Nieto Ramirez Luisa Maria, Mehaffy Carolina, Dobos Karen Marie
Department of Microbiology, Immunology and Pathology, Colorado State University, Fort Collins, CO, United States.
Front Immunol. 2025 Jan 30;15:1467016. doi: 10.3389/fimmu.2024.1467016. eCollection 2024.
complex (MTBC) includes ten species that affect mammals and pose a significant global health concern. Upon infection, induces various stages in the host, including early bacterial elimination, which may or may not involve memory responses. Deciphering the role of innate immune responses during MTBC infection is crucial for understanding disease progression or protection. Over the past decade, there has been growing interest in the innate immune response to , with new preclinical models emerging.
We conducted a systematic review following PRISMA guidelines, focused on innate immune mediators linked to protection or disease progression in animal models of MTBC infection. We searched two databases: National Library of Medicine and Web of Science. Two researchers independently extracted data based on specific inclusion and exclusion criteria.
Eighty-three articles were reviewed. Results were categorized in four groups: MTBC species, animal models, soluble factors and innate pathways, and other molecules (metabolites and drugs). and were the only species studied. P2X7R receptor's role in disease progression and higher macrophage recruitment were observed differentially after infection with hypervirulent strains. Mice and non-human primates (NHPs) were the most used mammals, with emerging models like and planarians also studied. NHPs provided insights into age-dependent immunity and markers for active tuberculosis (ATB). Key innate immune factors/pathways identified included TNF-α, neutrophil recruitment, ROS/RNS responses, autophagy, inflammasomes, and antimicrobial peptides, with homologous proteins identified in insects. Metabolites like vitamin B5 and prostaglandin E2 were associated with protection. Immunomodulatory drugs targeting autophagy and other mechanisms were studied, exhibiting their potential as therapeutic alternatives.
Simpler, physiologically relevant, and ethically sound models, such as , are needed for studying innate responses in MTBC infection. While insects lack adaptive immunity, they could provide insights into "pure" innate immune responses. The dissection of "pure," "sustained" (later than 7 days post-infection), and trained innate immunity presents additional challenges that require high-resolution temporospatial analytical methods. Identifying early innate immune mediators and targetable pathways in the blood and affected tissues could identify biomarkers for immunization efficiency, disease progression, and potential synergistic therapies for ATB.
结核分枝杆菌复合群(MTBC)包括十种可感染哺乳动物的菌种,是全球重大的健康问题。感染后,MTBC在宿主体内引发不同阶段的反应,包括早期细菌清除,这可能涉及或不涉及记忆反应。解读MTBC感染过程中固有免疫反应的作用对于理解疾病进展或保护机制至关重要。在过去十年中,人们对MTBC感染的固有免疫反应兴趣日增,新的临床前模型不断涌现。
我们按照PRISMA指南进行了系统综述,重点关注与MTBC感染动物模型中保护或疾病进展相关的固有免疫介质。我们检索了两个数据库:美国国立医学图书馆和科学网。两名研究人员根据特定的纳入和排除标准独立提取数据。
共审查了83篇文章。结果分为四组:MTBC菌种、动物模型、可溶性因子和固有途径以及其他分子(代谢物和药物)。仅研究了结核分枝杆菌和牛分枝杆菌。感染高毒力结核分枝杆菌菌株后,观察到P2X7R受体在疾病进展和更高的巨噬细胞募集中发挥不同作用。小鼠和非人类灵长类动物(NHPs)是最常用的哺乳动物,也研究了斑马鱼和涡虫等新兴模型。NHPs为年龄依赖性免疫和活动性结核病(ATB)标志物提供了见解。确定的关键固有免疫因子/途径包括TNF-α、中性粒细胞募集、ROS/RNS反应、自噬、炎性小体和抗菌肽,在昆虫中鉴定出了同源蛋白。维生素B5和前列腺素E2等代谢物与保护作用相关。研究了针对自噬和其他机制的免疫调节药物,显示出其作为治疗替代方案的潜力。
研究MTBC感染中的固有反应需要更简单、生理相关且符合伦理的模型,如斑马鱼。虽然昆虫缺乏适应性免疫,但它们可以为“纯粹”的固有免疫反应提供见解。剖析“纯粹”、“持续”(感染后7天以上)和训练有素的固有免疫带来了额外挑战,需要高分辨率的时空分析方法。确定血液和受影响组织中的早期固有免疫介质和可靶向途径可以识别免疫接种效率、疾病进展的生物标志物以及ATB的潜在协同治疗方法。
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