Differential effects of the tricyclic antidepressant amoxapine on glycine uptake mediated by the recombinant GLYT1 and GLYT2 glycine transporters.

Author: AragónC, GiménezC, López-CorcueraB, NúñezE, VázquezJ

Paper Details 
Original Abstract of the Article :
We examined the effects of nine different tricyclic antidepressant drugs on the glycine uptake mediated by the glycine transporter 1b (GLYT1b) and glycine transporter 2a (GLYT2a) stably expressed in human embryonic kidney 293 cells. Desipramine, imipramine, clomipramine, nomifensine and mianserin ha...See full text at original site
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引用元:
https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1621133/

データ提供:米国国立医学図書館(NLM)

Amoxapine: A Selective Inhibitor of Glycine Transporter 2a

This research explores the effects of tricyclic antidepressant drugs on the activity of glycine transporters, specifically GLYT1b and GLYT2a. The researchers investigated the impact of nine different tricyclic antidepressants on the uptake of glycine mediated by these transporters. They discovered that amoxapine exhibited a selective inhibition of GLYT2a, acting as a much more potent inhibitor of this isoform compared to GLYT1b. The findings suggest that this selective inhibition might play a role in the sedative and psychomotor side effects associated with amoxapine.

Selective Inhibition: A Key to Understanding Side Effects

The study's findings highlight the selective inhibition of GLYT2a by amoxapine. This selectivity is crucial for understanding the drug's potential side effects, particularly the sedative and psychomotor effects observed in some patients. The research provides a valuable link between pharmacological mechanisms and clinical observations, advancing our knowledge of the complex interplay between drug actions and patient responses.

Implications for Drug Development and Patient Care

This study offers valuable insights into the pharmacological mechanisms of amoxapine and its potential implications for patient care. The understanding of the selective inhibition of GLYT2a provides a foundation for developing strategies to mitigate or manage potential side effects. The researchers' findings encourage further research to explore the precise mechanisms of action and clinical implications of this selective inhibition.

Dr. Camel's Conclusion

Think of amoxapine as a desert oasis, offering relief from the mental aridity of depression. This research helps us understand the subtle nuances of this oasis, reminding us that sometimes, even the most refreshing waters can have a slightly calming effect.

Date :
  1. Date Completed 2000-04-18
  2. Date Revised 2018-11-13
Further Info :

Pubmed ID

10694221

DOI: Digital Object Identifier

PMC1621133

Related Literature

SNS
PICO Info
in preparation
Languages

English

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