Amphiphilic nanocarrier-induced modulation of PLK1 and miR-34a leads to improved therapeutic response in pancreatic cancer.
Hadas GiboriShay EliyahuAdva KrivitskyDikla Ben-ShushanYana EpshteinGalia TiramRachel BlauPaula OfekJoo Sang LeeEytan RuppinLimor LandsmanIris BarshackTalia GolanEmmanuelle MerquiolGalia BlumRonit Satchi-FainaroPublished in: Nature communications (2018)
The heterogeneity of pancreatic ductal adenocarcinoma (PDAC) suggests that successful treatment might rely on simultaneous targeting of multiple genes, which can be achieved by RNA interference-based therapeutic strategies. Here we show a potent combination of microRNA and siRNA delivered by an efficient nanocarrier to PDAC tumors. Using proteomic-microRNA profiles and survival data of PDAC patients from TCGA, we found a novel signature for prolonged survival. Accordingly, we used a microRNA-mimic to increase miR-34a together with siRNA to silence PLK1 oncogene. For in vivo dual-targeting of this combination, we developed a biodegradable amphiphilic polyglutamate amine polymeric nanocarrier (APA). APA-miRNA-siRNA polyplexes systemically administered to orthotopically inoculated PDAC-bearing mice showed no toxicity and accumulated at the tumor, resulting in an enhanced antitumor effect due to inhibition of MYC oncogene, a common target of both miR-34a and PLK1. Taken together, our findings warrant this unique combined polyplex's potential as a novel nanotherapeutic for PDAC.
Keyphrases
- drug delivery
- cancer therapy
- cell proliferation
- long non coding rna
- long noncoding rna
- end stage renal disease
- drug release
- newly diagnosed
- ejection fraction
- oxidative stress
- peritoneal dialysis
- chronic kidney disease
- prognostic factors
- machine learning
- type diabetes
- artificial intelligence
- transcription factor
- drug induced
- anti inflammatory
- deep learning
- stress induced