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小鼠实验性变应性睾丸炎。VII. 引发主动和被动诱导疾病的无精子生成自身抗原的初步特征。

Experimental allergic orchitis in mice. VII. Preliminary characterization of the aspermatogenic autoantigens responsible for eliciting actively and passively induced disease.

作者信息

Teuscher C, Meeker N D, Livingstone K D, Sudweeks J D, Griffith J S, Wardell B B, Hickey W F

机构信息

Department of Microbiology, Brigham Young University, Provo, UT 84602.

出版信息

J Reprod Immunol. 1994 May;26(3):233-49. doi: 10.1016/0165-0378(94)90021-3.

Abstract

Experimental allergic orchitis (EAO) can be induced actively and passively in mice by either immunization with mouse testicular homogenate (MTH) in conjunction with the appropriate adjuvants or by transferring CD4+ T cells isolated from sensitized donors into non-immunized, naive recipients. The distribution of inflammatory lesions seen in active and passive EAO are markedly different. In active EAO maximal disease is observed in the seminiferous tubules, whereas in passive EAO lesions occur primarily in the straight tubules, rete testis, and ductus efferentes. These observations suggest that different immunopathogenic mechanisms and/or aspermatogenic autoantigens may be responsible for the distinct histopathologic profiles. Two murine testis-specific aspermatogenic autoantigens (mAP1 and mAP2) were partially purified from MT acetone powder by extraction in 7-M urea under reducing conditions, gel filtration, ion-exchange chromatography, and preparative isoelectric focusing from pH 3 to 10. In gel filtration on Sephacryl S-400 in 7-M urea, mAP1 is confined to the V0 peak, while mAP2 is in the major included peak. mAP1 has an isoelectric point of 4.4-4.9, is sensitive to both pronase and DNase but not RNase, and is active at a minimal dose of 250-500 micrograms (dry wt). Dose-response bioassays for active and passive EAO revealed that mAP1 preferentially elicits active disease, whereas mAP2 is most effective at eliciting passive disease. These results support the concept that the different histopathologic profiles seen in active and passive EAO are, in part, the result of different immunopathologic responses elicited by separate aspermatogenic autoantigens.

摘要

实验性变应性睾丸炎(EAO)可通过用小鼠睾丸匀浆(MTH)结合适当佐剂进行免疫,或通过将从致敏供体分离的CD4 + T细胞转移到未免疫的幼稚受体中,在小鼠中主动和被动诱导。在主动和被动EAO中观察到的炎性病变分布明显不同。在主动EAO中,在生精小管中观察到最大程度的病变,而在被动EAO中,病变主要发生在直小管、睾丸网和输出小管。这些观察结果表明,不同的免疫致病机制和/或生精自身抗原可能是导致不同组织病理学特征的原因。两种小鼠睾丸特异性生精自身抗原(mAP1和mAP2)通过在还原条件下用7-M尿素提取、凝胶过滤、离子交换色谱以及从pH 3至10的制备性等电聚焦,从MT丙酮粉末中部分纯化。在7-M尿素中于Sephacryl S-400上进行凝胶过滤时,mAP1局限于V0峰,而mAP2位于主要的包含峰中。mAP1的等电点为4.4 - 4.9,对链霉蛋白酶和脱氧核糖核酸酶敏感,但对核糖核酸酶不敏感,并且在最小剂量为250 - 500微克(干重)时具有活性。主动和被动EAO的剂量反应生物测定表明,mAP1优先引发主动疾病,而mAP2在引发被动疾病方面最有效。这些结果支持这样的概念,即在主动和被动EAO中看到的不同组织病理学特征部分是由单独的生精自身抗原引发的不同免疫病理反应的结果。

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