Foundation Medicine, Cambridge, Massachusetts.
Department of Clinical Oncology, Hospital Sírio Libanes, Sao Paulo, Brazil.
Cancer. 2019 Apr 1;125(7):1185-1199. doi: 10.1002/cncr.31921. Epub 2018 Dec 24.
The phosphatidylinositol 3-kinase (PI3K) pathway is frequently altered in cancer. This report describes the landscape of PI3K alterations in solid tumors as well as co-alterations serving as potential resistance/attenuation mechanisms.
Consecutive samples were analyzed in a commercial Clinical Laboratory Improvement Amendment-certified laboratory using comprehensive genomic profiling performed by next-generation sequencing (315 genes). The co-alterations evaluated included the Erb-B2 receptor tyrosine kinase 2 (ERBB2), ERBB3, ERBB4, RAS, MET proto-oncogene tyrosine kinase (MET), and mitogen-activated protein kinase kinase (MAP2K) genes as well as tumor protein 53 (TP53), estrogen receptor 1 (ESR1), and androgen receptor (AR).
Alterations in any of 18 PI3K-pathway associated genes were identified in 44% of 60,991 tumors. Although single base and insertions/deletions (indels) were the most frequent alterations, copy number changes and rearrangements were identified in 11% and 0.9% of patients, respectively. Overall, the most frequently altered genes were PIK3 catalytic subunit α (PIK3CA) (13%), phosphatase and tensin homolog (PTEN) (9%), and serine/threonine kinase 11 (STK11) (5%). Tumor types that frequently harbored at least 1 PI3K alteration were uterine (77%), cervical (62%), anal (59%), and breast (58%) cancers. Alterations also were discerned frequently in tumors with carcinosarcoma (89%) and squamous cell carcinoma (62%) histologies. Tumors with a greater likelihood of co-occurring PI3K pathway and MAPK pathway alterations included colorectal cancers (odds ratio [OR], 1.64; P < .001), mesotheliomas (OR, 2.67; P = .024), anal cancers (OR, 1.98; P = .03), and nonsquamous head and neck cancers (OR, 2.03; P = .019). The co-occurrence of ESR1 and/or AR alterations with PI3K alterations was statistically significant in bladder, colorectal, uterine, prostate, and unknown primary cancers.
Comprehensive genomic profiling reveals altered PI3K-related genes in 44% of solid malignancies, including rare disease and histology types. The frequency of alterations and the co-occurrence of resistance pathways vary by tumor type, directly affecting opportunities for targeted therapy.
磷脂酰肌醇 3-激酶(PI3K)通路在癌症中经常发生改变。本报告描述了实体瘤中 PI3K 改变的情况,以及作为潜在耐药/衰减机制的共同改变。
在一家经过商业临床实验室改进修正案认证的实验室中,使用下一代测序(315 个基因)进行全面基因组分析,对连续样本进行分析。评估的共同改变包括表皮生长因子受体 2(ERBB2)、表皮生长因子受体 3(ERBB3)、表皮生长因子受体 4(ERBB4)、RAS、原癌基因酪氨酸激酶 MET(MET)和丝裂原激活蛋白激酶激酶 2(MAP2K)基因以及肿瘤蛋白 53(TP53)、雌激素受体 1(ESR1)和雄激素受体(AR)。
在 60991 个肿瘤中,有 44%的肿瘤存在 18 个与 PI3K 通路相关的基因中的任何一个改变。虽然单个碱基和插入/缺失(indels)是最常见的改变,但在 11%和 0.9%的患者中分别发现了拷贝数改变和重排。总体而言,最常改变的基因是 PIK3 催化亚基 α(PIK3CA)(13%)、磷酸酶和张力蛋白同源物(PTEN)(9%)和丝氨酸/苏氨酸激酶 11(STK11)(5%)。最常发生至少 1 种 PI3K 改变的肿瘤类型为子宫(77%)、宫颈(62%)、肛门(59%)和乳腺(58%)癌。在具有癌肉瘤(89%)和鳞状细胞癌(62%)组织学的肿瘤中也经常发现改变。更有可能同时发生 PI3K 通路和 MAPK 通路改变的肿瘤包括结直肠癌(比值比[OR],1.64;P<.001)、间皮瘤(OR,2.67;P=.024)、肛门癌(OR,1.98;P=.03)和非鳞状头颈部癌症(OR,2.03;P=.019)。在膀胱癌、结直肠癌、子宫癌、前列腺癌和未知原发性癌症中,ESR1 和/或 AR 改变与 PI3K 改变同时发生具有统计学意义。
全面基因组分析显示,44%的实体恶性肿瘤存在改变的 PI3K 相关基因,包括罕见疾病和组织学类型。改变的频率和耐药途径的共同发生因肿瘤类型而异,直接影响靶向治疗的机会。
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