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一类新的抑制模块对于酵母转录激活因子Hap1的血红素调节至关重要。

A new class of repression modules is critical for heme regulation of the yeast transcriptional activator Hap1.

作者信息

Hach A, Hon T, Zhang L

机构信息

Department of Biochemistry, NYU Medical Center, New York, New York 10016, USA.

出版信息

Mol Cell Biol. 1999 Jun;19(6):4324-33. doi: 10.1128/MCB.19.6.4324.

Abstract

Heme plays key regulatory roles in numerous molecular and cellular processes for systems that sense or use oxygen. In the yeast Saccharomyces cerevisiae, oxygen sensing and heme signaling are mediated by heme activator protein 1 (Hap1). Hap1 contains seven heme-responsive motifs (HRMs): six are clustered in the heme domain, and a seventh is near the activation domain. To determine the functional role of HRMs and to define which parts of Hap1 mediate heme regulation, we carried out a systematic analysis of Hap1 mutants with various regions deleted or mutated. Strikingly, the data show that HRM1 to -6, located in the previously designated Hap1 heme domain, have little impact on heme regulation. All seven HRMs are dispensable for Hap1 repression in the absence of heme, but HRM7 is required for Hap1 activation by heme. More importantly, we show that a novel class of repression modules-RPM1, encompassing residues 245 to 278; RPM2, encompassing residues 1061 to 1185; and RPM3, encompassing residues 203 to 244-is critical for Hap1 repression in the absence of heme. Biochemical analysis indicates that RPMs mediate Hap1 repression, at least partly, by the formation of a previously identified higher-order complex termed the high-molecular-weight complex (HMC), while HRMs mediate heme activation by permitting heme binding and the disassembly of the HMC. These findings provide significant new insights into the molecular interactions critical for Hap1 repression in the absence of heme and Hap1 activation by heme.

摘要

血红素在众多感知或利用氧气的系统的分子和细胞过程中发挥着关键的调节作用。在酿酒酵母中,氧气感知和血红素信号传导由血红素激活蛋白1(Hap1)介导。Hap1包含七个血红素反应基序(HRM):六个聚集在血红素结构域中,第七个靠近激活结构域。为了确定HRM的功能作用并定义Hap1的哪些部分介导血红素调节,我们对缺失或突变了不同区域的Hap1突变体进行了系统分析。令人惊讶的是,数据表明位于先前指定的Hap1血红素结构域中的HRM1至 -6对血红素调节影响很小。在没有血红素的情况下,所有七个HRM对于Hap1的抑制都是可有可无的,但HRM7是血红素激活Hap1所必需的。更重要的是,我们表明一类新的抑制模块——RPM1,包含245至278位残基;RPM2,包含1061至1185位残基;以及RPM3,包含203至244位残基——对于在没有血红素的情况下Hap1的抑制至关重要。生化分析表明,RPM至少部分地通过形成先前鉴定的称为高分子量复合物(HMC)的高阶复合物来介导Hap1的抑制,而HRM通过允许血红素结合和HMC的解离来介导血红素激活。这些发现为在没有血红素的情况下Hap1抑制和血红素激活Hap1所必需的分子相互作用提供了重要的新见解。

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