Fenitoin sýçanlarda tüp mide ameliyatýndan sonra zýmba hattýnýn iyileþmesi için güvenli bir madde midir?

AMAÇ: Tüp mide ameliyatýnýn (SG) en zorlu ve ölümcül komplikasyonu stapler hattýnýn kaçmasýdýr. Stapler hattýnda doku iyileþmesini hýzlandýrmak için birçok ajan kullanýlmasýna raðmen hala etkinliði ve etkinliði konusunda fikir birliði yoktur. Çalýþmanýn amacý, fenitoinin sýçanlarda tüp mide ame-liyatýnýn iyileþme sürecine etkisini belirlemektir.
GEREÇ VE YÖNTEM: Patohistolojik incelemelerin yaný sýra postoperatif 10. günde fenitoinin stabiler hatta patlama basýncý analizine etkisi belirlendi. Fenitoinin VEGF, TGF-β, FGF2 ve p53 genlerinin ekspresyonu üzerindeki moleküler etkisi qRT-PCR ile araþtýrýldý. Ayrýca immünohistokimyasal analiz ile protein seviyesindeki gen ifadeleri belirlendi.
BULGULAR: Rezeke edilen örneklerde intraabdominal kaçak bulgusuna rastlanmadý. Stabil hat patlama basýncý deðerlerinde kontrol ve fenitoin uygulama gruplarý arasýnda istatistiksel olarak anlamlý artýþlar olmuþtur. Patohistolojik sonuçlar, çalýþma grubunun ortalama kollajen skorunun (3.2±0.42) kontrol grubuna (2.3±0.48) göre anlamlý derecede yüksek olduðunu göstermektedir (p=0.003). Ayrýca çalýþma grubunun ortalama epitelizasyon skoru (3.4±0.52) kontrol grubuna göre (2.1±0.57) anlamlý olarak yüksekti (p=0.001). VEGF, TGF-β, FGF2 ve p53 genlerinin mRNA'sý fenitoin verilen grupta önemli ölçüde arttý. Fenitoin kullanýmýnda kontrol grubuna göre yüksek FGF2 protein ekspresyon seviyeleri belirlendi.
SONUÇ: Moleküler çalýþmalar, fenitoinin sýçanlarda SG'yi takiben mide tüpünün iyileþme sürecini artýrabileceðini ve insan mide kaçaklarýnýn önlen-mesi için yeni bir ajan olabileceðini düþündürmektedir.

Is phenytoin a safe agent for staple line recovery after gastric sleeve surgery in rats?

BACKGROUND: The most challenging and mortal complication of gastric sleeve surgery (SG) is staple line leakage. Although many agents have been used for increasing tissue healing on the stapler line, there is still no consensus on its effectiveness and efficacy. The aim of study is to determine the effect of phenytoin on the healing process of gastric sleeve surgery in rats.
METHODS: On the 10th post-operative day, the effects of phenytoin on bursting pressure in the stapler line were evaluated along-side pathohistological examinations. To investigate the molecular impact of phenytoin on the expression of TGF-β, VEGF, FGF2, and p53 genes, quantitative real-time polymerase chain reaction was utilized. In addition, gene expressions at the protein level were deter-mined by immunohistochemical analysis.
RESULTS: No signs of intra-abdominal leakage were observed in the resected samples. A statistically essential extend in stable line bursting pressure measure was observed between the control group and the group treated with phenytoin application. Pathohisto-logical results indicate that the mean score of collagens of the study group (3.2±0.42) was significantly higher than the control group (2.3±0.48) (P=0.003). In addition, the mean epithelization score of the study group (3.4±0.52) was significantly higher than the control group (2.1±0.57) (P=0.001). mRNA of TGFβ, FGF2, VEGF, and p53 genes drastically increased phenytoin treated group. High FGF2 protein expression levels were determined from phenytoin use compared to the control group.
CONCLUSION: Molecular studies suggest that phenytoin may increase the healing process of Gastric sleeve following SG in rats and may become a new agent for the prevention of human gastric leaks.