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影响抗体单链Fv片段二聚体向单体转变的因素。

Factors influencing the dimer to monomer transition of an antibody single-chain Fv fragment.

作者信息

Arndt K M, Müller K M, Plückthun A

机构信息

Biochemisches Institut, Universität Zürich, Switzerland.

出版信息

Biochemistry. 1998 Sep 15;37(37):12918-26. doi: 10.1021/bi9810407.

Abstract

Antibody single-chain Fv (scFv) fragments are able to form dimers under certain conditions, and the extent of dimerization appears to depend on linker length, antibody sequence, and external factors. We analyzed the factors influencing dimer-monomer equilibrium as well as the rate of interconversion, using the scFv McPC603 as a model system. In this molecule, the stability of the VH-VL interaction can be conveniently varied by adjusting the ionic strength (because of its influence on the hydrophobic effect), by pH (presumably because of the presence of titratable groups in the interface), and by the presence or absence of the antigen phosphorylcholine, which can be rapidly removed due to its very fast off-rate. It was found that the monomer is the thermodynamically stable form with linkers of 15 and 25 amino acids length under all conditions tested (35 microM or less). The dimer is initially formed in periplasmic expression, presumably by domain swapping, and can be trapped by all factors which stabilize the VH-VL interface, such as the presence of the antigen, high ionic strength, and pH below 7.5. Under all other conditions, it converts to the monomer. Predominantly monomer is obtained during in vitro folding. Monomer is stabilized against dimerization at very high concentrations by the same factors which stabilize the VH-VL interaction. These results should be helpful in producing molecules with defined oligomerization states.

摘要

抗体单链Fv(scFv)片段在某些条件下能够形成二聚体,二聚化程度似乎取决于连接子长度、抗体序列和外部因素。我们以scFv McPC603作为模型系统,分析了影响二聚体 - 单体平衡以及相互转化速率的因素。在这个分子中,通过调节离子强度(因其对疏水作用的影响)、pH值(可能是由于界面中存在可滴定基团)以及抗原磷酸胆碱的存在与否,可以方便地改变VH - VL相互作用的稳定性,由于抗原磷酸胆碱的解离速率非常快,所以可以迅速去除。研究发现,在所有测试条件下(35 microM或更低),对于长度为15和25个氨基酸的连接子,单体是热力学稳定形式。二聚体最初在周质表达中形成,推测是通过结构域交换形成的,并且可以被所有稳定VH - VL界面的因素捕获,例如抗原的存在、高离子强度和pH值低于7.5。在所有其他条件下,它会转化为单体。在体外折叠过程中主要获得单体。通过稳定VH - VL相互作用的相同因素,在非常高的浓度下,单体可以稳定地防止二聚化。这些结果对于生产具有确定寡聚化状态的分子应该是有帮助的。

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