Toll-like receptor 4 mutation mitigates gut microbiota-mediated hypertensive kidney injury

Suravi Majumder; Sathnur B. Pushpakumar; Hebah Almarshood; Rosemary Ouseph; Dibson D. Gondim; Venkatakrishna R. Jala; Utpal Sen

Pharmacological Research (Aug 2024)

Toll-like receptor 4 mutation mitigates gut microbiota-mediated hypertensive kidney injury

Suravi Majumder,
Sathnur B. Pushpakumar,
Hebah Almarshood,
Rosemary Ouseph,
Dibson D. Gondim,
Venkatakrishna R. Jala,
Utpal Sen

Affiliations

Suravi Majumder: Department of Internal Medicine, McGovern Medical School, University of Texas Health Science Center, Houston, TX, United States; Department of Physiology, University of Louisville, School of Medicine, Louisville, KY, United States
Sathnur B. Pushpakumar: Department of Physiology, University of Louisville, School of Medicine, Louisville, KY, United States
Hebah Almarshood: Department of Physiology, University of Louisville, School of Medicine, Louisville, KY, United States
Rosemary Ouseph: Division of Nephrology and Hypertension, University of Louisville, School of Medicine, Louisville, KY, United States
Dibson D. Gondim: Department of Pathology and Laboratory Medicine, and University of Louisville, School of Medicine, Louisville, KY, United States
Venkatakrishna R. Jala: Department of Microbiology and Immunology, University of Louisville, School of Medicine, Louisville, KY, United States
Utpal Sen: Department of Physiology, University of Louisville, School of Medicine, Louisville, KY, United States; Correspondence to: Department of Physiology University of Louisville School of Medicine Louisville, Kentucky 40202, United States.

Journal volume & issue: Vol. 206
p. 107303

Abstract

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Hypertension-associated dysbiosis is linked to several clinical complications, including inflammation and possible kidney dysfunction. Inflammation and TLR4 activation during hypertension result from gut dysbiosis-related impairment of intestinal integrity. However, the contribution of TLR4 in kidney dysfunction during hypertension-induced gut dysbiosis is unclear. We designed this study to address this knowledge gap by utilizing TLR4 normal (TLR4N) and TLR4 mutant (TLR4M) mice. These mice were infused with high doses of Angiotensin-II for four weeks to induce hypertension. Results suggest that Ang-II significantly increased renal arterial resistive index (RI), decreased renal vascularity, and renal function (GFR) in TLR4N mice compared to TLR4M. 16 S rRNA sequencing analysis of gut microbiome revealed that Ang-II-induced hypertension resulted in alteration of Firmicutes: Bacteroidetes ratio in the gut of both TLR4N and TLR4M mice; however, it was not comparably rather differentially. Additionally, Ang-II-hypertension decreased the expression of tight junction proteins and increased gut permeability, which were more prominent in TLR4N mice than in TLR4M mice. Concomitant with gut hyperpermeability, an increased bacterial component translocation to the kidney was observed in TLR4N mice treated with Ang-II compared to TLR4N plus saline. Interestingly, microbiota translocation was mitigated in Ang-II-hypertensive TLR4M mice. Furthermore, Ang-II altered the expression of inflammatory (IL-1β, IL-6) and anti-inflammatory IL-10) markers, and extracellular matrix proteins, including MMP-2, −9, −14, and TIMP-2 in the kidney of TLR4N mice, which were blunted in TLR4M mice. Our data demonstrate that ablation of TLR4 attenuates hypertension-induced gut dysbiosis resulting in preventing gut hyperpermeability, bacterial translocation, mitigation of renal inflammation and alleviation of kidney dysfunction.

Published in Pharmacological Research

ISSN: 1096-1186 (Online)
Publisher: Elsevier
Country of publisher: United Kingdom
LCC subjects: Medicine: Therapeutics. Pharmacology
Website: https://www.sciencedirect.com/journal/pharmacological-research

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