Celecoxib-induced gastrointestinal, liver and brain lesions in rats, counteraction by BPC 157 or L-arginine, aggravation by L-NAME.
Drmic. Domagoj D; Kolenc. Danijela D; Ilic. Spomenko S; Bauk. Lara L; Sever. Marko M; Zenko Sever. Anita A; Luetic. Kresimir K; Suran. Jelena J; Seiwerth. Sven S; Sikiric. Predrag P
Key Findings
- Celecoxib at 1 g/kg caused severe gastrointestinal, liver and brain lesions in rats.
- Co‑administration of L‑arginine reduced the celecoxib‑induced damage.
- BPC‑157 (10 µg/kg down to 1 ng/kg) completely prevented the lesions, even when nitric‑oxide production was blocked by L‑NAME.
Practical Outcomes
- BPC‑157 appears to shield the gut, liver and brain from the toxic effects of high‑dose NSAIDs, suggesting it could be used to mitigate NSAID‑related side effects. For biohackers, this hints that low‑dose BPC‑157 might be a protective supplement when taking strong COX‑2 inhibitors, but human dosing and safety are not established yet, so caution and further research are needed.
Summary
In rats, a very high dose of the NSAID celecoxib caused stomach, liver and brain damage, but giving the peptide BPC‑157 (at very low doses) or the amino acid L‑arginine prevented those injuries. Even when the nitric‑oxide system was blocked (with L‑NAME), BPC‑157 still protected the organs.
Abstract
To counteract/reveal celecoxib-induced toxicity and NO system involvement. Celecoxib (1 g/kg b.w. ip) was combined with therapy with stable gastric pentadecapeptide BPC 157 (known to inhibit these lesions, 10 μg/kg, 10 ng/kg, or 1 ng/kg ip) and L-arginine (100 mg/kg ip), as well as NOS blockade [N(G)-nitro-L-arginine methyl ester (L-NAME)] (5 mg/kg ip) given alone and/or combined immediately after celecoxib. Gastrointestinal, liver, and brain lesions and liver enzyme serum values in rats were assessed at 24 h and 48 h thereafter. This high-dose celecoxib administration, as a result of NO system dysfunction, led to gastric, liver, and brain lesions and increased liver enzyme serum values. The L-NAME-induced aggravation of the lesions was notable for gastric lesions, while in liver and brain lesions the beneficial effect of L-arginine was blunted. L-arginine counteracted gastric, liver and brain lesions. These findings support the NO system mechanism(s), both NO system agonization (L-arginine) and NO system antagonization (L-NAME), that on the whole are behind all of these COX phenomena. An even more complete antagonization was identified with BPC 157 (at both 24 h and 48 h). A beneficial effect was evident on all the increasingly negative effects of celecoxib and L-NAME application and in all the BPC 157 groups (L-arginine + BPC 157; L-NAME + BPC 157; L-NAME + L-arginine + BPC 157). Thus, these findings demonstrated that BPC 157 may equally counteract both COX-2 inhibition (counteracting the noxious effects of celecoxib on all lesions) and additional NOS blockade (equally counteracting the noxious effects of celecoxib + L-NAME). BPC 157 and L-arginine alleviate gastrointestinal, liver and brain lesions, redressing NSAIDs' post-surgery application and NO system involvement.
Study Information
pubmed
2017
2017-08-07T00:00:00.000Z
10.3748/wjg.v23.i29.5304
52
45