Sage Journals: Discover world-class research

Abstract

Charcot–Marie–Tooth disease (CMT) is a heritable neurodegenerative disease of peripheral nervous system diseases in which more than 100 genes and their mutations are associated. Two consanguineous families Dera Ghazi Khan (PAK-CMT1-DG KHAN) and Layyah (PAK-CMT2-LAYYAH) with multiple CMT-affected subjects were enrolled from Punjab province in Pakistan. Basic epidemiological data were collected for the subjects. Nerve conduction study (NCS) and electromyography (EMG) were performed for the patients. Whole-exome sequencing (WES) followed by Sanger sequencing was applied to report the genetic basic of CMT. The NCS findings revealed that sensory and motor nerve conduction velocities for both families were <38 m/s. EMG presented denervation, neuropathic motor unit potential, and reduced interference pattern of peripheral nerves. WES identified that a novel nonsense mutation (c. 226 G>T) in GADP1 gene and a previously known missense mutation in MFN2 gene (c. 334 G>A) cause CMT4A (Charcot–Marie–Tooth disease type 4A) in the PAK-CMT1-DG KHAN family and CMT2A (Charcot–Marie–Tooth disease type 2A) in the PAK-CMT2-LAYYAH family, respectively. Mutations followed Mendelian pattern with autosomal recessive mode of inheritance. Multiple sequence alignment by Clustal Omega indicated that mutation-containing domain in both genes is highly conserved, and in situ analysis revealed that both mutations are likely to be pathogenic. We reported that a novel nonsense mutation and a previously known missense mutation in GAPD1 gene and MFN2 gene, respectively, cause CMT in consanguineous Pakistani families.

Get full access to this article

View all access options for this article.

References

Amiott

, Lott

, Soto

, et al. Mitochondrial fusion and function in Charcot-Marie-Tooth type 2A patient fibroblasts with mitofusin 2 mutations. Exp Neurol, 2008; 211(1):115–127.

Chen

, Leyendecker

, van den Bedem

. Kinematic vibrational entropy assessment and analysis of SARS CoV-2 main protease. J Chem Info Model, 2022; 62(11):2869–2879.

Civera-Tregón

, Domínguez

, Martínez-Valero

, et al. Mitochondria and calcium defects correlate with axonal dysfunction in GDAP1-related Charcot-Marie-Tooth mouse model. Neurobiol Dis, 2021; 152:105300; doi: 10.1016/j.nbd.2021.105300

Cuesta

, Pedrola

, Sevilla

, et al. The gene encoding ganglioside-induced differentiation-associated protein 1 is mutated in axonal Charcot-Marie-Tooth type 4A disease. Nat Genet, 2002; 30(1):22–25.

Frappier

, Chartier

, Najmanovich

. ENCoM server: Exploring protein conformational space and the effect of mutations on protein function and stability. Nucleic Acid Res, 2015; 43(W1):W395–W400.

Fridman

, Bundy

, Reilly

, et al. CMT subtypes and disease burden in patients enrolled in the Inherited Neuropathies Consortium natural history study: A cross-sectional analysis. J Neurol Neurosurg Psychiatry, 2015; 86:873–878.

Fortelny

, Pavlidis

, Overall

. The path of no return-truncated protein N-termini and current ignorance of their genesis. Proteomics, 2015; 15(14):2547–2552.

Geng

, Xue

, Roel-Touris

et al. Finding the ΔΔG spot: Are predictors of binding affinity changes upon mutations in protein–protein interactions ready for it?. WIREs Comput Mol Sci, 2019; 9:e1410; doi: 10.1002/wcms.1410

Hassan

, Abbas

, Raza

, et al. Computational analysis of histidine mutations on the structural stability of human tyrosinases leading to albinism insurgence. Mol Biosyst, 2017; 13(8):1534–1544.

10.

Higuchi

, Takashima

. Clinical genetics of Charcot–Marie–Tooth disease. J Hum Genet, 2023; 68:199–214.

11.

Houlden

, Laura

, Wavrant-De Vrièze

, et al. Mutations in the HSP27 (HSPB1) gene cause dominant, recessive, and sporadic distal HMN/CMT type 2. Neurology, 2008; 71:1660–1668.

12.

Huang

, Rodgers

, Hemley

, et al. Effects of pressure and temperature on the atomic fluctuations of dihydrofolate reductase from a psychropiezophile and a mesophile. Int J Mol Sci, 2019; 20(6):1452.

13.

Kabzińska

, Kochański

, Drac

, et al. A novel Met116Thr mutation in the GDAP1 gene in a Polish family with the axonal recessive Charcot–Marie–Tooth type 4 disease. J Neurol Sci, 2006; 241(1–2):7–11.

14.

Kabzińska

, Saifi

, Drac

, et al. Charcot-Marie-Tooth disease type 4C4 caused by a novel Pro153Leu substitution in the GDAP1 gene. Acta Myol, 2007; 26(2):108–111.

15.

Kabzińska

, Strugalska-Cynowska

, Kostera-Pruszczyk

, et al. L239F founder mutation in GDAP1 is associated with a mild Charcot-Marie-Tooth type 4C4 (CMT4C4) phenotype. Neurogenetics, 2010; 11(3):357–366.

16.

Kanwal

, Choi

, Lim

, et al. Novel homozygous mutations in Pakistani families with Charcot-Marie-Tooth disease. BMC Med Genomics, 2021; 14(1):174.

17.

Kim

, Kim

, Nam

, et al. Clinical and neuroimaging features in Charcot-Marie-Tooth patients with GDAP1 mutations. J Clin Neurol, 2021; 17(1):52–62.

18.

Larrea

, Pera

, Gonnelli

, et al. MFN2 mutations in Charcot-Marie-Tooth disease alter mitochondria-associated ER membrane function but do not impair bioenergetics. Hum Mol Genet, 2019; 28(11):1782–1800.

19.

Lehtilahti

, Kallio

, Majamaa

, et al. Phenotype of patients with Charcot-Marie-Tooth with the p.His123Arg Mutation in GDAP1 in Northern Finland. Neurol Genet, 2021; 7(6):e629 doi: 10.1212/NXG.0000000000000629

20.

Miressi

, Benslimane

, Favreau

, et al. GDAP1 involvement in mitochondrial function and oxidative stress, investigated in a Charcot-Marie-Tooth model of hiPSCs-Derived Motor Neurons. Biomedicines, 2021; 9:945.

21.

Mustafa

, Akhtar

, Asif

, et al. Novel missense variants in FGFR1 and FGFR3 causes short stature in enrolled families from Pakistan. Meta Gene, 2020; 26:100778; doi: 10.1016/j.mgene.2020.100778

22.

Nelis

, Erdem

, Van Den Bergh

, et al. Mutations in GDAP1: Autosomal recessive CMT with demyelination and axonopathy. Neurology, 2002; 59(12):1865–1872.

23.

Nicholson

, Magdelaine

, Zhu

, et al. Severe early-onset axonal neuropathy with homozygous and compound heterozygous MFN2 mutations. Neurology, 2008; 70(19):1678–1681.

24.

Niemann

, Ruegg

, La Padula

, et al. Ganglioside-induced differentiation associated protein 1 is a regulator of the mitochondrial network: New implications for Charcot-Marie-Tooth disease. J Cell Biol, 2005; 170(7):1067–1078.

25.

Pedurupillay

, Amundsen

, Barøy

, et al. Clinical and molecular characteristics in three families with biallelic mutations in IGHMBP2. Neuromuscul Disord, 2016; 26(9):570–575.

26.

Pettersen

, Goddard

, Huang

, et al. UCSF Chimera—A visualization system for exploratory research and analysis. J Comput Chem, 2004; 25(13):1605–1612.

27.

Pires

, Ascher

, Blundell

. DUET: A server for predicting effects of mutations on protein stability using an integrated computational approach. Nucleic Acid Res, 2014a;42(Web Server issue):W314–W319.

28.

Pires

, Ascher

, Blundell

. mCSM: Predicting the effects of mutations in proteins using graph-based signatures. Bioinformatics, 2014b;30(3):335–342.

29.

Pisciotta

, Saveri

, Pareyson

. Challenges in treating Charcot-Marie-Tooth disease and related neuropathies: Current management and future perspectives. Brain Sci, 2021; 11(11):1447.

30.

Rodrigues

, Pires

, Ascher

. DynaMut: Predicting the impact of mutations on protein conformation, flexibility and stability. Nucleic Acid Res, 2018; 46(W1):W350–W355.

31.

Studer

, Tauriello

, Bienert

, et al. ProMod3—A versatile homology modelling toolbox. PLoS Comp Biol, 2021; 17(1):e1008667.

32.

Worth

, Preissner

, Blundell

. SDM—A server for predicting effects of mutations on protein stability and malfunction. Nucleic Acid Res, 2011; 39(Web Server issue):W215–W222; doi: 10.1093/nar/gkr363

33.

Wright

, Brown

, Grayton

, et al. Clinical and radiological characterization of novel FIG4-related combined system disease with neuropathy. Clin Genet, 2020; 98:147–154.

34.

Zambon

, Natali Sora

, Cantarella

, et al. Vocal cord paralysis in Charcot–Marie–Tooth type 4b1 disease associated with a novel mutation in the myotubularin-related protein 2 gene: A case report and review of the literature. Neuromuscul Disord, 2017; 27:487–491.

35.

Zanfardino

, Longo

, Amati

, et al. Mitofusin 2 mutation drives cell proliferation in Charcot-Marie-Tooth 2A fibroblasts. Hum Mol Genet, 2023; 32(2):333–350.

36.

Zhou

, Yang

, Ombrello

, et al. Early-onset stroke and vasculopathy associated with mutations in ADA2. N Engl J Med, 2014; 370(10):911–920.

37.

Züchner

, De Jonghe

, Jordanova

, et al. Axonal neuropathy with optic atrophy is caused by mutations in mitofusin 2. Ann Neurol, 2006; 59:276–281.

38.

Züchner

, Mersiyanova

, Muglia

, et al. Mutations in the mitochondrial GTPase mitofusin 2 cause Charcot–Marie–Tooth neuropathy type 2A. Nat Genet, 2004; 36:449–451.

Supplementary Material

Please find the following supplemental material available below.

For Open Access articles published under a Creative Commons License, all supplemental material carries the same license as the article it is associated with.

For non-Open Access articles published, all supplemental material carries a non-exclusive license, and permission requests for re-use of supplemental material or any part of supplemental material shall be sent directly to the copyright owner as specified in the copyright notice associated with the article.

0.00 MB

0.61 MB

0.02 MB

Homozygous Mutations in GDAP1 and MFN2 Genes Resulted in Autosomal Recessive Forms of Charcot–Marie–Tooth Disease in Consanguineous Pakistani Families

Abstract

Get full access to this article

References

Supplementary Material