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人乳头瘤病毒载量是否为临床有用的预测标志物?一项纵向研究。

Is human papillomavirus viral load a clinically useful predictive marker? A longitudinal study.

机构信息

Cancer Research UK Institute for Cancer Studies, University of Birmingham, Edgbaston, Birmingham, United Kingdom.

出版信息

Cancer Epidemiol Biomarkers Prev. 2010 Mar;19(3):832-7. doi: 10.1158/1055-9965.EPI-09-0838. Epub 2010 Mar 3.

Abstract

BACKGROUND

It has been suggested that in women who test positive for high-risk human papillomavirus (HPV) types, viral load can distinguish women who are at increased risk of cervical neoplasia from those who are not.

METHODS

Quantitative PCR (qPCR) was used to measure HPV copy number in serial samples taken from 60 and 58 young women previously found to have incident cervical HPV16 or HPV18 infections, respectively, using GP5+/GP6+ primers; women provided at least three samples for qPCR testing, at least one of which was positive.

RESULTS

A 10-fold increase in HPV16 or HPV18 copy number was associated with a modestly increased risk of acquiring a cytologic abnormality [HPV16: hazards ratio, 1.76 (95% confidence interval, 1.38-2.25); HPV18: hazards ratio, 1.59 (95% confidence interval, 1.25-2.03)]. However, in most women, copy number increased during follow-up, before decreasing again. In women with a HPV16 infection, the median copy number per 1,000 cells was 7.7 in their first qPCR HPV-positive sample, 1,237 in the sample yielding the maximum copy number, and 7.8 in their last qPCR HPV-positive sample; corresponding copy numbers for women with HPV18 infection were 2.3, 87, and 2.4. Maximum HPV16 and HPV18 copy number did not differ significantly between women who acquired an incident cervical cytologic abnormality and those who did not.

CONCLUSION

Whereas large relative increases in copy number are associated with an increased risk of abnormality, a single measurement of viral load made at an indeterminate point during the natural history of HPV infection does not reliably predict the risk of acquiring cervical neoplasia. Therefore, a single measure of HPV viral load cannot be considered a clinically useful biomarker.

摘要

背景

有研究表明,对于 HPV 高危型阳性的女性,病毒载量可以区分出宫颈癌前病变风险增加的女性和没有增加的女性。

方法

采用 GP5+/GP6+引物,对 60 名和 58 名分别新发现 HPV16 或 HPV18 感染的年轻女性的连续样本进行定量 PCR(qPCR)检测,以测量 HPV 拷贝数;这些女性为 qPCR 检测至少提供了 3 个样本,其中至少有一个样本为阳性。

结果

HPV16 或 HPV18 拷贝数增加 10 倍与细胞学异常发生风险略有增加相关[HPV16:风险比 1.76(95%置信区间,1.38-2.25);HPV18:风险比 1.59(95%置信区间,1.25-2.03)]。然而,在大多数女性中,在再次降低之前,在随访过程中病毒载量会增加。HPV16 感染的女性中,其首次 qPCR HPV 阳性样本的每 1000 个细胞的中位数拷贝数为 7.7,获得最大拷贝数的样本为 1237,最后一次 qPCR HPV 阳性样本为 7.8;HPV18 感染的女性的相应拷贝数为 2.3、87 和 2.4。在获得宫颈细胞学异常的女性和未获得的女性之间,HPV16 和 HPV18 的最大拷贝数没有显著差异。

结论

虽然拷贝数的相对大幅增加与异常风险增加相关,但在 HPV 感染自然史的不确定点进行的单次病毒载量测量不能可靠地预测获得宫颈癌前病变的风险。因此,单次 HPV 病毒载量测量不能被认为是一种有临床意义的生物标志物。

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