<i>MPV17</i>-related mitochondrial DNA maintenance defect: New cases and review of clinical, biochemical, and molecular aspects

El‐Hattab, Ayman W.; Wang, Julia; Dai, Hongzheng; Almannai, Mohammed; Staufner, Christian; Alfadhel, Majid; Gambello, Michael J.; Prasun, Pankaj; Raza, Saleem; Lyons, Hernando; Afqi, Manal; Saleh, Mohammed A.; Faqeih, Eissa; Alzaidan, Hamad; Alshenqiti, Abduljabbar; Flore, Leigh Anne; Hertecant, Jozef; Sacharow, Stephanie; Barbouth, Deborah; Murayama, Kei; Shah, Ankur; Lin, Henry C.; Wong, Lee Jun

doi:10.1002/humu.23387

Cited by 52 publications

(74 citation statements)

References 33 publications

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“…We describe five patients from two unrelated families with homozygous MPV17 mutations with isolated, juvenile‐onset peripheral neuropathy. MPV17 ‐related disease generally presents with peripheral nerve dysfunction, but neuropathy is rarely the predominant feature, as infantile‐ or early‐childhood‐onset chronic liver failure and progressive CNS involvement usually cause severe morbidity and early mortality . This constellation is similar in other mitochondrial conditions in which a peripheral neuropathy is part of the clinical picture, for example, ataxia‐neuropathy spectrum ( POLG1 mutations), mitochondrial neurogastrointestinal encephalopathy ( TYMP mutations) or neuropathy, ataxia, and retinitis pigmentosa ( MTATP6 mutations) .…”

Section: Discussionsupporting

confidence: 91%

“…MPV17-related disease generally presents with peripheral nerve dysfunction, but neuropathy is rarely the predominant feature, as infantile-or early-childhood-onset chronic liver failure and progressive CNS involvement usually cause severe morbidity and early mortality. 4,9 This constellation is similar in other mitochondrial conditions in which a peripheral neuropathy is part of the clinical picture, for example, ataxia-neuropathy spectrum (POLG1 mutations), mitochondrial neurogastrointestinal encephalopathy (TYMP mutations) or neuropathy, ataxia, and retinitis pigmentosa (MTATP6 mutations). 10 Mitochondrial neuropathies presenting as isolated Charcot-Marie-Tooth disease arise from MFN2 (CMT2A2), GDAP1 (CMT2K, CMT4A, CMTRIA) and-in few families-MTATP6 mutations.…”

Section: Discussionmentioning

confidence: 68%

“…Patients F2.1, F2.2 and F2.3 carry a newly described homozygous splice‐region mutation (c.376‐9T>G), leading to an in‐frame deletion due to skipping of exon 6 in a considerable proportion of MPV17 mRNA. Notably, similar c.376‐1G>A and c.376‐2A>C variants were recently reported in cases with neurohepatopathy . Although no mRNA studies were presented for these variants, it is conceivable that they have more serious effects on splicing, probably resulting in skipping of exon 6 in all transcripts, which may explain the more severe phenotype.…”

Section: Discussionmentioning

confidence: 99%

“…These findings are most similar to those in two patients reported by Choi et al, who were diagnosed with neuropathy at age 9 and 13 years and have remained without signs of liver or brain involvement until age 22 and 34 years, respectively (Table S1). 8 9 Although no mRNA studies were presented for these variants, it is conceivable that they have more serious effects on splicing, probably resulting in skipping of exon 6 in all transcripts, which may explain the more severe phenotype. On the other hand, the c.122G>A (Table S1).…”

Section: Discussionmentioning

confidence: 99%

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MPV17 mutations in juvenile‐ and adult‐onset axonal sensorimotor polyneuropathy

Baumann

Schreiber²,

Schlotter‐Weigel

et al. 2018

Clinical Genetics

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MPV17 encodes a putative channel‐forming protein of the inner mitochondrial membrane and is involved in mitochondrial deoxynucleotide homeostasis. MPV17 mutations were first reported in patients with Navajo neurohepatopathy, an autosomal recessive mitochondrial DNA depletion syndrome, characterized by early‐onset liver failure, failure to thrive as well as central and peripheral neurological involvement. Recently, two patients with juvenile‐onset peripheral sensorimotor neuropathy associated with an MVP17 c.122G>A (p.Arg41Gln) variant have been reported. Here, we describe five additional patients from two unrelated families with sensorimotor axonal neuropathy without hepatocerebral affection caused by homozygous MPV17 variants. Patients of the first family carried the known c.122G>A variant and affected individuals of the second family had a novel c.376‐9T>G near‐splice variant, which was shown to result in an in‐frame deletion of 11 amino acids. This report provides further evidence that MPV17 mutations should be considered in patients with pure, non‐syndromic axonal neuropathy.

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Section: Discussionsupporting

confidence: 91%

Section: Discussionmentioning

confidence: 68%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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MPV17 mutations in juvenile‐ and adult‐onset axonal sensorimotor polyneuropathy

Baumann

Schreiber²,

Schlotter‐Weigel

et al. 2018

Clinical Genetics

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“…To date, MPV17-related hepatocerebral MTDPS has been reported in 96 patients [4,5, . Disease prognosis is severe, given that ~80% of patients die from liver failure during early childhood [30] . Hepatic cirrhosis has been diagnosed in 20 patients, while three patients had hepatocellular carcinoma (HCC) [10,15,25] .…”

Section: Introductionmentioning

confidence: 99%

First cases of MPV17 related mitochondrial DNA depletion syndrome with compound heterozygous mutations in p.R50Q/p.R50W: a case report

Umetsu¹,

Inui²,

Kobayashi³

et al. 2020

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Mutations in MPV17 lead to severe mitochondrial DNA depletion syndrome (MTDPS). All known p.R50W variants in MPV17 are lethal. The homozygous variant p.R50Q in MPV17 among patients with Navajo neurohepatopathy is known to allow longer survival, although heterozygous variants p.R50Q have not been reported. This is the first clinical report in compound heterozygosity MPV17 mutation (p.R50W/p.R50Q). Three siblings were admitted due to multiple hepatic nodules; none presented neurological abnormalities. However, they suffered from severe hypoglycemia and cyclic vomiting. The diagnosis of MPV17-related MTDPS was confirmed by detection of a compound heterozygous MPV17 mutation (p.R50W/p.R50Q), and striking reduction of hepatic mitochondrial DNA. One patient developed pediatric-onset of hepatocellular carcinoma. Notably, all patients survived for extended periods, including two patients who received liver transplantation, which contrasted the high mortality rate associated with p.R50W mutations, as previously reported. The p.R50Q mutation might be associated with longer survival and improved liver transplantation outcomes.

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Clan genomics: From OMIM phenotypic traits to genes and biology

Lupski

2021

American J of Med Genetics Pt A

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Clinical characterization of a patient phenotype has been the quintessential approach for elucidating a differential diagnosis and a hypothesis to explore a potential clinical diagnosis. This has resulted in a language of medicine and a semantic ontology, with both specialty‐ and subspecialty‐specific lexicons, that can be challenging to translate and interpret. There is no ‘Rosetta Stone’ of clinical medicine such as the genetic code that can assist translation and interpretation of the language of genetics. Nevertheless, the information content embodied within a clinical diagnosis can guide management, therapeutic intervention, and potentially prognostic outlook of disease enabling anticipatory guidance for patients and families. Clinical genomics is now established firmly in medical practice. The granularity and informative content of a personal genome is immense. Yet, we are limited in our utility of much of that personal genome information by the lack of functional characterization of the overwhelming majority of computationally annotated genes in the haploid human reference genome sequence. Whereas DNA and the genetic code have provided a ‘Rosetta Stone’ to translate genetic variant information, clinical medicine, and clinical genomics provide the context to understand human biology and disease. A path forward will integrate deep phenotyping, such as available in a clinical synopsis in the Online Mendelian Inheritance in Man (OMIM) entries, with personal genome analyses.

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MPV17-related mitochondrial DNA maintenance defect: New cases and review of clinical, biochemical, and molecular aspects

Cited by 52 publications

References 33 publications

MPV17 mutations in juvenile‐ and adult‐onset axonal sensorimotor polyneuropathy

MPV17 mutations in juvenile‐ and adult‐onset axonal sensorimotor polyneuropathy

First cases of MPV17 related mitochondrial DNA depletion syndrome with compound heterozygous mutations in p.R50Q/p.R50W: a case report

Clan genomics: From OMIM phenotypic traits to genes and biology

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