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当前位置:药品说明书与价格首页 >> 心血管系统 >> 高血脂症 >> 药品推荐 >> 波生坦片|Tracleer(Bosentan Tablets)

波生坦片|Tracleer(Bosentan Tablets)

2011-11-20 13:45:24  作者:新特药房  来源:中国新特药网天津分站  浏览次数:884  文字大小:【】【】【
简介: 英文药名: Tracleer(Bosentan Tablets) 中文药名: 全可利(波生坦片 药品名称 【通用名】 波生坦片   【商品名】 全可利   【英文名】 Bosentan Tablets   【性状】 本品为橙白色薄膜衣片。 规 ...

英文药名: Tracleer(Bosentan Tablets)

中文药名: 全可利(波生坦片

药品名称

【通用名】 波生坦片   
【商品名】 全可利   
【英文名】 Bosentan Tablets   
【性状】 本品为橙白色薄膜衣片。
规格

62.5mg; 125mg/片
药理毒理

本品是一种双重内皮素受体拮抗剂,具有对ETA 和ETB 受体的亲和作用。波生坦可降低肺和全身血管阻力,从而在不增加心率的情况下增加心脏输出量。 神经激素内皮素是一种有力的血管收缩素,能够促进纤维化、细胞增生和组织重构。在许多心血管失调疾病,包括肺动脉高压,血浆和组织的内皮素浓度增加,表明内皮素在这些疾病中起病理作用。在肺动脉高压,血浆内皮素浓度与预后不良紧密相关。 波生坦是特异性内皮素受体。波生坦与ETA 和ETB 受体竞争结合,与ETA 受体的亲和力比与ETB 受体的亲和力稍高。在动物肺动脉高压模型中,长期口服波生坦能减少肺血管阻力、逆转肺血管和右心室肥大。在动物肺纤维化模型中,波生坦能减少胶原沉积。
药代动力学

波生坦的绝对生物利用度大约为50%,而且不受食物影响。最大血浆浓度在口服给药后3-5 小时后达到。分布体积大约为18L,清除率大约为8L/h。表面消除半衰期(t1/2)为5.4 小时。波生坦与血浆蛋白高度结合(>98%),主要是白蛋白。波生坦不会渗透到红细胞。 波生坦在肝脏中被细胞色素P450 同工酶CYP3A4 和CYP2C9 代谢。在人血浆中有三种波生坦代谢物。只有一种代谢物Ro 48-5033 具有药学活性,占化合物活性的10-20%。波生坦代谢通过胆汁清除。 在严重肾功能受损的病人(肌酐清除率为15-30mL/min),波生坦血浆浓度减少大约10%,与肾功能正常的志愿者相比,三种代谢物的血浆浓度增加约2 倍。因为低于3%的剂量通过尿排出,对于肾功能受损的病人不需调整剂量。 未在肝脏损伤的病人中进行波生坦药代动力学影响的评估。由于波生坦被肝脏广泛代谢并通过胆汁排出,肝脏受损预计影响其药代动力学和代谢。因此,有轻度肝脏损伤病人应慎用波生坦。仅仅当潜在益处高于风险时才在这些病人中使用波生坦。严重肝损伤的病人禁忌用波生坦(见禁忌和警告)。
适应症

本品用于治疗WHO III 期和IV 期原发性肺高压病人的肺动脉高压,或者硬皮病引起的肺高压。
用法用量

本品初始剂量为一天2 次、每次62.5mg,持续4 周,随后增加至维持剂量 125mg,一天2 次。高于一天2 次、一次125mg 的剂量不会带来足以抵消肝脏损伤风险的益处。可在进食前或后,早、晚服用本品。
肾功能受损病人: 肾功能受损对本品药代动力学的影响很小。不需作剂量调整。
老年人: 本品的临床研究没有包括足够的年龄在65 岁及大于65 岁的病人并测定他们的反应是否与年轻病人相同。通常来说,因为肾和/或心脏功能下降、有伴随疾病、其它药物治疗,尤其有肝功能降低,所以老年病人的剂量应该慎重选择。
肝脏损害病人: 肝脏轻度损害病人应慎用本品。中度和重度肝脏损害病人严禁使用。 治疗中止: 没有在推荐剂量下肺动脉高压病人突然中止使用本品的经验。为了避免临床突然恶化,应紧密监视病人,在停药前的3-7 天应将剂量减至一半。
任何疑问,请遵医嘱!
不良反应

在安慰剂对照研究中,165 名肺动脉高压病人每日接受本品250mg(n=95)以及500mg(n=70)。对667名肺动脉高压或者其它症状病人进行安慰剂对照和开放研究中,获得本品的安全性数据。剂量高达给予肺动脉高压推荐剂量的8倍。治疗期为1天到4.1年。
在推荐的维持剂量125mg、b.i.d.,本品治疗的肺动脉高压病人中发生率超过1%的不良事件见下表:
肺动脉高压安慰剂对照研究中,本品(125mg b.i.d.)治疗病人中发生率超过1%的不良事件,不考虑药物因果 在肺动脉高压和其它疾病的本品安慰剂对照研究中,共677名病人接受本品治疗,288名病人接受安慰剂治疗,剂量范围为每天100~2000mg。治疗期为4周至6个月。
本品治疗病人中发生率高于1%的不良事件见下表:
安慰剂对照研究中,本品治疗病人中发生率超过1%的不良事件,不考虑药物因果 注意:病人数量包括肺动脉高压病人和其它症状病人。在某些安慰剂对照研究中,使用高于推荐治疗肺动脉高压的剂量。本品治疗的病人比安慰剂组病人发生率高的不良事件为头疼、潮红、肝功能异常、贫血和腿水肿。
本品治疗病人中发生率低于1%的不良事件为:
碱性磷酸酶增加、过敏性休克、厌食、腹水、吸引、哮喘、房室完全阻滞、血尿素增加、支气管痉挛、心跳停止、中枢神经系统阻抑、脑血管病、胸痛(非心脏)、凝血时间延长、凝血时间缩短、结膜炎、膀胱炎、脱水、皮炎、注意力失调、皮肤干燥、十二指肠溃疡、排尿困难、淤斑、湿疹、嗜酸性细胞计数增加、鼻出血、红斑、眼炎、情绪激动、气胀、胃肠炎、糖耐量受损、痛风、血尿、咯血、轻偏瘫、脑积水、高血糖、感染、失眠、肠梗阻、过敏、乳酸脱氢酶增加、疲劳、性欲增加、易排便、情绪不宁、嘴溃疡、肌肉痉挛、颤搐、肌肉骨骼疼痛、心肌梗塞、鼻充血、梦魇、疼痛、恐慌、感觉异常、外周局部出血、畏光、肺炎、肾衰、肾功能不全、呼吸抑制、呼吸衰竭、不宁腿综合征、负重感、颤抖、皮肤变色、瞌睡、痰液增加、Stevens-Johnson 综合症、蛛网膜下腔出血、出汗增加、心动过速、口渴、血小板减少、耳鸣、震颤、尿频、尿深、荨麻疹、迷走发射、心室心率失常、心动过速、眩晕、虚弱、体重降低以及眼球干燥。
实验室异常:
安慰剂对照研究中,丙氨酸转氨酶(ALT)和天冬氨酸转氨酶(AST)高于正常上限值3 倍的发生率,在本品治疗病人中为11%(n=658),在安慰剂治疗组中为2%(n=280)。95 名肺动脉高压病人接受本品125mg、b.i.d.治疗,12%病人ALT 和AST 增加3 倍;70 名肺动脉高压病人接受本品 250mg、b.i.d.治疗,14%病人ALT 和AST 增加3 倍。在接受125mg、b.i.d 治疗的病人中,2%病人ALT 和AST 增加8 倍;接受250mg、b.i.d.治疗的病人中,7%病人ALT 和AST 增加8 倍。胆红素升高至超过正常值上限的3 倍,与本品治疗的658 名病人中的2名(0.3%)转氨酶升高有关。 本品引起的ALT 和AST 升高是剂量相关的,发生于治疗的早期,偶尔晚期发生。通常进展缓慢,无典型症状,当治疗中断或者停止后是可逆的。
持续用本品治疗,转氨酶升高也可能自然逆转。在所有使用本品的安慰剂对照试验中,治疗组6.2%的病人和安慰剂组2.9%病人出现显著血红蛋白降低(比基线值降低超过15%,且 <11 g/dL)。在125 和250 mg b.i.d.剂量治疗的肺动脉高压病人中,3%的病人血红蛋白显著减少,安慰剂对照组为1%。 观察到治疗组57%的病人和安慰剂组29%病人血红蛋白浓度至少下降1g/dL。血红蛋白降低至少1g/dL 的病人中,80%的病人血红蛋白减少出现在本品治疗的前6周。 治疗组68%病人和安慰剂组76%病人的血红蛋白浓度在治疗期间保持在正常范围。还不清楚血红蛋白变化的原因,但并没有出血、溶血或者骨髓毒性。 建议在治疗后的第一和第三个月以及随后每隔3 个月检查血红蛋白浓度。
体液潴留:
在安慰剂对照研究中,1611名严重慢性心衰病人接受本品治疗,治疗期平均1.5年。在研究中,发现以前肺动脉高压研究中没有观察到的新的安全性结果。由于慢性心衰恶化而导致早期入院率增加,本品和安慰剂组间的死亡率没有差异。在研究末期,本品和安慰剂组病人间的总体入院人数或者死亡率均没有差异。本品治疗的前4-8 周中观察到的入院率增加可能是由于体液潴留的结果。
在试验中,下面这些症状表明体液潴留:早期体重增加、血红蛋白浓度降低和腿水肿发生率增加。 在肺动脉高压病人的安慰剂对照试验中,外周水肿和血红蛋白浓度降低,没有因临床恶化而很早入院的证据。 建议监测病人的体液潴留症状(例如体重增加)。建议在出现体液潴留时采用利尿剂治疗,或者增加正在使用的利尿剂剂量。建议在本品治疗前,对有体液潴留症状的病人用利尿剂治疗。
禁忌症

以下病人禁用本品:
*对于本品任何组分过敏者;
*怀孕或者可能怀孕者,除非采取了充分的避孕措施。在动物中报道有胎儿畸形;
*中度或严重肝功能损害和/或肝脏转氨酶即天冬氨酸转氨酶(AST)和/或丙氨酸转氨酶的基线值高于正常值上限的3倍(ULN),尤其是总胆红素增加超过正常值上限的2倍;
*伴随使用环孢素A 者;
*伴随使用格列本脲者。
注意事项

如果病人系统收缩压低于85mm Hg,须慎用本品。
血液学变化: 用本品治疗伴随剂量相关的血红蛋白浓度降低(平均0.9 g/dL),可能是由于血液的稀释。多数在本品治疗开始的数周内观察到,治疗4-12 周后稳定,一般不需要输血。建议在开始治疗前、治疗后第1 个月和第3 个月检测血红蛋白浓度,随后每3 个月检查一次。如果出现血红蛋白显著降低,须进一步评估来决定原因以及是否需要特殊治疗。
体液潴留: 严重慢性心脏衰竭的病人用本品治疗伴随住院率升高,因为在本品治疗的前4-8 周慢性心脏衰竭恶化,可能是体液潴留的结果。建议监测病人体液潴留的症状(例如体重增加)。出现症状后,建议开始用利尿剂或者增加正在使用利尿剂的剂量。建议在开始本品治疗前,对体液潴留症状的病人用利尿剂治疗。
警告
肝功能: 波生坦伴随可逆性、剂量相关的天冬氨酸转氨酶(AST)和丙氨酸转氨酶(ALT)增加,在某些病例中还伴随有胆红素升高。肝酶升高通常在开始治疗前16周内出现,然后在数天至9周内恢复到治疗前水平,或者减少剂量或者停药后自动恢复。 在治疗前需检测肝脏转氨酶水平,随后最初12 个月内每个月检测一次,以后4个月一次。
先前存在肝脏损伤: 在以下病人中,中度或严重肝损伤和/或肝脏转氨酶即天冬氨酸转氨酶(AST)和/或丙氨酸转氨酶的基线值高于正常值上限的3倍(ULN),尤其当总胆红素增加超过正常值上限2倍,禁用本品。(见警告)
肝脏转氨酶升高病人的处理: ALT/AST 水平> 3 及≤5 ULN,治疗和监测的建议如下: 再做一次肝功能检验证实,如果证实,减少每日剂量或者停止治疗,至少每2周监测一次转氨酶水平。如果转氨酶恢复到治疗前水平,考虑继续或者再次使用波生坦(见再次治疗)。
ALT/AST 水平> 5 及≤8 ULN,治疗和监测的建议如下: 再做一次肝功能检验证实;如果证实,减少每日剂量或者停止治疗,至少每2周监测一次转氨酶水平。一旦转氨酶恢复到治疗前水平,考虑继续或者再次使用波生坦(见再次治疗)。
ALT/AST 水平> 8 × ULN,治疗和监测的建议如下: 必需停止治疗,不考虑再使用波生坦。 在转氨酶升高,伴随有肝脏损伤的临床症状(例如恶心、呕吐、发热、腹痛、黄疸或者罕见嗜睡或疲劳)或者胆红素升高超过正常值上限水平2倍时,治疗必需停止,不考虑使用波生坦。
再次治疗
仅当本品治疗的潜在益处高于风险,而且转氨酶位于正常值内,才考虑再次使用波生坦。本品以开始的剂量再次使用,转氨酶必须在再次使用后3 天内进行检测,过2 周后再检测,随后根据以上建议进行。
孕妇及哺乳期妇女用药

波生坦被认为对人具有潜在致畸性。当给予大鼠≥60 mg/kg/day(人口服治疗剂量的2 倍,每次125mg,每日2次,基于mg/m2)时, 波生坦显示有致畸性。在大鼠的胚胎毒性研究中,波生坦表现出剂量相关的致畸性作用,包括头部、脸部和主要血管畸形。剂量高达1500 mg/kg/day 时,在家兔中没有观察到出生缺陷;但其血浆浓度低于大鼠的血浆浓度。波生坦诱导的畸形和内皮素-1 基因剔除小鼠和以其它内皮素受体拮抗剂治疗的动物中所观察到的畸形相似,表明这些药物有类致畸性效应。没有对孕妇进行研究。在本品治疗前必须排除妊娠,之后必须采用充分的避孕措施防止妊娠。(见药物相互作用:激素避孕药)。 尚不清楚本品是否分泌进入人乳汁。因为大多数药物都分泌到乳汁中,应建议服用波生坦的哺乳妇女停止哺乳。
儿童用药

还没有建立波生坦在儿童中的安全性和有效性,不建议用于儿童。
老年患者用药

年龄65岁或以上病人有限的临床经验表明,老年人和年轻人对药物的反应没有差异,但应考虑老年人肝功能低下的可能性(见用法用量)。
药物相互作用

细胞色素P450 系统: 波生坦对细胞色素P450 同工酶CYP1A2、CYP3A4、 CYP2C9、CYP2C19 和CYP2D6 没有相关的抑制作用。本品不会增加这些酶所代谢药物的血浆浓度。 波生坦是CYP3A4 和CYP2C9 的轻微至中度的诱导剂。伴随使用本品时,被这2种酶代谢的药物血浆浓度可能降低。
华法令: 伴随使用本品,500mg 每日2次,可使S-华法令和R-华法令的血浆浓度降低大约30%。长期接受华法令治疗的肺动脉高压病人服用本品 125mg, b.i.d.,对凝血时间/INR 没有临床显著的影响。对华法令无须另外调整剂量,但建议进行常规INR 监测。
辛伐他汀和其它他汀:伴随使用本品时会降低辛伐他汀和它的主要活性β- 氢氧基酸代谢物的血浆浓度,大约50%。本品的血浆浓度不受影响。本品也降低其它主要受CYP3A4 代谢的他汀类的血浆浓度。对于这些他汀类,须考虑他汀功效下降。
格列本脲:在接受格列本脲伴随治疗的病人中观察到转氨酶升高的风险。因此,禁止本品和格列本脲联合使用,应考虑用其它替代的降血糖药物(见禁忌)。联用本品可使格列本脲的血浆浓度降低约40%。本品的血浆浓度也降低30%。本品也可能降低其它主要由CYP2C9 和CYP3A4 代谢的降血糖药物的血浆浓度。使用这些药物病人,须考虑血糖失控的可能性。
酮康唑:本品和酮康唑伴随使用可使本品的血浆浓度增加大约2倍。无需剂量调整,但应考虑本品作用增加。
尼莫地平、地高辛、洛沙坦:本品与地高辛和尼莫地平之间没有药代动力学的相互作用。洛沙坦对本品血浆水平没有影响。
环孢素A:伴随使用本品可使血液中环孢素A的浓度降低大约50%。联用本品的初始谷浓度比单独使用时高大约30倍。但在稳态时,本品的血浆浓度仅仅高出3-4倍。禁止本品和环孢素A联用。
没有进行他克莫司的药物相互作用的研究,但可预计有相似的相互作用。建议避免将本品和他克莫司伴随使用。
激素避孕药: 没有进行与口服、注射或者植入避孕药的特殊相互作用研究。许多这类药物被CYP3A4代谢,当与本品联用时有避孕失败的可能性。因此应采用另外或者替代的避孕方法。
药物过量

本品在健康志愿者中单次给药2400mg,病人持续2 个月给予剂量2000mg/天,没有任何主要临床症状。最主要的副作用是轻度到中度的头疼。在环孢素A 药物相互作用研究中,剂量500 和1000mg 的本品与环孢素A 共同使用时,初始血浆谷浓度增加30 倍,结果导致严重头疼、恶心和呕吐,但没有出现严重不良事件。观察到轻微的血压降低和心率增加。没有超过上述剂量的药物过量研究。严重过量可能导致低血压,需要给予积极的心血管支持治疗。
贮藏

室温保存,15-30℃。

 

注:以下产品不同规格和不同价格,购买时请以电话咨询为准!
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原产地英文商品名:
TRACLEER 125mg/tablet 60tablets/bottle
原产地英文药品名:
BOSENTAN
中文参考商品译名:
TRACLEER 125毫克/片 60片/瓶
中文参考药品译名:
波生坦
生产厂家中文参考译名:
ACTELION
生产厂家英文名:
ACTELION
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原产地英文商品名:
TRACLEER 62.5mg/tablet 60tablets/bottle
原产地英文药品名:
BOSENTAN
中文参考商品译名:
TRACLEER 62.5毫克/片 60片/瓶
中文参考药品译名:
波生坦
生产厂家中文参考译名:
ACTELION
生产厂家英文名:
ACTELION

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TRACLEER (bosentan) tablet, film coated
[Actelion Pharmaceuticals US, Inc.]

HIGHLIGHTS OF PRESCRIBING INFORMATION
These highlights do not include all the information needed to use TRACLEER safely and effectively. See full prescribing information for TRACLEER.
TRACLEER (bosentan) tablets
Initial U.S. Approval: 2001
WARNING: RISKS OF LIVER INJURY and TERATOGENICITY
See full prescribing information for complete boxed warning.
Tracleer can be prescribed and dispensed only through a restricted distribution program (Tracleer Access Program) because of these risks:
Elevations of liver aminotransferases (ALT, AST) and liver failure have been reported with Tracleer (5.1).
Measure liver aminotransferases prior to initiation of treatment and then monthly (5.1).
Discontinue Tracleer if aminotransferase elevations are accompanied by signs or symptoms of liver dysfunction or injury or increases in bilirubin ≥2 × ULN (2.2, 5.1).
Based on animal data, Tracleer is likely to cause major birth defects if used during pregnancy (4.1, 8.1).
Must exclude pregnancy before and during treatment (4.1, 8.1) .
To prevent pregnancy, females of childbearing potential must use two reliable forms of contraception during treatment and for one month after stopping Tracleer (2.4, 8.

INDICATIONS AND USAGE
Tracleer is an endothelin receptor antagonist indicated for the treatment of pulmonary arterial hypertension (PAH) (WHO Group 1) to improve exercise ability and to decrease clinical worsening. Studies establishing effectiveness included predominately patients with NYHA Functional Class II-IV symptoms and etiologies of idiopathic or heritable PAH (60%), PAH associated with connective tissue diseases (21%), and PAH associated with congenital systemic-to-pulmonary shunts (18%) (1.1).
Considerations for use:

Consider whether benefits offset the risk of liver injury in WHO Class II patients. Early liver injury may preclude future use as disease progresses (1.1).
 
DOSAGE AND ADMINISTRATION
Initiate at 62.5 mg twice daily with or without food for 4 weeks, and then increase to 125 mg twice daily (2.1).
Patients with low body weight (<40 kg) and >12 years old: Initial and maintenance dose is 62.5 mg twice daily (2.6).
Reduce the dose and closely monitor patients developing aminotransferase elevations >3 × ULN (2.2).
Discontinue Tracleer 36 hours prior to initiation of ritonavir. Patients on ritonavir: Initiate Tracleer at 62.5 mg once daily or every other day (2.7).
 
DOSAGE FORMS AND STRENGTHS
62.5 mg and 125 mg unscored tablets (3)
 
CONTRAINDICATIONS
Pregnancy (4.1)
Use with Cyclosporine A (4.2)
Use with Glyburide (4.3)
Hypersensitivity (4.4)
 
WARNINGS AND PRECAUTIONS
Pre-existing hepatic impairment: Avoid use in moderate and severe impairment. Use with caution in mild impairment (5.2).
Fluid retention: May require intervention (5.3).
Decreased sperm counts: it cannot be excluded that endothelin receptor antagonists such as Tracleer have an adverse effect on spermatogenesis. (5.4)
Decreases in hemoglobin and hematocrit: Monitor hemoglobin levels after 1 and 3 months of treatment, then every 3 months thereafter (5.5).
Pulmonary veno-occlusive disease: If signs of pulmonary edema occur, consider the possibility of underlying pulmonary veno-occlusive disease and discontinue treatment if necessary (5.6).
 
ADVERSE REACTIONS
Most common (≥3%) placebo-adjusted adverse reactions are respiratory tract infection and anemia (6.1).

To report SUSPECTED ADVERSE REACTIONS, contact Actelion at 1-866-228-3546 or FDA at 1-800-FDA-1088 or www.fda.gov/medwatch.
 
DRUG INTERACTIONS
Hormonal contraceptives: Use with Tracleer decreases exposure and reduces contraceptive effectiveness (7.2).
Cyclosporine A, glyburide: Concomitant administration of each drug with Tracleer is contraindicated (7.3, 7.4).
Simvastatin and other CYP3A-metabolized statins: Combination use decreases statin levels and may reduce efficacy (7.6).
Rifampin: Alters bosentan levels. Monitor hepatic function weekly for 4 weeks, followed by normal monitoring (7.7).
 
USE IN SPECIFIC POPULATIONS
Nursing mothers: Discontinue nursing or the drug taking into consideration the importance of the drug to the mother (8.3).

See 17 for PATIENT COUNSELING INFORMATION and the FDA-approved Medication Guide 

Revised: 02/2011

FULL PRESCRIBING INFORMATION
WARNING: RISKS OF LIVER INJURY and TERATOGENICITY
Because of the risk of liver injury and birth defects, Tracleer is available only through a special restricted distribution program called the Tracleer Access Program (T.A.P.), by calling 1 866 228 3546. Only prescribers and pharmacies registered with T.A.P. may prescribe and distribute Tracleer. In addition, Tracleer may be dispensed only to patients who are enrolled in and meet all conditions of T.A.P. [see Warnings and Precautions (5.7)].
Liver Injury
In clinical studies, Tracleer caused at least 3-fold upper limit of normal (ULN) elevation of liver aminotransferases (ALT and AST) in about 11% of patients, accompanied by elevated bilirubin in a small number of cases. Because these changes are a marker for potential serious liver injury, serum aminotransferase levels must be measured prior to initiation of treatment and then monthly [see Dosage and Administration (2.2), Warnings and Precautions (5.1)]. In the postmarketing period, in the setting of close monitoring, rare cases of unexplained hepatic cirrhosis were reported after prolonged (> 12 months) therapy with Tracleer in patients with multiple co-morbidities and drug therapies. There have also been reports of liver failure. The contribution of Tracleer in these cases could not be excluded.
In at least one case, the initial presentation (after > 20 months of treatment) included pronounced elevations in aminotransferases and bilirubin levels accompanied by non-specific symptoms, all of which resolved slowly over time after discontinuation of Tracleer. This case reinforces the importance of strict adherence to the monthly monitoring schedule for the duration of treatment and the treatment algorithm, which includes stopping Tracleer with a rise of aminotransferases accompanied by signs or symptoms of liver dysfunction [see Dosage and Administration (2.2)].
Elevations in aminotransferases require close attention [see Dosage and Administration (2.2)]. Tracleer should generally be avoided in patients with elevated aminotransferases (> 3 × ULN) at baseline because monitoring liver injury may be more difficult. If liver aminotransferase elevations are accompanied by clinical symptoms of liver injury (such as nausea, vomiting, fever, abdominal pain, jaundice, or unusual lethargy or fatigue) or increases in bilirubin ≥ 2 × ULN, treatment with Tracleer should be stopped. There is no experience with the re-introduction of Tracleer in these circumstances.
Teratogenicity
Tracleer is likely to cause major birth defects if used by pregnant females based on animal data [see Contraindications (4.1)]. Therefore, pregnancy must be excluded before the start of treatment with Tracleer. Throughout treatment and for one month after stopping Tracleer, females of childbearing potential must use two reliable methods of contraception unless the patient has a tubal sterilization or Copper T 380A IUD or LNg 20 IUS inserted, in which case no other contraception is needed. Hormonal contraceptives, including oral, injectable, transdermal, and implantable contraceptives should not be used as the sole means of contraception because these may not be effective in patients receiving Tracleer [see Drug Interactions (7.2)]. Monthly pregnancy tests should be obtained.
1. INDICATIONS AND USAGE

1.1 Pulmonary Arterial Hypertension

Tracleer® is indicated for the treatment of pulmonary arterial hypertension (PAH) (WHO Group 1) to improve exercise ability and to decrease clinical worsening. Studies establishing effectiveness included predominately patients with NYHA Functional Class II-IV symptoms and etiologies of idiopathic or heritable PAH (60%), PAH associated with connective tissue diseases (21%), and PAH associated with congenital systemic-to-pulmonary shunts (18%) [see Clinical Studies (14.1)].

Considerations for use

Patients with WHO Class II symptoms showed reduction in the rate of clinical deterioration and a trend for improvement in walk distance. Physicians should consider whether these benefits are sufficient to offset the risk of liver injury in WHO Class II patients, which may preclude future use as their disease progresses.

2. DOSAGE AND ADMINISTRATION

2.1 Recommended Dosing

Tracleer treatment should be initiated at a dose of 62.5 mg twice daily for 4 weeks and then increased to the maintenance dose of 125 mg twice daily. Doses above 125 mg twice daily did not appear to confer additional benefit sufficient to offset the increased risk of liver injury.

Tablets should be administered morning and evening with or without food.

2.2 Required Monitoring

Liver aminotransferase levels must be measured prior to initiation of treatment and then monthly. If elevated aminotransferase levels are seen, changes in monitoring and treatment must be initiated.

2.3 Dosage Adjustments for Patients Developing Aminotransferase Elevations

The table below summarizes the dosage adjustment and monitoring recommendations for patients who develop aminotransferase elevations >3 × ULN during therapy with Tracleer. If liver aminotransferase elevations are accompanied by clinical symptoms of liver injury (such as nausea, vomiting, fever, abdominal pain, jaundice, or unusual lethargy or fatigue) or increases in bilirubin ≥ 2 × ULN, treatment with Tracleer should be stopped. There is no experience with the re-introduction of Tracleer in these circumstances.

Table 1: Dosage Adjustment and Monitoring in Patients Developing Aminotransferase Elevations >3 × ULN
ALT/AST levels Treatment and monitoring recommendations
> 3 and ≤ 5 × ULN Confirm by another aminotransferase test; if confirmed, reduce the daily dose to 62.5 mg twice daily or interrupt treatment, and monitor aminotransferase levels at least every 2 weeks. If the aminotransferase levels return to pre-treatment values, continue or re-introduce the treatment as appropriate (see below).
   
> 5 and ≤ 8 × ULN Confirm by another aminotransferase test; if confirmed, stop treatment and monitor aminotransferase levels at least every 2 weeks. Once the aminotransferase levels return to pre-treatment values, consider re-introduction of the treatment (see below).
   
> 8 × ULN Treatment should be stopped and re-introduction of Tracleer should not be considered. There is no experience with re-introduction of Tracleer in these circumstances.

If Tracleer is re-introduced it should be at the starting dose; aminotransferase levels should be checked within 3 days and thereafter according to the recommendations above.

2.4 Use in Females of Childbearing Potential

Initiate treatment in females of child-bearing potential only after a negative pregnancy test and only in females who are using two reliable methods of contraception. Females who have had a tubal sterilization or a Copper T 380A IUD or LNg 20 IUS inserted do not require other forms of contraception. Effective contraception must be practiced throughout treatment and for one month after stopping Tracleer. Females should seek contraceptive advice as needed from a gynecologist or similar expert. Urine or serum pregnancy tests should be obtained monthly in females of childbearing potential taking Tracleer [see Boxed Warning, Contraindications (4.1), Drug Interactions (7.2)].

2.5 Use in Patients with Pre-existing Hepatic Impairment

Tracleer should generally be avoided in patients with moderate or severe liver impairment. There are no specific data to guide dosing in hepatically impaired patients; caution should be exercised in patients with mildly impaired liver function [see Warnings and Precautions (5.2)].

2.6 Patients with Low Body Weight

In patients with a body weight below 40 kg but who are over 12 years of age the recommended initial and maintenance dose is 62.5 mg twice daily. There is limited information about the safety and efficacy of Tracleer in children between the ages of 12 and 18 years.

2.7 Use with Ritonavir

Co-administration of Tracleer in Patients on Ritonavir

In patients who have been receiving ritonavir for at least 10 days, start Tracleer at 62.5 mg once daily or every other day based upon individual tolerability [see Drug Interactions (7.5)].

Co-administration of Ritonavir in Patients on Tracleer

Discontinue use of Tracleer at least 36 hours prior to initiation of ritonavir. After at least 10 days following the initiation of ritonavir, resume Tracleer at 62.5 mg once daily or every other day based upon individual tolerability [see Dosage and Administration (2.8) and Drug Interactions (7.5)].

2.8 Treatment Discontinuation

There is limited experience with abrupt discontinuation of Tracleer. No evidence for acute rebound has been observed. Nevertheless, to avoid the potential for clinical deterioration, gradual dose reduction (62.5 mg twice daily for 3 to 7 days) should be considered.

3. DOSAGE FORMS AND STRENGTHS

Tracleer is available as 62.5 mg and 125 mg film-coated, unscored tablets for oral administration.

62.5 mg tablets: film-coated, round, biconvex, orange-white tablets, embossed with identification marking "62,5"

125 mg tablets: film-coated, oval, biconvex, orange-white tablets, embossed with identification marking "125"

4. CONTRAINDICATIONS

4.1 Pregnancy Category X

[see BOXED WARNING]

Use of Tracleer is contraindicated in females who are or may become pregnant. While there are no adequate and well controlled studies in pregnant females, animal studies show that Tracleer is likely to cause major birth defects when administered during pregnancy. In animal studies, bosentan caused teratogenic effects including malformations of the head, mouth, face, and large blood vessels. Therefore, pregnancy must be excluded before the start of treatment with Tracleer. Throughout treatment and for one month after stopping Tracleer, females of child bearing potential must use two reliable methods of contraception unless the patient has a tubal sterilization or Copper T 380A IUD or LNg 20 IUS inserted, in which case no other contraception is needed. Monthly pregnancy tests should also be obtained. If this drug is used during pregnancy or if a patient becomes pregnant while taking this drug, the patient should be apprised of the potential hazard to the fetus. [see Use in Specific Populations (8.1)].

4.2 Use with Cyclosporine A

Co-administration of cyclosporine A and bosentan resulted in markedly increased plasma concentrations of bosentan. Therefore, concomitant use of Tracleer and cyclosporine A is contraindicated [see Drug Interactions (7.3)].

4.3 Use with Glyburide

An increased risk of liver enzyme elevations was observed in patients receiving glyburide concomitantly with bosentan. Therefore co-administration of glyburide and Tracleer is contraindicated [see Drug Interactions (7.4)].

4.4 Hypersensitivity

Tracleer is contraindicated in patients who are hypersensitive to bosentan or any component of the product. Observed reactions include rash and angioedema [see Adverse Reactions (6.2)].

5 WARNINGS AND PRECAUTIONS

5.1 Potential Liver Injury

Elevations in ALT or AST by more than 3 × ULN were observed in 11% of bosentan-treated patients (N = 658) compared to 2% of placebo-treated patients (N = 280). Three-fold increases were seen in 12% of 95 pulmonary arterial hypertension (PAH) patients on 125 mg twice daily and 14% of 70 PAH patients on 250 mg twice daily. Eight-fold increases were seen in 2% of PAH patients on 125 mg twice daily and 7% of PAH patients on 250 mg twice daily. Bilirubin increases to ≥3 × ULN were associated with aminotransferase increases in 2 of 658 (0.3%) of patients treated with bosentan. The combination of hepatocellular injury (increases in aminotransferases of > 3 × ULN) and increases in total bilirubin (≥ 3 × ULN) is a marker for potential serious liver injury.

Elevations of AST and/or ALT associated with bosentan are dose-dependent, occur both early and late in treatment, usually progress slowly, are typically asymptomatic, and usually have been reversible after treatment interruption or cessation. Aminotransferase elevations also may reverse spontaneously while continuing treatment with Tracleer.

Liver aminotransferase levels must be measured prior to initiation of treatment and then monthly. If elevated aminotransferase levels are seen, changes in monitoring and treatment must be initiated. If liver aminotransferase elevations are accompanied by clinical symptoms of liver injury (such as nausea, vomiting, fever, abdominal pain, jaundice, or unusual lethargy or fatigue) or increases in bilirubin ≥ 2 × ULN, treatment should be stopped. There is no experience with the re-introduction of Tracleer in these circumstances [see Dosage and Administration (2.2)].

5.2 Patients with Pre-existing Hepatic Impairment

Liver aminotransferase levels must be measured prior to initiation of treatment and then monthly. Tracleer should generally be avoided in patients with moderate or severe liver impairment [see Dosage and Administration (2.5)]. In addition, Tracleer should generally be avoided in patients with elevated aminotransferases (> 3 × ULN) because monitoring liver injury in these patients may be more difficult [see Boxed Warning].

5.3 Fluid Retention

Peripheral edema is a known clinical consequence of PAH and worsening PAH and is also a known effect of other endothelin receptor antagonists. In PAH clinical trials with Tracleer, combined adverse events of fluid retention or edema were reported in 1.7 percent (placebo-corrected) of patients [see Clinical Studies (14.2)].

In addition, there have been numerous post-marketing reports of fluid retention in patients with pulmonary hypertension occurring within weeks after starting Tracleer. Patients required intervention with a diuretic, fluid management, or hospitalization for decompensating heart failure.

If clinically significant fluid retention develops, with or without associated weight gain, further evaluation should be undertaken to determine the cause, such as Tracleer or underlying heart failure, and the possible need for treatment or discontinuation of Tracleer therapy.

5.4 Decreased Sperm Counts

An open-label, single arm, multicenter, safety study evaluated the effect on testicular function of Tracleer 62.5 mg twice daily for 4 weeks, followed by 125 mg twice daily for 5 months. Twenty-five male patients with WHO functional class III and IV PAH and normal baseline sperm count were enrolled. Twenty-three completed the study and 2 discontinued due to adverse events not related to testicular function. There was a decline in sperm count of at least 50% in 25% of the patients after 3 or 6 months of treatment with Tracleer. Sperm count remained within the normal range in all 22 patients with data after 6 months and no changes in sperm morphology, sperm motility, or hormone levels were observed. One patient developed marked oligospermia at 3 months and the sperm count remained low with 2 follow-up measurements over the subsequent 6 weeks. Tracleer was discontinued and after two months the sperm count had returned to baseline levels. Based on these findings and preclinical data from endothelin receptor antagonists, it cannot be excluded that endothelin receptor antagonists such as Tracleer have an adverse effect on spermatogenesis.

5.5 Decreases in Hemoglobin and Hematocrit

Treatment with Tracleer can cause a dose-related decrease in hemoglobin and hematocrit. It is recommended that hemoglobin concentrations be checked after 1 and 3 months, and every 3 months thereafter. If a marked decrease in hemoglobin concentration occurs, further evaluation should be undertaken to determine the cause and need for specific treatment.

The overall mean decrease in hemoglobin concentration for bosentan-treated patients was 0.9 g/dL (change to end of treatment). Most of this decrease of hemoglobin concentration was detected during the first few weeks of bosentan treatment and hemoglobin levels stabilized by 4–12 weeks of bosentan treatment. In placebo-controlled studies of all uses of bosentan, marked decreases in hemoglobin (> 15% decrease from baseline resulting in values < 11 g/dL) were observed in 6% of bosentan-treated patients and 3% of placebo-treated patients. In patients with PAH treated with doses of 125 and 250 mg twice daily, marked decreases in hemoglobin occurred in 3% compared to 1% in placebo-treated patients.

A decrease in hemoglobin concentration by at least 1 g/dL was observed in 57% of bosentan-treated patients as compared to 29% of placebo-treated patients. In 80% of those patients whose hemoglobin decreased by at least 1 g/dL, the decrease occurred during the first 6 weeks of bosentan treatment.

During the course of treatment the hemoglobin concentration remained within normal limits in 68% of bosentan-treated patients compared to 76% of placebo patients. The explanation for the change in hemoglobin is not known, but it does not appear to be hemorrhage or hemolysis.

5.6 Pulmonary Veno-Occlusive Disease

Should signs of pulmonary edema occur when Tracleer is administered, the possibility of associated pulmonary veno-occlusive disease should be considered and Tracleer should be discontinued.

5.7 Prescribing and Distribution Program for Tracleer

Because of the risks of liver injury and birth defects, Tracleer is available only through a special restricted distribution program called the Tracleer Access Program (T.A.P.). Only prescribers and pharmacies registered with T.A.P. may prescribe and distribute Tracleer. In addition, Tracleer may be dispensed only to patients who are enrolled in and meet all conditions of T.A.P. Information about Tracleer and T.A.P. can be obtained by calling 1-866-228-3546.

To enroll in T.A.P., prescribers must complete the T.A.P. Tracleer (bosentan) Enrollment and Renewal Form (see T.A.P. Tracleer (bosentan) Enrollment and Renewal Form for full prescribing physician agreement) indicating agreement to:

  • Read and understand the communication and educational materials for prescribers regarding the risks of Tracleer.
  • Review and discuss the Tracleer Medication Guide and the risks of bosentan (including the risks of teratogenicity and hepatotoxicity) with every patient prior to prescribing Tracleer.
  • Review pretreatment liver function tests (ALT/AST/bilirubin) and, for females of childbearing potential, confirm that the patient is not pregnant.
  • Agree to order and monitor monthly liver function tests and, for females of childbearing potential, pregnancy tests.
  • Enroll all patients in T.A.P. and renew patients' enrollment annually thereafter.
  • Educate and counsel females of childbearing potential to use reliable contraception, as defined on the Tracleer Enrollment and Renewal Form, during treatment with Tracleer and for one month after treatment discontinuation.
  • Counsel patients who fail to comply with the program requirements.
  • Notify Actelion Pharmaceuticals US, Inc. of any adverse events, including liver injury, and report any pregnancy during Tracleer treatment.

Throughout treatment and for one month after stopping Tracleer, females of childbearing potential must use two reliable methods of contraception unless the patient has a tubal sterilization or Copper T 380A IUD or LNg 20 IUS inserted, in which case no other contraception is needed. Hormonal contraceptives, including oral, injectable, transdermal, and implantable contraceptives should not be used as the sole means of contraception because these may not be effective in patients receiving Tracleer.

6. ADVERSE REACTIONS

The following important adverse reactions are described elsewhere in the labeling:

  • Potential liver injury [see Boxed Warning, Warnings and Precautions (5.1)]
  • Fluid retention [see Warnings and Precautions (5.3)]

6.1 Clinical Studies Experience

Safety data on bosentan were obtained from 13 clinical studies (9 placebo-controlled and 4 open-label) in 870 patients with pulmonary arterial hypertension and other diseases. Doses up to 8 times the currently recommended clinical dose (125 mg twice daily) were administered for a variety of durations. The exposure to bosentan in these trials ranged from 1 day to 4.1 years (N=94 for 1 year; N=61 for 1.5 years and N=39 for more than 2 years). Exposure of pulmonary arterial hypertension patients (N=328) to bosentan ranged from 1 day to 1.7 years (N=174 more than 6 months and N=28 more than 12 months).

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.

Treatment discontinuations due to adverse events other than those related to pulmonary hypertension during the clinical trials in patients with pulmonary arterial hypertension were more frequent on bosentan (6%; 15/258 patients) than on placebo (3%; 5/172 patients). In this database the only cause of discontinuations > 1% and occurring more often on bosentan was abnormal liver function.

The adverse drug events that occurred in ≥3% of the bosentan-treated patients and were more common on bosentan in placebo-controlled trials in pulmonary arterial hypertension at doses of 125 or 250 mg twice daily are shown in Table 2:

Table 2. Adverse events* occurring in ≥3% of patients treated with bosentan 125-250 mg twice daily and more common on bosentan in placebo-controlled studies in pulmonary arterial hypertension
Adverse Event Bosentan
N = 258
Placebo
N = 172

Note: only AEs with onset from start of treatment to 1 calendar day after end of treatment are included. All reported events (at least 3%) are included except those too general to be informative, and those not reasonably associated with the use of the drug because they were associated with the condition being treated or are very common in the treated population.
Combined data from Study-351, BREATHE-1 and EARLY

No. % No. %
Respiratory Tract Infection 56 22% 30 17%
Headache 39 15% 25 14%
Edema 28 11% 16 9%
Chest Pain 13 5% 8 5%
Syncope 12 5% 7 4%
Flushing 10 4% 5 3%
Hypotension 10 4% 3 2%
Sinusitis 9 4% 4 2%
Arthralgia 9 4% 3 2%
Liver Function Test Abnormal 9 4% 3 2%
Palpitations 9 4% 3 2%
Anemia 8 3% -

6.2 Postmarketing Experience

There have been several post-marketing reports of angioedema associated with the use of bosentan. The onset of the reported cases occurred within a range of 8 hours to 21 days after starting therapy. Some patients were treated with an antihistamine and their signs of angioedema resolved without discontinuing Tracleer.

The following additional adverse reactions have been reported during the post approval use of Tracleer. Because these adverse reactions are reported from a population of uncertain size, it is not always possible to reliably estimate their frequency or establish a causal relationship to Tracleer exposure:

Unexplained hepatic cirrhosis [see Boxed Warning]
Liver failure [see Boxed Warning]
Hypersensitivity [see Contraindications (4.4)]
Thrombocytopenia
Rash
Jaundice
Anemia requiring transfusion
Neutropenia and leukopenia

7. DRUG INTERACTIONS

7.1 Cytochrome P450 Summary

Bosentan is metabolized by CYP2C9 and CYP3A. Inhibition of these enzymes may increase the plasma concentration of bosentan (see ketoconazole). Concomitant administration of both a CYP2C9 inhibitor (such as fluconazole or amiodarone) and a strong CYP3A inhibitor (e.g., ketoconazole, itraconazole) or a moderate CYP3A inhibitor (e.g., amprenavir, erythromycin, fluconazole, diltiazem) with bosentan will likely lead to large increases in plasma concentrations of bosentan. Co-administration of such combinations of a CYP2C9 inhibitor plus a strong or moderate CYP3A inhibitor with Tracleer is not recommended.

Bosentan is an inducer of CYP3A and CYP2C9. Consequently plasma concentrations of drugs metabolized by these two isozymes will be decreased when Tracleer is co-administered. Bosentan had no relevant inhibitory effect on any CYP isozyme in vitro (CYP1A2, CYP2C9, CYP2C19, CYP2D6, CYP3A). Consequently, Tracleer is not expected to increase the plasma concentrations of drugs metabolized by these enzymes.

7.2 Hormonal Contraceptives

Hormonal contraceptives, including oral, injectable, transdermal, and implantable forms, may not be reliable when Tracleer is co-administered. Females should practice additional methods of contraception and not rely on hormonal contraception alone when taking Tracleer [see Boxed Warning, Contraindications (4.1)].

An interaction study demonstrated that co-administration of bosentan and a combination oral hormonal contraceptive produced average decreases of norethindrone and ethinyl estradiol levels of 14% and 31%, respectively. However, decreases in exposure were as much as 56% and 66%, respectively, in individual subjects.

7.3 Cyclosporine A

The concomitant administration of bosentan and cyclosporine A is contraindicated [see Contraindications (4.2)].

During the first day of concomitant administration, trough concentrations of bosentan were increased by about 30-fold. The mechanism of this interaction is most likely inhibition of transport protein-mediated uptake of bosentan into hepatocytes by cyclosporine. Steady-state bosentan plasma concentrations were 3- to 4-fold higher than in the absence of cyclosporine A. Co-administration of bosentan decreased the plasma concentrations of cyclosporine A (a CYP3A substrate) by approximately 50%.

7.4 Glyburide

An increased risk of elevated liver aminotransferases was observed in patients receiving concomitant therapy with glyburide. Therefore, the concomitant administration of Tracleer and glyburide is contraindicated, and alternative hypoglycemic agents should be considered [see Contraindications (4.3)].

Co-administration of bosentan decreased the plasma concentrations of glyburide by approximately 40%. The plasma concentrations of bosentan were also decreased by approximately 30%. Bosentan is also expected to reduce plasma concentrations of other oral hypoglycemic agents that are predominantly metabolized by CYP2C9 or CYP3A. The possibility of worsened glucose control in patients using these agents should be considered.

7.5 Lopinavir/Ritonavir or Other Ritonavir-containing HIV Regimens

In vitro data indicate that bosentan is a substrate of the Organic Anion Transport Protein (OATP), CYP3A and CYP2C9. Ritonavir inhibits OATP and inhibits and induces CYP3A. However, the impact of ritonavir on the pharmacokinetics of bosentan may largely result from its effect on OATP.

In normal volunteers, co-administration of Tracleer 125 mg twice daily and lopinavir/ritonavir 400/100 mg twice daily increased the trough concentrations of bosentan on Days 4 and 10 approximately 48-fold and 5-fold, respectively, compared with those measured after Tracleer administered alone. Therefore, adjust the dose of Tracleer when initiating lopinavir/ritonavir [see Dosage and Administration (2.7)].

Co-administration of Tracleer 125 mg twice daily had no substantial impact on the pharmacokinetics of lopinavir/ritonavir 400/100 mg twice daily.

7.6 Simvastatin and Other Statins

Co-administration of bosentan decreased the plasma concentrations of simvastatin (a CYP3A substrate), and its active β-hydroxy acid metabolite, by approximately 50%. The plasma concentrations of bosentan were not affected. Bosentan is also expected to reduce plasma concentrations of other statins that are significantly metabolized by CYP3A, such as lovastatin and atorvastatin. The possibility of reduced statin efficacy should be considered. Patients using CYP3A-metabolized statins should have cholesterol levels monitored after Tracleer is initiated to see whether the statin dose needs adjustment.

7.7 Rifampin

Co-administration of bosentan and rifampin in normal volunteers resulted in a mean 6-fold increase in bosentan trough levels after the first concomitant dose (likely due to inhibition of OATP by rifampin), but about a 60% decrease in bosentan levels at steady-state. The effect of bosentan on rifampin levels has not been assessed. When consideration of the potential benefits and known and unknown risks leads to concomitant use, measure liver function weekly for the first 4 weeks before reverting to normal monitoring.

7.8 Tacrolimus

Co-administration of tacrolimus and bosentan has not been studied in humans. Co-administration of tacrolimus and bosentan resulted in markedly increased plasma concentrations of bosentan in animals. Caution should be exercised if tacrolimus and bosentan are used together.

7.9 Ketoconazole

Co-administration of bosentan 125 mg twice daily and ketoconazole, a potent CYP3A inhibitor, increased the plasma concentrations of bosentan by approximately 2-fold in normal volunteers. No dose adjustment of bosentan is necessary, but increased effects of bosentan should be considered.

7.10 Warfarin

Co-administration of bosentan 500 mg twice daily for 6 days in normal volunteers, decreased the plasma concentrations of both S-warfarin (a CYP2C9 substrate) and R-warfarin (a CYP3A substrate) by 29 and 38%, respectively. Clinical experience with concomitant administration of bosentan and warfarin in patients with pulmonary arterial hypertension did not show clinically relevant changes in INR or warfarin dose (baseline vs. end of the clinical studies), and the need to change the warfarin dose during the trials due to changes in INR or due to adverse events was similar among bosentan- and placebo-treated patients.

7.11 Digoxin, Nimodipine, and Losartan

Bosentan has no significant pharmacokinetic interactions with digoxin and nimodipine, and losartan has no significant effect on plasma levels of bosentan.

7.12 Sildenafil

In normal volunteers, co-administration of multiple doses of 125 mg twice daily bosentan and 80 mg three times daily sildenafil resulted in a reduction of sildenafil plasma concentrations by 63% and increased bosentan plasma concentrations by 50%. The changes in plasma concentrations were not considered clinically relevant and dose adjustments are not necessary. This recommendation holds true when sildenafil is used for the treatment of pulmonary arterial hypertension or erectile dysfunction.

7.13 Iloprost

In a small, randomized, double-blind, placebo-controlled study, 34 patients treated with bosentan 125 mg twice daily for at least 16 weeks tolerated the addition of inhaled iloprost (up to 5 mcg 6 to 9 times per day during waking hours). The mean daily inhaled dose was 27 mcg and the mean number of inhalations per day was 5.6.

8. USE IN SPECIFIC POPULATIONS

8.1 Pregnancy

Pregnancy Category X: Teratogenic Effects [see Contraindications (4.1)]

Use of Tracleer is contraindicated in females who are or may become pregnant. While there are no adequate and well controlled studies in pregnant females, animal studies show that Tracleer is likely to cause major birth defects when administered during pregnancy. Bosentan caused teratogenic effects in animals including malformations of the head, mouth, face, and large blood vessels. If this drug is used during pregnancy or if a patient becomes pregnant while taking this drug, the patient should be apprised of the potential hazard to the fetus.

Females of childbearing potential should have a negative pregnancy test before starting treatment with Tracleer. The prescriber should not dispense a prescription for Tracleer without documenting a negative urine or serum pregnancy test performed during the first 5 days of a normal menstrual period and at least 11 days after the last unprotected act of sexual intercourse. Follow-up urine or serum pregnancy tests should be obtained monthly in females of childbearing potential taking Tracleer. The patient should contact her physician immediately for pregnancy testing if onset of menses is delayed or pregnancy is suspected. If the pregnancy test is positive, the physician and patient must discuss the risks to her, the pregnancy, and the fetus.

Drug interaction studies show that Tracleer reduces serum levels of the estrogen and progestin in oral contraceptives. Based on these findings, hormonal contraceptives (including oral, injectable, transdermal, and implantable contraceptives) may be less effective for preventing pregnancy in patients using Tracleer and should not be used as a patient's only contraceptive method [see Drug Interactions (7.2)]. Females of childbearing potential using Tracleer must use two reliable forms of contraception unless she has a tubal sterilization or has a Copper T 380A IUD or LNg 20 IUS. In these cases, no additional contraception is needed. Contraception should be continued until one month after completing Tracleer therapy. Females of childbearing potential using Tracleer should seek contraception counseling from a gynecologist or other expert as needed.

Bosentan was teratogenic in rats given oral doses two times the maximum recommended human dose [MRHD] (on a mg/ m2 basis). In an embryo-fetal toxicity study in rats, bosentan showed dose-dependent teratogenic effects, including malformations of the head, mouth, face and large blood vessels. Bosentan increased stillbirths and pup mortality at oral doses 2 and 10 times the MRHD (on a mg/m2 basis). Although birth defects were not observed in rabbits given oral doses of up to the equivalent of 10.5 g/day in a 70 kg person, plasma concentrations of bosentan in rabbits were lower than those reached in the rat. The similarity of malformations induced by bosentan and those observed in endothelin-1 knockout mice and in animals treated with other endothelin receptor antagonists indicates that teratogenicity is a class effect of these drugs [see Nonclinical Toxicology (13.1)].

8.3 Nursing mothers

It is not known whether Tracleer is excreted into human milk. Because many drugs are excreted in human milk, and because of the potential for serious adverse reactions in nursing infants from Tracleer, a decision should be made to discontinue nursing or to discontinue the drug, taking into account the importance of the drug to the mother.

8.4 Pediatric use

Safety and efficacy in pediatric patients have not been established.

8.5 Geriatric use

Clinical studies of Tracleer did not include sufficient numbers of subjects aged 65 and older to determine whether they respond differently from younger subjects. Clinical experience has not identified differences in responses between elderly and younger patients. In general, caution should be exercised in dose selection for elderly patients given the greater frequency of decreased hepatic, renal, or cardiac function, and of concomitant disease or other drug therapy in this age group.

8.6 Hepatic Impairment

Because there is in vitro and in vivo evidence that the main route of excretion of bosentan is biliary, liver impairment could be expected to increase exposure (Cmax and AUC) of bosentan. Mild liver impairment was shown not to impact the pharmacokinetics of bosentan. The influence of moderate or severe liver impairment on the pharmacokinetics of Tracleer has not been evaluated. There are no specific data to guide dosing in hepatically impaired patients; caution should be exercised in patients with mildly impaired liver function. Tracleer should generally be avoided in patients with moderate or severe liver impairment [see Dosage and Administration (2.5), Warnings and Precautions (5.2), Pharmacokinetics (12.3)].

8.7 Renal Impairment

The effect of renal impairment on the pharmacokinetics of bosentan is small and does not require dosing adjustment [see Pharmacokinetics (12.3)].

8.8 Patients with Low Body Weight

[See Dosage and Administration (2.6)].

10. OVERDOSAGE

Bosentan has been given as a single dose of up to 2400 mg in normal volunteers, or up to 2000 mg/day for 2 months in patients, without any major clinical consequences. The most common side effect was headache of mild to moderate intensity. In the cyclosporine A interaction study, in which doses of 500 and 1000 mg twice daily of bosentan were given concomitantly with cyclosporine A, trough plasma concentrations of bosentan increased 30-fold, resulting in severe headache, nausea, and vomiting, but no serious adverse events. Mild decreases in blood pressure and increases in heart rate were observed.

In the postmarketing period, there was one reported overdose of 10,000 mg of bosentan taken by an adolescent male patient. He had symptoms of nausea, vomiting, hypotension, dizziness, sweating, and blurred vision. He recovered within 24 hours with blood pressure support.

Bosentan is unlikely to be effectively removed by dialysis due to the high molecular weight and extensive plasma protein binding.

11. DESCRIPTION

Bosentan is an endothelin receptor antagonist, belonging to a class of highly substituted pyrimidine derivatives, with no chiral centers. It is designated chemically as 4-tert-butyl-N-[6-(2-hydroxy-ethoxy)-5-(2-methoxy-phenoxy)-[2,2´]-bipyrimidin-4-yl]- benzenesulfonamide monohydrate and has the following structural formula:

Chemical Structure

Bosentan has a molecular weight of 569.64 and a molecular formula of C27H29N5O6S•H2O. Bosentan is a white to yellowish powder. It is poorly soluble in water (1.0 mg/100 mL) and in aqueous solutions at low pH (0.1 mg/100 mL at pH 1.1 and 4.0; 0.2 mg/100 mL at pH 5.0). Solubility increases at higher pH values (43 mg/100 mL at pH 7.5). In the solid state, bosentan is very stable, is not hygroscopic and is not light sensitive.

Tracleer is available as 62.5 mg and 125 mg film-coated tablets for oral administration, and contains the following excipients: corn starch, pregelatinized starch, sodium starch glycolate, povidone, glyceryl behenate, magnesium stearate, hydroxypropylmethylcellulose, triacetin, talc, titanium dioxide, iron oxide yellow, iron oxide red, and ethylcellulose. Each Tracleer 62.5 mg tablet contains 64.541 mg of bosentan, equivalent to 62.5 mg of anhydrous bosentan. Each Tracleer 125 mg tablet contains 129.082 mg of bosentan, equivalent to 125 mg of anhydrous bosentan.

12. CLINICAL PHARMACOLOGY

12.1 Mechanism of action

Endothelin-1 (ET-1) is a neurohormone, the effects of which are mediated by binding to ETA and ETB receptors in the endothelium and vascular smooth muscle. ET-1 concentrations are elevated in plasma and lung tissue of patients with pulmonary arterial hypertension, suggesting a pathogenic role for ET-1 in this disease. Bosentan is a specific and competitive antagonist at endothelin receptor types ETA and ETB. Bosentan has a slightly higher affinity for ETA receptors than for ETB receptors. The clinical impact of dual endothelin blockage is unknown.

12.3 Pharmacokinetics

General: After oral administration, maximum plasma concentrations of bosentan are attained within 3–5 hours and the terminal elimination half-life (t1/2) is about 5 hours in healthy adult subjects. The exposure to bosentan after intravenous and oral administration is about 2-fold greater in adult patients with pulmonary arterial hypertension than in healthy adult subjects.

Absorption and Distribution: The absolute bioavailability of bosentan in normal volunteers is about 50% and is unaffected by food. The volume of distribution is about 18 L. Bosentan is highly bound (> 98%) to plasma proteins, mainly albumin. Bosentan does not penetrate into erythrocytes.

Metabolism and Elimination: Bosentan has three metabolites, one of which is pharmacologically active and may contribute 10%–20% of the effect of bosentan. Bosentan is an inducer of CYP2C9 and CYP3A and possibly also of CYP2C19. Total clearance after a single intravenous dose is about 4 L/hr in patients with pulmonary arterial hypertension. Upon multiple oral dosing, plasma concentrations in healthy adults decrease gradually to 50-65% of those seen after single dose administration, probably the effect of auto-induction of the metabolizing liver enzymes. Steady-state is reached within 3-5 days. Bosentan is eliminated by biliary excretion following metabolism in the liver. Less than 3% of an administered oral dose is recovered in urine.

Special Populations: It is not known whether bosentan's pharmacokinetics is influenced by gender, body weight, race, or age.

Hepatic Impairment: In vitro and in vivo evidence showing extensive hepatic metabolism of bosentan suggests that liver impairment could significantly increase exposure of bosentan. In a study comparing 8 patients with mild liver impairment (as indicated by the Child-Pugh method) to 8 controls, the single- and multiple-dose pharmacokinetics of bosentan was not altered in patients with mild hepatic impairment. The influence of moderate or severe liver impairment on the pharmacokinetics of bosentan has not been evaluated. Bosentan should generally be avoided in patients with moderate or severe liver abnormalities and/or elevated aminotransferases >3 × ULN [see Dosage and Administration (2.5), Warnings and Precautions (5.2)].

Renal Impairment: In patients with severe renal impairment (creatinine clearance 15–30 mL/min), plasma concentrations of bosentan were essentially unchanged and plasma concentrations of the three metabolites were increased about 2-fold compared to people with normal renal function. These differences do not appear to be clinically important.

13. NONCLINICAL TOXICOLOGY

13.1 Carcinogenesis, Mutagenesis, Impairment of Fertility

Carinogenesis and Mutagenesis

Two years of dietary administration of bosentan to mice produced an increased incidence of hepatocellular adenomas and carcinomas in males at doses as low as 450 mg/kg/day (about 8 times the maximum recommended human dose [MRHD] of 125 mg twice daily, on a mg/m2 basis). In the same study, doses greater than 2000 mg/kg/day (about 32 times the MRHD) were associated with an increased incidence of colon adenomas in both males and females. In rats, dietary administration of bosentan for two years was associated with an increased incidence of brain astrocytomas in males at doses as low as 500 mg/kg/day (about 16 times the MRHD). In a comprehensive battery of in vitro tests (the microbial mutagenesis assay, the unscheduled DNA synthesis assay, the V-79 mammalian cell mutagenesis assay, and human lymphocyte assay) and an in vivo mouse micronucleus assay, there was no evidence for any mutagenic or clastogenic activity of bosentan.

Reproductive and Developmental Toxicology

Bosentan was teratogenic in rats given oral doses ≥60 mg/kg/day. In an embryo-fetal toxicity study in rats, bosentan showed dose-dependent teratogenic effects, including malformations of the head, mouth, face and large blood vessels. Bosentan increased stillbirths and pup mortality at oral doses of 60 and 300 mg/kg/day. Although birth defects were not observed in rabbits given oral doses of up to 1500 mg/kg/day, plasma concentrations of bosentan in rabbits were lower than those reached in the rat. The similarity of malformations induced by bosentan and those observed in endothelin-1 knockout mice and in animals treated with other endothelin receptor antagonists indicates that teratogenicity is a class effect of these drugs.

Impairment of Fertility/Testicular Function

The development of testicular tubular atrophy and impaired fertility has been linked with the chronic administration of certain endothelin receptor antagonists in rodents.

Treatment with bosentan at oral doses of up to 1500 mg/kg/day (50 times the MRHD on a mg/m2 basis) or intravenous doses up to 40 mg/kg/day had no effects on sperm count, sperm motility, mating performance or fertility in male and female rats. An increased incidence of testicular tubular atrophy was observed in rats given bosentan orally at doses as low as 125 mg/kg/ day (about 4 times the MRHD and the lowest doses tested) for two years but not at doses as high as 1500 mg/kg/day (about 50 times the MRHD) for 6 months. Effects on sperm count and motility were evaluated only in the much shorter duration fertility studies in which males had been exposed to the drug for 4-6 weeks. An increased incidence of tubular atrophy was not observed in mice treated for 2 years at doses up to 4500 mg/kg/day (about 75 times the MRHD) or in dogs treated up to 12 months at doses up to 500 mg/kg/day (about 50 times the MRHD).

14. CLINICAL STUDIES

14.1 Pulmonary Arterial Hypertension

WHO Functional Class III-IV

Two randomized, double-blind, multi-center, placebo-controlled trials were conducted in 32 and 213 patients. The larger study (BREATHE-1) compared 2 doses (125 mg twice daily and 250 mg twice daily) of Tracleer with placebo. The smaller study (Study 351) compared 125 mg twice daily with placebo. Patients had severe (WHO functional Class III–IV) pulmonary arterial hypertension: idiopathic or heritable pulmonary arterial hypertension (72%) or pulmonary arterial hypertension associated with scleroderma or other connective tissue diseases (21%), or to autoimmune diseases (7%). There were no patients with pulmonary arterial hypertension associated with other conditions such as HIV disease or recurrent pulmonary emboli.

In both studies, Tracleer or placebo was added to patients' current therapy, which could have included a combination of digoxin, anticoagulants, diuretics, and vasodilators (e.g., calcium channel blockers, ACE inhibitors), but not epoprostenol. Tracleer was given at a dose of 62.5 mg twice daily for 4 weeks and then at 125 mg twice daily or 250 mg twice daily for either 12 (BREATHE-1) or 8 (Study 351) additional weeks. The primary study endpoint was 6-minute walk distance. In addition, symptoms and functional status were assessed. Hemodynamic measurements were made at 12 weeks in Study 351.

The mean age was about 49 years. About 80% of patients were female, and about 80% were Caucasian. Patients had been diagnosed with pulmonary hypertension for a mean of 2.4 years.

Submaximal Exercise Ability

Results of the 6-minute walk distance at 3 months (Study 351) or 4 months (BREATHE-1) are shown in Table 3.

Table 3. Effects of bosentan on 6-minute walk distance
BREATHE-1 Study 351
Bosentan
125 mg twice daily
(n = 74)
Bosentan
250 mg twice daily
(n = 70)
Placebo

(n = 69)
Bosentan
125 mg twice daily
(n = 21)
Placebo

(n = 11)
Distance in meters: mean ± standard deviation. Changes are to week 16 for BREATHE-1 and to week 12 for Study 351.

p=0.01; by Wilcoxon;

p=0.0001; by Wilcoxon;  

p=0.02; by Student's t-test.

Baseline
326 ± 73

333 ± 75

344 ± 76

360 ± 86

355 ± 82
End point
353 ± 115

379 ± 101

336 ± 129

431 ± 66

350 ± 147
Change from baseline

27 ± 75

46 ± 62

-8 ± 96

70 ± 56

-6 ± 121
Placebo – subtracted
35

54


76

In both trials, treatment with Tracleer resulted in a significant increase in exercise ability. The improvement in walk distance was apparent after 1 month of treatment (with 62.5 mg twice daily) and fully developed by about 2 months of treatment (Figure 1). It was maintained for up to 7 months of double-blind treatment. Walking distance was somewhat greater with 250 mg twice daily, but the potential for increased liver injury causes this dose not to be recommended [see Dosage and Administration (2.1)]. There were no apparent differences in treatment effects on walk distance among subgroups analyzed by demographic factors, baseline disease severity, or disease etiology, but the studies had little power to detect such differences.

Change from baseline in 6-minute walking distance from start of therapy to week 16 in the placebo and combined bosentan (125 mg twice daily and 250 mg twice daily) groups. Values are expressed as mean ± standard error of the mean.

Hemodynamic Changes

Invasive hemodynamic parameters were assessed in Study 351. Treatment with Tracleer led to a significant increase in cardiac index (CI) associated with a significant reduction in pulmonary artery pressure (PAP), pulmonary vascular resistance (PVR), and mean right atrial pressure (RAP) (Table 4).

The relationship between hemodynamic effects and improvements in 6-minute walk distance is unknown.

Table 4: Change from Baseline to Week 12: Hemodynamic Parameters
Bosentan 125 mg twice daily Placebo
Values shown are means ± SD
p≤0.001;
p<0.02
Mean CI (L/min/m2) N=20 N=10
Baseline 2.35±0.73 2.48±1.03
Absolute Change 0.50±0.46 -0.52±0.48
Treatment Effect 1.02*
Mean PAP (mmHg) N=20 N=10
Baseline 53.7±13.4 55.7±10.5
Absolute Change -1.6±5.1 5.1±8.8
Treatment Effect -6.7†
Mean PVR (dyn∙sec∙cm-5) N=19 N=10
Baseline 896±425 942±430
Absolute Change -223±245 191±235
Treatment Effect -415*
Mean RAP (mmHg) N=19 N=10
Baseline 9.7±5.6 9.9±4.1
Absolute Change -1.3±4.1 4.9±4.6
Treatment Effect -6.2*

Symptoms and Functional Status

Symptoms of pulmonary arterial hypertension were assessed by Borg dyspnea score, WHO functional class, and rate of "clinical worsening." Clinical worsening was assessed as the sum of death, hospitalizations for PAH, discontinuation of therapy because of PAH, and need for epoprostenol. There was a significant reduction in dyspnea during walk tests (Borg dyspnea score), and significant improvement in WHO functional class in Tracleer-treated patients. There was a significant reduction in the rate of clinical worsening (Table 5 and Figure 2). Figure 2 shows the Log-rank test reflecting clinical worsening over 28 weeks.

Table 5: Incidence of Clinical Worsening, Intent To Treat Population

BREATHE-1

Study 351
Bosentan
125/250 mg twice daily
(N = 144)
Placebo
(N = 69)
Bosentan
125 mg twice daily
(N = 21)
Placebo
(N = 11)
Note: Patients may have had more than one reason for clinical worsening.
p=0.0015 vs. placebo by log-rank test. There was no relevant difference between the 125 mg and 250 mg twice daily groups.
p=0.033 vs. placebo by Fisher's exact test.
Receipt of epoprostenol was always a consequence of clinical worsening.
Patients with clinical worsening
[n (%)]
9 (6%)* 14 (20%) 0 (0%)† 3 (27%)
Death 1 (1%) 2 (3%) 0 (0%) 0 (0%)
Hospitalization for PAH 6 (4%) 9 (13%) 0 (0%) 3 (27%)
Discontinuation due to worsening of PAH 5 (3%) 6 (9%) 0 (0%) 3 (27%)
Receipt of epoprostenol‡ 4 (3%) 3 (4%) 0 (0%) 3 (27%)

Time from randomization to clinical worsening with Kaplan-Meier estimate of the proportions of failures in BREATHE-1. All patients (N=144 in the bosentan group and N=69 in the placebo group) participated in the first 16 weeks of the study. A subset of this population (N=35 in the bosentan group and 13 in the placebo group) continued double-blind therapy for up to 28 weeks.

WHO Functional Class II

In a randomized, double-blind, multicenter, placebo-controlled trial, 185 mildly symptomatic PAH patients with WHO Functional Class II (mean baseline 6-minute walk distance of 443 meters) received bosentan 62.5 mg twice daily for 4 weeks followed by 125 mg twice daily (n = 93), or placebo (n = 92) for 6 months. Enrolled patients were treatment-naïve (n = 156) or on a stable dose of sildenafil (n = 29). The co-primary endpoints were change from baseline to month 6 in PVR and 6-minute walk distance. Time to clinical worsening (assessed as the sum of death, hospitalization due to PAH complications, or symptomatic progression of PAH), Borg dyspnea index, change in WHO functional class and hemodynamics were assessed as secondary endpoints.

Compared with placebo, bosentan treatment was associated with a reduced incidence of worsening of at least one functional class (3% bosentan vs. 13% placebo, p = 0.03), and improvement in hemodynamic variables (PVR, mPAP, TPR, cardiac index, and SVO2; p < 0.05). The + 19 m mean (+14 m median) increase in 6-minute walk distance with bosentan vs. placebo was not significant (p = 0.08). There was a significant delay in time to clinical worsening (first seen primarily as symptomatic progression of PAH) with bosentan compared with placebo (hazard ratio 0.2, p = 0.01). Findings were consistent in strata with or without treatment with sildenafil at baseline.

Long-term Treatment of PAH

Long-term follow-up of patients with Class III and IV PAH who were treated with Tracleer in open-label extensions of trials (N=235) showed that 93% and 84% of patients were still alive at 1 and 2 years, respectively, after the start of treatment. These uncontrolled observations do not allow comparison with a group not given Tracleer and cannot be used to determine the long-term effect of Tracleer on mortality.

Pulmonary Arterial Hypertension related to Congenital Systemic-to-Pulmonary Shunts

A small study with patients (n=54) with Eisenmenger physiology demonstrated effects of bosentan on exercise and safety that were similar to those seen in other trials in patients with PAH (WHO Group 1).

14.2 Lack of Benefit in Congestive Heart Failure

Tracleer is not effective in the treatment of congestive heart failure with left ventricular dysfunction. In a pair of studies, 1613 subjects with NYHA Class III-IV heart failure, left ventricular ejection fraction <35%, on diuretics, ACE inhibitor, and other therapies, were randomized to placebo or Tracleer (62.5 mg twice daily titrated as tolerated to 125 mg twice daily) and followed for up to 70 weeks. Use of Tracleer was associated with no benefit on patient global assessment (the primary end point) or mortality. However, hospitalizations for heart failure were more common during the first 4 to 8 weeks after bosentan was initiated. In a placebo-controlled trial of patients with severe chronic heart failure, there was an increased incidence of hospitalization for CHF associated with weight gain and increased leg edema during the first 4-8 weeks of treatment with Tracleer. Patients required intervention with a diuretic, fluid management, or hospitalization for decompensating heart failure.

16. HOW SUPPLIED/STORAGE AND HANDLING

62.5 mg film-coated, round, biconvex, orange-white tablets, embossed with identification marking "62,5", packaged in a white high-density polyethylene bottle and a white polypropylene child-resistant cap.

NDC 66215-101-06: Bottle containing 60 tablets.

125 mg film-coated, oval, biconvex, orange-white tablets, embossed with identification marking "125", packaged in a white high-density polyethylene bottle and a white polypropylene child-resistant cap.

NDC 66215-102-06: Bottle containing 60 tablets.

Store at 20°C – 25°C (68°F – 77°F). Excursions are permitted between 15°C and 30°C (59°F and 86°F). [See USP Controlled Room Temperature].

Manufactured for:

Actelion Pharmaceuticals US, Inc.

South San Francisco, CA 94080, USA

ACT20110210

17. PATIENT COUNSELING INFORMATION

Advise patients to consult the Medication Guide on the safe use of Tracleer [see Medication Guide (17.2)].

17.1 Important Information

  • Monthly monitoring of serum aminotransferases

The physician should discuss with the patient the importance of monthly monitoring of serum aminotransferases.

  • Pregnancy testing and avoidance of pregnancy

Patients should be advised that Tracleer is likely to cause birth defects based on animal studies. Tracleer treatment should only be initiated in females of childbearing potential following a negative pregnancy test. Females of childbearing potential must have monthly pregnancy tests and need to use two different forms of contraception while taking Tracleer and for one month after discontinuing Tracleer. Females who have a tubal ligation or a Copper T 380A IUD or LNg 20 IUS can use these contraceptive methods alone. Patients should be instructed to immediately contact their physician if they suspect they may be pregnant and should seek contraceptive advice from a gynecologist or similar expert as needed.

  • Drug Interactions

The physician should discuss with the patient possible drug interactions with Tracleer, and which medications should not be taken with Tracleer. The physician should discuss the importance of disclosing all concomitant or new medications.

17.2 Medication Guide

See accompanying Medication Guide

Medication Guide

Tracleer (tra-KLEER)
(bosentan)
Tablets

Read the Medication Guide that comes with Tracleer before you start taking it and each time you get a refill. There may be new information. This Medication Guide does not take the place of talking with your healthcare provider about your medical condition or your treatment.

What is the most important information I should know about Tracleer?

Tracleer is only available through the Tracleer Access Program (T.A.P.). Before you begin taking Tracleer, you must read and agree to all of the instructions in T.A.P.

Tracleer can cause serious side effects including:

Liver damage.

  • Liver damage may not cause symptoms at first. Only a blood test can show if you have early liver damage. You must have a blood test to check your liver function before you start Tracleer and each month after that. Your healthcare provider will order these tests. Regular blood tests are important because they will help your healthcare provider adjust or stop your treatment before there is permanent damage.
  • Tell your healthcare provider if you have had liver problems, including liver problems while taking other medicines. Call your healthcare provider right away if you have any of these symptoms of liver problems while taking Tracleer:
    • nausea
    • vomiting
    • fever
    • unusual tiredness
    • stomach area (abdominal) pain
    • yellowing of the skin or the whites of your eyes (jaundice)

Serious birth defects.

  • Tracleer can cause serious birth defects if taken during pregnancy. You must not be pregnant when you start taking Tracleer or during Tracleer treatment. Serious birth defects from Tracleer can happen early in pregnancy. Females who are able to get pregnant must have a negative pregnancy test before starting treatment and each month during Tracleer treatment.
  • Talk with your healthcare provider or gynecologist (a doctor who specializes in female reproduction) to find out about how to prevent pregnancy. Do not have unprotected sex. Tell your healthcare provider right away if you miss a menstrual period or think you may be pregnant.
  • Females who are able to get pregnant must use birth control (contraception) during Tracleer treatment. You must choose and use two reliable forms of birth control at the same time, unless you have had a tubal sterilization, or have a Copper T 380A IUD or LNg 20 IUS These methods can be used alone.

Talk with your healthcare provider about which 2 methods of reliable birth control you should use. Your healthcare provider may recommend that you use a different method of birth control to help lower your risk of problems with your pulmonary arterial hypertension. See the end of this Medication Guide for more information about reliable methods of contraception during treatment with Tracleer.

See "What are the possible side effects of Tracleer?" for more information about side effects.

What is Tracleer?

Tracleer is a prescription medicine used to treat people with certain types of pulmonary arterial hypertension (PAH), which is high blood pressure in the vessels of the lungs.

Tracleer can improve your ability to exercise and can slow the worsening of your physical condition and symptoms. Tracleer lowers high blood pressure in your lungs and lets your heart pump blood more efficiently.

Tracleer is only:

  • prescribed by healthcare providers who are enrolled in T.A.P.
  • available to people who understand and agree to enroll in T.A.P.

It is not known if Tracleer is safe and works in children below 12 years of age.

Who should not take Tracleer?

Do not take Tracleer if you:

  • are pregnant, plan to become pregnant, or become pregnant during Tracleer treatment. Tracleer can cause serious birth defects. All females should read the birth defects section of "What is the most important information I should know about Tracleer?"
  • have a blood test that shows possible liver injury.
  • take one of these medicines:
    • cyclosporine A used for psoriasis and rheumatoid arthritis, and to prevent rejection of heart or kidney transplants
    • glyburide used for diabetes
  • you are allergic to any of the ingredients in Tracleer. See the end of this Medication Guide for a list of the ingredients in Tracleer. If you have a rash, hives or your lips swell after taking Tracleer, it may be a sign of allergy. You should stop taking your Tracleer and talk to your healthcare provider.

What should I tell my healthcare provider before taking Tracleer?

Tracleer may not be right for you. Tell your healthcare provider about all your medical conditions, including if you:

  • have liver problems.
  • are breast-feeding or plan to breast feed. It is not known if Tracleer passes into your milk. You and your healthcare provider should decide if you will take Tracleer or breast-feed. You should not do both.
  • Tell your healthcare provider about all the medicines you take, including prescription and non-prescription medicines, vitamins, and herbal supplements. Tracleer and other medicines may affect how each other works and cause side effects. Especially tell your healthcare provider if you take:
    • hormone-based birth control, such as pills, shots, patches, and implants. These birth control methods may not work as well when taken with Tracleer.
    • simvastatin or other "-statin" medicines used to lower cholesterol
    • rifampin used for tuberculosis
    • tacrolimus used to prevent rejection of liver or kidney transplant
    • ketoconazole, fluconazole, itraconazole, or voriconazole used for fungal infections
    • warfarin sodium used to prevent blood clots
    • ritonavir used to treat HIV

There may be more than one brand name medicine. Ask your healthcare provider if you are not sure if your medicine is one that is listed above.

How should I take Tracleer?

Your healthcare provider will give you detailed information about T.A.P..

  • Tracleer will be mailed to you by a specialty pharmacy. You will only receive a 30-day supply of Tracleer at one time.
  • Take Tracleer exactly as prescribed.
  • Your healthcare provider will tell you how much Tracleer to take and when to take it.
  • In most cases, you will take 1 tablet in the morning and 1 in the evening.
  • You can take Tracleer with or without food.
  • If you take more than the prescribed dose of Tracleer, call your healthcare provider right away.
  • If you miss a dose of Tracleer, take your tablet as soon as you remember. Do not take 2 doses at the same time. If it is almost time for your next dose, skip the missed dose. Just take the next dose at your regular time.
  • Do not stop taking Tracleer unless your healthcare provider tells you to. Suddenly stopping your treatment may cause your symptoms to get worse. If you need to stop taking Tracleer, speak with your healthcare provider about the right way to stop.

What are the possible side effects of Tracleer?

Tracleer can cause serious side effects, including:

  • See "What is the most important information I should know about Tracleer?"
  • Fluid retention and swelling of your ankles and legs. Tracleer can cause your body to hold too much water, and you may get swelling of your ankles and legs. Tell your healthcare provider if you have swelling of your ankles and legs that happens either with or without weight gain, or if you have more trouble with your breathing than normal. Your healthcare provider will look for the cause of this.
  • Lower Sperm Count. Some men who take Tracleer may have lower sperm counts. This may affect your ability to father a child. Tell your healthcare provider if fertility is a concern for you.
  • Low red blood cell levels (anemia). Your healthcare provider will do blood tests to check your red blood cells during treatment with Tracleer.

The most common side effects of Tracleer are:

  • respiratory tract infection
  • headache
  • fainting
  • flushing
  • low blood pressure
  • inflamed nose passages (sinusitis)
  • joint pain
  • irregular heart beats

Tell your doctor if you have any side effect that bothers you or that does not go away. These are not all the possible side effects of Tracleer. For more information, ask your doctor 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 Tracleer?

  • Store Tracleer at 68°F to 77°F (20°C-25°C).
  • Keep Tracleer and all medicines out of the reach of children.

General information about Tracleer

Medicines are sometimes prescribed for purposes other than those listed in a Medication Guide. Do not use Tracleer for a condition for which it was not prescribed. Do not give Tracleer to other people, even if they have the same symptoms that you have. It may harm them.

This Medication Guide summarizes the most important information about Tracleer. If you would like more information, talk with your healthcare provider. You can ask your pharmacist or healthcare provider for information about Tracleer that is written for health professionals. For more information, go to www.TRACLEER.com or call 1-866-228-3546.

What are the ingredients in Tracleer?

Active ingredient: bosentan

Inactive ingredients: corn starch, pregelatinized starch, sodium starch glycolate, povidone, glyceryl behenate, magnesium stearate, hydroxypropylmethylcellulose, triacetin, talc, titanium dioxide, iron oxide yellow, iron oxide red, ethylcellulose.

Reliable methods of contraception during treatment with Tracleer
Methods to use alone Hormone
(choose 1 and use with a barrier method)
Barrier
(use both OR choose 1 and use with a hormone method)
  • Intrauterine devices (IUDs)
    Copper T 380A IUD
    LNg-20 IUS
    (progesterone IUD)
  • Tubal sterilization
  • Estrogen and progesterone
    Oral contraceptives
    Transdermal patch
    Vaginal ring
  • Progesterone only
    Injection
    Implant
  • Male condom with spermicide
  • Diaphragm with spermicide
    OR
    Cervical cap with spermicide
A partner's vasectomy still requires 1 additional method of contraception.

Distributed by:

Actelion Pharmaceuticals US, Inc.
South San Francisco, CA 94080, USA

ACT20090730

Revised August 2009

This Medication Guide has been approved by the U.S. Food and Drug Administration.

PRINCIPAL DISPLAY PANEL - 62.5 mg Bottle Carton

NDC 66215-101-06

Tracleer®
BOSENTAN
62.5 mg

Rx only
ACTELION

60 tablets

责任编辑:admin


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