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  1. Article ; Online: A dual-receptor T-cell platform with Ab-TCR and costimulatory receptor achieves specificity and potency against AML.

    Dao, Tao / Xiong, Guangyan / Mun, Sung Soo / Meyerberg, Jeremy / Korontsvit, Tatyana / Xiang, Jingyi / Cui, Ziyou / Chang, Aaron Y / Jarvis, Casey / Cai, Winson / Luo, Hanzhi / Pierson, Aspen / Daniyan, Anthony / Yoo, Sarah / Takao, Sumiko / Kharas, Michael / Kentsis, Alex / Liu, Cheng / Scheinberg, David A

    Blood

    2024  Volume 143, Issue 6, Page(s) 507–521

    Abstract: Abstract: Chimeric antigen receptor T-cell (CAR T) therapy has produced remarkable clinical responses in B-cell neoplasms. However, many challenges limit this class of agents for the treatment of other cancer types, in particular the lack of tumor- ... ...

    Abstract Abstract: Chimeric antigen receptor T-cell (CAR T) therapy has produced remarkable clinical responses in B-cell neoplasms. However, many challenges limit this class of agents for the treatment of other cancer types, in particular the lack of tumor-selective antigens for solid tumors and other hematological malignancies, such as acute myeloid leukemia (AML), which may be addressed without significant risk of severe toxicities while providing sufficient abundance for efficient tumor suppression. One approach to overcome this hurdle is dual targeting by an antibody-T-cell receptor (AbTCR) and a chimeric costimulatory signaling receptor (CSR) to 2 different antigens, in which both antigens are found together on the cancer cells but not together on normal cells. To explore this proof of concept in AML, we engineered a new T-cell format targeting Wilms tumor 1 protein (WT1) and CD33; both are highly expressed on most AML cells. Using an AbTCR comprising a newly developed TCR-mimic monoclonal antibody against the WT1 RMFPNAPYL (RMF) epitope/HLA-A2 complex, ESK2, and a secondary CSR comprising a single-chain variable fragment directed to CD33 linked to a truncated CD28 costimulatory fragment, this unique platform confers specific T-cell cytotoxicity to the AML cells while sparing healthy hematopoietic cells, including CD33+ myelomonocytic normal cells. These data suggest that this new platform, named AbTCR-CSR, through the combination of a AbTCR CAR and CSR could be an effective strategy to reduce toxicity and improve specificity and clinical outcomes in adoptive T-cell therapy in AML.
    MeSH term(s) Humans ; T-Lymphocytes ; Receptors, Antigen, T-Cell ; Leukemia, Myeloid, Acute/pathology ; Immunotherapy, Adoptive ; Single-Chain Antibodies
    Chemical Substances Receptors, Antigen, T-Cell ; Single-Chain Antibodies
    Language English
    Publishing date 2024-05-01
    Publishing country United States
    Document type Journal Article
    ZDB-ID 80069-7
    ISSN 1528-0020 ; 0006-4971
    ISSN (online) 1528-0020
    ISSN 0006-4971
    DOI 10.1182/blood.2023021054
    Database MEDical Literature Analysis and Retrieval System OnLINE

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  2. Article: Dual targeting ovarian cancer by Muc16 CAR-T cells secreting a bispecific T cell engager antibody for an intracellular tumor antigen WT1.

    Mun, Sung Soo / Peraro, Leila / Meyerberg, Jeremy / Korontsvit, Tatyana / Malviya, Manish / Gardner, Thomas / Kyi, Chrisann / O'Cearbhaill, Roisin E / Liu, Cheng / Dao, Tao / Scheinberg, David A

    Research square

    2023  

    Abstract: Epithelial ovarian cancer is the most lethal of gynecological cancers. The therapeutic efficacy of chimeric antigen receptor (CAR) T cell directed against single antigens is limited by the heterogeneous target antigen expression in epithelial ovarian ... ...

    Abstract Epithelial ovarian cancer is the most lethal of gynecological cancers. The therapeutic efficacy of chimeric antigen receptor (CAR) T cell directed against single antigens is limited by the heterogeneous target antigen expression in epithelial ovarian tumors. To overcome this limitation, we describe an engineered cell with both dual targeting and orthogonal cytotoxic modalities directed against two tumor antigens that are highly expressed on ovarian cancer cells: cell surface Muc16 and intracellular WT1. Muc16-specific CAR-T cells (4H11) were engineered to secrete a bispecific T cell engager (BiTE) constructed from a TCR mimic antibody (ESK1) reactive with the WT1-derived epitope RMFPNAPYL (RMF) presented by HLA-A2 molecules. The secreted ESK1 BiTE recruited and redirected other T cells to WT1 on the tumor cells. We show that ESK1 BiTE-secreting 4H11 CAR-T cells exhibited enhanced anticancer activity against cancer cells with low Muc16 expression, compared to 4H11 CAR-T cells alone, both in vitro and in mouse tumor models. Dual orthogonal cytotoxic modalities with different specificities targeting both surface and intracellular tumor-associated antigens present a promising strategy to overcome resistance to CAR-T cell therapy in epithelial ovarian cancer and other cancers.
    Language English
    Publishing date 2023-05-08
    Publishing country United States
    Document type Preprint
    DOI 10.21203/rs.3.rs-2887299/v1
    Database MEDical Literature Analysis and Retrieval System OnLINE

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  3. Article ; Online: Dual targeting ovarian cancer by Muc16 CAR T cells secreting a bispecific T cell engager antibody for an intracellular tumor antigen WT1.

    Mun, Sung Soo / Meyerberg, Jeremy / Peraro, Leila / Korontsvit, Tatyana / Gardner, Thomas / Malviya, Manish / Kyi, Chrisann / O'Cearbhaill, Roisin E / Liu, Cheng / Dao, Tao / Scheinberg, David A

    Cancer immunology, immunotherapy : CII

    2023  Volume 72, Issue 11, Page(s) 3773–3786

    Abstract: Epithelial ovarian cancer is the most lethal of gynecological cancers. The therapeutic efficacy of chimeric antigen receptor (CAR) T cell directed against single antigens is limited by the heterogeneous target antigen expression in epithelial ovarian ... ...

    Abstract Epithelial ovarian cancer is the most lethal of gynecological cancers. The therapeutic efficacy of chimeric antigen receptor (CAR) T cell directed against single antigens is limited by the heterogeneous target antigen expression in epithelial ovarian tumors. To overcome this limitation, we describe an engineered cell with both dual targeting and orthogonal cytotoxic modalities directed against two tumor antigens that are highly expressed on ovarian cancer cells: cell surface Muc16 and intracellular WT1. Muc16-specific CAR T cells (4H11) were engineered to secrete a bispecific T cell engager (BiTE) constructed from a TCR mimic antibody (ESK1) reactive with the WT1-derived epitope RMFPNAPYL (RMF) presented by HLA-A2 molecules. The secreted ESK1 BiTE recruited and redirected other T cells to WT1 on the tumor cells. We show that ESK1 BiTE-secreting 4H11 CAR T cells exhibited enhanced anticancer activity against cancer cells with low Muc16 expression, compared to 4H11 CAR T cells alone, both in vitro and in mouse tumor models. Dual orthogonal cytotoxic modalities with different specificities targeting both surface and intracellular tumor-associated antigens present a promising strategy to overcome resistance to CAR T cell therapy in epithelial ovarian cancer and other cancers.
    MeSH term(s) Humans ; Mice ; Female ; Animals ; Carcinoma, Ovarian Epithelial/therapy ; Receptors, Chimeric Antigen ; Ovarian Neoplasms/therapy ; Antigens, Neoplasm ; T-Lymphocytes ; WT1 Proteins
    Chemical Substances Receptors, Chimeric Antigen ; Antigens, Neoplasm ; WT1 protein, human ; WT1 Proteins ; WT1 protein, mouse
    Language English
    Publishing date 2023-08-27
    Publishing country Germany
    Document type Journal Article
    ZDB-ID 195342-4
    ISSN 1432-0851 ; 0340-7004
    ISSN (online) 1432-0851
    ISSN 0340-7004
    DOI 10.1007/s00262-023-03529-w
    Database MEDical Literature Analysis and Retrieval System OnLINE

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