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Gut microbiota related steroid hormone biosynthesis provide novel insights into high-salt diet related renal injury vit gut-kidney axis
by
Xie, Ting
, Zhu, Sheng-yi
, Chen, Li-guo
, Wang, Tong-tong
, Bai, Zhen-yu
, Liu, Tian-hao
, Niu, Yu-hao
, Xiao, Ya
, Zhang, Chen-yang
, Yu, Yu-sheng
, Wei, Hong
in
Animal models
/ Bioinformatics
/ Biological Microscopy
/ Biomedical and Life Sciences
/ Biosynthesis
/ Blood pressure
/ Cytochrome P450
/ Cytokines
/ Dehydroepiandrosterone
/ Development and progression
/ Diet
/ Digestive system
/ Enrichment
/ Feces
/ Gastrointestinal tract
/ Gene expression
/ Germ-free mice
/ Germfree
/ Gut microbiota
/ Gut-kidney axis
/ Health aspects
/ Injuries
/ Intestinal microflora
/ Kidney diseases
/ Kidneys
/ Life expectancy
/ Life Sciences
/ Metabolism
/ Metabolites
/ Metabolomics
/ Microbiology
/ Microbiota
/ Microbiota (Symbiotic organisms)
/ Microorganisms
/ Mycology
/ Parasitology
/ Quality control
/ Renal function
/ Renal injury
/ Risk factors
/ Salt
/ Solvents
/ Steroid hormone biosynthesis pathway
/ Steroid hormones
/ Steroids
/ Transcriptomics
/ Verification
/ Virology
2025
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Gut microbiota related steroid hormone biosynthesis provide novel insights into high-salt diet related renal injury vit gut-kidney axis
by
Xie, Ting
, Zhu, Sheng-yi
, Chen, Li-guo
, Wang, Tong-tong
, Bai, Zhen-yu
, Liu, Tian-hao
, Niu, Yu-hao
, Xiao, Ya
, Zhang, Chen-yang
, Yu, Yu-sheng
, Wei, Hong
in
Animal models
/ Bioinformatics
/ Biological Microscopy
/ Biomedical and Life Sciences
/ Biosynthesis
/ Blood pressure
/ Cytochrome P450
/ Cytokines
/ Dehydroepiandrosterone
/ Development and progression
/ Diet
/ Digestive system
/ Enrichment
/ Feces
/ Gastrointestinal tract
/ Gene expression
/ Germ-free mice
/ Germfree
/ Gut microbiota
/ Gut-kidney axis
/ Health aspects
/ Injuries
/ Intestinal microflora
/ Kidney diseases
/ Kidneys
/ Life expectancy
/ Life Sciences
/ Metabolism
/ Metabolites
/ Metabolomics
/ Microbiology
/ Microbiota
/ Microbiota (Symbiotic organisms)
/ Microorganisms
/ Mycology
/ Parasitology
/ Quality control
/ Renal function
/ Renal injury
/ Risk factors
/ Salt
/ Solvents
/ Steroid hormone biosynthesis pathway
/ Steroid hormones
/ Steroids
/ Transcriptomics
/ Verification
/ Virology
2025
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Gut microbiota related steroid hormone biosynthesis provide novel insights into high-salt diet related renal injury vit gut-kidney axis
by
Xie, Ting
, Zhu, Sheng-yi
, Chen, Li-guo
, Wang, Tong-tong
, Bai, Zhen-yu
, Liu, Tian-hao
, Niu, Yu-hao
, Xiao, Ya
, Zhang, Chen-yang
, Yu, Yu-sheng
, Wei, Hong
in
Animal models
/ Bioinformatics
/ Biological Microscopy
/ Biomedical and Life Sciences
/ Biosynthesis
/ Blood pressure
/ Cytochrome P450
/ Cytokines
/ Dehydroepiandrosterone
/ Development and progression
/ Diet
/ Digestive system
/ Enrichment
/ Feces
/ Gastrointestinal tract
/ Gene expression
/ Germ-free mice
/ Germfree
/ Gut microbiota
/ Gut-kidney axis
/ Health aspects
/ Injuries
/ Intestinal microflora
/ Kidney diseases
/ Kidneys
/ Life expectancy
/ Life Sciences
/ Metabolism
/ Metabolites
/ Metabolomics
/ Microbiology
/ Microbiota
/ Microbiota (Symbiotic organisms)
/ Microorganisms
/ Mycology
/ Parasitology
/ Quality control
/ Renal function
/ Renal injury
/ Risk factors
/ Salt
/ Solvents
/ Steroid hormone biosynthesis pathway
/ Steroid hormones
/ Steroids
/ Transcriptomics
/ Verification
/ Virology
2025
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Gut microbiota related steroid hormone biosynthesis provide novel insights into high-salt diet related renal injury vit gut-kidney axis
Journal Article
Gut microbiota related steroid hormone biosynthesis provide novel insights into high-salt diet related renal injury vit gut-kidney axis
2025
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Overview
High-salt diet (HSD) is a major risk factor for renal injury, and gut microbiota may play a role in this process. In this study, we investigated the potential role of gut microbiota in HSD-related renal injury and the microbial mechanisms involved. Through function observation, mechanism screening, and further verification using transcriptomic and metabolomic profiling and bioinformatics, we found that HSD caused renal dysfunction, inflammation, hypoimmunity, and serious renal damage in conventional mice, but this effect was absent in germ-free (GF) mice. Differential gene set enrichment analyses of the gut and kidney identified the steroid hormone biosynthesis pathway as a main culprit. For further verification, differential metabolite set enrichment analyses of feces indicated the involvement of the steroid hormone biosynthesis pathway. Through comprehensive profiling of intestinal and renal tissues along with fecal samples, we detected three genes and two metabolites showing prominent enrichment in the steroid hormone biosynthesis pathway. RT-qPCR suggested that the core gene
Cyp1a1
, which depends on the interplay between HSD and gut microbiota, was inhibited in both the gut and kidney in HSD-related renal injury. Finally, dehydroepiandrosterone decreased the mRNA expression of
Cyp1a1
in the gut and kidney. The data suggest that HSD promotes renal injury by manipulating the gut-kidney axis via gut microbiota and strengthening the steroid hormone biosynthesis pathway. The study expands the current knowledge on the gut microbial control of the gut-kidney axis in HSD-related renal injury, which finally provides novel insights into the therapeutic strategies for preventing or attenuating HSD-related kidney diseases.
Publisher
BioMed Central,BioMed Central Ltd,Springer Nature B.V,BMC
Subject
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