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用于绘制亲环蛋白相互作用组图谱的邻近标记和正交纳米抗体下拉(ID-oPD)方法揭示了亲环蛋白在蛋白质稳态中的假定作用。

Proximity labeling and orthogonal nanobody pulldown (ID-oPD) approaches to map the spinophilin interactome uncover a putative role for spinophilin in protein homeostasis.

作者信息

Claeboe Emily T, Blake Keyana L, Shah Nikhil R, Morris Cameron W, Hens Basant, Atwood Brady K, Absalon Sabrina, Mosley Amber L, Doud Emma H, Baucum Anthony J

机构信息

Department of Biochemistry, Molecular Biology, and Pharmacology, Indiana University School of Medicine.

Post-Baccalaureate Research Education Program, Indiana University Indianapolis.

出版信息

bioRxiv. 2025 Jan 23:2025.01.23.634546. doi: 10.1101/2025.01.23.634546.

Abstract

Spinophilin is a dendritic spine enriched scaffolding and protein phosphatase 1 targeting protein. To detail spinophilin interacting proteins, we created an Ultra-ID and ALFA-tagged spinophilin encoding construct that permits proximity labeling and orthogonal nanobody pulldown (ID-oPD) of spinophilin-associated protein complexes in heterologous cells. We identified 614 specific, and 312 specific and selective, spinophilin interacting proteins in HEK293 cells and validated a subset of these using orthogonal approaches. Many of these proteins are involved in mRNA processing and translation. In the brain, we determined that spinophilin mRNA is highly neuropil localized and that spinophilin may normally function to limit its own expression but promote the expression of other PSD-associated proteins. Overall, our use of an ID-oPD approach uncovers a novel putative role for spinophilin in mRNA translation and synaptic protein expression specifically within dendritic spines.

摘要

亲嗜素是一种富含树突棘的支架蛋白和蛋白磷酸酶1靶向蛋白。为了详细研究亲嗜素相互作用蛋白,我们构建了一个带有超分辨成像标签(Ultra-ID)和亲和标签(ALFA-tag)的亲嗜素编码构建体,该构建体能够对异源细胞中与亲嗜素相关的蛋白复合物进行邻近标记和正交纳米抗体下拉实验(ID-oPD)。我们在人胚肾293(HEK293)细胞中鉴定出614种特异性的以及312种特异性和选择性的亲嗜素相互作用蛋白,并使用正交方法验证了其中一部分。这些蛋白中有许多参与mRNA加工和翻译过程。在大脑中,我们确定亲嗜素mRNA高度定位于神经毡,并且亲嗜素通常可能发挥限制自身表达的作用,但会促进其他突触后致密区(PSD)相关蛋白的表达。总体而言,我们使用ID-oPD方法揭示了亲嗜素在mRNA翻译和突触蛋白表达中一种新的假定作用,特别是在树突棘内。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/977f/11785182/fb17996027ca/nihpp-2025.01.23.634546v1-f0001.jpg

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