FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2059408934> ?p ?o ?g. }

• W2059408934 endingPage "7951" @default.
• W2059408934 startingPage "7941" @default.
• W2059408934 abstract "Nuclear factor κB (NF-κB) plays important roles in innate immune responses by regulating the expression of a large number of target genes involved in the immune and inflammatory response, apoptosis, cell proliferation, differentiation, and survival. To survive in the host cells, viruses have evolved multiple strategies to evade and subvert the host immune response. Herpes simplex virus 1 (HSV-1) bears a large DNA genome, with the capacity to encode many different viral proteins to counteract the host immune responses. In the present study, we demonstrated that HSV-1 protein kinase US3 significantly inhibited NF-κB activation and decreased the expression of inflammatory chemokine interleukin-8 (IL-8). US3 was also shown to hyperphosphorylate p65 at serine 75 and block its nuclear translocation. Two US3 mutants, K220M and D305A, still interacted with p65; however, they could not hyperphosphorylate p65, indicating that the kinase activity of US3 was indispensable for the function. The attenuation of NF-κB activation by HSV-1 US3 protein kinase may represent a critical adaptation to enable virus persistence within the host. Importance: This study demonstrated that HSV-1 protein kinase US3 significantly inhibited NF-κB activation and decreased the expression of inflammatory chemokine interleukin-8 (IL-8). US3 hyperphosphorylated p65 at serine 75 to inhibit NF-κB activation. The kinase activity of US3 was indispensable for its hyperphosphorylation of p65 and abrogation of the nuclear translocation of p65. The present study elaborated a novel mechanism of HSV-1 US3 to evade the host innate immunity." @default.
• W2059408934 created "2016-06-24" @default.
• W2059408934 creator A5002029182 @default.
• W2059408934 creator A5006901857 @default.
• W2059408934 creator A5038495452 @default.
• W2059408934 creator A5067048636 @default.
• W2059408934 date "2014-07-15" @default.
• W2059408934 modified "2023-10-16" @default.
• W2059408934 title "Herpes Simplex Virus 1 Protein Kinase US3 Hyperphosphorylates p65/RelA and Dampens NF-κB Activation" @default.
• W2059408934 cites W1507472194 @default.
• W2059408934 cites W1535444616 @default.
• W2059408934 cites W184020152 @default.
• W2059408934 cites W1892689796 @default.
• W2059408934 cites W1912303405 @default.
• W2059408934 cites W1969165297 @default.
• W2059408934 cites W1969883219 @default.
• W2059408934 cites W1970098146 @default.
• W2059408934 cites W1971663674 @default.
• W2059408934 cites W1977707794 @default.
• W2059408934 cites W1981272989 @default.
• W2059408934 cites W1982198536 @default.
• W2059408934 cites W1988924112 @default.
• W2059408934 cites W1993881377 @default.
• W2059408934 cites W1996131673 @default.
• W2059408934 cites W1996217096 @default.
• W2059408934 cites W1996696918 @default.
• W2059408934 cites W1999177172 @default.
• W2059408934 cites W2004038084 @default.
• W2059408934 cites W2005210883 @default.
• W2059408934 cites W2006470470 @default.
• W2059408934 cites W2006615448 @default.
• W2059408934 cites W2009173868 @default.
• W2059408934 cites W2010830522 @default.
• W2059408934 cites W2020257412 @default.
• W2059408934 cites W2024887781 @default.
• W2059408934 cites W2027007768 @default.
• W2059408934 cites W2028499936 @default.
• W2059408934 cites W2031182394 @default.
• W2059408934 cites W2031426696 @default.
• W2059408934 cites W2031584044 @default.
• W2059408934 cites W2032908627 @default.
• W2059408934 cites W2035109828 @default.
• W2059408934 cites W2037925416 @default.
• W2059408934 cites W2039667276 @default.
• W2059408934 cites W2049483592 @default.
• W2059408934 cites W2053557358 @default.
• W2059408934 cites W2061903251 @default.
• W2059408934 cites W2065840126 @default.
• W2059408934 cites W2066032479 @default.
• W2059408934 cites W2067498099 @default.
• W2059408934 cites W2067938485 @default.
• W2059408934 cites W2080995946 @default.
• W2059408934 cites W2083139702 @default.
• W2059408934 cites W2094863064 @default.
• W2059408934 cites W2097906368 @default.
• W2059408934 cites W2100280306 @default.
• W2059408934 cites W2103817756 @default.
• W2059408934 cites W2106877484 @default.
• W2059408934 cites W2110722265 @default.
• W2059408934 cites W2113303165 @default.
• W2059408934 cites W2114972655 @default.
• W2059408934 cites W2115616959 @default.
• W2059408934 cites W2115718472 @default.
• W2059408934 cites W2118391342 @default.
• W2059408934 cites W2119628526 @default.
• W2059408934 cites W2120055283 @default.
• W2059408934 cites W2120312885 @default.
• W2059408934 cites W2122044177 @default.
• W2059408934 cites W2124219221 @default.
• W2059408934 cites W2129313145 @default.
• W2059408934 cites W2131423211 @default.
• W2059408934 cites W2131820144 @default.
• W2059408934 cites W2135342726 @default.
• W2059408934 cites W2135433503 @default.
• W2059408934 cites W2135814779 @default.
• W2059408934 cites W2138395245 @default.
• W2059408934 cites W2143813693 @default.
• W2059408934 cites W2145728570 @default.
• W2059408934 cites W2148119611 @default.
• W2059408934 cites W2155356753 @default.
• W2059408934 cites W2156638064 @default.
• W2059408934 cites W2157942810 @default.
• W2059408934 cites W2159979956 @default.
• W2059408934 cites W2160148642 @default.
• W2059408934 cites W2163598864 @default.
• W2059408934 cites W2167262402 @default.
• W2059408934 cites W2168837438 @default.
• W2059408934 cites W2168960441 @default.
• W2059408934 cites W2290936009 @default.
• W2059408934 cites W2766221641 @default.
• W2059408934 cites W2999065750 @default.
• W2059408934 cites W4379365691 @default.
• W2059408934 doi "https://doi.org/10.1128/jvi.03394-13" @default.
• W2059408934 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/4097809" @default.
• W2059408934 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/24807716" @default.
• W2059408934 hasPublicationYear "2014" @default.
• W2059408934 type Work @default.
• W2059408934 sameAs 2059408934 @default.

• next