生物
发病机制
败血症
SIMD公司
疾病
基因
生物信息学
遗传学
计算生物学
内科学
免疫学
医学
计算机科学
并行计算
作者
Hanyi Yao,Zixi Xiao,Shufang Liu,Xingjian Gao,Zehong Wu,Dongping Li,Zhangqing Yi,Haojie Zhou,Weizhi Zhang
出处
期刊:Genomics
[Elsevier BV]
日期:2024-08-05
卷期号:116 (5): 110911-110911
标识
DOI:10.1016/j.ygeno.2024.110911
摘要
There is still a lack of effective treatment for sepsis-induced myocardial dysfunction (SIMD), while the pathogenesis of SIMD still remains largely unexplained. RNA sequencing results (GSE267388 and GSE79962) were used for cross-species integrative analysis. Bioinformatic analyses were used to delve into function, tissue- and cell- specificity, and interactions of genes. External datasets and qRT-PCR experiments were used for validation. L1000 FWD was used to predict targeted drugs, and 3D structure files were used for molecular docking. Based on bioinformatic analyses, ten differentially expressed genes were selected as genes of interest, seven of which were verified to be significantly differential expression. Bucladesine was considered as a potential targeted drug for SIMD, which banded to seven target proteins primarily by forming hydrogen bonds. It was considered that Cebpd, Timp1, Pnp, Osmr, Tgm2, Cp, and Asb2 were novel disease genes, while bucladesine was a potential therapeutic drug, of SIMD.
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