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与极早发型炎症性肠病相关的新型分子缺陷

Novel molecular defects associated with very early-onset inflammatory bowel.

作者信息

Ciullini Mannurita Sara, Gambineri Eleonora

机构信息

aDepartment of 'NEUROFARBA', Section of Child's Health, University of Florence bHematology-Oncology Department, 'Anna Meyer Children's Hospital', Florence, Italy.

出版信息

Curr Opin Allergy Clin Immunol. 2017 Oct;17(5):317-324. doi: 10.1097/ACI.0000000000000393.

Abstract

PURPOSE OF REVIEW

Immune dysregulation disorders present with common clinical features of multiorgan autoimmunity. Gastrointestinal involvement is the hallmark of an impaired immune homeostasis. This review will give an overview on the novel phenotypes, highlighting the major points that will help to enable early diagnosis and treatment.

RECENT FINDINGS

The rapid progress on DNA sequencing technologies have led to the identification of monogenic defects that adversely impact the control of immune homeostasis. Lymphocytes may be present but dysfunctional, allowing for the development of excessive autoreactivity and resultant autoimmune disease. Regulatory T cells (Tregs) play an essential role in enforcing immune tolerance. Here we illustrate disorders caused by impairment of mechanisms ensuring Tregs function (Tregs related) in which autoimmunity is a hallmark of the clinical disease presentation and other disorders, affecting molecules more broadly involved in immune responses and indirectly causing immune dysregulation (Tregs unrelated). Clinical presentation is sometime mischievous and often symptoms are analogous in different diseases and can mislead diagnosis.

SUMMARY

The increasing comprehension of immunological concepts behind immune dysregulation diseases will allow better and in some cases possibly even targeted treatment. A genetic diagnosis therefore becomes important information in this group of patients, especially as some patients might require hematopoietic stem cell transplantation.

摘要

综述目的

免疫失调疾病具有多器官自身免疫的常见临床特征。胃肠道受累是免疫稳态受损的标志。本综述将概述新的表型,突出有助于早期诊断和治疗的要点。

最新发现

DNA测序技术的快速发展已导致鉴定出对免疫稳态控制产生不利影响的单基因缺陷。淋巴细胞可能存在但功能失调,从而导致过度的自身反应性发展并引发自身免疫性疾病。调节性T细胞(Tregs)在维持免疫耐受中起重要作用。在此,我们阐述由确保Tregs功能的机制受损(与Tregs相关)引起的疾病,其中自身免疫是临床疾病表现的标志,以及其他疾病,这些疾病影响更广泛参与免疫反应的分子并间接导致免疫失调(与Tregs不相关)。临床表现有时具有误导性,而且不同疾病的症状往往相似,可能会导致误诊。

总结

对免疫失调疾病背后免疫学概念的日益理解将带来更好的治疗,在某些情况下甚至可能实现靶向治疗。因此,基因诊断在这类患者中成为重要信息,特别是因为一些患者可能需要造血干细胞移植。

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