Vertex Announces Results From Phase 2 Study of Suzetrigine for the Treatment of Painful Lumbosacral Radiculopathy
Vertex Announces Results From Phase 2 Study of Suzetrigine for the Treatment of Painful Lumbosacral Radiculopathy
– Treatment with the highly selective NaV1.8 pain signal inhibitor suzetrigine met the primary endpoint with a statistically significant and clinically meaningful 2.02 point within-group reduction from baseline in the Numeric Pain Rating Scale (NPRS) –
– 使用高度選擇性的NaV1.8疼痛信號抑制劑suzetrigine的治療達到了主要終點,在數值疼痛評定量表(NPRS)中,從基線起組內減少了統計學上顯著且臨牀上有意義的2.02分 –
– Placebo arm showed similar within-group reduction in NPRS –
– 安慰劑組在NPRS中顯示出類似的組內減少 –
– Suzetrigine was generally well tolerated –
– suzetrigine通常耐受良好 –
– Advancement to Phase 3 in painful lumbosacral radiculopathy planned, pending discussions with regulators –
– 計劃推進到第3階段針對疼痛性腰骶根神經痛的研究,待與監管機構討論後進行 –
– Vertex to host investor call on December 19 at 8:00 a.m. ET –
– Vertex將於12月19日上午8:00(東部時間)舉行投資者看漲 –
BOSTON--(BUSINESS WIRE)--Vertex Pharmaceuticals Incorporated (Nasdaq: VRTX) today announced results from its Phase 2 study of suzetrigine, an investigational, oral, highly selective NaV1.8 pain signal inhibitor in people with painful lumbosacral radiculopathy (LSR). The study met its primary endpoint with statistically significant and clinically meaningful reduction in pain on the numeric pain rating scale (NPRS).
波士頓--(商業資訊)--福泰製藥公司(納斯達克:VRTX)今天宣佈了其針對於疼痛性腰骶根神經痛(LSR)的人群進行的suzetrigine二期研究結果,該研究作爲一種實驗性的口服高度選擇性的NaV1.8疼痛信號抑制劑。該研究達成了其主要終點,在數值疼痛評定量表(NPRS)上實現了統計學上顯著且臨牀上有意義的疼痛減少。
Efficacy Results
療效結果
The study's primary endpoint was a within-group change from baseline in the weekly average of daily leg pain intensity on the NPRS at Week 12. This 11-point scale ranges from 0 (no pain) to 10 (worst pain imaginable).
該研究的主要終點是在第12周,對來自基線的組內每日腿部疼痛強度的周平均值的變化。此11分制評分範圍從0(無疼痛)到10(最嚴重的疼痛)。
The suzetrigine arm showed a statistically significant and clinically meaningful within-group reduction from baseline in pain with a mean change in NPRS at Week 12 of -2.02.
蘇澤曲丁組在12周時的NPRS平均變化爲-2.02,顯示出從基線到組內在疼痛上的統計顯著性和臨牀意義的減少。
The study also included a placebo reference arm which showed a similar within-group reduction from baseline in pain with a mean change in NPRS at Week 12 of -1.98. The study was not designed nor powered for statistical comparison between suzetrigine and placebo.
該研究還包括一個安慰劑參考組,顯示出從基線到組內在疼痛上的類似減少,12周時NPRS的平均變化爲-1.98。該研究並不是爲了蘇澤曲丁與安慰劑之間的統計比較而設計或賦予統計能力。
Suzetrigine |
Placebo |
|
Baseline NPRS |
||
Mean NPRS (SD) |
6.33 (1.22) |
6.05 (1.07) |
Change in NPRS from baseline at Week 12 |
||
LS mean |
-2.02 |
-1.98 |
95% CI |
(-2.40, -1.64) |
(-2.36, -1.60) |
P value |
<0.0001 |
<0.0001 |
蘇澤曲丁 |
安慰劑 |
|
基線NPRS |
||
平均NPRS (SD) |
6.33 (1.22) |
6.05 (1.07) |
第12周基線時NPRS的變化 |
||
LS意味着 |
-2.02 |
-1.98 |
95%置信區間 |
(-2.40, -1.64) |
(-2.36, -1.60) |
P值 |
Secondary and other endpoints were consistent with the study's primary endpoint.
次要和其他終點與研究的主要終點一致。
Vertex also conducted post-hoc analyses to further evaluate the efficacy results. These showed that there was variability in the placebo response across study sites, a recognized issue in pain trials. In the ~40% of sites that had lower placebo responses, the suzetrigine arm within-group reduction in pain was similar to the overall study and had greater separation from the placebo arm. These analyses suggest that trial design innovation may better control the placebo response and separate the treatment effect of suzetrigine from placebo in future studies, which Vertex will incorporate as it designs the pivotal program.
福泰製藥還進行了事後分析,以進一步評估療效結果。這些結果顯示,各個研究中心的安慰劑反應存在差異,這是疼痛試驗中一個公認的問題。在大約40%的安慰劑反應較低的中心,suzetrigine組內減痛幅度與總體研究類似,並且與安慰劑組的分離度更大。這些分析表明,試驗設計的創新可能更好地控制安慰劑反應,並在未來的研究中將suzetrigine的治療效果與安慰劑區分開來,福泰製藥將在設計關鍵項目時納入這些創新。
Safety Results
安全結果
Suzetrigine was generally well tolerated in the study. The incidence of adverse events (AEs) was 22.9% in the suzetrigine arm and 32.4% in the placebo arm. In both treatment arms, most AEs were mild to moderate. There were no serious adverse events (SAEs) related or possibly related to suzetrigine. There were no AEs leading to treatment discontinuation in patients treated with suzetrigine.
在研究中,suzetrigine通常耐受良好。suzetrigine組的不良事件(AE)發生率爲22.9%,安慰劑組爲32.4%。在兩組治療中,大多數不良事件爲輕度至中度。沒有與suzetrigine相關或可能相關的嚴重不良事件(SAE)。在接受suzetrigine治療的患者中,沒有導致治療中斷的不良事件。
Suzetrigine |
Placebo |
|
Subjects with any AEs |
25 (22.9) |
35 (32.4) |
Subjects with AEs by strongest relationship | ||
Not related |
16 (14.7) |
20 (18.5) |
Unlikely related |
1 (0.9) |
6 (5.6) |
Possibly related |
6 (5.5) |
8 (7.4) |
Related |
2 (1.8) |
1 (0.9) |
Subjects with AEs by maximum severity | ||
Grade 1/Mild |
15 (13.8) |
17 (15.7) |
Grade 2/Moderate |
10 (9.2) |
17 (15.7) |
Grade 3/Severe |
0 |
1 (0.9) |
Grade 4/Life-threatening |
0 |
0 |
Grade 5/Death |
0 |
0 |
Subjects with serious AEs |
1 (0.9) |
2 (1.9) |
Subjects with AEs leading to treatment discontinuation |
0 |
1 (0.9) |
Subjects with AEs leading to death |
0 |
0 |
蘇澤曲丁 |
安慰劑 |
|
有任何不良事件的受試者 |
25 (22.9) |
35 (32.4) |
按最強關係分類的不良事件患者 | ||
無關 |
16 (14.7) |
20 (18.5) |
不太相關 |
1 (0.9) |
6 (5.6) |
可能相關 |
6 (5.5) |
8 (7.4) |
相關 |
2 (1.8) |
1 (0.9) |
按最大嚴重程度分類的有不良事件的受試者 | ||
等級 1/輕度 |
15 (13.8) |
17 (15.7) |
二級/中等 |
10 (9.2) |
17 (15.7) |
三級/嚴重 |
0 |
1 (0.9) |
4級/生命危險 |
0 |
0 |
5級/死亡 |
0 |
0 |
有嚴重不良事件的受試者 |
1 (0.9) |
2 (1.9) |
因不良事件導致停止治療的受試者 |
0 |
1 (0.9) |
因不良事件導致死亡的受試者 |
0 |
0 |
"Suzetrigine has again demonstrated its potential to fill an important unmet need in the treatment of pain. Today's LSR results are consistent with previous studies of this pain signal inhibitor in terms of showing a meaningful treatment effect across pain conditions and a favorable safety profile," said Carmen Bozic, M.D., Executive Vice President, Global Medicines Development and Medical Affairs, and Chief Medical Officer at Vertex. "We did not see separation between the suzetrigine and the placebo arms. Yet our post-hoc analyses suggest that this could be due to the high placebo response in this study. We remain committed to studying LSR and innovating our Phase 3 study design to control for the placebo effect as we advance suzetrigine into pivotal development for this condition."
「Suzetrigine再次證明其在治療疼痛方面填補了一個重要的未滿足需求。今天的LSR結果與之前關於這種疼痛信號抑制劑的研究一致,顯示了在各種疼痛控制項中具有顯著的治療效果和良好的安全性,」Vertex的執行副總裁、全球藥物開發和醫療事務以及首席醫療官克莉絲汀·博齊克(D.)說道。「我們沒有看到suzetrigine與安慰劑組之間的分離。然而,我們的事後分析表明,這可能是由於該研究中安慰劑的高反應率。我們仍然致力於研究LSR,並創新我們的第三階段研究設計,以控制安慰劑效應,同時推進suzetrigine進入此控制項的關鍵開發。」
"The suzetrigine Phase 2 results clearly show reduced pain intensity from baseline in the active drug arm, and the potential for suzetrigine to fill an unmet need in relieving LSR pain, a heterogeneous condition that is notoriously difficult to treat," said Christine Sang, M.D., M.P.H., FASA, Director, Translational Pain Research, Brigham and Women's Hospital, Associate Professor of Anesthesia, Harvard Medical School, co-chair of Vertex's Peripheral Neuropathic Pain steering committee, and lead principal investigator on the study. "Managing the placebo response in pain trials is a complex challenge. We look forward to innovating in clinical trial design, including for the pivotal study, with the aim of bringing a potentially safe and effective treatment to patients suffering from LSR."
"su Zetrigine 第二階段的結果清楚顯示,活性藥物組的疼痛強度相比基線有所降低,並且 su Zetrigine 可能滿足緩解 LSR 疼痛的需求,這是一種 notoriously 難以治療的異質性病症," 哈佛醫學院麻醉學副教授、福泰製藥外周神經性疼痛指導委員會的共同主席及此項研究的首席研究員 克莉絲汀·桑萬.D.萬.P.H., FASA 說道。"在疼痛試驗中管理安慰劑反應是一個複雜的挑戰。我們期待在臨牀試驗設計中進行創新,包括針對關鍵研究,旨在爲遭受 LSR 疼痛的患者帶來潛在安全有效的治療。"
Next Steps for the Pain Portfolio
疼痛產品組合的下一步
Neuropathic Pain
神經痛
Vertex plans to advance suzetrigine into pivotal development for painful LSR following discussions with regulators on the study design and regulatory package. The company will apply learnings from analysis of the full Phase 2 data set and post-hoc analyses to inform the Phase 3 study design.
福泰製藥計劃在與監管機構討論研究設計和監管方案後,將 su Zetrigine 推進到針對疼痛性 LSR 的關鍵開發階段。公司將借鑑對完整第二階段數據集及事後分析的分析結果,以指導第三階段研究設計。
Earlier this year, Vertex initiated its suzetrigine pivotal program in painful diabetic peripheral neuropathy (DPN), another type of peripheral neuropathic pain (PNP). That study is ongoing.
今年早些時候,福泰製藥在疼痛性糖尿病周圍神經病(DPN)的 su Zetrigine 關鍵計劃中啓動了另一種類型的外周神經病痛(PNP)。該研究正在進行中。
Acute Pain
急性疼痛
Additionally, as previously announced, suzetrigine is under FDA review for the treatment of moderate-to-severe acute pain. The agency granted priority review and assigned a Prescription Drug User Fee Act (PDUFA) target action date of January 30, 2025.
此外,正如之前所宣佈的,su Zetrigine 正在針對中度至重度急性疼痛進行 FDA 審查。該機構已授予優先審查,並指定了 2025 年 1 月 30 日的處方藥用戶收費法案(PDUFA)目標行動日期。
In line with its portfolio strategy, Vertex continues to advance preclinical and clinical development of additional NaV1.8 and NaV1.7 inhibitors, for use alone or in combination, in acute and neuropathic pain.
與其產品組合策略一致,福泰製藥繼續推進額外 NaV1.8 和 NaV1.7 抑制劑的臨牀前和臨牀開發,單獨或組合使用於急性和神經痛。
Conference Call and Webcast
電話會議和網絡直播
The company will host a conference call and webcast at 8:00 a.m. ET on Thursday, December 19, 2024. To access the call, please dial (833) 630-2124 (U.S.) or +1 (412) 317-0651 (International) and reference the "Vertex Pharmaceuticals Conference Call."
公司將在2024年12月19日星期四美國東部時間上午8:00舉辦電話會議和網絡廣播。要參加電話會議,請撥打(833)630-2124(美國)或 +1(412)317-0651(國際),並提及「福泰製藥電話會議」。
The conference call will be webcast live and a link to the webcast can be accessed through Vertex's website at in the "Investors" section. To ensure a timely connection, it is recommended that participants register at least 15 minutes prior to the scheduled webcast. An archived webcast will be available on the company's website.
電話會議將進行實時網絡廣播,可以通過福泰製藥的網站在「投資者」部分訪問網絡廣播鏈接。爲確保及時連接,建議參與者至少在預定網絡廣播前15分鐘註冊。公司網站上將提供存檔的網絡廣播。
About the Phase 2 Suzetrigine Lumbosacral Radiculopathy (LSR) Study
關於第二階段蘇澤曲明腰骶神經根病(LSR)研究
This phase 2, 12-week, randomized, double-blind, placebo-controlled study evaluated the efficacy and safety of suzetrigine in treating patients with painful LSR. A total of 218 patients were enrolled in the study and randomized 1:1 with suzetrigine or placebo. The primary endpoint was the within-group change from baseline in the weekly average of daily leg pain intensity on a numeric pain rating scale (NPRS) at Week 12. The study also included a placebo reference arm; however, the study was not designed nor powered for comparison between suzetrigine and placebo.
該第二階段爲期12周的隨機、雙盲、安慰劑對照研究評估了蘇澤曲明在治療痛苦的LSR患者中的療效和安全性。共有218名患者參與了該研究,並隨機分爲1:1接受蘇澤曲明或安慰劑。主要終點是在第12周,每週平均每日腿部疼痛強度在數字疼痛評分量表(NPRS)上相對於基線的組內變化。該研究還包括一個安慰劑對照組;然而,該研究並未設計或有能力進行蘇澤曲明與安慰劑之間的比較。
Secondary endpoints assessed the within-group change from baseline in the weekly average of the daily sleep interference scale at Week 12 and safety and tolerability. By blocking the pain signal from the peripheral sensory neurons, Vertex believes that suzetrigine may alleviate the suffering for millions of patients with painful LSR.
次要終點評估了在第12周相對於基線每週平均的每天睡眠干擾量表的組內變化,以及安全性和耐受性。福泰製藥相信,通過阻斷外周感覺神經的疼痛信號,蘇澤曲明可能減輕數百萬痛苦LSR患者的痛苦。
About Painful Lumbosacral Radiculopathy (LSR)
關於痛苦的腰骶神經根病(LSR)
Painful lumbosacral radiculopathy, or LSR, is one of the most common causes of peripheral neuropathic pain. It is pain caused by impairment of nerve roots in the area of the lumbar spine. It often results in radiating pain along the distribution of the impacted nerve in the body, and patients can experience back and leg pain, sensory issues or motor dysfunction. Common causes of LSR include nerve compression from a herniated disk, or arthritic or degenerative changes in the area of the lower spine. LSR is a neuropathic pain condition because the impacted nerve roots are part of the peripheral nervous system and not part of the spinal cord. Millions of patients suffer from pain due to LSR every year.
痛苦的腰骶神經根病,或稱LSR,是外周神經性疼痛最常見的原因之一。它是由腰椎區域神經根損傷引起的疼痛。通常會導致沿受影響神經在身體上的分佈放射性疼痛,患者可能會體驗到背部和腿部疼痛、感覺問題或運動功能障礙。LSR的常見原因包括因椎間盤突出、關節炎或下部脊柱區域的退行性變化引起的神經壓迫。LSR是一種神經性疼痛狀態,因爲受影響的神經根是外周神經系統的一部分,而不是脊髓的一部分。每年有數百萬患者因LSR而受到疼痛困擾。
About Suzetrigine
About Suzetrigine
Suzetrigine is an investigational oral, highly selective pain signal inhibitor that is selective for NaV1.8 relative to other NaV channels. NaV1.8 is a voltage-gated sodium channel that is selectively expressed in peripheral pain-sensing neurons (nociceptors), where its role is to transmit pain signals (action potentials). Vertex's approach is to selectively inhibit NaV1.8 using small molecules with the objective of creating a new class of pain signal inhibitors that have the potential to provide effective relief of pain without the limitations of currently available therapies, including the addictive potential of opioids. Suzetrigine has demonstrated a favorable benefit/risk profile in multiple Phase 2 and Phase 3 studies in patients with moderate-to-severe acute pain and has been granted FDA Fast Track and Breakthrough Therapy designations in moderate-to-severe acute pain in the U.S. It is currently under priority review by the FDA for the treatment of moderate-to-severe acute pain with a Prescription Drug User Fee Act (PDUFA) target action date of January 30, 2025. The Phase 3 pivotal program for suzetrigine in patients with painful diabetic peripheral neuropathy is ongoing, and the company plans to advance its pivotal program evaluating suzetrigine in patients with painful lumbosacral radiculopathy pending discussions with regulators. Suzetrigine is investigational and has not been approved by any health authority.
Suzetrigine is an investigational oral, highly selective pain signal inhibitor that is selective for NaV1.8 relative to other NaV channels. NaV1.8 is a voltage-gated sodium channel that is selectively expressed in peripheral pain-sensing neurons (nociceptors), where its role is to transmit pain signals (action potentials). Vertex's approach is to selectively inhibit NaV1.8 using small molecules with the objective of creating a new class of pain signal inhibitors that have the potential to provide effective relief of pain without the limitations of currently available therapies, including the addictive potential of opioids. Suzetrigine has demonstrated a favorable benefit/risk profile in multiple Phase 2 and Phase 3 studies in patients with moderate-to-severe acute pain and has been granted FDA Fast Track and Breakthrough Therapy designations in moderate-to-severe acute pain in the U.S. It is currently under priority review by the FDA for the treatment of moderate-to-severe acute pain with a Prescription Drug User Fee Act (PDUFA) target action date of January 30, 2025. The Phase 3 pivotal program for suzetrigine in patients with painful diabetic peripheral neuropathy is ongoing, and the company plans to advance its pivotal program evaluating suzetrigine in patients with painful lumbosacral radiculopathy pending discussions with regulators. Suzetrigine is investigational and has not been approved by any health authority.
About Vertex
Vertex是一家全球性的生物技術公司,致力於通過科學創新爲患有嚴重疾病的人創造變革性藥物。該公司已經獲批准的藥物治療多種慢性、縮短壽命的遺傳病的基本原因,包括囊性纖維化、鐮狀細胞病和輸血依賴性β地中海貧血,並在這些疾病中不斷推進臨牀和研究計劃。Vertex在其他嚴重疾病領域也有一系列調查治療法的豐富臨牀流水線,包括急性和神經性疼痛、APOL1介導的腎臟疾病、常染色體顯性多囊腎病、1型糖尿病、肌強直性營養不良型1和α-1抗胰蛋白酶缺乏症。
Vertex is a global biotechnology company that invests in scientific innovation to create transformative medicines for people with serious diseases. The company has approved medicines that treat the underlying causes of multiple chronic, life-shortening genetic diseases — cystic fibrosis, sickle cell disease and transfusion-dependent beta thalassemia — and continues to advance clinical and research programs in these diseases. Vertex also has a robust clinical pipeline of investigational therapies across a range of modalities in other serious diseases where it has deep insight into causal human biology, including acute and neuropathic pain, APOL1-mediated kidney disease, IgA nephropathy, primary membranous nephropathy, autosomal dominant polycystic kidney disease, type 1 diabetes and myotonic dystrophy type 1.
Vertex is a global biotechnology company that invests in scientific innovation to create transformative medicines for people with serious diseases. The company has approved medicines that treat the underlying causes of multiple chronic, life-shortening genetic diseases — cystic fibrosis, sickle cell disease and transfusion-dependent beta thalassemia — and continues to advance clinical and research programs in these diseases. Vertex also has a robust clinical pipeline of investigational therapies across a range of modalities in other serious diseases where it has deep insight into causal human biology, including acute and neuropathic pain, APOL1-mediated kidney disease, IgA nephropathy, primary membranous nephropathy, autosomal dominant polycystic kidney disease, type 1 diabetes and myotonic dystrophy type 1.
Vertex was founded in 1989 and has its global headquarters in Boston, with international headquarters in London. Additionally, the company has research and development sites and commercial offices in North America, Europe, Australia, Latin America and the Middle East. Vertex is consistently recognized as one of the industry's top places to work, including 15 consecutive years on Science magazine's Top Employers list and one of Fortune's 100 Best Companies to Work For.
福泰製藥成立於1989年,總部位於波士頓,國際總部設在倫敦。此外,公司在北美、歐洲、澳洲、拉丁美洲和中東設有研究和開發機構以及商業辦公室。福泰製藥始終被公認爲行業板塊中最佳的工作場所之一,包括連續15年入選《科學》雜誌的最佳僱主名單,以及《財富》雜誌評選的100家最佳公司之一。
譯文內容由第三人軟體翻譯。