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PEPT1 is essential for the growth of pancreatic cancer cells: a viable drug target

PEPT1 is a proton-coupled peptide transporter that is up-regulated in PDAC cell lines and PDXs, with little expression in the normal pancreas. However, the relevance of this up-regulation to cancer progression and the mechanism of up-regulation have not been investigated. Herein, we show that PEPT1...

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Autores principales: Schniers, Bradley K., Rajasekaran, Devaraja, Korac, Ksenija, Sniegowski, Tyler, Ganapathy, Vadivel, Bhutia, Yangzom D.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Portland Press Ltd. 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8589330/
https://www.ncbi.nlm.nih.gov/pubmed/34569600
http://dx.doi.org/10.1042/BCJ20210377
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author Schniers, Bradley K.
Rajasekaran, Devaraja
Korac, Ksenija
Sniegowski, Tyler
Ganapathy, Vadivel
Bhutia, Yangzom D.
author_facet Schniers, Bradley K.
Rajasekaran, Devaraja
Korac, Ksenija
Sniegowski, Tyler
Ganapathy, Vadivel
Bhutia, Yangzom D.
author_sort Schniers, Bradley K.
collection PubMed
description PEPT1 is a proton-coupled peptide transporter that is up-regulated in PDAC cell lines and PDXs, with little expression in the normal pancreas. However, the relevance of this up-regulation to cancer progression and the mechanism of up-regulation have not been investigated. Herein, we show that PEPT1 is not just up-regulated in a large panel of PDAC cell lines and PDXs but is also functional and transport-competent. PEPT2, another proton-coupled peptide transporter, is also overexpressed in PDAC cell lines and PDXs, but is not functional due to its intracellular localization. Using glibenclamide as a pharmacological inhibitor of PEPT1, we demonstrate in cell lines in vitro and mouse xenografts in vivo that inhibition of PEPT1 reduces the proliferation of the cancer cells. These findings are supported by genetic knockdown of PEPT1 with shRNA, wherein the absence of the transporter significantly attenuates the growth of cancer cells, both in vitro and in vivo, suggesting that PEPT1 is critical for the survival of cancer cells. We also establish that the tumor-derived lactic acid (Warburg effect) in the tumor microenvironment supports the transport function of PEPT1 in the maintenance of amino acid nutrition in cancer cells by inducing MMPs and DPPIV to generate peptide substrates for PEPT1 and by generating a H(+) gradient across the plasma membrane to energize PEPT1. Taken collectively, these studies demonstrate a functional link between PEPT1 and extracellular protein breakdown in the tumor microenvironment as a key determinant of pancreatic cancer growth, thus identifying PEPT1 as a potential therapeutic target for PDAC.
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spelling pubmed-85893302021-11-18 PEPT1 is essential for the growth of pancreatic cancer cells: a viable drug target Schniers, Bradley K. Rajasekaran, Devaraja Korac, Ksenija Sniegowski, Tyler Ganapathy, Vadivel Bhutia, Yangzom D. Biochem J Cancer PEPT1 is a proton-coupled peptide transporter that is up-regulated in PDAC cell lines and PDXs, with little expression in the normal pancreas. However, the relevance of this up-regulation to cancer progression and the mechanism of up-regulation have not been investigated. Herein, we show that PEPT1 is not just up-regulated in a large panel of PDAC cell lines and PDXs but is also functional and transport-competent. PEPT2, another proton-coupled peptide transporter, is also overexpressed in PDAC cell lines and PDXs, but is not functional due to its intracellular localization. Using glibenclamide as a pharmacological inhibitor of PEPT1, we demonstrate in cell lines in vitro and mouse xenografts in vivo that inhibition of PEPT1 reduces the proliferation of the cancer cells. These findings are supported by genetic knockdown of PEPT1 with shRNA, wherein the absence of the transporter significantly attenuates the growth of cancer cells, both in vitro and in vivo, suggesting that PEPT1 is critical for the survival of cancer cells. We also establish that the tumor-derived lactic acid (Warburg effect) in the tumor microenvironment supports the transport function of PEPT1 in the maintenance of amino acid nutrition in cancer cells by inducing MMPs and DPPIV to generate peptide substrates for PEPT1 and by generating a H(+) gradient across the plasma membrane to energize PEPT1. Taken collectively, these studies demonstrate a functional link between PEPT1 and extracellular protein breakdown in the tumor microenvironment as a key determinant of pancreatic cancer growth, thus identifying PEPT1 as a potential therapeutic target for PDAC. Portland Press Ltd. 2021-10-29 2021-10-21 /pmc/articles/PMC8589330/ /pubmed/34569600 http://dx.doi.org/10.1042/BCJ20210377 Text en © 2021 The Author(s) https://creativecommons.org/licenses/by/4.0/This is an open access article published by Portland Press Limited on behalf of the Biochemical Society and distributed under the Creative Commons Attribution License 4.0 (CC BY) (https://creativecommons.org/licenses/by/4.0/) . Open access for this article was enabled by the participation of Texas Tech University Health Sciences Center in an all-inclusive Read & Publish pilot with Portland Press and the Biochemical Society under a transformative agreement with EBSCO.
spellingShingle Cancer
Schniers, Bradley K.
Rajasekaran, Devaraja
Korac, Ksenija
Sniegowski, Tyler
Ganapathy, Vadivel
Bhutia, Yangzom D.
PEPT1 is essential for the growth of pancreatic cancer cells: a viable drug target
title PEPT1 is essential for the growth of pancreatic cancer cells: a viable drug target
title_full PEPT1 is essential for the growth of pancreatic cancer cells: a viable drug target
title_fullStr PEPT1 is essential for the growth of pancreatic cancer cells: a viable drug target
title_full_unstemmed PEPT1 is essential for the growth of pancreatic cancer cells: a viable drug target
title_short PEPT1 is essential for the growth of pancreatic cancer cells: a viable drug target
title_sort pept1 is essential for the growth of pancreatic cancer cells: a viable drug target
topic Cancer
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8589330/
https://www.ncbi.nlm.nih.gov/pubmed/34569600
http://dx.doi.org/10.1042/BCJ20210377
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