Chronic cytoprotection: pentadecapeptide BPC 157, ranitidine and propranolol prevent, attenuate and reverse the gastric lesions appearance in chronic alcohol drinking rats.
Prkacin. I I; Aralica. G G; Perovic. D D; Separovic. J J; Gjurasin. M M; Lovric-Bencic. M M; Stancic-Rokotov. D D; Ziger. T T; Anic. T T; Sikiric. P P; Seiwerth. S S; Staresinic. M M; Mise. S S; Rotkvic. I I; Jagic. V V; Rucman. R R; Petek. M M; Turkovic. B B; Marovic. A A; Sjekavica. I I; Sebecic. B B; Boban-Blagaic. A A; Ivasovic. Z Z
Key Findings
- BPC‑157 given prophylactically prevents gastric lesions in chronic alcohol‑drinking rats.
- Ranitidine and propranolol show similar preventive and therapeutic effects on stomach ulcers.
- Therapeutic dosing of BPC‑157 can reverse existing gastric lesions and also improves liver health and portal hypertension in this model.
Practical Outcomes
- For biohackers, BPC‑157 appears to act as a gut‑protective agent against chronic alcohol‑induced damage, suggesting it could be used as a preventive supplement for heavy drinkers. However, the evidence is limited to animal studies, so human dosing and safety are not established. If considering use, start at very low microgram doses and consult a healthcare professional.
Summary
In rats that drank alcohol for months, giving the peptide BPC‑157 (or the drugs ranitidine and propranolol) either before, during, or after the drinking stopped stomach ulcers from forming and even healed existing damage. The peptide also helped protect the liver and lower portal pressure, while the other drugs mainly helped the stomach.
Abstract
Unlike severe gastric damage acutely induced by ethanol administration in rat, the ulcerogenic effect of chronic alcohol administration (3.03 g/kg b.w. or 7.28 g/kg b.w.) given in drinking water, producing liver lesions and portal hypertension, is far less investigated. Therefore, focus was on the antiulcer effect of the gastric pentadecapeptide BPC 157, GEPPPGKPADDAGLV, M.W. 1419, known to have a beneficial effect in variety of gastrointestinal lesions models (10 microg or 10 ng/kg b.w. i.p. or i.g.), ranitidine (10 mg/kg b.w. i.g.) and propranol (10 mg/kg b.w. i.g.) or saline (5 ml/kg b.w. i.p./i.g.; control). They were given once daily (1) throughout 10 days preceding alcohol consumption, (2) since beginning of alcohol drinking till the end of the study, (3) throughout the last month of alcohol consumption, 2 months after alcohol drinking had been initiated. Gastric lesions were assessed, at the end of 3 months drinking [(1), (2)] or with respect to therapeutic effect of medication before medication or at the end of therapy. Pentadecapeptide BPC 157, ranitidine and propranolol may prevent gastric lesion development if given prophylactically, before alcohol drinking. Likewise, they attenuate the lesion appearance given once daily throughout the drinking period. Importantly, when given therapeutically, they may antagonize otherwise pertinent lesion presence in stomach mucosa of the drinking rats. Thus, these results demonstrate that pentadecapeptide BPC 157, ranitidine and propranol may prevent, attenuate or reverse the gastric lesions appearance in chronically alcohol drinking rats, and may be used for further therapy, while the other studies showed that their effect (except to ranitidine) is parallel with their beneficial effect on liver lesion and portal hypertension.
Study Information
pubmed
2001
10.1016/s0928-4257(01)00041-9