Exploring the role of the CXXC motif in the regulation of some enzymes involved in redox signaling.

探索 CXXC 基序在调节参与氧化还原信号传导的一些酶中的作用。

• 批准号: RGPIN-2017-04925
• 负责人: Mutus, Bulent
• 金额: $ 2.91万
• 依托单位: University of Windsor
• 依托单位国家: 加拿大
• 项目类别: Discovery Grants Program - Individual
• 财政年份: 2018
• 资助国家: 加拿大
• 起止时间: 2018-01-01 至 2019-12-31
• 项目状态: 已结题
• 来源: https://www.nserc-crsng.gc.ca/ase-oro/Details-Detailles_eng.asp?id=660522
• 关键词: Exploring; role; CXXC; motif; regulation

The CXXC-motif refers to a protein sequence where two cysteine residues are separated by intervening residues, denoted by 'X' (X=any amino acid). This motif is found in many enzyme active-sites i.e. thioredoxin and protein disulfide isomease (PDI). In addition, the CXXC-motif is found peripheral to the active sites, yet performing crucial functional and regulatory roles. Studies have also shown that variation in the XX residues or those N- or C- terminal to the CXXC-motif can modulate enzyme activity. ******In the short term, we will determine the role of the CXXC-motif and flanking residues in the regulation of PDI, S-nitrosoglutathione reductase (GSNOR) and cystathionine-gamma-lyase (CSE), some key enzymes involved in thiol redox, nitric oxide (NO) and hydrogen sulfide (H2S) signaling. The work on PDI and GSNOR will indicate whether a lysine (K) residue at the C-terminal end of the CXXC-motif or other lysine residues within PDI and GSNOR are the sites for post translational modification by acetylation. We will assess the consequences of lysine-acetylation on the regulation, secretion and extra-cellular and intra-cellular localization of PDI and GSNOR. CSE contains 2 CXXC-motifs. We will test CSE's CXXC-motifs for: a) a previously undiscovered PDI-like thiol reductase activity role; and b) thiol-disulfide mediated regulatory role of its activity. In addition, we will use CSE-generated (homo)cysteine persulfides to determine whether H2S directly participates in sulfide signaling. Our long term goals are to investigate the cross-talk between enzymes that participate in thiol-mediated signaling.******In terms of impact to the field, the research program will introduce acetylation as a newly discovered mode of regulation for PDI and GSNOR, key enzymes involved in thiol-mediated signaling and implicated in several pathologies. PDI-work will yield information on the regulation of its secretion, cell surface attachment and thiol reductase and chaperone activities. GSNOR will be characterized with respect to: a new allosteric site; the role of acetylation on its catalytic/allosteric behaviour; interaction with eNOS; and intracellular localization. The work on CSE will yield information on its redox regulation and a new PDI-like thiol reductase activity. The CSE-generated homocysteine persulfides will be used to answer the fundamental question of whether sulfide participates in protein signaling or is a bystander molecule. Furthermore, information gained with respect to the control of the activities of these enzymes will be invaluable for the development of pharmaceutical agents to control these enzymes and the signaling pathways they modulate.**************

cxxc基序是指一个蛋白质序列，其中两个半胱氨酸残基被中间残基隔开，用“X”表示（X=任何氨基酸）。该基元存在于许多酶活性位点，如硫氧还蛋白和蛋白二硫异构酶（PDI）。此外，cxxc基序位于活性位点的外围，但发挥着至关重要的功能和调节作用。研究还表明，XX残基或cxxc基序的N-或C-末端的变化可以调节酶的活性。******在短期内，我们将确定cxxc基序和侧翼残基在PDI、s -亚硝基谷胱甘肽还原酶（GSNOR）和胱氨酸- γ -裂解酶（CSE）调控中的作用，这些酶参与硫醇氧化还原、一氧化氮（NO）和硫化氢（H2S）信号传导。对PDI和GSNOR的研究将表明cxxc基序c末端的赖氨酸(K)残基或PDI和GSNOR内的其他赖氨酸残基是否是翻译后乙酰化修饰的位点。我们将评估赖氨酸乙酰化对PDI和GSNOR的调节、分泌以及细胞外和细胞内定位的影响。CSE包含2个cxxc -motif。我们将测试CSE的cxxc基序：a)以前未发现的pdi样硫醇还原酶活性作用；b)巯基二硫化物对其活性的调节作用。此外，我们将使用cse生成的（homo）过硫化物半胱氨酸来确定H2S是否直接参与硫化物信号传导。我们的长期目标是研究参与硫醇介导的信号传导的酶之间的串扰。******就该领域的影响而言，该研究计划将介绍乙酰化作为一种新发现的PDI和GSNOR调节模式，这些关键酶参与硫醇介导的信号传导并涉及多种病理。pdi工作将提供有关其分泌、细胞表面附着、硫醇还原酶和伴侣活性调节的信息。GSNOR将在以下方面进行表征：一个新的变构位点；乙酰化对其催化/变构行为的影响与eNOS交互；以及细胞内定位。对CSE的研究将提供有关其氧化还原调控和新的pdi样硫醇还原酶活性的信息。cse生成的同型半胱氨酸过硫化物将用于回答硫化物是否参与蛋白质信号传导还是旁观者分子的基本问题。此外，获得的有关这些酶的活性控制的信息对于开发控制这些酶及其调节的信号通路的药物制剂将是无价的。**************