Aparicio Ana M, Shen Li, Tapia Elsa Li Ning, Lu Jing-Fang, Chen Hsiang-Chun, Zhang Jiexin, Wu Guanglin, Wang Xuemei, Troncoso Patricia, Corn Paul, Thompson Timothy C, Broom Bradley, Baggerly Keith, Maity Sankar N, Logothetis Christopher J
Department of Genitourinary Medical Oncology, The University of Texas MD Anderson Cancer Center, Houston, Texas.
Department of Bioinformatics and Computational Biology, The University of Texas MD Anderson Cancer Center, Houston, Texas.
Clin Cancer Res. 2016 Mar 15;22(6):1520-30. doi: 10.1158/1078-0432.CCR-15-1259. Epub 2015 Nov 6.
Morphologically heterogeneous prostate cancers that behave clinically like small-cell prostate cancers (SCPC) share their chemotherapy responsiveness. We asked whether these clinically defined, morphologically diverse, "aggressive variant prostate cancer (AVPC)" also share molecular features with SCPC.
Fifty-nine prostate cancer samples from 40 clinical trial participants meeting AVPC criteria, and 8 patient-tumor derived xenografts (PDX) from 6 of them, were stained for markers aberrantly expressed in SCPC. DNA from 36 and 8 PDX was analyzed by Oncoscan for copy number gains (CNG) and losses (CNL). We used the AVPC PDX to expand observations and referenced publicly available datasets to arrive at a candidate molecular signature for the AVPC.
Irrespective of morphology, Ki67 and Tp53 stained ≥10% cells in 80% and 41% of samples, respectively. RB1 stained <10% cells in 61% of samples and AR in 36%. MYC (surrogate for 8q) CNG and RB1 CNL showed in 54% of 44 samples each and PTEN CNL in 48%. All but 1 of 8 PDX bore Tp53 missense mutations. RB1 CNL was the strongest discriminator between unselected castration-resistant prostate cancer (CRPC) and the AVPC. Combined alterations in RB1, Tp53, and/or PTEN were more frequent in the AVPC than in unselected CRPC and in The Cancer Genome Atlas samples.
Clinically defined AVPC share molecular features with SCPC and are characterized by combined alterations in RB1, Tp53, and/or PTEN.
形态学上异质性的前列腺癌在临床行为上类似于小细胞前列腺癌(SCPC),它们具有相同的化疗反应性。我们探讨了这些临床定义的、形态学上多样的“侵袭性变异型前列腺癌(AVPC)”是否也与SCPC具有共同的分子特征。
对40名符合AVPC标准的临床试验参与者的59份前列腺癌样本,以及其中6人的8个患者肿瘤来源异种移植瘤(PDX),进行SCPC中异常表达标志物的染色。对36个和8个PDX的DNA进行Oncoscan分析,以检测拷贝数增加(CNG)和缺失(CNL)。我们利用AVPC的PDX来扩展观察结果,并参考公开可用的数据集得出AVPC的候选分子特征。
无论形态如何,Ki67和Tp53分别在80%和41%的样本中染色≥10%的细胞。RB1在61%的样本中染色<10%的细胞,AR在36%的样本中染色<10%的细胞。44个样本中有54%显示MYC(8q的替代物)CNG和RB1 CNL,48%显示PTEN CNL。8个PDX中除1个外均存在Tp53错义突变。RB1 CNL是未选择的去势抵抗性前列腺癌(CRPC)和AVPC之间最强的鉴别指标。RB1、Tp53和/或PTEN的联合改变在AVPC中比在未选择的CRPC和癌症基因组图谱样本中更常见。
临床定义的AVPC与SCPC具有共同的分子特征,其特征是RB1、Tp53和/或PTEN的联合改变。