ZHANG Ning, LI Zi-hui, ZHAO Hong-wei, et al. Analysis of Intestinal Flora Diversity and Fecal Metabolic Characteristics in Rats with Cold Coagulation and Blood Stasis Syndrome[J]. Chinese journal of experimental traditional medical formulae, 2018, 24(2): 79-85.
DOI:
ZHANG Ning, LI Zi-hui, ZHAO Hong-wei, et al. Analysis of Intestinal Flora Diversity and Fecal Metabolic Characteristics in Rats with Cold Coagulation and Blood Stasis Syndrome[J]. Chinese journal of experimental traditional medical formulae, 2018, 24(2): 79-85. DOI: 10.13422/j.cnki.syfjx.2018020079.
Analysis of Intestinal Flora Diversity and Fecal Metabolic Characteristics in Rats with Cold Coagulation and Blood Stasis Syndrome
Objective:To explore the intestinal flora diversity and endogenous metabolites in fecal of rats with cold coagulation and blood stasis syndrome
and to investigate gut flora
metaboites and metabolic pathways closely related to cold coagulation and blood stasis syndrome. Method:The rats model of cold coagulation and blood stasis syndrome induced by ice-water bath was established
16S rRNA high-throughput gene sequencing coupled with UPLC-TOF-MS based on fecal metabonomics were used to analyze relativity between intestinal flora and endogenous biomarkers. Result:Based on Illumina MiSeq platform
V4 region was selected as the ideal variable regions.Compared with the blank group
it was found that Firmicutes was markedly up-regulated in model group(P<0.05) with Bacteroidetes decreased(P<0.01)
there were 23 genus with significant differences.Based on fecal metabonomics technology
seven biomarkers were identified in model rats
of which 6 metabolites was markedly up-regulated except for docosapentaenoic acid.Three key metabolic pathways including histidine metabolism
biosynthesis of valine
leucine and isoleucine
biosynthesis of pantothenic acid and coenzyme A(CoA) were founded.There was a strong correlation between gut microbiota genera and fecal metabolites. Conclusion:It is suggested that 16S rRNA high-throughput gene sequencing combined with metabolomics can be further applied to assess pathogenesis of cold coagulation and blood stasis syndrome.
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