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2017 | 77 | Suppl.1 |

Tytuł artykułu

NS398 (COX-2 INHIBITOR) potentiates the antidepressant-like effects of MTEP (MGLUR5 ANTAGONIST): Involvement of 5-HT system

Warianty tytułu

Języki publikacji

EN

Abstrakty

EN
INTRODUCTION: Compounds acting via metabotropic glutamate (mGlu) receptors, exhibit antidepressant activity. Moreover, development of depressive-like behavior in mice is accompanied by elevated level of prostaglandins. In our earlier study, augmentation of antidepressant-like effects of MTEP by NS398 was presented. AIM(S): The aim of this research was to verify the involvement of serotoninergic(5-HT) system in this interaction. METHOD(S): C57Bl/6J male mice were co-treated with MTEP(1 mg/kg; i.p.) and NS398 (3 mg/kg; i.p.) for 7 or 14 days. 24 h after last injection, hippocampus(Hp) and prefrontal cortex(pFC) were collected. The tissue 5-HT and 5-HIAA levels were measured using P680 HPLC system(Dionex, Sunnyvale, CA, USA). Data presented as the mean ±SEM, using one-way ANOVA(n=7–9, Newman-Keuls test), p<0.05 was considered as statistically significant. RESULTS: 14 days co-administration of MTEP with NS398 resulted in statistical significant increase (by 48%) of 5-HT level in pFC [p<0.0001], comparing to the 5-HT level observed after 7 days of administration. Similar picture (increase by 47%) was observed in pFC in 5‑HIAA level [p<0.01]. Quite different picture of changes was observed in Hp, as 5‑HT level was significantly decreased (by 36%) between 7 and 14 days of co-administration of both MTEP with NS398 [p<0.01]. 5-HT:5-HIAA turnover in pFC and Hp, comparing 7 vs. 14 days of co-treatment MTEP with NS398, showed no significant changes[ns]. CONCLUSIONS: Our findings revealed that, chronic co‑treatment MTEP with NS398 affects 5‑HT level in examined brain structures of mice. Observed effect was without changes in 5-HT:5-HIAA turnover, between 7 and 14 days of administration, in pFC and HP of C57Bl/6J mice. This kind of modulation of 5-HT system maybe interesting in the field of psychopharmacology. Further studies are necessary to determine the precise mechanism of interaction of mentioned pathways. FINANCIAL SUPPORT: Study supported by grant UMO-2014/13/D/NZ7/00292.

Słowa kluczowe

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-

Rocznik

Tom

77

Numer

Opis fizyczny

p.121-122

Twórcy

  • Department of Neurobiology, Institute of Pharmacology Polish Academy of Sciences, Cracow, Poland
  • Department of Neurobiology, Institute of Pharmacology Polish Academy of Sciences, Cracow, Poland
autor
  • Department of Neuropsychopharmacology, Institute of Pharmacology Polish Academy of Sciences, Cracow, Poland
autor
  • Department of Neurobiology, Institute of Pharmacology Polish Academy of Sciences, Cracow, Poland
  • Department of Pharmacobiology Cracow, Jagiellonian University Medical College, Cracow, Poland
  • Department of Neurobiology, Institute of Pharmacology Polish Academy of Sciences, Cracow, Poland
autor
  • Department of Neurobiology, Institute of Pharmacology Polish Academy of Sciences, Cracow, Poland
  • Department of Pharmacobiology Cracow, Jagiellonian University Medical College, Cracow, Poland
autor
  • Department of Neurobiology, Institute of Pharmacology Polish Academy of Sciences, Cracow, Poland

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Bibliografia

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