Expanding the genetic and clinical spectrum of SLC25A42-associated disorders and testing of pantothenic acid to improve CoA level in vitro

Katharina Heckmann; Arcangela Iuso; Janine Reunert; Marianne Grüneberg; Anja Seelhöfer; Stephan Rust; Giuseppe Fiermonte; Eleonora Paradies; Carmela Piazzolla; Manoj Mannil; Thorsten Marquardt

doi:10.1002/jmd2.12441

Expanding the genetic and clinical spectrum of SLC25A42-associated disorders and testing of pantothenic acid to improve CoA level in vitro

JIMD Rep. 2024 Aug 21;65(6):417-425. doi: 10.1002/jmd2.12441. eCollection 2024 Nov.

Authors

Affiliations

¹ Department of General Pediatrics University Hospital Münster Münster Germany.
² Institute of Neurogenomics, Helmholtz Zentrum München Neuherberg Germany.
³ Institute of Human Genetics Technical University of Munich Munich Germany.
⁴ Department of Biosciences, Biotechnologies and Biopharmaceutics University of Bari Bari Italy.
⁵ Clinic of Radiology University Hospital Münster Münster Germany.

Abstract

SLC25A42 encodes the mitochondrial coenzyme A (CoA) transporter localized at the inner mitochondrial membrane. SLC25A42 deficiency leads to a congenital disease with a heterogeneous clinical presentation, including myopathy, developmental delay, lactic acidosis, and encephalopathy. Twenty-one patients have been described so far. In the current study, we report on the identification of new biallelic variants in SLC25A42 in three siblings. Patients presented with symmetrical T2 hyperintensity of the putamen with minor volume depression at the brain MRI, elevated lactate, reduced oxygen consumption rates in muscle and fibroblasts, and reduced CoA levels in fibroblasts. Administration of pantothenic acid led to clinical stabilization and increased CoA levels in fibroblasts, thus confirming a role for SLC25A42 in energy metabolism and CoA homeostasis.

Keywords: SLC25A42; cellular CoA; mitochondrial coenzyme transporter; mitochondrial respiration; pantothenic acid.