Chen Shuhui, Cavazza Elisa, Barlier Catherine, Salleron Julia, Filhine-Tresarrieu Pierre, Gavoilles Céline, Merlin Jean-Louis, Harlé Alexandre
Faculty of Pharmacy, Université de Lorraine, 54001 Nancy, France; CNRS UMR 7039 CRAN, Université de Lorraine, 54506 Vandoeuvre-les-Nancy, France; Department of Biopathology, Institut de Cancérologie de Lorraine, 54519 Vandoeuvre-les-Nancy, France; Department of Gynecological Oncology, Zhongnan Hospital, Wuhan University, Wuhan, Hubei 430071, P.R. China.
Faculty of Pharmacy, Université de Lorraine, 54001 Nancy, France.
Oncol Lett. 2016 Nov;12(5):3264-3272. doi: 10.3892/ol.2016.5083. Epub 2016 Sep 2.
Despite great histological and molecular heterogeneity, the clinical management of high-grade ovarian carcinomas remains unspecialized. As a major subgroup, high-grade serous ovarian carcinomas (HGSOCs) require novel therapies. In addition to utilizing conventional histological prognostic markers and performing oncogenetic investigations, the molecular diagnostic method of next generation sequencing (NGS) was performed to identify 'druggable' targets that could provide access to innovative therapy. The present study was performed in 45 HGSOC patients (mean age, 59.1 years; range, 25-87 years) with histologically proven HGSOC. Breast cancer 1/2 (/2) germline mutations were screened in 17 patients with a familial or personal history of cancer, which was justified by oncogenetic investigations. Tumor protein 53 (P53) and phosphatase and tensin homolog (PTEN) expression were assessed in formalin-fixed paraffin-embedded tissues using immunohistochemistry. Somatic mutations of Kirsten rat sarcoma viral oncogene homolog, neuroblastoma RAS viral oncogene homolog (), B-Raf proto-oncogene, serine/threonine kinase, phosphatidylinositol-4,5-bisphosphate 3-kinase catalytic subunit α () and MET proto-oncogene, receptor tyrosine kinase () were screened using NGS on DNA extracts from frozen tumor specimens obtained at diagnosis. With a median follow-up of 38 months (range, 6-93 months), 20 patients are alive, 10 patients are disease-free and 14 patients progressed within 6 months following platinum-based therapy. P53 overexpression was detected in 67% of patients and PTEN loss was detected in 38% of the patients. The overexpression of mutant P53 was found to be associated with a longer progression-free and overall survival. In total, 2 (exon 3), 3 (exon 5 and 10) and 5 mutations (exons 14 and 18) were detected. In HGSOCs, in addition to P53 and PTEN alterations, somatic genetic abnormalities can be detected using NGS and provide molecular rationale for targeted therapies, potentially offering novel therapeutic opportunities to patients.
尽管高级别卵巢癌在组织学和分子层面存在很大异质性,但其临床管理仍缺乏针对性。作为一个主要亚组,高级别浆液性卵巢癌(HGSOC)需要新的治疗方法。除了利用传统的组织学预后标志物并进行肿瘤遗传学研究外,还采用了下一代测序(NGS)分子诊断方法来识别可提供创新治疗途径的“可靶向治疗”靶点。本研究纳入了45例经组织学证实为HGSOC的患者(平均年龄59.1岁;范围25 - 87岁)。对17例有家族或个人癌症病史的患者进行了乳腺癌1/2(/2)种系突变筛查,肿瘤遗传学研究证明了其合理性。使用免疫组织化学方法在福尔马林固定石蜡包埋组织中评估肿瘤蛋白53(P53)和磷酸酶及张力蛋白同源物(PTEN)的表达。使用NGS对诊断时获取的冷冻肿瘤标本的DNA提取物进行筛查,以检测 Kirsten 大鼠肉瘤病毒癌基因同源物、神经母细胞瘤RAS病毒癌基因同源物()、B-Raf原癌基因、丝氨酸/苏氨酸激酶、磷脂酰肌醇-4,5-二磷酸3-激酶催化亚基α()和MET原癌基因、受体酪氨酸激酶()的体细胞突变。中位随访38个月(范围6 - 93个月),20例患者存活,10例患者无疾病进展,14例患者在铂类治疗后6个月内病情进展。在67%的患者中检测到P53过表达,在38%的患者中检测到PTEN缺失。发现突变型P53的过表达与更长的无进展生存期和总生存期相关。总共检测到2个(外显子3)、3个(外显子5和10)和5个 突变(外显子14和18)。在HGSOC中,除了P53和PTEN改变外,使用NGS可以检测到体细胞遗传异常,并为靶向治疗提供分子依据,可能为患者提供新的治疗机会。
