Your search keyword '"Mirjam Meiners"' showing total 2 results

1. Bitter tastants relax the mouse gallbladder smooth muscle independent of signaling through tuft cells and bitter taste receptors

Author

Maryam Keshavarz, Anna-Lena Ruppert, Mirjam Meiners, Krupali Poharkar, Shuya Liu, Wafaa Mahmoud, Sarah Winterberg, Petra Hartmann, Petra Mermer, Alexander Perniss, Stefan Offermanns, Wolfgang Kummer, and Burkhard Schütz

Subjects

Cholecystokinin, Denatonium, Dextromethorphan, Taste transduction cascade, Transient receptor potential family member 5, Quinine, Medicine, Science

Abstract

Abstract Disorders of gallbladder motility can lead to serious pathology. Bitter tastants acting upon bitter taste receptors (TAS2R family) have been proposed as a novel class of smooth muscle relaxants to combat excessive contraction in the airways and other organs. To explore whether this might also emerge as an option for gallbladder diseases, we here tested bitter tastants for relaxant properties and profiled Tas2r expression in the mouse gallbladder. In organ bath experiments, the bitter tastants denatonium, quinine, dextromethorphan, and noscapine, dose-dependently relaxed the pre-contracted gallbladder. Utilizing gene-deficient mouse strains, neither transient receptor potential family member 5 (TRPM5), nor the Tas2r143/Tas2r135/Tas2r126 gene cluster, nor tuft cells proved to be required for this relaxation, indicating direct action upon smooth muscle cells (SMC). Accordingly, denatonium, quinine and dextromethorphan increased intracellular calcium concentration preferentially in isolated gallbladder SMC and, again, this effect was independent of TRPM5. RT-PCR revealed transcripts of Tas2r108, Tas2r126, Tas2r135, Tas2r137, and Tas2r143, and analysis of gallbladders from mice lacking tuft cells revealed preferential expression of Tas2r108 and Tas2r137 in tuft cells. A TAS2R143-mCherry reporter mouse labeled tuft cells in the gallbladder epithelium. An in silico analysis of a scRNA sequencing data set revealed Tas2r expression in only few cells of different identity, and from in situ hybridization histochemistry, which did not label distinct cells. Our findings demonstrate profound tuft cell- and TRPM5-independent relaxing effects of bitter tastants on gallbladder smooth muscle, but do not support the concept that these effects are mediated by bitter receptors.

Published

2024

2. Cysteinyl leukotrienes and acetylcholine are biliary tuft cell cotransmitters

Author

Maryam Keshavarz, Schayan Faraj Tabrizi, Anna-Lena Ruppert, Uwe Pfeil, Yannick Schreiber, Jochen Klein, Isabell Brandenburger, Günter Lochnit, Sudhanshu Bhushan, Alexander Perniss, Klaus Deckmann, Petra Hartmann, Mirjam Meiners, Petra Mermer, Amir Rafiq, Sarah Winterberg, Tamara Papadakis, Dominique Thomas, Carlo Angioni, Johannes Oberwinkler, Vladimir Chubanov, Thomas Gudermann, Ulrich Gärtner, Stefan Offermanns, Burkhard Schütz, Wolfgang Kummer, and Publica

Subjects

Immunology, ddc:610, General Medicine

Abstract

The gallbladder stores bile between meals and empties into the duodenum upon demand and is thereby exposed to the intestinal microbiome. This exposure raises the need for antimicrobial factors, among them, mucins produced by cholangiocytes, the dominant epithelial cell type in the gallbladder. The role of the much less frequent biliary tuft cells is still unknown. We here show that propionate, a major metabolite of intestinal bacteria, activates tuft cells via the short-chain free fatty acid receptor 2 and downstream signaling involving the cation channel transient receptor potential cation channel subfamily M member 5. This results in corelease of acetylcholine and cysteinyl leukotrienes from tuft cells and evokes synergistic paracrine effects upon the epithelium and the gallbladder smooth muscle, respectively. Acetylcholine triggers mucin release from cholangiocytes, an epithelial defense mechanism, through the muscarinic acetylcholine receptor M3. Cysteinyl leukotrienes cause gallbladder contraction through their cognate receptor CysLTR1, prompting emptying and closing. Our results establish gallbladder tuft cells as sensors of the microbial metabolite propionate, initiating dichotomous innate defense mechanisms through simultaneous release of acetylcholine and cysteinyl leukotrienes.

Published

2022