Kodiak Sciences Data at ARVO 2024 Highlight Depth of Early and Late-Phase Retina Pipeline Including Advancements With High Drug-Antibody-Ratio Therapeutics Built on Kodiak's Antibody Biopolymer Conjugate (ABC) Platform
Kodiak Sciences Data at ARVO 2024 Highlight Depth of Early and Late-Phase Retina Pipeline Including Advancements With High Drug-Antibody-Ratio Therapeutics Built on Kodiak's Antibody Biopolymer Conjugate (ABC) Platform
- Tarcocimab clinical and non-clinical data highlight strong 6-month efficacy profile in diabetic retinopathy patients and continued favorable safety profile.
- KSI-501 clinical and non-clinical data highlight multiple ascending dose safety, bioactivity and durability in treatment-naïve and treatment-experienced patients and next steps of Phase 3 development for KSI-501 and Phase 1b development for KSI-101.
- Novel small molecules and protein therapeutics highlight potential for targeted, high drug-antibody-ratio (DAR) conjugates built on Kodiak's ABC Platform.
- Tarcocimab的临床和非临床数据突显了糖尿病视网膜病变患者6个月的强劲疗效和持续良好的安全性。
- KSI-501 临床和非临床数据突显了治疗天真和有治疗经验的患者的多重递增剂量安全性、生物活性和耐久性,以及 KSI-501 的第三阶段开发和 KSI-101 1b 期开发的后续步骤。
- 新的小分子和蛋白质疗法突显了基于科迪亚克ABC平台的靶向高药物抗体比例(DAR)偶联物的潜力。
PALO ALTO, Calif., May 2, 2024 /PRNewswire/ -- Kodiak Sciences Inc. (Nasdaq: KOD), a biopharmaceutical company committed to researching, developing and commercializing transformative therapeutics to treat high prevalence retinal diseases, announced today that nine scientific presentations on its clinical and research pipeline programs will be made at the Association for Research in Vision and Ophthalmology (ARVO) 2024 Annual Meeting, being held from May 5 – 9 in Seattle, Washington.
加利福尼亚州帕洛阿尔托,2024年5月2日 /PRNewswire/ — 致力于研究、开发和商业化治疗高患病率视网膜疾病的变革性疗法的生物制药公司科迪亚克科学公司(纳斯达克股票代码:KOD)今天宣布,将在视觉与眼科学研究协会(ARVO)2024年年会上就其临床和研究管线项目进行九次科学演讲,将于5月5日至9日在华盛顿州西雅图举行。
"We present clinical and non-clinical data on our ABC Platform medicines tarcocimab and KSI-501. We also begin to disclose the progress and potential for our duet and triplet drug platform. Conjugates of different active pharmaceutical intermediates (API) such as proteins, peptides, macrocycles, oligonucleotides, and small molecules, all with high drug antibody ratio (DAR) and tailored release, can be designed and manufactured. We wrap these within the 15 years of science and development experience with our ABC Platform and its thousands of patient years of clinical safety data and our commercial scale manufacturing facility Ursus," said Dr. Victor Perlroth, Chief Executive Officer of Kodiak Sciences. "With many companies focused on engineering a better biologic or a better small molecule, we are instead extending our ABC Platform to make copolymer conjugates that power a next generation of targeted, high-DAR, multi-specific and multi-modality therapeutic candidates with relevance for retinal and systemic diseases."
“我们提供了有关我们的ABC平台药物tarcocimab和 KSI-501 的临床和非临床数据。我们还开始披露我们的二重奏和三联药物平台的进展和潜力。可以设计和制造不同活性药物中间体(API)的偶联物,例如蛋白质、肽、大环素、寡核苷酸和小分子,均具有较高的药物抗体比(DAR)和量身定制的释放。科迪亚克科学首席执行官维克多·珀洛斯博士说,我们将这些总结在15年的科学和开发经验中,使用我们的ABC平台及其数千年的患者年临床安全数据和我们的商业规模制造设施Ursus。“由于许多公司专注于设计更好的生物制剂或更好的小分子,我们改为扩展ABC平台,生产共聚物偶联物,为下一代与视网膜和全身性疾病相关的靶向、高达尔、多特异性和多模式的候选治疗提供动力。”
Presentations on tarcocimab tedromer (KSI-301):
关于tarcocimab tedromer(KSI-301)的演讲:
Title: Tarcocimab tedromer (KSI-301) 5mg: outcomes of the Phase 3 GLOW1 Study in patients with non-proliferative diabetic retinopathy.
Session Title: Diabetic retinopathy I
Session Date and Time: May 6, 2024; 8:30 – 10:15 AM PT
Presentation Type: Poster Session
Poster Number: 221 – B0116
标题: Tarcocimab tedromer (KSI-301) 5mg:针对非增殖性糖尿病视网膜病变患者的三期 GLOW1 研究结果。
会议标题:糖尿病视网膜病变 I
会议日期和时间:2024 年 5 月 6 日;太平洋时间上午 8:30 — 10:15
演示类型:海报会议
海报编号:221 — B0116
Approximately eight million people in the U.S. live with diabetic retinopathy (DR), which is the leading cause of vision loss in the working-age population. The adoption of approved anti-VEGF therapies for DR patients is constrained by their high treatment burden. Kodiak's GLOW1 study with tarcocimab showed for the first time that a therapeutic agent dosed in all patients on an every 6-month interval can successfully treat and prevent disease worsening in DR patients. Tarcocimab offers the hope of an achievable prevention and treatment strategy in real-world clinical practice for DR patients at risk of vision loss. Currently, the Phase 3 GLOW2 study is enrolling patients with DR, with the goal to enable tarcocimab's marketing authorization application.
美国约有800万人患有糖尿病视网膜病变(DR),这是工作年龄人口视力丧失的主要原因。DR 患者采用经批准的抗血管内皮生长因子疗法受到高额治疗负担的限制。科迪亚克对tarcocimab进行的 GLOW1 研究首次表明,每隔6个月给所有患者服用一次治疗药物可以成功治疗和预防DR患者的疾病恶化。Tarcocimab为面临视力丧失风险的DR患者提供了现实临床实践中可实现的预防和治疗策略的希望。目前,GLOW2 的三期研究正在招收DR患者,目标是启用tarcocimab的上市许可申请。
Title: Metabolic control in patients with non-proliferative diabetic retinopathy (NPDR) treated with anti-VEGF active injections or sham injections. Prespecified results from the Phase 3 GLOW Study in patients treated with tarcocimab tedromer.
Session Title: Diabetic retinopathy II
Session Date and Time: May 7, 2024; 8:30 – 10:15 AM PT
Presentation Type: Poster Session
Poster Number: 323 – B0508
标题: 接受抗血管内皮生长因子活性注射或假注射治疗的非增殖性糖尿病视网膜病变(NPDR)患者的代谢控制。针对使用tarcocimab tedromer治疗的患者的3期GLOW研究的预设结果。
会议标题:糖尿病视网膜病变 II
会议日期和时间:2024 年 5 月 7 日;太平洋时间上午 8:30 — 10:15
演示类型:海报会议
海报编号:323 — B0508
The prespecified analysis of the GLOW1 study demonstrated that both the tarcocimab treatment arm and sham arm had negligible change in systemic metabolic control as measured by HbA1c levels, and both arms showed similar distribution of change in HbA1c from baseline to primary endpoint at Week 48. These results suggest that subjects in the tarcocimab arm achieved superiority in ≥2-step improvement in DRSS over sham injections irrespective of baseline and systemic metabolic control, as evidenced by HbA1c levels, and any potential presumed knowledge by the patient about treatment assignment due to the use of sham as a comparator did not systematically influence their glycemic control.
GLOW1 研究的预先设定分析表明,根据HbA1c水平测量,tarcocimab治疗组和假组的全身代谢控制变化可以忽略不计,并且两个组在第48周显示出从基线到主要终点的HbA1c变化分布相似。这些结果表明,与假注射相比,无论基线和全身代谢控制如何,tarcocimab组的受试者在DRSS改善≥2步方面都取得了优势,HbA1c水平就证明了这一点,而且由于使用假药作为比较物,患者对治疗分配的任何潜在了解都不会系统地影响其血糖控制。
Title: An embryo-fetal development study of tarcocimab after intravenous injection in rabbits
Session Title: Retina/RPE: New drugs, mechanisms of action, and toxicity
Session Date and Time: May 8, 2024; 2:15 – 4:00 PM PT
Presentation Type: Poster Session
Poster Number: 5100 – A0357
标题: 兔子静脉注射后tarcocimab的胚胎-胎儿发育研究
会议标题:视网膜/RPE:新药、作用机制和毒性
会议日期和时间:2024 年 5 月 8 日;太平洋时间下午 2:15 — 4:00
演示类型:海报会议
海报编号:5100 — A0357
The non-clinical study demonstrated that maternal administration of tarcocimab to New Zealand White female rabbits by intravenous injection at the highest tested dose of 5 mg/kg during the organogenesis period of pregnancy was well tolerated. There were no tarcocimab related mortality or abortions for any dosage regimen, and no effects on embryo-fetal viability or fetal body weights, as well as no malformations or variations at external, visceral, or skeletal examination. These results continue to highlight the favorable safety profile of tarcocimab and of Kodiak's ABC platform and compare favorably to published results with marketed anti-VEGF agents which have demonstrated embryo-fetal development effects in animal studies.
非临床研究表明,孕产妇在妊娠器官发生期以最高测试剂量5 mg/kg静脉注射方式向新西兰白兔注射tarcocimab的耐受性良好。任何剂量方案均未出现与tarcocimab相关的死亡率或流产情况,对胚胎-胎儿活力或胎儿体重没有影响,在外部、内脏或骨骼检查中也没有畸形或变异。这些结果继续凸显了tarcocimab和Kodiak的ABC平台的良好安全性,与已发布的抗VEGF药物相比,这些结果与已发布的在动物研究中显示出胚胎-胎儿发育作用的抗血管内皮生长因子药物的结果相比还是不错的。
Presentations on KSI-501:
关于 KSI-501 的演讲:
Title: Ocular and systemic toxicity study of KSI-501 demonstrates tolerability after intravitreal and intravenous administration in cynomolgus monkeys
Session Title: Retina/RPE: New drugs, mechanisms of action, and toxicity
Session Date and Time: May 8, 2024; 2:15 – 4:00 PM PT
Presentation Type: Poster Session
Poster Number: 5094 – A0351
标题: KSI-501 的眼部和全身毒性研究表明 cynomolgus 猴在玻璃体内和静脉注射后的耐受性
会议标题:视网膜/RPE:新药、作用机制和毒性
会议日期和时间:2024 年 5 月 8 日;太平洋时间下午 2:15 — 4:00
演示类型:海报会议
海报编号:5094 — A0351
The non-clinical study demonstrated that repeated monthly bilateral intravitreal administration of up to 5.25 mg/eye/dose (maximum feasible dose) or intravenous dosing of up to 5 mg/kg/dose (maximum tested dose) of KSI-501 in cynomolgus monkeys was safe and well tolerated. Due to the mild severity of findings and the lack of impact on the health and well‐being of animals administered 5 mg/kg IV or 5.25 mg/eye IVT, these doses were considered the No Observed Adverse Effect Levels (NOAELs) for systemic and ocular administration, respectively. These results provide a clear margin of safety for repeat dosing and information for adequate safety monitoring to support further clinical investigations with KSI-501 (bioconjugate) and KSI-101 (bispecific protein) which are ongoing. These results are also consistent with non-clinical data generated with tarcocimab, another ABC Platform derived therapeutic candidate, and suggest the continued safety profile of the ABC Platform.
非临床研究表明,在食腐猴中,每月重复双侧玻璃体内注射高达 5.25 mg/眼/剂量(最大可行剂量)或静脉注射高达 5 mg/kg/剂量(最大测试剂量)的 KSI-501 是安全且耐受性良好。由于发现的严重程度较轻且对给药5 mg/kg IVT或5.25 mg/眼静脉注射的动物的健康和福祉没有影响,这些剂量分别被视为全身和眼部给药的无观测不良反应水平(NOAEL)。这些结果为重复给药提供了明确的安全余地,也为充分的安全性监测提供了信息,以支持正在进行的 KSI-501(生物偶联物)和 KSI-101(双特异蛋白)的进一步临床研究。这些结果也与另一种由ABC平台衍生的候选治疗药物tarcocimab生成的非临床数据一致,表明ABC平台仍具有持续的安全性。
Title: KSI-501: a bispecific fusion protein antibody inhibiting both interleukin-6 and vascular endothelial growth factor. First-in-human trial results of multiple ascending doses in patients with diabetic macular edema
Session Title: Diabetic macular edema
Session Date and Time: May 9, 2024; 11:45 AM – 1:30 PM PT
Presentation Type: Poster Session
Poster Number: 530 – B0162
标题: KSI-501:一种抑制白介素-6 和血管内皮生长因子的双特异融合蛋白抗体。糖尿病黄斑水肿患者多次递增剂量的首次人体试验结果
会议标题:糖尿病性黄斑水肿
会议日期和时间:2024 年 5 月 9 日;太平洋时间上午 11:45 — 下午 1:30
演示类型:海报会议
海报编号:530 — B0162
This first-in-human study was Part 1 of a Phase 1 multiple ascending dose study of KSI-501 in both treatment naïve and treatment experienced patients with DME. Part 1 demonstrated that repeated monthly dosing of KSI-501 was safe and well tolerated and achieved meaningful and sustained improvement in BCVA and OCT CST. These results support further clinical development of both (1) KSI-501, a bispecific antibody biopolymer conjugate, for high prevalence retinal diseases to address the leading unmet needs of durability and targeting multiple disease biologies; and (2) KSI-101, a bispecific protein with high potency and high formulation strength for inflammatory diseases of the eye.
这项首次人体研究是针对 KSI-501 进行的 1 期多次递增剂量研究的第 1 部分,该研究既适用于未接受治疗的患者,也适用于有治疗经验的 DME 患者。第 1 部分表明,每月重复给药 KSI-501 是安全的,耐受性良好,并且在 BCVA 和 OCT CST 方面取得了有意义的持续改善。这些结果支持了 (1) KSI-501(一种用于高患病率视网膜疾病的双特异性抗体生物聚合物偶联物)的进一步临床开发,以满足尚未满足的耐久性需求并靶向多种疾病生物学;以及 (2) KSI-101,一种针对眼部炎症性疾病的高效和高配方强度的双特异蛋白。
Presentations on Research Pipeline:
关于研究管道的演讲:
Title: Identification and characterization of novel NLRP3 inflammasome Inhibitors for the potential treatment of retinal disease
Session Title: Treatment strategies for inherited retinal disease
Presentation Date and Time: May 6, 2024; 3:00 – 4:45 PM PT
Presentation Type: Poster Session
Poster Number: 2208 – A0062
标题: 用于潜在治疗视网膜疾病的新型 NLRP3 炎症体抑制剂的鉴定和表征
会议标题:遗传性视网膜疾病的治疗策略
演讲日期和时间:2024 年 5 月 6 日;太平洋时间下午 3:00 — 4:45
演示类型:海报会议
海报编号:2208 — A0062
We disclose for the first time the discovery and characterization of novel NLRP3 pathway inhibitors that are potent and act on all levels of the NLRP3 pathway without non-specific anti-inflammatory action. This work highlights Kodiak's small molecule discovery capabilities, which play an important part in our development of duet and triplet therapeutic candidates designed to provide targeted high drug-antibody-ratio (DAR) and sustained therapeutic benefit for both ophthalmic and systemic diseases.
我们首次披露了新型 NLRP3 途径抑制剂的发现和表征,这些抑制剂有效且作用于所有 NLRP3 途径水平,没有非特异性抗炎作用。这项工作突显了科迪亚克的小分子发现能力,这在我们开发二联和三联候选疗法中发挥了重要作用,旨在为眼科和全身性疾病提供靶向高药物抗体比(DAR)和持续的治疗益处。
Title: Development of anti-inflammatory bispecific trap-antibodies
Session Title: Diabetic retinopathy, anti-inflammatory agents, antibiotics and antivirals
Session Date and Time: May 8, 2024; 10:30 AM - 12:15 PM PT
Presentation Type: Poster Session
Poster Number: 4599 – A0328
标题:抗炎双特异性陷阱抗体的开发
会议标题:糖尿病视网膜病变、抗炎药、抗生素和抗病毒药物
会议日期和时间:2024 年 5 月 8 日;太平洋时间上午 10:30-下午 12:15
演示类型:海报会议
海报编号:4599 — A0328
We present a portfolio of novel bispecific anti-inflammatory biologics targeting proinflammatory cytokines. This work highlights the expansion of our modular trap-antibody platform and presents a group of promising therapeutic candidates with the potential to mitigate the complex effects of ocular inflammation in a controlled, multi-specific manner.
我们提供了一系列针对促炎细胞因子的新型双特异性抗炎生物制剂。这项工作突显了我们模块化陷阱抗体平台的扩展,并提出了一组有前景的候选疗法,这些候选治疗有可能以可控的多特异性方式减轻眼部炎症的复杂影响。
Title: Internalization of antibody biopolymer conjugate via receptor-mediated mechanism
Session Title: AMD New drugs, delivery systems and mechanisms of action II
Session Date/Times: May 9, 2024; 8:00 - 9:45 AM PT
Presentation Type: Poster Session
Poster Number: 6120 – B1019
标题:通过受体介导机制内化抗体生物聚合物偶联物
会议标题:AMD 新药、递送系统和作用机制 II
会议日期/时间:2024 年 5 月 9 日;太平洋时间上午 8:00-9:45
演示类型:海报会议
海报编号:6120 — B1019
We demonstrate that antibody biopolymer conjugates built on our ABC platform can be internalized upon binding to cell-surface receptors, a key step enabling the use of our ABC platform for cell-specific drug deliveries. The ABC platform, combined with diverse drug modalities such as oligonucleotides, small molecules and peptides including macrocycles, can overcome current limits on drug-antibody-ratio (DAR) and provide a broad range of options for multi-specific bioactive loading and targeted delivery.
我们证明,建立在我们ABC平台上的抗体生物聚合物偶联物可以在与细胞表面受体结合后内化,这是使我们的ABC平台能够用于细胞特异性药物递送的关键步骤。ABC平台与寡核苷酸、小分子和包括大环在内的肽等多种药物模式相结合,可以克服目前药物抗体比例(DAR)的限制,为多特异性生物活性载荷和靶向递送提供广泛的选择。
Title: Development of enhanced complement regulators for the treatment of geographic atrophy
Session Title: AMD New drugs, delivery systems and mechanisms of action II
Session Date/Times: May 9, 2024; 8:00 – 9:45 AM PT
Presentation Type: Poster Session
Posterboard Number: 6119 – B1018
标题:开发用于治疗地理萎缩的增强补体调节剂
会议标题:AMD 新药、递送系统和作用机制 II
会议日期/时间:2024 年 5 月 9 日;太平洋时间上午 8:00 — 9:45
演示类型:海报会议
海报板编号:6119 — B1018
Geographic atrophy (GA), the advanced form of dry age-related macular degeneration, affects approximately one million patients in the U.S. and is characterized by atrophic lesions in the retina that progressively expand to the central macular and fovea, leading to irreversible vision loss. Currently there are two approved therapies for GA, both are anti-complement therapies that offer modest therapeutic benefit and require monthly or every other month intravitreal injections. Here we present a promising therapeutic strategy to treat GA and potentially wet AMD by combining complement regulators with an anti-VEGF Fab to achieve potent, concurrent inhibition of complement pathway activation and VEGF pathway signaling.
地理萎缩(GA)是与年龄相关的干性黄斑变性的晚期形式,在美国影响约一百万名患者,其特征是视网膜萎缩性病变逐渐扩张到中央黄斑和中央凹处,导致不可逆转的视力丧失。目前有两种获批准的胃肠炎疗法,均为抗补体疗法,治疗效果适中,需要每月或每隔一个月进行一次玻璃体内注射。在这里,我们提出了一种前景看好的治疗策略,通过将补体调节剂与抗血管内皮生长因子Fab相结合,实现对补体通路激活和血管内皮生长因子通路信号传导的强效、同时抑制。
About Kodiak Sciences Inc.
关于 Kodiak Sciences Inc.
Kodiak Sciences (Nasdaq: KOD) is a biopharmaceutical company committed to researching, developing, and commercializing transformative therapeutics to treat a broad spectrum of retinal diseases. We are focused on bringing new science to the design and manufacture of next generation retinal medicines to prevent and treat the leading causes of blindness globally. Our ABC Platform uses molecular engineering to merge the fields of protein-based and chemistry-based therapies and has been at the core of Kodiak's discovery engine. We are developing a portfolio of three clinical programs, two of which are late-stage today and derived from our ABC Platform and one which is platform-independent and which we believe can progress rapidly into pivotal studies.
柯迪亚克科学(纳斯达克股票代码:KOD)是一家生物制药公司,致力于研究、开发和商业化治疗各种视网膜疾病的变革性疗法。我们致力于将新科学引入下一代视网膜药物的设计和制造,以预防和治疗全球主要的失明原因。我们的ABC平台使用分子工程将基于蛋白质和基于化学的疗法领域融为一体,一直是科迪亚克发现引擎的核心。我们正在开发由三个临床项目组成的产品组合,其中两个项目目前处于后期阶段,源自我们的ABC平台,另一个独立于平台,我们认为可以迅速进入关键研究。
Kodiak's lead investigational medicine, tarcocimab, is a novel anti-VEGF antibody biopolymer conjugate under development for the treatment of high prevalence retinal vascular diseases including diabetic retinopathy, the leading cause of blindness in working-age patients in the developed world, and wet age-related macular degeneration, the leading cause of blindness in elderly patients in the developed world.
柯迪亚克的主要研究药物tarcocimab是一种正在开发的新型抗血管内皮生长因子抗体生物聚合物偶联物,用于治疗高患病率的视网膜血管疾病,包括糖尿病视网膜病变(发达国家工作年龄患者失明的主要原因)和湿性年龄相关性黄斑变性,后者是发达国家老年患者失明的主要原因。
KSI-501 is our second investigational medicine, a first-in-class anti-IL-6, VEGF-trap bispecific antibody biopolymer conjugate designed to inhibit both IL-6 mediated inflammation and VEGF-mediated angiogenesis and vascular permeability. KSI-501 is being developed for the treatment of high prevalence retinal vascular diseases to address the unmet needs of targeting multiple biologies and extended durability.
KSI-501 是我们的第二种在研药物,是同类首创的抗 IL-6、VEGF-Trap 双特异性抗体生物聚合物偶联物,旨在抑制 IL-6 介导的炎症和血管内皮生长因子介导的血管生成和血管通透性。KSI-501 正在开发用于治疗高患病率的视网膜血管疾病,以满足靶向多种生物学和延长耐久性的未满足的需求。
Additionally, Kodiak is developing a third product candidate, KSI-101, a novel anti-IL-6, VEGF-trap bispecific protein, the unconjugated protein portion of KSI-501. Kodiak intends to develop KSI-101 for the treatment of retinal inflammatory diseases, as currently there are no available intravitreal biologic therapies addressing the spectrum of inflammatory conditions of the retina.
此外,科迪亚克正在开发第三种候选产品,即 KSI-101,这是一种新型的抗IL-6、VEGF-Trap双特异蛋白,是 KSI-501 的非偶联蛋白部分。科迪亚克打算开发用于治疗视网膜炎性疾病的 KSI-101,因为目前没有针对视网膜炎症性疾病的玻璃体内生物疗法。
Kodiak has expanded its early research pipeline of duet and triplet inhibitors that embed small molecules and other bioactive molecules in the biopolymer backbone to provide a high drug-antibody ratio ("DAR"). The diverse active pharmaceutical intermediates (API) are designed to be released over time to achieve sustained modulation of targeted biological pathways. The unique combination of high DAR and tailored therapeutic benefit offers potential for broad application to multifactorial ophthalmic and systemic diseases.
柯迪亚克扩大了其早期的二联和三联抑制剂研究渠道,这些抑制剂将小分子和其他生物活性分子嵌入生物聚合物骨干中,以提供较高的药物抗体比(“DAR”)。各种活性药物中间体(API)旨在随着时间的推移而释放,以实现靶向生物通路的持续调节。高 DAR 和量身定制的治疗益处的独特组合为广泛应用于多因素眼科和全身性疾病提供了潜力。
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Kodiak, Kodiak Sciences, ABC, ABC Platform and the Kodiak logo are registered trademarks or trademarks of Kodiak Sciences Inc. in various global jurisdictions.
柯迪亚克、科迪亚克科学、ABC、ABC平台和科迪亚克徽标是科迪亚克科学公司在全球各个司法管辖区的注册商标或商标。
Forward-Looking Statements
前瞻性陈述
This release contains "forward-looking statements" within the meaning of Section 27A of the Securities Act of 1933, Section 21E of the Securities Exchange Act of 1934 and the Private Securities Litigation Reform Act of 1995. These forward-looking statements are not based on historical fact and include statements regarding: the continued favorable safety profile of tarcocimab; next steps of Phase 3 development for KSI-501 and Phase 1b development for KSI-101; the potential for targeted, high drug-antibody-ratio conjugates built on Kodiak's ABC Platform; the potential for the duet and triplet drug platform; promising therapeutic candidates with the potential to mitigate the complex effects of ocular inflammation; and a promising therapeutic strategy to treat GA and potentially wet AMD by combining complement regulators with an anti-VEGF Fab to achieve potent, concurrent inhibition of complement pathway activation and VEGF pathway signaling. Forward-looking statements generally include statements that are predictive in nature and depend upon or refer to future events or conditions, and include words such as "may," "will," "should," "would," "could," "expect," "plan," "believe," "intend," "pursue," and other similar expressions among others. Any forward-looking statements are based on management's current expectations of future events and are subject to a risks and uncertainties that could cause actual results to differ materially and adversely from those in or implied by such forward-looking statements. These risks and uncertainties include, but are not limited to: cessation or delay of any clinical studies and/or development of KSI-501 may occur; the risk that KSI-501 may not inhibit VEGF and IL-6, provide extended durability or have an impact on the treatment of patients as expected; adverse economic conditions may significantly impact our business and operations, including our clinical trial sites, and those of our manufacturers, contract research organizations or others with whom we conduct business; as well as the other risks identified in our filings with the Securities and Exchange Commission (SEC). For a discussion of other risks and uncertainties, and other important factors, any of which could cause our actual results to differ from those contained in the forward-looking statements, see the section entitled "Risk Factors" in our most recent Form 10-K, as well as discussions of potential risks, uncertainties, and other important factors in our subsequent filings with the SEC. These forward-looking statements speak only as of the date hereof and Kodiak undertakes no obligation to update forward-looking statements, and readers are cautioned not to place undue reliance on such forward-looking statements.
本新闻稿包含1933年《证券法》第27A条、1934年《证券交易法》第21E条和1995年《私人证券诉讼改革法》所指的 “前瞻性陈述”。这些前瞻性陈述并非基于历史事实,包括以下方面的陈述:tarcocimab持续保持良好的安全性;KSI-501 的第三阶段开发和 KSI-101 的1b期开发的后续步骤;基于Kodiak的ABC平台的靶向高药物抗体比偶联物的潜力;二联和三联药物平台的潜力;有望缓解眼部炎症复杂影响的候选疗法;以及治疗GA和潜在湿性AMD的有前途的治疗策略通过将补体调节剂与抗血管内皮生长因子Fab相结合,实现对补体通路激活和血管内皮生长因子通路信号的有效抑制。前瞻性陈述通常包括本质上是预测性的、取决于或提及未来事件或条件的陈述,并包括 “可能”、“将”、“应该”、“将”、“可以”、“期望”、“计划”、“相信”、“打算”、“追求” 等词语以及其他类似表述。任何前瞻性陈述均基于管理层当前对未来事件的预期,并存在风险和不确定性,可能导致实际业绩与此类前瞻性陈述中或暗示的业绩存在重大不利差异。这些风险和不确定性包括但不限于:可能会停止或延迟任何 KSI-501 的临床研究和/或开发;KSI-501 可能无法按预期抑制 VEGF 和 IL-6、延长耐久性或对患者治疗产生影响的风险;不利的经济状况可能会严重影响我们的业务和运营,包括我们的临床试验基地,以及我们的制造商、合同研究机构或其他与我们有业务往来的机构的业务和运营;以及其他风险在我们的文件中确定了证券交易委员会(SEC)。有关其他风险和不确定性以及其他重要因素的讨论,其中任何一个都可能导致我们的实际业绩与前瞻性陈述中包含的有所不同,请参阅我们最新的10-K表格中标题为 “风险因素” 的部分,以及我们随后向美国证券交易委员会提交的文件中对潜在风险、不确定性和其他重要因素的讨论。这些前瞻性陈述仅代表截至本文发布之日,科迪亚克没有义务更新前瞻性陈述,并提醒读者不要过分依赖此类前瞻性陈述。
SOURCE Kodiak Sciences Inc.
来源 Kodiak Sciences Inc.
译文内容由第三方软件翻译。