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      Molecular Pathways: Mucins and Drug Delivery in Cancer

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          Abstract

          Over the past few decades, clinical and preclinical studies have clearly demonstrated the role of mucins in tumor development. It is well established that mucins form a barrier impeding drug access to target sites, leading to cancer chemoresistance. Recently gained knowledge regarding core enzyme synthesis has opened avenues to explore the possibility of disrupting mucin synthesis to improve drug efficacy. Cancer cells exploit aberrant mucin synthesis to efficiently mask the epithelial cells and ensure survival under hostile tumor microenvironment conditions. However, O-glycan synthesis enzyme core 2 beta 1,6 N-acetylglucosaminyltransferase (GCNT3/C2GnT-2) is overexpressed in Kras-driven mouse and human cancer, and inhibition of GCNT3 has been shown to disrupt mucin synthesis. This previously unrecognized developmental pathway might be responsible for aberrant mucin biosynthesis and chemoresistance. In this molecular pathways article, we briefly discuss the potential role of mucin synthesis in cancers, ways to improve drug delivery and disrupt mucin mesh to overcome chemoresistance by targeting mucin synthesis, and the unique opportunity to target the GCNT3 pathway for the prevention and treatment of cancers.

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          Author and article information

          Journal
          9502500
          8794
          Clin Cancer Res
          Clin. Cancer Res.
          Clinical cancer research : an official journal of the American Association for Cancer Research
          1078-0432
          27 June 2018
          30 December 2016
          15 March 2017
          10 July 2018
          : 23
          : 6
          : 1373-1378
          Affiliations
          Center for Cancer Prevention and Drug Development, Hematology and Oncology Section, Stephenson Cancer Center, University of Oklahoma Health Sciences Center, Oklahoma City, OK, USA
          Author notes
          [* ] Corresponding Author: Center for Cancer Prevention and Drug Development, 975 NE 10 th Street, BRC II, Room 211, OUHSC, Oklahoma City, OK, 73104, USA. Phone: +1 405-271-3224, Fax: +1 405-271-3225, altaf-mohammed@ 123456ouhsc.edu (Altaf Mohammed); cv-rao@ 123456ouhsc.edu (C.V. Rao)
          Article
          PMC6038927 PMC6038927 6038927 nihpa839545
          10.1158/1078-0432.CCR-16-0862
          6038927
          28039261
          dec4aeb7-f099-4265-a48d-8b3ff2ac12c9
          History
          Categories
          Article

          prevention,talniflumate,GCNT3,cancer,drug delivery,mucins,molecular pathways,treatment

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