Abstract

A paucity of clinically applicable biomarkers to screen therapies in laboratory is a limitation in the development of countermeasures against cutaneous injuries by chemical weapon, sulfur mustard (SM), and its analog nitrogen mustard (NM). Consequently, we assessed NM-caused progression of clinical cutaneous lesions; notably, skin injury with NM is comparable to SM. Exposure of SKH-1 hairless and C57BL/6 (haired) mice to NM (3.2 mg) for 12–120 h caused clinical sequelae of toxicity, including microblister formation, edema, erythema, altered pigmentation, wounding, xerosis and scaly dry skin. These toxic effects of NM were similar in both mouse strains, except that wounding and altered pigmentation at 12–24 h and appearance of dry skin at 24 and 72 h post-NM exposure were more pronounced in C57BL/6 compared to SKH-1 mice. Conversely, edema, erythema and microblister formation were more prominent in SKH-1 than C57BL/6 mice at 24–72 h after NM exposure. In addition, 40–60% mortality was observed following 120 h of NM exposure in the both mouse strains. Overall, these toxic effects of NM are comparable to those reported in humans and other animal species with SM, and thus represent clinically-relevant cutaneous injury endpoints in screening and optimization of therapies for skin injuries by vesicating agents.

Highlights

  • Among its multi-organ effects, one of the major concerns regarding exposure to chemical warfare agent, sulfur mustard (SM), is its toxic and inflammatory effects in skin, with delayed vesication in exposed regions [1,2,3,4,5]

  • The present study reports the effects of nitrogen mustard (NM) exposure in both hairless SKH-1 and haired C57BL/6 mice, and identifies clinically relevant skin lesions, which were characterized during injury progression and quantitatively scored for the first time

  • Following NM exposure, comparable skin injury lesions were observed in both mouse strains; there were slight differences in their appearance and progression with time from 12–120 h post-NM exposure as shown in representative illustrations (Fig. 1, Table 1)

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Summary

Introduction

Among its multi-organ effects, one of the major concerns regarding exposure to chemical warfare agent, sulfur mustard (SM), is its toxic and inflammatory effects in skin, with delayed vesication in exposed regions [1,2,3,4,5]. Acute effects of SM on human skin occurring within 2–24 h include edema, erythema, blister, and bullae formation. The latter can burst and form a necrotic layer or eschar on the skin surface. Blistering and necrosis of skin could lead to long-term effects. Additional residual effects can include acne, cherry angiomas, scars, and chronic dermatitis [6,11,12,14,15]. These potentially debilitating effects can persist for many years

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