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小鼠主要组织相容性复合体转染的I类基因在L细胞中的表达。

Expression in L cells of transfected class I genes from the mouse major histocompatibility complex.

作者信息

Schepart B S, Woodward J G, Palmer M J, Macchi M J, Basta P, McLaughlin-Taylor E, Frelinger J A

出版信息

Proc Natl Acad Sci U S A. 1985 Aug;82(16):5505-9. doi: 10.1073/pnas.82.16.5505.

Abstract

One of the major surprises of the molecular analysis of major histocompatibility complex (MHC) genes is the large number of class I (K/D)-related sequences in the genome. Both restriction fragment length polymorphisms and cosmid cloning experiments showed them all to be closely linked to the MHC. Until now little information was available concerning either their expression or recognition by the immune system. Here we report that these non-K/D genes can provoke antibody responses and be recognized by cytolytic T cells. Immunization of C3H mice with L cells transfected with class I genomic clones resulted in antisera that reacted preferentially with cells from strain B10.P (the gene donor). Thus, these genes can be expressed by L cells. These products were recognized by cytolytic T cells produced by mixed lymphocyte culture with B10.P stimulators. One gene, represented in clone lambda 3a, was chosen for further analysis. A restriction fragment length polymorphism, detected between B10.P (KpDp) and B10.F(14R) (KbDp) and between B10 (KbDb) and B10.F(13R) (KpDb), has enabled us to map the lambda 3a sequence to the D or Tla region. Restriction endonuclease mapping of the lambda 3a clone shows that the gene is intact and that, although many restriction sites are conserved, the gene in lambda 3a differs from other class I genes. When the lambda 3a clone was transfected into mouse L cells, a new product was expressed. Cells expressing this product (designated L3a cells) were killed by primary D-end-reactive, allospecific cytolytic T lymphocytes. The L3a cells were unreactive with monoclonal antibodies specific for the Kp,Dp,Qa-2, Tla.3, and Tla.5 molecules.

摘要

主要组织相容性复合体(MHC)基因分子分析的一大意外发现是基因组中存在大量与I类(K/D)相关的序列。限制性片段长度多态性分析和黏粒克隆实验均表明,它们都与MHC紧密连锁。到目前为止,关于它们的表达或免疫系统的识别,几乎没有可用信息。在此我们报告,这些非K/D基因可引发抗体反应,并被细胞毒性T细胞识别。用转染了I类基因组克隆的L细胞免疫C3H小鼠,产生的抗血清优先与B10.P品系(基因供体)的细胞发生反应。因此,这些基因可由L细胞表达。这些产物可被与B10.P刺激细胞进行混合淋巴细胞培养产生的细胞毒性T细胞识别。选择克隆λ3a中代表的一个基因进行进一步分析。在B10.P(KpDp)与B10.F(14R)(KbDp)之间以及B10(KbDb)与B10.F(13R)(KpDb)之间检测到的限制性片段长度多态性,使我们能够将λ3a序列定位到D或Tla区域。λ3a克隆的限制性内切酶图谱显示该基因完整,尽管许多限制性位点是保守的,但λ3a中的基因与其他I类基因不同。当将λ3a克隆转染到小鼠L细胞中时,表达了一种新产物。表达该产物的细胞(称为L3a细胞)被原发性D端反应性、同种异体特异性细胞毒性T淋巴细胞杀伤。L3a细胞与针对Kp、Dp、Qa-2、Tla.3和Tla.5分子的单克隆抗体无反应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/64e9/391151/c8855b05be18/pnas00356-0279-a.jpg

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