Evaluation of the in vivo role of vaccinia virus complement control protein (VCP) following renal ischemia

Doctoral Thesis

2006

Permanent link to this Item
http://hdl.handle.net/11427/2726
Files
thesis_hsf_2006_ghebremariam_y.pdf (26.91 MB)
Authors
Ghebremariam, Yohannes T
Supervisors
Kotwal, Girish J
Kahn, Del
Journal Title
Link to Journal
Journal ISSN
Volume Title
Publisher
Publisher

University of Cape Town

Department
Division of Virology
Faculty
Faculty of Health Sciences
License
Series
Abstract
In transplantation, vascularized organs often suffer the consequences of ischemic damage as well as reperfusion injury following the reestablishment of blood flow. The induced ischemialreperfusion (I/R) damage is usually associated with the accumulation of injurious complement components. The vaccinia virus complement control protein (VCP) has the ability to simultaneously inhibit the classical and the alternative complement pathways by binding to the early components C3b and C4b. The complement component C3 is known to be the central route to all of the known complement activation pathways. As a result, it is involved in a number of complement-mediated ailments including renal ischemia/reperfusion injury. The objectives of this study were to initially evaluate the in vitro roles of the natural VCP and the humanized recombinant VCP (hrVCP), and then to establish their in vivo roles in a renal I/R injury model.
Description

Includes bibliographical references (leaves 133-147)

Keywords
Medical Virology

Reference:

Ghebremariam, Y. 2006. Evaluation of the in vivo role of vaccinia virus complement control protein (VCP) following renal ischemia. University of Cape Town.

Collections
PhD / Doctoral