Defects in TRPM7 channel function deregulate thrombopoiesis through altered cellular Mg(2+) homeostasis and cytoskeletal architecture.
Simon StrittPaquita NurdenRemi FavierMarie FavierSilvia FerioliSanjeev K GotruJudith M M van EeuwijkHarald SchulzeAlan T NurdenMichele P LambertErnest TurroStephanie Burger-StrittMasayuki MatsushitaLorenz MittermeierPaola BalleriniSusanna ZierlerMichael A LaffanVladimir ChubanovThomas GudermannBernhard NieswandtAttila BraunPublished in: Nature communications (2016)
Mg(2+) plays a vital role in platelet function, but despite implications for life-threatening conditions such as stroke or myocardial infarction, the mechanisms controlling [Mg(2+)]i in megakaryocytes (MKs) and platelets are largely unknown. Transient receptor potential melastatin-like 7 channel (TRPM7) is a ubiquitous, constitutively active cation channel with a cytosolic α-kinase domain that is critical for embryonic development and cell survival. Here we report that impaired channel function of TRPM7 in MKs causes macrothrombocytopenia in mice (Trpm7(fl/fl-Pf4Cre)) and likely in several members of a human pedigree that, in addition, suffer from atrial fibrillation. The defect in platelet biogenesis is mainly caused by cytoskeletal alterations resulting in impaired proplatelet formation by Trpm7(fl/fl-Pf4Cre) MKs, which is rescued by Mg(2+) supplementation or chemical inhibition of non-muscle myosin IIA heavy chain activity. Collectively, our findings reveal that TRPM7 dysfunction may cause macrothrombocytopenia in humans and mice.
Keyphrases
- atrial fibrillation
- heart failure
- endothelial cells
- high fat diet induced
- skeletal muscle
- type diabetes
- left atrial
- left ventricular
- cerebral ischemia
- metabolic syndrome
- climate change
- ionic liquid
- single cell
- risk assessment
- catheter ablation
- gene expression
- coronary artery disease
- protein kinase
- acute coronary syndrome
- human health