通用中文 | 图卡替尼片 | 通用外文 | Tucatinib |
品牌中文 | 品牌外文 | Tukysa | |
其他名称 | 靶点HER2 | ||
公司 | 西雅图遗传(SEATTLE GENETICS) | 产地 | 美国(USA) |
含量 | 150mg | 包装 | 60片/盒 |
剂型给药 | 片剂 口服 | 储存 | 室温 |
适用范围 | 与曲妥珠单抗和卡培他滨联用,可用于治疗晚期不可切除或转移性HER2阳性乳腺癌患者。 |
通用中文 | 图卡替尼片 |
通用外文 | Tucatinib |
品牌中文 | |
品牌外文 | Tukysa |
其他名称 | 靶点HER2 |
公司 | 西雅图遗传(SEATTLE GENETICS) |
产地 | 美国(USA) |
含量 | 150mg |
包装 | 60片/盒 |
剂型给药 | 片剂 口服 |
储存 | 室温 |
适用范围 | 与曲妥珠单抗和卡培他滨联用,可用于治疗晚期不可切除或转移性HER2阳性乳腺癌患者。 |
生产企业】:西雅图基因技术公司(Seattle Genetics Inc.)
【规格】: 150mg/60片/瓶
【商标】:TUKYSA
【中文名】:妥卡替尼片剂
【英文名称】:Tucatinib tablets
【性状】:黄色涂层的片剂
【贮藏】:请在室温下68-77°F(20-25ºC) 储存TUKYSA。
【TUKYSA妥卡替尼适应症和用途】
TUKYSA是一种处方药,可与曲妥珠单抗和卡培他滨联用治疗人类表皮生长因子受体2 (HER2)阳性且已出现转移(如脑转移)或无法进行乳房切除术的乳腺癌成人患者,患者应接受过一种或多种抗HER2乳腺癌药物治疗。
【TUKYSA妥卡替尼剂量和给药方法】
剂量:TUKYSA推荐的起始剂量是300mg,一天两次。
【应该怎么服用TUKYSA?】
●请严格遵照医嘱服用TUKYSA。TUKYSA将与曲妥珠单抗和卡培他滨这两种药物一起使用,医生会告诉你曲妥珠单抗和卡培他滨的服用剂量以及如何服用它们。
●TUKYSA是口服给药,每天服用2次TUKYSA,可以与食物一起服用。
●每天服药时间应间隔12小时。
●请整粒吞咽药片,不要咀嚼或压碎、弄碎药片。如果药片破裂,请不要服用。
●如果你服药后出现呕吐或不慎错过了一剂剂量,请不要补充服用,而应直接在正常时间服用下一剂。
【TUKYSA妥卡替尼不良反应】
TUKYSA可能会导致严重的副作用,包括:
●腹泻;腹泻是TUKYSA常见的不良反应且有时可能很严重。如果你出现严重腹泻,请立刻告诉你的医生,因为严重的腹泻会导致大量体液流失(脱水)、低血压、肾脏问题甚至死亡。
●肝脏疾病;TUKYSA可能会导致严重的肝脏疾病。您的医生将根据需要在治疗前和治疗期间每3周对您的肝功能进行检测。如果您在治疗期间出现下列肝脏疾病的症状,请立即告诉您的医生:
■瘙痒
■皮肤或眼睛黄染
■尿液呈深褐色
■腹部右上侧疼痛
■觉得很累
■食欲下降
■易出血或易出现瘀伤
TUKYSA最常见的副作用:
●腹泻
●手掌或脚掌红肿、疼痛、肿胀或出现红疹、水泡
●口腔溃疡
●食欲下降
●腹部疼痛
●恶心想吐
●疲劳
●肝功能检测指标水平上升
●呕吐
●头疼
●贫血
●皮疹
●TUKYSA可能会影响男性和女性的生育能力。
如果您出现上述副作用,医生可能会改变您的治疗剂量或停止治疗。如有任何疑问,请咨询您的医生。
【TUKYSA妥卡替尼药物相互作用】
如果您正在使用TUKYSA治疗,请不要服用下列药物:
●强CYP3A抑制剂药物,包括抗真菌药物酮康唑等;该类药物会增加TUKYSA的药效。
●强CYP3A诱导剂药物,包括抗结核药物利福平等;该类药物会减少TUKYSA的药效。
●p-糖蛋白底物药物,包括钙通道阻滞剂维拉帕米、类固醇药物地塞米松等;因为该类药物会增加TUKYSA的药效。
【TUKYSA妥卡替尼在特殊人群中使用】
(1) 孕妇
TUKYSA可能会伤害发育中的胎儿,因此孕妇不应服用TUKYSA。如果您在TUKYSA治疗期间可能怀孕,请务必在TUKYSA治疗期间和治疗后一星期内采取有效的避孕措施。
(2) 母乳喂养
正在或计划母乳喂养的女性不应服用TUKYSA。
【TUKYSA妥卡替尼一般描述】
1.TUKYSA是什么?
TUKYSA是一种处方药,可与曲妥珠单抗和卡培他滨联用用于治疗:
●人类表皮生长因子受体2 (HER2)阳性的且已出现转移(如脑转移) 或无法进行乳房切除术的乳腺癌成人患者,患者应接受过一种或多种抗HER2乳腺癌药物治疗。
●TUKYSA应与曲妥珠单抗和卡培他滨联合使用。目前还不知道这种药对儿童是否安全有效。
2.TUKYSA的成分是什么?
●活性成分:妥卡替尼(Tucatinib);
●非活性成分:片芯:共聚维酮,交聚维酮,氯化钠,氯化钾,碳酸氢钠,胶体二氧化硅,硬脂酸镁,微晶纤维素;片剂涂层:聚乙烯醇、二氧化钛、聚乙二醇、滑石粉和黄色氧化铁。
【TUKYSA妥卡替尼作用机制】
TUKYSA是一种酪氨酸激酶抑制剂。酪氨酸激酶是一种帮助控制细胞生长和分裂等功能的酶。如果酶太活跃或者细胞中酶太多,就会使细胞无法控制地生长。TUKYSA阻断了癌细胞中HER2基因的一个特定区域,从而阻止癌细胞的生长和扩散。
【患者资讯资料】
关于TUKYSA妥卡替尼我应该知道的最重要的信息是什么?
在服用TUKYSA之前,请告诉医生你的所有健康状况,包括你是否:
●患有肝脏疾病;
●正在怀孕或计划怀孕;因为TUKYSA可能会伤害你未出生的宝宝。
对于可能怀孕的女性:医生会在开始治疗前为您做怀孕测试。请您在TUKYSA治疗期间和治疗后一星期内采取有效的避孕措施。如果您在治疗期间怀孕,请立刻告诉你的医生。
男性患者应在治疗期间和治疗后一星期内采取有效避孕措施,以防止伴侣在其治疗期间怀孕。
●正在或计划母乳喂养;目前还不知道TUKYSA是否会进入乳汁中,因此在治疗期间和治疗后一星期内请不要进行母乳喂养。
●请告诉医生正在你服用的所有药物,包括处方药、非处方药、维生素和草药补充剂;因为TUKYSA可能会与这些药物发生相互作用。
【我应该如何存储TUKYSA妥卡替尼?】
●请在室温下68-77°F(20- 25ºC) 储存TUKYSA。
●请把TUKYSA置于原容器内保存。瓶内干燥剂可使药片保持干燥。
●服完药后,请拧紧药瓶。TUKYSA必须在开瓶后3个月内使用,请不要使用过期药物。
●请将药品放在儿童接触不到的地方。
●请不要在没有医嘱的情况下擅自给其他人服用TUKYSA,即使他们有与你相似的症状。
【TUKYSA妥卡替尼临床试验经验】
TUKYSA治疗HER2阳性乳腺癌的批准是基于一项随机、双盲、安慰剂对照、阳性药物对照的临床试验。该试验在局部晚期不可切除性或转移性HER2阳性乳腺癌患者中开展,且入组的患者先前已接受过曲妥珠单抗、帕妥珠单抗、T-DM1(ado-trastuzumab emtansine)治疗,48%的患者在入组时存在脑转移。该试验将TUKYSA与曲妥珠单抗、卡培他滨联合用药与单独曲妥珠单抗、卡培他滨联合用药进行了对比。结果显示,与单独曲妥珠单抗、卡培他滨联用相比,TUKYSA与曲妥珠单抗、卡培他滨联合用药的方案表现出更优的疗效,患者的疾病进展和死亡风险降低了46%。在中期分析时,TUKYSA与曲妥珠单抗、卡培他滨联合用药方案的总生存期提高、死亡风险降低约34%、客观缓解率提高近一倍。脑转移的患者,TUKYSA与曲妥珠单抗、卡培他滨联合用药方案的疾病进展和死亡风险也显著降低(约52%)。
TUKYSA与曲妥珠单抗、卡培他滨联合用药的安全性良好,最常见的不良反应包括腹泻、手足综合征、恶心、疲劳和呕吐。3级或以上不良事件包括腹泻、天冬氨酸转氨酶、丙氨酸转氨酶和胆红素升高
生产企业】:西雅图基因技术公司(Seattle Genetics Inc.)
【规格】: 150mg/60片/瓶
【商标】:TUKYSA
【中文名】:妥卡替尼片剂
【英文名称】:Tucatinib tablets
【性状】:黄色涂层的片剂
【贮藏】:请在室温下68-77°F(20-25ºC) 储存TUKYSA。
【TUKYSA妥卡替尼适应症和用途】
TUKYSA是一种处方药,可与曲妥珠单抗和卡培他滨联用治疗人类表皮生长因子受体2 (HER2)阳性且已出现转移(如脑转移)或无法进行乳房切除术的乳腺癌成人患者,患者应接受过一种或多种抗HER2乳腺癌药物治疗。
【TUKYSA妥卡替尼剂量和给药方法】
剂量:TUKYSA推荐的起始剂量是300mg,一天两次。
【应该怎么服用TUKYSA?】
●请严格遵照医嘱服用TUKYSA。TUKYSA将与曲妥珠单抗和卡培他滨这两种药物一起使用,医生会告诉你曲妥珠单抗和卡培他滨的服用剂量以及如何服用它们。
●TUKYSA是口服给药,每天服用2次TUKYSA,可以与食物一起服用。
●每天服药时间应间隔12小时。
●请整粒吞咽药片,不要咀嚼或压碎、弄碎药片。如果药片破裂,请不要服用。
●如果你服药后出现呕吐或不慎错过了一剂剂量,请不要补充服用,而应直接在正常时间服用下一剂。
【TUKYSA妥卡替尼不良反应】
TUKYSA可能会导致严重的副作用,包括:
●腹泻;腹泻是TUKYSA常见的不良反应且有时可能很严重。如果你出现严重腹泻,请立刻告诉你的医生,因为严重的腹泻会导致大量体液流失(脱水)、低血压、肾脏问题甚至死亡。
●肝脏疾病;TUKYSA可能会导致严重的肝脏疾病。您的医生将根据需要在治疗前和治疗期间每3周对您的肝功能进行检测。如果您在治疗期间出现下列肝脏疾病的症状,请立即告诉您的医生:
■瘙痒
■皮肤或眼睛黄染
■尿液呈深褐色
■腹部右上侧疼痛
■觉得很累
■食欲下降
■易出血或易出现瘀伤
TUKYSA最常见的副作用:
●腹泻
●手掌或脚掌红肿、疼痛、肿胀或出现红疹、水泡
●口腔溃疡
●食欲下降
●腹部疼痛
●恶心想吐
●疲劳
●肝功能检测指标水平上升
●呕吐
●头疼
●贫血
●皮疹
●TUKYSA可能会影响男性和女性的生育能力。
如果您出现上述副作用,医生可能会改变您的治疗剂量或停止治疗。如有任何疑问,请咨询您的医生。
【TUKYSA妥卡替尼药物相互作用】
如果您正在使用TUKYSA治疗,请不要服用下列药物:
●强CYP3A抑制剂药物,包括抗真菌药物酮康唑等;该类药物会增加TUKYSA的药效。
●强CYP3A诱导剂药物,包括抗结核药物利福平等;该类药物会减少TUKYSA的药效。
●p-糖蛋白底物药物,包括钙通道阻滞剂维拉帕米、类固醇药物地塞米松等;因为该类药物会增加TUKYSA的药效。
【TUKYSA妥卡替尼在特殊人群中使用】
(1) 孕妇
TUKYSA可能会伤害发育中的胎儿,因此孕妇不应服用TUKYSA。如果您在TUKYSA治疗期间可能怀孕,请务必在TUKYSA治疗期间和治疗后一星期内采取有效的避孕措施。
(2) 母乳喂养
正在或计划母乳喂养的女性不应服用TUKYSA。
【TUKYSA妥卡替尼一般描述】
1.TUKYSA是什么?
TUKYSA是一种处方药,可与曲妥珠单抗和卡培他滨联用用于治疗:
●人类表皮生长因子受体2 (HER2)阳性的且已出现转移(如脑转移) 或无法进行乳房切除术的乳腺癌成人患者,患者应接受过一种或多种抗HER2乳腺癌药物治疗。
●TUKYSA应与曲妥珠单抗和卡培他滨联合使用。目前还不知道这种药对儿童是否安全有效。
2.TUKYSA的成分是什么?
●活性成分:妥卡替尼(Tucatinib);
●非活性成分:片芯:共聚维酮,交聚维酮,氯化钠,氯化钾,碳酸氢钠,胶体二氧化硅,硬脂酸镁,微晶纤维素;片剂涂层:聚乙烯醇、二氧化钛、聚乙二醇、滑石粉和黄色氧化铁。
【TUKYSA妥卡替尼作用机制】
TUKYSA是一种酪氨酸激酶抑制剂。酪氨酸激酶是一种帮助控制细胞生长和分裂等功能的酶。如果酶太活跃或者细胞中酶太多,就会使细胞无法控制地生长。TUKYSA阻断了癌细胞中HER2基因的一个特定区域,从而阻止癌细胞的生长和扩散。
【患者资讯资料】
关于TUKYSA妥卡替尼我应该知道的最重要的信息是什么?
在服用TUKYSA之前,请告诉医生你的所有健康状况,包括你是否:
●患有肝脏疾病;
●正在怀孕或计划怀孕;因为TUKYSA可能会伤害你未出生的宝宝。
对于可能怀孕的女性:医生会在开始治疗前为您做怀孕测试。请您在TUKYSA治疗期间和治疗后一星期内采取有效的避孕措施。如果您在治疗期间怀孕,请立刻告诉你的医生。
男性患者应在治疗期间和治疗后一星期内采取有效避孕措施,以防止伴侣在其治疗期间怀孕。
●正在或计划母乳喂养;目前还不知道TUKYSA是否会进入乳汁中,因此在治疗期间和治疗后一星期内请不要进行母乳喂养。
●请告诉医生正在你服用的所有药物,包括处方药、非处方药、维生素和草药补充剂;因为TUKYSA可能会与这些药物发生相互作用。
【我应该如何存储TUKYSA妥卡替尼?】
●请在室温下68-77°F(20- 25ºC) 储存TUKYSA。
●请把TUKYSA置于原容器内保存。瓶内干燥剂可使药片保持干燥。
●服完药后,请拧紧药瓶。TUKYSA必须在开瓶后3个月内使用,请不要使用过期药物。
●请将药品放在儿童接触不到的地方。
●请不要在没有医嘱的情况下擅自给其他人服用TUKYSA,即使他们有与你相似的症状。
【TUKYSA妥卡替尼临床试验经验】
TUKYSA治疗HER2阳性乳腺癌的批准是基于一项随机、双盲、安慰剂对照、阳性药物对照的临床试验。该试验在局部晚期不可切除性或转移性HER2阳性乳腺癌患者中开展,且入组的患者先前已接受过曲妥珠单抗、帕妥珠单抗、T-DM1(ado-trastuzumab emtansine)治疗,48%的患者在入组时存在脑转移。该试验将TUKYSA与曲妥珠单抗、卡培他滨联合用药与单独曲妥珠单抗、卡培他滨联合用药进行了对比。结果显示,与单独曲妥珠单抗、卡培他滨联用相比,TUKYSA与曲妥珠单抗、卡培他滨联合用药的方案表现出更优的疗效,患者的疾病进展和死亡风险降低了46%。在中期分析时,TUKYSA与曲妥珠单抗、卡培他滨联合用药方案的总生存期提高、死亡风险降低约34%、客观缓解率提高近一倍。脑转移的患者,TUKYSA与曲妥珠单抗、卡培他滨联合用药方案的疾病进展和死亡风险也显著降低(约52%)。
TUKYSA与曲妥珠单抗、卡培他滨联合用药的安全性良好,最常见的不良反应包括腹泻、手足综合征、恶心、疲劳和呕吐。3级或以上不良事件包括腹泻、天冬氨酸转氨酶、丙氨酸转氨酶和胆红素升高
Company: Seattle Genetics, Inc.
Date of Approval: April 17, 2020
Treatment for: Breast Cancer
Tukysa (tucatinib) is a kinase inhibitor indicated in combination with trastuzumab and capecitabine for the treatment of patients with advanced unresectable or metastatic HER2-positive breast cancer.
BOTHELL, Wash.--(BUSINESS WIRE) April 17, 2020 -- Seattle Genetics, Inc. (Nasdaq:SGEN) today announced the U.S. Food and Drug Administration (FDA) granted approval to Tukysa™ (tucatinib) tablets in combination with trastuzumab and capecitabine for adult patients with advanced unresectable (cannot be surgically removed) or metastatic HER2-positive breast cancer, including patients with brain metastases (disease that has spread to the brain), who have received one or more prior anti-HER2-based regimens in the metastatic setting. The FDA previously granted Breakthrough Therapy designation and Priority Review for Tukysa and reviewed this application for approval under the Real-Time Oncology Review (RTOR) pilot program. The Tukysa New Drug Application (NDA) is also part of Project Orbis, an initiative of the FDA Oncology Center of Excellence that provides a framework for concurrent submission and review of oncology drugs among participating international health authorities. Tukysa is an oral, small molecule tyrosine kinase inhibitor (TKI) of HER2, a protein that contributes to cancer cell growth.1,2
“With highly significant and clinically important results for overall and progression-free survival, the addition of Tukysa to trastuzumab and capecitabine has the potential to become a standard of care for people with HER2-positive metastatic breast cancer after having received one or more previous anti-HER2 therapies in the metastatic setting,” said Eric P. Winer, MD, Chief of the Division of Breast Oncology, Susan F. Smith Center for Women's Cancers at Dana-Farber. “Cancer spreads to the brain in up to half of patients with HER2-positive metastatic breast cancer; and this approval is based on a unique clinical trial that included patients with active brain metastases, either untreated or progressing. Tukysa is well tolerated by patients and is a valuable addition to the agents we have for HER2-positive metastatic breast cancer.”
“We’re pleased to have collaborated with the FDA on our second expedited real-time oncology review, enabling us to rapidly bring this new targeted medicine to patients,” said Clay Siegall, Ph.D., Chief Executive Officer at Seattle Genetics. “Tukysa has shown impressive results in people with HER2-positive metastatic breast cancer, including in patients with active brain metastases, and offers patients an effective medicine following previous treatment with other anti-HER2 agents in the metastatic setting.”
Tukysa, in combination with trastuzumab and capecitabine, was evaluated in the trial HER2CLIMB, a randomized (2:1), double-blind, placebo-controlled trial that enrolled 612 patients with HER2-positive unresectable locally advanced or metastatic breast cancer who had previously received, either separately or in combination, trastuzumab, pertuzumab, and ado-trastuzumab emtansine (T-DM1). Forty-eight percent of patients in the study had a presence or history of brain metastases. The primary efficacy outcome measure was progression-free survival (PFS) as assessed by blinded independent central review (BICR) in the first 480 randomized patients.1 Additional efficacy outcome measures were evaluated in all randomized patients and included overall survival (OS), PFS in patients with a history or presence of brain metastases, and confirmed objective response rate (ORR).
Patients who received Tukysa in combination with trastuzumab and capecitabine had a 46 percent reduction in the risk of cancer progression or death (PFS) compared to patients who received trastuzumab and capecitabine alone (hazard ratio (HR)=0.54 [95% Confidence Interval (CI): 0.42, 0.71]; p<0.00001). The addition of Tukysa reduced the risk of death (OS) by 34 percent compared to trastuzumab and capecitabine alone (HR=0.66 [95% CI: 0.50, 0.87]; p=0.0048). Nearly twice the number of patients who received Tukysa in combination with trastuzumab and capecitabine had a confirmed objective response compared to those who received trastuzumab and capecitabine alone (40.6 percent (95% CI: 35.3, 46.0) vs. 22.8 percent (95% CI: 16.7, 29.8); p=0.00008). For patients with brain metastases, the addition of Tukysa reduced the risk of cancer progression or death (PFS) by 52 percent compared to trastuzumab and capecitabine alone (HR=0.48 [95% CI: 0.34, 0.69]; p<0.00001).
Serious adverse reactions occurred in 26 percent of patients who received Tukysa. Serious adverse reactions occurring in 2 percent or more of patients who received Tukysa were diarrhea (4%), vomiting (2.5%), nausea, abdominal pain, and seizure (2% each). The most common adverse reactions occurring in 20 percent or more of patients who received Tukysa were diarrhea, palmar-plantar erythrodysesthesia, nausea, fatigue, hepatotoxicity, vomiting, stomatitis, decreased appetite, abdominal pain, headache, anemia, and rash. Adverse reactions leading to treatment discontinuation occurred in 6 percent of patients who received Tukysa; adverse reactions leading to treatment discontinuation of Tukysa (in 1 percent or more of patients) were hepatotoxicity (1.5%) and diarrhea (1%).
The data were published in The New England Journal of Medicine in December 2019.
About Tukysa (tucatinib)
TUKYSA is an oral medicine that is a tyrosine kinase inhibitor of the HER2 protein. In vitro (in lab studies), Tukysa inhibited phosphorylation of HER2 and HER3, resulting in inhibition of downstream MAPK and AKT signaling and cell growth (proliferation), and showed anti-tumor activity in HER2-expressing tumor cells. In vivo (in living organisms), Tukysa inhibited the growth of HER2-expressing tumors. The combination of Tukysa and the anti-HER2 antibody trastuzumab showed increased anti-tumor activity in vitro and in vivo compared to either medicine alone.1
SeaGen Secure offers access and reimbursement support to help patients access TUKYSA. For more information, go to SeaGenSecure.com.
About HER2-Positive Breast Cancer
Patients with HER2-positive breast cancer have tumors with high levels of a protein called human epidermal growth factor receptor 2 (HER2), which promotes the growth of cancer cells. An estimated 279,100 new cases of breast cancer will be diagnosed in the U.S. in 2020.3 Between 15 and 20 percent of breast cancer cases are HER2-positive.3 Historically, HER2-positive breast cancer tends to be more aggressive and more likely to recur than HER2-negative breast cancer.4,5,6 Up to 50 percent of metastatic HER2-positive breast cancer patients develop brain metastases over time.7,8,9
Important Safety Information
Warnings and Precautions
· Diarrhea – Tukysa can cause severe diarrhea including dehydration, hypotension, acute kidney injury, and death. In HER2CLIMB, 81% of patients who received Tukysa experienced diarrhea, including 12% with Grade 3 diarrhea and 0.5% with Grade 4 diarrhea. Both patients who developed Grade 4 diarrhea subsequently died, with diarrhea as a contributor to death. The median time to onset of the first episode of diarrhea was 12 days and the median time to resolution was 8 days. Diarrhea led to dose reductions of Tukysa in 6% of patients and discontinuation of Tukysa in 1% of patients. Prophylactic use of antidiarrheal treatment was not required on HER2CLIMB.
If diarrhea occurs, administer antidiarrheal treatment as clinically indicated. Perform diagnostic tests as clinically indicated to exclude other causes of diarrhea. Based on the severity of the diarrhea, interrupt dose, then dose reduce or permanently discontinue Tukysa.
· Hepatotoxicity – TUKYSA can cause severe hepatotoxicity. In HER2CLIMB, 8% of patients who received Tukysa had an ALT increase >5 × ULN, 5% had an AST increase >5 × ULN, and 1.5% had a bilirubin increase >3 × ULN (Grade ≥3). Hepatotoxicity led to dose reduction of Tukysa in 8% of patients and discontinuation of Tukysa in 1.5% of patients.
Monitor ALT, AST, and bilirubin prior to starting Tukysa, every 3 weeks during treatment, and as clinically indicated. Based on the severity of hepatoxicity, interrupt dose, then dose reduce or permanently discontinue Tukysa.
· Embryo-Fetal Toxicity – Tukysa can cause fetal harm. Advise pregnant women and females of reproductive potential risk to a fetus. Advise females of reproductive potential, and male patients with female partners of reproductive potential, to use effective contraception during Tukysa treatment and for at least 1 week after the last dose.
Adverse Reactions
Serious adverse reactions occurred in 26% of patients who received Tukysa. Serious adverse reactions in ≥2% of patients who received Tukysa were diarrhea (4%), vomiting (2.5%), nausea (2%), abdominal pain (2%), and seizure (2%). Fatal adverse reactions occurred in 2% of patients who received Tukysa including sudden death, sepsis, dehydration, and cardiogenic shock.
Adverse reactions led to treatment discontinuation in 6% of patients who received Tukysa; those occurring in ≥1% of patients were hepatotoxicity (1.5%) and diarrhea (1%). Adverse reactions led to dose reduction in 21% of patients who received Tukysa; those occurring in ≥2% of patients were hepatotoxicity (8%) and diarrhea (6%).
The most common adverse reactions in patients who received Tukysa (≥20%) were diarrhea, palmar-plantar erythrodysesthesia, nausea, fatigue, hepatotoxicity, vomiting, stomatitis, decreased appetite, abdominal pain, headache, anemia, and rash.
Lab Abnormalities
In HER2CLIMB, Grade ≥3 laboratory abnormalities reported in ≥5% of patients who received TUKYSA were: decreased phosphate, increased ALT, decreased potassium, and increased AST. The mean increase in serum creatinine was 32% within the first 21 days of treatment with TUKYSA. The serum creatinine increases persisted throughout treatment and were reversible upon treatment completion. Consider alternative markers of renal function if persistent elevations in serum creatinine are observed.
Drug Interactions
· Strong CYP3A or Moderate CYP2C8 Inducers: Concomitant use may decrease Tukysa activity. Avoid concomitant use of Tukysa.
· Strong or Moderate CYP2C8 Inhibitors: Concomitant use of Tukysa with a strong CYP2C8 inhibitor may increase the risk of Tukysa toxicity; avoid concomitant use. Increase monitoring for TUKYSA toxicity with moderate CYP2C8 inhibitors.
· CYP3A Substrates: Concomitant use may increase the toxicity associated with a CYP3A substrate. Avoid concomitant use of Tukysa where minimal concentration changes may lead to serious or life-threatening toxicities. If concomitant use is unavoidable, decrease the CYP3A substrate dosage.
· P-gp Substrates: Concomitant use may increase the toxicity associated with a P-gp substrate. Consider reducing the dosage of P-gp substrates where minimal concentration changes may lead to serious or life-threatening toxicity.
Use in Specific Populations
· Lactation: Advise women not to breastfeed while taking Tukysa and for at least 1 week after the last dose.
· Renal Impairment: Use of Tukysa in combination with capecitabine and trastuzumab is not recommended in patients with severe renal impairment (CLcr < 30 mL/min), because capecitabine is contraindicated in patients with severe renal impairment.
· Hepatic Impairment: Reduce the dose of TUKYSA for patients with severe (Child-Pugh C) hepatic impairment.
For more information, please see the full Prescribing Information for Tukysa.
About Seattle Genetics
Seattle Genetics, Inc. is a global biotechnology company that discovers, develops and commercializes transformative medicines targeting cancer to make a meaningful difference in people’s lives. The company is headquartered in Bothell, Washington, and has offices in California, Switzerland and the European Union. For more information on our robust pipeline, visit www.seattlegenetics.com and follow @SeattleGenetics on Twitter.
Forward Looking Statements
Certain statements made in this press release are forward looking, such as those, among others, relating to the therapeutic potential of TUKYSA including its efficacy, safety and therapeutic uses and the potential of TUKYSA in combination with trastuzumab and capecitabine to become a standard of care for people with HER2-positive metastatic breast cancer who have received one or more previous anti-HER2 therapies. Actual results or developments may differ materially from those projected or implied in these forward-looking statements. Factors that may cause such a difference include the possibility that adverse events or safety signals may occur; that utilization and adoption of TUKYSA by prescribing physicians may be limited due to impacts related to the COVID-19 pandemic, including potential difficulties associated with commercializing a new therapeutic agent during the global disruptions created by the COVID pandemic, availability and extent of reimbursement or other factors; and that adverse regulatory actions may occur. More information about the risks and uncertainties faced by Seattle Genetics is contained under the caption “Risk Factors” included in the company’s Annual Report on Form 10-K for the year ended December 31, 2019 filed with the Securities and Exchange Commission. Seattle Genetics disclaims any intention or obligation to update or revise any forward-looking statements, whether as a result of new information, future events or otherwise, except as required by law.
1. [1] TUKYSA [package insert]. Bothell, WA: Seattle Genetics, Inc.
2. [2] Anita Kulukian, Patrice Lee, Janelle Taylor, et al. Preclinical Activity of HER2-Selective Tyrosine Kinase Inhibitor Tucatinib as a Single Agent or in Combination with Trastuzumab or Docetaxel in Solid Tumor ModelsMol Cancer Ther2020;19:976-987.
3. [3] Cancer Facts & Figures 2020. American Cancer Society website. https://www.cancer.org/content/dam/cancer-org/research/cancer-facts-and-statistics/annual-cancer-facts-and-figures/2020/cancer-facts-and-figures-2020.pdf. Accessed March 10, 2020.
4. [3] Loibli S, Gianni L. HER2-positive breast cancer. Lancet. 2017; 389(10087): 2415-29.
5. [4] Slamon D, Clark G, Wong S, et al. Human breast cancer: correlation of relapse and survival with amplification of the HER-2/neu oncogene. Science. 1987; 235(4785): 177-82.
6. [5] Breast Cancer HER2 Status. American Cancer Society website. https://www.cancer.org/cancer/breast-cancer/understanding-a-breast-cancer-diagnosis/breast-cancer-her2-status.html. Accessed March 9, 2020.
7. [6] Freedman RA, Gelman RS, Anders CK, et al. TBCRC 022: a phase II trial of neratinib and capecitabine for patients with human epidermal growth factor receptor 2-positive breast cancer and brain metastases. J Clin Oncol. 2019;37:1081-1089.
8. [7] Olson EM, Najita JS, Sohl J, et al. Clinical outcomes and treatment practice patterns of patients with HER2-positive metastatic breast cancer in the post-trastuzumab era. Breast. 2013;22:525-531.
9. [8] Bendell JC, Domchek SM, Burstein HJ, et al. Central nervous system metastases in women who receive trastuzumab-based therapy for metastatic breast carcinoma. Cancer. 2003;97:2972-2977.
10.
11. Source: Seattle Genetics, Inc.
Posted: April 2020