Gollob J A, Li J, Reinherz E L, Ritz J
Division of Hematologic Malignancies, Dana-Farber Cancer Institute, Boston, Massachusetts 02115, USA.
J Exp Med. 1995 Sep 1;182(3):721-31. doi: 10.1084/jem.182.3.721.
Interleukin (IL) 12 is a 70-kD heterodimeric cytokine produced by antigen-presenting cells (APCs) such as macrophages in response to infectious pathogens and interferon (IFN) gamma. The varied immunomodulatory effects of IL-12 include the stimulation of proliferation and IFN-gamma production by T cells, and it also has a central role in the development of the T helper cell type 1 immune phenotype. We undertook the production of antibodies capable of modulating the response of T cells to IL-12, and in the process we discovered two antibodies that inhibited the ability of IL-12 to stimulate T cell proliferation. In this report, we demonstrate that these anti-bodies recognize CD2, and we show how antibodies directed toward either the adhesion domain of CD2 or its ligand, CD58, specifically inhibit IL-12 induced proliferation and IFN-gamma production by phytohemagglutinin-activated T cells, leaving the response to IL-12 unaffected. A three-to fourfold reduction in proliferation and IFN-gamma production was observed at IL-12 concentrations as high as 1 nM, with complete inhibition occurring at < or = 1 pM. This novel effect is not directly mediated at the level of the IL-12 receptor, as shown by the inability of these antibodies to block IL-12 binding to activated T cells. Furthermore, by using activating pairs of CD2 antibodies, we show that CD2 stimulation strongly synergizes with IL-12, even at 0.1 pM, in inducing both T cell proliferation and IFN-gamma production. Cytolytic T lymphocyte-associated antigen 4-immunoglobulin-mediated inhibition of the B7/CD28 interaction did not affect the T cell response to either IL-12 or IL-2, but the removal of APCs selectively diminished the proliferative response to IL-12. Based on this data, we hypothesize that CD2 has a central role in an IL-12/IFN-gamma positive feedback loop between T cell and APC, providing the key functional link via a CD2/CD58 interaction that controls T cell responsiveness to IL-12. This model provides a basis for future investigations aimed at defining the signaling mechanisms that mediate this cytokine-specific regulatory effect of CD2, and it offers insight into how a cytokine receptor and distinct adhesion molecule can interact to modulate responsiveness to that cytokine. In addition, it underscores the possibility that the clinical potential of an immunomodulatory drug like IL-12 may be governed by the presence or absence of specific costimulation.
白细胞介素(IL)-12是一种70-kD的异二聚体细胞因子,由抗原呈递细胞(APC)如巨噬细胞在对感染性病原体和干扰素(IFN)-γ作出反应时产生。IL-12具有多种免疫调节作用,包括刺激T细胞增殖和产生IFN-γ,并且在1型辅助性T细胞免疫表型的发育中也起着核心作用。我们致力于生产能够调节T细胞对IL-12反应的抗体,在此过程中我们发现了两种抑制IL-12刺激T细胞增殖能力的抗体。在本报告中,我们证明这些抗体识别CD2,并且我们展示了针对CD2的粘附结构域或其配体CD58的抗体如何特异性抑制植物血凝素激活的T细胞对IL-12诱导的增殖和IFN-γ产生,而对IL-12的反应不受影响。在高达1 nM的IL-12浓度下观察到增殖和IFN-γ产生减少三到四倍,在≤1 pM时完全抑制。这些抗体无法阻断IL-12与活化T细胞的结合,这表明这种新效应不是直接在IL-12受体水平介导的。此外,通过使用激活对的CD2抗体,我们表明CD2刺激即使在0.1 pM时也能与IL-12强烈协同作用,诱导T细胞增殖和IFN-γ产生。细胞毒性T淋巴细胞相关抗原4-免疫球蛋白介导的B7/CD28相互作用的抑制并不影响T细胞对IL-12或IL-2的反应,但去除APC选择性地降低了对IL-12的增殖反应。基于这些数据,我们假设CD2在T细胞和APC之间的IL-12/IFN-γ正反馈回路中起核心作用,通过控制T细胞对IL-12反应性的CD2/CD58相互作用提供关键的功能联系。该模型为未来旨在确定介导CD2这种细胞因子特异性调节作用的信号传导机制的研究提供了基础,并且它提供了对细胞因子受体和独特粘附分子如何相互作用以调节对该细胞因子反应性的深入了解。此外,它强调了像IL-12这样的免疫调节药物的临床潜力可能受特定共刺激存在与否支配的可能性。
