Media Update: New Data Presented at ATS Demonstrate Sanofi's Leadership in Advancing Potential New Therapies for Patients With Immune-mediated Respiratory Diseases
Media Update: New Data Presented at ATS Demonstrate Sanofi's Leadership in Advancing Potential New Therapies for Patients With Immune-mediated Respiratory Diseases
New data presented at ATS demonstrate Sanofi's leadership in advancing potential new therapies for patients with immune-mediated respiratory diseases
ATS上公佈的新數據表明,賽諾菲在爲免疫介導的呼吸系統疾病患者推進潛在新療法方面處於領先地位
- Late-breaking data from the landmark NOTUS and BOREAS phase 3 studies support Dupixent's role as a potential first-in-class biologic treatment for certain adult patients with uncontrolled COPD with type 2 inflammation
- New findings from BOREAS study evaluate the role of biomarkers in predicting improvement in exacerbations and other responses to treatment
- First presentation of phase 2b results for rilzabrutinib in asthma which forms the basis for a phase 3 program
- 來自具有里程碑意義的NOTUS和BOREAS三期研究的最新數據支持了Dupixent作爲某些2型炎症不受控制的慢性阻塞性肺病成年患者的潛在首創生物治療的作用
- BOREAS研究的新發現評估了生物標誌物在預測惡化和其他治療反應改善方面的作用
- 首次公佈利扎布替尼治療哮喘的2b期結果,該結果構成了3期計劃的基礎
Paris, April 26, 2024. Twenty-five abstracts across approved and investigational medicines will be presented at this year's American Thoracic Society (ATS) International Conference taking place from May 17-22 in San Diego. Oral presentations will be given on data for Dupixent (dupilumab), in partnership with Regeneron, evaluating its potential as a treatment for patients with chronic obstructive pulmonary disease (COPD) from two landmark phase 3 studies. Notable data presentations for Sanofi's immunology pipeline include the first presentation of phase 2b asthma data for rilzabrutinib, a novel oral BTK inhibitor, and an oral presentation for lunsekimig, a novel IL-13/TSLP Nanobody VHH, currently in phase 2b development for asthma.
巴黎,2024年4月26日。今年5月17日至22日在聖地亞哥舉行的美國胸科學會(ATS)國際會議上,將發佈25份有關已批准和在研藥物的摘要。將就Dupixent的數據進行口頭陳述 (dupilumab)與Regeneron合作,從兩項具有里程碑意義的3期研究中評估了其治療慢性阻塞性肺病(COPD)患者的潛力。賽諾菲免疫學產品線的重要數據展示包括首次公佈新型口服BTK抑制劑利扎布替尼的2b期哮喘數據,以及新型IL-13/TSLP納米體lunsekimig的口頭陳述 VHH,目前處於哮喘的2b期開發階段。
Naimish Patel, M.D.
Global Head of Development, Immunology and Inflammation at Sanofi
"Our robust presence at this year's ATS conference showcases our novel research across inflammatory respiratory conditions, including COPD and asthma. The results from the pivotal NOTUS and BOREAS phase 3 studies for Dupixent further deepen our understanding of the role that type 2 inflammation plays in COPD and underscore the potential for Dupixent to be the first biologic approved for the treatment of COPD. We're also excited to present new data for our two pipeline molecules, rilzabrutinib, an oral BTKi, and lunsekimig, our IL-13/TSLP Nanobody VHH, showing their first- and best-in-class potential in asthma. Our collective data at the meeting underscores our commitment and progress to improving the lives of patients suffering from devastating respiratory diseases."
Dupixent
Notable presentations include new findings from the pivotal phase 3 Dupixent COPD program (NOTUS and BOREAS studies), which showed significant reduction in COPD exacerbations and improvements in lung function. Additionally, research from the VESTIGE phase 4 study, a novel imaging study evaluating the effects of Dupixent on lung function in adult patients with uncontrolled moderate-to-severe asthma, will be featured as a late-breaking oral presentation. Lastly, multiple poster presentations demonstrate the impact of Dupixent on asthma.
奈米什·帕特爾,醫學博士
賽諾菲開發、免疫學和炎症全球主管
“我們在今年的ATS會議上的強大參與展示了我們對炎症性呼吸系統疾病(包括慢性阻塞性肺病和哮喘)的新研究。Dupixent的關鍵NOTUS和BOREAS三期研究的結果進一步加深了我們對2型炎症在慢性阻塞性肺病中的作用的理解,也凸顯了Dupixent有可能成爲第一種獲准用於治療慢性阻塞性肺病的生物製劑。我們還很高興爲我們的兩種管道分子,即口服btKi的rilzabrutinib和我們的IL-13/TSLP納米體VHHlunsekimig提供新的數據,顯示出它們在哮喘領域的首創和同類最佳潛力。我們在會議上的集體數據凸顯了我們在改善患有毀滅性呼吸系統疾病的患者生活方面的承諾和進展。”
Dupixent
值得注意的演示包括關鍵的3期Dupixent慢性阻塞性肺病項目(NOTUS和BOREAS研究)的新發現,該項目顯示慢性阻塞性肺病發作顯著減少,肺功能得到改善。此外,VESTIGE 4期研究是一項新的影像學研究,旨在評估Dupixent對未控制的中度至重度哮喘成年患者肺功能的影響,該研究將作爲最新口頭陳述進行介紹。最後,多張海報展示了Dupixent對哮喘的影響。
Clinical data in COPD
慢性阻塞性肺病的臨床數據
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NOTUS study: detailed efficacy and safety results from the NOTUS phase 3 study evaluating Dupixent in patients with uncontrolled COPD and evidence of type 2 inflammation will be featured in a late-breaking oral presentation. Positive topline data from the study, which showed that Dupixent significantly reduced exacerbations, were previously announced in November 2023.
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BOREAS study: findings across six abstracts from the BOREAS phase 3 study will be shared, including an analysis evaluating the treatment-by-biomarker interaction effects in patients with COPD, which will be presented in an oral abstract session as well as data on lung function.
- NOTUS研究:評估不受控制的慢性阻塞性肺病患者Dupixent的NOTUS 3期研究的詳細療效和安全性結果以及2型炎症的證據,將在最新的口頭陳述中介紹。該研究的積極數據顯示,Dupixent顯著減少了惡化,此前曾出現過 宣佈了 2023 年 11 月。
- BOREAS研究:將分享BOREAS 3期研究的六份摘要的研究結果,包括一項評估慢性阻塞性肺病患者不同治療標誌物相互作用的分析,該分析將在口頭摘要會議上呈現,還將提供有關肺功能的數據。
Clinical data in uncontrolled moderate-to-severe asthma
不受控制的中度至重度哮喘的臨床數據
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VESTIGE clinical study: an oral abstract session will feature data on the effect of Dupixent on airway inflammation and mucus plugging in adults with uncontrolled moderate-to-severe asthma.
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LIBERTY and VOYAGE studies: additional post-hoc analyses will be shared, including evaluating the impact of asthma duration on the efficacy of Dupixent in patients with uncontrolled moderate-to-severe asthma, clinical outcomes in patients with uncontrolled moderate-to-severe asthma who received Dupixent as an add-on to medium-dose inhaled corticosteroid, and the efficacy of Dupixent amongst children aged 6-11 with uncontrolled moderate-to-severe asthma.
- VESTIGE臨床研究:口頭摘要會議將介紹Dupixent對未受控制的中度至重度哮喘的成年人氣道炎症和粘液堵塞的影響的數據。
- LIBERTY和VOYAGE研究:將分享其他事後分析,包括評估哮喘持續時間對不受控制的中度至重度哮喘患者Dupixent療效的影響、接受Dupixent作爲中劑量吸入性皮質類固醇補充劑的未受控制的中度至重度哮喘患者的臨床結果,以及Dupixent對患有未控制的中度至重度哮喘患者的療效,以及Dupixent對未受控制的中度至重度哮喘患者的療效。
The safety results of these studies were generally consistent with the known safety profile of Dupixent in its approved respiratory conditions.
這些研究的安全性結果與Dupixent在其批准的呼吸系統疾病中的已知安全性概況基本一致。
Respiratory pipeline
Presentations include data for investigational compounds rilzabrutinib, an oral BTK inhibitor, and lunsekimig, a new IL-13/TSLP Nanobody VHH, in asthma.
呼吸管道
演示文稿包括治療哮喘的研究化合物利扎布替尼(一種口服BTK抑制劑)和lunsekimig(一種新的IL-13/TSLP納米體VHH)的數據。
- Phase 2b study of rilzabrutinib: a poster presentation will show the impact of treatment with rilzabrutinib on loss of asthma control (LOAC) events, asthma symptoms and quality of life in patients with moderate-to-severe asthma.
- Lunsekimig: an oral presentation will show the impact of lunsekimig on multiple pathological immune cell populations and epithelial cell subpopulations.
- rilzabrutinib的2b期研究:海報展示將展示利扎布替尼治療對中度至重度哮喘患者哮喘控制喪失(LOAC)事件、哮喘症狀和生活質量的影響。
- Lunsekimig:口頭陳述將顯示lunsekimig對多種病理免疫細胞群和上皮細胞亞群的影響。
Complete List of ATS 2024 presentations:
ATS 2024 演示文稿的完整清單:
| Presenting author | Abstract title | Presentation details |
| COPD | ||
| Bafadhel | Dupilumab Does Not Impact Blood Eosinophil Levels in Patients with Moderate-to-Severe COPD and Type 2 Inflammation: From the Phase 3 Boreas Trial | 7498 Poster Presentation Sunday, May 19 9:15 – 11:15 AM PDT |
| Bhatt | A 3-year Descriptive Assessment of Exacerbations and Double/Triple Inhaler Use among chronic obstructive pulmonary disease (COPD) patients in the United States (US) | P584 Poster Presentation Monday, May 20 11:30 AM – 1:15 PM PDT |
| Bhatt | Characterization of Chronic Obstructive Pulmonary Disease (COPD) in the United States | P585 Poster Presentation Monday, May 20 11:30 AM – 1:15 PM PDT |
| Bhatt | Efficacy and Safety of Dupilumab in Patients With Moderate-to-Severe COPD and Type 2 Inflammation: Phase 3 NOTUS Trial | 15018 Oral Presentation Monday, May 20 9:15 – 11:15 AM PDT |
| Bhatt | In the Phase 3 BOREAS Trial, Dupilumab Reduced FeNO Levels Over Time in Patients with Moderate-To-Severe COPD with Type 2 Inflammation | 7547 Poster Presentation Sunday, May 19 9:15 – 11:15 AM PDT |
| Buhl/Vogelmeier | Clinical and Economic Burden of COPD in Patients Poorly Controlled on LABA/LAMA or Inhaled Triple Therapy in Germany - A Retrospective Claims Data Analysis | P583 Poster Presentation Monday, May 20 11:30 AM – 1:15 PM PDT |
| Christenson | Dupilumab Increases the Proportion of Patients With Fractional Exhaled Nitric Oxide Levels <20 ppb Over Time in Patients With Moderate-to-Severe Chronic Obstructive Pulmonary Disease and Type 2 Inflammation: From Phase 3 BOREAS | 7636 Poster Presentation Monday, May 20 11:30 AM – 1:15 PM PDT |
| Christenson | In the Phase 3 BOREAS Trial, Baseline Blood Eosinophils and Baseline Fractional Exhaled Nitric Oxide Levels Predict the Response to Dupilumab in Patients with Moderate-to-Severe Chronic Obstructive Pulmonary Disease and Type 2 Inflammation | 7654 Oral Presentation Tuesday, May 21 2:15 – 4:15 PM PDT |
| Hanania | Dupilumab Improves Post-Bronchodilator Lung Function in Patients with Moderate-to-Severe Chronic Obstructive Pulmonary Disease (COPD) with Type 2 Inflammation: Data from The Phase 3 BOREAS Trial | 7422 Poster Presentation Sunday, May 19 9:15 – 11:15 AM PDT |
| Heble | Treatment And Disease Burden Among Patients With Moderate Or Severe COPD: Real World Study | P604 Poster Presentation Monday, May 20 11:30 AM – 1:15 PM PDT |
| Mularski | Association Between Serial Spirometric Improver Phenotype (Improved FEV1 Over Time) Versus Decliner Phenotype in Healthcare Utilization in Chronic Obstructive Pulmonary Disease | P133 Poster Presentation Sunday, May 19 11:30 AM – 1:15 PM PDT |
| Papi | Dupilumab Improves Pre-Bronchodilator Lung Function Measures in Patients with Chronic Obstructive Pulmonary Disease (COPD) with Type 2 Inflammation: Data from The Phase 3 BOREAS Trial | 7401 Poster Presentation Sunday, May 19 9:15 – 11:15 AM PDT |
| Qureshi | Healthcare Resource Utilization and Disease Burden in Chronic Obstructive Pulmonary Disease (COPD) Patients With Type 2 Inflammation in the United States: Real-world Evidence | 713 Poster Presentation Sunday, May 19 2:15 – 4:15 PM PDT |
| Asthma | ||
| Washko | Effect of Dupilumab on Airway Oscillometry, Ventilation/Perfusion, and Mucus Plugging in Moderate-to-Severe Asthma: The Vestige Trial | 14998 Oral Presentation Monday, May 20 9:51 – 10:03 AM PDT |
| Bacharier | Improved Lung Function Is Associated With Better Asthma Control in Children With Moderate-To-Severe Type 2 Asthma: VOYAGE Study | 8324 Poster Presentation Tuesday, May 21 11:30 AM – 1:15 PM PDT |
| Bourdin | Dupilumab Asthma ADVANTAGE-EU: Real-World Evidence on the Association Between Dupilumab and Use of Corticosteroid and Asthma Exacerbations in Patients with Severe Asthma in Europe | 10135 Poster Presentation Tuesday, May 21 2:15 – 4:15 PM PDT |
| Busse | Dupilumab Add-On to Medium-Dose Inhaled Corticosteroid (ICS) Increases Odds of Asthma Control and Reduces FeNO Compared With Placebo Add-On to High-Dose ICS | 7437 Poster Presentation Tuesday, May 21 11:30 AM – 1:15 PM PDT |
| Busse | Dupilumab Reduces Severe Exacerbations and Improves Lung Function in Patients with Type 2 Asthma Irrespective of Asthma Duration | 8322 Poster Presentation Tuesday, May 21 11:30 AM – 1:15 PM PDT |
| Do | Characterization of Patients with Severe Asthma Who Initiated Biologic Treatment Within ≤90 and >90 days After Biologic Eligibility | 8484 Poster Presentation Wednesday, May 22 8:15 – 10:15 AM PDT |
| Jackson | Dupilumab Efficacy by Baseline Disease Severity Among Children with Uncontrolled Moderate-to-severe Asthma: Post-hoc Results from the Randomized, Placebo-controlled VOYAGE Trial | 8302 Poster Presentation Tuesday, May 21 2:15 – 4:15 PM PDT |
| Lipworth | Improved Lung Function Is Associated With Better Asthma Control in Adolescents and Adults Aged 12 Years and Older With Moderate-to-Severe Type 2 Asthma: A Post hoc Analysis of QUEST | 7469 Poster Presentation Tuesday, May 21 11:30 AM – 1:15 PM PDT |
| Pavord | Impact of Early Transient Increase in Eosinophil Count on the Long-Term Efficacy of Dupilumab in Patients With Moderate-to-Severe Asthma: LIBERTY ASTHMA TRAVERSE | 7451 Poster Presentation Tuesday, May 21 11:30 AM – 1:15 PM PDT |
| Porsbjerg | Effect of Dupilumab Treatment on Mucus Plugging and Mucus Volume in Type 2 Asthma: The Phase 4 VESTIGE Trial | 15171 Poster Presentation Sunday, May 19 11:30 AM – 1:15 PM PDT |
| Laidlaw | Efficacy and Safety of Rilzabrutinib - A Novel Oral Treatment in Asthma: Results From a Double Blind Placebo Controlled Phase 2b Study | 15074 Poster Presentation Wednesday, May 22 8:15 – 10:15 AM PDT |
| Brahmachary |
Single-Cell RNA Sequencing Analysis of Blood and Nasal Brushing From Asthma Patients Receiving a Single Dose of SAR443765, a novel, bispecific anti-TSLP/anti-IL-13 NANOBODYMolecule Reveals Significant Impact on Multiple Pathological Immune Cell Populations and Downregulation of CCL26 Expression in Epithelial Cell Subpopulations | Oral Presentation Monday, May 20 10:15 – 10:27 AM PDT |
| 主講作者 | 摘要標題 | 演示詳情 |
| 慢性阻塞性 | ||
| Bafadhel | Dupilumab 不會影響中度至重度慢性阻塞性肺病和 2 型炎症患者的血液中嗜酸性粒細胞水平:摘自 Boreas 3 期試驗 | 7498 海報演示 5 月 19 日星期日 太平洋夏令時間上午 9:15 — 11:15 |
| Bhatt | 爲期三年的美國(美國)慢性阻塞性肺病(COPD)患者病情加重和雙/三吸入器使用情況描述性評估 | P584 海報演示 5月20日星期一 太平洋夏令時間上午 11:30 — 下午 1:15 |
| Bhatt | 美國慢性阻塞性肺病(COPD)的特徵 | P585 海報演示 5月20日星期一 太平洋夏令時間上午 11:30 — 下午 1:15 |
| Bhatt | Dupilumab對中度至重度慢性阻塞性肺病和2型炎症患者的療效和安全性:3期NOTUS試驗 | 15018 口頭演講 5月20日星期一 太平洋夏令時間上午 9:15 — 11:15 |
| Bhatt | 在BOREAS的3期試驗中,Dupilumab在一段時間內降低了伴有2型炎症的中度至重度慢性阻塞性肺病患者的FeNo水平 | 7547 海報演示 5 月 19 日星期日 太平洋夏令時間上午 9:15 — 11:15 |
| Buhl/Vogelmeier | 德國LABA/LAMA或吸入三聯療法控制不力的患者慢性阻塞性肺病的臨床和經濟負擔——回顧性索賠數據分析 | P583 海報演示 5月20日星期一 太平洋夏令時間上午 11:30 — 下午 1:15 |
| 克里斯滕森 | 在中度至重度慢性阻塞性肺病和 2 型炎症患者中,隨着時間的推移,Dupilumab 會增加部分呼出一氧化氮水平 | 7636 海報演示 5月20日星期一 太平洋夏令時間上午 11:30 — 下午 1:15 |
| 克里斯滕森 | 在BOREAS的3期試驗中,基線血液嗜酸性粒細胞和基線部分呼出的一氧化氮水平預測了中度至重度慢性阻塞性肺病和2型炎症患者對dupilumab的反應 | 7654 口頭演講 5月21日,星期二 太平洋夏令時間下午 2:15 — 4:15 |
| 哈納尼亞 | Dupilumab改善了伴有2型炎症的中度至重度慢性阻塞性肺病(COPD)患者的支氣管擴張後肺功能:來自BOREAS三期試驗的數據 | 7422 海報演示 5 月 19 日星期日 太平洋夏令時間上午 9:15 — 11:15 |
| Heble | 中度或重度慢性阻塞性肺病患者的治療和疾病負擔:真實世界研究 | P604 海報演示 5月20日星期一 太平洋夏令時間上午 11:30 — 下午 1:15 |
| 穆拉爾斯基 | 慢性阻塞性肺病醫療保健利用中序列肺活量計改進劑表型(FEV1 隨時間推移得到改善)與下降表型之間的關聯 | P133 海報演示 5 月 19 日星期日 太平洋夏令時間上午 11:30 — 下午 1:15 |
| Papi | Dupilumab改善了伴有2型炎症的慢性阻塞性肺病(COPD)患者的支氣管擴張劑前肺功能測量:來自3期BOREAS試驗的數據 | 7401 海報演示 5 月 19 日星期日 太平洋夏令時間上午 9:15 — 11:15 |
| 庫雷希 | 美國慢性阻塞性肺病(COPD)2型炎症患者的醫療資源利用率和疾病負擔:真實世界的證據 | 713 海報演示 5 月 19 日星期日 太平洋夏令時間下午 2:15 — 4:15 |
| 哮喘 | ||
| Washko | Dupilumab對中度至重度哮喘中氣道振盪、通氣/灌注和粘液堵塞的影響:Vestige試驗 | 14998 口頭演講 5月20日星期一 太平洋夏令時間上午 9:51 — 10:03 |
| Bacharier | VOYAGE研究:改善肺功能與改善中度至重度 2 型哮喘患兒的哮喘控制有關 | 8324 海報演示 5月21日,星期二 太平洋夏令時間上午 11:30 — 下午 1:15 |
| 布爾丁 | Dupilumab 哮喘優勢-歐盟:關於歐洲嚴重哮喘患者使用皮質類固醇和哮喘發作之間關聯的真實證據 | 10135 海報演示 5月21日,星期二 太平洋夏令時間下午 2:15 — 4:15 |
| 巴士 | 與高劑量ICS的安慰劑相比,在中劑量吸入性皮質類固醇(ICS)中添加Dupilumab可增加控制哮喘的幾率並降低FeNO | 7437 海報演示 5月21日,星期二 太平洋夏令時間上午 11:30 — 下午 1:15 |
| 巴士 | 無論哮喘持續時間長短,Dupilumab都能減少2型哮喘患者的嚴重發作並改善肺功能 | 8322 海報演示 5月21日,星期二 太平洋夏令時間上午 11:30 — 下午 1:15 |
| 做 | 在生物製劑合格後 ≤90 天和 >90 天內開始生物治療的嚴重哮喘患者的特徵 | 8484 海報演示 5月22日星期三 太平洋夏令時間上午 8:15 — 10:15 |
| 傑克遜 | 在未受控制的中度至重度哮喘患兒中按基線疾病嚴重程度劃分的Dupilumab療效:隨機、安慰劑對照的VOYAGE試驗的後結果 | 8302 海報演示 5月21日,星期二 太平洋夏令時間下午 2:15 — 4:15 |
| 利普沃思 | 肺功能改善與12歲及以上患有中度至重度2型哮喘的青少年和成年人更好地控制哮喘有關:對QUEST的事後分析 | 7469 海報演示 5月21日,星期二 太平洋夏令時間上午 11:30 — 下午 1:15 |
| 帕沃德 | 嗜酸粒細胞數量的早期短暫增加對中度至重度哮喘患者杜匹魯單抗長期療效的影響:LIBERTY ASTRAMA TRAVERSE | 7451 海報演示 5月21日,星期二 太平洋夏令時間上午 11:30 — 下午 1:15 |
| Porsbjerg | Dupilumab治療對2型哮喘粘液堵塞和粘液體積的影響:4期VESTIGE試驗 | 15171 海報演示 5 月 19 日星期日 太平洋夏令時間上午 11:30 — 下午 1:15 |
| Laidlaw | 利扎布替尼——一種治療哮喘的新型口服療法的療效和安全性:一項雙盲安慰劑對照的2b期研究結果 | 15074 海報演示 5月22日星期三 太平洋夏令時間上午 8:15 — 10:15 |
| 勃拉馬查裏 |
對接受單劑量 SAR443765(一種新型雙特異性抗 TSLP/抗 IL-13 納米體)的哮喘患者的血液和鼻刷的單細胞 RNA 測序分析分子顯示出對多種病理免疫細胞群的重大影響以及上皮細胞亞群中 CCL26 表達的下調 | 口頭陳述 5月20日星期一 太平洋夏令時間上午 10:15 — 10:27 |
About Dupixent
Dupixent is a fully human monoclonal antibody that inhibits the signaling of the interleukin-4 (IL-4) and interleukin-13 (IL-13) pathways and is not an immunosuppressant. The Dupixent development program has shown significant clinical benefit and a decrease in type 2 inflammation in phase 3 trials, establishing that IL-4 and IL-13 are two of the key and central drivers of the type 2 inflammation that plays a major role in multiple related and often co-morbid diseases.
關於 Dupixent
Dupixent是一種全人源單克隆抗體,可抑制白介素-4(IL-4)和白介素-13(IL-13)通路的信號傳導,不是免疫抑制劑。在 3 期試驗中,Dupixent 開發計劃顯示出顯著的臨床益處和 2 型炎症的減少,這表明 IL-4 和 IL-13 是 2 型炎症的兩個關鍵和核心驅動因素,二型炎症在多種相關且往往是併發疾病中起着重要作用。
Dupixent has received regulatory approvals in more than 60 countries in one or more indications including in certain patients with atopic dermatitis, asthma, chronic rhinosinusitis with nasal polyposis (CRSwNP), eosinophilic esophagitis (EoE), prurigo nodularis, and chronic spontaneous urticaria (CSU) in different age populations. More than 850,000 patients are being treated with Dupixent globally. Dupixent is currently under Priority Review by the U.S. Food and Drug Administration as an add-on maintenance treatment in certain adult patients with uncontrolled COPD.
Dupixent在一項或多項適應症中已獲得60多個國家的監管批准,包括不同年齡人群中的某些特應性皮炎、哮喘、慢性鼻竇炎伴鼻息肉(crsWnP)、嗜酸性食管炎(EoE)、結節性瘙癢症和慢性自發性蕁麻疹(CSU)患者。全球有超過85萬名患者正在接受Dupixent的治療。Dupixent目前正在接受美國食品藥品監督管理局的優先審查,作爲某些不受控制的慢性阻塞性肺病的成年患者的附加維持療法。
About rilzabrutinib
Rilzabrutinib is an investigational oral, reversible, covalent BTK inhibitor that has the potential to be a first- or best-in-class treatment of a number of immune-mediated diseases, including CSU, prurigo nodularis, asthma, immune thrombocytopenia (ITP), IgG4-related disease and warm autoimmune hemolytic anemia (wAIHA). BTK is expressed in B cells, mast cells, eosinophils, basophils and macrophages which play a critical role in multiple immune-mediated disease processes. With the application of Sanofi's TAILORED COVALENCY technology, rilzabrutinib can selectively inhibit the BTK target while potentially reducing the risk of off-target side effects.
關於利扎布替尼
Rilzabrutinib是一種在研的口服、可逆的共價BTK抑制劑,有可能成爲許多免疫介導疾病的首創或同類最佳治療藥物,包括CSU、結節性瘙癢、哮喘、免疫血小板減少症(ITP)、IgG4相關疾病和溫熱性自身免疫溶血性貧血(WaiHA)。BTK 在 B 細胞、肥大細胞、嗜酸性粒細胞、嗜鹼性粒細胞和巨噬細胞中表達,它們在多種免疫介導的疾病過程中起着至關重要的作用。通過應用賽諾菲的TAILORED COVALENCY技術,rilzabrutinib可以選擇性地抑制BTK靶點,同時有可能降低脫靶副作用的風險。
About lunsekimig
Lunsekimig is an investigational novel nanobody VHH that combines targeting of IL-13, a downstream cytokine causing tissue organ damage in respiratory diseases and TSLP, an upstream initiator of inflammation. Pre-clinical research suggests that the combination of these targets can create more potent effect on type-2 inflammation, making lunsekimig a potentially best-in-class treatment for asthma and a range of other respiratory diseases.
關於 lunsekimig
Lunsekimig 是一種正在研究的新型納米體 VHH,它結合了對呼吸系統疾病中造成組織器官損傷的下游細胞因子 IL-13 和上游炎症引發劑 TSLP 的靶向。臨床前研究表明,這些靶點的組合可以對2型炎症產生更有效的影響,這使得lunsekimig可能成爲治療哮喘和一系列其他呼吸系統疾病的最佳治療方法。
Rilzabrutinib and Lunsekimig are under clinical investigation and their safety and efficacy have not been evaluated by any regulatory authority.
Rilzabrutinib和Lunsekimig正在臨床研究中,其安全性和有效性尚未經過任何監管機構的評估。
Dupilumab development program
Dupilumab is being jointly developed by Sanofi and Regeneron under a global collaboration agreement. To date, dupilumab has been studied across more than 60 clinical trials involving more than 10,000 patients with various chronic diseases driven in part by type 2 inflammation.
Dupilumab 開發計劃
Dupilumab由賽諾菲和Regeneron根據一項全球合作協議共同開發。迄今爲止,dupilumab已在60多項臨床試驗中進行了研究,涉及10,000多名患有各種慢性病的患者,部分原因是2型炎症。
In addition to the currently approved indications, Sanofi and Regeneron are studying dupilumab in a broad range of diseases driven by type 2 inflammation or other allergic processes in phase 3 trials, including chronic pruritus of unknown origin, chronic obstructive pulmonary disease (COPD) with evidence of type 2 inflammation, and bullous pemphigoid. These potential uses of dupilumab are currently under clinical investigation, and the safety and efficacy in these conditions have not been fully evaluated by any regulatory authority.
除了目前批准的適應症外,賽諾菲和Regeneron還在3期試驗中研究dupilumab用於由2型炎症或其他過敏過程驅動的各種疾病,包括來歷不明的慢性瘙癢、有2型炎症證據的慢性阻塞性肺病(COPD)和大皰性類天皰瘡。dupilumab的這些潛在用途目前正在臨床研究中,任何監管機構尚未對這些疾病的安全性和有效性進行全面評估。
About Sanofi
We are an innovative global healthcare company, driven by one purpose: we chase the miracles of science to improve people's lives. Our team, across the world, is dedicated to transforming the practice of medicine by working to turn the impossible into the possible. We provide potentially life-changing treatment options and life-saving vaccine protection to millions of people globally, while putting sustainability and social responsibility at the center of our ambitions.
Sanofi is listed on EURONEXT: SAN and NASDAQ: SNY
關於賽諾菲
我們是一家創新的全球醫療保健公司,我們的目標只有一個:我們追逐科學奇蹟以改善人們的生活。我們的團隊遍佈世界各地,致力於將不可能變爲可能,從而改變醫學實踐。我們爲全球數百萬人提供可能改變生活的治療選擇和挽救生命的疫苗保護,同時將可持續發展和社會責任置於我們雄心壯志的中心。
賽諾菲在泛歐交易所:SAN 和納斯達克上市:SNY
Sanofi Media Relations
Sally Bain | + 1 617 834 6026 | sally.bain@sanofi.com
Victor Rouault | + 33 6 70 93 71 40 | victor.rouault@sanofi.com
Timothy Gilbert | + 1 516 521 2929 | timothy.gilbert@sanofi.com
賽諾菲媒體關係
Sally Bain | + 1 617 834 6026 | sally.bain@sanofi.com
Victor Rouault | + 33 6 70 93 71 40 | victor.rouault@sanofi.com
蒂莫西·吉爾伯特 | + 1 516 521 2929 | timothy.gilbert@sanofi.com
Sanofi Investor Relations
Thomas Kudsk Larsen | +44 7545 513 693 | thomas.larsen@sanofi.com
Alizé Kaisserian | + 33 06 47 04 12 11 | alize.kaisserian@sanofi.com
Arnaud Delépine | + 33 06 73 69 36 93 | arnaud.delepine@sanofi.com
Corentine Driancourt | + 33 06 40 56 92 | corentine.driancourt@sanofi.com
Felix Lauscher | + 1 908 612 7239 | felix.lauscher@sanofi.com
Tarik Elgoutni | + 1 617 710 3587 | tarik.elgoutni@sanofi.com
Nathalie Pham | + 33 07 85 93 30 17 | nathalie.pham@sanofi.com
賽諾菲投資者關係
托馬斯·庫德斯克·拉森 | +44 7545 513 693 | thomas.larsen@sanofi.com
Alizeé Kaisserian | + 33 06 47 04 12 11 | alize.kaisserian@sanofi.com
Arnaud Delépine | + 33 06 73 69 36 93 | 一個rnaud.delepine@sanofi.com
Corentine Driancourt | + 33 06 40 56 92 | corentine.driancourt@sanofi.com
Felix Lauscher | + 1 908 612 7239 | felix.lauscher@sanofi.com
Tarik Elgoutni | + 1 617 710 3587 | tarik.elgoutni@sanofi.com
Nathalie Pham | + 33 07 85 93 30 17 | nathalie.pham@sanofi.com
Regeneron Media Relations
Anna Hodge | +1 914-255-6475| anna.hodge@regeneron.com
Regeneron 媒體關係
安娜·霍奇 | +1 914-255-6475| anna.hodge@regeneron.com
Regeneron Investor Relations
Vesna Tosic | + 914 847 5443 | vesna.tosic@regeneron.com
Regeneron 投資者關係
Vesna Tosic | + 914 847 5443 | vesna.tosic@regeneron.com
Sanofi Forward-Looking Statements
賽諾菲前瞻性陳述
This press release 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 and their underlying assumptions, statements regarding plans, objectives, intentions and expectations with respect to future financial results, events, operations, services, product development and potential, and statements regarding future performance. 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, the uncertainties inherent in research and development, future clinical data and analysis, including post marketing, decisions by regulatory authorities, such as the FDA or the EMA, regarding whether and when to approve any drug, device or biological application that may be filed for any such product candidates as well as their decisions regarding labelling and other matters that could affect the availability or commercial potential of such product candidates, the fact that product candidates if approved may not be commercially successful, the future approval and commercial success of therapeutic alternatives, Sanofi's ability to benefit from external growth opportunities, to complete related transactions and/or obtain regulatory clearances, risks associated with intellectual property and any related pending or future litigation and the ultimate outcome of such litigation, trends in exchange rates and prevailing interest rates, volatile economic and market conditions, cost containment initiatives and subsequent changes thereto, 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.
本新聞稿包含經修訂的1995年《私人證券訴訟改革法》中定義的前瞻性陳述。前瞻性陳述是不是歷史事實的陳述。這些陳述包括預測和估計及其基本假設,有關未來財務業績、事件、運營、服務、產品開發和潛力的計劃、目標、意圖和預期的陳述,以及有關未來業績的陳述。前瞻性陳述通常由 “期望”、“預期”、“相信”、“打算”、“估計”、“計劃” 和類似表述來識別。儘管賽諾菲管理層認爲此類前瞻性陳述中反映的預期是合理的,但提醒投資者,前瞻性信息和陳述存在各種風險和不確定性,其中許多風險和不確定性難以預測,通常超出賽諾菲的控制範圍,這可能導致實際業績和發展與前瞻性信息和陳述所表達、暗示或預測的業績和發展存在重大差異。除其他外,這些風險和不確定性包括研發固有的不確定性、未來的臨床數據和分析,包括上市後的分析、監管機構(例如FDA或EMA)關於是否及何時批准任何此類候選產品可能申請的任何藥物、設備或生物學應用的決定,以及他們關於標籤和其他可能影響此類候選產品可用性或商業潛力的事項的決定,候選產品如果獲得批准的事實可能不會在商業上取得成功、替代療法的未來批准和商業成功、賽諾菲從外部增長機會中受益、完成關聯交易和/或獲得監管許可的能力、與知識產權和任何相關的未決或未來訴訟相關的風險以及此類訴訟的最終結果、匯率和現行利率的趨勢、動盪的經濟和市場狀況、成本控制舉措及其後續變化,以及疫情的影響其他全球危機可能對我們、我們的客戶、供應商、供應商和其他商業夥伴以及其中任何一個的財務狀況以及我們的員工和整個全球經濟造成影響。風險和不確定性還包括賽諾菲在向美國證券交易委員會和AMF提交的公開文件中討論或確定的不確定性,包括賽諾菲截至2023年12月31日止年度的20-F表年度報告中 “風險因素” 和 “關於前瞻性陳述的警示性聲明” 中列出的不確定性。除適用法律的要求外,賽諾菲不承擔任何更新或修改任何前瞻性信息或陳述的義務。
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