HPV genotype-specific distribution and attributable risk in cervical intraepithelial neoplasia in a referral population with a history of LSIL.

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS
Sam Ratnam, Dan Jang, Reza Alaghehbandan, Laura Gilbert, Yunwen Xu, Wei Wang, Phillip Andrews, Ashley Green, David J Speicher, Max Chernesky
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引用次数: 0

Abstract

Background and objective: CINtec PLUS and cobas HPV tests (Roche) were previously ascertained for triaging an LSIL referral population [1]. As part of this study, genotype-specific distribution and attributable risk of high-risk (HR)-HPV in cervical intraepithelial neoplasia (CIN) were determined.

Methods: Archived cervical specimens in ThinPrep PreservCyt (Hologic Inc) from the LSIL referral population (n= 533) were genotyped using the Anyplex II HPV HR test (Anyplex, Seegene Inc). Since the study specimens had been in storage in ambient temperature for 31-47 months since collection, Anyplex results were compared with that of the initial cobas testing of fresh specimens to validate the suitability and stability of specimens for the present study.

Results: Overall, Anyplex test was positive in 63% (336/533) vs. 55.7% (297/533) for cobas test. Anyplex test performed identical to cobas test identifying 93.2% (82/88) of ⩾CIN2/adenocarcinoma in situ (AIS). Anyplex test detected genotypes 16/18 in 15.7% (36/230) ⩽CIN1 vs. 45.5% (40/88) ⩾CIN2/AIS; the corresponding figures were 13.5% (31/230) and 45.5% (40/48) for the cobas test. Genotype 16 showed increasing attribution, 13.2% in CIN1, 27.1% in CIN2 and 40% in CIN3/AIS. Of the 12 other high-risk (OHR) types collectively identified by cobas, Anyplex test specifically detected, in decreasing order, genotypes 51, 31, 35, 56, 39, and 45 as the most frequent types, often in multiple-type infections, in 64.8% ⩾CIN2. Regardless, estimated attribution was evident for each of the 12 OHR types in ⩾CIN2. Multiple-type infections were more frequent than single-type infections in all CIN grades.

Conclusions: Attributable risk of all HR-HPV genotypes targeted by both Anyplex and cobas tests was evident in ⩾CIN2/AIS Testing for these genotypes in HPV primary cervical screening and cytology triage could identify those at increased risk of cervical cancer and also be beneficial in the management of LSIL referral populations.

有LSIL病史的转诊人群中宫颈上皮内瘤变的HPV基因型特异性分布和归因风险
背景和目的:CINtec PLUS和cobas HPV检测(罗氏)先前被确定用于诊断LSIL转诊人群[1]。作为本研究的一部分,确定了高危(HR) hpv在宫颈上皮内瘤变(CIN)中的基因型特异性分布和归因风险。方法:使用Anyplex II型人乳头瘤病毒HR检测(Anyplex, Seegene Inc),对来自LSIL转诊人群(n= 533)的ThinPrep PreservCyt (Hologic Inc)存档的宫颈标本进行基因分型。由于研究标本自采集以来已在室温下保存了31-47个月,因此将Anyplex结果与新鲜标本的初始cobas测试结果进行比较,以验证标本对本研究的适用性和稳定性。结果:总体而言,Anyplex试验阳性率为63% (336/533),cobas试验阳性率为55.7%(297/533)。Anyplex测试执行与cobas测试相同,确定了93.2%(82/88)的小于或等于CIN2/原位腺癌(AIS)。Anyplex测试在15.7%(36/230)≤CIN1 vs. 45.5%(40/88)≤CIN2/AIS中检测到16/18基因型;cobas试验的相应数据分别为13.5%(31/230)和45.5%(40/48)。基因型16在CIN1、CIN2和CIN3/AIS中分别增加了13.2%、27.1%和40%的归因。在cobas共同确定的12种其他高风险(OHR)类型中,Anyplex测试以减少的顺序特异性检测到基因型51、31、35、56、39和45是最常见的类型,通常在多型感染中,在64.8%大于或小于CIN2中。无论如何,对于大于或等于CIN2的12种OHR类型中的每一种,估计归因都是明显的。在所有CIN分级中,多型感染均高于单型感染。结论:Anyplex和cobas测试针对的所有HR-HPV基因型的归因风险在小于或小于CIN2/AIS中是明显的,在HPV初级宫颈筛查和细胞学分类中对这些基因型进行测试可以识别那些宫颈癌风险增加的人,并且在LSIL转诊人群的管理中也有益。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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