Rare event of histone demethylation can initiate singular gene expression of olfactory receptors

Tan, Longzhi; Zong, Chenghang; Xie, X. Sunney

doi:10.1073/pnas.1321511111

Cited by 28 publications

(36 citation statements)

References 35 publications

(42 reference statements)

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“…Thus, for most ORs, H3K9 demethylation is necessary but not sufficient for expression at high cellular levels. Although recent theoretical calculations support that a slow demethylation process combined with a fast feedback can explain singular OR expression (Tan et al, 2013), our experimental findings suggest that an additional regulatory layer may also contribute to the singularity of OR choice. Were the absence of H3K9 methylation sufficient for robust OR transcription, then most G9a/GLP KO OSNs should express multiple ORs at high levels.…”

Section: Discussioncontrasting

confidence: 76%

“…Because perturbations in the OR-elicited feedback result in frequent OR switching but not simultaneous co-expression of multiple OR alleles (Dalton et al, 2013; Lyons et al, 2013), the latter hypothesis is more likely. However, recent theoretical models suggest that singular OR expression could also be explained just by a combination of a slow H3K9 demethylation process and a fast feedback that blocks further demethylation(Tan et al, 2013). In this scenario, removal of the repressive histone marks from a randomly chosen OR allele could be essential and sufficient for OR expression, a hypothesis supported by pharmacological inhibition of G9a/GLP in zebrafish embryos(Ferreira et al, 2014).…”

Section: Introductionmentioning

confidence: 99%

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Heterochromatin-Mediated Gene Silencing Facilitates the Diversification of Olfactory Neurons

et al. 2014

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SUMMARY An astounding property of the nervous system is its cellular diversity. This diversity, which was initially realized by morphological and electrophysiological differences, is ultimately produced by variations in gene expression programs. In most cases these variations are determined by external cues. However, a growing number of neuronal types have been identified in which inductive signals cannot explain the few but decisive transcriptional differences that cause cell diversification. Here, we show that heterochromatic silencing, which we find is governed by histone methyltransferases G9a (KMT1C) and GLP (KMT1D), is essential for stochastic and singular OR expression. Deletion of G9a and GLP dramatically reduces the complexity of the OR transcriptome, resulting in transcriptional domination by a few ORs and loss of singularity in OR expression. Thus, in addition to its previously known functions, our data suggest that heterochromatin creates an epigenetic platform that affords stochastic, mutually exclusive gene choices and promotes cellular diversity.

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Section: Discussioncontrasting

confidence: 76%

Section: Introductionmentioning

confidence: 99%

Heterochromatin-Mediated Gene Silencing Facilitates the Diversification of Olfactory Neurons

et al. 2014

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“…Recent theoretical studies have shown that monoallelic OR choice can be modeled with mechanisms similar to those described above, namely OR derepression and the subsequent inhibition of the derepressing mechanism (Alsing & Sneppen 2013, Tan et al 2013). The success of this simple activation–feedback mechanism depends on the ratio between the average time it takes to activate an OR and the time it takes for feedback inhibition to occur (Tan et al 2013). Coexpression occurs if the activation of a second OR occurs shortly after the activation of the first—that is, before feedback inhibition can shut off the derepression mechanism.…”

Section: Chromatin-mediated Silencing Of Olfactory Receptor Genes Ismentioning

confidence: 99%

Monoallelic Expression of Olfactory Receptors

Monahan

Lomvardas

2015

Annu. Rev. Cell Dev. Biol.

149

148

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The sense of smell collects vital information about the environment by detecting a multitude of chemical odorants. Breadth and sensitivity are provided by a huge number of chemosensory receptor proteins, including more than 1,400 olfactory receptors (ORs). Organizing the sensory information generated by these receptors so that it can be processed and evaluated by the central nervous system is a major challenge. This challenge is overcome by monogenic and monoallelic expression of OR genes. The single OR expressed by each olfactory sensory neuron determines the neuron’s odor sensitivity and the axonal connections it will make to downstream neurons in the olfactory bulb. The expression of a single OR per neuron is accomplished by coupling a slow chromatin-mediated activation process to a fast negative-feedback signal that prevents activation of additional ORs. Singular OR activation is likely orchestrated by a network of interchromosomal enhancer interactions and large-scale changes in nuclear architecture.

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“…Once a functional OR has been activated, rapid induction of Adenylyl Cyclase 3 provides feedback downregulation of KDM1A, preventing both the activation of other OR genes and downregulation of the OR by repressive KDM1A complexes. This allows for terminal differentiation and locks each individual OSN in a state of sustained expression of a single olfactory receptor ( Figure 3D) [86,87].…”

Section: Kdm1a In the Normal Brain And In Neurodegenerative Diseasementioning

confidence: 99%

“…If the OR is functional, Adcy3 is activated and KDM1A expression downregulated, allowing for the continued expression of that OR. If the OR is not functional, Adcy is not activated and the expression of another OR is attempted [86,87] future science group KDM1 treatments of oncological & neurodegenerative disease Review out that they could not exclude the possibility that the effect was provoked by inhibition of MAOs, which can perturb glucocorticoid receptors in the hippocampus and affect memory consolidation [109]. Indeed, RN-1 was administered as a single high dose which is incompatible with repeated administration [tamara maes, unpublished Data].…”

Section: Figure 3 Feedback Inhibition Mechanisms Of Kdm1a Activity Imentioning

confidence: 99%

KDM1 Histone Lysine Demethylases as Targets for Treatments of Oncological and Neurodegenerative Disease

et al. 2015

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Histone methylation and demethylation are important processes associated with the regulation of gene transcription, and alterations in histone methylation status have been linked to a large number of human diseases. Initially thought to be an irreversible process, histone methylation is now known to be reversed by two families of proteins containing over 30 members that act to remove methyl groups from specific lysine residues present in the tails of histone H3 and histone H4. A rapidly growing number of reports have implicated the FAD-dependent lysine specific demethylase (KDM1) family in cancer, and several small-molecule inhibitors are in development for the treatment of cancer. An additional role has emerged for KDM1 in brain function, offering additional opportunities for the development of novel therapeutic strategies in neurodegenerative disease. A decade after the identification of KDM1A as a histone demethylase, the first selective inhibitors have now reached the clinic.

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Rare event of histone demethylation can initiate singular gene expression of olfactory receptors

Cited by 28 publications

References 35 publications

Heterochromatin-Mediated Gene Silencing Facilitates the Diversification of Olfactory Neurons

Heterochromatin-Mediated Gene Silencing Facilitates the Diversification of Olfactory Neurons

Monoallelic Expression of Olfactory Receptors

KDM1 Histone Lysine Demethylases as Targets for Treatments of Oncological and Neurodegenerative Disease

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