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Comparison of c-met Expression in Ovarian Epithelial Tumors and Normal Epithelia of the Female Reproductive Tract by Quantitative Laser Scan Microscopy

机译:定量激光扫描显微镜比较女性生殖道卵巢上皮肿瘤和正常上皮中c-met的表达

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摘要

The transmembrane tyrosine kinase receptor c-met with its ligand, hepatocyte growth factor/scatter factor (HGF/SF), acts as a mitogen, motogen, and morphogen in many normal epithelia. HGF/SF-met signaling has also been implicated in neoplastic progression and metastasis. In this study, immunofluorescence staining and quantitative laser scanning confocal microscopy were used to measure c-met expression in ovarian surface epithelial tumors from 17 oophorectomy specimens. These specimens were from patients aged 25 to 81 (mean age, 52) and included 10 malignant tumors, 4 borderline tumors, and five benign tumors including a Brenner tumor. For comparison, c-met expression was measured in normal tissues from the same patients, including 4 ovarian surface epithelia, 4 fallopian tube epithelia, 2 endometria, and 3 endocervical epithelia, as well as 3 cases of endometriosis. Relative pixel intensity values of c-met expression ranged from 0.4 in a normal ovarian surface epithelium to 22.3 in a borderline serous tumor. Malignant tumors (mean, 9.6) and borderline tumors (mean, 12.9) had higher average c-met expression levels than normal tissues (mean, 3.6) and endometriosis (mean, 1.8). The expression levels of benign tumors were intermediate (mean, 7.9). Among the normal tissues, c-met expression in fallopian tubes (mean, 8.2; range, 3.4–12.9) was higher than that of the other normal epithelia (mean, 1.6; range, 0.4–4.3). In eight cases where both normal and malignant tissues were sampled, c-met expression was significantly greater in malignant than in normal epithelia (P = 0.01). These findings indicate that c-met plays a role in the biology of the normal tissues examined. They confirm that its expression increases in the malignant progression of ovarian surface epithelial tumors, and suggest that increases comparable to those in frankly malignant carcinomas have already been reached in borderline lesions, ie, early in the neoplastic process.
机译:跨膜酪氨酸激酶受体c-met及其配体肝细胞生长因子/散射因子(HGF / SF)在许多正常上皮细胞中充当有丝分裂原,运动原和形态发生原。 HGF / SF-met信号转导也涉及肿瘤的进展和转移。在这项研究中,使用免疫荧光染色和定量激光扫描共聚焦显微镜从17例卵巢切除术标本中检测c-met在卵巢表面上皮肿瘤中的表达。这些标本来自25至81岁(平均年龄52岁)的患者,包括10例恶性肿瘤,4例交界性肿瘤和5例良性肿瘤,包括Brenner肿瘤。为了比较,在相同患者的正常组织中测量了c-met表达,包括4个卵巢表面上皮,4个输卵管上皮,2个子宫内膜和3个宫颈内膜上皮以及3例子宫内膜异位。 c-met表达的相对像素强度值范围从正常卵巢表面上皮中的0.4到边缘性浆液性肿瘤中的22.3。恶性肿瘤(平均9.6)和交界性肿瘤(平均12.9)的平均c-met表达水平高于正常组织(平均3.6)和子宫内膜异位症(平均1.8)。良性肿瘤的表达水平为中等水平(平均7.9)。在正常组织中,输卵管中的c-met表达(平均值8.2;范围3.4-12.9)高于其他正常上皮组织(平均值1.6;范围0.4-4.3)。在同时采集了正常和恶性组织的八例病例中,恶性肿瘤的c-met表达明显高于正常上皮组织(P = 0.01)。这些发现表明c-met在所检查的正常组织的生物学中起作用。他们证实了其表达在卵巢表面上皮肿瘤的恶性进展中增加,并且表明在边缘性病变中,即在肿瘤形成过程的早期,已经达到了与坦率的恶性癌相当的表达。

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