Using a GFP-tagged TMEM184A Construct for Confirmation of Heparin Receptor Identity

Overview

Journal J Vis Exp

Specialties Biology
General Medicine

Date 2017 Mar 14

PMID 28287514

Citations 1

Authors

Sara Lynn N Farwell

Joshua B Slee

Yaqiu Li

Linda J Lowe-Krentz

Affiliations

Soon will be listed here.

Abstract

When novel proteins are identified through affinity-based isolation and bioinformatics analysis, they are often largely uncharacterized. Antibodies against specific peptides within the predicted sequence allow some localization experiments. However, other possible interactions with the antibodies often cannot be excluded. This situation provided an opportunity to develop a set of assays dependent on the protein sequence. Specifically, a construct containing the gene sequence coupled to the GFP coding sequence at the C-terminal end of the protein was obtained and employed for these purposes. Experiments to characterize localization, ligand affinity, and gain of function were originally designed and carried out to confirm the identification of TMEM184A as a heparin receptor. In addition, the construct can be employed for studies addressing membrane topology questions and detailed protein-ligand interactions. The present report presents a range of experimental protocols based on the GFP-TMEM184A construct expressed in vascular cells that could easily be adapted for other novel proteins.

Citing Articles

Novel Heparin Receptor Transmembrane Protein 184a Regulates Angiogenesis in the Adult Zebrafish Caudal Fin.

Farwell S, Reylander K, Iovine M, Lowe-Krentz L Front Physiol. 2017; 8:671.

PMID: 28936181 PMC: 5594097. DOI: 10.3389/fphys.2017.00671.

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