Thioredoxin 1 (TRX1) Overexpression Cancels the Slow Force Response (SFR) Development

ZAVALA, MAITE R.; DÍAZ, ROMINA G.; VILLA-ABRILLE, MARÍA C.; PÉREZ, NÉSTOR G.

Frontiers in Cardiovascular Medicine

FFrontiers Media S.A

Año: 2021 vol. 8

AbstractThe stretch of cardiac muscle increases developed force in two phases. The first phase occurs immediately after stretch and is the expression of the Frank-Starling mechanism, while the second one or slow force response (SFR) occurs gradually and is due to an increase in the calcium transient amplitude. An important step in the chain of events leading to the SFR generation is the increased production of reactive oxygen species (ROS) leading to redox sensitive ERK1/2, p90RSK and NHE1 phosphorylation/activation. Conversely, suppression of ROS production blunts the SFR. The purpose of this study was to explore whether overexpression of the ubiquitously expressed antioxidant molecule TRX1 affects the SFR development and NHE1 phosphorylation. We did not detect any change in basal phopho-ERK1/2, phopho-p90RSK and NHE1 expression in mice with TRX1 overexpression compared to wild-type (WT). Isolated papillary muscles from WT or TRX1 overexpressing mice were stretched from 92 to 98 % of its maximal length. A prominent SFR was observed in WT mice that was completely cancelled in TRX1 animals. Interestingly, myocardial stretch induced a significant increase in NHE1 phosphorylation in WT mice that was not detected in TRX1 overexpressing mice. These novel results suggest that magnification of cardiac antioxidant defense power by overexpression of TRX1 precludes NHE1 phosphorylation/activation after stretch, consequently blunting the SFR development.