Thrombomodulin (p.Cys537Stop) is released from cells by an unusual membrane insertion/leakage mechanism.

IF 7.4 1区 医学 Q1 HEMATOLOGY Blood advances Pub Date : 2024-11-12 DOI:10.1182/bloodadvances.2024013546
Clara Bernard, Andréa Pin, Nathalie Hézard, Vincent Ernest, Céline Falaise, Camille Roze, Stéphanie Simoncini, Romaric Lacroix, Pierre-Emmanuel Morange, Franck Peiretti
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Abstract

Abstract: Expression of the thrombomodulin (TM) variant c.1611C>A (p.Cys537Stop) leads to the synthesis of a protein with no cytoplasmic tail and a transmembrane domain shortened by 3 amino acids (TM536). However, little is known regarding the release mechanism and properties of TM536. Using umbilical vein endothelial cells and peripheral blood-derived endothelial colony-forming cells from a heterozygous carrier of the TM536 variant as well as overexpression cell models, we demonstrated that TM536 is released from cells by an unusual mechanism. First, TM536 is inserted into the endoplasmic reticulum (ER) membrane, then, because of the low hydrophobicity of its intramembrane domain, it escapes from it and follows the conventional secretory pathway to be released into the extracellular compartment without the involvement of proteolysis. This particular secretion mechanism yields a soluble TM536, which is poorly modified by chondroitin sulfate glycosaminoglycan compared with conventionally secreted soluble forms of TM, and therefore has a suboptimal capacity to mediate thrombin-dependent activation of protein C (PC). We also showed that TM536 cellular trafficking was altered, with retention in the early secretory pathway and increased sensitivity to ER-associated degradation. As expected, activation of ER-associated degradation increased TM536 degradation and reduced its release. The expression of TM536 at the cell surface was low, and its distribution in lipid raft-like membrane microdomains was altered, resulting in low thrombin-dependent PC activation on the cell surface.

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血栓调节蛋白(p.Cys537Stop)通过一种不寻常的膜插入/泄漏机制从细胞中释放出来。
血栓调节蛋白变体 c.1611C>A(p.Cys537Stop)的表达会导致合成一种没有胞质尾部、跨膜结构域缩短 3 个氨基酸(TM536)的蛋白质。人们对 TM536 的释放机制和特性知之甚少。我们利用来自 TM536 变异杂合子携带者的脐静脉内皮细胞和外周血来源的内皮集落形成细胞以及过表达细胞模型,证明了 TM536 是通过不寻常的机制从细胞中释放出来的。首先,TM536 被插入内质网膜,然后,由于其膜内结构域的疏水性较低,TM536 从内质网膜中逃脱,并遵循传统的分泌途径释放到细胞外,而不参与蛋白水解。这种特殊的分泌机制产生了一种可溶性 TM536,与血栓调节蛋白的常规分泌可溶性形式相比,这种 TM536 被硫酸软骨素氨基糖修饰的程度很低,因此它介导凝血酶依赖性激活蛋白 C 的能力也不理想。正如预期的那样,激活内质网相关降解会增加 TM536 的降解并减少其释放。TM536 在细胞表面的表达量较低,其在脂筏状膜微域中的分布也发生了改变,从而导致细胞表面凝血酶依赖性 PC 活化率较低。
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来源期刊
Blood advances
Blood advances Medicine-Hematology
CiteScore
12.70
自引率
2.70%
发文量
840
期刊介绍: Blood Advances, a semimonthly medical journal published by the American Society of Hematology, marks the first addition to the Blood family in 70 years. This peer-reviewed, online-only, open-access journal was launched under the leadership of founding editor-in-chief Robert Negrin, MD, from Stanford University Medical Center in Stanford, CA, with its inaugural issue released on November 29, 2016. Blood Advances serves as an international platform for original articles detailing basic laboratory, translational, and clinical investigations in hematology. The journal comprehensively covers all aspects of hematology, including disorders of leukocytes (both benign and malignant), erythrocytes, platelets, hemostatic mechanisms, vascular biology, immunology, and hematologic oncology. Each article undergoes a rigorous peer-review process, with selection based on the originality of the findings, the high quality of the work presented, and the clarity of the presentation.
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