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骨桥蛋白在多种肿瘤组织学类型中的蛋白表达与病理分期的相关性。

Correlation of osteopontin protein expression and pathological stage across a wide variety of tumor histologies.

作者信息

Coppola Domenico, Szabo Marianna, Boulware David, Muraca Patrick, Alsarraj Marwan, Chambers Ann F, Yeatman Timothy J

机构信息

Department of Pathology, University of South Florida College of Medicine, Tampa, Florida, USA.

出版信息

Clin Cancer Res. 2004 Jan 1;10(1 Pt 1):184-90. doi: 10.1158/1078-0432.ccr-1405-2.

Abstract

PURPOSE

Osteopontin (OPN) is an integrin-binding protein overexpressed in various experimental models of malignancy and appears to be involved in tumorigenesis and metastasis. Although various studies have assessed OPN protein levels in several tumor types, a broad survey of OPN expression in human neoplasia under the same experimental conditions has not been carried out.

EXPERIMENTAL DESIGN

We used immunohistochemistry to detect OPN in a selection of 350 human tumors and 113 normal tissues, from a variety of body sites, using stage-oriented human cancer tissue arrays. Tumors included malignancies from breast (26), ovary (22), endometrium (14), esophagus (10), stomach (11), pancreas (16), bile duct (1), liver (9), colon (20), kidney (53), bladder (33), prostate (28), head and neck (60), salivary glands (14), lung (17), skin (6), and brain (10).

RESULTS

High cytoplasmic OPN staining was observed in 100% of gastric carcinomas, 85% of colorectal carcinomas, 82% of transitional cell carcinomas of the renal pelvis, 81% of pancreatic carcinomas, 72% of renal cell carcinomas, 71% of lung and endometrial carcinomas, 70% of esophageal carcinomas, 58% of squamous cell carcinomas of the head and neck, and 59% of ovarian carcinomas. Although OPN expression was identified in a good number of bladder, prostate, and brain tumors, the majority of 6 skin cancers, 11 of 14 salivary gland cancers, 2 thyroid carcinomas, and 23 of 26 breast cancers revealed low OPN positivity or were negative. When considering all sites, OPN expression significantly correlated with tumor stage (Spearman's correlation coefficient, P = 0.0002). OPN score and stage were also significantly correlated for specific cancer sites including bladder (P = 0.01), colon (P = 0.004), kidney (P = 0.0001), larynx (P = 0.035), mouth (P = 0.046), and salivary gland (P = 0.011).

CONCLUSIONS

This study reports the broad distribution of OPN in human tumors from different body sites, suggesting involvement of this protein in tumor formation. The strong correlation between pathological stage and OPN across multiple tumor types suggests a role for OPN in tumor progression.

摘要

目的

骨桥蛋白(OPN)是一种整合素结合蛋白,在多种恶性肿瘤实验模型中过度表达,似乎参与肿瘤发生和转移。尽管多项研究评估了几种肿瘤类型中OPN蛋白水平,但尚未在相同实验条件下对人类肿瘤中OPN表达进行广泛调查。

实验设计

我们使用免疫组织化学方法,通过面向阶段的人类癌症组织芯片,检测了来自350例人类肿瘤和113例正常组织(来自身体不同部位)中的OPN。肿瘤包括来自乳腺(26例)、卵巢(22例)、子宫内膜(14例)、食管(10例)、胃(11例)、胰腺(16例)、胆管(1例)、肝脏(9例)、结肠(20例)、肾脏(53例)、膀胱(33例)、前列腺(28例)、头颈部(60例)、唾液腺(14例)、肺(17例)、皮肤(6例)和脑(10例)的恶性肿瘤。

结果

在100%的胃癌、85%的结直肠癌、82%的肾盂移行细胞癌、81%的胰腺癌、72%的肾细胞癌、71%的肺癌和子宫内膜癌、70%的食管癌、58%的头颈部鳞状细胞癌以及59%的卵巢癌中观察到高细胞质OPN染色。尽管在大量膀胱、前列腺和脑肿瘤中发现了OPN表达,但6例皮肤癌中的大多数、14例唾液腺癌中的11例、2例甲状腺癌以及26例乳腺癌中的23例显示低OPN阳性或阴性。考虑所有部位时,OPN表达与肿瘤分期显著相关(Spearman相关系数,P = 0.0002)。OPN评分与包括膀胱(P = 0.01)、结肠(P = 0.004)、肾脏(P = 0.0001)、喉(P = 0.035)、口腔(P = 0.046)和唾液腺(P = 0.011)在内的特定癌症部位的分期也显著相关。

结论

本研究报告了OPN在来自不同身体部位的人类肿瘤中的广泛分布,表明该蛋白参与肿瘤形成。多种肿瘤类型中病理分期与OPN之间的强相关性表明OPN在肿瘤进展中起作用。

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