Engineering the pregnane X receptor and estrogen receptor alpha to bind novel small molecules using negative chemical complementation

Files
shaffer_hally_a_201105_phd.pdf (13.97 MB)
Author(s)
Shaffer, Hally A.
Advisor(s)
Azizi, Bahareh
Doyle, Donald F.
Editor(s)
Associated Organization(s)
Organizational Unit
Organizational Unit
Series
Series
Collections
Theses and Dissertations
Supplementary to:
Permanent Link
http://hdl.handle.net/1853/39620
Abstract
Nuclear receptors are ligand-activated transcription factors that play significant roles in various biological processes within the body, such as cell development, hormone metabolism, reproduction, and cardiac function. As transcription factors, nuclear receptors are involved in many diseases, such as diabetes, cancer, and arthritis, resulting in approximately 10-15% of the pharmaceutical drugs presently on the market being targeted toward nuclear receptors. Structurally, nuclear receptors consist of a DNA-binding domain (DBD), responsible for binding specific sequences of DNA called response elements, fused to a ligand-binding domain (LBD) through a hinge region. The LBD binds a small molecule ligand. Upon ligand binding, the LBD changes to an active conformation leading to the recruitment of coactivator (CoAC) proteins and initiation of transcription. As a result of their involvement in disease, there is an emphasis on engineering nuclear receptors for applications in gene therapy, drug discovery and metabolic engineering.
Sponsor
Date
2011-04-05
Extent
Resource Type
Text
Resource Subtype
Dissertation
Rights Statement
Rights URI