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Efficient Gene Silencing in Brain Tumors with Hydrophobically Modified siRNAs.


ABSTRACT: Glioblastoma (GBM) is the most common and lethal form of primary brain tumor with dismal median and 2-year survivals of 14.5 months and 18%, respectively. The paucity of new therapeutic agents stems from the complex biology of a highly adaptable tumor that uses multiple survival and proliferation mechanisms to circumvent current treatment approaches. Here, we investigated the potency of a new generation of siRNAs to silence gene expression in orthotopic brain tumors generated by transplantation of human glioma stem-like cells in athymic nude mice. We demonstrate that cholesterol-conjugated, nuclease-resistant siRNAs (Chol-hsiRNAs) decrease mRNA and silence luciferase expression by 90% in vitro in GBM neurospheres. Furthermore, Chol-hsiRNAs distribute broadly in brain tumors after a single intratumoral injection, achieving sustained and potent (>45% mRNA and >90% protein) tumor-specific gene silencing. This readily available platform is sequence-independent and can be adapted to target one or more candidate GBM driver genes, providing a straightforward means of modulating GBM biology in vivoMol Cancer Ther; 17(6); 1251-8. ©2018 AACR.

SUBMITTER: Osborn MF 

PROVIDER: S-EPMC5984726 | biostudies-literature | 2018 Jun

REPOSITORIES: biostudies-literature

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Efficient Gene Silencing in Brain Tumors with Hydrophobically Modified siRNAs.

Osborn Maire F MF   Coles Andrew H AH   Golebiowski Diane D   Echeverria Dimas D   Moazami Michael P MP   Watts Jonathan K JK   Sena-Esteves Miguel M   Khvorova Anastasia A  

Molecular cancer therapeutics 20180413 6


Glioblastoma (GBM) is the most common and lethal form of primary brain tumor with dismal median and 2-year survivals of 14.5 months and 18%, respectively. The paucity of new therapeutic agents stems from the complex biology of a highly adaptable tumor that uses multiple survival and proliferation mechanisms to circumvent current treatment approaches. Here, we investigated the potency of a new generation of siRNAs to silence gene expression in orthotopic brain tumors generated by transplantation  ...[more]

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