Oncogenic KRAS mutations enhance amino acid uptake by colorectal cancer cells via the hippo signaling effector YAP1

Oncogenic KRAS mutations enhance amino acid uptake by colorectal cancer cells via the hippo signaling effector YAP1

Oncogenic KRAS mutations develop unique metabolic dependencies on nutrients to support tumor metabolism and cell proliferation. In particular, KRAS mutant cancer cells exploit amino acids (AAs) such as glutamine and leucine, to accelerate energy metabolism, redox balance through glutathione synthesi...

Full description

Bibliographic Details
Main Authors: Palanivel Kandasamy, Inti Zlobec, Damian T. Nydegger, Jonai Pujol‐Giménez, Rajesh Bhardwaj, Senji Shirasawa, Toshiyuki Tsunoda, Matthias A. Hediger
Format: Article
Language:English
Published: Wiley 2021-10-01
Series:Molecular Oncology
Subjects:
amino acid transporters
oncogene
SLC1A5/ASCT2
SLC38A2/SNAT2
SLC7A5/LAT1
solute carriers
Online Access:https://doi.org/10.1002/1878-0261.12999
id doaj-b6fc7ae16925449f8d9d9da78bd65412
record_format Article
spelling doaj-b6fc7ae16925449f8d9d9da78bd654122021-10-02T00:23:46ZengWileyMolecular Oncology1574-78911878-02612021-10-0115102782280010.1002/1878-0261.12999Oncogenic KRAS mutations enhance amino acid uptake by colorectal cancer cells via the hippo signaling effector YAP1Palanivel Kandasamy0Inti Zlobec1Damian T. Nydegger2Jonai Pujol‐Giménez3Rajesh Bhardwaj4Senji Shirasawa5Toshiyuki Tsunoda6Matthias A. Hediger7Membrane Transport Discovery Lab Department of Nephrology and Hypertension, Inselspital University of Bern SwitzerlandTranslational Research Unit (TRU) Institute of Pathology University of Bern SwitzerlandMembrane Transport Discovery Lab Department of Nephrology and Hypertension, Inselspital University of Bern SwitzerlandMembrane Transport Discovery Lab Department of Nephrology and Hypertension, Inselspital University of Bern SwitzerlandMembrane Transport Discovery Lab Department of Nephrology and Hypertension, Inselspital University of Bern SwitzerlandDepartment of Cell Biology Faculty of Medicine Fukuoka University JapanDepartment of Cell Biology Faculty of Medicine Fukuoka University JapanMembrane Transport Discovery Lab Department of Nephrology and Hypertension, Inselspital University of Bern SwitzerlandOncogenic KRAS mutations develop unique metabolic dependencies on nutrients to support tumor metabolism and cell proliferation. In particular, KRAS mutant cancer cells exploit amino acids (AAs) such as glutamine and leucine, to accelerate energy metabolism, redox balance through glutathione synthesis and macromolecule biosynthesis. However, the identities of the amino acid transporters (AATs) that are prominently upregulated in KRAS mutant cancer cells, and the mechanism regulating their expression have not yet been systematically investigated. Here, we report that the majority of the KRAS mutant colorectal cancer (CRC) cells upregulate selected AATs (SLC7A5/LAT1, SLC38A2/SNAT2, and SLC1A5/ASCT2), which correlates with enhanced uptake of AAs such as glutamine and leucine. Consistently, knockdown of oncogenic KRAS downregulated the expression of AATs, thereby decreasing the levels of amino acids taken up by CRC cells. Moreover, overexpression of mutant KRAS upregulated the expression of AATs (SLC7A5/LAT1, SLC38A2/SNAT2, and SLC1A5/ASCT2) in KRAS wild‐type CRC cells and mouse embryonic fibroblasts. In addition, we show that the YAP1 (Yes‐associated protein 1) transcriptional coactivator accounts for increased expression of AATs and mTOR activation in KRAS mutant CRC cells. Specific knockdown of AATs by shRNAs or pharmacological blockage of AATs effectively inhibited AA uptake, mTOR activation, and cell proliferation. Collectively, we conclude that oncogenic KRAS mutations enhance the expression of AATs via the hippo effector YAP1, leading to mTOR activation and CRC cell proliferation.https://doi.org/10.1002/1878-0261.12999amino acid transportersoncogeneSLC1A5/ASCT2SLC38A2/SNAT2SLC7A5/LAT1solute carriers
collection DOAJ
language English
format Article
sources DOAJ
author Palanivel Kandasamy
Inti Zlobec
Damian T. Nydegger
Jonai Pujol‐Giménez
Rajesh Bhardwaj
Senji Shirasawa
Toshiyuki Tsunoda
Matthias A. Hediger
spellingShingle Palanivel Kandasamy
Inti Zlobec
Damian T. Nydegger
Jonai Pujol‐Giménez
Rajesh Bhardwaj
Senji Shirasawa
Toshiyuki Tsunoda
Matthias A. Hediger
Oncogenic KRAS mutations enhance amino acid uptake by colorectal cancer cells via the hippo signaling effector YAP1
Molecular Oncology
amino acid transporters
oncogene
SLC1A5/ASCT2
SLC38A2/SNAT2
SLC7A5/LAT1
solute carriers
author_facet Palanivel Kandasamy
Inti Zlobec
Damian T. Nydegger
Jonai Pujol‐Giménez
Rajesh Bhardwaj
Senji Shirasawa
Toshiyuki Tsunoda
Matthias A. Hediger
author_sort Palanivel Kandasamy
title Oncogenic KRAS mutations enhance amino acid uptake by colorectal cancer cells via the hippo signaling effector YAP1
title_short Oncogenic KRAS mutations enhance amino acid uptake by colorectal cancer cells via the hippo signaling effector YAP1
title_full Oncogenic KRAS mutations enhance amino acid uptake by colorectal cancer cells via the hippo signaling effector YAP1
title_fullStr Oncogenic KRAS mutations enhance amino acid uptake by colorectal cancer cells via the hippo signaling effector YAP1
title_full_unstemmed Oncogenic KRAS mutations enhance amino acid uptake by colorectal cancer cells via the hippo signaling effector YAP1
title_sort oncogenic kras mutations enhance amino acid uptake by colorectal cancer cells via the hippo signaling effector yap1
publisher Wiley
series Molecular Oncology
issn 1574-7891
1878-0261
publishDate 2021-10-01
description Oncogenic KRAS mutations develop unique metabolic dependencies on nutrients to support tumor metabolism and cell proliferation. In particular, KRAS mutant cancer cells exploit amino acids (AAs) such as glutamine and leucine, to accelerate energy metabolism, redox balance through glutathione synthesis and macromolecule biosynthesis. However, the identities of the amino acid transporters (AATs) that are prominently upregulated in KRAS mutant cancer cells, and the mechanism regulating their expression have not yet been systematically investigated. Here, we report that the majority of the KRAS mutant colorectal cancer (CRC) cells upregulate selected AATs (SLC7A5/LAT1, SLC38A2/SNAT2, and SLC1A5/ASCT2), which correlates with enhanced uptake of AAs such as glutamine and leucine. Consistently, knockdown of oncogenic KRAS downregulated the expression of AATs, thereby decreasing the levels of amino acids taken up by CRC cells. Moreover, overexpression of mutant KRAS upregulated the expression of AATs (SLC7A5/LAT1, SLC38A2/SNAT2, and SLC1A5/ASCT2) in KRAS wild‐type CRC cells and mouse embryonic fibroblasts. In addition, we show that the YAP1 (Yes‐associated protein 1) transcriptional coactivator accounts for increased expression of AATs and mTOR activation in KRAS mutant CRC cells. Specific knockdown of AATs by shRNAs or pharmacological blockage of AATs effectively inhibited AA uptake, mTOR activation, and cell proliferation. Collectively, we conclude that oncogenic KRAS mutations enhance the expression of AATs via the hippo effector YAP1, leading to mTOR activation and CRC cell proliferation.
topic amino acid transporters
oncogene
SLC1A5/ASCT2
SLC38A2/SNAT2
SLC7A5/LAT1
solute carriers
url https://doi.org/10.1002/1878-0261.12999
work_keys_str_mv AT palanivelkandasamy oncogenickrasmutationsenhanceaminoaciduptakebycolorectalcancercellsviathehipposignalingeffectoryap1
AT intizlobec oncogenickrasmutationsenhanceaminoaciduptakebycolorectalcancercellsviathehipposignalingeffectoryap1
AT damiantnydegger oncogenickrasmutationsenhanceaminoaciduptakebycolorectalcancercellsviathehipposignalingeffectoryap1
AT jonaipujolgimenez oncogenickrasmutationsenhanceaminoaciduptakebycolorectalcancercellsviathehipposignalingeffectoryap1
AT rajeshbhardwaj oncogenickrasmutationsenhanceaminoaciduptakebycolorectalcancercellsviathehipposignalingeffectoryap1
AT senjishirasawa oncogenickrasmutationsenhanceaminoaciduptakebycolorectalcancercellsviathehipposignalingeffectoryap1
AT toshiyukitsunoda oncogenickrasmutationsenhanceaminoaciduptakebycolorectalcancercellsviathehipposignalingeffectoryap1
AT matthiasahediger oncogenickrasmutationsenhanceaminoaciduptakebycolorectalcancercellsviathehipposignalingeffectoryap1
_version_ 1716860707761291264

Similar Items