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豚鼠皮下结膜移植的衣原体感染

Chlamydial infection of subcutaneous conjunctival transplants in guinea pigs.

作者信息

Pham R T, Sung M, Dawson C R, Schachter J

机构信息

Francis I. Proctor Foundation, University of California, San Francisco 94143-0412.

出版信息

Invest Ophthalmol Vis Sci. 1990 Jul;31(7):1367-73.

PMID:2365567
Abstract

The development and testing of candidate vaccines for trachoma are constrained because only humans and nonhuman primates are susceptible to conjunctival infection with Chlamydia trachomatis. Guinea pig inclusion conjunctivitis (GPIC), an analogous disease of guinea pigs, provides a useful, less expensive model to study ocular chlamydial infections. GPIC is caused by a Chlamydia psittaci strain whose external constituents are very similar to those of C. trachomatis. To develop a better model for studying GPIC immunity, conjunctival pockets were established under the abdominal skin of guinea pigs by subcutaneous implantation. Up to six implants could be produced in each animal. The success rate of implantation was 79.0% (n = 148). These pockets were then infected with GPIC. The organism was recovered from the autografts indicating local replication, and tests for serum antibody by microimmunofluorescence showed production of GPIC-specific antibody of IgG and IgM classes after infection. There was minimal antibody response after moderate inoculating doses to the implants, and the titers increased more slowly than after eye infection with GPIC; with higher concentration of the inoculum, however, the antibody response increased to the same levels as with the ocular challenge but more slowly. Inoculation of pockets with GPIC also produced acute inflammatory changes in infected autografts (n = 101). Histologic examination of infected grafts showed chlamydial inclusions in epithelial cells and significant infiltration with lymphocytes and polymorphonuclear cells. Subcutaneous autografts may provide a useful model for chronologic studies of chlamydial infection. The delayed immunologic response, however, suggests that these pockets of implanted epithelium do not have full access to the immune system.

摘要

沙眼候选疫苗的研发和测试受到限制,因为只有人类和非人类灵长类动物易受沙眼衣原体结膜感染。豚鼠包涵体结膜炎(GPIC)是豚鼠的一种类似疾病,为研究眼部衣原体感染提供了一种有用且成本较低的模型。GPIC由一株鹦鹉热衣原体引起,其外部成分与沙眼衣原体非常相似。为了开发更好的研究GPIC免疫的模型,通过皮下植入在豚鼠腹部皮肤下建立结膜囊。每只动物最多可产生6个植入物。植入成功率为79.0%(n = 148)。然后用GPIC感染这些囊。从自体移植组织中回收了该病原体,表明其在局部复制,通过微量免疫荧光检测血清抗体显示感染后产生了IgG和IgM类的GPIC特异性抗体。中等接种剂量接种植入物后抗体反应最小,且滴度升高比眼部感染GPIC后更慢;然而,接种物浓度较高时,抗体反应升高到与眼部激发相同的水平,但更慢。用GPIC接种囊也在感染的自体移植组织中产生了急性炎症变化(n = 101)。对感染移植组织的组织学检查显示上皮细胞中有衣原体包涵体,并有淋巴细胞和多形核细胞的显著浸润。皮下自体移植可为衣原体感染的时间顺序研究提供有用的模型。然而,延迟的免疫反应表明这些植入上皮的囊不能完全接触免疫系统。

相似文献

1
Chlamydial infection of subcutaneous conjunctival transplants in guinea pigs.豚鼠皮下结膜移植的衣原体感染
Invest Ophthalmol Vis Sci. 1990 Jul;31(7):1367-73.
2
Serum and tear antibodies to Chlamydia after reinfection with guinea pig inclusion conjunctivitis agent.豚鼠包涵体结膜炎病原体再次感染后血清及泪液中抗衣原体抗体
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