TRPM4 channels are Ca2+ activated, non-selective cation channels that participate in a plethora of cardiac functions including the myocyte`s electrical excitability. Dominantly inherited mutations in the TRPM4 gene are associated with several forms of cardiac arrhythmias and conduction diseases. We identified TRPM4’s Ca2+-dependent gating behavior as a novel contributor to the aberrant membrane current and introduced that as the causal mechanism of TRPM4 mutation dependent human arrhythmia. Taking advantage of CRISPR/Cas9-mediated TRPM4 knock-out hiPSC lines, hiPSC-derived 3D cardiac organoids and engineered heart patches , this project aims at investigating how exactly TRPM4 mutations contribute to malfunction of the heart and whether functional characteristics of TRPM4 mutants correlate with a specific clinical phenotype.

DFG Programme CRC/Transregios

Subproject of TRR 152:  TRiPs to Homeostasis: Maintenance of Body Homeostasis by Transient Receptor Potential Channel Modules

Applicant Institution Ludwig-Maximilians-Universität München

Project Heads Professor Dr. Karl-Ludwig Laugwitz; Professor Peter Lipp, Ph.D.; Professorin Alessandra Moretti, Ph.D.