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合成核酸在诊断和治疗中的作用不断扩大。

The expanding role of synthetic nucleic acids for diagnosis and treatment.

机构信息

Department of Rheumatology and Infectious Diseases, Kitasato University School of Medicine, Kanagawa, Japan.

出版信息

Curr Opin Neurol. 2022 Jun 1;35(3):423-426. doi: 10.1097/WCO.0000000000001047. Epub 2022 Mar 11.

Abstract

PURPOSE OF REVIEW

The presence of autoantibodies is a characteristic and diagnostic index of systemic lupus erythematosus (SLE). Antidouble-stranded DNA (antids-DNA) antibodies are the most frequent autoantibodies found in SLE related to the diagnosis and disease activity of SLE, and are measured by established methods like ELISA as a polyclonal autoantibody. However, there is no reliable data on the relationship between the respective reactivity of these polyclonal antids-DNA antibodies against different epitopes generated from the original antigen and the disease phenotype. Of the complications in SLE, neuropsychiatric SLE (NPSLE) is a troublesome and frequent phenotype of the disease but no specific diagnostic autoantibodies in serum have been found. First in this review, the possibility of antids-DNA antibodies for identifying primary NPSLE in patients with SLE based on the reactivity of different synthetic nucleic acids is described as a diagnostic marker. The purpose of this review is to examine diagnostic and therapeutic opportunities to modulate autoimmune in the central nervous system (CNS) developing the CNS inflammatory disorders.

RECENT FINDINGS

Khatri et al. investigated antids-DNA antibodies in order to develop a reliable method based on the application of synthetic nucleic acids and protein-based antigen arrays to characterize autoreactive antibodies specially for NPSLE. They found autoantibodies in three particular synthetic double stranded antigens and the antinuclear antibody patterns in ordinary lupus and NPSLE. These discoveries are leading to precision medicine in the CNS inflammatory disorders.

SUMMARY

Verifying the similarity of antids-DNA obtained from patients with NPSLE can be useful as a diagnostic marker. mRNA vaccination can locally suppress autoimmunity in the CNS associated with critical steps for the develop of CNS autoinflammation. Synthetic nuclei acids may provide a diagnostic and therapeutic target in patients with autoimmune CNS inflammatory disorders.

摘要

综述目的

自身抗体的存在是系统性红斑狼疮(SLE)的特征和诊断指标。抗双链 DNA(抗 ds-DNA)抗体是 SLE 相关的最常见的自身抗体,与 SLE 的诊断和疾病活动有关,通过 ELISA 等已建立的方法作为多克隆自身抗体进行测量。然而,关于这些多克隆抗 ds-DNA 抗体针对原始抗原产生的不同表位的各自反应性与疾病表型之间的关系,尚无可靠数据。在 SLE 的并发症中,神经精神性 SLE(NPSLE)是一种麻烦且频繁的疾病表型,但在血清中尚未发现特异性的诊断自身抗体。在这篇综述中,首先描述了基于不同合成核酸的反应性,抗 ds-DNA 抗体作为一种诊断标志物,用于识别 SLE 患者的原发性 NPSLE 的可能性。本综述的目的是研究诊断和治疗机会,以调节中枢神经系统(CNS)中的自身免疫,从而开发治疗中枢神经系统炎症性疾病的方法。

最近的发现

Khatri 等人研究了抗 ds-DNA 抗体,以开发一种基于合成核酸应用和基于蛋白质的抗原阵列的可靠方法,专门用于表征针对 NPSLE 的自身反应性抗体。他们在三种特定的合成双链抗原中发现了自身抗体,以及普通狼疮和 NPSLE 中的核抗体模式。这些发现为 CNS 炎症性疾病的精准医学提供了依据。

总结

验证来自 NPSLE 患者的抗 ds-DNA 的相似性可用作诊断标志物。mRNA 疫苗可以局部抑制与 CNS 自身炎症发展相关的关键步骤中的 CNS 自身免疫。合成核酸可能为自身免疫性中枢神经系统炎症性疾病患者提供诊断和治疗靶点。

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