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Novel biallelic variants expand the SLC5A6-related phenotypic spectrum

Tess Holling, Sheela Nampoothiri, Bedirhan Tarhan, Pauline E. Schneeberger, Kollencheri Puthenveettil Vinayan, Dhanya Yesodharan, Arun Grace Roy, Periyasamy Radhakrishnan, Malik Alawi, Lindsay Rhodes, Katta Mohan Girisha, Peter B. Kang, Kerstin Kutsche

2022European Journal of Human Genetics23 citationsDOIOpen Access PDF

Abstract

-dependent uptake of biotin (vitamin B7), pantothenic acid (vitamin B5), the vitamin-like substance α-lipoic acid, and iodide. Compound heterozygous SLC5A6 variants have been reported in individuals with variable multisystemic disorder, including failure to thrive, developmental delay, seizures, cerebral palsy, brain atrophy, gastrointestinal problems, immunodeficiency, and/or osteopenia. We expand the phenotypic spectrum associated with biallelic SLC5A6 variants affecting function by reporting five individuals from three families with motor neuropathies. We identified the homozygous variant c.1285 A > G [p.(Ser429Gly)] in three affected siblings and a simplex patient and the maternally inherited c.280 C > T [p.(Arg94*)] variant and the paternally inherited c.485 A > G [p.(Tyr162Cys)] variant in the simplex patient of the third family. Both missense variants were predicted to affect function by in silico tools. 3D homology modeling of the human SMVT revealed 13 transmembrane helices (TMs) and Tyr162 and Ser429 to be located at the cytoplasmic facing region of TM4 and within TM11, respectively. The SLC5A6 missense variants p.(Tyr162Cys) and p.(Ser429Gly) did not affect plasma membrane localization of the ectopically expressed multivitamin transporter suggesting reduced but not abolished function, such as lower catalytic activity. Targeted therapeutic intervention yielded clinical improvement in four of the five patients. Early molecular diagnosis by exome sequencing is essential for timely replacement therapy in affected individuals.

Topics & Concepts

Missense mutationBiologyGeneticsCompound heterozygosityIn silicoPhenotypeExome sequencingAlleleExonTransmembrane domainLocus (genetics)Loss functionSymporterHuman geneticsGeneExomeSolute carrier familyHaplotypeMutationAllelic heterogeneityTransmembrane proteinTransporterBiotin and Related StudiesBiochemical Acid Research StudiesAmino Acid Enzymes and Metabolism
Novel biallelic variants expand the SLC5A6-related phenotypic spectrum | Litcius