Australian Institute for Bioengineering and Nanotechnology (AIBN), University of Queensland (UQ), Brisbane, QLD 4072, Australia.
Centre for Advanced Imaging, University of Queensland (UQ), Brisbane, QLD 4072, Australia.
Sci Rep. 2016 Nov 22;5:37348. doi: 10.1038/srep37348.
Human Chaperonin 10 (hCpn10) was utilised as a novel scaffold for presenting peptides of therapeutic and diagnostic significance. Molecular dynamic simulations and protein sizing analyses identified a peptide linker (P1) optimal for the formation of the quarternary hCpn10 heptamer structure. hCpn10 scaffold displaying peptides targeting Factor VIIa (CE76) and CD44 (CP7) were expressed in E. coli. Functional studies of CE76 indicated nanomolar affinity for Factor VIIa (3 nM) similar to the E-76 peptide (6 nM), with undetectable binding to Factor X. CE76 was a potent inhibitor of FX activity (via inhibition of Factor VIIa) and prolonged clot formation 4 times longer than achieved by E-76 peptide as determined by prothrombin time (PT) assays. This improvement in clotting function by CE76, highlights the advantages of a heptamer-based scaffold for improving avidity by multiple peptide presentation. In another example of hCPn10 utility as a scaffold, CP7 bound to native CD44 overexpressed on cancer cells and bound rCD44 with high affinity (K 9.6 nM). The ability to present various peptides through substitution of the hCpn10 mobile loop demonstrates its utility as a novel protein scaffold.
人热休克蛋白 10(hCpn10)被用作展示具有治疗和诊断意义的肽的新型支架。分子动力学模拟和蛋白质尺寸分析确定了一种肽接头(P1),最适合形成四元 hCpn10 七聚体结构。在大肠杆菌中表达了针对因子 VIIa(CE76)和 CD44(CP7)的靶向肽的 hCpn10 支架。CE76 的功能研究表明,其对因子 VIIa 的亲和力为纳摩尔级(3 nM),与 E-76 肽(6 nM)相似,与因子 X 几乎没有结合。CE76 是 FX 活性的有效抑制剂(通过抑制因子 VIIa),并通过凝血酶原时间(PT)测定比 E-76 肽延长了 4 倍的血栓形成时间。CE76 在凝血功能方面的这种改善,突出了基于七聚体支架通过多种肽展示来提高亲和力的优势。在 hCPn10 用作支架的另一个例子中,CP7 与癌细胞上过表达的天然 CD44 结合,并与 rCD44 具有高亲和力(K 9.6 nM)。通过替代 hCpn10 可移动环来呈现各种肽的能力证明了它作为一种新型蛋白质支架的实用性。
Zotero 插件
