首页> 美国卫生研究院文献>Immunology >Characterization of suppressor cells in anterior chamber-associated immune deviation (ACAID) induced by soluble antigen. Evidence of two functionally and phenotypically distinct T-suppressor cell populations.
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Characterization of suppressor cells in anterior chamber-associated immune deviation (ACAID) induced by soluble antigen. Evidence of two functionally and phenotypically distinct T-suppressor cell populations.

机译:可溶性抗原诱导的前房相关免疫偏差(ACAID)中抑制细胞的表征。两个功能和表型上不同的T抑制细胞群体的证据。

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摘要

A large body of information exists describing the inability of animals receiving inoculations of antigen either intravenously (i.v.) or via the anterior chamber of the eye (AC) to mount delayed hypersensitivity (DH) responses to the injected antigen. Evidence indicates that the deviant humoral and cellular immunity that follows AC and i.v. inoculations of antigen is mediated, in part, by active suppression. Because of these similarities, it has been argued that immune deviation resulting from the AC inoculation [anterior chamber-associated immune deviation (ACAID)] of antigen represents nothing more than deviant immune responses known to be induced by the i.v. inoculation of antigens. Since circumstantial evidence suggests that AC injections may have unique immune effects, we wished to test the hypothesis that AC exposure to antigen elicits a unique form of systemic immune regulation. We have studied and compared the functional and phenotypic properties of suppressor cell populations induced by AC and i.v. inoculations of a soluble antigen, bovine serum albumin (BSA). Results indicate that AC inoculations of BSA (but not i.v. inoculations) activate antigen-specific. CD8+, I-J+ T lymphocytes which suppress the expression of DH responses, i.e. efferent suppression. We further report that AC and i.v. injection routes both activate antigen-specific afferent suppressor cell populations which impair the inductive phase of the immune response. However, the i.v.-induced afferent suppressor cells are CD8+ I-J+, whereas the AC-induced afferent suppressor cells are CD4+. We conclude that AC and i.v. exposures to soluble antigens are not immunologically equivalent, and that ACAID represents a uniquely regulated systemic immune response to intraocular antigens.
机译:存在大量信息,描述了动物无法通过静脉内(i.v.)或通过眼前房(AC)接受抗原接种而对注射的抗原产生迟发型超敏反应(DH)。证据表明,AC和i.v.之后出现了异常的体液和细胞免疫。抗原的接种部分地由主动抑制介导。由于这些相似性,已经提出由抗原的AC接种[前房相关免疫偏差(ACAID)]引起的免疫偏差仅代表已知由静脉内诱导的异常免疫应答。接种抗原。由于间接证据表明AC注射液可能具有独特的免疫作用,因此我们希望检验以下假设,即AC暴露于抗原会引起系统免疫调节的独特形式。我们已经研究并比较了由AC和i.v诱导的抑制细胞群的功能和表型特性。接种可溶性抗原牛血清白蛋白(BSA)。结果表明,BSA的AC接种(但不是静脉内接种)激活抗原特异性。抑制DH反应表达的CD8 +,I-J + T淋巴细胞,即传出抑制。我们进一步报告AC和i.v.注射途径均激活了抗原特异性传入抑制细胞群,这削弱了免疫反应的诱导期。然而,静脉内诱导的传入抑制细胞为CD8 + I-J +,而交流电诱导的传入抑制细胞为CD4 +。我们得出结论,AC和i.v.可溶性抗原的暴露在免疫学上是不等同的,并且ACAID代表对眼内抗原的独特调节的全身免疫应答。

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