针对自身免疫中的 BAFF。
Targeting BAFF in autoimmunity.
机构信息
Center for Autoimmune and Musculoskeletal Diseases, Feinstein Institute for Medical Research, United States.
出版信息
Curr Opin Immunol. 2010 Dec;22(6):732-9. doi: 10.1016/j.coi.2010.09.010. Epub 2010 Oct 21.
Abstract
BAFF and APRIL are TNF-like cytokines that support survival and differentiation of B cells. The early appreciation that overexpression of BAFF leads to B cell expansion and a lupus-like syndrome in mice, and the demonstration that BAFF inhibition delays lupus onset in spontaneous mouse models of SLE and other autoimmune diseases has rapidly led to the development of strategies for inhibiting both BAFF and APRIL. The commercialization of this new class of drugs has proceeded in parallel with the continuing elucidation of the biology of the cytokines and their receptors. Recent studies have uncovered a role for BAFF in enhancing both innate and adaptive immune responses and in amplifying aberrant pathways that arise during inflammation. Two phase III studies of an anti-BAFF antibody have yielded positive, although modest, results in SLE and alternate inhibitors are being tested in a variety of autoimmune diseases in which BAFF may play a pathogenic role.
摘要
BAFF 和 APRIL 是 TNF 样细胞因子,可支持 B 细胞的存活和分化。早期人们发现,BAFF 的过度表达可导致 B 细胞扩增和狼疮样综合征,并且证明 BAFF 抑制可延迟自发性 SLE 小鼠模型和其他自身免疫性疾病中狼疮的发病,这迅速导致了抑制 BAFF 和 APRIL 的策略的发展。这类新药的商业化与细胞因子及其受体生物学的不断阐明齐头并进。最近的研究揭示了 BAFF 在增强先天和适应性免疫反应以及放大炎症过程中出现的异常途径方面的作用。两项抗 BAFF 抗体的 III 期研究在 SLE 中取得了阳性但适度的结果,而其他抑制剂正在各种可能发挥致病作用的自身免疫性疾病中进行测试。
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