Late-onset metachromatic leukodystrophy: Genotype strongly influences phenotype

H. Rauschka; B. Colsch; N. Baumann; R. Wevers; M. Schmidbauer; M. Krammer; J. C. Turpin; M. Lefevre; C. Olivier; S. Tardieu; W. Krivit; H. Moser; A. Moser; V. Gieselmann; B. Zalc; T. Cox; U. Reuner; A. Tylki-Szymanska; F. Aboul-Enein; E. LeGuern; H. Bernheimer; J. Berger

doi:10.1212/01.wnl.0000234129.97727.4d

Late-onset metachromatic leukodystrophy: Genotype strongly influences phenotype

H. Rauschka, B. Colsch, N. Baumann, R. Wevers, M. Schmidbauer, M. Krammer, J. C. Turpin, M. Lefevre, C. Olivier, S. Tardieu, W. Krivit, H. Moser, A. Moser, V. Gieselmann, B. Zalc, T. Cox, U. Reuner, A. Tylki-Szymanska, F. Aboul-Enein, E. LeGuernH. Bernheimer, J. Berger

Kennedy Krieger Institute

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

80 Scopus citations

Abstract

BACKGROUND: P426L and I179S are the two most frequent mutations in juvenile and adult metachromatic leukodystrophy (late-onset MLD), which, in contrast to infantile MLD, show marked phenotypic heterogeneity. OBJECTIVE: To search for genotype-phenotype correlations in late-onset MLD. METHODS: The authors reviewed the clinical course of 22 patients homozygous for mutation P426L vs 20 patients heterozygous for mutation I179S, in which the second arylsulfatase A (ASA) mutation had also been determined. RESULTS: P426L homozygotes principally presented with progressive gait disturbance caused by spastic paraparesis or cerebellar ataxia; mental disturbance was absent or insignificant at the onset of disease but became more apparent as the disease evolved. In contrast, compound heterozygotes for I179S presented with schizophrenia-like behavioral abnormalities, social dysfunction, and mental decline, but motor deficits were scarce. Reduced peripheral nerve conduction velocities and less residual ASA activity were present in P426L homozygotes vs I179S heterozygotes. CONCLUSION: The characteristic clinical differences between homozygous P426L and compound heterozygous I179S patients establish a distinct genotype-phenotype correlation in late-onset metachromatic leukodystrophy.

Original language	English (US)
Pages (from-to)	859-863
Number of pages	5
Journal	Neurology
Volume	67
Issue number	5
DOIs	https://doi.org/10.1212/01.wnl.0000234129.97727.4d
State	Published - Sep 2006

ASJC Scopus subject areas

Clinical Neurology

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Rauschka, H., Colsch, B., Baumann, N., Wevers, R., Schmidbauer, M., Krammer, M., Turpin, J. C., Lefevre, M., Olivier, C., Tardieu, S., Krivit, W., Moser, H., Moser, A., Gieselmann, V., Zalc, B., Cox, T., Reuner, U., Tylki-Szymanska, A., Aboul-Enein, F., ... Berger, J. (2006). Late-onset metachromatic leukodystrophy: Genotype strongly influences phenotype. Neurology, 67(5), 859-863. https://doi.org/10.1212/01.wnl.0000234129.97727.4d

Rauschka, H, Colsch, B, Baumann, N, Wevers, R, Schmidbauer, M, Krammer, M, Turpin, JC, Lefevre, M, Olivier, C, Tardieu, S, Krivit, W, Moser, H, Moser, A, Gieselmann, V, Zalc, B, Cox, T, Reuner, U, Tylki-Szymanska, A, Aboul-Enein, F, LeGuern, E, Bernheimer, H & Berger, J 2006, 'Late-onset metachromatic leukodystrophy: Genotype strongly influences phenotype', Neurology, vol. 67, no. 5, pp. 859-863. https://doi.org/10.1212/01.wnl.0000234129.97727.4d

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abstract = "BACKGROUND: P426L and I179S are the two most frequent mutations in juvenile and adult metachromatic leukodystrophy (late-onset MLD), which, in contrast to infantile MLD, show marked phenotypic heterogeneity. OBJECTIVE: To search for genotype-phenotype correlations in late-onset MLD. METHODS: The authors reviewed the clinical course of 22 patients homozygous for mutation P426L vs 20 patients heterozygous for mutation I179S, in which the second arylsulfatase A (ASA) mutation had also been determined. RESULTS: P426L homozygotes principally presented with progressive gait disturbance caused by spastic paraparesis or cerebellar ataxia; mental disturbance was absent or insignificant at the onset of disease but became more apparent as the disease evolved. In contrast, compound heterozygotes for I179S presented with schizophrenia-like behavioral abnormalities, social dysfunction, and mental decline, but motor deficits were scarce. Reduced peripheral nerve conduction velocities and less residual ASA activity were present in P426L homozygotes vs I179S heterozygotes. CONCLUSION: The characteristic clinical differences between homozygous P426L and compound heterozygous I179S patients establish a distinct genotype-phenotype correlation in late-onset metachromatic leukodystrophy.",

author = "H. Rauschka and B. Colsch and N. Baumann and R. Wevers and M. Schmidbauer and M. Krammer and Turpin, {J. C.} and M. Lefevre and C. Olivier and S. Tardieu and W. Krivit and H. Moser and A. Moser and V. Gieselmann and B. Zalc and T. Cox and U. Reuner and A. Tylki-Szymanska and F. Aboul-Enein and E. LeGuern and H. Bernheimer and J. Berger",

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doi = "10.1212/01.wnl.0000234129.97727.4d",

language = "English (US)",

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T1 - Late-onset metachromatic leukodystrophy

T2 - Genotype strongly influences phenotype

AU - Rauschka, H.

AU - Colsch, B.

AU - Baumann, N.

AU - Wevers, R.

AU - Schmidbauer, M.

AU - Krammer, M.

AU - Turpin, J. C.

AU - Lefevre, M.

AU - Olivier, C.

AU - Tardieu, S.

AU - Krivit, W.

AU - Moser, H.

AU - Moser, A.

AU - Gieselmann, V.

AU - Zalc, B.

AU - Cox, T.

AU - Reuner, U.

AU - Tylki-Szymanska, A.

AU - Aboul-Enein, F.

AU - LeGuern, E.

AU - Bernheimer, H.

AU - Berger, J.

PY - 2006/9

Y1 - 2006/9

N2 - BACKGROUND: P426L and I179S are the two most frequent mutations in juvenile and adult metachromatic leukodystrophy (late-onset MLD), which, in contrast to infantile MLD, show marked phenotypic heterogeneity. OBJECTIVE: To search for genotype-phenotype correlations in late-onset MLD. METHODS: The authors reviewed the clinical course of 22 patients homozygous for mutation P426L vs 20 patients heterozygous for mutation I179S, in which the second arylsulfatase A (ASA) mutation had also been determined. RESULTS: P426L homozygotes principally presented with progressive gait disturbance caused by spastic paraparesis or cerebellar ataxia; mental disturbance was absent or insignificant at the onset of disease but became more apparent as the disease evolved. In contrast, compound heterozygotes for I179S presented with schizophrenia-like behavioral abnormalities, social dysfunction, and mental decline, but motor deficits were scarce. Reduced peripheral nerve conduction velocities and less residual ASA activity were present in P426L homozygotes vs I179S heterozygotes. CONCLUSION: The characteristic clinical differences between homozygous P426L and compound heterozygous I179S patients establish a distinct genotype-phenotype correlation in late-onset metachromatic leukodystrophy.

AB - BACKGROUND: P426L and I179S are the two most frequent mutations in juvenile and adult metachromatic leukodystrophy (late-onset MLD), which, in contrast to infantile MLD, show marked phenotypic heterogeneity. OBJECTIVE: To search for genotype-phenotype correlations in late-onset MLD. METHODS: The authors reviewed the clinical course of 22 patients homozygous for mutation P426L vs 20 patients heterozygous for mutation I179S, in which the second arylsulfatase A (ASA) mutation had also been determined. RESULTS: P426L homozygotes principally presented with progressive gait disturbance caused by spastic paraparesis or cerebellar ataxia; mental disturbance was absent or insignificant at the onset of disease but became more apparent as the disease evolved. In contrast, compound heterozygotes for I179S presented with schizophrenia-like behavioral abnormalities, social dysfunction, and mental decline, but motor deficits were scarce. Reduced peripheral nerve conduction velocities and less residual ASA activity were present in P426L homozygotes vs I179S heterozygotes. CONCLUSION: The characteristic clinical differences between homozygous P426L and compound heterozygous I179S patients establish a distinct genotype-phenotype correlation in late-onset metachromatic leukodystrophy.

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Late-onset metachromatic leukodystrophy: Genotype strongly influences phenotype

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