MN1 C-terminal truncation syndrome is a novel neurodevelopmental and craniofacial disorder with partial rhombencephalosynapsis

Mak, Christopher Chun Yu; Doherty, Dan; Lin, Angela E.; Vegas, Nancy; Cho, Megan T.; Viot, Géraldine; Dimartino, Clémantine; Weisfeld-Adams, James D.; Lessel, Davor; Joss, Shelagh; Li, Chumei; Gonzaga‐Jauregui, Claudia; Zárate, Yuri A.; Ehmke, Nadja; Horn, Denise; Troyer, Caitlin; Kant, Sarina G.; Lee, Youngha; Ishak, Gisele E.; Leung, Gordon; Pritchard, Amanda Barone; Yang, Sandra; Bend, Eric G.; Filippini, Francesca; Roadhouse, Chelsea; Lebrun, Nicolas; Mehaffey, Michele G.; Martin, P.; Apple, Benjamin; Millan, Francisca; Puk, Oliver; Hoffer, Mariëtte J.V.; Henderson, Lindsay B.; McGowan, Ruth; Wentzensen, Ingrid M.; Pei, Steven L. C.; Zahir, Farah; Yu, Mullin H.C.; Gibson, William T.; Seman, Ann; Steeves, Marcie; Murrell, Jill R.; Luettgen, Sabine; Francisco, E. Nicolás; Strom, Tim M.; Amlie‐Wolf, Louise; Kaindl, Angela M.; Wilson, William G.; Halbach, Sara; Basel‐Salmon, Lina; Lev-El, Noa; Denecke, Jonas; Vissers, Lisenka E L M; Radtke, Kelly; Chelly, Jamel; Zackai, Elaine H.; Friedman, Jan M.; Bamshad, Michael J.; Nickerson, Deborah A.; Reid, Russell R.; Devriendt, Koenraad; Chae, Jong‐Hee; Stolerman, Elliot; McDougall, Carey; Powis, Zöe; Bienvenu, Thierry; Tan, Tiong Yang; Orenstein, Naama; Dobyns, William B.; Shieh, Joseph T.C.; Choi, Murim; Waggoner, Darrel; Gripp, Karen W.; Parker, Michael; Stoler, Joan M.; Lyonnet, Stanislas; Cormier‐Daire, Valérie; Viskochil, David; Hoffman, Trevor L.; Amiel, Jeanne; Chung, Brian Hon‐Yin; Gordon, Christopher T.

doi:10.1093/brain/awz379

Cited by 41 publications

(51 citation statements)

References 50 publications

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“…Lastly, the diagnosis of individual U036 was confirmed through international collaboration for new syndrome discovery: MN1 C-terminal truncation syndrome, where 23 individuals who harbor truncating variants at C-terminal of MN1 gene were found to share strikingly similar neurodevelopmental and craniofacial features 51 . It is postulated that these C-terminal truncating variants have escaped nonsense-mediated mRNA decay, thus creating a gain-of-function effect that increased protein stability, diminished cell proliferation, and enhanced MN1 aggregation 51 , 52 .…”

Section: Resultsmentioning

confidence: 96%

A three-year follow-up study evaluating clinical utility of exome sequencing and diagnostic potential of reanalysis

Fung

Huang

et al. 2020

npj Genom. Med.

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Exome sequencing (ES) has become one of the important diagnostic tools in clinical genetics with a reported diagnostic rate of 25–58%. Many studies have illustrated the diagnostic and immediate clinical impact of ES. However, up to 75% of individuals remain undiagnosed and there is scarce evidence supporting clinical utility beyond a follow-up period of >1 year. This is a 3-year follow-up analysis to our previous publication by Mak et al. (NPJ Genom. Med. 3:19, 2018), to evaluate the long-term clinical utility of ES and the diagnostic potential of exome reanalysis. The diagnostic yield of the initial study was 41% (43/104). Exome reanalysis in 46 undiagnosed individuals has achieved 12 new diagnoses. The additional yield compared with the initial analysis was at least 12% (increased from 41% to at least 53%). After a median follow-up period of 3.4 years, change in clinical management was observed in 72.2% of the individuals (26/36), leading to positive change in clinical outcome in four individuals (11%). There was a minimum healthcare cost saving of HKD$152,078 (USD$19,497; €17,282) annually for these four individuals. There were a total of six pregnancies from five families within the period. Prenatal diagnosis was performed in four pregnancies; one fetus was affected and resulted in termination. None of the parents underwent preimplantation genetic diagnosis. This 3-year follow-up study demonstrated the long-term clinical utility of ES at individual, familial and health system level, and the promising diagnostic potential of subsequent reanalysis. This highlights the benefits of implementing ES and regular reanalysis in the clinical setting.

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Section: Resultsmentioning

confidence: 96%

A three-year follow-up study evaluating clinical utility of exome sequencing and diagnostic potential of reanalysis

Fung

Huang

et al. 2020

npj Genom. Med.

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“…MN1 C-Terminal Truncation (MCTT) syndrome is a genetic disorder caused by an MN1 gene alteration. A genetic modification of the MN1 gene was related to intellectual disability (ID) [20].…”

Section: Resultsmentioning

confidence: 99%

The features of novel miRNAs interaction with mRNA candidate genes having trinucleotide repeats in coding sequences and untranslated regions

Belkozhayev

Niyazova

Wilson

2020

ijbch

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“…In the last step, variants in ACP2 were analyzed because an Acp2 ‐ knockout mouse model had a similar phenotype to GLHS (Mannan et al, 2004). We also analyzed variants in MN1 because loss‐of‐function variants in MN1 were identified in patients with RES and dysmorphic features such as mid‐face hypoplasia (Mak et al, 2020).…”

Section: Methodsmentioning

confidence: 99%

Clinical and molecular evaluation of 13 Brazilian patients with Gomez‐López‐Hernández syndrome

Perrone

Perez

D’Almeida

et al. 2020

American J of Med Genetics Pt A

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We aim to characterize patients with Gomez‐López‐Hernández syndrome (GLHS) clinically and to investigate them molecularly. A clinical protocol, including a morphological and neuropsychological assessment, was applied to 13 patients with GLHS. Single‐nucleotide polymorphism (SNP) array and whole‐exome sequencing were undertaken; magnetic resonance imaging was performed in 12 patients, including high‐resolution, heavily T2‐weighted sequences (HRT2) in 6 patients to analyze the trigeminal nerves. All patients presented alopecia; two did not present rhombencephalosynapsis (RES); trigeminal anesthesia was present in 5 of the 11 patients (45.4%); brachycephaly/brachyturricephaly and mid‐face retrusion were found in 84.6 and 92.3% of the patients, respectively. One patient had intellectual disability. HRT2 sequences showed trigeminal nerve hypoplasia in four of the six patients; all four had clinical signs of trigeminal anesthesia. No common candidate gene was found to explain GLHS phenotype. RES does not seem to be an obligatory finding in respect of GLHS diagnosis. We propose that a diagnosis of GLHS should be considered in patients with at least two of the following criteria: focal non‐scarring alopecia, rhombencephalosynapsis, craniofacial anomalies (brachyturrycephaly, brachycephaly or mid‐face retrusion), trigeminal anesthesia or anatomic abnormalities of the trigeminal nerve. Studies focusing on germline whole genome sequencing or DNA and/or RNA sequencing of the alopecia tissue may be the next step for the better understanding of GLHS etiology.

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MN1 C-terminal truncation syndrome is a novel neurodevelopmental and craniofacial disorder with partial rhombencephalosynapsis

Cited by 41 publications

References 50 publications

A three-year follow-up study evaluating clinical utility of exome sequencing and diagnostic potential of reanalysis

A three-year follow-up study evaluating clinical utility of exome sequencing and diagnostic potential of reanalysis

The features of novel miRNAs interaction with mRNA candidate genes having trinucleotide repeats in coding sequences and untranslated regions

Clinical and molecular evaluation of 13 Brazilian patients with Gomez‐López‐Hernández syndrome

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