Program on Inflammatory Disease Research, Infectious and Inflammatory Disease Center, Sanford-Burnham Medical Research Institute, 10901 N. Torrey Pines Rd., La Jolla, CA 92037, USA.
Mol Cell Biol. 2011 Jan;31(1):127-37. doi: 10.1128/MCB.00650-10. Epub 2010 Oct 18.
The generation of robust T-cell-dependent humoral immune responses requires the formation and expansion of germinal center structures within the follicular regions of the secondary lymphoid tissues. B-cell proliferation in the germinal center drives ongoing antigen-dependent selection and the generation of high-affinity class-switched plasma and memory B cells. However, the mechanisms regulating B-cell proliferation within this microenvironment are largely unknown. Here, we report that cyclin D3 is uniquely required for germinal center progression. Ccnd3(-/-) mice exhibit a B-cell-intrinsic defect in germinal center maturation and fail to generate an affinity-matured IgG response. We determined that the defect resulted from failed proliferative expansion of GL7(+) IgD(-) PNA(+) B cells. Mechanistically, sustained expression of cyclin D3 was found to be regulated at the level of protein stability and controlled by glycogen synthase kinase 3 in a cyclic AMP-protein kinase A-dependent manner. The specific defect in proliferative expansion of GL7(+) IgD(-) PNA(+) B cells in Ccnd3(-/-) mice defines an underappreciated step in germinal center progression and solidifies a role for cyclin D3 in the immune response, and as a potential therapeutic target for germinal center-derived B-cell malignancies.
产生稳健的 T 细胞依赖性体液免疫应答需要在次级淋巴组织的滤泡区域形成和扩展生发中心结构。生发中心内的 B 细胞增殖驱动持续的抗原依赖性选择和高亲和力类别转换的浆细胞和记忆 B 细胞的产生。然而,调节该微环境中 B 细胞增殖的机制在很大程度上尚不清楚。在这里,我们报告 cyclin D3 是生发中心进展所必需的。Ccnd3(-/-) 小鼠表现出生发中心成熟的 B 细胞内在缺陷,并且不能产生亲和力成熟的 IgG 应答。我们确定该缺陷是由于 GL7(+) IgD(-) PNA(+) B 细胞的增殖性扩张失败所致。从机制上讲,发现 cyclin D3 的持续表达受到蛋白质稳定性水平的调节,并通过 cAMP 依赖性蛋白激酶 A 依赖性糖原合酶激酶 3 控制。Ccnd3(-/-) 小鼠中 GL7(+) IgD(-) PNA(+) B 细胞增殖性扩张的特异性缺陷定义了生发中心进展中一个被低估的步骤,并巩固了 cyclin D3 在免疫应答中的作用,以及作为生发中心源性 B 细胞恶性肿瘤的潜在治疗靶点。
