灭活全病毒流感疫苗(KM Biologics KK)(Inactivated whole virus influenza vaccine(KM Biologics KK))

概要

基本信息

药物类型

灭活疫苗、预防性疫苗

别名

KD 404、KD-404

靶点-

作用机制

免疫刺激剂

治疗领域

感染呼吸系统疾病

在研适应症

流感病毒感染

非在研适应症-

原研机构

KM Biologics KK

在研机构

Hokkaido UniversityMeiji Seika Kaisha Ltd.

KM Biologics KK

非在研机构-

最高研发阶段临床2期

首次获批日期-

最高研发阶段(中国)-

特殊审评-

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关联

2

项与灭活全病毒流感疫苗(KM Biologics KK) 相关的临床试验

JPRN-JapicCTI-184176 / Completed临床1/2期

KD-404 Phase I/II Study

开始日期2018-10-29

申办/合作机构-

JPRN-jRCT2080224115 / Completed临床1/2期

KD-404 Phase I/II Study

开始日期2018-10-29

申办/合作机构-

100 项与灭活全病毒流感疫苗(KM Biologics KK) 相关的临床结果

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100 项与灭活全病毒流感疫苗(KM Biologics KK) 相关的转化医学

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100 项与灭活全病毒流感疫苗(KM Biologics KK) 相关的专利（医药）

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92

项与灭活全病毒流感疫苗(KM Biologics KK) 相关的文献（医药）

2024-03-01·European journal of immunology

Inactivated whole virion vaccine protects K18‐hACE2 Tg mice against the Omicron SARS‐CoV‐2 variant via cross‐reactive T cells and nonneutralizing antibody responses

Article

作者: Astrakhantseva, Irina V ; Bondareva, Marina A ; Kruglov, Andrey A ; Volok, Viktor P ; Drutskaya, Marina S ; Apolokhov, Vasiliy D ; Zvartsev, Ruslan ; Semin, Iaroslav K ; Nedospasov, Sergei A ; Gogoleva, Violetta S ; Shustova, Elena Yu ; Kozlovskaya, Liubov I ; Ishmukhametov, Aydar A ; Lunin, Aleksandr S ; Ustyugov, Aleksey A

Abstract:

COVID‐19 is a systemic inflammatory disease initiated by SARS‐CoV‐2 virus infection. Multiple vaccines against the Wuhan variant of SARS‐CoV‐2 have been developed including a whole virion beta‐propiolactone‐inactivated vaccine based on the B.1.1 strain (CoviVac). Since most of the population has been vaccinated by targeting the original or early variants of SARS‐CoV‐2, the emergence of novel mutant variants raises concern over possible evasion of vaccine‐induced immune responses. Here, we report on the mechanism of protection by CoviVac, a whole virion‐based vaccine, against the Omicron variant. CoviVac‐immunized K18‐hACE2 Tg mice were protected against both prototype B.1.1 and BA.1‐like (Omicron) variants. Subsequently, vaccinated K18‐hACE2 Tg mice rapidly cleared the infection via cross‐reactive T‐cell responses and cross‐reactive, non‐neutralizing antibodies recognizing the Omicron variant Spike protein. Thus, our data indicate that efficient protection from SARS‐CoV‐2 variants can be achieved by the orchestrated action of cross‐reactive T cells and non‐neutralizing antibodies.

2023-01-01·Frontiers in immunology

Prolonging the delivery of influenza virus vaccine improves the quantity and quality of the induced immune responses in mice.

Article

作者: Beukema, Martin ; Huckriede, Anke ; Gong, Shuran ; Krammer, Florian ; Cox, Rebecca Jane ; Zhou, Fan ; Al-Jaawni, Kasem ; de Vries-Idema, Jacqueline J

Introduction:

Influenza vaccines play a vital role in protecting individuals from influenza virus infection and severe illness. However, current influenza vaccines have suboptimal efficacy, which is further reduced in cases where the vaccine strains do not match the circulating strains. One strategy to enhance the efficacy of influenza vaccines is by extended antigen delivery, thereby mimicking the antigen kinetics of a natural infection. Prolonging antigen availability was shown to quantitatively enhance influenza virus-specific immune responses but how it affects the quality of the induced immune response is unknown. Therefore, the current study aimed to investigate whether prolongation of the delivery of influenza vaccine improves the quality of the induced immune responses over that induced by prime-boost immunization.

Methods:

Mice were given daily doses of whole inactivated influenza virus vaccine for periods of 14, 21, or 28 days; the control group received prime-boost immunization with a 28 days interval.

Results:

Our data show that the highest levels of cellular and humoral immune responses were induced by 28 days of extended antigen delivery, followed by 21, and 14 days of delivery, and prime-boost immunization. Moreover, prolonging vaccine delivery also improved the quality of the induced antibody response, as indicated by higher level of high avidity antibodies, a balanced IgG subclass profile, and a higher level of cross-reactive antibodies.

Conclusions:

Our findings contribute to a better understanding of the immune response to influenza vaccination and have important implications for the design and development of future slow-release influenza vaccines.

2022-10-01·Emerging infectious diseases

Effectiveness of Whole-Virus COVID-19 Vaccine among Healthcare Personnel, Lima, Peru

Review

作者: Soto, Giselle ; Espinoza, Angelica ; Lessa, Fernanda C. ; Smith, Rachel ; Romero, Candice ; Grogl, Max ; Azziz-Baumgartner, Eduardo ; Bollinger, Susan ; Matos, Eduardo ; Silva, Maria ; Llanos-Cuentas, Alejandro ; Arriola, Carmen S. ; Prouty, Michael ; Olson, Natalie ; Westercamp, Matthew

In February 2021, Peru launched a COVID-19 vaccination campaign among healthcare personnel using an inactivated whole-virus vaccine. The manufacturer recommended 2 vaccine doses 21 days apart. We evaluated vaccine effectiveness among an existing multiyear influenza vaccine cohort at 2 hospitals in Lima. We analyzed data on 290 participants followed during February-May 2021. Participants completed a baseline questionnaire and provided weekly self-collected nasal swab samples; samples were tested by real-time reverse transcription PCR. Median participant follow-up was 2 (range 1-11) weeks. We performed multivariable logistic regression and adjusted for preselected characteristics. During the study, 25 (9%) participants tested SARS-CoV-2-positive. We estimated adjusted vaccine effectiveness at 95% (95% CI 70%-99%) among fully vaccinated participants and 100% (95% CI 88%-100%) among partially vaccinated participants. These data can inform the use and acceptance of inactivated whole-virus vaccine and support vaccination efforts in the region.

100 项与灭活全病毒流感疫苗(KM Biologics KK) 相关的药物交易

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