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炎症状态决定间充质干细胞或基质细胞对B细胞功能的影响。

Inflammatory Conditions Dictate the Effect of Mesenchymal Stem or Stromal Cells on B Cell Function.

作者信息

Luk Franka, Carreras-Planella Laura, Korevaar Sander S, de Witte Samantha F H, Borràs Francesc E, Betjes Michiel G H, Baan Carla C, Hoogduijn Martin J, Franquesa Marcella

机构信息

Nephrology and Transplantation, Department of Internal Medicine, Erasmus MC, University Medical Center, Rotterdam, Netherlands.

REMAR Group and Nephrology Service, Germans Trias i Pujol Health Science Institute & University Hospital, Badalona, Spain.

出版信息

Front Immunol. 2017 Aug 28;8:1042. doi: 10.3389/fimmu.2017.01042. eCollection 2017.

Abstract

The immunomodulatory capacity of mesenchymal stem or stromal cells (MSC) makes them a promising tool for treatment of immune disease and organ transplantation. The effects of MSC on B cells are characterized by an abrogation of plasmablast formation and induction of regulatory B cells (Bregs). It is, however, unknown how MSC interact with B cells under inflammatory conditions. In this study, adipose tissue-derived MSC were pretreated with 50 ng/ml IFN-γ for 96 h (MSC-IFN-γ) to simulate inflammatory conditions. Mature B cells were obtained from spleens by CD43 selection. B cells were co-cultured with MSC and stimulated with anti-IgM, anti-CD40, and IL-2; and after 7 days, B cell proliferation, phenotype, Immunoglobulin-G (IgG), and IL-10 production were analyzed. MSC did not inhibit B cell proliferation but increased the percentage of CD38 CD24 B cells (Bregs) and IL-10 production, while MSC-IFN-γ significantly reduced B cell proliferation and inhibited IgG production by B cells in a more potent fashion but did not induce Bregs or IL-10 production. Both MSC and MSC-IFN-γ required proximity to target cells and being metabolically active to exert their effects. Indoleamine 2,3 dioxygenase expression was highly induced in MSC-IFN-γ and was responsible of the anti-proliferative and Breg reduction since addition of tryptophan (TRP) restored MSC properties. Immunological conditions dictate the effect of MSC on B cell function. Under immunological quiescent conditions, MSC stimulate Breg induction; whereas, under inflammatory conditions, MSC inhibit B cell proliferation and maturation through depletion of TRP. This knowledge is useful for customizing MSC therapy for specific purposes by appropriate pretreatment of MSC.

摘要

间充质干细胞(MSC)的免疫调节能力使其成为治疗免疫疾病和器官移植的一种有前景的工具。MSC对B细胞的作用表现为抑制浆母细胞形成和诱导调节性B细胞(Breg)。然而,尚不清楚MSC在炎症条件下如何与B细胞相互作用。在本研究中,脂肪组织来源的MSC用50 ng/ml IFN-γ预处理96小时(MSC-IFN-γ)以模拟炎症条件。通过CD43分选从脾脏中获得成熟B细胞。将B细胞与MSC共培养,并用抗IgM、抗CD40和IL-2刺激;7天后,分析B细胞增殖、表型、免疫球蛋白G(IgG)和IL-10产生情况。MSC不抑制B细胞增殖,但增加了CD38⁺CD24⁺ B细胞(Breg)的百分比和IL-10产生,而MSC-IFN-γ显著降低B细胞增殖并更有效地抑制B细胞产生IgG,但不诱导Breg或IL-10产生。MSC和MSC-IFN-γ都需要与靶细胞接近并具有代谢活性才能发挥其作用。吲哚胺2,3双加氧酶表达在MSC-IFN-γ中高度诱导,并且由于添加色氨酸(TRP)恢复了MSC特性,所以其是抗增殖和Breg减少的原因。免疫条件决定了MSC对B细胞功能的影响。在免疫静止条件下,MSC刺激Breg诱导;而在炎症条件下,MSC通过消耗TRP抑制B细胞增殖和成熟。这些知识对于通过对MSC进行适当预处理来定制特定目的的MSC治疗是有用的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3490/5581385/d3a087bdbc8d/fimmu-08-01042-g001.jpg

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