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Involvement of carbon monoxide produced by heme oxygenase in ABA-induced stomatal closure in Vicia faba and its proposed signal transduction pathway
作者姓名:CAO  ZeYu  HUANG  BenKai  WANG  QingYa  XUAN  Wei  LING  TengFang  ZHANG  Bo  CHEN  Xi  NIE  Li  SHEN  WenBiaot
作者单位:College of Life Sciences, Laboratory Centre of Life Sciences, Nanjing Agricultural University, Nanjing 210095, China
基金项目:Supported by the National Natural Science Foundation of China (Grant No. 30671248), and “Blue Project” of Jiangsu Province and the Student Research Training (SRT) Project of Nanjing Agricultural University (Grant No. 0506A 11 )
摘    要:Carbon monoxide (CO) has recently proven to be an important bioactive or signaling molecule in mammalian cells. Its effects are mainly mediated by nitric oxide (NO) and cyclic GMP (cGMP). In Vicia faba leaves, CO production and heme oxygenase (HO) activity, an important CO synthetic enzyme, are first reported to increase in response to ABA treatment, which could result in stomatal closure. Inter- estingly, ABA-induced stomatal closure in V. faba guard cells is partially blocked when the synthetic CO inhibitor ZnPP, or the CO/NO scavenger Hb is added. Furthermore, we show that, exogenously applied CO donor, hematin, and CO aqueous solution not only result in the enhancement of CO release, but also time-dependently induce stomatal closure, and the latter is mimicked by the application of an NO donor SNP. The above-mentioned stomatal closure effects are differentially reversed by the addition of tungstate, a potent inhibitor of NO synthetic enzyme nitrate reductase (NR), the specific NO scavenger cPTIO, ZnPP, or Hb. During treatment for 4 h, SNP, 0.01% CO aqueous solution or hematin significantly triggers NO synthesis, whereas cPTIO, or tungstate approximately fully inhibits NO fluorescence. Ad- ditionally, application of the GC inhibitor ODQ blocks CO-induced stomatal closure. This inhibition could be reversed when 8-Br-cGMP is added. Thus, the above results suggest that CO produced by HO is involved in ABA-induced stomatal closure, and NO and cGMP may function as downstream interme- diates in the CO signaling responsible for stomatal closure.

关 键 词:一氧化碳  血红素加氧酶  气孔关闭  信号传递  一氧化氮
收稿时间:5 February 2007
修稿时间:2007-02-05

Involvement of carbon monoxide produced by heme oxygenase in ABA-induced stomatal closure in <Emphasis Type="Italic">Vicia faba</Emphasis> and its proposed signal transduction pathway
CAO ZeYu HUANG BenKai WANG QingYa XUAN Wei LING TengFang ZHANG Bo CHEN Xi NIE Li SHEN WenBiaot.Involvement of carbon monoxide produced by heme oxygenase in ABA-induced stomatal closure in Vicia faba and its proposed signal transduction pathway[J].Chinese Science Bulletin,2007,52(17):2365-2373.
Authors:Cao ZeYu  Huang BenKai  Wang QingYa  Xuan Wei  Ling TengFang  Zhang Bo  Chen Xi  Nie Li  Shen WenBiao
Institution:(1) College of Life Sciences, Laboratory Centre of Life Sciences, Nanjing Agricultural University, Nanjing, 210095, China
Abstract:Carbon monoxide (CO) has recently proven to be an important bioactive or signaling molecule in mammalian cells. Its effects are mainly mediated by nitric oxide (NO) and cyclic GMP (cGMP). In Vicia faba leaves, CO production and heme oxygenase (HO) activity, an important CO synthetic enzyme, are first reported to increase in response to ABA treatment, which could result in stomatal closure. Inter- estingly, ABA-induced stomatal closure in V. faba guard cells is partially blocked when the synthetic CO inhibitor ZnPP, or the CO/NO scavenger Hb is added. Furthermore, we show that, exogenously applied CO donor, hematin, and CO aqueous solution not only result in the enhancement of CO release, but also time-dependently induce stomatal closure, and the latter is mimicked by the application of an NO donor SNP. The above-mentioned stomatal closure effects are differentially reversed by the addition of tungstate, a potent inhibitor of NO synthetic enzyme nitrate reductase (NR), the specific NO scavenger cPTIO, ZnPP, or Hb. During treatment for 4 h, SNP, 0.01% CO aqueous solution or hematin significantly triggers NO synthesis, whereas cPTIO, or tungstate approximately fully inhibits NO fluorescence. Ad- ditionally, application of the GC inhibitor ODQ blocks CO-induced stomatal closure. This inhibition could be reversed when 8-Br-cGMP is added. Thus, the above results suggest that CO produced by HO is involved in ABA-induced stomatal closure, and NO and cGMP may function as downstream interme- diates in the CO signaling responsible for stomatal closure.
Keywords:carbon monoxide  ABA  heme oxygenase  cyclic GMP  nitric oxide  stomatal closure  Vicia faba
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