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Virus Details


VHFID1957

Host Factor Information

Pathogen Information

Publication Information

Host Factor Information

Gene Name BPIFB6
HF Protein Name BPI fold-containing family B member 6
HF Function Essential for viral RNA replication
Uniprot ID Q8NFQ5
Protein Sequence View Fasta Sequence
NCBI Gene ID 128859
Host Factor (HF) Name in Paper BPIFB6
Gene synonyms BPIL3
Ensemble Gene ID ENSG00000167104
Ensemble Transcript ENST00000349552
KEGG ID Go to KEGG Database
Gene Ontology ID(s) GO:0005576, GO:0008289,
MINT ID N.A.
STRING Click to see interaction map
GWAS Analysis Click to see gwas analysis
OMIM ID 614110
PANTHER ID PTHR10504;PTHR10504:SF71
PDB ID(s) N.A.,
pfam ID PF01273, PF02886,
Drug Bank ID N.A.,
ChEMBL ID N.A.
Organism Homo sapiens (Human)

Pathogen Information

Virus Name Enterovirus 71
Virus Short Name EV-71
Order Picornavirales
Virus Family Picornaviridae
Virus Subfamily N.A.
Genus Enterovirus
Species Enterovirus A
Host Human, mammals
Cell Tropism The gastrointestinal trac
Associated Disease Hand, foot and mouth disease, meningitis
Mode of Transmission Either fecal-oral or respiratory
VIPR DB link https://www.viprbrc.org/brc/home.spg?decorator=picorna
ICTV DB link https://talk.ictvonline.org/ictv-reports/ictv_9th_report/positive-sense-rna-viruses-2011/w/posrna_viruses/234/picornaviridae
Virus Host DB link http://www.genome.jp/virushostdb/view/?virus_lineage=Picornaviridae

Publication Information

Paper Title BPIFB6 Regulates Secretory Pathway Trafficking and Enterovirus Replication
Author's Name Stefanie Morosky, Nicholas J. Lennemann, Carolyn B. Coyne
Journal Name JOURNAL OF VIROLOGY
Pubmed ID 26962226
Abstract Bactericidal/permeability-increasing protein (BPI) fold-containing family B, member 3 (BPIFB3) is an endoplasmic reticulum (ER)-localized host factor that negatively regulates coxsackievirus B (CVB) replication through its control of the autophagic pathway. Here, we show that another member of the BPIFB family, BPIFB6, functions as a positive regulator of CVB, and other enterovirus, replication by controlling secretory pathway trafficking and Golgi complex morphology. We show that similar to BPIFB3, BPIFB6 localizes exclusively to the ER, where it associates with other members of the BPIFB family. However, in contrast to our findings that RNA interference (RNAi)-mediated silencing of BPIFB3 greatly enhances CVB replication, we show that silencing of BPIFB6 expression dramatically suppresses enterovirus replication in a pan-viral manner. Mechanistically, we show that loss of BPIFB6 expression induces pronounced alterations in retrograde and anterograde trafficking, which correlate with dramatic fragmentation of the Golgi complex. Taken together, these data implicate BPIFB6 as a key regulator of secretory pathway trafficking and viral replication and suggest that members of the BPIFB family participate in diverse host cell functions to regulate virus infections. IMPORTANCE: Enterovirus infections are associated with a number of severe pathologies, such as aseptic meningitis, dilated cardiomyopathy, type I diabetes, paralysis, and even death. These viruses, which include coxsackievirus B (CVB), poliovirus (PV), and enterovirus 71 (EV71), co-opt the host cell secretory pathway, which controls the transport of proteins from the endoplasmic reticulum to the Golgi complex, to facilitate their replication. Here we report on the identification of a novel regulator of the secretory pathway, bactericidal/permeability-increasing protein (BPI) fold-containing family B, member 6 (BPIFB6), whose expression is required for enterovirus replication. We show that loss of BPIFB6 expression correlates with pronounced defects in the secretory pathway and greatly reduces the replication of CVB, PV, and EV71. Our results thus identify a novel host cell therapeutic target whose function could be targeted to alter enterovirus replication.
Used Model RD cells
DOI 10.1128/JVI.00170-16