首页> 美国卫生研究院文献>Immunology >The comparative effects of cyclosporin A and 1616 dimethyl prostaglandin E2 on the allogeneic induction of monocyte/macrophage procoagulant activity and the cytokines macrophage procoagulant inducing factor and interleukin-2.
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The comparative effects of cyclosporin A and 1616 dimethyl prostaglandin E2 on the allogeneic induction of monocyte/macrophage procoagulant activity and the cytokines macrophage procoagulant inducing factor and interleukin-2.

机译:环孢菌素A和1616二甲基前列腺素E2对同种异体诱导单核细胞/巨噬细胞促凝活性以及细胞因子巨噬细胞促凝因子和白介素2的比较作用。

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摘要

It has recently been reported that combination immunotherapy utilizing cyclosporin A (CsA) and prostaglandin E (PGE) reduced the frequency of acute renal allograft rejection; however, the mechanism for the benefit of this combination therapy is uncertain. Since our previous studies have suggested that macrophage procoagulant activity (PCA) is an important mediator of allograft rejection, in this study we have examined the effects of CsA and 16,16 dimethyl prostaglandin E2 (dmPGE2) alone and in combination on the induction of macrophage PCA and on the lymphokines macrophage procoagulant-inducing factor (MPIF) and interleukin-2 (IL-2) in vitro. Alloantigen-induced MPIF activity could be detected within 8 hr, reaching maximal levels by 12 hr and could still be detected at 24 hr. Allogeneic induction of PCA in splenic mononuclear cells was detectable by 24 hr, reaching maximal levels at 72 hr and was still detectable after 120 hr. CsA at concentrations from 100 ng/ml to 1000 ng/ml completely inhibited production of MPIF and IL-2, but had minimal effects on the ability of MPIF to induce isolated macrophage to express PCA. In contrast, dmPGE2 (10(-12)-10(-6) M) inhibited both the induction of MPIF and the ability of MPIF directly to induce macrophages to express PCA, with lesser effects on the induction of IL-2. The effects of minimal inhibitory concentrations of CsA and dmPGE2 in combination resulted in synergistic inhibition of PCA induction. These data demonstrate the disparate actions of CsA and dmPGE2 on inhibition of PCA, MPIF and IL-2, and provide a possible mechanism for the beneficial effects of combination CsA and dmPGE2 in patients receiving organ allografts.
机译:最近有报道说,使用环孢菌素A(CsA)和前列腺素E(PGE)的联合免疫疗法可降低急性肾移植排斥反应的发生率。但是,这种联合治疗的获益机制尚不确定。由于我们先前的研究表明巨噬细胞促凝活性(PCA)是同种异体移植排斥的重要介质,因此在这项研究中,我们研究了单独和联合使用CsA和16,16二甲基前列腺素E2(dmPGE2)对巨噬细胞诱导的影响。 PCA以及对淋巴因子巨噬细胞促凝剂诱导因子(MPIF)和白介素2(IL-2)的体外作用。异体抗原诱导的MPIF活性可以在8小时内检测到,到12小时达到最高水平,并且在24小时仍可以检测到。脾单核细胞中PCA的同种异体诱导可在24小时内检测到,在72小时达到最高水平,在120小时后仍可检测到。 100 ng / ml至1000 ng / ml浓度的CsA完全抑制MPIF和IL-2的产生,但对MPIF诱导分离的巨噬细胞表达PCA的能力影响很小。相反,dmPGE2(10(-12)-10(-6)M)抑制了MPIF的诱导和MPIF直接诱导巨噬细胞表达PCA的能力,对IL-2的诱导作用较小。最小抑制浓度的CsA和dmPGE2联合使用可协同抑制PCA诱导。这些数据证明了CsA和dmPGE2在抑制PCA,MPIF和IL-2方面的不同作用,并为接受器官同种异体移植的患者组合CsA和dmPGE2的有益作用提供了可能的机制。

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