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分离的大鼠肝细胞中去唾液酸糖蛋白受体的循环利用。ATP耗竭会阻断受体循环利用,但不会阻断单次内吞作用。

Recycling of the asialoglycoprotein receptor in isolated rat hepatocytes. ATP depletion blocks receptor recycling but not a single round of endocytosis.

作者信息

Clarke B L, Weigel P H

出版信息

J Biol Chem. 1985 Jan 10;260(1):128-33.

PMID:3965443
Abstract

Continuous endocytosis of 125I-asialo-orosomucoid (ASOR) mediated by the galactosyl receptor in rat hepatocytes is a cyclic process. 125I-ASOR-receptor complexes are internalized, processed, and the ligand is degraded while the receptor is returned to the cell surface for reutilization. Since a true cycle has a thermodynamic requirement for the input of external energy, we examined the effects of changes in intracellular ATP levels on the function of the receptor cycle. Hepatocytes were depleted of ATP to various extents prior to endocytosis by incubating cells at 15 degrees C in the presence of 2 mM NaF and 0-20 mM NaN3. A luciferase-luciferin bioluminescence assay was used to quantitate the amount of cellular ATP. ATP-depleted cells were allowed to bind 125I-ASOR at 0 degrees C, washed through discontinuous Percoll gradients, and only viable cells were isolated and incubated at 37 degrees C to initiate a synchronous single round of endocytosis. The extent of internalization of this surface-bound 125I-ASOR was unaffected by an ATP depletion to less than 1% of the control level. The rate of internalization of surface-bound ligand was unaffected until the ATP levels decreased to 30% or less; at greater than 98% ATP depletion the initial rate decreased by a maximum of 55% and the kinetics became biphasic. In contrast, continuous endocytosis in the presence of excess ASOR was inhibited by only a 25% decline in cellular ATP content and demonstrated a very sharp threshold response to changing ATP levels. Continuous endocytosis, which requires receptor recycling, was completely inhibited when the total cellular ATP level decreased by only 40%. We conclude that the internalization phase of endocytosis is not dependent on ATP but that the processing and/or externalization phases of the complete receptor cycle are either directly or indirectly dependent on ATP and very sensitive to changes in cellular ATP content.

摘要

大鼠肝细胞中半乳糖基受体介导的125I-去唾液酸血清类黏蛋白(ASOR)的持续内吞作用是一个循环过程。125I-ASOR-受体复合物被内化、加工,配体被降解,而受体返回细胞表面以供再利用。由于一个真正的循环在热力学上需要外部能量输入,我们研究了细胞内ATP水平变化对受体循环功能的影响。在15℃、存在2 mM NaF和0 - 20 mM叠氮化钠的条件下孵育细胞,使肝细胞在进行内吞作用之前不同程度地消耗ATP。采用荧光素酶-荧光素生物发光测定法对细胞ATP含量进行定量。使ATP耗竭的细胞在0℃结合125I-ASOR,通过不连续的Percoll梯度洗涤,仅分离出活细胞并在37℃孵育以启动同步的单轮内吞作用。这种表面结合的125I-ASOR的内化程度不受ATP耗竭至对照水平的1%以下的影响。表面结合配体的内化速率在ATP水平降至30%或更低之前不受影响;当ATP耗竭超过98%时,初始速率最多降低55%,动力学变为双相。相比之下,在存在过量ASOR的情况下持续内吞作用仅在细胞ATP含量下降25%时受到抑制,并且对ATP水平变化表现出非常敏锐的阈值反应。当细胞总ATP水平仅下降40%时,需要受体循环的持续内吞作用就被完全抑制。我们得出结论,内吞作用的内化阶段不依赖于ATP,但完整受体循环的加工和/或外化阶段直接或间接依赖于ATP,并且对细胞ATP含量的变化非常敏感。

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