Cellular senescence in acute human infectious disease: a systematic review.

IF 3.3 Q2 GERIATRICS & GERONTOLOGY

Frontiers in aging Pub Date : 2024-11-15 eCollection Date: 2024-01-01 DOI:10.3389/fragi.2024.1500741

William C Miller, Stephanie Wallace, William Kamm, Erin Reardon, Nicole Theis-Mahon, Matthew J Yousefzadeh, Elizabeth L Schmidt, Laura J Niedernhofer, Michael A Puskarich

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Abstract

Introduction: Acute infectious disease represents a significant cause of mortality and morbidity in elderly individuals admitted to the hospital. In its extreme, it presents as sepsis, a systematic inflammatory and immunologic response responsible for self-injurious organ injury. As individuals age, a unique set of factors including immunosenescence predispose them to acquiring an infection and a worse clinical prognosis. This systematic review explores the relationship between cellular senescence, an age-related inflammatory phenomenon, with acute human infectious disease.

Methods: Embase via OVID, Scopus, Web of Science, Global Index Medicus, Cochrane Library via Wiley, and ClinicalTrials.gov were queried. Included studies must have compared at least one of the following measures of cellular senescence between patients with an infection and without an infection: cell cycle inhibition measured via levels of p16 ^INK4a and/or p21 ^CIP1 , short telomere length, DNA damage via ɣH2AX, high senescence-associated β galactosidase activity, and inflammation via the detection of senescence associated secretory phenotype (SASP). Manuscripts were screened and data collected via two independent reviewers.

Results: A total of 15,828 studies were screened after duplicates were removed. One hundred and fifty-three full-text articles were assessed for eligibility and a total of 16 original articles were included in analysis. Of the 16 original articles included, 12 (75%) articles were centered on SARS-CoV-2, 2 (12.5%) articles utilized patients infected with Leishmania braziliensis, 1 (6.25%) with Plasmodium falciparum, and 1 (6.25%) with Hepatitis C.

Conclusion: Current literature demonstrates robust upregulation of markers of cellular senescence in the setting of acute SARS-CoV-2, P. falciparum, L. braziliensis, and hepatitis C virus, and that markers of senescence correlate with disease severity and persist for months after resolution. Limitations in the number and types of infectious organisms studied, low sample sizes, modest longitudinal sampling, and a lack of consistency in markers measured, the method of measurement, and the definition of normal values represent ongoing gaps in the literature.

Systematic review registration: https://www.crd.york.ac.uk/prospero/display_record.php?RecordID=421473, Identifier CRD42023421473.

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急性人类传染病的细胞衰老：系统综述。

简介：急性传染病是入院老年人死亡和发病的重要原因。在极端情况下，它表现为败血症，一种系统性的炎症和免疫反应，导致自我伤害性器官损伤。随着个体年龄的增长，包括免疫衰老在内的一系列独特因素使他们容易感染和临床预后更差。本系统综述探讨了细胞衰老（一种与年龄相关的炎症现象）与急性人类传染病之间的关系。方法：通过OVID、Scopus、Web of Science、Global Index Medicus、Cochrane Library via Wiley和ClinicalTrials.gov对Embase进行查询。纳入的研究必须比较感染患者和未感染患者之间细胞衰老的至少以下一项测量：通过p16 INK4a和/或p21 CIP1水平测量的细胞周期抑制，端粒长度短，通过H2AX测量的DNA损伤，高衰老相关β半乳糖苷酶活性，以及通过检测衰老相关分泌表型（SASP）检测的炎症。通过两名独立审稿人对稿件进行筛选和数据收集。结果：剔除重复项后，共筛选了15828项研究。153篇全文文章被评估为合格，共有16篇原创文章被纳入分析。在纳入的16篇原始文献中，12篇（75%）以SARS-CoV-2为中心，2篇（12.5%）以巴西利什曼原虫感染为中心，1篇（6.25%）以恶性疟原虫感染为中心，1篇（6.25%）以丙型肝炎感染为中心。目前的文献表明，在急性SARS-CoV-2、恶性疟原虫、巴西疟原虫和丙型肝炎病毒的情况下，细胞衰老标志物明显上调，衰老标志物与疾病严重程度相关，并在消退后持续数月。研究的传染性生物的数量和类型的限制，低样本量，适度的纵向抽样，以及测量的标记物，测量方法和正常值的定义缺乏一致性，这些都是文献中持续存在的空白。系统评价注册：https://www.crd.york.ac.uk/prospero/display_record.php?RecordID=421473，标识符CRD42023421473。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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