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Regulation of nucleocytoplasmic trafficking of viral proteins: An integral role in pathogenesis?☆

Authors :
Alex J. Fulcher
David A. Jans
Source :
Biochimica et Biophysica Acta. Molecular Cell Research
Publication Year :
2011
Publisher :
Elsevier B.V., 2011.

Abstract

Signal-dependent targeting of proteins into and out of the nucleus is mediated by members of the importin (IMP) family of transport receptors, which recognise targeting signals within a cargo protein and mediate passage through the nuclear envelope-embedded nuclear pore complexes. Regulation of this process is paramount to processes such as cell division and differentiation, but is also critically important for viral replication and pathogenesis; phosphorylation appears to play a major role in regulating viral protein nucleocytoplasmic trafficking, along with other posttranslational modifications. This review focuses on viral proteins that utilise the host cell IMP machinery in order to traffic into/out of the nucleus, and in particular those where trafficking is critical to viral replication and/or pathogenesis, such as simian virus SV40 large tumour antigen (T-ag), human papilloma virus E1 protein, human cytomegalovirus processivity factor ppUL44, and various gene products from RNA viruses such as Rabies. Understanding of the mechanisms regulating viral protein nucleocytoplasmic trafficking is paramount to the future development of urgently needed specific and effective anti-viral therapeutics. This article was originally intended for the special issue “Regulation of Signaling and Cellular Fate through Modulation of Nuclear Protein Import”. The Publisher apologizes for any inconvenience caused.<br />Research highlights ► Nucleocytoplasmic trafficking of viral proteins is central to viral infection. ► Posttranslational modification is a key means to regulate viral protein trafficking. ► Nuclear trafficking of viral proteins can be a target for development of anti-virals.

Subjects

Subjects :
Simian virus 40 T-ag
Nuclear import
viruses
PML, promyelocytic leukaemia protein
Human papillomavirus E1
BRAP2, BRCA1-associated protein 2
RbBS, retinoblastoma binding site
medicine.disease_cause
Nup, nucleoporin
HTLV, human T-cell leukaemia virus
Nuclear protein
Nuclear pore
RPP, Rabies virus phospho-protein
Phosphorylation
Rb, retinoblastoma
biology
CK2, protein kinase CK2
NES, nuclear export sequence
CTD, C-terminal domain
Cell biology
STAT, signal transducer and activator of transcription
medicine.anatomical_structure
Virus Diseases
T-ag, large tumour antigen
dsDNA-PK, double stranded DNA-dependent protein kinase
EBV, Epstein–Barr virus
BPV, bovine papillomavirus
CK1, protein kinase CK1
IMP, importin
Viral protein
CBP, CREB binding protein
Active Transport, Cell Nucleus
KSHV, Kaposi's sarcoma-associated herpes virus
NPC, nuclear pore complex
Importin
DLC-AS, DLC-association sequence
NLS, nuclear localisation sequence
Article
VZV, varicella zoster virus
Viral Proteins
MT-AS, MT-association sequence
Cyclin-dependent kinase
PKC, protein kinase C
medicine
GSK3, glycogen synthase kinase 3
Animals
Humans
DLC, dynein light chain
EXP, exportin
IFN, interferon
SARS, severe acute respiratory syndrome
Molecular Biology
PKA, protein kinase A PKC, protein kinase C
SV40, simian virus 40
FG, phenylalanine–glycine
HCMV, human cytomegalovirus
Cell Biology
Crm1, chromosome region maintenance protein 1
Virology
HPV, human papilloma virus
Rabies virus P
CAV, chicken anaemia virus
Human cytomegalovirus ppUL44
Cell nucleus
RV, Rabies virus
Viral replication
biology.protein
NE, nuclear envelope
Cdk, cyclin dependent kinase
LANA2, latency associated nuclear antigen 2
Nuclear transport
MT, microtubule

Details

Language :
English
ISSN :
18792596 and 01674889
Volume :
1813
Issue :
12
Database :
OpenAIRE
Journal :
Biochimica et Biophysica Acta. Molecular Cell Research
Accession number :
edsair.doi.dedup.....6ab7c90709803fd1a280dbdbc20c49e2