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HAND1转录因子的MEF2依赖性募集导致靶启动子的协同激活。

MEF2-dependent recruitment of the HAND1 transcription factor results in synergistic activation of target promoters.

作者信息

Morin Steves, Pozzulo Gina, Robitaille Lynda, Cross Jay, Nemer Mona

机构信息

Laboratory of Cardiac Growth and Differentiation, Institut de Recherches Cliniques de Montréal (IRCM), Quebec, Canada.

出版信息

J Biol Chem. 2005 Sep 16;280(37):32272-8. doi: 10.1074/jbc.M507640200. Epub 2005 Jul 25.

DOI:10.1074/jbc.M507640200
PMID:16043483
Abstract

HAND proteins are tissue-restricted members of the basic helix-loop-helix transcription factor family that play critical roles in cell differentiation and organogenesis including placental, cardiovascular, and craniofacial development. Nevertheless, the molecular basis underlying the developmental action of HAND proteins remains undefined. Within the embryo, HAND1 is first detected in the developing heart where it becomes restricted to the atrial and left ventricular compartments, a pattern identical to that of the Nppa gene, which encodes atrial natriuretic factor, the major secretory product of the heart. We hereby report that the cardiac atrial natriuretic factor promoter is directly activated by HAND1, making it the first known HAND1 transcriptional target. The action of HAND1 does not require heterodimerization with class I basic helix-loop-helix factors or DNA binding through E-box elements. Instead, HAND1 is recruited to the promoter via physical interaction with MEF2 proteins. MEF2/HAND1 interaction results in synergistic activation of MEF2-dependent promoters, and MEF2 binding sites are sufficient to mediate this synergy. MEF2 binding to DNA is not enhanced in the presence of HAND1. Instead, cooperativity likely results from corecruitment of co-activators such as CREB-binding protein. The related HAND2 protein can also synergize with MEF2. Thus, HAND proteins act as cell-specific developmental co-activators of the MEF2 family of transcription factors. These findings identify a novel mechanism for HAND action in the heart and provide a general paradigm to understand the mechanism of HAND action in organogenesis.

摘要

HAND蛋白是碱性螺旋-环-螺旋转录因子家族中组织限制性成员,在细胞分化和器官形成中发挥关键作用,包括胎盘、心血管和颅面发育。然而,HAND蛋白发育作用的分子基础仍不明确。在胚胎中,HAND1首先在发育中的心脏中被检测到,随后局限于心房和左心室区域,这种模式与Nppa基因相同,Nppa基因编码心钠素,即心脏的主要分泌产物。我们在此报告,心钠素启动子被HAND1直接激活,使其成为首个已知的HAND1转录靶点。HAND1的作用不需要与I类碱性螺旋-环-螺旋因子异二聚化或通过E-box元件结合DNA。相反,HAND1通过与MEF2蛋白的物理相互作用被招募到启动子。MEF2/HAND1相互作用导致MEF2依赖性启动子的协同激活,且MEF2结合位点足以介导这种协同作用。在HAND1存在的情况下,MEF2与DNA的结合并未增强。相反,协同作用可能源于共激活因子如CREB结合蛋白的共同招募。相关的HAND2蛋白也能与MEF2协同作用。因此,HAND蛋白作为MEF2转录因子家族的细胞特异性发育共激活因子。这些发现确定了HAND在心脏中作用的新机制,并为理解HAND在器官形成中作用的机制提供了一个通用范例。

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