Atea Pharmaceuticals Presents Positive Initial Phase 2 Data for Bemnifosbuvir and Ruzasvir Combination for Treatment of Hepatitis C Virus at EASL Congress 2024
Atea Pharmaceuticals Presents Positive Initial Phase 2 Data for Bemnifosbuvir and Ruzasvir Combination for Treatment of Hepatitis C Virus at EASL Congress 2024
97% SVR12 Rate Observed with 8 Weeks of Treatment in Lead-In Cohort of HCV-Infected Patients in Ongoing Phase 2 Clinical Study
在進行中的第二期臨床研究的HCV感染患者的前導隊列中,8周的治療表現出了97%的SVR12率。
EASL Presentations Continue to Support Best-in-Class Potential with High Antiviral Potency, Short Treatment Duration, Low Risk of Drug Interaction and High Barrier to Resistance
EASL展示了高抗病毒效力,短時間治療,低藥物相互作用風險和高抗性阻礙潛力的最佳潛力。
BOSTON, June 05, 2024 (GLOBE NEWSWIRE) -- Atea Pharmaceuticals, Inc. (Nasdaq: AVIR) ("Atea"), a clinical-stage biopharmaceutical company engaged in the discovery and development of oral antiviral therapeutics for serious viral diseases, today announced new data from the lead-in cohort (n=60) of the Company's ongoing Phase 2 combination study of bemnifosbuvir, an oral nucleotide NS5B polymerase inhibitor, and ruzasvir, an oral NS5A inhibitor, for the treatment of hepatitis C virus (HCV). With an 8-week treatment duration, the Phase 2 data from the lead-in cohort of non-cirrhotic patients showed a 97% sustained virologic response rate at 12 weeks post-treatment (SVR12), which is the primary efficacy endpoint of the study.
2024年6月5日,波士頓(GLOBE NEWSWIRE) - Atea Pharmaceuticals,Inc.(納斯達克:AVIR)(“Atea”)是一家處於臨床階段的生物製藥公司,致力於發現和開發口服抗病毒治療劑治療嚴重病毒性疾病,今天宣佈新的數據來自公司正在進行的研究的前導隊列(n = 60),該研究是bemnifosbuvir和ruzasvir的組合研究,經口服核苷酸NS5B聚合酶抑制劑和口服NS5A抑制劑用於治療丙型肝炎病毒(HCV)。根據8周的治療經歷,非肝硬化患者的第二期數據顯示,12周後治療(SVR12)的持久病毒學反應率達到97%,這是該研究的主要療效終點。
The Company will also present preclinical data further demonstrating a high barrier to resistance and pharmacokinetics for bemnifosbuvir and a low risk of drug-drug interactions for ruzasvir. These data are being presented at the European Association for the Study of the Liver (EASL) Congress taking place June 5-8, 2024, in Milan, Italy.
該公司還將展示預臨床數據,進一步證明bemnifosbuvir具有高抗性阻礙和藥代動力學,而ruzasvir的藥物-藥物相互作用風險低。這些數據將於2024年6月5日至8日在意大利米蘭舉行的歐洲肝病研究協會(EASL)大會上展示。
"Today, new challenges are hindering progress towards our goal of HCV elimination in the U.S. and globally. Patient demographics have changed, and the pace of new HCV infections is quickly outpacing the rate of those being treated. It is apparent that further innovations are required to address the needs of today's HCV-infected patients," said Jean-Pierre Sommadossi, PhD, Chief Executive Officer and Founder of Atea Pharmaceuticals. "The data being presented at EASL demonstrate a potential best-in-class profile that combines the most compelling attributes of current HCV drug treatments through the innovative combination of bemnifosbuvir and ruzasvir. We look forward to reporting the full results from our ongoing Phase 2 study during the second half of this year."
“今天,新的挑戰正在阻礙在美國和全球實現HCV消除的進展。患者人口統計數據已經改變,新發HCV感染病例的速度正在迅速超過正在接受治療的病例的速度。顯然,需要進一步創新來滿足今天HCV感染患者的需求,”Atea Pharmaceuticals的首席執行官兼創始人Jean-Pierre Sommadossi博士說道。“在EASL展示的數據展示出了一種潛在的最佳組合,將當前HCV藥物治療的最具吸引力的特點集於一體,通過bemnifosbuvir和ruzasvir的創新組合。我們期待在今年下半年報告正在進行的第二階段研究的完整結果。”
Results from the lead-in cohort of the Phase 2 study also showed a 100% SVR12 rate in participants infected with genotype 3 (n=13), a historically difficult-to-treat genotype of HCV. The combination regimen was well tolerated, with no drug-related severe adverse events (SAEs) or treatment discontinuations. Based on these positive data from the lead-in cohort, the Phase 2 study continues, with the aim of enrolling up to an additional 220 subjects, including those with compensated cirrhosis.
第二期研究的前導隊列結果還顯示,基因型3感染者(n = 13)的SVR12率達到100%,這是歷史上難以治療的HCV基因型。該組合方案耐受性良好,沒有藥物相關的嚴重不良事件(SAE)或治療中止。基於前導隊列的這些積極數據,第二期研究正在繼續進行,旨在招募最多220名受試者,包括那些有代償性肝硬化的人。
"Today, many of my HCV patients present with other conditions requiring multiple concurrent therapies and complicated lives," said Eric Lawitz, MD, The Texas Liver Institute, Clinical Professor of Medicine, University of Texas Health San Antonio. "I am excited about the initial bemnifosbuvir and ruzasvir combination data. The combination of a short 8-week treatment duration, a low risk of drug-drug interactions, and robust antiviral efficacy across all genotypes makes this an attractive regimen."
“今天,我的HCV患者中有很多人因患其他病症而需要接受多種同時治療和複雜的生活方式,”德州肝臟研究所的Eric Lawitz醫學博士,德克薩斯大學健康聖安東尼奧分校醫學臨床教授說。我對bemnifosbuvir和ruzasvir組合的初始數據感到興奮。將短短的8周療程,低藥物相互作用的風險和所有基因型的強有力的抗病毒效力結合起來,使該療法更具吸引力。”
More than 2 million people in the U.S. are living with chronic HCV, and approximately 100,000 new chronic cases are diagnosed each year. HCV diagnoses continually outpace annual treatment rates, as less than a third of those diagnosed with HCV receive timely treatment.
美國有超過200萬人患有慢性HCV,每年診斷大約10萬例新的慢性病例。HCV的診斷不斷超過年度治療率,因爲僅有不到三分之一被HCV診斷的人接受及時治療。
Data Presented at EASL Include:
EASL演示數據:
Poster Title: Lead-in Cohort Results From a Phase 2 Study of a Novel 8-Week Combination Regimen of Bemnifosbuvir and Ruzasvir in Patients with Chronic Hepatitis C Virus Infection (THU-382)
Conclusion: Data from the lead-in cohort of 60 patients in the Phase 2 clinical trial of bemnifosbuvir and ruzasvir in HCV-infected subjects showed a high SVR12 rate of 97% in the lead-in cohort with a short 8-week duration of treatment. The primary endpoints of the study are safety and SVR12. Viral kinetics were similar in genotype 1 and genotype 3 infected subjects, including a 100% SVR12 rate in historically difficult-to-treat genotype 3 infected subjects. The combination was generally safe and well tolerated. There were no drug-related serious adverse events or treatment discontinuations, and adverse events were mostly mild.
海報標題:慢性丙型肝炎病毒感染患者新型8周組合方案Bemnifosbuvir和Ruzasvir的第二期研究的前導隊列結果(THU-382)
結論:在HCV感染的受試者中,bemnifosbuvir和ruzasvir的臨床試驗的第二期研究中,前導隊列中的60名患者的數據顯示,8周的療程具有高達97%的高SVR12率。研究的主要終點是安全性和SVR12。各基因型感染者的病毒動力學類似,包括在歷史上難以治療的基因型3感染者中實現的100%的SVR12率。這種組合通常是安全和耐受的。沒有藥物相關的嚴重不良事件或治療中止,不良反應大多是輕微的。
Poster Title: Bemnifosbuvir is a Potent HCV NS5B Inhibitor with a Favorable Antiviral Profile and High Resistance Barrier (SAT-402)
Conclusion: Viral resistance is an important consideration for direct-acting antiviral (DAA) use as it may impact the efficacy of treatments for HCV infection. Results demonstrated that bemnifosbuvir is at least ten-fold more potent than sofosbuvir, a medication to treat HCV infections, across all genotypes tested and is not resistant to resistance-associated substitutions (RASs) that have been found to alter the activity of sofosbuvir. While the C223H mutation was found to be the primary bemnifosbuvir RAS in genotype 1b, multiple additional substitutions at other NS5B regions were required to confer meaningful resistance, suggesting that bemnifosbuvir provides a high barrier to resistance. Based upon the data demonstrated to date, it is expected that the bemnifosbuvir and ruzasvir combination should have a more compelling antiviral profile against major HCV NS5A RAVs than the current standard of care.
海報標題:Bemnifosbuvir是一種具有良好抗病毒特性和高抗性阻礙的HCV NS5B抑制劑(SAT-402)
結論:病毒抗性是直接作用抗病毒(DAA)使用的重要考慮因素,因爲它可能影響HCV感染的治療效果。結果表明,與用於治療HCV感染的藥物sofosbuvir相比,bemnifosbuvir在所有測試的基因型中至少比sofosbuvir強10倍,並且對已發現會改變sofosbuvir活性的耐藥菌株(RAS)沒有抗性。儘管發現C223H突變是基因型1b的主要bemnifosbuvir RAS,但在其他NS5B區域需要多個附加替換才能產生有意義的抗性,這表明bemnifosbuvir提供了很高的抗性阻礙潛力。根據迄今展示的數據,預期bemnifosbuvir和ruzasvir組合應比當前的標準療法具有更有力的抗HCV NS5A RAVs的抗病毒特性。
Poster Title: Absorption, Distribution, Metabolism, and Excretion of [14C]-Bemnifosbuvir in Rats (SAT-411)
Conclusion: This preclinical study in rats was conducted to better understand the tissue distribution, metabolites, and excretion routes following bemnifosbuvir treatment. Following a single oral dose in rats, bemnifosbuvir has favorable overall absorption, distribution, metabolism, and excretion (ADME) properties, including good bioavailability (>60%) and wide distribution to tissues with low penetration into the brain. Bemnifosbuvir was highly and rapidly metabolized to the metabolite AT-273, consistent with the proposed metabolic and activation pathway.
海報標題:大鼠中[14C] - Bemnifosbuvir的吸收,分佈,代謝和排出(SAT-411)
結論:在大鼠中進行的這項臨床前研究旨在更好地了解經bemnifosbuvir治療後的組織分佈,代謝物和排出途徑。在大鼠中單次口服後,bemnifosbuvir具有有利的全局吸收,分佈,代謝和排出(ADME)特性,包括良好的生物利用度(> 60%)和廣泛的低腦組織分佈。Bemnifosbuvir在短時間內高度迅速被代謝爲類似於其代謝物AT-273,與擬定的代謝和活化途徑一致。
Poster Title: Low Risk of Drug-Drug Interactions for Ruzasvir Based Upon In Vitro Metabolism and Transporter Interaction Studies (SAT-412)
Conclusion: Many patients infected with HCV are also taking multiple co-medications, which may impact treatment decisions. This preclinical study aimed to further understand the risk of drug-drug interactions (DDIs) for ruzasvir by analyzing its metabolism in human liver microsomes and cells. Based on these in vitro data and static DDI risk assessment models, ruzasvir has a low potential to be a perpetrator of DDIs via inhibition or induction of CYP450. Similarly, it has a low potential to inhibit OATP1B1 and OATP1B3 transporters. The relevance of bile salt export pump (BSEP) inhibition to DDIs is limited.
海報標題:根據體外代謝和轉運蛋白相互作用研究,Ruzasvir對藥物-藥物相互作用風險的低風險(SAT-412)體外評估Sulopenem對結論:許多HCV感染的患者還服用多種伴隨治療,可能影響治療決策。這項臨床前研究旨在進一步了解ruzasvir通過分析其在人類肝微粒體和細胞中的代謝率的藥物-藥物相互作用(DDI)的風險。根據這些數據和靜態DDI風險評估模型,通過CYP450的抑制或誘導,ruzasvir有很低的作爲施害者DDI的潛力。同樣,它有很低的抑制OATP1B1和OATP1B3轉運蛋白的潛力。BSEP的抑制對DDIs的相關性有限。
結論:許多HCV患者正在服用多種共同藥物,這可能會影響治療決策。這項臨床前研究旨在通過分析人類肝臟微粒體和細胞中的代謝作用,進一步了解魯扎斯韋的藥物-藥物相互作用(DDI)風險。基於這些數據和靜態DDI風險評估模型,魯扎斯韋具有對CYP450的抑制或誘導導致DDI的低潛力。同樣,它對OATP1B1和OATP1B3轉運蛋白的抑制潛力也很低。關於膽鹽泵(BSEP)的抑制與DDI的相關性受到限制。在體外根據這些數據和靜態DDI風險評估模型,魯扎斯韋通過抑制或誘導CYP450具有DDI作用的潛力很低。同樣,它對OATP1B1和OATP1B3轉運蛋白的抑制潛力也很低。膽鹽泵(BSEP)的抑制與DDI相關性有限。
About Hepatitis C Virus
關於丙型肝炎病毒
Hepatitis C virus (HCV) is a blood-borne, positive-sense, single-stranded (ss)RNA virus that primarily infects liver cells. HCV is a leading cause of chronic liver disease and liver transplants, spreading via blood transfusion, hemodialysis, and needle sticks. An estimated 50 million people globally live with chronic HCV infection, with approximately 1 million new infections and 242,000 deaths occurring each year. Most HCV-related deaths are due to liver scarring (cirrhosis) and liver cancer (hepatocellular carcinoma). Injection drug use accounts for around 30% of new HCV cases globally and approximately 60% in the U.S. Annually, HCV diagnoses in the U.S. outpace treatment rates, as less than a third of those diagnosed with HCV receive timely treatment.
丙型肝炎病毒(HCV)是一種通過血液傳播的陽性單鏈RNA病毒,主要感染肝細胞。HCV是慢性肝病和肝移植的主要原因,通過輸血、透析和針刺傳播。全球約有5000萬人患有慢性HCV感染,每年約有100萬新感染和24.2萬人死亡。大多數HCV相關死亡是由肝硬化和肝癌造成的。注射毒品在全球新HCV病例中佔約30%,在美國約佔60%。在美國,HCV的診斷數量超過治療率,因爲僅有不到三分之一的HCV患者能及時接受治療。
About Bemnifosbuvir and Ruzasvir for Hepatitis C Virus (HCV)
關於伯曼膚巴和魯扎維ρ治療丙型肝炎病毒(HCV)
Bemnifosbuvir is an oral, purine nucleotide prodrug designed to inhibit viral replication by impairing viral RNA polymerase, a key component in the replication machinery of enveloped positive single-stranded RNA viruses, such as human coronaviruses and HCV. Atea is developing bemnifosbuvir in combination with ruzasvir, an oral NS5A inhibitor for the treatment of HCV. As single agents, both bemnifosbuvir and ruzasvir have demonstrated potent pan-genotypic antiviral activity against HCV. The combination of bemnifosbuvir and ruzasvir has exhibited synergistic in vitro activity against HCV with no pharmacokinetic (PK) drug-drug interactions in healthy volunteers.
伯曼膚巴是一種口服嘌呤核苷酸類藥物,通過損害病毒RNA聚合酶,這是隔膜型正單鏈RNA病毒如人類冠狀病毒和HCV複製機器中的關鍵組成部分,以抑制病毒複製。 Atea正在研究伯曼膚巴與魯扎維ρ,一種口服NS5A抑制劑結合起來治療HCV。 作爲單一藥物,伯曼膚巴和魯扎維ρ都表現出強有力的泛基因型抗病毒活性針對HCV。 伯曼膚巴和魯扎維ρ的聯合使用表現出對HCV的協同作用,並且在健康志願者中沒有藥物動力學(PK)藥物相互作用。在體外這種HCV的區間透析應進行抗病毒治療,建議在透析前進行治療以防止感染。 研究表明,伯曼膚巴和魯扎維ρ合用,可以對抗HCV的活性,且與健康志願者中沒有PK藥物相互作用。
In vitro studies have shown bemnifosbuvir to be approximately 10-fold more active than sofosbuvir (SOF) against a panel of laboratory strains and clinical isolates of HCV GT 1–5. In vitro studies have also demonstrated that bemnifosbuvir remained fully active against SOF resistance-associated strains (S282T), with up to 58-fold more potency than SOF. The PK profile of bemnifosbuvir supports once-daily dosing for the treatment of HCV. Across both HCV and COVID-19 programs, bemnifosbuvir has been administered to over 2,100 subjects and has been well-tolerated at doses up to 550 mg for durations up 12 weeks in healthy subjects and patients.
體外小鼠數據表明,用UNO局部治療固體腫瘤癌症模型可以刺激抗腫瘤免疫反應。Beyond Cancer, Ltd. 相信UNO具有防止復發或轉移性疾病的潛力,僅需單次5分鐘的治療,並具有有限的毒性或非靶向效果。研究表明,伯曼膚巴對HCV的實驗室株和臨床分離物(HCV GT 1-5)的活性約爲索磷布韋(SOF)的10倍。體外小鼠數據表明,用UNO局部治療固體腫瘤癌症模型可以刺激抗腫瘤免疫反應。Beyond Cancer, Ltd. 相信UNO具有防止復發或轉移性疾病的潛力,僅需單次5分鐘的治療,並具有有限的毒性或非靶向效果。研究還表明,伯曼膚巴對SOF抵抗相關株(S282T)保持完全活性,比SOF具有最高高達58倍的藥效。伯曼膚巴的PK藥代動力學特性支持一日一次口服,用於HCV治療。 伯曼膚巴已在HCV和COVID-19項目中向超過2100名受試者給予劑量最高可達550 mg的長達12周的治療,患者很好地耐受了伯曼膚巴。
Ruzasvir has demonstrated highly potent and pan-genotypic antiviral activity in preclinical (picomolar range) and clinical studies. Ruzasvir has been administered to over 1,200 HCV-infected patients at daily doses of up to 180 mg for 12 weeks and has demonstrated a favorable safety profile. Ruzasvir's PK profile supports once-daily dosing.
魯扎維ρ在大規模的臨床前(pico摩爾級)和臨床研究中顯示出高度強大的泛基因型抗病毒活性。 魯扎維ρ已經以每天180毫克的劑量給超過1,200名HCV感染患者治療了12周,顯示出良好的安全性。
About the Phase 2 Study
關於第2期研究
Atea is currently conducting a global Phase 2 clinical trial in treatment-naïve, chronic HCV-infected patients either without cirrhosis or with compensated cirrhosis. This study is designed to evaluate the safety and efficacy of eight weeks of treatment with the combination consisting of once-daily bemnifosbuvir 550 mg and ruzasvir 180 mg. Up to approximately 280 treatment-naïve patients across all HCV genotypes, including the lead-in cohort of 60 patients without cirrhosis, are expected to be enrolled in this Phase 2 clinical trial.
Atea目前正在針對處於無肝硬化或有代償性肝硬化狀態的未接受治療的慢性HCV感染患者進行全球第2期臨床試驗。該研究旨在評估每日一次伯曼膚巴550 mg和魯扎維ρ180 mg的聯合治療8周的安全性和療效。 預計將在該第2期臨床試驗中招募近280名處於各種HCV基因型狀態下的未接受治療的患者,包括60例無肝硬化的患者。
The primary endpoints of the study are safety and sustained virologic response (SVR) at 12 weeks post-treatment (SVR12). Other virologic endpoints include virologic failure, SVR at 24 weeks post-treatment (SVR24) and resistance. Topline results from all patients enrolled in the Phase 2 study are anticipated in the second half of 2024.
該研究的主要終點是安全性和12周治療後持續病毒學反應(SVR)(SVR12)。其他病毒學終點包括病毒學失敗、24周治療後的持續病毒學反應(SVR24)和抗藥性。 預計將在2024年下半年公佈第2期研究中招募的所有患者的結果。
About Atea Pharmaceuticals
關於Atea製藥公司
Atea is a clinical-stage biopharmaceutical company focused on discovering, developing and commercializing oral antiviral therapies to address the unmet medical needs of patients with serious viral infections. Leveraging the Company's deep understanding of antiviral drug development, nucleos(t)ide chemistry, biology, biochemistry and virology, Atea has built a proprietary nucleos(t)ide prodrug platform to develop novel product candidates to treat single stranded ribonucleic acid, or ssRNA, viruses, which are a prevalent cause of serious viral diseases. Atea plans to continue to build its pipeline of antiviral product candidates by augmenting its nucleos(t)ide platform with other classes of antivirals that may be used in combination with its nucleos(t)ide product candidates. Currently, Atea is focused on the development of orally-available antiviral agents for severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), the virus that causes COVID-19, and hepatitis C virus (HCV). For more information, please visit .
Atea是一家臨床階段的生物製藥公司,專注於發現,開發和商業化口服抗病毒治療藥物,以滿足患有嚴重病毒感染的患者的未滿足的醫療需求。 Atea基於公司對抗病毒藥物開發,核苷(酸)化學,生物學,生物化學和病毒學的深刻理解,構建了專有的核苷(酸)脂肪酸類藥物平台,以開發治療單鏈核糖核酸,或ssRNA病毒的新產品候選藥物,這是嚴重病毒性疾病流行的原因。Atea計劃通過使用可與其核苷(酸)類藥物平台組合使用的其他類別的抗病毒藥物來增加其抗病毒產品候選藥物的管線。目前,Atea專注於開發口服抗病毒治療嚴重急性呼吸綜合症冠狀病毒2(SARS-CoV-2)和丙型肝炎病毒(HCV)的藥物。欲了解更多信息,請訪問 。
Forward-Looking Statements
前瞻性聲明
This press release includes "forward-looking statements" within the meaning of the Private Securities Litigation Reform Act of 1995. Forward-looking statements in this press release include but are not limited to the Company's plans relating to the date and time of the presentations at the conference, the time of anticipated release of additional clinical data and the potential of bemnifosbuvir in combination with ruzasvir to treat HCV. When used herein, words including "expects," "may," "will," "anticipates," "plans," and similar expressions are intended to identify forward-looking statements. In addition, any statements or information that refer to expectations, beliefs, plans, projections, objectives, performance or other characterizations of future events or circumstances, including any underlying assumptions, are forward-looking. All forward-looking statements are based upon the Company's current expectations and various assumptions. The Company believes there is a reasonable basis for its expectations and beliefs, but they are inherently uncertain. The Company may not realize its expectations, and its beliefs may not prove correct. Actual results could differ materially from those described or implied by such forward-looking statements as a result of various important factors, including, without limitation, the important factors discussed and updated from time to time under the caption "Risk Factors" in the reports the Company files with the SEC, including annual reports on Form10-K, quarterly reports on Form10-Q, current reports on Form 8-K and other filings each of which are accessible on the SEC's website at www.sec.gov. These and other important factors could cause actual results to differ materially from those indicated by the forward-looking statements made in this press release. Any such forward-looking statements represent management's estimates as of the date of this press release. While the Company may elect to update such forward-looking statements at some point in the future, except as required by law, it disclaims any obligation to do so, even if subsequent events cause our views to change. These forward-looking statements should not be relied upon as representing the Company's views as of any date subsequent to the date of this press release.
本新聞稿包括《1995年私人證券訴訟改革法案》(PSLRA)範圍內的“前瞻性聲明”。本新聞稿中的前瞻性聲明包括但不限於公司有關會議演示日期和時間、預計發佈的額外臨床數據時間以及伯曼膚巴與魯扎維ρ治療HCV的潛力的計劃。在本文中使用“期望”、“可能”、“將”、“預計”、“計劃”和類似表達意願的話語旨在識別前瞻性聲明。此外,任何涉及對未來事件或情況的期望、信仰、計劃、投射、目標、表現或其他表徵,包括任何基礎假設的任何陳述或信息,均屬於前瞻性聲明。所有前瞻性聲明均基於公司當前的預期和各種假設。公司認爲存在合理的依據支持其預期和信仰,但它們本質上是不確定的。公司可能無法實現其預期,而其信仰可能證明不正確。根據各種重要因素,實際結果可能會與在本新聞稿中作出的前瞻性聲明所具體描述或暗示的結果有所不同,包括但不限於公司提交給SEC的報告中每個重要因素的信息,包括10-K年度報告、10-Q季度報告、8-K年度報告和其他備案文件,可在SEC的網站上www.sec.gov爲之提供參考。這些和其他重要因素可能會導致實際結果與在本新聞稿中提出的前瞻性聲明所表示的有所不同。這種前瞻性聲明僅代表管理層在本新聞稿發佈之日的估計值。儘管公司可能會在將來某個時候選擇更新此類前瞻性聲明,但在法律要求之外,它不承擔更新的義務,即使隨後的事件導致我們的看法發生變化。這些前瞻性聲明不應視爲代表公司在本新聞稿之後任何日期的觀點。
Contacts
聯繫方式
Jonae Barnes
SVP, Investor Relations and Corporate Communications
617-818-2985
Barnes.jonae@ateapharma.com
Jonae Barnes
投資者關係和企業傳播高級副總裁
617-818-2985
Barnes.jonae@ateapharma.com
Will O'Connor
Precision AQ
212-362-1200
will.oconnor@precisionaq.com
威爾·奧康納
Josh.Rappaport@precisionaq.com
212-362-1200
will.oconnor@precisionaq.com
譯文內容由第三人軟體翻譯。