Media Update: ERS: New Data Highlight Sanofi's Scientific Innovation and Leadership in Immune-mediated Respiratory Diseases
Media Update: ERS: New Data Highlight Sanofi's Scientific Innovation and Leadership in Immune-mediated Respiratory Diseases
Notable presentations include:ERS: New data highlight Sanofi's scientific innovation and leadership in immune-mediated respiratory diseases
ERS:新数据突显赛诺菲安万特在免疫介导的呼吸道疾病中的科学创新和领导地位
- Dupixent presentations of new pooled analyses from the two landmark COPD phase 3 studies, and novel imaging technology insights on airway inflammation in asthma
- Itepekimab phase 2 study oral presentation evaluating the impact on exacerbations in former smokers with COPD
- Additional phase 2 presentations in asthma for rilzabrutinib, a novel oral BTK inhibitor, and lunsekimig, an IL-13/TSLP Nanobody compound
- Dupixent对两个重要COPD三期研究的新汇总分析报告以及关于哮喘气道炎症的新型成像技术的洞见
- Itepekimab二期研究口头报告评估在患有COPD的过去吸烟者中对急性加重的影响
- rilzabrutinib二期哮喘研究以及lunsekimig一种新型口服BTk抑制剂和一种IL-13/TSLP融合物的口服哮喘研究的补充报告
Paris, August 26, 2024. Sanofi will present twenty-four abstracts across approved and pipeline medicines at the European Respiratory Society (ERS) International Congress from September 7th-11th in Vienna, Austria. Presentations will feature clinical and real-world data for Dupixent (dupilumab) and data for investigational therapy itepekimab (in collaboration with Regeneron) demonstrating the potential of targeting specific types of underlying inflammation across chronic obstructive pulmonary disease (COPD) and asthma to improve patient outcomes. Notable data presentations for Sanofi's extensive immunology pipeline include oral presentations for rilzabrutinib, a novel oral BTK inhibitor, evaluating safety and demonstrating efficacy on asthma symptom control, as well as poster presentations for lunsekimig, a novel IL13/TSLP Nanobody compound in asthma, evaluating its impact on type-2 inflammation.
2024年8月26日,赛诺菲安万特将在奥地利维也纳的欧洲呼吸学会(ERS)国际大会上,展示所批准和正在研发的二十四个药物的摘要。报告将重点介绍Dupixent(dupilumab)的临床和实际数据,以及与Regeneron合作的研究性疗法itepekimab的数据,这些数据展示了靶向不同类型潜在炎症在慢阻肺(COPD)和哮喘中的潜力,以改善患者结局。赛诺菲全面的免疫学生产线的重要数据报告包括rilzabrutinib的口头报告,这是一种新型口服BTk抑制剂,评估其对哮喘症状控制的安全性和疗效,以及lunsekimig的海报报告,这是一种新型IL13/TSLP融合物,评估其对2型炎症的影响。
Dietmar Berger, MD, PhD
Chief Medical Officer, Global Head of Development at Sanofi
"Our strong presence at this year's ERS conference highlights our diverse, novel research across inflammatory respiratory conditions, including COPD and asthma. For the first time, we will share pooled analyses from the landmark BOREAS and NOTUS trials that reinforce pivotal data, which led to the first approval of a biologic for COPD in the EU. In addition, we look forward to sharing data for two pipeline molecules, rilzabrutinib, a novel oral BTK inhibitor, and lunsekimig, an IL13/TSLP Nanobody compound, showing their potential in asthma. These data underscore our commitment to progressing science to better serve patients suffering from devastating respiratory diseases."
Dietmar Berger博士
赛诺菲安万特的首席医疗官,全球研发负责人
我们在今年的ERS会议上的强大存在凸显了我们在炎症性呼吸道疾病领域的多样化、创新性的研究成果,包括COPD和哮喘。首次,我们将分享来自具有里程碑意义的BOREAS和NOTUS试验的合并分析结果,这些结果强化了关于在欧盟获批用于COPD的首个生物药物的关键数据。此外,我们期待分享两种正在进行中的新药分子rilzabrutinib和lunsekimig的数据,rilzabrutinib是一种新型口服BTk抑制剂,lunsekimig是一种IL13/TSLP Nanobodycompound,展示了它们在哮喘治疗方面的潜力。这些数据进一步证明了我们致力于推进科学研究,以更好地服务于患有严重呼吸道疾病的患者。
Notable presentations include:
值得注意的演示包括:
Dupixent
Dupixent
Data from new analyses of the BOREAS and NOTUS phase 3 clinical studies in adults with uncontrolled COPD with evidence of type-2 inflammation, and new research from the phase 4 VESTIGE study, a novel imaging study evaluating the effects of Dupixent on airway remodeling measures in certain adults with asthma.
来自BOREAS和NOTUS的三期临床研究在控制不佳且存在2型炎症证据的成年COPD患者的新分析数据以及来自第四期VESTIGE研究的新研究,该研究是一项评估Dupixent对某些成年哮喘患者气道重塑指标影响的新型成像研究。
COPD
COPD
- BOREAS and NOTUS studies: poster presentation with a new pooled analysis of both pivotal studies, including data on exacerbations and lung function.
- BOREAS study: several poster presentations with detailed outcome assessments of Dupixent on daily symptom frequency and severity, the effect on exacerbations and lung function regardless of baseline body mass index, airflow obstruction, dyspnea (shortness of breath), and exercise capacity measures for adults with uncontrolled COPD with evidence of type-2 inflammation (i.e., raised blood eosinophils). Additional Dupixent data of its impact on quality of life, lung function and symptoms in patients who do not exacerbate.
- BOREAS和NOTUS研究:其中一项新的综合分析海报提出,包括对加重和肺功能的数据。
- BOREAS研究:几个海报展示了Dupixent对每日症状频率和严重程度,以及对COPD未受控制的成年人的加重和肺功能的效果,不论基线身体质量指数、气流阻塞、呼吸困难(气喘)和运动能力测量。此外,还有Dupixent对不加重的患者的生活质量、肺功能和症状的影响的额外数据。
Asthma
哮喘
- VESTIGE study: two poster presentations with new data on the impact within four weeks of Dupixent treatment on airway inflammation, volume and flow, and mucus plugging, as well as outcomes for clinical remission at four and 24 weeks of treatment in adults with uncontrolled moderate-to-severe asthma. Additionally, an oral presentation on mucus plugging and volume.
- Real-world data: two poster presentations of real-world outcomes from the EU-ADVANTAGE study, including symptoms and oral corticosteroid use, for Dupixent compared to the IL5 antibodies benralizumab and mepolizumab, or omalizumab, an IgE antibody.
- VESTIGE研究:两个海报展示了Dupixent治疗四周对呼吸道炎症、容积和气流以及粘液堵塞的影响的新数据,以及对未控制的中度至重度哮喘成年人治疗四周和治疗24周的临床缓解结果的口头报告。此外,还有关于粘液堵塞和容积的口头报告。
- 真实世界的数据:EU-ADVANTAGE研究中两个发帖介绍了Dupixent与IL5抗体Benralizumab和Mepolizumab,以及IgE抗体Omalizumab在症状和口服类固醇使用方面的实测结果。
The safety results of these studies were generally consistent with the known safety profile of Dupixent in its approved respiratory conditions.
这些研究的安全性结果与Dupixent在其已批准的呼吸道疾病中已知的安全性概况基本一致。
Respiratory pipeline
Data include new analyses for itepekimab, an IL33 antibody, in COPD, and rilzabrutinib, a novel oral BTK inhibitor, and lunsekimig, a IL13/TSLP Nanobody compound, in asthma.
数据包括COPD中IL33抗体Itepekimab、一种新型口服BTk抑制剂Rilzabrutinib和一种ASThMA中IL13/TSLP Nanobody复合物Lunsekimig的新分析。
COPD
COPD
- itepekimab: an oral presentation with new analyses from a COPD phase 2 study on the impact on exacerbations in former smokers regardless of exacerbation history.
- itepekimab:一个口头报告,涵盖了COPD第2期研究的新分析,重点讨论了在既往吸烟者中,无论发作史如何,对加重症状的影响。
Asthma
哮喘
- rilzabrutinib: two oral presentations on the impact of treatment with rilzabrutinib in improving asthma control in adults with moderate-to-severe asthma, and on the role of BTK inhibition in eosinophilic inflammatory response.
- lunsekimig: two poster presentations on the broader benefits of lunsekimig, an IL-13/TSLP Nanobody compound on type-2 inflammation and the prevalence of elevated fractional exhaled nitric oxide in patients with mild-to-moderate asthma.
- rilzabrutinib:两个口头报告,探讨了使用rilzabrutinib治疗对中重度哮喘成年患者提高哮喘控制的影响,以及BTk抑制在嗜酸性炎症反应中的作用。
- lunsekimig:两个海报展示,介绍了lunsekimig的更广泛益处,作为一种IL-13/TSLP纳米抗体复合物,对于2型炎症的作用,以及对轻中度哮喘患者中气道过氧化亚硝化物的升高率的影响。
Itepekimab, rilzabrutinib and lunsekimig are investigational agents for which safety and efficacy have not been evaluated by any regulatory authority.
Itepekimab、rilzabrutinib和lunsekimig是正在研究的药物,尚未得到任何监管机构的安全性和有效性评估。
Complete list of ERS 2024 presentations:
ERS 2024演示会完整列表:
| Presenting author | Abstract title | Presentation details |
| COPD | ||
| Rabe | Reduction in exacerbations with itepekimab in former smokers with chronic obstructive pulmonary disease (COPD) by prior exacerbation frequency (itepekimab) | OA3645 Oral Presentation Monday, September 9 2:15-3:30 PM CEST |
| Bhatt | Dupilumab Efficacy and Safety in Patients with Moderate-to-Severe COPD with Type 2 Inflammation: Pooled Analysis of BOREAS and NOTUS Trials (dupilumab) | PA4787 Poster Presentation Tuesday, September 10 12:30-2:00 PM CEST |
| Papi | Dupilumab improves respiratory symptoms in patients with moderate-to-severe COPD with type 2 inflammation in phase 3 BOREAS trial (dupilumab) | PA4786 Poster Presentation Tuesday, September 10 12:30-2:00 PM CEST |
| Rabe | Dupilumab improves quality of life in non-exacerbators with moderate-to-severe COPD and type 2 inflammation: phase 3 BOREAS trial (dupilumab) | PA4784 Poster Presentation Tuesday, September 10 12:30-2:00 PM CEST |
| Rabe | Dupilumab improves lung function in non-exacerbators with moderate-to-severe COPD with type 2 inflammation in phase 3 BOREAS trial (dupilumab) | PA4785 Poster Presentation Tuesday, September 10 12:30-2:00 PM CEST |
| Vogelmeier | Dupilumab efficacy in patients with COPD and type 2 inflammation irrespective of mortality risk score (dupilumab) | PA4782 Poster Presentation Tuesday, September 10 12:30-2:00 CEST |
| Asthma | ||
| Bacharier | Clinical remission with dupilumab in children with uncontrolled, moderate-to-severe, type 2 asthma (dupilumab) | RCT3719 Late-Breaking Oral Presentation Monday, September 9 3:30-5:00 PM CEST |
| Pavord | Impact of early transient increase in eosinophils in patients with moderate-to-severe asthma on the long-term efficacy of dupilumab in TRAVERSE (dupilumab) | OA2779 Oral Presentation Monday, September 9 9:30-10:45 AM CEST |
| Porsberg | Dupilumab reduces mucus plugging and volume: phase 4 VESTIGE trial (dupilumab) | OA3649 Oral Presentation Monday, September 9 2:35-3:30 PM CEST |
| Canonica | Effectiveness of dupilumab vs omalizumab in patients with severe asthma – The EU-ADVANTAGE study (dupilumab) | PA2171 Poster Presentation Monday, September 9 8:00-9:30 AM CEST |
| Chan | Characteristics of long-term oral corticosteroid users stratified by blood eosinophil count in the International Severe Asthma Registry (dupilumab) | PA439 Poster Presentation Sunday, September 8 8:00-9:30 AM CEST |
| Chan | Phenotype and biomarkers in patients who initiated biologic therapy stratified by oral corticosteroids use in the International Severe Asthma Registry (dupilumab) | PA438 Poster Presentation Sunday, September 8 8:00-9:30 AM CEST |
| Lugogo | Dupilumab-treated patients with moderate-to-severe asthma are more likely to meet clinical remission criteria: results from the VESTIGE trial (dupilumab) | PA1202 Poster Presentation Sunday, September 8 12:30-2:00 PM CEST |
| Lugogo | Baseline Characteristics of Patients with Asthma Initiating Dupilumab in a Real-World Setting: the RAPID Registry (dupilumab) | PA4484 Poster Presentation Tuesday, September 10 8:00-9:30 AM CEST |
| Papi | Early treatment response to dupilumab on airway inflammation, airway dynamics, and mucus plugging in VESTIGE (dupilumab) | PA3933 Poster Presentation Tuesday, September 10 8:00-9:30 AM CEST |
| Virchow | Real-world effectiveness of dupilumab vs benralizumab and vs mepolizumab in severe asthma: The EU-ADVANTAGE study (dupilumab) | PA2170 Poster Presentation Monday, September 9 8:00-9:30 AM CEST |
| Wechsler | Dupilumab Reduces Exacerbations and FeNO Levels and Improves Asthma Control with Inhaled Corticosteroid Withdrawal: a Phase 2 Study (dupilumab) | PA5371 Poster Presentation Tuesday, September 10 12:30-2:00 PM CEST |
| Wechsler | Dupilumab improves lung function and reduces exacerbations despite withdrawal of inhaled corticosteroids/long-acting beta agonists (dupilumab) | PA1172 Poster Presentation Sunday, September 8 12:30-2:00 PM CEST |
| Shade | Rilzabrutinib, a potent and selective Bruton's tyrosine kinase inhibitor, suppresses reactive oxygen species production and CD11b activation in human eosinophils (rilzabrutinib) | OA1077 Oral Presentation Sunday, September 8 11:40-11:45 AM ET |
| Pavord | Efficacy of High- and Low-Dose Rilzabrutinib On Asthma Control From a Phase 2 Study (rilzabrutinib) | OA2774 Oral presentation Monday, September 9 9:30-10:45 AM CEST |
| Deiteren | Elevated fractional exhaled nitric oxide is prevalent in those with mild-to-moderate asthma with self-reported asthma control (lunsekimig) | PA1222 Poster Presentation Sunday, September 8 12:30-2:00 PM CEST |
| Wang | TSLP AND IL-13 Dual Blockade By Lunsekimig Provides Broader Benefits On Type-2 Inflammation (lunsekimig) | PA4861 Poster Presentation Tuesday, September 10 12:30-2:00 PM CEST |
| Chronic rhinosinusitis with nasal polyps (CRSwNP) | ||
| Heffler | Baseline Characteristics of Patients with Chronic Rhinosinusitis with Nasal Polyps and Coexisting Asthma Initiating Dupilumab in the AROMA Global Registry (dupilumab) | PA425 Poster Presentation Sunday, September 8 8:00-9:30 AM CEST |
| Lee | Initiation of dupilumab led to reduced use of oral corticosteroids (OCS) and other medications over 12 months in patients with chronic rhinosinusitis with nasal polyps (CRSwNP): A US real-world practice study (dupilumab) | PA2177 Poster Presentation Monday, September 9 8:00-9:30 AM CEST |
| 报告人 | 摘要标题 | 展示详情 |
| 慢阻肺 | ||
| 龙 | 以往吸烟者慢性阻塞性肺疾病(COPD)在先前加重频率下使用itepekimab后发作减少(itepekimab) | OA3645 口头演讲 星期一,九月九号 下午2:15-3:30 CEST |
| Bhatt | BOREAS和NOTUS试验中中度至重度COPD患者的dupilumab疗效和安全性:汇总分析 (dupilumab) | PA4787 海报展示 九月十日,星期二 中欧夏令时间12:30-2:00 PM |
| 爸比 | 在3期BOREAS试验中,Dupilumab改善了中度至重度COPD患者的呼吸症状(type 2炎症) | PA4786 海报展示 九月十日,星期二 12:30-2:00 下午 CEST |
| Rabe | Dupilumab改善了非恶化期中度至重度COPD和2型炎症患者的生活质量:第3阶段BOREAS试验(Dupilumab) | PA4784 海报展示 九月十日,星期二 12:30-2:00 下午 CEST |
| Rabe | Dupilumab改善了BOREAS试验中无急性加重的中度至重度COPD并有第2型炎症的肺功能 | PA4785 海报展示 九月十日,星期二 12:30-2:00 Pm CESt |
| Vogelmeier | Dupilumab无视死亡风险评分在COPD患者和第2型炎症中的功效 | PA4782 海报展示 九月十日,星期二 12:30-2:00中欧夏令时 |
| 哮喘 | ||
| 巴沙列 | dupilumab治疗对于控制不佳、中至重度的2型哮喘的儿童患者(dupilumab)可以导致临床缓解。 | RCT3719 晚期口头报告 周一,9月9日 下午3:30-5:00 CEST |
| Pavord | 早期嗜酸性细胞短暂增加对中重度哮喘患者 TRAVERSE(dupilumab)长期效力的影响 | OA2779 口头演讲 星期一,9月9日 上午9:30-10:45 CEST |
| 波尔斯堡 | D化密度在dupilumab减少痰栓和成交量: 4期VESTIGE试验(dupilumab) | OA3649 口头演讲 星期一,9月9日 下午2:35-3:30 CEST |
| Canonica | dupilumab与omalizumab在严重哮喘患者中的有效性-欧洲优势研究(dupilumab) | PA2171 海报展示 星期一,9月9日 上午8:00-9:30 CESt |
| Chan | 在国际严重哮喘注册表中,长期使用口服皮质类固醇的特征,按血嗜酸性粒细胞计数划分(dupilumab) | PA439 海报展示 九月八日,星期日 CEST上午8:00-9:30 |
| Chan | 在国际严重哮喘登记处开始生物治疗的患者中,根据口服类固醇的使用分层,观察表型和生物标志物(Dupilumab) | PA438 海报展示 九月八日,星期日 上午8:00-9:30 中欧夏令时间 |
| Lugogo | Dupilumab治疗的中重度哮喘患者更有可能满足临床缓解标准:来自VESTIGE试验(dupilumab)的结果 | PA1202 海报展示 九月八日,星期日 下午12:30-2:00 中欧夏令时间 |
| Lugogo | 哮喘患者在真实环境中开始使用杜比育单抗的基线特征:RAPID注册表(杜比育单抗) | PA4484 海报展示 九月十日,星期二 8:00-9:30上午中欧夏令时间 |
| Papi | VESTIGE研究中杜比育单抗对气道炎症、气道动力学和粘液充盈的早期治疗反应(杜比育单抗) | PA3933 海报展示 九月十日,星期二 上午8:00-9:30 中欧夏令时间 |
| Virchow | 重度哮喘中度甲型流感疫苗与苯肌醇注射液的实际效果:EU-ADVANTAGE研究(dupilumab) | PA2170 海报展示 周一,9月9日 上午8:00-9:30 CESt |
| Wechsler | Dupilumab通过停用吸入性皮质类固醇来减少哮喘发作和FeNO水平,并改善哮喘控制:一项2期研究(Dupilumab) | PA5371 海报展示 九月十日,星期二 下午12:30-2:00 CESt |
| 韦氏 | Dupilumab在停用吸入型皮质类固醇/长效β2受体激动剂(dupilumab)后改善了肺功能并减少了急性加重。 | PA1172 海报展示 九月八日,星期日 中欧夏令时间12:30-2:00 PM |
| 阴影 | Rilzabrutinib是一种强力且选择性的布鲁顿酪氨酸激酶抑制剂,可以抑制人类嗜酸性粒细胞的活化与产生活性氧自由基(rilzabrutinib) | OA1077口头报告 九月八日,星期日 东部时间11:40-11:45 AM |
| 帕沃德 | 来自第2期研究的高剂量和低剂量Rilzabrutinib对哮喘控制的疗效(rilzabrutinib) | OA2774口头报告 9月9日星期一 上午9:30-10:45(中欧夏令时) |
| Deiteren | 在自我报告的哮喘控制度(lunsekimig)中,轻至中度哮喘患者中普遍存在升高的呼气一氧化氮 | PA1222 海报展示 九月八日,星期日 12:30-2:00下午CESt |
| 王 | Lunsekimig通过TSLP和IL-13双重阻断在第二型炎症上提供更广泛的益处 | PA4861 海报展示 九月十日,星期二 12:30-2:00下午CESt |
| 慢性鼻窦炎伴鼻息肉(CRSwNP) | ||
| 罗盖特全球注册中的患有慢性鼻窦炎合并哮喘并开始使用度磷单抗的患者的基线特征(度磷单抗) | PA425 海报展示 九月八日,星期日 上午8:00-9:30 中欧夏令时间 |
|
| 李 | 在慢性鼻窦炎伴鼻息肉(CRSwNP)患者中,起始使用杜匹单抗能够在12个月内减少口服类固醇(OCS)和其他药物的使用:一项美国实际临床实践研究(杜匹单抗) | PA2177 海报展示 星期一,9月9日 上午8点至9点30分CEST |
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Thomas Kudsk Larsen |+ 44 7545 513 693 | thomas.larsen@sanofi.comthomas.larsen@赛诺菲安万特.com
Alizé Kaisserian |+33 6 47 04 12 11 | alize.kaisserian@sanofi.com
Arnaud Delépine | + 33 6 73 69 36 93 |arnaud.delepine@sanofi.com
Felix Lauscher | + 1 908 612 7239 | felix.lauscher@sanofi.com
Keita Browne | + 1 781 249 1766 | keita.browne@赛诺菲安万特.com
Nathalie Pham | + 33 7 85 93 30 17 | nathalie.pham@sanofi.com
Tarik Elgoutni | + 1 617 710 3587 | tarik.elgoutni@sanofi.com
Thibaud Châtelet | + 33 6 80 80 89 90 | thibaud.chatelet@赛诺菲安万特.com
Sanofi Forward-Looking Statements
This media update contains forward-looking statements as defined in the Private Securities Litigation Reform Act of 1995, as amended. Forward-looking statements are statements that are not historical facts. These statements include projections and estimates regarding the marketing and other potential of the product, or regarding potential future revenues from the product. Forward-looking statements are generally identified by the words "expects", "anticipates", "believes", "intends", "estimates", "plans" and similar expressions. Although Sanofi's management believes that the expectations reflected in such forward-looking statements are reasonable, investors are cautioned that forward-looking information and statements are subject to various risks and uncertainties, many of which are difficult to predict and generally beyond the control of Sanofi, that could cause actual results and developments to differ materially from those expressed in, or implied or projected by, the forward-looking information and statements. These risks and uncertainties include among other things, unexpected regulatory actions or delays, or government regulation generally, that could affect the availability or commercial potential of the product, the fact that product may not be commercially successful, the uncertainties inherent in research and development, including future clinical data and analysis of existing clinical data relating to the product, including post marketing, unexpected safety, quality or manufacturing issues, competition in general, risks associated with intellectual property and any related future litigation and the ultimate outcome of such litigation, and volatile economic and market conditions, and the impact that pandemics or other global crises may have on us, our customers, suppliers, vendors, and other business partners, and the financial condition of any one of them, as well as on our employees and on the global economy as a whole. The risks and uncertainties also include the uncertainties discussed or identified in the public filings with the SEC and the AMF made by Sanofi, including those listed under "Risk Factors" and "Cautionary Statement Regarding Forward-Looking Statements" in Sanofi's annual report on Form 20-F for the year ended December 31, 2023. Other than as required by applicable law, Sanofi does not undertake any obligation to update or revise any forward-looking information or statements.
赛诺菲安万特前瞻性声明
All trademarks mentioned in this media update are the property of the Sanofi group.
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- Media Update