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ミカミ ヨシノリ
Mikami Yoshinori
三上 義礼 所属 東邦大学 医学部 医学科 職種 助教 |
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| 言語種別 | 英語 |
| 発表タイトル | Polysulfides derived from H2S, are possible signaling molecules that activate TRPA1 channels in rat brain |
| 会議名 | 第38回日本神経科学大会 |
| 学会区分 | 国内学会 |
| 発表形式 | 口頭 |
| 講演区分 | 一般 |
| 発表者・共同発表者 | ◎木村由佳, 三上義礼†, 大隅貴美子, 津金麻美子, 岡淳一郎, 木村英雄 |
| 発表年月日 | 2015/07/28 |
| 開催地 (都市, 国名) |
神戸 |
| 概要 | Hydrogen sulfide (H2S) is established as a bioactive substance with various physiological functions. H2S, which is enzymatically produced from cysteine,is oxidized to produce polysulfides (H2Sn,n>2). We previously reported that polysulfides induce Ca2+ influx in astrocytes more potently than H2S. However, the receptor that mediates the response has not been identified. Here, we have shown that polysulfides induce Ca2+ influx by activating transient receptor potential ankyrin-1 (TRPA1) channels in rat astrocytes. The response induced by 0.5 μM polysulfide requires approximately 300 times greater concentrations of H2S. TRPA1-selective agonists, allyl isothiocyanate and cinnamaldehyde, induced Ca2+ influx, and responses to polysulfides were suppressed by TRPA1-selective inhibitors, HC-030031 and AP-18, as well as by siRNAs selective to TRPA1. The present study suggests that polysulfides are potential H2S-derived signaling molecules that stimulate TRPA1 channels in the brain. Above study also suggests that some of the functions ascribes to H2S are mediated by polysulfides. |