Myocardial Fibrosis in Transforming Growth Factor β1Heterozygous Mice

• Published in: Journal of molecular and cellular cardiology Vol. 32; no. 2; pp. 187 - 195
• Main Authors: Brooks, Wesley W., Conrad, Chester H.
• Format: Journal Article
• Language: English
• Published: Elsevier Ltd 01.02.2000
• Subjects: Fibrosis; TGF- β1; Ventricular remodeling; TGF- β1; Ventricular remodeling; Fibrosis
• ISSN: 0022-2828; 1095-8584
• DOI: 10.1006/jmcc.1999.1065

Aging is associated with an increase in myocardial extracellular matrix components and contractile dysfunction. Transforming growth factor- β1(TGF- β1) has been shown to regulate expression of collagen genes and extracellular matrix component synthesis in the heart, and may contribute to the increase in myocardial fibrosis with aging. Therefore, we examined whether TGF- β1heterozygous mutant mice would exhibit less age-associated myocardial fibrosis than normal mice. Twelve heterozygous TGF- β1(+/−) deficient mice and 26 wild-type controls were examined to determine if there was a difference in development of myocardial fibrosis or mortality at 24 months of age due to the loss of one TGF- β1allele. Animals which survived to 24 months of age were killed, and morphometric and functional studies were performed in isolated perfused hearts and in hearts from 6 month old control mice. Pressure–volume relations of the LV were assessed in the isovolumic (balloon in LV) Langendorff preparation. Eleven of 12 (92%) TGF- β1deficient mice survived to 24 months of age in comparison to 66% (12/18) age-matched controls (P<0.05). Hearts from the 24 month old TGF- β1deficient mice exhibited a decrease in myocardial fibrosis (4±1 v. 10±1% average LV fibrosis in TGF- β1(+/−) and age-matched controls, respectively (P<0.05) and greater compliance (i.elower LV end-diastolic pressure at a given balloon volume), decreased myocardial stiffness, and shorter contractile duration in comparison to 24-month-old wild-type controls. This suggests that modulation of collagen production and/or degradation by TGF- β1may contribute to changes in myocardial structure and function with age. Thus, loss of one TGF- β1allele appears to ameliorate age associated myocardial fibrosis and improve LV compliance, which may contribute to increased survival over the life span of these mice.