Gaibar Maria, Beltrán Laura, Romero-Lorca Alicia, Fernández-Santander Ana, Novillo Apolonia
Faculty of Biomedical Sciences and Health, Universidad Europea de Madrid, C/Tajo, S/N, 28670 Villaviciosa de Odón, Madrid, Spain.
J Oncol. 2020 Mar 7;2020:6375956. doi: 10.1155/2020/6375956. eCollection 2020.
In one of every four or five cases of breast cancer, the human epidermal growth factor receptor-2 () gene is overexpressed. These carcinomas are known as HER2-positive. HER2 overexpression is linked to an aggressive phenotype and a lower rate of disease-free and overall survival. Drugs such as trastuzumab, pertuzumab, lapatinib, neratinib, and the more recent afatinib target the deregulation of HER2 expression. Some authors have attributed somatic mutations in HER2, a role in resistance to anti-HER2 therapy as differential regulation of HER2 has been observed among patients. Recently, studies in metastatic ER + tumors suggest that some HER2 mutations emerge as a mechanism of acquired resistance to endocrine therapy. In an effort to identify possible biomarkers of the efficacy of anti-HER2 therapy, we here review the known single-nucleotide polymorphisms (SNPs) of the HER2 gene found in HER2-positive breast cancer patients and their relationship with clinical outcomes. Information was recompiled on 11 somatic HER2 SNPs. Seven polymorphisms are located in the tyrosine kinase domain region of the gene contrasting with the low number of mutations found in extracellular and transmembrane areas. HER2-positive patients carrying S310F, S310Y, R678Q, D769H, or I767M mutations seem good candidates for anti-HER2 therapy as they show favorable outcomes and a good response to current pharmacological treatments. Carrying the L755S or D769Y mutation could also confer benefits when receiving neratinib or afatinib. By contrast, patients with mutations L755S, V842I, K753I, or D769Y do not seem to benefit from trastuzumab. Resistance to lapatinib has been reported in patients with L755S, V842I, and K753I. These data suggest that exploring HER2 SNPs in each patient could help individualize anti-HER2 therapies. Advances in our understanding of the genetics of the HER2 gene and its relations with the efficacy of anti-HER2 treatments are needed to improve the outcomes of patients with this aggressive breast cancer.
在每四到五例乳腺癌病例中,就有一例人类表皮生长因子受体2(HER2)基因过度表达。这些癌被称为HER2阳性。HER2过度表达与侵袭性表型以及较低的无病生存率和总生存率相关。曲妥珠单抗、帕妥珠单抗、拉帕替尼、来那替尼以及最近的阿法替尼等药物靶向HER2表达失调。一些作者认为HER2的体细胞突变在抗HER2治疗耐药中起作用,因为在患者中观察到HER2存在差异调节。最近,转移性雌激素受体阳性肿瘤的研究表明,一些HER2突变是获得性内分泌治疗耐药的一种机制。为了确定抗HER2治疗疗效的可能生物标志物,我们在此综述HER2阳性乳腺癌患者中发现的HER2基因已知单核苷酸多态性(SNP)及其与临床结局的关系。重新收集了11个HER2体细胞SNP的信息。七个多态性位于该基因的酪氨酸激酶结构域区域,与之形成对比的是,在细胞外和跨膜区域发现的突变数量较少。携带S310F、S310Y、R678Q、D769H或I767M突变的HER2阳性患者似乎是抗HER2治疗的良好候选者,因为他们显示出良好的结局以及对当前药物治疗的良好反应。携带L755S或D769Y突变在接受来那替尼或阿法替尼治疗时也可能带来益处。相比之下,携带L755S、V842I、K753I或D769Y突变的患者似乎无法从曲妥珠单抗治疗中获益。据报道,携带L755S、V842I和K753I突变的患者对拉帕替尼耐药。这些数据表明,探究每位患者的HER2 SNP有助于实现抗HER2治疗的个体化。需要加深我们对HER2基因遗传学及其与抗HER2治疗疗效关系的理解,以改善这种侵袭性乳腺癌患者的预后。
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