Sirnaomics Announces Completion of STP707 Phase I Clinical Study With Strong Safety Profile and Disease Activity for the Treatment of Pancreatic Cancer Patients
Sirnaomics Announces Completion of STP707 Phase I Clinical Study With Strong Safety Profile and Disease Activity for the Treatment of Pancreatic Cancer Patients
HONG KONG, GERMANTOWN, Md. and SUZHOU, China, June 28, 2024 /PRNewswire/ -- Sirnaomics Ltd. (the "Company", together with its subsidiaries, the "Group" or "Sirnaomics"; stock code: 2257), a leading biopharmaceutical company engaging in discovery and development of advanced RNAi therapeutics, today announced that the Group has completed STP707 Phase I clinical study with strong safety profile and stable disease activity for treatment of pancreatic cancer patients. This is a dose escalation study conducted in 11 oncology clinics in the U.S. The study involved six cohorts, consisting of 50 patients with various cancers, of which 11 had pancreatic cancer.
2024年6月28日,中國蘇州,香港和美國馬里蘭州傑曼敦(Germantown)——全球領先的RNAi治療創新藥物研發商及生產商——股份有限公司,及其附屬公司(以下簡稱“集團”;股份代號:2257)宣佈,集團已經完成用於治療胰腺癌患者的STP707一期臨床研究,結果顯示該藥物不僅安全,而且能提供一定的療效。在美國的11家腫瘤門診進行的劑量遞增研究涉及六個隊列,共有50名患有癌症的患者參與,其中11人患有胰腺癌。蘇州方正證券有限公司(Sirnaomics Ltd.)是一家領先的生物製藥公司,致力於發現和開發先進的RNAi治療藥物。該公司(以下簡稱“集團”)及其子公司是一家領先的生物製藥公司,致力於發現和開發先進的RNAi治療藥物。公司這裏的“集團”是指股份有限公司及其子公司。集團計劃議程Sirnaomics該公司的臨床研究STP707針對不同的癌症患者,進行了劑量遞增的研究,共涉及50名患有各種癌症的患者,其中11人患有胰腺癌。
In an earlier news release from the Company in August 2023, the Group noted completion of all dosing regimens for its Phase I study of STP707 for the treatment of multiple solid tumors. This basket study has enrolled patients suffering from various types of late-stage cancers and failing after multiple rounds of treatments. The study is to evaluate the safety, tolerability and anti-tumor activity of the Group's siRNA (small interfering RNA) drug candidate, STP707, through intravenous infusion (IV) with six cohorts of escalating doses. Patients including pancreatic, colorectal, liver, melanoma and other cancers, with advanced/ metastatic or surgically unresectable solid tumors, refractory to standard therapy, were recruited. Six dose levels (3mg, 6mg, 12mg, 24mg, 36mg and 48mg) were explored in ascending doses. Patients received IV infusion on Day 1, 8, 15 and 22 of a 28-days cycle.
公司在2023年8月發表的一份新聞稿中指出,已完成了用於治療多種實體腫瘤的STP707第一階段研究的所有給藥方案。該草藥研究涉及多組病人,共有多種晚期癌症,而且病人都在接受多次治療失敗後才參加了這次研究。該研究旨在評估該公司的siRNA(小干擾RNA)候選藥物STP707的安全性、耐受性和抗腫瘤活性,通過靜脈輸注(IV)六個遞增劑量的隊列。招募了患有胰腺癌、結直腸癌、肝癌、黑色素瘤和其他癌症的患者,乃至於晚期/轉移或無法手術摘除的實體腫瘤,不受標準治療。
11 pancreatic patients (five males and six females, average age 64 years) were enrolled in the study. Patients were heavily pre-treated and received, on average, three lines of therapy prior to enrollment in the study (including Gemcitabine, Paclitaxel and Folfirinox). The preliminary results indicated that the mean treatment cycles completed was three cycles (average 12 doses). The average days for stable disease for all 11 patients with STP707 treatment was 92 days, while 31 days for the 12mg group, 65 days for 24mg group and 112 days for 48mg group, including one patient ongoing at 281 days. No treatment related adverse events (TRAE) were reported for the 11 patients, except for one patient with a Grade 2 infusion reaction. Non-treatment related adverse events were secondary to their advanced metastatic disease including intestinal obstruction, abdominal distention, gastrointestinal obstruction, embolism, gastrointestinal hemorrhage, tumor pain, hypoxia and dyspnea.
該階段試驗納入了11名患有胰腺癌的患者(5名男性和6名女性,平均年齡64歲)。這些患者都曾接受過多次治療,平均接受過三個療程(包括吉西他濱(Gemcitabine)、紫杉醇(Paclitaxel)和Folfirinox)。初步結果表明,這些患者完成的平均治療週期爲三個療程(平均12劑量)。STP707治療的所有11名患者的穩定疾病平均持續時間爲92天,其中12mg組爲31天,24mg組爲65天,48mg組爲112天,其中一名患者至今已持續281天。除一名患者發生2度輸入反應外,這11名患者均未報告發生與治療相關的不良事件(TRAE)。未治療相關的不良事件是由於他們的晚期轉移性疾病,包括腸梗阻、腹部脹氣、胃腸梗阻、栓塞、胃腸道出血、腫瘤疼痛、缺氧和呼吸困難等。
The maximum tolerated dose of STP707 for all 50 late-stage cancer patients was not reached even at 48mg dosage level. STP707 was very well-tolerated in a heavily pretreated cancer patient population. The 11 pancreatic subset of patients showed low toxicity and relatively long stable disease at various dosages (106, 281 and 302 days), and warrants further study with STP707 alone or in combination with immune check point inhibitors, given the preclinical documented ability of STP707 to recruit T-cells to the tumor microenvironment (TME). This is the first time a polypeptide nanoparticle-based siRNA cancer therapeutic has demonstrated early positive safety and efficacy results for the treatment of late-stage pancreatic cancer patients.
對於所有50名晚期癌症患者,STP707的最大可耐受劑量甚至在48mg劑量下也沒有達到。這個藥物在一個接受過多次治療的癌症患者中表現得非常良好。對於其中11名胰腺癌患者而言,副作用很小,長時間具有穩定疾病的影響,要求進一步研究STP707単獨治療或結合免疫檢查點抑制劑治療。這是首個基於多肽納米粒子技術相關的siRNA癌症治療藥物,它證明了能在晚期胰腺癌患者身上及早顯示出安全和有效治療的跡象。
"We are very excited to see STP707, our leading siRNA drug product for the treatment of heavily pre-treated pancreatic cancer (one of the deadliest tumor types), shows these strong results upon intravenous administration. This is a very promising result for RNAibased cancer therapeutics for the treatment of metastasized tumors." said Dr. Patrick Lu, Ph.D., Founder, Chairman of the Board, Executive Director, President and Chief Executive Officer of Sirnaomics. "The strong safety profile, long-lasting stable disease efficacy and dose-dependent antitumor activity of this intravenously administered STP707 formulation, present a potential novel cancer therapeutic, either as a single drug or in combination with immune check point inhibitor drugs."
“我們很高興看到STP707,在靜脈給藥後能夠顯示出重度預處理胰腺癌的強力療效。這對於RNAi治療腫瘤是十分有前景的。在YKF系列藥物中,這是首次顯示出通過靜脈輸注這種形式賦予的藥物具有很強的穩定疾病和劑量依賴性抗腫瘤活性。這可以成爲潛在的新型癌症治療藥物,無論是作爲單一藥物還是與免疫檢查點抑制劑藥物結合使用。”方正證券有限公司(Sirnaomics Ltd.)的創始人、董事長、執行董事、總裁和首席執行官博士帕特里克•呂博士說道。帕特里克•呂(Dr. Patrick Lu) 方正證券有限公司(Sirnaomics Ltd.)的創始人、董事長、執行董事、總裁和首席執行官 有限公司(Sirnaomics Ltd.)“通過靜脈輸注(STP707)這種方式提供的這種領先的RNAi藥物,爲治療晚期腫瘤患者(其中之一是最致命的腫瘤類型之一——胰腺癌患者)提供了這樣的強健有效的結果,這令人非常興奮。”
For more information about Sirnaomics' clinical trials please visit ClinicalTrials.gov (Identifier NCT05037149) and the Company's website at .
有關方正證券公司臨床試驗的更多信息,請訪問ClinicalTrials.gov(標識符NCT05037149)和公司網站。
About STP707
關於STP707 STP707由兩種靶向TGF-β1和COX-2 mRNA的siRNA寡核苷酸組成,配合組成納米粒子的組合的組合物,並以組合物內的組合多肽作爲載體載體進行配製,該載體多肽與Sirnaomics的STP705產品中使用的載體不同。 每個siRNA的單獨應用均顯示出抑制其靶向mRNA表達,而兩個siRNA的結合則呈現出減輕炎症因子的協同效應。 TGF-β1和COX-2的過表達在腫瘤發生中扮演了關鍵的調節作用,在STP707的體外研究中,靜脈輸注導致了對肝臟,肺和異種移植腫瘤等各種器官的TGF-β1和COX-2基因表達的抑制。 此外,在體外研究中,STP707在各種實體腫瘤類型中均表現出了強大的抗腫瘤活性。 在小鼠肝臟原位移植腫瘤模型中,實驗結果表明,STP707與免疫檢查點抗體的聯合治療方案具有強烈的抗腫瘤活性。
STP707 is composed of two siRNA oligonucleotides, targeting TGF-β1 and COX-2 mRNA respectively, formulated in nanoparticles with a Histidine-Lysine Co-Polymer (HKP+H) peptide as the carrier. The specific carrier peptide is distinct from the carrier used in Sirnaomics' STP705 product. Each individual siRNA was demonstrated to inhibit the expression of their target mRNAs and combining the two siRNA's produces a synergistic effect that diminishes pro-inflammatory factors. Over-expression of TGF-β1 and COX-2 have been well-characterized in playing key regulatory roles in tumorigenesis. In preclinical studies with STP707, IV administration resulted in knock-down of TGF-β1 and COX-2 gene expressions in various organs including liver, lung and xenograft tumor. In addition, in preclinical models STP707 had shown strong antitumor activity in various solid tumor types. Using a mouse liver orthotopic tumor model, a combination regimen of STP707 with an immune checkpoint antibody has demonstrated a potent antitumor activity.
關於方正證券有限公司(Sirnaomics Ltd.) 方正證券有限公司(Sirnaomics Ltd.)是一家RNA療法生物製劑公司,其產品候選病人針對具有醫療需求和大市場機會的難以治療的疾病。Sirnaomics是第一家在亞洲和美國都有強大影響力的RNA療法生物製劑公司。基於其專有的遞送技術(多肽納米粒子製劑和2代GalNAc偶聯物),該集團建立了一套實體藥物候選研發管道。Sirnaomics正在推進用於腫瘤應用的RNAi治療,其臨床項目STP705和STP707都已取得了多項成功。 STP122G代表了進入臨床開發的首個GalAhead技術藥物候選者。該公司目前正在進行從生物科技公司到生物製藥公司的轉型。了解更多信息,請訪問公司網站。
About Sirnaomics
方正證券有限公司(Sirnaomics Ltd.)是一家RNA療法生物製劑公司,其產品候選病人針對具有醫療需求和大市場機會的難以治療的疾病。方正證券是第一家在亞洲和美國都有強大影響力的RNA療法生物製劑公司。基於其專有的遞送技術(多肽納米粒子製劑和2代GalNAc偶聯物),該集團建立了一套實體藥物候選研發管道。方正證券正在推進用於腫瘤應用的RNAi治療,其臨床項目STP705和STP707都已取得了多項成功。 STP122G代表了進入臨床開發的首個GalAhead技術藥物候選者。該公司目前正在進行從生物科技公司到生物製藥公司的轉型。了解更多信息,請訪問公司網站。
Sirnaomics is an RNA therapeutics biopharmaceutical company with product candidates in preclinical and clinical stages that focuses on the discovery and development of innovative drugs for indications with medical needs and large market opportunities. Sirnaomics is the first clinical-stage RNA therapeutics company to have a strong presence in both Asia and the United States. Based on its proprietary delivery technologies: Polypeptide Nanoparticle Formulation and the 2nd generation of GalNAc conjugates, the Group has established an enriched drug candidate pipeline. Sirnaomics is advancing RNAi therapeutics for oncology application with multiple successes of its clinical programs for STP705 and STP707. STP122G represents the first drug candidate of GalAhead technology entering clinical development. With the establishment of the Group's manufacturing facility, Sirnaomics currently is undergoing a transition from a biotech company to a biopharma corporation. Learn more at: .
蘇州方正證券有限公司(Sirnaomics Ltd.)
SOURCE Sirnaomics
來源:方正證券有限公司(Sirnaomics Ltd.)
譯文內容由第三人軟體翻譯。