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一种针对葡萄球菌肠毒素B的DNA适配体。

A DNA Spiegelmer to staphylococcal enterotoxin B.

作者信息

Purschke Werner G, Radtke Falko, Kleinjung Frank, Klussmann Sven

机构信息

NOXXON Pharma AG, Max-Dohrn-Strasse 8-10, 10589 Berlin, Germany.

出版信息

Nucleic Acids Res. 2003 Jun 15;31(12):3027-32. doi: 10.1093/nar/gkg413.

Abstract

Bacterial staphylococcal enterotoxin B is involved in several severe disease patterns and it was therefore used as a target for the generation of biologically stable mirror-image oligonucleotide ligands, so called Spiegelmers. The toxin is a 28 kDa protein consisting of 239 amino acids. Since the full-length protein is not accessible to chemical peptide synthesis, a stable domain of 25 amino acids was identified as a suitable selection target. DNA in vitro selection experiments were carried out against the equivalent mirror-image D-peptide domain resulting in high affinity D-DNA aptamers. As expected, the corresponding enantiomeric L-DNA Spiegelmer showed comparable binding characteristics to the L-peptide domain. Moreover, the Spiegelmer bound the whole protein target with only slightly reduced affinity. Dissociation constants of both peptide-oligonucleotide complexes were measured in the range of 200 nM, whereas the Spiegelmer binding to the full-length protein was determined at approximately 420 nM. These data demonstrate the possibility to identify Spiegelmers against large protein targets by a domain approach.

摘要

细菌葡萄球菌肠毒素B涉及多种严重疾病模式,因此它被用作生成生物稳定的镜像寡核苷酸配体(即所谓的镜像体)的靶标。该毒素是一种由239个氨基酸组成的28 kDa蛋白质。由于全长蛋白质无法通过化学肽合成获得,因此一个由25个氨基酸组成的稳定结构域被确定为合适的筛选靶标。针对等效的镜像D-肽结构域进行了DNA体外筛选实验,得到了高亲和力的D-DNA适配体。正如预期的那样,相应的对映体L-DNA镜像体对L-肽结构域表现出类似的结合特性。此外,镜像体与整个蛋白质靶标的结合亲和力仅略有降低。两种肽-寡核苷酸复合物的解离常数在200 nM范围内测定,而镜像体与全长蛋白质的结合亲和力约为420 nM。这些数据证明了通过结构域方法鉴定针对大蛋白质靶标的镜像体的可能性。

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A DNA Spiegelmer to staphylococcal enterotoxin B.一种针对葡萄球菌肠毒素B的DNA适配体。
Nucleic Acids Res. 2003 Jun 15;31(12):3027-32. doi: 10.1093/nar/gkg413.

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