A genomic approach to mutation analysis of holocarboxylase synthetase gene in three Chinese patients with late-onset holocarboxylase synthetase deficiency

Nelson L.S. Tang; Joannie Hui; Collin K.K. Yong; Lawrence T.K. Wong; Derek A. Applegarth; Hilary D. Vallance; L. K. Law; Simon L.M. Fung; Tony W.L. Mak; Y. M. Sung; K. L. Cheung; T. F. Fok

doi:10.1016/S0009-9120(02)00432-0

A genomic approach to mutation analysis of holocarboxylase synthetase gene in three Chinese patients with late-onset holocarboxylase synthetase deficiency

Nelson L.S. Tang
, Joannie Hui
, Collin K.K. Yong
, Lawrence T.K. Wong
, Derek A. Applegarth
, Hilary D. Vallance
, L. K. Law
, Simon L.M. Fung
, Tony W.L. Mak
, Y. M. Sung
, K. L. Cheung
, T. F. Fok

Research output: Contribution to journal › Article › peer-review

18 Citations (Scopus)

Abstract

Objective: Multiple carboxylase deficiency (MCD, MIM:253270) is a common organic aciduria and caused by deficiency of either biotinidase or holocarboxylase synthetase (HLCS; EC 6.3.4.10). Patients commonly present during early infancy with acute metabolic derangements and severe metabolic acidosis. Recently, a late onset form of HLCS deficiency was also described. The different phenotypes (early and late presenting) may be related to a spectrum of mutations in HLCS gene. Applications of mutation analysis in HLCS had been limited previously by the requirement of cDNA from living tissue for study. We described here a genomic approach for molecular diagnosis of HLCS deficiency which we have used to detect mutations in Chinese patients who had the late-onset form of HLCS deficiency. In addition, a fibroblast cell line with MCD from Coriell Cell repositories was also studied. Design and methods: Three Chinese patients with late onset HLCS deficiency were studied. The genomic sequence of HLCS was retrieved and newly designed primers were used to cover all coding sequences of the gene. PCR products were analyzed by direct sequencing. Population allelic frequencies of mutations detected were determined by genotyping of control samples by restriction fragment length polymorphism. Results: We found a recurrent mutation, R508W, in the three unrelated Chinese patients. Two were homozygous for this mutation. The other patient was a compound heterozygote of R508W and a novel mutation, D634N. The results suggest that R508W may be an important and relatively prevalent disease-causing mutation in Chinese MCD patients. A fibroblast cell-line from an African patient revealed an additional novel mutation, R565X and a known mutation, V550M. Conclusion: R508W is a recurrent mutation in Chinese MCD patients which is associated with the late onset phenotype. This new genomic approach for mutation analysis of HLCS gene provides new opportunities in studies of MCD.

Original language	English
Pages (from-to)	145-149
Number of pages	5
Journal	Clinical Biochemistry
Volume	36
Issue number	2
DOIs	https://doi.org/10.1016/S0009-9120(02)00432-0
Publication status	Published - Mar 2003
Externally published	Yes

Keywords

Holocarboxylase synthetase deficiency
Inherited metabolic diseases
Multiple carboxylase deficiency
Organic aciduria

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10.1016/S0009-9120(02)00432-0

Cite this

Tang, N. L. S., Hui, J., Yong, C. K. K., Wong, L. T. K., Applegarth, D. A., Vallance, H. D., Law, L. K., Fung, S. L. M., Mak, T. W. L., Sung, Y. M., Cheung, K. L., & Fok, T. F. (2003). A genomic approach to mutation analysis of holocarboxylase synthetase gene in three Chinese patients with late-onset holocarboxylase synthetase deficiency. Clinical Biochemistry, 36(2), 145-149. https://doi.org/10.1016/S0009-9120(02)00432-0

@article{520e6f92027947aab2a4c8ce42714ae7,

title = "A genomic approach to mutation analysis of holocarboxylase synthetase gene in three Chinese patients with late-onset holocarboxylase synthetase deficiency",

abstract = "Objective: Multiple carboxylase deficiency (MCD, MIM:253270) is a common organic aciduria and caused by deficiency of either biotinidase or holocarboxylase synthetase (HLCS; EC 6.3.4.10). Patients commonly present during early infancy with acute metabolic derangements and severe metabolic acidosis. Recently, a late onset form of HLCS deficiency was also described. The different phenotypes (early and late presenting) may be related to a spectrum of mutations in HLCS gene. Applications of mutation analysis in HLCS had been limited previously by the requirement of cDNA from living tissue for study. We described here a genomic approach for molecular diagnosis of HLCS deficiency which we have used to detect mutations in Chinese patients who had the late-onset form of HLCS deficiency. In addition, a fibroblast cell line with MCD from Coriell Cell repositories was also studied. Design and methods: Three Chinese patients with late onset HLCS deficiency were studied. The genomic sequence of HLCS was retrieved and newly designed primers were used to cover all coding sequences of the gene. PCR products were analyzed by direct sequencing. Population allelic frequencies of mutations detected were determined by genotyping of control samples by restriction fragment length polymorphism. Results: We found a recurrent mutation, R508W, in the three unrelated Chinese patients. Two were homozygous for this mutation. The other patient was a compound heterozygote of R508W and a novel mutation, D634N. The results suggest that R508W may be an important and relatively prevalent disease-causing mutation in Chinese MCD patients. A fibroblast cell-line from an African patient revealed an additional novel mutation, R565X and a known mutation, V550M. Conclusion: R508W is a recurrent mutation in Chinese MCD patients which is associated with the late onset phenotype. This new genomic approach for mutation analysis of HLCS gene provides new opportunities in studies of MCD.",

keywords = "Holocarboxylase synthetase deficiency, Inherited metabolic diseases, Multiple carboxylase deficiency, Organic aciduria",

author = "Tang, \{Nelson L.S.\} and Joannie Hui and Yong, \{Collin K.K.\} and Wong, \{Lawrence T.K.\} and Applegarth, \{Derek A.\} and Vallance, \{Hilary D.\} and Law, \{L. K.\} and Fung, \{Simon L.M.\} and Mak, \{Tony W.L.\} and Sung, \{Y. M.\} and Cheung, \{K. L.\} and Fok, \{T. F.\}",

year = "2003",

month = mar,

doi = "10.1016/S0009-9120(02)00432-0",

language = "English",

volume = "36",

pages = "145--149",

number = "2",

}

Tang, NLS, Hui, J, Yong, CKK, Wong, LTK, Applegarth, DA, Vallance, HD, Law, LK, Fung, SLM, Mak, TWL, Sung, YM, Cheung, KL & Fok, TF 2003, 'A genomic approach to mutation analysis of holocarboxylase synthetase gene in three Chinese patients with late-onset holocarboxylase synthetase deficiency', Clinical Biochemistry, vol. 36, no. 2, pp. 145-149. https://doi.org/10.1016/S0009-9120(02)00432-0

TY - JOUR

T1 - A genomic approach to mutation analysis of holocarboxylase synthetase gene in three Chinese patients with late-onset holocarboxylase synthetase deficiency

AU - Tang, Nelson L.S.

AU - Hui, Joannie

AU - Yong, Collin K.K.

AU - Wong, Lawrence T.K.

AU - Applegarth, Derek A.

AU - Vallance, Hilary D.

AU - Law, L. K.

AU - Fung, Simon L.M.

AU - Mak, Tony W.L.

AU - Sung, Y. M.

AU - Cheung, K. L.

AU - Fok, T. F.

PY - 2003/3

Y1 - 2003/3

N2 - Objective: Multiple carboxylase deficiency (MCD, MIM:253270) is a common organic aciduria and caused by deficiency of either biotinidase or holocarboxylase synthetase (HLCS; EC 6.3.4.10). Patients commonly present during early infancy with acute metabolic derangements and severe metabolic acidosis. Recently, a late onset form of HLCS deficiency was also described. The different phenotypes (early and late presenting) may be related to a spectrum of mutations in HLCS gene. Applications of mutation analysis in HLCS had been limited previously by the requirement of cDNA from living tissue for study. We described here a genomic approach for molecular diagnosis of HLCS deficiency which we have used to detect mutations in Chinese patients who had the late-onset form of HLCS deficiency. In addition, a fibroblast cell line with MCD from Coriell Cell repositories was also studied. Design and methods: Three Chinese patients with late onset HLCS deficiency were studied. The genomic sequence of HLCS was retrieved and newly designed primers were used to cover all coding sequences of the gene. PCR products were analyzed by direct sequencing. Population allelic frequencies of mutations detected were determined by genotyping of control samples by restriction fragment length polymorphism. Results: We found a recurrent mutation, R508W, in the three unrelated Chinese patients. Two were homozygous for this mutation. The other patient was a compound heterozygote of R508W and a novel mutation, D634N. The results suggest that R508W may be an important and relatively prevalent disease-causing mutation in Chinese MCD patients. A fibroblast cell-line from an African patient revealed an additional novel mutation, R565X and a known mutation, V550M. Conclusion: R508W is a recurrent mutation in Chinese MCD patients which is associated with the late onset phenotype. This new genomic approach for mutation analysis of HLCS gene provides new opportunities in studies of MCD.

AB - Objective: Multiple carboxylase deficiency (MCD, MIM:253270) is a common organic aciduria and caused by deficiency of either biotinidase or holocarboxylase synthetase (HLCS; EC 6.3.4.10). Patients commonly present during early infancy with acute metabolic derangements and severe metabolic acidosis. Recently, a late onset form of HLCS deficiency was also described. The different phenotypes (early and late presenting) may be related to a spectrum of mutations in HLCS gene. Applications of mutation analysis in HLCS had been limited previously by the requirement of cDNA from living tissue for study. We described here a genomic approach for molecular diagnosis of HLCS deficiency which we have used to detect mutations in Chinese patients who had the late-onset form of HLCS deficiency. In addition, a fibroblast cell line with MCD from Coriell Cell repositories was also studied. Design and methods: Three Chinese patients with late onset HLCS deficiency were studied. The genomic sequence of HLCS was retrieved and newly designed primers were used to cover all coding sequences of the gene. PCR products were analyzed by direct sequencing. Population allelic frequencies of mutations detected were determined by genotyping of control samples by restriction fragment length polymorphism. Results: We found a recurrent mutation, R508W, in the three unrelated Chinese patients. Two were homozygous for this mutation. The other patient was a compound heterozygote of R508W and a novel mutation, D634N. The results suggest that R508W may be an important and relatively prevalent disease-causing mutation in Chinese MCD patients. A fibroblast cell-line from an African patient revealed an additional novel mutation, R565X and a known mutation, V550M. Conclusion: R508W is a recurrent mutation in Chinese MCD patients which is associated with the late onset phenotype. This new genomic approach for mutation analysis of HLCS gene provides new opportunities in studies of MCD.

KW - Holocarboxylase synthetase deficiency

KW - Inherited metabolic diseases

KW - Multiple carboxylase deficiency

KW - Organic aciduria

UR - https://www.scopus.com/pages/publications/0037337776

U2 - 10.1016/S0009-9120(02)00432-0

DO - 10.1016/S0009-9120(02)00432-0

M3 - Article

C2 - 12633764

AN - SCOPUS:0037337776

SN - 0009-9120

VL - 36

SP - 145

EP - 149

JO - Clinical Biochemistry

JF - Clinical Biochemistry

IS - 2

ER -

A genomic approach to mutation analysis of holocarboxylase synthetase gene in three Chinese patients with late-onset holocarboxylase synthetase deficiency

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Keywords

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