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经钙离子载体处理的外周血单核细胞和树突状细胞迅速呈现出活化树突状细胞的特征。

Calcium ionophore-treated peripheral blood monocytes and dendritic cells rapidly display characteristics of activated dendritic cells.

作者信息

Czerniecki B J, Carter C, Rivoltini L, Koski G K, Kim H I, Weng D E, Roros J G, Hijazi Y M, Xu S, Rosenberg S A, Cohen P A

机构信息

Department of Surgery, University of Pennsylvania Medical Center, Philadelphia 19104, USA.

出版信息

J Immunol. 1997 Oct 15;159(8):3823-37.

PMID:9378970
Abstract

Human peripheral blood contains a small subpopulation of immature dendritic cells (iDC) distinguished from circulating monocytes by their low expression of CD14. We utilized leukapheresis and countercurrent centrifugal elutriation to obtain myeloid origin mononuclear cell (MOMC) fractions of monocytes and iDC for study. These subpopulations were ultrastructurally and immunophenotypically similar before culture. After a 20- to 96-h culture either alone, with recombinant human granulocyte-monocyte CSF, or with endotoxin, greater up-regulation of costimulatory molecule expression was observed among iDC than among monocytes, and only iDC expressed the activation molecule CD83. Treatment with rhIL-4 caused many MOMC to develop morphologic properties of dendritic cells within 96 h, but costimulatory molecule up-regulation and CD14 down-regulation were heterogeneous, and CD83 expression was infrequent. In contrast, calcium ionophore (CI) treatment induced rapid and consistent effects in MOMC from both healthy volunteers and cancer patients, including down-regulated CD14 expression, acquisition of dendritic cell morphologic properties, up-regulated MHC and costimulatory molecule expression, and de novo CD83 expression. Many such effects occurred within 20 h of treatment. CI treatment activated purified CD14+ monocytes and also enhanced the spontaneous activation of purified CD14-/dim iDC in culture. Unfractionated MOMC, purified monocytes, and purified iDC displayed equivalently enhanced T cell-sensitizing efficiency following CI treatment. CD4+ T cell sensitization to keyhole limpet hemocyanin and CD8+ T cell sensitization to MART-1 melanoma-associated peptide were achieved in a single culture stimulation. Therefore, circulating monocytes and iDC can be induced by CI to manifest properties of activated DC, providing large numbers of efficient, nontransformed autologous APC for T cell sensitization strategies.

摘要

人外周血含有一小部分未成熟树突状细胞(iDC),其与循环单核细胞的区别在于CD14表达水平较低。我们利用白细胞单采术和逆流离心淘析法获取单核细胞和iDC的髓系来源单核细胞(MOMC)组分用于研究。这些亚群在培养前在超微结构和免疫表型上相似。单独培养、与重组人粒细胞 - 单核细胞集落刺激因子或内毒素共同培养20至96小时后,iDC中协同刺激分子表达的上调比单核细胞中更明显,并且只有iDC表达激活分子CD83。用重组人白细胞介素 - 4处理可使许多MOMC在96小时内发育出树突状细胞的形态学特性,但协同刺激分子上调和CD14下调是异质性的,且CD83表达很少见。相比之下,钙离子载体(CI)处理对健康志愿者和癌症患者的MOMC均诱导出快速且一致的效应,包括CD14表达下调、获得树突状细胞形态学特性、MHC和协同刺激分子表达上调以及从头表达CD83。许多此类效应在处理后20小时内出现。CI处理激活纯化的CD14 +单核细胞,还增强了培养中纯化的CD14 - / dim iDC的自发激活。CI处理后,未分级的MOMC、纯化的单核细胞和纯化的iDC表现出同等增强的T细胞致敏效率。在单次培养刺激中实现了对钥孔戚血蓝蛋白的CD4 + T细胞致敏和对MART - 1黑色素瘤相关肽的CD8 + T细胞致敏。因此,循环单核细胞和iDC可被CI诱导表现出活化DC的特性,为T细胞致敏策略提供大量高效、未转化的自体抗原呈递细胞。

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