Your search keyword '"Zaidel-Bar, Ronen"' showing total 8 results

1. Opening the floodgates: proteomics and the integrin adhesome.

Author

Geiger T and Zaidel-Bar R

Subjects

Animals, Extracellular Matrix metabolism, Focal Adhesions genetics, Focal Adhesions metabolism, Humans, Integrins chemistry, Proteomics, Signal Transduction, Cell Adhesion, Integrins metabolism, Proteome metabolism

Abstract

Cell biologists studying cell adhesion have already figured out that cell-extracellular matrix connections, mediated by integrin receptors, are diverse and extremely complex structures. Dozens of adaptors-linking integrins with the cytoskeleton, and numerous enzymes and signaling proteins-regulating adhesion site dynamics, collectively referred to as the integrin adhesome, cooperate in mediating adhesion and activating specific signaling networks. Recent proteomic studies indicate that the known adhesome complexity is just the tip of the iceberg. In each existing category of molecular function the number of candidate components more than double the known components and several new categories are suggested. Proteomic analysis of different integrin heterodimers points to integrin-specific variations in composition and analysis of adhesion complexes under varying tension regimes highlights the force-dependent recruitment of different components, most notably LIM domain proteins., (Copyright © 2012 Elsevier Ltd. All rights reserved.)

Published

2012

2. The switchable integrin adhesome.

Author

Zaidel-Bar R and Geiger B

Subjects

Animals, Cell Adhesion, Humans, Extracellular Matrix metabolism, Integrins metabolism, Signal Transduction

Published

2010

3. Evolution of complexity in the integrin adhesome.

Author

Zaidel-Bar R

Subjects

Animals, Cell Adhesion physiology, Humans, Integrins metabolism

Abstract

Integrin-mediated adhesion is as ancient as multicellularity, but it was not always as complex as it is in humans. Here, I examine the extent of conservation of 192 adhesome proteins across the genomes of nine model organisms spanning one and a half billion years of evolution. The work reveals that Rho GTPases, lipid- and serine/threonine-kinases, and phosphatases existed before integrins, but tyrosine phosphorylation developed concomitant with integrins. The expansion of specific functional groups such as GAPs, GEFs, adaptors, and receptors is demonstrated, along with the expansion of specific protein domains, such as SH3, PH, SH2, CH, and LIM. Expansion is due to gene duplication and creation of families of paralogues. Apparently, these paralogues share few partners and create new sets of interactions, thus increasing specificity and the repertoire of integrin-mediated signaling. Interestingly, the average number of interactions positively correlates with the evolutionary age of proteins. While shedding light on the evolution of adhesome complexity, this analysis also highlights the relevance and creates a framework for studying integrin-mediated adhesion in simpler model organisms.

Published

2009

4. Functional atlas of the integrin adhesome.

Author

Zaidel-Bar R, Itzkovitz S, Ma'ayan A, Iyengar R, and Geiger B

Subjects

Animals, Cytoskeleton metabolism, Databases, Factual, Integrins genetics, Signal Transduction physiology, Cell Adhesion physiology, Cell-Matrix Junctions physiology, Integrins metabolism

Abstract

A detailed depiction of the 'integrin adhesome', consisting of a complex network of 156 components linked together and modified by 690 interactions is presented. Different views of the network reveal several functional 'subnets' that are involved in switching on or off many of the molecular interactions within the network, consequently affecting cell adhesion, migration and cytoskeletal organization. Examination of the adhesome network motifs reveals a relatively small number of key motifs, dominated by three-component complexes in which a scaffolding molecule recruits both a signalling molecule and its downstream target. We discuss the role of the different network modules in regulating the structural and signalling functions of cell-matrix adhesions.

Published

2007

5. Molting-specific downregulation of C. elegans body-wall muscle attachment sites: The role of RNF-5 E3 ligase

Author

Zaidel-Bar, Ronen, Miller, Shahar, Kaminsky, Rachel, and Broday, Limor

Subjects

*MOLTING, *CAENORHABDITIS elegans, *LIGASES, *MUSCLE cells, *GENE expression, *INTEGRINS, *ECDYSIS

Abstract

Abstract: Repeated molting of the cuticula is an integral part of arthropod and nematode development. Shedding of the old cuticle takes place on the surface of hypodermal cells, which are also responsible for secretion and synthesis of a new cuticle. Here, we use the model nematode Caenorhabditis elegans to show that muscle cells, laying beneath and mechanically linked to the hypodermis, play an important role during molting. We followed the molecular composition and distribution of integrin mediated adhesion structures called dense bodies (DB), which indirectly connect muscles to the hypodermis. We found the concentration of two DB proteins (PAT-3/β-integrin and UNC-95) to decrease during the quiescent phase of molting, concomitant with an apparent increase in lateral movement of the DB. We show that levels of the E3-ligase RNF-5 increase specifically during molting, and that RNF-5 acts to ubiquitinate the DB protein UNC-95. Persistent high levels of RNF-5 driven by a heatshock or unc-95 promoter lead to failure of ecdysis, and in non-molting worms to a progressive detachment of the cuticle from the hypodermis. These observations indicate that increased DB dynamics characterizes the lethargus phase of molting in parallel to decreased levels of DB components and that temporal expression of RNF-5 contributes to an efficient molting process. [Copyright &y& Elsevier]

Published

2010

6. Job-splitting among integrins.

Author

Zaidel-Bar, Ronen

Subjects

*INTEGRINS, *CELL adhesion molecules, *MYOSIN genetics, *CONTRACTILITY (Biology), *ACTIN research

Abstract

How different integrin receptors for the same extracellular ligand transduce distinct cellular responses is unclear. The characterization of the class-specific adhesomes of β1 and αV integrins now shows that whereas αV integrins promote unbranched actin polymerization, β1 integrins induce myosin-II-dependent contractility, and both integrin subtypes synergistically mediate rigidity sensing. [ABSTRACT FROM AUTHOR]

Published

2013

7. A paxillin tyrosine phosphorylation switch regulates the assembly and form of cell-matrix adhesions.

Author

Zaidel-Bar, Ronen, Milo, Ron, Kam, Zvi, and Geiger, Benjamin

Subjects

*CELL adhesion, *INTEGRINS, *PHOSPHORYLATION, *TYROSINE, *FIBRONECTINS, *BLOOD proteins

Abstract

Diverse cellular processes are carried out by distinct integrin-mediated adhesions. Cell spreading and migration are driven by focal complexes; robust adhesion to the extracellular matrix by focal adhesions; and matrix remodeling by fibrillar adhesions. The mechanism(s) regulating the spatio-temporal distribution and dynamics of the three types of adhesion are unknown. Here, we combine live-cell imaging, labeling with phosphospecific-antibodies and overexpression of a novel tyrosine phosphomimetic mutant of paxillin, to demonstrate that the modulation of tyrosine phosphorylation of paxillin regulates both the assembly and turnover of adhesion sites. Moreover, phosphorylated paxillin enhanced lamellipodial protrusions, whereas non-phosphorylated paxillin was essential for fibrillar adhesion formation and for fibronectin fibrillogenesis. We further show that focal adhesion kinase preferentially interacted with the tyrosine phosphomimetic paxillin and its recruitment is implicated in high turnover of focal complexes and translocation of focal adhesions. We created a mathematical model that recapitulates the salient features of the measured dynamics, and conclude that tyrosine phosphorylation of the adaptor protein paxillin functions as a major switch, regulating the adhesive phenotype of cells. [ABSTRACT FROM AUTHOR]

Published

2007

8. Directed cell invasion and asymmetric adhesion drive tissue elongation and turning in C. elegans gonad morphogenesis.

Author

Agarwal, Priti, Shemesh, Tom, and Zaidel-Bar, Ronen

Subjects

*GONADS, *CAENORHABDITIS elegans, *TISSUE adhesions, *BENDING moment, *MORPHOGENESIS, *EXTRACELLULAR matrix

Abstract

Development of the C. elegans gonad has long been studied as a model of organogenesis driven by collective cell migration. A somatic cell named the distal tip cell (DTC) is thought to serve as the leader of following germ cells; yet, the mechanism for DTC propulsion and maneuvering remains elusive. Here, we demonstrate that the DTC is not self-propelled but rather is pushed by the proliferating germ cells. Proliferative pressure pushes the DTC forward, against the resistance of the basement membrane in front. The DTC locally secretes metalloproteases that degrade the impeding membrane, resulting in gonad elongation. Turning of the gonad is achieved by polarized DTC-matrix adhesions. The asymmetrical traction results in a bending moment on the DTC. Src and Cdc42 regulate integrin adhesion polarity, whereas an external netrin signal determines DTC orientation. Our findings challenge the current view of DTC migration and offer a distinct framework to understand organogenesis. [Display omitted] • Distal tip cell (DTC) in C. elegans hermaphrodite gonad is pushed by proliferating germ cells • Extracellular matrix (ECM) degradation by the DTC directs gonad elongation • DTC-ECM adhesion polarity drives gonadal turning • CDC-42 and SRC regulate DTC integrin polarity during the turn Agarwal et al. investigate the mechanics of C. elegans gonad morphogenesis in this study. They show that tissue elongation results from leader cell invasion powered by localized matrix degradation and the proliferative pressure of follower cells, while asymmetric cell-ECM adhesion creates torque that drives the U-turning of the gonad. [ABSTRACT FROM AUTHOR]

Published

2022