Specific members of the Jun protein family regulate collagenase expression in response to various extracellular stimuli.

P Angel, M Karin
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Abstract

The transcription factor AP1 which regulates expression of collagenase in response to various extracellular signals is a multimeric complex composed of members of the Jun- and Fos families. To examine the biological role of the various components in signal transduction we analyzed the expression of two of them (cJun, JunB) and collagenase in response to phorbol esters, cAMP and TGF-beta. While all three genes are induced by phorbol ester and TGF-beta only JunB is induced by cAMP. In contrast expression of cJun and collagenase is reduced by cAMP indicating that cJun and JunB are not coordinately regulated. In addition JunB is not an efficient activator of the cJun and collagenase promoters although both cJun and JunB exhibit similar DNA binding properties, indicating that the differences in biological activity is due to differences in their activation domains. Our results imply that enhanced expression of collagenase (and cJun) depends on the activation of cJun. Expression of cJun and collagenase is inhibited under certain conditions of high levels of JunB. This suggests a negative regulatory function of JunB which greatly expands the potential of the Jun protein family in changing the transcription of specific genes involved in triggering complex biological processes.

Jun蛋白家族的特定成员在响应各种细胞外刺激时调节胶原酶的表达。
转录因子AP1是由Jun-和Fos家族成员组成的多聚复合体,它调节胶原酶对各种细胞外信号的表达。为了研究各种成分在信号转导中的生物学作用,我们分析了其中两种成分(cJun, JunB)和胶原酶对磷酯、cAMP和tgf - β的表达。这三个基因都是由佛波酯和tgf - β诱导的,只有JunB是由cAMP诱导的。相反,cJun和胶原酶的表达被cAMP降低,表明cJun和JunB不是协调调节的。此外,尽管cJun和JunB具有相似的DNA结合特性,但JunB并不是cJun和胶原酶启动子的有效激活剂,这表明生物活性的差异是由于它们的激活域不同。我们的结果表明,胶原酶(和cJun)的表达增强取决于cJun的激活。在一定条件下,高水平的JunB抑制了cJun和胶原酶的表达。这表明JunB具有负调控功能,这极大地扩展了Jun蛋白家族在改变参与触发复杂生物过程的特定基因转录方面的潜力。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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