Relevance of Abnormal KCNN1 Expression and Osmotic Hypersensitivity in Ewing Sarcoma

SIMPLE SUMMARY: The main oncogene in Ewing sarcoma directly drives a high expression of a previously unknown variant KCNN1 (encoding the K(Ca)2.1 channel) that we also verified in samples from >200 patients. Yet, we found that the channel is not functional and does not modulate Ewing sarcoma cell...

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Autores principales: Fuest, Sebastian, Post, Christoph, Balbach, Sebastian T., Jabar, Susanne, Neumann, Ilka, Schimmelpfennig, Sandra, Sargin, Sarah, Nass, Elke, Budde, Thomas, Kailayangiri, Sareetha, Altvater, Bianca, Ranft, Andreas, Hartmann, Wolfgang, Dirksen, Uta, Rössig, Claudia, Schwab, Albrecht, Pethő, Zoltán
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9564116/
https://www.ncbi.nlm.nih.gov/pubmed/36230742
http://dx.doi.org/10.3390/cancers14194819
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author Fuest, Sebastian
Post, Christoph
Balbach, Sebastian T.
Jabar, Susanne
Neumann, Ilka
Schimmelpfennig, Sandra
Sargin, Sarah
Nass, Elke
Budde, Thomas
Kailayangiri, Sareetha
Altvater, Bianca
Ranft, Andreas
Hartmann, Wolfgang
Dirksen, Uta
Rössig, Claudia
Schwab, Albrecht
Pethő, Zoltán
author_facet Fuest, Sebastian
Post, Christoph
Balbach, Sebastian T.
Jabar, Susanne
Neumann, Ilka
Schimmelpfennig, Sandra
Sargin, Sarah
Nass, Elke
Budde, Thomas
Kailayangiri, Sareetha
Altvater, Bianca
Ranft, Andreas
Hartmann, Wolfgang
Dirksen, Uta
Rössig, Claudia
Schwab, Albrecht
Pethő, Zoltán
author_sort Fuest, Sebastian
collection PubMed
description SIMPLE SUMMARY: The main oncogene in Ewing sarcoma directly drives a high expression of a previously unknown variant KCNN1 (encoding the K(Ca)2.1 channel) that we also verified in samples from >200 patients. Yet, we found that the channel is not functional and does not modulate Ewing sarcoma cell behavior. We could explain this lack of functional impact by the surprising absence of any K(Ca)2.1-carried K(+) current in Ewing sarcoma cells. However, we show in a proof-of-principle study that the essential lack of a K(+) conductance can be exploited by applying hypoosmotic stress and effectively and selectively killing the Ewing sarcoma cells. ABSTRACT: Ewing sarcoma (EwS) is a rare and highly malignant bone tumor occurring mainly in childhood and adolescence. Physiologically, the bone is a central hub for Ca(2+) homeostasis, which is severely disturbed by osteolytic processes in EwS. Therefore, we aimed to investigate how ion transport proteins involved in Ca(2+) homeostasis affect EwS pathophysiology. We characterized the expression of 22 candidate genes of Ca(2+)-permeable or Ca(2+)-regulated ion channels in three EwS cell lines and found the Ca(2+)-activated K(+) channel K(Ca)2.1 (KCNN1) to be exceptionally highly expressed. We revealed that KCNN1 expression is directly regulated by the disease-driving oncoprotein EWSR1-FL1. Due to its consistent overexpression in EwS, KCNN1 mRNA could be a prognostic marker in EwS. In a large cohort of EwS patients, however, KCNN1 mRNA quantity does not correlate with clinical parameters. Several functional studies including patch clamp electrophysiology revealed no evidence for K(Ca)2.1 function in EwS cells. Thus, elevated KCNN1 expression is not translated to K(Ca)2.1 channel activity in EwS cells. However, we found that the low K(+) conductance of EwS cells renders them susceptible to hypoosmotic solutions. The absence of a relevant K(+) conductance in EwS thereby provides an opportunity for hypoosmotic therapy that can be exploited during tumor surgery.
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spelling pubmed-95641162022-10-15 Relevance of Abnormal KCNN1 Expression and Osmotic Hypersensitivity in Ewing Sarcoma Fuest, Sebastian Post, Christoph Balbach, Sebastian T. Jabar, Susanne Neumann, Ilka Schimmelpfennig, Sandra Sargin, Sarah Nass, Elke Budde, Thomas Kailayangiri, Sareetha Altvater, Bianca Ranft, Andreas Hartmann, Wolfgang Dirksen, Uta Rössig, Claudia Schwab, Albrecht Pethő, Zoltán Cancers (Basel) Article SIMPLE SUMMARY: The main oncogene in Ewing sarcoma directly drives a high expression of a previously unknown variant KCNN1 (encoding the K(Ca)2.1 channel) that we also verified in samples from >200 patients. Yet, we found that the channel is not functional and does not modulate Ewing sarcoma cell behavior. We could explain this lack of functional impact by the surprising absence of any K(Ca)2.1-carried K(+) current in Ewing sarcoma cells. However, we show in a proof-of-principle study that the essential lack of a K(+) conductance can be exploited by applying hypoosmotic stress and effectively and selectively killing the Ewing sarcoma cells. ABSTRACT: Ewing sarcoma (EwS) is a rare and highly malignant bone tumor occurring mainly in childhood and adolescence. Physiologically, the bone is a central hub for Ca(2+) homeostasis, which is severely disturbed by osteolytic processes in EwS. Therefore, we aimed to investigate how ion transport proteins involved in Ca(2+) homeostasis affect EwS pathophysiology. We characterized the expression of 22 candidate genes of Ca(2+)-permeable or Ca(2+)-regulated ion channels in three EwS cell lines and found the Ca(2+)-activated K(+) channel K(Ca)2.1 (KCNN1) to be exceptionally highly expressed. We revealed that KCNN1 expression is directly regulated by the disease-driving oncoprotein EWSR1-FL1. Due to its consistent overexpression in EwS, KCNN1 mRNA could be a prognostic marker in EwS. In a large cohort of EwS patients, however, KCNN1 mRNA quantity does not correlate with clinical parameters. Several functional studies including patch clamp electrophysiology revealed no evidence for K(Ca)2.1 function in EwS cells. Thus, elevated KCNN1 expression is not translated to K(Ca)2.1 channel activity in EwS cells. However, we found that the low K(+) conductance of EwS cells renders them susceptible to hypoosmotic solutions. The absence of a relevant K(+) conductance in EwS thereby provides an opportunity for hypoosmotic therapy that can be exploited during tumor surgery. MDPI 2022-10-01 /pmc/articles/PMC9564116/ /pubmed/36230742 http://dx.doi.org/10.3390/cancers14194819 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/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 (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Fuest, Sebastian
Post, Christoph
Balbach, Sebastian T.
Jabar, Susanne
Neumann, Ilka
Schimmelpfennig, Sandra
Sargin, Sarah
Nass, Elke
Budde, Thomas
Kailayangiri, Sareetha
Altvater, Bianca
Ranft, Andreas
Hartmann, Wolfgang
Dirksen, Uta
Rössig, Claudia
Schwab, Albrecht
Pethő, Zoltán
Relevance of Abnormal KCNN1 Expression and Osmotic Hypersensitivity in Ewing Sarcoma
title Relevance of Abnormal KCNN1 Expression and Osmotic Hypersensitivity in Ewing Sarcoma
title_full Relevance of Abnormal KCNN1 Expression and Osmotic Hypersensitivity in Ewing Sarcoma
title_fullStr Relevance of Abnormal KCNN1 Expression and Osmotic Hypersensitivity in Ewing Sarcoma
title_full_unstemmed Relevance of Abnormal KCNN1 Expression and Osmotic Hypersensitivity in Ewing Sarcoma
title_short Relevance of Abnormal KCNN1 Expression and Osmotic Hypersensitivity in Ewing Sarcoma
title_sort relevance of abnormal kcnn1 expression and osmotic hypersensitivity in ewing sarcoma
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9564116/
https://www.ncbi.nlm.nih.gov/pubmed/36230742
http://dx.doi.org/10.3390/cancers14194819
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