Genetic Variants in Stroke

NCT ID: NCT07186517

Last Updated: 2025-09-22

Basic Information

• Recruitment Status: NOT_YET_RECRUITING
• Total Enrollment: 1000 participants
• Study Classification: OBSERVATIONAL
• Study Start Date: 2025-10-01
• Study Completion Date: 2030-12-31

Brief Summary

Stroke is the leading cause of death and disability in Brazil and worldwide, with a significant socioeconomic impact. Despite advances in prevention and treatment, the role of genetic variants in ischemic stroke remains underexplored, especially in genetically diverse populations like Brazil's. International studies such as MEGASTROKE and GIGASTROKE have identified risk loci for stroke, but with low representation of the Latin American population. This study aims to fill that gap by evaluating the prevalence and clinical impact of genetic polymorphisms previously described in Brazilians, thereby laying the groundwork for precision medicine within Brazil's Unified Health System (SUS).

Detailed Description

Study Overview: ÁRTEMIS-Brazil is a multicenter, case-control study that will recruit 1,000 participants (500 stroke patients and 500 controls) across 10 hospitals in Brazil. All participants will be extensively phenotyped, including demographic, clinical, lifestyle, neuroimaging, and laboratory data, in order to create a comprehensive dataset that links genomic information with health outcomes. Peripheral blood samples will be collected and processed under strict biobanking standards. DNA will undergo whole genome sequencing (WGS), enabling high-resolution investigation of genetic variation in an admixed population.

2) Genomic and Bioinformatics Methodology: The analytical workflow has been designed to ensure high-quality, reproducible results and includes the following components: Pre-processing Removal of adapters, low-quality bases, and contaminant sequences. Filtering of reads based on Phred quality scores to retain only high-confidence sequences.

Alignment and Assembly Mapping of cleaned reads to the human reference genome (GRCh38). Evaluation of coverage, depth, and mapping accuracy. Quality metrics will be benchmarked against international standards.

Variant Analysis Identification and annotation of genetic variants, including single nucleotide polymorphisms (SNPs) and insertions/deletions (indels).

Annotation pipelines (e.g., GATK, ANNOVAR, VEP) will classify variants by predicted functional effect, population frequency, and pathogenicity.

Integration with reference databases such as gnomAD, ClinVar, PharmGKB, and dbSNP to contextualize findings.

Ancestry Analysis Estimation of genetic ancestry proportions using population-specific markers. Adjustment for population stratification in association analyses. Exploration of ancestry contributions to stroke susceptibility and clinical outcomes in Brazil's admixed population.

Pharmacogenetic Analysis Evaluation of variants in genes related to drug metabolism, efficacy, and toxicity (e.g., CYP450 family, platelet receptor pathways, anticoagulant metabolism).

Analysis of implications for treatment of acute ischemic stroke and secondary prevention, with emphasis on tailoring therapy to genetic profiles.

3) Scientific and Clinical Impact: By combining genomic data with detailed phenotypic information, ARTEMIS-Brazil is uniquely positioned to: Identify novel genetic variants associated with stroke in an underrepresented population; Validate known variants in the context of Brazilian admixture; Characterize the contribution of ancestry to stroke risk and outcomes; Generate pharmacogenetic evidence to support personalized stroke care.

The project will advance global understanding of stroke genetics and contribute to the implementation of precision medicine strategies within the Brazilian Unified Health System (SUS). By ensuring representation of admixed populations in genomic research, ÁRTEMIS-Brazil will fill a major gap in current knowledge and create a foundation for more equitable healthcare.

Conditions

Stroke; Genetic Association Studies

Study Design

• Observational Model Type: CASE_CONTROL
• Study Time Perspective: PROSPECTIVE

Eligibility Criteria

Inclusion Criteria

Cases

• Age ≥18 years;
• Confirmed diagnosis by neuroimaging (CT or MRI) of a first episode of ischemic stroke in the last 12 months;
• TOAST classification of stroke available: cardioembolic, lacunar, atherosclerotic, or undetermined due to the presence of multiple sources (cardioembolic/atherosclerotic);
• Modified Rankin Scale (mRS) ≤4 at the time of inclusion;
• Ability and willingness to provide consent and participate in follow-up assessments.

Controls

• Age ≥18 years;
• Reside in the same household or, if not, in the same neighborhood as the case group participant;
• Not be a blood relative of the case group participant;
• Ability and willingness to provide consent and participate in follow-up assessments.

Exclusion Criteria

Cases

• Ischemic stroke with a distinct etiology based on TOAST criteria (e.g., infectious, autoimmune, endocarditis, reversible cerebral vasoconstriction syndrome, drug-related causes);
• Diagnosis of monogenic or mitochondrial disorders, such as CADASIL, Fabry disease, homocystinuria, MELAS, sickle cell disease, among others;
• Clinical conditions that reduce life expectancy to less than one year (e.g., neoplasia);
• Inability to undergo magnetic resonance imaging (due to metal artifacts, MRI-incompatible implants, claustrophobia);
• Other conditions that, at the investigator's discretion, prevent participation or compromise follow-up.

Controls

• Personal history of stroke, transient ischemic attack (TIA), coronary, or peripheral artery disease;
• Serious comorbidities that may impact participation or confound the results;
• Clinical conditions that reduce life expectancy to less than one year;
• Inability to provide consent due to cognitive impairment or other factors;
• Inability to undergo magnetic resonance imaging (due to metal artifacts, incompatible implants, claustrophobia);
• Diagnosis of monogenic or mitochondrial disorders, such as CADASIL, Fabry disease, homocystinuria, MELAS, or sickle cell disease;
• Other conditions that, at the investigator's discretion, prevent participation or compromise follow-up.

• Minimum Eligible Age: 18 Years
• Eligible Sex: ALL
• Accepts Healthy Volunteers: Yes

Sponsors

Ministry of Health, Brazil

OTHER_GOV

Sponsor Role: collaborator

Hospital Moinhos de Vento

OTHER

Sponsor Role: lead

Responsible Party

Responsibility Role: SPONSOR

Principal Investigators

Ana C de Souza, PhD

Role: PRINCIPAL_INVESTIGATOR

Hospital Moinhos de Vento

Locations

Hospital de Clínicas de Porto Alegre

Porto Alegre, Rio Grande do Sul, Brazil

Hospital Ophir Loyola

Belém, , Brazil

Hospital Metropolitano Dr. Célio de Castro

Belo Horizonte, , Brazil

Hospital Geral de Roraima

Boa Vista, , Brazil

Hospital Universitário Maria Aparecida Pedrossian

Campo Grande, , Brazil

Hospital Geral de Fortaleza

Fortaleza, , Brazil

Clínica Neurológica

Joinville, , Brazil

Hospital Geral de Palmas

Palmas, , Brazil

Hospital da Restauração Governador Paulo Guerra

Recife, , Brazil

Hospital Universitário Edgar Santos

Salvador, , Brazil

Hospital São Paulo

São Paulo, , Brazil

Countries

Brazil

Central Contacts

Ana C de Souza, PhD

Role: CONTACT

neuroana87@gmail.com

+55 51 33143434

Facility Contacts

Sheila C Martins, PhD

Role: primary

Antonio de Matos

Role: primary

Fidel Meira

Role: primary

Livia Martins

Role: primary

Gabriel Braga

Role: primary

Fabrício Oliveira Lima, PhD

Role: primary

Carla Moro, PhD

Role: primary

Priscila Leite

Role: primary

Ana do Nascimento, PhD

Role: primary

Jamary Oliveira-Filho, PhD

Role: primary

Gisele Sampaio, PhD

Role: primary

Other Identifiers

86795025.0.1001.5330

Identifier Type: -

Identifier Source: org_study_id