Recombinant Hepatitis B virus genotype D subtype ayw Capsid protein (C)

1. In conclusion, the s identify filamin B as a novel host factor that can interact with core protein to promote hepatitis B virus replication in hepatocytes. PMID: 29594956
2. highly prevalent naturally occurring BCP and preCore mutations modulate HBV-induced autophagy. PMID: 29738548
3. RBM24 interacted with the 5' TR of HBV pregenomic RNA to block 80S ribosome assembly on HBV pgRNA and thus inhibited core protein translation, whereas the interaction between RBM24 and the 3' TR enhanced the stability of HBV RNA. PMID: 29760415
4. HBV basal core promoter variants was the strongest predictor of significant fibrosis in Hepatitis B virus infected patients PMID: 27988305
5. HBc promoted hepatocellular carcinoma cells motility by regulating the miR-382-5p/DLC-1 axis, which might provide a novel target for clinical diagnosis and treatment. PMID: 28982593
6. Together, these results indicate that Rab33B is an important player in intracellular hepatitis B virus trafficking events, guiding core transport to nucleocapsid assembly sites and/or nucleocapsid transport to budding sites. PMID: 28635671
7. Basal core promoter A1762T/G1764A dual mutations increase the risk of HBV-related hepatocellular carcinoma, particularly in an HBV genotype C population, even without progression to cirrhosis (meta-analysis). PMID: 26848866
8. The basal core promoter and preCore mutants induced higher levels of apoptosis in human hepatocytes than the wt virus. PMID: 29096158
9. KIR content genotypes associate with carriage of hepatitis B surface antigen, e antigen and HBV viral load in Gambians. PMID: 29149205
10. Western blotting and MS results indicated that rHBeAg and HBeAg are essentially structurally identical, although HBeAg from different patients exhibits minor carboxyl-terminal heterogeneity. PMID: 28842495
11. IL-15 mRNA and protein levels significantly increased in rhHBcAg stimulation group compared with non-stimulated group. PMID: 28274303
12. Data show that failure to achieve Hepatitis B e Antigens (HBeAg) seroclearance were the factors significantly associated with virological breakthrough (VBT). PMID: 28350873
13. In HBeAg (+) subjects, the AUROC of hepatitis B core antibody (anti-HBc) levels for predicting significant fibrosis was 0.734, while in HBeAg (-) subjects, the AUROC was 0.707. PMID: 28052021
14. HBeAg and its precursors promote HDM2-mediated degradation and impair transcriptional activity of p53 by interacting with NUMB, consequently contributing to hepatocellular carcinoma development. PMID: 27106262
15. Therefore, it is evident that the presence of G1862T in subgenotype A1 hepatitis B virus does not completely abolish HBeAg expression, but affects the rate of HBeAg maturation, its passage through the secretory pathway and activation of the unfolded protein response. PMID: 28678685
16. hepatitis B virus mutations in the basal core promoter/precore region are associated with an increase in the risk of hepatitis B-related acute-on-chronic liver failure (meta-analysis). PMID: 26984835
17. HBcAg contributes to the decrease of myeloid dendritic cells during chronic hepatitis B infection. PMID: 27617403
18. Among 124,865 patients with chronic hepatitis B (CHB)infection, 324 (0.3%) were concurrently positive for hepatitis B surface antigen (HBsAg), and 206 (0.2%) were concurrently positive for hepatitis B surface E antigen (HBeAg). PMID: 28252163
19. HBeAg negative hepatitis B patients tend to have HBV pre-core mutations. However, these mutations do not cause increased DNA copies, but associate with damage of liver function. PMID: 27004005
20. Patients with HBV genotype C viruses, high viral load and having mutations in the Hepatitis B virus basal core promoter/precore region, were more susceptible to developing liver cirrhosis. PMID: 26577140
21. study found that individuals infected with HBV withwith basal core promoter (BCP) double mutations (A1762T, G1764A)have lower concentrations of serum DLD than those with the wild-type BCP PMID: 27303803
22. The presence of BCP variant(s) was associated with aspartate aminotransferase-to-platelet index ratio >/=0.7 (P=0.029), but it was not associated with abnormal imagingbiopsy results in chronic hepatitis B patients. PMID: 26401823
23. Daata show that the empty patitis B virus (HBV) core (HBc) virus-like particles (VLPs) were able to effectively package the added DNA and RNA sequences. PMID: 26113394
24. Point mutation in Hepatitis B core Antigen is associated with acute on chronic liver failure. PMID: 25849554
25. Hepatitis B virus core protein activates Enhancer I through its binding to cAMP response element (CRE), increasing the concurrent accumulation of CREB/CBP on CRE, and thus increases CRE transcriptional activation. PMID: 25936964
26. PC/BCP mutants become predominant in a dynamic and continuous process in hepatitis B. PMID: 26074702
27. The basal core promoter/pre-core mutations T1753V, A1762T, G1764A, C1766T, T1768A, A1846T, G1896A and G1899A, and an HBeAg-negative status correlate with an increased risk of acute-on-chronic liver failure. PMID: 26063382
28. The naturally occurring mutations P5T/H/L of the HBV core antigen induced endoplasmic reticulum stress. PMID: 25828947
29. These findings highlight the role of HBeAg in regulating hepatitis B virus replication fitness and transcription efficiency and new insights on the early steps of replication in the G1896A mutant. PMID: 26119876
30. nine residues in HBV core under selection pressure in the presence of 10 different HLA class I alleles PMID: 25720337
31. Studied the prevalence of basal core promoter (BCP) and precore gene (PC) mutations in hepatitis B virus (HBV) isolates among the Nicobarese tribe and their relationship with genotypes and HBeAg status. PMID: 25323975
32. Capsid proteins plays a role in regulating genome replication. PMID: 25568211
33. These results revealed that carboxyl-terminal domain can inhibit multiple stages of viral replication, and its effects may be mediated at least in part through specific host interactions. PMID: 25540387
34. In conclusion, the expression of hepatitis B virus core protein sensitized hepatocytes to TNF-alpha-induced apoptosis by disrupting the interaction between MKK7 and RACK1. PMID: 25428880
35. Hepatitis B virus e antigen downregulated interleukin-18-mediated cell signaling and interferon gamma expression. PMID: 24872585
36. s postulate that key mutations throughout the X/preC region may be added to the basal core promoter double mutation and influence the complicated changes in genomic activity for HBeAg expression and HBV DNA replication. PMID: 24344773
37. These data highlight the essential role of precores propeptide in switching between different conformations for different functions and pinpoint the propeptide tryptophan residues as central in these properties. PMID: 24999840
38. Serum HBsAg levels should be monitored in the management of patients with HBeAg-seronegative chronic hepatitis B. PMID: 24700432
39. The hepatitis B core antigen P135Q mutant emergence during the inflammatory phase was associated with altered HBV capsid assembly, HBeAg biosynthesis, and reduced human immune responses following HBeAg seroconversion. PMID: 24273041
40. results showed the prevalence of HBc gene mutations is frequent in Iranian Hepatitis B virus (HBV)infected patients; it appears that escape from immune responses is a plausible reason for the high prevalence of HBc gene mutations among Iranian HBV infected patients PMID: 24600970
41. The C-terminal arginine-rich domain (ARD) and the ARD-bound RNAs of HBV core protein are partially-ordered and connected with the outer layer through linkers positioned around the two-fold axes. PMID: 24039702
42. Lower baseline levels of HBsAg might reflect the status of advanced liver fibrosis in HBeAg positive chronic hepatitis B patients. PMID: 23731848
43. The structure of HBV capsid in complex with AT-130, a member of the phenylpropenamide family of assembly effectors. PMID: 23871485
44. Combined HBV basal core promoter double mutations and pre-S deletion may not increase the risk of hepatocellular carcinoma, although these mutations are a risk factor of HCC when they present alone. PMID: 23517325
45. hepatitis B virus core protein promotes hepatocellular carcinoma cell proliferation by up-regulating the c-Ets2-dependent expression of human telomerase reverse transcriptase. PMID: 23542016
46. Identification of a novel antimicrobial peptide from human hepatitis B virus core protein arginine-rich domain (ARD). PMID: 23785287
47. Mutation at the aa 70 position of core protein is associated with disease progression in chronic hepatitis C. PMID: 23946458
48. The L60V variation in hepatitis B virus core protein elicits new epitope-specific cytotoxic T lymphocytes and enhances viral replication. PMID: 23678186
49. The predominant HBV subgenotype HBV/D5 with high viral load and basal core promoter mutations was significantly associated with advanced liver disease (liver cirrhosis and hepatocellular carcinoma) and might act as a predictor of severe hepatic complications. PMID: 22820088
50. Structural insight into how HBeAg may establish immune tolerance for HBcAg while evading its robust immunogenicity. PMID: 23219881

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KEGG: vg:944568