Tip60's Novel RNA-Binding Function Modulates Alternative Splicing of Pre-mRNA Targets Implicated in Alzheimer's Disease

Bhatnagar, Akanksha; Krick, Keegan S.; Karisetty, Bhanu Chandra; Armour, Ellen M.; Heller, Elizabeth A.; Elefant, Felice

doi:10.1523/jneurosci.2331-22.2023

Cited by 8 publications

(7 citation statements)

References 110 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…We conclude that the influence of RNA on the acetylation of the H4 N-terminus is a particular feature of the 4-MSL complex and not a property shared between the two MYST HAT family members, MOF and dTip60 ( 66 ).…”

Section: Resultsmentioning

confidence: 84%

Processivity and specificity of histone acetylation by the male-specific lethal complex

Kiss,

Venkatasubramani,

Pathirana

et al. 2024

Nucleic Acids Research

View full text Add to dashboard Cite

Acetylation of lysine 16 of histone H4 (H4K16ac) stands out among the histone modifications, because it decompacts the chromatin fiber. The metazoan acetyltransferase MOF (KAT8) regulates transcription through H4K16 acetylation. Antibody-based studies had yielded inconclusive results about the selectivity of MOF to acetylate the H4 N-terminus. We used targeted mass spectrometry to examine the activity of MOF in the male-specific lethal core (4-MSL) complex on nucleosome array substrates. This complex is part of the Dosage Compensation Complex (DCC) that activates X-chromosomal genes in male Drosophila. During short reaction times, MOF acetylated H4K16 efficiently and with excellent selectivity. Upon longer incubation, the enzyme progressively acetylated lysines 12, 8 and 5, leading to a mixture of oligo-acetylated H4. Mathematical modeling suggests that MOF recognizes and acetylates H4K16 with high selectivity, but remains substrate-bound and continues to acetylate more N-terminal H4 lysines in a processive manner. The 4-MSL complex lacks non-coding roX RNA, a critical component of the DCC. Remarkably, addition of RNA to the reaction non-specifically suppressed H4 oligo-acetylation in favor of specific H4K16 acetylation. Because RNA destabilizes the MSL-nucleosome interaction in vitro we speculate that RNA accelerates enzyme-substrate turn-over in vivo, thus limiting the processivity of MOF, thereby increasing specific H4K16 acetylation.

show abstract

Section: Resultsmentioning

confidence: 84%

Processivity and specificity of histone acetylation by the male-specific lethal complex

Kiss,

Venkatasubramani,

Pathirana

et al. 2024

Nucleic Acids Research

View full text Add to dashboard Cite

show abstract

“…Furthermore, dCasRx not only efficiently shifts alternative splicing outcome into the correct splicing isoform, evidenced by amplicon sequencing of the edited transcripts, but it can do so to more than one alternatively spliced event by cotransfecting multiple gRNAs. This will significantly increase the phenotypic impact when correcting complex splicing-associated anomalies in which more than one splicing isoform is implicated, as in cancer or brain diseases (50)(51)(52). However, as a second caveat, we encountered some difficulties reaching functionally-relevant dCasRx expression levels in difficult-to-transfect cells.…”

Section: Discussionmentioning

confidence: 99%

“A CRISPR-dCas13 RNA-editing tool to study alternative splicing”

Núñez‐Álvarez

Espie--Caullet

Luco

2022

Preprint

View full text Add to dashboard Cite

Alternative splicing is an RNA processing used by the cell to increase its protein diversity and genome plasticity through generation of several transcripts from the same gene. It affects the vast majority of biological processes, from stem cell differentiation to cell metabolism. However, tools to properly study the role of a specific splice variant are still missing. With the discovery of the bacterial CRISPR system, a new era in nucleic acid editing has emerged. RNA-directed CRISPR/Cas13 RNAses were recently shown to efficiently target the RNA with higher specificity than Cas9 to the DNA. In this work, we are taking advantage of the catalytic dead mutant dCas13 family member dCasRx to edit alternative splicing patterns in a physiological context. Thanks to our new strategy, isoform-switching splicing changes are easily obtained at endogenous genes without impacting overall gene expression levels. Moreover, we propose a new application for this dCasRx splicing editing system to identify the key regulatory elements involved in the alternative splicing of a given gene. This new approach will increase the RNA toolkit to properly understand the biological impact and regulatory mechanisms of alternative splicing in a given biological process or pathological scenario.

show abstract

“…as a contributor to the development of myeloid malignancies, illustrating the importance of proper splicing regulation in maintaining cellular homeostasis (S. P. Palangat et al, 2019). Changes in alternative splicing patterns that occur with age are most significant in the brain; nevertheless, dysregulation of RNA homeostasis compromises cellular and tissue function, leading to age-related diseases (Adusumalli et al, 2019;Bhatnagar et al, 2023;Howe et al, 2022).…”

Section: Splicing Dysregulationmentioning

confidence: 99%

“…For instance, somatic mutations in splicing factors, such as U2 small nuclear RNA auxiliary factor 1, splicing factor 3b subunit 1 (SF3B1), and splicing factor 3b subunit 2 (SRSF2), have been identified as a contributor to the development of myeloid malignancies, illustrating the importance of proper splicing regulation in maintaining cellular homeostasis (S. P. Kim et al., 2021; Palangat et al., 2019). Changes in alternative splicing patterns that occur with age are most significant in the brain; nevertheless, dysregulation of RNA homeostasis compromises cellular and tissue function, leading to age‐related diseases (Adusumalli et al., 2019; Bhatnagar et al., 2023; Howe et al., 2022). Defects in the splicing of genes could contribute to the aging process through a feedback loop mechanism, further impairing RNA processing and translation.…”

Section: “New” Hallmarks Of Aging—longevity Perspectivementioning

confidence: 99%

Nurturing longevity through natural compounds: Where do we stand, and where do we go?

Todorova,

Savova,

Mihaylova

et al. 2024

Food Frontiers

View full text Add to dashboard Cite

The revolution in aging research through the past decade has driven the progress in interventions that promote longevity. Dissection of the “old” hallmarks of aging has provided solid data for the definition of at least three “new” ones, opening avenues for the development of novel hallmark‐targeted pro‐longevity approaches. The quest for geroprotectors is of enormous interest with the ultimate goal of finding the alchemical stone that induces healthy aging and increases lifespan, pushing the limits of human longevity or even uncovering the absence of such limits. Several of the well‐appreciated geroprotectors that are recognized as longevity promoters are of natural origin such as metformin, resveratrol, aspirin, and spermidine. As the search for pharmacological modulators of healthspan and lifespan continues, numerous studies are focusing on the potential of plant secondary metabolites. The current review attempts to critically assess the available interventions and the breakthrough discoveries in the field of longevity research over the past decade. Correspondingly, novel approaches targeting the hallmarks of aging have been outlined, and the future goals in longevity research have been enlightened. Special emphasis has been placed on the potential of plant‐derived compounds as pro‐longevity agents.

show abstract

Tip60's Novel RNA-Binding Function Modulates Alternative Splicing of Pre-mRNA Targets Implicated in Alzheimer's Disease

Cited by 8 publications

References 110 publications

Processivity and specificity of histone acetylation by the male-specific lethal complex

Processivity and specificity of histone acetylation by the male-specific lethal complex

“A CRISPR-dCas13 RNA-editing tool to study alternative splicing”

Nurturing longevity through natural compounds: Where do we stand, and where do we go?

Contact Info

Product

Resources

About