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Query: UMLS:C0023418 (
leukemia
)
93,477
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The rhesus macaque tripartite motif containing protein
TRIM5alpha
specifically restricts HIV-1 infection at an early post-entry step before reverse transcription [Stremlau, M., Owens, C. M., Perron, M. J., Kiessling, M., Autissier, P. & Sodroski, J. (2004) Nature 427, 848-853]. Here, we show that the human and African green monkey (AGM)
TRIM5alpha
genes encode Ref1 and Lv1 antiretroviral activities, respectively. Expression of
TRIM5alpha
in permissive cat cells renders them resistant to restriction-sensitive murine
leukemia
virus but not closely related insensitive virus. Disruption of
TRIM5alpha
expression in human and AGM cells with small interfering RNA rescues infectivity of restricted virus without affecting unrestricted virus. We also demonstrate that the activity of the murine restriction factor Fv1 depends on
TRIM5alpha
expression when Fv1 is expressed in human cells. Furthermore, a drug that modifies the behavior of the related promyelocytic leukemia protein PML specifically rescues infection by viruses restricted by human
TRIM5alpha
. Alignment of the
TRIM5alpha
proteins from rhesus macaque and AGM indicates an 18-aa insertion. We speculate that this insertion may contribute to the broader specificity of the AGM
TRIM5alpha
restriction as compared with the human and rhesus macaque proteins.
...
PMID:The human and African green monkey TRIM5alpha genes encode Ref1 and Lv1 retroviral restriction factor activities. 1525 4
Murine
leukemia
viruses (MLVs) have been classified as N-tropic (N-MLV) or B-tropic (B-MLV), depending on their ability to infect particular mouse strains. The early phase of N-MLV infection is blocked in the cells of several mammalian species, including humans. This block is mediated by a dominant host factor that targets the viral capsid soon after virus entry into the cell has been achieved. A similar block to HIV-1 in rhesus monkey cells is mediated by
TRIM5alpha
. Here we show that human
TRIM5alpha
is both necessary and sufficient for the restriction of N-MLV in human cells. Rhesus monkey
TRIM5alpha
, which potently blocks HIV-1 infection, exhibited only modest inhibition of N-MLV infection. B-MLV was resistant to the antiviral effects of both human and rhesus monkey
TRIM5alpha
; susceptibility to
TRIM5alpha
-mediated restriction was conferred by alteration of residue 110 of the B-MLV capsid protein to the amino acid found in the N-MLV capsid. Our results demonstrate that species-specific variation in
TRIM5alpha
governs its ability to block infection by diverse retroviruses.
...
PMID:TRIM5alpha mediates the postentry block to N-tropic murine leukemia viruses in human cells. 1528 May 39
The
TRIM5alpha
proteins of humans and some Old World monkeys have been shown to block infection of particular retroviruses following virus entry into the host cell. Infection of most New World monkey cells by the simian immunodeficiency virus of macaques (SIVmac) is restricted at a similar point. Here we examine the antiretroviral activity of
TRIM5alpha
orthologs from humans, apes, Old World monkeys, and New World monkeys. Chimpanzee and orangutan
TRIM5alpha
proteins functionally resembled human
TRIM5alpha
, potently restricting infection by N-tropic murine
leukemia
virus (N-MLV) and moderately restricting human immunodeficiency virus type 1 (HIV-1) infection. Notably,
TRIM5alpha
proteins from several New World monkey species restricted infection by SIVmac and the SIV of African green monkeys, SIVagm. Spider monkey
TRIM5alpha
, which has an expanded B30.2 domain v3 region due to a tandem triplication, potently blocked infection by a range of retroviruses, including SIVmac, SIVagm, HIV-1, and N-MLV. Tandem duplications in the
TRIM5alpha
B30.2 domain v1 region of African green monkeys are also associated with broader antiretroviral activity. Thus, variation in
TRIM5alpha
proteins among primate species accounts for the observed patterns of postentry restrictions in cells from these animals. The
TRIM5alpha
proteins of some monkey species exhibit dramatic lengthening of particular B30.2 variable regions and an expanded range of susceptible retroviruses.
...
PMID:Retrovirus restriction by TRIM5alpha variants from Old World and New World primates. 1576 95
TRIM5 is a determinant of species-specific differences in susceptibility to infection by retroviruses bearing particular capsids. Human immunodeficiency virus type 1 (HIV-1) infection is blocked by the alpha isoform of macaque TRIM5 (
TRIM5alpha
(rh)) or by the product of the owl monkey TRIM5-cyclophilin A gene fusion (TRIMCyp). Human
TRIM5alpha
potently restricts specific strains of murine
leukemia
virus (N-MLV) but has only a modest effect on HIV-1. The amino termini of TRIM5 orthologues are highly conserved and possess a coiled-coil domain that promotes homomultimerization. Here we show that heterologous expression of
TRIM5alpha
(rh) or TRIMCyp in human cells interferes with the anti-N-MLV activity of endogenous human
TRIM5alpha
(
TRIM5alpha
(hu)). Deletion of the cyclophilin domain from TRIMCyp has no effect on heteromultimerization or colocalization with
TRIM5alpha
(hu) but prevents interference with anti-N-MLV activity. These data demonstrate that TRIM5 orthologues form heteromultimers and indicate that C-terminal extensions alter virus recognition by multimers of these proteins.
...
PMID:Disruption of human TRIM5alpha antiviral activity by nonhuman primate orthologues. 1591 43
Members of the tripartite motif (TRIM) protein family are involved in various cellular processes, including cell proliferation, differentiation, development, oncogenesis and apoptosis. Some TRIM proteins display antiviral properties, targeting retroviruses in particular. The potential activity of TRIM19, better known as promyelocytic
leukaemia
protein, against several viruses has been well documented and, recently,
TRIM5alpha
has been identified as the factor responsible for the previously described Lv1 and Ref1 antiretroviral activities. There is also evidence indicating that other TRIM proteins can influence viral replication. These findings are reviewed here, and the possibility that TRIMs represent a new and widespread class of antiviral proteins involved in innate immunity is also considered.
...
PMID:TRIM family proteins: retroviral restriction and antiviral defence. 1617 75
The Ref1 and Lv1 postentry restrictions in human and monkey cells have been analyzed for lentiviruses in the primate and ungulate groups, but no data exist for the third (feline) group. We compared feline immunodeficiency virus (FIV) to other restricted (human immunodeficiency virus type 1 [HIV-1], equine infectious anemia virus [EIAV]) and unrestricted (NB-tropic murine
leukemia
virus [NB-MLV]) retroviruses across wide ranges of viral inputs in cells from multiple primate and nonprimate species. We also characterized restrictions conferred to permissive feline and canine cells engineered to express rhesus and human
TRIM5alpha
proteins and performed RNA interference (RNAi) against endogenous
TRIM5alpha
. We find that expression of rhesus or human
TRIM5alpha
proteins in feline cells restricts FIV, impairing pseudotyped vector transduction and viral replication, but rhesus
TRIM5alpha
is more restricting than human
TRIM5alpha
. Notably, however, canine cells did not support restriction by human
TRIM5alpha
and supported minimal restriction by rhesus
TRIM5alpha
, suggesting that these proteins may not function autonomously or that a canine factor interferes. Stable RNAi knockdown of endogenous rhesus
TRIM5alpha
resulted in marked increases in FIV and HIV-1 infectivities while having no effect on NB-MLV. A panel of nonprimate cell lines varied widely in susceptibility to lentiviral vector transduction, but normalized FIV and HIV-1 vectors varied concordantly. In contrast, in human and monkey cells, relative restriction of FIV compared to HIV-1 varied from none to substantial, with the greatest relative infectivity deficit for FIV vectors observed in human T-cell lines. Endogenous and introduced
TRIM5alpha
restrictions of FIV could be titrated by coinfections with FIV, HIV-1, or EIAV virus-like particles. Arsenic trioxide had complex and
TRIM5alpha
-independent enhancing effects on lentiviral but not NB-MLV infection. Implications for human gene therapy are discussed.
...
PMID:Restriction of feline immunodeficiency virus by Ref1, Lv1, and primate TRIM5alpha proteins. 1630 89
The restriction factors Fv1 and
TRIM5alpha
provide dominant blocks to retroviral infection, targeting incoming capsids at a postentry, preintegration step. They both restrict N-tropic murine
leukemia
virus with similar specificity yet act at different points in the viral life cycle.
TRIM5alpha
-restricted virus is usually unable to reverse transcribe, whereas Fv1-restricted virus reverse transcribes normally. Here we investigate the relationship between these two restriction factors by expressing Fv1 alleles in human cells. We demonstrate that Fv1 is able to compete with
TRIM5alpha
for virus before reverse transcription. In human cells expressing Fv1(b), N-tropic restricted virus becomes less infectious but reverse transcribes more efficiently, indicating competition between the two antiviral molecules and protection of the virus from
TRIM5alpha
by Fv1. Our findings suggest that, like
TRIM5alpha
, Fv1 interacts with virus before reverse transcription, but the consequences of this interaction are not realized until a later stage of the life cycle. We also demonstrate that Fv1 is functionally independent of
TRIM5alpha
when expressed in human cells.
...
PMID:Retroviral restriction factors Fv1 and TRIM5alpha act independently and can compete for incoming virus before reverse transcription. 1647 18
Cyclophilin A (CypA), a cytoplasmic, human immunodeficiency virus type 1 (HIV-1) CA-binding protein, acts after virion membrane fusion with human cells to increase HIV-1 infectivity. HIV-1 CA is similarly greeted by CypA soon after entry into rhesus macaque or African green monkey cells, where, paradoxically, the interaction decreases HIV-1 infectivity by facilitating
TRIM5alpha
-mediated restriction. These observations conjure a model in which CA recognition by the human
TRIM5alpha
orthologue is precluded by CypA. Consistent with the model, selection of a human cell line for decreased restriction of the
TRIM5alpha
-sensitive, N-tropic murine
leukemia
virus (N-MLV) rendered HIV-1 transduction of these cells independent of CypA. Additionally, HIV-1 virus-like particles (VLPs) saturate N-MLV restriction activity, particularly when the CA-CypA interaction is disrupted. Here the effects of CypA and
TRIM5alpha
on HIV-1 restriction were examined directly. RNA interference was used to show that endogenous human
TRIM5alpha
does indeed restrict HIV-1, but the magnitude of this antiviral activity was not altered by disruption of the CA-CypA interaction or by elimination of CypA protein. Conversely, the stimulatory effect of CypA on HIV-1 infectivity was completely independent of human
TRIM5alpha
. Together with previous reports, these data suggest that CypA protects HIV-1 from an unknown antiviral activity in human cells. Additionally, target cell permissivity increased after loading with heterologous VLPs, consistent with a common saturable target that is epistatic to both
TRIM5alpha
and the putative CypA-regulated restriction factor.
...
PMID:Cyclophilin A and TRIM5alpha independently regulate human immunodeficiency virus type 1 infectivity in human cells. 1650 Oct 94
Human immunodeficiency virus type 1 (HIV-1) shows a very narrow host range limited only to humans and chimpanzees. HIV-1 dose not experimentally infect Old World monkeys, such as rhesus and cynomolgus monkeys, and fails to replicate in activated CD4 positive T lymphocytes obtained from those monkeys. Several lines of evidence have suggested that the block of HIV-1 replication in Old World monkey cells occurred at a post-entry step and appeared to result from a failure to initiate reverse transcription. Recently, the screening of a rhesus monkey cDNA library identified tripartite motif 5 (TRIM5) alpha, a component of cytoplasmic bodies, as a factor that confers resistance to HIV-1 infection. Shortly after,
TRIM5alpha
of African green monkey, another Old World monkey, was also shown to restrict HIV-1 infection, while human
TRIM5alpha
was reported to restrict N-tropic murine
leukemia
virus. Small amino acid differences in the SPRY domain among human and monkey TRIM5alphas were reported to determine species-specific restriction. This review discusses about anti-viral activity of
TRIM5alpha
.
...
PMID:[TRIM5alpha]. 1655 11
Human
TRIM5alpha
(
TRIM5alpha
(hu)) potently restricts N-tropic (N-MLV), but not B-tropic, murine
leukemia
virus in a manner dependent upon residue 110 of the viral capsid. Rhesus monkey
TRIM5alpha
(
TRIM5alpha
(rh)) inhibits N-MLV only weakly. The study of human-monkey
TRIM5alpha
chimerae revealed that both the v1 and v3 variable regions of the B30.2/SPRY domain contain potency determinants for N-MLV restriction. These variable regions are predicted to be surface-exposed elements on one face of the B30.2 domain. Acidic residues in v3 complement basic residue 110 of the N-MLV capsid. The results support recognition of the retroviral capsid by the
TRIM5alpha
B30.2 domain.
...
PMID:Two surface-exposed elements of the B30.2/SPRY domain as potency determinants of N-tropic murine leukemia virus restriction by human TRIM5alpha. 1669 44
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