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Affinity-based chemoproteomics with small molecule-peptide conjugates. | LitMetric

Affinity-based chemoproteomics with small molecule-peptide conjugates.

Methods Mol Biol

Shantani Proteome Analytics Pvt. Ltd., Pune, MH, India.

Published: March 2012

AI Article Synopsis

  • In affinity-based chemoproteomics, directly attaching small bioactive probes to a solid surface can reduce their ability to bind to target proteins effectively.
  • Typically, immobilized probes have lower affinity for their targets, leading to potential capture failures or significant losses in the washing process.
  • To address these issues, small molecule-peptide conjugates (SMPCs) have been developed, which facilitate the identification of protein targets in cells and tissues while allowing for customization and tracking cellular localization.

Article Abstract

In affinity-based chemoproteomics strategies, the direct immobilization of small bioactive probe molecules to a solid support may pose problems with respect to the preservation of the functional activity toward the target proteins. Typically, immobilized molecules on solid supports exhibit lower affinity for target proteins compared to the free parent molecule. This may lead to a failure to specifically capture the target proteins or to unacceptable losses during the washing steps. To circumvent these shortcomings, we have devised small molecule-peptide conjugates (SMPCs), which enable wide-ranging experimental strategies for the capturing of protein targets of small molecules from cells or tissues. With the possibilities of synthesizing peptides of tailored biochemical and biophysical properties, SMPCs enable the identification of protein targets of small molecules from cell-lysates and intact cells. Moreover, labeling of these conjugates with fluorophores can provide information on the cellular localization and distribution of the target.

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Source
http://dx.doi.org/10.1007/978-1-61779-364-6_4DOI Listing

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