Modulation of D 3 R Splicing, Signaling, and Expression by D 1 R through PKA→PTB Phosphorylation
The D R and D R receptors functionally and synergistically interact in striatonigral neurons. Dopaminergic denervation turns this interaction antagonistic, which is correlated with a decrement in D nf isoform and an increment in D R membranal expression. The mechanisms of such changes in D R are att...
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Veröffentlicht in: | Biomedicines 2024-01, Vol.12 (1) |
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Hauptverfasser: | , , , , , , , , , |
Format: | Artikel |
Sprache: | eng |
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Zusammenfassung: | The D
R and D
R receptors functionally and synergistically interact in striatonigral neurons. Dopaminergic denervation turns this interaction antagonistic, which is correlated with a decrement in D
nf isoform and an increment in D
R membranal expression. The mechanisms of such changes in D
R are attributed to the dysregulation of the expression of their isoforms. The cause and mechanism of this phenomenon remain unknown. Dopaminergic denervation produces a decrement in D
R and PKA activity; we propose that the lack of phosphorylation of PTB (regulator of alternative splicing) by PKA produces the dysregulation of D
R splicing and changes D
R functionality. By using in silico analysis, we found that D
R mRNA has motifs for PTB binding and, by RIP, co-precipitates with PTB. Moreover, D
R activation via PKA promotes PTB phosphorylation. Acute and 5-day D
R blockade decreases the expression of D
nf mRNA. The 5-day treatment reduces D
R, D
nf, and PTB protein in the cytoplasm and increases D
R in the membrane and PTB in the nucleus. Finally, the blockade of D
R mimics the effect of dopaminergic denervation in D
R and D
R signaling. Thus, our data indicate that through PKA→PTB, D
R modulates D
R splicing, expression, and signaling, which are altered during D
R blockade or the lack of stimulation in dopaminergic denervation. |
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ISSN: | 2227-9059 2227-9059 |