1. Changes in neuronal immunofluorescence in the C- versus N-terminal domains of hnRNP H following D1 dopamine receptor activation
- Author
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Kathryn M. Hixson, Karen K. Szumlinski, Karen Zheng, Neema Yazdani, Kimberly P. Luttik, Benjamin Wolozin, Daniel J. Apicco, Brandon F. Maziuk, Shelley J. Russek, Peter E.A. Ash, Qiu T Ruan, Camron D. Bryant, Jacob A Beierle, and Kristen E. Hokenson
- Subjects
0301 basic medicine ,Psychostimulant use disorder ,RNA-binding protein ,Heterogeneous ribonucleoprotein particle ,Methamphetamine ,Rats, Sprague-Dawley ,Substance Misuse ,0302 clinical medicine ,Cocaine ,Receptors ,Psychology ,5-Tetrahydro-7 ,8-dihydroxy-1-phenyl-1H-3-benzazepine ,Cells, Cultured ,0303 health sciences ,Cultured ,Chemistry ,General Neuroscience ,Dopaminergic ,Cell biology ,Dopamine receptor ,Neurological ,Dopamine Agonists ,Cognitive Sciences ,2,3,4,5-Tetrahydro-7,8-dihydroxy-1-phenyl-1H-3-benzazepine ,medicine.drug ,hnRNP ,Biotechnology ,Cells ,Addiction ,Article ,03 medical and health sciences ,Dopamine receptor D1 ,Dopamine ,Dopamine D1 ,medicine ,Genetics ,Animals ,030304 developmental biology ,Heterogeneous-Nuclear Ribonucleoprotein Group F-H ,Dopaminergic Neurons ,Receptors, Dopamine D1 ,Neurosciences ,RNA binding protein ,Rats ,Amphetamine ,030104 developmental biology ,Sprague-Dawley ,Drug Abuse (NIDA only) ,030217 neurology & neurosurgery ,Immunostaining - Abstract
RNA binding proteins are a diverse class of proteins that regulate all aspects of RNA metabolism. Accumulating studies indicate that heterogeneous nuclear ribonucleoproteins are associated with cellular adaptations in response to drugs of abuse. We recently mapped and validated heterogeneous nuclear ribonucleoprotein H1 (Hnrnph1) as a quantitative trait gene underlying differential behavioral sensitivity to methamphetamine. The molecular mechanisms by which hnRNP H1 alters methamphetamine behaviors are unknown but could involve preand/or post-synaptic changes in protein localization and function. Methamphetamine initiates post-synaptic D1 dopamine receptor signaling indirectly by binding to pre-synaptic dopamine transporters and vesicular monoamine transporters of midbrain dopaminergic neurons which triggers revers e transport and accumulation of dopamine at the synapse. Here, we examined changes in neuronal localization of hnRNP H in primary rat cortical neurons that express dopamine receptors that can be modulated by the D1 or D2 dopamine receptor agonists SKF38393 and (-)-Quinpirole HCl, respectively. Basal immunostaining of hnRNP H was localized primarily to the nucleus. D1 dopamine receptor activation induced an increase in hnRNP H nuclear immunostaining as detected by immunocytochemistry with a C-domain directed antibody containing epitope near the glycine-rich domain but not with an N-domain specific antibody. Although there was no change in hnRNP H protein in the nucleus or cytoplasm, there was a decrease in Hnrnph1 transcript following D1 receptor stimulation. Taken together, these results suggest that D1 receptor activation increases availability of the hnRNP H C-terminal epitope, which could potentially reflect changes in protein-protein interactions. Thus, D1 receptor signaling could represent a key molecular post-synaptic event linking Hnrnph1 polymorphisms to drug-induced behavior.HighlightsWe investigated immunofluorescence and localization of hnRNP H following dopamine receptor activation in primary rat cortical neurons.Activation of D1 dopamine receptor increased nuclear immunofluorescence of the C-terminal domain but not the N-terminal domain of hnRNP H with no change in either nuclear or cytoplasmic levels of hnRNP H protein.D1 dopamine signaling could alter interaction of hnRNP H with other proteins.
- Published
- 2018