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本文引用的文献

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Targeting of membrane proteins to endosomes and lysosomes.将膜蛋白靶向内体和溶酶体。
Trends Cell Biol. 1994 Aug;4(8):292-7. doi: 10.1016/0962-8924(94)90220-8.
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Cell surface accumulation of overexpressed hamster lysosomal membrane glycoproteins.过表达的仓鼠溶酶体膜糖蛋白在细胞表面的积累。
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3
In vitro binding of clathrin adaptors to sorting signals correlates with endocytosis and basolateral sorting.网格蛋白衔接蛋白与分选信号的体外结合与内吞作用及基底外侧分选相关。
EMBO J. 1996 Jun 3;15(11):2893-9.
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Cysteine34 of the cytoplasmic tail of the cation-dependent mannose 6-phosphate receptor is reversibly palmitoylated and required for normal trafficking and lysosomal enzyme sorting.阳离子依赖性甘露糖 6-磷酸受体胞质尾的半胱氨酸 34 可发生可逆性棕榈酰化,是正常运输和溶酶体酶分选所必需的。
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Endocytosis of VAMP is facilitated by a synaptic vesicle targeting signal.VAMP的内吞作用由一个突触小泡靶向信号促进。
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Recognition and specificity in protein tyrosine kinase-mediated signalling.蛋白质酪氨酸激酶介导信号传导中的识别与特异性
Trends Biochem Sci. 1995 Nov;20(11):470-5. doi: 10.1016/s0968-0004(00)89103-3.
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A casein kinase II phosphorylation site in the cytoplasmic domain of the cation-dependent mannose 6-phosphate receptor determines the high affinity interaction of the AP-1 Golgi assembly proteins with membranes.阳离子依赖性甘露糖6-磷酸受体胞质结构域中的酪蛋白激酶II磷酸化位点决定了AP-1高尔基体组装蛋白与膜的高亲和力相互作用。
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Cytoplasmic coat proteins involved in endosome function.参与内体功能的细胞质衣被蛋白。
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In vitro binding of plasma membrane-coated vesicle adaptors to the cytoplasmic domain of lysosomal acid phosphatase.质膜包被囊泡衔接蛋白与溶酶体酸性磷酸酶胞质结构域的体外结合
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基于酪氨酸和双亮氨酸信号的蛋白质靶向:不同饱和成分的证据

Protein targeting by tyrosine- and di-leucine-based signals: evidence for distinct saturable components.

作者信息

Marks M S, Woodruff L, Ohno H, Bonifacino J S

机构信息

Cell Biology and Metabolism Branch, National Institute of Child Health and Human Development, National Institutes of Health, Bethesda, Maryland 20892, USA.

出版信息

J Cell Biol. 1996 Oct;135(2):341-54. doi: 10.1083/jcb.135.2.341.

DOI:10.1083/jcb.135.2.341
PMID:8896593
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2121048/
Abstract

Targeting of transmembrane proteins to lysosomes, endosomal compartments, or the trans-Golgi network is largely dependent upon cytoplasmically exposed sorting signals. Among the most widely used signals are those that conform to the tyrosine-based motif, YXXO (where Y is tyrosine, X is any amino acid, and O is an amino acid with a bulky hydrophobic group), and to the di-leucine (or LL) motif. Signals conforming to both motifs have been implicated in protein localization to similar post-Golgi compartments. We have exploited the saturability of sorting to ask whether different YXXO or LL signals use shared components of the targeting machinery. Chimeric proteins containing various cytoplasmic domains and/or targeting signals were overexpressed in HeLa cells by transient transfection. Endogenous transferrin receptor and lysosomal proteins accumulated at the cell surface upon overexpression of chimeric proteins containing functional YXXO targeting signals, regardless of the compartmental destination imparted by the signal. Furthermore, overexpression of these chimeric proteins compromised YXXO-mediated endocytosis and lysosomal delivery. These activities were ablated by mutating the signals or by appending sequences that conformed to the YXXO motif but lacked targeting activity. Interestingly, overexpression of chimeric proteins containing cytoplasmic LL signals failed to induce surface displacement of endogenous YXXO-containing proteins, but did displace other proteins containing LL motifs. Our data demonstrate that: (a) Protein targeting and internalization mediated by either YXXO or LL motifs are saturable processes; (b) common saturable components are used in YXXO-mediated protein internalization and targeting to different post-Golgi compartments; and (c) YXXO- and LL-mediated targeting mechanisms use distinct saturable components.

摘要

跨膜蛋白靶向溶酶体、内体区室或反式高尔基体网络在很大程度上依赖于细胞质暴露的分选信号。最广泛使用的信号之一是符合基于酪氨酸的基序YXXO(其中Y是酪氨酸,X是任何氨基酸,O是具有大的疏水基团的氨基酸)和双亮氨酸(或LL)基序的信号。符合这两种基序的信号已被认为与蛋白质定位到类似的高尔基体后区室有关。我们利用分选的饱和性来探究不同的YXXO或LL信号是否使用靶向机制的共享成分。通过瞬时转染在HeLa细胞中过表达含有各种细胞质结构域和/或靶向信号的嵌合蛋白。当含有功能性YXXO靶向信号的嵌合蛋白过表达时,内源性转铁蛋白受体和溶酶体蛋白在细胞表面积累,而与信号赋予的区室目的地无关。此外,这些嵌合蛋白的过表达损害了YXXO介导的内吞作用和溶酶体递送。通过使信号突变或附加符合YXXO基序但缺乏靶向活性的序列,这些活性被消除。有趣的是,含有细胞质LL信号的嵌合蛋白的过表达未能诱导内源性含YXXO蛋白的表面位移,但确实使其他含LL基序的蛋白发生了位移。我们的数据表明:(a)由YXXO或LL基序介导的蛋白质靶向和内化是可饱和的过程;(b)在YXXO介导的蛋白质内化和靶向到不同的高尔基体后区室中使用共同的可饱和成分;(c)YXXO和LL介导的靶向机制使用不同的可饱和成分。