Abstract

Accumulating evidences implicate that gut microbiota play an important role in the onset and prolongation of fat inflammation and diabetes. Sennoside A, the main active ingredient of Rhizoma Rhei (rhubarb), is widely used for constipation as a kind of anthranoid laxative (e.g., senna). Here, we put forward the hypothesis that the structural alteration of gut microbiota in obesity mice may be involved in the pathogenesis of type 2 diabetes (T2D) which may be ameliorated by Sennoside A. We investigated the appearance of obesity, insulin resistance, host inflammation, and leaky gut phenotype with or without Sennoside A in db/db mice. Horizontal fecal microbiota transplantation (FMT) was used to confirm the critical roles of gut microbiota in the amelioration of the indices in T2D mice after Sennoside A treatment. As a result, we found that Sennoside A administration markedly improved the indices in T2D mice and obesity-related traits including blood glucose level, body weight, lipid metabolism disorder, and insulin resistance. The gut microbiota changed quickly during the onset of T2D in db/db mice, which confirmed the hypothesis that gut microbiota was involved in the pathogenesis of T2D. Sennoside A altered gut microbial composition which might mediate the antiobesogenic effects in T2D remission. Sennoside A also reduced inflammation and increased tight junction proteins in the ileum in gene-deficient mice via gut microbiota alteration. FMT lowered the blood glucose level and improved insulin resistance, corroborating that Sennoside A perhaps exerted its antiobesogenic effects through gut microbiota alteration. Chemical Compounds Studied in This Article. Compounds studied in this article include Sennoside A (PubChem CID: 73111) and metformin hydrochloride (PubChem CID: 14219).

Highlights

  • Obesity, commonly representing an imbalance between energy intake and expenditure, is a metabolic disorder characterized by insulin resistance and β-cell dysfunction associated with inflammation caused by overnutrition and other environmental factors [1]

  • The sizes of adipose cells in mice treated with Sennoside A or metformin were smaller (Figures 1(e)–1(f))

  • In order to corroborate that the effects of Sennoside A was interrelated with the gut microbiota, we examined the composition of intestinal bacteria following fecal transfer from Sennoside A-treated mice

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Summary

Introduction

Commonly representing an imbalance between energy intake and expenditure, is a metabolic disorder characterized by insulin resistance and β-cell dysfunction associated with inflammation caused by overnutrition and other environmental factors [1]. It is strongly correlated with various health problems such as heart disease, stroke, hypertension, and T2D [2, 3]. Targeting the gut microbiota with appropriate drugs is supposed to be an effective therapy for diabetes, hyperlipidemia, and other

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