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1
Barth syndrome: mechanisms and management.巴特综合征:发病机制与治疗
Appl Clin Genet. 2019 Jun 5;12:95-106. doi: 10.2147/TACG.S171481. eCollection 2019.
2
Intrafamilial variability for novel TAZ gene mutation: Barth syndrome with dilated cardiomyopathy and heart failure in an infant and left ventricular noncompaction in his great-uncle.家族内新型 TAZ 基因突变的变异性:婴儿期伴有扩张型心肌病和心力衰竭的巴尔综合征,以及他叔祖父的左心室心肌致密化不全。
Mol Genet Metab. 2012 Nov;107(3):428-32. doi: 10.1016/j.ymgme.2012.09.013. Epub 2012 Sep 18.
3
A Novel Exonic Splicing Mutation in the TAZ (G4.5) Gene in a Case with Atypical Barth Syndrome.一例非典型Barth综合征患者TAZ(G4.5)基因的新型外显子剪接突变
JIMD Rep. 2013;11:99-106. doi: 10.1007/8904_2013_228. Epub 2013 Apr 19.
4
Barth syndrome cardiomyopathy: targeting the mitochondria with elamipretide.巴特综合征心肌病:以线粒体为靶点的埃拉米肽治疗。
Heart Fail Rev. 2021 Mar;26(2):237-253. doi: 10.1007/s10741-020-10031-3. Epub 2020 Oct 1.
5
Barth syndrome.巴特综合征。
Orphanet J Rare Dis. 2013 Feb 12;8:23. doi: 10.1186/1750-1172-8-23.
6
When silence is noise: infantile-onset Barth syndrome caused by a synonymous substitution affecting TAZ gene transcription.沉默何时成噪音:由影响TAZ基因转录的同义替换引起的婴儿期起病的Barth综合征
Clin Genet. 2016 Nov;90(5):461-465. doi: 10.1111/cge.12756. Epub 2016 Mar 4.
7
Barth Syndrome: From Mitochondrial Dysfunctions Associated with Aberrant Production of Reactive Oxygen Species to Pluripotent Stem Cell Studies.巴斯综合征:从与活性氧异常产生相关的线粒体功能障碍到多能干细胞研究
Front Genet. 2016 Jan 20;6:359. doi: 10.3389/fgene.2015.00359. eCollection 2015.
8
Barth syndrome: cardiolipin, cellular pathophysiology, management, and novel therapeutic targets.巴特综合征:心磷脂、细胞病理生理学、管理和新的治疗靶点。
Mol Cell Biochem. 2021 Mar;476(3):1605-1629. doi: 10.1007/s11010-020-04021-0. Epub 2021 Jan 7.
9
Novel mutations in the TAZ gene in patients with Barth syndrome.Barth综合征患者TAZ基因的新突变
Prague Med Rep. 2013;114(3):139-53. doi: 10.14712/23362936.2014.16.
10
Atypical Clinical Presentations of TAZ Mutations: An Underdiagnosed Cause of Growth Retardation?TAZ 突变的非典型临床表现:生长发育迟缓的一个未被充分诊断的原因?
JIMD Rep. 2016;29:89-93. doi: 10.1007/8904_2015_525. Epub 2016 Jan 3.

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Mitochondrial cardiomyopathies: navigating through different clinical and management pictures between adult and paediatric forms.线粒体心肌病:梳理成人和儿童形式之间不同的临床及管理情况。
Front Cardiovasc Med. 2025 Jul 3;12:1621096. doi: 10.3389/fcvm.2025.1621096. eCollection 2025.
2
Expanded-access use of elamipretide in a newborn with Barth syndrome: a case report.依拉米肽在一名患有巴斯综合征新生儿中的扩大使用:病例报告
Eur Heart J Case Rep. 2025 Jan 22;9(2):ytaf030. doi: 10.1093/ehjcr/ytaf030. eCollection 2025 Feb.
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Precision Genetic Therapies: Balancing Risk and Benefit in Patients with Heart Failure.精准基因治疗:心力衰竭患者的风险与获益平衡。
Curr Cardiol Rep. 2024 Sep;26(9):973-983. doi: 10.1007/s11886-024-02096-5. Epub 2024 Aug 7.
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Mitochondrial bioenergetics and cardiolipin remodeling abnormalities in mitochondrial trifunctional protein deficiency.线粒体三功能蛋白缺陷中的线粒体生物能学和心磷脂重塑异常。
JCI Insight. 2024 Sep 10;9(17):e176887. doi: 10.1172/jci.insight.176887.
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Perturbations in mitochondrial metabolism associated with defective cardiolipin biosynthesis: An real-time NMR study.与心磷脂生物合成缺陷相关的线粒体代谢紊乱:一项实时核磁共振研究。
bioRxiv. 2024 Jun 22:2024.06.18.599628. doi: 10.1101/2024.06.18.599628.
6
Clinical and biochemical footprints of inherited metabolic disease. XVI. Hematological abnormalities.遗传性代谢疾病的临床与生化特征。十六、血液学异常。
Mol Genet Metab. 2023 Dec;140(4):107735. doi: 10.1016/j.ymgme.2023.107735. Epub 2023 Nov 13.
7
Metabolic switch from fatty acid oxidation to glycolysis in knock-in mouse model of Barth syndrome.Barth 综合征敲入鼠模型中脂肪酸氧化向糖酵解的代谢转换。
EMBO Mol Med. 2023 Sep 11;15(9):e17399. doi: 10.15252/emmm.202317399. Epub 2023 Aug 3.
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Clinical and Genetic Screening for Hypertrophic Cardiomyopathy in Paediatric Relatives: Changing Paradigms in Clinical Practice.儿科亲属肥厚型心肌病的临床与基因筛查:临床实践中的范式转变
J Clin Med. 2023 Apr 9;12(8):2788. doi: 10.3390/jcm12082788.
9
Mitochondrial Membranes and Mitochondrial Genome: Interactions and Clinical Syndromes.线粒体膜与线粒体基因组:相互作用及临床综合征
Membranes (Basel). 2022 Jun 15;12(6):625. doi: 10.3390/membranes12060625.
10
Application of the Pluripotent Stem Cells and Genomics in Cardiovascular Research-What We Have Learnt and Not Learnt until Now.多能干细胞和基因组在心血管研究中的应用——到目前为止我们已经学到和没有学到的东西。
Cells. 2021 Nov 10;10(11):3112. doi: 10.3390/cells10113112.

本文引用的文献

1
Barth syndrome: A life-threatening disorder caused by abnormal cardiolipin remodeling.巴特综合征:一种由心磷脂重塑异常引起的危及生命的疾病。
J Rare Dis Res Treat. 2017;2(2):58-62. doi: 10.29245/2572-9411/2017/2.1087. Epub 2017 Mar 21.
2
The role of cardiolipin concentration and acyl chain composition on mitochondrial inner membrane molecular organization and function.心磷脂浓度和酰基链组成对线粒体内膜分子组织和功能的作用。
Biochim Biophys Acta Mol Cell Biol Lipids. 2019 Jul;1864(7):1039-1052. doi: 10.1016/j.bbalip.2019.03.012. Epub 2019 Apr 2.
3
AAV9- Gene Replacement Ameliorates Cardiac TMT Proteomic Profiles in a Mouse Model of Barth Syndrome.腺相关病毒9型基因替代改善了Barth综合征小鼠模型的心脏TMT蛋白质组学图谱。
Mol Ther Methods Clin Dev. 2019 Jan 25;13:167-179. doi: 10.1016/j.omtm.2019.01.007. eCollection 2019 Jun 14.
4
Functional exercise capacity, strength, balance and motion reaction time in Barth syndrome.巴特综合征的功能运动能力、力量、平衡和运动反应时间。
Orphanet J Rare Dis. 2019 Jan 22;14(1):37. doi: 10.1186/s13023-019-1006-8.
5
Overexpression of branched-chain amino acid aminotransferases rescues the growth defects of cells lacking the Barth syndrome-related gene TAZ1.支链氨基酸转氨酶过表达可挽救缺乏 Barth 综合征相关基因 TAZ1 的细胞的生长缺陷。
J Mol Med (Berl). 2019 Feb;97(2):269-279. doi: 10.1007/s00109-018-1728-4. Epub 2019 Jan 3.
6
Neutropenia in Barth syndrome: characteristics, risks, and management.巴特综合征中性粒细胞减少症:特征、风险和管理。
Curr Opin Hematol. 2019 Jan;26(1):6-15. doi: 10.1097/MOH.0000000000000472.
7
Barth syndrome cells display widespread remodeling of mitochondrial complexes without affecting metabolic flux distribution.巴特综合征细胞显示线粒体复合物的广泛重塑,而不影响代谢通量分布。
Biochim Biophys Acta Mol Basis Dis. 2018 Nov;1864(11):3650-3658. doi: 10.1016/j.bbadis.2018.08.041. Epub 2018 Sep 1.
8
BARTH SYNDROME IN MALE AND FEMALE SIBLINGS CAUSED BY A NOVEL MUTATION IN THE TAZ GENE.TAZ基因新突变导致的男性和女性兄弟姐妹患巴特综合征
Genet Couns. 2016;27(4):495-501.
9
AAV-Mediated TAZ Gene Replacement Restores Mitochondrial and Cardioskeletal Function in Barth Syndrome.AAV 介导的 TAZ 基因替换恢复巴特综合征的线粒体和心脏骨骼功能。
Hum Gene Ther. 2019 Feb;30(2):139-154. doi: 10.1089/hum.2018.020. Epub 2018 Oct 3.
10
Aberrant cardiolipin metabolism is associated with cognitive deficiency and hippocampal alteration in tafazzin knockdown mice.心脏脂代谢异常与 tafazzin 敲低小鼠的认知缺陷和海马改变有关。
Biochim Biophys Acta Mol Basis Dis. 2018 Oct;1864(10):3353-3367. doi: 10.1016/j.bbadis.2018.07.022. Epub 2018 Jul 25.

巴特综合征:发病机制与治疗

Barth syndrome: mechanisms and management.

作者信息

Finsterer Josef

机构信息

Krankenanstalt Rudolfstiftung, Messerli Institute, Vienna, Austria.

出版信息

Appl Clin Genet. 2019 Jun 5;12:95-106. doi: 10.2147/TACG.S171481. eCollection 2019.

DOI:10.2147/TACG.S171481
PMID:31239752
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6558240/
Abstract

Barth syndrome is an ultra-rare, infantile-onset, X-linked recessive mitochondrial disorder, primarily affecting males, due to variants in encoding for the cardiolipin transacylase tafazzin. This review aimed to summarize and discuss recent and earlier findings concerning the etiology, pathogenesis, clinical presentation, diagnosis, treatment, and outcome of Barth syndrome. A literature review was undertaken through a MEDLINE search. The phenotype of Barth syndrome is highly variable but most frequently patients present with hypertrophic/dilated/non-compaction cardiomyopathy, fibroelastosis, arrhythmias, neutropenia, mitochondrial myopathy, growth retardation, dysmorphism, cognitive impairment, and other, rarer features. Lactic acid and creatine kinase, and blood and urine organic acids, particularly 3-methylglutaconic acid and monolysocardiolipin, are often elevated. Cardiolipin is decreased. Biochemical investigations may show decreased activity of various respiratory chain complexes. The diagnosis is confirmed by documentation of a causative variant. Treatment is symptomatic and directed toward treating heart failure, arrhythmias, neutropenia, and mitochondrial myopathy. Although Barth syndrome is still an orphan disease, with fewer than 200 cases described so far, there is extensive ongoing research with regard to its pathomechanism and new therapeutic approaches. Although most of these approaches are still experimental, it can be expected that causative strategies will be developed in the near future.

摘要

巴斯综合征是一种极其罕见的、婴儿期发病的、X连锁隐性线粒体疾病,主要影响男性,由心磷脂转酰基酶塔法兹蛋白编码基因的变异所致。本综述旨在总结和讨论关于巴斯综合征的病因、发病机制、临床表现、诊断、治疗及预后的近期和早期研究结果。通过医学文献数据库检索进行了文献综述。巴斯综合征的表型高度可变,但大多数患者常表现为肥厚型/扩张型/心肌致密化不全心肌病、纤维弹性组织增生、心律失常、中性粒细胞减少、线粒体肌病、生长发育迟缓、畸形、认知障碍以及其他较罕见的特征。乳酸和肌酸激酶以及血液和尿液中的有机酸,尤其是3-甲基戊二酸和单溶血心磷脂,通常会升高。心磷脂减少。生化检查可能显示各种呼吸链复合物的活性降低。通过记录致病变异来确诊。治疗是对症治疗,针对心力衰竭、心律失常、中性粒细胞减少和线粒体肌病进行治疗。尽管巴斯综合征仍然是一种罕见病,迄今为止报道的病例不到200例,但关于其发病机制和新治疗方法的研究正在广泛进行。尽管这些方法大多仍处于实验阶段,但有望在不久的将来开发出病因治疗策略。