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A modified Sequential Organ Failure Assessment score for dengue: development, evaluation and proposal for use in clinical trials.

McBride A., Vuong NL., Van Hao N., Huy NQ., Chanh HQ., Chau NTX., Nguyet NM., Ming DK., Ngoc NT., Nhat PTH., Phong NT., Tai LTH., Tho PV., Trung DT., Tam DTH., Trieu HT., Geskus RB., Llewelyn MJ., Thwaites CL., Yacoub S.

BackgroundDengue is a neglected tropical disease, for which no therapeutic agents have shown clinical efficacy to date. Clinical trials have used strikingly variable clinical endpoints, which hampers reproducibility and comparability of findings. We investigated a delta modified Sequential Organ Failure Assessment (delta mSOFA) score as a uniform composite clinical endpoint for use in clinical trials investigating therapeutics for moderate and severe dengue.MethodsWe developed a modified SOFA score for dengue, measured and evaluated its performance at baseline and 48 h after enrolment in a prospective observational cohort of 124 adults admitted to a tertiary referral hospital in Vietnam with dengue shock. The modified SOFA score included pulse pressure in the cardiovascular component. Binary logistic regression, cox proportional hazard and linear regression models were used to estimate association between mSOFA, delta mSOFA and clinical outcomes.ResultsThe analysis included 124 adults with dengue shock. 29 (23.4%) patients required ICU admission for organ support or due to persistent haemodynamic instability: 9/124 (7.3%) required mechanical ventilation, 8/124 (6.5%) required vasopressors, 6/124 (4.8%) required haemofiltration and 5/124 (4.0%) patients died. In univariate analyses, higher baseline and delta (48 h) mSOFA score for dengue were associated with admission to ICU, requirement for organ support and mortality, duration of ICU and hospital admission and IV fluid use.ConclusionsThe baseline and delta mSOFA scores for dengue performed well to discriminate patients with dengue shock by clinical outcomes, including duration of ICU and hospital admission, requirement for organ support and death. We plan to use delta mSOFA as the primary endpoint in an upcoming host-directed therapeutic trial and investigate the performance of this score in other phenotypes of severe dengue in adults and children.

Original publication

DOI

10.1186/s12879-022-07705-8

Type

Journal article

Journal

BMC infectious diseases

Publication Date

09/2022

Volume

22

Addresses

Oxford University Clinical Research Unit, Ho Chi Minh City, Vietnam.

Keywords

Humans, Multiple Organ Failure, Prognosis, Retrospective Studies, Reproducibility of Results, Intensive Care Units, Organ Dysfunction Scores, Tertiary Care Centers, Severe Dengue