SPG9A with the new occurrence of an ALDH18A1 mutation in a CMT1A family with PMP22 duplication: case report

SPG9A with the new occurrence of an ALDH18A1 mutation in a CMT1A family with PMP22 duplication: case report

Abstract Background ALDH18A1 mutations lead to delta-1-pyrroline-5-carboxylate-synthetase (P5CS) deficiency, which is a urea cycle-related disorder including SPG9A, SPG9B, autosomal dominant cutis laxa-3 (ADCL3), and autosomal recessive cutis laxa type 3A (ARCL3A). These diseases exhibit a broad cli...

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Main Authors: Kishin Koh, Ryusuke Takaki, Hiroyuki Ishiura, Shoji Tsuji, Yoshihisa Takiyama
Format: Article
Language:English
Published: BMC 2021-02-01
Series:BMC Neurology
Subjects:
SPG9A
ALDH18A1
de novo mutation
Gonadal mosaicism
Charcot-Marie-tooth disease
PMP22
Online Access:https://doi.org/10.1186/s12883-021-02087-x
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spelling doaj-3a0726ebaba047179a558007b48386e62021-02-14T12:23:48ZengBMCBMC Neurology1471-23772021-02-012111510.1186/s12883-021-02087-xSPG9A with the new occurrence of an ALDH18A1 mutation in a CMT1A family with PMP22 duplication: case reportKishin Koh0Ryusuke Takaki1Hiroyuki Ishiura2Shoji Tsuji3Yoshihisa Takiyama4Department of Neurology, Graduate School of Medical Sciences, University of YamanashiDepartment of Neurology, Graduate School of Medical Sciences, University of YamanashiDepartment of Neurology, Graduate School of Medicine, The University of TokyoDepartment of Molecular Neurology, University of Tokyo, Graduate School of MedicineDepartment of Neurology, Graduate School of Medical Sciences, University of YamanashiAbstract Background ALDH18A1 mutations lead to delta-1-pyrroline-5-carboxylate-synthetase (P5CS) deficiency, which is a urea cycle-related disorder including SPG9A, SPG9B, autosomal dominant cutis laxa-3 (ADCL3), and autosomal recessive cutis laxa type 3A (ARCL3A). These diseases exhibit a broad clinical spectrum, which makes the diagnosis of P5CS deficiency difficult. We report here a rare Japanese family including both patients with an ALDH18A1 mutation (SPG9A) and ones with CMT1A. Case presentation A Japanese family included five patients with the CMT phenotype and five with the HSP phenotype in four generations. The patients with the HSP phenotype showed a pure or complicated form, and intrafamilial clinical variability was noted. Genetically, FISH analysis revealed that two CMT patients had a PMP22 duplication (CMT1A). Exome analysis and Sanger sequencing revealed five HSP patients had an ALDH18A1 heterozygous mutation of c.755G > A, which led to SPG9A. Haplotype analysis revealed that the ALDH18A1 mutation must have newly occurred. To date, although de novo mutations of ALDH18A1 have been described in ADCL3A, they were not mentioned in SPG9A in earlier reports. Thus, this is the first SPG9A family with a de novo mutation or the new occurrence of gonadal mosaicism of ALDH18A1. Analysis of serum amino acid levels revealed that two SPG9A patients and two unaffected family members had low citrulline levels and one had a low level of ornithine. Conclusions Since the newly occurring ALDH18A1 mutation, c.755G > A, is the same as that in two ADHSP families and one sporadic patient with SPG9A reported previously, this genomic site might easily undergo mutation. The patients with the c.755G > A mutation in our family showed clinical variability of symptoms like in the earlier reported two families and one sporadic patient with this mutation. Further studies are required to clarify the relationship between the amino acid levels and clinical manifestations, which will reveal how P5CS deficiency influences disease phenotypes including ARCL3A, ADCL3, SPG9B, and SPG9A.https://doi.org/10.1186/s12883-021-02087-xSPG9AALDH18A1de novo mutationGonadal mosaicismCharcot-Marie-tooth diseasePMP22
collection DOAJ
language English
format Article
sources DOAJ
author Kishin Koh
Ryusuke Takaki
Hiroyuki Ishiura
Shoji Tsuji
Yoshihisa Takiyama
spellingShingle Kishin Koh
Ryusuke Takaki
Hiroyuki Ishiura
Shoji Tsuji
Yoshihisa Takiyama
SPG9A with the new occurrence of an ALDH18A1 mutation in a CMT1A family with PMP22 duplication: case report
BMC Neurology
SPG9A
ALDH18A1
de novo mutation
Gonadal mosaicism
Charcot-Marie-tooth disease
PMP22
author_facet Kishin Koh
Ryusuke Takaki
Hiroyuki Ishiura
Shoji Tsuji
Yoshihisa Takiyama
author_sort Kishin Koh
title SPG9A with the new occurrence of an ALDH18A1 mutation in a CMT1A family with PMP22 duplication: case report
title_short SPG9A with the new occurrence of an ALDH18A1 mutation in a CMT1A family with PMP22 duplication: case report
title_full SPG9A with the new occurrence of an ALDH18A1 mutation in a CMT1A family with PMP22 duplication: case report
title_fullStr SPG9A with the new occurrence of an ALDH18A1 mutation in a CMT1A family with PMP22 duplication: case report
title_full_unstemmed SPG9A with the new occurrence of an ALDH18A1 mutation in a CMT1A family with PMP22 duplication: case report
title_sort spg9a with the new occurrence of an aldh18a1 mutation in a cmt1a family with pmp22 duplication: case report
publisher BMC
series BMC Neurology
issn 1471-2377
publishDate 2021-02-01
description Abstract Background ALDH18A1 mutations lead to delta-1-pyrroline-5-carboxylate-synthetase (P5CS) deficiency, which is a urea cycle-related disorder including SPG9A, SPG9B, autosomal dominant cutis laxa-3 (ADCL3), and autosomal recessive cutis laxa type 3A (ARCL3A). These diseases exhibit a broad clinical spectrum, which makes the diagnosis of P5CS deficiency difficult. We report here a rare Japanese family including both patients with an ALDH18A1 mutation (SPG9A) and ones with CMT1A. Case presentation A Japanese family included five patients with the CMT phenotype and five with the HSP phenotype in four generations. The patients with the HSP phenotype showed a pure or complicated form, and intrafamilial clinical variability was noted. Genetically, FISH analysis revealed that two CMT patients had a PMP22 duplication (CMT1A). Exome analysis and Sanger sequencing revealed five HSP patients had an ALDH18A1 heterozygous mutation of c.755G > A, which led to SPG9A. Haplotype analysis revealed that the ALDH18A1 mutation must have newly occurred. To date, although de novo mutations of ALDH18A1 have been described in ADCL3A, they were not mentioned in SPG9A in earlier reports. Thus, this is the first SPG9A family with a de novo mutation or the new occurrence of gonadal mosaicism of ALDH18A1. Analysis of serum amino acid levels revealed that two SPG9A patients and two unaffected family members had low citrulline levels and one had a low level of ornithine. Conclusions Since the newly occurring ALDH18A1 mutation, c.755G > A, is the same as that in two ADHSP families and one sporadic patient with SPG9A reported previously, this genomic site might easily undergo mutation. The patients with the c.755G > A mutation in our family showed clinical variability of symptoms like in the earlier reported two families and one sporadic patient with this mutation. Further studies are required to clarify the relationship between the amino acid levels and clinical manifestations, which will reveal how P5CS deficiency influences disease phenotypes including ARCL3A, ADCL3, SPG9B, and SPG9A.
topic SPG9A
ALDH18A1
de novo mutation
Gonadal mosaicism
Charcot-Marie-tooth disease
PMP22
url https://doi.org/10.1186/s12883-021-02087-x
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