TMAO Suppresses Megalin Expression and Albumin Uptake in Human Proximal Tubular Cells Via PI3K and ERK Signaling

Kapetanaki, Stefania; Kumawat, Ashok Kumar; Persson, Katarina; Demirel, Isak

doi:10.3390/ijms23168856

Cited by 7 publications

(5 citation statements)

References 54 publications

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“…We have previously shown that TMAO induced increased renal fibroblast proliferation and collagen production via Akt and mTOR, but not via PI3K 22 . We have also shown that TMAO can reduce megalin expression in proximal tubular cells via PI3K and ERK 28 . In addition, TMAO has been linked to promote vascular inflammation via ERK activation 29 .…”

Section: Discussionmentioning

confidence: 55%

TMAO enhances TNF-α mediated fibrosis and release of inflammatory mediators from renal fibroblasts

Stefania,

Ashok,

Geena

et al. 2024

Sci Rep

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Trimethylamine-N-oxide (TMAO) is a gut microbiota-derived metabolite and TNF-α is proinflammatory cytokine, both known to be associated with renal inflammation, fibrosis and chronic kidney disease. However, today there are no data showing the combined effect of TMAO and TNF-α on renal fibrosis-and inflammation. The aim of this study was to investigate whether TMAO can enhance the inflammatory and fibrotic effects of TNF-α on renal fibroblasts. We found that the combination of TNF-α and TMAO synergistically increased fibronectin release and total collagen production from renal fibroblasts. The combination of TMAO and TNF-α also promoted increased cell proliferation. Both renal proliferation and collagen production were mediated through Akt/mTOR/ERK signaling. We also found that TMAO enhanced TNF-α mediated renal inflammation by inducing the release of several cytokines (IL-6, LAP TGF-beta-1), chemokines (CXCL-6, MCP-3), inflammatory-and growth mediators (VEGFA, CD40, HGF) from renal fibroblasts. In conclusion, we showed that TMAO can enhance TNF-α mediated renal fibrosis and release of inflammatory mediators from renal fibroblasts in vitro. Our results can promote further research evaluating the combined effect of TMAO and inflammatory mediators on the development of kidney disease.

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Section: Discussionmentioning

confidence: 55%

TMAO enhances TNF-α mediated fibrosis and release of inflammatory mediators from renal fibroblasts

Stefania,

Ashok,

Geena

et al. 2024

Sci Rep

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“…The suppression is mediated by an effect on PI3K (phosphoinositide 3-kinase) and ERK signaling and could be countered by candesartan, enalapril, and dapagliflozin. 125 A mediation analysis of the European MetaCardis study demonstrated a causal relation between TMAO and declined kidney function, which was corroborated by in vitro studies in human kidney fibroblasts showing that TMAO aggravated kidney fibrosis by ERK1/2 hyperactivation synergistically with TGF-β1 signaling. 126 A TMAO- or choline-supplemented diet in mice caused increased tubulointerstitial fibrosis and deposition of collagen, which was associated with an increased phosphorylation of Smad3.…”

Section: Kidney Toxicity Of Uremic Toxinsmentioning

confidence: 85%

Role of the Microbiome in Gut-Heart-Kidney Cross Talk

Glorieux

Nigám

Vanholder

et al. 2023

Circulation Research

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Homeostasis is a prerequisite for health. When homeostasis becomes disrupted, dysfunction occurs. This is especially the case for the gut microbiota, which under normal conditions lives in symbiosis with the host. As there are as many microbial cells in and on our body as human cells, it is unlikely they would not contribute to health or disease. The gut bacterial metabolism generates numerous beneficial metabolites but also uremic toxins and their precursors, which are transported into the circulation. Barrier function in the intestine, the heart, and the kidneys regulates metabolite transport and concentration and plays a role in inter-organ and inter-organism communication via small molecules. This communication is analyzed from the perspective of the remote sensing and signaling theory, which emphasizes the role of a large network of multispecific, oligospecific, and monospecific transporters and enzymes in regulating small-molecule homeostasis. The theory provides a systems biology framework for understanding organ cross talk and microbe-host communication involving metabolites, signaling molecules, nutrients, antioxidants, and uremic toxins. This remote small-molecule communication is critical for maintenance of homeostasis along the gut-heart-kidney axis and for responding to homeostatic perturbations. Chronic kidney disease is characterized by gut dysbiosis and accumulation of toxic metabolites. This slowly impacts the body, affecting the cardiovascular system and contributing to the progression of kidney dysfunction, which in its turn influences the gut microbiota. Preserving gut homeostasis and barrier functions or restoring gut dysbiosis and dysfunction could be a minimally invasive way to improve patient outcomes and quality of life in many diseases, including cardiovascular and kidney disease.

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“…We then showed that both CFT073 and TMAO could respectively increase the phosphorylation of ERK 1/2 in bladder epithelial cells. We and others have shown that ERK 1/2 is important for UPECmediated cytokine/chemokine release [15,21,22] and TMAO-mediated inflammation [23,24]. Furthermore, we also evaluated if TMAO by itself could increase the bacterial growth of CFT073 and through that be responsible for the increased release of inflammatory mediator.…”

Section: Discussionmentioning

confidence: 95%

“…We chose to use IL-8 as our inflammatory marker, as it is one of the most important chemokines during a UTI [19,20]. We investigated the involvement of ERK1/2, as it has been shown to be important for UPEC-mediated cytokine/chemokine release [15,21,22] and TMAO-mediated inflammation [23,24]. We found, by using a ERK 1/2 inhibitor, that the IL-8 release induced by CFT073 alone or in combination with TMAO was dependent on ERK 1/2 signaling (Figure 5A).…”

Section: Cft073 and Tmao Mediate The Release Of Il-8 From Bladder Epi...mentioning

confidence: 99%

Trimethylamine N-Oxide (TMAO) Mediates Increased Inflammation and Colonization of Bladder Epithelial Cells during a Uropathogenic E. coli Infection In Vitro

Kumawat

Demirel

2023

Pathogens

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Urinary tract infections (UTIs) are among the most common infections in humans and are often caused by uropathogenic E. coli (UPEC). Trimethylamine N-oxide (TMAO) is a proinflammatory metabolite that has been linked to vascular inflammation, atherosclerosis, and chronic kidney disease. As of today, no studies have investigated the effects of TMAO on infectious diseases like UTIs. The aim of this study was to investigate whether TMAO can aggravate bacterial colonization and the release of inflammatory mediators from bladder epithelial cells during a UPEC infection. We found that TMAO aggravated the release of several key cytokines (IL-1β and IL-6) and chemokines (IL-8, CXCL1 and CXCL6) from bladder epithelial cells during a CFT073 infection. We also found that CFT073 and TMAO mediate increased release of IL-8 from bladder epithelial cells via ERK 1/2 signaling and not bacterial growth. Furthermore, we showed that TMAO enhances UPEC colonization of bladder epithelial cells. The data suggest that TMAO may also play a role in infectious diseases. Our results can be the basis of further research to investigate the link between diet, gut microbiota, and urinary tract infection.

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TMAO Suppresses Megalin Expression and Albumin Uptake in Human Proximal Tubular Cells Via PI3K and ERK Signaling

Cited by 7 publications

References 54 publications

TMAO enhances TNF-α mediated fibrosis and release of inflammatory mediators from renal fibroblasts

TMAO enhances TNF-α mediated fibrosis and release of inflammatory mediators from renal fibroblasts

Role of the Microbiome in Gut-Heart-Kidney Cross Talk

Trimethylamine N-Oxide (TMAO) Mediates Increased Inflammation and Colonization of Bladder Epithelial Cells during a Uropathogenic E. coli Infection In Vitro

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