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Selective targeting of point-mutated KRAS through artificial microRNAs
by
Fattore, Luigi
, Acunzo, Mario
, Veneziano, Dario
, Fassan, Matteo
, Kladney, Raleigh
, Zanesi, Nicola
, Coppola, Vincenzo
, Laganà, Alessandro
, Rizzotto, Lara
, Croce, Carlo M.
, Romano, Giulia
, Nigita, Giovanni
, Fadda, Paolo
in
Biological Sciences
/ Cancer
/ Coding
/ Complementarity
/ Diseases
/ Genes
/ Genetic transformation
/ Genetics
/ In vitro methods and tests
/ K-Ras protein
/ Lungs
/ miRNA
/ Molecules
/ Mutation
/ Pancreas
/ Pathogenesis
/ PNAS Plus
/ Ribonucleic acid
/ RNA
/ siRNA
/ Transcription
2017
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Selective targeting of point-mutated KRAS through artificial microRNAs
by
Fattore, Luigi
, Acunzo, Mario
, Veneziano, Dario
, Fassan, Matteo
, Kladney, Raleigh
, Zanesi, Nicola
, Coppola, Vincenzo
, Laganà, Alessandro
, Rizzotto, Lara
, Croce, Carlo M.
, Romano, Giulia
, Nigita, Giovanni
, Fadda, Paolo
in
Biological Sciences
/ Cancer
/ Coding
/ Complementarity
/ Diseases
/ Genes
/ Genetic transformation
/ Genetics
/ In vitro methods and tests
/ K-Ras protein
/ Lungs
/ miRNA
/ Molecules
/ Mutation
/ Pancreas
/ Pathogenesis
/ PNAS Plus
/ Ribonucleic acid
/ RNA
/ siRNA
/ Transcription
2017
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Selective targeting of point-mutated KRAS through artificial microRNAs
by
Fattore, Luigi
, Acunzo, Mario
, Veneziano, Dario
, Fassan, Matteo
, Kladney, Raleigh
, Zanesi, Nicola
, Coppola, Vincenzo
, Laganà, Alessandro
, Rizzotto, Lara
, Croce, Carlo M.
, Romano, Giulia
, Nigita, Giovanni
, Fadda, Paolo
in
Biological Sciences
/ Cancer
/ Coding
/ Complementarity
/ Diseases
/ Genes
/ Genetic transformation
/ Genetics
/ In vitro methods and tests
/ K-Ras protein
/ Lungs
/ miRNA
/ Molecules
/ Mutation
/ Pancreas
/ Pathogenesis
/ PNAS Plus
/ Ribonucleic acid
/ RNA
/ siRNA
/ Transcription
2017
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Selective targeting of point-mutated KRAS through artificial microRNAs
Journal Article
Selective targeting of point-mutated KRAS through artificial microRNAs
2017
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Overview
Mutated protein-coding genes drive the molecular pathogenesis of many diseases, including cancer. Specifically, mutated KRAS is a documented driver for malignant transformation, occurring early during the pathogenesis of cancers such as lung and pancreatic adenocarcinomas. Therapeutically, the indiscriminate targeting of wild-type and point-mutated transcripts represents an important limitation. Here, we leveraged on the design of miRNA-like artificial molecules (amiRNAs) to specifically target point-mutated genes, such as KRAS, without affecting their wild-type counterparts. Compared with an siRNA-like approach, the requirement of perfect complementarity of the microRNA seed region to a given target sequence in the microRNA/target model has proven to be a more efficient strategy, accomplishing the selective targeting of point-mutated KRAS in vitro and in vivo.
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