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Hepatitis B subviral envelope particles use the COPII machinery for intracellular transport via selective exploitation of Sec24A and Sec23B

Cell Microbiol. 2020; 
Zeyen L, Döring T, Stieler JT, Prange R.
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Molecular Biology Reagents … The expression vector pcDNA31(+)-N-Myc-Sec24A encoding the long Sec24A isoform (NM_0219822; aa 1-1093) with an N-terminal Myc-tag was purchased from GenScript A plasmid carrying the human Sar1A cDNA (NM_01142648) was … Get A Quote

摘要

Hepatitis B virus (HBV) is a leading cause of liver disease. Its success as a human pathogen is related to the immense production of subviral envelope particles (SVPs) contributing to viral persistence by interfering with immune functions. To explore cellular pathways involved in SVP formation and egress, we investigated host-pathogen interactions. Yeast-based proteomics revealed Sec24A, a component of the coat protein complex II (COPII), as an interaction partner of the HBV envelope S domain. To understand how HBV co-opts COPII as a proviral machinery, we studied roles of key Sec proteins in HBV-expressing liver cells. Silencing of Sar1, Sec23, and Sec24, which promote COPII assembly concomitant with cargo loa... More

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