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One-shot dual gene editing for drug-resistant pancreatic cancer therapy
  • Won, Eun Jeong ;
  • Park, Hyeji ;
  • Chang, Seung Hee ;
  • Kim, Jin Hyun ;
  • Kwon, Hojeong ;
  • Cho, Young Seok ;
  • Yoon, Tae Jong
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Publication Year
2021-12-01
Journal
Biomaterials
Publisher
Elsevier Ltd
Citation
Biomaterials, Vol.279
Keyword
Drug-resistanceGene editingNanoliposomePancreatic cancerProtein delivery
Mesh Keyword
Cancer therapyDrug-resistanceDuctal adenocarcinomasGemcitabineGene editingGenes mutationNanoliposomesP53 genePancreatic cancersProtein deliveryCarcinoma, Pancreatic DuctalCell Line, TumorDrug Resistance, NeoplasmGene EditingHumansPancreatic NeoplasmsPharmaceutical Preparations
All Science Classification Codes (ASJC)
BioengineeringCeramics and CompositesBiophysicsBiomaterialsMechanics of Materials
Abstract
It is challenging to diagnose patients with pancreatic ductal adenocarcinoma (PDAC) early on, and their treatment is often complex. Gemcitabine (GEM) is the first-line treatment for PDAC, but its efficacy is limited in most patients due to the GEM resistance from KRAS and P53 gene mutations. We describe the correction of a double gene mutation and therapeutic effect for the GEM resistant PDAC. Bio-available nanoliposomes (NL) possessing Cas9-ribonucleoproteins and adenine-base editors were developed to conduct KRAS and P53 mutation gene editing directly. NLs were conjugated with EGFR antibodies to tumor-specific delivery, and the anti-cancer effect was verified in vitro and in vivo Model. Our GEM-combinatorial therapeutic strategies using double gene editing systems with one-shot may be a potent therapy for PDAC, overcoming chemoresistance.
ISSN
1878-5905
Language
eng
URI
https://aurora.ajou.ac.kr/handle/2018.oak/32372
https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=85118925316&origin=inward
DOI
https://doi.org/2-s2.0-85118925316
Journal URL
http://www.journals.elsevier.com/biomaterials/
Type
Article
Funding
This work was supported by the GRRC program of Gyeonggi province ( GRRC 2016B02 , Photonics-Medical Convergence Technology Research Center) and funded by a grant (No. 2019R1F1A1058879 ) from the National Foundation Research of Korea .
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