| Literature DB >> 31919777 |
Nirav J Patel1, Kirk J Hogan2, Elias Rizk1, Krista Stewart1, Andy Madrid1, Sivan Vadakkadath Meethal1, Reid Alisch1, Laura Borth1, Ligia A Papale1, Solomon Ondoma1, Logan R Gorges1, Kara Weber1, Wendell Lake1, Andrew Bauer1, Nithya Hariharan1, Thomas Kuehn1, Thomas Cook3, Sunduz Keles3,4, Michael A Newton3,4, Bermans J Iskandar5.
Abstract
Folate supplementation in F0 mating rodents increases regeneration of injured spinal axons in vivo in 4 or more generations of progeny (F1-F4) in the absence of interval folate administration to the progeny. Transmission of the enhanced regeneration phenotype to untreated progeny parallels axonal growth in neuron culture after in vivo folate administration to the F0 ancestors alone, in correlation with differential patterns of genomic DNA methylation and RNA transcription in treated lineages. Enhanced axonal regeneration phenotypes are observed with diverse folate preparations and routes of administration, in outbred and inbred rodent strains, and in two rodent genera comprising rats and mice, and are reversed in F4-F5 progeny by pretreatment with DNA demethylating agents prior to phenotyping. Uniform transmission of the enhanced regeneration phenotype to progeny together with differential patterns of DNA methylation and RNA expression is consistent with a non-Mendelian mechanism. The capacity of an essential nutritional co-factor to induce a beneficial transgenerational phenotype in untreated offspring carries broad implications for the diagnosis, prevention, and treatment of inborn and acquired disorders.Entities:
Keywords: Axonal regeneration; Central nervous system (CNS); DNA methylation; Epigenetics; Folic acid; Spinal cord injury; Transgenerational inheritance
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Year: 2020 PMID: 31919777 PMCID: PMC7125003 DOI: 10.1007/s12035-019-01812-5
Source DB: PubMed Journal: Mol Neurobiol ISSN: 0893-7648 Impact factor: 5.590