Roska A K, Johnson A R, Lipsky P E
J Immunol. 1984 Jan;132(1):136-45.
The possibility that vascular endothelial cells (EC), like macrophages (M phi), can function as accessory cells necessary for mitogen- and antigen-induced T cell activation was examined. EC were enzymatically detached from the luminal surfaces of guinea pig aortas and then propagated in culture. Lymph node T lymphocytes were rigorously depleted of adherent cells, such that they completely lost the capacity to respond to mitogenic stimulation with phytohemagglutinin or concanavalin A. In this system, EC restored mitogen-induced T cell DNA synthesis as effectively as did M phi. This effect could not be explained by a facilitation of residual accessory cell activity within the responding T cell population, because EC restored mitogen responsiveness to T cells that had been treated with anti-Ia antibody and complement. Support of mitogen responsiveness could not be accounted for by secreted products of M phi or EC in the absence of intact accessory cells. In addition to the capacity to serve as fully sufficient accessory cells for the induction of mitogen-stimulated T cell proliferation, EC exerted a number of modulatory influences on T lymphocyte responses in cultures supported by M phi. When such cultures were supplemented with small numbers of EC, responses were dramatically augmented; larger numbers of EC resulted in marked suppression. At least part of these immunomodulatory effects could be accounted for by the activity of secreted products of EC. EC did not express detectable Ia antigens assayed either by indirect immunofluorescence, with the use of the fluorescence-activated cell sorter, or by complement-mediated cytotoxicity. Moreover, treating the EC population with anti-Ia antibody and complement had no effect on its capacity to support mitogen-induced T cell DNA synthesis. As would be expected from the lack of Ia antigen expression, EC were incapable of presenting antigen to primed T cells. They did, however, carry enough antigen into the cultures such that effective antigen presentation could occur when the cultures were supplemented with M phi that were syngeneic but not allogeneic to the responding T cells. Moreover, EC were capable of dramatically augmenting antigen-specific responses stimulated by antigen-pulsed M phi. There was no genetic restriction for this EC-mediated augmentation of antigen responsiveness. These results indicate that EC are capable of functioning as completely sufficient accessory cells for mitogen-induced T cell DNA synthesis and, in addition, are able to modulate ongoing M phi-supported T lymphocyte responses in both a positive and negative manner.(ABSTRACT TRUNCATED AT 400 WORDS)
研究了血管内皮细胞(EC)是否像巨噬细胞(M phi)一样,能够作为丝裂原和抗原诱导的T细胞活化所必需的辅助细胞发挥作用。通过酶解法从豚鼠主动脉腔表面分离出EC,然后在培养中进行增殖。严格去除淋巴结T淋巴细胞中的贴壁细胞,使其完全丧失对植物血凝素或刀豆球蛋白A的丝裂原刺激产生反应的能力。在该系统中,EC恢复丝裂原诱导的T细胞DNA合成的效果与M phi一样有效。这种效应不能用反应性T细胞群体中残余辅助细胞活性的促进来解释,因为EC恢复了抗Ia抗体和补体处理过的T细胞对丝裂原的反应性。在没有完整辅助细胞的情况下,M phi或EC的分泌产物无法解释对丝裂原反应性的支持。除了能够作为诱导丝裂原刺激的T细胞增殖的完全充足的辅助细胞外,EC对M phi支持的培养物中的T淋巴细胞反应还发挥了多种调节作用。当向此类培养物中添加少量EC时,反应会显著增强;大量EC则导致明显抑制。这些免疫调节作用至少部分可由EC分泌产物的活性来解释。通过间接免疫荧光法、使用荧光激活细胞分选仪或补体介导的细胞毒性检测,EC均未表达可检测到的Ia抗原。此外,用抗Ia抗体和补体处理EC群体对其支持丝裂原诱导的T细胞DNA合成的能力没有影响。正如缺乏Ia抗原表达所预期的那样,EC无法将抗原呈递给致敏T细胞。然而,它们确实将足够的抗原带入培养物中,使得当培养物中添加与反应性T细胞同基因而非异基因的M phi时,能够发生有效的抗原呈递。此外,EC能够显著增强由抗原脉冲处理的M phi刺激的抗原特异性反应。这种EC介导的抗原反应性增强不存在遗传限制。这些结果表明,EC能够作为丝裂原诱导的T细胞DNA合成的完全充足的辅助细胞发挥作用,此外,还能够以正负两种方式调节正在进行的M phi支持的T淋巴细胞反应。(摘要截短至400字)
