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与原发性血小板增多症相关的钙网织蛋白突变体的结构和动态差异。

Structural and Dynamic Differences between Calreticulin Mutants Associated with Essential Thrombocythemia.

机构信息

Université Paris Cité and Université de la Réunion and Université des Antilles, INSERM, BIGR, DSIMB Bioinformatics Team, F-75014 Paris, France.

出版信息

Biomolecules. 2023 Mar 10;13(3):509. doi: 10.3390/biom13030509.

Abstract

Essential thrombocythemia (ET) is a blood cancer. ET is characterized by an overproduction of platelets that can lead to thrombosis formation. Platelet overproduction occurs in megakaryocytes through a signaling pathway that could involve JAK2, MPL, or CALR proteins. CALR mutations are associated with 25-30% of ET patients; CALR variants must be dimerized to induce ET. We classified these variants into five classes named A to E; classes A and B are the most frequent classes in patients with ET. The dynamic properties of these five classes using structural models of CALR's C-domain were analyzed using molecular dynamics simulations. Classes A, B, and C are associated with frameshifts in the C-domain. Their dimers can be stable only if a disulfide bond is formed; otherwise, the two monomers repulse each other. Classes D and E cannot be stable as dimers due to the absence of disulfide bonds. Class E and wild-type CALR have similar dynamic properties. These results suggest that the disulfide bond newly formed in classes A, B, and C may be essential for the pathogenicity of these variants. They also underline that class E cannot be directly related to ET but corresponds to human polymorphisms.

摘要

原发性血小板增多症(ET)是一种血液癌症。ET 的特征是血小板过度生成,这可能导致血栓形成。巨核细胞中的血小板过度生成是通过一种信号通路发生的,该通路可能涉及 JAK2、MPL 或 CALR 蛋白。CALR 突变与 25-30%的 ET 患者有关;CALR 变体必须二聚化才能诱导 ET。我们将这些变体分为 A 到 E 五类;A 类和 B 类是 ET 患者中最常见的两类。使用 CALR C 结构域的结构模型分析了这五类的动态特性,采用分子动力学模拟。A 类、B 类和 C 类与 C 结构域的移码突变有关。只有形成二硫键,它们的二聚体才能稳定;否则,两个单体就会相互排斥。由于缺乏二硫键,D 类和 E 类不能稳定地形成二聚体。E 类和野生型 CALR 具有相似的动力学特性。这些结果表明,A、B 和 C 类中新形成的二硫键可能对这些变体的致病性至关重要。它们还强调 E 类不能直接与 ET 相关,而是对应于人类多态性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bef2/10046389/27d0e87b17f4/biomolecules-13-00509-g001.jpg

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