語系:
繁體中文
English
說明(常見問題)
回圖書館首頁
手機版館藏查詢
登入
回首頁
切換:
標籤
|
MARC模式
|
ISBD
Development of monolithic supports a...
~
Mallik, Rangan.
FindBook
Google Book
Amazon
博客來
Development of monolithic supports and improved immobilization methods for high-performance affinity chromatography and free drug analysis.
紀錄類型:
書目-語言資料,印刷品 : Monograph/item
正題名/作者:
Development of monolithic supports and improved immobilization methods for high-performance affinity chromatography and free drug analysis./
作者:
Mallik, Rangan.
面頁冊數:
329 p.
附註:
Adviser: David S. Hage.
Contained By:
Dissertation Abstracts International68-01B.
標題:
Chemistry, Analytical. -
電子資源:
http://pqdd.sinica.edu.tw/twdaoapp/servlet/advanced?query=3249672
Development of monolithic supports and improved immobilization methods for high-performance affinity chromatography and free drug analysis.
Mallik, Rangan.
Development of monolithic supports and improved immobilization methods for high-performance affinity chromatography and free drug analysis.
- 329 p.
Adviser: David S. Hage.
Thesis (Ph.D.)--The University of Nebraska - Lincoln, 2007.
This work combines five projects. In the first project, affinity monoliths based on a copolymer of glycidyl methacrylate (GMA) and ethylene dimethacrylate (EDMA) were developed for ultrafast immunoextractions. Rabbit immunoglobulin G (IgG) and anti-FITC antibodies were used as model ligands for this work. The antibody content of the monoliths was optimized by varying both the polymerization and immobilization conditions for preparing such supports. When a 4.5 mm i.d. x 0.95 mm monolith disk containing anti-FITC antibodies was used, 95% extraction of fluorescein was achieved in 100 ms.Subjects--Topical Terms:
586156
Chemistry, Analytical.
Development of monolithic supports and improved immobilization methods for high-performance affinity chromatography and free drug analysis.
LDR
:03162nam 2200313 a 45
001
957333
005
20110630
008
110630s2007 ||||||||||||||||| ||eng d
035
$a
(UMI)AAI3249672
035
$a
AAI3249672
040
$a
UMI
$c
UMI
100
1
$a
Mallik, Rangan.
$3
1280689
245
1 0
$a
Development of monolithic supports and improved immobilization methods for high-performance affinity chromatography and free drug analysis.
300
$a
329 p.
500
$a
Adviser: David S. Hage.
500
$a
Source: Dissertation Abstracts International, Volume: 68-01, Section: B, page: 0265.
502
$a
Thesis (Ph.D.)--The University of Nebraska - Lincoln, 2007.
520
$a
This work combines five projects. In the first project, affinity monoliths based on a copolymer of glycidyl methacrylate (GMA) and ethylene dimethacrylate (EDMA) were developed for ultrafast immunoextractions. Rabbit immunoglobulin G (IgG) and anti-FITC antibodies were used as model ligands for this work. The antibody content of the monoliths was optimized by varying both the polymerization and immobilization conditions for preparing such supports. When a 4.5 mm i.d. x 0.95 mm monolith disk containing anti-FITC antibodies was used, 95% extraction of fluorescein was achieved in 100 ms.
520
$a
In the second project, several immobilization methods were explored for the preparation of high-performance affinity monolithic columns containing human serum albumin (HSA). These monoliths were based on a copolymer of GMA and EDMA. Each HSA monolith was evaluated in terms of its total protein content and its retention of (R/S)-warfarin and D/L-tryptophan.
520
$a
In the third project, affinity monoliths based on silica and containing immobilized HSA or alpha1-acid glycoprotein (AGP) were developed and evaluated in terms of their binding, efficiency and selectivity in chiral separations. It was found that the amount of immobilized protein per unit volume, retention, efficiency and resolving power (for chiral drugs) of silica monoliths containing HSA or AGP were better than columns containing silica particles or GMA/EDMA monoliths.
520
$a
The fourth project introduced two techniques using maleimide-activated silica (the SMCC method) or iodoacetyl-activated silica (the SIA method) for the immobilization of HSA and other ligands to silica through sulfhydryl groups. A key advantage of the supports developed in this work is that they offer the potential of giving greater site-selective immobilization and ligand activity than amine-based coupling methods.
520
$a
The fifth project introduced a new ultrafast extraction technique for free drug analysis and determination of association equilibrium constants for drug-protein binding. Some advantages of this method include its speed (approximately 5 min per run) and its ability to use the same affinity column for more than one type of drug.
590
$a
School code: 0138.
650
4
$a
Chemistry, Analytical.
$3
586156
650
4
$a
Chemistry, Polymer.
$3
1018428
690
$a
0486
690
$a
0495
710
2
$a
The University of Nebraska - Lincoln.
$3
1024939
773
0
$t
Dissertation Abstracts International
$g
68-01B.
790
$a
0138
790
1 0
$a
Hage, David S.,
$e
advisor
791
$a
Ph.D.
792
$a
2007
856
4 0
$u
http://pqdd.sinica.edu.tw/twdaoapp/servlet/advanced?query=3249672
筆 0 讀者評論
館藏地:
全部
電子資源
出版年:
卷號:
館藏
1 筆 • 頁數 1 •
1
條碼號
典藏地名稱
館藏流通類別
資料類型
索書號
使用類型
借閱狀態
預約狀態
備註欄
附件
W9121103
電子資源
11.線上閱覽_V
電子書
EB W9120978
一般使用(Normal)
在架
0
1 筆 • 頁數 1 •
1
多媒體
評論
新增評論
分享你的心得
Export
取書館
處理中
...
變更密碼
登入