Fatal infantile mitochondrial encephalomyopathy, hypertrophic cardiomyopathy and optic atrophy associated with a homozygous<i>OPA1</i>mutation

Spiegel, Ronen; Saada, Ann; Flannery, Padraig J.; Burté, Florence; Soiferman, Devorah; Khayat, Morad; Eisner, Verónica; Vladovski, Eugene; Taylor, Robert W.; Bindoff, Laurence A.; Shaag, Avraham; Mandel, Hanna; Schuler-Furman, Ora; Shalev, Stavit A.; Elpeleg, Orly; Yu‐Wai‐Man, Patrick

doi:10.1136/jmedgenet-2015-103361

Cited by 99 publications

(65 citation statements)

References 24 publications

(29 reference statements)

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“…Although OPA1 is highly expressed in the retina, it is broadly expressed throughout the body and this might reflect the multiple disorders that have presented themselves in patients harboring heterozygous mutations of OPA1, including deafness and dementia (Carelli et al, 2015). Until recently, all OPA1 mutations found in patients have been identified as heterozygous, with the only homozygous OPA1 mutation causing early-onset encephalomyopathy, cardiomyopathy and death during infancy (Spiegel et al, 2016). In mice, homozygous Opa1 mutants die in utero, but heterozygous mutants reflect the main features of human ADOA, as well as additional phenotypes including cardiomyopathy (Alavi et al, 2007;Chen et al, 2012;Davies et al, 2007).…”

Section: Opa1 and Fusion Of The Inner Membranementioning

confidence: 99%

OPA1 processing in cell death and disease – the long and short of it

MacVicar

Langer

2016

Journal of Cell Science

340

318

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The regulation of mitochondrial dynamics by the GTPase OPA1, which is located at the inner mitochondrial membrane, is crucial for adapting mitochondrial function and preserving cellular health. OPA1 governs the delicate balance between fusion and fission in the dynamic mitochondrial network. A disturbance of this balance, often observed under stress and pathologic conditions, causes mitochondrial fragmentation and can ultimately result in cell death. As discussed in this Commentary, these morphological changes are regulated by proteolytic processing of OPA1 by the inner-membrane peptidases YME1L (also known as YME1L1) and OMA1. Long, membrane-bound forms of OPA1 are required for mitochondrial fusion, but their processing to short, soluble forms limits fusion and can facilitate mitochondrial fission. Excessive OPA1 processing by the stress-activated protease OMA1 promotes mitochondrial fragmentation and, if persistent, triggers cell death and tissue degeneration in vivo. The prevention of OMA1-mediated OPA1 processing and mitochondrial fragmentation might thus offer exciting therapeutic potential for human diseases associated with mitochondrial dysfunction.

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Section: Opa1 and Fusion Of The Inner Membranementioning

confidence: 99%

OPA1 processing in cell death and disease – the long and short of it

MacVicar

Langer

2016

Journal of Cell Science

340

318

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“…Remarkably, two Italian families carrying different OPA1 missense mutations have been reported with an atypical combination of parkinsonism, dementia and CPEO, but with only subclinical optic neuropathy [34]. More recently, a compound homozygous OPA1 mutation has been identified for the first time in two affected Jewish sisters from consanguineous parents who developed a fatal infantile encephalomyopathy with hypertrophic cardiomyopathy and optic atrophy [123]. However, instead of multiple mtDNA deletions, the muscle biopsy from one sister showed marked mtDNA depletion.…”

Section: Doa Plus Phenotypesmentioning

confidence: 99%

A neurodegenerative perspective on mitochondrial optic neuropathies

et al. 2016

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Mitochondrial optic neuropathies constitute an important cause of chronic visual morbidity and registrable blindness in both the paediatric and adult population. It is a genetically heterogeneous group of disorders caused by both mitochondrial DNA (mtDNA) mutations and a growing list of nuclear genetic defects that invariably affect a critical component of the mitochondrial machinery. The two classical paradigms are Leber hereditary optic neuropathy (LHON), which is a primary mtDNA disorder, and autosomal dominant optic atrophy (DOA) secondary to pathogenic mutations within the nuclear gene OPA1 that encodes for a mitochondrial inner membrane protein. The defining neuropathological feature is the preferential loss of retinal ganglion cells (RGCs) within the inner retina but, rather strikingly, the smaller calibre RGCs that constitute the papillomacular bundle are particularly vulnerable, whereas melanopsin-containing RGCs are relatively spared. Although the majority of patients with LHON and DOA will present with isolated optic nerve involvement, some individuals will also develop additional neurological complications pointing towards a greater vulnerability of the central nervous system (CNS) in susceptible mutation carriers. These so-called “plus” phenotypes are mechanistically important as they put the loss of RGCs within the broader perspective of neuronal loss and mitochondrial dysfunction, highlighting common pathways that could be modulated to halt progressive neurodegeneration in other related CNS disorders. The management of patients with mitochondrial optic neuropathies still remains largely supportive, but the development of effective disease-modifying treatments is now within tantalising reach helped by major advances in drug discovery and delivery, and targeted genetic manipulation.Electronic supplementary materialThe online version of this article (doi:10.1007/s00401-016-1625-2) contains supplementary material, which is available to authorized users.

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“…10 Severe syndromes affecting young children, due to recessive OPA1 inheritance, were also recently reported. 5,11,12 Although ADOA is an ubiquitous condition, [13][14][15][16][17][18] several studies have reported its possibly lower incidence in Asia. 19,20 Our aim was to investigate, for the first time, its occurrence in the multiethnic population of Singapore.…”

Section: Introductionmentioning

confidence: 99%