Novel mechanisms of MITF regulation identified in a mouse suppressor screen.

IF 6.5 1区生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY

EMBO Reports Pub Date : 2024-10-01 Epub Date: 2024-08-21 DOI:10.1038/s44319-024-00225-3

Hong Nhung Vu, Matti Már Valdimarsson, Sara Sigurbjörnsdóttir, Kristín Bergsteinsdóttir, Julien Debbache, Keren Bismuth, Deborah A Swing, Jón H Hallsson, Lionel Larue, Heinz Arnheiter, Neal G Copeland, Nancy A Jenkins, Petur O Heidarsson, Eiríkur Steingrímsson

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引用次数: 0

Abstract

MITF, a basic Helix-Loop-Helix Zipper (bHLHZip) transcription factor, plays vital roles in melanocyte development and functions as an oncogene. We perform a genetic screen for suppressors of the Mitf-associated pigmentation phenotype in mice and identify an intragenic Mitf mutation that terminates MITF at the K316 SUMOylation site, leading to loss of the C-end intrinsically disordered region (IDR). The resulting protein is more nuclear but less stable than wild-type MITF and retains DNA-binding ability. As a dimer, it can translocate wild-type and mutant MITF partners into the nucleus, improving its own stability thus ensuring nuclear MITF supply. smFRET analysis shows interactions between K316 SUMOylation and S409 phosphorylation sites across monomers; these interactions largely explain the observed effects. The recurrent melanoma-associated E318K mutation in MITF, which affects K316 SUMOylation, also alters protein regulation in concert with S409. This suggests that residues K316 and S409 of MITF are impacted by SUMOylation and phosphorylation, respectively, mediating effects on nuclear localization and stability through conformational changes. Our work provides a novel mechanism of genetic suppression, and an example of how apparently deleterious mutations lead to normal phenotypes.

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在小鼠抑制因子筛选中发现新的 MITF 调节机制。

MITF是一种基本螺旋-环-螺旋拉链（bHLHZip）转录因子，在黑色素细胞发育过程中发挥着重要作用，同时也是一种致癌基因。我们对小鼠Mitf相关色素沉着表型的抑制因子进行了基因筛选，发现了一种基因内Mitf突变，该突变在K316 SUMOylation位点终止了MITF，导致C端内紊乱区（IDR）缺失。由此产生的蛋白质比野生型 MITF 更具有核功能，但稳定性较差，并保留了 DNA 结合能力。smFRET 分析表明，K316 SUMOylation 和 S409 磷酸化位点之间存在跨单体的相互作用；这些相互作用在很大程度上解释了所观察到的效应。MITF 中反复出现的黑色素瘤相关 E318K 突变会影响 K316 SUMOylation，也会与 S409 一起改变蛋白质的调节。这表明，MITF的K316和S409残基分别受到SUMO化和磷酸化的影响，通过构象变化介导对核定位和稳定性的影响。我们的工作提供了一种新的遗传抑制机制，也提供了一个例子，说明表面上看似有害的突变是如何导致正常表型的。

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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来源期刊

EMBO Reports 生物-生化与分子生物学

CiteScore

11.20

自引率

1.30%

发文量

267

审稿时长

1 months

期刊介绍： EMBO Reports is a scientific journal that specializes in publishing research articles in the fields of molecular biology, cell biology, and developmental biology. The journal is known for its commitment to publishing high-quality, impactful research that provides novel physiological and functional insights. These insights are expected to be supported by robust evidence, with independent lines of inquiry validating the findings. The journal's scope includes both long and short-format papers, catering to different types of research contributions. It values studies that: Communicate major findings: Articles that report significant discoveries or advancements in the understanding of biological processes at the molecular, cellular, and developmental levels. Confirm important findings: Research that validates or supports existing knowledge in the field, reinforcing the reliability of previous studies. Refute prominent claims: Studies that challenge or disprove widely accepted ideas or hypotheses in the biosciences, contributing to the correction and evolution of scientific understanding. Present null data: Papers that report negative results or findings that do not support a particular hypothesis, which are crucial for the scientific process as they help to refine or redirect research efforts. EMBO Reports is dedicated to maintaining high standards of scientific rigor and integrity, ensuring that the research it publishes contributes meaningfully to the advancement of knowledge in the life sciences. By covering a broad spectrum of topics and encouraging the publication of both positive and negative results, the journal plays a vital role in promoting a comprehensive and balanced view of scientific inquiry.