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    Home > Active Ingredient News > Drugs Articles > Co-founded by Dr. Wang Xiaodong!

    Co-founded by Dr. Wang Xiaodong!

    • Last Update: 2021-09-19
    • Source: Internet
    • Author: User
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    The latest announcement by the Center for Drug Evaluation (CDE) of the State Drug Administration of China, Viterilon (Beijing) Biotechnology Co.
    , Ltd.
    (Sironax, hereinafter referred to as Viterilon) declared a new class 1 drug SIR1-365 tablets, which has been implied by clinical trials Approved, intended to be developed for the treatment of infectious diseases related to systemic inflammatory response syndrome (SIRS)
    .

    Treatment of infectious diseases related to systemic inflammatory response syndrome (SIRS)
    .


    Viterilon is a global biomedical company focusing on the research and development of "first-in-class" new drugs , co-founded by Dr.
    Xiaodong Wang and Dr.
    Zhiyuan Zhang
    .


    Check the CDE official website.


    Co-founded by Dr.


    Screenshot source: CDE official website

    Public information shows that SIR1-365 is a receptor-interacting protein kinase 1 (receptor-interacting protein 1.
    RIP1) inhibitor
    .


    RIP1 is a serine/threonine protein kinase that can regulate a variety of biological signal transduction pathways, such as TNFα-mediated NFκB signal transduction, apoptosis, programmed cell necrosis, and inflammation


    SIR1-365 is a receptor-interacting protein 1.


    Inhibition of RIP1 kinase through small molecule drugs or gene editing can effectively prevent or reduce the development of a series of diseases

    Previously, Viterilon has registered in the United States to carry out a phase 1 clinical trial, which aims to study the safety and effectiveness of SIR1-365 in patients with severe COVID-19
    .

    Viterilon was established in 2018 to develop inhibitors for major discoveries in a variety of cell death fields , including apoptosis and necrosis
    .


    Public information shows that the company’s research and development projects are derived from the breakthrough scientific discoveries of apoptosis, necroptosis and other cell death mechanisms in Dr.


    Research and develop inhibitors for major discoveries in a variety of cell death fields including apoptosis and necrosis

    ▲The product pipeline of Viterilon (picture source: Viterilon's official website)

    ▲The product pipeline of Viterilon (picture source: Viterilon's official website)

    For the past many years, Dr.
    Xiaodong Wang’s laboratory has been studying the molecular mechanisms of programmed cell apoptosis and programmed cell necrosis, and discovered the important regulatory proteins RIP3 and MLKL (mixed lineage kinase domain-like protein) in cell necrosis
    .


    They used RIP3 and MLKL gene knockout mice to study the physiological significance of cell necrosis in the body, and found that the cell necrosis signaling pathway regulates the aging of the male mouse reproductive system


    The laboratory of Dr.
    Zhiyuan Zhang, co-founder of Viterilon, designed a RIP1 inhibitor
    .


    In mouse experiments, the compound can significantly inhibit the proliferation of seminal vesicle glands and delay the aging of fertility, while the level of male hormones is still maintained at a young level


    The compound can significantly inhibit the proliferation of seminal vesicle glands and delay the aging of reproductive functions, while the level of male hormones is still maintained at a young level

    ▲The management team of Viterilon (Image source: Viterilon's official website)

    ▲The management team of Viterilon (Image source: Viterilon's official website)

    According to the introduction of Viterilon's official website, the current RIP1 inhibitor project (SIR1) has become the fastest-growing product in the research pipeline of Viterilon
    .

    The clinical approval of SIR1-365 in China means that this RIP1 inhibitor is about to enter clinical studies in China
    .


    It is hoped that Viterilon SIR1-365 will progress smoothly in clinical research and make more breakthroughs as soon as possible


    Reference materials:

    Reference materials:

    [1] Center for Drug Evaluation of China National Medical Products Administration.


    [2] Weiteruilong official website.
    from http://122.
    10.
    100.
    59:8090/index.
    php/About/cpgx

    [3] Qiu Zhendong, Wang Weixing.
    Research progress of receptor-interacting protein 1 in some tumors of the digestive system[J].
    Abdominal Surgery, 2019.
    32(004):300-303.

    [3] Qiu Zhendong, Wang Weixing.
    Research progress of receptor-interacting protein 1 in some tumors of the digestive system[J].
    Abdominal Surgery, 2019.
    32(004):300-303.

    [4]He, S.
    , Wang, L.
    , Miao, L.
    , Wang, T.
    , Du, F.
    , Zhao, L.
    , and Wang, X.
    (2009).
    Receptor interacting protein kinase-3 determines cellular necrotic response to TNF-alpha.
    Cell 137.
    1100-1111.

    [4]He, S.
    , Wang, L.
    , Miao, L.
    , Wang, T.
    , Du, F.
    , Zhao, L.
    , and Wang, X.
    (2009).
    Receptor interacting protein kinase-3 determines cellular necrotic response to TNF-alpha.
    Cell 137.
    1100-1111.

    [5]Sun, L.
    , Wang, H.
    , Wang, Z.
    , He, S.
    , Chen, S.
    , Liao, D.
    , Wang, L.
    , Yan, J.
    , Liu, W.
    , Lei, X.
    , et al.
    (2012).
    Mixed lineage kinase domain-like protein mediates necrosis signaling downstream of RIP3 kinase.
    Cell 148.
    213-227.

    [5]Sun, L.
    , Wang, H.
    , Wang, Z.
    , He, S.
    , Chen, S.
    , Liao, D.
    , Wang, L.
    , Yan, J.
    , Liu, W.
    , Lei, X.
    , et al.
    (2012).
    Mixed lineage kinase domain-like protein mediates necrosis signaling downstream of RIP3 kinase.
    Cell 148.
    213-227.

    [6]Li, D.
    , Meng, L.
    , Xu, T.
    , Su, Y.
    , Liu, X.
    , Zhang, Z.
    , and Wang, X.
    (2017).
    RIPK1-RIPK3-MLKL-dependent necrosis promotes the aging of mouse male reproductive system.
    Elife 6.

    [6]Li, D.
    , Meng, L.
    , Xu, T.
    , Su, Y.
    , Liu, X.
    , Zhang, Z.
    , and Wang, X.
    (2017).
    RIPK1-RIPK3-MLKL-dependent necrosis promotes the aging of mouse male reproductive system.
    Elife 6.
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