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细胞中部分胞吐内容物释放和化学物质运输到纳米囊泡的可视化。

Visualization of Partial Exocytotic Content Release and Chemical Transport into Nanovesicles in Cells.

机构信息

Department of Chemistry and Molecular Biology, University of Gothenburg, Gothenburg SE-412 96, Sweden.

Department of Chemistry and Chemical Engineering, Chalmers University of Technology, Gothenburg SE-412 96, Sweden.

出版信息

ACS Nano. 2022 Mar 22;16(3):4831-4842. doi: 10.1021/acsnano.2c00344. Epub 2022 Feb 21.

Abstract

For decades, "all-or-none" and "kiss-and-run" were thought to be the only major exocytotic release modes in cell-to-cell communication, while the significance of partial release has not yet been widely recognized and accepted owing to the lack of direct evidence for exocytotic partial release. Correlative imaging with transmission electron microscopy and NanoSIMS imaging and a dual stable isotope labeling approach was used to study the cargo status of vesicles before and after exocytosis; demonstrating a measurable loss of transmitter in individual vesicles following stimulation due to partial release. Model secretory cells were incubated with C-labeled l-3,4-dihydroxyphenylalanine, resulting in the loading of C-labeled dopamine into their vesicles. A second label, di--desethylamiodarone, having the stable isotope I, was introduced during stimulation. A significant drop in the level of C-labeled dopamine and a reduction in vesicle size, with an increasing level of I, was observed in vesicles of stimulated cells. Colocalization of C and I in several vesicles was observed after stimulation. Thus, chemical visualization shows transient opening of vesicles to the exterior of the cell without full release the dopamine cargo. We present a direct calculation for the fraction of neurotransmitter release from combined imaging data. The average vesicular release is 60% of the total catecholamine. An important observation is that extracellular molecules can be introduced to cells during the partial exocytotic release process. This nonendocytic transport process appears to be a general route of entry that might be exploited pharmacologically.

摘要

几十年来,“全或无”和“亲吻并逃逸”被认为是细胞间通讯中唯一的主要胞吐释放模式,而由于缺乏胞吐部分释放的直接证据,部分释放的意义尚未得到广泛认可和接受。利用透射电子显微镜和 NanoSIMS 成像的相关成像和双重稳定同位素标记方法,研究了胞吐前后囊泡的货物状态;证明由于部分释放,刺激后单个囊泡中的递质可测量丢失。将 C 标记的 l-3,4-二羟基苯丙氨酸孵育模型分泌细胞,导致 C 标记的多巴胺加载到其囊泡中。在刺激过程中引入了第二个标记物,具有稳定同位素 I 的二-去乙基胺碘酮。在刺激的细胞中,观察到 C 标记的多巴胺水平显著下降,囊泡尺寸减小,而 I 的水平增加。刺激后观察到几个囊泡中 C 和 I 的共定位。因此,化学可视化显示囊泡短暂向细胞外部开放,而多巴胺货物没有完全释放。我们根据联合成像数据直接计算了神经递质释放的分数。囊泡释放的平均水平为总儿茶酚胺的 60%。一个重要的观察结果是,细胞外分子可以在部分胞吐释放过程中被引入细胞。这种非胞吞转运过程似乎是一种普遍的进入途径,可能在药理学上被利用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5b25/8945366/6327e407cf3e/nn2c00344_0001.jpg

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