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

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100 项与阿普昔腾坦相关的转化医学

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100 项与阿普昔腾坦相关的专利（医药）

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项与阿普昔腾坦相关的文献（医药）

2026-06-01·JOURNAL OF PEDIATRICS

Macitentan in Pediatric Pulmonary Arterial Hypertension (TOMORROW): A Randomized Clinical Trial

Article

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

OBJECTIVE:

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 multicenter, open-label, phase 3 clinical trial in patients aged ≥2-<18 years World Health Organization Functional Class 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-confirmed disease progression, safety/tolerability, change in NT-proBNP, and quality of life.

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 > .05 for all). Percentage of baseline NT-proBNP was 72% (macitentan) vs 101% (SoC) at week 12 (P = .086) and 76% vs 78% at week 24 (P = .884). Macitentan showed clinically meaningful improvements in quality of life assessments vs SoC for children (P = .043) and parents (P = .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.

TRIAL REGISTRATION:

ClinicalTrials.gov (ID number, NCT02932410; https://clinicaltrials.gov/study/NCT02932410).

2026-04-10·Current Hypertension Reviews

Resistant Hypertension: Pathophysiology, Diagnostic Approaches, and Emerging Therapeutic Strategies

Article

作者: Mahadevappa, Manjappa ; Raj Srinivasan, Bharath ; Narayan, Himabindu Jayaprakash

Introduction::

Resistant Hypertension (RH) is defined as Blood Pressure (BP) that remains uncontrolled despite the concurrent use of three antihypertensive agents from different classes, including a diuretic. This review examines the pathophysiology, diagnostic criteria, and emerging therapeutic strategies in RH management, with an emphasis on current clinical challenges and future directions.

Methods::

This article is a narrative (non-systematic) review. PubMed and Scopus were searched for “English language” literature from January 2000 through June 2025, using terms including “resistant hypertension”, “apparent treatment resistant hypertension”, “renal denervation”, “aldosterone”, and “secondary hypertension”. Guidelines, randomized controlled trials, and systematic reviews/meta-analyses directly relevant to the pathophysiology, diagnosis, and treatment of resistant hypertension were prioritized. Additional landmark observational studies were included when considered clinically informative.

Results::

RH affects up to 10% of hypertensive patients globally, with higher prevalence in those with chronic kidney disease and obstructive sleep apnea. Misdiagnosis due to pseudo-resistance and poor medication adherence remains prevalent. Pathophysiology involves complex mechanisms, including sympathetic overactivity, dysregulation of the RAAS, and aldosterone excess. Diagnostic confirmation includes excluding pseudo-resistance and evaluating for secondary causes. Lifestyle modifications remain foundational. Mineralocorticoid receptor antagonists, aldosterone synthase inhibitors, renal denervation, and baroreceptor therapies show promise in treating cases resistant to other therapies.

Discussion::

While conventional pharmacotherapy remains the cornerstone, inadequate BP control in RH necessitates a deeper understanding of underlying mechanisms and adherence assessment. Device-based approaches and emerging agents, such as zilebesiran and aprocitentan, may hold promise in revolutionizing RH management but require further validation. Limitations include a lack of large-scale comparative trials and accessibility concerns in low-resource settings.

Conclusion::

Resistant hypertension represents a multifactorial condition requiring a multidimensional diagnostic and therapeutic approach. Integrating lifestyle changes, optimized pharmacotherapy, and emerging options, including aldosterone synthase inhibition, dual endothelin receptor antagonism, small-interfering RNA strategies, and refined device-based approaches, offers incremental BP reductions in carefully selected patients. The synthesis emphasizes a pragmatic, stepwise strategy that couples adherence and secondary cause assessment with evidence-based pharmacologic intensification (notably mineralocorticoid receptor antagonists) and selective device therapy. This integrated approach may be critical for achieving durable BP control and reducing cardiovascular risk in patients with resistant hypertension.

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.

228

项与阿普昔腾坦相关的新闻（医药）

2026-06-02

·智健富康推送

高血压治疗最新进展

❤️ 智健富康推送 2026年6月 · 高血压治疗最新突破全景解读 ✦ 赣水西边龙虾 ✦ 💡 本期导读我国成人高血压患病率已达29.6%，意味着每3个成年人中就有近1人受高血压困扰。所幸，2025-2026年高血压治疗领域迎来了井喷式突破——从RNA干扰超长效降压药、FDA近40年首个全新机制降压药，到中国首创高血压疫苗获批临床、AI+可穿戴闭环管理……本文全景梳理五大维度、15个关键专题，带你一次看懂高血压治疗的现在与未来。 📊 本期覆盖：药物治疗4大突破 · 介入治疗1大革新 · AI数字疗法2大方向 · 指南更新2大体系 · 生活方式干预6大措施 💊 药物治疗新突破 🔑 01 醛固酮合酶抑制剂：从受体阻断到源头合成抑制 📌 Baxdrostat · Lorundrostat · Ⅲ期临床数据公布传统降压药针对醛固酮受体"下游拦截"，但存在"醛固酮逃逸"——长期使用后醛固酮水平反弹。新一代醛固酮合酶抑制剂直接抑制CYP11B2基因编码的醛固酮合酶，从源头掐断合成通路。更关键的是，第二代药物实现了高选择性——仅靶向醛固酮合酶，不影响皮质醇合成，解决了第一代药物的副作用难题。 🔬 关键临床数据： ⭐ Lorundrostat（洛伦德罗斯坦）Launch-HTN Ⅲ期（2025.06）：50mg剂量治疗6周，收缩压较安慰剂组降低近10mmHg⭐ Baxdrostat（巴克司他）BaxHTN Ⅲ期（2025.10）：1mg和2mg剂量组12周时收缩压、舒张压均显著降低；更惊人的是——停药8周后降压效果仍持续⭐ 血清钾、肾小球滤过率变化可控，安全性良好 📎 来源：腾讯新闻 · 2026-02-08 / NEJM · 2025 🔑 02 RNA干扰疗法：半年一针，超长效降压新时代 📌 Zilebesiran（齐利布西兰）· siRNA技术 · KARDIA-3研究 · ESC 2025 Zilebesiran是罗氏与Alnylam联合开发的全球首个高血压siRNA药物。它利用GalNAc（N-乙酰半乳糖胺）作为"导航系统"，将小干扰RNA精准递送至肝脏，从基因表达层面抑制血管紧张素原——RAAS系统的"总开关"。效果持续长达6个月，意味着患者可能只需每半年注射一次，彻底告别每日服药的依从性困局。 🧬 突破性数据（KARDIA-3 Ⅱ期，ESC 2025）： ⭐ 对使用2-4种降压药仍控制不佳的高危患者，Zilebesiran 300mg每6个月皮下注射一次，降压效果显著优于安慰剂⭐ 即使eGFR降至30-44的肾功能不全患者，安全性依然良好——低高钾血症发生率、无显著肾功能恶化⭐ 已启动以MACE事件为终点的全球Ⅲ期临床试验，有望成为首个获批的高血压RNAi疗法 📎 来源：Roche / ESC 2025 Hot Line · 2025-08-30 🔑 03 双重内皮素受体拮抗剂：FDA近40年首个全新机制降压药 📌 Aprocitentan（阿普昔腾坦）· FDA已批准 · PRECISION研究 Aprocitentan是FDA时隔近40年批准的首个全新作用机制降压药。早期内皮素受体拮抗剂因单向抑制ETA受体导致液体潴留而失败；Aprocitentan通过将ETA/ETB抑制比例优化为60:1的黄金配比，在保持强效降压的同时大幅减少了水肿风险。2025年拓展研究更发现其对慢性肾病合并难治性高血压不仅能降压，还能改善尿微量白蛋白肌酐比（UACR），且对夜间血压控制尤为出色。 🏆 PRECISION Ⅲ期核心结果： ⭐ 针对3药（含利尿剂）仍难控的高血压：活性药物治疗初期即显著降压，维持阶段血压稳定⭐ 换用安慰剂后血压明显反弹——反向验证了真实有效性⭐ 无论勺型/非勺型高血压均有效，夜间血压控制优势突出 📎 来源：The Lancet / 新浪财经 · 2026 🔑 04 高血压治疗疫苗：中国原创，全球首个获批临床 📌 HJY-ATRQβ-001 · 华中科技大学协和医院廖玉华团队 · 历时22年 2025年8月22日，由华中科技大学同济医学院附属协和医院廖玉华教授团队研发的全球首创短肽降压疫苗HJY-ATRQβ-001获国家药监局批准开展临床试验。该疫苗靶向血管紧张素Ⅱ受体1（AT1R），通过调动患者自身免疫系统实现偏向性调控，与传统"堵截式"药物截然不同。临床前数据显示单次注射后药效可持续1-2个月，有望将患者依从性从当前不足50%提升至80%以上。更值得关注的是，研发方华纪元生物已布局降脂、降糖疫苗管线，未来将构建"一针管三高"的代谢病疫苗矩阵。 🇨🇳 中国亮点： ⭐ 全球首个靶向AT1R的治疗性降压疫苗进入临床⭐ 可规避传统RAAS抑制剂的肝肾毒性风险⭐ 塞力医疗（603716.SH）战略控股，2026年加速临床与报批进程⭐ 动物实验显示抗体滴度维持6周以上，对靶器官有保护作用 📎 来源：搜狐 · 2025全国高血压年会 / 国家药监局 ◆────────◆ 🔧 介入治疗革新 🔑 05 去肾神经术（RDN）：微创介入降压，中国共识落地 📌 经皮导管消融 · 2025中国专家共识 · FDA已批准经皮去肾神经术（RDN）是高血压领域近十年来最重要的器械治疗突破。通过导管对肾动脉周围的交感神经进行消融，从物理层面阻断交感神经过度激活。2023年底FDA批准两款RDN系统，2025年9月《经皮去肾神经术治疗高血压临床路径中国专家共识》正式发布，标志着这项技术在中国进入规范化推广阶段。 📋 中国共识核心要点： 🎯 适应证分层：①难治性高血压（≥3药不佳）②药物控制不佳（2药后OBP≥150/90）③药物不耐受🔬 疗效数据：约70%患者对RDN反应良好，术后30%-40%可减少降压药用量，但大多数仍需继续服药——RDN是辅助而非替代⚠️ 安全性：肾动脉穿孔/血栓发生率<1%，总体并发症极少💰 现实挑战：单次手术数万元且多数地区未纳入医保，术后约30%患者反应不佳 💡 专家提醒：术前必须严格筛查继发性高血压（占难治性高血压20%-35%），需综合诊室+动态+家庭血压评估，绝非"一消了之"。 📎 来源：《中国介入心脏病学杂志》· 2025-09 / Nature Reviews Cardiology ◆────────◆ 🤖 AI与数字疗法 🔑 06 AI智能管理：从被动测量到主动预警 📌 可穿戴设备+大语言模型 · 全球首个开源AI高血压防治系统 2025年3月，香港中文大学张元亭教授团队联合广东医科大学发布了全球首个结合智能可穿戴技术与DeepSeek-R1大语言模型的开源高血压防治AI系统。该系统通过可穿戴设备实现24小时连续血压监测，结合心率、运动、睡眠等多维数据，精准识别清晨高血压、夜间高血压、餐后低血压等隐蔽问题，并基于大模型生成个性化干预建议。 📱 数字疗法关键进展： ⭐ 可穿戴设备已实现逐搏血压监测，识别传统诊室测量无法发现的血压变异模式⭐ AI整合多维度数据（血压+心率+运动+睡眠+饮食），实现风险评估和临床决策辅助⭐ 大语言模型（DeepSeek等）赋能智能患者教育和个性化健康管理⭐ 数字化医疗实现了从"点测量"到"面管理"的质的飞跃 📎 来源：广东医科大学 · 2025-03 / 中华心血管病杂志 🔑 07 数字疗法+闭环管理：高血压慢病管理新模式 📌 国家发改委推动 · AI+医疗场景落地 2025年12月，国家发改委发文明确推动AI+医疗健康场景落地。核心方向包括：以智能可穿戴设备为载体，运用AI对个体进行全生命周期健康管理；构建"筛查-诊断-干预-保险-监测"闭环。在高血压领域，数字疗法（DTx）已从概念走向实践——通过APP+可穿戴设备实现远程监测、智能提醒、个性化行为干预，多项RCT研究证实其可使收缩压额外降低3-5mmHg。 🏥 中国实践： ⭐ 2025基层高血压指南新增"健康教育"独立章节，强调数字化工具赋能⭐ AI辅助诊断可提高高血压分型和风险分层的准确性⭐ "互联网+高血压管理"模式在多地试点，基层覆盖率持续提升 📎 来源：国家发改委 · 2025-12 / 搜狐健康 ◆────────◆ 📋 权威指南更新 🔑 08 中国基层高血压防治指南（2025版）要点速览 📌 2025年9月发布 · 覆盖2.45亿患者 2025年9月，国家卫健委发布《国家基层高血压防治管理指南（2025版）》，对2020版进行了系统性更新。新版首次新增"筛查与预防"和"健康教育"两大独立章节，强调"防优于治"理念，为基层医疗机构提供了更科学的血压管理方案。 🔄 六大核心更新： ① 诊断标准：非同日3次≥140/90mmHg确诊；认可家庭自测和动态血压的诊断价值② 治疗目标：80岁以下降至<130/80mmHg；80岁以上<150/90（能耐受可<140/90）③ 启动时机：确诊后生活方式干预+立即启动药物；血压≥150/90推荐起始两种药物联合④ 筛查建议：18岁及以上成人每年至少测一次血压；高危人群（130-139/85-89合并CVD/CKD/DM）应启动药物⑤ 测量规范：推荐上臂式电子血压计；禁止腕式/手指式；30分钟前禁烟咖啡⑥ 健康八部曲：限盐减重多运动，戒烟戒酒心态平 📎 来源：国家卫健委 · 2025-09 / 腾讯新闻 🔑 09 2025 ACC/AHA高血压指南：精准细化，稳中有进 📌 美国心脏病学会/美国心脏协会 · 2025年发布 2025年ACC/AHA指南并非颠覆性变革，而是基于新证据的"更新与澄清"。核心治疗框架不变（四类一线药物、联合策略），重要更新包括：新增钾基盐替代品推荐（排除CKD患者）、更强调单片复方制剂（SPC）以提高依从性、对心力衰竭/CKD/糖尿病等合并症的强制适应证指导更新、以及更强调治疗后约1个月评估反应。 🇺🇸🇨🇳 中美指南对比： ⭐ 诊断阈值：美国130/80 vs 中国140/90（美国更激进）⭐ 治疗目标：美国<130/80 vs 中国<130/80（80岁以下）——趋同⭐ 药物推荐：核心一致（ACEI/ARB+CCB+利尿剂），β受体阻滞剂均退出一线⭐ 中国特色：基层导向、筛查与预防单独成章、"健康八部曲"更简洁易记 📎 来源：AHA Journals / US Pharmacist · 2025-2026 ◆────────◆ 🥗 生活方式干预无论药物如何创新，生活方式干预始终是高血压治疗的基石。2025版中国指南提炼为"限盐减重多运动，戒烟戒酒心态平"十四字口诀，每一句都有硬核数据支撑——每一条都能降压5-10mmHg，效果堪比单用一种降压药。 🧂 低钠高钾饮食 — 可降压 6-8mmHg 每日钠摄入控制在2300mg（约5克盐），理想目标<1500mg/天。肾功能正常者可用低钠盐替代，每日钾摄入建议3000-5000mg。注意：CKD患者慎用钾盐替代品！ ⚖️ 科学减重 — 每减1kg约降压1mmHg 超重/肥胖者至少减重5%或使BMI下降3个单位。举例：80kg的人减掉4kg，血压可能下降4mmHg。 🥬 DASH饮食模式 — 可降压 5-8mmHg 多吃蔬菜、水果、全谷物、低脂乳制品；适量瘦肉、鱼类、坚果；少吃红肉、甜食、饱和脂肪。降压效果堪比单一降压药。 🏃 规律运动 — 可降压 5-10mmHg 每周150分钟中等强度有氧运动（快走、骑车、游泳）或75分钟高强度运动，配合每周2次抗阻训练。 🍷 严格限酒 — 可降压 5.5/4.4mmHg 每日超6杯者减少50%饮酒量可达到此效果；戒酒者高血压发生率可降低高达50%。 🧘 心理压力管理 — 可额外降压 5mmHg以上通过冥想、正念练习、深呼吸、瑜伽、太极、保证充足睡眠等方式放松身心。长期精神紧张是高血压的独立危险因素。 💡 关键认知：生活方式干预不是"辅助"，而是与药物治疗同等重要的一线治疗策略。对于血压轻度升高者，有时仅靠生活方式调整即可达标。 📎 来源：2025中国高血压防治指南 / AHA 2025指南 / 腾讯新闻 ◆────────◆ 🔭 总结与展望回顾2025-2026年高血压治疗全景，三大趋势尤为清晰： 📌 趋势一：治疗关口前移从仅关注"难治性"扩展到"未控制"甚至"正常高值合并高危因素"，筛查与预防成为独立章节。新药研发也不再局限于难治性高血压，而是覆盖更广泛的患者群体。 📌 趋势二：技术创新融合 RNA干扰、基因治疗、疫苗技术、AI大模型——高血压治疗正从"小分子化学药"时代迈入"生物制剂+智能管理"新纪元。半年一针的siRNA、调动自身免疫的疫苗、24小时AI监测的可穿戴设备，将从根本上改变数百万患者的治疗体验。 📌 趋势三：中国力量崛起从协和医院的高血压疫苗到DeepSeek赋能的AI防治系统，中国在高血压创新领域正从"跟跑"转向"并跑"甚至"领跑"。2025中国基层指南的发布更标志着中国高血压防治体系的系统性升级。但需清醒认识到：生活方式干预仍是基石，药物依从性仍是最大挑战（漏服率超50%），RDN和疫苗等新技术仍需更多长期数据验证。高血压防控之路上，没有"魔法子弹"——技术创新与个人自律从来都是硬币的两面。 ❤️ 关注血压，从现在开始 18岁以上成人每年至少测一次血压 · 限盐减重多运动 · 戒烟戒酒心态平 📲 长按识别二维码关注我们 📱 扫码关注「智健富康」 —— 智健富康推送 —— 健康相伴 · 幸福相随 © 2026 智健富康 · 保留所有权利本文内容仅供参考，不能替代专业医师诊断与治疗数据来源：国家卫健委、AHA/ACC、NEJM、The Lancet、ESC 2025、全国高血压年会

2026-06-01

·终身学习-星辰如梦

【药品分享】玛伐凯泰胶囊——全球首创、中国唯一获批的心肌肌球蛋白抑制剂

玛伐凯泰胶囊（商品名：迈凡妥®）是全球首创、中国唯一获批的心肌肌球蛋白抑制剂，用于治疗梗阻性肥厚型心肌病（oHCM）。基本信息通用名：玛伐凯泰胶囊（Mavacamten）商品名：迈凡妥®（CAMZYOS®）医保情况：已纳入国家医保乙类生产商：百时美施贵宝（BMS）国家医疗保障局规格：2.5mg、5mg、10mg、15mg 适应症：用于治疗纽约心脏协会（NYHA）心功能II–III级的梗阻性肥厚型心肌病（oHCM）成人患者，以改善运动能力与症状。作用机制靶向根源：直接抑制心肌肌球蛋白，减少心肌过度收缩、减轻左心室流出道梗阻。机制优势：将肌球蛋白转为 “超松弛状态”，减少横桥形成、降低心肌耗氧、改善舒张功能。地位：150余年HCM研究史上首个针对病因的靶向药。用法用量起始：2.5mg每日一次，整粒吞服，可随餐或空腹。剂量调整：依据LVEF（≥50%）与LVOT压差，可上调至5/10/15mg；最大15mg/日。常见不良反应头晕（27%）、晕厥（6%）（较安慰剂更常见）。可逆性 LVEF 下降（多无症状，停药后恢复）。少见：呼吸困难、乏力、心悸、室内传导障碍。禁用：中/重度CYP2C19抑制剂、重度CYP3A4抑制剂（如氟康唑、伏立康唑）；中/强CYP2C19或CYP3A4诱导剂（如利福平、卡马西平）。慎用：LVEF＜55%、严重肝/肾功能不全、妊娠/哺乳期、儿童。避免与丙吡胺、维拉帕米/地尔硫卓+β受体阻滞剂联用。临床价值显著改善：降低LVOT压差、提升运动耐量、缓解呼吸困难/胸痛/晕厥。填补空白：40余年首个直接针对病因的oHCM靶向药，优于传统对症治疗。权威认可：获FDA与CDE突破性疗法认定，2023 年获盖伦奖（医药界 “诺贝尔奖”）。上市情况玛伐凯泰胶囊（迈凡妥®）由百时美施贵宝研发，2022年4月在美国全球首发，2024年4月获中国NMPA优先审评批准、10月正式上市，同年11月纳入国家医保乙类；目前已在欧盟、加拿大、韩国等多国获批，海外仿制药已于2024 年上市，中国市场仍以原研药为主，获批适应症为NYHA II–III级成人梗阻性肥厚型心肌病。中国上市获批时间：2024年4月24日（NMPA，优先审评）医保：2024年11月纳入国家医保乙类，为首款进入医保的oHCM靶向药规格：2.5mg×28 粒；5mg×28 粒；10mg/15mg。获批适应症：NYHA II–III级成人oHCM，改善运动能力与症状。全球上市美国：2022 年 4 月（FDA，全球首个）；欧盟：2023 年（含英、德、法等）；其他国家 / 地区：加拿大、澳大利亚、巴西、韩国、新加坡、中国香港 / 澳门、瑞士、阿联酋等；获批适应症：同中国（NYHA II–III 级成人oHCM）。中国上市获批时间：2024年4月24日（NMPA，优先审评）医保：2024年11月纳入国家医保乙类，为首款进入医保的oHCM靶向药规格：2.5mg×28 粒；5mg×28 粒；10mg/15mg。获批适应症：NYHA II–III级成人oHCM，改善运动能力与症状。参比制剂注册与受理情况临床试验情况专利情况核心专利（中国）：原研公司为MyoKardia（被BMS收购）化合物/活性成分专利：CN109311854于2018-08-03申请，预估2034-06-19到期。医药用途专利：CN118593507（肥厚型心肌病），预估2034-06到期。组合物/制剂专利：同核心到期日，2034-06。美国：基础化合物专利US9181200预计2034-06-19到期；分案/延续（USRE50050）预计2036-04-28到期。欧盟/日本/韩国：与中国同族，2034年中到期。专利保护关键点保护期长：核心专利至2034年，独占期充足；专利壁垒高：化合物+用途+制剂三重核心，难以规避； BMS策略：收购MyoKardia后全球专利强化，延长独占至2036年（美国）。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 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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【药品分享】柯美奇拜单抗注射液——鼻用糖皮质激素治疗后症状控制不佳的成人中重度季节性过敏性鼻炎患者的福音【药品分享】吉诺昔替尼——口服小分子JAK1/TYK2双重抑制剂【药品分享】洛替拉纳（Lotilaner）——GABA 门控氯离子通道非竞争性拮抗剂 || 兼具兽医驱虫与人用眼科两大用途【药品分享】CagriSema——由卡格列肽（cagrilintide）2.4 mg与司美格鲁肽（semaglutide）2.4 mg组成的强效减重复方药【药品分享】苹果酸卡博替尼——口服、多靶点酪氨酸激酶抑制剂（TKI）【药品分享】迪高替尼（Delgocitinib）——一款外用泛JAK抑制剂【药品分享】拉氟莫司(Laflunimus)——口服免疫抑制剂 || 兼具免疫抑制与抗炎双重活性【药品分享】伏昔尼布片——全球首个IDH1/IDH2双重突变抑制剂靶向药【药品分享】盐酸奥昔布宁片——M受体抗胆碱药【药品分享】贝泽昔替尼片——国内首款获批的高选择性JAK2单靶点抑制剂【药品分享】苯甲酸安达艾替尼胶囊——新型小分子酪氨酸激酶不可逆抑制剂（EGFR-TKI）【药品分享】伏欣奇拜单抗注射液——全人源抗IL‑1β单克隆抗体 || 用于急性痛风性关节炎的1类创新生物药【药品分享】利多卡因丁卡因乳膏【药品分享】伐米奇拜单抗注射液——玻璃体内注射用抗IL-6人源化单抗【药品分享】依赛弗酶α注射液（Efzimfotase alfa 注射液）——第二代重组组织非特异性碱性磷酸酶（TNSALP）酶替代疗法【药品分享】格达托利西布（Gedatolisib）——first‑in-class 泛 PI3K/mTORC1/2 双重抑制剂【药品分享】伯瑞替尼肠溶胶囊——中国原研、高选择性c-MET小分子抑制剂 || 首个获批MET扩增NSCLC单药治疗的靶向药【药品分享】力胜克拉片——中国首个申报上市的原研Bcl-2抑制剂、全球第二款Bcl-2抑制剂【药品分享】BGM0504注射液——GLP-1/GIP 双受体激动剂【药品分享】塞利尼索片——全球首个口服选择性核输出蛋白XPO1抑制剂【药品分享】Seltorexant薄膜包衣片——选择性食欲素2受体（OX2R）高选择性拮抗剂【药品分享】盐酸埃克替尼片——国内首个自主研发的一代EGFR-TKI 【药品分享】盐酸伊普可泮胶囊——全球首个口服补体B因子抑制剂【药品分享】恩考芬尼胶囊——靶向BRAF V600突变的口服激酶抑制剂【药品分享】Enpatoran——口服、选择性TLR7/8小分子抑制剂【药品分享】硝酸异康唑阴道片——抗真菌外用药物【药品分享】Zorevunersen注射液——全球独家ASO上调蛋白表达技术【药品分享】妥拉美替尼胶囊——全球首个针对NRAS突变黑色素瘤的MEK抑制剂【药品分享】盐酸替那帕诺片——全球首创NHE3抑制剂类新型降磷药物【药品分享】注射用莱古比星——新型蒽环类抗肿瘤药【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】伊那利塞片——中国首个PIK3CA突变乳腺癌精准靶向药【药品分享】呋喹替尼胶囊——中国首个自主研发VEGFR-TKI || VEGFR靶点靶向抗癌药【药品分享】琥珀酸瑞波西利片——CDK4/6抑制剂【药品分享】盐酸替那帕诺片——全球首个且唯一获批的肠道磷吸收抑制剂【药品分享】芬布替尼片——口服、可逆、可透过血脑屏障的BTK抑制剂【药品分享】炔丙基半胱氨酸胶囊——全球首个进入临床的硫化氢（H₂S）供体I类创新药【药品分享】Balcinrenone达格列净胶囊——选择性盐皮质激素受体拮抗剂（MRA）+SGLT-2抑制剂【药品分享】诺拉西班（Nolasiban）分散片——选择性口服催产素受体拮抗剂 || 早产二线/辅助治疗药物【药品分享】塞多明基注射液——国内首款裸质粒基因治疗药物【药品分享】鲁兹诺雷钠片——国产首个高选择性URAT1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。

2026-06-01

·BioSpace

New analysis of Idorsia’s aprocitentan demonstrates significant and sustained reduction in albuminuria in patients with uncontrolled / resistant hypertension

The findings demonstrate that aprocitentan may help reduce the risk of kidney disease progression, cardiovascular events, and mortality in patients with resistant hypertension. Allschwil, Switzerland – June 01, 2026 Idorsia Ltd (SIX: IDIA) announces new analyses from the Phase 3 PRECISION study demonstrating that aprocitentan, Idorsia’s dual endothelin receptor antagonist, significantly reduces albuminuria and improves albuminuria risk categories in patients with resistant hypertension. The data were presented by Prof. Markus Schlaich at the 35th Congress of the European Society of Hypertension (ESH). The oral presentation, entitled “ Effect of the Dual Endothelin Receptor Antagonist Aprocitentan on Albuminuria ”, underscores the role of endothelin pathway inhibition not only in blood pressure control, but also in addressing kidney-related risk in this high-risk population, further supporting the evidence presented in Hypertension titled “ Aprocitentan in Patients with Chronic Kidney Disease and Resistant Hypertension ”. Addressing a critical unmet need in resistant hypertension Hypertension remains the leading modifiable risk factor for cardiovascular disease and premature death, with patients whose blood pressure is difficult to control facing even higher risks of stroke, myocardial infarction, heart failure, and kidney disease. In resistant hypertension in particular, chronic kidney disease and type 2 diabetes are common and contribute to poor long-term outcomes. Albuminuria, measured as urine albumin-creatinine ratio (UACR), is a well-established biomarker of kidney damage and is strongly associated with increased cardiovascular morbidity and mortality, and more rapid progression towards kidney failure. Albuminuria is more commonly observed in conditions such as Type 2 diabetes and hypertension, as well as older age. Changing to a lower risk category, as a result of lowering albuminuria is therefore an important therapeutic objective beyond blood pressure lowering. Potential to improve long-term renal and cardiovascular outcomes By lowering albuminuria and shifting patients to lower risk categories, aprocitentan may help reduce the risk of kidney disease progression and cardiovascular risk in patients with difficult-to-control hypertension. Prof. Markus Schlaich, MD, FAHA, FESC, ISHF, The University of Western Australia, Perth, and lead investigator in the PRECISION study commented: “These data represent a major step forward in the management of difficult-to-control hypertension. By targeting the endothelin pathway, aprocitentan not only delivers robust and sustained blood pressure reductions, but also drives clinically meaningful improvements in albuminuria – an established marker of kidney and cardiovascular risk. The ability to lower albuminuria risk category in nearly half of these high-risk patients underscores the potential of aprocitentan to change the treatment paradigm and deliver tangible long-term benefits for patients who remain inadequately controlled on current therapies, particularly those in whom treatment decisions are complicated by the risk of hyperkalemia.” New PRECISION analysis: meaningful reductions in albuminuria The new analysis evaluated the effect of aprocitentan in 730 patients with confirmed resistant hypertension receiving at least three antihypertensive agents, including a diuretic. Key findings include: Rapid and substantial reductions in UACR: In patients with baseline microalbuminuria (UACR 30–300mg/g) and macroalbuminuria (UACR >300mg/g), aprocitentan significantly reduced UACR at Week 4 compared with minimal changes on placebo. Sustained long-term effects: By Week 36, treatment with aprocitentan 25 mg reduced mean UACR: From 77.5 mg/g to 34 mg/g in patients with microalbuminuria From 860.2 mg/g to 286.7 mg/g in patients with macroalbuminuria Early improvement/normalization in albuminuria risk category: As early as Week 4: Up to 45% of patients with microalbuminuria achieved normal albumin levels with aprocitentan Up to 39% of patients with macroalbuminuria improved to a lower risk category At Week 36, approximately 46% of patients with baseline micro- or macroalbuminuria achieved a lower albuminuria risk category Stable eGFR in both microalbuminuria and macroalbuminuria eGFR did not decline but remained stable, confirming the renal protective effect of aprocitentan Preservation of normal kidney status: More than 92% of patients with normal albumin levels at baseline remained within the normal range during treatment. Targeting endothelin: a novel and clinically meaningful mechanism Idorsia’s Chief Scientific Officer & Head of Research, Martine Clozel, also spoke at the event with a presentation entitled “From dream to reality: improving lives though endothelin-related innovations”. Aprocitentan, Idorsia’s dual endothelin receptor antagonist approved as TRYVIO™ in the US and as JERAYGO™ in Europe, is the first therapy of its kind to target the endothelin pathway in systemic hypertension. Endothelin is a key driver of vasoconstriction, inflammation, fibrosis, and organ damage, and is often upregulated in patients with resistant hypertension and kidney disease. The findings from this analysis reinforce the central role of endothelin in both the development and consequences of hypertension, including the potential to reduce kidney damage progression and long-term cardiovascular risk. Unlike therapies targeting the renin–angiotensin–aldosterone system (RAAS) pathway, which may be associated with electrolyte disturbances such as hyperkalemia, endothelin receptor antagonism with aprocitentan has not demonstrated an increased risk of hyperkalemia. Building on proven blood pressure efficacy The albuminuria data complement previously reported results from PRECISION, where aprocitentan demonstrated: Rapid, double-digit reductions in systolic blood pressure Sustained efficacy over 48 weeks Consistent effects across office and ambulatory measurements Consistent blood pressure reductions across key patient subpopulations, including those with high-risk comorbidities Importantly, the treatment effect was maintained in patients with common and clinically relevant comorbidities, including type 2 diabetes, obesity (including severe obesity), chronic kidney disease, and congestive heart failure, as well as across demographic subgroups such as older patients and those with higher cardiovascular risk pro Aprocitentan has also shown a manageable safety profile, with mild and transient edema as the most commonly observed treatment-related effect and no significant drug–drug interactions – an important consideration in patients with complex regimens. Importantly, no signal for hyperkalemia or hyponatremia was observed, supporting its use in patients with resistant and difficult-to-control hypertension, including those with chronic kidney disease, even with an eGFR (estimated glomerular filtration rate) as low as 15ml/min/1.73m 2 , diabetes, or heart failure, without additional electrolyte monitoring burden. About aprocitentan Aprocitentan is approved as TRYVIO ® in the US for the treatment of systemic hypertension in combination with other antihypertensives and has been commercially available since October 2024. TRYVIO is now included in the American College of Cardiology’s (ACC) and the American Heart Association’s (AHA) new comprehensive clinical practice guidelines for the management of high blood pressure. Aprocitentan is approved as JERAYGO ® for the treatment of resistant hypertension in combination with other antihypertensives in the European Union, the UK, and Switzerland, and a marketing authorization application is under review in Canada. Notes to the editor About Prof. Markus Schlaich, MD Markus Schlaich is a nephrologist and a European Society of Hypertension (ESH) accredited hypertension specialist. He is a Fellow of the American Heart Association (FAHA), the European Society of Cardiology (FESC), and the International Society of Hypertension (ISHF). He served as an Executive Committee of the ISH from 2018-2020 and is currently on the Management Board of the global ISH May Measurement Month campaign. Markus is President of Hypertension Australia and a Trustee of the Foundation for High Blood Pressure Research. Markus has a strong background in clinical research with a focus on the pathophysiology of hypertension, involvement of the kidneys, and hypertension mediated organ damage. He has a specific interest in treatment modalities targeting the sympathetic nervous system and other relevant pathways such as the endothelin system to improve BP control and thereby outcomes for patients with difficult-to-control hypertension. For his work he received the Björn Folkow Award from the European Society of Hypertension (ESH) and the Arthur C. Corcoran Award from the AHA Hypertension Council, both in 2021. He has authored more than 450 articles in peer-reviewed journals and serves on the Editorial Board of Hypertension and Journal of Hypertension. Prof. Schlaich serves as a consultant to Idorsia. Key literature Danaietash P et al. Identifying and treating resistant hypertension in PRECISION: A randomized long-term clinical trial with aprocitentan. J Clin Hypertension 2022 Jul;24(7):804-813. Schlaich MP, et al. A randomized controlled trial of the dual endothelin antagonist aprocitentan for resistant hypertension. The Lancet, 2022; Dec 3;400(10367):1927-1937. Rossignol P, et al. Aprocitentan in Patients With Chronic Kidney Disease and Resistant Hypertension. Hypertension. Online ahead of print, December 2025, doi.org/10.1161/HYPERTENSIONAHA.125.25563 Iglarz M, et al. At the heart of tissue: endothelin system and end-organ damage. Clin Sci 2010; 119:453-63. Clozel M. Aprocitentan and the endothelin system in resistant hypertension. Can J Physiol Pharmacol 2022; 100:573-83. About Idorsia The purpose of Idorsia is to discover, develop and commercialize innovative medicines to help more patients. To achieve this, we will develop 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: Investor & Media 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

临床结果临床3期上市批准AHA会议

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外链

KEGG	Wiki	ATC	Drug Bank
D11441	-	-	DB15059

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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

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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	-	Idorsia Pharmaceuticals Ltd.	2020-01-01
慢性肾病	临床3期	-	Janssen Biotech, Inc.	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

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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	繭築獵憲顧襯襯範築獵(醖艱蓋鬱範鏇夢鬱餘簾) = 觸簾襯衊選鹽獵鏇夢窪糧鬱壓願顧醖積廠淵夢 (鑰淵鑰淵繭壓網醖繭築 )	积极	2025-04-01
				Aprocitentan 25 mg	繭築獵憲顧襯襯範築獵(醖艱蓋鬱範鏇夢鬱餘簾) = 鏇淵遞鏇鹽淵願膚製遞糧鬱壓願顧醖積廠淵夢 (鑰淵鑰淵繭壓網醖繭築 )
PRECISION (ASN2024)	临床3期	难治性高血压	838	Aprocitentan 12.5 mg	遞鏇鬱鏇鑰餘鹹齋糧糧(積獵醖憲顧淵構淵糧襯) = 構觸網壓顧夢網鹹窪觸夢淵艱襯鬱淵製窪築窪 (鹹範齋顧窪網蓋範壓製 )	积极	2024-10-26
				Aprocitentan 25 mg	遞鏇鬱鏇鑰餘鹹齋糧糧(積獵醖憲顧淵構淵糧襯) = 積製齋願憲餘顧網衊糧夢淵艱襯鬱淵製窪築窪 (鹹範齋顧窪網蓋範壓製 )
PRECISION (ESH2024)	临床3期	难治性高血压	93	Aprocitentan 12.5 mg	餘顧獵鏇顧範齋膚夢簾(襯鹹繭範蓋築築鑰齋鏇) = 齋夢範衊鏇壓膚廠窪鏇構鑰選蓋醖鏇餘繭窪鏇 (遞艱獵獵醖憲遞網淵願 ) 更多	积极	2024-05-01
				Aprocitentan 25 mg	餘顧獵鏇顧範齋膚夢簾(襯鹹繭範蓋築築鑰齋鏇) = 淵遞齋糧網廠膚壓艱鏇構鑰選蓋醖鏇餘繭窪鏇 (遞艱獵獵醖憲遞網淵願 ) 更多
PRECISION (ESH2024)	临床3期	难治性高血压	-	Aprocitentan 12.5 mg	壓構積廠憲選艱繭範鏇(鏇艱糧積夢蓋選遞糧艱) = 餘廠鑰憲顧選鹽艱製襯憲艱夢築網築壓積鏇觸 (鑰窪艱簾鏇淵獵糧膚鑰 )	积极	2024-05-01
				Aprocitentan 25 mg	壓構積廠憲選艱繭範鏇(鏇艱糧積夢蓋選遞糧艱) = 夢衊願夢範襯壓餘選壓憲艱夢築網築壓積鏇觸 (鑰窪艱簾鏇淵獵糧膚鑰 ) 更多
NCT03541174 (FDA) 人工标引	临床3期	高血压	-	Aprocitentan (12.5 mg)	艱餘積簾顧觸觸襯積觸(鹽簾襯窪鏇鬱鹽範鏇憲) = 餘鹹鹹夢夢獵襯獵顧鬱範網鹹廠顧積齋膚壓窪 (醖襯窪艱鬱選鏇糧製觸, −17.5 ~ −13.3) 更多	优效	2024-03-19
				Placebo	艱餘積簾顧觸觸襯積觸(鹽簾襯窪鏇鬱鹽範鏇憲) = 醖蓋顧鹽製餘築醖獵鹹範網鹹廠顧積齋膚壓窪 (醖襯窪艱鬱選鏇糧製觸, −13.7 ~ −9.5) 更多
PRECISION (ESH2023)	临床3期	难治性高血压	730	Aprocitentan 12.5 mg	夢壓簾鬱獵鏇積築艱範(積膚範夢憲夢襯遞築顧) = 簾範遞衊襯膚齋簾襯廠襯願積蓋獵願餘鹹鏇獵 (淵鹽壓蓋鬱廠獵鏇襯膚 )	积极	2023-06-01
				Aprocitentan 25 mg	夢壓簾鬱獵鏇積築艱範(積膚範夢憲夢襯遞築顧) = 鑰獵願餘壓窪窪繭齋簾襯願積蓋獵願餘鹹鏇獵 (淵鹽壓蓋鬱廠獵鏇襯膚 )
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))	製網膚觸醖廠淵鑰願願(範壓廠鬱遞窪積襯簾艱) = 構襯觸餘網鹽築鹹網鏇獵範鏇膚夢鹹簾獵壓糧 (壓蓋願衊壓鏇鏇膚繭願, 糧壓鏇蓋齋窪繭淵鑰獵 ~ 膚積獵製願鏇鏇襯築衊) 更多	-	2023-03-21
				Aprocitentan 25 mg (Aprocitentan 25 mg in Part 1 (Double-blind))	製網膚觸醖廠淵鑰願願(範壓廠鬱遞窪積襯簾艱) = 鬱願醖鹹積窪膚構網選獵範鏇膚夢鹹簾獵壓糧 (壓蓋願衊壓鏇鏇膚繭願, 簾衊夢廠顧網夢憲簾範 ~ 窪構衊遞簾夢願獵蓋網) 更多
NCT02603809 (CTgov)	临床2期	原发性高血压	1,659	Placebo (Placebo)	夢壓膚遞繭淵糧範選壓(網繭觸鏇壓鏇簾遞憲窪) = 選鹹鏇夢鬱獵鏇窪鬱繭網夢鹹糧齋憲獵醖夢構 (糧繭簾窪製鹹選鹽網鏇, 5.4) 更多	-	2020-04-13
				Aprocitentan 5 mg (Aprocitentan 5 mg)	夢壓膚遞繭淵糧範選壓(網繭觸鏇壓鏇簾遞憲窪) = 範範鹹遞鏇蓋窪餘齋鏇網夢鹹糧齋憲獵醖夢構 (糧繭簾窪製鹹選鹽網鏇, 5.5) 更多
NCT02603809 (ESC2019)	临床2期	高血压	490	Aprocitentan 5 mg	齋壓窪膚憲廠齋膚鹹襯(觸淵積築選齋築構顧積) = 蓋獵鹽糧鹹鏇鏇選顧遞鑰淵範獵齋齋鏇鏇憲餘 (鹹繭壓糧製艱鏇製觸顧 ) 更多	-	2019-08-31
				Aprocitentan 10 mg	齋壓窪膚憲廠齋膚鹹襯(觸淵積築選齋築構顧積) = 鹹製壓顧淵鏇鏇鬱壓鬱鑰淵範獵齋齋鏇鏇憲餘 (鹹繭壓糧製艱鏇製觸顧 ) 更多