Building a rational model for the identification of allosteric sites

Thesis

Download PDF

Creator

Rights statement

Awarding institution

Date of award

Thesis identifier

Person Identifier (Local)

Qualification Level

Qualification Name

Department, School or Faculty

Abstract

Allostery is the regulation of protein function, structure and/or flexibility that is induced by the binding of a ligand at a site distinct from the orthosteric site.1, 2 Interaction of a small molecule with these sites can bring greater selectivity as they are not conserved within a family and therefore could lead to new opportunities in drug discovery. Unfortunately, no definitive technique has yet been identified to distinguish these allosteric sites. Al-Shar'i developed a new technique using a combination of fluctuation analysis, cross correlation, simple intrasequence difference (SID) and energy analysis.3 A potential site has been determined for the protein kinase DYRK2 using this technique. The potential allosteric pocket was studied through a virtual screen which gave a hit that was successfully prepared and showed good selectivity for DYRK2 over DYRK1A by Differential Scanning Fluorimetry (DSF). This oxyamidine hit was further investigated through a structure activity relationship (SAR) which enabled the synthesis of three compounds that showed a higher stabilization than the initial hit (Tm > 1.2 °C). A second library was synthesized based on the same core, but with an amide functionality instead of an oxyamidine. From this new library, a SAR study was also carried out. This led to the synthesis of five analogues that have shown great binding activity (IC50 < 240nM) and selectivity for DYRK2.

Resource Type

DOI

Date Created

Former identifier

Relations

Thumbnail	Title	Date Uploaded	Visibility	Actions
	PDF of thesis T14284	2021-07-02	Public	Download