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首页> 外文期刊>Annals of diagnostic pathology >Deceiving high-grade cervical dysplasias identified as human papillomavirus non-16 and non-18 types by Invader human papillomavirus assays
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Deceiving high-grade cervical dysplasias identified as human papillomavirus non-16 and non-18 types by Invader human papillomavirus assays

机译:通过Invader人乳头瘤病毒检测将欺骗性宫颈非典型增生鉴别为人乳头瘤病毒非16和非18型

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High-grade cervical intraepithelial lesions (HGCINs) are easily diagnosed by established histologic criteria. However, we encountered problematic cases that are difficult to diagnose because features intermediate between dysplasia and metaplasia are present. p16 and Ki-67 immunostains proved HGCIN in these difficult and unusual cases. Because these are unusual cases of cervical dysplasia, we decided to type the human papillomavirus (HPV) using the Invader HPV test with analyte-specific reagents developed by Third Wave Technologies (Madison, WI, USA) (a new HPV screening assay applicable to tissue and amenable to rapid, sensitive, and specific detection of 14 high- to intermediate-risk HPV types) and a panel of immunostains. Results of these difficult cases are compared with classic HGCIN cases. We searched our pathology files over a period of 16 months for high-grade squamous intraepithelial lesion, cervical intraepithelial neoplasia II, cervical intraepithelial neoplasia III, and p16. To identify cases of difficult HGCIN with features intermediate between dysplasia and metaplasia, we reviewed all surgical cases of HGCIN that required p16 and Ki-67 diagnosis confirmation. Cases of interest were also stained with ProExC. Human papillomavirus screening and HPV 16/18 typing were performed by the Invader assays as described previously. Ten cases of classic HGCIN were easily diagnosed by hypercellularity, significant atypia, mitotic figures, and diffuse staining by p16, Ki67 and ProExC. The Invader assay identified HPV 16 (A9 positive/HPV16 positive) in 7 of 10 cases; the 3 others were A7 positiveot HPV18 (1) and A9 positiveot HPV16 (2). Eight cases of difficult HGCIN were identified. These showed only mild-to-moderate cellularity, a lack of significant atypia, absent-to-rare mitotic figures, and diffuse staining by p16, Ki-67, and ProExC. Human papillomavirus DNA was detected in 5 of 8 cases: only 1 was A9 positive/HPV16 positive, 1 was A5/A6 positive, 1 was A7 positiveot HPV18, and 2 were A9 positiveot HPV16. Three remaining cases demonstrated sufficient DNA to be analyzed by the Invader assay, but results were negative. This is a poorly recognized unusual group of cervical HGCIN with features intermediate between dysplasia and metaplasia that is easily confused by histologic examination. Immunostains prove the high-grade nature of these lesions, and Invader assay demonstrates association with HPV types other than 16/18 (ie, other HPV types detected by Invader assay). In this study, we present an unusual group of cases of high-grade dysplasia, not recognized by hematoxylin and eosin but identified by Ki67 and P16. It is very important to emphasize that this unusual group of high-grade dysplasias is associated with high-risk HPV but with types other than 16/18.
机译:通过建立的组织学标准可轻松诊断出高度宫颈上皮内病变(HGCIN)。但是,我们遇到了难以诊断的问题病例,因为存在发育异常和化生之间的中间特征。在这些困难和异常情况下,p16和Ki-67免疫染色证明了HGCIN。由于这些是宫颈不典型增生的异常情况,因此我们决定使用由第三波技术公司(美国威斯康星州麦迪逊市)开发的分析物特异性试剂,使用Invader HPV测试对人乳头瘤病毒(HPV)进行分型(一种适用于组织的新HPV筛查方法并可以快速,灵敏和特异地检测出14种高危至中危HPV类型)和一组免疫印迹。将这些困难案例的结果与经典HGCIN案例进行比较。我们在16个月的时间里搜索了病理学文件,以查找高度鳞状上皮内病变,子宫颈上皮内瘤样变II,子宫颈上皮内瘤样变III和p16。为了鉴定具有在异型增生和化生之间的特征的困难HGCIN病例,我们回顾了所有需要p16和Ki-67诊断确认的HGCIN外科病例。感兴趣的病例也用ProExC染色。如先前所述,通过Invader测定法进行人乳头瘤病毒的筛选和HPV 16/18分型。十例经典的HGCIN可以通过细胞过多,明显的异型性,有丝分裂图形以及通过p16,Ki67和ProExC进行的弥漫性染色轻松诊断。入侵者试验在10例病例中的7例中鉴定出HPV 16(A9阳性/ HPV16阳性)。其他3个分别是A7阳性/非HPV18(1)和A9阳性/非HPV16(2)。确定了八例困难的HGCIN。这些仅显示轻度至中度的细胞性,缺乏明显的异型性,缺乏至罕见的有丝分裂图以及通过p16,Ki-67和ProExC的弥散染色。 8例中有5例检测到人乳头瘤病毒DNA:只有1例是A9阳性/ HPV16阳性,1例是A5 / A6阳性,1例是A7阳性/不是HPV18,2例是A9阳性/不是HPV16。剩下的三例表明有足够的DNA可通过Invader分析进行分析,但结果为阴性。这是一个公认的宫颈HGCIN异常组,具有异常的增生和化生之间的特征,很容易被组织学检查混淆。免疫染色证明了这些病变的高等级性质,并且Invader分析表明与16/18以外的HPV类型相关(即,其他通过Invader分析检测到的HPV类型)。在这项研究中,我们提出了一组异常的异常增生异常病例,未被苏木精和曙红识别,但由Ki67和P16识别。需要特别强调的是,这种异常的高度异常增生与高危型HPV有关,但与16/18以外的类型有关。

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