Large copy number variations in combination with point mutations in the TYMP and SCO2 genes found in two patients with mitochondrial disorders

Vondráčková, Alžběta; Veselá, Kateřina; Kratochvílová, Hana; Vidrová, Kučerová; Vinsova, Kamila; Stránecký, Viktor; Honzík, Tomáš; Hansı́ková, Hana; Zeman, Jiřı́; Tesařová, Markéta

doi:10.1038/ejhg.2013.148

Cited by 13 publications

(8 citation statements)

References 23 publications

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“…The TYMP gene has been mapped to the chromosomal locus 22q13.32-qter (Hirano et al, 1998; Nishino et al, 1999, 2000). Since the identification of TYMP as the gene responsible for MNGIE, 92 different mutations have been reported by the Human Gene Mutation Database (HGMD Professional 2018.2, accessed September 2018) (Stenson et al, 2014), including 56 missense/nonsense (Nishino et al, 1999, 2000; Gamez et al, 2002; Kocaefe et al, 2003; Hirano et al, 2004b; Martín et al, 2004; Marti et al, 2005; Said et al, 2005; Slama et al, 2005; Carod-Artal et al, 2007; Schupbach et al, 2007; Monroy et al, 2008; Massa et al, 2009; Poulton et al, 2009; Bariş et al, 2010; Garone et al, 2011; Nalini and Gayathri, 2011; Scarpelli et al, 2012; Mihaylova et al, 2013; Suh et al, 2013; Benureau et al, 2014; Vondrácková et al, 2014; Peedikayil et al, 2015; Wang et al, 2015; Karyampudi et al, 2016), 13 splice site mutations (Nishino et al, 1999, 2000; Kocaefe et al, 2003; Szigeti et al, 2004b; Slama et al, 2005; Laforce et al, 2009; Taanman et al, 2009; Garone et al, 2011; Libernini et al, 2012; Halter et al, 2015), 13 small deletions (Nishino et al, 1999, 2000; Blazquez et al, 2005; Slama et al, 2005; Poulton et al, 2009; Filosto et al, 2011; Garone et al, 2011; Torres-Torronteras et al, 2011; Halter et al, 2015; Karyampudi et al, 2016), 6 small insertions (Nishino et al, 1999; Gamez et al, 2002; Hirano et al, 2004b; Kintarak et al, 2007; Poulton et al, 2009; Cardaioli et al, 2010), 2 small indels (Garone et al, 2011; Libernini et al, 2012) 1 gross insertion (Wang et al, 2017) and 1 gross deletion (Vondrácková et al, 2014). These mutations have been mapped to either exonic or intronic regions, with some identified as benign and some as pathogenic variants.…”

Section: Molecular Etiologymentioning

confidence: 99%

Mitochondrial Neurogastrointestinal Encephalomyopathy: Into the Fourth Decade, What We Have Learned So Far

et al. 2018

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Mitochondrial neurogastrointestinal encephalomyopathy (MNGIE) is an ultra-rare metabolic autosomal recessive disease, caused by mutations in the nuclear gene TYMP which encodes the enzyme thymidine phosphorylase. The resulting enzyme deficiency leads to a systemic accumulation of the deoxyribonucleosides thymidine and deoxyuridine, and ultimately mitochondrial failure due to a progressive acquisition of secondary mitochondrial DNA (mtDNA) mutations and mtDNA depletion. Clinically, MNGIE is characterized by gastrointestinal and neurological manifestations, including cachexia, gastrointestinal dysmotility, peripheral neuropathy, leukoencephalopathy, ophthalmoplegia and ptosis. The disease is progressively degenerative and leads to death at an average age of 37.6 years. As with the vast majority of rare diseases, patients with MNGIE face a number of unmet needs related to diagnostic delays, a lack of approved therapies, and non-specific clinical management. We provide here a comprehensive collation of the available knowledge of MNGIE since the disease was first described 42 years ago. This review includes symptomatology, diagnostic procedures and hurdles, in vitro and in vivo disease models that have enhanced our understanding of the disease pathology, and finally experimental therapeutic approaches under development. The ultimate aim of this review is to increase clinical awareness of MNGIE, thereby reducing diagnostic delay and improving patient access to putative treatments under investigation.

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Section: Molecular Etiologymentioning

confidence: 99%

Mitochondrial Neurogastrointestinal Encephalomyopathy: Into the Fourth Decade, What We Have Learned So Far

et al. 2018

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“…This “neighboring effect” could explain the lack of specific genotype-phenotype and why there was no specific association between abnormalities in ETC Complex I activity and a specific deletions of the NDUFA6 gene. Alternatively, intact genes within regions of large chromosomal deletions have been shown to have point mutation, resulting in expression of recessive mitochondrial disorders 10 . This suggests that the same pathological processes that caused the copy number variation may also cause smaller changes in nearby genes that would not be detected by microarray.…”

Section: Discussionmentioning

confidence: 99%

“…Recently, Frye 4 noted that 6 mitochondrial genes are proximal to the SHANK3 gene within the 22q13 region, suggesting that copy number variations in this chromosomal region may have the potential to cause abnormal mitochondrial function. These genes include those essential for complex I (NDUFA6) and IV (SCO2) function of the electron transport chain (ETC) as well as mitochondrial DNA (TYMP), RNA (TRMU) and fatty acid (CPT1B) metabolism and tricaboxylic acid cycle function (ACO2) 5 6 7 8 9 10 11 12 13 14 15 16 17 18 . Table 1 outlines these genes as well as the mitochondrial diseases with which they have been associated.…”

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confidence: 99%

Mitochondrial Dysfunction may explain symptom variation in Phelan-McDermid Syndrome

Frye

Cox

Slattery

et al. 2016

Sci Rep

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Phelan-McDermid Syndrome (PMS), which is defined by a deletion within 22q13, demonstrates significant phenotypic variation. Given that six mitochondrial genes are located within 22q13, including complex I and IV genes, we hypothesize that mitochondrial complex activity abnormalities may explain phenotypic variation in PMS symptoms. Complex I, II, II + III and IV activity was measured in 51 PMS participants. Caretakers completed questionnaires and provided genetic information through the PMS foundation registry. Complex activity was abnormal in 59% of PMS participants. Abnormalities were found in complex I and IV but not complex II + III and II activity, consistent with disruption of genes within the 22q13 region. However, complex activity abnormalities were not related to specific gene deletions suggesting a “neighboring effect” of regional deletions on adjacent gene expression. A specific combination of symptoms (autism spectrum disorder, developmental regression, failure-to-thrive, exercise intolerance/fatigue) was associated with complex activity abnormalities. 64% of 106 individuals in the PMS foundation registry who did not have complex activity measured also endorsed this pattern of symptoms. These data suggest that mitochondrial abnormalities, specifically abnormalities in complex I and IV activity, may explain some phenotypic variation in PMS individuals. These results point to novel pathophysiology mechanisms and treatment targets for PMS patients.

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“…MtD was suspected because of the clinical presentation with occasional double vision and ptosis since 10 years earlier, hypertelorism, brachydactylia, renal insufficiency, bilateral progressive renal cysts, the suprarenal adenomas, hypertriglyceridemia, arterial hypertension, hypertrophic cardiomyopathy with a restrictive filling pattern, and psoriasis. Left ventricular hypertrophy was attributed to the suspected genetic defect because blood pressure was well controlled, hypertrophic cardiomyopathy has been reported as a mani- festation of MtD (Palecek et al 2012;Vondráčková et al 2013), and because left ventricular hypertrophy was extensive. Hypertelorism and brachydactylia were also suggestive of MtD since they have been reported as MtD manifestations (Pronicki et al 2002;Finsterer 2011).…”

Section: Discussionmentioning

confidence: 99%

Severe Hypokalemic Paralysis as a Manifestation of a Mitochondrial Disorder

Finsterer

Lässer

2013

Tohoku J. Exp. Med.

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Mitochondrial disorder (MtD) is usually a multisystem disease due to impaired mitochondrial energy production. Severe hypokalemia resulting in muscle weakness and rhabdomyolysis has not been reported as a phenotypic feature of MtD. Here we describe a 60-year-old male patient who developed myalgias followed by generalized muscle weakness a few days before admission. Symptoms were attributed to severe hypokalemia that occurred after the patient had discontinued spironolactone, a competitive antagonist of the aldosterone receptor, four months earlier on his own judgment. Spironolactone was given for 10 years to treat suspected primary hyperaldosteronism (Conn's syndrome). He presented with myopathic face, bilateral ptosis, hypertelorism, brachydactylia, weakness of the axial and limb muscles, and bilateral leg edema. Hypertelorism and brachydactylia are known as physical traits of MtD. Laboratory investigations revealed hypokalemia of 1.7 mmol/l and elevated serum levels of creatine kinase (2,772 U/l). Electrocardiogram showed sinus rhythm, left bundle-branch-block, repolarization abnormalities, and prolonged QTc (571 ms), which is associated with a propensity to ventricular arrhythmias. Diagnostic work-up revealed bilateral adenomas of the suprarenal glands. Conn's syndrome was regarded as a manifestation of MtD, since MtDs are frequently associated with endocrine abnormalities. The patient also presented with occasional double vision, ptosis, renal insufficiency, bilateral renal cysts, hypertriglyceridemia, arterial hypertension, and hypertrophic cardiomyopathy. Taken together, we have made the diagnosis of MtD. In conclusion, MtD may be associated with adrenal adenomas, which may cause severe symptomatic hypokalemia, manifesting as generalized weakness and myalgias due to rhabdomyolysis. Endocrine involvement may be a phenotypic feature of MtD.

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Large copy number variations in combination with point mutations in the TYMP and SCO2 genes found in two patients with mitochondrial disorders

Cited by 13 publications

References 23 publications

Mitochondrial Neurogastrointestinal Encephalomyopathy: Into the Fourth Decade, What We Have Learned So Far

Mitochondrial Neurogastrointestinal Encephalomyopathy: Into the Fourth Decade, What We Have Learned So Far

Mitochondrial Dysfunction may explain symptom variation in Phelan-McDermid Syndrome

Severe Hypokalemic Paralysis as a Manifestation of a Mitochondrial Disorder

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