Biallelic Variation in the Choline and Ethanolamine Transporter FLVCR1 Underlies a Severe Developmental Disorder Spectrum

Authors

Daniel G Calame
Jovi Huixin Wong
Puravi Panda
Dat Tuan Nguyen
Nancy C P Leong
Riccardo Sangermano
Sohil G Patankar
Mohamed S Abdel-Hamid
Lama AlAbdi
Sylvia Safwat
Kyle P Flannery
Zain Dardas
Jawid M Fatih
Chaya Murali
Varun Kannan
Timothy E Lotze
Isabella Herman
Farah Ammouri
Brianna Rezich
Stephanie Efthymiou
Shahryar Alavi
David Murphy
Zahra Firoozfar
Mahya Ebrahimi Nasab
Amir Bahreini
Majid Ghasemi
Nourelhoda A Haridy
Hamid Reza Goldouzi
Fatemeh Eghbal
Ehsan Ghayoor Karimiani
Amber Begtrup
Houda Elloumi
Varunvenkat M Srinivasan
Vykuntaraju K Gowda
Haowei Du
Shalini N Jhangiani
Zeynep Coban-Akdemir
Dana Marafi
Lance Rodan
Sedat Isikay
Jill A Rosenfeld
Subhadra Ramanathan
Michael Staton
Kerby C Oberg
Robin D Clark
Catharina Wenman
Sam Loughlin
Ramy Saad
Tazeen Ashraf
Alison Male
Shereen Tadros
Reza Boostani
Ghada M H Abdel-Salam
Maha Zaki
Ali Mardi
Farzad Hashemi-Gorji
Ebtesam Abdalla
M Chiara Manzini
Davut Pehlivan
Jennifer E Posey
Richard A Gibbs
Henry Houlden
Fowzan S Alkuraya
Kinga Bujakowska
Reza Maroofian
James R Lupski
Long N Nguyen

Language

English

Publication Date

1-1-2025

Journal

Genetics in Medicine

DOI

10.1016/j.gim.2024.101273

PMID

39306721

Abstract

Purpose: FLVCR1 encodes a solute carrier protein implicated in heme, choline, and ethanolamine transport. Although Flvcr1-/- mice exhibit skeletal malformations and defective erythropoiesis reminiscent of Diamond-Blackfan anemia (DBA), biallelic FLVCR1 variants in humans have previously only been linked to childhood or adult-onset ataxia, sensory neuropathy, and retinitis pigmentosa.

Methods: We identified individuals with undiagnosed neurodevelopmental disorders and biallelic FLVCR1 variants through international data sharing and characterized the functional consequences of their FLVCR1 variants.

Results: We ascertained 30 patients from 23 unrelated families with biallelic FLVCR1 variants and characterized a novel FLVCR1-related phenotype: severe developmental disorders with profound developmental delay, microcephaly (z-score -2.5 to -10.5), brain malformations, epilepsy, spasticity, and premature death. Brain malformations ranged from mild brain volume reduction to hydranencephaly. Severely affected patients share traits, including macrocytic anemia and skeletal malformations, with Flvcr1-/- mice and DBA. FLVCR1 variants significantly reduce choline and ethanolamine transport and/or disrupt mRNA splicing.

Conclusion: These data demonstrate a broad FLVCR1-related phenotypic spectrum ranging from severe multiorgan developmental disorders resembling DBA to adult-onset neurodegeneration. Our study expands our understanding of Mendelian choline and ethanolamine disorders and illustrates the importance of anticipating a wide phenotypic spectrum for known disease genes and incorporating model organism data into genome analysis to maximize genetic testing yield.

Keywords

Humans, Male, Female, Membrane Transport Proteins, Animals, Developmental Disabilities, Mice, Child, Child, Preschool, Alleles, Choline, Ethanolamine, Infant, Phenotype, Adolescent, Adult, Mutation, Receptors, Virus, Choline, Diamond-Blackfan anemia, FLVCR1, Neurodegeneration, Neurodevelopmental disorders

Published Open-Access

yes

Recommended Citation

Calame, Daniel G; Wong, Jovi Huixin; Panda, Puravi; et al., "Biallelic Variation in the Choline and Ethanolamine Transporter FLVCR1 Underlies a Severe Developmental Disorder Spectrum" (2025). Faculty, Staff and Students Publications. 6239.
https://digitalcommons.library.tmc.edu/baylor_docs/6239