Sinicrope Frank A, Half Elizabeth, Morris Jeffrey S, Lynch Patrick M, Morrow Jason D, Levin Bernard, Hawk Ernest T, Cohen Deborah S, Ayers Gregory D, Stephens L Clifton
Department of Gastrointestinal Medicine and Nutrition, University of Texas M. D. Anderson Cancer Center, Houston, USA.
Cancer Epidemiol Biomarkers Prev. 2004 Jun;13(6):920-7.
Celecoxib was shown to regress colorectal adenomas in familial adenomatous polyposis (FAP) patients relative to placebo. To address the mechanism of polyp regression, we determined whether celecoxib can modulate cell proliferation, apoptosis, and prostaglandin E(2) (PGE(2)) levels in colorectal epithelia from FAP trial participants and whether such alterations correlate with observed reductions in polyp number.
Colorectal mucosal biopsies were obtained at baseline and on last day of celecoxib (100 or 400 mg twice daily) or placebo administration (6 months). Residual paraffin-embedded adenomas and normal mucosa from the same patients (n = 17) or normal tissue alone (n = 15) were analyzed. Immunoperoxidase staining for Ki-67 was performed and apoptotic cells were identified by their morphology. Ki-67 and apoptotic labeling indices and their ratios were calculated in superficials (s) and nonsuperficial (ns) regions of adenomas and normal mucosa, and baseline to 6-month differences were calculated. PGE(2) levels were analyzed by mass spectroscopy (normal, n = 64; adenoma, n = 56). Biomarkers were analyzed by treatment arm and correlated with previously determined mean percentage reductions in colorectal polyp number.
In adenomas, a reduction in the superficial proliferative activity i.e., Ki-67(s) labeling index, accompanied polyp regression (r = -0.76, P = 0.006). An increase in the apoptotic ratio [i.e., superficial apoptotic index (AI(s))/nonsuperficial apoptotic index (AI(ns))] was found to correlate with reduced polyp counts in that higher apoptotic ratios correlated with better response to celecoxib (r = 0.71, P = 0.004). Furthermore, the AI(s)/Ki-67(s) ratio (r = 0.58, P = 0.026) accompanied polyp regression. In normal mucosa, a trend toward increased AI(s) (r = 0.33, P = 0.053) and polyp regression was found. PGE(2) levels did not significantly correlate with polyp regression. Changes in biomarker levels (baseline to 6 months) were correlated in adenomas and normal mucosa (AI(s), r = 0.29, P = 0.024; AI(ns), r = 0.34, P = 0.009; PGE(2), r = 0.50, P = 0.059) within individual patients.
Suppression of cell proliferation and an increased apoptotic ratio, as well as the ratio of apoptosis to cell proliferation, accompany polyp regression in a chemoprevention trial in FAP patients. These findings suggest potential mechanisms for the efficacy of celecoxib and warrant further study of these biomarkers as intermediate endpoints in FAP patients.
与安慰剂相比,塞来昔布可使家族性腺瘤性息肉病(FAP)患者的大肠腺瘤消退。为探讨息肉消退的机制,我们确定塞来昔布是否能调节FAP试验参与者大肠上皮细胞的增殖、凋亡及前列腺素E2(PGE2)水平,以及这些改变是否与观察到的息肉数量减少相关。
在基线时以及塞来昔布(每日两次,每次100或400 mg)或安慰剂给药(6个月)的最后一天获取大肠黏膜活检标本。分析来自同一患者(n = 17)的残留石蜡包埋腺瘤和正常黏膜或仅正常组织(n = 15)。进行Ki-67免疫过氧化物酶染色,并通过形态学鉴定凋亡细胞。计算腺瘤和正常黏膜浅表(s)和非浅表(ns)区域的Ki-67和凋亡标记指数及其比值,并计算基线至6个月的差异。通过质谱分析PGE2水平(正常,n = 64;腺瘤,n = 56)。按治疗组分析生物标志物,并与先前确定的大肠息肉数量平均减少百分比相关联。
在腺瘤中,浅表增殖活性即Ki-67(s)标记指数的降低伴随着息肉消退(r = -0.76,P = 0.006)。发现凋亡比值[即浅表凋亡指数(AI(s))/非浅表凋亡指数(AI(ns))]的增加与息肉数量减少相关,因为较高的凋亡比值与对塞来昔布的更好反应相关(r = 0.71,P = 0.004)。此外,AI(s)/Ki-67(s)比值(r = 0.58,P = 0.026)伴随着息肉消退。在正常黏膜中,发现AI(s)增加的趋势(r = 0.33,P = 0.053)与息肉消退相关。PGE2水平与息肉消退无显著相关性。个体患者腺瘤和正常黏膜中生物标志物水平的变化(基线至6个月)相关(AI(s),r = 0.29,P = 0.024;AI(ns),r = 0.34,P = 0.009;PGE2,r = 0.50,P = 0.059)。
在FAP患者的化学预防试验中,息肉消退伴随着细胞增殖的抑制、凋亡比值以及凋亡与细胞增殖比值的增加。这些发现提示了塞来昔布疗效的潜在机制,并值得进一步研究这些生物标志物作为FAP患者的中间终点。
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