儿童小血管中枢神经系统血管炎的组织学诊断。

IF 2.8 3区医学 Q1 PEDIATRICS

Pediatric Rheumatology Pub Date : 2024-12-28 DOI:10.1186/s12969-024-01053-4

Maryam Nabavi Nouri, Anastasia Dropol, Pascal N Tyrrell, Sheila Sheikh, Marinka Twilt, Jean Michaud, Benjamin Ellezam, Harvey B Sarnat, Christopher Dunham, Peter W Schutz, Julia Keith, David G Munoz, Harry V Vinters, Cynthia Hawkins, Susanne M Benseler

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引用次数: 0

摘要

背景：原发性小血管中枢神经系统血管炎（sv-cPACNS）是儿童中一种具有挑战性的炎症性脑疾病。脑部活检是确认诊断的必要手段。本研究旨在开发和验证一种诊断小血管中枢神经系统血管炎的组织学评分工具。方法：开发了一种标准化的脑活检评分仪，并将其应用于儿童病例和对照组在单一中心的连续全层脑活检。染色包括免疫组织化学染色和苏木精&伊红染色。九名北美神经病理学家，不知道患者的表现、诊断和治疗，独立地对去识别活检进行评分。结果：共纳入31例sv-cPACNS患儿、11例癫痫患儿和11例非血管炎性脑疾病对照患儿的脑组织活检标本。皮质或白质血管中心性炎症增加sv-cPACNS的可能性，优势比（or）为3.231 （95CI: 0.914-11.420, p = 0.067）和3.923 （95CI: 1.13-13.6, p = 0.031）。这些区域的中度至重度炎症与sv-cPACNS的高概率相关，皮质的or为5.56 (95CI: 1.02-29.47, p = 0.046)，白质的or为6.76 （95CI: 1.26-36.11, p = 0.025）。炎症浸润以CD3、CD4、CD8和CD20细胞为主。反应性内皮与sv-cPACNS密切相关，OR为8.93 （p = 0.001）。所有活检均未见成人sv-PACNS的特征，包括肉芽肿、坏死或纤维蛋白沉积。单独出现小脑膜炎是不能诊断的。结论：在sv-cPACNS活检中发现了明显的组织学特征，包括皮层或白质中至重度血管中心性炎症浸润，包括CD3、CD4、CD8和CD20细胞，以及反应性内皮细胞，特异性为95%。在此类研究中，我们首次提出了评估脑活检的组织学标准，旨在准确表征sv-cPACNS患者炎症反应的类型和严重程度；这可以使这些人群能够综合评估结果和治疗方法。

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Towards a histological diagnosis of childhood small vessel CNS vasculitis.

Background: Primary small vessel CNS vasculitis (sv-cPACNS) is a challenging inflammatory brain disease in children. Brain biopsy is mandatory to confirm the diagnosis. This study aims to develop and validate a histological scoring tool for diagnosing small vessel CNS vasculitis.

Methods: A standardized brain biopsy scoring instrument was developed and applied to consecutive full-thickness brain biopsies of pediatric cases and controls at a single center. Stains included immunohistochemistry and Hematoxylin & Eosin. Nine North American neuropathologists, blinded to patients' presentation, diagnosis, and therapy, scored de-identified biopsies independently.

Results: A total of 31 brain biopsy specimens from children with sv-cPACNS, 11 with epilepsy, and 11 with non-vasculitic inflammatory brain disease controls were included. Angiocentric inflammation in the cortex or white matter increases the likelihood of sv-cPACNS, with odds ratios (ORs) of 3.231 (95CI: 0.914-11.420, p = 0.067) and 3.923 (95CI: 1.13-13.6, p = 0.031). Moderate to severe inflammation in these regions is associated with a higher probability of sv-cPACNS, with ORs of 5.56 (95CI: 1.02-29.47, p = 0.046) in the cortex and 6.76 (95CI: 1.26-36.11, p = 0.025) in white matter. CD3, CD4, CD8, and CD20 cells predominated the inflammatory infiltrate. Reactive endothelium was strongly associated with sv-cPACNS, with an OR of 8.93 (p = 0.001). Features reported in adult sv-PACNS, including granulomas, necrosis, or fibrin deposits, were absent in all biopsies. The presence of leptomeningeal inflammation in isolation was non-diagnostic.

Conclusion: Distinct histological features were identified in sv-cPACNS biopsies, including moderate to severe angiocentric inflammatory infiltrates in the cortex or white matter, consisting of CD3, CD4, CD8, and CD20 cells, alongside reactive endothelium with specificity of 95%. In the first study of its kind proposing histological criteria for evaluating brain biopsies, we aim to precisely characterize the type and severity of the inflammatory response in patients with sv-cPACNS; this can enable consolidation of this population to assess outcomes and treatment methodologies comprehensively.

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来源期刊

Pediatric Rheumatology PEDIATRICS-RHEUMATOLOGY

CiteScore

4.10

自引率

8.00%

发文量

审稿时长

>12 weeks

期刊介绍： Pediatric Rheumatology is an open access, peer-reviewed, online journal encompassing all aspects of clinical and basic research related to pediatric rheumatology and allied subjects. The journal’s scope of diseases and syndromes include musculoskeletal pain syndromes, rheumatic fever and post-streptococcal syndromes, juvenile idiopathic arthritis, systemic lupus erythematosus, juvenile dermatomyositis, local and systemic scleroderma, Kawasaki disease, Henoch-Schonlein purpura and other vasculitides, sarcoidosis, inherited musculoskeletal syndromes, autoinflammatory syndromes, and others.