The gut-joint axis in spondyloarthritis: immunological, microbial, and clinical insights

失调 HLA-B27 微生物群 肠道菌群 免疫系统 获得性免疫系统 免疫学 亚临床感染 炎症 医学 先天免疫系统 关节炎 疾病 生物信息学 炎症性肠病 生物 人类白细胞抗原 病理 抗原
作者
Zoya Qaiyum,Melissa Lim,Robert D Inman
出处
期刊:Seminars in Immunopathology [Springer Science+Business Media]
卷期号:43 (2): 173-192 被引量:40
标识
DOI:10.1007/s00281-021-00845-0
摘要

The strong genetic and clinical overlaps between spondyloarthritis (SpA) and inflammatory bowel disease (IBD) have placed much needed focus on the gut-joint axis of inflammation in SpA, leading to three key hypotheses that attempt to unravel this complex relationship. The arthritogenic peptide hypothesis and the aberrant cellular trafficking hypothesis have been put forth to rationalize the manner by which the innate and adaptive immune systems cooperate and converge during SpA pathogenesis. The bacterial dysbiosis hypothesis discusses how changes in the microbiome lead to architectural and immunological consequences in SpA. These theories are not mutually exclusive, but can provide an explanation as to why subclinical gut inflammation may sometimes precede joint inflammation in SpA patients, thereby implying a causal relationship. Such investigations will be important in informing therapeutic decisions which may be common to both SpA and IBD. However, these hypotheses can also offer insights for a coincident inflammatory relationship between the gut and the joint, particularly when assessing the immunological players involved. Insights from understanding how these systems might affect the gut and joint differently will be equally imperative to address where the therapeutic differences lie between the two diseases. Collectively, this knowledge has practical implications in predicting the likelihood of IBD development in SpA or presence of coincident SpA-IBD, uncovering novel therapeutic targets, and redesigning currently approved treatments. It is evident that a multidisciplinary approach between the rheumatology and gastroenterology fields cannot be ignored, when it comes to the care of SpA patients at risk of IBD or vice versa.
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