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六氯苯诱导的免疫调节及皮肤和肺部病变:棕色挪威大鼠、刘易斯大鼠和Wistar大鼠之间的比较

Hexachlorobenzene-induced immunomodulation and skin and lung lesions: a comparison between brown Norway, Lewis, and Wistar rats.

作者信息

Michielsen C P, Bloksma N, Ultee A, van Mil F, Vos J G

机构信息

Faculty of Veterinary Medicine, Utrecht, The Netherlands.

出版信息

Toxicol Appl Pharmacol. 1997 May;144(1):12-26. doi: 10.1006/taap.1997.8104.

Abstract

Strain dependence of the induction of skin and lung lesions by hexachlorobenzene (HCB) in the rat was studied to further the insight into the etiology of the lesions. To this end, 3- to 4-week-old female Brown Norway (BN), Lewis, and Wistar rats received diets supplemented with 150 mg (BN and Lewis), 450 mg (BN, Lewis, and Wistar) or 900 mg (BN and Wistar) HCB per kilogram diet for 4 weeks. Gross skin lesion development during exposure as well as pathologic changes in skin and lungs and various parameters of immunomodulation after exposure were assessed. General toxicity as judged by a slight increase in body weight gain and induction of liver cell hypertrophy was similar in BN and Lewis rats exposed to 450 mg/kg HCB and in Wistar rats exposed to 900 mg/kg HCB. Skin lesions ranged from redness to large exudating sores with crusts. With regard to dose, time of onset, incidence, and severity, skin lesions were very severe in BN, moderate in Lewis, and negligible in Wistar. Porphyrins could not be detected in the skin, whereas porphyrins in the liver were seen only in Lewis rats. Histology showed epidermal hyperplasia, deep dermal venules with activated endothelium, and deep dermal inflammatory infiltrates mainly consisting of eosinophilic granulocytes in BN and of mononuclear cells in Lewis and Wistar. Nonlesional skin of HCB-exposed rats showed very similar, though less prominent, changes. Lung pathology appeared negligibly strain-dependent; histology showed venules with an activated endothelium surrounded by a perivascular infiltrate as well as focal alveolar macrophage accumulations in all strains. Parameters of immunomodulation showed moderate strain dependence; relative spleen weights were dose-dependently increased in BN and Wistar and in the 450 mg/kg group in Lewis rats. BN rats showed a more marked splenomegaly than the other strains. Relative popliteal lymph node weights were increased significantly in BN and Lewis rats exposed to 450 mg/kg HCB. In all strains, HCB increased lymph node HEVs. Serum IgE and IgG levels were increased significantly in a dose-dependent way in BN rats only. Total serum IgM levels were elevated significantly in BN, Lewis, and Wistar rats that received 450 mg/kg and in Wistar rats that received 900 mg/kg HCB. Serum IgM levels against ssDNA were dose-dependently increased in all strains, being more marked in BN and Lewis than in Wistar rats. It is concluded that the HCB-induced inflammatory skin and lung pathologies have different etiology. Pronounced strain differences in the skin lesions suggest a specific involvement of the immune system. Skin lesions correlated significantly with all assessed parameters of immunomodulation in BN, with some in Lewis and with none in Wistar rats. No correlation was observed between the parameters of immunomodulation and lung lesions.

摘要

研究了大鼠中六氯苯(HCB)诱导皮肤和肺部病变的品系依赖性,以进一步深入了解这些病变的病因。为此,3至4周龄的雌性棕色挪威(BN)、刘易斯和Wistar大鼠接受了每千克饮食补充150毫克(BN和刘易斯)、450毫克(BN、刘易斯和Wistar)或900毫克(BN和Wistar)HCB的饮食,持续4周。评估了暴露期间的总体皮肤病变发展以及皮肤和肺部的病理变化以及暴露后的各种免疫调节参数。暴露于450毫克/千克HCB的BN和刘易斯大鼠以及暴露于900毫克/千克HCB的Wistar大鼠中,通过体重增加略有增加和肝细胞肥大的诱导判断的一般毒性相似。皮肤病变范围从发红到带有结痂的大渗出性溃疡。就剂量、发病时间、发病率和严重程度而言,BN中的皮肤病变非常严重,刘易斯中的为中度,Wistar中的可忽略不计。皮肤中未检测到卟啉,而肝脏中的卟啉仅在刘易斯大鼠中可见。组织学显示表皮增生、内皮细胞活化的真皮深层小静脉以及BN中主要由嗜酸性粒细胞组成、刘易斯和Wistar中由单核细胞组成的真皮深层炎性浸润。暴露于HCB的大鼠的非病变皮肤显示出非常相似但不太明显的变化。肺部病理显示出可忽略不计的品系依赖性;组织学显示所有品系中内皮细胞活化的小静脉周围有血管周围浸润以及局灶性肺泡巨噬细胞聚集。免疫调节参数显示出适度的品系依赖性;BN和Wistar以及刘易斯大鼠450毫克/千克组中的相对脾脏重量呈剂量依赖性增加。BN大鼠的脾肿大比其他品系更明显。暴露于450毫克/千克HCB的BN和刘易斯大鼠中,相对腘窝淋巴结重量显著增加。在所有品系中,HCB增加了淋巴结的高内皮微静脉。仅在BN大鼠中,血清IgE和IgG水平呈剂量依赖性显著增加。接受450毫克/千克的BN、刘易斯和Wistar大鼠以及接受900毫克/千克HCB的Wistar大鼠中,总血清IgM水平显著升高。所有品系中针对单链DNA的血清IgM水平呈剂量依赖性增加,BN和刘易斯中比Wistar大鼠更明显。结论是,HCB诱导的炎性皮肤和肺部病理具有不同的病因。皮肤病变中明显的品系差异表明免疫系统有特定参与。在BN中,皮肤病变与所有评估的免疫调节参数显著相关,在刘易斯中有一些相关,在Wistar大鼠中无相关。未观察到免疫调节参数与肺部病变之间的相关性。

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