Lipid raft targeting of the TC10 amino terminal domain is responsible for disruption of adipocyte cortical actin

Hou JCQ.; Pessin JE.

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Lipid raft targeting of the TC10 amino terminal domain is responsible for disruption of adipocyte cortical actin

机译：TC10氨基末端结构域的脂筏靶向导致脂肪细胞皮层肌动蛋白的破坏。

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Overexpression of the Rho family member TC10alpha, disrupts adipocyte cortical actin structure and inhibits insulin-stimulated GLUT4 translocation when targeted to lipid raft microdomains. This appears to be independent of effecter domain function because overexpression of the wild-type (TC10/WT), constitutively GTP-bound (TC10/Q75L), and constitutively GDP bound (TC10/ T31N) all inhibit adipocyte cortical actin structure and GLUT4 translocation. To examine the structural determinants responsible for these effects, we generated a series of chimera proteins between TC10 with that of H-Ras and K-Ras. Chimera containing the 79 (TC10-79/1-1-Ras), 41 (TC10-41/H-Ras), or 16 (TC10-16/H-Ras) amino acids of the TC10 amino terminal extension fused to H-Ras disrupted cortical actin and inhibited insulin-stimulated GLUT4 translocation. In contrast, the same amino terminal TC10 extensions fused to K-Ras had no significant effect on either GLUT4 translocation or cortical actin structure. Similarly, expression of TC100 was without effect whereas fusion of the amino terminal 8 amino acid of TC10alpha onto TC10beta resulted in an inhibition of insulin-stimulated GLUT4 translocation. Within the amino terminal extension point mutation analysis demonstrated that both a GAG and GPG sequences when lipid raft targeted was essential for these effects. Furthermore, expression of the amino terminal TC10 deletions DeltaNT-TC10/WT or DeltaNT-TC10/T31N had no detectable effect on cortical actin organization and did not perturb insulin-stimulated GLUT4 translocation. Surprisingly, however, expression of DeltaNT-TC10/Q75L remained fully capable of inhibiting insulin-stimulated GLUT4 translocation without affecting cortical actin. These data demonstrate that inhibitory effect of TC10 overexpression on adipocyte cortical actin organization is due to the specific lipid raft targeting of the unusual TC10 amino terminal extension. [References: 74]

机译：Rho家族成员TC10alpha的过表达，当靶向脂质筏微结构域时，会破坏脂肪细胞皮层肌动蛋白结构并抑制胰岛素刺激的GLUT4易位。这似乎与效应域功能无关，因为野生型（TC10 / WT），组成型GTP结合（TC10 / Q75L）和GDP组成型（TC10 / T31N）的过表达均抑制脂肪细胞皮质肌动蛋白结构和GLUT4易位。为了检查负责这些作用的结构决定簇，我们在TC10与H-Ras和K-Ras之间产生了一系列嵌合蛋白。嵌合体，其包含与H-融合的TC10氨基末端延伸的79个（TC10-79 / 1-1-Ras），41个（TC10-41 / H-Ras）或16个（TC10-16 / H-Ras）氨基酸。 Ras破坏了皮质肌动蛋白并抑制了胰岛素刺激的GLUT4易位。相比之下，与K-Ras融合的相同氨基末端TC10延伸对GLUT4易位或皮质肌动蛋白结构均无显着影响。类似地，TC100的表达没有作用，而TC10alpha的氨基末端8个氨基酸融合到TC10beta上导致了胰岛素刺激的GLUT4易位的抑制。在氨基末端延伸点内的突变分析表明，脂筏靶向时的GAG和GPG序列对于这些作用至关重要。此外，氨基末端TC10缺失DeltaNT-TC10 / WT或DeltaNT-TC10 / T31N的表达对皮质肌动蛋白组织没有可检测的影响，并且不干扰胰岛素刺激的GLUT4易位。然而，令人惊讶的是，DeltaNT-TC10 / Q75L的表达仍然完全能够抑制胰岛素刺激的GLUT4易位而不影响皮质肌动蛋白。这些数据表明，TC10过表达对脂肪细胞皮质肌动蛋白组织的抑制作用是由于靶向非常规TC10氨基末端延伸的脂质筏所致。 [参考：74]

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《Molecular biology of the cell》 |2003年第9期|共14页
作者
Hou JCQ.; Pessin JE.;
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正文语种 eng
中图分类分子生物学;
关键词
Stimulated glut4 translocation; Activated protein-kinase; Phosphatidylinositol 3-kinase activation; Glucose-transporter translocation; Insulin-signaling pathway; 3t3-l1 adipocytes; Plasma-membrane; Phosphoinositide 3-kinase; 3t3l1 adipocytes; Rat adipocytes;

机译：刺激的glut4易位;活化的蛋白激酶;磷脂酰肌醇3激酶激活;葡萄糖转运蛋白易位;胰岛素信号通路;3t3-l1脂肪细胞;血浆膜;磷酸肌醇3激酶;3t3l1脂肪细胞;大鼠脂肪细胞;
入库时间 2022-08-18 11:54:50

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专利

1. Lipid raft targeting of the TC10 amino terminal domain is responsible for disruption of adipocyte cortical actin [J] . Hou JCQ., Pessin JE. Molecular biology of the cell . 2003,第9期

机译：TC10氨基末端结构域的脂筏靶向导致脂肪细胞皮层肌动蛋白的破坏。
2. Acetylation is the most abundant actin modification in Entamoeba histolytica Entamoeba histolyticaEntamoeba histolytica and modifications of actin's amino‐terminal domain change cytoskeleton activities [J] . Hernández‐Cuevas Nora Adriana, Jhingan Gagan Deep, Petropolis Debora, Cellular microbiology . 2019,第4期

机译：乙酰化是 entamoeba组织olytica中最丰富的肌动蛋白修饰术中最丰富的肌动蛋白修饰术语 entamoeba组织olytica entamoeba组织olytica和actin的氨基末端结构域的修饰改变细胞骨架活性
3. Molecular basis of the functional podocin-nephrin complex: mutations in the NPHS2 gene disrupt nephrin targeting to lipid raft microdomains. [J] . Huber TB, Simons M, Hartleben B, Human Molecular Genetics . 2003,第24期

机译：功能性podocin-nephrin复合物的分子基础：NPHS2基因中的突变破坏了将nephrin靶向脂质筏微结构域。
4. Cholera Toxin B Subunit Crosslinks Rafts Causing Confinement by Cortical Actin [C] . C. A. Day, A. K. Kenworthy International Metallographic Society Annual meeting;Microscopy Society of America Annual Meeting;Microanalysis Society Annual meeting . 2011

机译：霍乱毒素B亚基交联筏由皮质肌动蛋白的限制。
5. Contributions of amino-terminal domains to NMDA receptor functions. [D] . Ruvio, Stacy Ann. 2010

机译：氨基末端结构域对NMDA受体功能的贡献。
6. Lipid Raft Targeting of the TC10 Amino Terminal Domain Is Responsible for Disruption of Adipocyte Cortical Actin [O] . June Chunqiu Hou, Jeffrey E. Pessin 2003

机译：TC10氨基末端域的脂筏靶向是负责脂肪细胞皮层肌动蛋白的破坏。
7. Lipid Raft Targeting of the TC10 Amino Terminal Domain Is Responsible for Disruption of Adipocyte Cortical Actin [O] . Chunqiu Hou, June, Pessin, Jeffrey E. 2003

机译：TC10氨基末端域的脂筏靶向是负责脂肪细胞皮层肌动蛋白的破坏。

Lipid raft targeting of the TC10 amino terminal domain is responsible for disruption of adipocyte cortical actin

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