The clinical spectrum of the congenital myasthenic syndrome resulting from COL13A1 mutations.
Adolescent
Adult
Child
Collagen Type XIII
/ genetics
Female
Homozygote
Humans
Male
Muscle Proteins
/ genetics
Muscle, Skeletal
/ pathology
Mutation
/ genetics
Myasthenic Syndromes, Congenital
/ diagnosis
Neuromuscular Junction
/ genetics
Synapses
/ genetics
Synaptic Transmission
/ genetics
Young Adult
3,4-diaminopyridine
COL13A1
congenital myasthenic syndromes
salbutamol
synaptic basal lamina
Journal
Brain : a journal of neurology
ISSN: 1460-2156
Titre abrégé: Brain
Pays: England
ID NLM: 0372537
Informations de publication
Date de publication:
01 06 2019
01 06 2019
Historique:
received:
17
12
2018
revised:
08
02
2019
accepted:
22
02
2019
pubmed:
14
5
2019
medline:
13
3
2020
entrez:
14
5
2019
Statut:
ppublish
Résumé
Next generation sequencing techniques were recently used to show mutations in COL13A1 cause synaptic basal lamina-associated congenital myasthenic syndrome type 19. Animal studies showed COL13A1, a synaptic extracellular-matrix protein, is involved in the formation and maintenance of the neuromuscular synapse that appears independent of the Agrin-LRP4-MuSK-DOK7 acetylcholine receptor clustering pathway. Here, we report the phenotypic spectrum of 16 patients from 11 kinships harbouring homozygous or heteroallelic mutations in COL13A1. Clinical presentation was mostly at birth with hypotonia and breathing and feeding difficulties often requiring ventilation and artificial feeding. Respiratory crisis related to recurrent apnoeas, sometimes triggered by chest infections, were common early in life but resolved over time. The predominant pattern of muscle weakness included bilateral ptosis (non-fatigable in adulthood), myopathic facies and marked axial weakness, especially of neck flexion, while limb muscles were less involved. Other features included facial dysmorphism, skeletal abnormalities and mild learning difficulties. All patients tested had results consistent with abnormal neuromuscular transmission. Muscle biopsies were within normal limits or showed non-specific changes. Muscle MRI and serum creatine kinase levels were normal. In keeping with COL13A1 mutations affecting both synaptic structure and presynaptic function, treatment with 3,4-diaminopyridine and salbutamol resulted in motor and respiratory function improvement. In non-treated cases, disease severity and muscle strength improved gradually over time and several adults recovered normal muscle strength in the limbs. In summary, patients with COL13A1 mutations present mostly with severe early-onset myasthenic syndrome with feeding and breathing difficulties. Axial weakness is greater than limb weakness. Disease course improves gradually over time, which could be consistent with the less prominent role of COL13A1 once the neuromuscular junction is mature. This report emphasizes the role of collagens at the human muscle endplate and should facilitate the recognition of this disorder, which can benefit from pharmacological treatment.
Identifiants
pubmed: 31081514
pii: 5488581
doi: 10.1093/brain/awz107
pmc: PMC6752227
doi:
Substances chimiques
COL13A1 protein, human
0
Collagen Type XIII
0
Muscle Proteins
0
Types de publication
Journal Article
Research Support, Non-U.S. Gov't
Langues
eng
Sous-ensembles de citation
IM
Pagination
1547-1560Subventions
Organisme : Wellcome Trust
Pays : United Kingdom
Organisme : Medical Research Council
ID : MR/M006824/1
Pays : United Kingdom
Organisme : NHGRI NIH HHS
ID : UM1 HG008900
Pays : United States
Informations de copyright
© The Author(s) (2019). Published by Oxford University Press on behalf of the Guarantors of Brain. All rights reserved. For Permissions, please email: journals.permissions@oup.com.
Références
Am J Hum Genet. 1999 Jun;64(6):1570-9
pubmed: 10330344
J Biol Chem. 2000 Mar 17;275(11):8255-61
pubmed: 10713152
Neuron. 2001 Jul 19;31(1):15-22
pubmed: 11498047
J Biol Chem. 2002 Jun 21;277(25):23092-9
pubmed: 11956183
J Neurocytol. 2003 Jun-Sep;32(5-8):883-903
pubmed: 15034274
Rev Neurol. 2005 Aug 16-31;41(4):218-22
pubmed: 16075400
J Biol Chem. 1990 Oct 5;265(28):16922-8
pubmed: 1698771
Brain. 2007 Jun;130(Pt 6):1497-506
pubmed: 17439981
Neurology. 2008 Sep 2;71(10):776-7
pubmed: 18765655
J Med Genet. 2009 Mar;46(3):203-8
pubmed: 19251977
Nucleic Acids Res. 2009 May;37(9):e67
pubmed: 19339519
Nat Methods. 2010 Apr;7(4):248-9
pubmed: 20354512
Nat Methods. 2010 Aug;7(8):575-6
pubmed: 20676075
J Neurosci. 2010 Sep 15;30(37):12230-41
pubmed: 20844119
Neuromuscul Disord. 2011 Jun;21(6):420-7
pubmed: 21514828
Trends Neurosci. 2012 Jul;35(7):441-53
pubmed: 22633140
Nucleic Acids Res. 2012 Jul;40(Web Server issue):W452-7
pubmed: 22689647
Am J Hum Genet. 2012 Jul 13;91(1):193-201
pubmed: 22742743
Nat Methods. 2012 Jun 28;9(7):676-82
pubmed: 22743772
Brain. 2013 Mar;136(Pt 3):944-56
pubmed: 23404334
Hum Mol Genet. 2013 Jul 15;22(14):2905-13
pubmed: 23569079
Science. 2015 Jan 23;347(6220):1260419
pubmed: 25613900
Nat Genet. 2015 Jul;47(7):717-726
pubmed: 25985138
Nucleic Acids Res. 2016 Jan 4;44(D1):D746-52
pubmed: 26481351
Am J Hum Genet. 2015 Dec 3;97(6):878-85
pubmed: 26626625
Nature. 2016 Aug 17;536(7616):285-91
pubmed: 27535533
Hum Mol Genet. 2017 Jun 1;26(11):2076-2090
pubmed: 28369367
Am J Med Genet A. 2017 Aug;173(8):2240-2245
pubmed: 28544784
Nucleic Acids Res. 2018 Jan 4;46(D1):D754-D761
pubmed: 29155950
Hum Mol Genet. 2018 May 1;27(9):1556-1564
pubmed: 29462491
J Neurosci. 2018 Apr 25;38(17):4243-4258
pubmed: 29626165
J Neuromuscul Dis. 2018;5(2):231-240
pubmed: 29865088
Int J Mol Sci. 2018 Jun 05;19(6):null
pubmed: 29874875
J Pediatr. 1973 Jul;83(1):37-40
pubmed: 4149045
J Biol Chem. 1998 Jun 19;273(25):15590-7
pubmed: 9624150
Proc Natl Acad Sci U S A. 1998 Aug 4;95(16):9654-9
pubmed: 9689136