Controlled metabolic cell labeling and bioorthogonal click chemistry for cancer targeting

Wang, Hua

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https://hdl.handle.net/2142/90943 Copy

Description

Title

Controlled metabolic cell labeling and bioorthogonal click chemistry for cancer targeting

Author(s)

Wang, Hua

Issue Date

2016-04-22

Director of Research (if dissertation) or Advisor (if thesis)

Cheng, Jianjun

Doctoral Committee Chair(s)

Cheng, Jianjun

Committee Member(s)

• Kilian, Kristopher A.
• Lu, Yi
• Leal, Cecilia
• O'Brien, William D.

Department of Study

Materials Science & Engineerng

Discipline

Materials Science & Engr

Degree Granting Institution

University of Illinois at Urbana-Champaign

Degree Name

Ph.D.

Degree Level

Dissertation

Keyword(s)

• cancer targeting
• sugar
• cell labeling
• Click chemistry
• nanomedicine
• drug delivery
• cancer
• ultrasound

Abstract

The aim of my Ph.D. research is to develop a new, transformative cancer targeted therapy via the combination of unnatural sugar-mediated controlled metabolic cell labeling and bioorthogonal Click chemistry. By controlling the metabolic glycoengineering processes of unnatural sugars via rational chemistry designs, I was able to design a library of trigger-activatable sugar precursors that can label cell surface with chemical groups (e.g., azides) only in the presence of either exogenous triggers (ultraviolet (UV)) or endogenous triggers (H2O2, tumor hypoxia, NAD(P)H dehydrogenase quinone 1 (NQO1), and histone deacetylase (HDAC)/cathepsin L (CTSL)). Among them, HDAC/CTSL-responsive acetylated azidomannose (DCL-AAM) mediated excellent cancer-specific labeling in vitro and in vivo, which enhanced tumor accumulation of dibenzocyclooctyne (DBCO)-drug conjugates via efficient Click Chemistry between azides and DBCO and consequently exerted robust anticancer activities against LS174T colon cancer, MDA-MB-231 triple-negative breast cancer, and 4T1 metastatic breast cancer in murine models. DCL-AAM coupled with DBCO-drug conjugates, a new cancer targeted therapy which I name as Active Tissue Targeting via Anchored ClicK Chemistry (ATTACK), is essentially the small molecule version of antibody/antigen targeting technology and shows multiple advantages. Apart from the efforts in rational chemical designs of azido-sugars, I also developed sugar-loaded micelles and microbubbles for tumor labeling and targeting, in an effort to fully evaluate the advantages of Click chemistry-based cancer targeting strategy. Last but not least, I demonstrated that different types of unnatural sugars (e.g., azido-mannose and azido-galactose) have distinct labeling efficiencies in varying cancer types and that the use of reversible chemistries can impart the recyclability of cell-surface chemical receptors.

Graduation Semester

2016-05

Type of Resource

text

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http://hdl.handle.net/2142/90943

Copyright and License Information

Copyright 2016 Hua Wang

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