Thrombophilia and Immune-Related Genetic Markers in Long COVID

Author:

da Silva Rosilene12,de Sarges Kevin Matheus Lima12ORCID,Cantanhede Marcos Henrique Damasceno12ORCID,da Costa Flávia Póvoa12ORCID,dos Santos Erika Ferreira12ORCID,Rodrigues Fabíola Brasil Barbosa12ORCID,de Nazaré do Socorro de Almeida Viana Maria12,de Meira Leite Mauro12ORCID,da Silva Andréa Luciana Soares13ORCID,de Brito Mioni Thieli Magalhães13ORCID,da Silva Torres Maria Karoliny24ORCID,Queiroz Maria Alice Freitas24ORCID,Vallinoto Izaura Maria Vieira Cayres24,Henriques Daniele Freitas5,dos Santos Carla Pinheiro5,Viana Giselle Maria Rachid26,Quaresma Juarez Antônio Simões27ORCID,Falcão Luiz Fábio Magno7ORCID,Vallinoto Antonio Carlos Rosário24ORCID,dos Santos Eduardo José Melo123ORCID

Affiliation:

1. Laboratory of Genetics of Complex Diseases, Institute of Biological Sciences, Federal University of Pará, Belém 58255-000, Brazil

2. Graduate Program in Biology of Infectious and Parasitic Agents, Federal University of Pará, Belém 58255-000, Brazil

3. Graduate Program in Clinical Analysis, Federal University of Pará, Belém 58255-000, Brazil

4. Laboratory of Virology, Institute of Biological Sciences, Federal University of Pará, Belém 58255-000, Brazil

5. Section of Arbovirology and Hemorrhagic Fevers, Evandro Chagas Institute, Secretary of Health Surveillance, Ministry of Health of Brazil, Ananindeua 67000-000, Brazil

6. Malaria Basic Research Laboratory, Parasitology Section, Evandro Chagas Institute, Health Surveillance Secretariat, Brazilian Ministry of Health, Ananindeua 67000-000, Brazil

7. Center for Biological and Health Sciences, State University of Pará, Belém 58255-000, Brazil

Abstract

Aiming to evaluate the role of ten functional polymorphisms in long COVID, involved in major inflammatory, immune response and thrombophilia pathways, a cross-sectional sample composed of 199 long COVID (LC) patients and a cohort composed of 79 COVID-19 patients whose follow-up by over six months did not reveal any evidence of long COVID (NLC) were investigated to detect genetic susceptibility to long COVID. Ten functional polymorphisms located in thrombophilia-related and immune response genes were genotyped by real time PCR. In terms of clinical outcomes, LC patients presented higher prevalence of heart disease as preexistent comorbidity. In general, the proportions of symptoms in acute phase of the disease were higher among LC patients. The genotype AA of the interferon gamma (IFNG) gene was observed in higher frequency among LC patients (60%; p = 0.033). Moreover, the genotype CC of the methylenetetrahydrofolate reductase (MTHFR) gene was also more frequent among LC patients (49%; p = 0.045). Additionally, the frequencies of LC symptoms were higher among carriers of IFNG genotypes AA than among non-AA genotypes (Z = 5.08; p < 0.0001). Two polymorphisms were associated with LC in both inflammatory and thrombophilia pathways, thus reinforcing their role in LC. The higher frequencies of acute phase symptoms among LC and higher frequency of underlying comorbidities might suggest that acute disease severity and the triggering of preexisting condition may play a role in LC development.

Funder

Secretary of Science, Technology and Higher, Professional and Technological Education of the State of Pará

Amazon Foundation for Research Support

The Coordination for the Improvement of Higher Education Personnel (CAPES), National Council for Scientific and Technological Development

Publisher

MDPI AG

Subject

Virology,Infectious Diseases

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