| Literature DB >> 34516826 |
Christian Hotz1, Timothy R Wagenaar2, Friederike Gieseke1, Dinesh S Bangari2, Michelle Callahan2, Hui Cao2, Jan Diekmann1, Mustafa Diken1,3, Christian Grunwitz1, Andy Hebert2, Karl Hsu2, Marie Bernardo2, Katalin Karikó1, Sebastian Kreiter1,3, Andreas N Kuhn1, Mikhail Levit2, Natalia Malkova2, Serena Masciari2, Jack Pollard2, Hui Qu2, Sue Ryan2, Abderaouf Selmi3, Julia Schlereth1, Kuldeep Singh2, Fangxian Sun2, Bodo Tillmann3, Tatiana Tolstykh2, William Weber2, Lena Wicke1, Sonja Witzel3, Qunyan Yu2, Yu-An Zhang2, Gang Zheng2, Joanne Lager2, Gary J Nabel2, Ugur Sahin1,3, Dmitri Wiederschain2.
Abstract
Local immunotherapy ideally stimulates immune responses against tumors while avoiding toxicities associated with systemic administration. Current strategies for tumor-targeted, gene-based delivery, however, are limited by adverse effects such as off-targeting or antivector immunity. We investigated the intratumoral administration of saline-formulated messenger (m)RNA encoding four cytokines that were identified as mediators of tumor regression across different tumor models: interleukin-12 (IL-12) single chain, interferon-α (IFN-α), granulocyte-macrophage colony-stimulating factor, and IL-15 sushi. Effective antitumor activity of these cytokines relied on multiple immune cell populations and was accompanied by intratumoral IFN-γ induction, systemic antigen-specific T cell expansion, increased granzyme B+ T cell infiltration, and formation of immune memory. Antitumor activity extended beyond the treated lesions and inhibited growth of distant tumors and disseminated tumors. Combining the mRNAs with immunomodulatory antibodies enhanced antitumor responses in both injected and uninjected tumors, thus improving survival and tumor regression. Consequently, clinical testing of this cytokine-encoding mRNA mixture is now underway.Entities:
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Year: 2021 PMID: 34516826 DOI: 10.1126/scitranslmed.abc7804
Source DB: PubMed Journal: Sci Transl Med ISSN: 1946-6234 Impact factor: 17.956