Department of Cell Biology and Histology, Academic Medical Center, Amsterdam 1105AZ, The Netherlands.
J Biol Chem. 2013 Jun 14;288(24):17225-37. doi: 10.1074/jbc.M112.421685. Epub 2013 Apr 23.
Fragments of proteins containing an expanded polyglutamine (polyQ) tract are thought to initiate aggregation and toxicity in at least nine neurodegenerative diseases, including Huntington's disease. Because proteasomes appear unable to digest the polyQ tract, which can initiate intracellular protein aggregation, preventing polyQ peptide aggregation by chaperones should greatly improve polyQ clearance and prevent aggregate formation. Here we expressed polyQ peptides in cells and show that their intracellular aggregation is prevented by DNAJB6 and DNAJB8, members of the DNAJ (Hsp40) chaperone family. In contrast, HSPA/Hsp70 and DNAJB1, also members of the DNAJ chaperone family, did not prevent peptide-initiated aggregation. Intriguingly, DNAJB6 and DNAJB8 also affected the soluble levels of polyQ peptides, indicating that DNAJB6 and DNAJB8 inhibit polyQ peptide aggregation directly. Together with recent data showing that purified DNAJB6 can suppress fibrillation of polyQ peptides far more efficiently than polyQ expanded protein fragments in vitro, we conclude that the mechanism of DNAJB6 and DNAJB8 is suppression of polyQ protein aggregation by directly binding the polyQ tract.
含有扩展多聚谷氨酰胺(polyQ)片段的蛋白质片段被认为至少在包括亨廷顿病在内的九种神经退行性疾病中引发聚集和毒性。由于蛋白酶体似乎无法消化多聚 Q 片段,而该片段可以引发细胞内蛋白质聚集,因此通过伴侣蛋白来防止 polyQ 肽聚集应该可以大大提高 polyQ 的清除率并防止聚集体形成。在这里,我们在细胞中表达了 polyQ 肽,并表明它们的细胞内聚集被 DNAJB6 和 DNAJB8 阻止,后者是 DNAJ(Hsp40)伴侣蛋白家族的成员。相比之下,HSPA/Hsp70 和 DNAJB1 也是 DNAJ 伴侣蛋白家族的成员,它们不能防止肽引发的聚集。有趣的是,DNAJB6 和 DNAJB8 还影响 polyQ 肽的可溶性水平,这表明 DNAJB6 和 DNAJB8 直接抑制 polyQ 肽的聚集。结合最近的数据表明,纯化的 DNAJB6 可以在体外比多聚 Q 扩展蛋白片段更有效地抑制 polyQ 肽的纤丝化,我们得出结论,DNAJB6 和 DNAJB8 的机制是通过直接结合 polyQ 片段来抑制 polyQ 蛋白聚集。
