An Open-label, Dose-finding, Phase 1 Study to Assess the Safety, Tolerability, Efficacy, and Pharmacokinetic Profile, and to Explore the Pharmacodynamic Profile of DM5167 in Patients With Advanced Solid Tumors

DM5167 is a second-generation of PARP inhibitor that selectively targets the PARP-1 enzyme. This results in less haematological toxicity and a high level of safety.
The aim of the study is to assess the safety and tolerability of DM5167 in patients with advanced solid tumors not respond to other treatments.

开始日期2024-10-24

申办/合作机构

DigmBio. Inc.

100 项与 DM-5167 相关的临床结果

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100 项与 DM-5167 相关的转化医学

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100 项与 DM-5167 相关的专利（医药）

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项与 DM-5167 相关的文献（医药）

2025-10-01·PHARMACEUTICAL RESEARCH

Preclinical Pharmacokinetics of DM5167, a Novel Selective PARP1 Inhibitor

Article

作者: Kim, Jeongmin ; Koo, Tae-Sung ; Lee, Yoon Ha ; Kim, Eunhee ; Ahn, Sunjoo ; Jung, Myung Eun ; Jang, Ki-Hong ; Lee, Seung-Won ; Kim, Jin Woo ; Choi, Hae-In

PURPOSE:

First-generation PARP inhibitors, including olaparib, niraparib, and rucaparib, act as non-selective inhibitors of the PARP family, and are associated with hematological side effects. DM5167 is a selective PARP1 inhibitor, and its selectivity could reduce its side effects; however, its pharmacokinetic properties, tissue distribution, and excretion profiles remain unclear. This study aimed to characterize the pharmacokinetic properties of DM5167 to support the prediction of its pharmacokinetics in humans.

METHOD:

The pharmacokinetics of DM5167 were assessed in mice, rats, and dogs over a dose range of 3-30 mg/kg. Parameters included oral bioavailability, tissue distribution, plasma protein binding, enzyme inhibition, half-life in microsomes and hepatocytes across species, and in vitro-in vivo extrapolation to predict human clearance. Metabolite profiling was performed to identify whether any the human-specific metabolites.

RESULTS:

DM5167 demonstrated linear pharmacokinetics across the studied dose ranges in mice and rats. Oral bioavailability was moderate to high, and tissue distribution showed broad organ coverage. DM5167 exhibited high plasma protein binding across species, including humans, and did not inhibit cytochrome P450 enzymes. The half-life of the compound varied among species, with a notably longer half-life in humans. In vitro-in vivo extrapolation results indicated stable predicted clearance values in humans, and metabolite profiling did not reveal any human-specific metabolites.

CONCLUSION:

DM5167 exhibited a favorable pharmacokinetic profile in vivo and in vitro. These findings support its potential for further clinical development and provide valuable insights to guide future preclinical and clinical studies of DM5167 and other PARP inhibitors.

项与 DM-5167 相关的新闻（医药）

2024-05-16

·Pharmaceutical Technology

Uniquity Bio launches with $300m and an MSD Phase II asset to boot

Uniquity is eyeing pipeline growth alongside advancing solrikitug in COPD and asthma. Credit: Shutterstock/ peterschreiber.media. Private investment firm Blackstone Life Sciences has pulled back the covers on the latest pharma company to hit the immunology and inflammation arena. Based in Pennsylvania, US, Uniquity Bio has launched with $300m in capital from Blackstone. Uniquity Bio’s most valuable asset is arguably a monoclonal antibody in-licensed from MSD, solrikitug. The drug targets thymic stromal lymphopoietin (TSLP) and has recently been cleared for use in clinical trials by the US Food and Drug Administration (FDA). Uniquity said it will launch Phase II trials in chronic obstructive pulmonary disease (COPD) and asthma. The market size for COPD in the US was estimated to be about $18.6bn in 2023 while the size of the asthma market in the country was approximately $7.2bn in the same year, according to GlobalData’s Pharma Intelligence Centre. See Also: DM-5167 by Dime Bio for Solid Tumor: Likelihood of Approval BBI-825 by Boundless Bio for Metastatic Colorectal Cancer: Likelihood of Approval GlobalData is the parent company of Pharmaceutical Technology. While the upcoming trials will focus on these two diseases, Uniquity suggested the antibody could have applications in a wide range of immunology and inflammation programmes. Uniquity CEO Brian Lortie said solrikitug “has the potential to be a life-changing medication for a significant number of patients who currently have very limited treatment options”, and that the company is “excited to move into the next phase of development.” Uniquity gave no further details on the timings of the upcoming Phase II trials. But Blackstone Life Sciences’ global head Nicholas Galakatos reckons that the advancement of solrikitug will accompany an expanding pipeline for startups. Galakatos said: “We are proud to partner with Uniquity’s team of veteran industry leaders as they advance solrikitug and expand their immunology and inflammation pipeline with additional programs in the near future.” Immunology and inflammation are two of the hot areas to be a part of in the current pharma landscape. In February, inflammatory disease specialist Aiolos Bio was acquired by GSK in a $1.4bn deal . Aiolos had launched not long before in October 2023 with $200m and a monoclonal antibody that also targeted TSLP. Also in the space is Mirador Therapeutics which launched in late March 2024. Ushered in by the former head of MSD-bought Prometheus, the company secured $400m in Series A financing .

临床2期并购免疫疗法临床申请临床1期

2024-05-15

·Pharmaceutical Technology

Nabla Bio secures $26m in Series A funding round

Nabla Bio co-founders Surge Biswas and Frances Anastassacos at the company’s labs in Cambridge, Massachusetts in the US. Credit: Business Wire / Nabla Bio. US pharmaceutical company Nabla Bio has secured $26m for generative protein design in a Series A financing round led by Radical Ventures. The round included full participation from all existing investors. Nabla has also entered strategic partnerships with Bristol Myers Squibb , AstraZeneca and Takeda. These partnerships could exceed $550m in upfront and milestone payments, in addition to royalty payments. Nabla Bio specialises in the integration of AI and wet-lab technologies for atomically precise drug design and the high-throughput evaluation of drug function. See Also: CinDome Pharma secures $40m to advance gastroparesis treatment DM-5167 by Dime Bio for Solid Tumor: Likelihood of Approval The company’s initial focus is on antibodies that target multipass membrane proteins such as G protein-coupled receptors, ion channels and transporters. These proteins are challenging to treat because of their membrane-integrated nature, reduced extracellular availability and structural similarity across targets. Multipass membrane proteins, which constitute two-thirds of all cell surface proteins, play a central role in controlling cell behaviour. They have long been considered the “holy grail” of protein drug development. Nabla’s generative protein design platform is now making hundreds of these previously inaccessible targets available by enabling the accurate designing of conformation and target-selective antibody binders. To enhance the patient impact of its platform, Nabla is collaborating with other pharmaceutical companies known for successful drug development. These partnerships aim to enhance their pipelines with high-quality drug candidates targeting some of the most challenging and high-impact proteins. They are also aimed at generating insights into disease biology and platform development. Since its launch in December 2021 with support from Khosla Ventures and Zetta Venture Partners, Nabla Bio has secured $37m in funding. Nabla co-founder and CEO Surge Biswas stated: “We are unlocking new opportunities to build highly selective drugs against validated, but hard-to-drug targets with a degree of structural precision not previously possible. “We are excited to welcome Radical Ventures as our newest investor and to announce collaborations with three of the world’s largest pharmaceutical companies to help us bring our work closer to patients.”

蛋白降解靶向嵌合体

2024-03-26

·美通社

保诺-桑迪亚助力韩国选择性 PARP1 抑制剂项目IND 获MFDS 许可

IND一站式赋能上海 2024年3月26日 /美通社/ -- 近日，保诺-桑迪亚合作伙伴韩国生物技术公司DigmBio宣布，其自主研发的用于治疗三阴性乳腺癌的新型选择性 PARP1 抑制剂已获得韩国食品药品管理局（MFDS）新药临床试验(IND) 批准。保诺-桑迪亚对DigmBio这一重大里程碑事件表示热烈祝贺。 DigmBio 成立于 2020 年 4 月，是一家领先的生物技术公司，致力于针对肿瘤、神经退行性疾病及纤维化疾病等未满足的临床领域开发创新药物，其管理团队在新药开发和全球临床试验拥有数十年的丰富经验。该公司的主导候选药物DM5167是第二代选择性 PARP1 抑制剂。临床前研究结果表明，DM5167作为一种新型的选择性 PARP1 抑制剂，具有更高的体内安全性，同时在酶测定中显示高选择性，且DNA捕获效能更高。特别是DM5167具有优异的脑通透性，可应用于脑转移和脑癌。"我们很高兴获得食品药品安全部的正式批准，无需对临床药物进行任何特殊补充"，Daim Bio 首席执行官 Kim Jung -min 表示。"由于在各种动物模型中已经证明了其优异的抗肿瘤功效，因此与现有药物相比，预计在针对实际患者的 1 期临床试验中将具有积极的安全性和有效性。" 作为赋能全球新药研发的CRDMO，在此次合作中，保诺-桑迪亚与DigmBio紧密联系，进行了深度合作。保诺-桑迪亚整合CMC部门为DigmBio提供了一站式的IND-Enabling服务，包括工艺、制剂、分析、GMP生产以及IND 申报文件撰写等全流程服务，部门之间的高效沟通为快速获批韩国MFDS创造了良好的条件。DigmBio首席战略官 Jung-Ho Kim 博士称赞到："非常感谢保诺-桑迪亚团队在DM5176项目中所做的工作，反应高效及时，加快了我们项目的获批速度"。 "作为DigmBio全球合作伙伴，我们由衷地祝贺DM5167这一项目获批韩国IND。" 保诺-桑迪亚全球CMC亚太区总裁李建昌博士说到，"保诺-桑迪亚始终致力于为全球生物医药伙伴提供一站式新药研发解决方案，并不断提升服务质量、完善平台能力，助力合作伙伴不断推进新药好药的研发里程碑，最终为患者增加更多的治疗选择。我们很荣幸能与DigmBio这样的创新型公司合作，也期待DigmBio带来更多具有差异性、独具优势的药物，早日造福患者。" 保诺-桑迪亚一直致力于为全球生物医药公司提供全方位、一站式新药研发服务平台及专业的技术支持。综合CMC部门可以为客户提供从IND到NDA阶段药学部分研发及申报资料撰写的整合化服务，包括原料药、制剂、分析、药代动力学（DMPK）、药理学、毒理学，以及项目管理和IND申报支持，同时完善的EHS政策和IP保护制度也为双方的合作奠定了信任的基础。团队成员均拥有丰富的新药研发及注册申报经验，熟悉中、美、欧盟、日、韩以及澳洲等多国法规政策，搭配专业的项目管理体系和完善的质量管理系统，保诺-桑迪亚CMC团队已帮助全球客户成功完成了100+的IND项目，包括30+中美双报项目。放眼未来，保诺-桑迪亚将持续以质取胜，用心对待每一个项目，与客户携手共进、协同创新，实现共赢，共迎发展！关于保诺-桑迪亚保诺-桑迪亚，安宏资本旗下投资企业之一，拥有超过28年的历史，是一家值得信赖的全球化合同研究、开发和生产公司（CRDMO）。公司总部位于加州尔湾，在中国和美国6个城市设有7个研发生产中心，在全球拥有将近3000名员工。我们为生物技术和制药企业提供从早期靶点确证到商业化生产的全面整合服务，尤其擅长大小分子发现、开发、放大和生产服务。保诺-桑迪亚独特的技术平台和整合服务可加速新药研发进程、降低开发风险，从而创造更高的价值。我们遵循全球高标准的合规和运营准则，科学驱动、以客户为导向、多元化和以人为本的企业文化。保诺-桑迪亚专注于纯粹的CRDMO服务，在全球化质量标准体系下运营，提供先进、全面、快速和灵活的定制服务，以满足生物技术和制药企业的专属需求，加快新药开发进程。如需了解更多信息，请访问 www.bioduro-sundia.com。关于DigmBio DigmBio, founded in April 2020, is a pioneering biotech company headquartered in Korea, dedicated to developing innovative pharmaceuticals targeting critical unmet medical needs. Our management team has decades of collective experience in new drug development and global clinical trials, particularly in small-molecule therapeutics. DigmBio's primary focus lies in identifying and advancing first-in-class therapeutics with the potential to address unmet medical needs, with a strategic emphasis on leveraging early licensing-out opportunities during the preclinical or phase 1 stages. Their pipeline encompasses therapies for oncology, Alzheimer's disease, and other CNS diseases including Parkinson's disease, along with a KRAS-targeted molecular glue.

临床申请临床1期

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研发状态

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
晚期乳腺癌	临床1期	韩国	DigmBio. Inc.	2024-10-24
晚期恶性实体瘤	临床1期	韩国	DigmBio. Inc.	2024-10-24
三阴性乳腺癌	临床申请批准	韩国	DigmBio. Inc.	2024-03-26