Environmental microcystin targets the microbiome and increases the risk of intestinal inflammatory pathology via NOX2 in underlying murine model of Nonalcoholic Fatty Liver Disease

Sutapa Sarkar,Ratanesh K Seth,Hasan Alghetaa,Philip Busbee,Geoff I Scott,Diana Kimono,Muayad Albadrani,Dwayne E Porter,Saurabh Chatterjee,Mitzi Nagarkatti,Bryan Brooks,Prakash Nagarkatti

doi:10.1038/s41598-019-45009-1

Abstract

With increased climate change pressures likely to influence harmful algal blooms, exposure to microcystin, a known hepatotoxin and a byproduct of cyanobacterial blooms can be a risk factor for NAFLD associated comorbidities. Using both in vivo and in vitro experiments we show that microcystin exposure in NAFLD mice cause rapid alteration of gut microbiome, rise in bacterial genus known for mediating gut inflammation and lactate production. Changes in the microbiome were strongly associated with inflammatory pathology in the intestine, gut leaching, tight junction protein alterations and increased oxidative tyrosyl radicals. Increased lactate producing bacteria from the altered microbiome was associated with increased NOX-2, an NADPH oxidase isoform. Activationof NOX2 caused inflammasome activation as shown by NLRP3/ASCII and NLRP3/Casp-1 colocalizations in these cells while use of mice lacking a crucial NOX2 component attenuated inflammatory pathology and redox changes. Mechanistically, NOX2 mediated peroxynitrite species were primary to inflammasome activation and release of inflammatory mediators. Thus, in conclusion, microcystin exposure in NAFLD could significantly alter intestinal pathology especially by the effects on microbiome and resultant redox status thus advancing our understanding of the co-existence of NAFLD-linked inflammatory bowel disease phenotypes in the clinic.

Highlights

The prevalence of non-alcoholic fatty liver disease (NAFLD) is increasing proportionately[1]
To determine whether microcystin had a role in activating the Kupffer cells in the liver, the immunoreactivities of Kupffer cells were analyzed in liver tissue slices (Fig. 2Bi–iv,C)
The results showed a significant increase in CD68 immunoreactivity in the CHOW + MC group compared to the lean control mice (CHOW) (*p < 0.05), and simultaneously a significant increase in nonalcoholic fatty liver disease (NAFLD) + MC mice compared to the NAFLD only group (*p < 0.05)

Summary

Introduction

The prevalence of non-alcoholic fatty liver disease (NAFLD) is increasing proportionately[1]. A growing body of evidence including reports from our laboratory has emerged, shedding light on the potential impact of environmental pollutants on liver health and, in particular, on NAFLD occurrence and its translation into more progressive form of NASH12,13. These contaminants have a great steatogenic and inflammatory potential and need to be considered as tangible NAFLD risk factors[14]. Integrated analysis of proteomic, metabolic, histological and cytokine profiles revealed that microcystin significantly inhibited fatty acid β-oxidation and hepatic lipoprotein secretion and promoted hepatic inflammation, resulting in NASH19

Methods

Results

Conclusion