2018
DOI: 10.4049/jimmunol.1701726
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Hepatitis B Virus Blocks the CRE/CREB Complex and Prevents TLR9 Transcription and Function in Human B Cells

Abstract: Effective B cell responses such as cytokine secretion, proliferation, and Ab-specific responses are essential to clear hepatitis B virus (HBV) infection. However, HBV alters numerous immune pathways to persist in the host. B cell activity depends on activation of the innate sensor TLR9 by viral or bacterial DNA motifs. How HBV can deregulate B cell functions remains unknown. In this study, we show that HBV can enter and decrease TLR9 expression in human primary B cells. Using PBMCs from human blood donors, we … Show more

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Cited by 22 publications
(21 citation statements)
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“…These receptors are activated when they recognize structures that are not normally present in the host cells and/or that are shared by multiple pathogens (including viruses) [ 32 ]. A variety of TLRs have been specifically identified for different infectious agents, such as types 4, 7, 8, and 9 [ 25 , 29 , 33 ].…”
Section: Neutrophils and Netsmentioning
confidence: 99%
“…These receptors are activated when they recognize structures that are not normally present in the host cells and/or that are shared by multiple pathogens (including viruses) [ 32 ]. A variety of TLRs have been specifically identified for different infectious agents, such as types 4, 7, 8, and 9 [ 25 , 29 , 33 ].…”
Section: Neutrophils and Netsmentioning
confidence: 99%
“…In addition, these antiviral treatments are commonly used in two of the four clinical stages of chronic HBV infection: 1) immune activity (HBeAg-positive hepatitis); and 2) HBeAg negative hepatitis. In almost all patients with chronic HBV infection, these therapies display high efficacy, including disturbed B cell homeostasis, can be partially recovered ( 124 ); however, difficulties remain in achieving a loss of HBsAg and functional cure (persistently undetectable HBsAg) ( 125 ). A high load of HBsAg could further inhibit adaptive immune function and ultimately leads to specific tolerance that prevents patients from eradicating HBV infection.…”
Section: Immunotherapeutic Prospects Of B Cells In Chronic Hbv Infectmentioning
confidence: 99%
“…These differences may be explained by distinct transcriptional regulation mechanisms among TLRs. Sp1/Sp3 as well as NF-κB regulate TLR2 mRNA expression ( 44 ) and TLR9 mRNA is regulated by CRE/CREB ( 45 ), whereas transcription of TLR4 mRNA is mainly induced by NF-κB ( 46 ). Interestingly, mice deficient in TLR4 treated with apocynin did not show a better survival rate than WT mice after CLP (data not shown), which is in accordance with our previous data implicating TLRs in control of infection ( 21 , 47 ), which becomes irrelevant after the treatment of mice with antibiotics.…”
Section: Discussionmentioning
confidence: 99%