The combined activation of KCa3.1 and inhibition of Kv11.1/hERG1 currents contribute to overcome Cisplatin resistance in colorectal cancer cells
Background: Platinum-based drugs such as Cisplatin are commonly employed for cancer treatment. Despite an initial therapeutic response, Cisplatin treatment often results in the development of chemoresistance. To identify novel approaches to overcome Cisplatin resistance, we tested Cisplatin in combi...
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sg-ntu-dr.10356-1388512020-11-01T05:32:14Z The combined activation of KCa3.1 and inhibition of Kv11.1/hERG1 currents contribute to overcome Cisplatin resistance in colorectal cancer cells Pillozzi, Serena D'Amico, Massimo Bartoli, Gianluca Gasparoli, Luca Petroni, Giulia Crociani, Olivia Marzo, Tiziano Guerriero, Angela Messori, Luigi Severi, Mirko Udisti, Roberto Wulff, Heike Chandy, Kanianthara George Becchetti, Andrea Arcangeli, Annarosa Lee Kong Chian School of Medicine (LKCMedicine) Science::Medicine Riluzole SKA-31 Background: Platinum-based drugs such as Cisplatin are commonly employed for cancer treatment. Despite an initial therapeutic response, Cisplatin treatment often results in the development of chemoresistance. To identify novel approaches to overcome Cisplatin resistance, we tested Cisplatin in combination with K+ channel modulators on colorectal cancer (CRC) cells. Methods: The functional expression of Ca2+-activated (KCa3.1, also known as KCNN4) and voltage-dependent (Kv11.1, also known as KCNH2 or hERG1) K+ channels was determined in two CRC cell lines (HCT-116 and HCT-8) by molecular and electrophysiological techniques. Cisplatin and several K+ channel modulators were tested in vitro for their action on K+ currents, cell vitality, apoptosis, cell cycle, proliferation, intracellular signalling and Platinum uptake. These effects were also analysed in a mouse model mimicking Cisplatin resistance. Results: Cisplatin-resistant CRC cells expressed higher levels of KCa3.1 and Kv11.1 channels, compared with Cisplatin-sensitive CRC cells. In resistant cells, KCa3.1 activators (SKA-31) and Kv11.1 inhibitors (E4031) had a synergistic action with Cisplatin in triggering apoptosis and inhibiting proliferation. The effect was maximal when KCa3.1 activation and Kv11.1 inhibition were combined. In fact, similar results were produced by Riluzole, which is able to both activate KCa3.1 and inhibit Kv11.1. Cisplatin uptake into resistant cells depended on KCa3.1 channel activity, as it was potentiated by KCa3.1 activators. Kv11.1 blockade led to increased KCa3.1 expression and thereby stimulated Cisplatin uptake. Finally, the combined administration of a KCa3.1 activator and a Kv11.1 inhibitor also overcame Cisplatin resistance in vivo. Conclusions: As Riluzole, an activator of KCa3.1 and inhibitor of Kv11.1 channels, is in clinical use, our results suggest that this compound may be useful in the clinic to improve Cisplatin efficacy and overcome Cisplatin resistance in CRC. Published version 2020-05-13T06:19:58Z 2020-05-13T06:19:58Z 2018 Journal Article Pillozzi, S., D'Amico, M., Bartoli, G., Gasparoli, L., Petroni, G., Crociani, O., . . . Arcangeli, A. (2018). The combined activation of KCa3.1 and inhibition of Kv11.1/hERG1 currents contribute to overcome Cisplatin resistance in colorectal cancer cells. British Journal of Cancer, 118(2), 200-212. doi:10.1038/bjc.2017.392 0007-0920 https://hdl.handle.net/10356/138851 10.1038/bjc.2017.392 29161243 2-s2.0-85041082898 2 118 200 212 en British Journal of Cancer © 2018 Cancer Research UK. All rights reserved. This work is published under the standard license to publish agreement. After 12 months the work will become freely available and the license terms will switch to a Creative Commons AttributionNonCommercial-Share Alike 4.0 Unported License. application/pdf |
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Science::Medicine Riluzole SKA-31 Pillozzi, Serena D'Amico, Massimo Bartoli, Gianluca Gasparoli, Luca Petroni, Giulia Crociani, Olivia Marzo, Tiziano Guerriero, Angela Messori, Luigi Severi, Mirko Udisti, Roberto Wulff, Heike Chandy, Kanianthara George Becchetti, Andrea Arcangeli, Annarosa The combined activation of KCa3.1 and inhibition of Kv11.1/hERG1 currents contribute to overcome Cisplatin resistance in colorectal cancer cells |
| description |
Background: Platinum-based drugs such as Cisplatin are commonly employed for cancer treatment. Despite an initial therapeutic response, Cisplatin treatment often results in the development of chemoresistance. To identify novel approaches to overcome Cisplatin resistance, we tested Cisplatin in combination with K+ channel modulators on colorectal cancer (CRC) cells. Methods: The functional expression of Ca2+-activated (KCa3.1, also known as KCNN4) and voltage-dependent (Kv11.1, also known as KCNH2 or hERG1) K+ channels was determined in two CRC cell lines (HCT-116 and HCT-8) by molecular and electrophysiological techniques. Cisplatin and several K+ channel modulators were tested in vitro for their action on K+ currents, cell vitality, apoptosis, cell cycle, proliferation, intracellular signalling and Platinum uptake. These effects were also analysed in a mouse model mimicking Cisplatin resistance. Results: Cisplatin-resistant CRC cells expressed higher levels of KCa3.1 and Kv11.1 channels, compared with Cisplatin-sensitive CRC cells. In resistant cells, KCa3.1 activators (SKA-31) and Kv11.1 inhibitors (E4031) had a synergistic action with Cisplatin in triggering apoptosis and inhibiting proliferation. The effect was maximal when KCa3.1 activation and Kv11.1 inhibition were combined. In fact, similar results were produced by Riluzole, which is able to both activate KCa3.1 and inhibit Kv11.1. Cisplatin uptake into resistant cells depended on KCa3.1 channel activity, as it was potentiated by KCa3.1 activators. Kv11.1 blockade led to increased KCa3.1 expression and thereby stimulated Cisplatin uptake. Finally, the combined administration of a KCa3.1 activator and a Kv11.1 inhibitor also overcame Cisplatin resistance in vivo. Conclusions: As Riluzole, an activator of KCa3.1 and inhibitor of Kv11.1 channels, is in clinical use, our results suggest that this compound may be useful in the clinic to improve Cisplatin efficacy and overcome Cisplatin resistance in CRC. |
| author2 |
Lee Kong Chian School of Medicine (LKCMedicine) |
| author_facet |
Lee Kong Chian School of Medicine (LKCMedicine) Pillozzi, Serena D'Amico, Massimo Bartoli, Gianluca Gasparoli, Luca Petroni, Giulia Crociani, Olivia Marzo, Tiziano Guerriero, Angela Messori, Luigi Severi, Mirko Udisti, Roberto Wulff, Heike Chandy, Kanianthara George Becchetti, Andrea Arcangeli, Annarosa |
| format |
Article |
| author |
Pillozzi, Serena D'Amico, Massimo Bartoli, Gianluca Gasparoli, Luca Petroni, Giulia Crociani, Olivia Marzo, Tiziano Guerriero, Angela Messori, Luigi Severi, Mirko Udisti, Roberto Wulff, Heike Chandy, Kanianthara George Becchetti, Andrea Arcangeli, Annarosa |
| author_sort |
Pillozzi, Serena |
| title |
The combined activation of KCa3.1 and inhibition of Kv11.1/hERG1 currents contribute to overcome Cisplatin resistance in colorectal cancer cells |
| title_short |
The combined activation of KCa3.1 and inhibition of Kv11.1/hERG1 currents contribute to overcome Cisplatin resistance in colorectal cancer cells |
| title_full |
The combined activation of KCa3.1 and inhibition of Kv11.1/hERG1 currents contribute to overcome Cisplatin resistance in colorectal cancer cells |
| title_fullStr |
The combined activation of KCa3.1 and inhibition of Kv11.1/hERG1 currents contribute to overcome Cisplatin resistance in colorectal cancer cells |
| title_full_unstemmed |
The combined activation of KCa3.1 and inhibition of Kv11.1/hERG1 currents contribute to overcome Cisplatin resistance in colorectal cancer cells |
| title_sort |
combined activation of kca3.1 and inhibition of kv11.1/herg1 currents contribute to overcome cisplatin resistance in colorectal cancer cells |
| publishDate |
2020 |
| url |
https://hdl.handle.net/10356/138851 |
| _version_ |
1683494580383645696 |