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转铁蛋白铁加载、亚基组成和 NCOA4-铁硫簇对转铁蛋白-NCOA4 相互作用的影响:等温滴定量热研究。

Effects of ferritin iron loading, subunit composition, and the NCOA4-iron sulfur cluster on ferritin-NCOA4 interactions: An isothermal titration calorimetry study.

机构信息

Department of Chemistry, State University of New York, Potsdam, NY 13676, USA.

Department of Chemistry, State University of New York, Potsdam, NY 13676, USA.

出版信息

Int J Biol Macromol. 2024 Oct;278(Pt 4):135044. doi: 10.1016/j.ijbiomac.2024.135044. Epub 2024 Aug 23.

DOI:10.1016/j.ijbiomac.2024.135044
PMID:39182888
Abstract

Ferritin is a 24-mer protein nanocage that stores iron and regulates intracellular iron homeostasis. The nuclear receptor coactivator-4 (NCOA4) binds specifically to ferritin H subunits and facilitates the autophagic trafficking of ferritin to the lysosome for degradation and iron release. Using isothermal titration calorimetry (ITC), we studied the thermodynamics of the interactions between ferritin and the soluble fragment of NCOA4 (residues 383-522), focusing on the effects of the recently identified FeS cluster bound to NCOA4, ferritin subunit composition, and ferritin-iron loading. Our findings show that in the presence of the FeS cluster, the binding is driven by a more favorable enthalpy change and a decrease in entropy change, indicating a key role for the FeS cluster in the structural organization and stability of the complex. The ferritin iron core further enhances this association, increasing binding enthalpy and stabilizing the NCOA4-ferritin complex. The ferritin subunit composition primarily affects binding stoichiometry of the reaction based on the number of H subunits in the ferritin H/L oligomer. Our results demonstrate that both the FeS cluster and the ferritin iron core significantly affect the binding thermodynamics of the NCOA4-ferritin interactions, suggesting regulatory roles for the FeS cluster and ferritin iron content in ferritinophagy.

摘要

铁蛋白是一种 24 -mer 蛋白纳米笼,可储存铁并调节细胞内铁稳态。核受体共激活因子-4(NCOA4)特异性结合铁蛋白 H 亚基,并促进铁蛋白向溶酶体的自噬转运进行降解和铁释放。我们使用等温滴定量热法(ITC)研究了铁蛋白与 NCOA4 的可溶性片段(残基 383-522)之间相互作用的热力学特性,重点关注最近鉴定出与 NCOA4 结合的 FeS 簇、铁蛋白亚基组成和铁蛋白-铁装载的影响。我们的研究结果表明,在 FeS 簇存在的情况下,结合是由更有利的焓变和熵变减小驱动的,表明 FeS 簇在复合物的结构组织和稳定性中起着关键作用。铁蛋白铁核心进一步增强了这种结合,增加了结合焓并稳定了 NCOA4-铁蛋白复合物。铁蛋白亚基组成主要根据铁蛋白 H/L 寡聚物中 H 亚基的数量影响反应的结合化学计量。我们的结果表明,FeS 簇和铁蛋白铁核心都显著影响 NCOA4-铁蛋白相互作用的结合热力学,表明 FeS 簇和铁蛋白铁含量在铁蛋白自噬中的调节作用。

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