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Parameters of Reserpine Analogs That Induce MSH2/MSH6-Dependent Cytotoxic Response.


ABSTRACT: Mismatch repair proteins modulate the cytotoxicity of several chemotherapeutic agents. We have recently proposed a "death conformation" of the MutS homologous proteins that is distinguishable from their "repair conformation." This conformation can be induced by a small molecule, reserpine, leading to DNA-independent cell death. We investigated the parameters for a small reserpine-like molecule that are required to interact with MSH2/MSH6 to induce MSH2/MSH6-dependent cytotoxic response. A multidisciplinary approach involving structural modeling, chemical synthesis, and cell biology analyzed reserpine analogs and modifications. We demonstrate that the parameters controlling the induction of MSH2/MSH6-dependent cytotoxicity for reserpine-analogous molecules reside in the specific requirements for methoxy groups, the size of the molecule, and the orientation of molecules within the protein-binding pocket. Reserpine analog rescinnamine showed improved MSH2-dependent cytotoxicity. These results have important implications for the identification of compounds that require functional MMR proteins to exhibit their full cytotoxicity, which will avoid resistance in MMR-deficient cells.

SUBMITTER: Vasilyeva A 

PROVIDER: S-EPMC2946608 | biostudies-literature | 2010 Sep

REPOSITORIES: biostudies-literature

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Parameters of Reserpine Analogs That Induce MSH2/MSH6-Dependent Cytotoxic Response.

Vasilyeva Aksana A   Clodfelter Jill E JE   Gorczynski Michael J MJ   Gerardi Anthony R AR   King S Bruce SB   Salsbury Freddie F   Scarpinato Karin D KD  

Journal of nucleic acids 20100913


Mismatch repair proteins modulate the cytotoxicity of several chemotherapeutic agents. We have recently proposed a "death conformation" of the MutS homologous proteins that is distinguishable from their "repair conformation." This conformation can be induced by a small molecule, reserpine, leading to DNA-independent cell death. We investigated the parameters for a small reserpine-like molecule that are required to interact with MSH2/MSH6 to induce MSH2/MSH6-dependent cytotoxic response. A multid  ...[more]

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