Pharmacological or genetic inhibition of LTCC promotes cardiomyocyte proliferation through inhibition of calcineurin activity.
Riham R E AbouleisaLynn DeviléeJessica MillerJanice ReidAboubakr Mohamed SalamaQinghui OuMadiha JamalYibing NongDouglas AndresJonathan SatinTamer MohamedJames Edward HudsonPublished in: Research square (2023)
Cardiomyocytes (CMs) lost during ischemic cardiac injury cannot be replaced due to their limited proliferative capacity, which leads to progressive heart failure. Calcium (Ca2+) is an important signal transducer that regulates key cellular processes, but its role in regulating CM proliferation is incompletely understood. A drug screen targeting proteins involved in CM calcium cycling in human embryonic stem cell-derived cardiac organoids (hCOs) revealed that only the inhibition of L-Type Calcium Channel (LTCC), but not other Ca2+ regulatory proteins (SERCA or RYR), induced the CM cell cycle. Furthermore, overexpression of Ras-related associated with Diabetes (RRAD), an endogenous inhibitor of LTCC, induced CM cell cycle activity in vitro, in human cardiac slices, and in vivo. Mechanistically, LTCC inhibition by RRAD induces the cell cycle in CMs by modulating calcineurin activity and translocating Hoxb13 to the CM nucleus. Together, this represents a robust pathway for regenerative strategies.
Keyphrases
- cell cycle
- cell proliferation
- high glucose
- endothelial cells
- heart failure
- left ventricular
- signaling pathway
- induced pluripotent stem cells
- stem cells
- drug induced
- diabetic rats
- type diabetes
- cardiovascular disease
- multiple sclerosis
- bone marrow
- single cell
- drug delivery
- cancer therapy
- genome wide
- metabolic syndrome
- skeletal muscle
- protein kinase
- insulin resistance
- copy number