Akademik Veri Yönetim Sistemi
Turan B. (Yürütücü)
AB Destekli Diğer Projeler, 2024 - 2027
Cardiac regeneration in adult mammals is an extremely inefficient process. Massive
cardiomyocyte and vascular loss results in a permanent decline of contractile function. Our
team has contributed to understanding the mechanisms that halt cardiomyocyte proliferation
after birth and developed therapeutic strategies to promote cardiac regeneration by either
delivery of RNAs or mechanical unloading. So far, attempts at regenerating the cardiac muscle
have not considered the need to simultaneously induce adequate vascularization of the newly
formed myocardium.
RESCUE has the ambition to develop innovative RNA therapies to simultaneously induce
cardiomyocyte proliferation and angiogenesis, and thus to regenerate both the muscular and
vascular components of the heart after cardiac damage. Toward this goal, we will explore two,
non-mutually exclusive hypotheses. The first hypothesis is that any treatment promoting
cardiomyocyte proliferation, which depends on their partial de-differentiation, is sufficient to
elicit, in turn, an angiogenic response. This hypothesis is based on our preliminary data,
showing that adult, fully differentiated cardiomyocytes inhibit angiogenesis in the heart. The
second hypothesis is that cardiomyocyte proliferation needs to be complemented by a proangiogenic
therapy, to provide adequate trophic support to the regenerating myocardium. Also
in this case, we will leverage our preliminary data to validate existing candidates and to identify
novel molecules that can be overexpressed to stimulate effective cardiac angiogenesis. The
most effective molecules inducing both cardiomyocyte proliferation and vascular growth will be
produced as RNA therapeutics and encapsulated into lipid nanoparticles, optimized to target
the myocardium. The final products will be validated for their therapeutic potential in mouse
models of cardiac ischemia.