Molybdenum cofactor and isolated sulphite oxidase deficiencies: Clinical and molecular spectrum among Egyptian patients

Maha S Zaki; Laila Selim; Hala T El-Bassyouni; Mahmoud Y Issa; Iman Mahmoud; Samira Ismail; Mariane Girgis; Abdelrahim A Sadek; Joseph G Gleeson; Mohamed S Abdel Hamid

doi:10.1016/j.ejpn.2016.05.011

Molybdenum cofactor and isolated sulphite oxidase deficiencies: Clinical and molecular spectrum among Egyptian patients

Eur J Paediatr Neurol. 2016 Sep;20(5):714-22. doi: 10.1016/j.ejpn.2016.05.011. Epub 2016 May 30.

Authors

Affiliations

¹ Clinical Genetics Department, Human Genetics and Genome Research Division, National Research Centre, Cairo 12311, Egypt. Electronic address: dr_mahazaki@yahoo.com.
² Pediatric Department, Neurometabolic Clinic, Cairo University, Cairo 12613, Egypt.
³ Clinical Genetics Department, Human Genetics and Genome Research Division, National Research Centre, Cairo 12311, Egypt.
⁴ Pediatric Neurology Department, Faculty of Medicine, Sohag University, Sohag 82524, Egypt.
⁵ Laboratory for Pediatric Brain Disease, Howard Hughes Medical Institute, Department of Neurosciences, University of California, San Diego, CA 92093, USA.
⁶ Medical Molecular Genetics Department, Human Genetics and Genome Research Division, National Research Centre, Cairo 12311, Egypt.

Abstract

Aim: Molybdenum cofactor deficiency (MoCD) and Sulfite oxidase deficiency (SOD) are rare autosomal recessive conditions of sulfur-containing amino acid metabolism with overlapping clinical features and emerging therapies. The clinical phenotype is indistinguishable and they can only be differentiated biochemically. MOCS1, MOCS2, MOCS3, and GPRN genes contribute to the synthesis of molybdenum cofactor, and SUOX gene encodes sulfite oxidase. The aim of this study was to elucidate the clinical, radiological, biochemical and molecular findings in patients with SOD and MoCD.

Methods: Detailed clinical and radiological assessment of 9 cases referred for neonatal encephalopathy with hypotonia, microcephaly, and epilepsy led to a consideration of disorders of sulfur-containing amino acid metabolism. The diagnosis of six with MoCD and three with SOD was confirmed by biochemical tests, targeted sequencing, and whole exome sequencing where suspicion of disease was lower.

Results: Novel SUOX mutations were detected in 3 SOD cases and a novel MOCS2 mutation in 1 MoCD case. Most patients presented in the first 3 months of life with intractable tonic-clonic seizures, axial hypotonia, limb hypertonia, exaggerated startle response, feeding difficulties, and progressive cystic encephalomalacia on brain imaging. A single patient with MoCD had hypertrophic cardiomyopathy, hitherto unreported with these diseases.

Interpretation: Our results emphasize that intractable neonatal seizures, spasticity, and feeding difficulties can be important early signs for these disorders. Progressive microcephaly, intellectual disability and specific brain imaging findings in the first year were additional diagnostic aids. These clinical cues can be used to minimize delays in diagnosis, especially since promising treatments are emerging for MoCD type A.

Keywords: Epilepsy; MOCS1 gene; MOCS2 gene; Microcephaly; Molybdenum cofactor deficiency; SUOX gene; Sulfite oxidase deficiency.

MeSH terms

Amino Acid Metabolism, Inborn Errors* / genetics
Amino Acid Metabolism, Inborn Errors* / physiopathology
Coenzymes / genetics
Egypt
Humans
Infant, Newborn
Infant, Newborn, Diseases
Male
Metal Metabolism, Inborn Errors* / genetics
Metal Metabolism, Inborn Errors* / physiopathology
Metalloproteins / genetics
Molybdenum Cofactors
Molybdoferredoxin / genetics
Mutation
Phenotype
Pteridines
Sulfite Oxidase / deficiency*
Sulfite Oxidase / genetics

Substances

Coenzymes
Metalloproteins
Molybdenum Cofactors
Molybdoferredoxin
Pteridines
molybdenum cofactor
Sulfite Oxidase

Supplementary concepts

Molybdenum cofactor deficiency
Sulfite oxidase deficiency

Abstract

MeSH terms

Substances

Supplementary concepts

Grants and funding