Benzofuran Iboga‐Analogs Modulate Nociception and Inflammation in an Acute Mouse Pain Model

Author:

Bhattacharya Tuhin1,Gupta Abhishek2,Gupta Shalini2,Saha Samrat1,Ghosh Shatabdi1,Shireen Zofa1,Dey Sanjit1,Sinha Surajit2ORCID

Affiliation:

1. Department of Physiology University of Calcutta 92 APC Road West Bengal Kolkata 70009 India

2. School of Applied and Interdisciplinary Sciences Indian Association for the Cultivation of Science 2A Raja S.C. Mullick Road West Bengal Kolkata 700032 India

Abstract

AbstractPain management following acute injury or post‐operative procedures is highly necessary for proper recovery and quality of life. Opioids and non‐steroidal anti‐inflammatory drugs (NSAIDS) have been used for this purpose, but opioids cause addiction and withdrawal symptoms whereas NSAIDS have several systemic toxicities. Derivatives of the naturally occurring iboga alkaloids have previously shown promising behavior in anti‐addiction of morphine by virtue of their interaction with opioid receptors. On this frontier, four benzofuran analogs of the iboga family have been synthesized and their analgesic effects have been studied in formalin induced acute pain model in male Swiss albino mice at 30 mg/kg of body weight dose administered intraperitoneally. The antioxidant, anti‐inflammatory and neuro‐modulatory effects of the analogs were analyzed. Reversal of tail flick latency, restricted locomotion and anxiogenic behavior were observed in iboga alcohol, primary amide and secondary amide. Local neuroinflammatory mediators’ substance P, calcitonin gene related peptide, cyclooxygenase‐2 and p65 were significantly decreased whereas the depletion of brain derived neurotrophic factor and glia derived neurotrophic factor was overturned on iboga analog treatment. Behavioral patterns after oral administration of the best analog were also analyzed. Taken together, these results show that the iboga family of alkaloid has huge potential in pain management.

Publisher

Wiley

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