揭示 GPIbα 的脱落。

IF 3.1 3区 医学 Q2 HEMATOLOGY
Current Opinion in Hematology Pub Date : 2024-09-01 Epub Date: 2024-05-09 DOI:10.1097/MOH.0000000000000826
Caitlin Debaene, Hendrik B Feys, Katrijn R Six
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引用次数: 0

摘要

审查目的:自 20 世纪 80 年代末以来,人们一直在研究外结构域脱落问题。丰富的血小板特异性 GPIbα 受体被 ADAM17 裂解,从而释放出称为糖萼蛋白的外结构域。本综述将探讨糖钙蛋白作为血小板周转和储存病变的终末阶段标志物的作用,并将考虑其在止血以外过程中作为效应物的潜在功能:最近的研究结果:糖凝集素已被描述为血小板衰老、周转和储存病变的标志物,但由于其诊断价值不具鉴别性,因此未被常规用于临床。抑制糖钙蛋白脱落可改善输血后的恢复,但对其潜在的止血效果却知之甚少。在生理环境下,GPIbα脱落仅限于细胞内的 GPIbα 受体亚群,这表明脱落或甘钙化素的作用超出了止血范畴。摘要:迄今为止,所有证据都表明甘钙化素是血小板衰老的终末期生物标志物,也是血小板清除的潜在触发因素。GPIbα 在止血以外领域的大量相互作用伙伴为研究糖萼蛋白的特定效应功能提供了新的可能性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Shedding light on GPIbα shedding.

Purpose of review: Ectodomain shedding has been investigated since the late 1980s. The abundant and platelet specific GPIbα receptor is cleaved by ADAM17 resulting in the release of its ectodomain called glycocalicin. This review will address the role of glycocalicin as an end-stage marker of platelet turnover and storage lesion and will consider a potential function as effector in processes beyond hemostasis.

Recent findings: Glycocalicin has been described as a marker for platelet senescence, turnover and storage lesion but is not routinely used in a clinical setting because its diagnostic value is nondiscriminatory. Inhibition of glycocalicin shedding improves posttransfusion recovery but little is known (yet) about potential hemostatic improvements. In physiological settings, GPIbα shedding is restricted to the intracellular GPIbα receptor subpopulation suggesting a role for shedding or glycocalicin beyond hemostasis.

Summary: So far, all evidence represents glycocalicin as an end-stage biomarker of platelet senescence and a potential trigger for platelet clearance. The extensive list of interaction partners of GPIbα in fields beyond hemostasis opens new possibilities to investigate specific effector functions of glycocalicin.

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来源期刊
CiteScore
6.60
自引率
3.10%
发文量
78
审稿时长
6-12 weeks
期刊介绍: ​​​​​​​​Current Opinion in Hematology is an easy-to-digest bimonthly journal covering the most interesting and important advances in the field of hematology. Its hand-picked selection of editors ensure the highest quality selection of unbiased review articles on themes from nine key subject areas, including myeloid biology, Vascular biology, hematopoiesis and erythroid system and its diseases.
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