Geoffrey Pecar, Simeng Liu, Jagmohan Hooda, Jennifer M Atkinson, Steffi Oesterreich, Adrian V Lee
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引用次数: 0
摘要
RET 是一种编码在人类第 10 号染色体上的单通道受体酪氨酸激酶,因其在中枢神经系统、肠道神经系统和肾脏的本体发生过程中的作用而为发育生物学领域所熟知。在成人中,RET 改变已被定性为非小细胞肺癌和多种神经内分泌肿瘤的驱动因素。在乳腺癌中,RET 信号网络已被证明会影响多种功能,包括肿瘤发生、转移和耐药性。众所周知,RET 是多种实体瘤发生和发展的驱动因素,但选择性靶向 RET 的治疗药物却相对较新,尽管过去多种多激酶抑制剂已显示出作为 RET 抑制剂的前景;此外,尽管有越来越多的证据表明 RET 在内分泌难治性乳腺癌中起着关键的病理作用,并且反复描述了它与雌激素受体(大多数乳腺癌的主要驱动因素)之间的双向关系,但 RET 作为内分泌难治性乳腺癌的潜在治疗共同靶点却一直被忽视。此外,最近在乳腺癌脑转移灶中发现的 RET 富集现象表明,RET 抑制剂在晚期疾病中发挥着特殊作用。本综述评估了乳腺癌中 RET 的研究现状,并评估了主要乳腺癌亚型中 RET 选择性激酶抑制剂的治疗潜力。
RET signaling in breast cancer therapeutic resistance and metastasis.
RET, a single-pass receptor tyrosine kinase encoded on human chromosome 10, is well known to the field of developmental biology for its role in the ontogenesis of the central and enteric nervous systems and the kidney. In adults, RET alterations have been characterized as drivers of non-small cell lung cancer and multiple neuroendocrine neoplasms. In breast cancer, RET signaling networks have been shown to influence diverse functions including tumor development, metastasis, and therapeutic resistance. While RET is known to drive the development and progression of multiple solid tumors, therapeutic agents selectively targeting RET are relatively new, though multiple multi-kinase inhibitors have shown promise as RET inhibitors in the past; further, RET has been historically neglected as a potential therapeutic co-target in endocrine-refractory breast cancers despite mounting evidence for a key pathologic role and repeated description of a bi-directional relationship with the estrogen receptor, the principal driver of most breast tumors. Additionally, the recent discovery of RET enrichment in breast cancer brain metastases suggests a role for RET inhibition specific to advanced disease. This review assesses the status of research on RET in breast cancer and evaluates the therapeutic potential of RET-selective kinase inhibitors across major breast cancer subtypes.