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受磷蛋白和肌浆脂质蛋白通过从内质网-高尔基体中间区室的回收而维持在内质网中。

Phospholamban and sarcolipin are maintained in the endoplasmic reticulum by retrieval from the ER-Golgi intermediate compartment.

作者信息

Butler John, Lee Anthony G, Wilson David I, Spalluto Cosma, Hanley Neil A, East J Malcolm

机构信息

School of Biological Sciences, University of Southampton, Southampton SO16 7PX, UK.

出版信息

Cardiovasc Res. 2007 Apr 1;74(1):114-23. doi: 10.1016/j.cardiores.2007.01.006. Epub 2007 Jan 13.

Abstract

OBJECTIVE

Phospholamban and sarcolipin are small transmembrane proteins that modulate cardiac contractility through their interaction with the sarcoplasmic reticulum (SR) calcium pumps (SERCAs). We have examined the hypothesis that phospholamban and sarcolipin are maintained in the SR by a process of retrieval from post-SR compartments and the role of their transmembrane domains in targeting.

METHODS

Antibodies directed against phospholamban and protein markers of the endoplasmic reticulum/Golgi intermediate compartment (ERGIC) and the trans-Golgi were used in fluorescence microscopy studies of cultured human fetal cardiac myocytes. In addition, sarcolipin and phospholamban were tagged at the N-terminus with enhanced-green-fluorescent protein (EGFP) and expressed in COS 7 cells. The EGFP-tagged constructs were localised using fluorescence microscopy and cell fractionation. The length of the transmembrane domains of phospholamban and sarcolipin were extended and the effect on cellular location was also examined.

RESULTS

In fetal cardiac myocytes phospholamban was located in the SR and the ERGIC, but did not migrate to the trans-Golgi network. Tagged-phospholamban and sarcolipin were located in the endoplasmic reticulum (ER) of COS 7 cells indicating that their targeting was unaffected by the EGFP tag. Significant proportions of the tagged phospholamban and sarcolipin were also located in the ERGIC but not in the trans-Golgi. Increasing the length of the transmembranous domains of EGFP-tagged phospholamban and sarcolipin resulted in their mis-targeting to the plasma membrane.

CONCLUSIONS

Phospholamban and sarcolipin are maintained in the SR/ER by a process that includes their retrieval from the ERGIC following their passage from the SR/ER into the ERGIC. The transmembrane domains of phospholamban and sarcolipin are involved in the retrieval process.

摘要

目的

受磷蛋白和肌浆脂质蛋白是小的跨膜蛋白,它们通过与肌浆网(SR)钙泵(SERCA)相互作用来调节心脏收缩力。我们检验了这样一个假说,即受磷蛋白和肌浆脂质蛋白通过从SR后区室的回收过程而维持在SR中,以及它们的跨膜结构域在靶向定位中的作用。

方法

针对受磷蛋白以及内质网/高尔基体中间区室(ERGIC)和反式高尔基体的蛋白质标志物的抗体,用于培养的人胎儿心肌细胞的荧光显微镜研究。此外,肌浆脂质蛋白和受磷蛋白在N端用增强型绿色荧光蛋白(EGFP)标记,并在COS 7细胞中表达。使用荧光显微镜和细胞分级分离对EGFP标记的构建体进行定位。延长受磷蛋白和肌浆脂质蛋白跨膜结构域的长度,并检测其对细胞定位的影响。

结果

在胎儿心肌细胞中,受磷蛋白位于SR和ERGIC中,但未迁移至反式高尔基体网络。标记的受磷蛋白和肌浆脂质蛋白位于COS 7细胞的内质网(ER)中,表明它们的靶向定位不受EGFP标签的影响。相当一部分标记的受磷蛋白和肌浆脂质蛋白也位于ERGIC中,但不在反式高尔基体中。增加EGFP标记的受磷蛋白和肌浆脂质蛋白跨膜结构域的长度会导致它们错误定位于质膜。

结论

受磷蛋白和肌浆脂质蛋白通过一个过程维持在SR/ER中,该过程包括它们从SR/ER进入ERGIC后从ERGIC回收。受磷蛋白和肌浆脂质蛋白的跨膜结构域参与了回收过程。

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