TY - JOUR
T1 - Cutaneous injury by topical T-2 toxin
T2 - Involvement of microvessels and mast cells
AU - Yarom, R.
AU - Bergmann, F.
AU - Yagen, B.
PY - 1987
Y1 - 1987
N2 - Topical applications of various doses of T-2 toxin to rats led to delayed skin reactions. Following a dose-dependent latent period of 12 - 24 hr, there appeared vascular dilatation, stasis, edema and mononuclear cell infiltration, with many degranulating mast cells. These signs were earliest and strongest in the subcutis. Epidermal necrosis occurred 1 - 2 days later and was probably caused secondarily by ischemia, due to microcirculatory failure. Ultrastructurally, endothelial cells of small vessels were the earliest sites of change. While intercellular junctions remained closed and pinocytosis decreased, the cytoplasm contained many ribosomes, vacuoles, and abnormal mitochondria. Another early effect of topical T-2 toxin was an increase in number and degranulation of mast cells, especially in the subcutis. The resemblance of the skin injury to that produced by irradiation is noted.
AB - Topical applications of various doses of T-2 toxin to rats led to delayed skin reactions. Following a dose-dependent latent period of 12 - 24 hr, there appeared vascular dilatation, stasis, edema and mononuclear cell infiltration, with many degranulating mast cells. These signs were earliest and strongest in the subcutis. Epidermal necrosis occurred 1 - 2 days later and was probably caused secondarily by ischemia, due to microcirculatory failure. Ultrastructurally, endothelial cells of small vessels were the earliest sites of change. While intercellular junctions remained closed and pinocytosis decreased, the cytoplasm contained many ribosomes, vacuoles, and abnormal mitochondria. Another early effect of topical T-2 toxin was an increase in number and degranulation of mast cells, especially in the subcutis. The resemblance of the skin injury to that produced by irradiation is noted.
UR - http://www.scopus.com/inward/record.url?scp=0023156267&partnerID=8YFLogxK
U2 - 10.1016/0041-0101(87)90238-8
DO - 10.1016/0041-0101(87)90238-8
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C2 - 3576633
AN - SCOPUS:0023156267
SN - 0041-0101
VL - 25
SP - 167
EP - 174
JO - Toxicon
JF - Toxicon
IS - 2
ER -