Proteomic mapping by rapamycin-dependent targeting of APEX2 identifies binding partners of VAPB at the inner nuclear membrane

2019 | journal article; research paper. A publication with affiliation to the University of Göttingen.

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​Proteomic mapping by rapamycin-dependent targeting of APEX2 identifies binding partners of VAPB at the inner nuclear membrane​
James, C.; Müller, M.; Goldberg, M. W.; Lenz, C. ; Urlaub, H.   & Kehlenbach, R. H. ​ (2019) 
Journal of Biological Chemistry294(44) pp. 16241​-16254​.​ DOI: https://doi.org/10.1074/jbc.RA118.007283 

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Authors
James, Christina; Müller, Marret; Goldberg, Martin W.; Lenz, Christof ; Urlaub, Henning ; Kehlenbach, Ralph H. 
Abstract
Vesicle-associated membrane protein–associated protein B (VAPB) is a tail-anchored protein that is present at several contact sites of the endoplasmic reticulum (ER). We now show by immunoelectron microscopy that VAPB also localizes to the inner nuclear membrane (INM). Using a modified enhanced ascorbate peroxidase 2 (APEX2) approach with rapamycin-dependent targeting of the peroxidase to a protein of interest, we searched for proteins that are in close proximity to VAPB, particularly at the INM. In combination with stable isotope labeling with amino acids in cell culture (SILAC), we confirmed many well-known interaction partners at the level of the ER with a clear distinction between specific and nonspecific hits. Furthermore, we identified emerin, TMEM43, and ELYS as potential interaction partners of VAPB at the INM and the nuclear pore complex, respectively.
Issue Date
2019
Journal
Journal of Biological Chemistry 
Project
SFB 1190: Transportmaschinen und Kontaktstellen zellulärer Kompartimente 
SFB 1190 | P07: Dynamik von Proteinen der inneren Kernmembran 
Working Group
RG Kehlenbach (Nuclear Transport) 
RG Urlaub (Bioanalytische Massenspektrometrie) 
Language
English

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