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Literature DB >> 18620858

Using plasma membrane nanoclusters to build better signaling circuits.

Abstract

Cellular signaling pathways do not simply transmit data; they integrate and process signals to operate as switches, oscillators, logic gates, memory modules and many other types of control system. These complex processing capabilities enable cells to respond appropriately to the myriad of external cues that direct growth and development. The idea that crosstalk and feedback loops are used as control systems in biological signaling networks is well established. Signaling networks are also subject to exquisite spatial regulation, yet how spatial control modulates signal outputs is less well understood. Here, we explore the spatial organization of two different signal transduction circuits: receptor tyrosine kinase activation of the mitogen-activated protein kinase module; and glycosylphosphatidylinositol-anchored receptor activation of phospholipase C. With regards to these pathways, recent results have refocused attention on the crucial role of lipid rafts and plasma membrane nanodomains in signal transmission. We identify common design principals that highlight how the spatial organization of signal transduction circuits can be used as a fundamental control mechanism to modulate system outputs in vivo.

Entities: CellLine Chemical Disease Gene Species

Mesh：

Year: 2008 PMID： 18620858 PMCID： PMC2780343 DOI： 10.1016/j.tcb.2008.05.006

Source DB: PubMed Journal: Trends Cell Biol ISSN： 0962-8924 Impact factor: 20.808

69 in total

1. Single-molecule imaging analysis of Ras activation in living cells.

Authors: Hideji Murakoshi; Ryota Iino; Takeshi Kobayashi; Takahiro Fujiwara; Chika Ohshima; Akihiko Yoshimura; Akihiro Kusumi
Journal: Proc Natl Acad Sci U S A Date: 2004-04-29 Impact factor: 11.205

2. Three separable domains regulate GTP-dependent association of H-ras with the plasma membrane.

Authors: Barak Rotblat; Ian A Prior; Cornelia Muncke; Robert G Parton; Yoel Kloog; Yoav I Henis; John F Hancock
Journal: Mol Cell Biol Date: 2004-08 Impact factor: 4.272

3. The inner side of T cell lipid rafts.

Authors: Giorgia Gri; Barbara Molon; Santos Manes; Tullio Pozzan; Antonella Viola
Journal: Immunol Lett Date: 2004-07-15 Impact factor: 3.685

Review 4. Ras nanoclusters: combining digital and analog signaling.

Authors: Angus Harding; John F Hancock
Journal: Cell Cycle Date: 2007-10-26 Impact factor: 4.534

5. Electrostatic interactions positively regulate K-Ras nanocluster formation and function.

Authors: Sarah J Plowman; Nicholas Ariotti; Andrew Goodall; Robert G Parton; John F Hancock
Journal: Mol Cell Biol Date: 2008-05-05 Impact factor: 4.272

6. Galectin-1 is a novel structural component and a major regulator of h-ras nanoclusters.

Authors: Liron Belanis; Sarah J Plowman; Barak Rotblat; John F Hancock; Yoel Kloog
Journal: Mol Biol Cell Date: 2008-01-30 Impact factor: 4.138

7. Sef is a spatial regulator for Ras/MAP kinase signaling.

Authors: Satoru Torii; Morioh Kusakabe; Takuya Yamamoto; Momoko Maekawa; Eisuke Nishida
Journal: Dev Cell Date: 2004-07 Impact factor: 12.270

8. Nanoscale organization of multiple GPI-anchored proteins in living cell membranes.

Authors: Pranav Sharma; Rajat Varma; R C Sarasij; Karine Gousset; G Krishnamoorthy; Madan Rao; Satyajit Mayor
Journal: Cell Date: 2004-02-20 Impact factor: 41.582

9. A novel switch region regulates H-ras membrane orientation and signal output.

Authors: Daniel Abankwa; Michael Hanzal-Bayer; Nicolas Ariotti; Sarah J Plowman; Alemayehu A Gorfe; Robert G Parton; J Andrew McCammon; John F Hancock
Journal: EMBO J Date: 2008-02-14 Impact factor: 11.598

10. Paxillin: a new vinculin-binding protein present in focal adhesions.

Authors: C E Turner; J R Glenney; K Burridge
Journal: J Cell Biol Date: 1990-09 Impact factor: 10.539

55 in total

1. The tumor necrosis factor receptor stalk regions define responsiveness to soluble versus membrane-bound ligand.

Authors: Christine Richter; Sylvia Messerschmidt; Gerlinde Holeiter; Jessica Tepperink; Sylvia Osswald; Andrea Zappe; Marcus Branschädel; Verena Boschert; Derek A Mann; Peter Scheurich; Anja Krippner-Heidenreich
Journal: Mol Cell Biol Date: 2012-04-30 Impact factor: 4.272

2. Cell type-specific β2-adrenergic receptor clusters identified using photoactivated localization microscopy are not lipid raft related, but depend on actin cytoskeleton integrity.

Authors: Marco Scarselli; Paolo Annibale; Aleksandra Radenovic
Journal: J Biol Chem Date: 2012-03-22 Impact factor: 5.157

10. Nanoscale arrangement of apoptotic ligands reveals a demand for a minimal lateral distance for efficient death receptor activation.

Authors: Julia Ranzinger; Anja Krippner-Heidenreich; Tamas Haraszti; Eva Bock; Jessica Tepperink; Joachim P Spatz; Peter Scheurich
Journal: Nano Lett Date: 2009-12 Impact factor: 11.189

Using plasma membrane nanoclusters to build better signaling circuits.

1. Single-molecule imaging analysis of Ras activation in living cells.

2. Three separable domains regulate GTP-dependent association of H-ras with the plasma membrane.

3. The inner side of T cell lipid rafts.

Review 4. Ras nanoclusters: combining digital and analog signaling.

5. Electrostatic interactions positively regulate K-Ras nanocluster formation and function.

6. Galectin-1 is a novel structural component and a major regulator of h-ras nanoclusters.

7. Sef is a spatial regulator for Ras/MAP kinase signaling.

8. Nanoscale organization of multiple GPI-anchored proteins in living cell membranes.

9. A novel switch region regulates H-ras membrane orientation and signal output.

10. Paxillin: a new vinculin-binding protein present in focal adhesions.

1. The tumor necrosis factor receptor stalk regions define responsiveness to soluble versus membrane-bound ligand.

2. Cell type-specific β2-adrenergic receptor clusters identified using photoactivated localization microscopy are not lipid raft related, but depend on actin cytoskeleton integrity.

3. Mathematical modeling of K-Ras nanocluster formation on the plasma membrane.

4. Roles of the cytoskeleton in regulating EphA2 signals.

5. HIV-1 assembly differentially alters dynamics and partitioning of tetraspanins and raft components.

6. Chloroform alters interleaflet coupling in lipid bilayers: an entropic mechanism.

7. Negative feedback self-regulation contributes to robust and high-fidelity transmembrane signal transduction.

8. Activation of the MAPK module from different spatial locations generates distinct system outputs.

9. Dynamic transition states of ErbB1 phosphorylation predicted by spatial stochastic modeling.

10. Nanoscale arrangement of apoptotic ligands reveals a demand for a minimal lateral distance for efficient death receptor activation.