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在没有Fas/Fas配体相互作用的情况下,向前房接种脾细胞引发迟发型超敏反应,而不是诱导前房相关免疫偏离。

Anterior chamber inoculation of splenocytes without Fas/Fas-ligand interaction primes for a delayed-type hypersensitivity response rather than inducing anterior chamber-associated immune deviation.

作者信息

Kawashima H, Yamagami S, Tsuru T, Gregerson D S

机构信息

Department of Ophthalmology, Jichi Medical School, Tochigi, Japan.

出版信息

Eur J Immunol. 1997 Oct;27(10):2490-4. doi: 10.1002/eji.1830271005.

Abstract

The inoculation of antigens into the anterior chamber (AC) of the eye induces an antigen-specific immune response that inhibits delayed-type hypersensitivity (DTH). This regulatory response is known as anterior chamber-associated immune deviation (ACAID). The ACAID response appears to be complex, as it can be elicited by a wide variety of soluble and cell-associated antigens, including foreign, self, tumor, and alloantigens. To evaluate the contribution of Fas/Fas ligand (FasL) interaction to the induction of ACAID to alloantigens, gld and lpr mutant mice were used in conjunction with normal C3H, MRL, and BALB/c mice. ACAID was induced by inoculation of non-irradiated splenocytes from donor mice into the AC of various recipients. After 1 week, recipients were primed intradermally with donor splenocytes. One week later DTH was measured by ear swelling. C3Hgld mutants lacking functional FasL did not develop ACAID after the AC inoculation of BALB/c splenocytes. Conversely, the AC inoculation sensitized these mutants. MRL/pr mutants, which lack Fas, developed ACAID following inoculation of BALB/c cells. AC inoculation of lpr splenocytes did not induce ACAID, but sensitized C3H recipients. Treatment of the AC inoculum with an anti-Fas antibody blocked ACAID induction in a transient manner, as the recipients developed ACAID later. These results show that interaction of the Fas and FasL is required to induce ACAID to allogeneic cells. In the absence of Fas expression on donor splenocytes, or FasL expression by the recipient, AC inoculation primes for a DTH response rather than inducing ACAID.

摘要

将抗原接种到眼的前房(AC)可诱导抗原特异性免疫反应,该反应可抑制迟发型超敏反应(DTH)。这种调节性反应被称为前房相关免疫偏离(ACAID)。ACAID反应似乎很复杂,因为它可由多种可溶性和细胞相关抗原引发,包括外来抗原、自身抗原、肿瘤抗原和同种异体抗原。为了评估Fas/Fas配体(FasL)相互作用对诱导针对同种异体抗原的ACAID的贡献,将gld和lpr突变小鼠与正常的C3H、MRL和BALB/c小鼠一起使用。通过将来自供体小鼠的未照射脾细胞接种到各种受体的AC中来诱导ACAID。1周后,受体经皮内注射供体脾细胞进行致敏。1周后通过耳部肿胀测量DTH。缺乏功能性FasL的C3Hgld突变体在接种BALB/c脾细胞至AC后未产生ACAID。相反,AC接种使这些突变体致敏。缺乏Fas的MRL/pr突变体在接种BALB/c细胞后产生了ACAID。接种lpr脾细胞至AC未诱导ACAID,但使C3H受体致敏。用抗Fas抗体处理AC接种物可短暂阻断ACAID的诱导,因为受体随后会产生ACAID。这些结果表明,Fas和FasL的相互作用是诱导针对同种异体细胞的ACAID所必需的。在供体脾细胞上缺乏Fas表达或受体缺乏FasL表达的情况下,AC接种引发DTH反应而非诱导ACAID。

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