首页> 外文期刊>American journal of clinical pathology. >Up-regulation of plasminogen activator inhibitor-2 is associated with high-risk HPV and grade of cervical lesion at baseline but does not predict outcomes of high-risk HPV infections or incident CIN.
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Up-regulation of plasminogen activator inhibitor-2 is associated with high-risk HPV and grade of cervical lesion at baseline but does not predict outcomes of high-risk HPV infections or incident CIN.

机译:纤溶酶原激活物抑制剂2的上调与高危HPV和基线时宫颈病变的程度有关,但不能预测高危HPV感染或CIN的预后。

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摘要

Protease inhibitor serpin-B2 (plasminogen activator inhibitor-2 [PAI-2]) protects pRb from degradation in human papillomavirus (HPV)-18+ HeLa cells. Our objective was to assess whether the pRb-mediated HPV-suppressive effect of PAI-2 in cancer cell lines has implications in the outcome of HPV infections. Cervical biopsy specimens from 225 women were analyzed for PAI-2 expression to assess its value as a predictor of cervical intraepithelial neoplasia (CIN) grade, high-risk (HR) HPV at baseline, outcomes of HR-HPV infections, and the development of incident CIN. PAI-2 expression increased in parallel with lesion grade. Nuclear PAI-2 expression was significantly related to HR-HPV detection and had a linear relationship with HR-HPV load. PAI-2 expression was of no value in predicting the outcomes of HR-HPV infections. The same was true for PAI-2 as a predictor of surrogate end points (incident CIN 1+, CIN 2+) of progressive disease. PAI-2 expression is up-regulated on transition from CIN 2 to CIN 3. The HR-HPV suppressive effects of PAI-2 were not related to more favorable outcomes of HR-HPV infections or lower risk of disease progression to CIN.
机译:蛋白酶抑制剂serpin-B2(纤溶酶原激活物抑制剂2 [PAI-2])可保护pRb免受人乳头瘤病毒(HPV)-18+ HeLa细胞降解。我们的目的是评估PAI-2在癌细胞系中对pRb介导的HPV抑制作用是否对HPV感染的结果有影响。分析了225名妇女的宫颈活检标本中PAI-2的表达,以评估其作为宫颈上皮内瘤变(CIN)等级,基线高危(HR)HPV,HR-HPV感染结局和发展的预测指标的价值。事件CIN。 PAI-2表达与病变等级平行增加。核PAI-2表达与HR-HPV检测显着相关,并且与HR-HPV负荷呈线性关系。 PAI-2表达对于预测HR-HPV感染的结果没有价值。对于PAI-2,作为进行性疾病的替代终点(事件CIN 1 +,CIN 2+)的预测指标也是如此。从CIN 2过渡到CIN 3时,PAI-2的表达上调。PAI-2的HR-HPV抑制作用与HR-HPV感染更有利的结局或疾病进展为CIN的风险较低无关。

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