Campos-Fernandes Jean-Louis, Bastien Laurence, Nicolaiew Nathalie, Robert Grégoire, Terry Stéphane, Vacherot Francis, Salomon Laurent, Allory Yves, Vordos Dimitri, Hoznek Andras, Yiou René, Patard Jean Jacques, Abbou Claude Clément, de la Taille Alexandre
Department of Urology, CHU Mondor, Créteil, France.
Eur Urol. 2009 Mar;55(3):600-6. doi: 10.1016/j.eururo.2008.06.043. Epub 2008 Jun 23.
Prevalence of prostate cancer (PCa) after a negative first extended prostate needle biopsy protocol is unknown.
To evaluate the prevalence of significant PCa in patients who have had a negative first extended prostate biopsy protocol.
DESIGN, SETTING, AND PARTICIPANTS: Between March 2001 and May 2007, 2500 consecutive patients underwent an extended protocol of 21 biopsies. Of 953 patients who had a negative first extended prostate biopsy procedure, 231 patients underwent a second or more set of 21-core biopsies. Indications for repeated biopsies were persistently elevated prostate-specific antigen (PSA), PSA increase during the follow-up, or prior prostatic intraepithelial neoplasia (PIN), or atypical small acinar proliferation (ASAP).
All participants underwent at least two extended prostate needle biopsy protocols.
Clinical and pathologic factors (age, PSA, PSA doubling time, PIN, ASAP, digital rectal exam [DRE]) were analyzed for their ability to predict positive biopsy, and tumour parameters were assessed in patients undergoing radical prostatectomy.
Second, third, and fourth extended 21-sample biopsy procedures yielded a diagnosis of PCa in 18%, 17%, and 14% of patients respectively. Patients with prior PIN had 16% risk of prostate cancer; patients with ASAP had a 42% risk. The mean number of positive cores was 2.19. Prostate volume and PSA density were statistically significant predictors of positive biopsy (p<0.05). For the 43 patients who underwent radical prostatectomy, pathologic findings revealed mean Gleason score of 6.7 (6-8), pT2a-c in 72%, pT3a in16%, and pT4 in 7%. Mean cancer volume was 1.15 cc and 85.2% of tumours were clinically significant (tumour volume > 0.5 cc, Gleason > or = 7 and/or pT3).
Negative first extended biopsies should not reassure a patient of not having PCa. However, prostate cancers detected after two or more sets of extended procedures, appear to be localized (intracapsular disease) and well-differentiated prostate cancers, although they are still clinically significant.
首次前列腺穿刺活检方案结果为阴性后前列腺癌(PCa)的患病率尚不清楚。
评估首次前列腺穿刺活检方案结果为阴性的患者中显著PCa的患病率。
设计、地点和参与者:2001年3月至2007年5月期间,2500例连续患者接受了21针活检的扩展方案。在953例首次前列腺穿刺活检结果为阴性的患者中,231例患者接受了第二次或更多次21针活检。重复活检的指征包括前列腺特异性抗原(PSA)持续升高、随访期间PSA升高、既往前列腺上皮内瘤变(PIN)或非典型小腺泡增生(ASAP)。
所有参与者至少接受了两次前列腺穿刺活检扩展方案。
分析临床和病理因素(年龄、PSA、PSA倍增时间、PIN、ASAP、直肠指检[DRE])预测活检阳性的能力,并对接受根治性前列腺切除术的患者评估肿瘤参数。
第二次、第三次和第四次21针扩展活检分别在18%、17%和14%的患者中诊断出PCa。既往有PIN的患者患前列腺癌的风险为16%;有ASAP的患者风险为42%。阳性针数的平均值为2.19。前列腺体积和PSA密度是活检阳性的统计学显著预测因素(p<0.05)。对于43例接受根治性前列腺切除术的患者,病理结果显示Gleason评分平均为6.7(6 - 8),72%为pT2a - c,16%为pT3a,7%为pT4。平均癌体积为1.15立方厘米,85.2%的肿瘤具有临床意义(肿瘤体积>0.5立方厘米,Gleason评分>或 = 7和/或pT3)。
首次扩展活检结果为阴性并不能让患者放心其没有PCa。然而,在两组或更多组扩展检查后检测到的前列腺癌似乎是局限性的(包膜内疾病)且为高分化前列腺癌,尽管它们仍具有临床意义。