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免疫缺陷中的免疫失调。

Immunodysregulation in immunodeficiency.

出版信息

Allergy Asthma Proc. 2024 Sep 1;45(5):340-346. doi: 10.2500/aap.2024.45.240058.

DOI:10.2500/aap.2024.45.240058
Abstract

The primary immunodeficiency diseases are often accompanied by autoimmunity, autoinflammatory, or aberrant lymphoproliferation. The paradoxical nature of this association can be explained by the multiple cells and molecules involved in immune networks that interact with each other in synergistic, redundant, antagonistic, and parallel arrangements. Because progressively more immunodeficiencies are found to have a genetic etiology, in many cases, a monogenic pathology, an understanding of why immunodeficiency is really an immune dysfunction becomes evident. Understanding the role of specific genes allows us to better understand the complete nature of the inborn error of immunity (IEI); the latter is a term generally used when a clear genetic etiology can be discerned. Autoimmune cytopenias, inflammatory bowel disease, autoimmune thyroiditis, and autoimmune liver diseases as well as lymphomas and cancers frequently accompany primary immunodeficiencies, and it is important that the practitioner be aware of this association and to expect that this is more common than not. The treatment of autoimmune or immunodysregulation in primary immunodeficiencies often involves further immunosuppression, which places the patient at even greater risk of infection. Mitigating measures to prevent such an infection should be considered as part of the treatment regimen. Treatment of immunodysregulation should be mechanism based, as much as we understand the pathways that lead to the dysfunction. Focusing on abnormalities in specific cells or molecules, cytokines, will become increasingly used to provide a targeted approach to therapy, a prelude to the success of personalized medicine in the treatment of IEIs.

摘要

原发性免疫缺陷病常伴有自身免疫、自身炎症或异常淋巴增生。这种关联的矛盾性质可以用参与免疫网络的多种细胞和分子来解释,这些细胞和分子以协同、冗余、拮抗和并行的方式相互作用。由于越来越多的免疫缺陷被发现具有遗传病因,在许多情况下是单基因病理学,因此,为什么免疫缺陷实际上是一种免疫功能障碍的原因变得显而易见。了解特定基因的作用可以帮助我们更好地理解先天性免疫缺陷(IEI)的本质;后者通常用于可以识别明确遗传病因的情况。自身免疫性血细胞减少症、炎症性肠病、自身免疫性甲状腺炎、自身免疫性肝病以及淋巴瘤和癌症经常伴随原发性免疫缺陷病,临床医生了解这种关联并预计这种情况比不常见更为重要。原发性免疫缺陷病中的自身免疫或免疫失调的治疗通常涉及进一步的免疫抑制,这会使患者面临更大的感染风险。应该考虑减轻这些感染风险的措施作为治疗方案的一部分。免疫失调的治疗应基于机制,只要我们了解导致功能障碍的途径。关注特定细胞或分子、细胞因子的异常,将越来越多地用于提供针对治疗的方法,为个性化医学在 IEI 治疗中的成功奠定基础。

相似文献

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Immunodysregulation in immunodeficiency.免疫缺陷中的免疫失调。
Allergy Asthma Proc. 2024 Sep 1;45(5):340-346. doi: 10.2500/aap.2024.45.240058.
2
Immune deficiency disorders with autoimmunity and abnormalities in immune regulation-monogenic autoimmune diseases.伴有自身免疫和免疫调节异常的免疫缺陷疾病——单基因自身免疫性疾病。
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引用本文的文献

1
Immunodeficiency: Overview of primary immune regulatory disorders (PIRDs).免疫缺陷:原发性免疫调节紊乱疾病(PIRDs)概述。
Allergy Asthma Proc. 2024 Sep 1;45(5):332-339. doi: 10.2500/aap.2024.45.240070.
2
Essentials of an immunodeficiency primer: A practical reference for the allergist/immunologist and the allergy-immunology fellow-in-training (FIT).免疫缺陷入门要点:过敏症专科医生/免疫学家及过敏与免疫学住院医师培训学员(FIT)的实用参考资料。
Allergy Asthma Proc. 2024 Sep 1;45(5):291-293. doi: 10.2500/aap.2024.45.240062.