Labdane diterpenoids as potential anti-inflammatory agents.

Pharmacol Res

Department of Pharmacy, Faculty of Science, National University of Singapore, Block S4A, Level 3, 18 Science Drive 4, 117543, Singapore. Electronic address:

Published: October 2017

AI Article Synopsis

  • The search for new anti-inflammatory agents is complex due to the intricate nature of inflammation and its protective role in the body.
  • Significant research has highlighted labdane diterpenoids as effective in treating various inflammatory diseases, primarily by inhibiting NF-κB activity and modulating pathways related to arachidonic acid and nitric oxide.
  • The article reviews labdane diterpenes identified from 1981 to 2016, focusing on their mechanisms, specific structures like Michael acceptors linked to NF-κB inhibition, and includes discussions on relevant structural studies and clinical findings.

Article Abstract

The search for new anti-inflammatory agents is challenging due to the complexity of the inflammatory process and its role in host defense. Over the past few decades, a significant body of evidence has emerged, supporting the prominent role of labdane diterpenoids in therapeutic interventions of various inflammatory diseases. The anti-inflammatory activity of labdane diterpenoids has been attributed mainly to the inhibition of nuclear factor-κB (NF-κB) activity, the modulation of arachidonic acid (AA) metabolism and the reduction of nitric oxide (NO) production. This article provides extensive coverage of naturally occurring labdane diterpenes, discovered between 1981 and 2016, which have been verified as NF-κB, NO, or AA modulators. Herein, we also discuss the role of Michael acceptor, a common structural feature present in most of the active labdane diterpenes, and its association with NF-κB signaling inhibition. In the cases where a sufficient amount of data exists, structure-activity relationship (SAR) studies and clinical studies performed on the anti-inflammatory labdane diterpenoids are also discussed.

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Source
http://dx.doi.org/10.1016/j.phrs.2017.07.019DOI Listing

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