通用中文 | 阿尔贝利斯 | 通用外文 | Alpelisib |
品牌中文 | 品牌外文 | PIQRAY | |
其他名称 | 靶点PIK3CA,阿博利布,阿培利司 | ||
公司 | 诺华(Novartis) | 产地 | 美国(USA) |
含量 | 150mg | 包装 | 56片/盒 |
剂型给药 | 片剂 口服 | 储存 | 室温 |
适用范围 | 治疗患有晚期或转移性乳腺癌的绝经后女性和男性,为激素受体(HR)阳性,人表皮生长因子受体2 (HER2)阴性,PIK3CA突变,接受内分泌治疗方案之中或之后疾病进展。 |
通用中文 | 阿尔贝利斯 |
通用外文 | Alpelisib |
品牌中文 | |
品牌外文 | PIQRAY |
其他名称 | 靶点PIK3CA,阿博利布,阿培利司 |
公司 | 诺华(Novartis) |
产地 | 美国(USA) |
含量 | 150mg |
包装 | 56片/盒 |
剂型给药 | 片剂 口服 |
储存 | 室温 |
适用范围 | 治疗患有晚期或转移性乳腺癌的绝经后女性和男性,为激素受体(HR)阳性,人表皮生长因子受体2 (HER2)阴性,PIK3CA突变,接受内分泌治疗方案之中或之后疾病进展。 |
片剂 为50mg/150mg/200mg
口服管理· 饭前服用
· 每天大约在同一时间给药
· 吞下整片(不要咀嚼,压碎或分开)
· 如果片剂破损,破裂或不完整,请勿服用
错过剂量
· 错过剂量≤9小时的预定时间:服用原定剂量
· 错过剂量>预定时间9小时:当天略过剂量; 第二天,正常服用
· 如果剂量呕吐,建议当天不要服用额外的剂量; 在通常的时间第二天恢复给药时间表
存储储存温度为20-25°C(68-77°F),允许的温度为15-30°C(59-86°F)
乳腺癌激酶抑制剂与氟维司群联合用于治疗绝经后妇女和男性患有激素受体(HR)阳性,人表皮生长因子受体2(HER2)阴性,PIK3CA突变,晚期或转移性乳腺癌的进展或在以内分泌为基础的方案之后
· Alpelisib 300毫克口服 每天1次和
· 氟维司群500天IM在第1,15和29天,此后每月一次
· 继续治疗直至疾病进展或发生不可接受的毒性
· 请参阅氟维司群的完整说明书信息
剂量调整不良反应的剂量减少指南
· 首剂减量:250 mg 口服 每天1次
· 第二剂量减少:200毫克口服 每天1次
· 胰腺炎仅允许1剂量减少
· 如果需要将剂量减少至200 mg 每天1次以下,则停止治疗
高血糖
· 1级(空腹血糖[FPG]> ULN至160mg / dL OR> ULN至8.9 mmol / L):无需调整剂量; 启动/加强抗糖尿病治疗
· 2级(FPG> 160-250 mg / dL OR> 8.9-13.9 mmol / L)
· 无需调整剂量
· 开始或进一步加强抗糖尿病治疗
· 如果在适当的抗糖尿病治疗下,FPG在21天内未降低≤160mg/ dL或8.9 mmol / L,则将剂量降低1个剂量水平并遵循FPG值特异性推荐
· 3级(FPG> 250-500 mg / dL OR> 13.9-27.8 mmol / L)
· 中断alpelisib开始或加强口服抗糖尿病治疗,并考虑额外的抗糖尿病药物(如胰岛素)1-2天,直到高血糖改善
· 给予IV水合并考虑适当的治疗(例如,干预电解质/酮酸中毒/高渗性紊乱)
· 如果在适当的抗糖尿病治疗下,FPG在3-5天内降至≤160mg/ dL或8.9 mmol / L,则在1个较低剂量水平恢复
· 如果在适当的抗糖尿病治疗下,FPG在3-5天内没有降至≤160mg/ dL或8.9 mmol / L,建议咨询具有高血糖治疗专业知识的医生
· 如果在适当的抗糖尿病治疗后21天内FPG没有降至≤160mg/ dL或8.9 mmol / L,则永久停止治疗
· 4级(FPG> 500 mg / dL或≤27.8mmol/ L.
· 中断alpelisib启动或加强适当的抗糖尿病治疗
· 给予IV水合并考虑适当的治疗(例如,干预电解质/酮酸中毒/高渗性紊乱); 在24小时内按临床指示重新检查FPG
· 如果FPG降至≤500mg/ dL或27.8 mmol / L,请遵循3级高血糖的建议
· 如果确认FPG> 500 mg / dL或27.8 mmol / L,则永久停止治疗
皮疹
· 考虑咨询皮肤科医生,了解所有皮疹的等级
· 1级(<10%BSA,有活性皮肤毒性):无需调整剂量; 开始局部皮质类固醇治疗; 考虑加入口服抗组胺药来控制症状
· 2级(10-30%BSA,有活性皮肤毒性):无需调整剂量; 开始或加强外用皮质类固醇和口服抗组胺药治疗; 考虑低剂量全身皮质类固醇治疗
· 3级(例如严重皮疹对医疗管理无反应;> 30%BSA,有活性皮肤毒性):中断剂量; 开始或加强局部/全身皮质类固醇和口服抗组胺药治疗; 一旦改善至≤1级,在第一次出现时以相同剂量水平恢复alpelisib,或者如果第二次出现则恢复到下一次低剂量水平
· 4级(例如,严重的大疱,水疱或去角质皮肤状况;与广泛的重复感染相关的任何%BSA,指示使用IV抗生素;危及生命的后果):永久停止治疗
腹泻
· 所有等级:根据临床指示启动或加强适当的药物治疗和监测
· 1级:无需调整剂量
· 2级:中断剂量直至恢复到≤1级,然后恢复到相同的剂量水平
· 3级和4级:中断剂量直至恢复到≤1级,然后在下一个较低剂量水平恢复
其他毒性
· 1级或2级:无需调整剂量; 根据临床指示开始适当的药物治疗和监测
· 2级和3级胰腺炎:中断剂量直至恢复至<2级并在下次较低剂量水平恢复; 只允许减少1剂量; 如果毒性再次出现,则永久停止治疗
· 2级升高总胆红素:中断剂量直至恢复至≤1级,如果在≤14天内消退则恢复相同剂量,如果在> 14天内消退则恢复到下一个较低剂量水平
· 3级:中断剂量直至恢复到≤1级,然后在下一个较低剂量水平恢复
· 4级:永久停止治疗
肾功能不全
· 轻度至中度(CrCl 30至<90 mL / min):无需调整剂量
· 严重(CrCl <30 mL / min):药代动力学数据未知
剂量注意事项患者选择
· 根据肿瘤组织或血浆样本中≥1个PIK3CA突变的存在,选择治疗患者
· 基因检测:如果在血浆样本中未检测到突变,则测试肿瘤组织
老年人
· 与年龄<65岁的患者相比,≥65岁的患者3-4级高血糖发生率更高
· 年龄≥75岁的患者:患者数量不足,无法评估安全性和疗效的差异
不良反应> 10%(与氟维司群组合)· 葡萄糖增加(79%)
· 肌酐增加(67%)
· 腹泻(58%)
· 皮疹(52%)
· 淋巴细胞计数下降(52%)
· GGT增加(52%)
· 恶心(45%)
· ALT增加(44%)
· 疲劳(42%)
· 血红蛋白下降(42%)
· 脂肪酶增加(42%)
· 葡萄糖增加,3-4级(39%)
· 食欲下降(36%)
· 口腔炎(30%)
· 呕吐(27%)
· 减重(27%)
· 钙(校正)下降(27%)
· 葡萄糖减少(26%)
· aPTT延长(21%)
· 脱发(20%)
· 皮疹,3-4级(20%)
· 粘膜炎症(19%)
· 瘙痒症(18%)
· 皮肤干燥(18%)
· Dysgeusia(18%)
· 头痛(18%)
· 腹痛(17%)
· 周围水肿(15%)
· 发火(14%)
· 血小板计数下降(14%)
· 钾减少(14%)
· 白蛋白减少(14%)
· 粘膜干燥(12%)
· 消化不良(11%)
· 镁下降(11%)
· GGT增加,3-4级(11%)
1-10%(与氟维司群组合)· 尿路感染(10%)
· 淋巴细胞计数下降,3-4级(8%)
· 腹泻,3-4级(7%)
· 脂肪酶增加,3-4级(7%)
· 钾减少,3-4级(2.1%)
· 疲劳,3-4级(5%)
· 血红蛋白下降,3-4级(4.2%)
· 体重下降,3-4级(3.9%)
· ALT增加,3-4级(3.5%)
· 肌酐增加,3-4级(2.8%)
· 恶心,3-4级(2.5%)
· 口腔炎,3-4级(2.5%)
· 粘膜炎症,3-4级(2.1%)
· 钙(校正)下降(2.1%)
· 腹痛,3-4级(1.4%)
· 血小板计数下降,3-4级(1.1%)
> 1%(与氟维司群组合)· 瘙痒症,3-4级(0.7%)
· 尿路感染,3-4级(0.7%)
· 头痛,3-4级(0.7%)
· 食欲下降,3-4级(0.7%)
· 呕吐,3-4级(0.7%)
· aPTT延长,3-4级(0.7%)
· 干性皮肤,3-4级(0.4%)
· Dysgeusia,3-4级(0.4%)
· 粘膜干燥,3-4级(0.4%)
· 葡萄糖减少,3-4级(0.4%)
· 镁下降,3-4级(0.4%)
禁忌对alpelisib或其任何组分过敏
注意事项报告了严重的超敏反应(如过敏反应,过敏性休克); 症状包括但不限于呼吸困难,潮红,皮疹,发热或心动过速
严重的皮肤反应,包括Stevens-Johnson综合征(SJS)和多形性红斑(EM)报道; 不要接受SJS,EM或中毒性表皮坏死松解症(TEN)的病史; 如果SJS,TEN或EM确认,则永久停止; 不要重新介绍治疗期间曾经历过严重皮肤反应的患者
报道了严重的肺炎,包括急性间质性肺炎和间质性肺病; 考虑非特异性呼吸道症状和体征(如缺氧,咳嗽,呼吸困难或放射性检查时间质浸润)的患者的非感染性肺炎,以及排除感染,肿瘤和其他原因的患者
发生严重腹泻,包括脱水和急性肾损伤; 建议患者开始止泻治疗,增加口服液,并在腹泻发生时通知医务人员
根据动物的发现及其作用机制,给予孕妇时可能会发生胎儿伤害
严重的高血糖症
· 据报道,包括酮症酸中毒在内的严重高血糖症
· 在开始治疗之前,测试FPG和HbA1c,并优化血糖
· 开始后,在前2周至少qWeek监测血糖和/或FPG,然后至少q4周,并按临床指示; 每3个月监测一次HbA1c,并按临床指示进行监测
· 在使用抗糖尿病药物治疗期间,每周至少一次持续监测血糖或FPG,持续8周,然后进行一次q2周和临床指示
药物相互作用概述
· Alpelisib:CYP3A4和BCRP底物; CYP2C9诱导剂
· CYP3A4诱导剂
· 强CYP3A4诱导剂可降低alpelisib浓度和/或活性
· 避免与强CYP3A4诱导剂共同给药
· BCRP抑制剂
· 与BCRP抑制剂共同给药可能会增加alpelisib浓度和/或毒性风险
· 避免与BCRP抑制剂共同给药; 如果无法避免或使用交替药物,请密切监测alpelisib的不良反应
· CYP2C9基板
· 将alpelisib与CYP2C9底物(例如华法林)共同给药可降低CYP2C9底物的血浆浓度
· 当与CYP2C9底物组合使用时,密切监测这些药物可能降低的活性
市场资料
Alpelisib在近日获得了美国FDA的批准,可与FDA批准的内分泌治疗药物氟维司群联合使用,治疗患有晚期或转移性乳腺癌的绝经后女性和男性,这些患者通过FDA批准的试验检测为激素受体(HR)阳性,人表皮生长因子受体2 (HER2)阴性,PIK3CA突变,接受内分泌治疗方案之中或之后疾病进展。
该药物是一款口服小分子α特异性PI3K抑制剂,它的主要作用在于在携带PIK3CA基因突变的乳腺癌细胞系中显示出抑制PI3K通路的潜力,并具有抑制细胞增殖作用。在HR+/HER2-晚期乳腺癌中,PI3K通路的改变是肿瘤恶化、疾病进展和产生治疗耐药性的最常见原因。大约40%的HR+/HER2-晚期乳腺癌患者携带PIK3CA基因突变。
一项名为SOLAR-1的研究为此次批准提供了有力的依据,SOLAR-1研究是一项入组了572例绝经后ER+/HER2-晚期乳腺癌患者的Ⅲ期全球多中心临床研究,这些患者均接受芳香化酶抑制剂(AI)治疗的过程中或治疗后复发或进展,肿瘤组织法检测明确PIK3CA状态。
SOLAR-1研究分为2个队列,队列1入组PIK3CA的患者341例,队列2入组PIK3CA非突变患者231例,两个队列的患者均随机1:1分配接受氟维司群联合alpelisib或氟维司群单药治疗,直至疾病进展或不可耐受的毒性。
研究达到主要终点,在PIK3CA突变患者中,氟维司群+alpelisib对比氟维司群单药治疗,显著延长患者PFS,mPFS分别为11.0个月和5.7个月(HR=0.65;95%CI 0.50~0.85; P=0.00065) 。即对比氟维司群单药治疗,氟维司群联合alpelisib方案降低了35%的疾病进展或死亡风险。两组的mPFS分别为11.0个月和3.7个月,(HR=0.48;95%CI 0.32~0.71)。亚组分析结果显示,在所有亚组中均观察到显著一致的疗效,氟维司群联合alpelisib方案的PFS显著更优。在PIK3CA突变队列中,对比两组的ORR,也观察到氟维司群联合alpelisib组的ORR显著更优。
片剂 为50mg/150mg/200mg
口服管理· 饭前服用
· 每天大约在同一时间给药
· 吞下整片(不要咀嚼,压碎或分开)
· 如果片剂破损,破裂或不完整,请勿服用
错过剂量
· 错过剂量≤9小时的预定时间:服用原定剂量
· 错过剂量>预定时间9小时:当天略过剂量; 第二天,正常服用
· 如果剂量呕吐,建议当天不要服用额外的剂量; 在通常的时间第二天恢复给药时间表
存储储存温度为20-25°C(68-77°F),允许的温度为15-30°C(59-86°F)
乳腺癌激酶抑制剂与氟维司群联合用于治疗绝经后妇女和男性患有激素受体(HR)阳性,人表皮生长因子受体2(HER2)阴性,PIK3CA突变,晚期或转移性乳腺癌的进展或在以内分泌为基础的方案之后
· Alpelisib 300毫克口服 每天1次和
· 氟维司群500天IM在第1,15和29天,此后每月一次
· 继续治疗直至疾病进展或发生不可接受的毒性
· 请参阅氟维司群的完整说明书信息
剂量调整不良反应的剂量减少指南
· 首剂减量:250 mg 口服 每天1次
· 第二剂量减少:200毫克口服 每天1次
· 胰腺炎仅允许1剂量减少
· 如果需要将剂量减少至200 mg 每天1次以下,则停止治疗
高血糖
· 1级(空腹血糖[FPG]> ULN至160mg / dL OR> ULN至8.9 mmol / L):无需调整剂量; 启动/加强抗糖尿病治疗
· 2级(FPG> 160-250 mg / dL OR> 8.9-13.9 mmol / L)
· 无需调整剂量
· 开始或进一步加强抗糖尿病治疗
· 如果在适当的抗糖尿病治疗下,FPG在21天内未降低≤160mg/ dL或8.9 mmol / L,则将剂量降低1个剂量水平并遵循FPG值特异性推荐
· 3级(FPG> 250-500 mg / dL OR> 13.9-27.8 mmol / L)
· 中断alpelisib开始或加强口服抗糖尿病治疗,并考虑额外的抗糖尿病药物(如胰岛素)1-2天,直到高血糖改善
· 给予IV水合并考虑适当的治疗(例如,干预电解质/酮酸中毒/高渗性紊乱)
· 如果在适当的抗糖尿病治疗下,FPG在3-5天内降至≤160mg/ dL或8.9 mmol / L,则在1个较低剂量水平恢复
· 如果在适当的抗糖尿病治疗下,FPG在3-5天内没有降至≤160mg/ dL或8.9 mmol / L,建议咨询具有高血糖治疗专业知识的医生
· 如果在适当的抗糖尿病治疗后21天内FPG没有降至≤160mg/ dL或8.9 mmol / L,则永久停止治疗
· 4级(FPG> 500 mg / dL或≤27.8mmol/ L.
· 中断alpelisib启动或加强适当的抗糖尿病治疗
· 给予IV水合并考虑适当的治疗(例如,干预电解质/酮酸中毒/高渗性紊乱); 在24小时内按临床指示重新检查FPG
· 如果FPG降至≤500mg/ dL或27.8 mmol / L,请遵循3级高血糖的建议
· 如果确认FPG> 500 mg / dL或27.8 mmol / L,则永久停止治疗
皮疹
· 考虑咨询皮肤科医生,了解所有皮疹的等级
· 1级(<10%BSA,有活性皮肤毒性):无需调整剂量; 开始局部皮质类固醇治疗; 考虑加入口服抗组胺药来控制症状
· 2级(10-30%BSA,有活性皮肤毒性):无需调整剂量; 开始或加强外用皮质类固醇和口服抗组胺药治疗; 考虑低剂量全身皮质类固醇治疗
· 3级(例如严重皮疹对医疗管理无反应;> 30%BSA,有活性皮肤毒性):中断剂量; 开始或加强局部/全身皮质类固醇和口服抗组胺药治疗; 一旦改善至≤1级,在第一次出现时以相同剂量水平恢复alpelisib,或者如果第二次出现则恢复到下一次低剂量水平
· 4级(例如,严重的大疱,水疱或去角质皮肤状况;与广泛的重复感染相关的任何%BSA,指示使用IV抗生素;危及生命的后果):永久停止治疗
腹泻
· 所有等级:根据临床指示启动或加强适当的药物治疗和监测
· 1级:无需调整剂量
· 2级:中断剂量直至恢复到≤1级,然后恢复到相同的剂量水平
· 3级和4级:中断剂量直至恢复到≤1级,然后在下一个较低剂量水平恢复
其他毒性
· 1级或2级:无需调整剂量; 根据临床指示开始适当的药物治疗和监测
· 2级和3级胰腺炎:中断剂量直至恢复至<2级并在下次较低剂量水平恢复; 只允许减少1剂量; 如果毒性再次出现,则永久停止治疗
· 2级升高总胆红素:中断剂量直至恢复至≤1级,如果在≤14天内消退则恢复相同剂量,如果在> 14天内消退则恢复到下一个较低剂量水平
· 3级:中断剂量直至恢复到≤1级,然后在下一个较低剂量水平恢复
· 4级:永久停止治疗
肾功能不全
· 轻度至中度(CrCl 30至<90 mL / min):无需调整剂量
· 严重(CrCl <30 mL / min):药代动力学数据未知
剂量注意事项患者选择
· 根据肿瘤组织或血浆样本中≥1个PIK3CA突变的存在,选择治疗患者
· 基因检测:如果在血浆样本中未检测到突变,则测试肿瘤组织
老年人
· 与年龄<65岁的患者相比,≥65岁的患者3-4级高血糖发生率更高
· 年龄≥75岁的患者:患者数量不足,无法评估安全性和疗效的差异
不良反应> 10%(与氟维司群组合)· 葡萄糖增加(79%)
· 肌酐增加(67%)
· 腹泻(58%)
· 皮疹(52%)
· 淋巴细胞计数下降(52%)
· GGT增加(52%)
· 恶心(45%)
· ALT增加(44%)
· 疲劳(42%)
· 血红蛋白下降(42%)
· 脂肪酶增加(42%)
· 葡萄糖增加,3-4级(39%)
· 食欲下降(36%)
· 口腔炎(30%)
· 呕吐(27%)
· 减重(27%)
· 钙(校正)下降(27%)
· 葡萄糖减少(26%)
· aPTT延长(21%)
· 脱发(20%)
· 皮疹,3-4级(20%)
· 粘膜炎症(19%)
· 瘙痒症(18%)
· 皮肤干燥(18%)
· Dysgeusia(18%)
· 头痛(18%)
· 腹痛(17%)
· 周围水肿(15%)
· 发火(14%)
· 血小板计数下降(14%)
· 钾减少(14%)
· 白蛋白减少(14%)
· 粘膜干燥(12%)
· 消化不良(11%)
· 镁下降(11%)
· GGT增加,3-4级(11%)
1-10%(与氟维司群组合)· 尿路感染(10%)
· 淋巴细胞计数下降,3-4级(8%)
· 腹泻,3-4级(7%)
· 脂肪酶增加,3-4级(7%)
· 钾减少,3-4级(2.1%)
· 疲劳,3-4级(5%)
· 血红蛋白下降,3-4级(4.2%)
· 体重下降,3-4级(3.9%)
· ALT增加,3-4级(3.5%)
· 肌酐增加,3-4级(2.8%)
· 恶心,3-4级(2.5%)
· 口腔炎,3-4级(2.5%)
· 粘膜炎症,3-4级(2.1%)
· 钙(校正)下降(2.1%)
· 腹痛,3-4级(1.4%)
· 血小板计数下降,3-4级(1.1%)
> 1%(与氟维司群组合)· 瘙痒症,3-4级(0.7%)
· 尿路感染,3-4级(0.7%)
· 头痛,3-4级(0.7%)
· 食欲下降,3-4级(0.7%)
· 呕吐,3-4级(0.7%)
· aPTT延长,3-4级(0.7%)
· 干性皮肤,3-4级(0.4%)
· Dysgeusia,3-4级(0.4%)
· 粘膜干燥,3-4级(0.4%)
· 葡萄糖减少,3-4级(0.4%)
· 镁下降,3-4级(0.4%)
禁忌对alpelisib或其任何组分过敏
注意事项报告了严重的超敏反应(如过敏反应,过敏性休克); 症状包括但不限于呼吸困难,潮红,皮疹,发热或心动过速
严重的皮肤反应,包括Stevens-Johnson综合征(SJS)和多形性红斑(EM)报道; 不要接受SJS,EM或中毒性表皮坏死松解症(TEN)的病史; 如果SJS,TEN或EM确认,则永久停止; 不要重新介绍治疗期间曾经历过严重皮肤反应的患者
报道了严重的肺炎,包括急性间质性肺炎和间质性肺病; 考虑非特异性呼吸道症状和体征(如缺氧,咳嗽,呼吸困难或放射性检查时间质浸润)的患者的非感染性肺炎,以及排除感染,肿瘤和其他原因的患者
发生严重腹泻,包括脱水和急性肾损伤; 建议患者开始止泻治疗,增加口服液,并在腹泻发生时通知医务人员
根据动物的发现及其作用机制,给予孕妇时可能会发生胎儿伤害
严重的高血糖症
· 据报道,包括酮症酸中毒在内的严重高血糖症
· 在开始治疗之前,测试FPG和HbA1c,并优化血糖
· 开始后,在前2周至少qWeek监测血糖和/或FPG,然后至少q4周,并按临床指示; 每3个月监测一次HbA1c,并按临床指示进行监测
· 在使用抗糖尿病药物治疗期间,每周至少一次持续监测血糖或FPG,持续8周,然后进行一次q2周和临床指示
药物相互作用概述
· Alpelisib:CYP3A4和BCRP底物; CYP2C9诱导剂
· CYP3A4诱导剂
· 强CYP3A4诱导剂可降低alpelisib浓度和/或活性
· 避免与强CYP3A4诱导剂共同给药
· BCRP抑制剂
· 与BCRP抑制剂共同给药可能会增加alpelisib浓度和/或毒性风险
· 避免与BCRP抑制剂共同给药; 如果无法避免或使用交替药物,请密切监测alpelisib的不良反应
· CYP2C9基板
· 将alpelisib与CYP2C9底物(例如华法林)共同给药可降低CYP2C9底物的血浆浓度
· 当与CYP2C9底物组合使用时,密切监测这些药物可能降低的活性
市场资料
Alpelisib在近日获得了美国FDA的批准,可与FDA批准的内分泌治疗药物氟维司群联合使用,治疗患有晚期或转移性乳腺癌的绝经后女性和男性,这些患者通过FDA批准的试验检测为激素受体(HR)阳性,人表皮生长因子受体2 (HER2)阴性,PIK3CA突变,接受内分泌治疗方案之中或之后疾病进展。
该药物是一款口服小分子α特异性PI3K抑制剂,它的主要作用在于在携带PIK3CA基因突变的乳腺癌细胞系中显示出抑制PI3K通路的潜力,并具有抑制细胞增殖作用。在HR+/HER2-晚期乳腺癌中,PI3K通路的改变是肿瘤恶化、疾病进展和产生治疗耐药性的最常见原因。大约40%的HR+/HER2-晚期乳腺癌患者携带PIK3CA基因突变。
一项名为SOLAR-1的研究为此次批准提供了有力的依据,SOLAR-1研究是一项入组了572例绝经后ER+/HER2-晚期乳腺癌患者的Ⅲ期全球多中心临床研究,这些患者均接受芳香化酶抑制剂(AI)治疗的过程中或治疗后复发或进展,肿瘤组织法检测明确PIK3CA状态。
SOLAR-1研究分为2个队列,队列1入组PIK3CA的患者341例,队列2入组PIK3CA非突变患者231例,两个队列的患者均随机1:1分配接受氟维司群联合alpelisib或氟维司群单药治疗,直至疾病进展或不可耐受的毒性。
研究达到主要终点,在PIK3CA突变患者中,氟维司群+alpelisib对比氟维司群单药治疗,显著延长患者PFS,mPFS分别为11.0个月和5.7个月(HR=0.65;95%CI 0.50~0.85; P=0.00065) 。即对比氟维司群单药治疗,氟维司群联合alpelisib方案降低了35%的疾病进展或死亡风险。两组的mPFS分别为11.0个月和3.7个月,(HR=0.48;95%CI 0.32~0.71)。亚组分析结果显示,在所有亚组中均观察到显著一致的疗效,氟维司群联合alpelisib方案的PFS显著更优。在PIK3CA突变队列中,对比两组的ORR,也观察到氟维司群联合alpelisib组的ORR显著更优。
HIGHLIGHTS OF PRESCRIBING INFORMATION
These highlights do not include all the information needed to use PIQRAY safely and effectively. See full prescribing information for PIQRAY.
PIQRAY® (alpelisib) tablets, for oral use
Initial U.S. Approval: 2019
-----------------------------INDICATIONS AND USAGE--------------------------
PIQRAY is a kinase inhibitor indicated in combination with fulvestrant for the treatment of postmenopausal women, and men, with hormone receptor (HR)-positive, human epidermal growth factor receptor 2 (HER2)-negative, PIK3CA-mutated, advanced or metastatic breast cancer as detected by an FDA-approved test following progression on or after an endocrine-based regimen. (1)
----------------------DOSAGE AND ADMINISTRATION------------------------
Recommended dose: 300 mg (two 150 mg tablets) taken orally once daily with food. (2.2)
For adverse reactions, consider dose interruption, dose reduction, or discontinuation. (2.3)
---------------------DOSAGE FORMS AND STRENGTHS--------------------- Tablets: 50 mg, 150 mg, 200 mg (3)
-------------------------------CONTRAINDICATIONS----------------------------- Severe hypersensitivity to PIQRAY or to any of its components (4).
-----------------------WARNINGS AND PRECAUTIONS-----------------------
Severe Hypersensitivity: Permanently discontinue PIQRAY. Promptly initiate appropriate treatment. (5.1)
Severe Cutaneous Reactions: Cases of severe cutaneous reactions, including Stevens-Johnson syndrome (SJS) and Erythema Multiforme (EM) were reported. Do not initiate treatment in patients with a history of SJS, EM, or Toxic Epidermal Necrolysis (TEN). Interrupt PIQRAY if signs or symptoms of severe cutaneous reactions are present, until etiology of the reaction has been determined. Consider consultation with a dermatologist. Permanently discontinue PIQRAY if SJS, EM, or TEN is confirmed. (5.2)
Hyperglycemia: Severe hyperglycemia, including ketoacidosis, was reported. The safety of PIQRAY in patients with Type 1 or uncontrolled Type 2 diabetes has not been established. Before initiating treatment with PIQRAY, test fasting plasma glucose (FPG), HbA1c, and optimize blood glucose. After initiating treatment, monitor periodically. Initiate or optimize anti-hyperglycemic medications as clinically indicated. Interrupt, reduce dose, or discontinue PIQRAY if severe hyperglycemia occurs. (2.3, 5.3)
Pneumonitis: Severe cases of pneumonitis and interstitial lung disease have been reported. Monitor for clinical symptoms or radiological changes. Interrupt or discontinue PIQRAY if severe pneumonitis occurs. (2.3, 5.4)
Diarrhea: Severe cases of diarrhea, including dehydration and acute kidney injury, have been reported. Most patients experience diarrhea (Grade ≤ 2) during treatment with PIQRAY. Advise patients to start antidiarrheal treatment, increase oral fluids, and notify their healthcare provider if diarrhea occurs. Interrupt, reduce dose, or discontinue PIQRAY if severe diarrhea occurs. (2.3, 5.5)
Embryo-Fetal Toxicity: PIQRAY can cause fetal harm. Advise patients of potential risk to a fetus and to use effective contraception (5.6, 8.1, 8.3). Also, refer to the Full Prescribing Information of fulvestrant for pregnancy and contraception information.
------------------------------ADVERSE REACTIONS------------------------------
Most common adverse reactions including laboratory abnormalities (all grades, incidence ≥ 20%) were glucose increased, creatinine increased, diarrhea, rash, lymphocyte count decreased, GGT increased, nausea, ALT increased, fatigue, hemoglobin decreased, lipase increased, decreased appetite, stomatitis, vomiting, weight decreased, calcium decreased, glucose decreased, aPTT prolonged, and alopecia (6.1).
To report SUSPECTED ADVERSE REACTIONS, contact Novartis Pharmaceuticals Corporation at 1-888-669-6682 or FDA at 1-800-FDA-1088 or www.fda.gov/medwatch.
------------------------------DRUG INTERACTIONS------------------------------
CYP3A4 Inducers: Avoid coadministration of PIQRAY with a strong CYP3A4 inducer. (7.1)
BCRP Inhibitors: Avoid the use of BCRP inhibitors in patients treated with PIQRAY. If unable to use alternative drugs, closely monitor for increased adverse reactions. (7.1)
CYP2C9 Substrates: Closely monitor when PIQRAY is coadministered with CYP2C9 substrates where decreases in the plasma concentration of these drugs may reduce activity. (7.2)
----------------------------USE IN SPECIFIC POPULATIONS------------------ Lactation: Advise not to breastfeed. (8.2)
See 17 for PATIENT COUNSELING INFORMATION and FDA-approved patient labeling.
Revised: 5/2019
FULL PRESCRIBING INFORMATION: CONTENTS*
1 INDICATIONS AND USAGE
2 DOSAGE AND ADMINISTRATION
2.1Patient Selection
2.2Dosage and Administration
2.3Dose Modifications for Adverse Reactions
3 DOSAGE FORMS AND STRENGTHS
4 CONTRAINDICATIONS
5 WARNINGS AND PRECAUTIONS
5.1Severe Hypersensitivity
5.2Severe Cutaneous Reactions
5.3Hyperglycemia
5.4Pneumonitis
5.5Diarrhea
5.6Embryo-Fetal Toxicity
6 ADVERSE REACTIONS
6.1Clinical Trial Experience
7 DRUG INTERACTIONS
7.1Effect of Other Drugs on PIQRAY
7.2Effect of PIQRAY on Other Drugs
8 USE IN SPECIFIC POPULATIONS
8.1Pregnancy
8.2Lactation
8.3 Females and Males of Reproductive Potential
8.4 Pediatric Use
8.5 Geriatric Use
8.6 Renal Impairment
10 OVERDOSAGE
11 DESCRIPTION
12 CLINICAL PHARMACOLOGY 12.1 Mechanism of Action
12.2 Pharmacodynamics
12.3 Pharmacokinetics
13 NONCLINICAL TOXICOLOGY
13.1 Carcinogenesis, Mutagenesis, Impairment of Fertility
14 CLINICAL STUDIES
16 HOW SUPPLIED/STORAGE AND HANDLING
17 PATIENT COUNSELING INFORMATION
*Sections or subsections omitted from the full prescribing information are not listed.
FULL PRESCRIBING INFORMATION
1 INDICATIONS AND USAGE
PIQRAY is indicated in combination with fulvestrant for the treatment of postmenopausal women, and men, with hormone receptor (HR)-positive, human epidermal growth factor receptor 2 (HER2)-negative, PIK3CA-mutated, advanced or metastatic breast cancer as detected by an FDA-approved test following progression on or after an endocrine-based regimen.
2 DOSAGE AND ADMINISTRATION
2.1 Patient Selection
Select patients for the treatment of HR-positive, HER2-negative advanced or metastatic breast cancer with PIQRAY, based on the presence of one or more PIK3CA mutations in tumor tissue or plasma specimens[see Clinical Studies (14)]. If no mutation is detected in a plasma specimen, test tumor tissue. Information on FDA-approved tests for the detection of PIK3CA mutations in breast cancer is available at: http://www.fda.gov/CompanionDiagnostics.
2.2 Dosage and Administration
The recommended dose of PIQRAY is 300 mg (two 150 mg film-coated tablets) taken orally, once daily, with food[see Clinical Pharmacology (12.3)].
Continue treatment until disease progression or unacceptable toxicity occurs[see Dosage and Administration (2.3)].
Patients should take their dose of PIQRAY at approximately the same time each day.
Swallow PIQRAY tablets whole (tablets should not be chewed, crushed or split prior to swallowing). No tablet should be ingested if it is broken, cracked, or otherwise not intact.
If a dose of PIQRAY is missed, it can be taken with food within 9 hours after the time it is usually taken. After more than 9 hours, skip the dose for that day. The next day, take PIQRAY at the usual time.
If the patient vomits after taking the dose, advise the patient not to take an additional dose on that day, and to resume the dosing schedule the next day at the usual time.
When given with PIQRAY, the recommended dose of fulvestrant is 500 mg administered on Days 1, 15, and 29, and once monthly thereafter. Refer to the Full Prescribing Information for fulvestrant.
2.3 Dose Modifications for Adverse Reactions
The recommended dose modifications for adverse reactions (ARs) are listed in Table 1.
Table 1: PIQRAY Dose Reduction Guidelines for Adverse Reactions1
PIQRAY Dose Level |
Dose and Schedule |
Number and Strength of Tablets |
|
|
|
Starting dose |
300 mg once daily |
Two 150 mg tablets |
|
|
|
First-dose reduction |
250 mg once daily |
One 200 mg tablet and one 50 mg tablet |
|
|
|
Second-dose reduction |
200 mg once daily2 |
One 200 mg tablet |
1Only one dose reduction is permitted for pancreatitis.
2If further dose reduction below 200 mg once daily is required, discontinue PIQRAY.
Tables 2, 3, 4, and 5 summarize recommendations for dose interruption, reduction, or discontinuation of PIQRAY in the management of specific ARs.
Hyperglycemia
Table 2: Dose Modification and Management for Hyperglycemia
Fasting Plasma Glucose |
Recommendation |
(FPG)/Blood Glucose |
|
Values1 |
|
Grade 1 |
No PIQRAY dose adjustment required. |
FPG > ULN-160 mg/dL |
Initiate or intensify anti-diabetic treatment2. |
or > ULN-8.9 mmol/L |
|
Grade 2 |
No PIQRAY dose adjustment required. |
|
|
FPG > 160-250 mg/dL or > |
Initiate or further intensify anti-diabetic treatment2. |
8.9-13.9 mmol/L |
If FPG does not decrease to ≤ 160 mg/dL or 8.9 mmol/L within 21 days under appropriate anti- |
|
|
|
diabetic treatment, reduce PIQRAY dose by 1 dose level and follow FPG value specific |
|
recommendations. |
Grade 3 |
Interrupt PIQRAY. |
> 250-500 mg/dL |
Initiate or intensify oral anti-diabetic treatment2 and consider additional anti-diabetic medications3 |
or > 13.9-27.8 mmol/L |
for 1-2 days until hyperglycemia improves. |
|
Administer intravenous hydration and consider appropriate treatment (e.g., intervention for |
|
electrolyte/ketoacidosis/hyperosmolar disturbances). |
|
If FPG decreases to ≤ 160 mg/dL or 8.9 mmol/L within 3 to 5 days under appropriate anti-diabetic |
|
treatment, resume PIQRAY at 1 lower dose level. |
|
If FPG does not decrease to ≤ 160 mg/dL or 8.9 mmol/L within 3 to 5 days under appropriate anti- |
|
diabetic treatment, consultation with a physician with expertise in the treatment of hyperglycemia is |
|
recommended. |
|
If FPG does not decrease to ≤ 160 mg/dL or 8.9 mmol/L within 21 days following appropriate anti- |
|
diabetic treatment2, permanently discontinue PIQRAY treatment. |
Grade 4 |
Interrupt PIQRAY. |
> 500 mg/dL |
Initiate or intensify appropriate anti-diabetic treatment2 (administer intravenous hydration and |
or ≥ 27.8 mmol/L |
consider appropriate treatment (e.g., intervention for electrolyte/ketoacidosis/hyperosmolar |
|
disturbances)), re-check FPG within 24 hours and as clinically indicated. |
|
If FPG decreases to ≤ 500 mg/dL or 27.8 mmol/L, follow FPG value specific recommendations for |
|
Grade 3. |
|
If FPG is confirmed at > 500 mg/dL or 27.8 mmol/L, permanently discontinue PIQRAY treatment. |
1FPG/Blood Glucose/Grade levels reflect hyperglycemia grading according to CTCAE Version 4.03 (CTCAE=Common Terminology Criteria for Adverse Events)
2Initiate applicable anti-diabetic medications, including metformin and insulin sensitizers (such as thiazolidinediones or dipeptidyl peptidase-4 inhibitors), and review respective prescribing information for dosing and dose titration recommendations, including local diabetic treatment guidelines. Metformin was recommended in the SOLAR-1 trial with the following guidance:Initiate metformin 500 mg once daily. Based on tolerability, metformin dose may be increased to 500 mg twice daily, followed by 500 mg with breakfast, and 1000 mg with dinner, followed by further increase to 1000 mg twice daily if needed [see Warnings and Precautions (5.3)].
3As recommended in the SOLAR-1 trial, insulin may be used for 1-2 days until hyperglycemia resolves. However, this may not be necessary in the majority of PIQRAY-induced hyperglycemia, given the short half-life of PIQRAY and the expectation of glucose levels normalizing after interruption of PIQRAY.
Rash
Table 3: Dose Modification and Management for Rash
Grade1,2 |
Recommendation3 |
Grade 1 |
No PIQRAY dose adjustment required. |
(< 10% body surface area |
Initiate topical corticosteroid treatment. |
(BSA) with active skin |
Consider adding oral antihistamine to manage symptoms. |
toxicity) |
|
|
|
Grade 2 |
No PIQRAY dose adjustment required. |
(10-30% BSA with active |
Initiate or intensify topical corticosteroid and oral antihistamine treatment. |
skin toxicity) |
|
Consider low dose systemic corticosteroid treatment. |
|
|
|
Grade 3 (e.g., severe rash not |
Interrupt PIQRAY. |
responsive to medical |
Initiate or intensify topical/systemic corticosteroid and oral antihistamine treatment. |
management) |
|
|
|
(> 30% BSA with active skin |
Once improved to ≤ Grade 1, resume PIQRAY at the same dose level for first occurrence of |
rash, or at next lower dose level in case of second occurrence. |
|
toxicity) |
|
|
|
Grade 4 (e.g., severe bullous, |
Permanently discontinue PIQRAY. |
blistering or exfoliating skin |
|
conditions) |
|
(any % BSA associated with |
|
extensive superinfection, with |
|
IV antibiotics indicated; life- |
|
threatening consequences) |
|
1Grading according to CTCAE Version 5.0
2For all grades of rash, consider consultation with a dermatologist.
3Antihistamines administered prior to rash onset may decrease incidence and severity of rash based on the SOLAR-1 trial.
Diarrhea
Table 4: Dose Modification and Management for Diarrhea
Grade1 |
Recommendation |
Grade 1 |
No PIQRAY dose adjustment is required. Initiate appropriate medical therapy and monitor as clinically |
|
indicated. |
Grade 2 |
Initiate or intensify appropriate medical therapy and monitor as clinically indicated. Interrupt PIQRAY dose |
|
until recovery to Grade ≤ 1, then resume PIQRAY at same dose level. |
Grade 3 and 4 |
Initiate or intensify appropriate medical therapy and monitor as clinically indicated. Interrupt PIQRAY dose |
|
until recovery to Grade ≤ 1, then resume PIQRAY at the next lower dose level. |
1Grading according to CTCAE Version 5.0.
Other Toxicities
Table 5: Dose Modification and Management for Other Toxicities (Excluding Hyperglycemia, Rash, and Diarrhea)
Grade1 |
Recommendation |
Grade 1 or 2 |
No PIQRAY dose adjustment is required. Initiate appropriate medical therapy and monitor as clinically |
|
indicated2,3. |
Grade 3 |
Interrupt PIQRAY dose until recovery to Grade ≤ 1, then resume PIQRAY at the next lower dose level. |
Grade 4 |
Permanently discontinue PIQRAY. |
1Grading according to CTCAE Version 5.0
2For Grade 2 and 3 pancreatitis, interrupt PIQRAY dose until recovery to Grade < 2 and resume at next lower dose level. Only one dose reduction is permitted. If toxicity reoccurs, permanently discontinue PIQRAY treatment.
3For Grade 2 total bilirubin elevation, interrupt PIQRAY dose until recovery to Grade ≤ 1 and resume at the same dose if resolved in ≤ 14 days or resume at the next lower dose level if resolved in > 14 days.
Refer to the Full Prescribing Information of fulvestrant for dose modification guidelines in the event of toxicity and for other relevant safety information.
3 DOSAGE FORMS AND STRENGTHS Tablets: 50 mg, 150 mg, and 200 mg alpelisib
50 mg: Light pink, unscored, round and curved with beveled edges film-coated tablet, imprinted with “L7” on one side and “NVR” on the other side.
150 mg: Pale red, unscored, ovaloid and curved with beveled edges film-coated tablet, imprinted with “UL7” on one side and “NVR” on the other side.
200 mg: Light red, unscored, ovaloid and curved with beveled edges film-coated tablet, imprinted with “YL7” on one side and “NVR” on the other side.
4 CONTRAINDICATIONS
PIQRAY is contraindicated in patients with severe hypersensitivity to it or any of its components[see Warnings and Precautions (5.1)].
5 WARNINGS AND PRECAUTIONS
5.1 Severe Hypersensitivity
Severe hypersensitivity reactions, including anaphylaxis and anaphylactic shock, were reported in patients treated with PIQRAY. Severe hypersensitivity reactions were manifested by symptoms including, but not limited to, dyspnea, flushing, rash, fever, or tachycardia.
The incidence of Grade 3 and 4 hypersensitivity reactions was 0.7%[see Adverse Reactions (6)].
Advise patients of the signs and symptoms of severe hypersensitivity reactions. Permanently discontinue PIQRAY in the event of severe hypersensitivity.
5.2 Severe Cutaneous Reactions
Severe cutaneous reactions, including Stevens-Johnson Syndrome (SJS) and Erythema Multiforme (EM) were reported in patients treated with PIQRAY[see Adverse Reactions (6)].
SJS and EM were reported in 0.4% and 1.1% of patients, respectively. Do not initiate PIQRAY treatment in patients with a history of SJS, EM, or Toxic Epidermal Necrolysis (TEN).
If signs or symptoms of severe cutaneous reactions occur, interrupt PIQRAY until the etiology of the reaction has been determined. Consultation with a dermatologist is recommended.
If SJS, TEN, or EM is confirmed, permanently discontinue PIQRAY. Do not reintroduce PIQRAY in patients who have experienced previous severe cutaneous reactions during PIQRAY treatment.
If SJS, TEN, or EM is not confirmed, PIQRAY may require dose modifications, topical corticosteroids, or oral antihistamine treatment as described in Table 3[see Dosage and Administration (2.3)].
Advise patients of the signs and symptoms of severe cutaneous reactions (e.g., a prodrome of fever, flu-like symptoms, mucosal lesions or progressive skin rash).
5.3 Hyperglycemia
Severe hyperglycemia, including ketoacidosis, has been reported in patients treated with PIQRAY. Hyperglycemia was reported in 65% of patients treated with PIQRAY. Grade 3 (FPG > 250-500 mg/dL) and Grade 4 (FPG > 500 mg/dL) hyperglycemia was reported in 33% and 3.9% of patients, respectively. Ketoacidosis was reported in 0.7% of patients (n = 2) treated with PIQRAY.
Among the patients who experienced Grade ≥ 2 (FPG 160-250 mg/dL) hyperglycemia, the median time to first occurrence of hyperglycemia was 15 days (range: 5 to 517 days).
In the 187 patients with hyperglycemia, 87% (163/187) were managed with anti-diabetic medication, and 76% (142/187) reported use of metformin as single agent or in combination with other anti-diabetic medication [i.e., insulin, dipeptidyl peptidase-4 (DPP-4) inhibitors, and sulfonylureas]. In patients with Grade ≥ 2 hyperglycemia with at least 1 grade improvement (n = 153), median time to improvement from the first event was 8 days (range: 2 to 65 days).
In all patients with elevated FPG who continued fulvestrant treatment after discontinuing PIQRAY (n = 54), 96% (n = 52) of patients had FPG levels that returned to baseline.
Before initiating treatment with PIQRAY, test FPG, HbA1c, and optimize blood glucose. After initiating treatment with PIQRAY, monitor blood glucose and/or FPG at least once every week for the first 2 weeks, then at least once every 4 weeks, and as clinically indicated. Monitor HbA1c every 3 months and as clinically indicated.
If a patient experiences hyperglycemia after initiating treatment with PIQRAY, monitor blood glucose and/or FPG as clinically indicated, and at least twice weekly until blood glucose or FPG decreases to normal levels. During treatment with anti-diabetic medication, continue monitoring blood glucose or FPG at least once a week for 8 weeks, followed by once every 2 weeks and as clinically indicated. Consider consultation with a healthcare practitioner with expertise in the treatment of hyperglycemia and counsel patients on lifestyle changes.
The safety of PIQRAY in patients with Type 1 and uncontrolled Type 2 diabetes has not been established as these patients were excluded from the SOLAR-1 trial. Patients with a medical history of Type 2 diabetes were included. Patients with a history of diabetes mellitus may require intensified diabetic treatment. Closely monitor patients with diabetes.
Based on the severity of the hyperglycemia, PIQRAY may require dose interruption, reduction, or discontinuation as described in Table 2[see Dosage and Administration (2.3)].
Advise patients of the signs and symptoms of hyperglycemia (e.g., excessive thirst, urinating more often than usual or higher amount of urine than usual, or increased appetite with weight loss).
5.4 Pneumonitis
Severe pneumonitis, including acute interstitial pneumonitis and interstitial lung disease, has been reported in patients treated with PIQRAY.
Pneumonitis was reported in 1.8% of patients treated with PIQRAY.
In patients who have new or worsening respiratory symptoms or are suspected to have developed pneumonitis, interrupt PIQRAY immediately and evaluate the patient for pneumonitis. Consider a diagnosis of non-infectious pneumonitis in patients presenting with non-specific respiratory signs and symptoms such as hypoxia, cough, dyspnea, or interstitial infiltrates on radiologic exams and in whom infectious, neoplastic, and other causes have been excluded by means of appropriate investigations.
Permanently discontinue PIQRAY in all patients with confirmed pneumonitis.
Advise patients to immediately report new or worsening respiratory symptoms.
5.5 Diarrhea
Severe diarrhea, including dehydration and acute kidney injury, occurred in patients treated with PIQRAY. Most patients (58%) experienced diarrhea during treatment with PIQRAY. Grade 3 diarrhea occurred in 7% (n = 19) of patients. Among patients with Grade 2 or 3 diarrhea (n = 71), the median time to onset was 46 days (range: 1 to 442 days).
Dose reductions of PIQRAY were required in 6% of patients and 2.8% of patients permanently discontinued PIQRAY due to diarrhea. In the 164 patients that experienced diarrhea, anti-diarrheal medications (e.g., loperamide) were required to manage symptoms in 63% (104/164) of these patients.
Based on the severity of the diarrhea, PIQRAY may require dose interruption, reduction, or discontinuation as described in Table 4[see Dosage and Administration (2.3)].
Advise patients to start antidiarrheal treatment, increase oral fluids, and notify their healthcare provider if diarrhea occurs while taking PIQRAY.
5.6 Embryo-Fetal Toxicity
Based on findings in animals and its mechanism of action, PIQRAY can cause fetal harm when administered to a pregnant woman. In animal reproduction studies, oral administration of alpelisib to pregnant rats and rabbits during organogenesis caused adverse developmental outcomes including embryo-fetal mortality (post-implantation loss), reduced fetal weights, and increased incidences of fetal malformations at maternal exposures based on area under the curve (AUC) that were ≥ 0.8 times the exposure in humans at the recommended dose of 300 mg/day. Advise pregnant women and females of reproductive potential of the potential risk to a fetus. Advise females of reproductive potential to use effective contraception during treatment with PIQRAY and for 1 week after the last dose. Advise male patients with female partners of reproductive potential to use condoms and effective contraception during treatment with PIQRAY and for 1 week after the last dose[see Use in Specific Populations (8.1, 8.3) and Clinical Pharmacology (12.1)].
Refer to the Full Prescribing Information of fulvestrant for pregnancy and contraception information.
6 ADVERSE REACTIONS
The following adverse reactions are discussed in greater detail in other sections of the labeling:
Severe Hypersensitivity[see Warnings and Precautions (5.1)]
Severe Cutaneous Reactions[see Warnings and Precautions (5.2)] Hyperglycemia[see Warnings and Precautions (5.3)]
Pneumonitis[see Warnings and Precautions (5.4)] Diarrhea[see Warnings and Precautions (5.5)]
6.1 Clinical Trial Experience
Because clinical trials are conducted under widely varying conditions, adverse reaction rates observed in the clinical trials of a drug cannot be directly compared to rates in the clinical trials of another drug and may not reflect the rates observed in practice.
The safety of PIQRAY was evaluated in a randomized, double-blind, placebo-controlled trial (SOLAR-1) in 571 patients with HR-positive, HER2-negative, advanced or metastatic breast cancer enrolled into two cohorts, with or without a PIK3CA mutation[see Clinical Studies (14)].
Patients received either PIQRAY 300 mg plus fulvestrant (n = 284) or placebo plus fulvestrant (n = 287). Fulvestrant 500 mg was administered intramuscularly on Cycle 1, Day 1 and 15 and then at Day 1 of each 28-day cycle during treatment phase.
Two patients (0.7%) died while on treatment with PIQRAY plus fulvestrant due to causes other than the underlying malignancy. Causes of death included one cardio-respiratory arrest and one second primary malignancy. Neither was suspected to be related to study treatment.
Serious adverse reactions occurred in 35% of patients receiving PIQRAY plus fulvestrant. Serious adverse reactions in > 2% of patients receiving PIQRAY plus fulvestrant included hyperglycemia (10%), rash (3.5%), diarrhea (2.8%), acute kidney injury (2.5%), abdominal pain (2.1%), and anemia (2.1%).
Osteonecrosis of the jaw (ONJ) was reported in 4.2% of patients (12/284) in the PIQRAY plus fulvestrant arm compared to 1.4% of patients (4/287) in the placebo arm. All patients experiencing ONJ had prior or concomitant bisphosphonates or RANK-ligand inhibitor administration.
Among patients receiving PIQRAY plus fulvestrant, 4.6% permanently discontinued both PIQRAY and fulvestrant and 21% permanently discontinued PIQRAY alone, due to ARs. The most frequent ARs leading to treatment discontinuation of PIQRAY in > 2% patients receiving PIQRAY plus fulvestrant were hyperglycemia (6%), rash (4.2%), diarrhea (2.8%), and fatigue (2.5%).
Dose reductions due to ARs occurred in 55% of patients receiving PIQRAY plus fulvestrant. The most frequent ARs leading to dose reduction in > 2% patients receiving PIQRAY plus fulvestrant were hyperglycemia (29%), rash (9%), diarrhea (6%), stomatitis (3.5%) and mucosal inflammation (2.1%).
The most common adverse reactions including laboratory abnormalities (all grades, incidence ≥ 20%) were glucose increased, creatinine increased, diarrhea, rash, lymphocyte count decreased, GGT increased, nausea, ALT increased, fatigue, hemoglobin decreased, lipase increased, decreased appetite, stomatitis, vomiting, weight decreased, calcium decreased, glucose decreased, aPTT prolonged, and alopecia.
Adverse reactions and laboratory abnormalities are listed in Table 6 and Table 7, respectively.
Table 6: Adverse Reactions Occurring in ≥ 10% and ≥ 2% Higher than Placebo Arm in SOLAR-1 (All Grades)
|
PIQRAY plus fulvestrant |
Placebo plus fulvestrant |
||||
|
|
N = 284 |
|
N = 287 |
||
|
|
|
|
|
|
|
Adverse reactions |
All Grades |
|
Grade 3-4 |
All Grades |
|
Grade 3-4 |
|
% |
|
% |
% |
|
% |
Gastrointestinal disorders |
|
|
|
|
|
|
Diarrhea |
58 |
|
7* |
16 |
|
0.3* |
Nausea |
45 |
|
2.5* |
22 |
|
0.3* |
Stomatitis1 |
30 |
|
2.5* |
6 |
|
0* |
Vomiting |
27 |
|
0.7* |
10 |
|
0.3* |
Abdominal pain2 |
17 |
|
1.4* |
11 |
|
1* |
Dyspepsia |
11 |
|
0* |
6 |
|
0* |
|
|
|
PIQRAY plus fulvestrant |
Placebo plus fulvestrant |
||||
|
|
|
N = 284 |
|
|
N = 287 |
||
|
|
|
|
|
|
|
|
|
General disorders and administration site conditions |
|
|
|
|
|
|
||
|
Fatigue3 |
|
42 |
|
5* |
29 |
|
1* |
|
Mucosal inflammation |
|
19 |
|
2.1* |
1 |
|
0* |
|
Edema peripheral |
|
15 |
|
0* |
5 |
|
0.3* |
|
Pyrexia |
|
14 |
|
0.7 |
4.9 |
|
0.3* |
|
Mucosal dryness4 |
|
12 |
|
0.4* |
4.2 |
|
0* |
Infections and infestations |
|
|
|
|
|
|
||
|
Urinary tract infection5 |
|
10 |
|
0.7* |
5 |
|
1* |
Investigations |
|
|
|
|
|
|
||
|
Weight decreased |
|
27 |
|
3.9* |
2.1 |
|
0* |
Metabolism and nutrition disorders |
|
|
|
|
|
|
||
|
Decreased appetite |
|
36 |
|
0.7* |
10 |
|
0.3* |
Nervous system disorders |
|
|
|
|
|
|
||
|
Dysgeusia6 |
|
18 |
|
0.4* |
3.5 |
|
0* |
|
Headache |
|
18 |
|
0.7* |
13 |
|
0* |
Skin and subcutaneous tissue disorders |
|
|
|
|
|
|
||
|
Rash7 |
|
52 |
|
20* |
7 |
|
0.3* |
|
Alopecia |
|
20 |
|
0* |
2.4 |
|
0* |
|
Pruritus |
|
18 |
|
0.7* |
6 |
|
0* |
|
Dry skin8 |
|
18 |
|
0.4* |
3.8 |
|
0* |
Grading according to CTCAE Version 4.03 |
|
|
|
|
|
|
||
1 Stomatitis: including stomatitis, aphthous ulcer and mouth ulceration |
|
|
|
|
||||
2 |
Abdominal pain: abdominal pain, abdominal pain upper, abdominal pain lower |
|
|
|
|
|||
3 |
Fatigue: including fatigue, asthenia |
|
|
|
|
|
|
|
4 |
Mucosal dryness: including dry mouth, mucosal dryness, vulvovaginal dryness |
|
|
|
|
|||
5 |
Urinary tract infection: including UTI and single case of urosepsis |
|
|
|
|
|||
6 |
Dysgeusia: including dysgeusia, ageusia, hypogeusia |
|
|
|
|
|
|
|
7 |
Rash: including rash, rash maculo-papular, rash macular, rash generalized, rash papular, rash pruritic |
|
|
|
||||
8 |
Dry skin: including dry skin, skin fissures, xerosis, xeroderma |
|
|
|
|
|
|
* No Grade 4 adverse reactions were reported.
Among the patients with Grade 2 or 3 rash, the median time to first onset of Grade 2 or 3 rash was 12 days. A subgroup of 86 patients received prophylaxis, including anti-histamines, prior to onset of rash. In these patients, rash was reported less frequently than in the overall population, for all grades rash (27% vs 54%), Grade 3 rash (12% vs 20%) and rash leading to permanent discontinuation of PIQRAY (3.5% vs 4.2%). Of the 153 patients who experienced rash, 141 had resolution of the rash.
Table 7: Laboratory Abnormalities Occurring in ≥ 10% of Patients in SOLAR-1
|
PIQRAY plus fulvestrant |
Placebo plus fulvestrant |
||||
|
|
N = 284 |
|
N = 287 |
||
|
|
|
|
|
|
|
|
All Grades |
|
Grade 3-4 |
All Grades |
|
Grade 3-4 |
Laboratory Abnormality |
% |
|
% |
% |
|
% |
Hematological parameters |
|
|
|
|
|
|
Lymphocyte count decreased |
52 |
|
8 |
40 |
|
4.5* |
Hemoglobin decreased |
42 |
|
4.2* |
29 |
|
1* |
Activated Partial Thromboplastin Time (aPTT) |
21 |
|
0.7* |
16 |
|
0.3* |
prolonged |
|
|
|
|
|
|
Platelet count decreased |
14 |
|
1.1 |
6 |
|
0* |
Biochemical parameters |
|
|
|
|
|
|
Glucose increased1 |
79 |
|
39 |
34 |
|
1 |
Creatinine increased |
67 |
|
2.8* |
25 |
|
0.7* |
|
|
|
|
|
|
|
Gamma Glutamyl Transferase (GGT) increased |
52 |
|
11 |
44 |
|
10 |
Alanine Aminotransferase (ALT) increased |
44 |
|
3.5 |
34 |
|
2.4* |
Lipase increased |
42 |
|
7 |
25 |
|
6 |
Calcium (corrected) decreased |
27 |
|
2.1 |
20 |
|
1.4 |
Glucose decreased |
26 |
|
0.4 |
14 |
|
0* |
Potassium decreased |
14 |
|
6 |
2.8 |
|
0.7* |
Albumin decreased |
14 |
|
0* |
8 |
|
0* |
Magnesium decreased |
11 |
|
0.4* |
4.2 |
|
0* |
1Glucose increase is an expected laboratory abnormality of PI3K inhibition.
*No Grade 4 laboratory abnormalities were reported.
7 DRUG INTERACTIONS
7.1 Effect of Other Drugs on PIQRAY
CYP3A4 Inducer
Coadministration of PIQRAY with a strong CYP3A4 inducer may decrease alpelisib concentration[see Clinical Pharmacology (12.3)], which may decrease alpelisib activity. Avoid coadministration of PIQRAY with strong CYP3A4 inducers.
BCRP Inhibitors
Coadministration of PIQRAY with a BCRP inhibitor may increase alpelisib concentration[see Clinical Pharmacology (12.3)], which may increase the risk of toxicities. Avoid the use of BCRP inhibitors in patients treated with PIQRAY. If unable to use alternative drugs, when PIQRAY is used in combination with BCRP inhibitors, closely monitor for increased adverse reactions.
7.2 Effect of PIQRAY on Other Drugs
CYP2C9 Substrates
Coadministration of PIQRAY with CYP2C9 substrates (e.g., warfarin) may reduce plasma concentration of these drugs[see Clinical Pharmacology (12.3)]. Closely monitor when PIQRAY is used in combination with CYP2C9 substrates where decreases in the plasma concentration of CYP2C9 substrates may reduce activity of these drugs.
8 USE IN SPECIFIC POPULATIONS
8.1 Pregnancy
Risk Summary
PIQRAY is used in combination with fulvestrant. Refer to the Full Prescribing Information of fulvestrant for pregnancy information.
Based on animal data and mechanism of action, PIQRAY can cause fetal harm when administered to a pregnant woman[see Clinical Pharmacology (12.1)]. There are no available data in pregnant women to inform the drug-associated risk. In animal reproduction studies, oral administration of alpelisib to pregnant rats and rabbits during organogenesis caused adverse developmental outcomes including embryo-fetal mortality (post-implantation loss), reduced fetal weights, and increased incidences of fetal malformations at maternal exposures
≥ 0.8 times the exposure in humans based on AUC at the recommended dose of 300 mg/day(see Data). Advise pregnant women and females of reproductive potential of the potential risk to a fetus.
The estimated background risk of major birth defects and miscarriage for the indicated population is unknown. However, the estimated background risk of major birth defects is 2% to 4% and of miscarriage is 15% to 20% of clinically recognized pregnancies in the U.S. general population.
Data
Animal Data
In embryo-fetal development studies in rats and rabbits, pregnant animals received oral doses of alpelisib up to 30 mg/kg/day during the period of organogenesis.
In rats, oral administration of alpelisib resulted in maternal toxicity (body weight loss, low food consumption) and no viable fetuses (post-implantation loss) at 30 mg/kg/day (approximately 3 times the exposure in humans at the recommended dose of 300 mg/day based on AUC). At a dose of 10 mg/kg/day (approximately 0.8 times the exposure in humans at the recommended dose of 300 mg/day based on AUC), toxicities included reduced fetal weight and increased incidences of skeletal malformations (bent scapula and thickened or bent long bones) and fetal variations (enlarged brain ventricle, decreased bone ossification).
In a pilot embryo-fetal development study in rabbits, a dose of 30 mg/kg/day resulted in no viable fetuses (post-implantation loss). Doses ≥ 15 mg/kg/day resulted in increased embryo-fetal deaths, reduced fetal weights, and malformations, mostly related to the tail and head. At 15 mg/kg/day in rabbits, the maternal exposure was approximately 5 times the exposure achieved at the recommended human dose of 300 mg/day based on AUC.
8.2 Lactation
PIQRAY is used in combination with fulvestrant. Refer to the Full Prescribing Information of fulvestrant for lactation information.
There is no data on the presence of alpelisib in human milk, its effects on milk production, or the breastfed child. Because of the potential for serious adverse reactions in the breastfed child, advise lactating women to not breastfeed during treatment with PIQRAY and for 1 week after the last dose.
8.3 Females and Males of Reproductive Potential
PIQRAY is used in combination with fulvestrant. Refer to the Full Prescribing Information of fulvestrant for contraception and infertility information.
Pregnancy Testing
Verify the pregnancy status in females of reproductive potential prior to initiating PIQRAY.
Contraception
Females
PIQRAY can cause fetal harm when administered to a pregnant woman[see Use in Specific Populations (8.1)]. Advise females of reproductive potential to use effective contraception during treatment with PIQRAY and for 1 week after the last dose.
Males
Advise male patients with female partners of reproductive potential to use condoms and effective contraception during treatment with PIQRAY and for 1 week after the last dose.
Infertility
Based on findings from animal studies, PIQRAY may impair fertility in males and females of reproductive potential[see Nonclinical Toxicology (13.1)].
8.4 Pediatric Use
The safety and efficacy of PIQRAY in pediatric patients have not been established.
8.5 Geriatric Use
Of 284 patients who received PIQRAY in the SOLAR-1 trial, 117 patients were ≥ 65 years of age and 34 patients were ≥ 75 years of age. In patients treated with PIQRAY plus fulvestrant, there was a higher incidence of Grade 3-4 hyperglycemia in patients ≥ 65 years of age (44%) compared to patients < 65 years of age (32%). No overall differences in effectiveness of PIQRAY were observed between patients ≥ 65 years of age compared to younger patients. There are an insufficient number of patients ≥ 75 years of age to assess whether there are differences in safety or effectiveness.
8.6 Renal Impairment
The effect of severe renal impairment (CLcr < 30 mL/min) on alpelisib pharmacokinetics is unknown[see Clinical Pharmacology (12.3)].
No dose adjustment is recommended for patients with mild to moderate renal impairment (CLcr 30 to < 90 mL/min).
10 OVERDOSAGE
There is limited experience of overdose with PIQRAY in clinical trials. In the clinical studies, PIQRAY was administered at doses up to 450 mg once daily.
In cases where accidental overdosage of PIQRAY was reported in the clinical studies, the adverse reactions associated with the overdose were consistent with the known safety profile of PIQRAY and included hyperglycemia, nausea, asthenia, and rash.
Initiate general symptomatic and supportive measures in all cases of overdosage where necessary. There is no known antidote for PIQRAY.
11 DESCRIPTION
PIQRAY (alpelisib) is a kinase inhibitor. The chemical name of alpelisib is (2S)-N1-[4-Methyl-5-[2-(2,2,2-trifluoro-1,1-dimethylethyl)-4-pyridinyl]-2-thiazolyl]-1,2-pyrrolidinedicarboxamide. Alpelisib is a white to almost white powder. The molecular formula for alpelisib is C19H22F3N5O2S and the relative molecular mass is
441.47 g/mol. The chemical structure of alpelisib is shown below:
PIQRAY film-coated tablets are supplied for oral administration with three strengths that contain 50 mg, 150 mg and 200 mg of alpelisib. The tablets also contain hypromellose, magnesium stearate, mannitol, microcrystalline cellulose, and sodium starch glycolate. The film-coating contains hypromellose, iron oxide black, iron oxide red, macrogol/polyethylene glycol (PEG) 4000, talc, and titanium dioxide.
12 CLINICAL PHARMACOLOGY
12.1 Mechanism of Action
Alpelisib is an inhibitor of phosphatidylinositol-3-kinase (PI3K) with inhibitory activity predominantly against PI3Kα. Gain-of-function mutations in the gene encoding the catalytic α-subunit of PI3K (PIK3CA) lead to activation of PI3Kα and Akt-signaling, cellular transformation and the generation of tumors in in vitro and in vivo models.
In breast cancer cell lines, alpelisib inhibited the phosphorylation of PI3K downstream targets, including Akt and showed activity in cell lines harboring a PIK3CA mutation. In vivo, alpelisib inhibited the PI3K/Akt signaling pathway and reduced tumor growth in xenograft models, including models of breast cancer.
PI3K inhibition by alpelisib treatment has been shown to induce an increase in estrogen receptor (ER) transcription in breast cancer cells. The combination of alpelisib and fulvestrant demonstrated increased anti-tumor activity compared to either treatment alone in xenograft models derived from ER-positive, PIK3CA mutated breast cancer cell lines.
12.2 Pharmacodynamics
Cardiac Electrophysiology
Serial ECGs were collected following a single dose and at steady-state to evaluate the effect of alpelisib on the QTcF interval in patients with advanced cancer. An analysis of clinical ECG data demonstrates the absence of a large effect (i.e., > 20 ms) on QTcF prolongation at the recommended 300 mg dose with or without fulvestrant.
12.3 Pharmacokinetics
The pharmacokinetics of alpelisib has been studied in healthy subjects and adult patients with solid tumors. Steady-state alpelisib maximum plasma concentration (Cmax) and AUC increased proportionally over the dose range of 30 mg to 450 mg (0.1 to 1.5 times the approved recommended dosage) under fed conditions. The mean accumulation of alpelisib is 1.3 to 1.5 and steady-state plasma concentrations are reached within 3 days following daily dosage. In adult patients who received PIQRAY 300 mg once daily in the SOLAR-1 trial, population approach derived mean steady-state alpelisib [coefficient of variation (CV%)] for Cmax was 2480 (23%) ng/mL and AUC0-24hr was 33224 (21%) ng*h/mL.
Absorption
The median time to reach peak plasma concentration (Tmax) ranged between 2.0 to 4.0 hours.
Effect of food
A high-fat high-calorie meal (985 calories with 58.1 g of fat) increased alpelisib AUC by 73% and Cmax by 84%, and a low-fat low-calorie meal (334 calories with 8.7 g of fat) increased alpelisib AUC by 77% and Cmax by 145% following a single dose of PIQRAY. No clinically significant differences in alpelisib AUC were observed between low-fat low-calorie and high-fat high-calorie meals.
Distribution
The mean (% CV) apparent volume of distribution of alpelisib at steady-state is predicted to be 114 L (46%).
Protein binding of alpelisib is 89% and is independent of concentration.
Elimination
The half-life of alpelisib is predicted to be 8 to 9 hours. The mean (% CV) clearance of alpelisib is predicted to be 9.2 L/hr (21%) under fed conditions.
Metabolism
Alpelisib is primarily metabolized by chemical and enzymatic hydrolysis to form its metabolite BZG791 and to a lesser extent by CYP3A4, in vitro.
Excretion
Following a single oral dose of 400 mg radiolabeled alpelisib under fasted condition, 81% of the administered dose was recovered in feces (36% unchanged, 32% BZG791) and 14% (2% unchanged, 7.1% BZG791) in urine. CYP3A4-mediated metabolites (12%) and glucuronides amounted to approximately 15% of the dose.
Specific Populations
No clinically significant differences in the pharmacokinetics of alpelisib were predicted based on age (21 to 87 years), sex, race/ethnicity (Japanese or Caucasian), body weight (37 to 181 kg), mild to moderate renal impairment (CLcr 30 to < 90 mL/min based on the Cockcroft-Gault formula), or mild to severe hepatic impairment (Child-Pugh Class A, B, and C). The effect of severe renal impairment (CLcr < 30 mL/min) on the pharmacokinetics of alpelisib is unknown.
Drug Interaction Studies
Clinical Studies
Acid Reducing Agents: PIQRAY can be coadministered with acid reducing agents, since PIQRAY should be taken with food. Food exhibited a more pronounced effect on the solubility of alpelisib than the effect of gastric pH value.
Coadministration of the H2 receptor antagonist ranitidine in combination with a single 300 mg oral dose of alpelisib decreased the absorption and overall exposure of alpelisib. In the presence of a low-fat low-calorie meal, AUC was decreased on average by 21% and Cmax by 36% with ranitidine. Under the fasted state, AUC was decreased on average by 30% and Cmax by 51% with ranitidine.
CYP3A4 Substrates:No clinically significant differences in pharmacokinetics of everolimus (a substrate of CYP3A4 and P-gp) were observed when coadministered with alpelisib.
In Vitro Studies
Effect of Alpelisib on CYP Enzymes:Alpelisib inhibits CYP3A4 in a time-dependent manner and induces CYP2B6, CYP2C9 and CYP3A4.
Effect of Transporter on Alpelisib:Alpelisib is a substrate of BCRP.
Effect of Alpelisib on Transporters:Alpelisib is an inhibitor of P-gp. Alpelisib has a low potential to inhibit BCRP, MRP2, BSEP, OATP1B1, OATP1B3, OCT1, OAT1, OAT3, OCT2, MATE1, and MATE2K at clinically relevant concentrations.
13 NONCLINICAL TOXICOLOGY
13.1 Carcinogenesis, Mutagenesis, Impairment of Fertility
Carcinogenicity studies have not been conducted with alpelisib.
Alpelisib was not mutagenic in an in vitro bacterial reverse mutation (Ames) assay, or aneugenic or clastogenic in human cell micronucleus and chromosome aberration tests in vitro. Alpelisib was not genotoxic in an in vivo rat micronucleus test.
Fertility studies in animals have not been conducted. In repeated-dose toxicity studies up to 13 weeks duration, adverse effects were observed in reproductive organs including vaginal atrophy and estrous cycle variations in rats at doses ≥ 6 mg/kg/day (approximately 0.6 times the exposure in humans at the recommended dose of 300 mg/day based on AUC), and prostate atrophy in dogs at doses ≥ 15 mg/kg/day (approximately 2.6 times the exposure in humans at the recommended dose of 300 mg/day based on AUC).
14 CLINICAL STUDIES
SOLAR-1 (NCT02437318) was a randomized, double-blind, placebo-controlled trial of PIQRAY plus fulvestrant versus placebo plus fulvestrant in 572 patients with HR-positive, HER2-negative, advanced or metastatic breast cancer whose disease had progressed or recurred on or after an aromatase inhibitor-based treatment (with or without CDK4/6 combination). Patients were excluded if they had inflammatory breast cancer, diabetes mellitus Type 1 or uncontrolled Type 2, or pneumonitis. Randomization was stratified by presence of lung and/or liver metastasis and previous treatment with CDK4/6 inhibitor(s). Overall, 60% of enrolled patients had tumors with one or more PIK3CA mutations in tissue, 50% had liver/lung metastases, and 6% had previously been treated with a CDK4/6 inhibitor.
There were 341 patients enrolled by tumor tissue in the cohort with a PIK3CA mutation and 231 enrolled in the cohort without a PIK3CA mutation. Of the 341 patients in the cohort with a PIK3CA mutation, 336 (99%) patients had one or more PIK3CA mutations confirmed in tumor tissue using the FDA-approvedtherascreen® PIK3CA RGQ PCR Kit. Out of the 336 patients with PIK3CA mutations confirmed in tumor tissue, 19 patients had no plasma specimen available for testing with the FDA-approvedtherascreen® PIK3CA RGQ PCR Kit. Of the remaining 317 patients with PIK3CA mutations confirmed in tumor tissue, 177 patients (56%) had PIK3CA mutations identified in plasma specimen, and 140 patients (44%) did not have PIK3CA mutations identified in plasma specimen.
Patients received either PIQRAY (300 mg) or placebo orally once daily on a continuous basis, plus fulvestrant (500 mg) administered intramuscularly on Cycle 1, Days 1 and 15, and then on Day 1 of every 28-day cycle. Patients received treatment until radiographic disease progression or unacceptable toxicity. Tumor assessments were performed every 8 weeks for the first 18 months and every 12 weeks thereafter.
The median age of patients was 63 years (range 25 to 92). Most patients were women (99.8%) and most patients were White (66%), followed by Asian (22%), Other/Unknown (10%), Black or African American (1.4%), and American Indian or Alaskan Native (0.9%). Baseline ECOG performance status was 0 (68%) or 1 (32%).
Patient demographics for those with PIK3CA-mutated tumors were generally representative of the broader study population. The median duration of exposure to PIQRAY plus fulvestrant was 8.2 months with 59% of patients exposed for > 6 months.
The majority of patients (98%) received prior hormonal therapy as the last treatment (48% metastatic setting, 52% adjuvant setting). Primary endocrine resistance, defined as relapsed within 24 months on adjuvant endocrine therapy or progression within 6 months on endocrine therapy for advanced disease, was observed in 13% of patients and secondary endocrine resistance, defined as relapsed after 24 months on adjuvant endocrine therapy, relapsed within 12 months of the end of adjuvant endocrine therapy, or progression after 6 months on endocrine therapy for advanced disease, was observed in 72% of patients.
The major efficacy outcome was investigator-assessed progression-free survival (PFS) in the cohort with a PIK3CA mutation per Response Evaluation Criteria in Solid Tumors (RECIST) v1.1. Additional efficacy outcome measures were overall response rate (ORR) and overall survival (OS) in the cohort with a PIK3CA mutation.
Efficacy results for the cohort with a PIK3CA mutation in tumor tissue are presented in Table 8 and Figure 1. PFS results for the cohort with a PIK3CA mutation by investigator assessment were supported by consistent results from a blinded independent review committee (BIRC) assessment. Consistent results were seen in patients with tissue or plasma PIK3CA mutations. At the time of final PFS analysis, 27% (92/341) of patients had died, and overall survival follow-up was immature.
No PFS benefit was observed in patients whose tumors did not have a PIK3CA tissue mutation (HR = 0.85; 95% CI: 0.58, 1.25).
Table 8: Efficacy Results in SOLAR-1 (Per Investigator Assessment of Patients with a PIK3CA Tumor Mutation)
|
PIQRAY plus fulvestrant |
Placebo plus fulvestrant |
|
|
|
Progression-free survival |
N = 169 |
N = 172 |
Number of PFS events – n (%) |
103 (61) |
129 (75) |
|
|
|
Median PFS months (95% CI) |
11.0 (7.5, 14.5) |
5.7 (3.7, 7.4) |
|
|
|
Hazard ratio (95% CI) |
|
0.65 (0.50, 0.85) |
|
|
|
p-value1 |
|
0.0013 |
Overall Response Rate |
N = 126 |
N = 136 |
ORR2 (95% CI) |
35.7 (27.4, 44.7) |
16.2 (10.4, 23.5) |
1 Both log-rank test and Cox proportional hazards model are stratified by prior CDK4/6 inhibitor usage and presence of lung/liver metastases. P-value was compared to prespecified Haybittle-Peto stopping boundary (two-sided p ≤ 0.0398).
2 ORR = percentage of patients with confirmed Complete Response or Partial Response with measurable disease at baseline
Figure 1: Progression Free Survival in SOLAR-1 (Per Investigator Assessment of Patients with a PIK3CA Tumor Mutation)
Event-free probability (%) |
100 |
Censoring Times |
|
|
|
Alpelisib + Fulv |
|
Placebo + Fulv |
80 |
|
60
40
20
0
0 |
2 |
4 |
6 |
8 |
10 |
12 |
14 |
16 |
18 |
20 |
22 |
24 |
26 |
28 |
30 |
32 |
|
|
|
|
|
|
|
|
Time (Months) |
|
|
|
|
|
|
|
||
|
Number of subjects still at risk |
|
|
|
|
|
|
|
|
|
|
|
|
||||
Time (Months) |
0 |
2 |
4 |
6 |
8 |
10 |
12 |
14 |
16 |
18 |
20 |
22 |
24 |
26 |
28 |
30 |
32 |
Alpelisib + Fulv |
169 |
145 |
123 |
97 |
85 |
75 |
62 |
50 |
39 |
30 |
17 |
14 |
5 |
3 |
1 |
1 |
0 |
Placebo + Fulv |
172 |
120 |
89 |
80 |
67 |
58 |
48 |
37 |
29 |
20 |
14 |
9 |
3 |
2 |
0 |
0 |
0 |
16 HOW SUPPLIED/STORAGE AND HANDLING
PIQRAY (alpelisib) 50 mg, 150 mg, and 200 mg film-coated tablets[see Dosage Forms and Strengths (3)].
300 mg daily dose: Each carton contains 2 blister packs. Each blister pack contains a 14-day supply of 28 tablets (28 tablets, 150 mg alpelisib per tablet). NDC 0078-0708-02
250 mg daily dose: Each carton contains 2 blister packs. Each blister pack contains a 14-day supply of 28 tablets (14 tablets, 200 mg alpelisib per tablet and 14 tablets, 50 mg alpelisib per tablet). NDC 0078-0715-02
200 mg daily dose: Each carton contains 1 blister pack. Each blister pack contains a 28-day supply of 28 tablets
(28 tablets, 200 mg alpelisib per tablet). NDC 0078-0701-84
Store at 20°C to 25°C (68°F to 77°F), excursions permitted between 15°C and 30°C (59°F and 86°F)[see USP Controlled Room Temperature].
17 PATIENT COUNSELING INFORMATION
Advise the patient to read the FDA-approved patient labeling (Patient Information).
Severe Hypersensitivity
Inform patients of the signs and symptoms of hypersensitivity. Advise patients to contact their healthcare provider immediately for signs and symptoms of hypersensitivity[see Warnings and Precautions (5.1)].
Severe Cutaneous Reactions
Inform patients of the signs and symptoms of severe cutaneous reactions. Advise patients to contact their healthcare provider immediately for signs and symptoms of severe cutaneous reactions[see Warnings and Precautions (5.2)].
Hyperglycemia
Advise patients of the possibility of developing hyperglycemia and the need to monitor blood glucose periodically during therapy. Advise patients to contact their healthcare provider immediately for signs and symptoms of hyperglycemia[see Warnings and Precautions (5.3)].
Pneumonitis
Inform patients of the possibility of developing pneumonitis and to immediately contact their healthcare provider if they experience respiratory problems[see Warnings and Precautions (5.4)].
Diarrhea
Advise patients that PIQRAY may cause diarrhea, which may be severe in some cases. Inform patients to start antidiarrheal treatment, increase oral fluids, and notify their healthcare provider if diarrhea occurs while taking PIQRAY[see Warnings and Precautions (5.5)].
Embryo-Fetal Toxicity
Inform pregnant women and females of reproductive potential of the potential risk to a fetus. Advise females to inform their healthcare provider of a known or suspected pregnancy[see Warnings and Precautions (5.6) and Use in Specific Populations (8.1)].
Advise females of reproductive potential to use effective contraception during treatment with PIQRAY and for 1 week after the last dose[see Use in Specific Populations (8.3)].
Advise male patients with female partners of reproductive potential to use condoms and effective contraception during treatment with PIQRAY and for 1 week after the last dose[see Use in Specific Populations (8.3)].
Refer to the Full Prescribing Information of fulvestrant for pregnancy and contraception information.Lactation
Advise women not to breastfeed during treatment with PIQRAY and for 1 week after the last dose[see Use in Specific Populations (8.2)].Refer to the Full Prescribing Information of fulvestrant for lactation information.
Infertility
Advise males and females of reproductive potential that PIQRAY may impair fertility[see Use in Specific Populations (8.3)].Refer to the Full Prescribing Information of fulvestrant for infertility information.
Drug Interactions
Advise patients to avoid the use of strong CYP3A4 inducers in patients treated with PIQRAY. Advise patients to avoid the use of BCRP inhibitors in patients treated with PIQRAY. If unable to use alternative drugs, closely monitor for increased adverse reactions. Advise patients that close monitoring may be required when PIQRAY
is coadministered with CYP2C9 substrates where decreases in the plasma concentration of CYP2C9 substrates may reduce activity of these drugs[see Drug Interactions (7.1, 7.2)].
Dosing
Instruct patients to take PIQRAY at approximately the same time each day and to swallow the tablet(s) whole (tablets should not be chewed, crushed, or split prior to swallowing)[see Dosage and Administration (2.2)].
Advise patients to take PIQRAY with food[see Drug Interactions (7.4)].
Instruct patients that if a dose of PIQRAY is missed, it can be taken with food within 9 hours after the time it is usually taken. After more than 9 hours, skip the dose for that day. The next day, take PIQRAY at the usual time. Instruct patients not to take 2 doses to make up for a missed dose.
Instruct patients that if they vomit after taking the dose of PIQRAY, they should not take an additional dose on that day, and to resume the usual dosing schedule the next day at the usual time[see Dosage and Administration (2.2)].
Distributed by:
Novartis Pharmaceuticals Corporation
East Hanover, New Jersey 07936
© Novartis
T2019-57
PATIENT INFORMATION
PIQRAY® (pik' raye)
(alpelisib)
tablets
What is PIQRAY?
PIQRAY is a prescription medicine used in combination with the medicine fulvestrant to treat women who have gone through menopause and men:
who have hormone receptor (HR)-positive, human epidermal growth factor receptor 2 (HER2)-negative advanced breast cancer or breast cancer that has spread to other parts of the body (metastatic), with an abnormal phosphatidylinositol-3-kinase catalytic subunit alpha (PIK3CA) gene, and
whose disease has progressed on or after endocrine therapy.
Your healthcare provider will test your cancer for an abnormal “PIK3CA” gene to make sure that PIQRAY is right for you.
It is not known if PIQRAY is safe and effective in children.
Do not take PIQRAY if you have had a severe allergic reaction to PIQRAY or are allergic to any of the ingredients in PIQRAY.
See the end of this Patient Information leaflet for a complete list of the ingredients in PIQRAY.
See “What are the possible side effects of PIQRAY?” for signs and symptoms of severe allergic reactions.
Before you take PIQRAY, tell your healthcare provider about all of your medical conditions, including if you:
have a history of diabetes
have a history of skin rash, redness of skin, blistering of the lips, eyes or mouth, or skin peeling are pregnant or plan to become pregnant. PIQRAY can harm your unborn baby.
Females who are able to become pregnant:
o Your healthcare provider will check to see if you are pregnant before you start treatment with PIQRAY. o You should use effective birth control during treatment with PIQRAY and for 1 week after the last dose.
Talk to your healthcare provider about birth control methods that may be right for you during this time. o If you become pregnant or think you are pregnant, tell your healthcare provider right away.
Males with female partners who are able to become pregnant should use condoms and effective birth control during treatment with PIQRAY and for 1 week after the last dose. If your female partner becomes pregnant, tell your healthcare provider right away.
You should also read the Full Prescribing Information of fulvestrant for important pregnancy, contraception, and infertility information.
are breastfeeding or plan to breastfeed. It is not known if PIQRAY passes into your breast milk. Do not breastfeed during treatment with PIQRAY and for 1 week after the last dose. You should also read the Full Prescribing Information of fulvestrant for important lactation information.
Tell your healthcare provider about all of the medicines you take, including prescription and over-the-counter medicines, vitamins, and herbal supplements. PIQRAY and other medicines may affect each other causing side effects. Know the medicines you take. Keep a list of them to show your healthcare provider or pharmacist when you get a new medicine.
How should I take PIQRAY?
Take PIQRAY exactly as your healthcare provider tells you.
Do not change your dose or stop taking PIQRAY unless your healthcare provider tells you. Take PIQRAY 1 time each day, at about the same time each day.
Take PIQRAY with food.
Swallow PIQRAY tablets whole. Do not chew, crush or split the tablets.
Do not take any PIQRAY tablets that are broken, cracked, or that look damaged.
If you miss a dose of PIQRAY, you may still take it with food up to 9 hours after the time you usually take it. If it has been more than 9 hours after you usually take your dose, skip the dose for that day. The next day, take the dose at your usual time. Do not take 2 doses to make up for a missed dose.
If you vomit after taking a dose of PIQRAY, do not take another dose on that day. Take your next dose at your usual time.
If you take too much PIQRAY, call your healthcare provider or go to the nearest hospital emergency room right away.
What are the possible side effects of PIQRAY?
PIQRAY may cause serious side effects, including:
Severe allergic reactions. Tell your healthcare provider or get medical help right away if you have trouble breathing, flushing, rash, fever, or fast heart rate during treatment with PIQRAY.
Severe skin reactions. Tell your healthcare provider or get medical help right away if you get severe rash or rash that keeps getting worse, reddened skin, flu-like symptoms, blistering of the lips, eyes or mouth, blisters on the skin or skin peeling, with or without fever.
High blood sugar levels (hyperglycemia). Hyperglycemia is common with PIQRAY and can be severe. Your healthcare provider will monitor your blood sugar levels before you start and during treatment with PIQRAY. Your healthcare provider may monitor your blood sugar levels more often if you have a history of Type 2 diabetes. Tell your healthcare provider right away if you develop symptoms of hyperglycemia, including:
o |
excessive thirst |
o more frequent urination than usual or a higher amount |
o |
dry mouth |
of urine than normal |
o increased appetite with weight loss
Lung problems (pneumonitis). Tell your healthcare provider right away if you develop new or worsening symptoms of lung problems, including:
o shortness of breath or trouble o cough
breathing o chest pain
Diarrhea. Diarrhea is common with PIQRAY and can be severe. Severe diarrhea can lead to the loss of too much body water (dehydration) and kidney problems. If you develop diarrhea during treatment with PIQRAY, tell your healthcare provider right away. Your healthcare provider may tell you to drink more fluids or take medicines to treat diarrhea.
Your healthcare provider may tell you to decrease your dose, temporarily stop your treatment, or completely stop your treatment with PIQRAY if you get certain serious side effects.
The most common side effects of PIQRAY when used with fulvestrant include:
|
rash |
|
decreased appetite |
|
weight loss |
|
nausea |
|
mouth sores |
|
hair loss |
|
tiredness and weakness |
|
vomiting |
changes in certain blood tests |
PIQRAY may affect fertility in males and in females who are able to become pregnant. Talk to your healthcare provider if this is a concern for you. These are not all of the possible side effects of PIQRAY.
Call your doctor for medical advice about side effects. You may report side effects to FDA at 1-800-FDA-1088.
How should I store PIQRAY?
Store PIQRAY at room temperature between 68°F to 77°F (20°C to 25°C). Keep PIQRAY and all medicines out of the reach of children. General information about the safe and effective use of PIQRAY
Medicines are sometimes prescribed for purposes other than those listed in a Patient Information leaflet. Do not use PIQRAY for a condition for which it was not prescribed. Do not give PIQRAY to other people, even if they have the same symptoms you have. It may harm them. You can ask your healthcare provider or pharmacist for more information about PIQRAY that is written for health professionals.
What are the ingredients in PIQRAY?
Active ingredient: alpelisib
Inactive ingredients: hypromellose, magnesium stearate, mannitol, microcrystalline cellulose, and sodium starch glycolate. The film-coating contains hypromellose, iron oxide black, iron oxide red, macrogol/polyethylene glycol (PEG) 4000, talc, and titanium dioxide.
Distributed by: Novartis Pharmaceuticals Corporation, East Hanover, New Jersey 07936
This Patient Information has been approved by the U.S. Food and Drug Administration. Issued: May 2019