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Sirnaomics Announces Completion of IND-Enabling Studies of Safety and Efficacy for STP125G With NHP Models, Targeting ApoC3 for Treatment of Cardiovascular Diseases

Sirnaomics Announces Completion of IND-Enabling Studies of Safety and Efficacy for STP125G With NHP Models, Targeting ApoC3 for Treatment of Cardiovascular Diseases

Sirnaomics宣佈完成對STP125G進行非人靈長類動物(NHP)模型的安全性和有效性的IND啓動研究,旨在治療心血管疾病目標爲ApoC3。
PR Newswire ·  07/12 16:25

HONG KONG, GERMANTOWN, Md. and SUZHOU, China, July 12, 2024 /PRNewswire/ -- Sirnaomics Ltd. (the "Company", Stock Code: 2257.HK, together with its subsidiaries, the "Group" or "Sirnaomics"), a leading biopharmaceutical company engaging in discovery and development of advanced RNAi therapeutics, announced today that the Group has completed IND-enabling studies for STP125G, an siRNA therapeutics targeting Apolipoprotein C3 (ApoC3), based on its proprietary GalAhead mxRNA technology. The safety and efficacy results from the non-human primate (NHP) studies strongly support for an IND filing with the U.S. FDA for initiating a Phase I clinical study of STP125G for cardiovascular disease indications.

2024年7月12日,Sirnaomics Ltd.(以下簡稱“公司”,股票代碼:2257.HK,及其子公司,以下簡稱“集團”或“Sirnaomics”)宣佈,基於其專有的GalAhead mxRNA技術,集團已完成了STP125G的IND啓動研究,這是一種靶向載脂蛋白C3(ApoC3)的siRNA治療藥物。安全性和療效結果表明,非人靈長類動物實驗(NHP)研究強烈支持向美國FDA遞交IND以啓動STP125G用於心血管疾病指示的一期臨床研究。

ApoC3 is a widely known player in triglyceride metabolism, and it has been recently recognized as a polyhedric factor which may regulate several pathways beyond lipid metabolism by influencing cardiovascular, metabolic, and neurological disease risk. High levels of triglycerides (TG) have been shown to be associated with increased risk of cardiovascular diseases. For severe hypertriglyceridemia (sHTG) patients whose TG level is more than 1000 mg/dL, the risk of developing acute pancreatitis is 5 to 10 times to that in the general population. Down-regulation of ApoC3 using siRNA or antisense oligonucleotides has been shown to be effective in lowering TG in sHTG patients.

ApoC3是三酰甘油代謝中的重要參與者,最近被認爲是一個多面因素,可以通過影響心血管、代謝和神經系統疾病風險來調節幾個通路。高三酰甘油血癥(sHTG)患者的甘油三酯(TG)水平超過1000 mg/dL,急性胰腺炎發生的風險是普通人群的5到10倍。使用siRNA或反義寡核苷酸下調ApoC3已被證明能夠有效降低sHTG患者的TG水平。

During an efficacy evaluation of STP125G with non-human primate model (N = 4), we observed a dose-dependent silencing activity among 1 mg/kg, 3 mg/kg and 10 mg/kg doses with a strong safety profile. The maximum target silencing efficacy was achieved at 10 mg/kg dosage around week 4 and was maintained for an additional 9 weeks (the total length of this 13-week study). The safety evaluation of STP125G using non-human primate model (N = 4) demonstrated an excellent safety readout with a single subcutaneous administration at 50 mg/kg, 100 mg/kg or 250 mg/kg. The maximum target silencing efficacies were like the level of 10 mg/kg for all three high dosages.

在非人靈長類動物模型(N = 4)中,我們觀察到STP125G的劑量相關的沉默活性,其中1mg/kg、3mg/kg和10mg/kg劑量中間呈現強烈的安全性特徵。目標沉默功效最大的劑量是10mg/kg,大約在第四周實現,並在額外的9周內維持(這項13周的研究的總長度)。使用非人靈長類動物模型(N = 4)進行的STP125G安全性評估表明,在50 mg/kg、100 mg/kg或250 mg/kg的單次皮下給藥下,其評估結果非常良好。三個高劑量的最大目標沉默效應都像10mg/kg的水平一樣。

"STP125G is the second drug candidate based on our GalAhead mxRNA technology that has shown excellent safety and potent efficacy results with the NHP models. Its long-lasting silencing activity against ApoC3 may provide better therapeutic benefit to patients suffering cardiovascular conditions, than those of antisense and other siRNA drugs." Dr. Patrick Lu, Founder, Chairman of the Board, Executive Director, President and Chief Executive Officer of Sirnaomics, indicated. "Those data readouts further validated STP125G as a novel siRNA therapeutic candidate for treatment of hypertriglyceridemia and other cardiovascular diseases, using our proprietary GalAhead-based delivery technology".

“STP125G是基於我們的GalAhead mxRNA技術的第二個藥物候選物,它在非人靈長類動物模型中顯示出了優秀的安全性和有效性結果。其持久的抑制ApoC3的沉默活性,可能比反義寡核苷酸和其他siRNA藥物爲患者患有心血管疾病提供更好的治療效果。” 方正證券創始人、董事長、執行董事、總裁兼首席執行官呂燕博士指出。 “這些數據結果進一步驗證了STP125G作爲一種新型靶向ApoC3 mRNA治療候選藥物,具有治療高三酰甘油血癥和其他心血管疾病的潛力,使用我們的專有的GalAhead基於遞送技術” 。

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About ApoC3 and STP125G

關於ApoC3和STP125G

ApoC3 is an important emerging target linking hypertriglyceridemia with cardiovascular disease (CVD). ApoC3 is a potent modulator of many established CVD risk factors, and is found on chylomicrons, VLDL, LDL, and HDL particles. Many studies show that in humans, apoC3 levels are an independent risk factor for CVD, and its presence on lipoproteins may promote their atherogenicity. Recent findings of the role of ApoC3 has been implicated in HDL metabolism and in the development of atherosclerosis, inflammation, and ER stress in endothelial cells. ApoC3 has been recently considered an important player in insulin resistance mechanisms, lipodystrophy, diabetic dyslipidemia, and postprandial hypertriglyceridemia (PPT). The emerging evidence of the involvement of ApoC3 in the pathogenesis of Alzheimer's disease open the way to further study if modification of ApoC3 level slows disease progression. Furthermore, ApoC3 is clearly linked to cardiovascular disease (CVD) risk, and progression of coronary artery disease (CAD) as well as the calcification of aortic valve and recent clinical trials has pointed out the inhibition of ApoC3 as a promising approach to manage hypertriglyceridemia and prevent CVD. Several evidences highlight the role of ApoC3 not only in triglyceride metabolism but also in several cardio-metabolic pathways. STP125G is a single-stranded siRNA therapeutics targeting ApoC3 mRNA, based on Sirnaomics proprietary GalAhead mxRNA technology.

ApoC3是一種重要的新興靶點,將高三酰甘油血癥與心血管疾病(CVD)聯繫在一起。ApoC3是許多已知CVD危險因素的強效調節因子,出現在乳糜微粒、VLDL、LDL和HDL顆粒上。許多研究表明,在人類中,apoC3水平是CVD的獨立危險因素,其存在於脂蛋白上可能促進其動脈粥樣硬化病理。ApoC3的作用最近已被認爲與HDL代謝、動脈粥樣硬化、內皮細胞炎症和內質網應激方面有關。ApoC3最近被認爲在胰島素抵抗機制、脂肪萎縮、糖尿病失調以及餐後高三酰甘油血癥方面扮演着重要角色。關於ApoC3與阿爾茨海默病發病機制的新發現,開闢了進一步研究修改ApoC3水平是否能緩解疾病進展的途徑。此外,ApoC3明顯與心血管疾病(CVD)風險、冠狀動脈疾病(CAD)進展以及主動脈瓣鈣化有關,最近的臨床試驗指出抑制ApoC3是管理高三酰甘油血癥和預防CVD的有希望的方法。幾個證據突出了ApoC3不僅在甘油三酯代謝中的作用,而且在幾個心臟代謝通路中也扮演着角色。STP125G是一種基於Sirnaomics專有的GalAhead mxRNA技術的單鏈siRNA治療藥物,靶向ApoC3 mRNA。

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 that focuses on the discovery and development of innovative drugs for indications with unmet 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, a polypeptide nanoparticle RNAi platform and GalNAc RNAi platform, GalAhead, Sirnaomics has established an enriched drug candidate pipeline. STP122G, which represents the first drug candidate utilizing the Group's GalAhead mxRNA technology, is currently in Phase I development. STP125G is the second siRNA therapeutics based on Sirnaomics proprietary GalAhead mxRNA technology, targeting ApoC3 mRNA for cardiovascular disease treatment. STP237G is the first dual-targeted drug based on a GalAhead muRNA technology and is in the late stage of preclinical evaluation. The Group has also had multiple successes with oncology applications through its clinical programs for STP705 and STP707. With the expansion of the Group's clinical pipeline and establishment of the Group's manufacturing facility, Sirnaomics focuses on a transition from a biotech company to a biopharma corporation. Learn more at: .

Sirnaomics是一家RNA治療生物製藥公司,專注於爲未滿足的醫學需求和大市場機會研發創新藥物。Sirnaomics是第一家在亞洲和美國都具備強大影響力的RNA治療公司。基於其專有的遞送技術,即多肽納米顆粒RNAi平台和GalNAc RNAi平台(GalAhead),Sirnaomics建立了豐富的藥物候選管道。STP122G代表了利用集團的GalAhead mxRNA技術的第一個藥物候選物,目前正在進行一期臨床研究。STP125G是基於Sirnaomics專有的GalAhead mxRNA技術的第二種siRNA治療藥物,針對心血管疾病的ApoC3 mRNA。STP237G是第一個基於GalAhead muRNA技術的雙重靶向藥物,並處於臨床試驗的後期評估中。針對甲狀腺癌和非小細胞肺癌等腫瘤應用的臨床計劃,Sirnaomics也取得了多重成功。以建立製造工廠和擴大臨床管道爲目標,Sirnaomics從生物技術公司向生物製藥公司轉變。欲了解更多信息,請訪問:。

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。


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