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Mechanisms for Hsp70 secretion: crossing membranes without a leader.

机译:Hsp70分泌的机制:没有前导物穿过膜。

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Heat shock protein 70 (Hsp70) is released from cells of many types and plays a significant signaling role, particularly in the inflammatory and immune responses. However, Hsp70 does not contain a consensus secretory signal and thus cannot traverse the plasma membrane by conventional mechanisms. However, Hsp70 can be released from cells by active mechanism that are independent of de novo Hsp70 synthesis or cell death. This pathway is similar to one utilized by the leaderless protein interleukin 1beta. Hsp70 release involves transit through an endolysosomal compartment and is inhibited by lysosomotropic compounds. In addition, the rate of Hsp70 secretion correlates well with the appearance of the lysosomal marker LAMP1 on the cell surface, further suggesting the role for endolysosomes. The entry of Hsp70 into this secretory compartment appears to involve the ABC-family transporter proteins. While the cell signals involved in triggering Hsp70 release through this lysosomal pathway are largely unknown, recent data suggest a regulatory role for extracellular ATP. These mechanisms are also shared by interleukin 1beta secretion. Following release it has been shown that Hsp70 binds to adjacent cells, suggesting that the secreted protein participates in paracrine or autocrine interactions with adjacent cell surfaces. Thus an outline is beginning to of the mechanisms of Hsp70 secretion. Much further study will be required to fully elucidate mechanisms involved in targeting Hsp70 towards the non-canonical secretion pathways and its regulation.
机译:热休克蛋白70(Hsp70)从许多类型的细胞中释放出来,并起着重要的信号作用,尤其是在炎症和免疫反应中。但是,Hsp70不包含共有分泌信号,因此无法通过常规机制穿越质膜。但是,Hsp70可以通过独立于从头Hsp70合成或细胞死亡的活性机制从细胞中释放出来。此途径类似于无前导蛋白白介素1beta所利用的途径。 Hsp70释放涉及通过溶酶体区室的转运,并受到溶溶同性化合物的抑制。此外,Hsp70的分泌速率与溶酶体标记物LAMP1在细胞表面的出现密切相关,进一步暗示了溶酶体的作用。 Hsp70进入此分泌区室似乎涉及ABC家庭转运蛋白。虽然很大程度上未知通过该溶酶体途径触发Hsp70释放的细胞信号,但最近的数据表明细胞外ATP的调节作用。这些机制也由白介素1β分泌共享。释放后,已经显示Hsp70与相邻细胞结合,表明分泌的蛋白参与与相邻细胞表面的旁分泌或自分泌相互作用。因此,Hsp70分泌机制的概述已经开始。要充分阐明将Hsp70靶向非典型分泌途径及其调控的机制,还需要进行更多的研究。

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