Molecular and cellular mechanism of lung injuries due to exposure to sulfur mustard: a review

Ghanei, Mostafa; Harandi, Ali Amini

doi:10.3109/08958378.2011.576278

Cited by 73 publications

(51 citation statements)

References 117 publications

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“…The catalytic antioxidant treatment significantly attenuated SM-mediated increases in TNF-a, IL-6, KC/GRO, and IL-1b at 24 h. Transforming growth factor b1 (TGFb1) is commonly associated with lung injury and repair responses (Liu, 2008;Tatler and Jenkins, 2012). TGFb1 has been implicated in the development of pulmonary fibrosis in chronic models of SM exposure (Aghanouri et al, 2004;Emad and Emad, 2007;Ghanei and Harandi, 2011;Poursaleh et al, 2012). SM exposure significantly increased BALF TGFb1 levels nearly 10-fold over Sham PBS at 24 h post-exposure (Fig.…”

Section: Resultsmentioning

confidence: 99%

“…Inhaled SM may cause death or the development of severe chronic airway disorders in survivors (Poursaleh et al, 2012). Inhaled SM causes acute sloughing of the epithelial surfaces, formation of occlusive casts, and can lead to chronic respiratory problems such as bronchiolitis obliterans and COPD (Ghanei and Harandi, 2011;Veress et al, 2013). A hindrance in developing treatments for SM inhalation is due to our poor understanding of its pathogenesis.…”

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confidence: 99%

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From the Cover: Catalytic Antioxidant Rescue of Inhaled Sulfur Mustard Toxicity

et al. 2016

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Sulfur mustard (bis 2-chloroethyl ethyl sulfide, SM) is a powerful bi-functional vesicating chemical warfare agent. SM tissue injury is partially mediated by the overproduction of reactive oxygen species resulting in oxidative stress. We hypothesized that using a catalytic antioxidant (AEOL 10150) to alleviate oxidative stress and secondary inflammation following exposure to SM would attenuate the toxic effects of SM inhalation. Adult male rats were intubated and exposed to SM (1.4 mg/kg), a dose that produces an LD 50 at approximately 24 h. Rats were randomized and treated via subcutaneous injection with either sterile PBS or AEOL 10150 (5 mg/kg, sc, every 4 h) beginning 1 h post-SM exposure. Rats were euthanized between 6 and 48 h after exposure to SM and survival and markers of injury were determined. Catalytic antioxidant treatment improved survival after SM inhalation in a dose-dependent manner, up to 52% over SM PBS at 48 h post-exposure. This improvement was sustained for at least 72 h after SM exposure when treatments were stopped after 48 h. Non-invasive monitoring throughout the duration of the studies also revealed blood oxygen saturations were improved by 10% and clinical scores were reduced by 57% after SM exposure in the catalytic antioxidant treatment group. Tissue analysis showed catalytic antioxidant therapy was able to decrease airway cast formation by 69% at 48 h post-exposure. To investigate antioxidant induced changes at the peak of injury, several biomarkers of oxidative stress and inflammation were evaluated at 24 h post-exposure. AEOL 10150 attenuated SM-mediated lung lipid oxidation, nitrosative stress and many proinflammatory cytokines. The findings indicate that catalytic antioxidants may be useful medical countermeasure against inhaled SM exposure.Key words: sulfur mustard; chemical weapons; antioxidant.Sulfur mustard (SM) is a chemical warfare agent possessing strong alkylating properties that induces inflammation and tissue necrosis. SM exposure produces delayed and highly incapacitating injuries that can be lethal (Anderson, 2015). SM was used during World War I and is still maintained in the chemical weapons arsenals of several countries (Kehe and Szinicz, 2005). A specific and effective antidote is not available for use after SM exposure despite research conducted for nearly 100 years (Kehe and Szinicz, 2005). The population most at risk for exposure to SM is comprised of soldiers and individuals working or living near storage depots, but SM is also considered to be a potential terrorist threat due to its low cost of production and simple synthesis.Sulfur mustard (SM) vapor adversely affects the skin, eyes, and the respiratory tract. The respiratory tract is highly

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Section: Resultsmentioning

confidence: 99%

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confidence: 99%

From the Cover: Catalytic Antioxidant Rescue of Inhaled Sulfur Mustard Toxicity

et al. 2016

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“…It seems that late toxic effects of SM are more important and more serious than the acute effects (37). There are cellular and molecular evidences that support the late systemic impacts of SM.…”

Section: Biochemical and Laboratory Findingsmentioning

confidence: 99%

“…It has also been documented that COPD, as a form of local airway inflammation, releases inflammatory mediators into the systemic circulation and may contribute to an increase in cardiovascular disorders in these patients (42). Furthermore, it was recommended that TGF-β plays a significant role in the progression and development of both coronary atherosclerosis (43) and SM lung injury (37).…”

Section: Biochemical and Laboratory Findingsmentioning

confidence: 99%

“…When antioxidant supply is not sufficient (such as in SM injured patients, in whom the oxidative stressantioxidants balance is disturbed), the oxidative stress can damage the cardiovascular tissue more freely and effectively than in normal people (37). Therefore, although a definite heart toxicity of SM has not yet been explained, these patients have more predisposing factors (in terms of genomics, proteomics and metabolomics) to cardiovascular diseases, especially CAD.…”

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Sulfur Mustard Exposure and Cardiovascular Effects: A Review

Karbasi-Afshar¹,

Mohammadifard²,

Azdaki³

et al. 2016

Trauma Mon

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Sulfur mustard (SM) has been used as a chemical weapon in some conflicts, and many veterans and civilians have been injured thereby. Pulmonary, cutaneous, and ocular effects of SM have been frequently reported, although it seems that other organs such as the cardiovascular system are probably also affected. There are a number of studies evaluating the cardiovascular impacts of SM. However, these are dispersed and unfocused. In this paper, these studies have been reviewed to draw conclusions about the cardiovascular effects of SM. It seems that there is a probable relationship between SM exposure and cardiovascular toxicity in the long term. It appears that coronary artery diseases especially coronary ectasia and diastolic dysfunction are among the significant cardiovascular abnormalities frequently seen in these patients. Abnormal coronary arteries may occur due to direct endothelial injury by SM, sustained inflammatory status in patients with chronic lung disease, and abnormal mediators of tissue injury and repair or oxidative stressors.

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TGF‐β and Th17 cells related injuries in patients with sulfur mustard exposure

Panahi

Ghanei

Hassani

et al. 2017

Journal Cellular Physiology

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Sulfur mustard (SM) is a vesicating agent that has been employed as a chemical warfare agent. High-dose exposure to sulfur mustard may lead to the damage of rapidly proliferating cells of bone marrow and, therefore, suppression of the immune system. This may be continued as dysfunction of the immune system, and ultimately result in secondary immune disorders. Studies have suggested a role for T cells in SM-induced lung injury. Moreover, observations from animal studies indicate a delayed-type hypersensitivity (DTH) response after skin exposure to SM, providing an understanding that SM can stimulate specific T cell-mediated immune responses. On the other hand, T helper (Th) 17 cells, which are a subset of CD4+ T cells, have recently been reported to be involved in a number of inflammatory, autoimmune, and chronic fibrotic lung diseases. Furthermore, a strong association has been established between the overproduction of profibrotic cytokines like transforming growth factor (TGF)-β and Th17 cell number. In this review, we aimed to go through the new findings about the involvement and interactions of TGF-β and Th17 in SM-related injuries.

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Molecular and cellular mechanism of lung injuries due to exposure to sulfur mustard: a review

Cited by 73 publications

References 117 publications

From the Cover: Catalytic Antioxidant Rescue of Inhaled Sulfur Mustard Toxicity

From the Cover: Catalytic Antioxidant Rescue of Inhaled Sulfur Mustard Toxicity

Sulfur Mustard Exposure and Cardiovascular Effects: A Review

TGF‐β and Th17 cells related injuries in patients with sulfur mustard exposure

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