Characterization of a hybridoma-derived T cell factor that promotes the production of antibodies bearing a dominant cross-reactive idiotype(s).

A M Wardzala, M B Bowen, G S Jendrisak, C J Bellone
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Abstract

The participation of postulated subsets of T helper cells in antigen-specific antibody responses has generated both interest and controversy among immunologists. Specifically the import as well as the very existence of multiple populations of T helper cells has led to an intense search in recent years for cloned lines of such subsets that permit unambiguous classification and study. Furthermore, the means by which some of these T cells induce antibody responses may be via the elaboration of soluble factors mandating their characterization both biochemically and mechanistically. We have recently reported the existence of a T helper factor present in a 24-h Con A supernatant that specifically enhances an idiotype-bearing (Id+) response to trinitrophenol (TNP). The unique biochemical properties of this substance, namely, its capacity to bind both antigen and cross-reactive idiotype (CRI), has led to the generation of a cloned T cell hybridoma that constitutively "secretes" a factor which appears identical to the helper activity in Con A Sn. The cloned T cell hybridoma, herein designated LOP 1.4, elaborates a factor which selectively enhances the CRI+ anti-TNP antibody response in vitro. The specificity of the assay employed as well as its sensitivity for detecting significant enhancement of the percent CRI+ anti-TNP PFC response lent itself well as a useful vehicle for subsequent characterization of the factor. The LOP 1.4 factor, which can act at the later stages of the B cell response in a dose-dependent fashion, was characterized by affinity chromatography in order to probe the mechanism of its selective Id enhancement. The factor binds both the idiotype and the ligand for which one of the idiotype-bearing monoclonal antibodies is specific. That the factor binds idiotype and can be eluted selectively with ligand but not with noncross-reacting ligand suggests that the factor possesses separate but not independent binding sites, or alternatively, a single binding site that preferentially binds to a unique composite of antigen-idiotype. In addition, the factor bears I-J determinants, consistent with what we have previously detected on the surface of TH2-like cells. These results, collectively, suggest that the T cell hybridoma LOP 1.4 is a TH2-like cell (supporting the concept of multiple TH subsets) in light of its ability to enhance an idiotypic response to specific antigen through the production of a soluble factor that demonstrates affinity for both antigen and idiotype. In addition, like the I-J+ TH2 cell, the LOP 1.4 factor also bears I-J region determinants.(ABSTRACT TRUNCATED AT 400 WORDS)

杂交瘤衍生的T细胞因子的特性,促进具有显性交叉反应独特型的抗体的产生。
辅助T细胞亚群参与抗原特异性抗体反应在免疫学家中引起了兴趣和争议。近年来,由于辅助性T细胞的大量存在和引入,人们对此类亚群的克隆细胞系进行了大量的研究,以便进行明确的分类和研究。此外,其中一些T细胞诱导抗体反应的手段可能是通过可溶性因子的细化,这些可溶性因子要求它们在生化和机械上进行表征。我们最近报道了一种T辅助因子存在于24小时Con a上清液中,该上清液特异性地增强了对三硝基苯酚(TNP)的独特型(Id+)反应。这种物质独特的生化特性,即它结合抗原和交叉反应独特型(CRI)的能力,导致克隆T细胞杂交瘤的产生,该杂交瘤组成性地“分泌”一种与Con a Sn中的辅助活性相同的因子。克隆的T细胞杂杂瘤,本文命名为LOP 1.4,阐述了一个体外选择性增强CRI+抗tnp抗体应答的因子。所采用的检测方法的特异性以及检测CRI+抗tnp PFC反应百分比显着增强的敏感性使其本身成为随后表征该因素的有用载体。lop1.4因子以剂量依赖性的方式作用于B细胞应答的后期阶段,通过亲和层析对其进行表征,以探讨其选择性Id增强的机制。该因子结合独特型和配体,其中一个携带独特型的单克隆抗体是特异性的。该因子结合独特型并且可以选择性地与配体洗脱,而不能与非交叉反应的配体洗脱,这表明该因子具有单独而非独立的结合位点,或者具有优先结合独特抗原独特型复合物的单一结合位点。此外,该因子具有I-J决定因子,这与我们之前在th2样细胞表面检测到的结果一致。这些结果共同表明,T细胞杂交瘤LOP 1.4是一种th2样细胞(支持多个TH亚群的概念),因为它能够通过产生一种可溶性因子来增强对特定抗原的独特型反应,这种可溶性因子对抗原和独特型都有亲和力。此外,与I-J+ TH2细胞一样,lop1.4因子也具有I-J区决定因子。(摘要删节为400字)
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