Journal
CLINICAL INFECTIOUS DISEASES
Volume 73, Issue 7, Pages E2436-E2443Publisher
OXFORD UNIV PRESS INC
DOI: 10.1093/cid/ciaa1038
Keywords
chikungunya virus; Alphavirus; arthritogenic; arbovirus; fatal cases
Categories
Funding
- Sao Paulo Research Foundation, Brazil [2017/13981-0, 2018/09383-3, 2018/143890, 2018/00837-1, 2019/24251-9]
- Brazilian National Council for Scientific and Technological Development [302584/20153, 408338/2018-0]
- Clarendon Scholarship
- Department of Zoology, University of Oxford
- Fundacao Cearense de Apoio ao Desenvolvimento Cientifico e Tecnologico [FUNCAP 01/2017-SUS/PPSUS-CEFUNCAPSESADecit/SCTIE]
- Wellcome Trust
- Royal Society Sir Henry Dale Fellowship [204311/Z/16/Z]
- Network of Clinical and Applied Research into Chikungunya through Department of Science and Technology, Brazilian Ministry of Health
- MRC [MR/S019510/1] Funding Source: UKRI
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The investigation of fatal Chikungunya virus cases in Ceara state, Brazil, revealed co-infections with Dengue and Zika viruses, neurological symptoms as a major presentation in fatal cases, and no unique virus genomic mutation associated with fatal outcomes.
Background. Chikungunya virus (CHIKV) emerged in the Americas in 2013 and has caused approximately 2.1 million cases and >600 deaths. A retrospective investigation was undertaken to describe clinical, epidemiological, and viral genomic features associated with deaths caused by CHIKV in Ceara state, northeast Brazil. Methods. Sera, cerebrospinal fluid (CSF), and tissue samples from 100 fatal cases with suspected arbovirus infection were tested for CHIKV, dengue virus (DENV), and Zika virus (ZIKV). Clinical, epidemiological, and death reports were obtained for patients with confirmed CHIKV infection. Logistic regression analysis was undertaken to identify independent factors associated with risk of death during CHIKV infection. Phylogenetic analysis was conducted using whole genomes from a subset of cases. Results. Sixty-eight fatal cases had CHIKV infection confirmed by reverse-transcription quantitative polymerase chain reaction (52.9%), viral antigen (41.1%), and/or specific immunoglobulin M (63.2%). Co-detection of CHIKV with DENV was found in 22% of fatal cases, ZIKV in 2.9%, and DENV and ZIKV in 1.5%. A total of 39 CHIKV deaths presented with neurological signs and symptoms, and CHIKV-RNA was found in the CSF of 92.3% of these patients. Fatal outcomes were associated with irreversible multiple organ dysfunction syndrome. Patients with diabetes appear to die at a higher frequency during the subacute phase. Genetic analysis showed circulation of 2 CHIKV East-Central-South African (ECSA) lineages in Ceara and revealed no unique virus genomic mutation associated with fatal outcome. Conclusions. The investigation of the largest cross-sectional cohort of CHIKV deaths to date reveals that CHIKV-ECSA strains can cause death in individuals from both risk and nonrisk groups, including young adults.
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