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Abstract

Background:

Mutations within the myotubularin-related protein 9 gene (MTMR9) have been identified in several families with nonsyndromic intellectual disability (NSID), a generalized neurodevelopmental disorder; however, the relationship between MTMR9 and NSID needs to be verified using a larger sample size.

Aim:

To explore whether genetic variants in the MTMR9 gene are linked to susceptibility of NSID among the Chinese population.

Materials and Methods:

Seven single nucleotide polymorphisms (SNPs) of the MTMR9 gene (rs4559208, rs3824211, rs2164272, rs2164273, rs1897951, rs6991606, and rs7815802) were analyzed using family-based association testing among 258 Han Chinese NSID families.

Results:

Three SNPs of MTMR9 were significantly associated with NSID (z = 2.152, p = 0.031 for rs4559208; z = 2.403, p = 0.016 for rs2164273; and z = 2.758, p = 0.006 for rs7815802). Three alleles of these SNPs were more likely to be transferred from the carrier parents to the affected offspring. Haplotypes constructed using these SNPs also showed a similar transmitting trend (z = 2.505, p = 0.012, χ²₍₃₎ = 8.835, and global p = 0.032). Carriers with the G-G-C haplotype showed a higher risk of NSID (odds ratio = 1.46, 95% confidence interval [1.01-2.09], p = 0.04) than others. In silico functional predictions supported an etiological role for these three SNPs in NSID biology.

Conclusions:

This study provides additional insights into the association of NSID with specific alleles, and haplotypes within the MTMR9 gene. Genotypic analyses of the MTMR9 gene should be considered for patients presenting with NSID of unknown etiology.

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References

Barrett

, Fry

, Maller

, et al. (2005) Haploview: analysis and visualization of LD and haplotype maps. Bioinformatics, 21:263-265.

Basehore

, Marlowe

, Jones

, et al. (2012) Validation of a screening tool for the rapid and reliable detection of CGG trinucleotide repeat expansions in FMR1. Genet Test Mol Bioma, 16:465-470.

Baulac

, Gourfinkel-An

, Couarch

, et al. (2008) A novel locus for generalized epilepsy with febrile seizures plus in French families. Arch neurol, 65:943-951.

Boyle

, Hong

, Hariharan

, et al. (2012) Annotation of functional variation in personal genomes using RegulomeDB. Genome Res, 22:1790-1797.

Consortium

(2015) Human genomics. The Genotype-Tissue Expression (GTEx) pilot analysis: multitissue gene regulation in humans. Science, 348, 648-660.

Gabriel

, Schaffner

, Nguyen

, et al. (2002) The structure of haplotype blocks in the human genome. Science, 296:2225-2229.

Gauderman

(2002) Sample size requirements for matched case-control studies of gene-environment interaction. Stat Med, 21:35-50.

Gong

, Cai

(1993) Wechsler Intelligence Scale for Children Chinese Revision (C-WISC). Map Press, Changsha.

Gong

, Dai

(1992a) Chinese-Wechsler Yong Children Scale of Intelligence (C-WYCSI). Map Press, Changsha.

10.

Gong

, Dai

(1992b) The Manual of Chinese Revision of the Wechsler Adult Intelligence Scale (WAIS-RC). Map Press, Changsha.

11.

Hamdan

, Daoud

, Patry

, et al. (2013) Parent-child exome sequencing identifies a de novo truncating mutation in TCF4 in non-syndromic intellectual disability. Clin Genet, 83:198-200.

12.

Hnia

, Vaccari

, Bolino

, et al. (2012) Myotubularin phosphoinositide phosphatases: cellular functions and disease pathophysiology. Trends Mol Med, 18:317-327.

13.

Hotta

, Kitamoto

, et al. (2011) Association of variations in the FTO, SCG3 and MTMR9 genes with metabolic syndrome in a Japanese population. J Hum Genet, 56:647-651.

14.

Iwase

, Bérubé

, Zhou

, et al. (2017) Epigenetic etiology of intellectual disability. J Neurosci, 37:10773-10782.

15.

Jansen

, Hottenga

, Nivard

, et al. (2017) Conditional eQTL analysis reveals allelic heterogeneity of gene expression. Hum Mol Genet, 26:1444-1451.

16.

Joehanes

, Zhang

, Huan

, et al. (2017) Integrated genome-wide analysis of expression quantitative trait loci aids interpretation of genomic association studies. Genome Biol, 18:16.

17.

Kaufman

, Ayub

, Vincent

(2010) The genetic basis of non-syndromic intellectual disability: a review. J Neurodev Disord, 2:182-209.

18.

Lappalainen

, Sammeth

, Friedlander

, et al. (2013) Transcriptome and genome sequencing uncovers functional variation in humans. Nature, 501: 506-511.

19.

Leonard

, Wen

(2002) The epidemiology of mental retardation: challenges and opportunities in the new millennium. Dev Disabil Res Rev, 8:117-134.

20.

Liu

, Bankaitis

(2010) Phosphoinositide phosphatases in cell biology and disease. Prog Lipid Res, 49:201-217.

21.

, Hinds

, Tung

, et al. (2017) Genome-wide analyses for personality traits identify six genomic loci and show correlations with psychiatric disorders. Nat Genet, 49:152-156.

22.

Luque

, Zhang

(2017) Bioinformatics identifies a list of 368 common altered genes (candidate genes) including two possible gene subnetworks of disease in a Chinese family with non syndromic intellectual disability (NSID). Paper presented at the 2017 CajalXmas Meeting-Madrid (Spain).

23.

Mochizuki

, Majerus

(2003) Characterization of myotubularin-related protein 7 and its binding partner, myotubularin-related protein 9. Proc Natl Acad Sci U S A, 100:9768-9773.

24.

Monies

, Abouelhoda

, Alsayed

, et al. (2017) The landscape of genetic diseases in Saudi Arabia based on the first 1000 diagnostic panels and exomes. Hum Genet, 136:921-939.

25.

O'Connell

, Weeks

(1998) PedCheck: a program for identification of genotype incompatibilities in linkage analysis. Am J Hum Genet, 63:259-266.

26.

Robinson

, Dixon

(2006) Myotubularin phosphatases: policing 3-phosphoinositides. Trends Cell Biol, 16:403-412.

27.

Smith

, Escott-Price

, Davies

, et al. (2016) Genome-wide analysis of over 106 000 individuals identifies 9 neuroticism-associated loci. Mol Psychiatr, 21:749-757.

28.

Staley

, Blackshaw

, Kamat

, et al. (2016) PhenoScanner: a database of human genotype-phenotype associations. Bioinformatics, 32:3207-3209.

29.

Stephens

, Smith

, Donnelly

(2001) A new statistical method for haplotype reconstruction from population data. Am J Hum Genet, 68:978-989.

30.

Ward

, Kellis

(2012) HaploReg: a resource for exploring chromatin states, conservation, and regulatory motif alterations within sets of genetically linked variants. Nucleic Acids Res, 40:930-934.

31.

Zhang

, Li

, Gao

, et al. (2004) An investigation of mental retarded children aged 0-14 in Qinba mountain areas. J Fourth Mil Med Univ, 25:511-514.

32.

Zhang

, Xi

, Wang

, et al. (2012) A Family-Based Association Study of DIO2 and children mental retardation in the Qinba region of China. J Hum Genet, 57:14-17.

33.

Zhernakova

, Deelen

, Vermaat

, et al. (2017) Identification of context-dependent expression quantitative trait loci in whole blood. Nat Genet, 49:139-145.

34.

Zou

, Chang

, Marjanovic

, et al. (2009) MTMR9 increases MTMR6 enzyme activity, stability, and role in apoptosis. J Biol Chem, 284:2064-2071.

35.

Zou

, Zhang

, Marjanovic

, et al. (2012) Myotubularin-related protein (MTMR) 9 determines the enzymatic activity, substrate specificity, and role in autophagy of MTMR8. Proc Natl Acad Sci U S A, 109:9539-9544.

36.

Zuo

, Zhang

, Lei

(1988) Adaptive Scale of Children Chinese. Medical University of China, Beijing.

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Genetic Variants of the MTMR 9 Gene Are Associated with Nonspecific Intellectual Disability: A Family-Based Association Study

Abstract

Background:

Aim:

Materials and Methods:

Results:

Conclusions:

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References

Supplementary Material