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22q11.2 缺失综合征与 DiGeorge 综合征。

Chromosome 22q11.2 deletion syndrome and DiGeorge syndrome.

机构信息

The Children's Hospital of Philadelphia, The University of Pennsylvania Perelman School of Medicine, Philadelphia, Pennsylvania.

出版信息

Immunol Rev. 2019 Jan;287(1):186-201. doi: 10.1111/imr.12701.

Abstract

Chromosome 22q11.2 deletion syndrome is the most common microdeletion syndrome in humans. The effects are protean and highly variable, making a unified approach difficult. Nevertheless, commonalities have been identified and white papers with recommended evaluations and anticipatory guidance have been published. This review will cover the immune system in detail and discuss both the primary features and the secondary features related to thymic hypoplasia. A brief discussion of the other organ system involvement will be provided for context. The immune system, percolating throughout the body can impact the function of other organs through allergy or autoimmune disease affecting organs in deleterious manners. Our work has shown that the primary effect of thymic hypoplasia is to restrict T cell production. Subsequent homeostatic proliferation and perhaps other factors drive a Th2 polarization, most obvious in adulthood. This contributes to atopic risk in this population. Thymic hypoplasia also contributes to low regulatory T cells and this may be part of the overall increased risk of autoimmunity. Collectively, the effects are complex and often age-dependent. Future goals of improving thymic function or augmenting thymic volume may offer a direct intervention to ameliorate infections, atopy, and autoimmunity.

摘要

22q11.2 号染色体缺失综合征是人类最常见的微缺失综合征之一。其影响多样且变化极大,难以采用统一的方法进行治疗。尽管如此,已经确定了一些共同特征,并发布了附有推荐评估和预期指导的白皮书。本综述将详细介绍免疫系统,并讨论与胸腺发育不全相关的主要特征和次要特征。为了便于理解,还将简要讨论其他器官系统的受累情况。免疫系统遍及全身,可通过影响其他器官的过敏或自身免疫性疾病以有害的方式影响其功能。我们的研究表明,胸腺发育不全的主要影响是限制 T 细胞的产生。随后的体内平衡增殖和其他因素可能会导致 Th2 极化,这在成年期最为明显。这会增加该人群的特应性风险。胸腺发育不全还会导致调节性 T 细胞减少,这可能是自身免疫风险增加的整体原因之一。总的来说,这些影响是复杂的,且往往与年龄有关。未来改善胸腺功能或增加胸腺体积的目标可能提供一种直接干预措施,以改善感染、过敏和自身免疫。

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