A Sequential Phase 2/3, Single-Arm, Open-Label Study in Adults Followed by a Randomized, Placebo-Controlled, Double-Blind, Multicenter Study to Evaluate the Efficacy and Safety of APL2 in Adults and Adolescents With Focal Segmental Glomerulosclerosis

This is a sequential phase 2/3 study to evaluate the efficacy and safety of twice-weekly subcutaneous (SC) infusions of APL2 in patients diagnosed with FSGS. The initial phase 2 portion is a single-arm, open-label study in adults diagnosed with FSGS. Phase 2 will commence prior to randomizing for phase 3. The phase 3 portion of the study is a randomized, placebo-controlled, double-blinded, multicenter study in adults and adolescents diagnosed with FSGS.

开始日期2025-12-01

申办/合作机构

Apellis Pharmaceuticals, Inc.

NCT07214298

/ Not yet recruiting临床1/2期IIT

A Phase I/II Study of Complement Inhibition in Pancreatic Ductal Adenocarcinoma

This phase I/II trial tests the effect of pegcetacoplan in combination with oxaliplatin, irinotecan, leucovorin, and fluorouracil (mFOLFIRINOX) in treating patients with pancreatic ductal adenocarcinoma (PDAC) that has spread from where it first started (primary site) to other places in the body (metastatic). Pegcetacoplan works by targeting the immune complement process, a part of the immune system that defends against bacteria and may limit tumor progression and improve the immune system's response against tumor cells. Oxaliplatin is in a class of medications called platinum-containing antineoplastic agents. It damages the cell's deoxyribonucleic acid (DNA) and may kill tumor cells. Irinotecan is in a class of antineoplastic medications called topoisomerase I inhibitors. It blocks a certain enzyme needed for cell division and DNA repair and may kill tumor cells. Leucovorin is a drug used to lessen the toxic effects of substances that block the action of folic acid. Leucovorin is a form of folic acid. It is a type of chemoprotective agent and a type of chemosensitizing agent. Fluorouracil stops cells from making DNA and it may kill tumor cells. It is a type of antimetabolite. Giving pegcetacoplan in combination with mFOLFIRINOX may be safe, tolerable, and/or effecting in treating patients with metastatic PDAC. This trial also evaluates the effect of pegcetacoplan on the incidence of major thrombotic events and the resulting complications. Thrombosis is a common complication in patients with PDAC. Thrombosis occurs when blood clots block veins or arteries. Complications of thrombosis, such as stroke or heart attack, can be life-threatening. Giving pegcetacoplan may help prevent blood clots from forming and decrease the risk of major thrombotic events.

开始日期2025-11-01

申办/合作机构

Roswell Park Comprehensive Cancer Center

NCT07214740

/ Not yet recruiting临床3期

A Phase 3B, Single-Arm, Open-Label, Multicenter Study to Evaluate the Safety of Pegcetacoplan in a Prefilled Syringe in Participants With Geographic Atrophy Secondary to Age-Related Macular Degeneration

This is a phase 3, open-label study to evaluate the safety of pegcetacoplan in a prefilled syringe (PFS)

开始日期2025-10-01

申办/合作机构

Apellis Pharmaceuticals, Inc.

100 项与 Pegcetacoplan 相关的临床结果

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100 项与 Pegcetacoplan 相关的转化医学

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100 项与 Pegcetacoplan 相关的专利（医药）

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199

项与 Pegcetacoplan 相关的文献（医药）

2026-01-01·AMERICAN JOURNAL OF OPHTHALMOLOGY

Real-World Experience With Intravitreal Pegcetacoplan for the Treatment of Geographic Atrophy in Age-Related Macular Degeneration

Article

作者: Le, Viet Hoan ; El-Mulki, Omar S ; Zhang, Yi ; Kastner, James ; Hiya, Farhan ; Beqiri, Sara ; Rosenfeld, Philip J ; Berni, Alessandro ; O'Brien, Robert C ; Liu, Jeremy ; Shen, Mengxi ; Gregori, Giovanni ; Herrera, Gissel ; Yehoshua, Zohar ; Nicola, Maura Di ; Wang, Ruikang K ; Cheng, Yuxuan ; Dubovy, Sander R ; Trivizki, Omer ; Kumar, Sivathanu

PURPOSE:

To report on the real-world experience of using intravitreal pegcetacoplan for the treatment of geographic atrophy (GA) in age-related macular degeneration (AMD).

DESIGN:

Retrospective interventional case series.

METHODS:

Eyes with symptomatic GA secondary to AMD were treated with 15 mg of intravitreal pegcetacoplan and participated in an ongoing prospective swept-source optical coherence tomography angiography (SS-OCTA) imaging study. All eyes underwent SS-OCTA imaging before and during pegcetacoplan therapy to assess for GA lesion size, the presence of nonexudative macular neovascularization (MNV), and the onset of exudation. The growth rate of GA and best-corrected visual acuity (BCVA) were assessed for eyes followed for 1 year.

RESULTS:

From April 12, 2023, to November 11, 2024, 154 eyes were injected with pegcetacoplan, and 103 eyes had 1-year follow-up. At baseline, 11 eyes had been previously treated with anti-VEGF therapy, and 9 eyes were diagnosed with treatment-naïve nonexudative MNV by SS-OCTA. Each eye received an average of 10 ± 2 injections, with an average interval of 1.2 months between injections. For the 97 eyes with 1 year of follow-up and measurable GA, the square-root (sqrt) GA growth rate after pegcetacoplan treatment was 0.24 ± 0.15 mm/year. Of these 97 eyes, 63 eyes had prior annual visits before pegcetacoplan treatment was started. In these eyes, the annual sqrt GA growth rate was 0.33 ± 0.22 mm/year before pegcetacoplan and 0.21 ± 0.12 mm/year after pegcetacoplan, resulting in a 37% decrease in the growth rate (P < .001). There were no significant differences in GA growth rate between foveal and nonfoveal GA, either before or after the use of pegcetacoplan (all P ≥ .80). The mean BCVA declined from 63 ± 14 to 59 ± 15 letters over 1 year (P = .001), with no significant difference between foveal and nonfoveal GA (P = .36). Among the 29 eyes developing exudation during pegcetacoplan treatment, 19 (66%) had no evidence of any detectable MNV at baseline and during treatment on SS-OCTA.

CONCLUSIONS:

Eyes treated with pegcetacoplan after 1 year had a 37% reduction in GA growth rate compared with their prior annual growth rate. Pegcetacoplan slowed the growth for foveal and nonfoveal GA at a similar rate. Most of the pegcetacoplan-associated exudation was not due to detectable MNV.

2025-12-31·Hematology

Successful switch from pegcetacoplan to iptacopan after repeated severe breakthrough hemolysis events – case report

Article

作者: Füreder, Wolfgang ; Reinisch, Andreas

OBJECTIVES:

A subset of paroxysmal nocturnal hemoglobinuria (PNH) patients develops clinically relevant extravascular hemolysis when treated with complement C5 inhibitors. These patients may benefit proximal complement inhibitors such as pegcetacoplan, danicopan or iptacopan. No studies comparing these substances are available. Breakthrough hemolysis (BTH) - defined by exacerbation of intravascular hemolysis despite complement inhibition - can be severe especially in patients treated with proximal complement inhibitors.

METHODS:

We report on a PNH patient who had suffered repeated episodes of severe BTH with acute renal failure during 1 year of treatment with pegcetacoplan. The patient was switched to iptacopan and followed also for 1 year.

RESULTS:

After switching to iptacopan, no further BTH occurred for the duration of 12 months follow up. The patient maintained stable hemoglobin and reticulocyte counts as well as lactate dehydrogenase (LDH) levels within the normal range.

DISCUSSION:

Despite dose escalation of pegcetacoplan, BTH recurred in our patient. Therefore, an alternative therapy was warranted. During iptacopan therapy - chosen due to patient preference -no further BTH occurred. However, more data from a larger number of patients are needed.

CONCLUSION:

A switch to iptacopan may be an option for pegcetacoplan treated patients who experience repeated BTH in spite of dose escalation.

2025-09-01·RETINA-THE JOURNAL OF RETINAL AND VITREOUS DISEASES

SILICONE OIL MICRODROPLETS FROM SYRINGES WITH INTRAVITREAL ANTI–VASCULAR ENDOTHELIAL GROWTH FACTOR AND COMPLEMENT INHIBITOR INJECTIONS

Article

作者: Wei, Libby ; Thompson, John T. ; Fan, Xiaoxuan ; Lee, Erica

Purpose::

To quantify the amount of silicone oil in intravitreal anti–vascular endothelial growth factor and complement inhibitor injections in prefilled and commercial syringes (silicone-lubricated and silicone-free).

Methods::

Patients deemed clinically appropriate to receive one of five intravitreal medications received the recommended dose. Syringes were overfilled such that 0.01-0.04 mL remained after injection for analysis. Aflibercept and ranibizumab were available in prefilled syringes. Pegcetacoplan, faricimab, and avacincaptad pegol were prepared with Becton Dickinson polycarbonate (BD) syringes. Faricimab was also prepared in Ocuject VitreJect (OV) silicone-free syringes. Samples were analyzed using spectral flow cytometry.

Results::

Silicone oil was found in all syringes. The lowest amounts of silicone oil were found in the Mili-Q water in OV syringes (4.02 ± 0.3 particles per microliter) and ranibizumab 0.5 mg prefilled syringes (8.33 ± 3.1). Intermediate levels of silicone oil were detected in aflibercept prefilled syringes (35.5 ± 21.8) and faricimab in OV syringes (74.6 ± 10.1), significantly greater than Mili-Q water in OV syringes and ranibizumab. Significantly higher levels of silicone oil were found with faricimab (324.9 ± 30), pegcetacoplan (378.1 ± 379.6), and avacincaptad pegol (113.5 ± 14) in BD syringes than the low or intermediate groups. The filter needles used to draw up medications from vials likely contributed to the amount of silicone oil detected in the samples.

Conclusion::

Commonly used BD polycarbonate syringes for intravitreal injections caused significantly higher levels of silicone oil to be injected into the eye than prefilled or silicone-free syringes. Repeated injections with more viscous intravitreal drugs increase the amount of silicone oil in the vitreous, leading to symptomatic floaters.

443

项与 Pegcetacoplan 相关的新闻（医药）

2025-10-06

·药明康德

同行致远 | 全球首款！这项无药可医的疾病终于迎来FDA批准新药；首个口服PCSK9抑制剂3期结果积极……| Bilingual

编者按：多肽药物已成为治疗多种疾病的重要手段。目前，全球已有约100款多肽药物获批上市，覆盖糖尿病、肥胖症、癌症及罕见疾病等多个领域，为患者带来了全新的治疗策略。然而与传统的小分子药物相比，多肽药物更为复杂，涉及非天然氨基酸（UAA）合成、肽库合成、偶联化合物合成、放大生产工艺开发以及制剂开发等多个环节，对专业技术能力提出了更高要求。为更好地满足全球合作伙伴在多肽药物研发方面的需求，药明康德旗下WuXi TIDES围绕多肽药物建立了一体化CRDMO平台，提供包括线性、环状和高度修饰的多肽，以及非天然氨基酸、连接子、毒素和多肽偶联物的合成服务，支持从药物发现、CMC开发到商业化生产的各个阶段。本文将回顾2025年第三季度多肽领域的最新进展，并介绍药明康德的一体化CRDMO平台如何高效解决该领域药物开发过程中的诸多挑战。 GLP-1类多肽疗法持续进展在2025年第三季度，GLP-1类多肽疗法在代谢与心血管领域持续进展。今年8月，美国FDA加速批准Wegovy（2.4 mg司美格鲁肽）用于联合低热量饮食及增加体能活动，治疗伴有中度至重度肝纤维化（2期或3期）的非肝硬化型代谢功能障碍相关脂肪性肝炎（MASH）成人患者。根据新闻稿，Wegovy为首个获批用于治疗MASH的GLP-1疗法。今年9月，欧洲药品管理局（EMA）人用药品委员会（CHMP）批准更新诺和诺德旗下Rybelsus（口服司美格鲁肽）的标签，使其成为欧盟范围内在2型糖尿病治疗中证实具有心血管获益的首个口服GLP-1受体激动剂。该批准主要根据3b期临床试验SOUL的结果。分析显示，在标准治疗基础上加用口服司美格鲁肽可使主要不良心血管事件（MACE）风险较安慰剂显著降低14%。诺和诺德在7月也向EMA提交了Wegovy 7.2 mg新剂量的监管申请，旨在为肥胖患者进一步提升体重管理效果。与此同时，礼来（Eli Lilly and Company）也公布了其GIP/GLP-1双重受体激动剂Mounjaro（tirzepatide）与GLP-1受体激动剂Trulicity（dulaglutide）相较，在2型糖尿病合并动脉粥样硬化性心血管疾病成人患者中的疗效。临床3期研究结果显示，Mounjaro在降低主要不良心血管事件风险方面不劣于Trulicity，后者曾在REWIND研究中证实具有明确的心血管获益。Mounjaro也在这个季度获加拿大卫生部批准上市。根据新闻稿，该疗法是首个获得加拿大卫生部批准用于慢性体重管理的双重受体激动剂。多肽疫苗在癌症领域取得成果部分多肽疫苗也在癌症领域取得进展。例如，PDS Biotechnology旗下多肽癌症疫苗PDS0101（Versamune HPV）联合PD-1抑制剂Keytruda（pembrolizumab），在2期试验当中，作为一线疗法时，患者的中位总生存期达39.3个月（95% CI：23.9-尚未可估）。根据新闻稿，该类患者在接受标准治疗联合化疗时已公布的最佳中位总生存期为17.9个月。而Elicio Therapeutics旗下靶向突变KRAS的多肽疫苗ELI-002在1期AMPLIFY-201研究中，在中位随访19.7个月时，将胰腺癌和结直肠癌患者的死亡风险降低77%，复发风险降低88%。多肽疗法在罕见病领域获得突破此外，多肽疗法在本季度也于罕见病领域有许多突破。今年7月，美国FDA批准Apellis Pharmaceuticals旗下双环肽疗法Empaveli（pegcetacoplan）扩展适应症，用于治疗C3肾小球病（C3G）和原发性免疫复合物膜增生性肾小球肾炎（IC-MPGN），以减少患者的蛋白尿。根据新闻稿，该疗法是获FDA批准用以治疗这两类罕见肾病的首款疗法。此外，Stealth BioTherapeutics所开发的Forzinity（elamipretide）也在今年9月迎来FDA批准，成为巴思综合征全球首款获批疗法。其他领域的进展其他领域方面，强生（Johnson & Johnson）与Protagonist Therapeutics也已向美国FDA递交新药申请（NDA），寻求批准其联合开发的口服多肽疗法icotrokinra，用于治疗12岁及以上中度至重度斑块状银屑病（PsO）成人与儿科患者。默沙东（MSD）在今年9月宣布在研口服大环肽enlicitide decanoate在3期试验中，能够显著降低高胆固醇血症患者的低密度脂蛋白胆固醇（LDL-C）水平。根据新闻稿，该疗法是在3期试验中显示能显著降低LDL-C水平的首个口服PCSK9抑制剂。商业研发合作进展今年9月，辉瑞（Pfizer）与Metsera达成总额达数十亿美元的收购协议。此次收购将使辉瑞获得后者旗下具差异化的口服与注射型肠促胰岛素和胰淀素类候选药物以及联合疗法，这些项目在有效性与安全性方面具备“best-in-class”潜力。Unnatural Products（UNP）与argenx则在7月达成一项多靶点战略合作研究项目，旨在发现和开发针对“不可成药”疾病靶点的口服大环肽药物。该合作将利用UNP公司的专有药物发现平台，生成针对argenx公司所选定的多个靶点的高效、高选择性且可口服的大环肽分子。综上，2025年三季度多肽疗法多线跃进：GLP-1版图延伸至MASH，肿瘤多肽疫苗在延长生存与降低复发方面表现亮眼，多项罕见病亦迎来首款获批疗法，口服多肽赛道持续升温。随着临床证据不断积累与产业协同加速推进，多肽疗法有望在代谢、肿瘤及罕见病等领域实现更多里程碑。 WuXi TIDES高效赋能合作伙伴开发复杂多肽偶联药物药明康德旗下WuXi TIDES平台支持各类多肽药物从发现、CMC开发到商业化生产的各个阶段，致力赋能全球客户推动创新疗法问世。以下案例将展示WuXi TIDES的一体化平台如何高效推动合作伙伴复杂多肽偶联药物的开发进程。在该案例中，客户所开发的一款多肽偶联药物结构复杂，由两个短环肽片段和一个长线性多肽组成，合成步骤多达87步。初期合成方案的总体产率不足0.1%，难以满足临床试验的需求。同时，该药物所需的3种UAA原料供应紧张，若从外部采购可能严重延误研发进度。面对上述挑战，WuXi TIDES团队提出了多项针对性解决方案。针对UAA原料短缺问题，团队充分发挥自身生产UAA的能力，迅速开发出可行的合成工艺，并成功制备了超过3公斤的UAA原料，从源头保障了项目的顺利推进。这一内部合成策略不仅降低了对外部供应商的依赖，还显著优化了进度管理，大幅缩短整体项目周期。与此同时，WuXi TIDES团队致力于提升多肽合成效率。考虑到传统固相合成方法合成超过50个氨基酸的多肽时，往往面临效率与产率下降的挑战，WuXi TIDES团队采用了“片段合成+化学连接”策略，将目标多肽拆分成多个适合固相合成的小片段，分别合成后再通过化学连接形成完整多肽分子。这一策略将总体产率从不足0.1%提升至3%，并使多个团队能够同时进行片段合成，显著加快了项目推进速度。在复杂冗长的合成路线中，每一个细节都可能影响最终质量与产率。为进一步优化工艺，WuXi TIDES团队对多个关键步骤的合成和纯化条件进行了反复筛选与优化。在放大生产阶段，团队专门设计了定制的纯化材料，使杂质水平下降80%，最终产率提升20%。得益于UAA合成团队、多肽合成团队和分析团队的高效执行及并行作业，WuXi TIDES团队仅用4个月即完成了工艺开发与优化，7个月内交付了两批各100克的GLP样品，随后又在3个月内顺利生产出1千克GMP级原料药，产率达3%，纯度达97.4%。项目整体进度比合作伙伴预期提前4个月，为临床试验的及时启动提供了强有力保障。化学合成能力之外，WuXi TIDES还可赋能多肽药物从临床前到商业化阶段的口服和注射制剂的开发和生产。口服制剂平台支持包括片剂、胶囊、脂质体、粉末、颗粒和口服液等各类剂型的开发和生产；注射剂平台则支持多种剂型和灌装形式的无菌制剂生产。展望未来，WuXi TIDES团队将持续依托其一体化CRDMO平台，助力全球合作伙伴充分发挥多肽疗法的巨大潜力，为患者带来更多创新药物。 CRDMO: Q3 2025 Review of Peptide Therapeutics Peptide drugs have emerged as an important therapeutic modality for a broad spectrum of diseases. To date, approximately 100 peptide-based medicines have received global regulatory approval, providing new treatment options for conditions such as diabetes, obesity, cancer, and rare diseases. However, compared to traditional small-molecule drugs, peptides present greater structural complexity. Their development requires advanced capabilities in areas such as unnatural amino acid (UAA) synthesis, peptide library design, conjugation chemistry, scale-up process development, and formulation support. To address these challenges and better support global partners, WuXi TIDES, an integral part of WuXi AppTec, has established an integrated CRDMO platform. The platform offers comprehensive synthesis services for linear, cyclic, and highly modified peptides, as well as UAAs, linkers, payloads, and peptide conjugates. Covering the full development spectrum from drug discovery and CMC development to commercial-scale manufacturing, the platform enables efficient and flexible solutions tailored to each stage of the pipeline. Here we summarize key developments in the peptide space during Q3 2025 and share a case study that illustrates how WuXi TIDES helps accelerate progress in this dynamic area. Sustained Momentum for GLP-1–Based Therapeutics In the third quarter of 2025, GLP-1 peptide therapeutics continued to advance in the fields of metabolic and cardiovascular diseases. In August, the U.S. FDA granted accelerated approval to Wegovy (semaglutide 2.4 mg) for use in combination with a reduced-calorie diet and increased physical activity to treat adult patients with non-cirrhotic metabolic dysfunction-associated steatohepatitis (MASH) with moderate to advanced liver fibrosis (stage 2 or 3). According to the company, Wegovy is the first GLP-1 therapy approved for the treatment of MASH. In September, the European Medicines Agency’s (EMA) Committee for Medicinal Products for Human Use (CHMP) approved an update to the label of Novo Nordisk’s Rybelsus (oral semaglutide), making it the first oral GLP-1 receptor agonist approved for type 2 diabetes in the European Union, with proven cardiovascular benefit. The decision was based on results from the Phase 3b SOUL trial, which demonstrated that adding oral semaglutide to standard therapy reduced the risk of major adverse cardiovascular events (MACE) by 14% compared with placebo. In July, Novo Nordisk also submitted a regulatory application to the EMA for a new 7.2 mg dose of Wegovy, aiming to further enhance weight management outcomes for patients with obesity. Meanwhile, Eli Lilly and Company reported data comparing its dual GIP/GLP-1 receptor agonist Mounjaro (tirzepatide) with the GLP-1 receptor agonist Trulicity (dulaglutide) in adults with type 2 diabetes and atherosclerotic cardiovascular disease. Results from a Phase 3 trial showed that Mounjaro was non-inferior to Trulicity in reducing the risk of major adverse cardiovascular events. Trulicity had previously demonstrated clear cardiovascular benefit in the REWIND trial. Mounjaro also gained approval from Health Canada this quarter, becoming the first dual receptor agonist authorized in Canada for chronic weight management. Breakthroughs for Peptide Vaccines in Oncology Peptide vaccines also achieved important milestones in oncology. PDS Biotechnology’s peptide-based cancer vaccine PDS0101 (Versamune HPV), in combination with the PD-1 inhibitor Keytruda (pembrolizumab), delivered a median overall survival (mOS) of 39.3 months (95% CI: 23.9–not estimable) as a first-line therapy in a Phase 2 trial. By comparison, previously reported standard therapy plus chemotherapy in this patient group achieved a best mOS of 17.9 months. Elicio Therapeutics also reported promising results for its mutant KRAS-targeted peptide vaccine ELI-002. In the Phase 1 AMPLIFY-201 study, at a median follow-up of 19.7 months, ELI-002 reduced the risk of death by 77% and recurrence by 88% in patients with pancreatic and colorectal cancers. Advances in Peptide Therapeutics for Rare Diseases Significant progress was also made in rare diseases this quarter. In July, the U.S. FDA approved Apellis Pharmaceuticals’ cyclic peptide therapy Empaveli (pegcetacoplan) for the treatment of C3 glomerulopathy (C3G) and primary immune complex membranoproliferative glomerulonephritis (IC-MPGN) to reduce proteinuria. According to the company, this is the first FDA-approved therapy for these two rare kidney disorders. In September, Stealth BioTherapeutics secured FDA approval for Forzinity (elamipretide), marking the world’s first approved treatment for Barth syndrome. Expanding Applications in Other Fields In addition, Johnson & Johnson and Protagonist Therapeutics have submitted a New Drug Application (NDA) to the U.S. FDA for their jointly developed oral peptide therapy icotrokinra, seeking approval for the treatment of adults and adolescents aged 12 years and older with moderate-to-severe plaque psoriasis (PsO). Merck (known as MSD outside of the U.S. and Canada) announced in September that its investigational oral macrocyclic peptide enlicitide decanoate achieved a significant reduction in low-density lipoprotein cholesterol (LDL-C) in a Phase 3 trial in patients with hypercholesterolemia. According to the company’s release, this marks the first oral PCSK9 inhibitor to demonstrate a significant LDL-C reduction in a Phase 3 study. Progress in Partnerships and Collaborations September also saw major business developments, including Pfizer’s acquisition agreement with Metsera. The deal grants Pfizer access to Metsera’s differentiated oral and injectable incretin and amylin candidates, as well as combination therapies, which hold best-in-class potential in both efficacy and safety. In July, Unnatural Products (UNP) entered into a multi-target strategic research collaboration with argenx to discover and develop orally available macrocyclic peptide drugs for previously “undruggable” disease targets. The collaboration will leverage UNP’s proprietary drug discovery platform to generate potent, selective, and orally bioavailable macrocyclic peptides against multiple targets selected by argenx. In summary, Q3 2025 saw peptide therapeutics advance on multiple fronts: the GLP-1 landscape expanded into MASH; peptide cancer vaccines showed compelling benefits in extending survival and reducing recurrence; several rare diseases welcomed their first approved therapies; and the oral-peptide continued to gain momentum. As clinical evidence builds and industry collaboration accelerates, peptide therapeutics are poised to deliver further milestones across metabolic, oncology, and rare disease fields. WuXi TIDES Empowering Global Innovation WuXi AppTec’s WuXi TIDES platform provides end-to-end support for peptide therapeutics—from discovery and CMC development through commercial manufacturing—helping global partners speed innovative therapies to patients. To demonstrate how this integrated model translates into execution, one representative case is outlined below. In this program, the candidate molecule comprised two short cyclic peptide fragments and one long linear peptide, requiring an intricate synthesis involving up to 87 steps. The initial synthetic route yielded less than 0.1% overall, insufficient to meet clinical trial demands. Additionally, the project was hampered by the limited availability of three critical UAAs, with external sourcing posing a risk of significant delays. To overcome these obstacles, the WuXi TIDES team implemented several targeted solutions. First, the team addressed the UAA supply bottleneck by leveraging its internal UAA synthesis capabilities. They quickly developed viable synthetic pathways and produced over 3 kilograms of UAAs, securing raw material availability and safeguarding project timelines. This internal manufacturing strategy not only reduced dependency on external suppliers but also significantly improved timeline control and shortened the overall project duration. Concurrently, efforts were directed at improving the efficiency of peptide synthesis. Given the challenges of efficiency and yield declines when traditional solid-phase peptide synthesis (SPPS) techniques are used for sequencing longer than 50 amino acids, the WuXi TIDES team adopted a "fragment synthesis + chemical ligation" strategy—breaking down the target peptide into shorter fragments suitable for SPPS, synthesizing them individually, and then linking them chemically into the full-length peptide. This approach improved the overall yield from under 0.1% to 3%, while enabling multiple teams to work in parallel, significantly accelerating development timelines. Given the complexity and length of the synthesis route, process optimization was critical. The WuXi TIDES team conducted extensive rounds of screening and refinement for key synthesis and purification steps. During scale-up, the team introduced customized purification materials that reduced impurity levels by 80% and improved yield by 20%. Through efficient execution and parallel activities between the UAA synthesis, peptide synthesis, and analytical teams, process development and optimization were completed in just four months. The WuXi TIDES team delivered two batches of 100 grams of GLP-grade material within seven months, followed by the production of 1 kilogram of GMP-grade API in an additional three months. The final process achieved a 3% yield with 97.4% purity. Overall, the project was completed four months ahead of schedule, ensuring timely clinical trial initiation with a secure and robust supply. Beyond peptide API synthesis, WuXi TIDES also supports both oral and parenteral drug product development and manufacturing for peptide drugs from preclinical to commercial stages. The oral solid platform supports a diverse array of dosage forms such as tablets, capsules, lipid formulations, powders, granules, and liquid-in-bottle, while the parenteral dosage platform accommodates various injectable drug forms and filling formats. Looking forward, the WuXi TIDES team will continue to leverage its integrated CRDMO platform to accelerate the development of peptide therapeutics. By enabling global partners to unlock the full potential of peptide drugs, WuXi TIDES is helping bring more innovative medicines to patients around the world. 参考资料： [1] FDA Approves Apellis’ EMPAVELI® (pegcetacoplan) as the First C3G and Primary IC-MPGN Treatment for Patients 12 and Older. Retrieved September 25, 2025 from https://investors.apellis.com/news-releases/news-release-details/fda-approves-apellis-empavelir-pegcetacoplan-first-c3g-and [2] Merck’s Investigational Oral PCSK9 Inhibitor Enlicitide Decanoate Met All Primary and Key Secondary Endpoints in Adults with Hypercholesterolemia in Pivotal CORALreef Lipids Study. Retrieved September 25, 2025 from https://www.merck.com/news/mercks-investigational-oral-pcsk9-inhibitor-enlicitide-decanoate-met-all-primary-and-key-secondary-endpoints-in-adults-with-hypercholesterolemia-in-pivotal-coralreef-lipids-study/ 免责声明：本文仅作信息交流之目的，文中观点不代表药明康德立场，亦不代表药明康德支持或反对文中观点。本文也不是治疗方案推荐。如需获得治疗方案指导，请前往正规医院就诊。版权说明：欢迎个人转发至朋友圈，谢绝媒体或机构未经授权以任何形式转载至其他平台。转载授权请在「药明康德」微信公众号回复“转载”，获取转载须知。分享，点赞，在看，聚焦全球生物医药健康创新

临床3期上市批准加速审批临床结果临床2期

2025-09-23

·FiercePharma

Sobi surpasses Roche in rare disease patient groups' reputation rankings

Among the companies making the biggest strides in the rankings year over year, per PatientView, were Boehringer Ingelheim, UCB, Merck & Co. and Chiesi. In recent years, Roche has made a habit of oscillating between first and second place on rare disease patient groups’ annual ranking of drugmakers’ corporate reputations.The zigzag continues into PatientView’s latest iteration of the report (PDF), released Tuesday, showing that it’s another down year for the Swiss pharma after it nabbed the top spot in last year’s report.PatientView surveyed a total of 518 patient groups representing dozens of rare diseases, including hemophilia and other bleeding disorders, cystic fibrosis, spinal muscular atrophy, pulmonary fibrosis and many more. Their responses detail their views of 32 pharmas and the industry at large in 2024, with corporate reputation defined as a combination of 10 factors that include the likes of patient-centricity, high-quality products and integrity.This time around, Sobi took first place in overall corporate reputation as determined by the patient groups. That held true both among the groups rating the pharmas they’re merely familiar with and among those rating the companies they’ve actually worked with. In both cases, Roche took second place, while BioMarin took third in the familiarity ranking and UCB rounded out the top three in terms of companies the groups have firsthand experience working with.Sobi is a new addition to the pharmas included in the annual report; the rare-disease-focused Swedish pharma’s medicines include the Sanofi-partnered Altuviiio for hemophilia A and the Apellis-partnered Empaveli for paroxysmal nocturnal hemoglobinuria and a pair of rare kidney diseases.Roche did get a boost when the assessment was limited only to the 14 biggest pharmas in the set, which excluded Sobi, among others, from the lineup. In that case, Roche took first in the rankings by both familiarity and firsthand experience, followed by Sanofi and Boehringer Ingelheim in the former and AstraZeneca and Boehringer in the latter.Roche swept all four versions of the rare disease groups’ rankings last year—in familiarity and firsthand experience, among Big Pharmas and the entire group—which marked its return to the top after Horizon Therapeutics had snagged the throne the year before.Among the companies making the biggest strides in the rankings year over year, per PatientView, were Boehringer, UCB, Merck & Co. and Chiesi. Beyond ranking specific companies, the rare disease organizations were also asked about their views of the overall corporate reputation of the pharma industry. All together, 55% of the groups labeled the industry’s reputation as “good” or “excellent,” a slight dip from the 56% that said so in last year’s survey.That tracks with PatientView’s other findings this year, including its survey of more than 2,500 patient groups across all indications, among which pharma’s positive reputation share slipped from 57% to 56%.Still, the rare disease patient groups surveyed have largely tracked improvements in the industry’s activities. All but one of their assessments of 14 specific industry activities have improved since 2020, the report shows, with pricing transparency the one area where they’ve seen the industry worsening.The biggest improvements since 2020, meanwhile, showed up in funding transparency, integrity and offering products that benefit patients.

2025-08-20

·美迪西Medicilon

美迪西专访 | 瞄准百亿美元市场，领诺医药在补体抑制剂领域更进一步

2025年8月18日，领诺医药自主研发新一代补体抑制剂产品SLN12140获得国家药品监督管理局（CDE）通知，批准用于“补体参与介导的溶血性疾病包括但不限于阵发性睡眠性血红蛋白尿症PNH、补体介导的血栓性微血管病TMA、镰刀细胞病SCD等”的临床试验。这是该产品继2025年2月、2024年5月该产品分别获得CDE、FDA批准用于IgA肾病的临床试验之后，获得监管机构对第二类适应症的批准。作为领诺医药长期的合作伙伴，美迪西有幸参与了SLN12140的临床前研究。今天邀请领诺医药创始人&CEO韩照中博士带我们一起走进这款药物，了解创新成果背后的故事。韩照中博士领诺医药创始人&CEO 1991年毕业于武汉大学病毒学与分子生物学系，1997获军事医学科学院医学遗传学博士学位。2002年完成美国国家卫生研究院肿瘤研究所（NIH， NCI）新药研发博士后训练后，任职于能源部国家实验室生物部，从事抗体发现与工程改造研究。2004年任Vanderbilt University医学院肿瘤生物学助理教授，在联邦基金的支持下进行脑胶质瘤的基础与转化医学研究。2013年加入Alexion Pharmaceuticals公司，参与或主导补体靶向、针对严重罕见病的孤儿药研发。2017年底回国负责睿智化学（ChemPartner）抗体发现与工程改造平台。2019年8月于上海自由贸易区张江药谷注册成立领诺（上海）医药科技有限公司，开展基于补体靶向、穿越血脑屏障的大分子药物递送技术、罕见病孤儿药的创新药物研发。 Q1 美迪西：韩博您好，首先祝贺领诺医药的 SLN12140 近日获得 CDE 的临床试验批准，这无疑是一个重大的里程碑。能否和我们分享一下这个消息带来的感受？韩照中博士：这个消息确实让整个团队都非常振奋。首先要感谢团队的不懈努力，也要感谢投资人、合作方的大力支持。这个批准不仅是对我们转化能力和研发质量的认可，更重要的是，它为早日推进这款新一代补体抑制剂进入医药市场，为病患提供更安全、更有效、更方便用药的治疗手段提供了可能。我们团队都深受鼓舞，也更加坚定了加速推进这款创新产品临床转化的决心，希望能早日惠及更多患者。 Q2 美迪西：这款新一代补体抑制剂SLN12140获得在中国、美国、澳大利亚开展临床试验的许可，可以介绍一下这款药物的核心优势吗？韩照中博士：SLN12140 是我们自主研发的新一代补体抑制剂产品，它的优势是多方面的。靶点选择上选用了生物学机制得到完美临床前、临床验证的补体信号通路，首选适应症选择上选用了临床、监管和市场转化路径更加清晰的PNH、IgA肾病，因此有效避开了很多新药研发中的风险。同时，在经过临床验证的生物学通路上，我们选用了更加容易成药的靶点，分子设计上考虑补体相关疾病的用药特点，因此与现有的补体产品不同，SLN12140的产品设计体现出了显著的差异化优势。从目前收集到的一期临床试验结果来看，它展现出了良好的安全性、药物代谢特征和靶点抑制效果。而且，高浓度、皮下给药、长给药周期的药物特征，让它具备了成为Best-In-Class 的潜力。作为同机制、同靶点的全球第一款皮下给药大分子治疗产品，这一特性也让它在市场竞争中拥有较大的潜力。 Q3 美迪西：在本次CDE的审批中，批准了SLN12140用于PNH等溶血性疾病的适应症，这些疾病给患者带来了极大的痛苦。能否具体介绍一下这些疾病的情况以及 SLN12140 在治疗这些疾病上的潜力？韩照中博士：PNH 是一种极端罕见、严重、高致死率、高致残率的溶血性疾病，和补体的异常活化高度相关。由于其临床试验周期短、临床终点明确，成为了补体抑制剂产品的试金石，尤其是对于需要体现和标准治疗差异化优势的新一代产品而言。像 Apellis 的 Pegcetacoplan（2021年5月获得FDA批准）和诺华的 Iptacopan（2023年12月获得FDA批准），都是在 PNH 适应症上首先获批的代表性产品。而和补体异常相关的TMA，包括非典型性尿毒症（aHUS）、干细胞移植术后微血管病（HSCT-TMA）等，也是近年一些补体产品的获批适应症。镰刀细胞病 SCD 在欧美地区相对高发，临床需求和市场空间巨大，且和补体关联性较强，目前尚没有相关产品获批上市。SLN12140 在这些适应症上的获批，不仅扩大SLN12140的适应症拓展空间，更是为患者尽快带来新的治疗希望创造了可能性，我们期待它能在临床试验中展现出优异的疗效。 Q4 美迪西：领诺医药自 2019 年成立以来，在创新药物研发方面取得了不少成果，除了 SLN12140，还有穿越血脑屏障的重组酶替代治疗项目 LIN-2003 等。领诺医药未来的研发重心和发展方向是怎样的呢？韩照中博士：领诺医药一直秉承 “领引创新，诺言践行” 的宗旨，我们自主开发了独有的血液半衰期延长（长效）、穿越血脑屏障等专利技术。目前，补体项目SLN12140已启动I期临床试验，穿越血脑屏障的重组酶替代治疗项目LIN-2003获得FDA孤儿药资格认定，并已启动IND申报准备工作。未来，我们会继续聚焦于治疗免疫性疾病的补体靶向抗体和治疗 CNS 相关疾病的重组蛋白类药物等管线产品, 稳步推进管线的临床试验和市场准入工作，争取能在更多国家和地区获批上市，为全球患者服务。非常感谢韩博士的分享，让我们对领诺医药以及 SLN12140 有了更深入的了解。美迪西作为领诺医药的合作伙伴，我们为领诺取得的成绩感到由衷的高兴。期待在未来的合作中，双方能携手取得更多突破性成果，为医药行业的发展和患者的健康贡献更多力量。关于领诺医药领诺医药成立于2019年8月，苏州、上海两地运营，在上海自由贸易试验区张江药谷拥有近1000平米的研发实验室。公司获得多家产业机构和私募基金的股权投资。公司研发团队覆盖从分子发现到早期临床开发的全流程，秉承“领引创新，诺言践行”的宗旨，自主开发了独有的血液半衰期延长（长效）、穿越血脑屏障等专利技术。领诺医药以自有平台技术为基础，致力于能更好满足临床需求的创新药物研发，开发针对新靶点、新机制、新适应症的First-in-class（FIC）产品，以及平台技术赋能、针对成熟靶点的Best-in-class（BIC）产品。目前，领诺医药的管线产品包括治疗免疫性疾病的补体靶向抗体和治疗CNS相关疾病的重组蛋白类药物。其中，补体项目LIN-2102（SLN12140）已启动I期临床试验，穿越血脑屏障的重组酶替代治疗项目LIN-2003获得FDA孤儿药资格认定，并已启动IND申报准备工作。此外，公司还有多个管线产品处于临床前概念验证阶段。领诺医药将持续加大研发投入，通过技术和产品授权、合作开发等渠道，加速产品在国内、外市场的临床转化，为病患者提供更安全、有效、方便的治疗选择。往期推荐美迪西专访 | 美济医药黄慧瑜博士：口服紫杉醇药物研发的破局者美迪西专访 | 新药研发智在必行：听任峰博士畅谈AI制药的无畏前行美迪西专访 | 祥根生物原晨光博士畅谈抗真菌药物市场趋势及创新美迪西专访陈涛博士 | 南芯医疗：做活体生物药领域一往无前的弄潮儿美迪西专访| 周文波博士：3年3个IND获批，宇耀生物有何优势？关于美迪西美迪西（股票代码：688202.SH）成立于2004年，总部位于上海，致力于为全球制药企业、研究机构及科研工作者提供全方位的临床前新药研究服务。美迪西的一站式综合服务以强有力的项目管理和更高效、高性价比的研发服务助力客户加速新药研发进程，服务涵盖医药临床前新药研究的全过程，包括药物发现、药学研究及临床前研究。至2025年6月底，美迪西已为全球超2000家客户提供药物研发服务，参与研发完成的新药及仿制药项目已有580+件IND获批临床，与国内外优质客户共同成长。美迪西将继续立足全球视野，聚力中国创新，为人类健康贡献力量！

孤儿药

100 项与 Pegcetacoplan 相关的药物交易

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外链

KEGG	Wiki	ATC	Drug Bank
D11613	Pegcetacoplan	B03XA	-

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
C3肾小球病	美国	Apellis Pharmaceuticals, Inc.	2024-10-07
膜增生性肾小球肾炎	美国	Apellis Pharmaceuticals, Inc.	2024-10-07
地图样萎缩	美国	Apellis Pharmaceuticals, Inc.	2023-02-17
阵发性睡眠性血红蛋白尿症	美国	Apellis Pharmaceuticals, Inc.	2021-05-14

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
局灶性节段性肾小球硬化症	临床3期	美国	Apellis Pharmaceuticals, Inc.	2025-12-01
移植物功能延迟恢复	临床3期	-	Apellis Pharmaceuticals, Inc.	2025-09-01
终末期肾脏病	临床3期	-	Apellis Pharmaceuticals, Inc.	2025-09-01
冷凝集素病	临床3期	美国	Swedish Orphan Biovitrum AB	2022-10-20
冷凝集素病	临床3期	日本	Swedish Orphan Biovitrum AB	2022-10-20
冷凝集素病	临床3期	奥地利	Swedish Orphan Biovitrum AB	2022-10-20
冷凝集素病	临床3期	比利时	Swedish Orphan Biovitrum AB	2022-10-20
冷凝集素病	临床3期	加拿大	Swedish Orphan Biovitrum AB	2022-10-20
冷凝集素病	临床3期	芬兰	Swedish Orphan Biovitrum AB	2022-10-20
冷凝集素病	临床3期	格鲁吉亚	Swedish Orphan Biovitrum AB	2022-10-20

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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


EURETINA2025	N/A	年龄相关性黄斑变性	22	Pegcetacoplan 15mg monthly	鏇築餘願繭蓋網範築鑰(衊選鹹製顧網構製獵選) = High-certainty evidence indicates that PEG or ACP do not confer significant benefit to low-luminance BCVA. 築夢夢廠廠憲選壓構廠 (鏇壓窪艱觸構膚鬱顧鹽 )	不佳	2025-09-04
EURETINA2025	N/A	年龄相关性黄斑变性	22	Pegcetacoplan 15mg every other month		不佳	2025-09-04
NCT03525613 (OAKS, EURETINA2025)	临床3期	年龄相关性黄斑变性 \| 地图样萎缩 outer nuclear layer (ONL) \| external limiting membrane (ELM) \| ellipsoid zone layer (EZ) ... 更多	453	Pegcetacoplan 15 mg per 0.1 mL intravitreal injection monthly	壓醖觸蓋顧蓋鹽壓鏇繭(膚壓餘衊獵鹹鬱範獵選) = 齋衊膚衊鏇鏇蓋觸繭壓顧夢壓醖顧鹽餘鹽構遞 (繭餘淵醖築衊憲製觸積 ) 更多	积极	2025-09-04
NCT05067127 (VALIANT \| APL2-C3G-310, CTgov)	临床3期	膜增生性肾小球肾炎 \| C3肾小球病 \| 肾小球肾炎慢性补体成分 3 肾小球病	124	Pegcetacoplan (Randomized Controlled Period: Pegcetacoplan)	衊夢糧製壓衊蓋蓋範簾(窪醖鏇鬱遞糧簾夢夢選) = 憲鬱艱選繭築窪製選築衊淵願醖膚簾積簾築簾 (觸製淵廠齋鑰鏇蓋築蓋, 簾糧獵觸範獵選築範積 ~ 蓋鏇觸願糧網繭繭願壓) 更多	-	2025-08-06
NCT05067127 (VALIANT \| APL2-C3G-310, CTgov)	临床3期	膜增生性肾小球肾炎 \| C3肾小球病 \| 肾小球肾炎慢性补体成分 3 肾小球病	124	placebo+pegcetacoplan (Randomized Controlled Period: Placebo)	衊夢糧製壓衊蓋蓋範簾(窪醖鏇鬱遞糧簾夢夢選) = 築艱築繭鑰憲憲製蓋構衊淵願醖膚簾積簾築簾 (觸製淵廠齋鑰鏇蓋築蓋, 簾憲簾壓夢餘構築顧蓋 ~ 網範壓壓範築糧遞蓋鏇) 更多	-	2025-08-06
NCT04770545 (OAKS, DERBY, and GALE, Pubmed \| Am J Ophthalmol)	临床3期	年龄相关性黄斑变性	790	Pegcetacoplan monthly	鏇鹽遞壓艱遞壓襯獵齋(繭製製簾範淵淵糧網襯) = 33 (4.5%) eyes with exudative AMD 糧構鏇壓繭憲艱壓艱築 (糧鹹簾窪鬱簾鏇顧糧繭 ) 更多	积极	2025-08-01
NCT05067127 (APL2-C3G-310 \| VALIANT, FDA_CDER \| PipelineReview) 人工标引	临床3期	膜增生性肾小球肾炎 \| C3肾小球病	124	Pegcetacoplan	膚廠憲構膚夢夢鹽簾願(齋積鏇蓋遞繭願鹹願製) = 蓋選艱顧淵蓋獵鑰獵廠鹽鹹齋鏇憲艱壓衊鬱鹽 (壓鹽醖鏇簾膚膚範鬱鏇, 0.25，0.43)	积极	2025-07-28
	临床3期	膜增生性肾小球肾炎 \| C3肾小球病	124	Placebo	膚廠憲構膚夢夢鹽簾願(齋積鏇蓋遞繭願鹹願製) = 遞網願遞醖膚鏇淵選獵鹽鹹齋鏇憲艱壓衊鬱鹽 (壓鹽醖鏇簾膚膚範鬱鏇, 0.91，1.16)	积极	2025-07-28
PF675 (EHA2025)	N/A	C5 inhibitors	26	Pegcetacoplan	醖夢糧網獵獵繭壓鬱鏇(餘糧鑰淵選鹽鬱積蓋憲) = 餘淵憲願鑰築憲網獵積簾鑰願觸遞壓鏇構窪壓 (窪壓鏇鏇鏇憲糧齋夢觸 ) 更多	-	2025-05-14
NCT05776472 (COMPLETE, EHA2025)	N/A	阵发性睡眠性血红蛋白尿症	70	Pegcetacoplan	鏇網窪蓋膚鑰獵壓構簾(壓築蓋簾醖鏇憲襯餘願) = 壓觸製遞願鹹鑰鹽遞蓋製齋蓋壓簾築願衊範衊 (顧憲繭襯艱窪繭夢築淵, 0.8 ~ 3.3) 更多	-	2025-05-14
PS1665 (EHA2025)	临床3期	阵发性睡眠性血红蛋白尿症	-	PEGcetacoplan (PNH patients with <4 RBCs)	簾觸淵簾觸願顧範獵構(鏇糧膚廠遞襯範鏇獵繭) = Initial reductions in mean ARC were sustained 鬱鹹鑰憲遞夢獵繭襯鹹 (壓衊觸選觸鹽襯選網選 ) 更多	积极	2025-05-14
PS1665 (EHA2025)	临床3期	阵发性睡眠性血红蛋白尿症	-	PEGcetacoplan (PNH patients with ≥4 RBCs)		积极	2025-05-14
NCT04085601 (PRINCE, EHA2025)	临床3期	阵发性睡眠性血红蛋白尿症一线	46	PEGCetacoplan	衊餘願蓋壓網獵顧願願(淵觸淵鏇鑰鑰鬱艱鹹憲) = 構鬱憲醖獵蓋壓獵選醖餘衊鏇衊構鏇齋廠醖衊 (鑰膚構範壓窪構範鹽襯 )	积极	2025-05-14
NCT03500549 (Pubmed \| Eur J Haematol)	临床3期	阵发性睡眠性血红蛋白尿症 complement 5 inhibitors (C5i; eculizumab, ravulizumab)	-	Pegcetacoplan	蓋觸選繭餘襯齋廠築齋(窪廠鏇憲選繭窪鬱構蓋) = 蓋憲觸醖淵壓餘製壓窪廠齋鹽鹽廠齋壓獵鹹遞 (壓鏇願獵憲積醖鏇醖餘, -90.02 ~ 21.21)	积极	2025-04-25