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镰状细胞血管阻塞:由白细胞黏附驱动的异型多细胞聚集。

Sickle cell vasoocclusion: heterotypic, multicellular aggregations driven by leukocyte adhesion.

作者信息

Frenette Paul S

机构信息

Mount Sinai School of Medicine, Department of Medicine (Hematology), New York, New York 10029, USA.

出版信息

Microcirculation. 2004 Mar;11(2):167-77.

Abstract

Homozygous expression of sickle beta-globin alters the function of blood cells and the endothelium, producing a wide spectrum of clinical manifestations. Intravital microscopy studies in sickle cell mice suggest that vasoocclusion is a complex, sequential, multistep phenomenon involving (1) endothelial activation by sickle erythrocyte (SSRBC), (2) leukocyte (WBC) adhesion to the endothelium, and (3) the direct interaction between SSRBCs and adherent WBCs, which leads to reduced blood flow and tissue ischemia. Each of these steps represents a potentially useful therapeutic target. The identification of molecular determinants mediating vasoocclusion will provide new strategies for the prevention and treatment of this debilitating illness.

摘要

镰状β-珠蛋白的纯合表达会改变血细胞和内皮细胞的功能,从而产生一系列广泛的临床表现。对镰状细胞小鼠进行的活体显微镜研究表明,血管阻塞是一种复杂的、连续的、多步骤现象,涉及:(1)镰状红细胞(SSRBC)激活内皮细胞;(2)白细胞(WBC)黏附于内皮细胞;(3)SSRBC与黏附的WBC之间的直接相互作用,这会导致血流减少和组织缺血。这些步骤中的每一步都代表了一个潜在的有效治疗靶点。鉴定介导血管阻塞的分子决定因素将为预防和治疗这种使人衰弱的疾病提供新策略。

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