Transcenta Holding Limited (Stock Code: 6628.HK) Announce 2024 Interim Results
Transcenta Holding Limited (Stock Code: 6628.HK) Announce 2024 Interim Results
Company continued the collaboration with Agilent Technologies, Inc. (Agilent), a world leader in CDx development, for Claudin18.2 specific IHC CDx Assay to support TranStar301 global Phase III pivotal trial of osemitamab (TST001) in combination with checkpoint inhibitor and chemotherapy. 2024 Interim Result Highlights (For the six months ended June 30, 2024)
2024年中期業績亮點(截至2024年6月30日)
Company published the efficacy and safety data of Cohort-G of TranStar102 study for osemitamab (TST001), plus checkpoint inhibitor and CAPOX as the first-line treatment of patients with locally advanced or metastatic G/GEJ cancer at ASCO annual meeting, showing that high/medium Claudin18.2 expression is associated with a median PFS of 12.6 months.
Company published the safety and PK data of TranStar101 study at the 2024 AACR annual meeting. The safety and pharmacokinetic profile of osemitamab (TST001) in the U.S. patients, is consistent with the profile reported in Chinese patients from TranStar102 study.
Company continued the collaboration with Agilent Technologies, Inc. (Agilent), a world leader in CDx development, for Claudin18.2 specific IHC CDx Assay to support TranStar301 global Phase III pivotal trial of osemitamab (TST001) in combination with checkpoint inhibitor and chemotherapy.
For Company's lead non-oncology asset, the anti-sclerostin antibody blosozumab (TST002), has been published Single Ascending Dose (SAD) study result in the 2024 World Congress on Osteoporosis, Osteoarthritis and Musculoskeletal Diseases (WCO-IOF-ESCEO Congress) in April. After a single dose of blosozumab (TST002) up to 1,200 mg, the average increase of lumbar spine BMD at day 85 (D85) ranged from 3.52% to 6.20% and total hip BMD from 1.30% to 2.24% across dose cohorts. The lumbar spine BMD increase exceeded the least significant difference level (2.77%) and was clinically meaningful.
Company has completed the enrolment of patients in the dose-escalation part for the First-in-Human (FIH) trial of the first-in-class anti-GREMLIN-1 antibody TST003 and the trial is ongoing at multiple clinical centers in the U.S. and China. Presented one Trial in Progress (TiP) poster of TST003-1001 study at the 2024 American Association for Cancer Research (AACR) annual meeting in April.
公司在ASCO年會上發佈了Cohort-G的TranStar102研究osemitamab(TST001)與PD-1抑制劑和CAPOX作爲局部晚期或轉移性G/GEJ癌症的一線治療的療效和安全性數據,顯示高/中度Claudin18.2表達與中位無進展生存期爲12.6個月相關。
公司在2024年AACR年會上發佈了TranStar101研究的安全性和藥動學數據。osemitamab(TST001)在美國患者中的安全性和藥動學特點與TranStar102研究中的中國患者報告的特點一致。
公司與全球CDx開發領先者艾捷倫科技(Agilent Technologies, Inc.)繼續合作,爲Claudin18.2特異性IHC CDx Assay提供支持,以支持osemitamab(TST001)與PD-1抑制劑和化療聯合治療的TranStar301全球III期關鍵試驗。
公司的主力非腫瘤資產anti-sclerostin抗體blosozumab(TST002)在2024年骨質疏鬆症、骨關節炎和肌肉骨骼疾病世界大會(WCO-IOF-ESCEO Congress)上發表了單劑量升級(SAD)研究結果。在單劑量blosozumab(TST002)高達1,200毫克後,腰椎骨密度(BMD)在第85天(D85)的平均增加範圍爲3.52%至6.20%,總髖骨BMD範圍爲1.30%至2.24%,腰椎骨密度的增加超過最小明顯差異水平(2.77%),具有臨床意義。
公司已完成了第一類抗GREMLIN-1抗體TST003的首度人類體驗(FIH)試驗的患者招募,並在美國和中國的多個臨床中心進行中。在2024年American Association for Cancer Research (AACR)年會上展示了TST003-1001研究的一項正在進行的試驗(TiP)展板。
HONG KONG, Aug. 29, 2024 /PRNewswire/ -- A clinical stage biopharmaceutical company – Transcenta Holding Limited ("Company"; stock code: 6628.HK) is pleased to announce the unaudited consolidated results of the Company and its subsidiaries (collectively, the "Group") for the six months ended June 30, 2024 (the "Reporting Period")
2024年8月29日香港/新聞稿/ -- 臨床階段的生物製藥公司--Transcenta Holding Limited("公司";股票代碼:6628.HK)很高興宣佈截至2024年6月30日("報告期")公司及其子公司(合稱"集團")的未經審計合併財務結果。
In the first half of 2024, the Company continued to accelerate clinical progress across both the oncology and non-oncology pipelines.
2024年上半年,公司在腫瘤學和非腫瘤學領域持續加速臨床進展。
For company's lead oncology asset, the Claudin18.2-targeting antibody osemitamab (TST001, A Humanized ADCC Enhanced Claudin18.2 mAb for Solid Tumors), reached key milestones for the treatment of gastric or gastroesophageal junction (G/GEJ) cancer. Company published the encouraging Phase II data of osemitamab (TST001) in combination with checkpoint inhibitor and standard chemotherapy as first-line treatment of G/GEJ cancer at American Society of Clinical Oncology annual meeting (ASCO), showing that high/medium Claudin18.2 expression is associated with a median PFS of 12.6 months. At the same period, Company published the safety and PK data of TranStar101 study at the 2024 AACR annual meeting. The safety and pharmacokinetic profile of osemitamab (TST001) in the U.S. patients, is consistent with the profile reported in Chinese patients from TranStar102 study.
對於公司的領先腫瘤學資產,克魯芯18.2靶向抗體osemitamab (TST001,用於實體瘤的人化ADCC增強型克魯芯18.2單抗)在胃或胃食管交界 (G/GEJ)癌症的治療中達到了重要里程碑。公司在美國臨床腫瘤學年會上發表了osemitamab (TST001)與檢查點抑制劑和標準化療聯合一線治療G/GEJ癌症的鼓舞人心的二期數據,顯示高/中等克魯芯18.2表達與中位進展生存期爲12.6個月。在同一時期,公司在2024 AACR年會上發佈了TranStar101研究的安全性和Pk數據。osemitamab (TST001)在美國患者中的安全性和藥代動力學特徵與TranStar102研究中報告的中國患者特徵一致。
Worked with Agilent Technologies, Inc. (Agilent), a world leader in CDx development, and developed a Claudin18.2 companion diagnostic test that can fully support the global pivotal trial of osemitamab (TST001). Successfully received regulatory clearances from the U.S. Food and Drug Administration (FDA), China Center for Drug Evaluation (CDE) and South Korea Ministry of Food and Drug Safety (MFDS). All the achievements validate and further support strategy for the Global Phase III trial (TranStar301). Osemitamab (TST001) is on track to become the first global therapy that delivers the next wave of innovation in the first-line treatment of patients with Claudin18.2 expressing locally advanced or metastatic G/GEJ cancer. Company also plans to explore several Claudin18.2 expressing advanced solid tumors other than G/GEJ cancer.
與Agilent Technologies, Inc. (Agilent)合作,開發了一種克魯芯18.2伴隨診斷試劑盒,可以完全支持osemitamab (TST001)的全球關鍵試驗。成功獲得了美國食品藥品監督管理局(FDA)、中國藥品評價中心(CDE)和韓國食品藥品安全處(MFDS)的監管審批。所有這些成就驗證並進一步支持全球三期試驗(TranStar301)的策略。osemitamab (TST001)有望成爲首個爲表達克魯芯18.2的局部晚期或轉移性G/GEJ癌症患者提供下一波創新的全球療法。公司還計劃探索除G/GEJ癌症以外的幾種表達克魯芯18.2的晚期實體瘤。
For lead non-oncology asset, the anti-sclerostin antibody blosozumab (TST002, A Humanized Sclerostin mAb for Osteoporosis), published Single Ascending Dose (SAD) study result in the 2024 World Congress on Osteoporosis, Osteoarthritis and Musculoskeletal Diseases (WCO-IOF-ESCEO Congress) in April. After a single dose of blosozumab (TST002) up to 1,200 mg, the average increase of lumbar spine BMD at day 85 (D85) ranged from 3.52% to 6.20% and total hip BMD from 1.30% to 2.24% across dose cohorts. The lumbar spine BMD increase exceeded the least significant difference level (2.77%) and was clinically meaningful.
對於非腫瘤學領域的領先資產,抗Sclerostin抗體blosozumab (TST002,用於骨質疏鬆症的人化Sclerostin單抗)在2024年骨質疏鬆症、骨關節炎和肌肉骨骼疾病全球大會(WCO-IOF-ESCEO Congress)上發佈了單次遞增劑量(SAD)研究結果。在blosozumab (TST002)單劑量達到1,200 mg後,腰椎骨密度在D85 (第85天)平均增加了3.52%至6.20%,總髖部骨密度在1.30%至2.24%之間。腰椎骨密度的增加超過了最低顯著差異水平 (2.77%),且具有臨床意義。
In addition, Company has completed the enrolment of patients in the dose-escalation part for the First-in-Human (FIH) trial of first-in-class anti-GREMLIN-1 antibody TST003 and the trial is ongoing at multiple clinical centers in the U.S. and China. Have presented one Trial in Progress (TiP) poster of TST003-1001 study at the 2024 American Association for Cancer Research (AACR) annual meeting in April.
此外,公司已完成首款抗GREMLIN-1抗體TST003的一期人體試驗的劑量逐步增加部分的患者招募工作,並該試驗正在美國和中國的多個臨床中心進行中。已在2024年4月美國癌症研究協會(AACR)年會上展示了TST003-1001研究的其中一個進行中試驗(TiP)海報。
Furthermore, progress had been made in improving the continuous bioprocessing platform technology HiCB (Highly Intensified Continuous Bioprocessing) and the technology was successfully implemented in the GMP manufacturing of osemitamab (TST001).
此外,在改善持續生物加工平台技術HiCb(高度強化的持續生物加工)方面取得了進展,併成功將該技術應用於osemitamab(TST001)的GMP製造。
Research/Early Development Update:
研究/早期開發更新:
TST013 (An ADC Candidate Targeting a Validated Tumor Antigen)- TST013 displayed significantly improved anti-tumor activity relative to benchmark ADC and improved tolerability profile which warrants further development
TST808 (A Humanized Antibody Neutralizing One of the Validated Key Targets Regulating B/Plasma Cell Proliferation and Survival) - TST808 has the potential to treat multiple autoimmune renal disorders including IgA nephropathy. Company has obtained the lead molecules and initiated the IND-enabling studies
TST013(一個ADC候選靶向一個經過驗證的腫瘤抗原)- TST013相對於基準ADC顯示出明顯改善的抗腫瘤活性,以及改善的可耐受性,有必要進一步開發
TST808(一種人源抗體,可以中和一個經過驗證的調節B/漿細胞增生和存活的關鍵靶點的抗體)- TST808具有治療多種自身免疫性腎臟疾病的潛力,包括IgA腎病。公司已獲得首選分子並啓動了IND的研究。
Business Development Achievements:
業務發展成果:
Company has continued the collaboration with Agilent for the Claudin18.2 specific IHC CDx Assay to support TranStar301 global Phase III pivotal trial of osemitamab (TST001) in combination with checkpoint inhibitor and chemotherapy
Company has continued the clinical trial collaboration with BMS, and completed the enrolment with osemitamab (TST001),checkpoint inhibitor and chemotherapy combination in TranStar102 in China and in TranStar101 in the U.S.
公司繼續與Agilent合作開展Claudin18.2特異性IHC CDx檢測以支持在全球範圍內進行的osemitamab(TST001)與檢查點抑制劑和化療藥物聯合用於TranStar301全球第三期關鍵試驗。
公司繼續與BMS進行臨床試驗合作,並完成了osemitamab(TST001)、檢查點抑制劑和化療聯合用於在中國的TranStar102和在美國的TranStar101的招募工作。
Technology Partnership & Advancement:
技術合作與進步:
Company has formed a strategic alliance with a company specialized in siRNA drug substance synthesis, to provide CDMO services in siRNA formulation development and F&F
Company's in-house cell culture media ExcelPro CHO are being evaluated for its performance against market standards for fed-batch, intensified fed-batch and perfusion processes by several external partners including a global leading company of media. This is part of potential collaboration for global commercialization of ExcelPro CHO
公司與一家專門從事siRNA藥物物質合成的公司建立了戰略聯盟,以提供siRNA配方開發和CDMO服務
公司內部培養基ExcelPro CHO正在被多個外部合作伙伴評估其在滿負荷、加強滿負荷和灌流過程中的性能,其中包括一家全球領先的培養基公司。這是潛在的ExcelPro CHO全球商業化合作的一部分
