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利用绿色荧光蛋白融合蛋白对构巢曲霉中野生型和突变型I类肌球蛋白蛋白进行定位。

Localization of wild type and mutant class I myosin proteins in Aspergillus nidulans using GFP-fusion proteins.

作者信息

Yamashita R A, Osherov N, May G S

机构信息

Division of Pathology and Laboratory Medicine, University of Texas, M.D. Anderson Cancer Center, Houston, TX 77030, USA.

出版信息

Cell Motil Cytoskeleton. 2000 Feb;45(2):163-72. doi: 10.1002/(SICI)1097-0169(200002)45:2<163::AID-CM7>3.0.CO;2-D.

Abstract

We have examined the distribution of MYOA, the class I myosin protein of the filamentous fungus Aspergillus nidulans, as a GFP fusion protein. Wild type GFP-MYOA expressed from the myoA promoter is able to rescue a conditional myoA null mutant. Growth of a strain expressing GFP-MYOA as the only class I myosin was approximately 50% that of a control strain, demonstrating that the fusion protein retains substantial myosin function. The distribution of the wild type GFP-MYOA fusion is enriched in growing hyphal tips and at sites of septum formation. In addition, we find that GFP-MYOA is also found in patches at the cell cortex. We have also investigated the effects of deletion or truncation mutations in the tail domain on MYOA localization. Mutant GFP-MYOA fusions that lacked either the C-terminal SH3 or a portion of the C-terminal proline-rich domain had subcellular distributions like wild type MYOA, consistent with their ability to complement a myoA null mutant. In contrast, mutants lacking all of the C-terminal proline-rich domain or the TH-1-like domain were mainly localized diffusely throughout the cytoplasm, but could less frequently be found in patches, and were unable to complement a myoA null mutant. The GFP-MYOA DeltaIQ mutant was localized into large bright fluorescent patches in the cytoplasm. This mutant protein was subsequently found to be insoluble.

摘要

我们研究了丝状真菌构巢曲霉的I类肌球蛋白蛋白MYOA作为绿色荧光蛋白(GFP)融合蛋白的分布情况。从肌动蛋白A(myoA)启动子表达的野生型GFP-MYOA能够挽救条件性myoA基因敲除突变体。将GFP-MYOA作为唯一的I类肌球蛋白进行表达的菌株的生长速度约为对照菌株的50%,这表明融合蛋白保留了相当程度的肌球蛋白功能。野生型GFP-MYOA融合蛋白的分布在生长的菌丝尖端和隔膜形成部位富集。此外,我们发现GFP-MYOA在细胞皮层的斑块中也有分布。我们还研究了尾部结构域的缺失或截短突变对MYOA定位的影响。缺少C端SH3结构域或部分C端富含脯氨酸结构域的突变型GFP-MYOA融合蛋白具有与野生型MYOA相似的亚细胞分布,这与其能够互补myoA基因敲除突变体的能力一致。相比之下,缺少全部C端富含脯氨酸结构域或TH-1样结构域的突变体主要在整个细胞质中呈弥散分布,但在斑块中较少见,并且无法互补myoA基因敲除突变体。GFP-MYOA ΔIQ突变体定位于细胞质中的大的明亮荧光斑块中。随后发现这种突变蛋白是不溶性的。

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