Cerebral folate deficiency in two siblings caused by biallelic variants including a novel mutation of FOLR1 gene: Intrafamilial heterogeneity following early treatment and the role of ketogenic diet

Cerebral folate deficiency in two siblings caused by biallelic variants including a novel mutation of FOLR1 gene: Intrafamilial heterogeneity following early treatment and the role of ketogenic diet

Mutations in the FOLR1 gene, encoding for the folate alpha receptor (FRa), represent a rare recessive genetic cause of cerebral folate deficiency (CFD), a potentially reversible neurometabolic condition. Patients typically present with developmental delay, seizures, abnormal movements, and delayed m...

Full description

Saved in:
Bibliographic Details
Published in:JIMD reports Vol. 60; no. 1; pp. 3 - 9
Main Authors: Papadopoulou, Maria T., Dalpa, Efterpi, Portokalas, Michalis, Katsanika, Irene, Tirothoulaki, Katerina, Spilioti, Martha, Gerou, Spyros, Plecko, Barbara, Evangeliou, Athanasios E.
Format: Journal Article
Language:English
Published: Hoboken, USA John Wiley & Sons, Inc 01-07-2021
Wiley
Subjects:
Age
Ataxia
Autism
Case Report
Case Reports
cerebral folate deficiency
Convulsions & seizures
Dihydrofolate reductase
Drug dosages
Epilepsy
epileptic spasms
folinic acid
FORL1
FRa
ketogenic diet
Metabolism
Metabolites
Motor ability
Mutation
Nervous system
Patients
Siblings
Vitamin B
Vitamin deficiency
FORL1
cerebral folate deficiency
FRa
folinic acid
ketogenic diet
epileptic spasms
Online Access:Get full text
Tags: Add Tag
No Tags, Be the first to tag this record!
Description
Summary:Mutations in the FOLR1 gene, encoding for the folate alpha receptor (FRa), represent a rare recessive genetic cause of cerebral folate deficiency (CFD), a potentially reversible neurometabolic condition. Patients typically present with developmental delay, seizures, abnormal movements, and delayed myelination. We hereby expand the phenotypic and genotypic spectrum of the disease with the report of the first two Greek siblings that were found compound heterozygous for one known FOLR1 gene mutation (p.Cys65Trp) and a mutation (p.Trp143Arg) that has not yet been reported in the literature (class 3 variant according to ASHG classification). A distinguishing feature of the older sibling is the manifestation of drug‐resistant epileptic spasms beyond infancy. These had a relatively good response to a ketogenic diet, as an additional treatment to topiramate and valproate. A further clinical improvement was observed when folinic acid was combined with the above treatment. While a response to folinic acid is well established in the disorder, the efficacy of its combination with the ketogenic diet needs further evaluation, but we suggest considering it early in the course of drug resistant epilepsy in the setting of CFD. The younger sibling was diagnosed and treated with folinic acid at an early‐symptomatic stage. Both patients had moderately low age‐related CSF 5‐methyltetrahydrofolate levels at diagnosis with the older sibling (that was already treated at base line collection) averaging 19 nmol/L (normal range: 44‐122 nmol/L) and the younger one 49 nmol/L (normal range 63‐122 nmol/L). These levels were restored to normal limits after folinic supplementation.
Bibliography:Brian Fowler
Communicating Editor
Communicating Editor: Brian Fowler
ISSN:2192-8312
2192-8304
2192-8312
DOI:10.1002/jmd2.12206