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Identification of Abundant and Evolutionarily Conserved Opioid Receptor Circular RNAs in the Nervous System Modulated by Morphine. | LitMetric

Identification of Abundant and Evolutionarily Conserved Opioid Receptor Circular RNAs in the Nervous System Modulated by Morphine.

Mol Pharmacol

Departments of Anesthesiology and Critical Care Medicine (T.I., R.W., G.W.F.) and Neurology (G.W.P., Y.-X.P.), and Molecular Pharmacology Program (R.S., I.D., A.H., V.L.R., J.X., G.W.P.), Memorial Sloan-Kettering Cancer Center, New York, New York

Published: August 2019

AI Article Synopsis

  • Circular RNAs (circRNAs) are unique RNA molecules generated by backsplicing, and their functions remain largely unknown, but they have been found in opioid receptor genes across various species.
  • Research demonstrated that circRNAs, like circOprm1, are present in the brains and spinal cords of mice, rats, and humans, indicating evolutionary conservation and resistance to degradation.
  • Chronic morphine exposure significantly raises the levels of certain circRNAs in the brain, hinting at their potential involvement in the mechanisms of opioid tolerance through interactions with microRNAs.

Article Abstract

Circular RNAs (circRNAs) are a distinct category of single-stranded, covalently closed RNAs formed by backsplicing. The functions of circRNAs are incompletely known and are under active investigation. Here, we report that in addition to traditional linear mRNAs (linRNA), mouse, rat, and human opioid receptor genes generate exonic circRNA isoforms. Using standard molecular biologic methods, circRNAs (circOprm1) were detected in RNAs of rodent and human brains and spinal cords, as well as human neuroblastoma cells, suggesting evolutionary conservation. Sequencing confirmed backsplicing using canonical splice sites. circRNAs were sense-stranded circRNAs resistant to RNase R digestion. The relative abundance of circRNA to linRNA determined by quantitative reverse transcription polymerase chain reaction varied among mouse brain regions, with circRNA isoforms predominating in rostral structures and less abundant in brain stem. Chronic morphine exposure in mice increased brain circe2.3 and circOprm1.e2.e3.e4(302) levels by 1.5- to 1.6-fold relative to linRNA. Sequence analysis predicted numerous microRNA binding sites within circRNA sequences, suggesting a potential role in microRNA sequestration through sponging. In addition, we observed that other opioid receptor genes including , , and nociceptin receptor genes produced similar circRNAs. In conclusion, all members of the opioid receptor gene family express circRNAs, with circRNA levels exceeding those of linear forms in some regions. SIGNIFICANCE STATEMENT: The modulation of circular RNA (circRNA) expression by morphine, coupled with the high abundance and existence of potential miRNA binding sites with circRNA sequences suggests the potential role of circRNAs in chronic opioid effects such as tolerance.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6666384PMC
http://dx.doi.org/10.1124/mol.118.113977DOI Listing

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