Wayne Widdison

Publications of Wayne Widdison

  • Design of antibody-maytansinoid conjugates allows for efficient detoxification via liver metabolism.

    Authors: Xiuxia Sun, Wayne Widdison, Michele Mayo, Sharon Wilhelm, Barbara Leece, Ravi Chari, Rajeeva Singh, Hans Erickson

    Bioconjugate chemistry. 03/2011; 22(4):728-35.

    Antibody-maytansinoid conjugates (AMCs) are targeted chemotherapeutic agents consisting of a potent microtubule-depolymerizing maytansinoid (DM1 or DM4) attached to lysine residues of a monoclonal
  • Disulfide-linked antibody-maytansinoid conjugates: optimization of in vivo activity by varying the steric hindrance at carbon atoms adjacent to the disulfide linkage.

    Authors: Brenda A Kellogg, Lisa Garrett, Yelena Kovtun, Katharine C Lai, Barbara Leece, Michael Miller, Gillian Payne, Rita Steeves, Kathleen R Whiteman, Wayne Widdison, Hongsheng Xie, Rajeeva Singh, Ravi V J Chari, John M Lambert, Robert J Lutz

    Bioconjugate chemistry. 03/2011; 22(4):717-27.

    In this report, we describe the synthesis of a panel of disulfide-linked huC242 (anti-CanAg) antibody maytansinoid conjugates (AMCs), which have varying levels of steric hindrance around the
  • Maytansine and cellular metabolites of antibody-maytansinoid conjugates strongly suppress microtubule dynamics by binding to microtubules.

    Authors: Manu Lopus, Emin Oroudjev, Leslie Wilson, Sharon Wilhelm, Wayne Widdison, Ravi Chari, Mary Ann Jordan

    Molecular cancer therapeutics. 10/2010; 9(10):2689-99.

    Maytansine is a potent microtubule-targeted compound that induces mitotic arrest and kills tumor cells at subnanomolar concentrations. However, its side effects and lack of tumor specificity have

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Keywords of Wayne Widdison

37 high-affinity sites
 
analogous lysine-linked maytansinoid metabolites
 
antibody-conjugated maytansine derivatives
 
disulfide-linked antibody-maytansinoid conjugates
 
dynamic instability
 
high-affinity sites
 
intermediate disulfide bond stability
 
maytansine derivatives
 
S-methyl-DM4 inhibited polymerization
 
tumor cells
 
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