通用中文 | 吉非替尼片 | 通用外文 | Gefitinib Tablets |
品牌中文 | 品牌外文 | geftinat | |
其他名称 | 易瑞沙、印度易瑞沙、Iressa靶点EGFR | ||
公司 | NATCO(NATCO) | 产地 | 印度(India) |
含量 | 250mg | 包装 | 30片/瓶 |
剂型给药 | 片剂 口服 | 储存 | 室温 |
适用范围 | 非小细胞肺癌 肺癌 |
通用中文 | 吉非替尼片 |
通用外文 | Gefitinib Tablets |
品牌中文 | |
品牌外文 | geftinat |
其他名称 | 易瑞沙、印度易瑞沙、Iressa靶点EGFR |
公司 | NATCO(NATCO) |
产地 | 印度(India) |
含量 | 250mg |
包装 | 30片/瓶 |
剂型给药 | 片剂 口服 |
储存 | 室温 |
适用范围 | 非小细胞肺癌 肺癌 |
以下资料仅供参考:
文案整理: Dr. Jasmine Ding
吉非替尼使用说明:
美国FDA初次批准:2015
请仔细阅读说明书并在医师指导下使用:
【商品名称】
通用名称: 吉非替尼
品牌名称:Giftinat
通用英文名称:Gefitinib
其他名称:IRESSA, 易瑞沙,印度易瑞沙
【成分】
本品主要成分为Gefitinib
化学名:4-[(4-甲基-1-哌嗪)甲基]-N-[4-甲基-3-[[4-(3-吡啶)-2-嘧啶]氨基]苯基]-苯胺甲磺酸盐。
分子式:C32H33ClFN5O11
[适应症/功能主治】
适用于转移性非小细胞肺癌(NSCLC)的一线治疗,适用于具有表皮生长因子受体(EGFR)外显子19缺失或外显子21(L858R)替代突变的肿瘤。(FDA批准的检测方法)
使用限制:吉非替尼在肿瘤细胞有其他EGFR突变的患者身上的的安全性和有效性尚未确定。
【规格型号】250mg片剂*30片/盒
【用法用量】
吉非替尼的成人推荐剂量为250mg,每日1次,口服,空腹或与食物同服。直至疾病进展或患者耐受。
若漏服,请勿在下次剂量的12小时内加服漏药。
如果有吞咽困难,可将片剂分散于半杯饮用水中(非碳酸饮料),不得使用其他液体。将片剂丢入水中, 无需压碎,搅拌至完全分散(约需10分钟),即刻饮下药液。以半杯水冲洗杯子,饮下。也可通过鼻-胃管给予该药液。
无需因下述情况不同调整给药剂量:年龄、体重、性别、种族,肾功能,因肝转移而引起的中至重度肝功能损害。
剂量调整:当患者出现不能耐受的腹泻或皮肤不良反应时,可通过短期暂停治疗(多14天)解决,随后恢复每天250mg的剂量。
【不良反应】
常见(发生率20%以上)的药物不良反应为:腹泻、皮疹、瘙痒、皮肤干燥和痤疮。
一般见于服药后的第1个月内,通常是可逆性的。
大约8%的患者出现严重的药物不良反应(CTC标准3或4级)。
因不良反应停止治疗的患者仅有1%。
各身体系统发生的不良反应按发生频率以降序排列:(多见:≥10%;常见:≥1%且<10%;少见:≥0.1%且<1%;罕见:≥0.01%且<0.1%;极罕见:<0.01%)。
可出现的不良事件总结如下:
消化系统:
多见腹泻,主要为轻度(CTC1级),少有中度(CTC2级),个别报道严重伴脱水的腹泻(CTC3级)。
常见恶心,主要为轻度(CTC1级);呕吐,主要为轻度或中度(CTC1或2级);厌食,轻度或中度(CTC1或2级);口腔粘膜炎,多为轻度(CTC1级);继发于腹泻,恶心,呕吐或厌食的脱水口腔溃疡。
少见胰腺炎。
皮肤及附件:
多见皮肤反应,主要为轻度或中度(CTC1或2级);脓疱性皮疹,在红斑的基础上有时伴皮肤干燥发痒。常见指甲异常。极罕见中毒性表皮坏死松懈症和多形红斑的报道,过敏反应,包括血管形水肿和荨麻疹。
代谢和营养:
常见肝功能异常,主要包括无症状性的轻度或中度转氨酶升高(CTC1或2级)。
全身:常见乏力,多为轻度(CTC1级);脱发;体重下降;外周性水肿。
眼科:
常见结膜炎和睑炎,主要为轻度(CTC1级);弱视。
少见可逆性角膜糜烂,有时伴睫毛生长异常。
极罕见角膜脱落;眼部缺血/出血。
血液和淋巴:
常见出血,如鼻衄和血尿。
少见在服用华法林的一些患者中出现INR(International Normalised Ratio)升高及/或出血事件;出血性膀胱炎。
呼吸:
常见呼吸困难。
少见间质性肺病,常较严重(CTC3-4级。在全球进行的临床研究,扩大用药/同情用药,上市后使用中,约有158348名患者接受了吉非替尼治疗,在日本以外的地区,包括约92821名患者,间质性肺病总的发生率约为0.28%,在日本其发生率约为1.70%,包括约65527名患者,数据截至2004年6月2日),已有致死性病例的报道。
【禁忌】无
【注意事项】
偶尔观察到发生间质性肺病,患者通常出现急性的呼吸困难,伴有咳嗽,低热,呼吸道不适和动脉血氧不饱和。短期内该症状可发展得很严重,并报告有死亡。放射学检查常显示肺浸润或间质有毛玻璃样阴影。已观察到在出现该状况的患者中,伴有原发性肺纤维化/间质性肺炎/尘肺/放射性肺炎/药物诱导性肺炎的患者死亡率较高。
处方医生应密切监测间质性肺病发生的迹象,如果患者呼吸道症状加重,应中断治疗,立即进行检查。当证实有间质性肺病时,应停止使用,并对患者进行相应的治疗。
已观察到无症状性肝转氨酶升高。因此,建议定期检查肝功能。肝转氨酶轻中度升高的患者应慎用。如果肝转氨酶升高加重,应考虑停药。
已报道在服用华法林的一些患者中出现INR(InternationalNormalisedRatio,国际标准化比率)升高及/或出血事件。服用华法林的患者应定期监测凝血酶原时间或INR的改变。应告诫患者当以下情况加重时即刻就医:
眼部症状;
严重或持续的腹泻,恶心,呕吐或厌食;这些症状应按临床需要进行处理。
对驾驶及操纵机器能力的影响:在治疗期间,可出现乏力的症状,出现这些症状的患者在驾驶或操纵机器时应给予提醒。
【孕妇及哺乳期妇女用药】
妊娠期使用:目前尚无吉非替尼用于妊娠期女性的资料。在接受吉非替尼治疗期间,要劝告育龄女性避免妊娠。
哺乳期使用:在接受吉非替尼治疗期间,应建议哺乳母亲停止母乳喂养。
目前尚无吉非替尼用于哺乳期女性的资料。
【儿童用药】
目前尚无吉非替尼用于儿童或青春期患者安全性与疗效的资料,故不推荐使用。
【老年用药】
老年人用药安全性方面与年轻患者无显著差异。有效性方面的数据尚不足。
【药理作用】
表皮生长因子受体(EGFR)在正常细胞和癌细胞的细胞表面均有表达,他们在细胞生长和增殖过程中起作用。一些NSCLC细胞的EGFR激活突变(外显子19缺失或外显子21的点突变L858R)已被鉴定为促进肿瘤细胞生长,阻断凋亡,增加血管生成因子的产生并促进肿瘤的转移过程。
吉非替尼可逆地抑制EGFR的野生型和某些EGFR激活突变的激酶活性,阻止受体相关的酪氨酸残基的自磷酸化,从而抑制进一步的下游信号传导并阻断EGFR依赖性增殖。
吉非替尼对EGFR外显子19缺失或外显子21点突变L858R突变的结合亲和力高于其对野生型EGFR的亲和力。在临床上,吉非替尼还能抑制IGF和PDGF介导的信号的相关浓度;对其他酪氨酸激酶受体的抑制作用尚未被充分定性。
[药代动力学】
吸收和分布
吉非替尼的平均口服生物利用度为60%,给药后3-7小时出现峰值血浆水平。 食物对吉非替尼的生物利用度改变无临床有意 义。 可以与食物一起服用。
吉非替尼广泛分布在全身,静脉给药后平均稳态体积分布为1400升。 在体外,吉非替尼与人血浆蛋白(血清白蛋白α1-酸性 糖蛋白结合和. 1酸 糖蛋白)的体外结合率为90%,与药物浓度无关。 吉非替尼是膜转运糖蛋白的底物 (P-gp),但是当 P-gp在较高浓度下饱和时,不太可能影响吉非替尼吸收。
代谢与清除:
体外研究数据表明参与吉非替尼氧化代谢的P450同工酶主要是CYP3A4。
体外研究显示吉非替尼可有限地抑制CYP2D6。
吉非替尼的代谢中三个生物转化的位点已被确定:N-丙基吗啉基团的代谢,喹唑啉上甲氧取代基的脱甲基作用及卤化苯基基团类的氧化脱氟作用。
在人血浆中鉴别到的主要代谢物是O-去甲基吉非替尼。它对EGFR刺激细胞生长的抑制作用比吉非替尼弱14倍,因此对吉非替尼的临床活性不太可能有显著作用。
吉非替尼总的血浆清除率约为500mL/分。主要通过粪便排泄,少于4%通过肾脏以原型和代谢物的形式清除。
【药物相互作用】
吉非替尼主要通过肝细胞色素P-450系的CYP3A4代谢。所以吉非替尼可能会与诱导、抑制同一肝酶代谢的药物发生相互作用。
以下列出了与吉非替尼产生或可能产生有临床意义地药物相互作用地药物或药物类别:
影响吉非替尼的药物:
CYP3A4抑制剂:伊曲康唑,酮康唑,克霉唑,利托那韦可能抑制吉非替尼的代谢。
升高胃pH值的药物:可能降低吉非替尼疗效。
利福平:吉非替尼与利福平(已知的强CYP3A4诱导剂)同时给药吉非替尼的平均AUC比单服时降低83%。
理论上可能有相互作用的药物-其他CYP3A4诱导剂:诱导CYP3A4活性的物质可增加吉非替尼的代谢并降低其血浆浓度。因此,与CYP3A4诱导剂(如苯妥因、卡马西平、巴比妥类或圣约翰草)合用可降低疗效。
吉非替尼对其他药物的作用:已证明的相互作用-通过CYP2D6代谢的药物:吉非替尼与美托洛尔(一种CYP2D6酶底物)合用,使美托洛尔的暴露量升高35%。吉非替尼与其他由CYP2D6代谢的药物同服,可能会升高后者的血药浓度。
理论上可能有相互作用的药物-华法林:虽然迄今尚未进行正规的药物相互作用研究,在一些服用华法林的患者中报告了INR增高和/或出血事件。服用华法林的患者应定期监测其凝血酶原时间或INR的改变。
【药物过量】
对于服用过量吉非替尼还没有专门的治疗方法,现在尚不知过量服用可能的症状。
【药理毒理】
非临床(体外)研究资料表明,吉非替尼具有抑制心脏动作电位复极化过程(如QT间期)的可能性。但由临床研究和上市后监测获得的安全性资料未提示吉非替尼对心脏有任何不良作用。
致癌,致畸和生殖毒性未进行吉非替尼的致癌研究。在基因突变分析(细菌和体外哺乳动物细胞)和裂解试验(体外哺乳动物细胞和体内大鼠微核试验)中,吉非替尼未显示基因毒性作用。
在器官发生期给予可产生母体毒性剂量的吉非替尼,在大鼠中可观察到成骨不全的发生率升高,在家兔中可观察到胎儿体重下降。在大鼠中未观察到畸形,仅在产生严重母体毒性的剂量下可在家兔中观察到畸形。
当给予哺乳大鼠口服5mg/kg吉非替尼(按体表面积计为临床用药剂量的0.2倍),吉非替尼及某些代谢产物广泛分泌入乳汁。
【贮藏】
20--25°C保存。
文案整理: Dr. Jasmine Ding
吉非替尼使用说明:
美国FDA初次批准:2015
请仔细阅读说明书并在医师指导下使用:
【商品名称】
通用名称: 吉非替尼
品牌名称:IRESSA
通用英文名称:Gefitinib
其他名称:Giftinat, 易瑞沙,印度易瑞沙
【成分】
本品主要成分为Gefitinib
化学名:4-[(4-甲基-1-哌嗪)甲基]-N-[4-甲基-3-[[4-(3-吡啶)-2-嘧啶]氨基]苯基]-苯胺甲磺酸盐。
分子式:C32H33ClFN5O11
[适应症/功能主治】
适用于转移性非小细胞肺癌(NSCLC)的一线治疗,适用于具有表皮生长因子受体(EGFR)外显子19缺失或外显子21(L858R)替代突变的肿瘤。(FDA批准的检测方法)
使用限制:吉非替尼在肿瘤细胞有其他EGFR突变的患者身上的的安全性和有效性尚未确定。
【规格型号】250mg片剂*30片/盒
褐色,圆形,双面,薄膜衣片;一面印有"IRESSA250"。
【用法用量】
易瑞沙的成人推荐剂量为250mg,每日1次,口服,空腹或与食物同服。直至疾病进展或患者耐受。
若漏服,请勿在下次剂量的12小时内加服漏药。
如果有吞咽困难,可将片剂分散于半杯饮用水中(非碳酸饮料),不得使用其他液体。将片剂丢入水中, 无需压碎,搅拌至完全分散(约需10分钟),即刻饮下药液。以半杯水冲洗杯子,饮下。也可通过鼻-胃管给予该药液。
无需因下述情况不同调整给药剂量:年龄、体重、性别、种族,肾功能,因肝转移而引起的中至重度肝功能损害。
剂量调整:当患者出现不能耐受的腹泻或皮肤不良反应时,可通过短期暂停治疗(多14天)解决,随后恢复每天250mg的剂量。
【不良反应】
常见(发生率20%以上)的药物不良反应为:腹泻、皮疹、瘙痒、皮肤干燥和痤疮。
一般见于服药后的第1个月内,通常是可逆性的。
大约8%的患者出现严重的药物不良反应(CTC标准3或4级)。
因不良反应停止治疗的患者仅有1%。
各身体系统发生的不良反应按发生频率以降序排列:(多见:≥10%;常见:≥1%且<10%;少见:≥0.1%且<1%;罕见:≥0.01%且<0.1%;极罕见:<0.01%)。
可出现的不良事件总结如下:
消化系统:
多见腹泻,主要为轻度(CTC1级),少有中度(CTC2级),个别报道严重伴脱水的腹泻(CTC3级)。
常见恶心,主要为轻度(CTC1级);呕吐,主要为轻度或中度(CTC1或2级);厌食,轻度或中度(CTC1或2级);口腔粘膜炎,多为轻度(CTC1级);继发于腹泻,恶心,呕吐或厌食的脱水口腔溃疡。
少见胰腺炎。
皮肤及附件:
多见皮肤反应,主要为轻度或中度(CTC1或2级);脓疱性皮疹,在红斑的基础上有时伴皮肤干燥发痒。常见指甲异常。极罕见中毒性表皮坏死松懈症和多形红斑的报道,过敏反应,包括血管形水肿和荨麻疹。
代谢和营养:
常见肝功能异常,主要包括无症状性的轻度或中度转氨酶升高(CTC1或2级)。
全身:常见乏力,多为轻度(CTC1级);脱发;体重下降;外周性水肿。
眼科:
常见结膜炎和睑炎,主要为轻度(CTC1级);弱视。
少见可逆性角膜糜烂,有时伴睫毛生长异常。
极罕见角膜脱落;眼部缺血/出血。
血液和淋巴:
常见出血,如鼻衄和血尿。
少见在服用华法林的一些患者中出现INR(International Normalised Ratio)升高及/或出血事件;出血性膀胱炎。
呼吸:
常见呼吸困难。
少见间质性肺病,常较严重(CTC3-4级。在全球进行的临床研究,扩大用药/同情用药,上市后使用中,约有158348名患者接受了易瑞沙治疗,在日本以外的地区,包括约92821名患者,间质性肺病总的发生率约为0.28%,在日本其发生率约为1.70%,包括约65527名患者,数据截至2004年6月2日),已有致死性病例的报道。
【禁忌】无
【注意事项】
偶尔观察到发生间质性肺病,患者通常出现急性的呼吸困难,伴有咳嗽,低热,呼吸道不适和动脉血氧不饱和。短期内该症状可发展得很严重,并报告有死亡。放射学检查常显示肺浸润或间质有毛玻璃样阴影。已观察到在出现该状况的患者中,伴有原发性肺纤维化/间质性肺炎/尘肺/放射性肺炎/药物诱导性肺炎的患者死亡率较高。
处方医生应密切监测间质性肺病发生的迹象,如果患者呼吸道症状加重,应中断易瑞沙治疗,立即进行检查。当证实有间质性肺病时,应停止使用易瑞沙,并对患者进行相应的治疗。
已观察到无症状性肝转氨酶升高。因此,建议定期检查肝功能。肝转氨酶轻中度升高的患者应慎用易瑞沙。如果肝转氨酶升高加重,应考虑停药。
已报道在服用华法林的一些患者中出现INR(InternationalNormalisedRatio,国际标准化比率)升高及/或出血事件。服用华法林的患者应定期监测凝血酶原时间或INR的改变。应告诫患者当以下情况加重时即刻就医:
眼部症状;
严重或持续的腹泻,恶心,呕吐或厌食;这些症状应按临床需要进行处理。
随机对照试验证明,在晚期非小细胞肺癌患者中将易瑞沙和以铂类为基础的标准两药联合化疗方案合用,不会有额外的益处。因此,易瑞沙应单用于既往接受过细胞毒性化疗的非小细胞肺癌患者。
在一项对儿科患者进行易瑞沙和放疗治疗的I/II期临床研究中,33名入选患者(这些患者为新诊断出脑干神经胶质瘤或未完全切除的幕上恶性神经胶质瘤)中,发生4例(1例死亡)中枢神经系统出血。在一项单用易瑞沙治疗的临床研究中,一位患者有室管膜瘤的儿童也出现了中枢神经系统出血。接受易瑞沙治疗的成年非小细胞肺癌患者脑出血风险不太可能增高。
对驾驶及操纵机器能力的影响:在易瑞沙治疗期间,可出现乏力的症状,出现这些症状的患者在驾驶或操纵机器时应给予提醒。
【孕妇及哺乳期妇女用药】
妊娠期使用:目前尚无易瑞沙用于妊娠期女性的资料。在器官发生期给予可产生母体毒性剂量的吉非替尼,在大鼠中可观察到成骨不全的发生率升高,在家兔中可观察到胎儿体重下降。在大鼠中未观察到畸形,仅在产生严重母体毒性的剂量下可在家兔中观察到畸形。在接受易瑞沙治疗期间,要劝告育龄女性避免妊娠。
哺乳期使用:在接受易瑞沙治疗期间,应建议哺乳母亲停止母乳喂养。
目前尚无易瑞沙用于哺乳期女性的资料。尚不知吉非替尼或其代谢产物是否会分泌入人乳,但当给予哺乳大鼠口服5mg/kg吉非替尼(按体表面积计为临床用药剂量的0.2倍),吉非替尼及某些代谢产物广泛分泌入乳汁。
在大鼠妊娠及分娩期间给于吉非替尼20mg/kg/天(按体表面积计为临床用药剂量的0.7倍)的剂量,可减少幼鼠的存活率。
【儿童用药】
目前尚无易瑞沙用于儿童或青春期患者安全性与疗效的资料,故不推荐使用。
【老年用药】
老年人用药安全性方面与年轻患者无显著差异。有效性方面的数据尚不足。
【药理作用】
表皮生长因子受体(EGFR)在正常细胞和癌细胞的细胞表面均有表达,他们在细胞生长和增殖过程中起作用。一些NSCLC细胞的EGFR激活突变(外显子19缺失或外显子21的点突变L858R)已被鉴定为促进肿瘤细胞生长,阻断凋亡,增加血管生成因子的产生并促进肿瘤的转移过程。
吉非替尼可逆地抑制EGFR的野生型和某些EGFR激活突变的激酶活性,阻止受体相关的酪氨酸残基的自磷酸化,从而抑制进一步的下游信号传导并阻断EGFR依赖性增殖。
吉非替尼对EGFR外显子19缺失或外显子21点突变L858R突变的结合亲和力高于其
对野生型EGFR的亲和力。在临床上,吉非替尼还能抑制IGF和PDGF介导的信号的相关
浓度;对其他酪氨酸激酶受体的抑制作用尚未被充分定性。
【药代动力学】
吸收和分布
吉非替尼的平均口服生物利用度为60%,给药后3-7小时出现峰值血浆水平。 食物对吉非替尼的生物利用度改变无临床有意 义。 IRESSA可以与食物一起服用。
吉非替尼广泛分布在全身,静脉给药后平均稳态体积分布为1400升。 在体外,吉非替尼与人血浆蛋白(血清白蛋白α1-酸性 糖蛋白结合和. 1酸 糖蛋白)的体外结合率为90%,与药物浓度无关。 吉非替尼是膜转运糖蛋白的底物 (P-gp),但是当 P-gp在较高浓度下饱和时,不太可能影响吉非替尼吸收。
代谢与清除:
体外研究数据表明参与吉非替尼氧化代谢的P450同工酶主要是CYP3A4。
体外研究显示吉非替尼可有限地抑制CYP2D6。
吉非替尼的代谢中三个生物转化的位点已被确定:N-丙基吗啉基团的代谢,喹唑啉上甲氧取代基的脱甲基作用及卤化苯基基团类的氧化脱氟作用。
在人血浆中鉴别到的主要代谢物是O-去甲基吉非替尼。它对EGFR刺激细胞生长的抑制作用比吉非替尼弱14倍,因此对吉非替尼的临床活性不太可能有显著作用。
吉非替尼总的血浆清除率约为500mL/分。主要通过粪便排泄,少于4%通过肾脏以原型和代谢物的形式清除。
特殊人群人群动力学:在以人群为基础的数据分析中,未发现预期的稳态血药谷浓度与患者年龄、体重、性别、种族、或肌酐清除率之间有任何关系。
肝功能损害在一项有31名实体瘤患者(他们中肝功能为正常的有14名,中度肝功能损害的有13名,由于肝转移出现重度肝功能损害的有4名)参加的临床研究中对吉非替尼进行了药代动力学评价。研究表明,日服250mg易瑞沙28天后,达到稳态的时间,总血浆清除率及稳态值(Cmaxss,AUC24SS)在肝功能正常组和中度肝功能损害组之间是相似的。4名由于肝转移出现重度肝功能损害的患者其稳态值与肝功能正常组也相似。未在有肝硬化或肝炎引起肝功能损害的患者中进行易瑞沙的研究。
【药物相互作用】
对人肝微粒体进行的体外试验证实,吉非替尼主要通过肝细胞色素P-450系的CYP3A4代谢。所以吉非替尼可能会与诱导、抑制同一肝酶代谢的药物发生相互作用。动物研究表明吉非替尼很少有酶诱导作用,体外研究显示吉非替尼可有限地抑制CYP2D6。
以下列出了与吉非替尼产生或可能产生有临床意义地药物相互作用地药物或药物类别:
影响吉非替尼的药物:
已证明的相互作用-抑制CYP3A4的药物:在健康志愿者中将吉非替尼与伊曲康唑(一种CYP3A4抑制剂)合用,吉非替尼的平均AUC升高80%。由于药物不良反应与剂量及暴露量相关,该升高可能有临床意义。虽然未进行与其他CYP3A4抑制剂相互作用的研究,但这一类药物如酮康唑,克霉唑,利托那韦同样可能抑制吉非替尼的代谢。
升高胃pH值的药物:在健康志愿者中进行临床研究,表明与能明显持续升高胃pH至≥(greaterthanorequalto)5的药物合用,可使吉非替尼的平均AUC降低47%,这可能降低吉非替尼疗效。
利福平:在健康志愿者中将吉非替尼与利福平(已知的强CYP3A4诱导剂)同时给药吉非替尼的平均AUC比单服时降低83%。
理论上可能有相互作用的药物-其他CYP3A4诱导剂:诱导CYP3A4活性的物质可增加吉非替尼的代谢并降低其血浆浓度。因此,与CYP3A4诱导剂(如苯妥因、卡马西平、巴比妥类或圣约翰草)合用可降低疗效。
吉非替尼对其他药物的作用:已证明的相互作用-通过CYP2D6代谢的药物:在一项临床试验中,吉非替尼与美托洛尔(一种CYP2D6酶底物)合用,使美托洛尔的暴露量升高35%。吉非替尼与其他由CYP2D6代谢的药物同服,可能会升高后者的血药浓度。
理论上可能有相互作用的药物-华法林:虽然迄今尚未进行正规的药物相互作用研究,在一些服用华法林的患者中报告了INR增高和/或出血事件。服用华法林的患者应定期监测其凝血酶原时间或INR的改变。
【药物过量】
对于服用过量易瑞沙还没有专门的治疗方法,现在尚不知过量服用可能的症状。
在I期临床试验中,少量患者服用到每天1000mg的剂量,观察到一些不良反应的发生频率增加和严重程度升高,主要是腹泻和皮疹。对于药物过量引起的不良反应应给予对症处理,特别是严重腹泻应给予适当的治疗。
【药理毒理】
非临床(体外)研究资料表明,吉非替尼具有抑制心脏动作电位复极化过程(如QT间期)的可能性。但由临床研究和上市后监测获得的安全性资料未提示吉非替尼对心脏有任何不良作用。
致癌,致畸和生殖毒性未进行吉非替尼的致癌研究。在基因突变分析(细菌和体外哺乳动物细胞)和裂解试验(体外哺乳动物细胞和体内大鼠微核试验)中,吉非替尼未显示基因毒性作用。
在交配前4周至妊娠7天期间给予吉非替尼20mg/kg/天(按体表面积计为临床用药剂量的0.7倍),可对雌鼠排卵产生影响,导致黄体量下降。
在器官发生期给予可产生母体毒性剂量的吉非替尼,在大鼠中可观察到成骨不全的发生率升高,在家兔中可观察到胎儿体重下降。在大鼠中未观察到畸形,仅在产生严重母体毒性的剂量下可在家兔中观察到畸形。
当给予哺乳大鼠口服5mg/kg吉非替尼(按体表面积计为临床用药剂量的0.2倍),吉非替尼及某些代谢产物广泛分泌入乳汁。
【临床资料】
两项大型的II期临床研究评估了易瑞沙单药治疗局部晚期或转移性非小细胞肺癌(NSCLC)的有效性和安全性。患者的WHO体力状况评分为0-2,并且必须为既往化疗失败者:
IDEAL1(研究0016),既往接受了1或2个化疗方案,并且至少有一个包括铂类治疗(中位年龄为59.6岁[28-85岁];n=209)。
IDEAL2(研究0039),既往接受了2个或以上化疗方案,该化疗方案包括同时或先后接受了铂类和多西紫杉醇的治疗(中位年龄为61岁[30-84岁];n=216)。
两个研究设计相似,均为双盲、平行组、多中心,评估了两个吉非替尼口服剂量:250mg/天和500mg/天。患者被随机分配在这两个剂量组。在IDEAL1中主要研究终点为肿瘤客观缓解率,次要研究终点为疾病相关症状改善;在IDEAL2中主要研究终点为肿瘤客观缓解率以及疾病相关症状改善率(每周以LCS进行测定)。
疗效结果对于IDEAL1和IDEAL2疗效结果的总结见下表。不考虑WHO体力状况评分(0,1或2)和既往接受的化疗次数,两个研究中得到的肿瘤客观缓解率以及疾病相关症状改善率结果相似。大多数患者肿瘤客观缓解发生于治疗的第1个月,少部分患者的客观缓解可迟至治疗的第4个月发生。
a在IDEAL1试验中,无论是250mg还是500mg,日本患者的客观缓解率要比非日本患者的高(250mg为27.5%:9.6%,500mg为27.5%:11.1%),未调整的比值比(两组合并)为3.27,p=0.002。在多变量分析时,调整了性别,组织学和身体状况后,这一差异不再有统计学意义(调整后的比值比为2.13,p=0.068)。
b基于症状改善可评估人群(250mg,n=67;500mg,n=73)。
+数据截止时仍在继续。
FACT-L肺癌患者生活质量测定量表。
NC未计算。
PFS无进展生存。
安全性易瑞沙的安全性情况在两项研究中是相似的,不良事件的发生率和严重程度呈剂量相关性。
结论临床研究资料证明局部晚期或转移性非小细胞肺癌患者以易瑞沙进行治疗可达到持续的客观缓解。
在中国进行的临床研究在中国的5个临床研究基地中进行了临床研究,以评估吉非替尼片250mg/日在既往接受过化学治疗的非小细胞肺癌患者中的客观缓解率。
共有159名受试者至少服用了一次吉非替尼片250mg,受试者的人口学和疾病特征情况如下:
男性91人(57.2),女性68人(42.8);
年龄均数(标准差)为56.5岁(11.3),中位数为57岁,范围(小值,值)在31.0-84.0岁。
年龄组情况:18-60岁组有91人(57.2%),60-70岁组有46人(28.9%),70岁以上组有22人(13.8%)。
吸烟状况:不吸烟者有90人(56.6%),曾吸烟者有37人(23.3%),偶尔吸烟者有3人(1.9%),经常吸烟者有29人(18.2%)。
组织学分型:鳞癌有29人(18.2%),腺癌有105人(66%),未分化癌有5人(3.1%),大细胞癌有1人(0.6%),腺鳞癌有7人(4.4%),细支气管肺泡癌(BAC)有12人(7.5%)。
入选时非小细胞肺癌状态:局部晚期MO有26人(16.4%),转移性M1有133人(83.6%)。
WHO体力状况:0分有23人(14.5%),1分有101人(63.5%),2分有34人(21.4%),3分有1人(0.6%)。
其中在入选前曾接受过1个化疗方案治疗的受试者有75名(47.2%),2个及3个以上(含3个)化疗方案治疗的受试者分别为50名(31.4%)和34名(21.4%)。对于159名受试者(意向性治疗人群集)进行了有效性分析。
以下为疗效总结:
客观缓解率为27.0%,
95%可信区间为20.3-34.7%,
中位PFS为97天,
95%可信区间为67-120天,
中位生存期为11.1月(生存期数据截止至2004年11月22日)。
在不同治疗亚组中客观缓解率显示有一定的差异性(根据入组时基线特征进行分组,受试者的客观缓解率情况如下表,类似的差异性同样见于其他国际临床研究。尽管在某些亚组的受试者数不够多,但吉非替尼对这些受试者的效果和预期的相一致。
【安全性】
吉非替尼的总体耐受性良好。大部分不良事件为轻度,无需处理。超过10%的受试者报告的不良事件为皮疹(44.0%)、皮肤瘙痒(15.7%)和腹泻(11.3%)。所出现的不良事件严重程度及发生频率与在其他临床研究中观察到的相一致。
【药理毒理】
非临床(体外)研究资料表明,吉非替尼具有抑制心脏动作电位复极化过程(如QT间期)的可能性。但由临床研究和上市后监测获得的安全性资料未提示吉非替尼对心脏有任何不良作用。
致癌,致畸和生殖毒性未进行吉非替尼的致癌研究。在基因突变分析(细菌和体外哺乳动物细胞)和裂解试验(体外哺乳动物细胞和体内大鼠微核试验)中,吉非替尼未显示基因毒性作用。
在交配前4周至妊娠7天期间给予吉非替尼20mg/kg/天(按体表面积计为临床用药剂量的0.7倍),可对雌鼠排卵产生影响,导致黄体量下降。
在器官发生期给予可产生母体毒性剂量的吉非替尼,在大鼠中可观察到成骨不全的发生率升高,在家兔中可观察到胎儿体重下降。在大鼠中未观察到畸形,仅在产生严重母体毒性的剂量下可在家兔中观察到畸形。
当给予哺乳大鼠口服5mg/kg吉非替尼(按体表面积计为临床用药剂量的0.2倍),吉非替尼及某些代谢产物广泛分泌入乳汁。
在大鼠妊娠及分娩期间给于吉非替尼20mg/kg/天(按体表面积计为临床用药剂量的0.7倍)的剂量,可减少幼鼠的存活率。
【贮藏】
20--25°C保存。
文案整理: Dr. Jasmine Ding
HIGHLIGHTS OF PRESCRIBING INFORMATION
These highlights do not include all the information needed to use IRESSA® safely and effectively.
See full prescribing information for IRESSA (gefitinib) tablets for oral use
Initial U.S. Approval: 2015
INDICATIONS AND USAGE :
IRESSA is a tyrosine kinase inhibitor indicated for the first-line treatment of patients with metastatic non-small cell lung cancer (NSCLC) whose tumors have epidermal growth factor receptor (EGFR) exon 19 deletions or exon 21 (L858R) substitution mutations as detected by an FDA-approved test. (1) Limitation of Use: Safety and efficacy of IRESSA have not been established in patients whose tumors have EGFR mutations other than exon 19 deletions or exon 21 (L858R) substitution mutations. (1)
DOSAGE AND ADMINISTRATION
Recommended dose is 250 mg orally, once daily with or without food. (2.2)
DOSAGE FORMS AND STRENGTHS
Tablets: 250 mg. (3)
CONTRAINDICATIONS ----------------------------- None.
WARNINGS AND PRECAUTIONS
Interstitial lung disease (ILD):
ILD occurred in patients taking IRESSA. Withhold IRESSA for worsening of respiratory symptoms. Discontinue IRESSA if ILD is confirmed. (2.4, 5.1)
Hepatotoxicity: Obtain periodic liver function testing. Withhold IRESSA for Grade 2 or higher for ALT and/or AST elevations. Discontinue for severe hepatic impairment. (2.4, 5.2)
Gastrointestinal perforation: Discontinue IRESSA for gastrointestinal perforation. (2.4, 5.3)
Diarrhea: Withhold IRESSA for Grade 3 or higher diarrhea. (2.4, 5.4)
Ocular Disorders including Keratitis:
Withhold IRESSA for signs and symptoms of severe or worsening ocular disorders including keratitis. Discontinue for persistent ulcerative keratitis. (2.4, 5.5)
Bullous and Exfoliative Skin Disorders
Withhold IRESSA for Grade 3 or higher skin reactions or exfoliative conditions. (2.4, 5.6)
Embryo-fetal Toxicity:
Can cause fetal harm. Advise of potential risk to a fetus and use of effective contraception. (5.7, 8.1, 8.3)
ADVERSE REACTIONS
The most commonly reported adverse drug reactions (ADRs), reported in more than 20% of the patients and greater than placebo were skin reactions and diarrhea. (6.1)
To report SUSPECTED ADVERSE REACTIONS, contact AstraZeneca at 1-800-236-9933 or FDA at 1-800-FDA-1088 or www.fda.gov/me
DRUG INTERACTIONS
CYP3A4 Inducer:
Increase IRESSA to 500 mg daily in patients receiving a strong CYP3A4 inducer. (2.4, 7.1)
CYP3A4 Inhibitor:
Monitor adverse reactions if concomitant use with IRESSA. (7.1)
Drugs Ating Gastric pH: Avoid concomitant use of IRESSA with proton pump inhibitors, if possible. (7.1)
Hemorrhage in patients taking warfarin: Monitor changes in prothrombin time or INR. (7.2)
USE IN SPECIFIC POPULATIONS
Lactation: Discontinue breast-feeding. (8.2) See 17 for PATIENT COUNSELING INFORMATION and FDA approved patient labeling Revised: 07/2015
FULL PRESCRIBING INFORMATION:
CONTENTS* 1 INDICATIONS AND USAGE 2 DOSAGE AND ADMINISTRATION
2.1 Patient Selection
2.2 Recommended Dose
2.3 Administration to Patients Who Have Difficulty Swallowing Solids
2.4 Dose Modification
3 DOSAGE FORMS AND STRENGTHS
4 CONTRAINDICATIONS 5 WARNINGS AND PRECAUTIONS
5.1 Interstitial Lung Disease (ILD)
5.2 Hepatotoxicity
5.3 Gastrointestinal Perforation
5.4 Severe or Persistent Diarrhea
5.5 Ocular Disorders including Keratitis
5.6 Bullous and Exfoliative Skin Disorders
5.7 Embryo-fetal Toxicity
6 ADVERSE REACTIONS
6.1 Clinical Trials Experience
6.3 Postmarketing Experience
7 DRUG INTERACTIONS
7.1 Drugs Affecting Gefitinib Exposure
7.2 Hemorrhage in Patients taking Warfarin
8 USE IN SPECIFIC POPULATIONS
8.1 Pregnancy
8.2 Lactation
8.3 Females and Males of Reproductive Potential
8.4 Pediatric Use
8.5 Geriatric Use
8.6 Renal Impairment
8.7 Hepatic Impairment
10 OVERDOSAGE
11 DESCRIPTION
12 CLINICAL PHARMACOLOGY
12.1 Mechanism of Action
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.
Reference ID: 3791123
FULL PRESCRIBING INFORMATION
1 INDICATIONS AND USAGE
IRESSA is indicated for the first-line treatment of patients with metastatic non-small cell lung cancer (NSCLC) whose tumors have epidermal growth factor receptor (EGFR) exon 19 deletions or exon 21 (L858R) substitution mutations as detected by an FDA-approved test [see Clinical Studies (14)].
Limitation of Use: Safety and efficacy of IRESSA have not been established in patients with metastatic NSCLC whose tumors have EGFR mutations other than exon 19 deletions or exon 21 (L858R) substitution mutations [see Clinical Studies (14)].
2 DOSAGE AND ADMINISTRATION
2.1 Patient Selection
Select patients for the first-line treatment of metastatic NSCLC with IRESSA based on the presence of EGFR exon 19 deletion or exon 21 (L858R) substitution mutations in their tumor [see Indications and Usage (1), Clinical Studies (14)]. Information on FDA-approved tests for the detection of EGFR mutations in NSCLC is available at: http://www.fda.gov/CompanionDiagnostics.
2.2 Recommended Dose
The recommended dose of IRESSA is 250 mg orally once daily with or without food until disease progression or unacceptable toxicity. Do not take a missed dose within 12 hours of the next dose.
2.3 Administration to Patients
Who Have Difficulty Swallowing Solids Immerse IRESSA tablets in 4 to 8 ounces of water by dropping the tablet in water, and stir for approximately 15 minutes. Immediately drink the liquid or administer through a naso-gastric tube. Rinse the container with 4 to 8 ounces of water and immediately drink or administer through the naso-gastric tube.
2.4 Dose Modification
Dose Modifications for Adverse Drug Reactions Withhold IRESSA (for up to 14 days) for any of the following:
Acute onset or worsening of pulmonary symptoms (dyspnea, cough, fever) [see Warnings and Precautions (5.1)]
NCI CTCAE Grade 2 or higher in ALT and/or AST elevations [see Warnings and Precautions (5.2)]
NCI CTCAE Grade 3 or higher diarrhea [see Warnings and Precautions (5.4)]
Signs and symptoms of severe or worsening ocular disorders including keratitis [see Warnings and Precautions (5.5)]
NCI CTCAE Grade 3 or higher skin reactions [see Warnings and Precautions (5.6)]
Resume treatment with IRESSA when the adverse reaction fully resolves or improves to NCI CTCAE Grade 1.
Permanently discontinue IRESSA for:
Confirmed interstitial lung disease (ILD) [see Warnings and Precautions (5.1)]
Severe hepatic impairment [see Warnings and Precautions (5.2)]
Gastrointestinal perforation [see Warnings and Precautions (5.3)]
Persistent ulcerative keratitis [see Warnings and Precautions (5.5)] Reference ID: 3791123
Dose Modifications for Drug Interactions Strong CYP3A4 Inducers Increase IRESSA to 500 mg daily in the absence of severe adverse drug reaction, and resume IRESSA at 250 mg seven days after discontinuation of the strong CYP3A4 inducer [see Drug Interactions (7), Clinical Pharmacology (12.3)].
3 DOSAGE FORMS AND STRENGTHS
250 mg tablets: round, biconvex, brown film-coated, debossed with "IRESSA 250" on one side and plain on the other side.
4 CONTRAINDICATIONS
None.
5 WARNINGS AND PRECAUTIONS
5.1 Interstitial Lung Disease (ILD)
ILD or ILD-like adverse drug reactions (e.g., lung infiltration, pneumonitis, acute respiratory distress syndrome, or pulmonary fibrosis) occurred in 1.3% of the 2462 patients who received IRESSA across clinical trials; of these, 0.7% were Grade 3 or higher and 3 cases were fatal. Withhold IRESSA and promptly investigate for ILD in any patient who presents with worsening of respiratory symptoms such as dyspnea, cough and fever. Permanently discontinue IRESSA if ILD is confirmed [see Dosage and Administration (2.4), Adverse Reactions (6.1)].
5.2 Hepatotoxicity
In patients who received IRESSA across clinical trials, 11.4% of patients had increased alanine aminotransferase (ALT), 7.9% of patients had increased aspartate aminotransferase (AST), and 2.7% of patients had increased bilirubin. Grade 3 or higher liver test abnormalities occurred in 5.1% (ALT), 3.0% (AST), and 0.7% (bilirubin) of patients. The incidence of fatal hepatotoxicity was 0.04%. Obtain periodic liver function testing. Withhold IRESSA in patients with worsening liver function and discontinue in patients with severe hepatic impairment [see Dosage and Administration (2.4), Adverse Reactions (6.1), Use in Specific Populations (8.7)]. 5.3 Gastrointestinal Perforation Gastrointestinal perforation occurred in three (0.1%) of the 2462 IRESSA-treated patients across clinical trials [see Adverse Reactions (6.1)]. Permanently discontinue IRESSA in patients who develop gastrointestinal perforation [see Dosage and Administration (2.4)]. 5.4 Severe or Persistent Diarrhea Grade 3 or 4 diarrhea occurred in 3% of 2462 IRESSA-treated patients across clinical trials. Withhold IRESSA for severe or persistent (up to 14 days) diarrhea [see Dosage and Administration (2.4), Adverse Reactions (6.1)]. 5.5 Ocular Disorders including Keratitis Ocular disorders [keratitis (0.1%), corneal erosion and aberrant eyelash growth (0.2%), conjunctivitis, blephritis and dry eye (6.7%)] occurred in the 2462 IRESSA-treated patients across clinical trials. The incidence of Grade 3 ocular Reference ID: 3791123 disorders was 0.1% [see Adverse Reactions (6.1)]. Interrupt or discontinue IRESSA for severe, or worsening ocular disorders [see Dosage and Administration (2.4)]. 5.6 Bullous and Exfoliative Skin Disorders Bullous conditions including toxic epidermal necrolysis, Stevens Johnson syndrome and erythema multiforme have been reported from treatment with IRESSA. Erythema multiforme and dermatitis bullous have been reported in two patients (0.08%) across NSCLC trials (Study 2, Study 3 and Study 4). IRESSA treatment should be interrupted or discontinued if the patient develops severe bullous, blistering or exfoliating conditions. 5.7 Embryo-fetal Toxicity Based on its mechanism of action and data from animal reproduction studies IRESSA can cause fetal harm when administered to a pregnant woman. In animal reproductive studies, oral administration of gefitinib from organogenesis through weaning resulted in fetotoxicity and neonatal death at doses below the recommended human dose. Advise pregnant women of the potential risk to a fetus. Advise females of reproductive potential to use effective contraception during treatment with IRESSA and for at least two weeks following completion of therapy [see Use in Specific Populations (8.1, 8.3)].
6 ADVERSE REACTIONS
The following adverse drug reactions are discussed in more detail in other sections of the labeling: Interstitial Lung Disease [see Warnings and Precautions (5.1)]
Hepatotoxicity [see Warnings and Precautions (5.2)]
Gastrointestinal Perforation [see Warnings and Precautions (5.3)]
Severe or Persistent Diarrhea [see Warnings and Precautions (5.4)]
Ocular Disorders including Keratitis [see Warnings and Precautions (5.5)]
Bullous and Exfoliative Skin Disorders [see Warning and Precautions (5.6)]
6.1 Clinical Trials 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 IRESSA is based on the data from 2462 patients with NSCLC who received IRESSA 250 mg daily monotherapy in three randomized clinical studies (Study 2, Study 3 and Study 4). Patients with a history of interstitial lung disease, drug-induced interstitial disease, radiation pneumonitis that required steroid treatment or any evidence of clinically active interstitial lung disease were excluded from these studies. Controlled Studies: Study 2 was a randomized, multicenter, open-label trial in which 1217 patients were randomized to receive first-line treatment for metastatic NSCLC; 607 patients received IRESSA 250 mg daily and 589 patients received carboplatin/paclitaxel. The median duration of treatment with IRESSA was 5.9 months. The study population characteristics were: median age 57 years, age less than 65 years (73%), female (79%), Asian (100%), NSCLC adenocarcinoma histology (100%), never smoker (94%), light ex-smoker (6%), ECOG PS 0 or 1 (90%). Study 3 was a randomized, multicenter, double-blind, placebo-controlled trial in which 1692 patients were randomized to receive second- or third-line treatment for metastatic NSCLC; of which 1126 patients received IRESSA 250 mg daily and 562 patients received placebo. The median duration of treatment with IRESSA was 2.9 months. The study population characteristics were: median age 62 years, age less than 65 years (60%), female (33%), Caucasian (75%), Asian (21%), Reference ID: 3791123 NSCLC adenocarcinoma histology (48%), never smoker (22%), ECOG PS 0 or 1 (65%), PS 2 (29%), PS 3 (5%) and two or more prior therapies (51%). Study 4 was a randomized, multicenter, open-label trial in which 1466 patients were randomized to receive second-line treatment for metastatic NSCLC; 729 patients received IRESSA 250 mg daily and 715 patients received docetaxel. The median duration of treatment with IRESSA was 2.4 months. The study population characteristics were: median age 61 years, age less than 65 years (61%), female (36%), Caucasian (79%), Asian (21%), NSCLC adenocarcinoma histology (54%), never smoker (20%), ECOG PS 0 or 1 (88%) and two or more prior therapies (16%). The pooled safety database from the three randomized trials was used to evaluate for serious and uncommon adverse drug reactions. Common adverse reactions were evaluated in Study 3. The most frequent adverse reactions in Study 3 (incidence of >20% and greater than placebo) reported in IRESSA-treated patients were skin reactions (47%) and diarrhea (29%). The most frequent fatal adverse reactions in IRESSA-treated patients were respiratory failure (0.9%), pneumonia (0.8%), and pulmonary embolism (0.5%). Approximately 5% of IRESSA-treated patients and 2.3% of placebo-treated patients discontinued treatment due to an adverse event. The most frequent adverse reactions that led to discontinuation in patients treated with IRESSA were nausea (0.5%), vomiting (0.5%) and diarrhea (0.4%). Table 1- Selected Adverse Drug Reactions Occurring with an Incidence Rate ≥5% and an Increase of >2% of IRESSA-treated Patients in Study 3 Adverse Reaction Percentage (%) of patients IRESSA (N=1126) Placebo (N=562) All Grades Grade 3 and 4 All Grades Grade 3 and 4 Skin and subcutaneous tissue disorders Skin reactions1 47% 2% 17% 0.4% Nail disorders2 5% 0.1% 0.7% 0% Gastrointestinal disorders Diarrhea3 29% 3% 10% 1% Vomiting 14% 1.2% 10% 0.4% Stomatitis4 7% 0.3% 4% 0.2% Metabolism and nutrition disorders Decreased appetite 17% 2.3% 14% 2.0% Eye disorders Conjunctivitis/blepharitis/dry eye5 6% 0% 3.2% 0% 1 Includes Acne, Acne pustular, Dermatitis, Dermatitis acneiform, Dermatitis exfoliative, Drug eruption, Dry skin, Erythema, Exfoliative rash, Folliculitis, Pruritus, Pruritus generalized, Rash, Rash erythematous, Rash generalized, Rash macular, Rash maculo-papular, Rash papular, Rash pruritic, Rash pustular, Rash vesicular, Skin exfoliation, Skin toxicity, Xeroderma 2 Includes Ingrowing nail, Nail bed infection, Nail disorder, Nail infection, Onychoclasis, Onycholysis, Paronychia 3 Includes Diarrhea, Feces soft, Frequent bowel movements 4 Includes Aphthous stomatitis, Cheilitis, Glossodynia, Mouth ulceration, Mucosal inflammation, Oral mucosal blistering, Stomatitis, Tongue disorder, Tongue ulceration 5 Includes Blepharitis, Conjunctival hyperemia, Conjunctivitis, Dry eye, Eye irritation, Eye pruritus, Eye swelling, Eyelid irritation, Eyelid edema, Eyelids pruritus Reference ID: 3791123 Table 2 – Treatment Emergent Laboratory Abnormalities Occurring More Frequently in IRESSATreated Patients in Study 3 Adverse Reaction IRESSA Placebo All Grades % Grade 3 and 4 % All Grades % Grade 3 and 4 % Alanine aminotransferase increased1 38%2 2.4% 23%2 1.4%4 Aspartate aminotransferase increased1 40%3 2.0% 25%3 1.3%5 Proteinuria 35% 4.7% 31% 3.3% 1 Patients were allowed to enter the clinical study with lab values of ALT or AST CTCAE grade 1 or 2 2 14% gefitinib patients and 10% placebo patients were CTC grade 1 or 2 ALT at baseline 3 15% gefitinib patients and 12% placebo patients were CTC grade 1 or 2 AST at baseline 4 0.2% of placebo patients were CTC grade 3 at baseline 5 0.4% of placebo patients were CTC grade 3 at baseline The following adverse reactions have been reported with IRESSA across NSCLC trials (Study 2, Study 3 and Study 4) and are not listed elsewhere in Section 6: nausea (18%), asthenia (17%), pyrexia (9%), alopecia (4.7%), hemorrhage (including epistaxis and hematuria) (4.3%), dry mouth (2%), dehydration (1.8%), allergic reactions including angioedema and urticaria (1.1%), elevations in blood creatinine (1.5%), and pancreatitis (0.1%). 6.3 Postmarketing Experience The following adverse reactions have been identified during post-approval use of IRESSA. Because these reactions are reported voluntarily from a population of uncertain size, it is not always possible to reliably estimate their frequency or establish a causal relationship to drug exposure. Renal and urinary disorders: cystitis, hemorrhagic cystitis Skin and subcutaneous tissue disorders: cutaneous vasculitis
7 DRUG INTERACTIONS
7.1 Drugs Affecting Gefitinib Exposure CYP3A4 Inducer Drugs that are strong inducers of CYP3A4 increase the metabolism of gefitinib and decrease gefitinib plasma concentrations. Increase IRESSA to 500 mg daily in patients receiving a strong CYP3A4 inducer (e.g., rifampicin, phenytoin, or tricyclic antidepressant) and resume IRESSA at 250 mg 7 days after discontinuation of the strong inducer [see Dosage and Administration (2.4), Clinical Pharmacology (12.3)]. CYP3A4 Inhibitor Drugs that are strong inhibitors of CYP3A4 (e.g., ketoconazole and itraconazole) decrease gefitinib metabolism and increase gefitinib plasma concentrations. Monitor adverse reactions when administering strong CYP3A4 inhibitors with IRESSA. Drugs Affecting Gastric pH Drugs that elevate gastric pH (e.g., proton pump inhibitors, histamine H2-receptor antagonists, and antacids) may reduce plasma concentrations of gefitinib. Avoid concomitant use of IRESSA with proton pump inhibitors, if possible. If Reference ID: 3791123 treatment with a proton-pump inhibitor is required, take IRESSA 12 hours after the last dose or 12 hours before the next dose of the proton-pump inhibitor. Take IRESSA 6 hours after or 6 hours before an H2-receptor antagonist or an antacid [see Clinical Pharmacology (12.3)].
7.2 Hemorrhage in Patients taking Warfarin International Normalized Ratio (INR) elevations and/or hemorrhage have been reported in some patients taking warfarin while on IRESSA therapy. Patients taking warfarin should be monitored regularly for changes in prothrombin time or INR. 8 USE IN SPECIFIC POPULATIONS 8.1 Pregnancy Risk Summary Based on its mechanism of action and animal data, IRESSA can cause fetal harm when administered to a pregnant woman. In animal reproductive studies, oral administration of gefitinib from organogenesis through weaning resulted in fetotoxicity and neonatal death at doses below the recommended human dose (see Animal Data). Advise pregnant women of the potential hazard to a fetus or potential risk for loss of the pregnancy. The background risk of major birth defects and miscarriage for the indicated population is unknown; however, the background risk in the U.S. general population of major birth defects is 2-4% and miscarriage is 15-20% of clinically recognized pregnancies. Data Animal Data A single dose study in rats showed that gefitinib crosses the placenta after an oral dose of 5 mg/kg (30 mg/m2 , about 0.2 times the recommended human dose on a mg/m2 basis). When pregnant rats were treated with 5 mg/kg from the beginning of organogenesis to the end of weaning there was a reduction in the number of offspring born alive. This effect was more severe at 20 mg/kg (approximate the human clinical dose on a mg/m2 basis) and was accompanied by high neonatal mortality soon after parturition. In rabbits, a dose of 20 mg/kg/day (240 mg/m2 , about twice the recommended dose in humans on a mg/m2 basis) caused reduced fetal weight. 8.2 Lactation Risk Summary It is not known whether IRESSA is excreted in human milk. Animal studies indicate the gefitinib and its metabolites are present in rat milk at a concentration higher than those in maternal plasma. Because of the potential for serious adverse reactions in nursing infants from IRESSA, advise women to discontinue breast-feeding during treatment with IRESSA. Data Animal Data Levels of gefitinib and its metabolites were 11-to-19-fold higher in milk than in blood, after oral exposure of lactating rats to a dose of 5 mg/kg. Reference ID: 3791123 8.3 Females and Males of Reproductive Potential Contraception Based on its mechanism of action and animal data, IRESSA 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 IRESSA and for at least two weeks following completion of therapy. Infertility IRESSA may result in reduced fertility in females of reproductive potential [see Nonclinical Toxicology (13.1)].
8.4 Pediatric Use
The safety and effectiveness of IRESSA in pediatric patients have not been established.
8.5 Geriatric Use
Of the 823 patients enrolled in two randomized, active-controlled clinical trials 374 patients (45%) were 65 years and older, and 93 patients (11%) were 75 years and older. No overall differences in safety were observed between patients 65 years and older and those younger than 65 years. There is insufficient information to assess for differences in efficacy between older and younger patients.
8.6 Renal Impairment
Less than four percent (<4%) of gefitinib and its metabolites are excreted via the kidney. No clinical studies were conducted with IRESSA in patients with severe renal impairment.
8.7 Hepatic Impairment
The systemic exposure of gefitinib was compared in patients with mild, moderate, or severe hepatic impairment due to cirrhosis (according to Child-Pugh classification) and healthy subjects with normal hepatic function (N=10/group). The mean systemic exposure (AUC0-∞) was increased by 40% in patients with mild impairment, 263% in patients with moderate impairment, and 166% in patients with severe hepatic impairment. Monitor adverse reactions when IRESSA is administered to patients with moderate and severe hepatic impairment. In a study comparing 13 patients with liver metastases and moderate hepatic impairment (addition of CTC grade of baseline AST/SGOT, ALP, and bilirubin equals 3 to 5) to 14 patients with liver metastases and normal hepatic function, the systemic exposure of gefitinib was similar [see Warnings and Precautions (5.2)].
10 OVERDOSAGE
Twenty three patients were treated weekly with doses from 1500 mg to 3500 mg, and IRESSA exposure did not increase with increasing dose. Adverse events were mostly mild to moderate in severity, and were consistent with the known safety profile of IRESSA. In the event of suspected overdose, interrupt IRESSA, institute supportive care, and observe until clinical stabilization. There are no specific measures/treatments that should be taken following IRESSA overdosing.
11 DESCRIPTION
Gefitinib is a kinase inhibitor. The chemical name of gefitinib is 4-Quinazolinamine N-(3-chloro-4-fluorophenyl)-7-methoxy-6-[3-(4-morpholinyl) propoxy] and the following structural formula: Reference ID: 3791123 Gefitinib has the molecular formula C22H24ClFN4O3, a relative molecular mass of 446.9 daltons and is a white-colored powder. Gefitinib is a free base. The molecule has pKas of 5.4 and 7.2. Gefitinib can be defined as sparingly soluble at pH 1, but is practically insoluble above pH 7, with the solubility decreasing sharply between pH 4 and pH 6. In nonaqueous solvents, gefitinib is freely soluble in glacial acetic acid and dimethyl sulfoxide, soluble in pyridine, sparingly soluble in tetrahydrofuran, and slightly soluble in methanol, ethanol (99.5%), ethyl acetate, propan-2-ol and acetonitrile. IRESSA® (gefitinib) tablets are available as brown film-coated tablets, containing 250 mg of gefitinib, for oral administration. The inactive ingredients of the tablet core of IRESSA tablets are lactose monohydrate, microcrystalline cellulose, croscarmellose sodium, povidone, sodium lauryl sulfate and magnesium stearate. The tablet coating is composed of hypromellose, polyethylene glycol 300, titanium dioxide, red ferric oxide and yellow ferric oxide.
12 CLINICAL PHARMACOLOGY
12.1 Mechanism of Action
The epidermal growth factor receptor (EGFR) is expressed on the cell surface of both normal and cancer cells and plays a role in the processes of cell growth and proliferation. Some EGFR activating mutations (exon 19 deletion or exon 21 point mutation L858R) within NSCLC cells have been identified as contributing to the promotion of tumor cell growth, blocking of apoptosis, increasing the production of angiogenic factors and facilitating the processes of metastasis. Gefitinib reversibly inhibits the kinase activity of wild-type and certain activating mutations of EGFR, preventing autophosphorylation of tyrosine residues associated with the receptor, thereby inhibiting further downstream signalling and blocking EGFR-dependent proliferation. Gefitinib binding affinity for EGFR exon 19 deletion or exon 21 point mutation L858R mutations is higher than its affinity for the wild-type EGFR. Gefitinib also inhibits IGF and PDGF-mediated signalling at clinically relevant concentrations; inhibition of other tyrosine kinase receptors has not been fully characterized. 12.3 Pharmacokinetics Absorption and Distribution The mean oral bioavailability of gefitinib is 60%, with peak plasma levels occurring 3-7 hours after dosing. Food does not alter gefitinib bioavailability to a clinically meaningful extent. IRESSA can be administered with or without food. Gefitinib is extensively distributed throughout the body with a mean steady state volume of distribution of 1400 L following intravenous administration. In vitro binding of gefitinib to human plasma proteins (serum albumin and 1-acid glycoprotein) is 90%, independent of drug concentrations. Gefitinib is a substrate for the membrane transport Pglycoprotein (P-gp), but it is unlikely to influence gefitinib absorption as P-gp is saturated at higher concentrations. Reference ID: 3791123 Metabolism and Elimination Gefitinib undergoes extensive hepatic metabolism in humans, predominantly by CYP3A4. Three sites of biotransformation have been identified: metabolism of the N-propoxymorpholino-group, demethylation of the methoxysubstituent on the quinazoline, and oxidative defluorination of the halogenated phenyl group. Five metabolites have been fully identified in fecal extracts and the major active component was O-desmethyl gefitinib produced by CYP2D6 metabolism and accounted for 14% of the dose. Eight metabolites were identified in human plasma. Only O-desmethyl gefitinib has exposure comparable to gefitinib. Although this metabolite has similar EGFR-TK activity to gefitinib in the isolated enzyme assay, it had only 1/14 of the potency of gefitinib in one of the cell-based assays. Gefitinib is cleared primarily by the liver, with total plasma clearance and elimination half-life of 48 hours after intravenous administration. The inter-subject variability (coefficient of variation) for AUC in healthy subjects was 67%. Daily oral administration of gefitinib to cancer patients resulted in a two-fold accumulation compared to single dose administration. Steady state plasma concentrations are achieved within 10 days after daily dosing. Excretion of gefitinib and its metabolites is predominantly via the feces (86%), with renal elimination accounting for less than 4% of the administered dose. Specific Populations Age, gender, body weight, ethnicity or renal function: Population pharmacokinetic analyses suggest that patient age, body weight, ethnicity (populations included) or creatinine clearance (above 20 mL/min) has no clinically meaningful effect on predicted steady state trough concentration of gefitinib. Population pharmacokinetic analyses of Study 1 showed that women had 27% higher exposure than men; however, this difference was not identified in the analyses of other gefitinib clinical studies. No dose adjustment based on patient gender is recommended. Hepatic Impairment: The systemic exposure of gefitinib was compared between patients with mild, moderate, or severe hepatic impairment due to cirrhosis (according to Child-Pugh classification) and healthy subjects with normal hepatic function (N=10/group). The mean systemic exposure (AUC0-∞) was increased by 40% in patients with mild impairment, 263% in patients with moderate impairment, and 166% in patients with severe hepatic impairment. In a study comparing 13 patients with liver metastases and moderate hepatic impairment to 14 patients with liver metastases and normal hepatic function, the systemic exposure of gefitinib was similar [see Warnings and Precautions (5.2), Use in Specific Populations (8.7)]. CYP2D6 Poor metabolizer: CYP2D6 metabolizes gefitinib to O-desmethyl gefitinib in vitro. In healthy CYP2D6 poor metabolizers, O-desmethyl gefitinib concentration was not measurable and the mean exposure to gefitinib was 2-fold higher as compared to the extensive metabolizers. This increase in exposure in CYP2D6 poor metabolizers may be clinically important because some adverse drug reactions are related to higher exposure of gefitinib. No dose adjustment is recommended in patients with a known CYP2D6 poor metabolizer genotype, but these patients should be closely monitored for adverse reactions. The impact of CYP2D6 inhibiting drugs on gefitinib pharmacokinetics has not been evaluated. However, similar precautions should be used when administering CYP2D6 inhibitors with IRESSA because of the possibility of increased exposure in these patients. An exploratory exposure response analysis showed an increase in the incidence of interstitial lung disease (ILD) with a greater than 2 fold increase in the gefitinib exposure [see Warnings and Precautions (5.1)]. Reference ID: 3791123 Drug-Drug Interactions Strong CYP3A4 Inducer: Concomitant administration of rifampicin (600 mg QD for 16 days), a strong inducer of CYP3A4, with gefitinib (500 mg single dose on Day 10 of gefitinib administration) reduced mean AUC of gefitinib by 83% [see Dosage and Administration (2.4), Drug Interactions (7)].
CYP3A4 Inhibitor: Concomitant administration of itraconazole (200 mg QD for 12 days), an inhibitor of CYP3A4, with gefitinib (250 mg single dose on Day 4 of itraconazole administration) to healthy male subjects, increased mean gefitinib AUC by 80% [see Drug Interactions (7)]. Drugs Affecting Gastric pH: Co-administration of high doses of ranitidine with sodium bicarbonate (to maintain the gastric pH above pH 5.0) to healthy subjects decreased mean gefitinib AUC by 47% [see Drug Interactions (7)]. In human liver microsome studies, gefitinib had no inhibitory effect on CYP1A2, CYP2C9, and CYP3A4 activities at concentrations ranging from 2-5000 ng/mL. At the highest concentration studied (5000 ng/mL), gefitinib inhibited CYP2C19 by 24% and CYP2D6 by 43%. Exposure to metoprolol, a substrate of CYP2D6, was increased by 30% when it was given on Day 15 of gefitinib dosing (500 mg daily for 28 days) in patients with solid tumors. 13 NONCLINICAL TOXICOLOGY 13.1 Carcinogenesis, Mutagenesis, Impairment of Fertility Gefitinib has been tested for genotoxicity in a series of in vitro (bacterial mutation, mouse lymphoma, and human lymphocyte) assays and an in vivo rat micronucleus test. Under the conditions of these assays, gefitinib did not cause genetic damage. In a two-year carcinogenicity study in mice, administration of gefitinib at a dose of 270 mg/m2 /day (approximately twice the recommended daily dose of 250 mg on a mg/m2 basis; dose reduced from 375 mg/m2 /day from week 22) caused hepatocellular adenomas in females. In a two-year carcinogenicity study in rats, administration of gefitinib at 60 mg/m2 /day (approximately 0.4 times the recommended daily clinical dose on a mg/m2 basis) caused hepatocellular adenomas and hemangiomas/hemagiosarcomas of the mesenteric lymph nodes in female rats. The clinical relevance of these findings is unknown. In a dedicated fertility study in rats at doses ≥120 mg/m2 (approximately equal to the recommended human dose of gefitinib on a mg/m2 basis), animals presented with an increased incidence of irregular estrous, decreased corpora lutea, and decreases in uterine implants and live embryos per litter.
14 CLINICAL STUDIES
Non-Small Cell Lung Cancer (NSCLC) Study 1
The efficacy and safety of IRESSA for the first-line treatment of patients with metastatic NSCLC containing EGFR exon 19 deletions or L858R substitution mutations was demonstrated in a multicenter, single-arm, open-label clinical study (Study 1). A total of 106 treatment-naive patients with metastatic EGFR mutation positive NSCLC received IRESSA at a Reference ID: 3791123 dose of 250 mg once daily until disease progression or intolerable toxicity. The major efficacy outcome measure was objective response rate (ORR) according to RECIST v1.1 as evaluated by both a Blinded Independent Central Review (BICR) and investigators. Duration of response (DOR) was an additional outcome measure. Eligible patients were required to have a deletion in EGFR exon 19 or L858R, L861Q, or G719X substitution mutation and no T790M or S768I mutation or exon 20 insertion in tumor specimens as prospectively determined by a clinical trial assay. Tumor samples from 87 patients were tested retrospectively using the therascreen® EGFR RGQ PCR Kit. The study population characteristics were: median age 65 years, age 75 years or older (25%), age less than 65 years (49%), white (100%), female (71%), never smokers (64%), WHO PS 0 (45%), WHO PS 1 (48%), WHO PS 2 (7%), and adenocarcinoma histology (97%). Sixty patients had exon 19 deletions (65%), 29 patients had L858R substitution (31%), while two patients each had tumors harboring L861Q or G719X substitution mutation. The median duration of treatment was 8.0 months. Efficacy results from Study 1 are summarized below. Table 3 – Efficacy Results in Study 1 Efficacy Parameter BICR1 Assessment (n=106)2 Investigator Assessment (n=106) Objective Response Rate3 (95% CI) 50% (41, 59) 70% (61, 78) Complete Response Rate 0.9% 1.9% Partial Response Rate 49% 68% Median Duration of Response (months) (95% CI) 6.0 (5.6, 11.1) 8.3 (7.6, 11.3) 1 BICR, Blinded Independent Central Review 2 17 patients without target lesion at baseline detected by BICR were deemed non responders 3 Determined by RECIST v 1.1 The response rates were similar in patients whose tumors had EGFR exon 19 deletions and exon 21 L858R substitution mutations. Two partial responses were observed in both patients whose tumors had G719X substitution mutation with duration of response of at least 2.8 months and 5.6 months, respectively. One of two patients whose tumors had L861Q substitution mutation also achieved a partial response with duration of response of at least 2.8 months. Study 2 The results of Study 1 were supported by an exploratory analysis of a subset of a randomized, multicenter, open-label trial (Study 2) conducted in patients with metastatic adenocarcinoma histology NSCLC receiving first-line treatment. Patients were randomized (1:1) to receive IRESSA 250 mg orally once daily or up to 6 cycles of carboplatin/paclitaxel. The efficacy outcomes included progression-free survival (PFS) and objective response rate (ORR) as assessed by BICR. The subset population consisted of 186 of 1217 patients (15%) determined to be EGFR positive by the same clinical trial assay as used in Study 1 and had radiographic scans available for a retrospective assessment by BICR. In this subset, there were 88 IRESSA-treated patients and 98 carboplatin/paclitaxel-treated patients. Demographic and baseline characteristics of this subset were a median age of 59 years, age 75 years or older (7%), age less than 65 (70%), Asian (100%), female (83%), never smokers (96%), adenocarcinoma histology (100%), and PS 0-1 (94%). Reference ID: 3791123 The median duration of treatment for IRESSA-treated patients was 9.8 months. The hazard ratio for PFS favored the IRESSA-treated patients [HR of 0.54 (95% CI: 0.38, 0.79)] with a median PFS of 10.9 months for the IRESSA-treated patients and 7.4 months for the carboplatin/paclitaxel-treated patients as assessed by BICR. In addition, the objective response rate was 67% (95% CI: 56, 77) for IRESSA-treated patients and 41% (95% CI: 31, 51) for carboplatin/paclitaxel-treated patients based on BICR assessment. The median duration of response was 9.6 months for IRESSA-treated patients and 5.5 months for carboplatin/paclitaxel-treated patients. 16 HOW SUPPLIED/STORAGE AND HANDLING IRESSA® (gefitinib) is available as 250 mg tablets. IRESSA 250 mg tablets are round, biconvex, brown film-coated, debossed with "IRESSA 250" on one side and plain on the other side. IRESSA® (gefitinib) tablets are supplied as: Bottles of 30 Tablets (NDC 0310-0482-30) Store at controlled room temperature 20C-25C (68F-77F) [see USP Controlled Room Temperature]. 17 PATIENT COUNSELING INFORMATION Advise the patient to read the FDA-approved patient labelling (Patient Information). Interstitial Lung Disease: Advise patients to immediately contact their healthcare provider for new onset or worsening of pulmonary symptoms such as dyspnea, cough and fever [see Warnings and Precautions (5.1)]. Hepatotoxicity: Inform patients that they will need to undergo lab tests to monitor for liver function. Advise patients to contact their healthcare provider to report any new symptoms indicating hepatic toxicity [see Warnings and Precautions (5.2)]. Gastrointestinal Perforation: Advise patients that IRESSA can increase the risk of gastrointestinal perforation and to seek immediate medical attention for severe abdominal pain [see Warnings and Precautions (5.3)]. Severe or Persistent Diarrhea: Advise patients to contact their healthcare provider for severe or persistent diarrhea [see Warnings and Precautions (5.4)]. Ocular Disorders including Keratitis: Advise patients promptly to contact their healthcare provider if they develop eye symptoms, lacrimation, light sensitivity, blurred vision, eye pain, red eye or changes in vision [see Warnings and Precautions (5.5)] Bullous and Exfoliative Skin Disorders: Advise patients that IRESSA can increase the risk of bullous and exfoliative skin disorders and to seek immediately medical attention for severe skin reactions [see Warnings and Precautions (5.6)]. Embryo-fetal Toxicity: Advise pregnant women of the potential risk to a fetus or potential risk for loss of the pregnancy [see Warnings and Precautions (5.7), Use in Specific Populations (8.1)]. Advise females of reproductive potential to use effective contraception during treatment with IRESSA and for at least two weeks following completion of therapy [see Use in Specific Populations (8.3)]. Lactation: Advise women to discontinue breast-feeding during treatment with IRESSA [see Use in Specific Populations (8.2)]. IRESSA is a trademark of the AstraZeneca group of companies. Reference ID: 3791123 ©AstraZeneca 2015 Manufactured for: AstraZeneca Pharmaceuticals LP Wilmington, DE 19850 By: AstraZeneca UK Limited Macclesfield, Cheshire, England Product of Belgium Reference ID: 3791123 Patient Information IRESSA (eye-RES-sah) (gefitinib) tablets What is IRESSA? IRESSA is a prescription medicine used to treat people with non-small cell lung cancer (NSCLC) that has spread to other parts of the body and: that have certain types of abnormal epidermal growth factor receptor (EGFR) genes, and who have not had previous treatment for cancer Your healthcare provider will perform a test to make sure that IRESSA is right for you. It is not known if IRESSA is safe and effective in people with NSCLC that have other types of EGFR genes. It is not known if IRESSA is safe and effective in children. Before taking IRESSA, tell your healthcare provider about all of your medical conditions, including if you: have lung or breathing problems ever had liver problems have vision or eye problems are pregnant or plan to become pregnant. IRESSA can harm your unborn baby. o Females who are able to become pregnant should use an effective method of birth control during treatment with IRESSA and for at least 2 weeks after the last dose of IRESSA. You should avoid becoming pregnant during treatment with IRESSA. o Tell your healthcare provider right away if you become pregnant during treatment with IRESSA. are breastfeeding or plan to breastfeed. It is not known if IRESSA passes into your breast milk. Do not breastfeed during treatment with IRESSA. Talk to your healthcare provider about the best way to feed your baby during this time. Tell your healthcare provider about all the medicines you take, including prescription and over-the-counter medicines, vitamins, or herbal supplements. If you take a proton pump inhibitor (PPI), H2 blocker, or an antacid medicine, talk to your healthcare provider about the best time to take it during treatment with IRESSA. If you take a blood thinner called warfarin, your healthcare provider should do blood tests regularly to check how fast your blood clots, during treatment with IRESSA. How should I take IRESSA? Take IRESSA exactly as your healthcare provider tells you to take it. Your healthcare provider may change your dose, temporarily stop, or permanently stop treatment with IRESSA if you have side effects. Take IRESSA 1 time each day. You can take IRESSA with or without food. If you miss a dose of IRESSA, take it as soon as you remember. If it is less than 12 hours until your next dose, skip the missed dose. Take your next dose at your regular time. If you take too much IRESSA, call your healthcare provider or go to the nearest emergency room right away. If you cannot swallow IRESSA tablets whole: o place your dose of IRESSA in a container with 4 to 8 ounces of water and stir for about 15 minutes o drink the mixture right away Reference ID: 3791123 o place another 4 to 8 ounces of water in the same container, and drink it right away What are the possible side effects of IRESSA? IRESSA may cause serious side effects, including: lung or breathing problems. IRESSA may cause inflammation of the lung that may lead to death. Symptoms may be similar to those symptoms from lung cancer. Tell your healthcare provider right away if you have any new or worsening lung problems, or any combination of the following symptoms: trouble breathing or shortness of breath, cough, or fever. Iiver problems. IRESSA may cause inflammation of the liver that may lead to death. Tell your healthcare provider right away if you have any symptoms of a liver problem which may include: o yellowing of your skin or the white part of your eyes (jaundice) o dark or brown (tea colored) urine o light-colored bowel movements (stools) o decreased appetite o pain on the right side of your stomach (abdomen) Your healthcare provider will do blood tests to check your liver function during your treatment with IRESSA. a tear in the wall of your stomach or intestines (perforation). Get emergency medical help right away if you have severe stomach (abdomen) pain. diarrhea. Diarrhea is common with IRESSA and can sometimes be severe. Tell your healthcare provider right away if you have severe diarrhea or diarrhea that will not go away. eye problems. Tell your healthcare provider if you get watery eyes, sensitivity to light, blurred vision, eye pain, eye redness, or vision changes. skin reactions. Skin redness, rash, itching, and acne are common with IRESSA. This may occur on any part of your body. Get medical help right away if you develop severe skin reactions such as peeling or blistering of your skin. IRESSA may cause fertility problems in females. Talk to your healthcare provider if you plan to become pregnant. Tell your healthcare provider if you have any side effect that bothers you or that does not go away. These are not all the possible side effects of IRESSA. For more information, ask your healthcare provider or pharmacist. 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 IRESSA? Store IRESSA at room temperature between 68˚F to 77˚F (20˚C to 25˚C) Keep IRESSA and all medicines out of the reach of children. General information about the safe and effective use IRESSA. Medicines are sometimes prescribed for purposes other than those listed in Patient Information leaflet. Do not use IRESSA for a condition for which it was not prescribed. Do not give IRESSA 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 information about IRESSA that is written for health professionals. What are the ingredients in IRESSA? Active ingredient: gefitinib Inactive ingredients: lactose monohydrate, microcrystalline cellulose, croscarmellose sodium, povidone, sodium lauryl sulfate, magnesium stearate Reference ID: 3791123 Tablet coating contains: hypromellose, polyethylene glycol 300, titanium dioxide, yellow iron oxide and red iron oxide.
IRESSA is a trademark of the AstraZeneca group of companies.
©AstraZeneca 2015 Manufactured for: AstraZeneca Pharmaceuticals LP Wilmington, DE 19850
Manufacture by: AstraZeneca UK Limited Macclesfield, Cheshire, England Product of Belgium
For more information, go to www.iressa.com or call 1-800-236-9933
This Patient Information has been approved by the U.S. Food and Drug Administration. Issued: July 2015
Reference ID: 3791123