SERAC1 Deficiency- A New Phenotype

Emanuel Martins; João Durães; Célia Nogueira; João Gomes; Laura Vilarinho; Carmo Macário

doi:10.2174/1871530323666230914114456

SERAC1 Deficiency- A New Phenotype

Endocr Metab Immune Disord Drug Targets. 2023 Sep 14. doi: 10.2174/1871530323666230914114456. Online ahead of print.

Authors

Emanuel Martins¹, João Durães², Célia Nogueira³, João Gomes³, Laura Vilarinho³, Carmo Macário²

Affiliations

¹ Centro Hospitalar Universitário de Coimbra Neurology Department Coimbra Portugal.
² Centro Hospitalar Universitário de Coimbra Centro de Referência de Doenças Hereditárias do Metabolismo (Portugal); MetabERN (Portugal) Coimbra Portugal.
³ Instituto Nacional de Saúde Doutor Ricardo Jorge Unidade de Rastreio Neonatal Metabolismo e Genética, Departamento de Genética Humana Porto Portugal.

PMID: 37711114
DOI: 10.2174/1871530323666230914114456

Abstract

Introduction - SERAC1 deficiency phenotype range from MEGD(H)EL syndrome, the most severe, to juvenile complicated spastic paraplegia, to adult-onset dystonic features (in only one patient). The MEGD(H)EL syndrome is characterized by (3-methylglutaconic aciduria with deafness-dystonia, [hepatopathy], encephalopathy, and Leigh-like syndrome). Biochemical abnormalities: elevated urinary 3 - metilglutaconic and 3-metilglutaric acids, high lactate and alanine in serum. Diagnosis is confirmed when biallelic pathogenic variants in SERAC1 gene are found. Brain MRI: basal ganglia lesions and generalized atrophy. Results/Case report - A 30-year-old patient with a moderate intellectual disability, developed, since the age of 25, a progressive loss of previous capacities (hand dexterity, oral language), and later subacute generalized dystonic features. Currently he has spastic tetraparesis, dystonia, scoliosis and autistic behavior, with bilateral basal ganglia lesions on brain MRI. Genetic study revealed biallelic pathogenic variants in SERAC1 gene, confirm MEGD(H)EL. A 73 years old patient with cognitive impairment and progressive spastic tetraparesis had multiple periventricular T2 hyperintense lesions. She has a homozygotic SERAC1 variant NM_032861: exon4:c.T139A: p.F471 (rs112780453), considered benign. Biochemical study revealed elevated plasmatic alanine and urinary3-metilglutaconic and 3-metilglutaric acid. This profile is concordant with mitochondrial dysfunction and SERAC1 Deficit. Conclusion - The first patient has the clinical symptoms associated to the MEGD(H)EL syndrome, and the biochemical and genetic confirmation of the diagnosis, without reservations. However, in the second patient, the progressive paraparesis and cognitive impairment did not appear to be caused by multiple sclerosis nor subcortical vascular leukoencephalopathy (without vascular risk factors). The abnormal biochemical profile is suggestive of SERAC1 Deficiency, even without genetic confirmation. In what should we believe?

Keywords: 3-methylglutaconic aciduria; MEGD(H)EL syndrome; MEGDEL syndrome; SERAC1 deficiency.