Three novel mutations in 20 patients with hereditary spastic paraparesis.

Tytuł:: Three novel mutations in 20 patients with hereditary spastic paraparesis.
Autorzy:: Duz MB; Department of Medical Genetics, Cerrahpaşa Medical School, Istanbul University-Cerrahpaşa, 34098, Fatih, Istanbul, Turkey.
Dasdemir S; Department of Medical Genetics, Cerrahpaşa Medical School, Istanbul University-Cerrahpaşa, 34098, Fatih, Istanbul, Turkey.
Kalayci Yigin A; Department of Medical Genetics, Cerrahpaşa Medical School, Istanbul University-Cerrahpaşa, 34098, Fatih, Istanbul, Turkey.
Akalin MA; Department of Neurology, Cerrahpaşa Medical School, Istanbul University-Cerrahpaşa, 34098, Fatih, Istanbul, Turkey.
Seven M; Department of Medical Genetics, Cerrahpaşa Medical School, Istanbul University-Cerrahpaşa, 34098, Fatih, Istanbul, Turkey. .
Źródło:: Neurological sciences : official journal of the Italian Neurological Society and of the Italian Society of Clinical Neurophysiology [Neurol Sci] 2018 Sep; Vol. 39 (9), pp. 1551-1557. Date of Electronic Publication: 2018 Jun 16.
Typ publikacji:: Journal Article
Język:: English
Imprint Name(s):: Original Publication: Milano, Italy : Springer-Verlag Italia, c2000-
MeSH Terms:: Genetic Predisposition to Disease*
Mutation*
GTP-Binding Proteins/*genetics
Membrane Proteins/*genetics
Paraparesis, Spastic/*genetics
Spastin/*genetics
Adolescent ; Adult ; Aged ; Child ; Cohort Studies ; Family ; Female ; Genes, Dominant ; Genetic Association Studies ; Humans ; Male ; Membrane Transport Proteins/genetics ; Middle Aged ; Phenotype ; Proteins/genetics ; Turkey ; Exome Sequencing
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Grant Information:: 22323 Bilimsel Araştirma Projeleri Birimi, Istanbul Üniversitesi
Contributed Indexing:: Keywords: Genetic heterogeneity; Hereditary spastic paraparesis; Novel mutation; Whole-exome sequencing
Substance Nomenclature:: 0 (Membrane Proteins)
0 (Membrane Transport Proteins)
0 (Proteins)
0 (REEP1 protein, human)
0 (WASHC5 protein, human)
EC 3.6.1.- (ATL1 protein, human)
EC 3.6.1.- (GTP-Binding Proteins)
EC 3.6.4.3 (Spastin)
EC 5.6.1.1 (SPAST protein, human)
Entry Date(s):: Date Created: 20180617 Date Completed: 20190403 Latest Revision: 20221207
Update Code:: 20240105
DOI:: 10.1007/s10072-018-3454-7
PMID:: 29907907
: Czasopismo naukowe

Pełny tekst

Hereditary spastic paraparesis (HSP) constitutes both genetic and clinically heterogeneous group of upper motor neuron diseases. Half of the individuals with autosomal dominant (AD) HSP have mutations in SPAST, ATL1, and REEP1 genes. This study was conducted to elucidate the genetic etiology of patients with the pure type AD-HSP diagnosis. The patient group consisted of 23 individuals from 6 families in Turkey. In the first step of work, Sanger sequencing (SS) was performed in ATL1, SPAST, and REEP1 genes and the second phase whole-exome sequencing (WES) was performed following SS analysis for the patients with no detected mutations in these genes. The results of this study revealed that in ATL1, 6 patients have previously reported c.776C > A mutation and 6 patients have novel c.470 T > C mutation. In SPAST, 3 patients have novel c.1072G > C mutation and 2 patients have novel c.1099-1G > C mutation. WES was performed in three patients, who had no detected mutation in these genes with SS analysis. In this approach, as previously reported c.1859 T > C mutation in KIAA0196 was detected, and it was confirmed with the patient's relatives by SS. In three of patients, no HSP-associated variant could be identified in SS and WES. With this study, the molecular genetic etiology in 20 of 23 (87%) individuals that were included in this study with the utilization of SS and WES was elucidated. Utilization of SS and WES methods have enabled the identification of genetic etiology of HSP further with appropriate genetic counseling that was provided to the patients.

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