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T-2毒素诱导Wistar衍生的低毛量WBN/ILA-Ht大鼠出现急性皮肤损伤。

T-2 toxin-induced acute skin lesions in Wistar-derived hypotrichotic WBN/ILA-Ht rats.

作者信息

Albarenque S M, Shinozuka J, Iwamoto S, Nakayama H, Doi K

机构信息

Department of Veterinary Pathology, Faculty of Agriculture, University of Tokyo, Japan.

出版信息

Histol Histopathol. 1999 Apr;14(2):337-42. doi: 10.14670/HH-14.337.

Abstract

Acute lesions in the dorsal skin topically applied with T-2 toxin (10 microliters of 0.5 mg/ml-solution to 1 cm2) were examined in Wistar-derived hypotrichotic WBN/ILA-Ht rats up to 24 hours after treatment (24HAT). In the epidermis, depression of basal cell proliferating activity was detected at 3HAT by immunostaining for proliferating cell nuclear antigen (PCNA), and the percentage of PCNA-positive basal cells decreased thereafter. At 12HAT, in addition to intracytoplasmic edema of spinous cells, acidophilic degeneration of basal cells characterized by shrinkage of cell body with acidophilic cytoplasm and pyknotic or karyorrhectic nuclei became prominent. Most of these nuclei were positive for TUNEL which is a widely used immunostaining for the in situ detection of fragmented DNA, i.e. apoptosis, and the percentage of TUNEL-positive basal cells increased thereafter. The nuclei of these basal cells also showed ultrastructural changes characteristic for apoptosis. On the other hand, in the dermis, infiltration of inflammatory cells including mast cells started at 3HAT and increased thereafter. In addition, capillary and small vessel endothelial degeneration developed at 6HAT and progressed thereafter. These results suggest that T-2 toxin directly affects the epidermis and produces apoptosis in basal cells.

摘要

在经皮局部涂抹T-2毒素(每1平方厘米涂抹10微升0.5毫克/毫升溶液)的Wistar衍生低毛WBN/ILA-Ht大鼠中,观察处理后24小时(24HAT)内背部皮肤的急性损伤情况。在表皮,于处理后3小时(3HAT)通过增殖细胞核抗原(PCNA)免疫染色检测到基底细胞增殖活性降低,此后PCNA阳性基底细胞的百分比下降。在12HAT时,除棘细胞胞浆内水肿外,以细胞体收缩、胞浆嗜酸性变及核固缩或核溶解为特征的基底细胞嗜酸性变性变得明显。这些细胞核中的大多数对TUNEL呈阳性,TUNEL是一种广泛用于原位检测DNA片段化(即凋亡)的免疫染色方法,此后TUNEL阳性基底细胞的百分比增加。这些基底细胞的细胞核还显示出凋亡特征性的超微结构变化。另一方面,在真皮中,包括肥大细胞在内的炎性细胞浸润在3HAT时开始并随后增加。此外,毛细血管和小血管内皮变性在6HAT时出现并随后进展。这些结果表明,T-2毒素直接影响表皮并在基底细胞中产生凋亡。

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