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健康个体中真菌病相关的先天性免疫缺陷。

Inborn errors of immunity underlying fungal diseases in otherwise healthy individuals.

机构信息

St. Giles Laboratory of Human Genetics of Infectious Diseases, Rockefeller Branch, The Rockefeller University, New York, NY 10065, USA.

Infectious Disease Susceptibility Program, McGill University Health Centre (MUHC) and Research Institute-MUHC (RI-MUHC), Montreal, Quebec, Canada.

出版信息

Curr Opin Microbiol. 2017 Dec;40:46-57. doi: 10.1016/j.mib.2017.10.016. Epub 2017 Nov 10.

Abstract

It has been estimated that there are at least 1.5 million fungal species, mostly present in the environment, but only a few of these fungi cause human disease. Most fungal diseases are self-healing and benign, but some are chronic or life-threatening. Acquired and inherited defects of immunity, including breaches of mucocutaneous barriers and circulating leukocyte deficiencies, account for most severe modern-day mycoses. Other types of infection typically accompany these fungal infections. More rarely, severe fungal diseases can strike otherwise healthy individuals. Historical reports of fungi causing chronic peripheral infections (e.g. affecting the nails, skin, hair), and invasive diseases (e.g. brain, lungs, liver), in otherwise healthy patients, can be traced back to the mid-20 century. These fungi typically cause endemic, but not epidemic diseases, are more likely to underlie sporadic than familial cases, and only threaten a small proportion of infected individuals. The basis of this 'idiosyncratic' susceptibility has long remained unexplained, but it has recently become apparent that 'idiopathic' fungal diseases, in children, teenagers, and even adults, may be caused by single-gene inborn errors of immunity. The study of these unusual primary immunodeficiencies (PIDs) has led to the identification of molecules and cells playing a crucial role in human host defenses against certain fungi at particular anatomic sites. A picture is emerging of inborn errors of IL-17 immunity selectively underlying chronic mucocutaneous candidiasis, with little inter-individual variability, and of inborn errors of CARD9 immunity underlying various life-threatening invasive fungal diseases, differing between patients.

摘要

据估计,真菌物种至少有 150 万种,大多数存在于环境中,但只有少数几种真菌会导致人类疾病。大多数真菌病是自限性的,良性的,但有些是慢性的或危及生命的。获得性和遗传性免疫缺陷,包括黏膜屏障和循环白细胞缺陷的破裂,是大多数现代真菌感染的主要原因。其他类型的感染通常伴随着这些真菌感染。更罕见的是,严重的真菌感染会侵袭健康个体。历史上有关于真菌引起慢性周围感染(如指甲、皮肤、头发感染)和侵袭性疾病(如大脑、肺部、肝脏感染)的报道,这些感染发生在健康个体中,可以追溯到 20 世纪中期。这些真菌通常引起地方性疾病,而不是流行性疾病,更可能是散发性病例,而不是家族性病例,并且只威胁一小部分受感染的个体。这种“特发性”易感性的基础长期以来一直无法解释,但最近已经清楚的是,儿童、青少年甚至成年人的“特发性”真菌病可能是由单个基因的先天性免疫缺陷引起的。对这些异常原发性免疫缺陷(PID)的研究导致了鉴定出在特定解剖部位对某些真菌具有关键防御作用的分子和细胞。人们对 IL-17 免疫的先天性错误选择性地导致慢性黏膜皮肤念珠菌病的发生,其个体间差异很小,对 CARD9 免疫的先天性错误导致各种危及生命的侵袭性真菌感染,不同患者之间存在差异。

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