Cardiac pathology in a patient with a novel pathogenic variant c.703del (p.Ile235SerfsTer4) of the TAFAZZIN gene

IF 2.3 4区医学 Q2 CARDIAC & CARDIOVASCULAR SYSTEMS

Cardiovascular Pathology Pub Date : 2025-07-10 DOI:10.1016/j.carpath.2025.107749

Marisa Prasanpanich , Majid Husain , Nancy J. Halnon , Richard Chang , Neda Zadeh , Jason Knight , Gregory A. Fishbein

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引用次数: 0

Abstract

Introduction

Barth syndrome is a mitochondrial disease caused by loss-of-function mutations in the TAFAZZIN gene located on chromosome Xq28 encoding a transacylase essential for cardiolipin remodeling. Most patients develop dilated cardiomyopathy and progressive heart failure within the first year of life with some requiring cardiac transplantation.

Case Report

A full-term male infant with an anatomically normal heart presented postnatally with cardiogenic shock necessitating VA-ECMO within the second day of life. WGS revealed a pathogenic c.703del (p.Ile235SerfsTer4) variant in the TAFAZZIN gene. While on the waitlist for cardiac transplantation, he was treated with intravenous Elamipretide, a mitochondrially-targeted tetrapeptide interacting with cardiolipin, without significant side effects, started at three weeks old and continued through transplantation. He underwent a successful orthotopic cardiac transplantation at five months of age. The explanted heart showed dilated left ventricle with hypertrabeculation and was remarkable for endocardial fibroelastosis and diffuse sarcoplasmic vacuolization with coarse granularity. Ultrastructurally, mitochondria displayed megaconia and replacement of cristae by circular, vesicular, cylindrical, and fingerprint-like structures. He continues to do well as an outpatient and remains on subcutaneous Elamipretide.

Summary

We describe a case of Barth syndrome harboring a novel pathogenic variant of the TAFAZZIN gene exhibiting dilated cardiomyopathy, hypertrabeculation, endocardial fibroelastosis, and prominent mitochondrial abnormality. Elamipretide was well tolerated.

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TAFAZZIN基因c.703del （p.p ile235serfster4）新型致病变异患者的心脏病理

简介：Barth综合征是一种线粒体疾病，由位于染色体Xq28上的TAFAZZIN基因的功能缺失突变引起，该基因编码心磷脂重塑所必需的转酰基酶。大多数患者在出生后一年内发展为扩张型心肌病和进行性心力衰竭，其中一些患者需要心脏移植。病例报告：一个解剖心脏正常的足月男婴在出生后出现心源性休克，需要在生命的第二天进行VA-ECMO。WGS在TAFAZZIN基因中发现致病性c.703del （p.e ile235serfster4）变异。在等待心脏移植的过程中，他从三周大开始静脉注射埃拉米pretide，这是一种线粒体靶向的四肽，与心磷脂相互作用，没有明显的副作用。他在5个月大时成功接受了原位心脏移植手术。移植心脏左心室扩张伴小梁亢进，心内膜纤维弹性增生，弥漫性肌浆空泡形成，颗粒粗大。超微结构上，线粒体呈巨缩状，嵴被圆形、水泡状、圆柱形和指纹状结构所取代。作为门诊病人，他继续做得很好，并继续皮下使用埃拉米普肽。摘要：我们描述了一例Barth综合征，其中TAFAZZIN基因具有一种新的致病变异，表现为扩张性心肌病、小梁亢进、心内膜纤维弹性增生和显著的线粒体异常。埃拉米普肽耐受性良好。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Cardiovascular Pathology 医学-病理学

CiteScore

7.50

自引率

2.70%

发文量

审稿时长

18 days

期刊介绍： Cardiovascular Pathology is a bimonthly journal that presents articles on topics covering the entire spectrum of cardiovascular disease. The Journal''s primary objective is to publish papers on disease-oriented morphology and pathogenesis from clinicians and scientists in the cardiovascular field. Subjects covered include cardiovascular biology, prosthetic devices, molecular biology and experimental models of cardiovascular disease.