces mitogenesis in nontransformed 3T3 T-cells. To investigate the possible mechanisms by which mitogenesis is induced in CSV3-1 cells, the effects of insulin and vanadate on the expression of growth-related genes were examined. Whereas insulin and vanadate had no effect on the expression of c-fos, c-myc, c-jun, jun-B, or ornithine decarboxylase activity in nontransformed 3T3 T-cells, insulin and vanadate showed different effects on the expression of these genes in CSV3-1 cells. Insulin induced a rapid and transient accumulation of c-fos mRNA followed by induction of c-myc, c-jun, jun-B, and ornithine decarboxylase. In contrast, vanadate induced the expression of c-jun, jun-B, and ornithine decarboxylase without inducing c-fos and c-myc. These observations suggest that SV40 large T antigen may play an important role in insulin- and vanadate-induced mitogenesis and that insulin and vanadate may mediate their mitogenic effects by different signal transduction pathways.

摘要

最近有报道称,胰岛素对SV40大T抗原转化的3T3 T细胞(命名为CSV3-1)具有完全促有丝分裂原的功能,但对未转化的3T3 T细胞则无此功能(H. Wang和R. E. Scott,《细胞生理学杂志》,147: 102 - 110,1991)。现在有报道称原钒酸钠可模拟胰岛素的这种作用。例如,当暴露于1 - 5微摩尔钒酸盐时,大多数预分化生长停滞的CSV3-1细胞在24小时内会进行DNA合成,但钒酸盐和胰岛素均不会在未转化的3T3 T细胞中诱导有丝分裂。为了研究在CSV3-1细胞中诱导有丝分裂的可能机制,检测了胰岛素和钒酸盐对生长相关基因表达的影响。胰岛素和钒酸盐对未转化的3T3 T细胞中c-fos、c-myc、c-jun、jun-B或鸟氨酸脱羧酶活性的表达没有影响,但胰岛素和钒酸盐在CSV3-1细胞中对这些基因的表达表现出不同的影响。胰岛素诱导c-fos mRNA快速短暂积累,随后诱导c-myc、c-jun、jun-B和鸟氨酸脱羧酶。相反,钒酸盐诱导c-jun、jun-B和鸟氨酸脱羧酶的表达,但不诱导c-fos和c-myc。这些观察结果表明,SV40大T抗原可能在胰岛素和钒酸盐诱导的有丝分裂中起重要作用,并且胰岛素和钒酸盐可能通过不同的信号转导途径介导它们的促有丝分裂作用。

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Selective induction of c-jun and jun-B but not c-fos or c-myc during mitogenesis in SV40-transformed cells at the predifferentiation growth arrest state.在SV40转化细胞处于预分化生长停滞状态的有丝分裂过程中,选择性诱导c-jun和jun-B,而不诱导c-fos或c-myc。
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