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抗血栓素-前列腺素受体作为治疗肌营养不良性心肌病的一种潜在疗法。

Antagonism of the Thromboxane-Prostanoid Receptor as a Potential Therapy for Cardiomyopathy of Muscular Dystrophy.

机构信息

Division of Allergy, Pulmonary, and Critical Care Vanderbilt University Medical Center Nashville TN.

Division of Cardiology Vanderbilt University Medical Center Nashville TN.

出版信息

J Am Heart Assoc. 2019 Nov 5;8(21):e011902. doi: 10.1161/JAHA.118.011902. Epub 2019 Oct 30.

DOI:10.1161/JAHA.118.011902
PMID:31662020
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6898850/
Abstract

Background Muscular dystrophy (MD) causes a progressive cardiomyopathy characterized by diffuse fibrosis, arrhythmia, heart failure, and early death. Activation of the thromboxane-prostanoid receptor (TPr) increases calcium transients in cardiomyocytes and is proarrhythmic and profibrotic. We hypothesized that TPr activation contributes to the cardiac phenotype of MD, and that TPr antagonism would improve cardiac fibrosis and function in preclinical models of MD. Methods and Results Three different mouse models of MD (mdx/utrn double knockout, second generation mdx/mTR double knockout, and delta-sarcoglycan knockout) were given normal drinking water or water containing 25 mg/kg per day of the TPr antagonist ifetroban, beginning at weaning. After 6 months (10 weeks for mdx/utrn double knockout), mice were evaluated for cardiac and skeletal muscle function before euthanization. There was a 100% survival rate of ifetroban-treated mice to the predetermined end point, compared with 60%, 43%, and 90% for mdx/utrn double knockout, mdx/mTR double knockout, and delta-sarcoglycan knockout mice, respectively. TPr antagonism improved cardiac output in mdx/utrn double knockout and mdx/mTR mice, and normalized fractional shortening, ejection fraction, and other parameters in delta-sarcoglycan knockout mice. Cardiac fibrosis in delta-sarcoglycan knockout was reduced with TPr antagonism, which also normalized cardiac expression of claudin-5 and neuronal nitric oxide synthase proteins and multiple signature genes of Duchenne MD. Conclusions TPr antagonism reduced cardiomyopathy and spontaneous death in mouse models of Duchenne and limb-girdle MD. Based on these studies, ifetroban and other TPr antagonists could be novel therapeutics for treatment of the cardiac phenotype in patients with MD.

摘要

背景

肌营养不良症(MD)导致进行性心肌病,其特征为弥漫性纤维化、心律失常、心力衰竭和早期死亡。血栓素-前列腺素受体(TPr)的激活增加心肌细胞中的钙瞬变,并具有致心律失常和促纤维化作用。我们假设 TPr 激活导致 MD 的心脏表型,并认为 TPr 拮抗作用将改善 MD 的临床前模型中的心脏纤维化和功能。

方法和结果

三种不同的 MD 小鼠模型(mdx/utrn 双敲除、第二代 mdx/mTR 双敲除和δ-横纹肌聚糖缺失)在断奶后开始饮用正常饮用水或含有 25mg/kg/天 TPr 拮抗剂 ifetroban 的水。6 个月(mdx/utrn 双敲除 10 周)后,在安乐死前评估小鼠的心脏和骨骼肌功能。与 mdx/utrn 双敲除、mdx/mTR 双敲除和δ-横纹肌聚糖缺失小鼠分别为 60%、43%和 90%的预定终点生存率相比,ifetroban 治疗的小鼠有 100%的存活率。TPr 拮抗作用改善了 mdx/utrn 双敲除和 mdx/mTR 小鼠的心输出量,并使 δ-横纹肌聚糖缺失小鼠的分数缩短、射血分数和其他参数正常化。TPr 拮抗作用降低了 δ-横纹肌聚糖缺失小鼠的心脏纤维化,同时还使心脏 Claudin-5 和神经元型一氧化氮合酶蛋白以及杜氏肌营养不良症的多个特征基因的表达正常化。

结论

TPr 拮抗作用减少了杜氏和肢带型 MD 小鼠模型中的心肌病和自发性死亡。基于这些研究,ifetroban 和其他 TPr 拮抗剂可能成为治疗 MD 患者心脏表型的新型治疗方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/99fe/6898850/9264dd2bbc15/JAH3-8-e011902-g008.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/99fe/6898850/d43c7edcf9b2/JAH3-8-e011902-g001.jpg
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https://cdn.ncbi.nlm.nih.gov/pmc/blobs/99fe/6898850/82a2106d8a0a/JAH3-8-e011902-g003.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/99fe/6898850/f68be08670ba/JAH3-8-e011902-g004.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/99fe/6898850/d3a8780d0739/JAH3-8-e011902-g005.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/99fe/6898850/872f70196056/JAH3-8-e011902-g006.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/99fe/6898850/2656404fd8b2/JAH3-8-e011902-g007.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/99fe/6898850/9264dd2bbc15/JAH3-8-e011902-g008.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/99fe/6898850/d43c7edcf9b2/JAH3-8-e011902-g001.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/99fe/6898850/55a96d7030c0/JAH3-8-e011902-g002.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/99fe/6898850/82a2106d8a0a/JAH3-8-e011902-g003.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/99fe/6898850/f68be08670ba/JAH3-8-e011902-g004.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/99fe/6898850/d3a8780d0739/JAH3-8-e011902-g005.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/99fe/6898850/872f70196056/JAH3-8-e011902-g006.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/99fe/6898850/2656404fd8b2/JAH3-8-e011902-g007.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/99fe/6898850/9264dd2bbc15/JAH3-8-e011902-g008.jpg

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