Your search keyword '"Jenna, Sarah"' showing total 11 results

1. Endocytic protein intersectin-l regulates actin assembly via Cdc42 and N-WASP.

Author

Hussain, Natasha K., Jenna, Sarah, Glogauer, Michael, Quinn, Christopher C., Wasiak, Sylwia, Guipponi, Michel, Antonarakis, Stylianos E., Kay, Brian K., Stossel, Thomas P., Lamarche-Vane, Nathalie, and McPherson, Peter S.

Subjects

*PROTEINS, *ACTIN

Abstract

Intersectin-s is a modular scaffolding protein regulating the formation of clathrin-coated vesicles. In addition to the Eps15 homology (EH) and Src homology 3 (SH3) domains of intersectin-s, the neuronal variant (intersectinI) also has Dbl homology (DH), pleckstrin homology (PH) and C2 domains. We now show that intersectin-I functions through its DH domain as a guanine nucleotide exchange factor (GEF) for Cdc42. In cultured cells, expression of DH-domain-containing constructs cause actin rearrangements specific for Cdc42 activation. Moreover, in vivo studies reveal that stimulation of Cdc42 by intersectin-I accelerates actin assembly via N-WASP and the Arp2/3 complex. N-WASP binds directly to intersectin-I and upregulates its GEF activity, thereby generating GTP-bound Cdc42, a critical activator of N-WASP. These studies reveal a role for intersectin-I in a novel mechanism of N-WASP activation and in regulation of the actin cytoskeleton. [ABSTRACT FROM AUTHOR]

Published

2001

2. AMPK and autophagy control embryonic elongation as part of a RhoA-like morphogenic program in nematode.

Author

Martin, Emmanuel, Bonnamour, Grégoire, and Jenna, Sarah

Subjects

*CAENORHABDITIS elegans, *PROTEIN kinases, *CAENORHABDITIS, *CELL morphology, *CELL migration, *RHO GTPases

Abstract

Autophagy is the process where cytosolic components are digested by the cell. This process is required for cell survival in stressful conditions. It was also shown to control cell division and more recently, cell morphology and migration. We characterized signalling pathways enabling embryonic epidermal cells of the nematode Caenorhabditis elegans to elongate along their antero-posterior axis. Previous studies revealed that epidermal cells can adopt either a RhoA-like or a Rac1-like morphogenic program. We show here that the AMP-activated protein kinase (AMPK) and genes controlling autophagy are required for proper elongation of epidermal cells following the RhoA-like program and are dispensable for other cells. This suggests that AMPK-autophagy is used by the embryo to fuel the most energy-demanding morphogenic processes promoting early elongation. [ABSTRACT FROM AUTHOR]

Published

2020

3. GTPase-Mediated Regulation of the Unfolded Protein Response in Caenorhabditis elegans Is Dependent on the AAA+ ATPase CDC-48.

Author

Caruso, Marie-Elaine, Jenna, Sarah, Bouchecareilh, Marion, Baillie, David L., Boismenu, Daniel, Halawani, Dalia, Latterich, Martin, and Chevet, Eric

Subjects

*CAENORHABDITIS elegans, *CAENORHABDITIS, *APOPTOSIS, *CELL death, *NUCLEIC acids

Abstract

When endoplasmic reticulum (ER) homeostasis is perturbed, an adaptive mechanism is triggered and named the unfolded protein response (UPR). Thus far, three known UPR signaling branches (IRE-1, PERK, and ATF-6) mediate the reestablishment of ER functions but can also lead to apoptosis if ER stress is not alleviated. However, the understanding of the molecular mechanisms integrating the UPR to other ER functions, such as membrane traffic or endomembrane signaling, remains incomplete. We consequently sought to identify new regulators of UPR-dependent transcriptional mechanisms and focused on a family of proteins known to mediate, among other, ER-related functions: the small GTP-binding proteins of the RAS superfamily. To this end, we used transgenic UPR reporter Caenorhabditis elegans strains as a model to specifically silence small-GTPase expression. We show that the Rho subfamily member CRP-1 is an essential component of UPR-induced transcriptional events through its physical and genetic interactions with the AAA+ ATPase CDC-48. In addition, we describe a novel signaling module involving CRP-1 and CDC-48 which may directly link the UPR to DNA remodeling and transcription control. [ABSTRACT FROM AUTHOR]

Published

2008

4. Rac1/RhoA antagonism defines cell-to-cell heterogeneity during epidermal morphogenesis in nematodes.

Author

Martin, Emmanuel, Ouellette, Marie-Hélène, and Jenna, Sarah

Subjects

*EPIDERMIS, *CELL physiology, *GTPASE-activating protein, *CELL imaging, *CAENORHABDITIS elegans, *CELL morphology

Abstract

The antagonism between the GTPases Rac1 and RhoA controls cell-to-cell heterogeneity in isogenic populations of cells in vitro and epithelial morphogenesis in vivo. Its involvement in the regulation of cell-to-cell heterogeneity during epidermal morphogenesis has, however, never been addressed. We used a quantitative cell imaging approach to characterize epidermal morphogenesis at a single-cell level during early elongation of Caenorhabditis elegans embryos. This study reveals that a Rac1-like pathway, involving the Rac/Cdc42 guanine-exchange factor β-PIX/PIX-1 and effector PAK1/ PAK-1, and a RhoA-like pathway, involving ROCK/LET-502, control the remodeling of apical junctions and the formation of basolateral protrusions in distinct subsets of hypodermal cells. In these contexts, protrusions adopt lamellipodia or an amoeboid morphology. We propose that lamella formation may reduce tension building at cell-cell junctions during morphogenesis. Cell-autonomous antagonism between these pathways enables cells to switch between Rac1- and RhoA-like morphogenetic programs. This study identifies the first case of cell-to-cell heterogeneity controlled by Rac1/RhoA antagonism during epidermal morphogenesis. [ABSTRACT FROM AUTHOR]

Published

2016

5. Extracellular Signal-Regulated Kinase 1 Interacts with and Phosphorylates CdGAP at an Important Regulatory Site.

Author

Tcherkezian, Joseph, Danek, Eric I., Jenna, Sarah, Triki, Ibtissem, and Lamarche-Vane, Nathalie

Subjects

*PROTEIN kinases, *GUANOSINE triphosphatase, *CELL proliferation, *G proteins, *CYTOLOGY, *MOLECULAR biology

Abstract

Rho GTPases regulate multiple cellular processes affecting both cell proliferation and cytoskeletal dynamics. Their cycling between inactive GDP- and active GTP-bound states is tightly regulated by guanine nucleotide exchange factors and GTPase-activating proteins (GAPs). We have previously identified CdGAP (for Cdc42 GTPase-activating protein) as a specific GAP for Rac1 and Cdc42. CdGAP consists of an N-terminal RhoGAP domain and a C-terminal proline-rich region. In addition, CdGAP is a member of the impressively large number of mammalian RhoGAP proteins that is well conserved among both vertebrates and invertebrates. In mice, we find two predominant isoforms of CdGAP differentially expressed in specific tissues. We report here that CdGAP is highly phosphorylated in vivo on serine and threonine residues. We find that CdGAP is phosphorylated downstream of the MEK-extracellular signal-regulated kinase (ERK) pathway in response to serum or platelet-derived growth factor stimulation. Furthermore, CdGAP interacts with and is phosphorylated by ERK-1 and RSK-1 in vitro. A putative DEF (docking for ERK FXFP) domain located in the proline-rich region of CdGAP is required for efficient binding and phosphorylation by ERK½. We identify Thr776 as an in vivo target site of ERK½ and as an important regulatory site of CdGAP activity. Together, these data suggest that CdGAP is a novel substrate of ERK½ and mediates cross talk between the Ras/ mitogen-activated protein kinase pathway and regulation of Rac1 activity. [ABSTRACT FROM AUTHOR]

Published

2005

6. Abnormal expression and processing of the proprotein convertases PC1 and PC2 in human colorectal liver metastases.

Author

Tzimas, George N., Chevet, Eric, Jenna, Sarah, Duc Thang Nguyên, Khatib, Abdel M., Marcus, Victoria, Yi Zhang, Chrétien, Michel, Seidah, Nabil, and Metrakos, Peter

Subjects

*PROTEINS, *CARCINOGENESIS, *IMMUNOHISTOCHEMISTRY, *MOLECULAR chaperones, *METASTASIS

Abstract

Background: The family of proprotein convertases has been recently implicated in tumorigenesis and metastasis in animal models. However, these studies have not yet been completely corroborated in human tumors. Methods: Using RT PCR, immunoblot and immunohistochemistry we assessed the presence and the processing patterns of the convertases PC1 and PC2 as well as the PC2 specific chaperone 7B2 in human liver metastases originating from colorectal cancer and compared them to unaffected and normal liver. Furthermore, we assessed the presence and processing profiles of PC1, PC2 and 7B2 in primary colon cancers. Results: mRNA, protein expression, and protein cleavage profiles of proprotein convertases 1 and 2 are altered in liver colorectal metastasis, compared to unaffected and normal liver. Active PC1 protein is overexpressed in tumor, correlating with its mRNA profile. Moreover, the enhanced PC2 processing pattern in tumor correlates with the overexpression of its specific binding protein 7B2. These results were corroborated by immunohistochemistry. The specific and uniform convertase pattern observed in the metastases was present only in a fraction of primary colon cancers. Conclusion: The uniformly altered proprotein convertase profile in liver metastases is observed only in a fraction of primary colon cancers, suggesting possible selection processes involving PCs during metastasis as well as an active role of PCs in liver metastasis. In addition, the exclusive presence of 7B2 in metastatic tumors may represent a new target for early diagnosis, prognosis and/or treatment. [ABSTRACT FROM AUTHOR]

Published

2005

7. Structural and Functional Characterization of a Caenorhabditis elegans Genetic Interaction Network within Pathways.

Author

Boucher, Benjamin, Lee, Anna Y., Hallett, Michael, and Jenna, Sarah

Subjects

*CAENORHABDITIS elegans, *MICROBIAL mutation, *MICROBIAL genomes, *MOLECULAR microbiology, *PROTEIN-protein interactions

Abstract

A genetic interaction (GI) is defined when the mutation of one gene modifies the phenotypic expression associated with the mutation of a second gene. Genome-wide efforts to map GIs in yeast revealed structural and functional properties of a GI network. This provided insights into the mechanisms underlying the robustness of yeast to genetic and environmental insults, and also into the link existing between genotype and phenotype. While a significant conservation of GIs and GI network structure has been reported between distant yeast species, such a conservation is not clear between unicellular and multicellular organisms. Structural and functional characterization of a GI network in these latter organisms is consequently of high interest. In this study, we present an in-depth characterization of ~1.5K GIs in the nematode Caenorhabditis elegans. We identify and characterize six distinct classes of GIs by examining a wide-range of structural and functional properties of genes and network, including co-expression, phenotypical manifestations, relationship with protein-protein interaction dense subnetworks (PDS) and pathways, molecular and biological functions, gene essentiality and pleiotropy. Our study shows that GI classes link genes within pathways and display distinctive properties, specifically towards PDS. It suggests a model in which pathways are composed of PDS-centric and PDS-independent GIs coordinating molecular machines through two specific classes of GIs involving pleiotropic and non-pleiotropic connectors. Our study provides the first in-depth characterization of a GI network within pathways of a multicellular organism. It also suggests a model to understand better how GIs control system robustness and evolution. [ABSTRACT FROM AUTHOR]

Published

2016

8. pix-1 Controls Early Elongation in Parallel with mel-11 and let-502 in Caenorhabditis elegans.

Author

Martin, Emmanuel, Harel, Sharon, Nkengfac, Bernard, Hamiche, Karim, Neault, Mathieu, and Jenna, Sarah

Subjects

*ELONGATION factors (Biochemistry), *CAENORHABDITIS elegans, *CELL morphology, *GUANINE nucleotide exchange factors, *CELLULAR signal transduction, *ANIMAL genetics

Abstract

Cell shape changes are crucial for metazoan development. During Caenorhabditis elegans embryogenesis, epidermal cell shape changes transform ovoid embryos into vermiform larvae. This process is divided into two phases: early and late elongation. Early elongation involves the contraction of filamentous actin bundles by phosphorylated non-muscle myosin in a subset of epidermal (hypodermal) cells. The genes controlling early elongation are associated with two parallel pathways. The first one involves the rho-1/RHOA-specific effector let-502/Rho-kinase and mel-11/myosin phosphatase regulatory subunit. The second pathway involves the CDC42/RAC-specific effector pak-1. Late elongation is driven by mechanotransduction in ventral and dorsal hypodermal cells in response to body-wall muscle contractions, and involves the CDC42/RAC-specific Guanine-nucleotide Exchange Factor (GEF) pix-1, the GTPase ced-10/RAC and pak-1. In this study, pix-1 is shown to control early elongation in parallel with let-502/mel-11, as previously shown for pak-1. We show that pix-1, pak-1 and let-502 control the rate of elongation, and the antero-posterior morphology of the embryos. In particular, pix-1 and pak-1 are shown to control head, but not tail width, while let-502 controls both head and tail width. This suggests that let-502 function is required throughout the antero-posterior axis of the embryo during early elongation, while pix-1/pak-1 function may be mostly required in the anterior part of the embryo. Supporting this hypothesis we show that low pix-1 expression level in the dorsal-posterior hypodermal cells is required to ensure high elongation rate during early elongation. [ABSTRACT FROM AUTHOR]

Published

2014

9. Potential role of the membrane in hERG channel functioning and drug-induced long QT syndrome

Author

Chartrand, Étienne, Arnold, Alexandre A., Gravel, Andrée, Jenna, Sarah, and Marcotte, Isabelle

Subjects

*LONG QT syndrome, *CELL membranes, *POTASSIUM channels, *NUCLEAR magnetic resonance spectroscopy, *MYOCARDIUM, *PHARMACODYNAMICS, *MICELLES

Abstract

Abstract: The human ether-à-go-go related gene (hERG) potassium channels are located in the myocardium cell membrane where they ensure normal cardiac activity. The binding of drugs to this channel, a side effect known as drug-induced (acquired) long QT syndrome (ALQTS), can lead to arrhythmia or sudden cardiac death. The hERG channel is a unique member of the family of voltage-gated K+ channels because of the long extracellular loop connecting its transmembrane S5 helix to the pore helix in the pore domain. Considering the proximal position of the S5-P linker to the membrane surface, we have investigated the interaction of its central segment I583–Y597 with bicelles. Liquid and solid-state NMR experiments as well as circular dichroism results show a strong affinity of the I583–Y597 segment for the membrane where it would sit on the surface with no defined secondary structure. A structural dependence of this segment on model membrane composition was observed. A helical conformation is favoured in detergent micelles and in the presence of negative charges. Our results suggest that the interaction of the S5-P linker with the membrane could participate in the stabilization of transient channel conformations, but helix formation would be triggered by interactions with other hERG domains. Because potential drug binding sites on the S5-P linker have been identified, we have explored the role of this segment in ALQTS. Four LQTS-liable drugs were studied which showed more affinity for the membrane than this hERG segment. Our results, therefore, identify two possible roles for the membrane in channel functioning and ALQTS. [ABSTRACT FROM AUTHOR]

Published

2010

10. Searching for Signaling Balance through the Identification of Genetic Interactors of the Rab Guanine-Nucleotide Dissociation Inhibitor gdi-1.

Author

Lee, Anna Y., Perreault, Richard, Harel, Sharon, Boulier, Elodie L., Suderman, Matthew, Hallett, Michael, and Jenna, Sarah

Subjects

*GENES, *GENETIC mutation, *DISSOCIATION (Psychology), *HOMEOSTASIS, *SYMPTOMS, *CAENORHABDITIS elegans, *INTELLECTUAL disabilities, *GENE mapping, *ANIMAL models in research

Abstract

Background: The symptoms of numerous diseases result from genetic mutations that disrupt the homeostasis maintained by the appropriate integration of signaling gene activities. The relationships between signaling genes suggest avenues through which homeostasis can be restored and disease symptoms subsequently reduced. Specifically, disease symptoms caused by loss-of-function mutations in a particular gene may be reduced by concomitant perturbations in genes with antagonistic activities. Methodology/Principal Findings: Here we use network-neighborhood analyses to predict genetic interactions in Caenorhabditis elegans towards mapping antagonisms and synergisms between genes in an animal model. Most of the predicted interactions are novel, and the experimental validation establishes that our approach provides a gain in accuracy compared to previous efforts. In particular, we identified genetic interactors of gdi-1, the orthologue of GDI1, a gene associated with mental retardation in human. Interestingly, some gdi-1 interactors have human orthologues with known neurological functions, and upon validation of the interactions in mammalian systems, these orthologues would be potential therapeutic targets for GDI1-associated neurological disorders. We also observed the conservation of a gdi-1 interaction between different cellular systems in C. elegans, suggesting the involvement of GDI1 in human muscle degeneration. Conclusions/Significance: We developed a novel predictor of genetic interactions that may have the ability to significantly streamline the identification of therapeutic targets for monogenic disorders involving genes conserved between human and C. elegans. [ABSTRACT FROM AUTHOR]

Published

2010

11. C. elegans ORFeome version 1.1: experimental verification of the genome annotation and resource for proteome-scale protein expression.

Author

Reboul, Jerome, Vaglio, Philippe, Rual, Jean-Francois, Lamesch, Philippe, Martinez, Monica, Armstrong, Christopher M., Li, Siming, Jacotot, Laurent, Bertin, Nicolas, Janky, Rekin's, Moore, Troy, Hudson, James R., Hartley, James L., Brasch, Michael A., Vandenhaute, Jean, Boulton, Simon, Endress, Gregory A., Jenna, Sarah, and Chevet, Eric

Subjects

*GENOMES, *CAENORHABDITIS, *GENES, *GENETICS, *RHABDITIDAE, *PROTEINS

Abstract

To verify the genome annotation and to create a resource to functionally characterize the proteome, we attempted to Gateway-clone all predicted protein-encoding open reading frames (ORFs), or the 'ORFeome,' of Caenorhabditis elegans. We successfully cloned approximately 12,000 ORFs (ORFeome 1.1), of which roughly 4,000 correspond to genes that are untouched by any cDNA or expressed-sequence tag (EST). More than 504570360f predicted genes needed corrections in their intron-exon structures. Notably, approximately 11,000 C. elegans proteins can now be expressed under many conditions and characterized using various high-throughput strategies, including large-scale interactome mapping. We suggest that similar ORFeome projects will be valuable for other organisms, including humans. [ABSTRACT FROM AUTHOR]

Published

2003