Necrosis plays a role in the concentration of mycobacterial antigens in granulomas from Mycobacterium bovis naturally infected cattle

IF 1.4 3区农林科学 Q4 IMMUNOLOGY

Veterinary immunology and immunopathology Pub Date : 2024-05-05 DOI:10.1016/j.vetimm.2024.110757

Paola A. Ortega-Portilla , Jacobo Carrisoza-Urbina , Mario A. Bedolla-Alva , Omar Cortéz-Hernández , Mireya Juárez-Ramírez , Guillermina Baay-Guzmán , Sara Huerta-Yepez , José A. Gutiérrez-Pabello

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Abstract

The dynamics that develop between cells and molecules in the host against infection by Mycobacterium bovis, leads to the formation of granulomas mainly present in the lungs and regional lymph nodes in cattle. Cell death is one of the main features in granuloma organization, however, it has not been characterized in granulomatous lesions caused by M. bovis. In this study we aimed to identify the profiles of cell death in the granuloma stages and its relationship with the accumulation of bacteria. We identified necrosis, activated caspase-3, LC3B/p62 using immunohistochemistry and digital pathology analysis on 484 granulomatous lesions in mediastinal lymph nodes from 23 naturally infected cattle. Conclusions: greater amounts of mycobacterial antigens were identified in granulomas from calves compared with adult cattle. The highest percentage of necrosis and quantity of mycobacterial antigens were identified in granuloma stages (III/IV) from adults. The LC3B/p62 profile was heterogeneous in granulomas between adults and calves. Our data suggest that necrosis is associated with a higher amount of mycobacterial antigens in the late stages of granuloma and the development of autophagy appears to play an heterogeneous effector response against infection in adults and calves. These results represent one of the first approaches in the identification of cell death in the four stages of granulomas in bovine tuberculosis.

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牛分枝杆菌自然感染牛肉芽肿中的分枝杆菌抗原浓度与坏死有关

牛分枝杆菌感染宿主后，宿主体内细胞和分子之间的动态变化导致肉芽肿的形成，肉芽肿主要出现在牛的肺部和区域淋巴结。细胞死亡是肉芽肿组织的主要特征之一，但在由牛分枝杆菌引起的肉芽肿病变中，细胞死亡的特征还不明显。在这项研究中，我们旨在确定肉芽肿阶段的细胞死亡特征及其与细菌积累的关系。我们对 23 头自然感染牛纵隔淋巴结的 484 个肉芽肿病灶进行了免疫组化和数字病理学分析，确定了坏死、活化的 caspase-3、LC3B/p62。结论：与成年牛相比，犊牛肉芽肿中的分枝杆菌抗原含量更高。成年牛肉芽肿阶段（III/IV）的坏死比例和霉菌抗原数量最高。成年牛和犊牛肉芽肿中的 LC3B/p62 图谱不尽相同。我们的数据表明，在肉芽肿晚期，坏死与较多的分枝杆菌抗原有关，自噬的发展似乎在成年和犊牛的感染中起着不同的效应反应。这些结果代表了鉴定牛结核肉芽肿四个阶段中细胞死亡的首批方法之一。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Veterinary immunology and immunopathology 农林科学-免疫学

CiteScore

3.40

自引率

5.60%

发文量

审稿时长

70 days

期刊介绍： The journal reports basic, comparative and clinical immunology as they pertain to the animal species designated here: livestock, poultry, and fish species that are major food animals and companion animals such as cats, dogs, horses and camels, and wildlife species that act as reservoirs for food, companion or human infectious diseases, or as models for human disease. Rodent models of infectious diseases that are of importance in the animal species indicated above,when the disease requires a level of containment that is not readily available for larger animal experimentation (ABSL3), will be considered. Papers on rabbits, lizards, guinea pigs, badgers, armadillos, elephants, antelope, and buffalo will be reviewed if the research advances our fundamental understanding of immunology, or if they act as a reservoir of infectious disease for the primary animal species designated above, or for humans. Manuscripts employing other species will be reviewed if justified as fitting into the categories above. The following topics are appropriate: biology of cells and mechanisms of the immune system, immunochemistry, immunodeficiencies, immunodiagnosis, immunogenetics, immunopathology, immunology of infectious disease and tumors, immunoprophylaxis including vaccine development and delivery, immunological aspects of pregnancy including passive immunity, autoimmuity, neuroimmunology, and transplanatation immunology. Manuscripts that describe new genes and development of tools such as monoclonal antibodies are also of interest when part of a larger biological study. Studies employing extracts or constituents (plant extracts, feed additives or microbiome) must be sufficiently defined to be reproduced in other laboratories and also provide evidence for possible mechanisms and not simply show an effect on the immune system.