Poison exons (PEs); also called premature termination codon (PTC) exons or nonsense-mediated decay (NMD) exons] are a class of Alternative splicing#Modes, cassette exons that contain PTCs. Inclusion of a PE in a transcript targets the transcript for degradation via NMD. PEs are generally highly conserved elements of the genome and are thought to have important regulatory roles in biology. Targeting PE inclusion or exclusion in certain transcripts is being evaluated as a therapeutic strategy.

Discovery

In 2002, a model termed regulated unproductive splicing and translation (RUST) was proposed based on the finding that many (~one-third) alternatively spliced transcripts contain PEs. In this model, coupling alternative splicing to NMD (AS-NMD) is thought to tune transcript levels to regulate protein expression. Alternative splicing may also lead to NMD via other pathways besides PE inclusion, e.g., intron retention. PEs were initially characterized in

RNA-binding protein RNA-binding proteins (often abbreviated as RBPs) are proteins that bind to the double or single stranded RNA in cell (biology), cells and participate in forming ribonucleoprotein complexes. RBPs contain various structural motifs, such as RNA reco ...

s from the SR protein family. Genes for other RNA-binding proteins (RBPs) such as those for heterogenous nuclear ribonucleoprotein (hnRNP) also contain PEs. Numerous

chromatin Chromatin is a complex of DNA and protein found in eukaryote, eukaryotic cells. The primary function is to package long DNA molecules into more compact, denser structures. This prevents the strands from becoming tangled and also plays important r ...

regulators also contain PEs, though these are less conserved than PEs within RBPs such as the SR proteins. Multiple spliceosomal components contain PEs. Certain PEs may occur only in specific tissues. PE-containing transcripts generally represent a minority of the overall transcript population, in part due to their active degradation via NMD, though this relative abundance can be elevated upon inhibition of NMD or certain biological states. Certain PE-containing transcripts are resistant to NMD and may be translated into truncated proteins.

Regulation

''Cis''-regulatory elements neighboring PEs have been found to affect PE inclusion. Many proteins whose corresponding genes contain PEs autoregulate PE inclusion in their respective transcripts and thereby control their own levels via a feedback loop. Cross-regulation of PE inclusion has also been observed. Differential splicing of PEs is implicated in biological processes such as differentiation,

neurodevelopment The development of the nervous system in humans, or neural development, or neurodevelopment involves the studies of embryology, developmental biology, and neuroscience. These describe the cellular and molecular mechanisms by which the complex ...

, dispersal of nuclear speckles during hypoxia,

tumorigenesis Carcinogenesis, also called oncogenesis or tumorigenesis, is the formation of a cancer, whereby normal cells are transformed into cancer cells. The process is characterized by changes at the cellular, genetic, and epigenetic levels and abn ...

, organism growth, and

T cell T cells (also known as T lymphocytes) are an important part of the immune system and play a central role in the adaptive immune response. T cells can be distinguished from other lymphocytes by the presence of a T-cell receptor (TCR) on their cell ...

expansion.

Protein kinase A protein kinase is a kinase which selectively modifies other proteins by covalently adding phosphates to them ( phosphorylation) as opposed to kinases which modify lipids, carbohydrates, or other molecules. Phosphorylation usually results in a f ...

s that regulate phosphorylation of splicing factors can affect splicing processes, thus kinase inhibitors may affect inclusion of PEs. For example, CMGC kinase inhibitors and

CDK9 Cyclin-dependent kinase 9 or CDK9 is a cyclin-dependent kinase associated with P-TEFb. Function The protein encoded by this gene is a member of the cyclin-dependent kinase (CDK) family. CDK family members are highly similar to the gene produ ...

inhibitors have been found to induce PE inclusion in '' RBM39''. Small molecules that modulate chromatin accessibility can affect PE inclusion. Mutations in splicing factors can lead to inclusion of PEs in certain transcripts. PE inclusion can be regulated by external variables such as temperature and electrical activity. For example, PE inclusion in '' RBM3'' transcript is lowered during

hypothermia Hypothermia is defined as a body core temperature below in humans. Symptoms depend on the temperature. In mild hypothermia, there is shivering and mental confusion. In moderate hypothermia, shivering stops and confusion increases. In severe ...

. This is mediated by temperature-dependent binding of the splicing factor HNRNPH1 to the ''RBM3'' transcript. The neuronal RBPs NOVA1/2 are translocated from the nucleus to the cytoplasm during

pilocarpine Pilocarpine, sold under the brand name Pilopine HS among others, is a lactone alkaloid originally extracted from plants of the Pilocarpus genus. It is used as a medication to reduce pressure inside the eye and treat dry mouth. As an eye drop ...

-induced seizure in mice, and it was found that NOVA1/2 regulates the expression of cryptic PEs. The glycosyltransferase O-GlcNAc transferase is responsible for installing the

O-GlcNAc ''O''-GlcNAc (short for ''O''-linked GlcNAc or ''O''-linked β-''N''-acetylglucosamine) is a reversible Enzyme, enzymatic post-translational modification that is found on serine and threonine residues of Cell nucleus, nucleoCytoplasm, cytoplasmi ...

post-translational modification In molecular biology, post-translational modification (PTM) is the covalent process of changing proteins following protein biosynthesis. PTMs may involve enzymes or occur spontaneously. Proteins are created by ribosomes, which translation (biolog ...

and contains a PE. It has been frequently observed that pharmacological or genetic perturbations that elevate cellular O-GlcNAc levels increase PE inclusion in the ''OGT'' transcript.

Disease

Proper regulation of PE inclusion and exclusion is important for health. Genetic mutations can affect inclusion of PEs and cause disease. For example, loss of CCAR1 leads to PE inclusion in the ''

FANCA Fanconi anaemia, complementation group A, also known as FAA, FACA and FANCA, is a protein which in humans is encoded by the ''FANCA'' gene. It belongs to the Fanconi anaemia complementation group (FANC) family of genes of which 12 complementatio ...

'' transcript, resulting in a

Fanconi anemia Fanconi anemia (FA) is a rare, autosomal recessive genetic disease characterized by aplastic anemia, congenital defects, endocrinological abnormalities, and an increased incidence of developing cancer. The study of Fanconi anemia has improve ...

phenotype. Dysregulation of components of the splicing machinery can also cause dysregulation of PE inclusion. Mutations in the splicing factor '' SF3B1'' have been found to promote PE inclusion in '' BRD9'', reducing BRD9 mRNA and protein levels and leading to

melanoma Melanoma is the most dangerous type of skin cancer; it develops from the melanin-producing cells known as melanocytes. It typically occurs in the skin, but may rarely occur in the mouth, intestines, or eye (uveal melanoma). In very rare case ...

genesis. Mutations in '' U2AF1'' promote PE inclusion in '' EIF4A2'', leading to impaired global mRNA translation and acute myeloid leukemia (AML) chemoresistance through the integrated stress response pathway. The splicing factor ''SRSF6'' contains a PE whose skipping is connected to T cell acute lymphoblastic leukemia (T-ALL), and PE inclusion in ''SRSF10'' is linked to acute lymphoblastic leukemia (ALL). Intronic mutations can lead to PE inclusion, such as in the case of ''

SCN1A Sodium channel protein type 1 subunit alpha (SCN1A), is a protein which in humans is encoded by the ''SCN1A'' gene. Gene location The ''SCN1A'' gene is located on chromosome 2 of humans, and is made up of 26 exons spanning a total length of 6 ...

'', where mutations within intron 20 promote inclusion of the nearby PE 20N, leading to

Dravet syndrome Dravet syndrome (DS), previously known as severe myoclonic epilepsy of infancy (SMEI), is an autosomal dominant genetic disorder which causes a catastrophic form of epilepsy, with prolonged seizures that are often triggered by hot temperatures o ...

-like phenotypes in mouse models. An intronic mutation in '' FLNA'' has been found to impair binding of the splicing regulator PTBP1, leading to inclusion of a poison exon in ''FLNA'' transcripts that causes a brain-specific malformation. In ''

RAD50 DNA repair protein RAD50, also known as RAD50, is a protein that in humans is encoded by the ''RAD50'' gene. Function The protein encoded by this gene is highly similar to ''Saccharomyces cerevisiae'' Rad50, a protein involved in DNA double- ...

'', TGAGT deletion is associated with a cryptic poison exon that occurs 30 nucleotides downstream within intron 21 mediated by altered U2AF recognition. Differential inclusion of PEs in various splicing factor and hnRNP genes has been reported in

type 1 diabetes Type 1 diabetes (T1D), formerly known as juvenile diabetes, is an autoimmune disease that occurs when the body's immune system destroys pancreatic cells (beta cells). In healthy persons, beta cells produce insulin. Insulin is a hormone require ...

. ''SRSF2'' mutations have been found to promote PE inclusion in the epigenetic regulator '' EZH2'', resulting in impaired hematopoietic differentiation. The ''TRA2B'' PE is essential for male fertility and meiotic cell division in mouse models. Deletion of this PE leads to an

azoospermia Azoospermia is the medical condition of a man whose semen contains no sperm. It is associated with male infertility, but many forms are amenable to medical treatment. In humans, azoospermia affects about 1% of the male population and may be see ...

phenotype.

Clinical relevance

Diagnostics

With the advent of

next-generation sequencing Massive parallel sequencing or massively parallel sequencing is any of several high-throughput approaches to DNA sequencing using the concept of massively parallel processing; it is also called next-generation sequencing (NGS) or second-generation ...

technologies, diagnostic genetic testing has emerged as a powerful tool to diagnose afflictions associated with specific genetic variants. Many diagnostic genetic testing efforts have focused on

exome sequencing Exome sequencing, also known as whole exome sequencing (WES), is a genomic technique for sequencing all of the protein-coding regions of genes in a genome (known as the exome). It consists of two steps: the first step is to select only the subs ...

. PE annotations may improve the diagnostic yield of these tests for certain diseases. For example, variants that affect PE inclusion in sodium channel genes (''SCN1A'', '' SCN2A'', and '' SCN8A'') have been found to be associated with epilepsies, and analogous variants in '' SNRPB'' have been found to be associated with cerebrocostomandibular syndrome.

Therapeutic discovery

As PE inclusion results in transcript degradation, targeted PE inclusion or exclusion is being evaluated as a therapeutic strategy. This strategy may prove especially applicable towards targets whose gene products are not easily ligandable such as "undruggable" proteins. Targeting PE inclusion/exlusion has been demonstrated with both

small molecule In molecular biology and pharmacology, a small molecule or micromolecule is a low molecular weight (≤ 1000 daltons) organic compound that may regulate a biological process, with a size on the order of 1 nm. Many drugs are small molecules; ...

s and antisense oligonucleotides (ASOs). Small molecules may modulate splicing by stabilizing alternative splice sites. ASOs may block specific splice sites or target certain ''cis''-regulatory elements to promote splicing at other sites. These ASOs may also be referred to as splice-switching oligonucleotides (SSOs). ASO walks tiling different ASOs across a gene sequence may be necessary to identify ASOs that have the desired effect on PE inclusion. Stoke Therapeutics is evaluating a strategy termed Targeted Augmentation of Nuclear Gene Output (TANGO). Targeting exon 20N in ''SCN1A'' mRNA with the antisense oligonucleotide zorevunersen (STK-001) blocks inclusion of this PE, leading to elevated levels of the productive ''SCN1A'' transcript and the gene product sodium channel protein 1 subunit alpha (Na_V1.1). In mouse models of Dravet syndrome, which is driven by mutations in ''SCN1A'', zorevunersen was able to reduce incidence of electrographic seizures and sudden unexpected death in epilepsy and prolong survival. As of October 2024, zorevunersen is being evaluated in phase 2 clinical trials (NCT04740476). Zorevunersen received FDA Breakthrough Therapy Designation in December 2024. Also in December 2024, Stoke Therapeutics disclosed that zorevunersen is generally well tolerated and shows substantial and sustained reductions in convulsive seizure frequency. Stoke Therapeutics expects to launch a phase 3 clinical trial in 2025 evaluating zorevunersen for reduction in seizure frequency as the primary endpoint and cognition and behavioral changes as secondary endpoints. Stoke Therapeutics is also evaluating the ASO STK-002 for treatment of autosomal dominant optic atrophy (ADOA). STK-002 promotes removal of a PE in the transcript of ''

OPA1 Dynamin-like 120 kDa protein, mitochondrial is a protein that in humans is encoded by the ''OPA1'' gene. This protein regulates mitochondrial fusion and cristae structure in the inner mitochondrial membrane (IMM) and contributes to ATP synthesis ...

'', leading to elevated OPA1 protein levels. Remix Therapeutics developed REM-422, which is an oral small molecule that promotes PE inclusion in the oncogene '' MYB''. REM-422 was discovered through a screening campaign for molecules that promote PE inclusion in ''MYB''. Subsequent ''in vitro'' experiments showed that REM-422 selectively facilitates binding of the U1 snRNP complex to oligonucleotides containing the ''MYB'' 5' splice site sequence. In various AML cell lines, REM-422 leads to degradation of ''MYB'' mRNA and lower MYB protein levels. REM-422 demonstrated antitumor activity in mouse xenograft models of acute myeloid leukemia. As of October 2024, REM-422 is being evaluated in phase 1 clinical trials (NCT06118086, NCT06297941). The splicing modulator small molecule risdiplam, originally developed to promote exon 7 inclusion in the ''SMN2'' transcript for treatment of spinal muscular atrophy, dose-dependently promotes PE inclusion in the ''MYB'' transcript as well. Rgenta Therapeutics has also developed RGT-61159, an oral small molecule that promotes PE inclusion in ''MYB'', as a potential treatment for adenoid cystic carcinoma (ACC). RGT-61159 is being evaluated in phase 1 clinical trials (NCT06462183). PTC Therapeutics is evaluating the oral small molecule PTC518 as a treatment for

Huntington's disease Huntington's disease (HD), also known as Huntington's chorea, is an incurable neurodegenerative disease that is mostly Genetic disorder#Autosomal dominant, inherited. It typically presents as a triad of progressive psychiatric, cognitive, and ...

. PTC518 was well-tolerated and showed dose-dependent decreases in '' HTT'' mRNA and HTT protein levels in a phase 1 clinical trial. As of October 2024, PTC518 is being evaluated in phase 2 clinical trials (NCT05358717). In December 2024,

Novartis Novartis AG is a Swiss multinational corporation, multinational pharmaceutical company, pharmaceutical corporation based in Basel, Switzerland. Novartis is one of the largest pharmaceutical companies in the world and was the eighth largest by re ...

entered a global license and collaboration agreement with PTC Therapeutics for PTC518 with an upfront payment of $1.0 billion and up to $1.9 billion in development, regulatory, and sales milestones. Therapeutic targeting of poison exon inclusion/exclusion has also been proposed for oncogenic splicing factors, BRD9 (for treatment of cancer), SYNGAP1, RBM3 (for treatment of neurodegeneration), and '' CFTR'' (for treatment of

cystic fibrosis Cystic fibrosis (CF) is a genetic disorder inherited in an autosomal recessive manner that impairs the normal clearance of Sputum, mucus from the lungs, which facilitates the colonization and infection of the lungs by bacteria, notably ''Staphy ...

References

{{Improve categories, date=November 2024 Genetics Medicine Spliceosome Gene expression RNA RNA splicing Drug discovery Nucleic acids Molecular biology Cellular processes Cell biology Biology