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C末端标记、跨膜结构域疏水性和内质网滞留基序影响内核膜蛋白emerin的分泌运输。

C-terminal tagging, transmembrane domain hydrophobicity, and an ER retention motif influence the secretory trafficking of the inner nuclear membrane protein emerin.

作者信息

Mella Jessica, Volk Regan, Zaro Balyn, Buchwalter Abigail

机构信息

Cardiovascular Research Institute, University of California, San Francisco, CA, USA.

Department of Pharmaceutical Chemistry, University of California, San Francisco, CA, USA.

出版信息

bioRxiv. 2025 Jan 20:2025.01.19.633811. doi: 10.1101/2025.01.19.633811.

Abstract

The inner nuclear membrane (INM), a subdomain of the endoplasmic reticulum (ER), sequesters hundreds of transmembrane proteins within the nucleus. We previously found that one INM protein, emerin, can evade the INM by secretory transport to the lysosome, where it is degraded. In this work, we used targeted mutagenesis to identify intrinsic sequences that promote or inhibit emerin's secretory trafficking. By manipulating these sequences across several tag and expression level combinations, we now find that emerin's localization is sensitive to C-terminal GFP tagging. While emerin's long, hydrophobic C-terminal transmembrane domain facilitates trafficking to the lysosome, extending its lumenal terminus with a GFP tag biases the protein toward this pathway. In contrast, we identify a conserved ER retention sequence that stabilizes N- and C-terminally tagged emerin by limiting its lysosomal flux. These findings underscore long-standing concerns about tagging artifacts and reveal novel determinants of tail-anchored INM protein targeting.

摘要

内核膜(INM)是内质网(ER)的一个亚结构域,它在细胞核内隔离了数百种跨膜蛋白。我们之前发现,一种内核膜蛋白埃默菌素(emerin)可以通过分泌运输到溶酶体从而避开内核膜,并在那里被降解。在这项研究中,我们使用靶向诱变来鉴定促进或抑制埃默菌素分泌运输的内在序列。通过在几种标签和表达水平组合中操纵这些序列,我们现在发现埃默菌素的定位对C端绿色荧光蛋白(GFP)标签敏感。虽然埃默菌素长的疏水C端跨膜结构域有助于其运输到溶酶体,但用GFP标签延长其腔端会使该蛋白偏向于这条途径。相反,我们鉴定出一个保守的内质网保留序列,该序列通过限制其溶酶体通量来稳定N端和C端标记的埃默菌素。这些发现强调了长期以来对标签假象的担忧,并揭示了尾锚定内核膜蛋白靶向的新决定因素。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6d69/12218776/6ca1194293d3/nihpp-2025.01.19.633811v2-f0001.jpg

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