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Effect of riboflavin deficiency on development of the cerebral cortex in Slc52a3 knockout mice

Congyun Jin, Atsushi Yonezawa, Hiroki‎ Yoshimatsu, Satoshi Imai, Madoka Koyanagi, Kaori Yamanishi, Shunsaku Nakagawa, Kotaro Itohara, Tomohiro Omura, Takayuki Nakagawa, Junya Nagai, Kazuo Matsubara

2020Scientific Reports19 citationsDOIOpen Access PDF

Abstract

Abstract Riboflavin transporter 3 (RFVT3), encoded by the SLC52A3 gene, is important for riboflavin homeostasis in the small intestine, kidney, and placenta. Our previous study demonstrated that Slc52a3 knockout ( Slc52a3 −/−) mice exhibited neonatal lethality and metabolic disorder due to riboflavin deficiency. Here, we investigated the influence of Slc52a3 gene disruption on brain development using Slc52a3 −/− embryos. Slc52a3 −/− mice at postnatal day 0 showed hypoplasia of the brain and reduced thickness of cortical layers. At embryonic day 13.5, the formation of Tuj1 + neurons and Tbr2 + intermediate neural progenitors was significantly decreased; no significant difference was observed in the total number and proliferative rate of Pax6 + radial glia. Importantly, the hypoplastic phenotype was rescued upon riboflavin supplementation. Thus, it can be concluded that RFVT3 contributes to riboflavin homeostasis in embryos and that riboflavin itself is required during embryonic development of the cerebral cortex in mice.

Topics & Concepts

RiboflavinCerebral cortexBiologyPAX6Knockout mouseEmbryogenesisHomeostasisHypoplasiaCortex (anatomy)EndocrinologyEmbryoInternal medicineCell biologyNeuroscienceBiochemistryAnatomyMedicineGeneTranscription factorDiet and metabolism studiesBirth, Development, and HealthMetabolism and Genetic Disorders