Molecular switches in the TGFβ signalling cascade mediate the progression from compensated cardiac hypertrophy to heart failure, offering potential therapeutic targets.
Cardiac hypertrophy is a mechanism to compensate for increased cardiac work load, that is, after myocardial infarction or upon pressure overload. However, in the long run cardiac hypertrophy is a prevailing risk factor for the development of heart failure. During pathological remodelling processes leading to heart failure, decompensated hypertrophy, death of cardiomyocytes by apoptosis or necroptosis and fibrosis as well as a progressive dysfunction of cardiomyocytes are apparent. Interestingly, the induction of hypertrophy, cell death or fibrosis is mediated by similar signalling pathways. Therefore, tiny changes in the signalling cascade are able to switch physiological cardiac remodelling to the development of heart failure. In the present review, we will describe examples of these molecular switches that change compensated hypertrophy to the development of heart failure and will focus on the importance of the signalling cascades of the TGFβ superfamily in this process. In this context, potential therapeutic targets for pharmacological interventions that could attenuate the progression of heart failure will be discussed.
Heger et al. (Fri,) conducted a review in Cardiac hypertrophy and heart failure. TGFβ signalling was evaluated. Molecular switches in the TGFβ signalling cascade mediate the progression from compensated cardiac hypertrophy to heart failure, offering potential therapeutic targets.
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