泛硫乙胺可改善患者和细胞系模型中PPCS缺乏症患者的扩张型心肌病特征。
Pantethine ameliorates dilated cardiomyopathy features in PPCS deficiency disorder in patients and cell line models.
作者信息
Zhang Fangfang, Dorn Tatjana, Gnutti Barbara, Anikster Yair, Kuebler Sarah, Ahrens-Nicklas Rebecca, Gosselin Rachel, Rahman Shamima, Durst Ronen, Zanuttigh Enrica, Güra Miriam A, Poch Christine M, Meier Anna B, Laugwitz Karl-Ludwig, Schüller Hans-Joachim, Messias Ana C, Sibon Ody C, Finazzi Dario, Rippert Alyssa, Li Dong, Truxal Kristen, Nandi Deipanjan, Lampert Brent C, Yeo Mildrid, Gardham Alice, Nissan Batel, Horowitz Cederboim Smadar, Moretti Alessandra, Iuso Arcangela
机构信息
Regenerative Medicine in Cardiovascular Diseases, First Department of Medicine, TUM University Hospital, Klinikum Rechts der Isar, Technical University of Munich, School of Medicine and Health, Munich, Germany.
Institute of Neurogenomics, Helmholtz Zentrum München, Neuherberg, Germany.
出版信息
Commun Med (Lond). 2025 Jul 31;5(1):323. doi: 10.1038/s43856-025-01017-z.
BACKGROUND
PPCS deficiency disorder (PPCS DD) is an ultra-rare, autosomal recessive form of dilated cardiomyopathy (DCM) caused by pathogenic variants in PPCS, which encodes the enzyme catalyzing the second step in the coenzyme A (CoA) biosynthesis pathway. To date, only six patients worldwide have been identified.
METHODS
Whole-exome sequencing was performed to identify pathogenic PPCS variants in affected individuals. Protein stability was assessed by Western blotting. CoA levels were quantified using a microplate-based assay in patient-derived fibroblasts, cardiac progenitor cells, and cardiomyocytes. Functional evaluation of cardiac cells and engineered heart patches was conducted to investigate contractile performance and arrhythmogenicity. Pantethine was tested as a potential therapeutic agent both in vitro and through long-term clinical follow-up in patients.
RESULTS
Causative PPCS variants are identified in six individuals with DCM and variable associated features, including neuromuscular and neurological symptoms. Identified variants lead to reduced PPCS protein stability and decreased cellular CoA levels. Cardiac cells exhibit impaired contractility and arrhythmias, which are partially rescued by pantethine treatment. Clinically, patients receiving pantethine show sustained improvement over time.
CONCLUSIONS
Our study expands the genetic and clinical spectrum of PPCS deficiency disorder, identifying six new cases with diverse phenotypes. Functional investigations reveal reduced CoA levels and dysfunction in patient-derived cardiac cells. Pantethine treatment shows promise in partially rescuing DCM phenotypes, both in vitro and in patients. However, complete reversal may require early intervention. These findings underscore the importance of timely diagnosis and treatment in PPCS DD. Future research should focus on optimizing pantethine supplementation and exploring additional therapies to enhance CoA levels and cardiac function in affected individuals.
背景
PPCS缺乏症(PPCS DD)是一种极为罕见的常染色体隐性扩张型心肌病(DCM),由PPCS的致病变异引起,PPCS编码催化辅酶A(CoA)生物合成途径第二步的酶。迄今为止,全球仅确诊了6例患者。
方法
对受影响个体进行全外显子组测序以鉴定致病的PPCS变异。通过蛋白质印迹法评估蛋白质稳定性。使用基于微孔板的检测方法对患者来源的成纤维细胞、心脏祖细胞和心肌细胞中的CoA水平进行定量。对心脏细胞和工程化心脏补片进行功能评估,以研究收缩性能和致心律失常性。在体外以及对患者进行长期临床随访时,测试泛硫乙胺作为一种潜在治疗药物的效果。
结果
在6例患有DCM及包括神经肌肉和神经症状在内的各种相关特征的个体中鉴定出致病的PPCS变异。所鉴定的变异导致PPCS蛋白稳定性降低以及细胞CoA水平下降。心脏细胞表现出收缩功能受损和心律失常,泛硫乙胺治疗可部分缓解这些症状。临床上,接受泛硫乙胺治疗的患者随时间推移病情持续改善。
结论
我们的研究扩展了PPCS缺乏症的遗传和临床谱,鉴定出6例具有不同表型的新病例。功能研究揭示患者来源的心脏细胞中CoA水平降低和功能障碍。泛硫乙胺治疗在体外和患者中均显示出部分挽救DCM表型的前景。然而,完全逆转可能需要早期干预。这些发现强调了PPCS DD及时诊断和治疗的重要性。未来的研究应侧重于优化泛硫乙胺补充,并探索其他疗法以提高受影响个体的CoA水平和心脏功能。
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