Ritwick Mondal1, Shramana Deb2, Durjoy Lahiri3, Gourav Shome4
doi: http://dx.doi.org/10.5195/ijms.2020.727
Volume 8, Number 3: 311-313
Received 03 09 2020: Rev-request 28 09 2020: Rev-request 24 11 2020: Rev-recd 30 09 2020: Rev-recd 30 11 2020: Accepted 01 12 2020
The etiological agent for the ongoing pandemic of COVID-19 is a novel coronavirus, known as Severe Acute Respiratory Syndrome Coronavirus 2 (SARS-CoV-2). The most common symptoms of COVID-19 include fever, dry cough, sore throat, and headache.1 Severe disease can progress to the highly morbid outcome of Acute Respiratory Distress Syndrome (ARDS).2 The number of infected individuals during this pandemic is high while the worldwide mortality rate remain slow.3 According to World Health Organization (WHO) guidelines, the infected patient should be discharged from hospital after containment period of 14 days along with two consecutive negative Quantitative Reverse Transcription Polymerase Chain Reaction (RT-qPCR) results of respiratory specimens at least 24 hours apart.4 During January 28 to March 13, COVID-19 relapse cases have been documented in Shangqui, Henan province and later in Korea.5,6 Pathogenesis of these relapse cases needs further exploration as they hold important links towards the development of a second wave of the pandemic. Here in this article, we propose the following hypotheses on how COVID-19 relapse can play a significant role in disease burden and further horizontal transmission based on available evidence.
The second wave of infection among COVID-19 patients has dazed the scientific world, but it has to be decided whether the second wave of infection is due to reinfection or relapse. According to recent documentation from China5 and Korea,6 there have been recovered patients testing positive after one or two consecutive negative results. Various methods for the diagnosis of the infection are used. These include RT-qPCR, high-throughput sequencing, CT scan, and immunological detection kits.7 Furthermore, improper sampling procedure, different source of swab samples, and variable specificity/sensitivity of nucleic acid tests can lead to the false negative RT-qPCR results implying the persistence of infection rather than recurrence or relapse.7,8 This particular limitation of antibody testing method should be carefully considered before declaration of reinfection or relapse. The durability of the infected patient's immune response plays a significant role to determine the reinfection. The presence of CD4+ T cells and memory CD8+ T cells are found to be protective in case of Coronavirus mediated infection by producing effector cytokines and IFN-gamma.9 It is also noted that immunoglobulins alone are not sufficient to provide long-term immunity.10 Accumulating evidence have shown that virus specific CD8+ T cells were persistent up to 6 years after Severe Acute Respiratory Syndrome Coronavirus 1 (SARS-CoV-1) infection, but memory B cells and accompanying antibodies were undetectable at that time.11 A similar scenario may result from SARS-CoV-2 infection as it shows phylogenetic similarity with SARS-CoV-1.12 A recent study performed by Zhang and colleagues investigated monocyte expression of Angiotensin Converting Enzyme 2 (ACE2), the endogenous entry receptor of SARS-CoV-2. They came to the conclusion that monocytes of COVID-19 patients express a lower concentration of ACE2 in comparison to healthy individuals.13 Therefore, it can be interpreted that SARS-CoV-2 might exist in human Peripheral Blood Mononuclear Cells (PBMCs) (monocytes mainly) and cause relapse after negative PCR on samples from the respiratory tract.14 Considering the aforementioned facts, further research work is required for fine delineation between relapse and reinfection.
Distinct viral clades of SARS-CoV-2 (e.g., A2a, B1) appears to result in variation of virulence.15 Considering this fact, there is a possibility that duration between primary infection and relapse may vary across different clades. Furthermore, there is a possibility that the nature and affinity of protective neutralizing antibodies (NAbs) may vary for different strains as well. Hence, it can be hypothesized that NAbs of primary infection may be unable to protect re-infection by other strains. It also remains to be seen whether, in the case of relapse, there is an insufficient increase in NAbs during the second course of infection.
Viral latency period might be considered as a potential factor in order to determine relapse or reactivation. Reports have suggested disparity amongst proposed viral latency period with a maximum duration of 24 days.16 According to an article by Ye et al, the reported reactivation among 5 patients was a maximum time period of 17 days, but proper clinical characteristics to distinguish reactivation with relapse was not properly demarcated.17 It might be suggested that the virus causes latent infection of cells, while later on the genome gets transcribed and translated into viral proteins. Hence, it could be inferred that the virus gets reactivated from a latent stage to a lytic stage where manifestation of symptoms might be observed as similar phenomenon were already observed for many other viruses.18 Additionally, SARS-CoV-2 can survive and replicate in neuronal cell lines.19 Therefore, another indication towards viral latency through neuro-invasion of virus and reactivation at a later stage is suggested. Considering the abovementioned fact, an important question can be raised: Can an asymptomatic individual with a latent infection spread the virus without being detected? Proper clinical investigation into the potential reactivation of this virus requires immediate further study.
Another undermined and potentially influential factor might be the viral shedding which may cause transmission from an apparently recovered individual or asymptomatic individual to a healthy individual.20 The viral shedding may begin 2-3 days before the appearance of symptoms with viral loads decreasing monotonically after onset of symptoms.21 The virus has been detected in patients at a median of 20 days and up to 37 days post-infection.22 The viral transmission not only comes through droplet or aerosol route but also through the fecal-oral route.23,24 The participation of tears and conjunctival secretions in viral shedding has also been speculated.25 All of these non-classical or non-respiratory tract routes of virus shedding might go unrecognized during discharge of patients who are tested negative through nasopharynageal swab RT-qPCR alone. It is possible that viral titers are still relatively high in various non-classical transmission sites of recovered patients, indicating that they are not only able to spread the infection but also may relapse themselves.
In conclusion, the ongoing public health emergency should look after protocols regarding both molecular testing and antibody testing to contain the pandemic. The infected individuals should strictly be discharged only after two proper consecutive RT-PCR negative results of swab samples from various sources so that it can reduce clinically recovered individuals with apparently hidden viral source. Even after that, the convalescent patients should be monitored by the health system during the post-discharge domiciliary quarantine period of 14 days, and on completion of this period they should be tested again. This should thereby avoid increment in numbers of asymptomatic individuals with reactivation or relapse. Moreover, antibody testing should not be authorized at the time of discharge as its variation of sensitivity/specificity has potential to provide unfounded confidence. That said, there remain a few unanswered questions at this point in time - Does the virus really clear out from the system after the primary infection?; Is it safe to assume that the fragments of virus residing inside the body cannot infect someone after the first course of infection?; Have patients acquired immunity against the diseases for rest of their life?
None.
The Authors have no funding, financial relationships or conflicts of interest to disclose.
Conceptualization: RM, SD, DL and GS. Data Curation: SD and GS. Formal Analysis: RM and SD. Investigation: SD and GS. Methodology: RM and SD. Project Administration: DL and GS. Resources: SD and GS. Software: RM and DL. Supervision: GS and DL. Validation: GS and SD. Visualization: RM and SD. Writing – Original Draft: GS, RM and SD. Writing – Review & Editing: RM, SD, DL and GS.
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Ritwick Mondal, 1 MBBS. Department of Internal Medicine, Institute of Postgraduate Medical Education and Research, SSKM Hospital, Kolkata, India
Shramana Deb, 2 MSc, S.N. Pradhan Centre for Neurosciences, University of Calcutta, India
Durjoy Lahiri, 3 MD, DM. Bangur Institute of Neurosciences, Institute of Postgraduate Medical Education and Research, SSKM Hospital, Kolkata, India
Gourav Shome, 4 MSc. Department of Microbiology, College of Science, Technology & Agriculture. University of Calcutta, India
About the Author: Dr. Ritwick Mondal is a first class MBBS graduate from Institute of Postgraduate and Medical Education and SSKM Hospital, Kolkata, India. He is currently engaged as a Junior Resident Department of Internal Medicine at the above institution. He has received various notable awards like ICMR-STS, international ambassador for the UMCG, Groningen etc. He is currently exposed to laboratory research at Bangur institute of Neurosciences.
Correspondence: Gourav Shome. Address: 35 Ballygunge Circular Road. Kolkata – 700019, India. Email: gshome007@gmail.com
Editor: Francisco J. Bonilla-Escobar Reviewers: Mihnea-Alexandru Gaman, Paul MacDaragh Ryan Copyeditor: Sohaib Haseeb Proofreader: Leah Komer Layout Editor: Annora A. Kumar
Cite as: Mondal R, Deb S, Lahiri D, Shome G. Recurrence of COVID-19: Treading the Fine Line Between Relapse and Re-infection. Int J Med Students. 2020 Sep-Dec;8(3):311-3.
Copyright © 2020 Ritwick Mondal, Shramana Deb, Durjoy Lahiri, Gourav Shome
This work is licensed under a Creative Commons Attribution 4.0 International License.
International Journal of Medical Students, VOLUME 8, NUMBER 3, December 2020