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人 junctophilin-2 蛋白核定位和相分离的序列决定因素。

Sequence determinants of human junctophilin-2 protein nuclear localization and phase separation.

机构信息

Department of Pharmaceutical Sciences, North Dakota State University, 1401 Albrecht Blvd, Fargo, ND, 58102, USA.

Department of Pharmaceutical Sciences, North Dakota State University, 1401 Albrecht Blvd, Fargo, ND, 58102, USA.

出版信息

Biochem Biophys Res Commun. 2021 Jul 23;563:79-84. doi: 10.1016/j.bbrc.2021.05.078. Epub 2021 May 29.

DOI:10.1016/j.bbrc.2021.05.078
PMID:34062390
Abstract

Junctophilin-2 (JPH2) was conventionally considered as a structural membrane binding protein. Recently, it was shown that proteolytically truncated mouse JPH2 variants are imported into nucleus to exert alternative functions. However, the intranuclear behaviors of human JPH2 (hJPH2) and underlying molecular determinants have not been explored. Here, we demonstrate that full-length hJPH2 is imported into nucleus in human cells by two nuclear localization signals (NLSs), including a newly discovered one at the C-terminus. Importantly, unlike the JPH2 N-terminal truncation which diffuses throughout the nucleus, full-length hJPH2 forms nuclear bodies behaving like liquid-liquid phase separated droplets that are separated from chromatin. The C-terminal transmembrane domain is required for the formation of hJPH2 droplets. Oxidation mimicking substitution of residues C678 and M679 augments the formation of hJPH2 nuclear droplets, suggesting nuclear hJPH2 liquid-liquid phase separation could be modulated by oxidative stress. Mutation A405D, which introduces a negatively charged residue into an intrinsic disordered region (IDR) of hJPH2, turns liquid-like droplets into amyloid-like aggregates. Depletion of an Alanine Rich Region in the IDR recapitulates the liquid-amyloid phase transition. The MORN repeat regions of hJPH2 encodes intrinsic tendency to form amyloid-like structure. Together, these data revealed the novel intrinsic properties of hJPH2 to form nuclear liquid droplets, and identified critical functional domains encoding these properties. We propose that hJPH2 droplets could function as membrane-less organelles participating in nuclear regulatory processes.

摘要

衔接蛋白-2(Junctophilin-2,JPH2)通常被认为是一种结构性的膜结合蛋白。最近的研究表明,经蛋白水解截断的小鼠 JPH2 变体可被导入细胞核以发挥替代功能。然而,尚未探索人源 JPH2(hJPH2)的核内行为及其潜在的分子决定因素。在此,我们证明全长 hJPH2 可通过两个核定位信号(NLS)被导入人细胞的细胞核,其中包括新发现的 C 端 NLS。重要的是,与 JPH2 N 端截断不同,全长 hJPH2 形成的核体类似于液-液相分离的液滴,与染色质分离。C 端跨膜结构域对于 hJPH2 液滴的形成是必需的。模拟氧化取代残基 C678 和 M679 可增强 hJPH2 核液滴的形成,表明核 hJPH2 的液-液相分离可能受到氧化应激的调节。将一个带负电荷的残基引入 hJPH2 无规卷曲结构域的 A405D 突变将液态液滴转化为淀粉样纤维聚集物。无规卷曲结构域中的丙氨酸丰富区的缺失可再现液-胶相转变。hJPH2 的 MORN 重复区编码形成淀粉样结构的内在倾向。综上所述,这些数据揭示了 hJPH2 形成核液滴的新的内在特性,并确定了编码这些特性的关键功能域。我们提出 hJPH2 液滴可作为无膜细胞器参与核调节过程。

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引用本文的文献

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Junctophilin-2 is a double-stranded RNA-binding protein that regulates cardiomyocyte-autonomous innate immune response.衔接蛋白-2 是一种双链 RNA 结合蛋白,可调节心肌细胞自主固有免疫反应。
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Membrane Curvature Promotes ER-PM Contact Formation via Junctophilin-EHD Interactions.膜曲率通过连接蛋白- EHD相互作用促进内质网-质膜接触的形成。
bioRxiv. 2024 Jun 30:2024.06.29.601287. doi: 10.1101/2024.06.29.601287.
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The Sarcoplasmic Reticulum of Skeletal Muscle Cells: A Labyrinth of Membrane Contact Sites.
骨骼肌细胞的肌浆网:膜接触位点的迷宫。
Biomolecules. 2022 Mar 23;12(4):488. doi: 10.3390/biom12040488.
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The role of junctophilin proteins in cellular function.衔接蛋白在细胞功能中的作用。
Physiol Rev. 2022 Jul 1;102(3):1211-1261. doi: 10.1152/physrev.00024.2021. Epub 2022 Jan 10.
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Calpain-2 specifically cleaves Junctophilin-2 at the same site as Calpain-1 but with less efficacy.钙蛋白酶-2 特异性地在与钙蛋白酶-1 相同的位点切割连接蛋白-2,但效率较低。
Biochem J. 2021 Oct 15;478(19):3539-3553. doi: 10.1042/BCJ20210629.