主要目的：以石药集团中诺药业（石家庄）有限公司生产的阿普昔腾坦片为受试制剂，以Idorsia Pharmaceuticals ltd.持证的阿普昔腾坦片（商品名：TRYVIO™，规格：12.5 mg）为参比制剂，按生物等效性试验的相关规定，比较阿普昔腾坦片在健康参与者体内的药代动力学行为，评价空腹状态下两种制剂的生物等效性。次要目的：评价健康参与者单次口服阿普昔腾坦片受试制剂和参比制剂后的安全性。

开始日期2026-03-12

申办/合作机构

石药集团中诺药业（石家庄）有限公司

NCT06799884

/ Completed临床1期

A Single-center, Open-label, Fixed-sequence Trial to Investigate the Effect of Multiple-dose Aprocitentan on the Single-dose Pharmacokinetics of Combined Oral Contraceptives in Healthy Female Participants

The goal of this clinical trial is to learn if drug aprocitentan has an effect on hormonal contraceptives in healthy female volunteers. The main question it aims to answer is:
Does aprocitentan modify the fate of hormonal contraceptives in the body?
Trial participants will:
* Take a single dose of hormonal contraceptives (fixed combination) alone
* Take aprocitentan every day for 2 weeks
* Take a single dose of the same hormonal contraceptives at the same time as the 10th administration of aprocitentan.

开始日期2025-01-18

申办/合作机构

Idorsia Pharmaceuticals Ltd.

NCT05196399

/ Completed临床1期

A Single-center, Open-label, Randomized, Two-way Crossover Phase 1 Study to Compare the Single-dose Pharmacokinetics of Different Tablet Formulations of Aprocitentan in Healthy Subjects

The main purpose is to study the pharmacokinetics of aprocitentan (ACT-132577) using 2 different tablet formulations. The clinical pharmacology data will be used to determine bioequivalence of 2 different tablet formulations.

开始日期2022-02-02

申办/合作机构

Idorsia Pharmaceuticals Ltd.

100 项与阿普昔腾坦相关的临床结果

登录后查看更多信息

100 项与阿普昔腾坦相关的转化医学

登录后查看更多信息

100 项与阿普昔腾坦相关的专利（医药）

登录后查看更多信息

项与阿普昔腾坦相关的文献（医药）

2026-03-01·JOURNAL OF PEDIATRICS

Macitentan vs Standard of Care in Pediatric Pulmonary Arterial Hypertension (TOMORROW): A Randomized Clinical Trial

Article

作者: Ivy, D Dunbar ; Borissoff, Julian I ; Cerovic, Sofija ; Csonka, Dénes ; Beghetti, Maurice ; Berger, Rolf M F ; Remeňová, Tatiana ; Villeneuve, Matthieu ; Richard, Dominik

OBJECTIVES:

To evaluate pharmacokinetics (PK), efficacy, and safety of macitentan vs standard of care (SoC) in pediatric pulmonary arterial hypertension (PAH).

STUDY DESIGN:

TOMORROW was a multi-center, open-label, phase 3 clinical trial in patients aged ≥2-<18 years with WHO-FC I-III. Patients were randomized (1:1) to macitentan (bodyweight-based dosing) or SoC (≤2 PAH-specific therapies). The primary endpoint was steady-state C_trough plasma concentration of macitentan and aprocitentan (active metabolite) at week 12. Secondary endpoints included: time-to-first clinical event committee (CEC)-confirmed disease progression, safety/tolerability, change in NT-proBNP, and quality of life (QoL).

RESULTS:

We randomized 148 patients (macitentan: n=73; SoC: n=75). The PK profile was consistent with adults; mean (SD) steady-state C_trough concentrations were 185 (114.3) and 983 (324.1) ng/mL. Mean treatment duration was 183.36 weeks (macitentan) and 130.59 weeks (SoC). Hazard ratios (95% CI) for time-to-event analyses (macitentan vs SoC) were 0.828 (0.460-1.492) for disease progression, 0.912 (0.393-2.118) for PAH hospitalization and 1.530 (0.429-5.457) for PAH mortality (P>0.05 for all). Percentage of baseline NT-proBNP was 72% (macitentan) vs 101% (SoC) at week 12 (P=0.086) and 76% vs 78% at week 24 (P=0.884). Macitentan showed clinically meaningful improvements in QoL assessments vs SoC for children (P=0.043) and parents (P=0.020) at week 24. The safety profile of macitentan was consistent with that seen in adults.

CONCLUSIONS:

TOMORROW was a novel study assessing PK and the long-term efficacy and safety of macitentan vs SoC in pediatric PAH. The results confirm the adequacy of the macitentan dosing in this population and provided signals of potential benefit of macitentan over SoC for children with PAH.

2026-03-01·Pregnancy Hypertension-An International Journal of Womens Cardiovascular Health

Placental transfer of the novel endothelin-1 receptor antagonist aprocitentan

Article

作者: Kluivers, Anna C M ; Tan, Lunbo ; Danser, A H Jan ; van der Meeren, Lotte E ; Delahaye, Stephane ; Harhangi, Madhavi S ; Broekhuizen, Michelle

RATIONALE:

The vasoconstrictor endothelin-1 is elevated in preeclampsia, making endothelin receptor antagonists (ERAs) a logical therapeutic strategy. Here we evaluated the placental transfer of the novel ERA aprocitentan, which has recently been approved for hypertension treatment.

MATERIALS AND METHODS:

Dual-sided placental cotyledon perfusion was used to study transfer of aprocitentan, added maternally at a clinically relevant concentration of 150 ng/mL. Subsequently, these placentas were fetally exposed to endothelin-1. Antipyrine, which freely transfers to the fetal compartment, and fluorescein isothiocyanate [FITC]-dextran, which does not transfer, were used as comparator substances.

RESULTS:

After 3 h of perfusion, the fetal-to-maternal ratio for total (free + protein-bound) aprocitentan was 0.25 ± 0.04, while for free aprocitentan it was 0.42 ± 0.08. The fetal aprocitentan concentrations were too low to block the contractile effects of endothelin-1 in the fetal compartment, although experiments in isolated chorionic plate arteries confirmed that aprocitentan can block these effects when given at higher concentrations. After perfusion, 50-60% of aprocitentan was recovered in the maternal and fetal fluid compartments. Around 20-30% was present in tissue, as intact aprocitentan or as its hydrolysis product ACT-080803. Since the recovery of maternally applied antipyrine and FITC-dextran was 85-90%, while fetally applied FITC-dextran was fully recovered, the missing 10-15% is likely present in the intervillous space.

DISCUSSION:

Aprocitentan transfers across the human placental barrier, although its fetal levels following maternal application of 150 ng/mL were insufficient to block endothelin-1. Drug studies in isolated cotyledons should consider the intervillous space when calculating recovery.

2026-02-01·HYPERTENSION

Aprocitentan in Patients With Chronic Kidney Disease and Resistant Hypertension

Article

作者: Mann, Johannes ; Wang, Ji-Guang ; Sassi-Sayadi, Mouna ; Rossignol, Patrick ; Flamion, Bruno ; Flack, John M. ; Weber, Michael A. ; Schlaich, Markus P. ; Clozel, Martine ; Dreier, Roland F. ; Narkiewicz, Krzysztof

BACKGROUND::

Hypertension is a cause and consequence of chronic kidney disease (CKD). Resistant hypertension is common and often difficult to control in patients with CKD. This post hoc analysis evaluated the efficacy and safety of aprocitentan (with standardized background antihypertensive therapy) in patients with CKD and resistant hypertension, a group with high morbidity and mortality risk and limited treatment options.

METHODS::

The PRECISION study (Parallel-Group, Phase 3 Study With Aprocitentan in Subjects With Resistant Hypertension) consisted of part 1: 4-week, double-blind (aprocitentan 12.5 and 25 mg versus placebo); part 2: 32-week, single-blind (aprocitentan 25 mg); and part 3: 12-week, double-blind withdrawal (aprocitentan 25 mg versus placebo). In participants with CKD, aprocitentan’s effect on blood pressure (BP), urine albumin-to-creatinine ratio, and safety was evaluated.

RESULTS::

Of 730 participants in PRECISION, 147 had CKD categorized as KDIGO high risk or very high risk. At week 4, aprocitentan 12.5 mg, aprocitentan 25 mg, and placebo reduced office systolic BP by −13.5, −16.6, and −4.4 mm Hg, respectively; this was maintained with aprocitentan 25 mg to week 36 (−16.4 mm Hg). At week 4, reductions in nighttime ambulatory systolic BP were −9.6, −13.8, and −2.5 mm Hg, respectively. Changes in urine albumin-to-creatinine ratio were −47.1%, −59.6%, and −2.4%, respectively, maintained with aprocitentan 25 mg to week 36 (−61.6%). Aprocitentan was generally well tolerated (no change in potassium or estimated glomerular filtration rate); early peripheral edema was the most common adverse event.

CONCLUSIONS::

Aprocitentan was well tolerated; efficiently lowered BP, particularly nighttime ambulatory BP; and markedly reduced urine albumin-to-creatinine ratio in participants with CKD and resistant hypertension. Aprocitentan may confer considerable cardiovascular and kidney-protective benefits in these difficult-to-treat patients.

REGISTRATION::

URL: https://www.clinicaltrials.gov ; Unique identifier: NCT03541174.

180

项与阿普昔腾坦相关的新闻（医药）

2026-04-28

·中华老年心脑血管病杂志

述评 | 高血压防治及个体化管理的新进展

高血压防治及个体化管理的新进展作者: 王运红，蔡军正文：近年来，高血压领域的循证医学证据持续更新，一系列高质量随机对照试验和创新技术的应用正在重塑对血压管理的认识。从控制血压到改善心血管预后，从长期服药到长效干预，从被动管理到促进主动健康，再到远程监测及人工智能驱动的个体化决策，尤其是老年高血压的个体化管理，高血压领域将迎来防治模式的变革。现结合最新发布的多项重要研究，系统评述当前高血压诊疗的核心进展。 1 强化降压从争议走向共识长期以来，“强化降压是否获益，以及强化降压的靶目标”始终是研究的焦点和热点，SPRINT、STEP和ESPRIT等研究表明，强化降压显著降低心血管事件风险[1-3]。本团队的STEP研究（老年高血压患者血压干预策略）结果显示，相较于收缩压控制目标130~150mmHg（1mmHg=0.133kPa），收缩压目标设为110~130mmHg可显著降低既往未发生过脑卒中的60~80岁的中国高血压患者心血管事件风险[2]。继主研究结束后，所有存活的患者都接受了强化降压治疗，形成“持续强化治疗”与“延迟强化治疗”的对比，延长随访阶段（至2023年7月），中位随访时间为6.11年，持续强化治疗组的复合心血管事件风险降低18%，其中，脑卒中风险下降最显著达28%[4]。此外，BPROAD研究发现，年龄≥50岁合并收缩压升高的糖尿病患者，强化降压（控制收缩压<120mmHg）使主要终点事件风险降低21%[5]。 2025年公布的BPRULE研究整合了6项具有里程碑意义的随机对照试验，即ACCORD-BP、SPRINT、ESPRIT、BPROAD、STEP和CRHCP研究，共纳入8万余例患者，结果显示，强化降压无论将收缩压目标设定在<130mmHg或<120mmHg，心血管复合终点风险下降24%，虽不良事件绝对风险增加1.82%，但净获益仍达1.14，强化降压总体利大于弊[6]。因此，对于具备一定耐受能力的高危患者，更严格的血压控制是改善长期预后的关键策略。目前，降压的下限值仍是悬而未决的问题，暂时无循证医学证据。2024年欧洲心脏病学会《血压升高和高血压管理指南》推荐降压目标范围为120~129/70~79mmHg，包括老年及衰弱人群，但重点指出，对于特别高龄（≥85岁）且衰弱的人群，个体化决策应放在第一位考量[7]。《老年高血压特点及临床诊治流程专家共识》（2024）对于衰弱合并血压≥160/90mmHg的老年人，建议个体化制定血压目标值，但收缩压尽量不低于130mmHg[8]。对于舒张压<60mmHg的高危和非高危老年单纯收缩期高血压患者的收缩压低限都应在120mmHg以上,舒张压尽可能不低于50mmHg[8]。就血压管理的复杂性，降压靶目标建议遵循个体化决策，“个体化强化”而非“一刀切强化”应成为强化降压的整体理念。 2 高血压领域新药研发不断突破近年来，新型靶向药物的涌现标志着高血压治疗进入“精准靶向”时代。最有潜力的靶点之一为肾素-血管紧张素-醛固酮系统的最下游分子-醛固酮。2025年美国心脏病协会（AmericanHeartAssociation，AHA）公布的BREAKTHROUGH研究分析了真实世界数据，结果显示，39.5%的原发性高血压患者存在醛固酮失调，醛固酮失调患者未控制高血压的风险比显著增加至1.41。既往醛固酮受体拮抗剂类药物被推荐作为难治性高血压的第四种药物选择[9-10]。但醛固酮受体拮抗剂类药物仅通过阻断醛固酮受体的途径，不能充分抑制醛固酮介导高血压的发病机制，因此，直接抑制醛固酮合成的药物备受关注。目前，研究较多的两个醛固酮合酶抑制剂为Lorundrostat和Baxdrostat。针对Lorundrostat开展的两项Ⅱ期研究Target-HTN、Advance-HTN，以及Ⅲ期Launch-HTN研究，均显示其可显著降低难治性高血压患者的收缩压水平[11-13]。Ⅲ期研究显示，第6周时Lorundrostat50mg组降低收缩压达-16.9mmHg，显著优于安慰剂组的-7.9mmHg[13]。BaxdrostatⅢ期研究BaxHTN显示，在未控制/难治性高血压患者中，2mg剂量组经安慰剂校正后收缩压净降幅达9.8mmHg[14]。内皮素双受体拮抗剂Aprocitentan于2024年3月被美国食品与药物管理局批准用于治疗高血压。尽管其Ⅲ期试验中的收缩压降低幅度为4~6mmHg，但因其不升高血钾且不影响肾功能，成为难治性高血压的一种选择[15]。另一个非常值得关注的靶点是肾素-血管紧张素-醛固酮系统的上游分子-血管紧张素原。目前，针对该靶点的新型长效制剂Zilebesiran为一种小干扰RNA疗法，该药通过沉默肝脏血管紧张素原基因表达，单次皮下注射即可维持长达6个月的降压效应[16]。KARDIA-1研究显示，在不服药的轻中度高血压人群中，Zilebesiran不同剂量组与安慰剂组比较，3个月收缩压显著下降达14.1~16.7mmHg[17]。但2025年欧洲心脏病学会大会公布的KARDIA-3研究纳入的未控制或难治性高血压人群中，其总降压幅度相对较小（与安慰剂组比较收缩压降低3.3~5mmHg），未达主要终点。不过亚组分析显示，Zilebesiran联用利尿剂时具有较强的降压效果，在第三个月时安慰剂校正的收缩压降幅高达9.2mmHg，第六个月时降低8.3mmHg，为后续以心血管结局事件为终点的Ⅲ期ZENITH试验的设计提供了重要依据。国内已经有企业开展同类药物的研发，有望为我国众多高血压患者提供更经济的长效降压药物，提升患者治疗依从性。新型的降糖药物在降压方面也初见成效。SURMOUNT-OSAⅢ期研究显示，新型胰高血糖素样肽（glucagon-likepeptide，GLP）-1/GIP双受体激动剂替尔泊肽在肥胖合并中重度阻塞性睡眠呼吸暂停综合征患者中可降低收缩压3.7~7.6mmHg[18]。近期一项荟萃分析汇总三项随机对照研究显示，GLP-1受体激动剂司美格鲁肽用于肥胖患者，可降低收缩压接近5mmHg，而收缩压每降低5mmHg对心血管事件的风险降低是显著的[19]。 3 低剂量多重药物联合降压方案未来有望推广因高血压发病机制复杂，单一个体的高血压并不局限于单一通路的异常调节机制。多药联合的理念不断深化，逐步向“起始即联合用药”迈进[9]。新近发表的TOPSPIN试验证实，氨氯地平+培哚普利、氨氯地平+吲达帕胺、培哚普利+吲达帕胺三种双联方案，启动6个月后24h平均收缩压较基线下降约14mmHg，约70%患者达标（<140/90mmHg）[20]。关于三药组合制剂（由替米沙坦、氨氯地平和吲达帕胺组成）降压疗效的研究同样显示，三药全剂量、半剂量甚或四分之一剂量，较任意两种药物组合，6个月时家庭平均收缩压降低最高达5.8mmHg[21-22]。2024年欧洲心脏病学会大会上公布的QUADROⅢ期研究显示，四联疗法（培哚普利/吲达帕胺/氨氯地平/比索洛尔）治疗难治性高血压，相较于三联方案，诊室收缩压额外降低8.04mmHg，24h动态收缩压下降7.53mmHg。由不同低剂量的降压药组成的复方制剂可改善血压，主要由于其具有叠加效应且不良反应低，提升了高血压患者的治疗依从性。 4 低钠代盐获得国内外指南推荐生活方式干预是贯穿血压管理的重要措施，包括高血压的一级预防。2025年高血压管理指南提出了“预防高血压发生”的理念，收缩压≥120mmHg或舒张压≥80mmHg会导致不可逆的血管损伤和残余风险，高血压患者即使治疗后血压低于120/80mmHg，心血管疾病风险也是正常血压人群的2倍[23]。低钠代盐将是实现这一关口前移策略较为可行的防治手段。 DECIDE-Salt研究显示，在血压正常老年人中使用低钠盐替代普通食盐，可使高血压发病率降低40%，收缩压平均下降8.0mmHg[24]。该研究入选的是养老院中的老年人，尽管老年人肾功能有一定程度的生理性下降，低钠高钾盐仍安全有效，因此有望推广至更广泛的人群，延缓血压的增龄性增长。因此，2024年《中国高血压临床实践指南》和2025年AHA/ACC高血压管理指南均将低钠代盐进行了较高类别的推荐（ⅠB、2a类）[9，23]。 5 高血压领域迎来器械治疗的新时代随着器械改进、术式更新、患者筛选策略的优化，对于药物难以控制的高血压，肾去交感神经术（renaldenervation，RDN）具有长效持久降压的作用。2025年美国经导管心血管治疗学大会公布了3项研究数据：SPYRALHTN-ONMED研究3年随访数据显示，治疗后患者血压达标率显著提升，与假手术组相比，RDN组患者24h动态收缩压下降4.7mmHg，诊室收缩压下降7.4mmHg；全球Paradise系统注册研究数据分析显示，超声RDN治疗6个月后诊室收缩压平均下降19.6mmHg；RADIANCE汇总分析RecorRADIANCE全球三项研究共243例患者、随访至24个月的数据，包括难治性高血压患者以及轻中度高血压患者，结果显示，24个月时诊室收缩压仍维持15.7mmHg的降幅。基于RDN的显著降压效果，美国已经将该技术纳入医保系统。但鉴于既往研究均将高龄人群排除在外，且老年人交感神经兴奋性较低，目前，RDN暂时不适合用于高龄及动脉硬化较重的老年人。随着对交感神经在高血压发病机制中的探索发现，沿肝总动脉的交感神经密度高于肾动脉，肝肾动脉联合去神经术能更有效地减少交感神经输出，产生协同降压作用。2025年5月欧洲冠脉介入大会上公布的SPYRALGEMINI探索性临床试验与临床前动物模型研究，显示实施肝肾联合交感神经消融，去甲肾上腺素水平下降近90%，远超单纯肾动脉消融效果。RDN技术未来可能迈向多器官神经联合消融的时代。针对继发性高血压中较常见的病因即原发性醛固酮增多症，传统的治疗方法主要是使用醛固酮受体拮抗剂药物和手术切除整个肾上腺。近期英国研究人员报道了通过内镜超声引导射频消融术治疗左侧肾上腺腺瘤的术式，选择性地破坏小的肾上腺结节而不切除肾上腺，这种微创方法只需20min，概念验证研究纳入了28例受试者，显示术后3个月21例患者实现了部分或完全生化治愈，43%患者实现了部分或完全临床治愈，为原发性醛固酮增多症提供了新治疗选择[25]。 6 血压管理应该关注老龄和衰弱群体随着人口老龄化，更加强调对老年、衰弱等特殊群体进行个体化降压管理。通常临床研究将老年和衰弱群体排除在外，尤其对80岁以上的老年人。新近RETREAT-FRAIL研究在≥80岁养老院居民中发现，在血压已控制良好（<130mmHg）且多药治疗背景下，逐步减药既不减少也不增加全因死亡，不良事件风险亦无升高，提示对高龄虚弱患者应权衡药物负担与获益，必要的减药方案在不增加不良事件的情况下是可行的[26]。但若老年患者耐受良好，即使年龄超过85岁也建议终身维持降压药物治疗[7]。因老年人更容易发生体位性低血压和心动过缓，β受体阻滞剂、α受体阻滞剂、直接血管扩张剂因易增加上述不良反应，应谨慎选用[7]。老年人常合并衰弱，ESPRIT预设研究分析显示，无论虚弱程度如何，强化降压治疗（收缩压<120mmHg）预防主要不良心血管事件和全因死亡的作用是一致的，但强化降压可使肾脏功能损害的风险增加[27]。 7 血压管理在智能化基础上应兼顾老年人在基层医疗机构电子系统中嵌入临床决策支持系统后，干预组中接受适当治疗的就诊比例高于对照组（77.8%vs62.2%），血压控制率提升了4.4%，收缩压额外降低1.5mmHg，尽管并没有达到降压的显著性差异，但在基层医疗单位，辅助决策管理高血压仍是可考虑的低成本方式[28]。IMPACT-BP研究则证明，在资源匮乏地区，通过社区健康工作者+移动应用远程决策的模式，无论是否有自动上传血压数据，6个月平均收缩压下降7.9~9.1mmHg，均可使血压控制率从57.6%提升至76.9%~82.8%，采用远程护理模式可改善高血压控制率[29]。 2025年AHA大会上公布的本团队的“健康家庭计划”研究，是一项在河南省汝阳县各村镇开展的多中心、开放标签、整群随机对照试验。研究显示，通过家庭负责人、村庄健康指导员和村医共同建立血压管理团队，基于预设算法的血压监测方案，结合多元化综合干预措施，与对照组比较，干预组6个月时收缩压平均降低10.7mmHg。尽管该研究并非针对老年高血压人口设计，但老年人更加需要家庭成员及社会力量的帮助，有组织的“健康家庭血压计划”将有助于为该群体提供个体化的血压管理支持。 8 总结高血压研究领域的新进展具有三大趋势。首先，未来降压治疗目标更加积极，对于高危患者应该更积极地达到强化降压的靶目标，但对老年人的降压管理仍应个体化，且亟需更多随机对照试验证据。其次，治疗手段更加多元化，形成新型靶向药物、长效制剂、多联单片复方制剂、器械治疗的多层次干预体系。最后，高血压管理模式将更加智能，从“被动治疗”转向“主动预防”。未来的高血压管理，将是“精准评估—靶向干预—智能管理”三位一体的综合体系，并重点关注老年高血压群体。利益冲突所有作者均声明不存在利益冲突参考文献 [1] SPRINT Research Group, Wright JT Jr, Williamson JD, et al. A randomized trial of intensive versus standard blood-pressure control[J]. N Engl J Med, 2015, 373(22):2103-2116. DOI:10.1056/NEJMoa1511939. [2] Zhang W, Zhang S, Deng Y, et al. Trial of intensive blood-pressure control in older patients with hypertension[J]. N Engl J Med, 2021, 385(14):1268-1279. DOI:10.1056/NEJMoa2111437. [3] Liu J, Li Y, Ge J, et al. Lowering systolic blood pressure to less than 120 mmHg versus less than 140 mmHg in patients with high cardiovascular risk with and without diabetes or previous stroke: an open-label, blinded-outcome, randomised trial[J]. Lancet, 2024, 404(10449):245-255. DOI:10.1016/S0140-6736(24)01028-6. [4] Song Q, Peng X, Bai J, et al. Intensive blood pressure control in older patients with hypertension:6-year results of the STEP trial[J]. J Am Coll Cardiol, 2025, 86(17):1421-1433. DOI:10.1016/j.jacc.2025. 06.045. [5] Bi Y, Li M, Liu Y, et al. Intensive blood-pressure control in patients with type 2 diabetes[J]. N Engl J Med, 2025, 392(12):1155- 1167. DOI:10.1056/NEJMoa2412006. [6] Guo X, Sun G, Xu Y, et al. Benefit-harm trade-offs of intensive blood pressure control versus standard blood pressure control on cardiovascular and renal outcomes:an individual participant data analysis of randomised controlled trials[J]. Lancet, 2025, 406(10507):1009- 1019. DOI:10.1016/S0140-6736(25)01391-1. [7] McEvoy JW, McCarthy CP, Bruno RM, et al. 2024 ESC Guidelines for the management of elevated blood pressure and hypertension[J]. Eur Heart J, 2024, 45(38):3912-4018. DOI:10.1093/eurheartj/ ehae178. [8] 中华医学会老年医学分会，中国医疗保健国际交流促进会高血压病分会.老年高血压特点及临床诊治流程专家共识(2024)[J]. 中华老年医学杂志，2024，43(3):257-268. DOI:10.3760/cma. j.issn.0254-9026.2024.03.001. [9] 中华医学会心血管病学分会，海峡两岸医药卫生交流协会高血压专业委员会，中国康复医学会心血管疾病预防与康复专业委员会.中国高血压临床实践指南[J]. 中华心血管病杂志，2024， 52(9):985-1032. DOI:10.3760/cma.j.cn112148-20240709-00377. [10] Uchida HA, Wada J, Motoki H, et al. Efficacy and safety of esaxerenone in hypertensive patients with chronic kidney disease, with or without type 2 diabetes mellitus:a pooled analysis of five clinical studies[J]. Hypertens Res, 2025, 48(9):2413-2426. DOI:10.1038/ s41440-025-02259-z. [11] Laffin LJ, Rodman D, Luther JM, et al. Aldosterone synthase inhibition with lorundrostat for uncontrolled hypertension:the target-HTN randomized clinical trial[J]. JAMA, 2023, 330(12):1140-1150. DOI:10.1001/jama.2023.16029. [12] Laffin LJ, Kopjar B, Melgaard C, et al. Lorundrostat efficacy and safety in patients with uncontrolled hypertension[J]. N Engl J Med, 2025, 392(18):1813-1823. DOI:10.1056/NEJMoa2501440. [13] Saxena M, Laffin L, Borghi C, et al. Lorundrostat in participants with uncontrolled hypertension and treatment-resistant hypertension:the launch-HTN randomized clinical trial[J]. JAMA, 2025, 334(5):409- 418. DOI:10.1001/jama.2025.9413. [14] Flack JM, Azizi M, Brown JM, et al. Efficacy and safety of Baxdrostat in uncontrolled and resistant hypertension[J]. N Engl J Med, 2025, 393(14):1363-1374. DOI:10.1056/NEJMoa2507109. [15] Schlaich MP, Bellet M, Weber MA, et al. Dual endothelin antagonist aprocitentan for resistant hypertension (PRECISION):a multicentre, blinded, randomised, parallel-group, phase 3 trial[J]. Lancet, 2022, 400(10367):1927-1937. DOI:10.1016/S0140-6736(22)02034-7. [16] Desai AS, Webb DJ, Taubel J, et al. Zilebesiran, an RNA interference therapeutic agent for hypertension[J]. N Engl J Med, 2023, 389(3): 228-238. DOI:10.1056/NEJMoa2208391. [17] Bakris GL, Saxena M, Gupta A, et al. RNA interference with zilebesiran for mild to moderate hypertension:the KARDIA-1 randomized clinical trial[J]. JAMA, 2024, 331(9):740-749. DOI:10.1001/jama.2024.0728. [18] Malhotra A, Grunstein RR, Fietze I, et al. Tirzepatide for the treatment of obstructive sleep apnea and obesity[J]. N Engl J Med, 2024, 391(13):1193-1205. DOI:10.1056/NEJMoa2404881. [19] Rajagopalan S, Brook RD, Münzel T. Environmental hypertensionology and the mosaic theory of hypertension[J]. Hypertension, 2025, 82(4):561-572. DOI:10.1161/HYPERTENSIONAHA.124.18733. [20] Prabhakaran D, Roy A, Chandrasekaran AM, et al. Comparison of dual therapies for hypertension treatment in India:a randomized clinical trial[J]. Nat Med, 2025, 31(9):3169-3175. DOI:10.1038/ s41591-025-03854-w. [21] Rodgers A, Salam A, Schutte AE, et al. Efficacy and safety of a novel low-dose triple single-pill combination of telmisartan, amlodipine and indapamide, compared with dual combinations for treatment of hypertension:a randomised, double-blind, active-controlled, international clinical trial[J]. Lancet, 2024, 404(10462):1536- 1546. DOI:10.1016/S0140-6736(24)01744-6. [22] Ojji DB, Salam A, Sani MU, et al. Low-dose triple-pill vs standard-care protocols for hypertension treatment in Nigeria:a randomized clinical trial[J]. JAMA, 2024, 332(13):1070- 1079. DOI:10.1001/jama.2024.18080. [23] Jones DW, Ferdinand KC, Taler SJ, et al. 2025 AHA/ACC/AANP/AAPA/ABC/ACCP/ACPM/AGS/AMA/ASPC/NMA/PCNA/ SGIM guideline for the prevention, detection, evaluation and management of high blood pressure in adults:a report of the American College of Cardiology/American Heart Association Joint Committee on Clinical Practice Guidelines[J]. Circulation, 2025, 152(11):e114-e218. DOI:10.1161/CIR.0000000000001356. [24] Zhang X, Yuan Y, Li C, et al. Effect of a salt substitute on incidence of hypertension and hypotension among normotensive adults[J]. J Am Coll Cardiol, 2024, 83(7):711-722. DOI:10.1016/ j.jacc.2023.12.013. [25] Argentesi G, Wu X, Ney A, et al. Endoscopic, ultrasound-guided, radiofrequency ablation of aldosterone-producing adenomas (FABULAS):a UK, multicentre, prospective, proof-of-concept trial[J]. Lancet, 2025, 405(10479):637-647. DOI:10.1016/S0140-6736(24) 02755-7. [26] Benetos A, Gautier S, Freminet A, et al. Reduction of antihypertensive treatment in nursing home residents[J]. N Engl J Med, 2025, 393(20):1990-2000. DOI:10.1056/NEJMoa2508157. [27] Li S, Peng Y, Li Y, et al. Effects of intensive blood pressure control in patients with frailty:a post hoc analysis from ESPRIT[J]. J Am Coll Cardiol, 2026, 87(1):4-16. DOI:10.1016/j.jacc.2025.08.092. [28] Song J, Wang X, Wang B, et al. Learning implementation of a guideline based decision support system to improve hypertension treatment in primary care in China:pragmatic cluster randomised controlled trial[J]. BMJ, 2024, 386:e079143. DOI:10.1136/bmj-2023-079143. [29] Siedner MJ, Magula N, Mazibuko L, et al. Home-based care for hypertension in Rural South Africa[J]. N Engl J Med, 2025, 393(13): 1304-1314. DOI:10.1056/NEJMoa2509958. （中华老年心脑血管病杂志 2026 年4月第28卷第4期） END 中华老年心脑血管病杂志扫码关注我们 HISTORY / 往期推荐述评 | 血管衰老临床评估与干预概述述评 | 卒中后认知障碍的预测因素是早诊早治的关键急性冠状动脉综合征的最新研究进展与未来展望老年神经疾病精准治疗与功能评估

2026-04-28

·BioSpace

Idorsia reports strong Q1 2026 performance with 74% QUVIVIQ sales growth year-on-year

Ad hoc announcement pursuant to Art. 53 LR Preparation is underway to publish the strong pediatric daridorexant data and engage with regulatory authorities on next steps Co-promotion of QUVIVIQ is being expanded across additional European markets to further accelerate growth Partnering discussions for TRYVIO™/JERAYGO™ are ongoing with several parties Allschwil, Switzerland – April 28, 2026 Idorsia Ltd (SIX: IDIA), a commercial-stage biopharmaceutical company with a portfolio of first- or best-in-class assets, today announced its financial results for the first quarter of 2026. Jean-Paul Clozel, Chairman and interim CEO of Idorsia, commented: “We have made a strong start to 2026. QUVIVIQ sales are tracking in line with our expectations, our pipeline is advancing, and we have delivered excellent results with daridorexant in children. Our focus is now firmly on executing the actions that will accelerate growth and unlock Idorsia’s full value. Building on the solid foundation established by our commercial team, we are working to further change the sales trajectory and accelerate growth, generating the cash flow required to continue advancing our breakthrough portfolio.” QUVIVIQ ® (daridorexant) QUVIVIQ continues to reshape the insomnia treatment landscape, and Idorsia is investing to accelerate its trajectory toward blockbuster status. Net sales increased 74% to CHF 44 million in Q1 2026 (Q1 2025: CHF 25 million) across North America and Europe. QUVIVIQ is now available in 13 countries across Europe, North America, China, and Japan, reflecting the continued global expansion of the franchise. Further market introductions are planned in Benelux, Ireland, Norway, Denmark, and Central and Eastern Europe, complemented by new strategic commercial alliances, most recently in Latin America, United Arab Emirates, Kuwait, Qatar, Oman, and Bahrain, to extend geographic reach and scale. QUVIVIQ has secured public reimbursement in key European markets, including France, Germany, the United Kingdom, and Austria. Efforts to further expand reimbursed access are ongoing, with active discussions in Spain – the largest insomnia market in Europe – and in the Nordics. In the United States, QUVIVIQ benefits from broad insurance coverage, although the current scheduled status continues to limit prescribing; the descheduling process for the DORA class remains ongoing. In Europe and Canada, Idorsia promotes QUVIVIQ to specialist prescribers, supported by co-promotion partnerships extending to primary care. Following partnerships in France in 2024 and Germany in 2025, co-promotions in the United Kingdom and Switzerland were launched in the first quarter of 2026. Additional co-promotion agreements are planned to further expand reach into primary care. Further sales acceleration is expected to be driven by increased private market awareness, including a strengthened presence in rapidly growing online prescription channels, alongside scalable direct-to-patient and adherence-focused initiatives designed to improve patient access. In parallel, Idorsia’s medical teams continue to generate additional clinical evidence, with ongoing studies in real‑world settings and in patients with co‑morbidities, including depression and anxiety, COMISA, major depressive disorder, alcohol and opioid use disorder, smoking cessation, and Alzheimer’s disease, reinforcing QUVIVIQ’s differentiated pro a broad range of patient populations. Daridorexant in pediatrics Outstanding Phase 2 results in children: statistically significant dose-dependent response on total sleep time with clinically meaningful improvements across multiple sleep measures in children with insomnia disorder, with especially pronounced efficacy in those with co-morbid neurodevelopmental disorders. Excellent safety and tolerability, confirmed for the first time in a pediatric population, including at the adult‑recommended 50 mg dose. Full analysis is ongoing with scientific publications and discussions with health authorities in preparation. TRYVIO™ / JERAYGO™ (aprocitentan) Growing base of HCP advocates across nephrology, cardiology, and internal medicine, with increasing uptake in leading academic centers and hypertension centers of excellence. On-market use is generating evidence that supports TRYVIO’s unique clinical profile, addressing a major unmet medical need by achieving meaningful reductions in both blood pressure and UACR in patients who previously could not reach treatment goals. New analyses of the PRECISION study to be presented by Prof. Markus Schlaich at the 35th Congress of the European Society of Hypertension on May 29, 2026. The oral presentation is entitled "Effect of the Dual Endothelin Receptor Antagonist Aprocitentan on Albuminuria". Idorsia’s CSO, Martine Clozel, will also speak at the event with a presentation entitled “From dream to reality: improving lives though endothelin-related innovations”. Ongoing partnering discussions to maximize the global value of TRYVIO/JERAYGO with several parties. Research & Development On track to initiate the Phase 3 program with lucerastat – potentially the first oral therapy for all patients with Fabry disease – in mid‑2026, with a potential regulatory filing as early as 2029. First-in-class, oral, selective CCR6 receptor antagonist for effective treatment of CCR6- and Th17-associated autoimmune indications. Proof‑of‑concept study in psoriasis is fully enrolled ahead of schedule – results now expected in Q4 2026. First-in-class, oral, CXCR7 (ACKR3) receptor antagonist, tailored to reduce central nervous system inflammation and promote remyelination through a dual mechanism of action. Proof‑of‑concept study in multiple sclerosis initiated in Q1 2026. First-in-class, oral, CXCR3 receptor antagonist with unique dual targeting of CD8+ CXCR3+ T cells offers potential for effective and safer treatment of immuno-dermatology and autoimmune disorders. Proof‑of‑concept study in vitiligo on track to initiating in Q2 2026. Daridorexant daytime functioning (IDSIQ) label‑enabling study in consultation with the US FDA. Idorsia’s synthetic glycan vaccine platform expected to deliver its next results in Q2 2026. Focused drug discovery efforts advancing on prioritized breakthrough projects such as Idorsia’s potential best-in-class orexin receptor agonist for narcolepsy and other orexin-related CNS disorders and Idorsia’s novel CFTR Type-IV corrector for cystic fibrosis. Financial highlights for Q1 2026 QUVIVIQ sales: CHF 44 million (excluding sales to partners) Contract revenues (one-off): CHF 11 million Non-GAAP operating expenses: CHF 78 million Non-GAAP operating loss: CHF 24 million (US GAAP: CHF 26 million) Financial Guidance for 2026 (unchanged) QUVIVIQ sales: CHF 200 million Non-GAAP operating expenses: ~CHF 330 million Non-GAAP operating loss: ~CHF 120 million (US GAAP operating loss: ~CHF 160 million) The financial guidance for 2026 reflects continued growth of QUVIVIQ (approximately 50% increase in sales in North America and Europe compared to 2025), investment in the lucerastat registration program, and development of the company’s immunology portfolio. TRYVIO/JERAYGO revenues and investments are not included, as these will be considered in any potential partnership agreement. All amounts exclude unforeseen events and any potential upsides from new direct-to-patient distribution models currently being implemented in several geographies and revenue related to additional business development activities. Financial results Q1 2026 US GAAP results First Quarter in CHF millions, except EPS (CHF) and number of shares (millions) 2026 2025 Net revenue 57 59 Operating expenses (84) 5 Operating income (loss) (26) 67 Net income (loss) (46) 63 Basic EPS (0.18) 0.33 Diluted EPS (0.18) 0.23 Basic weighted average number of shares 253 189 Diluted weighted average number of shares 253 271 Net revenue of CHF 57 million in the first quarter of 2026 resulted from product sales (CHF 44 million), product sales to partners (CHF 2 million), and contract revenues (CHF 11 million). This compares to net revenue of CHF 59 million in the first quarter of 2025 as a result of QUVIVIQ product sales (CHF 25 million), product sales to partners (CHF 1 million), and contract revenue (CHF 32 million). US GAAP operating expenses were CHF 84 million in the first quarter of 2026. In the first quarter of 2025, US GAAP operating expenses of CHF 5 million (income) were positively impacted by a one-off gain of CHF 90 million from the Viatris deal amendment. Excluding this one-off gain, US GAAP operating expenses were stable with, cost of sales of CHF 8 million increased by CHF 6 million due to higher product sales, R&D expenses of CHF 24 million decreased by CHF 3 million and SG&A expenses of CHF 53 million decreased by CHF 1 million compared to the first quarter of 2025. US GAAP net loss in the first quarter of 2026 amounted to CHF 46 million compared to CHF 63 million (net income) in the first quarter of 2025. The increased net loss in the first quarter of 2026 was primarily driven by the increase of the financial expenses and the one of gain of CHF 90 million in the first quarter of 2025. The US GAAP net loss resulted in a net loss per share of CHF 0.18 (basic and diluted) in the first quarter of 2026, compared to a net income per share of CHF 0.33 basic and CHF 0.23 diluted in the first quarter of 2025. Non-GAAP* measures First Quarter in CHF millions, except EPS (CHF) and number of shares (millions) 2026 2025 Net revenue 53 58 Operating expenses (78) (78) Operating income (loss) (24) (17) Net income (loss) (36) (25) Basic and diluted EPS (0.14) (0.13) Basic and diluted weighted average number of shares 253 189 * Idorsia measures, reports, and issues guidance on non-GAAP operating performance. Idorsia believes that these non-GAAP financial measurements more accurately reflect the underlying business performance and therefore provide useful supplementary information to investors. These non-GAAP measures are reported in addition to, not as a substitute for, US GAAP financial performance. Non-GAAP net loss in the first quarter of 2026 amounted to CHF 36 million; the difference versus US GAAP net loss was mainly driven by depreciation and amortization (CHF 4 million), share-based compensation (CHF 3 m), non-cash revenue recognized under the R-Bridge royalty monetization agreement (CHF 4 m), and accretion and issuance cost amortization (CHF 6 m). The non-GAAP net loss resulted in a net loss per share of CHF 0.14 (basic and diluted) in the first quarter of 2026, compared to a net loss per share of CHF 0.13 (basic and diluted) in the first quarter of 2025. Liquidity and indebtedness Liquidity on March 31, 2026, amounted to CHF 95 million. This amount does not include the remaining CHF 45 million available under the new money facility (term loan). (in CHF millions) Mar 31, 2026 Dec 31, 2025 Liquidity Cash and cash equivalents 95 89 Total liquidity* 95 89 Indebtedness Convertible loan 335 335 Convertible bonds 49 49 Debt notes** 766 753 Term loan 60 18 Other financial debt 185 187 Total indebtedness 1,395 1,342 *rounding differences may occur ** The debt notes issued by Idorsia Investments SARL in exchange for convertible bonds are senior secured with the shares in Idorsia Investments SARL. The A Notes only benefit from a limited and subordinated Swiss-law governed guarantee by Idorsia Ltd. Results Day Center Investor community: To make your job easier, we provide all relevant documentation, including the financial report, via the Results Day Center on our corporate website: . Events Annual General Meeting of Shareholders on May 6, 2026 Half-Year 2026 Financial Results reporting on July 30, 2026 Nine-month 2026 Financial Results reporting on October 29, 2026 Notes to the editor About Idorsia The purpose of Idorsia is to challenge accepted medical paradigms, answering the questions that matter most. To achieve this, we will discover, develop, and commercialize transformative medicines – either with in-house capabilities or together with partners – and evolve Idorsia into a leading biopharmaceutical company, with a strong scientific core. Headquartered near Basel, Switzerland – a European biotech hub – Idorsia has a highly experienced team of dedicated professionals, covering all disciplines from bench to bedside; QUVIVIQ™ (daridorexant), a different kind of insomnia treatment with the potential to revolutionize this mounting public health concern; strong partners to maximize the value of our portfolio; a promising in-house development pipeline; and a specialized drug discovery engine focused on small-molecule drugs that can change the treatment paradigm for many patients. Idorsia is listed on the SIX Swiss Exchange (ticker symbol: IDIA). For further information, please contact Kevin Boss Director, Investor Relations Idorsia Pharmaceuticals Ltd, Hegenheimermattweg 91, CH-4123 Allschwil +41 58 844 10 10 investor.relations@idorsia.com – media.relations@idorsia.com – The above information contains certain "forward-looking statements", relating to the company's business, which can be identified by the use of forward-looking terminology such as “intend”, "estimates", "believes", "expects", "may", "are expected to", "will", "will continue", "should", "would be", "seeks", "pending" or "anticipates" or similar expressions, or by discussions of strategy, plans or intentions. Such statements include descriptions of the company's investment and research and development programs, business development activities and anticipated expenditures in connection therewith, descriptions of new products expected to be introduced by the company and anticipated customer demand for such products and products in the company's existing portfolio. Such statements reflect the current views of the company with respect to future events and are subject to certain risks, uncertainties and assumptions. Many factors could cause the actual results, performance or achievements of the company to be materially different from any future results, performances or achievements that may be expressed or implied by such forward-looking statements. Should one or more of these risks or uncertainties materialize, or should underlying assumptions prove incorrect, actual results may vary materially from those described herein as anticipated, believed, estimated or expected. Attachment Press Release PDF

临床2期疫苗财报

2026-04-27

·终身学习-星辰如梦

【药品分享】吉诺昔替尼——口服小分子JAK1/TYK2双重抑制剂

吉诺昔替尼（Girocitinib，研发代号：TLL-018）是杭州高光制药自主研发的口服小分子JAK1/TYK2双重抑制剂，属于1类创新药，目前处于Ⅲ期临床阶段，尚未获批上市。基本信息通用名：吉诺昔替尼（Girocitinib）研发代号：TLL-018 靶点：JAK1、TYK2（高选择性双重抑制）药物类型：口服小分子靶向药，JAK-STAT通路抑制剂开发企业：杭州高光制药股份有限公司作用机制：通过高选择性抑制JAK1与TYK2激酶活性，阻断JAK-STAT信号通路，从而抑制炎症因子（如 IL-12、IL-23、IFN-γ等）的信号传导，减少炎症反应与免疫细胞活化，用于治疗自身免疫性与炎症性疾病。与同类药物的区别靶点特异性：主打JAK1/TYK2双重高选择性，区别于泛JAK抑制剂（如托法替尼）或JAK2/JAK1抑制剂（如巴瑞替尼），理论上脱靶风险更低、安全性更优。研发定位：聚焦外周自身免疫/炎症疾病，与已上市JAK抑制剂的适应症布局形成差异化。临床研发进展慢性自发性荨麻疹（CSU）：Ⅲ期临床试验（NCT06396026）中期分析已达到主要终点，疗效显著优于安慰剂，安全性良好。类风湿关节炎（RA）：同步开展Ⅲ期临床试验（NCT06887127、NCT06020144）。其他潜在适应症：已布局特应性皮炎、银屑病、系统性红斑狼疮等自身免疫疾病的早期临床探索。专利情况吉诺昔替尼（TLL-018/Girocitinib）为杭州高光制药自主研发的JAK1/TYK2 双靶点抑制剂，目前处于Ⅲ期临床阶段，尚未上市。 1. 化合物核心专利杭州高光制药于2017年9月30日申请，同步提交PCT国际申请，进入美、欧、日、澳等十余个主要国家/地区，预计2037年9月到期。保护通式结构覆盖JAK1/TYK2 双靶点抑制剂骨架，明确保护2-[(2R,5S)-5-[2-甲基呋喃并 [3,2-b] 咪唑并 [4,5-d] 吡啶-1-基] 四氢吡喃-2-基] 乙腈（吉诺昔替尼）的绝对构型与盐型。用于自身免疫性疾病、炎症性疾病（类风湿关节炎、荨麻疹、银屑病、特应性皮炎、SLE等）。 2. 晶型/盐型专利已布局吉诺昔替尼游离碱、甲磺酸盐、盐酸盐等多晶型/盐型专利，覆盖稳定晶型、无定型、共晶。目的是延长专利保护期、提升制剂稳定性与生物利用度、阻挡仿制药晶型规避。 3. 制剂/组合物专利保护吉诺昔替尼片剂、缓释/控释制剂的处方、工艺、溶出特性，覆盖复方组合（如与甲氨蝶呤、抗组胺药联用），拓展适应症与市场空间。 4. 合成工艺专利保护吉诺昔替尼的关键中间体、手性合成路线、纯化方法（如以7-氯-6-硝基呋喃并 [3,2-b] 吡啶为起始原料的合成路径），形成工艺壁垒，降低仿制成本与合规风险。 5. 用途/适应症专利保护慢性自发性荨麻疹、类风湿关节炎、银屑病、特应性皮炎、SLE等单一适应症的治疗方法与医药用途，每获批一个新适应症，专利保护范围同步扩大。专利优势全球独家：JAK1/TYK2 双靶点的高选择性抑制剂，无直接竞品专利冲突。层级保护：化合物+晶型+制剂+工艺+用途的五层专利网，仿制药难度极高。期限长：核心化合物专利2037年到期，叠加晶型/制剂专利，有效保护期可至2040年以后。中国自主：高光制药100%持有全球专利权益，无对外授权（除TLL-041外）。专利风险尚未上市：专利期限补偿（PTA）需获批上市后申请，实际到期日存在不确定性。临床风险：若Ⅲ期失败，专利商业价值归零。规避风险：存在结构修饰、晶型规避、适应症外推等潜在侵权/规避可能。其他药品分享链接如下，欢迎点击查看： Ormeloxifene OTF慢性体重管理的新型药物-Tirzepatide新型的非阿片类小分子镇痛药-Suzetrigine奥麦利昔芬口腔薄膜立项调研报告纳米技术双氯芬酸乳胶剂药学研究2025年9月药品批准信息快讯（八）——利斯的明透皮贴剂分享2025年9月药品批准信息快讯（九）——米托坦片分享CDE-《化学仿制药参比制剂目录（第一百批）》（征求意见稿）[附: 药品分享——阿达苏(洛沙平吸入剂)]药品分享-塞来昔布盐酸曲马多片药品分享——伐莫洛龙口服混悬液【药品分享】盐酸菲优拉生片【药品分享】拉坦噻吗滴眼液【药品分享】Baxdrostat 片【药品分享】Omecamtiv Mecarbil缓释片【药品分享】曲地匹坦（Rolapitant）【药品分享】Zasocitinib 胶囊【药品分享】甲磺酸阿帕替尼片【药品分享】巴氯芬口服溶液【药品分享】奥德昔巴特胶囊【药品分享】扎维吉泮鼻喷雾剂【药品分享】左羟丙哌嗪糖浆【药品分享】利丙双卡因凝胶贴膏【药品分享】司来吉兰改良型新药（缓释片）【药品分享】复方甘菊利多卡因凝胶【药品分享】盐酸索安非托片【药品分享】地塞米松口溶膜【药品分享】盐酸来罗西利片【药品分享】马来酸噻吗洛尔凝胶【药品分享】褪黑素颗粒【药品分享】罗氟司特乳膏【药品分享】盐酸芬戈莫德胶囊【药品分享】示踪用盐酸米托蒽醌注射液【药品分享】美洛昔康纳米晶注射液【药品分享】Clascoterone 5%外用溶液【药品分享】马来酸依那普利口服溶液【药品分享】注射用双氯芬酸钠利多卡因【药品分享】马来酸依那普利叶酸片—复方降压药【药品分享】依曲帕米鼻喷雾剂—用于治疗成人阵发性室上性心动过速的可自行给药鼻喷雾剂【药品分享】奥卡西平口服混悬液—一款可用于儿童的钠通道调节类抗癫痫药【药品分享】泊沙康唑口服混悬液——一种常用的抗真菌药物【药品分享】舒沃替尼片【药品分享】依伏卡塞片——第二代口服拟钙剂【药品分享】西诺氨酯片——第三代抗癫痫发作药物【药品分享】匹妥布替尼片——非共价可逆 BTK 抑制剂（用于复发 / 难治套细胞淋巴瘤（MCL））【药品分享】贝美前列素【产品分享】达普司他片【药品分享】水合氯醛糖浆——镇静催眠药【产品分享】苏沃雷生（Suvorexant）——全球首个食欲素受体拮抗剂类催眠药【药品分享】贝沙罗汀【药品分享】地夫可特干混悬剂——一种糖皮质激素类药物【药品分享】伊卢多啉片——治疗成人腹泻型肠易激综合征（IBS‑D）的首创口服阿片受体调节剂【药品分享】卢美哌隆胶囊——一种新型的非典型抗精神病药物【药品分享】奥氟格列隆片——口服非肽类小分子 GLP-1 受体激动剂【药品分享】苯磺酸克利加巴林胶囊——一种新型的治疗神经病理性疼痛的药物【药品分享】苯磺酸美洛加巴林片——治疗周围神经病理性疼痛（PNP）的第三代钙离子通道调节剂【药品分享】Iberdomide胶囊——一款新一代cereblon（CRBN）E3连接酶调节剂（CELMoD）化合物【药品分享】酒石酸伐尼克兰鼻喷雾剂——一种用于治疗干眼症的西药【药品分享】赛沃替尼片——中国首个获批的高选择性 MET 酪氨酸激酶抑制剂【药品分享】盐酸阿夫唑嗪缓释片——一种用于治疗良性前列腺增生（BPH）的 α1 - 受体阻滞剂【药品分享】索格列净片——全球首个获批的SGLT1/SGLT2 双重抑制剂【药品分享】奥吡卡朋胶囊——新一代的儿茶酚-氧位-甲基转移酶抑制剂（COMT）【药品分享】奎扎替尼片——一种口服高选择性 FLT3 抑制剂【药品分享】硫酸拉罗替尼胶囊 / 口服溶液——全球首个高选择性口服 TRK 抑制剂【药品分享】司帕生坦片——成人IgA肾病领域首个非免疫抑制疗法【药品分享】黄体酮阴道栓剂/阴道缓释凝胶剂——主要用于辅助生殖技术（ART）中的黄体支持【药品分享】替戈拉生片——首款国产钾离子竞争性酸阻滞剂类药物（P-CAB）【药品分享】拉坦前列烯酯滴眼剂——一种新型眼科用药【药品分享】布比卡因脂质体注射液——一种长效局部麻醉药【药品分享】甲磺酸加诺沙星片——一种喹诺酮类抗菌药【药品分享】磷酸芦可替尼乳膏——中国首款且唯一获批的白癜风治疗靶向药【药品分享】甲磺酸洛美他派胶囊——全球唯一口服MTP抑制剂【药品分享】依达拉奉口服混悬液——肌萎缩侧索硬化症（ALS，渐冻人症）新药【药品分享】依达拉奉右莰醇舌下片——全球卒中领域首个获FDA突破性疗法认定的舌下脑保护剂【药品分享】马来酸氟诺替尼片——JAK2/FLT3/CDK6 三靶点抑制剂【药品分享】普拉替尼胶囊——国内首个获批的高选择性 RET（转染重排）酪氨酸激酶抑制剂【药品分享】右美托咪定舌下膜——新型 α₂肾上腺素受体激动剂舌下膜剂【药品分享】卡匹色替片——全球首个获批上市的AKT抑制剂【药品分享】库莫西利胶囊——全球首个CDK2/4/6抑制剂【药品分享】赛贝曲司他片——全球首个HAE急性发作口服疗法【药品分享】KYGEVVI（Doxecitine/Doxribtimine）——全球首款且唯一获批的TK2d针对性治疗药物【药品分享】Forzinity（Elamipretide）注射剂——全球首个用于治疗Barth综合征的药物【药品分享】Brinsupri（Brensocatib, 布伦索卡替布）片——全球首个获批上市的二肽基肽酶1（DPP-1）抑制剂【药品分享】维立西呱片——全球首个心衰适应症的可溶性鸟苷酸环化酶（sGC）刺激剂【药品分享】盐酸哌罗匹隆片——非典型抗精神病药【药品分享】盐酸托泊替康胶囊/注射用盐酸托泊替康——经典的拓扑异构酶Ⅰ抑制剂类抗肿瘤药【药品分享】阿普昔腾坦片——全球首个获批用于难治性高血压的口服双重内皮素受体拮抗剂（ERA）【药品分享】注射用盐酸依拉环素——全球首个氟环素类抗生素【药品分享】奥洛格列净胶囊——国内首款抑制SGLT1与SGLT2的1类创新药【药品分享】盐酸匹米替尼胶囊——国内首个、全球首个获批的腱鞘巨细胞瘤（TGCT）系统性靶向药，高选择性CSF-1R抑制剂【药品分享】布地奈德肠溶胶囊——全球首个、中国唯一获批用于原发性IgA肾病对因治疗的靶向药物【药品分享】艾拉莫德片——中国原研、全球首个上市的小分子抗风湿药（csDMARD）【药品分享】索托克拉片——新一代BCL2抑制剂【药品分享】利奈昔巴特片——口服、选择性、可逆性回肠胆汁酸转运体（IBAT/ASBT）抑制剂【药品分享】多替诺雷片——高选择性URAT1抑制剂【药品分享】瑞普泊肽片——口服GLP‑1/GIP双靶点激动剂【药品分享】硫酸索西美雷塞片——口服、强效的KRAS G12C共价抑制剂【药品分享】罗伐昔替尼片——全球首创JAK/ROCK双靶点口服小分子抑制剂【药品分享】埃诺格鲁肽注射液——全球首个获批上市的cAMP偏向型长效GLP-1受体激动剂【药品分享】维培那肽注射液——长效GLP-1受体激动剂【药品分享】普乐司兰钠注射液——全球首个靶向APOC3 mRNA的siRNA降脂药【药品分享】玛仕度肽注射液——全球首个GCG/GLP-1双激动剂【药品分享】瑞米布替尼片——全球首个获批用于CSU的口服靶向药【药品分享】溴莫尼定噻吗洛尔滴眼液——α₂受体激动剂与非选择性 β 受体阻滞剂组成的复方降眼压药【药品分享】吡洛西利片——国内首个CDK2/4/6多靶点抑制剂【药品分享】奥氟格列隆片（Orforglipron） ——中国首个、全球首批上市的口服小分子 GLP-1受体激动剂【药品分享】Copper Histidine注射液（Zycubo）——全球首个、唯一用于治疗儿童门克斯病（Menkes disease）的铜替代注射剂【药品分享】依来格列隆片（Elecoglipron）——口服小分子非肽类GLP-1受体激动剂【药品分享】阿利奈普仑（Aleniglipron）——口服小分子、非肽类、偏向性GLP-1受体激动剂【药品分享】甲磺酸阿美替尼片——中国首个原研三代EGFR酪氨酸激酶抑制剂（TKI）【药品分享】甲磺酸达麦利替尼片——口服高选择性c-MET酪氨酸激酶抑制剂【药品分享】盐酸Acoramidis片——转甲状腺素蛋白（TTR）稳定剂【药品分享】阿莫西林伏诺拉生胃漂浮片——3D打印胃漂浮片【药品分享】盐酸伊可白滞素片——全球首创口服IL‑23受体拮抗剂【药品分享】马来酸吡咯替尼片——中国首个自研的HER1/HER2/HER4不可逆酪氨酸激酶抑制剂（TKI）【药品分享】本维莫德乳膏——全球首创芳香烃受体（AhR）调节剂（TAMA）类皮肤病外用药【药品分享】盐酸莫托咪酯注射液——化药1类静脉麻醉新药【药品分享】注射用罗哌卡因微晶——长效缓释局部麻醉药【药品分享】盐酸伊立替康脂质体注射液——一款针对吉西他滨治疗失败的转移性胰腺癌的二线标准脂质体化疗药【药品分享】甲磺酸氟马替尼片——Bcr-Abl酪氨酸激酶选择性抑制剂【药品分享】注射用阿加糖酶β——国内获批的首个用于治疗法布雷病的药物【药品分享】甲苯磺酸尼拉帕利胶囊——高选择性PARP1/2抑制剂【药品分享】帕米帕利胶囊——强效、选择性PARP1/2抑制剂【药品分享】苯环喹溴铵鼻喷雾剂——选择性M胆碱能受体拮抗剂【药品分享】注射用拉罗尼酶浓溶液——MPS Ⅰ型的特异性酶替代治疗药物【药品分享】海博麦布片——国产自主原研的胆固醇吸收抑制剂【药品分享】盐酸可洛派韦胶囊——直接抗病毒药物（DAA）→ NS5A抑制剂【药品分享】克拉考特酮乳膏——外用、非甾体、选择性雄激素受体（AR）抑制剂【药品分享】非卢替尼片——全球首个用于多发性硬化的口服BTK抑制剂【药品分享】Brenipatide注射液——GLP-1R/GIPR双受体激动剂（继替尔泊肽之后的第二款）【药品分享】罗赛促红素α注射液——国产首个长效重组促红细胞生成素（EPO）创新药【药品分享】贝组替凡片——全球首个口服小分子HIF-2α抑制剂【药品分享】那米司特片——口服选择性PDE4B抑制剂【药品分享】富马酸立康可泮胶囊——一款针对罕见病PNH的口服补体B因子抑制剂【药品分享】醋酸索乐匹尼布片——高选择性脾酪氨酸激酶（Syk）抑制剂【药品分享】甲磺酸艾多替尼片——全球首款专为肺癌脑转移设计的第三代EGFR-TKI 【药品分享】安瑞克芬注射液——全球首个获批镇痛适应症的高选择性外周κ-阿片受体（KOR）激动剂【药品分享】Difelikefalin注射液——全球首个获批的外周选择性κ-阿片受体（KOR）激动剂【药品分享】Obefazimod——口服、靶向 CBC、特异性增强miR-124的首创小分子【药品分享】拉尼兰诺片——口服泛PPAR激动剂【药品分享】舒洛地特注射液——抗血栓药、血管保护剂【药品分享】贝普若韦生注射液——反义寡核苷酸（ASO）类乙肝新药【药品分享】氨酚右敏口服溶液（奥肯能®）——中国内地唯一获批的氨酚右敏口服溶液【药品分享】佩玛贝特片——新型过氧化物酶体增殖物激活受体α/δ双重激动剂 (PPARα/δ) 【药品分享】盐酸依匹斯汀乳膏——外用第二代非镇静抗组胺抗过敏药膏【药品分享】注射用双羟萘酸帕瑞肽微球——一款用于治疗肢端肥大症的第二代长效生长抑素类似物（SRL）微球制剂【药品分享】埃拉菲布拉诺片——治疗原发性胆汁性胆管炎（PBC）的口服靶向新药【药品分享】泽卢克布仑钠注射液——新一代皮下注射型C5补体抑制剂【药品分享】依达拉奉右莰醇注射用浓溶液——一款复方神经保护类注射剂【药品分享】醋酸戈那瑞林注射液——促性腺激素释放激素（GnRH）类药物【药品分享】甲磺酸贝舒地尔片——全球首个选择性ROCK2激酶抑制剂【药品分享】伊托法替布软膏——外用JAK抑制剂（JAK1/JAK3）【药品分享】注射用华卟啉钠——新型肿瘤光动力治疗（PDT）专用光敏剂【药品分享】优替德隆胶囊——口服埃博霉素类微管抑制剂【药品分享】艾普美妥司他片——EZH1/2双靶创新药【药品分享】精氨酸艾曲莫德片——新型选择性鞘氨醇1-磷酸受体（S1P₁）调节剂【药品分享】磷酸芦可替尼乳膏——全球/国内首款、唯一获批用于非节段型白癜风复色的外用JAK1/JAK2选择性抑制剂【药品分享】盐酸右哌甲酯缓释胶囊——治疗6岁及以上注意缺陷多动障碍（ADHD）的一线药物【药品分享】抗菌肽PL-3301口腔凝胶——中国首创的抗菌肽类抗口腔真菌感染药物【药品分享】Zasocitinib (TAK-279) 胶囊——新一代高选择性口服 TYK2 抑制剂【药品分享】注射用Abelacimab——一款全人源IgG1单克隆抗体，靶向凝血因子XI（FXI）【药品分享】Duvakitug注射液——首创性人源化IgG1-λ2单克隆抗体，靶向TL1A（TNFSF15）【药品分享】醋酸氟轻松/氢醌/维A酸乳膏——治疗中重度黄褐斑疗效明确的外用复方【药品分享】富马酸伏诺拉生氯化钠注射液——钾离子竞争性酸阻滞剂（P‑CAB）||东阳光药业研发的2.2,2.4类改良新型新药【药品分享】盐酸阿曲生坦片——诺华研发的高选择性内皮素 A（ETA）受体拮抗剂||中国首个获批用于IgA 肾病的非免疫性口服靶向药【药品分享】RGT-274-CR胶囊——上海齐鲁锐格医药研发的口服小分子GLP-1受体激动剂【药品分享】酒石酸西尼必利片——高选择性5-HT₄受体激动剂类胃肠动力药【药品分享】石杉碱甲控释片——采用双相控释/渗透泵技术的2.2类改良型新药【药品分享】塞伐艾替尼片——口服、可逆、选择性酪氨酸激酶抑制剂（TKI）【药品分享】Admilparant片——口服小分子LPA₁受体拮抗剂【药品分享】瑞拉可兰胶囊——全球首个选择性糖皮质激素受体（GR）拮抗剂【药品分享】盐酸依特卡肽注射液——全球首个、国内唯一获批的静脉注射型拟钙剂【药品分享】Avacincaptad pegol玻璃体内注射液——全球首批用于AMD继发地图样萎缩（GA）的靶向药物【药品分享】盐酸达利雷生片——新一代非管制、非苯二氮䓬类抗失眠药物【药品分享】甲磺酸瑞索利塞片——高选择性PI3Kα小分子靶向抑制剂 || 全球首个获批用于特定卵巢癌的靶向新药【药品分享】富马酸西他沙星注射液——新型喹诺酮类抗菌药物【药品分享】Icotrokinra——全球首个获批的口服 IL-23 受体（IL-23R）选择性拮抗多肽【药品分享】氘可来昔替尼片（Deucravacitinib）——全球首个口服、选择性 TYK2 变构抑制剂免责声明：本文仅作医药信息传播分享，并不构成投资或决策建议。

100 项与阿普昔腾坦相关的药物交易

登录后查看更多信息

外链

KEGG	Wiki	ATC	Drug Bank
D11441	-	-	DB15059

研发状态

批准上市

10 条最早获批的记录,

后查看更多信息

适应症	国家/地区	公司	日期
原发性高血压	加拿大	Idorsia Pharmaceuticals Ltd.	2025-12-01
难治性高血压	欧盟	IDORSIA LTD	2024-07-01
难治性高血压	冰岛	IDORSIA LTD	2024-07-01
难治性高血压	列支敦士登	IDORSIA LTD	2024-07-01
难治性高血压	挪威	IDORSIA LTD	2024-07-01
高血压	美国	Idorsia Pharmaceuticals Ltd.	2024-03-19

未上市

10 条进展最快的记录,

后查看更多信息

适应症	最高研发状态	国家/地区	公司	日期
慢性肾病	临床3期	-	Janssen Biotech, Inc.	2020-01-01
慢性肾病	临床3期	-	Idorsia Pharmaceuticals Ltd.	2020-01-01
肝硬化	临床1期	德国	Idorsia Pharmaceuticals Ltd.	2020-06-26
肝硬化	临床1期	波兰	Idorsia Pharmaceuticals Ltd.	2020-06-26
肝损伤	临床1期	德国	Idorsia Pharmaceuticals Ltd.	2020-06-26
肝损伤	临床1期	波兰	Idorsia Pharmaceuticals Ltd.	2020-06-26

登录后查看更多信息

临床结果

适应症

分期

评价

查看全部结果

研究	分期	人群特征	评价人数	分组	结果	评价	发布日期


NCT03541174 (PRECISION, Pubmed \| Hypertension)	临床3期	低血压	-	Aprocitentan 12.5 mg	積願鏇淵構製蓋願壓淵(網獵蓋鏇積範簾鏇餘觸) = 膚願獵鹽鏇夢窪鬱築選築鹽積壓築獵遞構艱醖 (獵壓夢蓋壓夢獵憲選遞 )	积极	2025-04-01
				Aprocitentan 25 mg	積願鏇淵構製蓋願壓淵(網獵蓋鏇積範簾鏇餘觸) = 鹽遞鑰餘廠鏇淵遞鏇繭築鹽積壓築獵遞構艱醖 (獵壓夢蓋壓夢獵憲選遞 )
PRECISION (ASN2024)	临床3期	难治性高血压	838	Aprocitentan 12.5 mg	鹹襯鏇遞鹹獵築鏇鏇淵(蓋窪廠積製蓋蓋簾獵夢) = 鏇獵選觸膚襯壓襯網築鏇網艱簾積壓築觸繭醖 (願繭願顧夢餘淵憲壓繭 )	积极	2024-10-26
				Aprocitentan 25 mg	鹹襯鏇遞鹹獵築鏇鏇淵(蓋窪廠積製蓋蓋簾獵夢) = 夢糧壓餘繭範憲醖構遞鏇網艱簾積壓築觸繭醖 (願繭願顧夢餘淵憲壓繭 )
PRECISION (ESH2024)	临床3期	难治性高血压	-	Aprocitentan 12.5 mg	遞壓艱鏇襯廠網膚願廠(憲齋簾壓醖觸憲網觸鏇) = 選簾構構窪餘願遞範遞衊鏇醖獵獵繭繭獵繭糧 (鹽觸鹹選憲範鏇餘範鏇 )	积极	2024-05-01
				Aprocitentan 25 mg	遞壓艱鏇襯廠網膚願廠(憲齋簾壓醖觸憲網觸鏇) = 積繭範積獵夢廠築選遞衊鏇醖獵獵繭繭獵繭糧 (鹽觸鹹選憲範鏇餘範鏇 ) 更多
PRECISION (ESH2024)	临床3期	难治性高血压	93	Aprocitentan 12.5 mg	鑰製廠廠積鹹衊醖艱蓋(網顧醖膚鏇範鏇糧鑰蓋) = 網製構艱簾襯襯淵鏇積鹽憲糧構衊觸鹽夢鬱積 (顧網糧鏇齋襯壓鏇願壓 ) 更多	积极	2024-05-01
				Aprocitentan 25 mg	鑰製廠廠積鹹衊醖艱蓋(網顧醖膚鏇範鏇糧鑰蓋) = 築鬱夢範範積壓構鬱膚鹽憲糧構衊觸鹽夢鬱積 (顧網糧鏇齋襯壓鏇願壓 ) 更多
NCT03541174 (FDA) 人工标引	临床3期	高血压	-	Aprocitentan (12.5 mg)	觸餘積夢構鏇築壓壓構(艱壓膚齋襯憲糧鹽範蓋) = 顧簾衊簾壓襯醖憲鬱壓構鹽網獵淵築衊蓋顧觸 (襯壓壓鹹淵積鑰衊鹹鑰, −17.5 ~ −13.3) 更多	优效	2024-03-19
				Placebo	觸餘積夢構鏇築壓壓構(艱壓膚齋襯憲糧鹽範蓋) = 鹹蓋壓齋網淵簾醖衊艱構鹽網獵淵築衊蓋顧觸 (襯壓壓鹹淵積鑰衊鹹鑰, −13.7 ~ −9.5) 更多
PRECISION (ESH2023)	临床3期	难治性高血压	730	Aprocitentan 12.5 mg	鏇淵選構淵鏇觸觸遞範(醖膚鑰鏇鑰餘餘鹽鏇簾) = 網餘醖糧壓選餘糧膚鹹選獵淵鬱繭憲齋淵顧廠 (範憲網窪製選壓顧夢築 )	积极	2023-06-01
				Aprocitentan 25 mg	鏇淵選構淵鏇觸觸遞範(醖膚鑰鏇鑰餘餘鹽鏇簾) = 網壓鹽簾製憲鹽繭鹹膚選獵淵鬱繭憲齋淵顧廠 (範憲網窪製選壓顧夢築 )
NCT03541174 (PRECISION, CTgov)	临床3期	难治性高血压	730	Aprocitentan 12.5 mg (Aprocitentan 12.5 mg in Part 1 (Double-blind))	醖鑰窪範鑰廠簾鏇繭淵(鬱齋遞簾積鏇簾齋廠選) = 壓繭鏇築積糧觸餘鑰鏇齋廠齋鑰觸製齋簾夢製 (憲衊構廠艱壓顧窪鬱鹽, 選蓋艱鹽蓋鏇鏇壓膚鹹 ~ 夢衊鬱觸選鏇鏇齋遞網) 更多	-	2023-03-21
				Aprocitentan 25 mg (Aprocitentan 25 mg in Part 1 (Double-blind))	醖鑰窪範鑰廠簾鏇繭淵(鬱齋遞簾積鏇簾齋廠選) = 繭積築鏇艱鑰遞襯製觸齋廠齋鑰觸製齋簾夢製 (憲衊構廠艱壓顧窪鬱鹽, 淵築繭鹽繭餘範網襯觸 ~ 醖鏇遞鹹積簾糧遞鑰襯) 更多
NCT02603809 (CTgov)	临床2期	原发性高血压	1,659	Placebo (Placebo)	選遞鏇艱觸構願艱蓋簾(衊觸顧遞憲顧獵選範糧) = 簾糧築選遞製鏇遞顧鏇壓範選壓鬱選壓獵窪餘 (願鏇窪膚選蓋齋窪衊繭, 5.4) 更多	-	2020-04-13
				Aprocitentan 5 mg (Aprocitentan 5 mg)	選遞鏇艱觸構願艱蓋簾(衊觸顧遞憲顧獵選範糧) = 構餘蓋餘餘蓋夢壓憲鑰壓範選壓鬱選壓獵窪餘 (願鏇窪膚選蓋齋窪衊繭, 5.5) 更多
NCT02603809 (ESC2019)	临床2期	高血压	490	Aprocitentan 5 mg	膚齋窪鹹廠廠夢膚壓鏇(築餘夢壓願範遞鹹艱膚) = 餘願鑰繭夢鏇獵選醖築鹹鹹願淵壓蓋衊觸構艱 (積膚選鹹鹽襯鹽願構壓 ) 更多	-	2019-08-31
				Aprocitentan 10 mg	膚齋窪鹹廠廠夢膚壓鏇(築餘夢壓願範遞鹹艱膚) = 鬱遞壓窪構廠鹹鑰構夢鹹鹹願淵壓蓋衊觸構艱 (積膚選鹹鹽襯鹽願構壓 ) 更多