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
The roles of leukocyte cell adhesion...
~
O'Quinn, Darrell B.
FindBook
Google Book
Amazon
博客來
The roles of leukocyte cell adhesion molecules in mucosal inflammation.
紀錄類型:
書目-語言資料,印刷品 : Monograph/item
正題名/作者:
The roles of leukocyte cell adhesion molecules in mucosal inflammation./
作者:
O'Quinn, Darrell B.
面頁冊數:
112 p.
附註:
Adviser: Daniel C. Bullard.
Contained By:
Dissertation Abstracts International67-01B.
標題:
Biology, Animal Physiology. -
電子資源:
http://pqdd.sinica.edu.tw/twdaoapp/servlet/advanced?query=3201173
ISBN:
9780542489334
The roles of leukocyte cell adhesion molecules in mucosal inflammation.
O'Quinn, Darrell B.
The roles of leukocyte cell adhesion molecules in mucosal inflammation.
- 112 p.
Adviser: Daniel C. Bullard.
Thesis (Ph.D.)--The University of Alabama at Birmingham, 2005.
The process by which leukocytes move from the blood to a site of tissue injury is mediated by cell surface proteins collectively called adhesion molecules. Elucidation of the specific adhesion molecule pathways required for the recruitment of leukocytes to sites of inflammation is essential not only for our understanding of disease pathogenesis, but also for the improved design of therapeutic approaches targeting these proteins. Based on a review of the literature, we hypothesized that there was considerable redundancy in adhesion molecule function, especially in mediating T lymphocyte interactions. Specifically, we proposed that the blocking or removal of multiple adhesion molecules is required to completely prevent all lymphocyte emigration. To test this hypothesis, we performed investigations targeting the adhesion molecules PSGL-1, LFA-1, alpha4beta 7, alphaEbeta7, and VLA-4 using primarily the Citrobacter rodentium infectious model to induce tissue injury in the colon and elicit the recruitment of inflammatory cells. Briefly, our findings showed that the development of colitis in PSGL-1 mutant mice was not significantly altered. In addition, recruitment of CD3+ cells to the lamina propria was only slightly delayed in these mice, despite our previous finding that PSGL-1 was required for T helper cell rolling in an in vitro parallel-plate flow chamber. Conversely, removal of the integrin LFA-1 caused a profound delay in the appearance of C. rodentium-induced colitic lesions that was associated with a significant early reduction of infiltrating CD3+ cells in the lamina propria. When C. rodentium-infected LFA-1 mutant mice were treated with a monoclonal antibody which blocks interactions mediated by VLA-4 and alpha 4beta7, lymphocyte recruitment was effectively blocked and the histologic appearance of the lesions resembled those in comparably infected Rag-2 mutant mice. Finally, resolution of C. rodentium-induced colitis lesions in beta7 mutant mice were significantly delayed at 15 days post-inoculation, and despite additional blocking of VLA-4 interactions in subsequent experiments, significant inflammation and CD3+ cell recruitment were not blocked. Taken together, the overall conclusion of this study is that blocking and/or removal of multiple adhesion molecules, namely LFA-1, VLA-4, and alpha4beta7, is required to completely prevent all lymphocyte recruitment to inflamed colonic lamina propria.
ISBN: 9780542489334Subjects--Topical Terms:
1017835
Biology, Animal Physiology.
The roles of leukocyte cell adhesion molecules in mucosal inflammation.
LDR
:03360nam 2200289 a 45
001
970621
005
20110921
008
110921s2005 eng d
020
$a
9780542489334
035
$a
(UMI)AAI3201173
035
$a
AAI3201173
040
$a
UMI
$c
UMI
100
1
$a
O'Quinn, Darrell B.
$3
1294660
245
1 4
$a
The roles of leukocyte cell adhesion molecules in mucosal inflammation.
300
$a
112 p.
500
$a
Adviser: Daniel C. Bullard.
500
$a
Source: Dissertation Abstracts International, Volume: 67-01, Section: B, page: 0204.
502
$a
Thesis (Ph.D.)--The University of Alabama at Birmingham, 2005.
520
$a
The process by which leukocytes move from the blood to a site of tissue injury is mediated by cell surface proteins collectively called adhesion molecules. Elucidation of the specific adhesion molecule pathways required for the recruitment of leukocytes to sites of inflammation is essential not only for our understanding of disease pathogenesis, but also for the improved design of therapeutic approaches targeting these proteins. Based on a review of the literature, we hypothesized that there was considerable redundancy in adhesion molecule function, especially in mediating T lymphocyte interactions. Specifically, we proposed that the blocking or removal of multiple adhesion molecules is required to completely prevent all lymphocyte emigration. To test this hypothesis, we performed investigations targeting the adhesion molecules PSGL-1, LFA-1, alpha4beta 7, alphaEbeta7, and VLA-4 using primarily the Citrobacter rodentium infectious model to induce tissue injury in the colon and elicit the recruitment of inflammatory cells. Briefly, our findings showed that the development of colitis in PSGL-1 mutant mice was not significantly altered. In addition, recruitment of CD3+ cells to the lamina propria was only slightly delayed in these mice, despite our previous finding that PSGL-1 was required for T helper cell rolling in an in vitro parallel-plate flow chamber. Conversely, removal of the integrin LFA-1 caused a profound delay in the appearance of C. rodentium-induced colitic lesions that was associated with a significant early reduction of infiltrating CD3+ cells in the lamina propria. When C. rodentium-infected LFA-1 mutant mice were treated with a monoclonal antibody which blocks interactions mediated by VLA-4 and alpha 4beta7, lymphocyte recruitment was effectively blocked and the histologic appearance of the lesions resembled those in comparably infected Rag-2 mutant mice. Finally, resolution of C. rodentium-induced colitis lesions in beta7 mutant mice were significantly delayed at 15 days post-inoculation, and despite additional blocking of VLA-4 interactions in subsequent experiments, significant inflammation and CD3+ cell recruitment were not blocked. Taken together, the overall conclusion of this study is that blocking and/or removal of multiple adhesion molecules, namely LFA-1, VLA-4, and alpha4beta7, is required to completely prevent all lymphocyte recruitment to inflamed colonic lamina propria.
590
$a
School code: 0005.
650
4
$a
Biology, Animal Physiology.
$3
1017835
650
4
$a
Health Sciences, Immunology.
$3
1017716
650
4
$a
Health Sciences, Pharmacy.
$3
1017737
690
$a
0433
690
$a
0572
690
$a
0982
710
2 0
$a
The University of Alabama at Birmingham.
$3
1019443
773
0
$t
Dissertation Abstracts International
$g
67-01B.
790
$a
0005
790
1 0
$a
Bullard, Daniel C.,
$e
advisor
791
$a
Ph.D.
792
$a
2005
856
4 0
$u
http://pqdd.sinica.edu.tw/twdaoapp/servlet/advanced?query=3201173
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
W9129109
電子資源
11.線上閱覽_V
電子書
EB W9129109
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
(1)帳號:一般為「身分證號」;外籍生或交換生則為「學號」。 (2)密碼:預設為帳號末四碼。
帳號
.
密碼
.
請在此電腦上記得個人資料
取消
忘記密碼? (請注意!您必須已在系統登記E-mail信箱方能使用。)