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Canonical structures of short CDR-L3 in antibodies

机译:抗体中短CDR-L3的规范结构

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Despite sequence diversity, five out of six hypervariable loops in antibodies assume a limited number of conformations called canonical structures. Their correct identification is essential for successful prediction of antibody structure. This in turn requires regular updates of the classification of canonical structures to match the expanding experimental database. Antibodies with the eight-residue CDR-L3 represent the second most common type of antibodies after those with the nine-residue CDR-L3. We have analyzed all crystal structures of Fab and Fv with the eight-residue CDR-L3 and identified three major canonical structures covering 82% of a nonredundant set. In most cases, the canonical structure is defined by the absence or presence and position of a proline residue within the CDR. (C) 2014 The Authors. Proteins published by Wiley Periodicals, Inc.
机译:尽管具有序列多样性,但抗体中六个高变环中的五个仍具有称为标准结构的有限数量的构象。它们的正确鉴定对于成功预测抗体结构至关重要。反过来,这需要定期更新规范结构的分类,以匹配不断扩展的实验数据库。具有八残基CDR-L3的抗体代表仅次于具有九残基CDR-L3的抗体的第二种最常见的抗体。我们已经用八残基CDR-L3分析了Fab和Fv的所有晶体结构,并确定了覆盖82%非冗余集的三个主要规范结构。在大多数情况下,规范结构由CDR中脯氨酸残基的存在或不存在及其位置来定义。 (C)2014作者。 Wiley Periodicals,Inc.发布的蛋白质

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