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FhCaBP4:一种具有 EF 手和动力蛋白轻链结构域的肝片形吸虫钙结合蛋白。

FhCaBP4: a Fasciola hepatica calcium-binding protein with EF-hand and dynein light chain domains.

机构信息

Medical Biology Centre, School of Biological Sciences, Queen's University Belfast, 97 Lisburn Road, Belfast, BT9 7BL, UK.

出版信息

Parasitol Res. 2012 Oct;111(4):1707-13. doi: 10.1007/s00436-012-3010-y. Epub 2012 Jul 8.

DOI:10.1007/s00436-012-3010-y
PMID:22773043
Abstract

In trematodes, there is a family of proteins which combine EF-hand-containing domains with dynein light chain (DLC)-like domains. A member of this family from the liver fluke, Fasciola hepatica-FhCaBP4-has been identified and characterised biochemically. FhCaBP4 has an N-terminal domain containing two imperfect EF-hand sequences and a C-terminal dynein light chain-like domain. Molecular modelling predicted that the two domains are joined by a flexible linker. Native gel electrophoresis demonstrated that FhCaBP4 binds to calcium, manganese, barium and strontium ions, but not to magnesium or zinc ions. The hydrophobic, fluorescent probe 8-anilinonaphthalene-1-sulphonate bound more tightly to FhCaBP4 in the presence of calcium ions. This suggests that the protein undergoes a conformational change on ion binding which increases the number of non-polar residues on the surface. FhCaBP4 was protected from limited proteolysis by the calmodulin antagonist W7, but not by trifluoperazine or praziquantel. Protein-protein cross-linking experiments showed that FhCaBP4 underwent calcium ion-dependent dimerisation. Since DLCs are commonly dimeric, it is likely that FhCaBP4 dimerises through this domain. The molecular model reveals that the calcium ion-binding site is located close to a key sequence in the DLC-like domain, suggesting a plausible mechanism for calcium-dependent dimerisation.

摘要

在吸虫中,有一种蛋白质家族,它将 EF 手结构域与动力蛋白轻链(DLC)样结构域结合在一起。从肝片吸虫(Fasciola hepatica)中鉴定并生化表征了该家族的一个成员-FhCaBP4。FhCaBP4 具有包含两个不完美 EF 手序列的 N 端结构域和 C 端动力蛋白轻链样结构域。分子建模预测这两个结构域由一个柔性接头连接。天然凝胶电泳表明,FhCaBP4 结合钙、锰、钡和锶离子,但不结合镁或锌离子。疏水性荧光探针 8-苯胺基萘-1-磺酸盐在钙离子存在下与 FhCaBP4 结合更紧密。这表明该蛋白在离子结合时发生构象变化,增加了表面的非极性残基数。FhCaBP4 被钙调蛋白拮抗剂 W7 保护免受有限的蛋白水解,但不受三氟拉嗪或吡喹酮的保护。蛋白-蛋白交联实验表明,FhCaBP4 发生钙离子依赖性二聚化。由于 DLC 通常是二聚体,因此 FhCaBP4 可能通过该结构域二聚化。分子模型揭示了钙离子结合位点位于 DLC 样结构域中的关键序列附近,这表明了钙离子依赖性二聚化的合理机制。

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