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麻风及其反应性病变中的血管生成和淋巴管生成。

Angiogenesis and lymphangiogenesis in the spectrum of leprosy and its reactional forms.

机构信息

Laboratory of Anatomic Pathology, Lauro de Souza Lima Institute, Bauru, São Paulo, Brazil.

出版信息

PLoS One. 2013 Sep 6;8(9):e74651. doi: 10.1371/journal.pone.0074651. eCollection 2013.

Abstract

BACKGROUND

Angiogenesis and lymphangiogenesis are the processes of neovascularization that evolve from preexisting blood and lymphatic vessels. There are few studies on angiogenesis and none on lymphangiogenesis in leprosy. Thus, the role of neovascularization in the pathophysiological mechanisms of the disease was studied across the spectrum of leprosy, its reactional states and its residual lesions.

METHODOLOGY/PRINCIPAL FINDINGS: Seventy-six biopsies of leprosy skin lesions and seven healthy controls were selected. Fifty-five serum samples were used for the detection of CD105 by ELISA. Histological sections were stained with antibodies against CD31 (blood and lymphatic vessels), D2-40/podoplanin (lymphatic vessels), and CD105/endoglin (neovessels). Microvessels were counted in 100 high-power fields (400x) and the number of vessels was evaluated in relation to the extension of the inflammatory infiltrate (0-3), to the bacillary index (0-6) and to the clinical forms. Angiogenesis, as marked by CD31 and CD105, was observed across the leprosy spectrum, compared with the controls. Additionally, there was a positive correlation between these markers with extension of the infiltrate (p <0.0001). For D2/40, lymphangiogenesis was observed in the tuberculoid form (p <0.0001). There was no statistical significance for values of CD105 detected in plasma by ELISA.

CONCLUSIONS/SIGNIFICANCE: Angiogenesis is present across the spectrum of leprosy and in its reactional forms. The increase in the number of vessels, as detected by CD31 and CD105 staining, is related to the extension of the inflammatory infiltrate. Samples from reactional lesions have a higher number of CD31+ and CD105+ stained vessels, which indicates their involvement in the pathophysiological mechanisms of the reactional states. The regression of lesions is accompanied by the regression of neovascularization. Drugs inhibiting angiogenesis may be relevant in the treatment of leprosy, in addition to multidrugtherapy, and in the prevention of the development of reactions.

摘要

背景

血管生成和淋巴管生成是从现有血管和淋巴管演变而来的新生血管过程。关于麻风病中的血管生成和淋巴管生成的研究很少。因此,研究了新血管生成在麻风病及其反应状态和残留病变的病理生理机制中的作用。

方法/主要发现:选择了 76 例麻风皮损活检和 7 例健康对照。使用 55 份血清样本通过 ELISA 检测 CD105。用针对 CD31(血管和淋巴管)、D2-40/podoplanin(淋巴管)和 CD105/endoglin(新血管)的抗体对组织学切片进行染色。在 100 个高倍视野(400x)中计数微血管,并根据炎症浸润的扩展(0-3)、杆菌指数(0-6)和临床形式评估血管数量。与对照组相比,在麻风病谱中观察到 CD31 和 CD105 标记的血管生成。此外,这些标志物与浸润的扩展呈正相关(p <0.0001)。对于 D2/40,在结核样型中观察到淋巴管生成(p <0.0001)。ELISA 检测到的血浆 CD105 值无统计学意义。

结论/意义:血管生成存在于麻风病及其反应形式中。通过 CD31 和 CD105 染色检测到的血管数量增加与炎症浸润的扩展有关。反应性病变的样本具有更多的 CD31+和 CD105+染色血管,这表明它们参与了反应性状态的病理生理机制。病变的消退伴随着新血管生成的消退。除了多药治疗外,抑制血管生成的药物可能在麻风病的治疗以及预防反应的发展中具有重要意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/becb/3765444/1093c9e7c85f/pone.0074651.g001.jpg

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