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使用二维基因模型对健康与疾病状态下的全身固有免疫进行定量和纵向评估。

Quantitative and Longitudinal Assessment of Systemic Innate Immunity in Health and Disease Using a 2D Gene Model.

作者信息

Lei Hongxing

机构信息

CAS Key Laboratory of Genome Sciences and Information, Beijing Institute of Genomics, Chinese Academy of Sciences, and China National Center for Bioinformation, Beijing 100101, China.

Cunji Medical School, University of Chinese Academy of Sciences, Beijing 101408, China.

出版信息

Biomedicines. 2024 Apr 27;12(5):969. doi: 10.3390/biomedicines12050969.

Abstract

Dysregulation of innate immunity is deeply involved in infectious and autoimmune diseases. For a better understanding of pathogenesis and improved management of these diseases, it is of vital importance to implement convenient monitoring of systemic innate immunity. Built upon our previous works on the host transcriptional response to infection in peripheral blood, we proposed a 2D gene model for the simultaneous assessment of two major components of systemic innate immunity, including VirSig as the signature of the host response to viral infection and BacSig as the signature of the host response to bacterial infection. The revelation of dysregulation in innate immunity by this 2D gene model was demonstrated with a wide variety of transcriptome datasets. In acute infection, distinctive patterns of VirSig and BacSig activation were observed in viral and bacterial infection. In comparison, both signatures were restricted to a defined range in the vast majority of healthy adults, regardless of age. In addition, BacSig showed significant elevation during pregnancy and an upward trend during development. In tuberculosis (TB), elevation of BacSig and VirSig was observed in a significant portion of active TB patients, and abnormal BacSig was also associated with a longer treatment course. In cystic fibrosis (CF), abnormal BacSig was observed in a subset of patients, and no overall change in BacSig abnormality was observed after the drug treatment. In systemic sclerosis-associated interstitial lung disease (SSc-ILD), significant elevation of VirSig and BacSig was observed in some patients, and treatment with a drug led to the further deviation of BacSig from the control level. In systemic lupus erythematosus (SLE), positivity for the anti-Ro autoantibody was associated with significant elevation of VirSig in SLE patients, and the additive effect of VirSig/BacSig activation was also observed in SLE patients during pregnancy. Overall, these data demonstrated that the 2D gene model can be used to assess systemic innate immunity in health and disease, with the potential clinical applications including patient stratification, prescription of antibiotics, understanding of pathogenesis, and longitudinal monitoring of treatment response.

摘要

天然免疫失调与感染性疾病和自身免疫性疾病密切相关。为了更好地理解这些疾病的发病机制并改善其治疗,实施便捷的全身天然免疫监测至关重要。基于我们之前关于宿主对外周血感染的转录反应的研究,我们提出了一个二维基因模型,用于同时评估全身天然免疫的两个主要成分,包括作为宿主对病毒感染反应特征的VirSig和作为宿主对细菌感染反应特征的BacSig。通过各种转录组数据集证明了该二维基因模型揭示的天然免疫失调情况。在急性感染中,在病毒感染和细菌感染中观察到VirSig和BacSig激活的独特模式。相比之下,在绝大多数健康成年人中,无论年龄大小,这两种特征都局限于一定范围内。此外,BacSig在怀孕期间显著升高,在发育过程中呈上升趋势。在结核病(TB)中,在相当一部分活动性TB患者中观察到BacSig和VirSig升高,异常的BacSig也与更长的治疗疗程相关。在囊性纤维化(CF)中,在一部分患者中观察到异常的BacSig,药物治疗后BacSig异常情况未观察到总体变化。在系统性硬化症相关间质性肺病(SSc-ILD)中,在一些患者中观察到VirSig和BacSig显著升高,药物治疗导致BacSig进一步偏离对照水平。在系统性红斑狼疮(SLE)中,抗Ro自身抗体阳性与SLE患者中VirSig显著升高相关,在SLE患者怀孕期间也观察到VirSig/BacSig激活的累加效应。总体而言,这些数据表明二维基因模型可用于评估健康和疾病状态下的全身天然免疫,其潜在的临床应用包括患者分层、抗生素处方、发病机制理解以及治疗反应的纵向监测。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7762/11117654/062de8e07ce8/biomedicines-12-00969-g001a.jpg

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