EGFR Modulates DNA Synthesis and Repair through Tyr Phosphorylation of Histone H4

Chou, Ruey Hwang; Wang, Ying-Nai; Hsieh, Yi‐Hsien; Li, Long-yuan; Xia, Weiya; Chang, Wei‐Chao; Chang, Ling‐Chu; Cheng, Chien-Chia; Lai, Chih-Sheng; Hsu, Jennifer L.; Chang, Wen Hsin; Chiang, Shu-Ya; Lee, Hong-Jen; Liao, Hsin-Wei; Chuang, Pei-Huan; Chen, Hui-Yu; Wang, Hung-Ling; Kuo, Sheng‐Chu; Chen, Chung-Hsuan; Yu, Yung-Luen; Hung, Mien‐Chie

doi:10.1016/j.devcel.2014.06.008

Cited by 70 publications

(59 citation statements)

References 53 publications

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“…Elevated levels of STAT1 positively regulate ISG expression independent of pY-STAT1 (Cheon and Stark, 2009). Furthermore, translocation of signaling receptors to the nucleus can positively regulate gene expression as shown for the insulin-like growth factor 1 receptor (Sehat et al, 2010), or the epidermal growth factor receptor that promotes epigenetic modifications (Chou et al, 2014). Thus, both IFNAR1 nuclear localization (Subramaniam and Johnson, 2004) and high STAT1 expression could contribute to ISG expression following IFN-I stimulation, despite the low activation of pY-STAT1.…”

Section: Discussionmentioning

confidence: 99%

Flavivirus Antagonism of Type I Interferon Signaling Reveals Prolidase as a Regulator of IFNAR1 Surface Expression

Lubick

Robertson

McNally

et al. 2015

Cell Host & Microbe

128

143

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Summary Type I interferon (IFN-α/β or IFN-I) signals through two receptor subunits, IFNAR1 and IFNAR2, to orchestrate sterile and infectious immunity. Cellular pathways that regulate IFNAR1 are often targeted by viruses to suppress the antiviral effects of IFN-I. Here we report that encephalitic flaviviruses, including tick-borne encephalitis virus and West Nile virus, antagonize IFN-I signaling by inhibiting IFNAR1 surface expression. Loss of IFNAR1 was associated with binding of the viral IFN-I antagonist, NS5, to prolidase (PEPD), a cellular dipeptidase implicated in primary immune deficiencies in humans. Prolidase was required for IFNAR1 maturation and accumulation, activation of IFNβ-stimulated gene induction, and IFN-I-dependent viral control. Human fibroblasts derived from patients with genetic prolidase deficiency exhibited decreased IFNAR1 surface expression and reduced IFNβ-stimulated signaling. Thus, by understanding flavivirus IFN-I antagonism, prolidase is revealed as a central regulator of IFN-I responses.

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Section: Discussionmentioning

confidence: 99%

Flavivirus Antagonism of Type I Interferon Signaling Reveals Prolidase as a Regulator of IFNAR1 Surface Expression

Lubick

Robertson

McNally

et al. 2015

Cell Host & Microbe

128

143

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“…Recently, identification of tyrosine phosphorylation at H4Y72 offers such an example. 189 In addition, for newly discovered lysine acylation marks, only one or a few cellular systems have been analyzed. Accordingly, additional histone sites bearing these types of modification should exist in other cells.…”

Section: Comprehensive List Of Histone Ptmsmentioning

confidence: 99%

Quantitative Proteomic Analysis of Histone Modifications

et al. 2015

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“…In addition, the association of AKAP8 with nuclear structures is involved in gene expression, DNA replication, and mitotic progression (26,56,57). Recently, the nuclear proteins KAT5, histone H4, and HDAC2 were reported to be tyrosinephosphorylated and to functionally associate with chromatin structures (22,54,58). Taken together, we assume that tyrosine phosphorylation of various nuclear proteins, including AKAP8, is attributable to nuclear tyrosine kinase-mediated chromatin structural changes, which could be involved in a variety of nuclear function, such as gene expression, DNA replication, and mitotic progression.…”

Section: Discussionmentioning

confidence: 99%

Role for Tyrosine Phosphorylation of A-kinase Anchoring Protein 8 (AKAP8) in Its Dissociation from Chromatin and the Nuclear Matrix

Kubota

Morii

Yuki

et al. 2015

Journal of Biological Chemistry

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Background: Tyrosine kinases are active in the cell nucleus and involved in global nuclear structure. Results: Phosphorylation of AKAP8 at multiple tyrosine residues by several nucleus-localized tyrosine kinases, including c-Src, induces AKAP8's dissociation from nuclear structures. Conclusion: Nuclear tyrosine phosphorylation of AKAP8 is involved in global nuclear structure changes. Significance: These findings highlight the importance of nuclear tyrosine phosphorylation in dynamic chromatin regulation.

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EGFR Modulates DNA Synthesis and Repair through Tyr Phosphorylation of Histone H4

Cited by 70 publications

References 53 publications

Flavivirus Antagonism of Type I Interferon Signaling Reveals Prolidase as a Regulator of IFNAR1 Surface Expression

Flavivirus Antagonism of Type I Interferon Signaling Reveals Prolidase as a Regulator of IFNAR1 Surface Expression

Quantitative Proteomic Analysis of Histone Modifications

Role for Tyrosine Phosphorylation of A-kinase Anchoring Protein 8 (AKAP8) in Its Dissociation from Chromatin and the Nuclear Matrix

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