Single nucleotide variations in ZBTB46 are associated with post-thrombolytic parenchymal haematoma.
Caty CarreraJara Cárcel-MárquezNatalia CullellNuria Torres-ÁguilaElena MuiñoJosé CastilloTomás SobrinoFrancisco CamposEmilio Rodríguez-CastroLaia Llucià-CarolMònica MillánLucía Muñoz-NarbonaElena López-CancioAlejandro BustamanteMarc RibóJosé Álvarez-SabínJordi Jiménez-CondeJaume RoquerEva Giralt-SteinhauerCarolina Soriano-TárragaMarina Mola-CaminalCristófol Vives-BauzaRosa Díaz NavarroSilvia TurVictor ObachJuan Francisco ArenillasTomás SeguraGemma Serrano-HerasJoan Martí-FàbregasRaquel Delgado-MederosM Mar Freijo-GuerreroFrancisco MonicheJuan Antonio CabezasMar CastellanosCristina Gallego-FábregaJonathan González-SanchezJurek KrupinskyDaniel StrbianTurgut TatlisumakVincent ThijsRobin LemmensAgnieszka SlowikJohanna PeraSteven KittnerJohn ColeLaura HeitschLaura IbañezCarlos CruchagaJin-Moo LeeJoan MontanerIsrael Fernández-CadenasPublished in: Brain : a journal of neurology (2021)
Haemorrhagic transformation is a complication of recombinant tissue-plasminogen activator treatment. The most severe form, parenchymal haematoma, can result in neurological deterioration, disability, and death. Our objective was to identify single nucleotide variations associated with a risk of parenchymal haematoma following thrombolytic therapy in patients with acute ischaemic stroke. A fixed-effect genome-wide meta-analysis was performed combining two-stage genome-wide association studies (n = 1904). The discovery stage (three cohorts) comprised 1324 ischaemic stroke individuals, 5.4% of whom had a parenchymal haematoma. Genetic variants yielding a P-value < 0.05 1 × 10-5 were analysed in the validation stage (six cohorts), formed by 580 ischaemic stroke patients with 12.1% haemorrhagic events. All participants received recombinant tissue-plasminogen activator; cases were parenchymal haematoma type 1 or 2 as defined by the European Cooperative Acute Stroke Study (ECASS) criteria. Genome-wide significant findings (P < 5 × 10-8) were characterized by in silico functional annotation, gene expression, and DNA regulatory elements. We analysed 7 989 272 single nucleotide polymorphisms and identified a genome-wide association locus on chromosome 20 in the discovery cohort; functional annotation indicated that the ZBTB46 gene was driving the association for chromosome 20. The top single nucleotide polymorphism was rs76484331 in the ZBTB46 gene [P = 2.49 × 10-8; odds ratio (OR): 11.21; 95% confidence interval (CI): 4.82-26.55]. In the replication cohort (n = 580), the rs76484331 polymorphism was associated with parenchymal haematoma (P = 0.01), and the overall association after meta-analysis increased (P = 1.61 × 10-8; OR: 5.84; 95% CI: 3.16-10.76). ZBTB46 codes the zinc finger and BTB domain-containing protein 46 that acts as a transcription factor. In silico studies indicated that ZBTB46 is expressed in brain tissue by neurons and endothelial cells. Moreover, rs76484331 interacts with the promoter sites located at 20q13. In conclusion, we identified single nucleotide variants in the ZBTB46 gene associated with a higher risk of parenchymal haematoma following recombinant tissue-plasminogen activator treatment.
Keyphrases
- genome wide
- copy number
- dna methylation
- genome wide association
- systematic review
- gene expression
- transcription factor
- case control
- endothelial cells
- small molecule
- cell free
- genome wide identification
- molecular docking
- high throughput
- meta analyses
- early onset
- binding protein
- randomized controlled trial
- stem cells
- multiple sclerosis
- acute ischemic stroke
- white matter
- protein protein
- circulating tumor
- brain injury
- drug induced
- smoking cessation
- single cell
- replacement therapy
- mesenchymal stem cells