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Publication : Noncanonical genomic imprinting in the monoamine system determines naturalistic foraging and brain-adrenal axis functions.

First Author  Bonthuis PJ Year  2022
Journal  Cell Rep Volume  38
Issue  10 Pages  110500
PubMed ID  35263575 Mgi Jnum  J:324028
Mgi Id  MGI:7266237 Doi  10.1016/j.celrep.2022.110500
Citation  Bonthuis PJ, et al. (2022) Noncanonical genomic imprinting in the monoamine system determines naturalistic foraging and brain-adrenal axis functions. Cell Rep 38(10):110500
abstractText  Noncanonical genomic imprinting can cause biased expression of one parental allele in a tissue; however, the functional relevance of such biases is unclear. To investigate ethological roles for noncanonical imprinting in dopa decarboxylase (Ddc) and tyrosine hydroxylase (Th), we use machine learning to decompose naturalistic foraging in maternal and paternal allele mutant heterozygous mice. We uncover distinct roles for the maternal versus paternal alleles on foraging, where maternal alleles affect sons while daughters are under paternal allelic control. Each parental allele controls specific action sequences reflecting decisions in naive or familiar contexts. The maternal Ddc allele is preferentially expressed in subsets of hypothalamic GABAergic neurons, while the paternal allele predominates in subsets of adrenal cells. Each Ddc allele affects distinct molecular and endocrine components of the brain-adrenal axis. Thus, monoaminergic noncanonical imprinting has ethological roles in foraging and endocrine functions and operates by affecting discrete subsets of cells.
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