Matriptase autoactivation is tightly regulated by the cellular chemical environments.
The ability of cells to rapidly detect and react to alterations in their chemical environment, such as pH, ionic strength and redox potential, is essential for cell function and survival. We present here evidence that cells can respond to such environmental alterations by rapid induction of matripta...
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Public Library of Science (PLoS)
2014-01-01
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| Series: | PLoS ONE |
| Online Access: | http://europepmc.org/articles/PMC3976350?pdf=render |
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doaj-756ee27957374452a7d6d2fe458370ae2020-11-25T00:48:22ZengPublic Library of Science (PLoS)PLoS ONE1932-62032014-01-0194e9389910.1371/journal.pone.0093899Matriptase autoactivation is tightly regulated by the cellular chemical environments.Jehng-Kang WangI-Jou TengTing-Jen LoSean MooreYee Hui YeoYun-Chung TengMalvika KaulChiann-Chyi ChenAnnie Hong ZuoFen-Pai ChouXiaoyu YangI-Chu TsengMichael D JohnsonChen-Yong LinThe ability of cells to rapidly detect and react to alterations in their chemical environment, such as pH, ionic strength and redox potential, is essential for cell function and survival. We present here evidence that cells can respond to such environmental alterations by rapid induction of matriptase autoactivation. Specifically, we show that matriptase autoactivation can occur spontaneously at physiological pH, and is significantly enhanced by acidic pH, both in a cell-free system and in living cells. The acid-accelerated autoactivation can be attenuated by chloride, a property that may be part of a safety mechanism to prevent unregulated matriptase autoactivation. Additionally, the thio-redox balance of the environment also modulates matriptase autoactivation. Using the cell-free system, we show that matriptase autoactivation is suppressed by cytosolic reductive factors, with this cytosolic suppression being reverted by the addition of oxidizing agents. In living cells, we observed rapid induction of matriptase autoactivation upon exposure to toxic metal ions known to induce oxidative stress, including CoCl2 and CdCl2. The metal-induced matriptase autoactivation is suppressed by N-acetylcysteine, supporting the putative role of altered cellular redox state in metal induced matriptase autoactivation. Furthermore, matriptase knockdown rendered cells more susceptible to CdCl2-induced cell death compared to control cells. This observation implies that the metal-induced matriptase autoactivation confers cells with the ability to survive exposure to toxic metals and/or oxidative stress. Our results suggest that matriptase can act as a cellular sensor of the chemical environment of the cell that allows the cell to respond to and protect itself from changes in the chemical milieu.http://europepmc.org/articles/PMC3976350?pdf=render |
| collection |
DOAJ |
| language |
English |
| format |
Article |
| sources |
DOAJ |
| author |
Jehng-Kang Wang I-Jou Teng Ting-Jen Lo Sean Moore Yee Hui Yeo Yun-Chung Teng Malvika Kaul Chiann-Chyi Chen Annie Hong Zuo Fen-Pai Chou Xiaoyu Yang I-Chu Tseng Michael D Johnson Chen-Yong Lin |
| spellingShingle |
Jehng-Kang Wang I-Jou Teng Ting-Jen Lo Sean Moore Yee Hui Yeo Yun-Chung Teng Malvika Kaul Chiann-Chyi Chen Annie Hong Zuo Fen-Pai Chou Xiaoyu Yang I-Chu Tseng Michael D Johnson Chen-Yong Lin Matriptase autoactivation is tightly regulated by the cellular chemical environments. PLoS ONE |
| author_facet |
Jehng-Kang Wang I-Jou Teng Ting-Jen Lo Sean Moore Yee Hui Yeo Yun-Chung Teng Malvika Kaul Chiann-Chyi Chen Annie Hong Zuo Fen-Pai Chou Xiaoyu Yang I-Chu Tseng Michael D Johnson Chen-Yong Lin |
| author_sort |
Jehng-Kang Wang |
| title |
Matriptase autoactivation is tightly regulated by the cellular chemical environments. |
| title_short |
Matriptase autoactivation is tightly regulated by the cellular chemical environments. |
| title_full |
Matriptase autoactivation is tightly regulated by the cellular chemical environments. |
| title_fullStr |
Matriptase autoactivation is tightly regulated by the cellular chemical environments. |
| title_full_unstemmed |
Matriptase autoactivation is tightly regulated by the cellular chemical environments. |
| title_sort |
matriptase autoactivation is tightly regulated by the cellular chemical environments. |
| publisher |
Public Library of Science (PLoS) |
| series |
PLoS ONE |
| issn |
1932-6203 |
| publishDate |
2014-01-01 |
| description |
The ability of cells to rapidly detect and react to alterations in their chemical environment, such as pH, ionic strength and redox potential, is essential for cell function and survival. We present here evidence that cells can respond to such environmental alterations by rapid induction of matriptase autoactivation. Specifically, we show that matriptase autoactivation can occur spontaneously at physiological pH, and is significantly enhanced by acidic pH, both in a cell-free system and in living cells. The acid-accelerated autoactivation can be attenuated by chloride, a property that may be part of a safety mechanism to prevent unregulated matriptase autoactivation. Additionally, the thio-redox balance of the environment also modulates matriptase autoactivation. Using the cell-free system, we show that matriptase autoactivation is suppressed by cytosolic reductive factors, with this cytosolic suppression being reverted by the addition of oxidizing agents. In living cells, we observed rapid induction of matriptase autoactivation upon exposure to toxic metal ions known to induce oxidative stress, including CoCl2 and CdCl2. The metal-induced matriptase autoactivation is suppressed by N-acetylcysteine, supporting the putative role of altered cellular redox state in metal induced matriptase autoactivation. Furthermore, matriptase knockdown rendered cells more susceptible to CdCl2-induced cell death compared to control cells. This observation implies that the metal-induced matriptase autoactivation confers cells with the ability to survive exposure to toxic metals and/or oxidative stress. Our results suggest that matriptase can act as a cellular sensor of the chemical environment of the cell that allows the cell to respond to and protect itself from changes in the chemical milieu. |
| url |
http://europepmc.org/articles/PMC3976350?pdf=render |
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