An Insight about Diclofenac induced hepato-renal toxicity: A Review Article

Khalil, Esraa Mohamed Naguib; Fahmy EL-baroudy, Nabila Hassan; Mahgoub, Laila Ahmed; Nageeb, Mahitab Mohamed

doi:10.21608/zumj.2024.277963.3265

An Insight about Diclofenac induced hepato-renal toxicity: A Review Article

Document Type : Review Articles

Authors

¹ Clinical Pharmacology Department, Faculty of Medicine, Zagazig university

² Clinical pharmacology department faculty of medicine zagazig university

10.21608/zumj.2024.277963.3265

Abstract

Background: Diclofenac is a medication that has received FDA approval for the treatment and management of acute and chronic pain brought on by inflammatory disorders, particularly those that affect the musculoskeletal system. Although diclofenac (DIC) has many beneficial therapeutic uses, it also carries the potential of serious adverse effects, such as kidney damage, liver damage, gastrointestinal problems, and cardiovascular hazards. We aimed to present an Insight about Diclofenac induced hepato-renal toxicity.

Conclusion: Diclofenac is the NSAID most frequently implicated in hepatocellular and renal injury development. Diclofenac sodium damages hepatic and renal tissues by generating malondialdehyde (MDA) and reducing glutathione (GSH) in hepatic tissues. This oxidative stress leads to the secretion of cytochrome c, which in turn activates the caspase cascade and causes hepatocytes to undergo apoptosis. Diclofenac's main harmful mechanism involves mitochondrial oxidative stress and ROS generation. Lysosomal dysfunction and impaired autophagy flux are brought on by intracellular ROS, which prevents the efficient destruction of damaged mitochondria to stop the creation of more ROS. Hepatotoxicity and cellular oxidative stress are made worse by the vicious loop of mitochondrial damage and impaired autophagy.

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