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Lysosomal acidification mechanisms.

机译:溶酶体酸化机制。

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Lysosomes, the terminal organelles on the endocytic pathway, digest macromolecules and make their components available to the cell as nutrients. Hydrolytic enzymes specific to a wide range of targets reside within the lysosome; these enzymes are activated by the highly acidic pH (between 4.5 and 5.0) in the organelles' interior. Lysosomes generate and maintain their pH gradients by using the activity of a proton-pumping V-type ATPase, which uses metabolic energy in the form of ATP to pump protons into the lysosome lumen. Because this activity separates electric charge and generates a transmembrane voltage, another ion must move to dissipate this voltage for net pumping to occur. This so-called counterion may be either a cation (moving out of the lysosome) or an anion (moving into the lysosome). Recent data support the involvement of ClC-7, a Cl(-)/H(+) antiporter, in this process, although many open questions remain as to this transporter's involvement. Although functional results also point to a cation transporter, its molecular identity remains uncertain. Both the V-ATPase and the counterion transporter are likely to be important players in the mechanisms determining the steady-state pH of the lysosome interior. Exciting new results suggest that lysosomal pH may be dynamically regulated in some cell types.
机译:溶酶体是内吞途径的末端细胞器,可消化大分子并使它们的成分作为营养物质供细胞使用。特异于多种靶标的水解酶位于溶酶体内。这些酶被细胞器内部的高酸性pH(4.5至5.0)激活。溶酶体通过利用质子泵浦的V型ATPase的活性来生成并维持其pH梯度,该酶利用ATP形式的代谢能将质子泵入溶酶体腔。由于此活动会分离电荷并生成跨膜电压,因此必须移动另一个离子以耗散该电压,以进行净泵浦。这种所谓的抗衡离子可以是阳离子(移出溶酶体),也可以是阴离子(移入溶酶体)。最近的数据支持ClC-7,一种Cl(-)/ H(+)反向转运蛋白的参与,尽管该转运蛋白的参与仍存在许多悬而未决的问题。尽管功能性结果也指向阳离子转运蛋白,但其分子身份仍然不确定。 V-ATPase和抗衡离子转运蛋白都可能在确定溶酶体内部稳态pH的机制中起重要作用。令人兴奋的新结果表明,溶酶体的pH值可能在某些细胞类型中得到动态调节。

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