| Literature DB >> 29845742 |
Raquel Díaz1,2,3, Victor Pallarès4, Olivia Cano-Garrido1,2,3, Naroa Serna1,2,3, Laura Sánchez-García1,2,3, Aïda Falgàs3,4, Mireia Pesarrodona1,2,3, Ugutz Unzueta3,4, Alejandro Sánchez-Chardi5, Julieta M Sánchez1,6, Isolda Casanova3,4, Esther Vázquez1,2,3, Ramón Mangues3,4, Antonio Villaverde1,2,3.
Abstract
Under the unmet need of efficient tumor-targeting drugs for oncology, a recombinant version of the plant toxin ricin (the modular protein T22-mRTA-H6) is engineered to self-assemble as protein-only, CXCR4-targeted nanoparticles. The soluble version of the construct self-organizes as regular 11 nm planar entities that are highly cytotoxic in cultured CXCR4+ cancer cells upon short time exposure, with a determined IC50 in the nanomolar order of magnitude. The chemical inhibition of CXCR4 binding sites in exposed cells results in a dramatic reduction of the cytotoxic potency, proving the receptor-dependent mechanism of cytotoxicity. The insoluble version of T22-mRTA-H6 is, contrarily, moderately active, indicating that free, nanostructured protein is the optimal drug form. In animal models of acute myeloid leukemia, T22-mRTA-H6 nanoparticles show an impressive and highly selective therapeutic effect, dramatically reducing the leukemia cells affectation of clinically relevant organs. Functionalized T22-mRTA-H6 nanoparticles are then promising prototypes of chemically homogeneous, highly potent antitumor nanostructured toxins for precise oncotherapies based on self-mediated intracellular drug delivery.Entities:
Keywords: acute myeloid leukemia; nanoparticles; protein engineering; self-assembling; targeted drug delivery
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Year: 2018 PMID: 29845742 DOI: 10.1002/smll.201800665
Source DB: PubMed Journal: Small ISSN: 1613-6810 Impact factor: 13.281