Molecular Characterization of the Human La Protein·Hepatitis B Virus RNA.B Interaction in Vitro

Horke, Sven; Reumann, Kerstin; Rang, Andreas; Heise, Tilman

doi:10.1074/jbc.m201911200

Cited by 40 publications

(59 citation statements)

References 54 publications

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“…In addition it has been shown that recombinant hLa interacts with in vitro transcribed HBV RNA.B (17). These data suggest an association of La and HBV RNA in living cells.…”

Section: Resultsmentioning

confidence: 67%

“…In contrast highly purified recombinant hLa binds HBV RNA.B with high affinity but with low specificity (17). It was concluded that accessory factors are required to specify the interaction between La and HBV RNA.B.…”

Section: Resultsmentioning

confidence: 99%

“…Expression, Purification, Phosphorylation, Dephosphorylation of Recombinant hLa Protein, and Preparation of Nuclear Extracts-Recombinant hLa protein was prepared as described previously (17). Phosphorylation of recombinant hLa was performed for 3 h at 37°C in 30-l reactions containing 1 g of hLa, 0.2 l of casein kinase II (New England Biolabs), 3 l of 10ϫ reaction buffer, and 6 l of 1 mM ATP.…”

Section: Methodsmentioning

confidence: 99%

“…While trying to evaluate the intracellular mechanism(s) responsible for the cytokine-mediated post-transcriptional destabilization of HBV RNA, the mouse La autoantigen (homologue to human La autoantigen) has been identified. The La protein interacts with a small cis-acting element located within the viral RNA between nt 1275 and 1291 (16,17). The tight temporal correlation between the cytokine-mediated down-regulation of HBV RNA and the cytokine-induced fragmentation of full-length La led to the assumption that full-length La stabilizes HBV RNA by interacting with the cis-acting element (18).…”

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confidence: 99%

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Functional Characterization of the Interaction between Human La and Hepatitis B Virus RNA

Ehlers

Horke

Reumann

et al. 2004

Journal of Biological Chemistry

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The La protein is a multifunctional RNA-binding protein and has also been suggested to be involved in the stabilization of hepatitis B virus (HBV) RNA. Here we demonstrate that antibodies against the human La protein specifically precipitate HBV RNA from HBV ribonucleoprotein-containing mammalian cell extracts, providing evidence for the association between human La and HBV RNA. Moreover, we report that the turnover of HBV RNA depends on structural features and less on the primary sequence of the La-binding site on the viral RNA. In addition we show that the interaction between human La and HBV RNA in vitro is modulated by accessory factor(s) in a phosphorylation-dependent manner. Taken together these data indicate that both structural features, the composition of La/HBV ribonucleoprotein particles as well as interacting cellular factors, are critical determinants in the regulation of the stability of the HBV RNA.RNA metabolism depends on the formation of ribonucleoprotein particles mediating diverse processes such as splicing, polyadenylation, nuclear export, and the regulation of mRNA stability (1, 2). The formation of RNPs 1 is a tightly controlled process, potentially regulated by several stimuli, including hormones and cytokines. Such stimuli can alter the RNA binding activity of proteins on the post-translational level by phosphorylation or dephosphorylation and thereby the processing and stability of RNAs (3-5). In addition, RNA processing depends on various cis-acting elements including splice sites, export elements, and endoribonucleolytic cleavage sites recognized by RNA-binding proteins. To understand fully the regulation of processing of a specific RNA, both trans-acting factors and cis-acting elements as well as their functions need to be known. The same applies for a detailed understanding of the metabolism of viral RNA. Such studies could lead to the identification of novel cellular targets valuable for the development of innovative antiviral strategies when focused on the post-transcriptional control of RNAs of viruses with global medical importance. This applies to hepatitis B virus (HBV) with more than 300 million chronically infected carriers worldwide who await more effective antiviral therapies.HBV is a noncytopathic, hepatotropic virus with a 3.2-kb circular DNA genome. After conversion into a covalently closed circular DNA, this genome serves in the nucleus as a template for transcription of all viral RNAs. Synthesis of these transcripts is driven by at least four promotors, leading to a large size heterogeneity with many different 5Ј-ends, whereas they all have very similar 3Ј-ends because of processing at the same polyadenylylation site (6). The so-called pregenomic RNA (slightly longer than genome length) is encapsidated into nucleocapsids where it is reverse-transcribed into viral DNA. This RNA serves also as messenger for synthesis of the viral P protein as well as for the core protein. The viral surface proteins as well as a regulatory protein with a role in hepatocarcinogenesis, des...

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“…In addition it has been shown that recombinant hLa interacts with in vitro transcribed HBV RNA.B (17). These data suggest an association of La and HBV RNA in living cells.…”

Section: Resultsmentioning

confidence: 67%

Section: Resultsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

mentioning

confidence: 99%

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Functional Characterization of the Interaction between Human La and Hepatitis B Virus RNA

Ehlers

Horke

Reumann

et al. 2004

Journal of Biological Chemistry

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“…Two conserved amino acid signatures within the RRMs, referred to as RNP-1 and RNP-2 (RNP consensus sequence), are essential for RNA binding (42). Recently, we have shown that the RNP-2 of RRM2 in hLa is required for binding of hepatitis B virus RNA (43), and it seems reasonable to assume that this motif is also required for the binding of cellular precursor transcripts. La interacts with RNA polymerase III products by binding the poly(U) stretch at the 3Ј-end common to this class of transcripts (44) or, in the case of the RNA polymerase II product U3 snoRNA, after partial processing exposing a poly(U) stretch (17).…”

mentioning

confidence: 99%

Nuclear Trafficking of La Protein Depends on a Newly Identified Nucleolar Localization Signal and the Ability to Bind RNA

Horke

Reumann

Schweizer

et al. 2004

Journal of Biological Chemistry

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Here we provide evidence for an interaction-dependent subnuclear trafficking of the human La (hLa) protein, known as transient interaction partner of a variety of RNAs. Among these, precursor transcripts of certain RNAs are located in the nucleoplasm or nucleolus. Here we examined which functional domains of hLa are involved in its nuclear trafficking. By using green fluorescent-hLa fusion proteins, we discovered a nucleolar localization signal and demonstrated its functionality in a heterologous context. In addition, we revealed that the RRM2 motif of hLa is essential both for its RNA binding competence in vitro and in vivo and its exit from the nucleolus. Our data imply that hLa traffics between different subnuclear compartments, which depend decisively on a functional nucleolar localization signal as well as on RNA binding. Directed trafficking of hLa is fully consistent with its function in the maturation of precursor RNAs located in different subnuclear compartments.The human La protein (hLa) 1 is a 47-kDa phosphoprotein predominantly localized in the nucleus. It was first discovered as an autoantigen recognized by antibodies present in the sera of patients suffering from systemic lupus erythematosus and Sjogren's syndrome (1, 2). The La protein is a member of a large group of RNA-binding proteins containing RNA recognition motifs (RRMs) (3-7) and interacts with a variety of small RNAs (for reviews see Refs. 8 -10). The La protein is implicated in several aspects of the RNA metabolism, including processing of precursors of tRNAs, U3 snoRNA, U1 RNA, U6 snRNA (11)(12)(13)(14)(15)(16)(17)(18)(19)(20), and stabilization of viral (21-23) as well as cellular RNAs (24). In the cytoplasm, La has been implicated in the translational control of viral (25-27) and cellular RNAs (28 -30).The human La protein contains a nuclear localization sequence at the very C-terminal end, and the staining for endogenous La as well as the distribution of GFP-tagged La reveal a predominantly diffuse nuclear staining, although this may appear different under certain conditions or treatments (31-33). Subcellular distribution of human and yeast La was assumed to be independent of phosphorylation (34, 35); however, recent studies (36, 37) revealed that phosphorylation at Ser-366 may well influence subcellular localization of La. A regulated, nonhomogeneous nuclear distribution of La may also be predicted from the distinct nuclear distribution of its various RNA interaction partners. For instance, pre-tRNAs are most likely synthesized in the nucleoplasm (38) but are processed, at least in part, in the nucleolus (39, 40), whereas in yeast the La-associated precursor of U3 snoRNA is probably processed in the nucleolar body and nucleolus (20). Nevertheless, interactions with precursor RNAs in different nuclear compartments implicate a highly dynamic and regulated nuclear distribution of La. Although a nucleolar localization of La has been reported (for review see Ref. 9), the hLa protein was not identified among the recently resolved protein ...

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Alteration of microRNA profiles by a novel inhibitor of human La protein in HBV‐transformed human hepatoma cells

Pan

Tong

Tang

2017

Journal of Medical Virology

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A pyrazolopyridine HBSC11 was previously identified as a novel inhibitor of human La protein with anti‐hepatitis B virus (HBV) activity. However, the underlying mechanism(s) of HBV inhibition by HBSC11 remains unclear. This study aimed to examine the regulation of microRNA (miRNA) by HBSC11 in HBV‐transformed human hepatoma HepG2.2.15 cells using microarray and quantitative real‐time PCR. Target genes of the differentially expressed miRNAs were predicted and subjected to bioinformatics analysis. Results showed that HBSC11 significantly upregulated the expression of miR‐3912‐5p, miR‐6793‐5p, and miR‐7159‐5p in HepG2.2.15 cells. Target genes of the three miRNAs were mainly involved in the regulation of nucleic acid‐templated transcription, negative regulation of gene expression, nucleic acid binding transcription factor activity and regulation of phosphorylation. In addition, target genes were enriched in certain regulatory pathways related to HBV infection and HBV‐associated disease progression, such as the transforming growth factor (TGF)‐β, Wnt, and p53 signaling. Our study demonstrates the involvement of miR‐3912‐5p, miR‐6793‐5p, and miR‐7159‐5p and the potential modulation of specific pathways (TGF‐β, Wnt, and p53 signaling) in HBSC11‐mediated inhibition of HBV replication. This study provides insight into the molecular mechanism of the action of HBSC11 against HBV infection and will support the development of antiviral drugs targeting La protein.

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Molecular Characterization of the Human La Protein·Hepatitis B Virus RNA.B Interaction in Vitro

Cited by 40 publications

References 54 publications

Functional Characterization of the Interaction between Human La and Hepatitis B Virus RNA

Functional Characterization of the Interaction between Human La and Hepatitis B Virus RNA

Nuclear Trafficking of La Protein Depends on a Newly Identified Nucleolar Localization Signal and the Ability to Bind RNA

Alteration of microRNA profiles by a novel inhibitor of human La protein in HBV‐transformed human hepatoma cells

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