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2025-12-01

申办/合作机构

Roswell Park Comprehensive Cancer Center

NCT07213960

/ Not yet recruiting临床2/3期

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.

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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205

项与 Pegcetacoplan 相关的文献（医药）

2026-02-01·CURRENT OPINION IN IMMUNOLOGY

Complement-targeting therapies in hemolytic diseases

Review

作者: Frémeaux-Bacchi, Véronique ; Roquigny, Julia ; Duval, Anna

Complement inhibition has revolutionized the management of hemolytic diseases by targeting the underlying drivers of red blood cell destruction in disorders such as paroxysmal nocturnal hemoglobinuria, atypical hemolytic uremic syndrome, and cold agglutinin disease. Recent advances have expanded the therapeutic landscape beyond terminal C5 inhibition to proximal strategies targeting C3, factor B, and factor D. These newer agents - such as pegcetacoplan, iptacopan, and danicopan - not only control intravascular hemolysis but also address extravascular hemolysis and offer oral or subcutaneous alternatives. In cold agglutinin disease, the efficacy of the classical pathway inhibitor sutimlimab provides compelling evidence for the therapeutic value of targeting early initiating molecules of the complement cascade. For clinicians, these innovations provide personalized treatment choices based on disease phenotype, hemolysis profile, patient preference, and risk stratification. The evolving complement inhibitor arsenal enables optimized, targeted care and pathway-specific interventions in hemolytic conditions.

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.

457

项与 Pegcetacoplan 相关的新闻（医药）

2025-11-18

·QQ浏览器

翰宇药业“双总裁”架构，瞄准GLP-1全球市场

翰宇药业正试图在GLP-1红海中杀出一条差异化路径。11月17日，国内多肽药物领军企业翰宇药业同步发布两条重磅人事公告：董事兼执行总裁PINXIANG YU（余品香）辞职，公司研发老将唐洋明、原恒瑞医药国际业务负责人沈亚平出任执行总裁。这一人事变动并非孤立事件。此前，翰宇药业人事变动频频，且正值公司重磅产品利拉鲁肽注射液全球“突围”之际。行业普遍认为，此次人事调整背后，既有翰宇药业应对市场竞争的战略考量，也折射出中国创新药企“研发+国际化”双轮驱动的发展趋势。翰宇正通过“外引经验+内提骨干”的组合拳，加速提升自身竞争力。翰宇药业“大换血”公告显示，余品香因到龄退休，申请辞职并不再担任公司及子公司任何职务。公司及董事会聘请两位新任执行总裁——分别是前恒瑞医药国际化业务负责人沈亚平，和效力翰宇20年、拥有丰富药品研发、申报经验的唐洋明。据悉，余品香的职业生涯始于海外，曾在加拿大Novocol与Apotex担任实验室主管及药政/审计专家。2005年回国后，历任凯默斯医药药政总监、洛比化学青岛公司总经理等职。她于2010年加入翰宇药业，历任副总裁、坪山与武汉基地总经理，以及董事兼执行总裁。翰宇药业新任执行总裁之一是沈亚平。加入翰宇药业前，他曾任加拿大Inflazyme公司医药化学与工艺总监、美国Chemwerth公司中国区总经理，以及恒瑞医药副总裁。据了解，沈亚平于2012年加入恒瑞医药，长期分管国际仿制药业务、国际业务部及海外子公司，负责海外市场开发、注册申报及上市销售。不仅如此，他还主导过多个对外合作项目，具备授权交易、国际临床试验布局等跨国运营的专业经验。业内认为，沈亚平的国际业务经验将为翰宇药业国际板块布局带来强大助力。出任翰宇药业的另一位执行总裁是唐洋明。资料显示，唐洋明自2005年2月加入翰宇药业，是一名任职超过20年的老将。他从研究员做起，历任质量研究总监、研发高级总监、副总裁，现任公司执行总裁并兼任翰宇药业（武汉）有限公司等子公司的董事长。他从事多肽药物研发超过15年，且拥有中、美、欧三地的药物申报经验。他先后主导过多个公司核心产品的研发和申报项目，例如于2024年获FDA批准上市的首仿利拉鲁肽注射液。行业观点认为，医药业务链条长、专业性强，单一高管很难覆盖研发、生产、销售、国际化等所有环节。“双轨制”管理模式在医药行业越来越常见。翰宇药业指出，此次管理架构升级，旨在实现强强联合，形成优势互补的管理格局。值得注意的是，自2025年起，翰宇药业已有多次高管变动。8月，原副总裁张宝乐因个人原因辞职，不再担任翰宇药业及其子公司任何职务。张宝乐自2018年加入翰宇药业，历任研发中心高级研究员、研发中心经理、执行总裁助理以及副总裁。自2024年，他分管公司海外营销业务。他的离职标志着公司的海外营销业务线率先启动换血。10月，同样因为个人原因，原公司董事、副总裁兼董事会秘书杨笛辞职。公司董事会宣布，拥有10年证券事务经验的李娉娉接任董事会秘书一职。据悉，杨笛有超过10年生物制药研发、风险投资，以及BD领域的相关经验。李娉娉于2021年9月加入翰宇药业，此前历任证券管理部经理、公司证券总监兼证券事务代表。高层变动频频，往往代表着公司正开启一轮深刻的战略性重塑。这是公司为了主动应对内外部挑战、谋划新发展路径所采取的关键举措。两位新任执行总裁正对应“技术攻坚”与“市场破局”两大核心需求，将驾驶翰宇药业这艘大船继续远航。市场潜力兑现在即翰宇药业GLP-1管线的商业化潜力正在加速释放，并有望凭借其丰富的在研产品线与全球化布局，开启新一轮增长周期。根据公司最新财报，翰宇药业2025年前三季度营业收入6.83亿元，同比增长82.06%，归母净利润7135.15万元同比扭亏为盈，经营活动现金流净额2.71亿元同比大幅增长。在此之前，2018年至2024年，公司扣非净利润连续7年处于亏损状态。翰宇药业转折的关键节点在2024年12月，其产品利拉鲁肽注射液获得美国FDA批准上市。在GLP-1产品数量不多、产能尚不能满足市场需求的前提下，翰宇药业凭借原料药－制剂一体化的独特优势，与药企Hikma签署了累计3.38亿元的合同，以“低出货价+高利润分成”的商业模式迅速开拓了美国市场。业内分析，随着GLP-1赛道的横空出世，翰宇药业凭借其二十年多肽全产业链的深厚沉淀与国际化的关键决策，实现了业绩暴增，为公司战略转型奠定了坚实基础。当前翰宇药业正站在新老交替的关键节点；双总裁架构下的发展既有机遇，也有挑战。一方面，需要尽快磨合架构；另一方面，要加速扩大在GLP-1红海中领先优势，才能真正脱离公司困境。为应对接下来的挑战，翰宇药业已形成清晰的梯队布局。公司在研超过50种管线中，司美格鲁肽减重及降糖适应症均已进入三期临床试验，预计于2026年在中美申报上市。此外，瑞他鲁肽、替尔泊肽等多肽药物也在加速推进。值得一提的是，GLP-1/GIP/GCG三受体激动剂HY3003，有望成为翰宇药业未来新的关键增长点。据了解，目前全球范围内尚无类似三靶点药品上市，仅有礼来的Retatrutide处于Ⅲ期临床阶段。HY3003还采用多剂型并行开发策略，包括周制剂、超长效月制剂（每月注射一次）和口服制剂。除此之外，翰宇药业还积极布局诸多前沿领域，如治疗高胆固醇血症的siRNA药物Inclisiran（英克司兰钠）、治疗高血压的Zilebesiran，以及治疗地图样萎缩的PEG修饰环肽药物Pegcetacoplan等一系列重磅产品。翰宇药业曾表示，公司未来10年还将有近20种面向国际市场的多肽及小核酸药物制剂产品有望陆续获批上市，涵盖减重、糖尿病、罕见病、骨质疏松、高血脂等多个疾病治疗领域。翰宇药业能否如期兑现，让我们拭目以待。参考资料来自网络公开信息，包括新闻资讯、企业官网、政府文件等。【免责声明】

高管变更

2025-11-17

·动脉网

避开药明，这些CDMO靠多肽突围

如何在龙头光环下找到生存之道？当前，CDMO行业呈现“头部集中、细分突围、分化加剧”的竞争格局。像具备产能储备+连续流技术+全球化布局+寡核苷酸协同能力的平台型巨头药明康德占据了主要市场份额。据相关统计数据，从2024年~2025H1，美国FDA批准的40款小分子药物中，有8款由药明康德业务平台服务。一方面说明药明康德作为头部CDMO的价值，短期内在全球市场难以被替代；另一方面，腰部CDMO企业想与其正面竞争也困难重重。值得注意的是，不管是以凯莱英、九洲药业为代表的、营收规模维持在30亿元左右的技术专长型企业；还是诺泰生物、圣诺生物、泰德医药等聚焦细分赛道的专家型企业，都选择了聚焦多肽CDMO这条业务线，并以超行业平均增速实现弯道超车，构成行业“高增长阵营”。行业龙头靠平台与产能统治了核心市场，但细分领域的技术壁垒为有技术积累的企业留下突围窗口。未来CDMO行业的竞争或将从单纯的成本优势竞争，演变到围绕技术深度展开，多肽CDMO的发展已经初步展示了行业格局的新变化。 01 多肽助推业绩起飞 GLP-1的扩张，带飞了多肽CDMO行业。据华福证券数据，2025年Q1~Q3，CXO板块收入同比增长12%，归母净利润同比增加58%，聚焦到2025Q3，收入同比增加10%，归母净利润同比增加51%。特别是CDMO龙头企业药明康德，在2025年前三季度业务在手订单同比增长41%，显示出良好增长态势，但真正值得关注的，是除药明之外的其他CDMO，他们的向上发展才是行业持续复苏的写照。医药细分板块业绩表现，图源华福证券值得注意的是，多肽业务成为部分CDMO企业主要的增长驱动力。如凯莱英在2025年前三季度，实现营业总收入46.3亿元，同比增长11.82%，可其中小分子CDMO业务收入基本持平，多肽、寡核苷酸、ADC等增量业务板块收入同比增长72%，而以多肽为代表的化学大分子业务收入更是同比增长超150%。与此同时，新业务订单保持双位数增长，从下半年待交付的订单分布看，Q4交付规模将显著高于Q3，预计全年营业收入将实现13%~15%增长。圣诺生物前三季度业绩同比增长54%，实现归母净利润同比增长123%，业绩攀升的主因也是因为多肽业务的快速增长。诺泰生物的增长同样依托多肽业务，2025前三季度实现营业收入15.27亿元，同比增长22%，归母净利润同比增长27%。还有专注于多肽业务的泰德医药，在报告期内也实现了项目数的大幅增长。当然，这一切都离不开GLP-1药物在全球的快速放量，据企业2025年第三季度财报数据显示，诺和诺德核心产品司美格鲁肽三大品牌药物前三季度合计销售约254亿美元，竞争对手礼来的替尔泊肽前三季度销售约248亿美元，仅两大巨头就占据了超500亿美元的市场。有了巨头打样，近几年全球众多药企纷纷加入GLP-1赛道进行竞争，他们的加入不仅使全球多肽市场规模迅速扩大，同样让多肽CDMO行业得以快速发展，国内CDMO行业稳稳接住了这波风口。只是由于有药明康德这家巨头的存在，使得其他企业的光芒被其掩盖。对于这些竞争者来说，如何在龙头压制下找到自身发展路径，对于行业的良性发展至关重要。 02 产能之外的突围策略规模红利正在远去，技术溢价助推多肽CDMO赛道兴起。过去，中国CDMO企业凭借大力扩产，形成规模优势参与全球竞争；近几年，随着各种新兴疗法的兴起，各类FIC药物的数量呈现逐年上升的态势。同时，新疗法也面临复杂工艺开发、规模化生产优化等技术问题亟待解决，市场需求的转变也推动了中国CDMO行业的从规模化红利向技术溢价转型，企业的产能并非多建工厂就能解决，而是要在技术源头进行突破，这就对企业提出了更高的要求。多肽正是CDMO行业向细分化、专业化发展过程中，逐渐走入成熟期的细分赛道。中国生物医药发展生命周期，图源沙利文近年来，凯莱英将以多肽为代表的化学大分子CDMO作为重点发展的新兴业务，并依托其在小分子CDMO领域积累的技术、客户和质量体系优势，向多肽等化学大分子领域进行能力延伸和横向拓展。不管是传统固相多肽合成技术上的持续打磨优化、还是攻克液相多肽合成技术后成功实现复杂多肽序列的高效液相合成、以及通过生物发酵合成精准调控多肽的表达与分泌，从而实现数种生物活性多肽的工业化生产、还有化学酶促多肽合成等路径，凯莱英都已走通。此外，凯莱英在连续流反应技术（CFCT）方面的深厚积累也被应用于多肽合成过程，有助于提升收率、纯度和生产安全性，并且针对多肽未来的发展方向，布局了环肽合成技术。另一方面，凭借在小分子CDMO领域与全球顶级制药公司积累的良好口碑和合作关系，凯莱英积极将合作延伸至多肽等新兴领域，目前其多肽业务增长驱动更多来自海外大制药公司。同时，凯莱英预计在2025年下半年到2026年，多肽业务来源将逐渐变为海外为主。多肽项目进入中后期后对产能需求较高，经过前期大规模扩张，目前凯莱英产能利用率还在爬坡阶段。由于在多肽减重领域共服务了十几个分子，近半数处于临床2和3期，预计明年部分项目将进入工艺性能确认阶段，产能需求还将持续增加。根据中报披露，企业2025年底多肽固相合成总产能达44000L，并且已启动第三栋多肽厂房的建设工作。当然，像凯莱英这样能力全面的CDMO企业并不太多，对于其他竞争者，找到适合自己的垂直细分路线才更为重要。如圣诺生物以API+制剂一体化为核心布局，覆盖多肽原料药研发、生产及制剂开发全流程。在多肽合成与修饰技术上，圣诺生物拥有长链肽偶联技术、单硫环肽规模化生产技术（其硫环肽合成纯度高达95%，远超行业均值）、多对二硫环肽合成技术、聚乙二醇化修饰等。正是有了这些积累，使得企业可以在多肽药研产业链上贯穿多肽CDMO、多肽原料药和多肽制剂三端业务。更为重要的是，GLP-1业务目前占比仅有30%左右，企业并未将多肽业务固定在代谢疾病领域，在目前服务的40多个项目中，不乏全球TOP10药企的早期研发项目，涉及抗肿瘤、抗感染等领域。这种合作不仅带来了稳定的收入，更让企业在多肽领域广阔的空间中肆意开拓，如能陪伴潜在重磅品种成长，还能反哺原料药业务。此外，圣诺生物还将其多肽技术拓展到医美领域，其美容肽产品按照欧盟EFfCI GMP规范生产，覆盖抗皱紧致、舒缓修护、美白淡斑、眼周护理、生发防脱等80多个产品。还有突破长链多肽药物规模化大生产技术瓶颈，成功建立了基于固液融合的多肽规模化生产技术平台，具备侧链化学修饰多肽、长链修饰多肽数公斤级大生产能力的诺泰生物，能在司美格鲁肽、替尔泊肽等品种实现单批次超10公斤量产能力。正是有了这些技术突破，才有产能的建设，自多肽创新药CDMO106车间于2024年底投产后，107车间、108车间也在2025年上半年陆续投入运营。此外，年产395千克多肽原料药生产线项目也已顺利投产。也就是说，凭借生产工艺的突破，诺泰能够为多肽创新药和仿制药提供从工艺路线设计，到工艺验证和质量研究，以及药物研发及商业化生产的全链条定制服务，覆盖从药物发现、临床前研究，到临床试验和上市销售的完整药物开发周期。专注于多肽CDMO业务的泰德医药凭借其成熟且高效的多肽API规模化生产技术，在多肽药物设计、修饰、合成等关键环节表现出色，且在长链肽及复杂修饰肽领域中积累了大量生产案例，目前合成新分子的平均成功率超过99.95%，具备多个100千克级订单的并行处理能力。此外，泰德医药还建立了PeptiConjuX（多肽偶联药物平台）和PeptiNuclide LinkTech（放射性核素偶联药物平台）两大特色技术平台，并合成了约1900种多肽前体分子，为创新药研发提供了关键资源。这些积累有助于复杂分子的开发，协助客户解决产品纯化和杂质消除等关键技术难题，并获得了吉利德的认可。还有CDMO订单数量增速超20%的九洲药业，今年以来，多肽业务引入新客户20多家，新签合同金额近千万美元，并已完成十多个项目的交付工作。吸引他们的，是九洲药业多肽合成技术平台包含固相合成、液相合成、固液相结合以及原创的非经典固相合成技术。目前，九洲药业已成功合成了最长可达78个氨基酸的蛋白片段，远超当前热门GLP-1药物（如替尔泊肽39个氨基酸、司美格鲁肽31个氨基酸）的长度，展示了处理高难度项目的技术实力。综合来看，在多肽CDMO业务的发展上，企业们根据自身的技术特点打造了差异化优势。像凯莱英利用规模和平台效应，快速完成技术平移和产能扩张；诺泰生物、圣诺生物这类企业则在于深耕特定技术环节形成的壁垒；而泰德医药的独特优势在于其前端CRO服务带来的项目源头优势和高度国际化的运营能力。只是，作为成熟期的多肽业务是否还能持续带来收入呢？ 03 多肽的风还能吹多久多肽仍有潜力，但比拼“内功”的时代已经到来。当前多肽CDMO的繁荣主要由GLP-1药物（司美格鲁肽、替尔泊肽）减重适应症的商业化爆发驱动，这一潜力已在业绩端得到充分验证。尽管GLP-1商业化潜力逐步兑现，但后续多肽药物或仍有多元化增长动力，这主要来自技术迭代和适应症拓展。首先是多肽技术路径的创新，例如多靶点多肽药物的强势崛起，包括已经进入临床3期的礼来Retatrutide（GLP-1/GIP/GCGR三靶点，减重效率较单靶点提升30%~50%），已经获批上市的全球首个GLP-1/GCGR双靶点激动剂信达生物的玛仕度肽，还有罗氏押注的兼具减重和肌肉保护作用的Amylin胰淀素多肽，以及安进选择的超长效GLP-1受体激动剂与GIP受体拮抗剂结合的双靶点减肥药MariTide。随着普通多肽产能逐渐普及，下一阶段的竞争还将转向长链肽、复杂修饰肽（如具有稳定环状结构和高靶点亲和力的环肽药物），还有多肽药物偶联策略（包括肽-药物偶联物PDC、肽-寡核苷酸偶联技术POC）等更高技术壁垒的领域。更为重要的是，AI辅助药物设计将在PDC、环肽药物发现中发挥重要作用。适应症方面，多肽疗法呈现多线发展态势。除了GLP-1药物拓展MASH适应症外，多肽疗法也在癌症领域取得进展，如PDS Biotechnology开发的多肽疫苗PDS0101联合K药的临床2期中，使HPV16阳性复发或转移性头颈鳞状细胞癌患者中位总生存期达39.3个月。还有Elicio开发的靶向突变KRAS的多肽疫苗ELI-002，也在临床1期中取得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%的结果。此外，强生与Protagonist联合开发的用于治疗银屑病的口服多肽疗法icotrokinra也已向FDA递交NDA申请；默沙东的口服大环肽enlicitide decanoate在3期试验中能显著降低高胆固醇血症患者的低密度脂蛋白胆固醇水平。在罕见病领域，Apellis的双环肽疗法Empaveli、Stealth Bio的多肽疗法Forzinity也获得了FDA的批准。总的来看，多肽药物已成为治疗多种疾病的重要研发方向，在多个领域为患者带来了全新的治疗方案。与传统的小分子药物相比，多肽药物更为复杂，对生产过程的多个环节提出了更高要求，因而对CDMO的要求会越来越高。当前竞争虽然还是围绕GLP-1等热门靶点的产能和交付能力展开，但需求结构正在发生变化。由于在欧、美、日等市场，司美格鲁肽的核心专利保护要等到2031年，很多CDMO还在囤积产能，如若在这个过程中忽略了技术的积累与行业发展的变化，当产能过剩、研发能力滞后、市场需求波动等问题出现后，没有准备的企业或将被直接波及。当市场从短缺走向过剩，当竞争从增量市场转向存量争夺，企业的核心竞争力必然会发生变化。多肽不仅是CDMO行业的“现在”，仍可能是“未来”，但行业价值将从单纯的产能规模转向技术创新和生态构建。相关企业只有专注复杂工艺、在早期与项目绑定和适应症开拓，才能在下一代多肽药物浪潮中持续获益。 *封面图片来源：神笔PRO 如果您认同文章中的观点、信息，或想进一步讨论，请与我们联系；也可加入动脉网行业社群，结交更多志同道合的好友。近期推荐声明：动脉网所刊载内容之知识产权为动脉网及相关权利人专属所有或持有。未经许可，禁止进行转载、摘编、复制及建立镜像等任何使用。文中如果涉及企业信息和数据，均由受访者向分析师提供并确认。动脉网，未来医疗服务平台

财报抗体药物偶联物寡核苷酸申请上市

2025-11-12

·investors.apellis.com

Apellis Announces 5-Year GALE Data Showing SYFOVRE® (pegcetacoplan injection) Delayed Progression of Geographic Atrophy by ~1.5 Years

WALTHAM, Mass., Nov. 12, 2025 (GLOBE NEWSWIRE) -- Apellis Pharmaceuticals, Inc. (Nasdaq: APLS) today announced data from a post hoc analysis of the GALE extension study following five years of continuous treatment with SYFOVRE® (pegcetacoplan injection), the leading treatment for geographic atrophy (GA) secondary to age-related macular degeneration (AMD). The results demonstrate that both every-other-month and monthly SYFOVRE delayed GA lesion growth by approximately 1.5 years in patients with nonsubfoveal GA when compared to sham/projected sham. “I’m very encouraged by these long-term results, which show that early and continuous treatment with SYFOVRE can meaningfully delay the progression of GA,” said Dilsher Dhoot, M.D., California Retina Consultants. “Importantly, these data indicate that SYFOVRE alters the natural course of this disease, which causes irreversible vision loss and profoundly impacts patients’ daily lives.” “These five-year results underscore the transformative and durable impact of targeting C3 with SYFOVRE to delay the progression of GA,” said Caroline Baumal, M.D., chief medical officer, Apellis. “With the most extensive data set in GA, our broad clinical and real-world experience has greatly advanced the retina community’s understanding of this devastating disease and reinforced Apellis’ leadership.” The safety profile of SYFOVRE through five years remained consistent with previously reported data. Detailed results will be presented at a future medical meeting. About the GALE Long-Term Extension Study GALE (n=792) is a Phase 3, multicenter, open-label, extension study to evaluate the long-term efficacy and safety of SYFOVRE® (pegcetacoplan injection) in patients with geographic atrophy (GA) secondary to age-related macular degeneration (AMD). The objectives of the study are to evaluate the long-term incidence and severity of ocular and systemic treatment emergent adverse events as well as change in the total area of GA lesions as measured by fundus autofluorescence. More than 80 percent of participants who completed the OAKS and DERBY studies entered the GALE study. Patients included in the 5-year GALE lesion growth reduction analyses were in the SYFOVRE treatment arms through Month 24 in the OAKS and DERBY studies and remained on the same regimen in GALE. Sham-treated patients in the Phase 3 OAKS and DERBY studies were eligible to transition to SYFOVRE treatment in GALE after Month 24, so a projected sham arm was used to estimate the growth of GA lesions without treatment between Months 24 and 60. The projected sham arm is based on the observed linear growth of GA lesions over two years and was validated by a fellow eye analysis. It was estimated as the average 12-month mean rate of change in the OAKS and DERBY sham arms through Month 24. About the Phase 3 OAKS and DERBY Studies OAKS (n=637) and DERBY (n=621) were Phase 3, multicenter, randomized, double-masked, sham-controlled studies that compared the efficacy and safety of SYFOVRE® (pegcetacoplan injection) with sham injections across a broad and heterogenous population of patients with geographic atrophy (GA) secondary to age-related macular degeneration (AMD). The studies evaluated the efficacy of monthly and every-other-month SYFOVRE in patients with GA assessed by change in the total area of GA lesions from baseline as measured by fundus autofluorescence. In these studies at 24 months, both every-other-month and monthly SYFOVRE reduced GA lesion growth with increasing effects over time and a well-demonstrated safety profile. About SYFOVRE® (pegcetacoplan injection) SYFOVRE® (pegcetacoplan injection) is the first-ever approved therapy for geographic atrophy (GA). By targeting C3, SYFOVRE is designed to provide comprehensive control of the complement cascade, part of the body’s immune system. SYFOVRE is approved in the United States for the treatment of GA secondary to age-related macular degeneration. About Geographic Atrophy (GA) Geographic atrophy (GA) is an advanced form of age-related macular degeneration and a leading cause of blindness worldwide, impacting more than one million Americans and five million people worldwide.1,2 It is a progressive and irreversible disease caused by the growth of lesions, which destroy the retinal cells responsible for vision. The vision loss caused by GA severely impairs independence and quality of life by making it difficult to participate in daily activities. On average, it takes only 2.5 years for GA lesions to start impacting the fovea, which is responsible for central vision.3 U.S. Important Safety Information for SYFOVRE® (pegcetacoplan injection) CONTRAINDICATIONS SYFOVRE is contraindicated in patients with ocular or periocular infections, in patients with active intraocular inflammation, and in patients with hypersensitivity to pegcetacoplan or any of the excipients in SYFOVRE. Systemic hypersensitivity reactions (e.g., anaphylaxis, rash, urticaria) have occurred. WARNINGS AND PRECAUTIONS Endophthalmitis and Retinal Detachments Intravitreal injections, including those with SYFOVRE, may be associated with endophthalmitis and retinal detachments. Proper aseptic injection technique must always be used when administering SYFOVRE to minimize the risk of endophthalmitis. Patients should be instructed to report any symptoms suggestive of endophthalmitis or retinal detachment without delay and should be managed appropriately. Retinal Vasculitis and/or Retinal Vascular Occlusion Retinal vasculitis and/or retinal vascular occlusion, typically in the presence of intraocular inflammation, have been reported with the use of SYFOVRE. Cases may occur with the first dose of SYFOVRE and may result in severe vision loss. Discontinue treatment with SYFOVRE in patients who develop these events. Patients should be instructed to report any change in vision without delay. Neovascular AMD In clinical trials, use of SYFOVRE was associated with increased rates of neovascular (wet) AMD or choroidal neovascularization (12% when administered monthly, 7% when administered every other month and 3% in the control group) by Month 24. Patients receiving SYFOVRE should be monitored for signs of neovascular AMD. In case anti-Vascular Endothelial Growth Factor (anti-VEGF) is required, it should be given separately from SYFOVRE administration. Intraocular Inflammation In clinical trials, use of SYFOVRE was associated with episodes of intraocular inflammation including: vitritis, vitreal cells, iridocyclitis, uveitis, anterior chamber cells, iritis, and anterior chamber flare. After inflammation resolves, patients may resume treatment with SYFOVRE. Increased Intraocular Pressure Acute increase in IOP may occur within minutes of any intravitreal injection, including with SYFOVRE. Perfusion of the optic nerve head should be monitored following the injection and managed as needed. Intravitreal injections, including those with SYFOVRE, may be associated with endophthalmitis and retinal detachments. Proper aseptic injection technique must always be used when administering SYFOVRE to minimize the risk of endophthalmitis. Patients should be instructed to report any symptoms suggestive of endophthalmitis or retinal detachment without delay and should be managed appropriately. Retinal vasculitis and/or retinal vascular occlusion, typically in the presence of intraocular inflammation, have been reported with the use of SYFOVRE. Cases may occur with the first dose of SYFOVRE and may result in severe vision loss. Discontinue treatment with SYFOVRE in patients who develop these events. Patients should be instructed to report any change in vision without delay. In clinical trials, use of SYFOVRE was associated with increased rates of neovascular (wet) AMD or choroidal neovascularization (12% when administered monthly, 7% when administered every other month and 3% in the control group) by Month 24. Patients receiving SYFOVRE should be monitored for signs of neovascular AMD. In case anti-Vascular Endothelial Growth Factor (anti-VEGF) is required, it should be given separately from SYFOVRE administration. In clinical trials, use of SYFOVRE was associated with episodes of intraocular inflammation including: vitritis, vitreal cells, iridocyclitis, uveitis, anterior chamber cells, iritis, and anterior chamber flare. After inflammation resolves, patients may resume treatment with SYFOVRE. Acute increase in IOP may occur within minutes of any intravitreal injection, including with SYFOVRE. Perfusion of the optic nerve head should be monitored following the injection and managed as needed. ADVERSE REACTIONS Most common adverse reactions (incidence ≥5%) are ocular discomfort, neovascular age-related macular degeneration, vitreous floaters, conjunctival hemorrhage. Please see full Prescribing Information for more information. About Apellis Apellis Pharmaceuticals, Inc. is a global biopharmaceutical company leading the way in complement science to develop life-changing therapies for some of the most challenging diseases patients face. We ushered in the first new class of complement medicine in 15 years and now have two C3-targeting medicines approved to treat four serious diseases. Breakthroughs for patients include the first-ever therapy for geographic atrophy, a leading cause of blindness, and the first treatment for patients 12 and older with C3G or primary IC-MPGN, two severe, rare kidney diseases. We believe we have only begun to unlock the potential of targeting C3 across many serious diseases. For more information, please visit http://apellis.com or follow us on LinkedIn and X. Apellis Forward-Looking Statement Statements in this press release about future expectations, plans and prospects, as well as any other statements regarding matters that are not historical facts, may constitute “forward-looking statements” within the meaning of The Private Securities Litigation Reform Act of 1995. The words “anticipate,” “believe,” “continue,” “could,” “estimate,” “expect,” “intend,” “may,” “plan,” “potential,” “predict,” “project,” “should,” “target,” “will,” “would” and similar expressions are intended to identify forward-looking statements, although not all forward-looking statements contain these identifying words. Actual results may differ materially from those indicated by such forward-looking statements as a result of various important factors, including whether the data analyses reported in this release indicate an apparent positive effect that is greater than the actual positive effect, and other factors discussed in the “Risk Factors” section of Apellis’ Annual Report on Form 10-K with the Securities and Exchange Commission on February 28, 2025 and the risks described in other filings that Apellis may make with the Securities and Exchange Commission. Any forward-looking statements contained in this press release speak only as of the date hereof, and Apellis specifically disclaims any obligation to update any forward-looking statement, whether as a result of new information, future events or otherwise. Media Contact: Tracy Vineis media@apellis.com 617.420.4839 Investor Contact: Eva Stroynowski ir@apellis.com 617.938.6229 1Rudnicka AR, Jarrar Z, Wormald R, et al. Age and gender variations in age-related macular degeneration prevalence in populations of European ancestry: a meta analysis. Ophthalmology 2012;119:571–580. 2Wong WL, Su X, Li X, et al. Global prevalence of age-related macular degeneration and disease burden projection for 2020 and 2040: a systematic review and meta-analysis. Lancet Glob Health 2014;2:e106–116. 3Lindblad AS, et al, and AREDS Research Group. Arch Ophthalmol. 2009;127(9):1168-1174. A graph accompanying this announcement is available at: https://www.globenewswire.com/NewsRoom/AttachmentNg/4b4f80eb-9369-4c1f-8754-5dccbe0b4553

临床结果临床3期上市批准

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	德国	Swedish Orphan Biovitrum AB	2022-10-20

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临床结果

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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


NCT05096403 (CTgov)	临床3期	冷凝集素病	24	Pegcetacoplan (Pegcetacoplan Double Blind During Part A)	齋襯醖構淵鹽鬱艱夢襯 = 壓憲鑰構遞製憲糧衊齋鏇膚網網願蓋餘夢獵觸 (糧鑰獵齋製選夢艱網獵, 鏇選醖顧構選襯齋鹹襯 ~ 鹽範製醖築願蓋鹹繭觸) 更多	-	2025-10-30
				Placebo matching Pegcetacoplan (Placebo Matching Pegcetacoplan-Double-blind During Part A)	齋襯醖構淵鹽鬱艱夢襯 = 觸憲鏇觸鬱鹹簾繭廠鬱鏇膚網網願蓋餘夢獵觸 (糧鑰獵齋製選夢艱網獵, 鑰鏇獵餘蓋製鹽構廠繭 ~ 憲積淵積鹹觸鬱膚鬱艱) 更多
EURETINA2025	N/A	年龄相关性黄斑变性	22	Pegcetacoplan 15mg monthly	鹽積獵衊顧醖膚醖築鹹(夢鬱憲獵願窪鏇簾餘繭) = High-certainty evidence indicates that PEG or ACP do not confer significant benefit to low-luminance BCVA. 網艱鑰蓋夢顧壓憲廠憲 (鬱願鹽鏇築顧獵選艱壓 )	不佳	2025-09-04
				Pegcetacoplan 15mg every other month
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	願鬱鏇鹽蓋淵選鬱獵膚(餘簾夢艱願鬱憲餘憲壓) = 衊顧糧衊鹹襯衊蓋繭膚膚積壓膚製願製願簾壓 (窪鬱襯鑰鏇醖廠夢蓋蓋 ) 更多	积极	2025-09-04
NCT04770545 (GALE, EURETINA2025)	临床3期	年龄相关性黄斑变性	782	Pegcetacoplan (Early Treatment group)	糧壓顧遞齋網獵簾餘鬱(淵齋餘齋膚範夢選夢憲): P-Value = <0.001 更多	积极	2025-09-04
				Pegcetacoplan (Sham treatment + Delayed Treatment group)
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)	積繭醖醖醖繭積憲鏇鹹(製願觸窪餘醖簾齋簾襯) = 淵繭膚願願窪衊窪鏇鏇廠淵範廠蓋壓選遞廠醖 (艱鏇廠醖壓鏇選鑰構繭, 鏇糧糧範鑰積觸艱觸鬱 ~ 網艱簾簾築構憲糧廠遞) 更多	-	2025-08-06
				placebo+pegcetacoplan (Randomized Controlled Period: Placebo)	積繭醖醖醖繭積憲鏇鹹(製願觸窪餘醖簾齋簾襯) = 製觸構鏇範鑰顧獵範艱廠淵範廠蓋壓選遞廠醖 (艱鏇廠醖壓鏇選鑰構繭, 膚鏇觸鏇構糧膚蓋窪衊 ~ 網淵觸壓壓齋鏇鏇鹽餘) 更多
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	糧憲積積築廠醖顧鏇鹽(選餘簾膚鹽選鹽顧構憲) = 33 (4.5%) eyes with exudative AMD 範獵壓艱選觸鹽遞糧齋 (窪襯願構鏇艱鹽糧淵窪 ) 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	願餘餘淵衊範齋壓鏇蓋(餘夢願膚艱餘遞製蓋窪) = 淵齋選願窪願壓蓋艱醖醖願艱獵淵醖衊獵簾築 (築壓蓋築餘製鹽憲襯艱, 0.25，0.43)	积极	2025-07-28
				Placebo	願餘餘淵衊範齋壓鏇蓋(餘夢願膚艱餘遞製蓋窪) = 獵襯遞簾鑰築築願願窪醖願艱獵淵醖衊獵簾築 (築壓蓋築餘製鹽憲襯艱, 0.91，1.16)
NCT04085601 \| NCT03531255 \| NCT03500549 (EHA2025)	临床3期	阵发性睡眠性血红蛋白尿症	-	PEGcetacoplan (PNH patients with <4 RBCs)	築築簾築鬱齋觸繭夢鬱(遞醖遞艱積遞餘積願積) = Initial reductions in mean ARC were sustained 窪壓淵餘構鹹淵選鹽鹽 (製鹹糧齋鑰衊壓鬱齋簾 ) 更多	积极	2025-05-14
				PEGcetacoplan (PNH patients with ≥4 RBCs)
NCT05776472 (COMPLETE, EHA2025)	N/A	阵发性睡眠性血红蛋白尿症	70	Pegcetacoplan	積糧鑰製鏇夢衊觸築艱(築範鹽夢鏇醖襯糧選淵) = 獵觸膚膚構膚鹽醖襯遞觸蓋繭觸選願窪淵夢簾 (襯壓鹹積窪糧構獵廠糧, 0.8 ~ 3.3) 更多	-	2025-05-14
PF675 (EHA2025)	N/A	C5 inhibitors	26	Pegcetacoplan	糧窪艱獵憲遞蓋窪鑰鹽(壓鹹窪鹽簾糧糧夢齋簾) = 製觸選襯遞蓋簾醖築廠繭願鑰鹹襯構選觸壓衊 (遞膚衊壓糧餘選糧築鑰 ) 更多	-	2025-05-14