Mechanisms of Organ Damage and Novel Treatment Targets in AL Amyloidosis

IF 0.9 Q4 HEMATOLOGY Hemato Pub Date : 2022-01-12 DOI:10.3390/hemato3010005
F. Lavatelli
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引用次数: 3

Abstract

The deposition of amyloid light chains (LCs) in target sites translates into tissue damage and organ dysfunction. Clinical and experimental advances have cast new light on the pathophysiology of damage in AL amyloidosis. The currently accepted view is that, besides the alterations caused by fibrillar deposits in the extracellular space, direct proteotoxicity exerted by prefibrillar LC species is an important pathogenic factor. As our knowledge on the pathological species and altered cellular pathways grows, novel potential therapeutic strategies to prevent or reduce damage can be rationally explored. Complementing chemotherapy with approaches aimed at disrupting the deposited fibrils and stabilizing prefibrillar amyloidogenic LC may allow halting or even reverting damage in target sites. This review recapitulates the current knowledge and the most recent acquisitions regarding the mechanisms of organ damage in AL amyloidosis, with special emphasis on the heart, and will provide a critical discussion on possible novel treatment targets.
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AL淀粉样变性的器官损伤机制及新的治疗靶点
淀粉样蛋白轻链(LC)在靶位点的沉积转化为组织损伤和器官功能障碍。临床和实验的进展为AL淀粉样变性损伤的病理生理学提供了新的线索。目前公认的观点是,除了由细胞外空间的原纤维沉积引起的改变外,原纤维前LC物种产生的直接蛋白毒性也是一个重要的致病因素。随着我们对病理物种和改变的细胞途径的了解不断增长,可以合理探索预防或减少损伤的新的潜在治疗策略。用旨在破坏沉积的原纤维和稳定原纤前淀粉样变性LC的方法来补充化疗,可以阻止甚至恢复靶位点的损伤。这篇综述概述了目前关于AL淀粉样变性器官损伤机制的知识和最新研究成果,特别强调心脏,并将对可能的新治疗靶点进行批判性讨论。
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来源期刊
CiteScore
1.30
自引率
0.00%
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0
审稿时长
11 weeks
期刊最新文献
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