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针对衰老和GATA4在年龄相关性心血管疾病中的综合方法。

Targeting senescence and GATA4 in age-related cardiovascular disease: a comprehensive approach.

作者信息

Imran Mohd, Altamimi Abdulmalik S A, Afzal Muhammad, Babu M Arockia, Goyal Kavita, Ballal Suhas, Sharma Pawan, Alanazi Fadiyah Jadid, Alruwaili Abeer Nuwayfi, Aldhafeeri Nouf Afit, Ali Haider

机构信息

Department of Pharmaceutical Chemistry, College of Pharmacy, Northern Border University, Rafha, 91911, Saudi Arabia.

Center for Health Research, Northern Border University, Arar, Saudi Arabia.

出版信息

Biogerontology. 2025 Jan 20;26(1):45. doi: 10.1007/s10522-025-10189-z.

Abstract

The growing prevalence of age-related cardiovascular diseases (CVDs) poses significant health challenges, necessitating the formulation of novel treatment approaches. GATA4, a vital transcription factor identified for modulating cardiovascular biology and cellular senescence, is recognized for its critical involvement in CVD pathogenesis. This review collected relevant studies from PubMed, Google Scholar, and Science Direct using search terms like 'GATA4,' 'cellular senescence,' 'coronary artery diseases,' 'hypertension,' 'heart failure,' 'arrhythmias,' 'congenital heart diseases,' 'cardiomyopathy,' and 'cardiovascular disease.' Additionally, studies investigating the molecular mechanisms underlying GATA4-mediated regulation of GATA4 and senescence in CVDs were analyzed to provide comprehensive insights into this critical aspect of potential treatment targeting. Dysregulation of GATA4 is involved in a variety of CVDs, as demonstrated by both experimental and clinical research, comprising CAD, hypertension, congenital heart diseases, cardiomyopathy, arrhythmias, and cardiac insufficiency. Furthermore, cellular senescence enhances the advancement of age-related CVDs. These observations suggested that therapies targeting GATA4, senescence pathways, or both as necessary may be an effective intervention in CVD progression and prognosis. Addressing age-related CVDs by targeting GATA4 and senescence is a broad mechanism approach. It implies further investigation of the molecular nature of these processes and elaboration of an effective therapeutic strategy. This review highlights the importance of GATA4 and senescence in CVD pathogenesis, emphasizing their potential as therapeutic targets for age-related CVDs.

摘要

与年龄相关的心血管疾病(CVD)患病率不断上升,带来了重大的健康挑战,因此需要制定新的治疗方法。GATA4是一种重要的转录因子,在调节心血管生物学和细胞衰老方面发挥着关键作用,其在CVD发病机制中的重要参与已得到认可。本综述从PubMed、谷歌学术和科学Direct收集了相关研究,使用了“GATA4”、“细胞衰老”、“冠状动脉疾病”、“高血压”、“心力衰竭”、“心律失常”、“先天性心脏病”、“心肌病”和“心血管疾病”等搜索词。此外,还分析了研究GATA4介导的CVD调控和衰老潜在分子机制的研究,以全面深入了解这一潜在治疗靶点的关键方面。实验和临床研究均表明,GATA4失调与多种CVD有关,包括CAD、高血压、先天性心脏病、心肌病、心律失常和心脏功能不全。此外,细胞衰老会加速与年龄相关的CVD的发展。这些观察结果表明,必要时针对GATA4、衰老途径或两者的治疗可能是干预CVD进展和预后的有效方法。通过靶向GATA4和衰老来解决与年龄相关的CVD是一种广泛的机制方法。这意味着需要进一步研究这些过程的分子本质,并制定有效的治疗策略。本综述强调了GATA4和衰老在CVD发病机制中的重要性,强调了它们作为与年龄相关的CVD治疗靶点的潜力。

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