36 个 COVID-19 尸检大脑中的急性中性粒细胞性血管炎(白细胞增生症)。

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS ACS Applied Bio Materials Pub Date : 2024-02-15 DOI:10.1186/s13000-024-01445-w
Roy H Rhodes, Gordon L Love, Fernanda Da Silva Lameira, Maryam Sadough Shahmirzadi, Sharon E Fox, Richard S Vander Heide
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引用次数: 0

摘要

背景:高细胞血症、肾素-血管紧张素系统、缺氧、免疫失调和有免疫相关损伤证据的血管病变与 COVID-19 脑部发病率有关,同时还受到各种基因组和环境的影响。COVID-19患者脑部直接感染SARS-CoV-2的证据相对较少:方法:研究了 36 例连续尸检的 SARS-CoV-2 RT-PCR 阳性患者的脑组织病理学,以及当代和大流行前历史对照组的研究结果。采用免疫染色法检测血清和血细胞蛋白以及补体成分。将 COVID-19 组群的微循环壁补体沉积情况与历史对照病例进行了比较。比较还包括 COVID-19 群组和对照组的其他相关临床病理和微循环结果:结果:COVID-19 队列以及当代和历史对照组的高血压、糖尿病和肥胖率相同。在所有病例中,COVID-19 组群都有不同程度的急性中性粒细胞性血管炎,脑微循环中出现白细胞增生。有几个病例发现了明显的血管中性粒细胞跨壁迁移,25 个病例出现了急性血管周围炎。在显示急性中性粒细胞血管炎较少的同组病例中,血管旁微小出血和瘀斑出血(脑实质小出血)略有增多趋势。急性中性粒细胞性血管炎合并白细胞减少症的组织负荷在对照组病例中相同,而在COVID-19病例中则明显较高。COVID-19队列大脑微循环通道中急性中性粒细胞性血管炎的组织负荷和补体成分(包括膜攻击复合物)的活化程度均明显高于历史对照组:结论:急性嗜中性粒细胞性血管炎伴有白细胞破损、急性血管周围炎以及相关的血管旁血液外渗进入脑实质,构成了与免疫相关的急性小血管炎的第一阶段,通常被称为 3 型超敏性血管炎或白细胞破损性血管炎。与大流行前的对照病例相比,COVID-19 病例中急性中性粒细胞性血管炎的组织负荷更高,微循环壁中的活化补体成分水平更高。这些发现与COVID-19病例比对照病例更广泛的小血管免疫相关性血管炎相一致。这些发现的途径和机制尚在推测中。
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Acute neutrophilic vasculitis (leukocytoclasia) in 36 COVID-19 autopsy brains.

Background: Hypercytokinemia, the renin-angiotensin system, hypoxia, immune dysregulation, and vasculopathy with evidence of immune-related damage are implicated in brain morbidity in COVID-19 along with a wide variety of genomic and environmental influences. There is relatively little evidence of direct SARS-CoV-2 brain infection in COVID-19 patients.

Methods: Brain histopathology of 36 consecutive autopsies of patients who were RT-PCR positive for SARS-CoV-2 was studied along with findings from contemporary and pre-pandemic historical control groups. Immunostaining for serum and blood cell proteins and for complement components was employed. Microcirculatory wall complement deposition in the COVID-19 cohort was compared to historical control cases. Comparisons also included other relevant clinicopathological and microcirculatory findings in the COVID-19 cohort and control groups.

Results: The COVID-19 cohort and both the contemporary and historical control groups had the same rate of hypertension, diabetes mellitus, and obesity. The COVID-19 cohort had varying amounts of acute neutrophilic vasculitis with leukocytoclasia in the microcirculation of the brain in all cases. Prominent vascular neutrophilic transmural migration was found in several cases and 25 cases had acute perivasculitis. Paravascular microhemorrhages and petechial hemorrhages (small brain parenchymal hemorrhages) had a slight tendency to be more numerous in cohort cases that displayed less acute neutrophilic vasculitis. Tissue burden of acute neutrophilic vasculitis with leukocytoclasia was the same in control cases as a group, while it was significantly higher in COVID-19 cases. Both the tissue burden of acute neutrophilic vasculitis and the activation of complement components, including membrane attack complex, were significantly higher in microcirculatory channels in COVID-19 cohort brains than in historical controls.

Conclusions: Acute neutrophilic vasculitis with leukocytoclasia, acute perivasculitis, and associated paravascular blood extravasation into brain parenchyma constitute the first phase of an immune-related, acute small-vessel inflammatory condition often termed type 3 hypersensitivity vasculitis or leukocytoclastic vasculitis. There is a higher tissue burden of acute neutrophilic vasculitis and an increased level of activated complement components in microcirculatory walls in COVID-19 cases than in pre-pandemic control cases. These findings are consistent with a more extensive small-vessel immune-related vasculitis in COVID-19 cases than in control cases. The pathway(s) and mechanism for these findings are speculative.

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ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
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2.10%
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464
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