Small heat shock proteins (sHsps) are molecular chaperones that act to prevent the aberrant aggregation of misfolded proteins. Whilst it is suggested that sHsps prevent aggregation by binding to misfolded client proteins, the dynamic and heterogeneous nature of sHsps has hindered attempts to establish the mechanistic details of how sHsp-client protein complexes form. Single-molecule approaches have emerged as a powerful tool to investigate dynamic and heterogeneous interactions such as those that can occur between sHsps and their client proteins. Here, we use total internal reflection fluorescence microscopy to observe and characterise the complexes formed between model aggregation-prone client proteins (firefly luciferase, rhodanese and chloride intracellular channel 1 protein), and the human sHsps αB-crystallin (αB-c; HSPB5) and Hsp27 (HSPB1). We show that small (monomeric or dimeric) forms of both αB-c and Hsp27 bind to misfolded or oligomeric forms of the client proteins at early stages of aggregation, resulting in the formation of soluble sHsp-client complexes. Stoichiometric analysis of these complexes revealed that additional αB-c subunits accumulate onto pre-existing sHsp-client complexes to form larger species - this does not occur to the same extent for Hsp27. Instead, Hsp27-client interactions tend to be more transient than those of αB-c. Elucidating these mechanisms of sHsp function is crucial to our understanding of how these molecular chaperones act to inhibit protein aggregation and maintain cellular proteostasis.
Single-molecule observations of human small heat shock proteins in complex with aggregation-prone client proteins.
利用单分子方法观察人类小热休克蛋白与易聚集底物蛋白的复合物
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作者:Rice Lauren, Marzano Nicholas, Cox Dezerae, Skewes Bailey, van Oijen Antoine M, Ecroyd Heath
| 期刊: | Biochemical Journal | 影响因子: | 4.300 |
| 时间: | 2025 | 起止号: | 2025 May 6; 482(9):413-432 |
| doi: | 10.1042/BCJ20240473 | 种属: | Human |
| 研究方向: | 免疫/内分泌 | ||
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