-- Achieved all co-primary endpoints of LS mean reduction in LDL-C on top of maximally tolerated lipid-modifying therapies versus each of placebo, ezetimibe 10 mg, and obicetrapib 10 mg monotherapy at day 84 with statistical significance (p<0.001) --
-- Obicetrapib and ezetimibe fixed-dose combination observed to lower LDL-C by approximately 50% at day 84, compared to placebo, with over 70% of patients achieving LDL-C levels below 55 mg/dL --
-- Data supports global regulatory filings of the obicetrapib 10 mg and ezetimibe 10 mg fixed-dose combination --
-- Observed to be well tolerated with safety results in line with prior studies --
-- NewAmsterdam to host conference call today at 8:00 a.m. ET --
NAARDEN, The Netherlands and MIAMI, Nov. 20, 2024 (GLOBE NEWSWIRE) -- NewAmsterdam Pharma Company N.V. (Nasdaq: NAMS or "NewAmsterdam" or the "Company"), a late-stage, clinical biopharmaceutical company developing oral, non-statin medicines for patients at risk of cardiovascular disease ("CVD") with elevated low-density lipoprotein cholesterol ("LDL-C"), for whom existing therapies are not sufficiently effective or well tolerated, today announced positive topline data from the Company's Phase 3 TANDEM clinical trial (NCT06005597). TANDEM will support global regulatory filings for the 10 mg obicetrapib and 10 mg ezetimibe fixed-dose combination in adult patients with heterozygous familial hypercholesterolemia ("HeFH") and/or atherosclerotic cardiovascular disease ("ASCVD") or multiple ASCVD risk factors, whose LDL-C is not adequately controlled, despite being on maximally tolerated lipid-lowering therapy.
The co-primary endpoints were percent change from baseline in LDL-C of the fixed-dose combination compared to each monotherapy arm after 84 days and obicetrapib 10 mg compared to placebo after day 84. Secondary endpoints incorporated percent changes from baseline in other biomarkers, including lipoprotein(a), non-high-density lipoprotein cholesterol and apolipoprotein B.
The TANDEM trial met all co-primary endpoints, including the obicetrapib-ezetimibe fixed dose combination achieving an LS mean reduction of 48.6% (p < 0.0001) compared to placebo at day 84. The observed reductions in all co-primary endpoints are summarized below.
LDL-C percentage change:
| | Ezetimibe
(n=101) | Obicetrapib
(n=102) | Obicetrapib and
Ezetimibe FDC
(n=102) |
| Day 84 – from placebo | | | |
| Mean % | -23.3 | -35.5 | -52.2 |
| Median % | -22.6 | -37.2 | -54.0 |
| LS mean % | -20.7 | -31.9 | -48.6 |
| Comparison to pbo | - | (p<0.0001) | (p<0.0001) |
| Comparison to eze 10 mg | - | - | (p<0.0001) |
| Comparison to obi 10 mg | - | - | (p=0.0007) |
"Millions of people across the world are impacted by cardiovascular disease and, despite lifestyle modifications and current treatment options, a substantial portion of those living with ASCVD and/or HeFH fail to meet their individual LDL-C goals," said John Kastelein, M.D., Ph.D., FESC, Chief Scientific Officer of NewAmsterdam. "We observed clinically meaningful and statistically significant LDL-C lowering, with safety results consistent with our previous clinical studies, in a once daily oral tablet of the fixed-dose combination of obicetrapib and ezetimibe. We believe these data highlight a potential new treatment that, if approved, could expand options for physicians and contribute to improved patient care for those impacted by CVD."
In the trial, the fixed-dose combination of obicetrapib and ezetimibe was observed to be well tolerated, with safety results comparable to placebo. The below table summarizes study drug-related treatment emergent adverse events ("TEAEs") and study drug-related treatment emergent serious adverse events ("TESAEs").
| | Placebo
(n=102) | Ezetimibe
(n=101) | Obicetrapib
(n=102) | Obicetrapib /
Ezetimibe FDC
(n=102) |
| Any study drug-related TEAEs | 4 (3.9%) | 3 (3.0%) | 7 (6.9%) | 3 (2.9%) |
Any study drug-related TEAEs leading
to discontinuation of study drug | 2 (2.0%) | 1 (1.0%) | 6 (5.9%) | 1 (1.0%) |
| Any study drug related TESAEs | 0 (0.0%) | 0 (0.0%) | 0 (0.0%) | 0 (0.0%) |
"Today's announcement represents a major achievement in our mission to bring a new and effective therapy to millions of patients struggling with dyslipidemia," said Michael Davidson, M.D., Chief Executive Officer of NewAmsterdam Pharma. "We expect these promising results will support our regulatory filings globally and they reinforce our belief that, if approved, obicetrapib in combination with ezetimibe will potentially offer a simple, once-daily treatment capable of significantly reducing LDL-C and improving cardiovascular outcomes. After the BROOKLYN trial's successful readout in July and the additional safety and efficacy data released this week, we strongly believe that obicetrapib as a monotherapy or in a fixed-dose combination with ezetimibe has the potential to help patients achieve LDL-C targets."
"Despite the availability of established therapies, a considerable number of patients still fail to achieve target LDL-C levels, leaving them vulnerable to future cardiovascular events. These top-line results advance our understanding of potential new tools for lipid management for patients at high risk of cardiovascular disease," said Ashish Sarraju, M.D., Cardiovascular Medicine, Cleveland Clinic.
NewAmsterdam plans to present additional results from TANDEM at an upcoming medical conference and to publish the data in a major medical journal.
Design of the Pivotal Phase 3 TANDEM Clinical Trial
The pivotal, Phase 3, randomized, double-blind, four-arm, placebo-controlled multicenter study evaluated the effect of 10 mg obicetrapib and 10 mg ezetimibe as a fixed-dose combination on LDL-C levels, compared to both ezetimibe 10 mg and obicetrapib 10 mg monotherapy and to placebo. The study was conducted at sites across the United States, and a total of 407 patients with HeFH and/or ASCVD or ASCVD risk equivalents, who had a baseline LDL-C of at least 70 mg/dL, were randomized 1:1:1:1 to receive 10 mg obicetrapib and 10 mg ezetimibe fixed-dose combination, 10 mg obicetrapib, 10 mg ezetimibe or placebo for an 84-day treatment period. The mean baseline LDL-C for enrolled patients in the obicetrapib-ezetimibe arm was 97 mg/dL despite high intensity statin use reported by approximately 74% of patients during screening. In addition to measuring the co-primary endpoints and secondary endpoints, the trial also evaluated the safety and tolerability profile of obicetrapib.
Conference Call and Webcast Information
NewAmsterdam will host a live webcast and conference call to review the topline results from TANDEM at 8:00 a.m. ET today. To access the live webcast, participants may register here. The live webcast will be available under the "Events" section of the Investor Relations page of the NewAmsterdam website at ir.newamsterdampharma.com
To participate via telephone, please register in advance here. Upon registration, all telephone participants will receive a confirmation email detailing how to join the conference call, including the dial-in number along with a unique passcode and registrant ID that can be used to access the call. While not required, it is recommended that participants join the call ten minutes prior to the scheduled start. An archived replay of the webcast will be available on NewAmsterdam's website.
About NewAmsterdam's Global Pivotal Phase 3 Program
NewAmsterdam's global, pivotal Phase 3 clinical development program consists of four studies in over 12,250 patients, three for obicetrapib monotherapy and one for a fixed-dose combination of obicetrapib and ezetimibe, including TANDEM. Details on the Company's pivotal Phase 3 programs are as follows:
- BROOKLYN evaluated obicetrapib in patients with HeFH, whose LDL-C is not adequately controlled, despite being on maximally tolerated lipid-lowering therapy. NewAmsterdam reported topline data in the third quarter of 2024 and presented additional data at the American Heart Association Scientific Sessions 2024 in November.
- TANDEM evaluated obicetrapib as part of a fixed-dose combination tablet with ezetimibe, a non-statin oral LDL-lowering therapy, in patients with established ASCVD or multiple risk factors for ASCVD and/or HeFH, whose LDL-C is not adequately controlled despite being on maximally tolerated lipid-lowering therapy. NewAmsterdam completed enrollment of over 400 patients in July 2024 and reported topline data in November 2024.
- BROADWAY is evaluating obicetrapib in adult patients with established ASCVD and/or HeFH, whose LDL-C is not adequately controlled, despite being on maximally tolerated lipid-lowering therapy. NewAmsterdam completed enrollment of over 2,500 patients in July 2023 and expects to report topline data in the fourth quarter of 2024.
- PREVAIL is a cardiovascular outcomes trial evaluating obicetrapib in patients with a history of ASCVD, whose LDL-C is not adequately controlled, despite being on maximally tolerated lipid-lowering therapy. NewAmsterdam completed enrollment of over 9,500 patients in April 2024.
About Obicetrapib
Obicetrapib is a novel, oral, low-dose CETP inhibitor that NewAmsterdam is developing to overcome the limitations of current LDL-lowering treatments. In each of the Company's Phase 2 trials, ROSE2, TULIP, ROSE, and OCEAN, as well as the Company's Phase 3 BROOKLYN and TANDEM trials, evaluating obicetrapib as monotherapy or combination therapy, the Company observed statistically significant LDL-lowering combined with a side effect profile similar to that of placebo. The Company is conducting an additional Phase 3 pivotal trial BROADWAY, to evaluate obicetrapib as a monotherapy used as an adjunct to maximally tolerated lipid-lowering therapies to provide additional LDL-lowering for CVD patients. The Company began enrolling patients in BROADWAY in January 2022 and completed enrollment of BROADWAY in July 2023. The Company also commenced the Phase 3 PREVAIL cardiovascular outcomes trial in March 2022, which is designed to assess the potential of obicetrapib to reduce occurrences of major adverse cardiovascular events, including cardiovascular death, non-fatal myocardial infarction, non-fatal stroke and non-elective coronary revascularization. NewAmsterdam completed enrollment of PREVAIL in April 2024 and randomized over 9,500 patients. Commercialization rights of obicetrapib in Europe, either as a monotherapy or as part of a fixed dose combination with ezetimibe, for cardiovascular diseases have been exclusively granted to the Menarini Group, an Italy-based, leading international pharmaceutical and diagnostics company.
About NewAmsterdam
NewAmsterdam Pharma (Nasdaq: NAMS) is a late-stage biopharmaceutical company whose mission is to improve patient care in populations with metabolic diseases where currently approved therapies have not been adequate or well tolerated. We seek to fill a significant unmet need for a safe, well-tolerated and convenient LDL-lowering therapy. In multiple phase 3 studies, NewAmsterdam is investigating obicetrapib, an oral, low-dose and once-daily CETP inhibitor, alone or as a fixed-dose combination with ezetimibe, as LDL-C lowering therapies to be used as an adjunct to statin therapy for patients at risk of CVD with elevated LDL-C, for whom existing therapies are not sufficiently effective or well tolerated.
Forward-Looking Statements
Certain statements included in this document that are not historical facts are forward-looking statements for purposes of the safe harbor provisions under the United States Private Securities Litigation Reform Act of 1995. Forward-looking statements generally are accompanied by words such as "believe," "may," "will," "estimate," "continue," "anticipate," "intend," "expect," "should," "would," "plan," "predict," "potential," "seem," "seek," "future," "outlook" and similar expressions that predict or indicate future events or trends or that are not statements of historical matters. These forward-looking statements include, but are not limited to, statements regarding the Company's business and strategic plans, the Company's commercial opportunity, the therapeutic and curative potential of the Company's product candidate, the Company's clinical trials and the timing for enrolling patients, the timing and forums for announcing data, the achievement and timing of regulatory approvals, and plans for commercialization. These statements are based on various assumptions, whether or not identified in this document, and on the current expectations of the Company's management and are not predictions of actual performance. These forward-looking statements are provided for illustrative purposes only and are not intended to serve as and must not be relied on as a guarantee, an assurance, a prediction, or a definitive statement of fact or probability. Actual events and circumstances are difficult or impossible to predict and may differ from assumptions. Many actual events and circumstances are beyond the control of the Company. These forward-looking statements are subject to a number of risks and uncertainties, including changes in domestic and foreign business, market, financial, political, and legal conditions; risks related to the approval of the Company's product candidate and the timing of expected regulatory and business milestones, including potential commercialization; ability to negotiate definitive contractual arrangements with potential customers; the impact of competitive product candidates; ability to obtain sufficient supply of materials; global economic and political conditions, including the Russia-Ukraine and Israel-Hamas conflict; the effects of competition on the Company's future business; and those factors described in the Company's public filings with the Securities Exchange Commission. Additional risks related to the Company's business include, but are not limited to: uncertainty regarding outcomes of the Company's ongoing clinical trials, particularly as they relate to regulatory review and potential approval for its product candidate; risks associated with the Company's efforts to commercialize a product candidate; the Company's ability to negotiate and enter into definitive agreements on favorable terms, if at all; the impact of competing product candidates on the Company's business; intellectual property related claims; the Company's ability to attract and retain qualified personnel; ability to continue to source the raw materials for its product candidate. If any of these risks materialize or the Company's assumptions prove incorrect, actual results could differ materially from the results implied by these forward-looking statements. There may be additional risks that the Company does not presently know or that the Company currently believes are immaterial that could also cause actual results to differ from those contained in the forward-looking statements. In addition, forward-looking statements reflect the Company's expectations, plans, or forecasts of future events and views as of the date of this document and are qualified in their entirety by reference to the cautionary statements herein. The Company anticipates that subsequent events and developments may cause the Company's assessments to change. These forward-looking statements should not be relied upon as representing the Company's assessment as of any date subsequent to the date of this communication. Accordingly, undue reliance should not be placed upon the forward-looking statements. Neither the Company nor any of its affiliates undertakes any obligation to update these forward-looking statements, except as may be required by law.
Company Contact
Matthew Philippe
P: 1-917-882-7512
matthew.philippe@newamsterdampharma.com
Media Contact
Spectrum Science on behalf of NewAmsterdam
Bryan Blatstein
P: 1-917-714-2609
bblatstein@spectrumscience.com
Investor Contact
Precision AQ on behalf of NewAmsterdam
Austin Murtagh
P: 1-212-698-8696
austin.murtagh@precisionaq.com
-- 在第84天,最大耐受脂质修饰治疗基础上,达成所有主要终点,LS均值LDL-C降低与安慰剂、依泽替米贝10毫克及obicetrapib 10毫克单药治疗比较,统计学显著性(p<0.001) --
-- 与安慰剂相比,obitrapib和依泽替米贝固定剂量组合在第84天观察到LDL-C降低约50%,超过70%的患者LDL-C水平低于55 mg/dL --
-- 数据支持obitrapib 10毫克和依泽替米贝10毫克固定剂量组合的全球监管申请 --
-- 观察到良好耐受,安全性结果与之前的研究一致 --
-- NewAmsterdam 今天上午8:00(东部时间)召开电话会议 --
荷兰纳尔登和美国迈阿密,2024年11月20日(全球新闻稿) -- NewAmsterdam制药公司N.V.(纳斯达克代码:NAMS或“NewAmsterdam”或“公司”),是一家处于后期阶段的临床生物制药公司,开发针对风险患有心血管疾病(“CVD”)并且低密度脂蛋白胆固醇(“LDL-C”)升高的患者的口服非他汀药物,对于这些患者现有疗法效果不佳或耐受性不佳,今天宣布了公司III期TANDEm临床试验(NCT06005597)的积极顶线数据。TANDEm将支持全球监管文件的提交,涉及10毫克obicetrapib和10毫克ezetimibe的固定剂量组合,适用于具有杂合型家族性高胆固醇血症(“HeFH”)和/或动脉粥样硬化性心血管疾病(“ASCVD”)或多个ASCVD风险因素的成年患者,尽管接受了最大耐受的降脂治疗,其LDL-C仍未得到充分控制。
共同主要终点是固定剂量组合在基线后84天与每个单药治疗组相比的LDL-C百分比变化,以及与安慰剂在第84天相比的obicetrapib 10毫克。次要终点包括其他生物标志物的基线变化百分比,包括脂蛋白(a)、非高密度脂蛋白胆固醇和载脂蛋白b。
TANDEm试验满足所有共同主要终点,包括obicetrapib-ezetimibe固定剂量组合在第84天相比安慰剂实现了48.6%的LS平均减少(p < 0.0001)。所有共同主要终点的观察减少总结如下。
LDL-C百分比变化:
| | 依泽替米
(n=101) | Obicetrapib
(n=102) | Obicetrapib和
依折麦布复方制剂
(n=102) |
| 第84天 - 来自安慰剂 | | | |
| 平均百分比 | -23.3 | -35.5 | -52.2 |
| 中位数百分比 | -22.6 | -37.2 | -54.0 |
| LS均值百分比 | -20.7 | -31.9 | -48.6 |
| 与pbo的比较 | - | (p<0.0001) | (p<0.0001) |
| 与eze 10毫克的比较 | - | - | (p<0.0001) |
| 与obi 10 mg的比较 | - | - | (p=0.0007) |
"全球有数百万人受到心血管疾病的影响,尽管进行生活方式的调整和现有的治疗方案,仍有相当一部分患有动脉粥样硬化性心血管疾病和/或家族性高胆固醇血症的人未能达到他们的个体LDL-C目标," 新阿姆斯特丹的首席科学官John Kastelein万.D., Ph.D., FESC表示。 "我们观察到具有临床意义且统计显著的LDL-C降低,安全性结果与我们之前的临床研究一致,这种固定剂量组合的每日一次口服片剂包含obicetrapib和ezetimibe。我们相信这些数据突出了潜在的新治疗方法,如果获得批准,可能会扩展医生的选择,并有助于改善受到心血管疾病影响的患者的护理。"
在试验中,obicetrapib和泽特米布的固定剂量联合疗法被认为耐受良好,安全性结果与安慰剂相当。以下表格总结了研究药物相关的治疗出现的不良事件("TEAEs")和研究药物相关的治疗出现的严重不良事件("TESAEs")。
| | 安慰剂
(n=102) | 依泽替米
(n=101) | Obicetrapib
(n=102) | Obicetrapib /
依折麦布复方制剂
(n=102) |
| 任何研究药物相关的不良事件 | 4 (3.9%) | 3 (3.0%) | 7 (6.9%) | 3 (2.9%) |
任何与药物相关的TEAE导致
停止使用研究药物 | 2 (2.0%) | 1 (1.0%) | 6 (5.9%) | 1 (1.0%) |
| 任何与研究药物相关的重大不良事件(TESAEs) | 0 (0.0%) | 0 (0.0%) | 0 (0.0%) | 0 (0.0%) |
"今天的公告代表了我们在将新型有效疗法带给数百万面临高脂血症的患者的使命中的重大成就," NewAmsterdam Pharma的首席执行官Michael Davidson万.D.表示。"我们预计这些有希望的结果将支持我们在全球的监管申请,并强化我们相信,如果获得批准,obicetrapib与ezetimibe联合使用将提供一种简单的每日一次治疗,能够显著降低LDL-C并改善心血管结果。在BROOKLYN试验于七月成功发布结果后,以及本周发布的额外安全性和有效性数据,我们坚信obicetrapib作为单一疗法或与ezetimibe固定剂量组合具有帮助患者达到LDL-C目标的潜力。"
“尽管已有成熟的治疗方案,仍有相当数量的患者未能达到目标LDL-C水平,这使他们在未来面临心血管事件的风险。这些关键结果推动了我们对高风险心血管疾病患者脂质管理潜在新工具的理解,”克利夫兰诊所心血管医学的Ashish Sarraju万.D.说道。
新阿姆斯特丹计划在即将举行的医疗会议上进一步展示TANDEm的结果,并将在主要医疗期刊上发表这些数据。
关键3期TANDEm临床试验设计
该关键的3期随机、双盲、四组、安慰剂对照多中心研究评估了10毫克obicetrapib和10毫克ezetimibe作为固定剂量组合对LDL-C水平的影响,比较了标准治疗下10毫克ezetimibe和10毫克obicetrapib的单药疗法以及安慰剂。该研究在美国各地进行,共有407名具有HeFH和/或ASCVD或ASCVD风险等效的患者,基线LDL-C至少为70毫克/分升,按照1:1:1:1的比例随机分配接受10毫克obicetrapib和10毫克ezetimibe固定剂量组合、10毫克obicetrapib、10毫克ezetimibe或安慰剂,治疗周期为84天。在入组患者中,obicetrapib-ezetimibe组的平均基线LDL-C为97毫克/分升,尽管在筛查过程中约74%的患者报告使用了高强度的他汀类药物。除了测量共同主要终点和次要终点外,该试验还评估了obicetrapib的安全性和耐受性。
电话会议和网络直播信息
NewAmsterdam将于今天东部时间上午8:00举行直播网络研讨会和电话会议,以回顾TANDEm的主要结果。要访问直播网络研讨会,参与者可以注册 这里。直播网络研讨会将在NewAmsterdam网站的投资者关系页面的“事件”部分提供 ir.newamsterdampharma.com
要通过电话参与,请提前注册 这里注册后,所有电话参与者将收到一封确认电子邮件,详细说明如何加入电话会议,包括拨入号码、唯一的密码和可用于访问电话的注册ID。尽管不是必需的,但建议参与者在预定开始前十分钟加入电话。网络研讨会的归档重播将在NewAmsterdam的网站上提供。
关于NewAmsterdam的全球关键性第三阶段项目
NewAmsterdam的全球关键第III期临床开发项目包括对超过12250名患者的四项研究,其中三项为obicetrapib单药治疗,一项为obicetrapib与依折麦布的固定剂量组合,包括TANDEm。有关公司关键第III期项目的详细信息如下:
- 布鲁克林(BROOKLYN)评估了在最大耐受的降脂治疗下,LDL-C无法得到充分控制的家族性高胆固醇血症患者中的obicetrapib。NewAmsterdam在2024年第三季度报告了顶线数据,并在2024年11月的美国心脏协会科学会议上展示了更多数据。
- TANDEm评估了obicetrapib作为与ezetimibe的固定剂量联合片剂的一部分,ezetimibe是一种非统计的口服降低LDL的疗法,适用于已确诊ASCVD或有多重ASCVD风险因素和/或遗传性高胆固醇血症(HeFH)患者,这些患者在最大耐受的降脂治疗下LDL-C仍未得到充分控制。NewAmsterdam在2024年7月完成了超过400名患者的入组,并在2024年11月报告了顶线数据。
- BROADWAY正在评估在最大耐受的降脂治疗下,LDL-C未得到充分控制的确诊ASCVD和/或HeFH成年患者中的obicetrapib。NewAmsterdam在2023年7月完成了超过2500名患者的入组,并预计将在2024年第四季度报告顶线数据。
- PREVAIL是一个心血管结果试验,评估在最大耐受的降脂治疗下,LDL-C未得到充分控制且有ASCVD病史的患者中的obicetrapib。NewAmsterdam在2024年4月完成了超过9500名患者的入组。
关于Obicetrapib
Obicetrapib是一种新型的口服低剂量CETP抑制剂,NewAmsterdam正在开发,以克服现有LDL降低治疗的局限性。在公司的每个2期试验ROSE2、TULIP、ROSE和OCEAN中,以及公司的3期BROOKLYN和TANDEm试验中,评估obicetrapib作为单一疗法或联合疗法,公司观察到显著降低LDL,并且副作用与安慰剂类似。公司正在进行一项额外的3期关键试验BROADWAY,以评估obicetrapib作为单一疗法用于最大耐受的降脂疗法的辅助,以为心血管疾病患者提供额外的LDL降低。公司于2022年1月开始在BROADWAY入组患者,并于2023年7月完成BROADWAY的入组。公司还于2022年3月开始了3期PREVAIL心血管结果试验,旨在评估obicetrapib减少重大不良心血管事件发生的潜力,包括心血管死亡、非致命性心肌梗死、非致命性中风和非选择性冠状再血管化。NewAmsterdam在2024年4月完成了PREVAIL的入组,并随机选择了超过9500名患者。obicetrapib在欧洲的商业化权利,作为单一疗法或与ezetimibe固定剂量联合用于心血管疾病,已独家授予意大利领先的国际药品和诊断公司Menarini Group。
关于新阿姆斯特丹,新阿姆斯特丹制药公司(NASDAQ:NAMS)是一家晚期的生物制药公司,其使命是改善代谢疾病患者的医疗护理,而当前已批准的治疗方法并不足够或耐受性不佳。我们寻求填补一个很大的需求,即需要一种安全、耐受、方便的降低低密度脂蛋白胆固醇的治疗方法。在多个3期研究中,新阿姆斯特丹正在研究obicetrapib,一种口服的、低剂量的、每日一次的CETP抑制剂,单独或与依他酸替代治疗联合使用,作为LDL-C降低疗法,用于心血管疾病风险患者,其LDL-C升高,现有治疗方法疗效不足或耐受性不佳。
纽约荷兰医药(纳斯达克:NAMS)是一家处于晚期的生物制药公司,旨在改善代谢性疾病人群的患者护理,目前批准的治疗方法并不足够有效或耐受。我们致力于填补一项重大未满足需要,即提供安全、耐受良好且便捷的降低低密度脂蛋白(LDL)药物疗法。在多个3期研究中,纽约荷兰正在研究obicetrapib,作为一种口服、低剂量、每日一次的CETP抑制剂,或与依非韦伯固定剂量组合一起使用,作为降低LDL-C疗法,用作降低患有心血管疾病风险的患者的辅助他汀治疗,对于那些现有疗法并不足够有效或耐受的患者。
前瞻性声明
本文件中包含的某些声明不属于历史事实,而是根据1995年美国私人证券诉讼改革法案安全港条款的前瞻性声明。前瞻性声明通常伴随着诸如“相信”、“可能”、“将会”、“估计”、“继续”、“预期”、“打算”、“期望”、“应该”、“会”、“计划”、“预测”、“潜在”、“似乎”、“寻求”、“未来”、“展望”等词汇,以及其他类似表达,这些词汇预测或指示未来事件或趋势,或不是关于历史事项的陈述。这些前瞻性声明包括但不限于关于公司的业务和战略计划、公司的商业机会、公司产品候选的治疗和治愈潜力、公司的临床试验及患者入组的时间、数据公布的时间和形式、监管批准的取得和时间,以及商业化的计划。这些陈述是基于各种假设,无论本文件中是否已明确列出,并基于公司管理层的当前预期,并不是对实际表现的预测。这些前瞻性声明仅用于说明目的,并不打算作为保证、保证、预测或确定的事实或可能性的陈述。实际事件和情况很难或不可能预测,并可能与假设有所不同。许多实际事件和情况超出了公司的控制范围。这些前瞻性声明受若干风险和不确定性的影响,包括国内和国际商业、市场、金融、政治和法律条件的变化;与公司产品候选的批准及预期的监管和业务里程碑的时间有关的风险,包括潜在的商业化;与潜在客户达成确定性合同的能力;竞争性产品候选对公司的影响;获得足够的原材料供应的能力;全球经济和政治状况,包括俄乌和以色列-哈马斯冲突;竞争对公司未来业务的影响;以及在公司向证券交易委员会的公共文件中描述的那些因素。与公司业务相关的其他风险包括但不限于:对公司正在进行的临床试验结果的未知性,特别是这些结果与监管审查和产品候选的潜在批准有关;与公司努力实现产品候选商业化相关的风险;公司与潜在客户谈判并达成有利条件的确定性协议的能力,如果可以;竞争性产品候选对公司业务的影响;与知识产权相关的索赔;公司吸引和留住合格人员的能力;继续为其产品候选获取原材料的能力。如果这些风险中的任何一个变为现实或公司的假设证明不正确,实际结果可能与这些前瞻性声明所暗示的结果有重大差异。可能还有其他公司目前不知道的或公司认为不重要的额外风险,这也可能导致实际结果与前瞻性声明中的结果不同。此外,前瞻性声明反映了公司对此文件日期的未来事件和观点的预期、计划或预测,并完全由本文件中的警示声明所限定。公司预计随后发生的事件和发展可能会导致公司的评估发生变化。这些前瞻性声明不应依赖于作为公司在本沟通日期之后的任何日期的评估。因此,不应对前瞻性声明给予过度依赖。公司或其任何附属公司没有任何更新这些前瞻性声明的义务,除非法律要求。
公司联系
Marcia Novero
Innodata Inc.
Mnovero@innodata.com
(201) 371-8015
Matthew Philippe
电话:1-917-882-7512
电子邮件:matthew.philippe@newamsterdampharma.com
媒体联系
NewAmsterdam的Spectrum Science代表
Bryan Blatstein
P: 1-917-714-2609
bblatstein@spectrumscience.com
投资者联系人
Precision AQ代表NewAmsterdam
Austin Murtagh
P: 1-212-698-8696
austin.murtagh@precisionaq.com
