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Chronic periglandular inflammation on prostate needle biopsy does not increase the likelihood of cancer on subsequent biopsy.

机译:前列腺穿刺活检的慢性周围性炎症不会增加随后进行活检的可能性。

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PURPOSE: Recent literature suggests a role for chronic inflammation in the development of prostate cancer. We investigated the association of chronic periglandular inflammation on prostate needle biopsy with subsequent prostate cancer development and clinical disease features at presentation. METHODS: Six hundred fifty-five patients were abstracted from a prostateeedle biopsy registry from Brigham and Women's Hospital presenting with prostate-specific antigen (PSA) > 4 ng/mL or abnormal digital rectal examination (DRE) between the years 1990 and 2004. DRE, PSA, PSA density, prostate volume, histology, and age were analyzed to identify clinical and pathologic associations with inflammation. Chronic inflammation was defined as an inflammatory cell infiltrate composed predominately of lymphocytes in a periglandular distribution. A subset of patients (n = 308) with follow-up biopsy results were used to identify if prostate inflammation predicted development of prostate cancer. RESULTS: Modeling performed based on 4 biopsy samples revealed prostate volume (P < .001) and DRE (P = .02) as significant predictors of inflammation; DRE lost significance in models accounting for volume. Kaplan-Meier analysis demonstrated inflammation does not predict subsequent prostate cancer (P = .2). Cox models with the same endpoint show inflammation at initial biopsy (P = .3), inflammation at last biopsy (P = .4), and inflammation on any previous biopsy (P = .08) are not associated with time-to-positive biopsy. CONCLUSIONS: Although inflammation on initial and subsequent biopsy does not predict prostate cancer in this cohort, we cannot dismiss its role in prostate cancer pathogenesis. Additional research is necessary to explore the relationship between prostate inflammation and prostate cancer development.
机译:目的:最近的文献表明慢性炎症在前列腺癌的发展中起作用。我们介绍了前列腺穿刺活检中慢性牙周炎与随后的前列腺癌发展和临床疾病特征的关系。方法:从1990年至2004年之间,从百老汇妇女医院的前列腺/针头活检注册表中提取了655例患者,这些患者的前列腺特异性抗原(PSA)> 4 ng / mL或直肠指检异常(DRE)分析DRE,PSA,PSA密度,前列腺体积,组织学和年龄,以鉴定与炎症的临床和病理学关联。慢性炎症被定义为炎性细胞浸润,主要由沿周缘分布的淋巴细胞组成。一组具有随访活检结果的患者(n = 308)被用于确定前列腺炎症是否预示着前列腺癌的发展。结果:根据4个活检样本进行的建模显示,前列腺体积(P <.001)和DRE(P = .02)是炎症的重要预测因子。 DRE在占体积的模型中失去了重要性。 Kaplan-Meier分析表明炎症不能预测随后的前列腺癌(P = 0.2)。具有相同终点的Cox模型显示,初次活检时发炎(P = .3),最后一次活检时发炎(P = .4),以及之前任何活检中的发炎(P = .08)与阳性反应时间无关活检。结论:尽管在最初和随后的活检中炎症不能预测该人群的前列腺癌,但我们不能忽视其在前列腺癌发病机理中的作用。有必要进行其他研究来探讨前列腺炎症与前列腺癌发展之间的关系。

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