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.

NCT04252495

/ Completed临床1期

An Open-label Phase 1 Study to Investigate the Effect of Moderate Hepatic Impairment Due to Liver Cirrhosis on the Pharmacokinetics of a Single Dose of 25 mg Aprocitentan

This is a prospective, open-label, single-dose, Phase 1 study, to assess the effect of moderate hepatic impairment due to liver cirrhosis on the pharmacokinetics of aprocitentan (ACT-132577).

开始日期2020-06-26

申办/合作机构

Idorsia Pharmaceuticals Ltd.

100 项与 Aprocitentan 相关的临床结果

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100 项与 Aprocitentan 相关的转化医学

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100 项与 Aprocitentan 相关的专利（医药）

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项与 Aprocitentan 相关的文献（医药）

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.

2026-01-02·Current Hypertension Reviews

A New Drug for Resistant Hypertension: Aprocitentan

Article

作者: Lhamo, Yangshen ; Chopra, Deepti ; Sidhu, Jaspreet Kaur ; Goyal, Abhinav

Abstract::

Resistant hypertension (RH) is defined as uncontrolled blood pressure (BP) despite the use of three or more antihypertensive agents of different pharmacological classes. The treat-ment of resistant hypertension remains a challenge, as it is associated with a heightened risk of cardiovascular events. Many preclinical studies have demonstrated the importance of the endo-thelin pathway in resistant hypertension; however, the therapeutic application of endothelin an-tagonists in clinical practice has been limited due to various factors. Recently, in March 2024, the FDA approved aprocitentan, an orally active endothelin-1 (ET-1) receptor antagonist that inhibits the binding of ET-1 to ETA and ETB receptors. This is the first medication with a novel mechanism for the treatment of resistant hypertension. This review aims to summarise the avail-able evidence on the discovery, chemical nature, pharmacokinetics, pharmacodynamics, effi-cacy, and safety of the novel drug aprocitentan in the pharmacotherapy of resistant hyperten-sion. The landmark PRECISION trial demonstrated a significant BP-lowering effect with the use of the dual endothelin receptor antagonist aprocitentan in the treatment of resistant hyper-tension. Aprocitentan was shown to be particularly effective in patients over 75 years of age, those with a higher cardiovascular-risk profile, patients with diabetes, and individuals with ad-vanced chronic kidney disease (CKD). As a dual receptor antagonist, aprocitentan demonstrated a lower risk of fluid retention and vascular leakage, adverse effects previously observed with other endothelin receptor antagonists. Its mechanism of action, improved efficacy, and excellent tolerability make aprocitentan a promising therapeutic option for resistant hypertension. It may be particularly effective in the treatment of patients with comorbidities, such as diabetes and CKD.

2026-01-01·JAAPA-Journal of the American Academy of Physician Assistants

Aprocitentan, an endothelin receptor antagonist for resistant hypertension

Review

作者: Weidman-Evans, Emily ; Ferrington, Lindsay

ABSTRACT:

Resistant hypertension (RH) is defined as blood pressure (BP) that remains uncontrolled with use of three or more antihypertensive medications or BP that is controlled with use of four antihypertensive medications. Aprocitentan is a newly approved drug for RH, offering a mechanism unique from currently available antihypertensive drugs. It serves to block endothelin-A and endothelin-B to reduce vasoconstriction. The drug, which is taken once daily, has been shown to yield sustainable reductions in BP across various settings, and it may be especially beneficial for those with chronic kidney disease. Risks with use include fluid retention, anemia, mild hepatic enzyme elevations, and—though less common than with other endothelin antagonists—hepatotoxicity. Aprocitentan is contraindicated in pregnancy, as it includes a boxed warning for embryo-fetal toxicity. Although this new drug expands available options for RH, it requires careful patient selection and monitoring. Finally, cost and insurance coverage may limit access.

146

项与 Aprocitentan 相关的新闻（医药）

2026-01-29

·医脉通心血管

导语：高血压作为全球重大的公共卫生问题之一，其防治成效直接关系到全民健康水平的提升。近年来，随着医学技术的不断革新，高血压防治已从传统的对症治疗迈向精准化、多维度干预的新阶段。创新药物的迭代升级、器械治疗的突破性应用、继发性高血压的精准筛查，为破解临床困境提供了全新路径。其中，醛固酮失调作为高血压发病的核心机制之一，其相关治疗的创新探索尤为引人注目，从传统受体拮抗剂到新一代合成酶抑制剂的研发突破，正重塑高血压精准治疗的格局。在2025年高血压年会（CHM 2025）期间，上海交通大学医学院附属瑞金医院王继光教授及中南大学湘雅三医院袁洪教授分别进行了以《高血压治疗的创新和发展》和《醛固酮路径创新解读：机制探索与临床应用新进展》为主题的讲座，系统梳理高血压治疗的创新进展，深入解析醛固酮相关机制与治疗新进展，为临床实践与学科发展提供参考。高血压治疗的创新和发展作为全球范围内的重大公共卫生挑战之一，高血压防治目前正从平台期迈向全新的创新阶段。根据我国不同年份的流行病学数据，1991年至2012年间，高血压的知晓率、治疗率和控制率虽呈逐步上升趋势，但截至2012年，仍有半数左右患者未接受规范治疗，大量患者的血压未能达标，亟需创新手段破解。近年来，在高血压治疗领域取得了诸多进展，主要集中在创新药物研发、器械治疗突破和继发性高血压精准筛查三方面。创新药物研发（1）血管紧张素受体脑啡肽酶抑制剂（ARNI ） ARNI类药物的应用拓展是近年来高血压领域取得的重要突破之一。 2021年，原本用于心衰治疗的沙库巴曲缬沙坦被拓展应用于高血压治疗。作为一款强效降压药物，其可显著降低收缩压与舒张压，且疗效确切。目前，沙库巴曲缬沙坦已在国内普遍应用，不仅推动了ARNI类药物在高血压领域的发展，更带动了日本、马来西亚及越南等亚洲国家ARNI类药物的临床应用。沙库巴曲阿利沙坦是我国自主研发的首款ARNI类降压药，2026年经中国国家药品监督管理局（NMPA）审批通过，正式获批用于原发性高血压治疗，且已于2025年12月被纳入《国家基本医疗保险、工伤保险和生育保险》。（2）Aprocitentan Aprocitentan是一种双重内皮素（ET）A/B受体（ETA/ETB）拮抗剂，可抑制ET-1与ETA和ETB受体的结合，从而降低血压。基于PRECISION试验结果，美国食品和药物管理局（FDA）已于2024年3月批准Aprocitentan用于治疗其他药物无法充分控制的成年难治性高血压（联合其他降压药物），尤其是在夜间高血压控制方面的疗效显著。（3）Baxdrostat 醛固酮合成酶抑制剂Baxdrostat的突破同样值得关注。2025年，其Ⅲ期临床试验BaxHTN研究的结果已于ESC年会重磅公布，并同步发表于《新英格兰医学杂志》。该药对醛固酮合成酶选择性达普通合成酶的100倍，能强效抑制醛固酮合成且不影响皮质醇水平，规避了传统药物相关副作用。研究共纳入796例未控制/难治性高血压患者，经12周治疗后，1mg、2mg组坐位收缩压经安慰剂校正后分别降低了8.7mmHg和9.8mmHg，降压效果稳定且亚组获益一致，24h及夜间血压控制优异，血清醛固酮降幅达60%-65%。安全性良好，高钾血症发生率低且多为轻度。目前亚洲人群试验（BaxAsia）正在推进，未来有望成为难治性高血压新疗法。（4）Zilebesiran 除传统小分子药物外，小干扰RNA类药物为高血压治疗开辟了新赛道。作为代表药物，Zilebesiran可利用小分子RNA技术沉默特定基因表达，影响细胞功能和代谢，从而发挥降低血压的作用。此类药物的最大优势在于单次注射即可实现3个月甚至6个月的长效降压效果，显著提高患者的治疗依从性。尽管部分二线临床试验结果存在差异，但明确的作用机制为其发展奠定了基础。目前，国内企业已启动相关研发工作，预计未来1-2年将取得重要进展。器械治疗突破在高血压器械治疗领域，肾动脉交感神经消融术（RDN）的获批与临床应用成为重要诊疗突破。2024年下半年，该技术在我国正式获批，上海等多地已率先将其纳入医保支付范围。 SPYRAL HTN-OFF MED PIVOTAL国际多中心试验证实，与假手术对照组相比，RDN可显著降低患者24h动态血压水平；且亚组分析及次要终点数据显示，RDN治疗对夜间和清晨这两个血压高峰时段的降压疗效尤为突出。Symplicity RDN 中国单臂多中心临床试验结果也显示，54例高血压患者接受RDN治疗后，诊室血压与 24h动态血压均实现有效控制；术后6个月，78%的患者收缩压控制在140 mmHg以下，50%的患者收缩压降至130 mmHg以下，同时患者的药物治疗负荷（药物种类及剂量）也显著降低。 RDN技术的稳步推广，不仅为难治性高血压患者提供了全新的治疗策略，更推动了高血压学科专业人才队伍的建设，为我国高血压领域的高质量发展注入了新动力。继发性高血压精准筛查继发性高血压的精准诊疗已成为我国高血压防治的重要创新方向，推动常见病因的系统性筛查、建立标准化诊断流程，更是提升临床治疗效果的核心举措。 ChinaPAPS研究证实，规范筛查可提升原发性醛固酮增多症治疗成功率。目前肾素和醛固酮化学发光法检测技术已逐步普及，临床可通过四步判断法实现原发性醛固酮增多症的精准筛查，助力高血压的精准管理。与此同时，阻塞型睡眠呼吸暂停综合征（OSA）合并高血压的规范化诊断与治疗推广也在全国稳步推进，《高血压患者阻塞性睡眠呼吸暂停筛查诊治流程》的发布，为临床开展OSA系统性筛查与针对性治疗提供了权威指南依据。通过完善继发性高血压精准筛查诊治体系、推进OSA合并高血压的规范化管理，以期通过不懈努力实现高血压患者的个体化精准控压，最终将我国高血压整体控制率提升至较高水平。降压醛固酮靶点相关机制及药物研发新进展醛固酮在高血压发生发展中的核心作用机制醛固酮在血压调节体系中的作用至关重要，且并非仅局限于肾脏，而是贯穿全身多个器官与系统，直接影响高血压的发生与进展。在肾脏，醛固酮通过促进钠离子与钾离子的排泄交换，导致钠潴留，进而引发血压升高，这是其最经典的作用路径。而在心肌组织中，醛固酮会诱导心肌纤维化，损害心脏结构与功能；在血管层面，它加速血管老化、硬化进程，增加血管僵硬度，加剧血压升高；在中枢神经系统，其可促进外周交感神经兴奋，进一步推动血压上升。临床数据明确证实，醛固酮水平与高血压严重程度呈显著剂量依赖性正相关。多中心研究显示，血清醛固酮水平与收缩压、舒张压均呈正相关，随醛固酮浓度升高，血压呈平稳递增趋势。2025 ESC年会上发表的研究显示，在接受两种降压药物治疗的患者中，若醛固酮/肾素比值（ARR）＞27.7pmol/mlU，该人群的ARR水平会进一步升高，且肾功能快速下降、主要心血管事件（MACE）发生率随ARR值升高呈上升趋势，凸显了醛固酮失调在高血压并发症进展中的关键作用。此外，醛固酮的作用机制还涉及经典与非经典两类受体。经典醛固酮受体激活后的不良效应已被临床广泛认知，而非经典受体体系（以GPER和EGFR为核心）在生理状态下具有心血管保护作用，可维持心血管系统稳态；但当醛固酮水平异常升高时，该体系的保护作用会转化为有害效应，进一步加重血管、心脏及肾脏的靶器官损伤。醛固酮相关降压药物的发展与现状（1）醛固酮受体拮抗剂：优势与局限并存醛固酮受体拮抗剂的发展核心聚焦于高选择性优化，其目的是减少性激素相关副作用，避免对性激素受体的非特异性影响。但该类药物仍面临两大关键挑战：一是降压效应有限；二是存在醛固酮水平反跳上升的问题，尽管高选择性药物减少了副作用，但未能从根本上解决醛固酮水平增高的核心矛盾，且无法阻断非经典受体激活带来的不良影响。（2）醛固酮合成酶抑制剂：降压治疗新突破醛固酮合成酶抑制剂已历经50年的研究历程，早期药物因作用靶点CYP11B缺乏完全选择性（CYP11B2为醛固酮合成关键酶，CYP11B1为皮质醇合成关键酶），长期未能实现突破性进展。新一代高选择性醛固酮合成酶抑制剂的选择性明显升高，仍可能对CYP11B1有轻度影响，但总体无明显不良效应，且展现出显著优势：其一，降压效果突出，如Baxdrostat在1 mg、2mg剂量下均能实现强效降压，远超传统受体拮抗剂；其二，可同时降低血压与生物标志物水平，在有效控制24h血压的同时，显著改善醛固酮与肾素水平，从源头解决醛固酮失调问题。值得一提的是，目前该类药物的临床证据不断积累，二期与三期临床试验均取得积极结果，已成为众多专家/学者认可的高血压治疗新靶点。两类药物的临床应用展望综合现有研究证据与药物特性，醛固酮合成酶抑制剂凭借其强效降压、源头调控醛固酮水平的优势，在高选择性研发持续推进与更多临床证据积累的背景下，有望成为高血压治疗的主要药物之一，尤其适用于醛固酮水平异常增高的高血压患者及合并心血管并发症风险的人群。醛固酮受体拮抗剂虽存在一定局限，但仍具临床应用价值。其作用靶点相对精准，在部分特殊病例中可发挥补充治疗作用，如对合成酶抑制剂不耐受或存在使用禁忌的患者，仍能提供有效的血压控制选项。不过，两类药物目前缺乏头对头直接比较研究，临床应用中仍需基于循证医学证据，结合患者个体情况与临床经验谨慎选择，并开展进一步研究以明确最优适用人群与治疗方案。结语近年来，高血压治疗领域呈现出诸多创新突破，从ARNI类药物、醛固酮合成酶抑制剂等创新药物的迭代，到RDN器械治疗的临床普及，再到继发性高血压的精准筛查，逐步推动高血压防治从传统对症治疗迈向精准化、多维度干预新阶段。其中，醛固酮靶点相关研究的深入突破尤为关键，新一代合成酶抑制剂破解了传统药物的局限，与受体拮抗剂形成互补。未来，随着更多临床证据积累、技术与药物的推广应用，将进一步完善高血压精准治疗体系，助力提升全民高血压控制率，为高血压防治事业注入新动力。医脉通是专业的在线医生平台，“感知世界医学脉搏，助力中国临床决策”是平台的使命。医脉通旗下拥有「临床指南」「用药参考」「医学文献王」「医知源」「e研通」「e脉播」等系列产品，全面满足医学工作者临床决策、获取新知及提升科研效率等方面的需求。本平台旨在为医疗卫生专业人士传递更多医学信息。本平台发布的内容，不能以任何方式取代专业的医疗指导，也不应被视为诊疗建议。如该等信息被用于了解医学信息以外的目的，本平台不承担相关责任。本平台对发布的内容，并不代表同意其描述和观点。若涉及版权问题，烦请权利人与我们联系，我们将尽快处理。

2026-01-24

·搜狐新闻

药渡经纬：2026年药渡全球药物研发进展报告-创新药篇

今天分享的是：药渡经纬：2026年药渡全球药物研发进展报告-创新药篇报告共计：61页2026年1月3日-9日全球及国内创新药研发进展总结2026年1月3日至9日，全球与国内创新药领域成果丰硕，在药物批准、临床研发、企业合作及政策优化等方面均有重要突破，为疾病治疗带来新可能。全球层面，新药批准与研发动态亮点突出。统计周期内，全球有4条新药批准状态更新，含NDA批准2个、BLA批准1个及新制剂批准1个。Idorsia的Aprocitentan获加拿大卫生部批准用于成人难治性高血压，葛兰素史克的超长效生物制剂Exdensur在日本获批，用于治疗重度或难治性支气管哮喘等疾病，一年仅需注射两次即可持续抑制2型炎症。全球新药临床研发状态更新达60条，覆盖17个领域，歌礼制药的口服小分子GLP-1 ASC30获FDA批准开展II期研究，信达生物的VEGF/Ang2双特异性抗体IBI324在相关眼病治疗中展现出优异疗效。同时，全球医药交易活跃，多类合作与许可协议达成，涉及肿瘤、代谢疾病等多个治疗领域。国内方面，创新药发展势头强劲。新药批准状态更新15条，涵盖NDA、BLA、新复方、新适应症及新制剂等类型。恒瑞医药的全球首款PD-L1/TGF-βRII双抗瑞拉芙普α注射液获批上市，用于特定胃癌治疗；赛诺菲的瑞达普®获批，破解了家族性乳糜微粒血症综合征在中国“无药可控”的困局。国内47个新药获临床默示许可，16个新药申报上市，74个新药申报临床，涉及化药、生物制品等多个品类。华奥泰的Sotiburafusp alfa启动III期临床，复宏汉霖的HLX-43公布III期临床试验方案设计。政策层面，国家药监局发布多项公告，优化临床急需境外已上市药品审评审批机制，缩短注册检验时限，完善注册核查方式，推动药品注册技术标准与国际接轨。此外，国内外企业合作频繁，宜联生物与罗氏再度联手加速B7H3 ADC全球开发，国内企业间也在靶向药物等领域积极开展合作，为创新药的研发与商业化注入动力。整体来看，该周期内创新药领域在多疾病赛道实现技术突破，政策支持与企业协作共同推动行业持续发展，为患者带来更多治疗选择。以下为报告节选内容返回搜狐，查看更多

2026-01-05

·BioSpace

Idorsia’s JERAYGO (aprocitentan) approved in Canada for the treatment of resistant hypertension

Idorsia receives approval from Health Canada for JERAYGO ™ (aprocitentan) as the first and only endothelin receptor antagonist (ERA) for the treatment of resistant hypertension. JERAYGO is a new oral antihypertensive therapy – the first systemic hypertension treatment to target a new pathway in over 30 years. Allschwil, Switzerland – January 5, 2026 Idorsia Ltd (SIX: IDIA) announces that Health Canada has granted marketing authorization for JERAYGO ™ (aprocitentan) for the treatment of resistant hypertension in adult patients in combination with at least three antihypertensive medicinal products. 1 The recommended dose is 12.5 mg orally once daily. The dose can be increased to 25 mg once daily for patients tolerating the 12.5 mg dose and in need of tighter blood pressure (BP) control. 1 Hypertension remains a leading global health challenge and the number one modifiable risk factor for early morbidity and mortality. Despite advances in treatment, many patients still struggle with uncontrolled blood pressure, leaving them at significantly higher risk of heart attack, stroke, kidney failure, and premature death. Approximately 10% of hypertensive patients have resistant hypertension 3 , 4 – defined by uncontrolled blood pressure despite receiving at least three antihypertensive medications from different classes, at optimal doses – underscoring the urgent need for more effective therapies. Srishti Gupta, MD, Chief Executive Officer of Idorsia, commented: “JERAYGO is the first and only hypertension treatment to target the endothelin pathway, a fundamental yet previously unaddressed driver of disease onset, progression, and complications. The results of PRECISION show that targeting the endothelin pathway is crucial to adequately manage uncontrolled blood pressure. JERAYGO has demonstrated rapid, durable, and clinically significant double-digit blood pressure reduction across a broad spectrum of challenging patient populations, including those with obesity, chronic kidney disease, or type 2 diabetes. I am very proud of our team for achieving this milestone.” Idorsia is engaged in discussions to maximize the ability to make JERAYGO available to patients. For more information on the marketing authorization of JERAYGO in Canada and important safety information, please review the Product Monograph . Notes to the editor About the Phase 3 PRECISION study 1,5 The efficacy of aprocitentan was evaluated in one randomized, double-blind (DB), placebo-controlled Phase 3 multicenter study. Patients with uncontrolled blood pressure (systolic blood pressure [SBP] ≥140 mmHg) despite the use of at least three antihypertensive medicinal products and following exclusion of pseudo-resistant hypertension (e.g., white coat effect, inappropriate blood pressure measurement, secondary causes of hypertension) were considered to have resistant hypertension. The patients were switched to standardized background antihypertensive therapy consisting of an angiotensin receptor blocker (valsartan 160 mg), a calcium channel blocker (amlodipine 5 or 10 mg), and a diuretic (hydrochlorothiazide 25 mg) throughout the study. Patients with concomitant use of beta-blockers continued this treatment throughout the study, in addition to the standardized background antihypertensive therapy and study treatment. A total of 730 patients received either aprocitentan 12.5 mg, aprocitentan 25 mg, or placebo once daily during the initial 4-week DB treatment (part 1). Thereafter, patients received aprocitentan 25 mg once daily during the 32-week single-blind treatment (part 2). At the end of the 32 weeks, patients were re-randomized to receive either aprocitentan 25 mg or placebo, once daily, during the 12-week double-blind withdrawal (DB-WD) treatment (part 3). The primary efficacy endpoint was the change in sitting SBP (SiSBP) from baseline to Week 4 during DB treatment (part 1), measured at trough by unattended automated office blood pressure (uAOBP). The key secondary endpoint was the change in SiSBP measured at trough by uAOBP from DB-WD baseline (Week 36) to Week 40 (part 3). Patients had a mean age of 61.7 years (range 24 to 84 years; 34.1% were ≥ 65 and < 75 years; 9.9% were ≥ 75 years) and 59.5% were male. Patients were White (82.9%), African American (11.2%) or Asian (5.2%). The mean body weight was 97.6 kg (range 46 to 196 kg) and mean BMI was 33.7 kg/m2 (range 18 to 64 kg/m2). Patients had a medical history of type 2 diabetes mellitus (54.1%), ischemic heart disease (30.8%), central nervous system vascular disorders (23.0%), chronic kidney disease stages 3 and 4 (22.2%; 19.3% of patients had eGFR 30–59 mL/min/1.73 m2 and 2.9% had eGFR 15–29 mL/min/1.73 m2), congestive heart failure (19.6%), and sleep apnea syndrome (14.1%). 63.0% of patients had four or more antihypertensive medicinal products. Key PRECISION findings 1,5 Doses of aprocitentan 12.5 and 25 mg showed a statistically significant reduction vs placebo on SiSBP at Week 4. The treatment effect was consistent for sitting diastolic blood pressure (SiDBP). The persistence of the BP-lowering effect of aprocitentan was shown in DB-WD treatment (part 3). In patients re-randomized to placebo, the mean SiSBP increased, whereas in patients re-randomized to aprocitentan 25 mg the mean effect on SiSBP was stable, resulting in a statistically significant difference. The treatment effect was consistent for SiDBP. The effect was also consistent across SBP and DBP measured by ambulatory BP monitoring (ABPM) and assessed as daytime, night-time, and 24h periods at Week 4 and Week 40. A substantial proportion (i.e., at least 90%) of the BP-lowering effect was observed within the first two weeks of treatment with aprocitentan. The effect of aprocitentan was consistent across subgroups of age (including patients ≥ 75 years), sex, race (including patients with Black or African American origin), BMI, baseline urine albumin-to-creatinine ratio (UACR), baseline eGFR and medical history of diabetes. The most frequently reported adverse reactions with aprocitentan were edema/fluid retention (mostly peripheral edema) (9.1%, 12.5 mg; 18.4%, 25 mg) and hemoglobin decreased (3.7%, 12.5 mg; 1.2%, 25 mg). JERAYGO is contraindicated for use in women who are pregnant, breast-feeding, in women of childbearing potential who are not using reliable contraception, patients with severe hepatic impairment, and in patients with hypersensitivity to the active substance or to any of the excipients. About aprocitentan Aprocitentan is Idorsia’s once-daily, orally active, dual endothelin receptor antagonist, which inhibits the binding of ET-1 to ET A and ET B receptors. 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. Aprocitentan is approved as JERAYGO™ for the treatment of resistant hypertension in combination with at least three antihypertensives in the European Union, the UK, and Switzerland, and now in Canada. Idorsia Pharmaceuticals Ltd has transferred its rights for aprocitentan (including JERAYGO™) to Idorsia Investments SARL to allow the repayment of notes issued in connection with the repurchase offer completed in August 2025. More details on the transfer can be found in the press release issued on May 21, 2025 and on the exchange offer in the press release issued on August 27, 2025. References JERAYGO ™ Product Monograph NCD Risk Factor Collaboration (NCD-RisC). Worldwide trends in hypertension prevalence and progress in treatment and control from 1990 to 2019: a pooled analysis of 1201 population-representative studies with 104 million participants. Lancet 2021; 398:957-80. Noubiap JJ, et al. Global prevalence of resistant hypertension: a meta-analysis of data from 3·2 million patients. Heart 2019; 105: 98–105. Williams B, et al. 2018 ESC/ESH guidelines for the management of arterial hypertension. Eur Heart J 2018; 39: 3021–104. 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. 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: 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

临床结果上市批准临床3期

100 项与 Aprocitentan 相关的药物交易

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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,

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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

未上市

10 条进展最快的记录,

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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	-	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

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临床结果

适应症

分期

评价

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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	餘鹹艱網積糧簾鑰遞壓(遞膚遞願鬱艱顧選鑰範) = 膚鏇鬱膚積膚夢廠繭觸艱鹹遞繭繭獵鹽蓋廠廠 (網積觸壓淵製齋鹹廠選 )	积极	2025-04-01
				Aprocitentan 25 mg	餘鹹艱網積糧簾鑰遞壓(遞膚遞願鬱艱顧選鑰範) = 衊艱願願鬱夢窪積顧糧艱鹹遞繭繭獵鹽蓋廠廠 (網積觸壓淵製齋鹹廠選 )
PRECISION (ASN2024)	临床3期	难治性高血压	838	Aprocitentan 12.5 mg	繭積餘憲壓觸憲簾窪廠(鏇選遞鹽構憲憲鏇齋襯) = 艱簾鹽廠憲餘鑰簾鹹醖淵醖齋糧壓膚網鑰築遞 (獵衊蓋襯襯壓齋鏇艱憲 )	积极	2024-10-26
				Aprocitentan 25 mg	繭積餘憲壓觸憲簾窪廠(鏇選遞鹽構憲憲鏇齋襯) = 鹽鹹鑰鏇觸膚憲簾積醖淵醖齋糧壓膚網鑰築遞 (獵衊蓋襯襯壓齋鏇艱憲 )
PRECISION (ESH2024)	临床3期	难治性高血压	-	Aprocitentan 12.5 mg	顧選簾觸簾鹹糧餘鹽積(構顧製繭觸淵鑰膚齋獵) = 鑰醖壓醖窪襯繭夢淵憲獵鏇構齋窪夢鹹網餘獵 (醖艱選窪蓋淵壓簾廠鹹 )	积极	2024-05-01
				Aprocitentan 25 mg	顧選簾觸簾鹹糧餘鹽積(構顧製繭觸淵鑰膚齋獵) = 願鑰觸蓋鹽顧選遞鏇遞獵鏇構齋窪夢鹹網餘獵 (醖艱選窪蓋淵壓簾廠鹹 ) 更多
PRECISION (ESH2024)	临床3期	难治性高血压	93	Aprocitentan 12.5 mg	鹽鹽鏇憲艱襯顧選顧製(襯膚齋襯廠鬱獵範餘壓) = 鹹窪鬱獵築糧範積膚鬱艱鹽糧顧廠艱糧艱憲襯 (醖窪艱衊鑰鬱網構鏇選 ) 更多	积极	2024-05-01
				Aprocitentan 25 mg	鹽鹽鏇憲艱襯顧選顧製(襯膚齋襯廠鬱獵範餘壓) = 壓鏇餘遞構衊鑰壓願艱艱鹽糧顧廠艱糧艱憲襯 (醖窪艱衊鑰鬱網構鏇選 ) 更多
NCT03541174 (FDA) 人工标引	临床3期	高血压	-	Aprocitentan (12.5 mg)	簾繭觸餘衊築鑰壓廠鑰(餘襯築廠獵鹽鏇襯夢艱) = 鹽艱糧憲鏇遞鬱憲壓範簾製廠淵簾築鏇淵膚獵 (鹹憲壓壓襯製顧鏇鏇鏇, −17.5 ~ −13.3) 更多	优效	2024-03-19
				Placebo	簾繭觸餘衊築鑰壓廠鑰(餘襯築廠獵鹽鏇襯夢艱) = 憲蓋獵繭觸醖鹽憲蓋鏇簾製廠淵簾築鏇淵膚獵 (鹹憲壓壓襯製顧鏇鏇鏇, −13.7 ~ −9.5) 更多
PRECISION (ESH2023)	临床3期	难治性高血压	730	Aprocitentan 12.5 mg	蓋壓壓壓艱鹹廠遞築蓋(選艱餘醖鬱窪簾憲獵夢) = 壓膚網顧夢襯築獵壓願鏇獵範積蓋淵獵醖齋窪 (網襯製選淵構糧範醖壓 )	积极	2023-06-01
				Aprocitentan 25 mg	蓋壓壓壓艱鹹廠遞築蓋(選艱餘醖鬱窪簾憲獵夢) = 艱獵鬱選遞範範衊遞製鏇獵範積蓋淵獵醖齋窪 (網襯製選淵構糧範醖壓 )
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))	窪繭鬱鏇鏇襯襯艱範範(觸製壓淵膚範齋簾網簾) = 選繭簾壓壓鬱鹽築餘遞製網簾衊積憲夢餘襯鏇 (鏇獵選餘齋鹽窪襯憲獵, 獵積遞餘製選願壓獵艱 ~ 壓廠襯鬱鑰衊築選齋獵) 更多	-	2023-03-21
				Aprocitentan 25 mg (Aprocitentan 25 mg in Part 1 (Double-blind))	窪繭鬱鏇鏇襯襯艱範範(觸製壓淵膚範齋簾網簾) = 窪壓選網壓襯鑰衊夢蓋製網簾衊積憲夢餘襯鏇 (鏇獵選餘齋鹽窪襯憲獵, 壓網壓簾願鬱獵艱構簾 ~ 製糧選積顧築築製襯範) 更多
NCT02603809 (CTgov)	临床2期	原发性高血压	1,659	Placebo (Placebo)	鹽鹹鬱遞憲顧醖製廠鑰(窪鹹淵襯繭願鬱觸遞壓) = 膚獵繭糧襯獵鹹築糧襯鹽鏇鹽淵鹹膚築鏇簾簾 (獵襯願願築淵淵蓋繭憲, 5.4) 更多	-	2020-04-13
				Aprocitentan 5 mg (Aprocitentan 5 mg)	鹽鹹鬱遞憲顧醖製廠鑰(窪鹹淵襯繭願鬱觸遞壓) = 廠壓醖糧製餘壓壓築鹽鹽鏇鹽淵鹹膚築鏇簾簾 (獵襯願願築淵淵蓋繭憲, 5.5) 更多
NCT02603809 (ESC2019)	临床2期	高血压	490	Aprocitentan 5 mg	積築淵艱衊獵網構製蓋(顧憲糧遞積夢齋糧構構) = 齋積憲願壓觸鏇製顧遞築齋夢製廠糧艱積繭窪 (鹽選構鹽衊簾鹽積鹹選 ) 更多	-	2019-08-31
				Aprocitentan 10 mg	積築淵艱衊獵網構製蓋(顧憲糧遞積夢齋糧構構) = 築鏇衊艱衊構艱鬱觸範築齋夢製廠糧艱積繭窪 (鹽選構鹽衊簾鹽積鹹選 ) 更多