PIEZO1 Channel Is a Potential Regulator of Synovial Sarcoma Cell-Viability

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Suzuki, Takahisa
Muraki, Yukiko
Hatano, Noriyuki
Suzuki, Hiroka
Muraki, Katsuhiko
Griffith University Author(s)
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2018
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Abstract

Detection of mechanical stress is essential for diverse biological functions including touch, audition, and maintenance of vascular myogenic tone. PIEZO1, a mechano-sensing cation channel, is widely expressed in neuronal and non-neuronal cells and is expected to be involved in important biological functions. Here, we examined the possibility that PIEZO1 is involved in the regulation of synovial sarcoma cell-viability. Application of a PIEZO1 agonist Yoda1 effectively induced Ca2+ response and cation channel currents in PIEZO1-expressing HEK (HEK-Piezo1) cells and synovial sarcoma SW982 (SW982) cells. Mechanical stress, as well as Yoda1, induced the activity of an identical channel of conductance with 21.6 pS in HEK-Piezo1 cells. In contrast, Yoda1 up to 10 μM had no effects on membrane currents in HEK cells without transfecting PIEZO1. A knockdown of PIEZO1 with siRNA in SW982 cells abolished Yoda1-induced Ca2+ response and significantly reduced cell cell-viability. Because PIEZO1 is highly expressed in SW982 cells and its knockdown affects cell-viability, this gene is a potential target against synovial sarcoma.

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International Journal of Molecular Sciences

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19

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5

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© 2018 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/) which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

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Other chemical sciences

Genetics

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Science & Technology

Life Sciences & Biomedicine

Physical Sciences

Biochemistry & Molecular Biology

Chemistry, Multidisciplinary

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Suzuki, T; Muraki, Y; Hatano, N; Suzuki, H; Muraki, K, PIEZO1 Channel Is a Potential Regulator of Synovial Sarcoma Cell-Viability, International Journal of Molecular Sciences, 2018, 19 (5), pp. 1452:1-1452:11

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