Vaxart Announces Positive Results for Its Bivalent Norovirus Vaccine Candidate in Lactating Mothers
Vaxart Announces Positive Results for Its Bivalent Norovirus Vaccine Candidate in Lactating Mothers
Antibody rise observed in lactating mothers and in their breast milk
在哺乳期母親及其母乳中觀察到抗體升高
Long-term goal is to provide protection to infants through passive antibody transfer
長期目標是通過被動抗體轉移爲嬰兒提供保護
SOUTH SAN FRANCISCO, Calif., April 30, 2024 (GLOBE NEWSWIRE) -- Vaxart, Inc. (Nasdaq: VXRT) today announced that it has completed the topline analysis for the Phase 1 clinical trial evaluating Vaxart's oral pill bivalent norovirus vaccine candidate.
加利福尼亞州南舊金山,2024年4月30日(GLOBE NEWSWIRE)——Vaxart, Inc.(納斯達克股票代碼:VXRT)今天宣佈,它已經完成了評估Vaxart口服藥丸二價諾如病毒候選疫苗的1期臨床試驗的頭條分析。
The trial was focused on lactating mothers. Antibodies to norovirus rose on average 4.0 fold for the G1.1 virus strain and 6.0 fold for the GII.4 virus strain in the breast milk of lactating mothers who received the Vaxart vaccine candidate in the high dose group. There were no vaccine-related serious adverse events (SAEs) and no dose-limiting pharmacotoxicity.
該試驗的重點是哺乳期母親。在高劑量組中接種Vaxart候選疫苗的哺乳期母親的母乳中,G1.1病毒株的諾如病毒抗體平均增加了4.0倍,GII.4病毒株的抗體平均增加了6.0倍。沒有疫苗相關的嚴重不良事件(SAE),也沒有劑量限制藥物毒性。
"This is an important step forward as we drive toward a vaccine candidate that may make it possible for mothers to protect their children against this highly contagious – and potentially lethal – virus. It can be difficult to immunize the youngest of children mucosally because the immune system is still developing. Passive transfer of antibodies from mothers to infants via breast milk is an innovative approach to potentially improve infection resistance in infants," said Dr. James F. Cummings, Vaxart's Chief Medical Officer. "We would like to thank the study subjects for their participation in this novel and important clinical trial."
“這是我們向前邁出的重要一步,因爲候選疫苗可能使母親能夠保護孩子免受這種高度傳染性且可能致命的病毒的侵害。由於免疫系統仍在發育,因此可能很難對最小的孩子進行粘膜免疫接種。Vaxart首席醫學官詹姆斯·卡明斯博士說,通過母乳將抗體從母乳被動轉移給嬰兒是一種有可能提高嬰兒抗感染能力的創新方法。“我們要感謝研究對象參與這項新穎而重要的臨床試驗。”
There is no approved vaccine against norovirus, which sickens approximately 21 million people in the United States each year, including the 15% of children under age 5 who contract norovirus annually. Approximately 3 million sets of parents are forced by this virus to miss work – approximately 2.2 days on average – to care for their children. The annual disease burden from norovirus is $10.6 billion in the United States alone.
目前尚無經批准的諾如病毒疫苗,諾如病毒每年使美國約2100萬人患病,其中包括每年感染諾如病毒的15%的5歲以下兒童。大約300萬組父母因這種病毒而被迫缺勤——平均約2.2天——以照顧孩子。僅在美國,諾如病毒造成的年度疾病負擔就達到106億美元。
Globally, norovirus has become the leading cause of pediatric gastroenteritis in health care settings in countries that have adopted a rotavirus vaccine program.1 Pediatric deaths in the United States due to norovirus are rare, but they are much more common in the developing world.
在全球範圍內,在已採用輪狀病毒疫苗計劃的國家,諾如病毒已成爲醫療機構中小兒胃腸炎的主要病因。1 在美國,諾如病毒導致的兒科死亡很少見,但在發展中國家更爲常見。
This Phase I trial was conducted in South Africa (trial #20230307), and partially funded by the Bill & Melinda Gates Foundation. More complete results, including other immunogenicity measures, will be reported in a future scientific manuscript.
該I期試驗在南非進行(試驗 #20230307),部分資金由比爾和梅琳達·蓋茨基金會提供。更完整的結果,包括其他免疫原性測量,將在未來的科學手稿中報告。
About the VXA-NVV-108 Clinical Trial
關於 VXA-NVV-108 臨床試驗
This Phase 1, multicenter, randomized, double-blind, placebo-controlled single dose, dose-ranging study is designed to evaluate the safety, tolerability, and immunogenicity of orally administered bivalent GI.1/GII.4 norovirus vaccine in healthy lactating females 18-43 years of age. The study enrolled 76 subjects at five sites in South Africa. Subjects were randomized into high- or medium-dose vaccine (N=30 for each arm) or placebo (N=16). The primary endpoint results were:
這項1期、多中心、隨機、雙盲、安慰劑對照的單劑量、劑量範圍研究旨在評估18-43歲健康哺乳期女性口服二價GI.1/GII.4諾如病毒疫苗的安全性、耐受性和免疫原性。該研究在南非的五個地點招收了76名受試者。受試者被隨機分成高劑量或中劑量疫苗(每組 N=30)或安慰劑(N = 16)。主要終點結果是:
- Serum VP1-specific IgA rose an average of 5.6 fold in response to GI.1 and 4.4 fold in response to GII.4 in the high dose group, similar to the response observed in a previous Vaxart bivalent study conducted in adults 18-55 years of age in the United States.
- Breastmilk VP1-specific IgA rose on average 4.0 fold in response to G1.1 and 6.0 fold in response to GII.4 in the high dose group.
- The vaccine was well tolerated, with no SAEs, no adverse events of special interest (AESIs) and no new onset of chronic illness (NOCIs) observed through the active period.
- 在高劑量組中,血清VP1特異性IgA對GI.1的反應平均上升了5.6倍,對GII.4的反應平均上升了4.4倍,這與先前在美國對18-55歲的成年人進行的Vaxart二價研究中觀察到的反應類似。
- 母乳VP1特異性IgA對G1.1的反應平均上升了4.0倍,在高劑量組中,對GII.4的反應平均上升了6.0倍。
- 該疫苗耐受性良好,在活躍期內沒有觀察到SAE,沒有特別關注的不良事件(AESI),也沒有觀察到新的慢性病發作(NOCI)。
Further information, including information about study funding, can be found in Vaxart's press release of December 1, 2022, as well as Vaxart's latest annual filing with the Securities and Exchange Commission.
更多信息,包括有關研究資助的信息,可以在Vaxart於2022年12月1日發佈的新聞稿以及Vaxart向美國證券交易委員會提交的最新年度文件中找到。
1 Shah and Hall, Infect Dis Clin North Am. 2018 Mar; 32(1): 103-118.
1 沙阿和霍爾, Infect Disclin,2018 年 3 月;32 (1):103-118。
About Vaxart
Vaxart is a clinical-stage biotechnology company developing a range of oral recombinant vaccines based on its proprietary delivery platform. Vaxart vaccines are designed to be administered using pills that can be stored and shipped without refrigeration and eliminate the risk of needle-stick injury. Vaxart believes that its proprietary pill vaccine delivery platform is suitable to deliver recombinant vaccines, positioning the company to develop oral versions of currently marketed vaccines and to design recombinant vaccines for new indications. Vaxart's development programs currently include pill vaccines designed to protect against coronavirus, norovirus, and influenza, as well as a therapeutic vaccine for human papillomavirus (HPV), Vaxart's first immune-oncology indication. Vaxart has filed broad domestic and international patent applications covering its proprietary technology and creations for oral vaccination using adenovirus and TLR3 agonists.
關於 Vaxart
Vaxart是一家臨床階段的生物技術公司,基於其專有的交付平台開發一系列口服重組疫苗。Vaxart疫苗設計爲使用藥丸接種,這些藥丸無需冷藏即可儲存和運輸,並消除了針刺受傷的風險。Vaxart認爲,其專有的藥丸疫苗交付平台適合提供重組疫苗,這使該公司能夠開發當前上市疫苗的口服版本併爲新適應症設計重組疫苗。Vaxart的開發計劃目前包括旨在預防冠狀病毒、諾如病毒和流感的藥丸疫苗,以及針對人乳頭瘤病毒(HPV)的治療性疫苗,這是Vaxart的第一個免疫腫瘤學適應症。Vaxart已經提交了廣泛的國內和國際專利申請,涵蓋了其使用腺病毒和TLR3激動劑進行口服疫苗的專有技術和創新。
Note Regarding Forward-Looking Statements
This press release contains forward-looking statements that involve substantial risks and uncertainties. All statements, other than statements of historical facts, included in this press release regarding Vaxart's strategy, prospects, plans and objectives, results from preclinical and clinical trials and the timing of such results, commercialization agreements and licenses, and beliefs and expectations of management are forward-looking statements. These forward-looking statements may be accompanied by such words as "should," "believe," "could," "potential," "will," "expected," "anticipate," "plan," and other words and terms of similar meaning. Examples of such statements include, but are not limited to, statements relating to Vaxart's ability to develop and commercialize its product candidates, including its vaccine booster products; Vaxart's expectations regarding clinical results and trial data, and the timing of receiving and reporting such clinical results and trial data; and Vaxart's expectations with respect to the effectiveness of its product candidates. Vaxart may not actually achieve the plans, carry out the intentions, or meet the expectations or projections disclosed in the forward-looking statements, and you should not place undue reliance on these forward-looking statements. Actual results or events could differ materially from the plans, intentions, expectations, and projections disclosed in the forward-looking statements. Various important factors could cause actual results or events to differ materially from the forward-looking statements that Vaxart makes, including uncertainties inherent in research and development, including the ability to meet anticipated clinical endpoints, commencement, and/or completion dates for clinical trials, regulatory submission dates, regulatory approval dates, and/or launch dates, as well as the possibility of unfavorable new clinical data and further analyses of existing clinical data; the risk that clinical trial data are subject to differing interpretations and assessments by regulatory authorities; whether regulatory authorities will be satisfied with the design of and results from the clinical studies; decisions by regulatory authorities impacting labeling, manufacturing processes, and safety that could affect the availability or commercial potential of any product candidate, including the possibility that Vaxart's product candidates may not be approved by the FDA or non-U.S. regulatory authorities; that, even if approved by the FDA or non-U.S. regulatory authorities, Vaxart's product candidates may not achieve broad market acceptance; that a Vaxart collaborator may not attain development and commercial milestones; that Vaxart or its partners may experience manufacturing issues and delays due to events within, or outside of, Vaxart's or its partners' control; difficulties in production, particularly in scaling up initial production, including difficulties with production costs and yields, quality control, including stability of the product candidate and quality assurance testing, shortages of qualified personnel or key raw materials, and compliance with strictly enforced federal, state, and foreign regulations; that Vaxart may not be able to obtain, maintain, and enforce necessary patent and other intellectual property protection; that Vaxart's capital resources may be inadequate; Vaxart's ability to resolve pending legal matters; Vaxart's ability to obtain sufficient capital to fund its operations on terms acceptable to Vaxart, if at all; the impact of government healthcare proposals and policies; competitive factors; and other risks described in the "Risk Factors" sections of Vaxart's Quarterly and Annual Reports filed with the SEC. Vaxart does not assume any obligation to update any forward-looking statements, except as required by law.
關於前瞻性陳述的說明
本新聞稿包含涉及重大風險和不確定性的前瞻性陳述。除歷史事實陳述外,本新聞稿中有關Vaxart的戰略、前景、計劃和目標、臨床前和臨床試驗結果以及這些結果的發佈時間、商業化協議和許可以及管理層的信念和期望的所有陳述,均爲前瞻性陳述。這些前瞻性陳述可能伴有 “應該”、“相信”、“可能”、“潛在”、“將”、“預期”、“預期”、“計劃” 等詞語以及其他具有類似含義的詞語和術語。此類聲明的示例包括但不限於與Vaxart開發和商業化其候選產品(包括疫苗增強產品)的能力有關的聲明;Vaxart對臨床結果和試驗數據的期望,以及接收和報告此類臨床結果和試驗數據的時機;以及Vaxart對其候選產品有效性的期望。Vaxart可能無法實際實現計劃、執行意圖或滿足前瞻性陳述中披露的預期或預測,您不應過分依賴這些前瞻性陳述。實際結果或事件可能與前瞻性陳述中披露的計劃、意圖、預期和預測存在重大差異。各種重要因素可能導致實際結果或事件與Vaxart的前瞻性陳述存在重大差異,包括研發中固有的不確定性,包括滿足預期臨床終點的能力、臨床試驗的開始和/或完成日期、監管機構提交日期、監管批准日期和/或啓動日期,以及可能出現不利的新臨床數據和對現有臨床數據的進一步分析;臨床試驗數據受到不同影響的風險監管機構的解釋和評估;監管機構是否會對臨床研究的設計和結果感到滿意;可能影響任何候選產品的可用性或商業潛力的監管機構做出的決定,包括Vaxart的候選產品可能未獲得FDA或非美國監管機構批准的可能性;即使獲得FDA或非美國監管機構的批准,Vaxart的候選產品也可能未獲得廣泛的市場接受;Vaxart合作者可能無法實現開發和商業里程碑;由於Vaxart或其合作伙伴控制範圍內或之外的事件,Vaxart或其合作伙伴可能會遇到製造問題和延誤;生產困難,特別是擴大初始生產方面的困難,包括生產成本和產量方面的困難,質量控制,包括候選產品的穩定性和質量保證測試,合格人員或關鍵原材料短缺,以及遵守情況嚴格執行聯邦、州和外國法規;Vaxart可能無法獲得、維持和執行必要的專利和其他知識產權保護;Vaxart的資本資源可能不足;Vaxart解決未決法律問題的能力;Vaxart獲得足夠資本以Vaxart可以接受的條件爲其運營提供資金的能力;政府醫療保健提案和政策的影響;競爭因素;以及其他風險在 Vaxart 季度和年度的 “風險因素” 部分中進行了描述向美國證券交易委員會提交的報告。除非法律要求,否則Vaxart不承擔任何更新任何前瞻性陳述的義務。
Contacts
聯繫人
Vaxart Media Relations:
Mark Herr
Vaxart, Inc.
mherr@vaxart.com
(203) 517-8957
Vaxart 媒體關係部:
馬克·赫爾
Vaxart, Inc.
mherr@vaxart.com
(203) 517-8957
Investor Relations:
Andrew Blazier
FINN Partners
IR@vaxart.com
(646) 871-8486
投資者關係:
安德魯·布拉齊爾
FINN 合作伙伴
IR@vaxart.com
(646) 871-8486
Source: Vaxart, Inc.
來源:Vaxart, Inc.