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鳞状细胞癌中缺氧与金属硫蛋白蛋白表达的临床研究

A clinical study of hypoxia and metallothionein protein expression in squamous cell carcinomas.

作者信息

Raleigh J A, Chou S C, Calkins-Adams D P, Ballenger C A, Novotny D B, Varia M A

机构信息

Department of Radiation Oncology, University of North Carolina School of Medicine, Chapel Hill 27599, USA.

出版信息

Clin Cancer Res. 2000 Mar;6(3):855-62.

Abstract

The objective was to discover whether the oxygen-regulated protein, metallothionein, is expressed in the hypoxic cells of squamous cell carcinomas. Twenty patients with squamous cell carcinoma of the uterine cervix or head and neck were infused with a solution of the hypoxia marker, pimonidazole hydrochloride, at a dose of 0.5 g/m2. The following day, biopsies were collected, formalin fixed, paraffin embedded, and sectioned at 4 microm. Sections from each biopsy were immunostained for pimonidazole binding, metallothioneins I and II, involucrin, and proliferating cell nuclear antigen. A total of 84 biopsies were analyzed. Sixty-four of 84 biopsy sections contained hypoxia. Of the hypoxia-containing sections, 43 of 64 or 67% showed no microregional overlap between hypoxia and metallothionein; 7 of 64 showed overlap; and 14 of 64 showed a combination of overlap and no overlap. On a tumor-by-tumor basis, 5 of 7 head and neck and 7 of 13 cervix tumors showed no overlap between metallothionein and hypoxia at the microregional level. Ranges for the percentage of the area of hypoxia in head and neck (<0.9 to 17%) and cervix (<0.1 to 14%) tumors were similar. In the hypoxia-containing sections, immunostaining for involucrin, a molecular marker for differentiation, overlapped with that for hypoxia in 82% of the cases. The majority of hypoxic cells in squamous cell carcinomas do not express metallothionein protein, although metallothionein is induced by hypoxia in human tumor cells in vitro. Hypoxic cells in human tumors tend to be in regions immunostaining for involucrin, and it seems possible that differentiation of hypoxic cells in squamous cell carcinomas might affect metallothionein I and II expression.

摘要

目的是探究氧调节蛋白金属硫蛋白是否在鳞状细胞癌的缺氧细胞中表达。20例子宫颈或头颈部鳞状细胞癌患者被输注了剂量为0.5 g/m²的缺氧标志物盐酸匹莫硝唑溶液。第二天,收集活检组织,用福尔马林固定,石蜡包埋,并切成4微米厚的切片。对每个活检组织的切片进行免疫染色,检测匹莫硝唑结合、金属硫蛋白I和II、内披蛋白以及增殖细胞核抗原。共分析了84个活检组织。84个活检切片中有64个含有缺氧区域。在含有缺氧区域的切片中,64个中有43个(67%)显示缺氧区域与金属硫蛋白之间无微观区域重叠;64个中有7个显示有重叠;64个中有14个显示既有重叠又有不重叠的情况。在逐个肿瘤分析中,7例头颈部肿瘤中有5例以及13例子宫颈肿瘤中有7例在微观区域水平上显示金属硫蛋白与缺氧之间无重叠。头颈部肿瘤(<0.9%至17%)和子宫颈肿瘤(<0.1%至14%)中缺氧区域面积的百分比范围相似。在含有缺氧区域的切片中,作为分化分子标志物的内披蛋白免疫染色在82%的病例中与缺氧区域重叠。鳞状细胞癌中的大多数缺氧细胞不表达金属硫蛋白,尽管金属硫蛋白在体外人肿瘤细胞中可被缺氧诱导。人类肿瘤中的缺氧细胞往往位于对内披蛋白免疫染色的区域,鳞状细胞癌中缺氧细胞的分化似乎可能影响金属硫蛋白I和II的表达。

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