Role of Alpelisib in the Treatment of PIK3CA-Mutated Breast Cancer: Patient Selection and Clinical Perspectives.

IF 2.3 3区医学 Q2 HEALTH CARE SCIENCES & SERVICES

Therapeutics and Clinical Risk Management Pub Date : 2021-01-01 DOI:10.2147/TCRM.S251668

Dwan-Ying Chang, Wei-Li Ma, Yen-Shen Lu

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引用次数: 26

Abstract

The PI3K/AKT/mTOR pathway has long been known to play a major role in the growth and survival of cancer cells. Breast tumors often harbor PIK3CA gene alterations, which therefore constitute a rational drug target. However, it has taken many years to demonstrate clinically-relevant efficacy of PI3K inhibition and eventually attain regulatory approvals. As data on PI3K inhibitors continue to mature, this review updates and summarizes the current state of the science, including the prognostic role of PIK3CA alterations in breast cancer; the evolution of PI3K inhibitors; the clinical utility of the first-in-class oral selective PI3Kα inhibitor, alpelisib; PIK3CA mutation detection techniques; and adverse effect management. PIK3CA-mutated breast carcinomas predict survival benefit from PI3K inhibitor therapy. The pan-PI3K inhibitor, buparlisib and the beta-isoform-sparing PI3K inhibitor, taselisib, met efficacy endpoints in clinical trials, but pictilisib did not; moreover, poor tolerability of these three drugs abrogated further clinical trials. Alpelisib is better tolerated, with a more manageable toxicity profile; the principal adverse events, hyperglycemia, rash and diarrhea, can be mitigated by intensive monitoring and timely intervention, thereby enabling patients to remain adherent to clinically beneficial treatment. Alpelisib plus endocrine therapy shows promising efficacy for treating postmenopausal women with HR+/HER2- advanced breast cancer. Available evidence supporting using alpelisib after disease progression on first-line endocrine therapy with or without CDK4/6 inhibitors justifies PIK3CA mutation testing upon diagnosing HR+/HER2- advanced breast cancer, which can be done using either tumor tissue or circulating tumor DNA. With appropriate toxicity management and patient selection using validated testing methods, all eligible patients can potentially benefit from this new treatment. Further clinical trials to assess combinations of hormone therapy with PI3K, AKT, mTOR, or CDK 4/6 inhibitors, or studies in men and women with other breast subtypes are ongoing.

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Alpelisib在治疗pik3ca突变乳腺癌中的作用:患者选择和临床观点

人们早就知道PI3K/AKT/mTOR通路在癌细胞的生长和存活中起着重要作用。乳腺肿瘤通常携带PIK3CA基因改变，因此构成合理的药物靶点。然而，证明PI3K抑制的临床相关功效并最终获得监管部门的批准需要很多年的时间。随着PI3K抑制剂的数据不断成熟，本综述更新和总结了当前的科学状况，包括PIK3CA改变在乳腺癌中的预后作用;PI3K抑制剂的进化;口服选择性PI3Kα抑制剂alpelisib的临床应用;PIK3CA突变检测技术;以及不良反应管理。pik3ca突变乳腺癌预测PI3K抑制剂治疗的生存获益在临床试验中，泛PI3K抑制剂布帕利西布和保留β -异构体的PI3K抑制剂taselisib达到了疗效终点，但pictilisib没有达到;此外，这三种药物的耐受性差，取消了进一步的临床试验。Alpelisib耐受性更好，毒性更可控;主要的不良事件，如高血糖、皮疹和腹泻，可以通过加强监测和及时干预来减轻，从而使患者能够坚持临床有益的治疗。Alpelisib联合内分泌疗法治疗绝经后妇女HR+/HER2-晚期乳腺癌疗效良好。现有证据支持在有或没有CDK4/6抑制剂的一线内分泌治疗中，在疾病进展后使用alpelisib，证明在诊断HR+/HER2晚期乳腺癌时进行PIK3CA突变检测是合理的，可以使用肿瘤组织或循环肿瘤DNA进行检测。通过适当的毒性管理和使用有效的测试方法选择患者，所有符合条件的患者都可以从这种新治疗中获益。进一步的临床试验评估激素治疗与PI3K、AKT、mTOR或cdk4 /6抑制剂的联合治疗，或其他乳腺癌亚型的男性和女性研究正在进行中。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Therapeutics and Clinical Risk Management HEALTH CARE SCIENCES & SERVICES-

CiteScore

4.80

自引率

3.60%

发文量

139

审稿时长

16 weeks

期刊介绍： Therapeutics and Clinical Risk Management is an international, peer-reviewed journal of clinical therapeutics and risk management, focusing on concise rapid reporting of clinical studies in all therapeutic areas, outcomes, safety, and programs for the effective, safe, and sustained use of medicines, therapeutic and surgical interventions in all clinical areas. The journal welcomes submissions covering original research, clinical and epidemiological studies, reviews, guidelines, expert opinion and commentary. The journal will consider case reports but only if they make a valuable and original contribution to the literature. As of 18th March 2019, Therapeutics and Clinical Risk Management will no longer consider meta-analyses for publication. The journal does not accept study protocols, animal-based or cell line-based studies.