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注入视网膜下间隙的抗原引发的免疫偏离分析。

Analysis of immune deviation elicited by antigens injected into the subretinal space.

作者信息

Wenkel H, Streilein J W

机构信息

Schepens Eye Research Institute, Department of Ophthalmology, Harvard Medical School, Boston, Massachusetts 02114, USA.

出版信息

Invest Ophthalmol Vis Sci. 1998 Sep;39(10):1823-34.

PMID:9727405
Abstract

PURPOSE

To determine whether the subretinal space supports the induction of deviant immune responses to cell-associated and soluble antigens and to elucidate factors influencing the immunologic properties of the subretinal space.

METHODS

P815 mastocytoma cells were used as cell-associated antigens and were inoculated into the anterior chamber (AC), the vitreous cavity (VC), the subretinal space, and subconjunctivally in H2-compatible, but minor H-incompatible, BALB/c mice. Ovalbumin, as a soluble antigen, was similarly injected into eyes, after which recipient animals were immunized with ovalbumin and complete Freund's adjuvant. Delayed-type hypersensitivity (DTH) was assessed by ear challenge. To alter the conditions in the subretinal space, the outer blood-retinal barrier was disrupted by compromising retinal pigment epithelial (RPE) cells with a systemic injection of sodium iodate. Immune privilege in the AC was abolished by mild corneal cauterization.

RESULTS

Antigen-specific DTH did not develop in mice in which alloantigenic tumor cells or ovalbumin was injected into the AC, the VC, or the subretinal space, and the mice's spleens contained lymphocytes capable of suppressing DTH when adoptively transferred into naive mice. When RPE cells were compromised with sodium iodate, tumor cells or ovalbumin injected into the subretinal space or the VC did not induce immune deviation, although the AC of these eyes still promoted AC-associated immune deviation. By contrast, when immune privilege in the AC was abolished by corneal cauterization, neither tumor cells nor ovalbumin injected into the subretinal space or the VC of eyes elicited immune deviation.

CONCLUSIONS

The subretinal space supports immune deviation for histoincompatible tumor cells and soluble protein antigens by actively suppressing antigen-specific DTH. Acute loss of immune privilege in the subretinal space and the VC does not cause loss of privilege in the AC, but abolition of immune privilege in the AC eliminates the capacity of the subretinal space and the VC to support immune deviation to antigens injected locally.

摘要

目的

确定视网膜下间隙是否支持对细胞相关抗原和可溶性抗原产生异常免疫反应,并阐明影响视网膜下间隙免疫特性的因素。

方法

将P815肥大细胞瘤细胞用作细胞相关抗原,接种到H2相容但次要H不相容的BALB/c小鼠的前房(AC)、玻璃体腔(VC)、视网膜下间隙和结膜下。将卵清蛋白作为可溶性抗原,同样注入眼内,之后用卵清蛋白和完全弗氏佐剂对受体动物进行免疫。通过耳部激发评估迟发型超敏反应(DTH)。为改变视网膜下间隙的条件,通过全身注射碘酸钠损害视网膜色素上皮(RPE)细胞来破坏外血视网膜屏障。通过轻度角膜烧灼消除AC中的免疫赦免。

结果

将同种异体肿瘤细胞或卵清蛋白注入AC、VC或视网膜下间隙的小鼠未发生抗原特异性DTH,并且这些小鼠的脾脏含有当被过继转移到未致敏小鼠时能够抑制DTH的淋巴细胞。当用碘酸钠损害RPE细胞时,注入视网膜下间隙或VC中的肿瘤细胞或卵清蛋白未诱导免疫偏离,尽管这些眼睛的AC仍促进AC相关的免疫偏离。相比之下,当通过角膜烧灼消除AC中的免疫赦免时,注入眼睛的视网膜下间隙或VC中的肿瘤细胞和卵清蛋白均未引发免疫偏离。

结论

视网膜下间隙通过积极抑制抗原特异性DTH来支持对组织不相容肿瘤细胞和可溶性蛋白抗原的免疫偏离。视网膜下间隙和VC中免疫赦免的急性丧失不会导致AC中免疫赦免的丧失,但AC中免疫赦免的消除会消除视网膜下间隙和VC支持对局部注射抗原产生免疫偏离的能力。

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