Glass is a Viable Substrate for Atomic Force Microscopy of Membrane Proteins

Nagaraju Chada; Krishna P. Sigdel; Tina R. Matin; Raghavendar Reddy Sanganna Gari; Chunfeng Mao; Linda L. Randall; Gavin M. King

doi:10.1016/j.bpj.2013.11.2596

What is it about?

Different microscope Like FRET, AFM and other optical techniques that study single molecule activity at the same time needs a common substrate. This work details about ways to treat glass coverslips, a widely used specimen support in biolody, to study same biological molecule enabling to achieve protein-protein interactions in real time.

Why is it important?

This work enables combining different microscopy techniques to study molecular activity at the same time

This page is a summary of: Glass is a Viable Substrate for Atomic Force Microscopy of Membrane Proteins, Biophysical Journal, January 2014, Elsevier,
DOI: 10.1016/j.bpj.2013.11.2596.
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Glass is a Viable Substrate for Atomic Force Microscopy of Membrane Proteins
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Glass is a Viable Substrate for Precision Force Microscopy of Membrane Proteins
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Nagaraju Chada
Johns Hopkins University

Common specimen support for different microscopy techniques

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