Beelen Karin, Opdam Mark, Severson Tesa M, Koornstra Rutger H T, Vincent Andrew D, Wesseling Jelle, Muris Jettie J, Berns Els M J J, Vermorken Jan B, van Diest Paul J, Linn Sabine C
Breast Cancer Res. 2014 Jan 27;16(1):R13. doi: 10.1186/bcr3606.
Inhibitors of the phosphatidylinositol-3-kinase/protein kinase B/mammalian target of rapamycin (PI3K/AKT/mTOR) pathway can overcome endocrine resistance in estrogen receptor (ER) α-positive breast cancer, but companion diagnostics indicating PI3K/AKT/mTOR activation and consequently endocrine resistance are lacking. PIK3CA mutations frequently occur in ERα-positive breast cancer and result in PI3K/AKT/mTOR activation in vitro. Nevertheless, the prognostic and treatment-predictive value of these mutations in ERα-positive breast cancer is contradictive. We tested the clinical validity of PIK3CA mutations and other canonic pathway drivers to predict intrinsic resistance to adjuvant tamoxifen. In addition, we tested the association between these drivers and downstream activated proteins.
Primary tumors from 563 ERα-positive postmenopausal patients, randomized between adjuvant tamoxifen (1 to 3 years) versus observation were recollected. PIK3CA hotspot mutations in exon 9 and exon 20 were assessed with Sequenom Mass Spectometry. Immunohistochemistry was performed for human epidermal growth factor receptor 2 (HER2), phosphatase and tensin homolog (PTEN), and insulin-like growth factor 1 receptor (IGF-1R). We tested the association between these molecular alterations and downstream activated proteins (like phospho-protein kinase B (p-AKT), phospho-mammalian target of rapamycin (p-mTOR), p-ERK1/2, and p-p70S6K). Recurrence-free interval improvement with tamoxifen versus control was assessed according to the presence or absence of canonic pathway drivers, by using Cox proportional hazard models, including a test for interaction.
PIK3CA mutations (both exon 9 and exon 20) were associated with low tumor grade. An enrichment of PIK3CA exon 20 mutations was observed in progesterone receptor- positive tumors. PIK3CA exon 20 mutations were not associated with downstream-activated proteins. No significant interaction between PIK3CA mutations or any of the other canonic pathway drivers and tamoxifen-treatment benefit was found.
PIK3CA mutations do not have clinical validity to predict intrinsic resistance to adjuvant tamoxifen and may therefore be unsuitable as companion diagnostic for PI3K/AKT/mTOR inhibitors in ERα- positive, postmenopausal, early breast cancer patients.
磷脂酰肌醇-3-激酶/蛋白激酶B/雷帕霉素哺乳动物靶点(PI3K/AKT/mTOR)通路抑制剂可克服雌激素受体(ER)α阳性乳腺癌的内分泌耐药性,但目前缺乏可指示PI3K/AKT/mTOR激活及由此导致的内分泌耐药性的伴随诊断方法。PIK3CA突变在ERα阳性乳腺癌中频繁发生,并在体外导致PI3K/AKT/mTOR激活。然而,这些突变在ERα阳性乳腺癌中的预后及治疗预测价值存在矛盾。我们测试了PIK3CA突变及其他经典通路驱动因素预测辅助性他莫昔芬内在耐药性的临床有效性。此外,我们还测试了这些驱动因素与下游激活蛋白之间的关联。
收集563例ERα阳性绝经后患者的原发性肿瘤,这些患者被随机分配接受辅助性他莫昔芬治疗(1至3年)或观察。采用Sequenom质谱分析法评估第9外显子和第20外显子的PIK3CA热点突变。对人表皮生长因子受体2(HER2)、磷酸酶和张力蛋白同源物(PTEN)以及胰岛素样生长因子1受体(IGF-1R)进行免疫组织化学检测。我们测试了这些分子改变与下游激活蛋白(如磷酸化蛋白激酶B(p-AKT)、磷酸化雷帕霉素哺乳动物靶点(p-mTOR)、p-ERK1/2和p-p70S6K)之间的关联。根据经典通路驱动因素的存在与否,使用Cox比例风险模型评估他莫昔芬与对照组相比无复发生存期的改善情况,包括交互作用检验。
PIK3CA突变(第9外显子和第20外显子)均与低肿瘤分级相关。在孕激素受体阳性肿瘤中观察到PIK3CA第20外显子突变富集。PIK3CA第20外显子突变与下游激活蛋白无关。未发现PIK3CA突变或任何其他经典通路驱动因素与他莫昔芬治疗获益之间存在显著交互作用。
PIK3CA突变对预测辅助性他莫昔芬的内在耐药性没有临床有效性,因此可能不适用于ERα阳性、绝经后早期乳腺癌患者中PI3K/AKT/mTOR抑制剂的伴随诊断。
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