4.4 Article

Morphine treatment is associated with diminished telomere length together with down-regulated TERT and TERF2 mRNA levels

Journal

DRUG AND ALCOHOL DEPENDENCE
Volume 227, Issue -, Pages -

Publisher

ELSEVIER IRELAND LTD
DOI: 10.1016/j.drugalcdep.2021.108982

Keywords

Telomerase; Morphine; hTERT; TERF2

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This study found that the mRNA levels of hTERT and TERF2 in cells treated with morphine decrease with increasing exposure time, but this alteration is reversible when morphine is removed from the culture medium. Additionally, there was no reduction in the relative expression of hTERT and TERF2 in cells co-treated with N-acetyl cysteine (NAC) and morphine.
Background: Drug dependence promotes accelerated aging and higher mortality compare with the general population. Telomere length is a biomarker of determination of cellular aging. Telomere attrition has been re -ported in heroin dependent patients. To investigate whether telomere length is affected by morphine or not, the expressions of hTERT and TERF2 in morphine treated human SH-SY5Y cells were determined and compared with untreated cells. Methods: The SH-SY5Y cells were treated with 1 and 5 mu M concentrations of morphine for different exposure times (1d, 2d, 3d, 7d and 60 days). The mRNA levels of hTERT and TERF2 were determined using quantitative real-time RCR. The relative telomere length was measured as the ratio of telomere/36B4. Results: The hTERT and TERF2 mRNA levels were down regulated in morphine treated cells as a function of exposure duration. These alterations were reversible if morphine was removed from the culture medium. No reduction in the relative expression of hTERT and TERF2 in the cells exposed to N-acetyl cysteine (NAC) plus morphine was observed. In the SH-SY5Y cells treated by 5 mu M morphine for 60 consecutive days, the hTERT and TERF2 mRNA levels and relative telomere lengths remarkably decreased. Conclusions: Reversible alteration of mRNA levels by removing morphine from culture medium, and effect of NAC in co-treatment of morphine plus NAC, emphasize the role of reactive oxygen species in down-regulation of the expression of hTERT and TERF2 by morphine. Telomere attrition in morphine treated cells is a consequence of down-regulation of the expression of hTERT and TERF2.

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