宫颈癌中脆性组氨酸三联体基因及互补DNA的异常：与人乳头瘤病毒类型的关联。

Abnormalities of fragile histidine triad genomic and complementary DNAs in cervical cancer: association with human papillomavirus type.

作者信息

Muller C Y, O'Boyle J D, Fong K M, Wistuba I I, Biesterveld E, Ahmadian M, Miller D S, Gazdar A F, Minna J D

机构信息

Department of Obstetrics and Gynecology, Hamon Center for Therapeutic Oncology Research, The University of Texas Southwestern Medical Center, Dallas 75235-9032, USA.

出版信息

J Natl Cancer Inst. 1998 Mar 18;90(6):433-9. doi: 10.1093/jnci/90.6.433.

DOI:10.1093/jnci/90.6.433

PMID:9521167

Abstract

BACKGROUND

Chromosome 3p14.2 contains FRA3B, the most active chromosome breakage site in the human genome. The fragile histidine triad (FHIT) gene, a putative tumor suppressor gene, overlaps FRA3B. Human papillomavirus (HPV), a known cofactor in cervical carcinogenesis, can integrate into FRA3B. We examined abnormalities in FHIT and its RNA transcripts in cervical cancer cell lines and tumors. We also investigated the relationship between loss of heterozygosity (LOH) in FHIT/FRA3B and the presence of oncogenic HPV types.

METHODS

Eleven cell lines, 40 tumors (20 fresh and 20 archival), and 10 normal cervical epithelia were examined. Two intragenic polymorphic markers (D3S1300 and D3S4103) and the polymerase chain reaction (PCR) were used to examine FHIT LOH. Reverse transcription-PCR (RT-PCR) analysis and single-strand conformation polymorphism analysis of RT-PCR products were used to characterize FHIT transcripts. Oncogenic HPV types were identified by PCR, using general and type-specific primers.

RESULTS

All normal epithelia, 19 of 20 fresh tumors and nine of 11 cell lines expressed wild-type and, occasionally, exon 8-deleted FHIT transcripts. Additional aberrant FHIT transcripts were seen in nine of 20 fresh tumors and in seven of 11 cell lines. DNA sequencing of the aberrant transcripts revealed a variety of insertions and deletions but no point mutations. Three cell lines also had homozygous FHIT deletions. Oncogenic HPV types (i.e., 16, 18, 31, and 33) were detected in 18 of 20 archival tumors, and, in these tumors, LOH within FHIT was identified in nine of 16 informative cases. HPV 16 was found to be associated with LOH in the FHIT/FRA3B region (P = .041).

CONCLUSION

FHIT/FRA3B is frequently altered in cervical cancer, demonstrating LOH, occasional homozygous deletions, and frequent aberrant transcripts not found in normal epithelia. However, the presence of wild-type transcripts and the lack of protein-altering point mutations raise questions about FHIT's function as a classic tumor suppressor gene in cervical tissue.

摘要

背景

3号染色体p14.2区域包含FRA3B，它是人类基因组中最活跃的染色体断裂位点。脆性组氨酸三联体（FHIT）基因是一种假定的肿瘤抑制基因，与FRA3B重叠。人乳头瘤病毒（HPV）是宫颈癌发生过程中一种已知的辅助因子，可整合到FRA3B中。我们检测了宫颈癌细胞系和肿瘤中FHIT及其RNA转录本的异常情况。我们还研究了FHIT/FRA3B杂合性缺失（LOH）与致癌性HPV类型存在之间的关系。

方法

检测了11个细胞系、40个肿瘤（20个新鲜肿瘤和20个存档肿瘤）以及10个正常宫颈上皮组织。使用两个基因内多态性标记（D3S1300和D3S4103）和聚合酶链反应（PCR）检测FHIT的LOH。采用逆转录PCR（RT-PCR）分析及RT-PCR产物的单链构象多态性分析来鉴定FHIT转录本。使用通用引物和型特异性引物通过PCR鉴定致癌性HPV类型。

结果

所有正常上皮组织、20个新鲜肿瘤中的19个以及11个细胞系中的9个均表达野生型FHIT转录本，偶尔也表达缺失外显子8的FHIT转录本。在20个新鲜肿瘤中的9个以及11个细胞系中的7个中发现了额外的异常FHIT转录本。对异常转录本进行DNA测序发现了多种插入和缺失，但未发现点突变。3个细胞系还存在FHIT纯合缺失。在20个存档肿瘤中的18个中检测到致癌性HPV类型（即16、18、31和33型），在这些肿瘤中，16例信息充分的病例中有9例存在FHIT内的LOH。发现HPV 16与FHIT/FRA3B区域的LOH相关（P = 0.041）。