Literature DB >> 24749405

Design of nanodrugs for miRNA targeting in tumor cells.

Byunghee Yoo, Subrata K Ghosh, Mohanraja Kumar, Anna Moore, Mehmet V Yigit, Zdravka Medarova.   

Abstract

The delivery of oligonucleotide antagonists to cytosolic RNA targets such as microRNA represents an avenue for the post-transcriptional control of cellular phenotype. In tumor cells, oncogenic miRNAs, termed oncomirs, are tightly linked to processes that ultimately determine cancer initiation, progression, and response to therapy. Therefore, the capacity to redirect tumor cell fate towards therapeutically beneficial phenotypes holds promise in a future clinical scenario. Previously, we have designed "nanodrugs" for the specific inhibition of oncogenic microRNAs in tumor cells. The basic design of these nanodrugs includes dextran coated iron oxide nanoparticles, conjugated to a tumor-targeting peptide, and a locked nucleic acid (LNA)-modified antisense oligonucleotide that stably binds and inhibits the complementary mature miRNA. Here, we focus on elucidating an optimal nanodrug design for effective miRNA inhibition in tumor cells. Specifically, we investigate the choice of chemical linker for the conjugation of the oligonucleotide to the nanoparticles and evaluate the contribution of tumor-cell targeting to nanodrug uptake and functionality. We find that short labile linkers (SPDP; N-Succinimidyl 3-(2-pyridyldithio)-propionate) are superior to non-labile short linkers (GMBS; N-(gamma-Maleimidobutyryloxy)succinimide ester) or non-labile long linkers (PEG24; Succinimidyl-([N-maleimidopropionamido]-24ethyleneglycol)ester) in terms of their capacity to gain access to the cytosolic cellular compartment and to engage their cognate miRNA. Furthermore, using the nanodrug design that incorporates SPDP as a linker, we establish that the addition of tumor-cell targeting through functionalization of the nanodrug with the alphavbeta3-specific cyclic RGDfK-PEG peptide does not confer an advantage in vitro at long incubation times required for inhibition.

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Year:  2014        PMID: 24749405      PMCID: PMC4174340          DOI: 10.1166/jbn.2014.1795

Source DB:  PubMed          Journal:  J Biomed Nanotechnol        ISSN: 1550-7033            Impact factor:   4.099


  26 in total

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  14 in total

1.  Combining miR-10b-Targeted Nanotherapy with Low-Dose Doxorubicin Elicits Durable Regressions of Metastatic Breast Cancer.

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Journal:  Cancer Res       Date:  2015-09-10       Impact factor: 12.701

2.  In Vivo Detection of miRNA Expression in Tumors Using an Activatable Nanosensor.

Authors:  Byunghee Yoo; Amol Kavishwar; Alana Ross; Pamela Pantazopoulos; Anna Moore; Zdravka Medarova
Journal:  Mol Imaging Biol       Date:  2016-02       Impact factor: 3.488

Review 3.  Next-generation superparamagnetic iron oxide nanoparticles for cancer theranostics.

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4.  Omniparticle Contrast Agent for Multimodal Imaging: Synthesis and Characterization in an Animal Model.

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5.  Switchable Fluorescence of Doxorubicin for Label-Free Imaging of Bioorthogonal Drug Release.

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6.  Therapy targeted to the metastatic niche is effective in a model of stage IV breast cancer.

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7.  Potent and selective effect of the mir-10b inhibitor MN-anti-mir10b in human cancer cells of diverse primary disease origin.

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8.  RNAi-Mediated PD-L1 Inhibition for Pancreatic Cancer Immunotherapy.

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Review 9.  Covalent Strategies for Targeting Messenger and Non-Coding RNAs: An Updated Review on siRNA, miRNA and antimiR Conjugates.

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10.  MicroRNA-710 regulates multiple pathways of carcinogenesis in murine metastatic breast cancer.

Authors:  Byunghee Yoo; Nikhil Meka; Patrick Sheedy; Ann-Marie Billig; Pamela Pantazopoulos; Zdravka Medarova
Journal:  PLoS One       Date:  2019-12-13       Impact factor: 3.240

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