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CD83⁺单核细胞来源树突状细胞的多种功能活性及其对癌症疫苗的意义。

Diverse functional activity of CD83+ monocyte-derived dendritic cells and the implications for cancer vaccines.

作者信息

Czerniecki B J, Cohen P A, Faries M, Xu S, Roros J G, Bedrosian I

机构信息

Department of Surgery and Harrison Surgical Research Center, University of Pennsylvania, Philadelphia 19104, USA.

出版信息

Crit Rev Immunol. 2001;21(1-3):157-78.

PMID:11642602
Abstract

Antigen-loaded dendritic cells (DCs) provide key regulatory signals to T cells during a developing antitumor response. In addition to providing costimulation, mature DC provides cytokine and chemokine signals that can define the T1 vs T2 nature of the antitumor T-cell response as well as whether T cells engage in direct interactions with tumor cells. In serum-free culture conditions that hasten the differentiation of monocytes into mature DCs, certain agents, such as CD40L, accelerate phenotypic maturation (e.g., CD83 and costimulatory molecule expression) without influencing the acquisition of Dc1/Dc2 characteristics. In contrast, exposure to serum-free medium and interferon-gamma (IFN-gamma) rapidly influences CD83+ DCs to secrete high levels of IL-12, IL-6, and MIP-1beta, and promotes Dcl differentiation. In contrast, CD83+ DCs matured in serum-free medium in the absence of IFN-gamma, or in the presence of calcium signaling agents, prostaglandin-E2, or IFN-alpha, produce no IL-12, scant IL-6, and prodigious IL-8, MDC, and TARC, and promote Dc2 differentiation. T cells sensitized via IL-12-secreting, peptide-pulsed DCs secrete cytokines when subsequently exposed to relevant peptide-pulsed antigen-presenting cells (APCs) or to HLA-compatible tumor cells endogenously expressing the peptide. In contrast, T cells sensitized via IL-12 nonsecreting DC were limited to antigenic reactivation through APC contact rather than tumor cell contact. Therefore, the development of antitumor responses can be dramatically influenced not only by costimulation, but also by the cytokine and chemokine production of DCs, which must be considered in the development of cancer vaccines.

摘要

负载抗原的树突状细胞(DCs)在抗肿瘤反应形成过程中为T细胞提供关键的调节信号。除了提供共刺激信号外,成熟的DC还提供细胞因子和趋化因子信号,这些信号可以决定抗肿瘤T细胞反应的T1与T2性质,以及T细胞是否与肿瘤细胞进行直接相互作用。在无血清培养条件下,可加速单核细胞分化为成熟DC,某些因子,如CD40L,可加速表型成熟(如CD83和共刺激分子表达),而不影响Dc1/Dc2特性的获得。相反,暴露于无血清培养基和干扰素-γ(IFN-γ)会迅速影响CD83+ DC分泌高水平的IL-12、IL-6和MIP-1β,并促进Dcl分化。相比之下,在无血清培养基中、不存在IFN-γ或存在钙信号剂、前列腺素-E2或IFN-α的情况下成熟的CD83+ DC不产生IL-12,产生少量IL-6,大量产生IL-8、MDC和TARC,并促进Dc2分化。通过分泌IL-12的肽脉冲DC致敏的T细胞,当随后暴露于相关的肽脉冲抗原呈递细胞(APC)或内源性表达该肽的HLA相容肿瘤细胞时会分泌细胞因子。相反,通过不分泌IL-12的DC致敏的T细胞仅限于通过APC接触而非肿瘤细胞接触进行抗原再激活。因此,抗肿瘤反应的形成不仅会受到共刺激的显著影响,还会受到DC产生的细胞因子和趋化因子的显著影响,这在癌症疫苗的研发中必须予以考虑。

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