首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Type II (tositumomab) anti-CD20 monoclonal antibody out performs type I (rituximab-like) reagents in B-cell depletion regardless of complement activation.
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Type II (tositumomab) anti-CD20 monoclonal antibody out performs type I (rituximab-like) reagents in B-cell depletion regardless of complement activation.

机译:II型(tositumomab)抗CD20单克隆抗体在B细胞耗竭时执行I型(rituximab样)试剂,而不考虑补体激活。

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摘要

Anti-CD20 monoclonal antibodies (mAbs) are classified into type I (rituximab-like) or type II (tositumomab-like) based on their ability to redistribute CD20 molecules in the plasma membrane and activate various effector functions. To compare type I and II mAbs directly in vivo and maximize Fc effector function, we selected and engineered mAbs with the same mouse IgG(2)a isotype and assessed their B-cell depleting activity in human CD20 transgenic mice. Despite being the same isotype, having similar affinity, opsonizing activity for phagocytosis, and in vivo half-life, the type II mAb tositumomab (B1) provided substantially longer depletion of B cells from the peripheral blood compared with the type I mAb rituximab (Rit m2a), and 1F5. This difference was also evident within the secondary lymphoid organs, in particular, the spleen. Failure to engage complement did not explain the efficacy of the type II reagents because type I mAbs mutated in the Fc domain (K322A) to prevent C1q binding still did not display equivalent efficacy. These results give support for the use of type II CD20 mAbs in human B-cell diseases.
机译:抗CD20单克隆抗体(mAb)根据其在质膜中重新分布CD20分子并激活各种效应子功能的能力,分为I型(利妥昔单抗)或II型(托西妥单抗)。为了直接在体内比较I型和II型mAb,并最大化Fc效应子功能,我们选择和工程改造了具有相同小鼠IgG(2)a同种型的mAb,并评估了其在人CD20转基因小鼠中的B细胞耗竭活性。尽管具有相同的同种型,具有相似的亲和力,对吞噬作用的调理活性以及体内半衰期,但与I型mAb利妥昔单抗(Rit)相比,II型mAb Tositumomab(B1)提供了更长的外周血B细胞耗竭时间m2a)和1F5。在次级淋巴器官,特别是脾脏内,这种差异也很明显。未能参与补体不能解释II型试剂的功效,因为在Fc结构域(K322A)中发生突变以阻止C1q结合的I型mAb仍未显示出等效的功效。这些结果支持II型CD20 mAb在人类B细胞疾病中的使用。

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