Topical efficacy of dimercapto-chelating agents against lewisite-induced skin lesions in SKH-1 hairless mice

Topical efficacy of dimercapto-chelating agents against lewisite-induced skin lesions in SKH-1 hairless mice

Lewisite is a potent chemical warfare arsenical vesicant that can cause severe skin lesions. Today, lewisite exposure remains possible during demilitarization of old ammunitions and as a result of deliberate use. Although its cutaneous toxicity is not fully elucidated, a specific antidote exists, th...

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Veröffentlicht in:Toxicology and applied pharmacology 2013-10, Vol.272 (2), p.291-298
Hauptverfasser: Mouret, Stéphane, Wartelle, Julien, Emorine, Sandy, Bertoni, Marine, Nguon, Nina, Cléry-Barraud, Cécile, Dorandeu, Frédéric, Boudry, Isabelle
Format: Artikel
Sprache:eng
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60 APPLIED LIFE SCIENCES
Administration, Topical
Animals
Arsenic Poisoning - etiology
Arsenic Poisoning - pathology
Arsenic Poisoning - prevention & control
Arsenicals - administration & dosage
Biological and medical sciences
British anti-lewisite (BAL)
Chelating Agents - administration & dosage
Chelating Agents - adverse effects
Chelating Agents - therapeutic use
CHEMICAL WARFARE
Dermatitis - etiology
Dermatitis - pathology
Dermatitis - prevention & control
DIMERCAPROL
Dimercaprol - administration & dosage
Dimercaprol - adverse effects
Dimercaprol - therapeutic use
Dimercaptosuccinic acid (DMSA)
HEAVY METALS
Injections, Subcutaneous
Lewisite
Male
Medical sciences
MICE
Mice, Hairless
NECROSIS
SIDE EFFECTS
SKIN
Skin lesion
Succimer - administration & dosage
Succimer - adverse effects
Succimer - therapeutic use
Topical application
TOXICITY
Toxicology
Treatment
VAPORS
Volatilization
WOUNDS
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Zusammenfassung:Lewisite is a potent chemical warfare arsenical vesicant that can cause severe skin lesions. Today, lewisite exposure remains possible during demilitarization of old ammunitions and as a result of deliberate use. Although its cutaneous toxicity is not fully elucidated, a specific antidote exists, the British anti-lewisite (BAL, dimercaprol) but it is not without untoward effects. Analogs of BAL, less toxic, have been developed such as meso-2,3-dimercaptosuccinic acid (DMSA) and have been employed for the treatment of heavy metal poisoning. However, efficacy of DMSA against lewisite-induced skin lesions remains to be determined in comparison with BAL. We have thus evaluated in this study the therapeutic efficacy of BAL and DMSA in two administration modes against skin lesions induced by lewisite vapor on SKH-1 hairless mice. Our data demonstrate a strong protective efficacy of topical application of dimercapto-chelating agents in contrast to a subcutaneous administration 1h after lewisite exposure, with attenuation of wound size, necrosis and impairment of skin barrier function. The histological evaluation also confirms the efficacy of topical application by showing that treatments were effective in reversing lewisite-induced neutrophil infiltration. This protective effect was associated with an epidermal hyperplasia. However, for all the parameters studied, BAL was more effective than DMSA in reducing lewisite-induced skin injury. Together, these findings support the use of a topical form of dimercaprol-chelating agent against lewisite-induced skin lesion within the first hour after exposure to increase the therapeutic management and that BAL, despite its side-effects, should not be abandoned. •Topically applied dimercapto-chelating agents reduce lewisite-induced skin damage.•One topical application of BAL or DMSA is sufficient to reverse lewisite effects.•Topical BAL is more effective than DMSA to counteract lewisite-induced skin damage.
ISSN:0041-008X
1096-0333
DOI:10.1016/j.taap.2013.06.012