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旨在减少与Fc-γ受体结合的Fc突变的系统分析。

Systematic analysis of Fc mutations designed to reduce binding to Fc-gamma receptors.

作者信息

Hale Geoff, De Vos Jelle, Davy Alastair Douglas, Sandra Koen, Wilkinson Ian

机构信息

mAbsolve Limited, Oxford, UK.

RIC group, Kortrijk, Belgium.

出版信息

MAbs. 2024 Jan-Dec;16(1):2402701. doi: 10.1080/19420862.2024.2402701. Epub 2024 Sep 15.

Abstract

Elimination of the binding of immunoglobulin Fc to Fc gamma receptors is highly desirable for the avoidance of unwanted inflammatory responses to therapeutic antibodies and fusion proteins. Many different approaches have been used in the clinic, but they have not been systematically compared. We have now produced a matched set of anti-CD20 antibodies with different Fc subclasses and variants and compared their activity for binding to C1q, Fc-gamma receptors and in cell-based assays. Most of the variants still have significant levels of activity in one or more of these assays and many of them have impaired temperature stability compared with the corresponding wild-type antibody.

摘要

消除免疫球蛋白Fc与Fcγ受体的结合对于避免治疗性抗体和融合蛋白引发不必要的炎症反应非常必要。临床上已经使用了许多不同的方法,但尚未对它们进行系统比较。我们现在制备了一组具有不同Fc亚类和变体的匹配抗CD20抗体,并比较了它们与C1q、Fcγ受体结合的活性以及在基于细胞的检测中的活性。大多数变体在这些检测中的一种或多种中仍具有显著的活性水平,并且与相应的野生型抗体相比,其中许多变体的温度稳定性受损。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2da7/11407402/a2d939ba46d5/KMAB_A_2402701_F0001_OC.jpg

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