COVID-19 DISEASE AND ITS OUTBREAK
On March 11, 2020, the World Health Organization (WHO) announced a pandemic of the new outbreak of coronavirus disease 2019 (COVID-19) due to a severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), which began in December 2019 in Wuhan, China. 1 As of March 25, 2020, a total of 198 countries and territories around the world and 1 international conveyance were affected, with 467,520 cases of COVID-19, and 21,174 deaths worldwide. Iran is also considered as the 25th country to be infected with SARS-CoV-2. As of March 25, 2020, there were 27,017 cases of infection (sixth, after China, Italy, United States, Spain, Germany), and 2077 deaths (fourth, after Italy, Spain, China) in Iran. 2
Although scientists and researchers around the world are currently working to discover more scientific knowledge about SARS-CoV-2 and its pathogenesis, specific effective antiviral drugs against this novel coronavirus have not been reported and approved. Current management, therefore, includes travel restrictions, patient isolation, home quarantine, and supportive and symptomatic medical care. Reference Farnoosh, Alishiri and Zijoud3
COVID-19 develops with the clinical presentation of pneumonia and infection, with an approximate incubation period of 2 to 14 days. In addition to respiratory symptoms, such as cough and shortness of breath, symptoms such as fever, myalgia, and fatigue have also been reported. The onset of the COVID-19 may rapidly progress to multiple organ damages, especially in the lung, presenting bilateral diffuse alveolar damage with cellular fibromyxoid exudates. Reference Xu, Shi and Wang4
The COVID-19 mortality rate is 4.3% worldwide, although in some countries, including Iran (7.8%) mortality is higher than worldwide. 2 It has also been shown that people with underlying health issues, including respiratory disease, heart failure, hypertension, diabetes, immunodeficiency, transplant recipients, cancer, and old age are more vulnerable, which means that some people are at higher risk. Reference Diaz5 Iranian survivors of mustard gas exposure seem to be another group that is at high risk of succumbing to SARS-CoV-2.
PULMONARY COMPLICATIONS IN IRANIAN SURVIVORS OF MUSTARD GAS EXPOSURE
According to an epidemiological estimate, there are now more than 100,000 chemical warfare survivors in Iranian society who were exposed to mustard gas during the Iran-Iraq War (1980-88) and are now suffering from long-term complications, including ophthalmic, cutaneous, respiratory, and pulmonary problems. Reference Balali-Mood and Hefazi6 Respiratory and pulmonary problems are the leading cause of long-term disability in these survivors. In a study of 34,000 Iranian survivors of mustard gas exposure, 14,450 (42.5%) of them had pulmonary lesions. These pulmonary lesions were divided into 3 categories: mild (75%), moderate (15%), and severe (10%) based on pulmonary function tests (PFTs) and physical examination findings. Reference Khateri, Ghanei and Keshavarz7
Mustard gas has both acute (early) and chronic (late) effects on the respiratory system. Routine exposure to mustard gas leads to acute symptoms of the upper respiratory tract, such as irritated throat, sore throat, rhinorrhea, sneezing, and discomfort in the nose and sinuses. With more severe exposure to mustard gas, nasal mucosa bleeding, dry cough, and tracheobronchitis occurs. Acute lower respiratory symptoms usually include cough, shortness of breath, and burning sensation in the chest, hemoptysis, inflammation of the airways, and pneumonia and acute respiratory distress syndrome. Over time, these symptoms gradually become chronic. Reference Balali-Mood and Hefazi6,Reference Razavi, Ghanei and Salamati8,Reference Taghadosi, Razi and Zarea9
Based on chest radiograph (CXR) findings in survivors late-onset chronic pulmonary complications of mustard gas include: increased bronchovascular marking, air retention, bronchiectasis, pneumonic infiltration, and radiographic evidence of pulmonary hypertension. Reference Balali-Mood, Hefazi and Mahmoudi10,Reference Bagheri, Hosseini and Mostafavi11 In 197 Iranian survivors, 10 years after severe mustard gas exposure, some pulmonary complications, such as chronic bronchitis (58%), asthma (10%), bronchiectasis (8%), airway obstruction by granulation tissue (9%), and pulmonary fibrosis (12%), had been reported. Reference Emad and Rezaian12
In many studies, in mustard-exposed survivors, chronic bronchitis has been reported as the most common late-onset respiratory event following exposure to mustard gas. Hypoxemia and hypercapnia are most commonly seen in moderate to severe cases, leading to core pulmonale and pulmonary hypertension in the severe stages of the complications. Airway infection with bronchopneumonia is also a common problem that often leads to septicemia. Reference Balali-Mood, Hefazi and Mahmoudi10,Reference Emad and Rezaian12
Increased airway sensitivity, characterized by typical attacks of dyspnea, wheezing, and nocturnal cough, and airflow obstruction patterns in spirometry have been reported between 4 weeks and 20 years after mustard gas inhalation. Bronchospasm attacks are typically triggered by lung infections, asthma, environmental allergens, and cold air. Reference Emad and Rezaian12,Reference Bijani and Moghadamnia13
The direct effects of mustard gas on the mucosa of the bronchial wall and, more importantly, recurrent respiratory infections following the inhalation of mustard gas, are responsible for the development of bronchiectasis. As shown in a study of 40 Iranian survivors with severe late complications of mustard gas, the severity, and prevalence of bronchiectasis lesions tend to increase over time. These lesions usually begin bilaterally in the lower lobe and then progress to the middle lobe and lingula segment. In severe cases with extensive bronchiectasis, pulmonary hypertension, and eventually, core pulmonale may occur. Reference Balali-Mood, Hefazi and Mahmoudi10,Reference Ghanei, Mokhtari and Mohammad14
Bronchoalveolar lavage (BAL) fluid analysis in patients who have inhaled mustard gas demonstrated that these patients have a persistent local inflammatory process in the lower respiratory tract resulting in pulmonary fibrosis, years after initial contact. Histopathologic evaluation of transbronchial lung biopsies in 73 mustard-exposed survivors showed variegated fibrosis, diffuse fibrosis, and an absence of fibrosis in 86%, 4%, and 10% of patients, respectively. Interstitial pneumonitis accounted for 97% of all fibrosis cases. Reference Emad and Rezaian15,Reference Samieepour and Ghanei16
THE PATHOGENESIS OF MUSTARD GAS IN ACUTE AND CHRONIC COMPLICATIONS
Sulfur mustard (SM) or mustard gas, (C4 H8 Cl2 S) (2,2′-dichloroethyl sulfide), is an alkylating agent. SM is absorbed through inhalation, the skin, the anterior surface of the eye, the lungs, and the gastrointestinal tract. Reference Kumar, Sugendran and Vijayaraghavan17 As noted, due to the effect of SM on the body, its complications are divided into acute and chronic/delayed effects. Even 4 decades after the Iran-Iraq war in the 1980s, the deleterious effects of SM poisoning on survivors are still not fully understood. The damage with varying severity to multiple organs of the body has been reported for many years in Iranian SM exposed survivors.
After adsorption, SM undergoes intramolecular cyclization, leading to the formation of an ethylene episulfonium ion intermediate. The cyclic intermediate reacts by alkylating various types of electron-rich biological molecules and attacking and breaking DNA at specific nucleotides. As a result, it inhibits the synthesis of DNA, RNA, and protein. Although SM reacts with RNA, proteins, and phospholipids, the consensus idea is that it is a DNA alkylating agent and has an effective role in delaying healing. The most important alkylating site in mammals is the residual guanine nitrogen. Cell death due to DNA cross-linking is delayed until DNA replication and cell division. However, at higher cellular exposures, other mechanisms are important and accelerate cell death. Another mechanism that may be involved in acute SM injury is the reduction of nicotinamide adenine dinucleotide. Other potential mechanisms thought to be involved include the rapid inactivation of sulfhydryl-containing proteins and peptides, such as glutathione. Glutathione and other sulfhydryl compounds are important in maintaining the proper oxidation-reduction state of cellular components as well as in reducing reactive oxygen species in the cell. Therefore, glutathione and other sulfhydryl compounds can act to prevent peroxidation and loss of membrane integrity. Reducing glutathione produces reactive oxygen species. Acute damage to the mucous membrane, which occurs after exposure to SM, is probably due to 1 or more of these mechanisms producing necrosis and cell death, which is continued by erythema, pain, vesicles formation, blisters, ulcer, and impaired wound healing. In addition to the mentioned mechanisms, SM has other side effects on cells, such as mitosis inhibition (effects on the immune system and hematopoietic as well as epithelial and reproductive tissues), mutagenesis, carcinogenesis, and cholinomimetic effects. Reference Ball and Roberts18,Reference Eklöw, Moldéus and Orrenius19
The mechanism of delayed complications of SM poisoning is not well understood. A strong possibility is the production of reactive oxygen and nitrogen radicals in the cell that react with target molecules such as DNA, protein, lipid, and carbohydrate. The result of these reactions is the necrosis, inflammation, and alteration in the activity of antioxidant enzymes (superoxide dismutase, glutathione peroxidase, and catalase) producing more free radicals and exacerbating oxidative stress. Reference Kumar, Sugendran and Vijayaraghavan17,Reference Sidell, Takafuji and Franz20 A study in SM-exposed survivors reported a significant decrease in glutathione transferase and paraoxonase activity and mutation in the R genotype of paraoxonase. Reference Taravati, Ardestani and Ziaee21 Decreased lung glutathione levels have been reported in survivors 20 years after SM exposure, which is directly related to altered pulmonary function. By identifying the role of free radicals in the acute effects of SM and activating pathways of its production in the body, this comes to mind that the late effects of exposure to SM, such as respiratory and pulmonary complications, can also be caused by the failure to control free radicals and continuous production of these compounds in the body. SM exerts its effects on the airways and lung parenchyma by free radicals and other agents. When it is absorbed by the respiratory system, SM causes inflammation of the tracheobronchial epithelium with severe leukocyte infiltration, alveolar hemorrhage with thrombus formation, and vacuolization of the lung parenchymal cells. The pathological changes that occur after exposure to SM are asthma, chronic obstructive pulmonary disease (COPD), and chronic bronchitis Reference Mansoor Ghanaei and Alizadeh22,Reference Pant and Vijayaraghavan23 (Figure 1).
Evidence suggests that SM can also cause cellular and humoral immune dysfunction. Most SM-exposed survivors have been shown to have elevated levels of immunoglobulin (Ig) G and IgM during the first weeks to 6 months after exposure. Even at 8 years postexposure, the frequency of patients with elevated levels of IgG, IgE, and IgM remained significantly higher than the control group. Reference Hassan and Ebtekar24 Sixteen to 20 years after exposure, IgM levels were still significantly higher than controls. Reference Balali-Mood, Hefazi and Mahmoudi10
In addition, SM affects the immune system decreasing lymphocytes and neutrophils and increasing monocytes. These changes in the immune system in many people exposed to SM cause 2 major problems: a high incidence of malignancy and recurrent infections, among which acute myelocytic leukemia (AML) and acute lymphoblastic leukemia (ALL) are more common. Reference Ghanei25,Reference Zakery Neia26
BAL fluid analysis in patients with SM-exposed has shown an ongoing local inflammatory process that tends to develop pulmonary fibrosis many years after initial exposure. BAL fluid analysis also shows that pulmonary fibrosis after SM exposure is associated with increased inflammatory cytokines and chemokines, including interleukin (IL) -1α, IL-1β, IL-5, IL-6, IL-8, IL-12, IL-13, tumor necrosis factor-alpha (TNF-α), and tumor growth factor- beta1(TGF-β1). Reference Balali-Mood and Hefazi27-Reference Emad and Emad29
At the molecular level, SM releases cytokines, prostaglandins, matrix metalloproteinases, and serine proteinases Reference Kehe, Balszuweit and Emmler30 (Figure 1).
Cellular immune suppression was reported in Iranian survivors 1, 2, and 3 years after SM exposure. Natural killer cells, an important component of cellular immunity, were significantly lower in patients suffering from severe respiratory complications 10 years as well as 16 to 20 years after exposure to SM. Reference Ghotbi and Hassan31-Reference Zandieh, Marzban and Hassiri33
In another study, 7 specimens of lung biopsies were examined with an electron microscope at the WHO Research Center in Japan. Abnormal findings included proliferation, desquamation, and degeneration of the bronchial epithelial cells; interstitial fibrosis or fibrosing alveolitis; and an increased alveolar epithelial type I and type II cells as well as hyperplasia of ciliated and goblet cells. Reference Sohrabpour34
One possible mechanism of lung injury with SM is the pulmonary renin-angiotensin system, which plays a role in the development of inflammatory and fibrotic responses of the lung. Reference Hosseini-khalili, Thompson and Kehoe35 Increased alveolar epithelial type I and type II cells have also been reported as abnormal findings in lung biopsy of SM-exposed. Reference Sohrabpour34 According to the findings of these studies, overexpression of alveolar epithelial type II cells (AECII) expressing a large amount of angiotensin-converting enzyme II (ACE2) in Iranian survivors of mustard gas exposure, make them a vulnerable and susceptible host for SARS-CoV-2 (Figure 1).
PATHOGENESIS OF SARS-CoV-2
The prerequisite for entry of SARS-CoV-2 into the host cell is for the virus to bind to its specific receptor on the cell surface. This binding is mediated by the transmembrane spike glycoprotein (S) that forms homotrimers and protrudes from the viral surface. Spike can be broken down by proteases into an S1 subunit (containing the receptor-binding domain [RBD] and responsible for binding to the host cell receptor) and an S2 subunit (responsible for fusion of viral and cell membranes). Reference Walls, Park and Tortorici36 Compared with other coronavirus proteins, the spike structural protein has the most variable amino acid sequence, which is the strongest option among all the coronavirus structural and nonstructural proteins to adapt to their hosts. Reference Hu, Zeng and Yang37
Like SARS-CoV, the SARS-CoV-2 spike protein has a strong affinity for human ACE2, based on biochemical interaction studies and crystal structure analysis. Reference Li, Li and Farzan38 It has also been directly shown that SARS-CoV-2 uses ACE2 as a cell entry receptor. It has been reported that residue 394 (glutamine) at RBD of SARS-CoV-2 can be recognized by lysine 31 on the human ACE2 receptor. Reference Wan, Shang and Graham39
After binding of the SARS-CoV-2 spike protein to ACE2, the spike protein is broken down via acid-dependent proteolysis by cathepsin, transmembrane protease serine 2 (TMPRSS2), or proteases furin. Consequently, the viral envelope merges with the cell membranes, allowing the virus to enter the host cell. ACE2 also plays a role in virus replication and spread in the host cell. Reference Hoffmann, Kleine-Weber and Krüger40,Reference Iwata-Yoshikawa, Okamura, Shimizu, Hasegawa, Takeda and Nagata41
In the normal human lung, ACE2 is mostly expressed on the surface of type I and II alveolar epithelial cells (AECI and AECII, respectively. In fact, 83% of ACE2-expressing cells are AECII, indicating that these cells can act as a reservoir for viral invasion.
Gene enrichment ontology analysis has shown that ACE2-expressing AECII have high levels of multiple viral process-related genes, including regulatory genes for viral processes, viral life cycle, viral assembly, and viral genome replication. These findings indicate that ACE2-expressing AECII facilitates the replication and spread of SARS-CoV-2 in the lung. Reference Zhao, Zhao, Wang, Zhou, Ma and Zuo42
Binding SARS-CoV-2 to ACE2 leads to overexpression of ACE2, that can damage alveolar cells, mostly due to increased inflammatory immune responses and cytokine storm leading to increased immune cell infiltration in the alveoli along with alveolar epithelial type II cells apoptosis. The damage to alveolar cells can, in turn, trigger a series of systemic reactions and even death. Notably, having a large area makes the lung highly susceptible to inhaled viruses, making it the most vulnerable target organ against SARS-CoV-2. Reference Wrapp, Wang, Corbett, Goldsmith, Hsieh, Abiona, Graham and McLellan43,Reference Zhang, Penninger and Li44
The latest report indicates the infection of SARS-CoV-2 increases the expression levels of multiple proinflammatory cytokines, including interferon-gamma (IFN-γ), TNF-α, CCL2, and IL-6 in the serum, which suggests the inflammation storm may be involved in pulmonary inflammation in COVID-19. These results suggest that the excess immune cells migrating into lung tissue may cause an uncontrolled immune response, leading to the inflammation storm, and aggravated disease. Reference Huang, Wang and Li45
Recent findings revealed that cluster of differentiation 147 (CD147) is a novel identified receptor for SARS-CoV-2 infection in binding with the spike protein. CD147 is a type I transmembrane glycoprotein expressed on epithelial cells. The glycoprotein is also highly expressed on activated T cells, which may facilitate the invasion of SARS-CoV-2 to lymphocytes by binding spike protein, suggesting that CD147 may be involved in lymphocytopenia. CD147 is also presented in activated inflammatory cells and participates in the regulation of cytokine secretion and leukocytes chemotaxis by binding with cyclophilin A (CyPA). CyPA is a proinflammatory cytokine that is up-regulated in response to virus infection. Reference Huang, Wang and Li45-Reference Li, Geng and Peng51
LETHAL RISK OF SARS-COV-2 FOR SM-EXPOSED SURVIVORS
In SM-exposed survivors, in addition to producing free and active radicals and inducing oxidative stress, as well as impaired cellular and humoral immune function, and increased production of inflammatory cytokines and chemokines (cytokine storm) that damage the lungs, the AECI and AECII increase in number in the lung. It has been shown that lymphopenia, increased neutrophils, and increased levels of acute phase proteins such as C-reactive protein (CRP) are the most important laboratory findings in people with Covid-19. Reference Hoffmann, Kleine-Weber and Krüger40,Reference Wang, Chen and Zhou46 It has been previously mentioned that AECII express ACE2, and this makes them suitable hosts for SARS-CoV-2 that play an important role in virus entry and proliferation. Therefore, due to the increased number of AECII and the overexpression of ACE2 receptor induced by SM in SM-exposed survivors, these cells are more likely to be infected by SARS-Cov-2 and also more likely to have pulmonary complications and death (Figure 1).
CONCLUSIONS
As described above, it is predicted that, in SM-exposed survivors, the respiratory and pulmonary clinical manifestations of COVID-19 will be more severe and have a shorter incubation period (from infection to clinical presentation), making SARS-CoV-2 more lethal in SM-exposed survivors. Therefore, it is suggested that more rigorous principles of infection prevention and control and special measures, such as isolation, should also be considered for SM-exposed survivors in hospitals. SM-exposed survivors must be more committed to the principles of health and adherence to home quarantine than others, because SM exposed survivors infected with COVID-19, have a much lower chance of surviving the associated respiratory and pulmonary symptoms.
Acknowledgments
The authors thank the Clinical Research Development Unit of Baqiyatallah Hospital, Tehran, Iran. Also special thanks to Jennifer Swann for English editing.
Authors’ contributions
G.F., S.R.H.Z., and H.K. wrote the manuscript. M.G., G.A., A.J.F., and A.S. provided advice in the design and comments for improvement. Figure 1 is designed by H.K. All authors read and approved the final manuscript.
Competing interests
The authors declare that they have no competing interests.