Prediction of outcome in isolated methylmalonic acidurias: Combined use of clinical and biochemical parameters

Friederike Hörster; S. F. Garbade; T. Zwickler; M. Lindner; S. Kölker; H. I. Aydin; O. A. Bodamer; A. B. Burlina; A. M. Das; J. B.C. De Klerk; C. Dionisi-Vici; S. Geb; G. Gökcay; N. Guffon; E. M. Maier; E. Morava; J. H. Walter; B. Schwahn; F. A. Wijburg; S. Grünewald; M. R. Baumgartner

doi:10.1007/s10545-009-1189-6

Prediction of outcome in isolated methylmalonic acidurias: Combined use of clinical and biochemical parameters

Friederike Hörster, S. F. Garbade, T. Zwickler, M. Lindner, S. Kölker, H. I. Aydin, O. A. Bodamer, A. B. Burlina, A. M. Das, J. B.C. De Klerk, C. Dionisi-Vici, S. Geb, G. Gökcay, N. Guffon, E. M. Maier, E. Morava, J. H. Walter, B. Schwahn, F. A. Wijburg, S. GrünewaldM. R. Baumgartner

Medical Genetics

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41 Scopus citations

Abstract

Objectives: Isolated methylmalonic acidurias (MMAurias) are caused by deficiency of methylmalonyl-CoA mutase or by defects in the synthesis of its cofactor 5′-deoxyadenosylcobalamin. The aim of this study was to evaluate which parameters best predicted the long-term outcome. Methods: Standardized questionnaires were sent to 20 European metabolic centres asking for age at diagnosis, birth decade, diagnostic work-up, cobalamin responsiveness, enzymatic subgroup (mut⁰, mut^-, cblA, cblB) and different aspects of long-term outcome. Results: 273 patients were included. Neonatal onset of the disease was associated with increased mortality rate, high frequency of developmental delay, and severe handicap. Cobalamin non-responsive patients with neonatal onset born in the 1970s and 1980s had a particularly poor outcome. A more favourable outcome was found in patients with late onset of symptoms, especially when cobalamin responsive or classified as mut^-. Prevention of neonatal crises in pre-symptomatically diagnosed newborns was identified as a protective factor concerning handicap. Chronic renal failure manifested earlier in mut⁰ patients than in other enzymatic subgroups. Conclusion: Outcome in MMAurias is best predicted by the enzymatic subgroup, cobalamin responsiveness, age at onset and birth decade. The prognosis is still unfavourable in patients with neonatal metabolic crises and non-responsiveness to cobalamin, in particular mut⁰ patients.

Original language	English (US)
Pages (from-to)	630-639
Number of pages	10
Journal	Journal of inherited metabolic disease
Volume	32
Issue number	5
DOIs	https://doi.org/10.1007/s10545-009-1189-6
State	Published - 2009

ASJC Scopus subject areas

Genetics
Genetics(clinical)

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10.1007/s10545-009-1189-6

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Hörster, F., Garbade, S. F., Zwickler, T., Lindner, M., Kölker, S., Aydin, H. I., Bodamer, O. A., Burlina, A. B., Das, A. M., De Klerk, J. B. C., Dionisi-Vici, C., Geb, S., Gökcay, G., Guffon, N., Maier, E. M., Morava, E., Walter, J. H., Schwahn, B., Wijburg, F. A., ... Baumgartner, M. R. (2009). Prediction of outcome in isolated methylmalonic acidurias: Combined use of clinical and biochemical parameters. Journal of inherited metabolic disease, 32(5), 630-639. https://doi.org/10.1007/s10545-009-1189-6

Hörster, F, Garbade, SF, Zwickler, T, Lindner, M, Kölker, S, Aydin, HI, Bodamer, OA, Burlina, AB, Das, AM, De Klerk, JBC, Dionisi-Vici, C, Geb, S, Gökcay, G, Guffon, N, Maier, EM, Morava, E, Walter, JH, Schwahn, B, Wijburg, FA, Grünewald, S & Baumgartner, MR 2009, 'Prediction of outcome in isolated methylmalonic acidurias: Combined use of clinical and biochemical parameters', Journal of inherited metabolic disease, vol. 32, no. 5, pp. 630-639. https://doi.org/10.1007/s10545-009-1189-6

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title = "Prediction of outcome in isolated methylmalonic acidurias: Combined use of clinical and biochemical parameters",

abstract = "Objectives: Isolated methylmalonic acidurias (MMAurias) are caused by deficiency of methylmalonyl-CoA mutase or by defects in the synthesis of its cofactor 5′-deoxyadenosylcobalamin. The aim of this study was to evaluate which parameters best predicted the long-term outcome. Methods: Standardized questionnaires were sent to 20 European metabolic centres asking for age at diagnosis, birth decade, diagnostic work-up, cobalamin responsiveness, enzymatic subgroup (mut0, mut-, cblA, cblB) and different aspects of long-term outcome. Results: 273 patients were included. Neonatal onset of the disease was associated with increased mortality rate, high frequency of developmental delay, and severe handicap. Cobalamin non-responsive patients with neonatal onset born in the 1970s and 1980s had a particularly poor outcome. A more favourable outcome was found in patients with late onset of symptoms, especially when cobalamin responsive or classified as mut-. Prevention of neonatal crises in pre-symptomatically diagnosed newborns was identified as a protective factor concerning handicap. Chronic renal failure manifested earlier in mut0 patients than in other enzymatic subgroups. Conclusion: Outcome in MMAurias is best predicted by the enzymatic subgroup, cobalamin responsiveness, age at onset and birth decade. The prognosis is still unfavourable in patients with neonatal metabolic crises and non-responsiveness to cobalamin, in particular mut0 patients.",

author = "Friederike H{\"o}rster and Garbade, {S. F.} and T. Zwickler and M. Lindner and S. K{\"o}lker and Aydin, {H. I.} and Bodamer, {O. A.} and Burlina, {A. B.} and Das, {A. M.} and {De Klerk}, {J. B.C.} and C. Dionisi-Vici and S. Geb and G. G{\"o}kcay and N. Guffon and Maier, {E. M.} and E. Morava and Walter, {J. H.} and B. Schwahn and Wijburg, {F. A.} and S. Gr{\"u}newald and Baumgartner, {M. R.}",

year = "2009",

doi = "10.1007/s10545-009-1189-6",

language = "English (US)",

volume = "32",

pages = "630--639",

journal = "Journal of inherited metabolic disease",

issn = "0141-8955",

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TY - JOUR

T1 - Prediction of outcome in isolated methylmalonic acidurias

T2 - Combined use of clinical and biochemical parameters

AU - Hörster, Friederike

AU - Garbade, S. F.

AU - Zwickler, T.

AU - Lindner, M.

AU - Kölker, S.

AU - Aydin, H. I.

AU - Bodamer, O. A.

AU - Burlina, A. B.

AU - Das, A. M.

AU - De Klerk, J. B.C.

AU - Dionisi-Vici, C.

AU - Geb, S.

AU - Gökcay, G.

AU - Guffon, N.

AU - Maier, E. M.

AU - Morava, E.

AU - Walter, J. H.

AU - Schwahn, B.

AU - Wijburg, F. A.

AU - Grünewald, S.

AU - Baumgartner, M. R.

PY - 2009

Y1 - 2009

N2 - Objectives: Isolated methylmalonic acidurias (MMAurias) are caused by deficiency of methylmalonyl-CoA mutase or by defects in the synthesis of its cofactor 5′-deoxyadenosylcobalamin. The aim of this study was to evaluate which parameters best predicted the long-term outcome. Methods: Standardized questionnaires were sent to 20 European metabolic centres asking for age at diagnosis, birth decade, diagnostic work-up, cobalamin responsiveness, enzymatic subgroup (mut0, mut-, cblA, cblB) and different aspects of long-term outcome. Results: 273 patients were included. Neonatal onset of the disease was associated with increased mortality rate, high frequency of developmental delay, and severe handicap. Cobalamin non-responsive patients with neonatal onset born in the 1970s and 1980s had a particularly poor outcome. A more favourable outcome was found in patients with late onset of symptoms, especially when cobalamin responsive or classified as mut-. Prevention of neonatal crises in pre-symptomatically diagnosed newborns was identified as a protective factor concerning handicap. Chronic renal failure manifested earlier in mut0 patients than in other enzymatic subgroups. Conclusion: Outcome in MMAurias is best predicted by the enzymatic subgroup, cobalamin responsiveness, age at onset and birth decade. The prognosis is still unfavourable in patients with neonatal metabolic crises and non-responsiveness to cobalamin, in particular mut0 patients.

AB - Objectives: Isolated methylmalonic acidurias (MMAurias) are caused by deficiency of methylmalonyl-CoA mutase or by defects in the synthesis of its cofactor 5′-deoxyadenosylcobalamin. The aim of this study was to evaluate which parameters best predicted the long-term outcome. Methods: Standardized questionnaires were sent to 20 European metabolic centres asking for age at diagnosis, birth decade, diagnostic work-up, cobalamin responsiveness, enzymatic subgroup (mut0, mut-, cblA, cblB) and different aspects of long-term outcome. Results: 273 patients were included. Neonatal onset of the disease was associated with increased mortality rate, high frequency of developmental delay, and severe handicap. Cobalamin non-responsive patients with neonatal onset born in the 1970s and 1980s had a particularly poor outcome. A more favourable outcome was found in patients with late onset of symptoms, especially when cobalamin responsive or classified as mut-. Prevention of neonatal crises in pre-symptomatically diagnosed newborns was identified as a protective factor concerning handicap. Chronic renal failure manifested earlier in mut0 patients than in other enzymatic subgroups. Conclusion: Outcome in MMAurias is best predicted by the enzymatic subgroup, cobalamin responsiveness, age at onset and birth decade. The prognosis is still unfavourable in patients with neonatal metabolic crises and non-responsiveness to cobalamin, in particular mut0 patients.

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AN - SCOPUS:70350294124

SN - 0141-8955

VL - 32

SP - 630

EP - 639

JO - Journal of inherited metabolic disease

JF - Journal of inherited metabolic disease

IS - 5

ER -

Prediction of outcome in isolated methylmalonic acidurias: Combined use of clinical and biochemical parameters

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