完整后设资料纪录
| DC 栏位 | 值 | 语言 |
|---|---|---|
| dc.contributor.author | 陈正伟 | en_US |
| dc.contributor.author | Cheng Wei Chen | en_US |
| dc.contributor.author | 杨裕雄 | en_US |
| dc.contributor.author | Yuh-Shyong Yang | en_US |
| dc.date.accessioned | 2014-12-12T02:22:22Z | - |
| dc.date.available | 2014-12-12T02:22:22Z | - |
| dc.date.issued | 1999 | en_US |
| dc.identifier.uri | http://140.113.39.130/cdrfb3/record/nctu/#NT880111004 | en_US |
| dc.identifier.uri | http://hdl.handle.net/11536/65225 | - |
| dc.description.abstract | 本实验使用类比法 (Homology) 来模拟酚亚硫酸基转移酵素的蛋白质结构,其骨架则是依据动情激素亚硫酸基转移酵素(Estrogen sulfotransferase)的X-ray单晶绕射结构(1aqu of PDB )。我们可利用模拟出的酚亚硫酸基转移酵素结构来解释突变种酚亚硫酸基转移酵素(K65ER68G)的独特活性,并说明胺基酸C66,C82和C232之间的相互关系与功能。由结构中我们发现环状区胺基酸序列区64~69是位于受质结合区的开口区附近而且可能作为控制受质进出的活动闸门。经过胺基酸序列的分析以及相关已解出结构的亚硫酸基转移酵素所提供给我们的资讯皆指出此环状区是属于易滑动的。由前人所做的实验数据以及我们所做的模拟结构中,我们可以证明此环状区域位于酵素活性区的通路上,对于调控产物的释出是非常重要的。主要的关键在于,序列C66 和C82 或是 C66 和 C232 所形成的双硫键能够固定住此易滑动的环状区域,并且防止它阻碍到受质的结合或是产物的放出。另外由模拟的结构我们可以发现序列K65与R68的正电荷对于环状区与酵素的活性区进出口之间的相互关系也是很重要的。这个发现也可以用来解释为什么突变种(K65ER68G)酵素只包含b 型(无受质PAP):此原因为突变后形成的负电荷使得原本可以挡住受质进出口的滑动环状区远离,同样的也可以解释为何突变种(K65ER68G)酵素的生理反应活性可以不需经由氧化就能达到与野生种酵素氧化后得到的活性一样。 | zh_TW |
| dc.description.abstract | The structure of phenol sulfotransferase (PST) is build by the method of Homology (Insight II) from the crystal structure of estrogen sulfotransferase (1aqu of PDB). The modeled PST structure is used to explain the unique activity of a mutant (K65ER68G) and to elucidate the function of and interaction among C66, C82 and C232. The loop region 64-69 is found outside of the substrate-binding site and may serve as a door of the entrance or exit of the active site. Data analysis of the amino acid sequence and information from know structure of sulfotransferases all indicate that this region is very flexible. From the previous experimental data and our modeling study, we are able to demonstrate that this region is in the way of the enzyme active site and is important for the regulation of the release of products. Formation of disulfide bonds between C66 and C82 or C66 and C232 immobilized this flexible region and prevent it from hindering substrate binding or product release. The modeled PST structure also shows that positive charges at K65 and R68 are important for the interaction of the loop region with PST active site. This observation explains why only b form (PAP free) of K65ER68G is obtained for the flexible loop region is no longer available as a cover after being mutated to contain a negative charge. The same reason explains the physiological activity of K65ER68G is obtained without oxidation, which is required by wild type PST. | en_US |
| dc.language.iso | zh_TW | en_US |
| dc.subject | 酚亚硫酸基转移酵素 | zh_TW |
| dc.subject | 分子模拟 | zh_TW |
| dc.subject | Phenol Sulfotransferase | en_US |
| dc.subject | computer modeling | en_US |
| dc.subject | PAP | en_US |
| dc.title | 用分子模拟探讨环状区胺基酸序列64~69对酚亚硫酸基转移酵素活性的影响 | zh_TW |
| dc.title | Effect of Loop Region 64~69 on the activity of Phenol Sulfotransferase: Analysis by Computer Modeling | en_US |
| dc.type | Thesis | en_US |
| dc.contributor.department | 生物科技学系 | zh_TW |
| 显示于类别: | Thesis | |
- 亚硫酸基转移之反应机制---酚亚硫酸基转移酵素之分子模拟、化学变性与定点突变 / 杨裕雄;YANG YUH-SHYONG
- 探讨半胱胺酸对酚亚硫酸基转移酵素的影响 / 陈姿尹;Tzu-Yin Chen;杨裕雄;Yuh-Shyong Yang
- 核□酸与酚亚硫酸基转移酵素结合诱导构型改变之研究 / 黄干吉;Huang, Chen-Ji;杨裕雄;Yuh-Shyong Yang
- 酚亚硫酸基转移酵素催化反应之管制与机制 / 杨裕雄;YANG YUH-SHYONG
- 半胱胺酸66与232协同调控氧化还原反应性酚亚硫酸基转移酵素之催化作用 / 林志衡;杨裕雄
- 酚亚硫酸基转移酵素催化机制之研究与修改(I) / 杨裕雄;YANG YUH-SHYONG
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