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[前列腺孤立性导管内癌:临床病理与分子分析]

[Isolated intraductal carcinoma of the prostate: a clinicopathological and molecular analysis].

作者信息

Zhang H Z, Wang S Y, Guo Y N, Zhao M

机构信息

Ningbo Clinical Pathology Diagnosis Center, Ningbo 315000, China.

出版信息

Zhonghua Bing Li Xue Za Zhi. 2024 Aug 8;53(8):803-808. doi: 10.3760/cma.j.cn112151-20240119-00051.

DOI:10.3760/cma.j.cn112151-20240119-00051
PMID:39103261
Abstract

To study the clinicopathological features, immunohistochemical phenotypes, molecular changes, differential diagnosis and prognosis of isolated intraductal carcinoma of the prostate (iIDC-P). Three iIDC-P cases were collected retrospectively from 2016 to 2022 at Ningbo Clinical Pathology Diagnosis Center, Ningbo, China. The clinicopathologic features and immunophenotypic profiles were studied using light microscopy and immunohistochemistry. A targeted next-generation sequencing panel was used to analyze cancer-associated mutations. Follow-up and literature review were also performed. The patients' ages were 61, 67 and 77 years, and their preoperative prostate specific antigen (PSA) levels were 7.99, 7.99 and 4.86 μg/L, respectively. Case 1 and 2 were diagnosed on needle biopsy and radical prostatectomy (RP) specimens, and case 3 was diagnosed on a specimen of transurethral resection of the prostate (TURP). The RP specimen was entirely submitted for histologic examination. In the case 1, iIDC-P was found in one tissue core (involving two ducts) in the biopsy specimen, and in 6 sections (diameter, 0.3-1.1 cm) from the radical prostatectomy specimen, and one section had separate foci of low-grade acinar adenocarcinoma (diameter, 0.05 cm). In the case 2, 6 tissue sections from the biopsy specimens showed iIDC-P, and 13 sections from RP specimen showed iIDC-P (diameter, 0.5-1.6 cm), and the other 3 sections had separate low grade acinar adenocarcinoma (diameter, 0.6 cm). In the case 3, 5 tissue blocks from the TURP specimen showed iIDC-P. The case 1 and 2 showed solid architecture with expansile proliferation of neoplastic cells in native ducts and acini. The case 3 showed dense or loose cribriform pattern, with marked cytological atypia, and frequent mitotic figures. Comedonecrosis was found in solid or dense cribriform glands in the case 2. Immunohistochemically, surrounding basal cells were highlighted using high-molecular-weight cytokeratin (34βE12 and CK5/6) and p63, while P504s was positive in the tumor cells. The tumor cells were also positive for AR and prostate markers (NKX3.1, PSA and PSAP), and negative for GATA3. The iIDC-P and acinar adenocarcinoma both showed weak PTEN expression and no ERG (nuclear) expression. In case 2 and 3, targeted sequencing revealed activated oncogenic driver mutations in MAPK and PI3K pathway genes (KRAS, MTOR and PTEN). In addition, pathogenic mutation in TP53 and FOXA1 mutation were found in the case 2 and 3, respectively. No case demonstrated TMPRSS2::ERG translocation. All cases were microsatellite stable and had lower tumor mutation burdens (range, 2.1-3.1 muts/Mb). The patients showed no biochemical recurrence or metastasis after follow-up of 16-91 months. iIDC-P is a special type of intraductal carcinoma of the prostate and differs from intraductal carcinoma within high-grade prostate cancer. iIDC-P has unique molecular characteristics and may represent as a molecularly unique in situ tumor of prostate cancer.

摘要

研究前列腺导管内癌(iIDC-P)的临床病理特征、免疫组化表型、分子改变、鉴别诊断及预后。回顾性收集2016年至2022年中国宁波临床病理诊断中心的3例iIDC-P病例。采用光学显微镜和免疫组化研究其临床病理特征和免疫表型。使用靶向二代测序panel分析癌症相关突变。同时进行随访和文献复习。患者年龄分别为61岁、67岁和77岁,术前前列腺特异性抗原(PSA)水平分别为7.99、7.99和4.86μg/L。病例1和2通过穿刺活检和前列腺根治性切除术(RP)标本确诊,病例3通过经尿道前列腺切除术(TURP)标本确诊。RP标本全部送检进行组织学检查。病例1中,穿刺活检标本的1个组织芯(累及2个导管)发现iIDC-P,前列腺根治性切除标本的6个切片(直径0.3 - 1.1cm)发现iIDC-P,其中1个切片有孤立的低级别腺泡腺癌灶(直径0.05cm)。病例2中,穿刺活检标本的6个组织切片显示iIDC-P,RP标本的13个切片显示iIDC-P(直径0.5 - 1.6cm),另外3个切片有孤立的低级别腺泡腺癌(直径0.6cm)。病例3中,TURP标本的5个组织块显示iIDC-P。病例1和2表现为实性结构,肿瘤细胞在原有导管和腺泡中呈膨胀性增殖。病例3表现为致密或疏松筛状结构,有明显的细胞学异型性和频繁的核分裂象。病例2的实性或致密筛状腺体中发现粉刺样坏死。免疫组化方面,使用高分子量细胞角蛋白(34βE12和CK5/6)和p63可突出显示周围基底细胞,而P504s在肿瘤细胞中呈阳性。肿瘤细胞AR和前列腺标志物(NKX3.1、PSA和PSAP)也呈阳性,GATA3呈阴性。iIDC-P和腺泡腺癌均显示PTEN表达减弱且无ERG(核)表达。病例2和3中,靶向测序显示MAPK和PI3K通路基因(KRAS、MTOR和PTEN)有激活的致癌驱动突变。此外,病例2和3分别发现TP53致病突变和FOXA1突变。所有病例均为微卫星稳定,肿瘤突变负荷较低(范围2.1 - 3.1个突变/Mb)。随访16 - 91个月,患者均未出现生化复发或转移。iIDC-P是前列腺导管内癌的一种特殊类型,与高级别前列腺癌中的导管内癌不同。iIDC-P具有独特的分子特征,可能代表前列腺癌一种分子独特的原位肿瘤。

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