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Bone Marrow Mesenchymal Stem Cells Enhance the Differentiation of Human Switched Memory B Lymphocytes into Plasma Cells in Serum-Free Medium

机译:骨髓间充质干细胞在无血清培养基中增强人类开关记忆B淋巴细胞向浆细胞的分化

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摘要

The differentiation of human B lymphocytes into plasma cells is one of the most stirring questions with regard to adaptive immunity. However, the terminal differentiation and survival of plasma cells are still topics with much to be discovered, especially when targeting switched memory B lymphocytes. Plasma cells can migrate to the bone marrow in response to a CXCL12 gradient and survive for several years while secreting antibodies. In this study, we aimed to get closer to niches favoring plasma cell survival. We tested low oxygen concentrations and coculture with mesenchymal stem cells (MSC) from human bone marrow. Besides, all cultures were performed using an animal protein-free medium. Overall, our model enables the generation of high proportions of CD38+CD138+CD31+ plasma cells (≥50%) when CD40-activated switched memory B lymphocytes were cultured in direct contact with mesenchymal stem cells. In these cultures, the secretion of CXCL12 and TGF-β, usually found in the bone marrow, was linked to the presence of MSC. The level of oxygen appeared less impactful than the contact with MSC. This study shows for the first time that expanded switched memory B lymphocytes can be differentiated into plasma cells using exclusively a serum-free medium.
机译:关于适应性免疫,人类B淋巴细胞向浆细胞的分化是最激动人心的问题之一。然而,浆细胞的终末分化和存活仍然是有待发现的主题,尤其是在靶向开关记忆B淋巴细胞时。浆细胞可以响应CXCL12梯度迁移至骨髓,并在分泌抗体的同时存活数年。在这项研究中,我们旨在更接近利于浆细胞存活的领域。我们测试了低氧浓度并与人骨髓间充质干细胞(MSC)共培养。此外,所有培养均使用无动物蛋白的培养基进行。总体而言,当CD40激活切换时,我们的模型能够生成高比例的CD38 + CD138 + CD31 + 浆细胞(≥50%)记忆B淋巴细胞与间充质干细胞直接接触培养。在这些培养物中,通常在骨髓中发现的CXCL12和TGF-β的分泌与MSC的存在有关。氧气的含量似乎不及与MSC接触的影响。这项研究首次表明,仅使用无血清培养基就可以将扩增的开关记忆B淋巴细胞分化为浆细胞。

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