缺血/再灌注在镰状细胞贫血中的多效性作用。
The multifaceted role of ischemia/reperfusion in sickle cell anemia.
出版信息
J Clin Invest. 2020 Mar 2;130(3):1062-1072. doi: 10.1172/JCI133639.
Abstract
Sickle cell anemia is a unique disease dominated by hemolytic anemia and vaso-occlusive events. The latter trigger a version of ischemia/reperfusion (I/R) pathobiology that is singular in its origin, cyclicity, complexity, instability, perpetuity, and breadth of clinical consequences. Specific clinical features are probably attributable to local I/R injury (e.g., stroke syndromes) or remote organ injury (e.g., acute chest syndrome) or the systematization of inflammation (e.g., multifocal arteriopathy). Indeed, by fashioning an underlying template of endothelial dysfunction and vulnerability, the robust inflammatory systematization no doubt contributes to all sickle pathology. In this Review, we highlight I/R-targeting therapeutics shown to improve microvascular blood flow in sickle transgenic mice undergoing I/R, and we suggest how such insights might be translated into human therapeutic strategies.
摘要
镰状细胞贫血是一种独特的疾病,以溶血性贫血和血管阻塞事件为主。后者引发的缺血/再灌注(I/R)病理生物学具有独特的起源、周期性、复杂性、不稳定性、持久性和广泛的临床后果。特定的临床特征可能归因于局部 I/R 损伤(例如,中风综合征)或远处器官损伤(例如,急性胸部综合征)或炎症的系统化(例如,多灶性血管病)。事实上,通过形成内皮功能障碍和脆弱性的潜在模板,强大的炎症系统化无疑有助于所有镰状细胞病的发生。在这篇综述中,我们强调了针对 I/R 的治疗方法,这些方法已被证明可改善经历 I/R 的镰状细胞转基因小鼠的微血管血流,我们还提出了如何将这些见解转化为人类治疗策略。
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