Segregation of an MSH1 RNAi transgene produces heritable non-genetic memory in association with methylome reprogramming
MSH1 is a plant-specific protein. RNAi suppression of MSH1 results in phenotype variability for developmental and stress response pathways. Segregation of the RNAi transgene produces non-genetic msh1 ‘memory’ with multi-generational inheritance. First-generation memory versus non-memory comparison,...
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Veröffentlicht in: | Nature communications 2020-05, Vol.11 (1), p.2214-2214, Article 2214 |
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Sprache: | eng |
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Zusammenfassung: | MSH1 is a plant-specific protein. RNAi suppression of
MSH1
results in phenotype variability for developmental and stress response pathways. Segregation of the RNAi transgene produces non-genetic
msh1
‘memory’ with multi-generational inheritance. First-generation memory versus non-memory comparison, and six-generation inheritance studies, identifies gene-associated, heritable methylation repatterning. Genome-wide methylome analysis integrated with RNAseq and network-based enrichment studies identifies altered circadian clock networks, and phytohormone and stress response pathways that intersect with circadian control. A total of 373 differentially methylated loci comprising these networks are sufficient to discriminate memory from nonmemory full sibs. Methylation inhibitor 5-azacytidine diminishes the differences between memory and wild type for growth, gene expression and methylation patterning. The
msh1
reprogramming is dependent on functional
HISTONE DEACETYLASE 6
and methyltransferase
MET1
, and transition to memory requires the RNA-directed DNA methylation pathway. This system of phenotypic plasticity may serve as a potent model for defining accelerated plant adaptation during environmental change.
Segregation of an MSH1 RNAi transgene produces non-genetic memory that displays transgenerational inheritance in Arabidopsis. Here, the authors compare memory and non-memory full-sib progenies to show the involvement of DNA methylation reprogramming, involving the RdDM pathway, in transition to a heritable memory state. |
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ISSN: | 2041-1723 2041-1723 |
DOI: | 10.1038/s41467-020-16036-8 |