BACKGROUND: Aging and the female sex are considered risk factors for the development of heart failure with preserved ejection fraction (HFpEF). Unlike other risk factors, such as hypertension, obesity, or diabetes, they do not represent therapeutic targets. METHODS: In a recently developed two-hit murine HFpEF model (angiotensin II + high-fat diet; MHS), we studied the relative contributions of the biological sex, aging, and gonadal hormones to cardiac remodeling and function. We aimed to reproduce a frequent HFpEF phenotype in mice characterized by aging, hypertension, the female sex, menopause, and metabolic alterations. Using the MHS mouse model, we studied cardiac remodeling and function in C57Bl6/J mice of both sexes, young (12 weeks) and old (20 months), that were gonadectomized (Gx) or not. RESULTS: We observed that in mice, aging was associated with body weight gain, cardiac hypertrophy (CH), left ventricle (LV) concentric remodeling, and left atrial (LA) enlargement. Diastolic parameters such as E and A wave velocities were modulated by aging but only in females. Submitting young and old mice to MHS for 28 days induced the expected HFpEF phenotype consisting of CH, LV wall thickening, LA enlargement, and diastolic dysfunction with a preserved EF except for old males, in which it was significantly reduced. Young mice were Gx at five weeks, and old mice at six months (over a year before MHS). Gx increased myocardial fibrosis in MHS females and helped preserve the EF in males. CONCLUSIONS: Our results suggest that MHS has sex-specific effects on old mice, and the loss of gonadal hormones significantly impacts the observed heart failure phenotype.
The Loss of Gonadal Hormones Has a Different Impact on Aging Female and Male Mice Submitted to Heart Failure-Inducing Metabolic Hypertensive Stress.
性腺激素的丧失对衰老雌性和雄性小鼠在诱发心力衰竭的代谢性高血压应激下的影响不同
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作者:Teou Diwaba Carmel, Labbé Emylie-Ann, Thibodeau Sara-Ãve, Walsh-Wilkinson Ãlisabeth, Morin-Grandmont Audrey, Trudeau Ann-Sarah, Arsenault Marie, Couet Jacques
| 期刊: | Cells | 影响因子: | 5.200 |
| 时间: | 2025 | 起止号: | 2025 Jun 9; 14(12):870 |
| doi: | 10.3390/cells14120870 | 研究方向: | 代谢 |
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