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PALM Imaging and Cluster Analysis of Protein Heterogeneity at the Cell Surface

Overview
Journal J Biophotonics
Date 2010 Feb 12
PMID 20148419
Citations 116
Authors
Dylan M Owen
Carles Rentero
Jeremie Rossy
Astrid Magenau
David Williamson
Macarena Rodriguez
Katharina Gaus
Affiliations
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Abstract

The authors employed photoactivatable localization microscopy (PALM) and direct stochastic optical reconstruction microscopy (dSTORM) imaging and image analysis based on Ripley's K-function to quantify the distribution and heterogeneity of proteins at the cell plasma membrane. The membrane targeting sequence of the N-terminal region of the T cell receptor-pathway kinase Lck fused to the photo-convertible fluorescent protein tdEos (Lck(N10)-tdEos), clusters into sub-100 nm regions which cover approximately 7% of the cell surface. 2-channel PALM imaging of Lck(N10)-tdEos and the N-terminus of the kinase Src (Src(N15)-PS-CFP2) are demonstrated. Finally, T cell microclusters at the immune synapse are imaged at super-resolution using dSTORM, showing that conventional TIRF images contain unresolved, small clusters. These methods are generally applicable to other cell and fluorophore systems to quantify 2-D molecular clustering at nanometer scales.

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