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Urotensin II receptor determines prognosis of bladder cancer regulating cell motility/invasion
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نویسنده
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franco r. ,zappavigna s. ,gigantino v. ,luce a. ,cantile m. ,cerrone m. ,facchini g. ,perdonà s. ,pignata s. ,di lorenzo g. ,chieffi s. ,vitale g. ,de sio m. ,sgambato a. ,botti g. ,yousif a.m. ,novellino e. ,grieco p. ,caraglia m.
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منبع
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journal of experimental and clinical cancer research - 2014 - دوره : 33 - شماره : 1
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چکیده
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Background: non muscle invasive bladder transitional cancer (nmibc) and muscle invasive bladder transitional cancer (mibc)/invasive have different gene profile and clinical course. nmibc prognosis is not completely predictable,since the relapse rate is higher than 20%,even in the form of mibc. the aim of this study is to evaluate if utr expression can discriminate between nmibc and mibc and predict the risk of relapses in nmibcs. methods. we have investigated upon urotensin-ii (uii) receptor (utr) expression in vivo in 159 patients affected by nmibc. the biological role of utr was also investigated in vitro. utr expression was evaluated in a tissue-micro-array,consisting of normal,nmibc and invasive btcc samples. results: utr discriminated between nmibc and mibc and showed a significant correlation between low utr expression and shorter disease free survival in nmibc. the superagonist upg84 induced growth suppression at nm concentrations on 3/4 cell lines. bladder cancer cell treatment with the antagonist urantide or the knock-down of utr with a specific shrna significantly blocked both the motility and invasion of bladder cancer cells. conclusions: the evaluation of utr expression can discriminate between nmibc at high and low risk of relapse. moreover,our data suggest that utr is involved in the regulation of motility,invasion and proliferation of bladder cancer cells. high utr expression is an independent prognostic factor of good prognosis for nmibc regulating motility and invasion of bladder cancer cells. © 2014franco et al.; licensee biomed central ltd.
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کلیدواژه
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Bladder cancer; Muscle invasive; Non-muscle invasive; Tumor progression; Urotensin-II
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آدرس
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pathology unit,national cancer institute g. pascale,naples, Italy, department of biochemistry,biophysics and general pathology,second university of naples,naples, Italy, pathology unit,national cancer institute g. pascale,naples, Italy, department of biochemistry,biophysics and general pathology,second university of naples,naples, Italy, pathology unit,national cancer institute g. pascale,naples, Italy, pathology unit,national cancer institute g. pascale,naples, Italy, urogynechologic oncology unit,national cancer institute g. pascale,naples, Italy, urogynechologic oncology unit,national cancer institute g. pascale,naples, Italy, urogynechologic oncology unit,national cancer institute g. pascale,naples, Italy, genitourinary cancer section and rare-cancer center,medical oncology division,university federico ii,naples, Italy, department of experimental medicine,second university of naples,naples, Italy, department of clinical sciences and community health,university of milan,italian auxologic institute irccs,milan, Italy, urology unit,second university of naples,naples, Italy, institute of general pathology,giovanni xxiii cancer research center,catholic university of sacred heart,rome, Italy, pathology unit,national cancer institute g. pascale,naples, Italy, department of pharmacy,university of naples federico ii,naples 80131, Italy, department of pharmacy,university of naples federico ii,naples 80131, Italy, department of pharmacy,university of naples federico ii,naples 80131, Italy, department of biochemistry,biophysics and general pathology,second university of naples,naples, Italy
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Authors
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