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Discovery of Functional Alternatively Spliced PKM Transcripts in Human Cancers

SIMPLE SUMMARY: Pyruvate kinase muscle type (PKM) is a key enzyme in glycolysis and is a mediator of the Warburg effect in tumors. The association of PKM with survival of cancer patients is controversial. In this study, we investigated the associations of the alternatively spliced transcripts of PKM...

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Autores principales: Li, Xiangyu, Kim, Woonghee, Arif, Muhammad, Gao, Chunxia, Hober, Andreas, Kotol, David, Strandberg, Linnéa, Forsström, Björn, Sivertsson, Åsa, Oksvold, Per, Turkez, Hasan, Grøtli, Morten, Sato, Yusuke, Kume, Haruki, Ogawa, Seishi, Boren, Jan, Nielsen, Jens, Uhlen, Mathias, Zhang, Cheng, Mardinoglu, Adil
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7835739/
https://www.ncbi.nlm.nih.gov/pubmed/33478099
http://dx.doi.org/10.3390/cancers13020348
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author Li, Xiangyu
Kim, Woonghee
Arif, Muhammad
Gao, Chunxia
Hober, Andreas
Kotol, David
Strandberg, Linnéa
Forsström, Björn
Sivertsson, Åsa
Oksvold, Per
Turkez, Hasan
Grøtli, Morten
Sato, Yusuke
Kume, Haruki
Ogawa, Seishi
Boren, Jan
Nielsen, Jens
Uhlen, Mathias
Zhang, Cheng
Mardinoglu, Adil
author_facet Li, Xiangyu
Kim, Woonghee
Arif, Muhammad
Gao, Chunxia
Hober, Andreas
Kotol, David
Strandberg, Linnéa
Forsström, Björn
Sivertsson, Åsa
Oksvold, Per
Turkez, Hasan
Grøtli, Morten
Sato, Yusuke
Kume, Haruki
Ogawa, Seishi
Boren, Jan
Nielsen, Jens
Uhlen, Mathias
Zhang, Cheng
Mardinoglu, Adil
author_sort Li, Xiangyu
collection PubMed
description SIMPLE SUMMARY: Pyruvate kinase muscle type (PKM) is a key enzyme in glycolysis and is a mediator of the Warburg effect in tumors. The association of PKM with survival of cancer patients is controversial. In this study, we investigated the associations of the alternatively spliced transcripts of PKM with cancer patients’ survival outcomes and explained the conflicts in previous studies. We discovered three poorly studied alternatively spliced PKM transcripts that exhibited opposite prognostic indications in different human cancers based on integrative systems analysis. We also detected their protein products and explored their potential biological functions based on in-vitro experiments. Our analysis demonstrated that alternatively spliced transcripts of not only PKM but also other genes should be considered in cancer studies, since it may enable the discovery and targeting of the right protein product for development of the efficient treatment strategies. ABSTRACT: Pyruvate kinase muscle type (PKM) is a key enzyme in glycolysis and plays an important oncological role in cancer. However, the association of PKM expression and the survival outcome of patients with different cancers is controversial. We employed systems biology methods to reveal prognostic value and potential biological functions of PKM transcripts in different human cancers. Protein products of transcripts were shown and detected by western blot and mass spectrometry analysis. We focused on different transcripts of PKM and investigated the associations between their mRNA expression and the clinical survival of the patients in 25 different cancers. We find that the transcripts encoding PKM2 and three previously unstudied transcripts, namely ENST00000389093, ENST00000568883, and ENST00000561609, exhibited opposite prognostic indications in different cancers. Moreover, we validated the prognostic effect of these transcripts in an independent kidney cancer cohort. Finally, we revealed that ENST00000389093 and ENST00000568883 possess pyruvate kinase enzymatic activity and may have functional roles in metabolism, cell invasion, and hypoxia response in cancer cells. Our study provided a potential explanation to the controversial prognostic indication of PKM, and could invoke future studies focusing on revealing the biological and oncological roles of these alternative spliced variants of PKM.
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spelling pubmed-78357392021-01-27 Discovery of Functional Alternatively Spliced PKM Transcripts in Human Cancers Li, Xiangyu Kim, Woonghee Arif, Muhammad Gao, Chunxia Hober, Andreas Kotol, David Strandberg, Linnéa Forsström, Björn Sivertsson, Åsa Oksvold, Per Turkez, Hasan Grøtli, Morten Sato, Yusuke Kume, Haruki Ogawa, Seishi Boren, Jan Nielsen, Jens Uhlen, Mathias Zhang, Cheng Mardinoglu, Adil Cancers (Basel) Article SIMPLE SUMMARY: Pyruvate kinase muscle type (PKM) is a key enzyme in glycolysis and is a mediator of the Warburg effect in tumors. The association of PKM with survival of cancer patients is controversial. In this study, we investigated the associations of the alternatively spliced transcripts of PKM with cancer patients’ survival outcomes and explained the conflicts in previous studies. We discovered three poorly studied alternatively spliced PKM transcripts that exhibited opposite prognostic indications in different human cancers based on integrative systems analysis. We also detected their protein products and explored their potential biological functions based on in-vitro experiments. Our analysis demonstrated that alternatively spliced transcripts of not only PKM but also other genes should be considered in cancer studies, since it may enable the discovery and targeting of the right protein product for development of the efficient treatment strategies. ABSTRACT: Pyruvate kinase muscle type (PKM) is a key enzyme in glycolysis and plays an important oncological role in cancer. However, the association of PKM expression and the survival outcome of patients with different cancers is controversial. We employed systems biology methods to reveal prognostic value and potential biological functions of PKM transcripts in different human cancers. Protein products of transcripts were shown and detected by western blot and mass spectrometry analysis. We focused on different transcripts of PKM and investigated the associations between their mRNA expression and the clinical survival of the patients in 25 different cancers. We find that the transcripts encoding PKM2 and three previously unstudied transcripts, namely ENST00000389093, ENST00000568883, and ENST00000561609, exhibited opposite prognostic indications in different cancers. Moreover, we validated the prognostic effect of these transcripts in an independent kidney cancer cohort. Finally, we revealed that ENST00000389093 and ENST00000568883 possess pyruvate kinase enzymatic activity and may have functional roles in metabolism, cell invasion, and hypoxia response in cancer cells. Our study provided a potential explanation to the controversial prognostic indication of PKM, and could invoke future studies focusing on revealing the biological and oncological roles of these alternative spliced variants of PKM. MDPI 2021-01-19 /pmc/articles/PMC7835739/ /pubmed/33478099 http://dx.doi.org/10.3390/cancers13020348 Text en © 2021 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Li, Xiangyu
Kim, Woonghee
Arif, Muhammad
Gao, Chunxia
Hober, Andreas
Kotol, David
Strandberg, Linnéa
Forsström, Björn
Sivertsson, Åsa
Oksvold, Per
Turkez, Hasan
Grøtli, Morten
Sato, Yusuke
Kume, Haruki
Ogawa, Seishi
Boren, Jan
Nielsen, Jens
Uhlen, Mathias
Zhang, Cheng
Mardinoglu, Adil
Discovery of Functional Alternatively Spliced PKM Transcripts in Human Cancers
title Discovery of Functional Alternatively Spliced PKM Transcripts in Human Cancers
title_full Discovery of Functional Alternatively Spliced PKM Transcripts in Human Cancers
title_fullStr Discovery of Functional Alternatively Spliced PKM Transcripts in Human Cancers
title_full_unstemmed Discovery of Functional Alternatively Spliced PKM Transcripts in Human Cancers
title_short Discovery of Functional Alternatively Spliced PKM Transcripts in Human Cancers
title_sort discovery of functional alternatively spliced pkm transcripts in human cancers
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7835739/
https://www.ncbi.nlm.nih.gov/pubmed/33478099
http://dx.doi.org/10.3390/cancers13020348
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