Abstract

BackgroundIn symptomatic patients, the diagnostic approach of COVID-19 should be holistic. We aimed to evaluate the concordance between RT-PCR and serological tests (IgM/IgG), and identify the factors that best predict mortality (clinical stages or viral load).MethodsThe study included 242 patients referred to the University hospital of Kinshasa for suspected COVID-19, dyspnea or ARDS between June 1st, 2020 and August 02, 2020. Both antibody-SARS-CoV2 IgM/IgG and RT-PCR method were performed on the day of admission to hospital. The clinical stages were established according to the COVID-19 WHO classification. The viral load was expressed by the CtN2 (cycle threshold value of the nucleoproteins) and the CtE (envelope) genes of SARS- CoV-2 detected using GeneXpert. Kappa test and Cox regression were used as appropriate.ResultsThe GeneXpert was positive in 74 patients (30.6%). Seventy two patients (29.8%) had positive IgM and 34 patients (14.0%) had positive IgG. The combination of RT-PCR and serological tests made it possible to treat 104 patients as having COVID-19, which represented an increase in cases of around 41% compared to the result based on GeneXpert alone. The comparison between the two tests has shown that 57 patients (23.5%) had discordant results. The Kappa coefficient was 0.451 (p < 0.001). We recorded 23 deaths (22.1%) among the COVID-19 patients vs 8 deaths (5.8%) among other patients. The severe-critical clinical stage increased the risk of mortality vs. mild-moderate stage (aHR: 26.8, p < 0.001). The values of CtE and CtN2 did not influence mortality significantly.ConclusionIn symptomatic patients, serological tests are a support which makes it possible to refer patients to the dedicated COVID-19 units and treat a greater number of COVID-19 patients. WHO Clinical classification seems to predict mortality better than SARS-Cov2 viral load.

Highlights

  • In symptomatic patients, the diagnostic approach of COVID-19 should be holistic

  • Virusspecific IgM and IgG become detectable approximately 3–5 days after the onset of the disease with a peak during the second and third week [4, 6]; IgM concentration gradually decreases during the fifth week until it becomes undetectable by the seventh week, while IgG persists beyond the seventh week and reaches a titer at least 4 times higher during convalescence compared to the acute phase [4, 7]

  • The main objective of the study was to assess the concordance between the SARS-CoV2 Reverse transcriptase polymerase chain reaction (RT-PCR) and serological tests (IgM/IgG) results performed in symptomatic patients admitted to hospital with suspected COVID19

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Summary

Introduction

The diagnostic approach of COVID-19 should be holistic. We aimed to evaluate the concordance between RT-PCR and serological tests (IgM/IgG), and identify the factors that best predict mortality (clinical stages or viral load). Severe patients usually present with dyspnea and/or hypoxemia 1 week after the onset of symptoms, and they can progress to acute respiratory distress syndrome (ARDS), septic shock and multiple organ dysfunctions [3]. It appears that from the second day after contact with the virus, SARS-Cov-2 nucleic acids can be detected in nasopharyngeal swabs using the “reverse transcriptase polymerase chain reaction” methods (RTPCR) or by “ generation sequency” (NGS) [4]. Virusspecific IgM and IgG become detectable approximately 3–5 days after the onset of the disease with a peak during the second and third week [4, 6]; IgM concentration gradually decreases during the fifth week until it becomes undetectable by the seventh week, while IgG persists beyond the seventh week and reaches a titer at least 4 times higher during convalescence compared to the acute phase [4, 7]

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