Department of Cardiology, University Medical Center Groningen, University of Groningen, Groningen, The Netherlands.
Department of Cardiology, Erasmus Medical Center, Rotterdam, The Netherlands.
Am J Physiol Heart Circ Physiol. 2023 Jul 1;325(1):H195-H201. doi: 10.1152/ajpheart.00223.2023. Epub 2023 Jun 9.
The transforming growth factor-β (TGF-β) superfamily member, myostatin, is a negative regulator of muscle growth and may contribute to adverse cardiac remodeling. Whether suppressing myostatin could benefit pressure-overloaded heart remains unclear. We investigated the effects of pharmacological inhibition of myostatin on cardiac fibrosis and hypertrophy in a mouse model of pressure overload induced by transverse aortic constriction (TAC). Two weeks after the surgery, TAC and sham mice were randomly divided into groups receiving mRK35, a monoclonal anti-myostatin antibody, or vehicle (PBS) for 8 wk. Significant progressive cardiac hypertrophy was observed in TAC mice, as reflected by the increased wall thickness, ventricular weight, and cross-sectional area of cardiomyocytes. In the groups treated with mRK35, compared with sham mice, cardiac fibrosis was increased in TAC mice, accompanied with elevated mRNA expression of fibrotic genes. However, among the TAC mice, mRK35 did not reduce cardiac hypertrophy or fibrosis. Body weight, lean mass, and wet weights of tibialis anterior and gastrocnemius muscle bundle were increased by mRK35. When compared with the TAC-PBS group, the TAC mice treated with mRK35 demonstrated greater forelimb grip strength and a larger mean size of gastrocnemius fibers. Our data suggest that mRK35 does not attenuate cardiac hypertrophy and fibrosis in a TAC mouse model but has positive effects on muscle mass and muscle strength. Anti-myostatin treatment may have therapeutic value against muscle wasting in cardiac vascular disease. Recent research has highlighted the importance of inhibiting TGF-β signaling in mitigating cardiac dysfunction and remodeling. As myostatin belongs to the TGF-β family, we evaluated the impact of myostatin inhibition using mRK35 in TAC-operated mice. Our data demonstrate that mRK35 significantly increased body weight, muscle mass, and muscle strength but did not attenuate cardiac hypertrophy or fibrosis. Pharmacological inhibition of myostatin may provide therapeutic benefits for the management of muscle wasting in cardiovascular diseases.
转化生长因子-β(TGF-β)超家族成员肌抑素是肌肉生长的负调节剂,可能导致心脏不良重构。抑制肌抑素是否有益于压力超负荷的心脏尚不清楚。我们研究了药物抑制肌抑素对压力超负荷诱导的横主动脉缩窄(TAC)小鼠模型中心脏纤维化和肥大的影响。手术后 2 周,TAC 和假手术小鼠随机分为接受 mRK35(一种单克隆抗肌抑素抗体)或载体(PBS)治疗 8 周的组。TAC 小鼠出现明显的进行性心肌肥大,表现为壁厚度、心室重量和心肌细胞横截面积增加。与假手术小鼠相比,mRK35 治疗的 TAC 小鼠心脏纤维化增加,纤维化基因的 mRNA 表达升高。然而,在 TAC 小鼠中,mRK35 并未减轻心脏肥大或纤维化。mRK35 增加了 TAC 小鼠的体重、瘦肉量以及比目鱼肌和腓肠肌束的湿重。与 TAC-PBS 组相比,mRK35 治疗的 TAC 小鼠具有更大的前肢握力和更大的腓肠肌纤维平均大小。我们的数据表明,mRK35 不能减轻 TAC 小鼠模型中的心脏肥大和纤维化,但对肌肉质量和肌肉力量有积极影响。抗肌抑素治疗可能对心血管疾病中的肌肉消耗具有治疗价值。最近的研究强调了抑制 TGF-β 信号转导减轻心脏功能障碍和重构的重要性。由于肌抑素属于 TGF-β 家族,我们使用 mRK35 在 TAC 手术小鼠中评估了肌抑素抑制的影响。我们的数据表明,mRK35 显著增加了体重、肌肉质量和肌肉力量,但没有减轻心脏肥大或纤维化。肌抑素的药物抑制可能为管理心血管疾病中的肌肉消耗提供治疗益处。
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