低风险前列腺癌的超级主动监测|意见:不

S. Ghodoussipour, A. Lebastchi, P. Pinto, André Berger
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引用次数: 0

摘要

诊断前列腺癌(PCa)是在美国每年超过170000人(1),这使得PCa最常见的固体男性恶性肿瘤之一,死亡率很低,大多数人死于不相关的原因(1)。事实上,几乎一半的男性筛查检测和局部PCa是延迟治疗或候选人积极监测()(2)。减少发病率与明确的治疗,许多供应商建议对于那些极低(VLR)”,低风险(LR)疾病和选择有利的中风险(IR) PCa(3-5)。AS的使用一直在稳步增加,并得到大型队列研究的支持,显示PCa特异性生存率为98-100%(6,7)。虽然推荐的AS随访时间各不相同,但安全性是基于密切监测和预定义的治疗阈值,这些阈值是基于确定癌症进展但仍可治愈的疾病。在已发表的最大的AS队列中,993名男性,中位随访6.4年,10年癌症特异性生存率(CSS)为98.1%。然而,这些患者中有27%最终因前列腺特异性抗原(PSA)进展、活检Gleason评分进展或患者偏好等适应症接受了手术。虽然该队列主要包括患有LR疾病的年轻男性(年龄<70岁,cT1/T2a疾病,PSA <10ng/ml),但他们也包括年龄大于70岁的Gleason 3+4=7或更低疾病的患者,因此20%患有IR(6)。Musunuru等人对该队列的单独分析显示,虽然只有3%的患者发生转移,但与LR组相比,IR中的无转移生存率(MFS)显着降低(84% vs 95%)。p=0.001)(8)。Yamamoto等人的另一项单独队列分析显示,Gleason评分较高的疾病15年PCa死亡率(PCM)的风险明显更高(Gleason 3+4=7 vs Gleason 3+3=6的HR为4.0,Gleason 4+3=7 vs Gleason 3+3=6的HR为10.5)(9)。PROTECT试验将1643名局限性PCa患者随机分为AS (n=545),最终治疗是根治性前列腺切除术(RP;n=553)或放射治疗(RT;n = 545)。3组间PCM无差异(p=0.48),但17例死亡患者中,AS组8例(5/8合并IR疾病),RP组5例,RT组4例。与RP或RT相比,AS组的疾病进展和转移率明显更高(分别为112人vs 46人vs 46人;p < 0.001)(10)。尽管有一部分患者在接受AS治疗后表现更差,但考虑到最终治疗的发病率,专家们建议扩大AS的适应症,并选择包括低容量IR疾病的患者(3,5,11,12)。随着As适应症的扩大,某些患者可能希望在他们的监测中更加“积极”。In 2018, Bloom et DiffereNce Of OpiNiON Vol. 45 (2): 215-219, March April, 2019
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Super active surveillance for low-risk prostate cancer | Opinion: No
Prostate cancer (PCa) is diagnosed in over 170,000 men in the United States each year (1). While this makes PCa one of the most common solid malignancies in men, the mortality is low and most men die from unrelated causes (1). In fact, almost half of men with screening detected and localized PCa are considered candidates for deferred treatment or active surveillance (AS) (2). To decrease the morbidity associated with definitive therapy, many providers recommend AS for those with very-low (VLR), low risk (LR) disease and in selected favorable, intermediate risk (IR) PCa (3-5). The use of AS has been steadily increasing and is supported by large cohort studies showing 98-100% PCa specific survival rates (6, 7). While the recommended follow-up for AS varies, safety is predicated on close surveillance with predefined thresholds for treatment based on identification of cancer progression yet still curable disease. In the largest published AS cohort of 993 men with median follow-up of 6.4 years, 10-year cancer specific survival (CSS) was 98.1%. However, 27% of these patients ultimately underwent surgery for indications ranging from prostate specific antigen (PSA) progression, biopsy Gleason score progression or patient preference. While this cohort included mostly younger men with LR disease (Age <70, cT1/T2a disease, PSA <10ng/ml), they also included patients older than 70 with Gleason 3+4=7 or lower disease, such that 20% had IR (6). A separate analysis of this cohort by Musunuru et al. showed that while only 3% of patients developed metastases, metastasis free survival (MFS) was significantly lower in the IR as compared to the LR group (84% vs 95%, p=0.001) (8). Another separate cohort analysis by Yamamoto et al. showed a significantly higher risk of 15-year PCa mortality (PCM) for higher Gleason score disease (HR of 4.0 for Gleason 3+4=7 vs Gleason 3+3=6 and HR 10.5 for Gleason 4+3=7 vs Gleason 3+3=6) (9). The PROTECT trial randomized 1643 patients with localized PCa into AS (n=545), definitive treatment with radical prostatectomy (RP; n=553) or radiation therapy (RT; n=545). There was no difference in PCM amongst the 3 groups (p=0.48), however, of those 17 patients who passed away, 8 were in the AS group (5/8 with IR disease), 5 in the RP group and 4 in the RT group. The rate of disease progression and development of metastases was significantly higher in the AS group as compared to RP or RT (112 vs 46 vs 46 men, respectively; p<0.001) (10). Despite a certain subset of patients who seem to do worse on AS, concerns with morbidity from definitive treatment have led experts to recommend a broadening of the indications for AS and to include selected patients with low volume IR disease (3, 5, 11, 12). As the indications for AS expand, certain patients may wish to be even more “active” in their surveillance. In 2018, Bloom et DiffereNce Of OpiNiON Vol. 45 (2): 215-219, March April, 2019
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