
Alternative splicing affects more than 90% of human genes. Coupling between transcription and splicing has become crucial in the complex network underlying alternative splicing regulation. Because chromatin is the real template for nuclear transcription, changes in its structure, but also in the "reading" and "writing" of the histone code, could modulate splicing choices. Here, we discuss the evidence supporting these ideas, from the first proposal of chromatin affecting alternative splicing, performed 20 years ago, to the latest findings including genome-wide evidence that nucleosomes are preferentially positioned in exons. We focus on two recent reports from our laboratories that add new evidence to this field. The first report shows that a physiological stimulus such as neuron depolarization promotes intragenic histone acetylation (H3K9ac) and chromatin relaxation, causing the skipping of exon 18 of the neural cell adhesion molecule gene. In the second report, we show how specific histone modifications can be created at targeted gene regions as a way to affect alternative splicing: Using small interfering RNAs (siRNAs), we increased the levels of H3K9me2 and H3K27me3 in the proximity of alternative exon 33 of the human fibronectin gene, favoring its inclusion into mature messenger RNA (mRNA) through a mechanism that recalls RNA-mediated transcriptional gene silencing.
medical literature, genetic association, Action Potentials, DNA fragmentation, trichostatin A, stimulus, nerve cell differentiation, gene targeting, Histones, gene silencing, depolarization, genetic linkage, alternative RNA splicing, double stranded RNA, molecular biology, histone modification, exon, virus replication, chromatin structure, Neurons, DNA methylation, nerve cell membrane steady potential, messenger RNA, mitogen activated protein kinase, article, histone acetylation, Exons, Chromatin, Nucleosomes, priority journal, RNA polymerase II, nerve cell, transcription regulation, gene insertion, DNA Replication, DNA sequence, histone, DNA replication, calcium signaling, chromatin assembly and disassembly, Models, Biological, Article, posttranscriptional gene silencing, promoter region, nerve cell adhesion molecule, fibronectin, Humans, human, nonhuman, genome-wide association study, RNA translation, nucleosome, heterochromatin, gene mapping, Chromatin Assembly and Disassembly, small interfering RNA, Alternative Splicing, chromatin, polypyrimidine tract binding protein, upregulation
medical literature, genetic association, Action Potentials, DNA fragmentation, trichostatin A, stimulus, nerve cell differentiation, gene targeting, Histones, gene silencing, depolarization, genetic linkage, alternative RNA splicing, double stranded RNA, molecular biology, histone modification, exon, virus replication, chromatin structure, Neurons, DNA methylation, nerve cell membrane steady potential, messenger RNA, mitogen activated protein kinase, article, histone acetylation, Exons, Chromatin, Nucleosomes, priority journal, RNA polymerase II, nerve cell, transcription regulation, gene insertion, DNA Replication, DNA sequence, histone, DNA replication, calcium signaling, chromatin assembly and disassembly, Models, Biological, Article, posttranscriptional gene silencing, promoter region, nerve cell adhesion molecule, fibronectin, Humans, human, nonhuman, genome-wide association study, RNA translation, nucleosome, heterochromatin, gene mapping, Chromatin Assembly and Disassembly, small interfering RNA, Alternative Splicing, chromatin, polypyrimidine tract binding protein, upregulation
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