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Journal of Inherited Metabolic Disease

Erschienen in:

01.03.2013 | Original Article

Molecular characterization of 355 mucopolysaccharidosis patients reveals 104 novel mutations

verfasst von: Laura M. Pollard, Julie R. Jones, Tim C. Wood

Erschienen in: Journal of Inherited Metabolic Disease | Ausgabe 2/2013

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Abstract

Mucopolysaccharidosis (MPS) disorders are heterogeneous and caused by deficient lysosomal degradation of glycosaminoglycans, resulting in distinct but sometimes overlapping phenotypes. Molecular analysis was performed for a total of 355 MPS patients with MPSI (n = 15), MPSII (n = 218), MPSIIIA (n = 86), MPSIIIB (n = 20), MPSIVA (n = 6) or MPSVI (n = 10). This analysis revealed 104 previously unreported mutations: seven in IDUA (MPSI), 61 in IDS (MPSII), 19 in SGSH (MPSIIIA), 11 in NAGLU (MPSIIIB), two in GALNS (MPSIVA) and four in ARSB (MPSVI). The intergenic comparison of the mutation data for these disorders has revealed interesting differences. Whereas IDUA, IDS, NAGLU and ARSB demonstrate similar levels of mutation heterogeneity (0.6–0.675 different mutations per total alleles), SGSH and GALNS have lower levels of mutation heterogeneity (0.282 and 0.455, respectively), due to more recurrent mutations. The type of mutation also varies significantly by gene. SGSH, GALNS and ARSB mutations are usually missense (76.5 %, 81.8 % and 85 %), while IDUA has many more nonsense mutations (56 %) than the other genes (≤20%). The mutation spectrum is most diverse for IDS, including intergenic inversions and multi-exon deletions. By testing 102 mothers of MPSII patients, we determined that 22.5 % of IDS mutations are de novo. We report the allele frequency of common mutations for each gene in our patient cohort and the exonic distribution of coding sequence alterations in the IDS, SGSH and NAGLU genes, which reveals several potential “hot-spots”. This further molecular characterization of these MPS disorders is expected to assist in the diagnosis and counseling of future patients.

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Adzhubei IA, Schmidt S, Peshkin L et al (2012) A method and server for predicting damaging missense mutations. Nat Methods 7(4):248–249CrossRef

Andria G, Di Natale P, Del Guidice E, Strisciuglio P, Murino P (1979) Sanfilippo B syndrome (MPS IIIB): attenuated and severe forms within same sibship. Clin Genet 15:500–504PubMedCrossRef

Auray-Blais C, Bherer P, Gagnon R et al (2011) Efficient analysis of urinary glycosaminoglycans by LC-MS/MS in mucopolysaccharidoses type I, II and VI. Mol Genet Metab 102:49–56PubMedCrossRef

Baum H, Dodgson KS, Spencer B (1959) The assay of arylsulfatases A and B in human urine. Clin Chim Acta 4(3):453–455PubMedCrossRef

Beesley CE, Meaney CA, Greenland G, Adams V, Vellodi A, Young EP, Winchester BG (2001) Mutational analysis of 85 mucopolysaccharidosis type I families: frequency of known mutations, identification of 17 novel mutations and in vitro expression of missense mutations. Hum Genet 109(5):503–511PubMedCrossRef

Blanchard S, Sadilek M, Scott CR, Turecek F, Gelb MH (2008) Tandem mass spectrometry for the direct assay of lysosomal enzymes in dried blood spots: application to screening newborns for mucopolysaccharidosis I. Clin Chem 54(12):2067–2070PubMedCrossRef

Bondeson ML, Dahl N, Malmgren H, Kleijer WJ, Tönnesen T, Carlberg BM, Pettersson U (1995) Inversion of the IDS gene resulting from recombination with IDS-related sequences is a common cause of the Hunter syndrome. Hum Mol Genet 4(4):615–621PubMedCrossRef

Camelier MV, Burin MG, De Mari J, Vieira TA, Marasca G, Giugliani R (2011) Practical and reliable enzyme test for the detection of mucopolysaccharidosis IVA (Morquio syndrome type A) in dried blood samples. Clin Chim Acta 412(19–20):1805–1808PubMedCrossRef

de Jong JGN, Wevers RA, Laarakkers C, Poorthuis BJHM (1989) Dimethylmethylene Blue-based spectrophotometry of glycosaminoglycans in untreated urine: a rapid screening procedure for mucopolysaccharidoses. Clin Chem 35(7):1472–1477PubMed

Dembure PP, Roesel RA (1991) Screening for mucopolysaccharidoses by analysis of urinary glycosaminoglycans. In: Hommes FA (ed) Techniques in diagnostic human biochemical genetics: a laboratory manual. Wiley-Liss, New York, pp 77–86

Duffey TA, Sadilek M, Scott CR, Turecek F, Gelb MH (2010) Tandem mass spectrometry for the direct assay of lysosomal enzymes in dried blood spots: application to screening newborns for mucopolysaccharidosis VI (Maroteaux-Lamy syndrome). Anal Chem 82(22):9587–9591PubMedCrossRef

Froissart R, Maire I, Bonnet V, Levade T, Bozon D (1997) Germline and somatic mosaicism in a female carrier of Hunter disease. J Med Genet 34(2):137–140PubMedCrossRef

Froissart R, Da Silva IM, Maire I (2007) Mucopolysaccharidosis type II: an update on mutation spectrum. Acta Paediatr Suppl 96(455):71–77PubMedCrossRef

Gottwald I, Hughes J, Stewart F, Tylee K, Church H, Jones SA (2011) Attenuated mucopolysaccharidosis type VI (Maroteaux-Lamy syndrome) due to homozygosity for the p.Y201C mutation in the ARSB gene. Mol Genet Metab 103(3):300–302PubMedCrossRef

Hopwood JJ, Harrison JR (1982) High-resolution electrophoresis of urinary glycosaminoglycans: an improved screening test for the mucopolysaccharidoses. Anal Biochem 119:120–127PubMedCrossRef

Imundo L, Leduc CA, Guha S et al (2011) A complete deficiency of hyaluronoglucosaminidase 1 (HYAL1) presenting as familial juvenile idiopathic arthritis. J Inherit Metab Dis 34(5):1013–1022PubMedCrossRef

Karageorgos L, Brooks DA, Pollard A et al (2007) Mutational analysis of 105 mucopolysaccharidosis type VI patients. Hum Mutat 28(9):897–903PubMedCrossRef

Karpova EA, YaV V, Keulemans JL et al (1996) A fluorimetric enzyme assay for the diagnosis of Sanfilippo disease type A (MPS IIIA). J Inherit Metab Dis 19(3):278–285PubMedCrossRef

Kowalewski B, Lamanna WC, Lawrence R et al (2012) Arylsulfatase G inactivation causes loss of heparan sulfate 3-O-sulfatase activity and mucopolysaccharidosis in mice. Proc Natl Acad Sci USA 109(26):10310–10315PubMedCrossRef

Kumar P, Henikoff S, Ng PC (2009) Predicting the effects of coding non-synonymous variants on protein function using the SIFT algorithm. Nat Protocols 4(8):1073–1082CrossRef

Matte U, Yogalingam G, Brooks D et al (2003) Identification and characterization of 13 new mutations in mucopolysaccharidosis type I patients. Mol Genet Metabol 78(1):37–43CrossRef

Meyer A, Kossow K, Gal A et al (2008) The mutation p.Ser298Pro in the sulphamidase gene (SGSH) is associated with a slowly progressive clinical phenotype in mucopolysaccharidosis type IIIA (Sanfilippo A syndrome). Hum Mutat. Mutation in Brief #1004

Montaño AM, Sukegawa K, Kato Z et al (2007) Effect of ‘attenuated’ mutations in mucopolysaccharidoss IVA on molecular phenotypes of N-acetylgalactosamine-6-sulfate sulfatase. J Inherit Metab Dis 30:758–767PubMedCrossRef

Neufeld EF, Muenzer J (1995) The mucopolysaccharidoses. In: Beaudet AL, Sly WS, Scriver C (eds) The metabolic basis of inherited disease. McGraw Hill, New York, pp 2465–2493

Nielsen TC, Rozek T, Hopwood JJ, Fuller M (2010) Determination of urinary oligosaccharides by high-performance liquid chromatography/electrospray ionization-tandem mass spectrometry: application to hunter syndrome. Anal Biochem 402(2):113–120PubMedCrossRef

Schmidtchen A, Greenberg D, Zhao HG et al (1998) NAGLU mutations underlying Sanfilippo syndrome type B. Am J Hum Genet 62:64–69PubMedCrossRef

Schouten JP, McElgunn CJ, Waaijer R, Zwijnenburg D, Diepvens F, Pals G (2002) Relative quantification of 40 nucleic acid sequences by multiplex ligation-dependent probe amplification. Nucleic Acids Res 30(12):e57PubMedCrossRef

Sukegawa K, Nakamura H, Kato Z et al (2000) Biochemical and structural analysis of missense mutations in N-acetylgalactosamine-6-sulfate sulfatase causing mucopolysaccharidosis IVA phenotypes. Hum Mol Genet 9(9):1283–1290PubMedCrossRef

Terlato NJ, Cox GF (2003) Can mucopolysaccharidosis type I disease severity be predicted based on a patient’s genotype? A comprehensive review of the literature. Genet Med 5(4):286–294PubMedCrossRef

Tolun AA, Graham C, Shi Q et al (2012) A novel fluorometric enzyme analysis method for Hunter syndrome using dried blood spots. Mol Genet Metab 105(3):519–521PubMedCrossRef

Tomatsu S, Montaño AM, Nishioka T et al (2005) Mutation and polymorphism spectrum of the GALNS gene in mucopolysaccharidosis IVA (Morquio A). Hum Mutat 26(6):500–512PubMedCrossRef

Tomatsu S, Montaño AM, Oguma T et al (2010) Validation of disaccharide compositions derived from dermatan sulfate and heparan sulfate in mucopolysaccharidoses and mucolipidoses II and III by tandem mass spectrometry. Mol Genet Metab 99(2):124–131PubMedCrossRef

Van Diggelen OP (2004) Laboratory protocol for enzyme analysis for Sanfilippo B disease (MPS IIIB). Written procedure provided with substrate purchased from Moscerdam substrates

Van Diggelen OP, Zhao H, Kleijer WJ et al (1990) A fluorimetric enzyme assay for the diagnosis of Morquio disease type A (MPS IVA). Clin Chim Acta 187(2):131–139PubMedCrossRef

Voznyi YV, Keulemans JL, van Diggelen OP (2001) A fluorometric enzyme assay for the diagnosis of MPS II (Hunter disease). J Inherit Metab Dis 24(6):675–680PubMedCrossRef

Weber B, Guo XH, Wraith JE, Cooper A, Kleijer WJ, Bunge S, Hopwood JJ (1997) Novel mutations in Sanfilippo A syndrome: implications for enzyme function. Hum Mol Genet 6:1573–1579PubMedCrossRef

Wenger DA, Williams C (1991) Screening for lysosomal disorders. In: Hommes FA (ed) Techniques in diagnostic human biochemical genetics: a laboratory manual. Wiley-Liss, New York, pp 587–617

Whitley CB, Ridnour MD, Draper KA, Dutton CM, Neglia JP (1989) Diagnostic test for mucopolysaccharidosis. I. Direct method for quantifying excessive urinary glycosaminoglycan excretion. Clin Chem 35:374–379PubMed

Wilson PJ, Morris CP, Anson DS, Occhiodoro T, Bielicki J, Clements PR, Hopwood JJ (1990) Hunter syndrome: Isolation of an iduronate-2-sulfatase cDNA clone and analysis of patient DNA. Proc Natl Acad Sci 87:8531–8535PubMedCrossRef

Wolfe BJ, Blanchard S, Sadilek M, Scott CR, Turecek F, Gelb MH (2011) Tandem mass spectrometry for the direct assay of lysosomal enzymes in dried blood spots: application to screening newborns for mucopolysaccharidosis II (Hunter syndrome). Anal Chem 83(3):1152–1156PubMedCrossRef

Yogalingam G, Hopwood JJ (2001) Molecular genetics of mucopolysaccharidosis type IIIA and IIIB: diagnostic, clinical and biological implications. Hum Mutat 18:264–281PubMedCrossRef

Titel: Molecular characterization of 355 mucopolysaccharidosis patients reveals 104 novel mutations
verfasst von: Laura M. Pollard
Julie R. Jones
Tim C. Wood
Publikationsdatum: 01.03.2013
Verlag: Springer Netherlands
Erschienen in: Journal of Inherited Metabolic Disease / Ausgabe 2/2013
Print ISSN: 0141-8955
Elektronische ISSN: 1573-2665
DOI: https://doi.org/10.1007/s10545-012-9533-7

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