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评估局限性前列腺癌并确定聚焦治疗的候选者。

Evaluating localized prostate cancer and identifying candidates for focal therapy.

作者信息

Sartor A Oliver, Hricak Hedvig, Wheeler Thomas M, Coleman Jonathan, Penson David F, Carroll Peter R, Rubin Mark A, Scardino Peter T

机构信息

Department of Medicine, Harvard Medical School, Lank Center for Genitourinary Oncology, Dana-Farber Cancer Institute, Boston, Massachusetts, USA.

出版信息

Urology. 2008 Dec;72(6 Suppl):S12-24. doi: 10.1016/j.urology.2008.10.004.

DOI:10.1016/j.urology.2008.10.004
PMID:19095124
Abstract

Can focal therapy successfully control prostate cancer? Also, if so, which patients should be considered eligible? With limited data available from relatively few patients, these questions are difficult to answer. At this writing, the most likely candidates for focal therapy are patients with low-risk, small-volume tumors, located in 1 region or sector of the prostate, who would benefit from early intervention. The difficulty lies in reliably identifying these men. The larger number of cores obtained in each needle biopsy session has increased both the detection of prostate cancer and the potential risk of overtreating many patients whose cancers pose very little risk to life or health. Urologists typically perform at least a 12-core template biopsy. Although the debate continues about the optimal template, laterally and peripherally directed biopsies have been shown to improve the diagnostic yield. However, as many as 25% of tumors arise anteriorly and can be missed with peripherally directed techniques. Prostate cancer tends to be multifocal, even in its earliest stages. However, the secondary cancers are usually smaller and less aggressive than the index cancer. They appear similar to the incidental cancers found in cystoprostatectomy specimens and appear to have little effect on prognosis in surgical series. When a single focus of cancer is found in 1 core, physicians rightly suspect that more foci of cancer are present in the prostate. Assessing the risk in these patients is challenging when determined by the biopsy data alone. To predict the presence of a very low-risk or "indolent" cancer, nomograms have been developed to incorporate clinical stage, Gleason grade, prostate-specific antigen levels, and prostate volume, along with the quantitative analysis of the biopsy results. Transperineal "mapping" or "saturation" biopsies have been advocated to detect cancers missed or underestimated by previous transrectal biopsies. This approach could provide the accurate staging, grading, and tumor localization needed for a focal therapy program. Nevertheless, for men with minimal cancer who are amenable to active surveillance or focal therapy, consensus about the most accurate biopsy strategy has not yet been reached. Imaging, particularly magnetic resonance imaging and magnetic resonance spectroscopic imaging, has been used to assess men with early-stage prostate cancer. Large-volume cancers can be seen reasonably well, but small lesions have been difficult to detect reliably or measure accurately. Factors such as voxel resolution, organ movement, biopsy artifact, and benign changes have limited the consistent estimation of the quantitative tumor volume. Nevertheless, magnetic resonance imaging and magnetic resonance spectroscopic imaging can aid in evaluating patients with prostate cancer being considered for focal therapy by providing additional evidence that the patient does not harbor an otherwise undetected high-risk, aggressive cancer. In some cases, imaging can usefully identify the location of even a limited-sized index cancer. When imaging findings are substantiated by mapping biopsy results, confidence in the accurate characterization of the cancer is enhanced. Correlating the imaging results with tissue changes during and after treatment can be of use in monitoring the ablative effects in the prostate and in assessing for tumor recurrence. More work is necessary before staging studies can uniformly characterize a prostate cancer before therapy, much less reliably identify and locate small-volume cancer within the prostate. However, exploring the role of focal ablation as a therapeutic option for selected men with low-risk, clinically localized, prostate cancer need not await the emergence of perfectly accurate staging studies, any more than the application of radical surgery or radiotherapy have. Modern biopsy strategies, combined with optimal imaging and nomograms to estimate the pathologic stage and risk, taken together, provide a sound basis for the selection of appropriate patients for entry into prospective clinical trials of focal therapy.

摘要

聚焦治疗能否成功控制前列腺癌?如果可以,哪些患者应被视为适合接受该治疗?由于相对较少患者的可用数据有限,这些问题难以回答。在撰写本文时,聚焦治疗最有可能的候选对象是患有低风险、小体积肿瘤的患者,肿瘤位于前列腺的1个区域或腺叶,这些患者将从早期干预中获益。难点在于可靠地识别出这些男性患者。每次穿刺活检获取的更多穿刺针芯既增加了前列腺癌的检出率,也增加了过度治疗许多癌症对生命或健康风险极小的患者的潜在风险。泌尿科医生通常至少进行12针的模板活检。尽管关于最佳模板的争论仍在继续,但已证明侧向和周边穿刺活检可提高诊断率。然而,多达25%的肿瘤发生在前部,采用周边穿刺技术可能会漏诊。前列腺癌往往是多灶性的,即使在其最早阶段也是如此。然而,继发性癌症通常比原发癌更小且侵袭性更弱。它们类似于在膀胱前列腺切除标本中发现的偶发性癌症,在手术系列研究中似乎对预后影响不大。当在1个针芯中发现单个癌灶时,医生有理由怀疑前列腺中还存在更多癌灶。仅根据活检数据来评估这些患者的风险具有挑战性。为了预测极低风险或“惰性”癌症的存在,已经开发了列线图,将临床分期、Gleason分级、前列腺特异性抗原水平、前列腺体积以及活检结果的定量分析纳入其中。经会阴“图谱”或“饱和”活检已被提倡用于检测先前经直肠活检遗漏或低估的癌症。这种方法可以提供聚焦治疗方案所需的准确分期、分级和肿瘤定位。然而,对于适合积极监测或聚焦治疗的癌症极少的男性患者,尚未就最准确的活检策略达成共识。影像学检查,尤其是磁共振成像和磁共振波谱成像,已被用于评估早期前列腺癌患者。大体积癌症能被较好地观察到,但小病灶一直难以可靠检测或准确测量。诸如体素分辨率、器官移动、活检伪影和良性改变等因素限制了对肿瘤定量体积的一致估计。尽管如此,磁共振成像和磁共振波谱成像可以通过提供额外证据,证明患者不存在未被发现的高风险、侵袭性癌症,从而有助于评估考虑接受聚焦治疗的前列腺癌患者。在某些情况下,影像学检查甚至可以有效地识别即使是有限大小的原发癌的位置。当影像学检查结果得到图谱活检结果证实时,对癌症准确特征的信心会增强。将影像学检查结果与治疗期间及治疗后的组织变化相关联,可用于监测前列腺的消融效果并评估肿瘤复发情况。在分期研究能够在治疗前统一表征前列腺癌之前,还需要做更多工作,更不用说可靠地识别和定位前列腺内的小体积癌症了。然而,探索聚焦消融作为选定的低风险、临床局限性前列腺癌男性患者的治疗选择,并不需要等待完美准确的分期研究出现,就如同根治性手术或放疗的应用一样。现代活检策略,结合最佳影像学检查和列线图来估计病理分期和风险,综合起来为选择合适的患者进入聚焦治疗的前瞻性临床试验提供了坚实的基础。

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