改良cd40l活化b细胞增殖模型验证CD40-CD154通路抑制剂抑制活性

IF 4.1 4区医学 Q2 MEDICINE, RESEARCH & EXPERIMENTAL

Xenotransplantation Pub Date : 2025-01-01 DOI:10.1111/xen.70029

Man Zhang, Hao Feng, Yahui Huang, Tianyi Hu, Jiaxiang Du, Yong Wang, Song Chen, Dengke Pan, Lan Zhu, Gang Chen

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引用次数: 0

摘要

背景：CD40-CD154途径抑制剂被认为是异种移植中不可缺少的免疫抑制药物。目前，新的抗cd154和抗cd40单克隆抗体（mab）正在不断开发中。建立一种简单有效的体外方法来评价这些治疗性单克隆抗体的有效性是很重要的。方法：以转染人CD40配体（hCD40L-NIH/3T3）的NIH/3T3细胞为刺激细胞，人或恒河猴外周血单个核细胞（PBMCs）为应答细胞，建立cd40l活化的b细胞增殖模型。培养8 d后，流式细胞术检测b细胞增殖情况。在共培养系统中加入不同浓度的抗cd40或抗cd154单克隆抗体作为干预。研究并比较了抗cd154和抗cd40单克隆抗体对人和恒河猴B细胞增殖的抑制作用。结果：共培养8 d后，人和恒河猴pbmc中B细胞的增殖率均大于80%，B细胞上MHC-II及共刺激分子CD80、CD86、CD40的表达均显著上调。3种抗cd154单抗对人B细胞增殖均表现出类似的较强抑制作用，但对恒河猴B细胞增殖的抑制作用弱于对人B细胞的抑制作用，表现出典型的剂量依赖性抑制作用。不同来源的三种抗cd40单抗具有不同的作用。其中一种单克隆抗体能有效抑制人和猴b细胞的增殖，而另外两种单克隆抗体对人b细胞增殖表现出强烈或中度抑制作用，而对猴b细胞增殖几乎没有抑制作用。结论：我们成功建立了一种改良的cd40l活化b细胞增殖模型，用于体外评价CD40-CD154通路抑制剂的作用，为异种移植选择合适的治疗抗体及剂量确定提供了重要依据。

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Modified CD40L-Activated B-Cell Proliferation Model for Validating the Suppressive Activity of CD40-CD154 Pathway Inhibitors.

Background: CD40-CD154 pathway inhibitors are considered indispensable immunosuppressive drugs in xenotransplantation. At present, novel anti-CD154 and anti-CD40 monoclonal antibodies (mAbs) are continuously being developed. It is important to establish a simple and efficient in vitro method to evaluate the effectiveness of these therapeutic mAbs.

Methods: A modified CD40L-activated B-cell proliferation model was established using irradiated NIH/3T3 cells transfected with human CD40 ligand (hCD40L-NIH/3T3) as stimulator cells and human or rhesus monkey peripheral blood mononuclear cells (PBMCs) as responder cells. After 8 days of culture, B-cell proliferation was detected by flow cytometry. Various concentrations of anti-CD40 or anti-CD154 mAbs were added to the co-culture system as an intervention. The inhibitory effects of anti-CD154 and anti-CD40 mAbs on the proliferation of B cells from humans and rhesus monkeys were studied and compared.

Results: After 8 days of co-culture, the proliferation rate of B cells in both human and rhesus monkey PBMCs was more than 80%, and the expression of MHC-II and the co-stimulatory molecules CD80, CD86, and CD40 on B cells was significantly up-regulated. All three anti-CD154 mAbs showed a similar strong inhibitory effect on human B-cell proliferation, but the inhibitory effect on the proliferation of rhesus monkey B cells was weaker than that on human B cells, which showed a typical dose-dependent inhibition. The three anti-CD40 mAbs from different sources had different effects. One mAbs potently inhibited both human and monkey B-cell proliferation, whereas the other two mAbs exhibited strong or moderate inhibitory effects on human B-cell proliferation but had little inhibitory effect on monkey B-cell proliferation.

Conclusion: We have successfully established a modified CD40L-activated B-cell proliferation model for the in vitro evaluation of CD40-CD154 pathway inhibitors, which may provide important evidence for the selection of appropriate therapeutic antibodies and their dose determination for xenotransplantation.

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来源期刊

Xenotransplantation 医学-医学：研究与实验

CiteScore

6.80

自引率

15.40%

发文量

审稿时长

>12 weeks

期刊介绍： Xenotransplantation provides its readership with rapid communication of new findings in the field of organ and tissue transplantation across species barriers.The journal is not only of interest to those whose primary area is xenotransplantation, but also to veterinarians, microbiologists and geneticists. It also investigates and reports on the controversial theological, ethical, legal and psychological implications of xenotransplantation.