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Multiple HPV infections among men who have sex with men engaged in anal cancer screening in Abuja, Nigeria

机译:与在阿布贾,尼日利亚阿布贾接种肛门癌筛查的男性发生性关系的多种HPV感染

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BackgroundAnal precancers and cancers can be detected during screening with high-resolution anoscopy (HRA). The sensitivity of HRA depends on the burden and duration of human papillomavirus (HPV) among those screened as well as anoscopist proficiency, which is highly correlated with prior screening experience. Our objective was to compare the identification and type of HPV and the likelihood of HRA-detected precancer for men who have sex with men (MSM) undergoing their first HRA-screening in Nigeria.MethodsMSM were recruited from an HIV test-and-treat cohort, TRUST/RV368, into a new anal cancer screening program. Anal swabs obtained during screening underwent Ion Torrent next-generation sequencing using barcoded HPV PCR broad-spectrum primers 5+/6+ to detect up to 161 HPVs. All high-risk (HR) HPVs and the most abundant low-risk (LR)-HPVs were evaluated as type-specific infections with some categorized as belonging to a multiple infection. HRA screening results included benign, low-grade squamous intraepithelial lesions (LSIL), or HSIL as detected by cytology or histology. Multivariable logistic regression was used to assess the association of HPV and other cofactors with any SIL.ResultsAmong 342 MSM, 60% were HIV-infected, 89% were under 35 years of age, and 51% had 8 or more years since anal coital debut. Of those with SIL, 89% had LSIL and only 11% had HSIL. Prevalence of any HPV and high-risk (HR)-HPV was 92% and 74%, respectively. The most prevalent genotypes in rank order were HPV6 (31%), HPV16 (23%), HPV42 (20%), HPV11 (18%), HPV45 (18%), and HPV51 (17%). For multiple HR-HPVs, 31% had a single HR-HPV, 32% had 2-3, and 10% had 4 or more. Low-risk HPVs, type 6 and/or 11, were common (42%) and were significantly associated with SIL (adjusted odds ratio [aOR]:1.8, 95% confidence interval [CI]: 1.1–3.1) together with perianal warts (aOR:6.7, 95% CI: 3.3–13.5). In contrast, HR-HPV and multiple HR-HPVs were not significantly associated with SIL (all p?>?0.05).ConclusionsDetection of HSIL was low. Although HR-HPV was abundant, HSIL development also depends on the duration of HR-HPV infections and the anoscopist's level of experience. As our cohort ages and the anoscopist becomes more skilled, detection of HSIL will likely improve.
机译:在筛选时,可以在用高分辨率无影症(HRA)期间检测到BackgroundAnal预癌。 HRA的敏感性取决于筛选的人乳头瘤病毒(HPV)的负担和持续时间以及镜片熟练程度,与先前的筛选经验高度相关。我们的目标是比较HPV的鉴定和类型,以及与在尼日利亚举行的第一次HRA筛查中发生性关系的HPV的识别和类型的人对尼日利亚的第一个黑暗筛查。方法是从艾滋病毒检测和治疗队列中招募的,信任/ rv368,进入新的肛门癌症筛查计划。在筛选在筛选离子血管下一代测序期间获得的肛门拭子,使用条形曲线的HPV PCR宽光谱引物5 + / 6 +检测高达161 HPV。所有高风险(HR)HPV和最丰富的低风险(LR)-HPV被评为特异性感染,其中一些分类为属于多种感染。 HRA筛选结果包括通过细胞学或组织学检测的良性,低级鳞状上皮内病变(LSIL)或HSIL。多变量逻辑回归用于评估HPV和其他辅助因子与任何SIL.Resultsamong 342 MSM的关联,60%是艾滋病毒感染,89%未来35岁,51%以来肛门CoiTIN亮相8年或更长时间。在SIL的那些中,89%的人有LSIL,只有11%的HSIL。任何HPV和高风险(HR)-HPV的患病率分别为92%和74%。等级顺序中最普遍的基因型是HPV6(31%),HPV16(23%),HPV42(20%),HPV11(18%),HPV45(18%)和HPV51(17%)。对于多种HR-HPV,31%具有单个HR-HPV,32%具有2-3,10%有4%以上。低风险HPV,6型和/或11,常见(42%),与SIL显着相关(调整的赔率比[AOR]:1.8,95%置信区间[CI]:1.1-3.1)与肛门疣一起(AOR:6.7,95%CI:3.3-13.5)。相比之下,HR-HPV和多个HR-HPV与SIL显着相关(所有P?> 0.05)。HSIL的抵消很低。虽然HR-HPV丰富,但HSIL开发也取决于HR-HPV感染的持续时间和镜镜的经验水平。随着我们的队员和主动镜头变得更加熟练,慧聪的检测可能会改善。

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