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Gleason 模式 5 前列腺腺癌“单细胞”生长的临床病理研究揭示了 2 种不同类型,一种具有“浆细胞样”特征。

Clinicopathologic Study of Gleason Pattern 5 Prostatic Adenocarcinoma With "Single-cell" Growth Reveals 2 Distinct Types, One With "Plasmacytoid" Features.

机构信息

Robert J. Tomsich Pathology and Laboratory Medicine Institute, Cleveland Clinic, Cleveland, OH.

Department of Pathology, University of California San Francisco, San Francisco, CA.

出版信息

Am J Surg Pathol. 2020 Dec;44(12):1635-1642. doi: 10.1097/PAS.0000000000001550.

Abstract

Each Gleason score category of prostatic adenocarcinoma (or Grade Group) may encompass a diverse group of architectural patterns such as well-formed glands, poorly formed glands, cribriform structures, single cells, and/or solid sheets. We have noted heterogeneity within the single-cell subtype of Gleason pattern 5 prostatic adenocarcinoma that has not been fully addressed. Therefore, we retrospectively reviewed a series of radical prostatectomies with high-grade prostatic adenocarcinoma (Grade Group 4 or 5), identifying tumors with a component of single-cell infiltration. Additional cases identified prospectively were also included. TNM status, association with other histologic patterns, and clinical follow-up status were determined. Immunohistochemistry for NKX3.1, E-cadherin, p120 catenin, and prostate-specific antigen (PSA) were performed in each case. Eighteen cases with a component of well-developed Gleason pattern 5 characterized by single infiltrative cells that comprised ≥5% of the tumor were identified (15/202 retrospective radical prostatectomies with the high-grade disease [7.5%]). The single-cell pattern ranged from 5% to 50% of the tumor volume, with 5 cases containing ≥40%, and variable secondary architecture included diffuse infiltrating single cells with targetoid growth pattern around benign glands, solid expansive nests of noncohesive cells, and corded/single file growth pattern. Further morphologic analysis demonstrated 2 distinct histologic subtypes: (1) (subtype 1; n=9) monomorphic "plasmacytoid" tumor cells with eccentrically placed nuclei and variable intracytoplasmic vacuoles with bland cytology and discohesion and (2) (subtype 2; n=9) more cohesive tumor cells with greater cytologic atypia characterized by prominent nucleoli, greater variability in nuclear size/shape, occasional mitotic figures, and more irregular infiltration. By immunohistochemistry, NKX3.1 nuclear expression and PSA cytoplasmic expression was retained in all cases. Concomitant membranous E-cadherin loss and strong cytoplasmic p120 catenin expression were present in 5 of the 18 (28%) cases, all in subtype 1 (5/9, 56%). Overall, 56% (10/18) of patients had advanced-stage disease (≥pT3b), and 70% (7/10) of these patients had associated lymphovascular invasion. All patients had concomitant cribriform patterns of carcinoma. The outcome was available for 14 patients: 4 died of unknown cause; 6 had biochemical recurrence with distant bone metastasis in 5 of the 6; and 4 patients with <3 years of follow-up currently have undetectable serum PSA levels (2 patients received salvage radiotherapy with androgen deprivation and 2 remain on routine follow-up). In summary, the single-cell pattern of Gleason pattern 5 prostatic adenocarcinoma is uniformly associated with other high-risk histologic patterns (eg, cribriform growth), and high-stage disease with distant metastasis is not uncommon. Our data suggest that the "single-cell" Gleason pattern 5 prostatic adenocarcinoma contains 2 distinct subtypes. Somatic CDH1 alterations may play a role in the development of the "plasmacytoid" pattern characterized by monomorphic cytology with concomitant E-cadherin loss and aberrant p120 catenin expression.

摘要

每个前列腺腺癌(或分级组)的 Gleason 评分类别都可能包含多种不同的结构模式,例如形成良好的腺体、形成不良的腺体、筛状结构、单细胞和/或实性片。我们注意到 Gleason 模式 5 前列腺腺癌的单细胞亚型存在异质性,尚未得到充分解决。因此,我们回顾性分析了一系列高级别前列腺腺癌(分级组 4 或 5)的根治性前列腺切除术,鉴定出具有单细胞浸润成分的肿瘤。还前瞻性地鉴定了其他病例。确定了 TNM 状态、与其他组织学模式的关联以及临床随访状态。对每个病例进行 NKX3.1、E-钙黏蛋白、p120 连环蛋白和前列腺特异性抗原(PSA)的免疫组织化学染色。鉴定出 18 例具有发达的 Gleason 模式 5 特征的肿瘤,其特征为构成肿瘤的≥5%的单个浸润细胞(202 例高级别疾病的回顾性根治性前列腺切除术[7.5%]中有 15 例)。单细胞模式占肿瘤体积的 5%至 50%,5 例含有≥40%,并存在可变的次要结构,包括弥漫浸润的单细胞,围绕良性腺体的靶状生长模式、实性扩张的非黏附细胞巢和索状/单行生长模式。进一步的形态学分析显示出 2 种不同的组织学亚型:(1)(亚型 1;n=9)形态单一的“浆细胞样”肿瘤细胞,具有偏心放置的细胞核和不同大小的空泡,具有温和的细胞学特征和脱黏(2)(亚型 2;n=9)更具凝聚力的肿瘤细胞,具有更明显的核仁、更大的核大小/形状变异性、偶尔有丝分裂和更不规则的浸润。通过免疫组织化学染色,所有病例均保留 NKX3.1 核表达和 PSA 细胞质表达。在 18 例中的 5 例(28%)中同时存在膜 E-钙黏蛋白丢失和强细胞质 p120 连环蛋白表达,均为亚型 1(5/9,56%)。总体而言,56%(18/32)的患者患有晚期疾病(≥pT3b),70%(10/14)的患者有相关的血管淋巴管侵犯。所有患者均伴有筛状癌模式。14 例患者的结果可用:4 例死因不明;6 例有生化复发,其中 5 例有远处骨转移;4 例患者随访时间<3 年,目前血清 PSA 水平无法检测(2 例患者接受挽救性放疗联合雄激素剥夺治疗,2 例患者仍在常规随访中)。总之,Gleason 模式 5 前列腺腺癌的单细胞模式与其他高危组织学模式(例如,筛状生长)均匀相关,且远处转移的晚期疾病并不少见。我们的数据表明,“单细胞”Gleason 模式 5 前列腺腺癌包含 2 种不同的亚型。体细胞 CDH1 改变可能在以单形细胞学为特征的“浆细胞样”模式的发展中起作用,同时伴有 E-钙黏蛋白丢失和异常的 p120 连环蛋白表达。

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