Pegcetacoplan

膜增生性肾小球肾炎（MPGN） 又称系膜毛细血管性肾小球肾炎，是一组以肾小球系膜细胞增生、基质扩张及毛细血管壁增厚（呈“双轨征”）为共同病理特征的慢性进展性肾小球疾病。临床上常表现为肾病综合征、血尿、高血压及进行性肾功能减退，预后较差，是导致终末期肾病的重要原因之一。 传统上， MPGN主要依赖病理形态学分类 （Ⅰ型、Ⅱ型、Ⅲ型）。然而，随着对发病机制认识的深化，现代分类更强调基于致病途径的划分，即补体异常介导的C3肾小球病（C3G，包括致密物沉积病和C3肾小球肾炎）与免疫复合物介导的MPGN。这一转变将疾病的诊断从纯粹的形态描述，推向以发病机制为核心的精准分型，对指导靶向治疗（如补体抑制剂）和判断预后具有革命性意义。 尽管诊断理念不断更新， MPGN/C3G的临床管理仍面临巨大挑战 ：发病机制复杂异质、诊断依赖侵入性肾活检、缺乏特异有效的治疗手段，且疾病易反复、进展迅速。因此，深入阐明其免疫学与分子机制、探索无创生物标志物、开发新型靶向疗法，成为该领域亟待突破的核心问题。 2025年，随着多组学技术、单细胞分析和靶向药物研发的飞速发展，MPGN/C3G领域在补体系统调控、疾病分子分型、新型治疗靶点及临床转化等方面涌现出一系列重要研究进展。本篇章旨在系统梳理与评述这些关键研究成果，以期为揭示疾病本质、改善临床实践提供新的视角与依据。 1. C3肾小球病与免疫复合物介导的膜增生性肾小球肾炎的蛋白尿与长期结局比较分析 2025年1月，《Kidney International Reports》杂志发表了一篇题为“Comparative Analysis of Proteinuria and Longitudinal Outcomes in Immune Complex Membranoproliferative Glomerulonephritis and C3 Glomerulopathy”的研究。该研究基于C3肾小球病与免疫复合物介导的膜增生性肾小球肾炎同为罕见肾病且发病机制相似，但蛋白尿减少对预后的影响尚不明确的背景，开展了一项回顾性、纵向、多中心观察性队列研究，旨在比较两者长期结局并评估蛋白尿变化对肾脏预后的预测价值。研究纳入149例患者，中位随访65个月，采用联合线性混合效应模型和Cox回归分析发现，蛋白尿随时间增加与肾功能衰竭风险显著相关，而蛋白尿减少≥50%可降低肾功能衰竭风险；进一步分析表明， 诊断后6个月内蛋白尿减少≥30%或12个月内减少≥50%与估算肾小球滤过率下降减缓及肾脏存活率改善显著相关 ，且时间平均蛋白尿维持在1克/天以下是改善预后的关键目标。该研究证实蛋白尿变化是评估C3肾小球病和免疫复合物介导的膜增生性肾小球肾炎疾病进展的有力替代指标，为临床治疗目标设定和临床试验终点选择提供了重要依据。 图1 eGFR与蛋白尿的个体纵向轨迹及其与肾功能衰竭风险的关系 2. Avacopan在C3肾小球病患者中的安全性和有效性：随机、双盲临床试验 2025年3月，《Journal of the American Society of Nephrology》杂志发表了一篇题为“Safety and Efficacy of Avacopan in Patients with C3 Glomerulopathy: Randomized, Double-Blind Clinical Trial”的研究。鉴于C3肾小球病是一种由补体替代途径异常激活驱动的罕见肾病，目前缺乏获批疗法，本研究开展了一项随机、双盲、安慰剂对照的Ⅱ期临床试验，旨在评估口服C5a受体拮抗剂Avacopan的疗效与安全性。研究纳入57例C3肾小球病患者（包括C3肾小球肾炎和致密物沉积病），随机分配接受Avacopan（30 mg，每日两次）或安慰剂治疗26周，主要终点为第26周时疾病活动的C3肾小球病组织学指数较基线的百分比变化。结果显示， 在主要终点上，Avacopan组与安慰剂组无显著差异 （95% CI=-0.0[-1.9，1.8]）；次要终点如疾病慢性化指数、尿蛋白肌酐比和估算肾小球滤过率在整体人群中也无显著组间差异。然而，亚组分析提示， 在基线尿蛋白肌酐比>1 g/g且估算肾小球滤过率<60 mL/（min·1.73 m²）的患者中，Avacopan可能改善蛋白尿和肾功能 。安全性方面，Avacopan耐受性良好，不良事件发生率与安慰剂组相当。该研究是迄今为止在C3肾小球病患者中规模最大的补体抑制剂随机试验，虽然未达到主要终点，但为理解C5a受体抑制在该疾病中的作用提供了重要数据，并提示Avacopan可能在特定疾病活动度较高的患者亚群中具有潜在治疗价值，为未来临床试验设计和患者选择提供了参考。 表1 ITT人群中主要和次要终点（基线至第26周） 3. 膜增生性肾小球肾炎的重复肾活检研究 2025年4月，《Kidney Diseases》发表了一篇题为“Repeated Kidney Biopsy in Membranoproliferative Glomerulonephritis”的研究。鉴于膜增生性肾小球肾炎（MPGN）是一组病因异质性大、诊断分类不断演变的疾病谱，且首次活检可能无法完全揭示疾病全貌，本研究开展了一项单中心、回顾性分析，旨在探究重复肾活检在MPGN患者中的价值及其对诊断与治疗的指导意义。研究纳入了82例在1997至2023年间至少接受过两次肾活检的MPGN患者，分析其两次活检间的临床与病理数据变化。结果显示， 在平均间隔2.3年后，患者肾功能显著恶化 [eGFR从70降至39 mL/（min·1.73 m²）]，蛋白尿增加（从3.9增至6.4 g/天），肾组织慢性化病变（肾小球硬化、间质纤维化）加重；更重要的是， 51%的患者在两次活检间出现了病理形态的重新分类 （如从膜性肾病等转变为MPGN）， 37%的患者实现了病因学的再分类 ，其中最主要的是确诊为肾脏意义未明的单克隆丙种球蛋白病（MGRS），且64%的MGRS患者血清或尿免疫固定电泳持续阴性；与特发性MPGN相比，MGRS患者年龄更大（53岁 vs 35岁）、基线肾功能更差[eGFR 57 vs 81 mL/（min·1.73 m²）]，但肾功能下降速度较慢[-7 vs -12 mL/（min·1.73 m²）/年]。该研究首次系统评估了MPGN重复活检的意义，证实重复活检能动态揭示疾病从非MPGN向MPGN表型演变、并强力驱动病因再分类（尤其是识别出血清学阴性的MGRS），从而从根本上改变治疗策略（从无效的免疫抑制转向克隆导向治疗），凸显了在常规治疗反应不佳时重复活检的必要性，并为未来开发无创性动态监测工具提供了依据。 表2 所有患者初次与重复肾活检的临床与病理特征比较 4. 因子H相关蛋白1和硫酸乙酰肝素结构导致C3肾小球病中补体失调的机制 2025年5月，《Frontiers in Immunology》杂志发表了一篇题为“Factor H-related 1 and heparan sulfate architecture contribute to complement dysregulation in C3 glomerulopathy”的研究。该研究针对由补体替代途径失调驱动的罕见肾脏疾病C3肾小球病（C3G），旨在探究补体调节蛋白因子H（FH）及其竞争性蛋白FHR-1、FHR-5在疾病中的作用机制。研究采用基因型分析、循环蛋白水平检测及体外功能实验相结合的方法，发现 CFHR3-CFHR1基因拷贝数变异影响C3G风险 ，且随着肾功能下降，患者体内FHR-1与FH的比率普遍升高，这一现象不仅见于C3G，也出现在其他原因导致的慢性肾病中。功能实验进一步表明，FHR-1能与FH竞争结合细胞表面，增强C3b沉积，而硫酸乙酰肝素（HS）结构的破坏（如经肝素酶处理）会进一步加剧该效应。该研究揭示了在肾功能减退背景下，FHR-1/FH比例失衡与HS结构损伤共同导致局部补体活性增强，可能推动慢性肾病的炎症进展与损伤恶化，为理解补体在肾病进展中的作用机制及未来抗补体治疗提供了重要依据。 图2 按慢性肾病分期划分的补体蛋白水平与比率 5. 量化C3肾小球病和免疫复合物膜增生性肾小球肾炎中早期蛋白尿与估算肾小球滤过率变化同长期肾功能衰竭的关联 2025年6月，《Kidney International》杂志发表了一篇题为“Quantifying association of early proteinuria and estimated glomerular filtration rate changes with long-term kidney failure in C3 glomerulopathy and immune-complex membranoproliferative glomerulonephritis using the United Kingdom RaDaR Registry”的研究。该研究针对常导致长期肾功能衰竭的罕见肾脏疾病C3肾小球病和免疫复合物膜增生性肾小球肾炎，旨在评估临床试验中可用的短期替代终点（如蛋白尿和eGFR变化）能否有效预测长期肾功能衰竭这一关键临床结局。研究基于英国罕见肾脏病登记处的纵向数据，纳入了371例患者，采用Cox回归与线性混合模型等方法，在中位随访11.0年间（40%患者进展至肾功能衰竭），分析了诊断后早期蛋白尿变化和eGFR斜率与长期肾功能衰竭风险的关系。结果显示，诊断后两年的eGFR斜率与肾功能衰竭仅有中度关联；相比之下，诊断后12个月内尿蛋白肌酐比值的降低（无论是绝对值减少50 mg/mmol，还是百分比降低20%或50%）与肾功能衰竭风险显著降低强烈相关，其中 在12个月时将UPCR控制在100 mg/mmol以下的患者，其肾功能衰竭风险降低了90% 。该研究首次大样本量化了C3肾小球病和免疫复合物膜增生性肾小球肾炎患者早期蛋白尿改善与长期预后的强劲关联，为在此类罕见病短期临床试验中将蛋白尿作为预测长期肾功能获益的有效替代终点提供了关键数据支持，对加速新疗法（如补体抑制剂）的评估和审批具有重要意义。 图3 按诊断时及诊断后12个月尿蛋白肌酐比值分组的肾功能衰竭生存曲线 6. 截短补体因子H Y402基因疗法可挽救C3肾小球肾炎 2025年8月，《Molecular Therapy》杂志发表了一篇题为“Truncated complement factor H Y402 gene therapy rescues C3 glomerulonephritis”的研究。该研究针对因补体因子H（CFH）缺陷导致补体失调、目前缺乏有效治疗方法的C3肾小球肾炎（C3G）以及年龄相关性黄斑变性（AMD），旨在探索基于腺相关病毒（AAV）的基因替代疗法。研究采用CFH基因敲除（CfH⁻/⁻）小鼠作为C3G模型，通过尾静脉注射靶向肝脏的AAV8病毒载体，递送三种不同截短版本的人CFH（12tCFH、18tCFH和内源性剪接变体FHL-1）基因，以驱动肝脏特异性表达并补充功能性CFH。结果显示，单次系统性AAV给药后，12tCFH与18tCFH均能有效恢复补体替代途径的调节，显著提升血浆中完整C3水平、降低C3b，并在长达12周的治疗期内成功逆转了C3G的关键病理特征：肾小球C3沉积显著减少，肾小球基底膜增厚和系膜基质扩张得到明显改善，且未引发针对外源蛋白的免疫排斥反应。该研究 首次在C3G动物模型中证实了AAV介导的截短CFH基因疗法的长期有效性 ，不仅为C3G提供了一种全新的潜在治愈性策略，也为病理机制相似的AMD（特别是干性AMD）的基因治疗开发提供了重要的概念验证和候选分子（如12tCFH）。 图4 AAV介导的CFH替代减少C3沉积积累并缓解C3G 7. 口服iptacopan治疗C3肾小球病患者：一项随机、双盲、平行组、多中心、安慰剂对照的Ⅲ期研究 2025年9月，《Lancet》杂志发表一篇题为“Oral ipitacopan therapy in patients with C3 glomerulopathy: a randomised, double-blind, parallel group, multicentre, placebo-controlled, phase 3 study”的研究。C3肾小球病是一种由补体替代途径过度激活引起的罕见进展性肾病，既往缺乏靶向治疗手段。本研究旨在评估口服补体因子B抑制剂iptacopan（联合支持治疗）的疗效与安全性。该Ⅲ期临床试验（APPEAR-C3G）纳入74例成年患者，随机分为iptacopan组（200 mg，每日两次）与安慰剂组，治疗6个月后进入6个月开放标签期。结果显示， 治疗6个月后，iptacopan组24小时尿蛋白肌酐比（UPCR）较基线相对降低35.1%，显著优于安慰剂组（P=0.0014） ，且蛋白尿减少迅速、持续至12个月；估算肾小球滤过率（eGFR）在iptacopan组趋于稳定，而安慰剂组呈下降趋势。安全性方面，iptacopan耐受性良好，无死亡或治疗中断事件，不良事件多为轻中度。该研究证实iptacopan能靶向抑制补体替代途径，显著降低蛋白尿并稳定肾功能，为C3肾小球病提供了首个具有病因针对性的治疗选择，有望改善患者长期预后。 图5 治疗6个月和12个月时蛋白尿（24小时UPCR）相对于基线的百分比变化 8. 层次聚类揭示疾病模式并进一步阐明免疫复合物介导的特发性MPGN与C3肾小球病的复杂性 2025年10月，《Kidney International》杂志在线发表一篇题为“Hierarchical clustering uncovered disease patterns and further untangled complexities in immune complex-mediated idiopathic MPGN and C3 glomerulopathy”的研究。膜增生性肾小球肾炎（MPGN）及其亚型C3肾小球病（C3G）与免疫复合物介导的MPGN（IC-MPGN）在病理机制和临床管理上存在重叠与争议，传统组织学分类难以指导精准治疗。本研究旨在通过层次聚类分析，整合临床、组织学、遗传及补体数据，揭示疾病内在亚型并评估其预后价值。研究对意大利MPGN登记系统中295例患者进行回顾性分析，使用29项变量进行层次聚类，识别出5个具有独特表型与补体特征的疾病簇：簇1和2表现为系统性补体激活至C5水平，簇3以C3受限性激活为主，簇4和5则呈正常循环补体谱但伴肾小球C3强沉积。聚类分析显示，簇4患者肾脏预后最差（10年内进展至终末期肾病风险最高），簇1预后最佳；簇1和2移植后复发风险较高。研究还开发了公开可用的网络应用程序，可基于诊断时数据将新患者归类至相应簇，分类准确率达85%~89%。该研究提出了一种 基于多维度特征的疾病分类新策略 ，其预后预测能力优于传统组织学分型，有望指导个体化抗补体治疗选择，推动C3G/IC-MPGN的精准医疗实践。 图6 不同患者簇的肾脏结局比较 9. C3肾小球病的十年——一项全国性队列研究 2025年11月，《Kidney International Reports》杂志发表一篇题为“A Decade of C3 Glomerulopathy—A Nationwide Cohort Study”的研究。C3肾小球病是一种罕见但严重的肾脏疾病，常导致终末期肾衰竭，其流行病学特征及亚型分布尚不明确。本研究旨在利用荷兰全国病理数据库（Palga），分析2014年至2023年间C3G的发病率、亚型分布及其与地理、组织学模式的关系。研究通过回顾性队列分析，共纳入280例经活检确诊的C3G患者，包括C3肾小球肾炎（C3GN，101例）、致密物沉积病（DDD，39例）、未分型C3G（106例）、感染后C3G（C3-PIGN，29例）及其他类型（5例）。结果显示， 荷兰C3G年平均发病率为每百万人年1.43例；DDD患者诊断中位年龄显著低于C3GN （19岁 vs 54岁，P<0.001）；各亚型与组织学模式存在关联，DDD与C3GN多表现为膜增生性肾小球肾炎模式，而C3-PIGN则以毛细血管内或渗出性模式为主；地理分析显示，C3G分布与人口密度相关，但无区域性聚集或亚型分布不均。该研究证实了全国范围内肾脏病理评估的一致性，强调免疫荧光与电镜检查对C3G精确分型的必要性，并为这一罕见疾病的流行病学、自然史及未来临床研究提供了重要基线数据。 图7 C3G各亚型的年龄分布与小提琴图 10. Pegcetacoplan在C3肾小球病和免疫复合物MPGN中的试验 2025年12月，《The New England Journal of Medicine》发表了一篇题为“Trial of Pegcetacoplan in C3 Glomerulopathy and Immune-Complex MPGN”的3期临床研究。C3肾小球病和原发性免疫复合物膜增生性肾小球肾炎（MPGN）是罕见的补体介导的肾脏疾病，常导致肾小球C3沉积和不可逆的肾功能损伤，现有治疗手段有限。该研究旨在通过一项多中心、双盲、安慰剂对照的Ⅲ期临床试验，评估补体C3/C3b抑制剂Pegcetacoplan在减少蛋白尿、稳定肾功能方面的疗效与安全性。研究共纳入124例患者，随机分为Pegcetacoplan组与安慰剂组，治疗26周后结果显示， Pegcetacoplan组尿蛋白肌酐比相较于基线平均下降67.2%，显著优于安慰剂组的2.9%（相对降低68.1%） ，且更多患者达到复合肾脏终点（49% vs 3%）和蛋白尿降低≥50%（60% vs 5%）。安全性方面，两组不良事件发生率相近，未出现封装细菌所致严重感染或移植物排斥。该研究证实Pegcetacoplan能显著减轻蛋白尿并有望延缓疾病进展，为C3肾小球病和免疫复合物MPGN提供了首个针对补体C3的高效靶向治疗选择，具有重要的临床转化意义。 图8 肾活检C3染色强度变化图 总结与展望 总体而言膜增生性肾小球肾炎（MPGN/C3G）的临床管理仍是一项艰巨挑战。尽管在疾病机制认识上有所深化，但将其转化为广泛有效的临床治疗手段仍有长路要走。未来研究需进一步在分子层面解析疾病的异质性，推动基于机制的精准分型，并加速新型靶向疗法的开发与验证。通过多学科协作与创新技术的融合，有望最终改善这类疾病患者的长期预后。 参考文献 参考文献 1.Caravaca-Fontán F, Toledo-Rojas R, Huerta A, Pérez-Canga JL, Martínez-Miguel P, Miquel R, Da Silva I, Verdalles Ú, Albornoz M, Durán López CM, Mon C, Fernández-Juárez G, Praga M; C3G study group from the Spanish Group for the Study of Glomerular Diseases. Comparative Analysis of Proteinuria and Longitudinal Outcomes in Immune Complex Membranoproliferative Glomerulonephritis and C3 Glomerulopathy. Kidney Int Rep. 2025 Jan 18;10(4):1223-1236. doi: 10.1016/j.ekir.2025.01.024. PMID: 40303231; PMCID: PMC12034854. 2.Bomback AS, Herlitz LC, Kedia PP, Petersen J, Yue H, Lafayette RA; ACCOLADE Study Group. Safety and Efficacy of Avacopan in Patients with Complement 3 Glomerulopathy: Randomized, Double-Blind Clinical Trial. J Am Soc Nephrol. 2025 Mar 1;36(3):487-499. doi: 10.1681/ASN.0000000526. Epub 2024 Oct 11. PMID: 39392695; PMCID: PMC11888959. 3.Li AH, Li Y, Li MS, Song ZR, Lv JC, Zhang H, Yu XJ, Zhou XJ. Repeated Kidney Biopsy in Membranoproliferative Glomerulonephritis. Kidney Dis (Basel). 2025 Apr 4;11(1):258-269. doi: 10.1159/000545727. PMID: 40337160; PMCID: PMC12058111. 4.Slagle AK, Ghiringhelli Borsa N, Wang K, Taylor AO, Meyer NC, Jones MB, Walls WD, Nelson AFM, Roberts SM, Sun M, Goicoechea de Jorge E, Rodriguez de Cordoba S, Jalal DI, Nester CM, Zhang Y, Smith RJH. Factor H-related 1 and heparan sulfate architecture contribute to complement dysregulation in C3 glomerulopathy. Front Immunol. 2025 May 16;16:1589674. doi: 10.3389/fimmu.2025.1589674. PMID: 40453077; PMCID: PMC12122740. 5.Masoud S, Wong K, Pitcher D, Downward L, Proudfoot C, Webb NJA; RaDaR Consortium; Wong EKS, Gale DP. Quantifying association of early proteinuria and estimated glomerular filtration rate changes with long-term kidney failure in C3 glomerulopathy and immune-complex membranoproliferative glomerulonephritis using the United Kingdom RaDaR Registry. Kidney Int. 2025 Sep;108(3):455-469. doi: 10.1016/j.kint.2025.06.003. Epub 2025 Jun 27. PMID: 40582408. 6.Chew LA, Grigsby D, Hester CG, Amason J, McPherson WK, Flynn EJ 3rd, Visel M, Starr CR, Flannery JG, Lewis TR, Bowes Rickman C. Truncated complement factor H Y402 gene therapy rescues C3 glomerulonephritis. Mol Ther. 2025 Aug 6;33(8):3746-3756. doi: 10.1016/j.ymthe.2025.04.035. Epub 2025 Apr 24. PMID: 40285355; PMCID: PMC12461626. 7.Kavanagh D, Bomback AS, Vivarelli M, Nester CM, Remuzzi G, Zhao MH, Wong EKS, Wang Y, Krishnan I, Schuhmann I, Trapani AJ, Webb NJA, Meier M, Israni RK, Smith RJH; APPEAR-C3G investigators. Oral iptacopan therapy in patients with C3 glomerulopathy: a randomised, double-blind, parallel group, multicentre, placebo-controlled, phase 3 study. Lancet. 2025 Oct 11;406(10512):1587-1598. doi: 10.1016/S0140-6736(25)01148-1. Epub 2025 Sep 25. PMID: 41016405. 8.Benigni A, Daina E, Löffler-Wirth H, Piras R, Rigoldi M, Schmidt M, Carrara C, Donadelli R, Imanifard Z, Mele C, Alberti M, Marasà M, Martinatto C, Bresin E, Gamba S, Quadri L, Nanchen G, Vivarelli M, Emma F, La Manna G, Vidal E, Pasini A, Ranghino A, Donati G, Verrina E, Angeletti A, Brunori G, Giordano M, Alberici F, Maggiore U, Malgieri G, Remuzzi G, Breno M, Noris M; Italian Registry of MPGN. Hierarchical clustering uncovered disease patterns and further untangled complexities in immune complex-mediated idiopathic MPGN and C3 glomerulopathy. Kidney Int. 2026 Jan;109(1):178-195. doi: 10.1016/j.kint.2025.08.035. Epub 2025 Oct 10. PMID: 41076080. 9.Overwijk RH, Kolbinger FR, Eijgelsheim M, Dekkers OM, Kronbichler A, Bajema IM. A Decade of C3 Glomerulopathy-A Nationwide Cohort Study. Kidney Int Rep. 2025 Nov 12;11(2):103681. doi: 10.1016/j.ekir.2025.11.007. PMID: 41537099; PMCID: PMC12795654. 10.Fakhouri F, Bomback AS, Ariceta G, Delmas Y, Dixon BP, Gale DP, Greenbaum LA, Han SH, Isbel N, Le Quintrec M, Licht C, Mastrangelo A, Mizuno M, Neves de Holanda MI, Pickering MC, Remuzzi G, Van De Kar N, Vivarelli M, Walker PD, Wallace D, Zecher D, Francois C, Deschatelets P, Li L, Wang Z, Abad-Franch L, Kinnman N, López-Lázaro L, Szamosi J, Nester CM; VALIANT Trial Investigators Group. Trial of Pegcetacoplan in C3 Glomerulopathy and Immune-Complex MPGN. N Engl J Med. 2025 Dec 4;393(22):2210-2220. doi: 10.1056/NEJMoa2501510. PMID: 41337715. 刘章锁 中原学者、国家教学名师。郑州大学第一附属医院首席教授、博士生（后）导师，河南省肾脏病研究中心主任、郑州大学肾脏病研究所所长。兼任中华医学会医学信息学分会主任委员、中国研究型医院学会肾脏病学专业委员会主任委员。研究方向：糖尿病肾病等代谢性疾病发病机制与临床转化研究，入选2025年全球前2%顶尖科学家榜单。 刘东伟 主任医师、博士生导师、国医大师张大宁师承弟子、郑州大学第一附属医院中西医结合肾病科主任。中华中医药学会补肾活血法分会副主任委员、中国研究型医院学会肾脏病学分会常委兼秘书长、河南省医学会医学科普分会主任委员，研究方向：膜性肾病发病机制研究与临床转化探索，入选2025年全球前2%顶尖科学家榜单。 田飞 研究实习员，郑州大学肾脏病研究所、河南省肾脏病研究中心成员。

Full-year 2025 net product revenues of $689 million SYFOVRE ® (pegcetacoplan injection) full year 2025 net product revenue of $587 million EMPAVELI ® (pegcetacoplan) full year 2025 net product revenue of $102 million Regulatory submission for SYFOVRE prefilled syringe planned for the first half of 2026 EMPAVELI franchise has strong momentum with successful launch in C3G and primary IC-MPGN, and pivotal trials underway in FSGS and DGF Cash and cash equivalents of $466 million as of December 31, 2025; projected revenues, cash, and cash equivalents expected to be sufficient to fund operations to profitability Management to host conference call today at 8:30 a.m. ET WALTHAM, Mass., Feb. 24, 2026 (GLOBE NEWSWIRE) -- Apellis Pharmaceuticals , Inc. (Nasdaq: APLS), today announced its fourth quarter and full year 2025 financial results and business highlights. “2025 was a year of disciplined execution and meaningful progress across the business, and we enter 2026 with clear priorities and a strong foundation,” said Cedric Francois, M.D., Ph.D., chief executive officer at Apellis. “We are focused on positioning SYFOVRE for its next phase of growth, maximizing EMPAVELI’s blockbuster opportunity in rare kidney diseases, and advancing a differentiated, self-funded pipeline leveraging our deep expertise in C3 biology.” Fourth Quarter and Full Year 2025 Business Highlights and Upcoming Milestones Transforming the treatment of geographic atrophy (GA) with SYFOVRE Reported $155 million and $587 million in U.S. net product revenues in the fourth quarter and full year 2025, respectively. Total injections increased 17% year-over-year, reflecting continued strong underlying demand. Continued market leadership in GA with total market share of approximately 60%. Delivered approximately 102K SYFOVRE doses to physician offices during the fourth quarter of 2025, including approximately 89K commercial doses and approximately 13K free goods doses. Advanced best-in-class prefilled syringe, with a regulatory submission planned in the first half of 2026. Presented new data on the OCT-F (Optical Coherence Tomography – Functional) program, an AI imaging tool designed to visualize functional decline and quantify treatment impact, at the virtual Angiogenesis (Angiogenesis, Exudation, and Degeneration) annual meeting in February 2026; the tool is expected to be available for research use in retina specialist practices in the second half of 2026. Eight abstracts were accepted for oral presentation at the upcoming Macula Society Annual Meeting, including the first presentation of comprehensive five-year results from the GALE open-label extension study. The Phase 2 study of SYFOVRE + APL-3007, a potential next generation treatment aimed at comprehensively blocking complement activity in the retina and choroid, is ongoing with topline data expected in 2027. Maximizing EMPAVELI’s impact in rare diseases Recorded $35 million and $102 million in U.S. net product revenues in the fourth quarter and full year 2025, respectively. Executed strong early launch in C3 glomerulopathy (C3G) and primary immune complex glomerulonephritis (IC-MPGN). Received 267 cumulative patient start forms as of December 31, 2025, representing more than 5% penetration of the U.S. patient population 1 following the first full quarter post-launch. Achieved favorable payer access with 95% of published policies covering to label or with minimal restrictions. Sobi recently received European Commission approval for Aspaveli in C3G and primary IC-MPGN, triggering a $25 million milestone payment to Apellis based on the July 2025 royalty purchase agreement. Initiated pivotal trials for focal segmental glomerulosclerosis (FSGS) and delayed graft function (DGF), two rare kidney diseases with significant complement pathway involvement and high unmet need. Advancing innovative pipeline, leveraging complement expertise Progressed investigational pre-clinical research of APL-9099 2 , a potential one-time neonatal Fc receptor (FcRn) treatment using base editing technology from Beam Therapeutics. An investigational new drug (IND) submission is planned for the second half of 2026. Fourth Quarter and Full Year 2025 Financial Results Total revenue for the three and twelve months ended December 31, 2025, was $199.9 million and $1.0 billion, respectively, compared to $212.5 million and $781.4 million for the same periods in 2024, and mainly consists of: Product net sales for SYFOVRE and EMPAVELI: SYFOVRE U.S. net product revenue for the three and twelve months ended December 31, 2025, was $155.2 million and $586.9 million, respectively, compared to $167.8 million and $611.8 million for the same periods in 2024. EMPAVELI U.S. net product revenue for the three and twelve months ended December 31, 2025, was $35.1 million and $102.4 million, respectively, compared to $23.4 million and $98.1 million for the same periods in 2024. Licensing and other revenue for the three and twelve months ended December 31, 2025, was $9.6 million and $314.4 million, respectively, compared to $21.4 million and $71.4 million for the same periods in 2024. This mainly relates to the Company’s licensing and other revenue associated with the Sobi collaboration, including the one-time $275.0 million upfront payment from the Sobi royalty repurchase agreement, which was recorded in the third quarter of 2025. Total operating expenses for the three and twelve months ended December 31, 2025, were $251.1 million and $948.4 million, respectively, compared to $238.7 million and $946.3 million for the same periods in 2024, and mainly consists of: Cost of sales for the three and twelve months ended December 31, 2025, were $29.7 million and $102.2 million, respectively, compared to $40.9 million and $117.7 million for the same periods in 2024. Cost of sales consists primarily of costs associated with the manufacturing of SYFOVRE and EMPAVELI, royalties owed to our licensor for such sales, costs associated with Sobi revenue, and certain period costs. R&D expenses for the three and twelve months ended December 31, 2025, were $74.2 million and $295.9 million, respectively, compared to $76.4 million and $327.6 million for the same periods in 2024. The decrease in R&D expenses for the full year ended December 31, 2025, was primarily attributable to a decrease in program specific external costs and compensation and related personnel costs. Selling, General and Administrative (SG&A) expenses for the three and twelve months ended December 31, 2025, were $147.1 million and $550.3 million, respectively, compared to $121.5 million and $501.1 million for the same periods in 2024. The increase was primarily attributable to an increase in professional and consulting fees, an increase in personnel related cost and an increase in general and administrative expenses, including contributions to patient assistance organizations, office expenses, travel expenses, insurance expenses, professional and consulting fees, and other general and administrative expenses, which was partially offset by a decrease in general commercial activities. Net Loss / Income: For the three months ended December 31, 2025, the Company reported a net loss of $58.9 million, compared to a net loss of $36.4 million for the same period in 2024. For the twelve months ended December 31, 2025, the Company reported net income of $22.4 million, compared to a net loss of $197.9 million for the full year 2024. Cash and cash equivalents of $466.2 million as of December 31, 2025, compared to $411.3 million in cash and cash equivalents as of December 31, 2024. Apellis continues to expect that its cash and cash equivalents, combined with expected product revenues, will fund the business to profitability. Conference Call and Webcast Apellis will host a conference call and webcast to discuss its fourth quarter and full year 2025 financial results and business highlights today, February 24, 2026, at 8:30 a.m. ET. To access the live call by phone, please pre-register for the call here . A live audio webcast of the event and accompanying slides may also be accessed through the “Events and Presentations” page of the “Investors and Media” section of the company’s website . A replay of the webcast will be available for 30 days following the event. 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 EMPAVELI ® /Aspaveli ® (pegcetacoplan) EMPAVELI ® /Aspaveli ® (pegcetacoplan) is a targeted C3 therapy designed to regulate excessive activation of the complement cascade, part of the body’s immune system, which can lead to the onset and progression of many serious diseases. It is the first treatment approved in the United States for C3 glomerulopathy (C3G) or primary immune complex membranoproliferative glomerulonephritis (IC-MPGN) in patients 12 years of age or older, to reduce proteinuria. EMPAVELI/Aspaveli ® is also approved for the treatment of adults with paroxysmal nocturnal hemoglobinuria (PNH) in the United States, European Union, and other countries globally, and for the treatment of C3G and primary IC-MPGN in the European Union and other countries globally. EMPAVELI is being evaluated for the treatment of additional rare diseases. About the Apellis and Sobi Collaboration Apellis and Sobi have global co-development rights for systemic pegcetacoplan. Sobi has exclusive ex-U.S. commercialization rights for systemic pegcetacoplan, and Apellis has exclusive U.S. commercialization rights for systemic pegcetacoplan and worldwide commercial rights for ophthalmological pegcetacoplan, including for geographic atrophy. 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. 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. for more information. U.S. Important Safety Information for EMPAVELI ® (pegcetacoplan) BOXED WARNING: SERIOUS INFECTIONS CAUSED BY ENCAPSULATED BACTERIA EMPAVELI, a complement inhibitor, increases the risk of serious infections, especially those caused by encapsulated bacteria, such as Streptococcus pneumoniae, Neisseria meningitidis , and Haemophilus influenzae type B. Life-threatening and fatal infections with encapsulated bacteria have occurred in patients treated with complement inhibitors. These infections may become rapidly life-threatening or fatal if not recognized and treated early. Complete or update vaccination for encapsulated bacteria at least 2 weeks prior to the first dose of EMPAVELI, unless the risks of delaying therapy with EMPAVELI outweigh the risks of developing a serious infection. Comply with the most current Advisory Committee on Immunization Practices (ACIP) recommendations for vaccinations against encapsulated bacteria in patients receiving a complement inhibitor. Patients receiving EMPAVELI are at increased risk for invasive disease caused by encapsulated bacteria, even if they develop antibodies following vaccination. Monitor patients for early signs and symptoms of serious infections and evaluate immediately if infection is suspected. Because of the risk of serious infections caused by encapsulated bacteria, EMPAVELI is available only through a restricted program under a Risk Evaluation and Mitigation Strategy (REMS) called the EMPAVELI REMS. CONTRAINDICATIONS Hypersensitivity to pegcetacoplan or to any of the excipients For initiation in patients with unresolved serious infection caused by encapsulated bacteria including Streptococcus pneumoniae , Neisseria meningitidis , and Haemophilus influenzae type B WARNINGS AND PRECAUTIONS Serious Infections Caused by Encapsulated Bacteria EMPAVELI, a complement inhibitor, increases a patient’s susceptibility to serious, life-threatening, or fatal infections caused by encapsulated bacteria including Streptococcus pneumoniae , Neisseria meningitidis (caused by any serogroup, including non-groupable strains), and Haemophilus influenzae type B. Life-threatening and fatal infections with encapsulated bacteria have occurred in both vaccinated and unvaccinated patients treated with complement inhibitors. The initiation of EMPAVELI treatment is contraindicated in patients with unresolved serious infection caused by encapsulated bacteria. Complete or update vaccination against encapsulated bacteria at least 2 weeks prior to administration of the first dose of EMPAVELI, according to the most current ACIP recommendations for patients receiving a complement inhibitor. Revaccinate patients in accordance with ACIP recommendations considering the duration of therapy with EMPAVELI. Note that ACIP recommends an administration schedule in patients receiving complement inhibitors that differs from the administration schedule in the vaccine prescribing information. If urgent EMPAVELI therapy is indicated in a patient who is not up to date with vaccines against encapsulated bacteria according to ACIP recommendations, provide the patient with antibacterial drug prophylaxis and administer these vaccines as soon as possible. The benefits and risks of treatment with EMPAVELI, as well as the benefits and risks of antibacterial drug prophylaxis in unvaccinated or vaccinated patients, must be considered against the known risks for serious infections caused by encapsulated bacteria. Vaccination does not eliminate the risk of serious encapsulated bacterial infections, despite development of antibodies following vaccination. Closely monitor patients for early signs and symptoms of serious infection and evaluate patients immediately if an infection is suspected. Inform patients of these signs and symptoms and instruct patients to seek immediate medical care if these signs and symptoms occur. Promptly treat known infections. Serious infection may become rapidly life-threatening or fatal if not recognized and treated early. Consider interruption of EMPAVELI in patients who are undergoing treatment for serious infections. EMPAVELI is available only through a restricted program under a REMS. EMPAVELI REMS EMPAVELI is available only through a restricted program under a REMS called EMPAVELI REMS, because of the risk of serious infections caused by encapsulated bacteria. Notable requirements of the EMPAVELI REMS include the following: Under the EMPAVELI REMS, prescribers must enroll in the program. Prescribers must counsel patients about the risks, signs, and symptoms of serious infections caused by encapsulated bacteria, provide patients with the REMS educational materials, ensure patients are vaccinated against encapsulated bacteria at least 2 weeks prior to the first dose of EMPAVELI, prescribe antibacterial drug prophylaxis if patients’ vaccine status is not up to date and treatment must be started urgently, and provide instructions to always carry the Patient Safety Card both during treatment, as well as for 2 months following last dose of EMPAVELI. Pharmacies that dispense EMPAVELI must be certified in the EMPAVELI REMS and must verify prescribers are certified. Further information is available at or 1-888-343-7073. Infusion-Related Reactions Systemic hypersensitivity reactions (eg, facial swelling, rash, urticaria, pyrexia) have occurred in patients treated with EMPAVELI, which may resolve after treatment with antihistamines. Cases of anaphylaxis leading to treatment discontinuation have been reported. If a severe hypersensitivity reaction (including anaphylaxis) occurs, discontinue EMPAVELI infusion immediately, institute appropriate treatment, per standard of care, and monitor until signs and symptoms are resolved. Monitoring Paroxysmal Nocturnal Hemoglobinuria (PNH) Manifestations after Discontinuation of EMPAVELI After discontinuing treatment with EMPAVELI, closely monitor for signs and symptoms of hemolysis, identified by elevated LDH levels along with sudden decrease in PNH clone size or hemoglobin, or reappearance of symptoms such as fatigue, hemoglobinuria, abdominal pain, dyspnea, major adverse vascular events (including thrombosis), dysphagia, or erectile dysfunction. Monitor any patient who discontinues EMPAVELI for at least 8 weeks to detect hemolysis and other reactions. If hemolysis, including elevated LDH, occurs after discontinuation of EMPAVELI, consider restarting treatment with EMPAVELI. Interference with Laboratory Tests There may be interference between silica reagents in coagulation panels and EMPAVELI that results in artificially prolonged activated partial thromboplastin time (aPTT); therefore, avoid the use of silica reagents in coagulation panels. ADVERSE REACTIONS Most common adverse reactions in adult patients with PNH (incidence ≥10%) were injection site reactions, infections, diarrhea, abdominal pain, respiratory tract infection, pain in extremity, hypokalemia, fatigue, viral infection, cough, arthralgia, dizziness, headache, and rash. Most common adverse reactions in adult and pediatric patients 12 years of age and older with C3 glomerulopathy (C3G) or primary immune-complex membranoproliferative glomerulonephritis (IC-MPGN) (incidence ≥10%) were injection-site reactions, pyrexia, nasopharyngitis, influenza, cough, and nausea. USE IN SPECIFIC POPULATIONS Females of Reproductive Potential EMPAVELI may cause embryo-fetal harm when administered to pregnant women. Pregnancy testing is recommended for females of reproductive potential prior to treatment with EMPAVELI. Advise female patients of reproductive potential to use effective contraception during treatment with EMPAVELI and for 40 days after the last dose. Please see full Prescribing Information , including Boxed WARNING regarding serious infections caused by encapsulated bacteria, and Medication Guide . 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 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 results of the Company’s clinical trials for EMPAVELI, SYFOVRE, or any of its future products will warrant regulatory submissions to the FDA or equivalent foreign regulatory agencies and whether the Company will make regulatory submissions when anticipated; the rate and degree of market acceptance and clinical utility of EMPAVELI, SYFOVRE and any future products for which we receive marketing approval will impact our commercialization efforts; whether data from the Company’s clinical trials will be available when anticipated; whether results obtained in clinical trials will be indicative of results that will be generated in future clinical trials or in the real world setting; whether the Company’s products will generate the revenues projected by the Company, the Company will achieve profitability or maintain profitability, if achieved; whether the Company cash resources, together with its projected revenues, will fund its operations through profitability; 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 24, 2026 and 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 me dia@ apellis.com 617.420.4839 Investor Contact: Eva Stroynowski ir@apellis.com 617.938.6229 APELLIS PHARMACEUTICALS, INC. CONSOLIDATED BALANCE SHEETS (Amounts in thousands, except per share amounts) December 31, December 31, 2025 2024 Assets Current assets: Cash and cash equivalents $ 466,233 $ 411,290 Accounts receivable 366,221 264,926 Inventory 142,556 81,404 Prepaid and other current assets 38,303 30,012 Restricted cash 1,527 1,322 Total current assets 1,014,840 788,954 Non-current assets: Right-of-use assets 18,195 16,083 Property and equipment, net 1,708 2,952 Long-term inventory 34,959 75,713 Other assets 5,555 1,349 Total assets $ 1,075,257 $ 885,051 Liabilities and Stockholders' Equity Current liabilities: Accounts payable 56,798 38,572 Accrued expenses 166,049 140,184 Convertible senior notes 93,662 — Current portion of lease liabilities 7,087 6,753 Total current liabilities 323,596 185,509 Long-term liabilities: Long-term credit facility 361,664 359,489 Convertible senior notes — 93,341 Lease liabilities 11,947 10,201 Other liabilities 7,903 7,972 Total liabilities 705,110 656,512 Stockholders' equity: Preferred stock, $0.0001 par value; 10,000 shares authorized and zero shares issued and outstanding at December 31, 2025 and 2024 — — Common stock, $0.0001 par value; 200,000 shares authorized at December 31, 2025 and 2024; 126,621 and 124,495 shares issued and outstanding at December 31, 2025 and 2024, respectively 12 12 Additional paid-in capital 3,385,216 3,267,201 Accumulated other comprehensive loss (2,103 ) (3,308 ) Accumulated deficit (3,012,978 ) (3,035,366 ) Total stockholders' equity 370,147 228,539 Total liabilities and stockholders' equity $ 1,075,257 $ 885,051 APELLIS PHARMACEUTICALS, INC. CONSOLIDATED STATEMENTS OF OPERATIONS AND COMPREHENSIVE (LOSS)/INCOME (Amounts in thousands, except per share amounts) For the Three Months Ended December 31, For the Year Ended December 31, 2025 2024 2025 2024 Revenue: Product revenue, net $ 190,341 $ 191,172 $ 689,383 $ 709,954 Licensing and other revenue 9,572 21,356 314,399 71,413 Total revenue: 199,913 212,528 1,003,782 781,367 Operating expenses: Cost of sales 29,719 40,856 102,236 117,723 Research and development 74,233 76,354 295,854 327,570 Selling, general and administrative 147,103 121,482 550,265 501,053 Operating expenses: 251,055 238,692 948,355 946,346 Net operating (loss)/income (51,142 ) (26,164 ) 55,427 (164,979 ) Loss on extinguishment of development liability — — — (1,949 ) Interest income 3,502 3,396 13,143 12,773 Interest expense (10,847 ) (11,534 ) (44,327 ) (40,391 ) Other expense, net (151 ) (1,765 ) (133 ) (2,170 ) Net (loss)/income before taxes (58,638 ) (36,067 ) 24,110 (196,716 ) Income tax expense 313 286 1,722 1,162 Net (loss)/income $ (58,951 ) $ (36,353 ) $ 22,388 $ (197,878 ) Other comprehensive (loss)/income: Unrealized (loss)/gain on pension plans (30 ) 591 107 591 Foreign currency translation 327 (759 ) 1,098 (357 ) Total other comprehensive income/(loss) 297 (168 ) 1,205 234 Comprehensive (loss)/income, net of tax $ (58,654 ) $ (36,521 ) $ 23,593 $ (197,644 ) Net (loss)/income per share Basic earnings per share $ 0.47 $ (0.29 ) $ 0.18 $ (1.60 ) Diluted earnings per share $ 0.47 $ (0.29 ) $ 0.20 $ (1.60 ) Weighted-average shares used in calculating: Basic earnings per share 126,661 124,523 126,145 123,905 Diluted earnings per share 126,661 124,523 129,855 123,905 1 Based on Apellis estimate of approximately 5,000 U.S. patient population for C3G and primary IC-MPGN. 2 Lipid nanoparticle (LNP) technology licensed from Acuitas Therapeutics, Inc.