De Marzo A M, Knudsen B, Chan-Tack K, Epstein J I
Department of Pathology, Johns Hopkins University Medical Institutions, Baltimore, Maryland, USA.
Urology. 1999 Apr;53(4):707-13. doi: 10.1016/s0090-4295(98)00577-9.
Approximately 30% of clinically localized prostate adenocarcinomas treated by radical prostatectomy (RP) will recur within 10 years. To prevent recurrence, new adjuvant therapies are in development that seek to treat high-risk patients after surgery. To identify patients as candidates for these treatments, improved biomarkers for predicting prognosis are needed. Reduced expression of E-cadherin has been proposed as a new marker for predicting prognosis in prostate adenocarcinoma. Since few studies have examined the relation between risk factors for disease progression and E-cadherin expression using routinely processed RP specimens, we used RP specimens to correlate downregulation of E-cadherin and pathologic stage at RP.
Primary adenocarcinomas (n = 76) from formalin-fixed and paraffin-embedded RP specimens were evaluated by immunohistochemistry against E-cadherin (HECD-1) using heat-induced epitope retrieval and automated staining (BioTek Solutions). Normal appearing prostate epithelium was used as an internal control for each specimen. Staining was scored as an estimate of the percentage of tumor cells in each specimen that showed strong plasma membrane staining.
Specimens were divided into three categories with respect to Gleason score: intermediate (score 5 to 6, n = 31), intermediate to high (score 7, n = 25), and high (score 8 to 9, n = 20). For pathologic stage, specimens were divided into three categories: low stage/organ confined (pT2, n = 30), intermediate stage/limited extraprostatic extension (pT3a, n = 25), and high stage/seminal vesicle-pelvic lymph node metastases (pT3b-any pTN1, n = 21). In univariate analysis, reduced levels of E-cadherin correlated with advanced Gleason score (P = 0.003) and advanced pathologic stage (P = 0.008). In multivariate analysis, E-cadherin, preoperative prostate-specific antigen, and Gleason score all contributed independently to the prediction of high-stage disease (P<0.0001). Ten pelvic lymph node metastases from this same patient cohort were stained for E-cadherin. All were positive and 9 of 10 were moderately to strongly positive.
Since essentially all patients in the high-stage category have a very high likelihood of disease recurrence, we conclude that the study of E-cadherin in a prospective manner as a potential biomarker of disease progression in patients with clinically organ-confined prostate cancer who undergo RP is warranted. Additionally, our finding that most metastatic tumor cells in pelvic lymph nodes express E-cadherin supports the notion that the establishment of the distant colonization and growth of metastatic tumor cells may be facilitated by expression or re-expression of previously downregulated E-cadherin. This would strongly suggest that irreversible genetic inactivation through mutation or allelic loss at 16q2.3 is probably not the mechanism of E-cadherin downregulation in most abnormally expressing primary prostate carcinomas.
接受根治性前列腺切除术(RP)治疗的临床局限性前列腺腺癌患者中,约30%会在10年内复发。为预防复发,正在研发新的辅助治疗方法,旨在术后治疗高危患者。为确定适合这些治疗的患者,需要改进用于预测预后的生物标志物。E-钙黏蛋白表达降低已被提出作为预测前列腺腺癌预后的新标志物。由于很少有研究使用常规处理的RP标本研究疾病进展风险因素与E-钙黏蛋白表达之间的关系,我们使用RP标本将E-钙黏蛋白下调与RP时的病理分期相关联。
对来自福尔马林固定石蜡包埋RP标本的原发性腺癌(n = 76)进行免疫组织化学评估,采用热诱导抗原修复和自动染色(BioTek Solutions)检测E-钙黏蛋白(HECD-1)。每个标本以外观正常的前列腺上皮作为内对照。染色评分作为每个标本中显示强细胞膜染色的肿瘤细胞百分比的估计值。
根据Gleason评分将标本分为三类:中等(评分5至6,n = 31)、中等至高(评分7,n = 25)和高(评分8至9,n = 20)。对于病理分期,标本分为三类:低分期/器官局限(pT2,n = 30)、中等分期/有限的前列腺外扩展(pT3a,n = 25)和高分期/精囊-盆腔淋巴结转移(pT3b-任何pTN1,n = 21)。在单变量分析中,E-钙黏蛋白水平降低与高级别Gleason评分(P = 0.003)和高级别病理分期(P = 0.008)相关。在多变量分析中,E-钙黏蛋白、术前前列腺特异性抗原和Gleason评分均独立有助于预测高分期疾病(P<0.0001)。对来自同一患者队列的10个盆腔淋巴结转移灶进行E-钙黏蛋白染色。所有转移灶均为阳性,10个中有9个为中度至强阳性。
由于高分期组中的所有患者基本上都有很高疾病复发可能性,我们得出结论,以前瞻性方式研究E-钙黏蛋白作为接受RP的临床器官局限性前列腺癌患者疾病进展的潜在生物标志物是有必要的。此外,我们发现盆腔淋巴结中的大多数转移肿瘤细胞表达E-钙黏蛋白,这支持了这样一种观点,即先前下调的E-钙黏蛋白的表达或重新表达可能促进转移肿瘤细胞的远处定植和生长。这强烈表明,在大多数异常表达的原发性前列腺癌中,通过16q2.3处的突变或等位基因缺失导致的不可逆基因失活可能不是E-钙黏蛋白下调的机制。
