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浆细胞库的维持独立于记忆B细胞。

Maintenance of the plasma cell pool is independent of memory B cells.

作者信息

Ahuja Anupama, Anderson Shannon M, Khalil Ashraf, Shlomchik Mark J

机构信息

Departments of Laboratory Medicine and Immunobiology, Yale University, New Haven, CT 06510, USA.

出版信息

Proc Natl Acad Sci U S A. 2008 Mar 25;105(12):4802-7. doi: 10.1073/pnas.0800555105. Epub 2008 Mar 13.

Abstract

Humoral memory to an antigen (Ag) is maintained for several decades in the form of memory B cells and serum Ab. In fact, plasma cells (PCs) that secrete Ab are known to be long-lived and could be solely responsible for maintaining the long-lived Ab titers. Alternatively, it has been proposed that the PC compartment is maintained for long periods by the differentiation of memory cells into long-lived PCs as a result of nonspecific stimulation. This model predicts accelerated decay of PC numbers in the absence of memory cells for the same Ag. To address this prediction, we have developed a mouse model system that combined the ability to deplete B cells with the ability to detect Ag-specific memory and PCs. After establishing an immune response, we depleted Ag-specific memory B cells with an anti-hCD20 mAb and determined the effect on the PC compartment over 16 weeks. Using a combination of surface markers, we demonstrated that memory B cells remained depleted over the course of the experiment. However, despite this absence of memory cells for an extended duration, PC numbers in spleen and bone marrow did not decline, which indicates that the PC compartment does not require a significant contribution from memory B cells for its maintenance and instead that PCs are sufficiently long-lived to maintain Ab titers over a long period without renewal. This observation settles an important controversy in B cell biology and has implications for the design of vaccines and for B cell depletion therapy in patients.

摘要

对抗原(Ag)的体液免疫记忆以记忆B细胞和血清抗体的形式维持数十年。事实上,已知分泌抗体的浆细胞(PC)寿命很长,可能是维持长期抗体滴度的唯一原因。另外,有人提出,由于非特异性刺激,记忆细胞分化为长寿浆细胞,从而使浆细胞区室长期维持。该模型预测,在缺乏针对相同抗原的记忆细胞的情况下,浆细胞数量会加速衰减。为了验证这一预测,我们开发了一种小鼠模型系统,该系统结合了消耗B细胞的能力和检测抗原特异性记忆及浆细胞的能力。建立免疫反应后,我们用抗人CD20单克隆抗体耗尽抗原特异性记忆B细胞,并在16周内确定其对浆细胞区室的影响。通过结合使用表面标志物,我们证明在实验过程中记忆B细胞一直处于耗尽状态。然而,尽管在很长一段时间内没有记忆细胞,但脾脏和骨髓中的浆细胞数量并未下降,这表明浆细胞区室的维持并不需要记忆B细胞的显著贡献,相反,浆细胞寿命足够长,无需更新就能长期维持抗体滴度。这一观察结果解决了B细胞生物学中的一个重要争议,对疫苗设计和患者的B细胞耗竭疗法具有启示意义。

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