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侵袭性宫颈癌及与侵袭性疾病相关的上皮内病变中FHIT表达缺失。

Loss of fhit expression in invasive cervical carcinomas and intraepithelial lesions associated with invasive disease.

作者信息

Connolly D C, Greenspan D L, Wu R, Ren X, Dunn R L, Shah K V, Jones R W, Bosch F X, Muñoz N, Cho K R

机构信息

Department of Pathology, The University of Michigan Medical School, Ann Arbor 48109, USA.

出版信息

Clin Cancer Res. 2000 Sep;6(9):3505-10.

Abstract

Allelic losses involving chromosome 3p are frequently observed in cervical cancers. Deletion mapping studies of primary cervical carcinomas have localized common regions of deletion to 3p14.2 and 3p21. The candidate tumor suppressor gene FHIT has been mapped to 3p14.2, and previous studies have demonstrated reduced or aberrant FHIT transcripts and reduced or absent Fhit protein expression in a large percentage of cervical cancer-derived cell lines and primary cervical carcinomas. To expand these observations to preinvasive cervical epithelial lesions and to determine whether loss of Fhit protein expression might be associated with tumor progression, immunohistochemical methods were used to examine Fhit expression in 95 invasive cervical carcinomas, 33 high-grade squamous intraepithelial lesions (HSILs) associated with concurrent invasive cancer, 38 HSILs unassociated with invasive cancer, 24 low-grade squamous intraepithelial lesions, and 22 normal cervix samples. All normal cervical epithelia and low-grade squamous intraepithelial lesions exhibited diffuse cytoplasmic immunostaining of moderate to strong intensity. Fhit protein expression was markedly reduced or absent in 67 of 95 (71%) invasive cancers, 17 of 33 (52%) HSILs associated with invasive cancer, and 8 of 38 (21%) HSILs without associated invasive cancer. The results confirm that Fhit protein expression is reduced or absent in the majority of cervical carcinomas and suggest that loss of Fhit expression often accompanies cervical tumor progression. Moreover, absent or reduced Fhit protein is observed at a significantly higher frequency in HSILs associated with progression to invasive cancer than in HSILs with unknown risk for progression (P = 0.012). These findings suggest that loss of Fhit expression in HSILs could serve as a useful marker of high-grade preinvasive lesions that have an increased likelihood of progression to invasive carcinoma.

摘要

在宫颈癌中经常观察到涉及3号染色体短臂(3p)的等位基因缺失。对原发性宫颈癌的缺失图谱研究已将常见的缺失区域定位到3p14.2和3p21。候选肿瘤抑制基因FHIT已被定位到3p14.2,先前的研究表明,在大部分源自宫颈癌的细胞系和原发性宫颈癌中,FHIT转录本减少或异常,Fhit蛋白表达降低或缺失。为了将这些观察结果扩展到宫颈上皮内瘤变,并确定Fhit蛋白表达缺失是否可能与肿瘤进展相关,采用免疫组化方法检测了95例浸润性宫颈癌、33例与同期浸润癌相关的高级别鳞状上皮内病变(HSIL)、38例与浸润癌无关的HSIL、24例低级别鳞状上皮内病变以及22例正常宫颈样本中的Fhit表达。所有正常宫颈上皮和低级别鳞状上皮内病变均表现为中等至强强度的弥漫性细胞质免疫染色。在95例浸润性癌中的67例(71%)、与浸润癌相关的33例HSIL中的17例(52%)以及与浸润癌无关的38例HSIL中的8例(21%)中,Fhit蛋白表达明显降低或缺失。结果证实,大多数宫颈癌中Fhit蛋白表达降低或缺失,提示Fhit表达缺失常伴随宫颈肿瘤进展。此外,与进展为浸润癌相关的HSIL中,Fhit蛋白缺失或减少的频率显著高于进展风险未知的HSIL(P = 0.012)。这些发现表明,HSIL中Fhit表达缺失可作为高级别上皮内瘤变进展为浸润癌可能性增加的有用标志物。

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