A Disease Mechanism Underlying Bleeding in Wiskott-Aldrich Syndrome

IF 3 Q2 Medicine Clinical Medicine Insights-Blood Disorders Pub Date : 2008-01-01 DOI:10.4137/CMBD.S536
S. Tsuboi
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引用次数: 1

Abstract

The Wiskott-Aldrich Syndrome (WAS) is an × chromosome-linked immunodeficiency disorder. The most common symptom in WAS is bleeding. Several clinical investigations indicate that low platelet counts and defective platelet aggregation are the major causes of bleeding in WAS patients. However, the molecular bases underlying these defects are unclear. This study focuses on the molecular mechanism of defective platelet aggregation of WAS patients. The gene responsible for WAS encodes WAS protein (WASP). The mutations or deletion of WASP causes various functional defects in hematopoietic cells. We previously showed that binding of WASP to calcium- and integrin-binding protein (CIB) is required for activation of platelet integrin, αIIbβ3. I here demonstrate that blocking WASP binding to CIB reduces binding of talin to the β3 cytoplasmic tail, resulting in impaired activation of αIIbβ3. Impaired αIIbβ3 activation causes defective platelet aggregation, resulting in bleeding. This finding suggests a potential disease mechanism underlying bleeding seen in WAS patients.
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Wiskott-Aldrich综合征出血的发病机制
Wiskott-Aldrich综合征(WAS)是一种x染色体相关免疫缺陷疾病。WAS最常见的症状是出血。一些临床研究表明,血小板计数低和血小板聚集缺陷是WAS患者出血的主要原因。然而,这些缺陷背后的分子基础尚不清楚。本研究主要探讨WAS患者血小板聚集缺陷的分子机制。负责WAS的基因编码WAS蛋白(WASP)。WASP的突变或缺失会导致造血细胞的各种功能缺陷。我们之前的研究表明,血小板整合素αIIbβ3的激活需要WASP与钙和整合素结合蛋白(CIB)的结合。我在这里证明阻断WASP与CIB的结合减少了talin与β3细胞质尾部的结合,导致αIIbβ3的激活受损。αIIbβ3活化受损导致血小板聚集缺陷,导致出血。这一发现提示了WAS患者出血的潜在疾病机制。
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来源期刊
CiteScore
3.70
自引率
0.00%
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0
审稿时长
8 weeks
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