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Harefield Heart Science Centre (E.L.-P., L.E.F., E.J.B., P.S., K.D.P., R.G., M.H.Y., N.R., P.J.R.B.), National Heart and Lung Institute, Imperial College London, and Harefield Hospital (E.J.B., R.G.), Royal Brompton and Harefield National Health Service Trust, London UB9 6JH, United Kingdom; Mouse Biology Unit (E.L.-P., N.R.), European Molecular Biology Laboratory, 00015 Monterotondo, Italy; and Cardiovascular Division (J.L.H.), Department of Medicine, University of Minnesota, Minneapolis, Minnesota 55455
Address all correspondence and requests for reprints to: Dr. Paul J. R. Barton, Harefield Heart Science Centre, Hill End Road, Harefield, Middlesex UB9 6JH, United Kingdom. E-mail: p.barton{at}imperial.ac.uk.
Follistatins play roles in diverse biological processes including cell proliferation, wound healing, inflammation, and skeletal muscle growth, yet their role in the heart is currently unknown. We have investigated the myocardial expression profile and cellular distribution of follistatin (FST) and the FST-like genes FSTL1 and FSTL3 in the normal and failing heart. Expression was further analyzed in the novel setting of recovery from heart failure in myocardium obtained from patients who received combined mechanical (left ventricular assist device) and pharmacological therapy. Real-time PCR revealed that FSTL1 and FSTL3 expression was elevated in heart failure but returned to normal after recovery. FSTL3 expression levels correlated with molecular markers of disease severity and FSTL1 with the endothelial cell marker CD31, suggesting a potential link with vascularization. FSTL1 levels before treatment correlated with cardiac function after recovery, suggesting initial levels may influence long-term outcome. Immunohistochemistry revealed that FST was primarily localized to fibroblasts and vascular endothelium within the heart, whereas FSTL1 was localized to myocytes, endothelium, and smooth muscle cells and FSLT3 to myocytes and endothelium. Microarray analysis revealed that FST and FSTL1 were associated with extracellular matrix-related and calcium-binding proteins, whereas FSTL3 was associated mainly with cell signaling and transcription. These data show for the first time that elevated myocardial expression of FST-like genes is a feature of heart failure and may be linked to both disease severity and mechanisms underlying recovery, revealing new insight into the pathogenesis of heart failure and offering novel therapeutic targets.
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