Redefining Calciphylaxis as a Uniquely Bone Forming Subcutaneous C5b-9-Mediated Microvascular Injury Syndrome Associated With Localized Subcutaneous and Systemic Complement Pathway Activation.

IF 1.1 4区 医学 Q4 DERMATOLOGY
American Journal of Dermatopathology Pub Date : 2024-12-01 Epub Date: 2024-09-17 DOI:10.1097/DAD.0000000000002783
Zachary Wolner, Luna Tello, Taylor Kalomeris, Robert Swerlick, Cynthia M Magro
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引用次数: 0

Abstract

Background: Microvascular thrombosis is key to the pathogenesis of calciphylaxis. C5b-9-mediated microvascular injury reflective of complement pathway activation could be a key pathophysiologic event.

Methods: We conducted a retrospective multicenter study of 24 patients who have had biopsy-supported calciphylaxis from the 2010-2022 data base from Emory where C5b-9 immunohistochemistry (IHC) had not been conducted and the 2019-2023 data base from Cornell where C5b-9 IHC was done as part of the routine calciphylaxis work up. IHC for C5b-9 on lesional biopsy specimens was assessed and correlated with routine light microscopic findings and clinical features.

Results: Most of the patients in our study had uremic calciphylaxis associated with obesity, diabetes, dialysis, hypertension, hyperparathyroidism and elevated serum phosphorus. Most patients did not have defined procoagulant and/or hyperviscosity states. The vascular pathology was predominantly limited to the subcutaneous fat and ranged from a calcific intimal arteriopathy to microvascular thrombosis with endothelial injury with or without endothelial calcification. In most cases (ie, in excess of 80%), there was prominent deposition of C5b-9 within the vasculature including the microvasculature and arteries of the fat at least localized to injured vessels suggesting a causal association. In about 40% of cases, there was evidence of systemic complement pathway activation revealed by concurrent dermal microvascular C5b-9 deposition.

Conclusions: Calciphylaxis is characterized by subcuticular vascular changes that reflect an interplay between complement triggered endothelial cell injury, resultant vascular thrombosis, and subsequent abluminal calcification. Complement inhibition therapy defines a potential intervention that should be explored.

将钙化病重新定义为与局部皮下和全身补体途径激活有关的独特的骨形成皮下 C5b-9 介导的微血管损伤综合征
背景:微血管血栓形成是钙血症发病机制的关键。反映补体途径激活的 C5b-9 介导的微血管损伤可能是一个关键的病理生理事件:我们对埃默里2010-2022年数据库中未进行C5b-9免疫组化(IHC)检查的24例活检支持的钙铁血症患者和康奈尔2019-2023年数据库中进行C5b-9 IHC检查作为常规钙铁血症检查一部分的患者进行了回顾性多中心研究。我们对病变活检标本上的C5b-9 IHC进行了评估,并将其与常规光学显微镜检查结果和临床特征进行了关联:我们研究中的大多数患者都患有尿毒症性钙化症,并伴有肥胖、糖尿病、透析、高血压、甲状旁腺功能亢进和血清磷升高。大多数患者没有明确的促凝血和/或高粘滞状态。血管病变主要局限于皮下脂肪,范围从钙化性内膜动脉病变到微血管血栓形成,伴有或不伴有内皮钙化的内皮损伤。在大多数病例中(即超过 80%),包括微血管和脂肪动脉在内的血管内都有明显的 C5b-9 沉积,至少与受损血管有局部联系。在约40%的病例中,真皮微血管中同时存在C5b-9沉积,显示有全身补体途径激活的证据:钙化病的特点是皮下血管发生变化,反映了补体引发的内皮细胞损伤、由此导致的血管血栓形成和随后的基底钙化之间的相互作用。补体抑制疗法是一种值得探讨的潜在干预措施。
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来源期刊
CiteScore
1.80
自引率
9.10%
发文量
453
审稿时长
3 months
期刊介绍: The American Journal of Dermatopathology offers outstanding coverage of the latest diagnostic approaches and laboratory techniques, as well as insights into contemporary social, legal, and ethical concerns. Each issue features review articles on clinical, technical, and basic science advances and illuminating, detailed case reports. With the The American Journal of Dermatopathology you''ll be able to: -Incorporate step-by-step coverage of new or difficult-to-diagnose conditions from their earliest histopathologic signs to confirmatory immunohistochemical and molecular studies. -Apply the latest basic science findings and clinical approaches to your work right away. -Tap into the skills and expertise of your peers and colleagues the world over peer-reviewed original articles, "Extraordinary cases reports", coverage of practical guidelines, and graphic presentations. -Expand your horizons through the Journal''s idea-generating forum for debating controversial issues and learning from preeminent researchers and clinicians
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