AI Article Synopsis
- Nuclear-envelope proteins like LAP2beta play a crucial role in regulating gene expression, particularly by repressing transcriptional activity of various factors, including E2F and p53.
- LAP2beta interacts with HDAC3, a histone deacetylase, which suggests a collaborative mechanism in gene repression at the nuclear envelope.
- The study reveals that LAP2beta not only interacts with HDAC3 but also induces histone-H4 deacetylation, highlighting a new repressive complex that may be significant in transcription regulation.
Article Abstract
Nuclear-envelope proteins have been implicated in diverse and fundamental cell functions, among them transcriptional regulation. Gene expression at the territory of the nuclear periphery is known to be repressed by epigenetic modifications such as histone deacetylation and methylation. However, the mechanism by which nuclear-envelope proteins are involved in such modifications is still obscure. We have previously shown that LAP2beta, an integral nuclear-envelope protein that contains the chromatin-binding LEM domain, was able to repress the transcriptional activity of the E2F5-DP3 heterodimer. Here, we show that LAP2beta's repressive activity is more general, encompassing various E2F members as well as other transcription factors such as p53 and NF-kappaB. We further show that LAP2beta interacts at the nuclear envelope with HDAC3, a class-I histone deacetylase, and that TSA (an HDAC inhibitor) abrogates LAP2beta's repressive activity. Finally, we show that LAP2beta is capable of inducing histone-H4 deacetylation. Our data provide evidence for the existence of a previously unknown repressive complex, composed of an integral nuclear membrane protein and a histone modifier, at the nuclear periphery.
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| http://dx.doi.org/10.1242/jcs.02521 | DOI Listing |
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