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Bidirectional Crosstalk between the Estrogen Receptor and Human Epidermal Growth Factor Receptor 2 Signaling Pathways in Breast Cancer: Molecular Basis and Clinical Implications

机译:乳腺癌中雌激素受体和人类表皮生长因子受体2信号通路之间的双向串扰:分子基础和临床意义。

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The estrogen receptor (ER) and/or the human epidermal growth factor receptor 2 (HER2) signaling pathways are the dominant drivers of cell proliferation and survival in the majority of human breast cancers. As a result, targeting these pathways provides the most effective therapies in appropriately selected patients. Nevertheless, resistance to both endocrine and anti-HER2 therapies occurs frequently and represents a major clinical challenge. Compelling preclinical and clinical evidence relates this treatment resistance to the presence of a complex bidirectional molecular crosstalk between the ER and HER2 pathways. As a consequence, treatment strategies targeting either pathway are associated with up-regulation of the other one, ultimately resulting in resistance to therapy. Therefore, a more promising strategy to prevent or overcome either endocrine or anti-HER2 resistance at least in some tumors is to combine targeted treatments that simultaneously block both signaling pathways. Many clinical trials exploring this strategy have shown positive results, and many more are currently ongoing. Future clinical trials with appropriate patient selection, based on biomarker evaluation of primary tumors and possibly of recurrent lesions, are warranted for the optimization of individualized therapeutic strategies.
机译:在大多数人乳腺癌中,雌激素受体(ER)和/或人表皮生长因子受体2(HER2)信号传导途径是细胞增殖和存活的主要驱动因素。其结果是,靶向这些通路提供了在适当选择的患者的最有效的疗法。然而,对内分泌和抗HER2疗法的抗药性经常发生并且代表了主要的临床挑战。令人信服的临床前和临床证据证明这种治疗耐药性与ER和HER2途径之间存在复杂的双向分子串扰有关。结果,靶向任一途径的治疗策略与另一途径的上调相关,最终导致对治疗的抵抗力。因此,至少在某些肿瘤中预防或克服内分泌或抗HER2耐药性的更有前途的策略是结合同时阻断两种信号通路的靶向治疗。探索这种策略的许多临床试验均显示出了积极的结果,而且目前仍在进行中。基于原发性肿瘤以及可能的复发性病变的生物标志物评估,未来有适当患者选择的临床试验有必要进行个性化治疗策略的优化。

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