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First two unrelated cases of isolated sedoheptulokinase deficiency: A benign disorder?

Authors :
Wamelink, M.M.C. (Mirjam)
Ramos, R.J.J.F. (Ruben J. J. F.)
van den Elzen, A.P.M. (Annette P. M.)
Ruijter, G.J.G. (George)
Bonte, R. (Ramon)
Diogo, L. (Luisa)
Garcia, P. (Paula)
Neves, N. (Nelson)
Nota, B. (Benjamin)
Haschemi, A. (Arvand)
Tavares de Almeida, I. (Isabel)
Salomons, G.S. (Gajja)
Wamelink, M.M.C. (Mirjam)
Ramos, R.J.J.F. (Ruben J. J. F.)
van den Elzen, A.P.M. (Annette P. M.)
Ruijter, G.J.G. (George)
Bonte, R. (Ramon)
Diogo, L. (Luisa)
Garcia, P. (Paula)
Neves, N. (Nelson)
Nota, B. (Benjamin)
Haschemi, A. (Arvand)
Tavares de Almeida, I. (Isabel)
Salomons, G.S. (Gajja)
Publication Year :
2015

Abstract

We present the first two reported unrelated patients with an isolated sedoheptulokinase (SHPK) deficiency. The first patient presented with neonatal cholestasis, hypoglycemia, and anemia, while the second patient presented with congenital arthrogryposis multiplex, multiple contractures, and dysmorphisms. Both patients had elevated excretion of erythritol and sedoheptulose, and each had a homozygous nonsense mutation in SHPK. SHPK is an enzyme that phosphorylates sedoheptulose to sedoheptulose-7-phosphate, which is an important intermediate of the pentose phosphate pathway. It is questionable whether SHPK deficiency is a causal factor for the clinical phenotypes of our patients. This study illustrates the necessity of extensive functional and clinical workup for interpreting a novel variant, including nonsense variants.

Details

Database :
OAIster
Notes :
application/pdf, Journal of Inherited Metabolic Disease vol. 38 no. 5, pp. 889-894, English
Publication Type :
Electronic Resource
Accession number :
edsoai.ocn957102885
Document Type :
Electronic Resource
Full Text :
https://doi.org/10.1007.s10545-014-9809-1