富含半胱氨酸的肠蛋白2是骨骼肌分化和金属稳态的铜响应调节因子。

IF 4 2区 生物学 Q1 GENETICS & HEREDITY PLoS Genetics Pub Date : 2024-12-05 eCollection Date: 2024-12-01 DOI:10.1371/journal.pgen.1011495
Odette Verdejo-Torres, David C Klein, Lorena Novoa-Aponte, Jaime Carrazco-Carrillo, Denzel Bonilla-Pinto, Antonio Rivera, Arpie Bakhshian, Fa'alataitaua M Fitisemanu, Martha L Jiménez-González, Lyra Flinn, Aidan T Pezacki, Antonio Lanzirotti, Luis Antonio Ortiz Frade, Christopher J Chang, Juan G Navea, Crysten E Blaby-Haas, Sarah J Hainer, Teresita Padilla-Benavides
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引用次数: 0

摘要

铜(Cu)对呼吸、神经递质合成、氧化应激反应和转录调节至关重要,其失衡会导致神经、认知和肌肉疾病。在这里,我们展示了一种新的cu结合蛋白(Cu-BP)在哺乳动物转录调节中的作用,特别是在小鼠原代成肌细胞的骨骼肌分化中。利用同步加速器x射线荧光-质谱技术,我们鉴定出小鼠富含半胱氨酸的肠道蛋白2 (mCrip2)是一个关键的Cu-BP,在细胞核和细胞质中都丰富。mCrip2以高亲和力结合2 ~ 4个Cu+离子,呈现有限的氧化还原电位。CRISPR/ cas9介导的mCrip2缺失损伤了肌肉生成,可能是由于细胞中的Cu积累。CUT&RUN和转录组分析揭示了它与基因启动子(包括MyoD1和金属硫蛋白)的关联,这表明mCrip2具有新的cu响应性调节作用。我们的工作描述了mCrip2在骨骼肌分化和金属稳态中的重要性,扩大了对成肌细胞cu网络的理解。铜(Cu)对各种细胞过程至关重要,包括呼吸和应激反应,但不平衡会导致严重的健康问题。本研究揭示了一种新的cu结合蛋白(Cu-BP)参与了原代成肌细胞的肌肉发育。利用无偏倚金属蛋白组学技术和高通量测序,我们发现mCrip2是细胞核和细胞质中发现的关键Cu-BP。mCrip2可以结合4个Cu+离子,并且具有有限的氧化还原电位。使用CRISPR/Cas9删除mCrip2破坏了Cu积累导致的肌肉形成。进一步的分析表明,mCrip2调节肌肉分化所必需的MyoD1和金属硫蛋白等基因的表达,以响应铜的补充。这项研究强调了mCrip2在肌肉发育和金属稳态中的重要性,为细胞中的cu网络提供了新的见解。
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Cysteine Rich Intestinal Protein 2 is a copper-responsive regulator of skeletal muscle differentiation and metal homeostasis.

Copper (Cu) is essential for respiration, neurotransmitter synthesis, oxidative stress response, and transcription regulation, with imbalances leading to neurological, cognitive, and muscular disorders. Here we show the role of a novel Cu-binding protein (Cu-BP) in mammalian transcriptional regulation, specifically on skeletal muscle differentiation using murine primary myoblasts. Utilizing synchrotron X-ray fluorescence-mass spectrometry, we identified murine cysteine-rich intestinal protein 2 (mCrip2) as a key Cu-BP abundant in both nuclear and cytosolic fractions. mCrip2 binds two to four Cu+ ions with high affinity and presents limited redox potential. CRISPR/Cas9-mediated deletion of mCrip2 impaired myogenesis, likely due to Cu accumulation in cells. CUT&RUN and transcriptome analyses revealed its association with gene promoters, including MyoD1 and metallothioneins, suggesting a novel Cu-responsive regulatory role for mCrip2. Our work describes the significance of mCrip2 in skeletal muscle differentiation and metal homeostasis, expanding understanding of the Cu-network in myoblasts. Copper (Cu) is essential for various cellular processes, including respiration and stress response, but imbalances can cause serious health issues. This study reveals a new Cu-binding protein (Cu-BP) involved in muscle development in primary myoblasts. Using unbiased metalloproteomic techniques and high throughput sequencing, we identified mCrip2 as a key Cu-BP found in cell nuclei and cytoplasm. mCrip2 binds up to four Cu+ ions and has a limited redox potential. Deleting mCrip2 using CRISPR/Cas9 disrupted muscle formation due to Cu accumulation. Further analyses showed that mCrip2 regulates the expression of genes like MyoD1, essential for muscle differentiation, and metallothioneins in response to copper supplementation. This research highlights the importance of mCrip2 in muscle development and metal homeostasis, providing new insights into the Cu-network in cells.

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PLoS Genetics
PLoS Genetics GENETICS & HEREDITY-
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期刊介绍: PLOS Genetics is run by an international Editorial Board, headed by the Editors-in-Chief, Greg Barsh (HudsonAlpha Institute of Biotechnology, and Stanford University School of Medicine) and Greg Copenhaver (The University of North Carolina at Chapel Hill). Articles published in PLOS Genetics are archived in PubMed Central and cited in PubMed.
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