key: cord-0714493-u5xnmsv8
authors: Farshi, Esmaeil; Kasmapur, Bahram; Arad, Anya
title: Investigation of immune cells on elimination of pulmonary‐Infected COVID‐19 and important role of innate immunity, phagocytes
date: 2020-09-18
journal: Rev Med Virol
DOI: 10.1002/rmv.2158
sha: be64b7811d8a02f872400ff37bce256b79774934
doc_id: 714493
cord_uid: u5xnmsv8

We identified types of immune cells that contribute to clearing COVID‐19 during the acute phase of the infection in mouse model and human. Our results suggest that both innate and adaptive immune responses are essential for controlling COVID‐19 infection. Mild infection report of children by COVID‐19 comparing adults' infection causes conclusion of higher resistance of immune system of children comparing adults. Our results show innate immune system including phagocytes contribute severely to the elimination of COVID‐19 in both mouse model and human. Our results also show the elimination of COVID‐19 required the activation of B cells by CD4+ T cells. CD4+ T cells play an important role in elimination of COVID‐19 in primary effection. We measured IgM and IgG in all patients including adults and kids (human) and found IgM and IgG in kids patients are much higher than other adults patients. It causes production of much more natural antibodies in kids' bodies to protect them against COVID‐19 that shows reason of mild effection of kids comparing adults. Our observations have important ramifications for the development of novel vaccination and medicine strategies to alleviate COVID‐19. The most important result is for producing any vaccine for COVID‐19, increasing and producing these factors must be included: (a) Phagocytes (IgM and IgG), (b) T Cells, and (c) White Cells.

Coronaviruses are important human and animal pathogens. At the end of 2019, a novel coronavirus, was identified as the cause of a cluster of pneumonia cases in Wuhan, China. It rapidly spread, resulting in an epidemic throughout China, with sporadic cases reported globally. From December 2019 till now, the disease, which resulted in several millions cases with many deaths, was caused by a novel type of coronavirus, termed COVID-19. Patients with COVID- 19 usually developed a high fever followed by clinical symptoms of cough and shortness of breath. Full-genome sequencing and phylogenic analysis indicated that the coronavirus that causes COVID-19 is a betacoronavirus in the same subgenus as the severe acute respiratory syndrome (SARS-CoV) virus (as well as several bat coronaviruses), but in a different clade. 1 The apparent structure of the receptor-binding gene region in COVID-19 is very similar to that of the SARS coronavirus, and there is speculation that it will be shown to use the same receptor for cell entry. Full-length genome sequences were obtained from five patients at the early stage of the outbreak show they are almost identical to each other and share 79.5% sequence identify to SARS-CoV. 2 Furthermore, it was found that COVID-19 is 96% identical at the whole-genome level to a bat coronavirus. 2 However, there has been no subsequent consensus regarding which treatment, if any, benefited COVID-19 patients during the outbreak.

The development of an effective treatment and vaccination strategy for COVID-19 cases will require clarifying the precise mechanisms by which host immune responses control COVID-19 infection. Cumulative evidence suggests that patients who recovered from COVID-19 possessed specific acquired immunity based on both T and B cells. 3 However, the effector cells or molecules that act to eliminate COVID-19 during the acute phase of the infection remain unclear. The mechanisms by which SARS-CoV infection causes the pathogenesis and host immune responses has been investigated using adequate animal infectious models. [4] [5] [6] [7] [8] Lethal disease in BALB/c mice infected with a mouse-adapted strain of SARS-CoV, MA15, showed a lack of activation of innate immune response, resulting in a barely detectable antivirus T cell response. 8 On the other hand, aged BALB/c mice that were infected with a human clinical isolate of SARS-CoV (Urbani strain) successfully eliminated the invasive virus within 1 week post-infection; these mice exhibited high and prolonged levels of viral replication, signs consistent with clinical symptoms, and pathologic changes in the lung resembling those seen in elderly SARS patients. 4 Therefore, the infection of these aged mice is considered a model for the successful elimination of SARS-CoV by host immune responses. A study reported that CD4 + T cells play an important role in the control of SARS-CoV infection. 9 These researchers also reported an important role for innate defense mechanisms in controlling SARS-CoV infection, as demonstrated by the clearance of SARS-CoV over 9 days post-infection (dpi) in BALB/c mice depleted of both CD4+ and CD8+ T cells. 9 These results suggest that both innate and adaptive immune responses are essential for controlling SARS-CoV infection. The results in Reference 10 show also that the cooperation of anti-SARS-CoV antibodies and phagocytic cells plays an important role in the elimination of SARS-CoV.

We studied the identity and role of effector cells and molecules participating in the elimination of COVID-19 during the acute phase of COVID-19 in our work. In this study, we attempted to identify the types of immune cells that contribute to clearing COVID-19 during the acute phase of the infection in mice models plus human. We demonstrate that phagocytic cells play an important role in the elimination of COVID-19 in both mouse and human models of infection.

The contributions of cellular vs humoral immune responses in the res- The intranasal (i.n.) infection of aged BALB/c mice with COVID-19 resulted in over 10 8 median tissue culture infectious dose (TCID 50)/g lung tissue at 2 dpi, 6 dbi, 9 dbi, 10 dbi, and 20 dbi. The infected mice at 2 dbi exhibited histological signs of severe pneumonia, including interstitial cell thickening, immune cell infiltration, and epithelial damage in the bronchus, at 10 dpi and 20 dpi. The observed titers in the aged-mouse model were considerably higher than those seen in infected young BALB/c mice and very young SCID mice, which did not show apparent histological signs of pneumonia. Titers in the aged mice remained high (~10 7 TCID 50/g lung tissue) at 6 dpi. However, the titers decreased to levels below the lower limit of detection (LLOD; <1000 TCID 50/g lung tissue) in the lungs of aged BALB/c mice and young BALB/c mice at 9 dpi. In contrast, very young SCID mice, which lack functional T and B cells, were persistently infected with COVID-19 during the experimental period (through 20 dpi). At this time, SCID mice did not exhibit histological signs of severe pneumonia at 9 and 20 dpi, although a high viral titer was detected in the lungs of these animals during the experimental period. Zhao and Perlman 7 and also Yasui and et al 10 

To determine host protection(s) involved in the elimination of COVID-19 in the lungs, we depleted CD4+ cells and/or CD8+ cells before and after COVID-19 infection in BALB/c mice. Depletion of CD4+ cells or CD8+ cells was done by intravenous (i.v.) injection of monoclonal antibody; control experiments showed that the injection of these mAbs caused an almost complete depletion of the corresponding cell populations. Unlike peripheral blood, the incidence of CD20 B cells was very low in BALB/c mice. We examined (using one of the two models) that CD4+ T cells can directly eliminate COVID-19 by secretion of IFN-y. The IFN-γ-deficient mice and the very young SCID mice that received splenocytes from IFN-γ deficient mice controlled the COVID-19 infection as well as the wild-type mice did. In summary, CD20 and CD8 T cell depletions were more profound (achieving 100% loss by day 0) and lasted longer than CD4+ T cell depletion.

Following depletion, recovery was very slow in all three lymphocyte subsets and the frequencies did not return to baseline by the end of the study. We found that loss of CD8+ T cells led to a very low peak viral load and the loss of CD4+ T cells led to significantly higher viral loads and disseminated COVID-19. We found also the elimination of Other blood cells also may serve as effectors for the control of COVID-19 Specifically, elevated levels of alveolar macrophages, monocyte-derived infiltrating macrophages, and neutrophils that were observed also in many SARS patients. 12 To investigate the role of these myeloid cells in the clearance of COVID-19-infected pulmonary tissue, each subset of these myeloid cells was depleted by administration of a specific mAb or reagent. Consistent with other reports in SARS, 13 alveolar macrophages were depleted for more than 5 days following i.n. administration of 100 μL of 33% clodronate liposome.

Neutrophils (CD11b + and Ly-6G hi) and Gr-1 int monocytes in blood and lung were significantly depleted for at least 3 days after i.p. treatment with 250 μg of anti-Gr-1 mAb, whereas neutrophils alone were depleted upon administration of anti-Ly-6G mAb (1A8).

The Gr-1+ cell-and/or alveolar macrophage-depleted groups failed to eliminate the pulmonary COVID-19 infection, whereas the alveolar macrophage-depleted group showed partial elimination of the virus.

In contrast, the neutrophil-depleted BALB/c animals (anti-Ly-6G mAb-treated mice) eliminated COVID-19 by 9 dpi. Importantly, the neutralizing Ab titer of these cell-depleted mice was comparable to that of untreated BALB/c mice. These results suggest that phagocytic cells, especially monocyte-derived infiltrating macrophages, cooperate with anti-COVID-19 Abs to provide control of COVID-19 infection in these mouse models while Abs individually have small role in control of COVID-19 infection.

The majority of COVID-19 cases (about 80%) is asymptomatic or exhibits mild to moderate symptoms, but approximately the 15% progresses to severe pneumonia and about 5% eventually develops acute respiratory distress syndrome (ARDS), septic shock and/or multiple organ failure.

gives great idea about critical role of phagocytes cells in COVID-19.

Finding a human (especially child) in early stage of COVID-19 is extremely difficult but we found 13 children in ages between 4 and 10 who were in the first days of infection. We also investigated 33 adults human with severe infection of COVID-19.

We investigated both innate and adaptive immune systems in all patients. Seroconversion curves of reference [14] were constructed from the data and showed that total antibodies and IgM isotype antibodies were 100% detectable approximately 1 month after symptom onset. However, in the first week after developing signs of illness, antibodies were present in less than 40% of patients tested. The seroconversion rate and antibody levels rose quickly during the fortnight after symptom onset, and the cumulative seropositive rate was 50% on day 11 and 100% on day 39.

Our purpose was to compare IgM isotype antibodies between We observed, in the early phases of infection in children, natural antibodies play a most important role. Natural antibodies, mostly of IgM isotype and generated independently of previous antigen encounters, have a broad reactivity and a variable affinity. They contain the infection during the 2 weeks necessary for production of high-affinity antibodies and MBCs that will clear the virus and prevent reinfection. In humans, natural antibodies are produced by innate or IgM MBCs, a population of MBCs that is generated independently of the germinal centers and is most abundant in children (Figures 1 and 2 and Table 1 ).

We measured IgM in all patients including adults and kids. As seen in Figure 3 one may see IgM and IgG in kids patinets are much higher than adults patients in beginning days of infection but it becomes equal almost after 30 days. Higher IgM and IgG in beginning days cause production of much more natural antibodies in kids' bodies to protect them against COVID-19. This clearly shows why kids are more immune against COVID-19. It gives also idea about novel vaccination and medicine strategies to alleviate COVID-19.

We observed adult patients with severe COVID-19 showed lower percentage and count in CD4+ and CD8+ lymphocytes populations, strong predictive values for in-hospital mortality, organ injury, and severe pneumonia. We also observed significantly lower number of total T cells, both helper T cells and suppressor T cells. Main effort of all researchers on COVID-19 in future should be on innate immune system especially phagocytes.

We express our gratitude to Dr. Kasmai of the Institute of Medical Science for technical assistance in the evaluation of lung histopathology.

F I G U R E 3 Average IgM and IgG in kids (13 kids in ages between 4 and 10) and adults patients (33 adults between ages 18 and 67) blood per days after infection to COVID-19. One may see IgM and IgG in kids patients are much higher than adult's patients in beginning days of infection but it becomes equal almost after 30 days. Higher IgM and IgG in beginning days cause production of much more natural antibodies in kids' bodies to protect them against COVID-19. This clearly shows why kids are more immune against COVID-19. It gives also idea about novel vaccination and medicine strategies to alleviate COVID-19

This study was supported financially 90% by Dr. Haghro owner of Peace and Health Organization, and other 10% by Prof. Emami from Teratron Inc.

Data available on request from the authors The data that support the findings of this study are available from the corresponding author upon reasonable request.

Esmaeil Farshi https://orcid.org/0000-0003-4591-9582

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How to cite this article: Farshi E, Kasmapur B, Arad A. Investigation of immune cells on elimination of pulmonary-Infected COVID-19 and important role of innate immunity, phagocytes