Transmembrane thiol isomerase TMX1 counterbalances the effect of ERp46 to inhibit platelet activation and integrin αIIbβ3 function

IF 3.4 3区 医学 Q2 HEMATOLOGY Research and Practice in Thrombosis and Haemostasis Pub Date : 2024-07-01 DOI:10.1016/j.rpth.2024.102524
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引用次数: 0

Abstract

Background

Previous studies have shown that thiol isomerases such as ERp46 positively regulate platelet function by reducing integrin αIIbβ3 disulfides, and the transmembrane thiol isomerase TMX1 negatively regulates integrin αIIbβ3 activation. However, whether and how the positive and negative thiol isomerases interact with each other and their interactions participate in platelet activation remain unknown.

Objectives

To investigate whether and how TMX1 regulates the effect of ERp46 on platelet function.

Methods

Using ERp46- and TMX1-deficient platelets, anti-TMX1 antibody, and wild-type TMX1 (TMX1-CPAC, TMX1-SS) and inactive TMX1 (TMX1-SPAS, TMX1-OO) proteins, we studied the antagonistic effect of TMX1 on ERp46 in platelet aggregation, clot retraction, and integrin αIIbβ3 signaling. The underlying mechanisms were further determined using thiol labeling, reductase activity, and other assays.

Results

Anti-TMX1 antibody and TMX1-OO reversed the decreased aggregation of ERp46-deficient platelets induced by thrombin, convulxin, and U46619. Anti-TMX1 antibody reversed the attenuated integrin αIIbβ3 function of ERp46-deficient platelets. TMX1 inhibited ERp46 reductase activity in a concentration-dependent manner. TMX1 oxidized thiols of ERp46 and those of integrin αIIbβ3 generated by ERp46. Moreover, TMX1 deficiency increased free thiols of ERp46 in platelets, which was reversed by the addition of wild-type TMX1 protein. Besides, anti-TMX1 antibody increased free thiols of ERp46 in wild-type activated platelets.

Conclusion

TMX1 not only oxidizes integrin αIIbβ3 disulfides that are reduced by ERp46 but also directly oxidizes ERp46 to suppress its reduction of integrin αIIbβ3. Thus, TMX1 is critical for maintaining platelets in a quiescent state and counterbalancing the effect of ERp46 to prevent platelet overactivation.

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跨膜硫醇异构酶 TMX1 可抵消 ERp46 对血小板活化和整合素 αIIbβ3 功能的抑制作用
背景先前的研究表明,ERp46等硫醇异构酶通过减少整合素αⅡbβ3的二硫化物来正向调节血小板功能,而跨膜硫醇异构酶TMX1则负向调节整合素αⅡbβ3的活化。目的研究 TMX1 是否以及如何调节 ERp46 对血小板功能的影响。方法利用ERp46和TMX1缺陷血小板、抗TMX1抗体、野生型TMX1(TMX1-CPAC、TMX1-SS)和非活性TMX1(TMX1-SPAS、TMX1-OO)蛋白,研究TMX1在血小板聚集、血块回缩和整合素αⅡbβ3信号传导中对ERp46的拮抗作用。结果 抗 TMX1 抗体和 TMX1-OO 逆转了凝血酶、旋覆花素和 U46619 诱导的 ERp46 缺失血小板聚集的降低。抗 TMX1 抗体可逆转 ERp46 缺陷血小板整合素 αⅡbβ3 功能的减弱。TMX1 以浓度依赖的方式抑制 ERp46 还原酶的活性。TMX1 氧化了 ERp46 和 ERp46 产生的整合素 αIIbβ3 的硫醇。此外,缺乏 TMX1 会增加血小板中 ERp46 的游离硫醇,而加入野生型 TMX1 蛋白则会逆转这种情况。结论 TMX1 不仅能氧化被 ERp46 还原的整合素 αIIbβ3 二硫化物,还能直接氧化 ERp46 以抑制其对整合素 αIIbβ3 的还原。因此,TMX1 对维持血小板处于静止状态和抵消 ERp46 的作用以防止血小板过度活化至关重要。
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来源期刊
CiteScore
5.60
自引率
13.00%
发文量
212
审稿时长
7 weeks
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