TRNA Modification Enzyme-dependent Redox Homeostasis Regulates Synapse Formation and Memory

Overview

Journal Proc Natl Acad Sci U S A

Specialty Science

Date 2024 Nov 4

PMID 39495910

Authors

Kimberly R Madhwani

Shanzeh Sayied

Carlson H Ogata

Caley A Hogan

Jenna M Lentini

Moushami Mallik

Jennifer L Dumouchel

Erik Storkebaum

Dragony Fu

Kate M OConnor-Giles

Affiliations

Soon will be listed here.

Abstract

Post-transcriptional modification of RNA regulates gene expression at multiple levels. ALKBH8 is a tRNA-modifying enzyme that methylates wobble uridines in a subset of tRNAs to modulate translation. Through methylation of tRNA-selenocysteine, ALKBH8 promotes selenoprotein synthesis and regulates redox homeostasis. Pathogenic variants in have been linked to intellectual disability disorders in the human population, but the role of ALKBH8 in the nervous system is unknown. Through in vivo studies in , we show that ALKBH8 controls oxidative stress in the brain to restrain synaptic growth and support learning and memory. null animals lack wobble uridine methylation and exhibit reduced protein synthesis in the nervous system, including a specific decrease in selenoprotein levels. Either loss of or independent disruption of selenoprotein synthesis results in ectopic synapse formation. Genetic expression of antioxidant enzymes fully suppresses synaptic overgrowth in null animals, confirming oxidative stress as the underlying cause of dysregulation. null animals also exhibit associative memory impairments that are reversed by pharmacological antioxidant treatment. Together, these findings demonstrate the critical role of tRNA wobble uridine modification in redox homeostasis in the developing nervous system and reveal antioxidants as a potential therapy for ALKBH8-associated intellectual disability.

Citing Articles

RNA dynamics in oxidative stress: From obscurity to mechanistic understanding in health and disease.

Contreras L, Belfort M Proc Natl Acad Sci U S A. 2024; 121(46):e2420445121.

PMID: 39495921 PMC: 11573495. DOI: 10.1073/pnas.2420445121.

tRNA modification enzyme-dependent redox homeostasis regulates synapse formation and memory.

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