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Reversible promoter methylation determines fluctuating expression of acute phase proteins.


ABSTRACT: Acute phase reactants (APRs) are secretory proteins exhibiting large expression changes in response to proinflammatory cytokines. Here we show that the expression pattern of a major human APR, that is C-reactive protein (CRP), is casually determined by DNMT3A and TET2-tuned promoter methylation status. CRP features a CpG-poor promoter with its CpG motifs located in binding sites of STAT3, C/EBP-? and NF-?B. These motifs are highly methylated at the resting state, but undergo STAT3- and NF-?B-dependent demethylation upon cytokine stimulation, leading to markedly enhanced recruitment of C/EBP-? that boosts CRP expression. Withdrawal of cytokines, by contrast, results in a rapid recovery of promoter methylation and termination of CRP induction. Further analysis suggests that reversible methylation also regulates the expression of highly inducible genes carrying CpG-poor promoters with APRs as representatives. Therefore, these CpG-poor promoters may evolve CpG-containing TF binding sites to harness dynamic methylation for prompt and reversible responses.

SUBMITTER: Zhang SC 

PROVIDER: S-EPMC7136028 | biostudies-literature | 2020 Mar

REPOSITORIES: biostudies-literature

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Reversible promoter methylation determines fluctuating expression of acute phase proteins.

Zhang Shi-Chao SC   Wang Ming-Yu MY   Feng Jun-Rui JR   Chang Yue Y   Ji Shang-Rong SR   Wu Yi Y  

eLife 20200330


Acute phase reactants (APRs) are secretory proteins exhibiting large expression changes in response to proinflammatory cytokines. Here we show that the expression pattern of a major human APR, that is <i>C-reactive protein</i> (<i>CRP</i>), is casually determined by DNMT3A and TET2-tuned promoter methylation status. <i>CRP</i> features a CpG-poor promoter with its CpG motifs located in binding sites of STAT3, C/EBP-β and NF-κB. These motifs are highly methylated at the resting state, but undergo  ...[more]

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