Deneysel nonalkolik steatohepatit modelinde genisteinin koruyucu rolü
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Abstract
1. ÖZETOksidatif stres nonalkolik steatohepatit (NASH) patogenezinde rol alan enönemli faktörlerden biridir. Birçok farmakolojik özelliklere sahip bir fitoöstrojenolan genisteinin (4',5, 7-trihydoxyisoflavone) antioksidan ve anti-inflammatuvarHWNLOHUL ROGX÷X ELOLQPHNWHGLU %X oDOÃúPDGD GHQH/VHO RODUDN ROXúWXUXODQ 1$6+PRGHOLQGHJHQLVWHLQLQNRUX/XFXUROÂQÂDUDúWÃUGÃN48 adet erkek Sprague-Dawley rat randomize olarak dört HúLW JUXED D/UÃOGÃ%LULQFLJUXSVDGHFHVWDQGDUWUDW /HPLDOGÃNRQWUROJUXEXJUXS.*UXSSODVHERVHUXPIL]/RORMLNJUXEXJUXSYH¶HLVH/D÷GDQ]HQJLQGL/HW<='DGOLELWXPRODUDNYHULOGL*UXS¶H<='¶HEDúODPDGDQELUJÂQQFHYHWÂPGHQH/süresince 0.2PJNJJÂQ GR]XQGD JHQLVWHLQ VXENXWDQ RODUDN X/JXODQGà JHQLVWHLQ NRUX/XFX *.grup). Grup 4'e dördüncü haftadan sonra iki hafta 0.2 mg/kg/gün dozunda genisteinVXENXWDQRODUDNX/JXODQGÃJHQLVWHLQWHGDYL*7JUXEXKDIWDELWWLNWHQVRQUDtümUDWODU OGÂUÂOG .DQ UQHNOHUL YH NDUDFL÷HU GRNXODUà DOÃQGà $PLQRWUDQVIHUD]ODUSOD]PDYHNDUDFL÷HUPDORQGLDOGHKLG0'$GÂ]H/OHULOoÂOGÂ+LVWRSDWRORMLNRODUDNNDUDFL÷HUGHVWHDWR]EDORQODúPDGHMHQHUDV/RQXLQIODPPDV/RQ0DOORU/FLVLPFL÷LYHfibro]LVGH÷HUOHQGLULOGL$67 YH $/7 GH÷HUOHUL S SOD]PD YH NDUDFL÷HU 0'$ YH SOD]PDTNF-DOID GÂ]H/OHUL S VÃUDVà LOH SODVHER JUXEXQGD NRQWUROgrubundan yüksekti. TGF-EHWD GÂ]H/OHULQGH DQODPOà IDUN /RNWX +LVWRSDWRORMLNolarak steatoz, mm2 GHNL RUWDODPD LQIODPDWXYDU KÂFUH VD/ÃVà YH EDORQODúPDGHMHQHUDV/RQX SODVHER JUXEXQGD NRQWURO JUXEXQD JUH DQODPOà RODUDN /ÂNVHNWL SKHSVLQGH )LEUR]LV YH 0DOORU/ FLVPL VDSWDQPDGà +HP *. KHP GH *7grubunda AST ve ALT düzeyleri (p hepsinGH SOD]PD YH NDUDFL÷HU 0'$düzeyleri ve TNF-DOID GÂ]H/OHUL SODVHER JUXEXQD JUH DQODPOà RODUDN GÂúÂNW SKHSVLQGH+LVWRSDWRORMLNLQFHOHPHGH*.YH*7JUXSODUÃQGDVWHDWR]VÃUDVÃLOHp<0.05 ve <0.01), mm2 deki ortalama inflamatuvar hücre sayÃVà KHU LNL JUXSWDS YH EDORQODúPD GHMHQHUDV/RQX KHU LNL JUXSWD SODVHER JUXEXQD JUHDQODPOÃRODUDNGÂúÂNWÂSonuç: *ÂoO ELU DQWLRNVLGDQ RODQ JHQLVWHLQ GHQH/VHO RODUDN 1$6+ JHOLúLPLQLbelirgin olarak önlemekte, histopatolojik ve biyokimyasal düzelme ile steatohepatitiD]DOWPDNWDGÃUAnahtar kelimeler: 1RQDONROLN VWHDWRKHSDWLW /D÷GDQ ]HQJLQ GL/HW RNVLGDWLI VWUHVgenistein. Oxidative stress is one of the important factors that are playing role in thepathogenesis of nonalcoholic steatohepatitis (NASH). Genistein (4?,5, 7-trihydoxyisoflavone), a phytoestrogen with several pharmacological features, hasalso antioxidant and anti-inflammatuar properties. In the present study, we evaluatedpreventive role of genistein in NASH model induced experimentally.48 Sprague-Dawley rats were divided into four equal groups randomly. Firstgroup received only standart rat chow diet (control group: grup C). Group 2 (groupplacebo), 3 and 4 were given high fat diet (HFD) ad libitum. 0.5 ml serumphysiologic injected daily to placebo group subcutaneously. 0.2 mg/kg/day genisteininjected subcutaneously to group 3 (genistein prevention (GP) group) starting oneday before HFD administration and during the whole experiment. After the fourthweek, genistein at 0.2 mg/kg/day injected subcutaneously to the fourth group(genistein treatment (GT) group). All rats killed after six weeks. Blood samplescollected and tissue samples prepared. Aminotransferases, plasma and livermalondialdehyde (MDA) levels were measured. Steatosis, ballooning degeneration,inflammation, Mallory body and fibrosis in the liver examined histopathologically.AST and ALT levels (p for each <0.001), plasma and liver tissue MDA andplasma TNF-alpha levels (p <0.001, <0.001, <0.01, respectively) were higher inplacebo group than in the control group. TGF-beta levels were comparable in theplacebo and control groups. In histopthological examination, steatosis, inflammatuarcells per mm2 and balloning degeneration were significantly higher in the placebogroup than in the control group (p for each <0.001). There was no fibrosis andMallory body. AST and ALT levels (p for each <0.05), plasma and liver tissueMDA and plasma TNF-alpha levels were significantly lower (p <0.05 for each)either in GP or in GT groups compared to the placebo group. Histopathologically,steatosis (p<0.05 and <0.01 respectively), mean number of inflammatuar cells permm2 (p<0.01 for each) and balloning degeneration (p <0.01 for each) in GP and GTgroups were significantly lower than in the placebo group.In conclusion; genistein, a strong antioxidant agent, not only remarkablyprevents the emergence of NASH, but also attenuates the existing steatohepatitis byimproving the biochemical and histopathological abnormalities.Key words: Nonalcoholic steatohepatitis, high fat diet, oxidative stress, genistein.
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