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靶向( )作为一种治疗炎症相关疾病的策略。

Targeting ) as a therapeutic strategy in inflammatory-related diseases.

机构信息

Department of Human Anatomy, Faculty of Medicine and Health Sciences, University Putra Malaysia, Serdang, Selangor, Malaysia.

Department of Pharmacology, College of Health Sciences, Umaru Musa Yar'adua University, Katsina, Nigeria.

出版信息

Immunopharmacol Immunotoxicol. 2024 Oct;46(5):685-694. doi: 10.1080/08923973.2024.2391471. Epub 2024 Aug 20.

Abstract

OBJECTIVE

Inflammatory diseases are influenced by oxidative stress. Oxidatively damaged 8-oxoG in DNA is linked to inflammation. The enzyme OGG1 is responsible for repairing the damaged base in the DNA which is linked to pro-inflammatory signaling and severe inflammation. This study aims to explore the potential of targeting OGG1 as a therapeutic strategy in inflammatory disease conditions.

METHODS

A comprehensive search and review of literature were conducted using appropriate scientific databases such as Google Scholar, Scopus, PubMed, Web of Science, and other references to obtain relevant information that suited the title and content of this article.

RESULTS

Compelling pieces of evidence from many previous studies have shown the crucial role of the OGG1/8oxoG pathway in inflammatory disease conditions, leading to severe inflammatory response and death. Therefore, based on these pieces of evidence, targeting this enzyme (OGG1) using specific pharmacological inhibitors or interventions might lead to downregulation and amelioration of severe inflammation to reduce the morbimortality related to several disease conditions.

CONCLUSION

This review highlighted the molecular mechanism of OGG1 activity the 8-oxo/OGG1 pathway and its role in inflammation and inflammatory disease conditions. Due to the paucity of studies involving OGG1in inflammatory infectious diseases, further research projects are needed to explore the therapeutic potential of various OGG1 inhibitors to serve as novel therapeutic strategies in infectious inflammatory diseases of medical importance in developing countries such as malaria, meningitis, tuberculosis among others.

摘要

目的

炎症性疾病受氧化应激的影响。氧化损伤的 DNA 中的 8-氧鸟嘌呤与炎症有关。酶 OGG1 负责修复 DNA 中受损的碱基,这与促炎信号和严重炎症有关。本研究旨在探讨靶向 OGG1 作为炎症性疾病治疗策略的潜力。

方法

使用适当的科学数据库(如 Google Scholar、Scopus、PubMed、Web of Science 等)进行全面的文献搜索和综述,以获取符合本文标题和内容的相关信息。

结果

许多先前的研究提供了令人信服的证据,表明 OGG1/8oxoG 途径在炎症性疾病中的关键作用,导致严重的炎症反应和死亡。因此,基于这些证据,使用特定的药理学抑制剂或干预措施靶向该酶(OGG1)可能导致下调和改善严重炎症,从而降低与几种疾病相关的发病率和死亡率。

结论

本综述强调了 OGG1 活性的分子机制 8-oxo/OGG1 途径及其在炎症和炎症性疾病中的作用。由于涉及炎症性传染病中 OGG1 的研究较少,因此需要进一步的研究项目来探索各种 OGG1 抑制剂的治疗潜力,作为发展中国家(如疟疾、脑膜炎、结核病等)具有医学重要性的感染性炎症疾病的新型治疗策略。

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