Serine phosphorylation of paxillin by heregulin-β1: role of p38 mitogen activated protein kinase

Vadlamudi, Ratna K.; Adam, Liana; Talukder, Amjad H.; Mendelsohn, John; Kumar, Rakesh

doi:10.1038/sj.onc.1203163

Cited by 61 publications

(60 citation statements)

References 50 publications

(48 reference statements)

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“…Additionally, cells expressing this mutant paxillin exhibit a defect in spreading and protrusive abilities and migrate more actively [66,85,86,117]. Collectively, this would suggest that paxillin serine phosphorylation regulates the degradation status of the protein, which in turn, is important in the modulation of paxillin-dependent membrane dynamics affecting cell motility.…”

Section: Paxillin Serine/threonine Phosphorylationmentioning

confidence: 94%

“…Whereas tyrosine phosphorylation of paxillin by FAK/Src is well documented, much less is known of the consequences of paxillin serine phosphorylation or the kinases that are involved [32,47,66,86,117]. Like tyrosine phosphorylation, paxillin serine/threonine phosphorylation is induced by a variety of stimuli: for example, cellular activation via integrin ligation has been documented to result in phosphorylation of S188/190 [47].…”

Section: Paxillin Serine/threonine Phosphorylationmentioning

confidence: 99%

“…Paxillin serine/threonine phosphorylation has also been shown to be stimulated by growth factors such as angiotensin II, activin A, TGF-β, EGF, heregulin and interleukin [47,117,118].…”

Section: Paxillin Serine/threonine Phosphorylationmentioning

confidence: 99%

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SLK-mediated phosphorylation of paxillin is required for focal adhesion turnover and cell migration

Baron

et al. 2012

Oncogene

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Section: Paxillin Serine/threonine Phosphorylationmentioning

confidence: 94%

Section: Paxillin Serine/threonine Phosphorylationmentioning

confidence: 99%

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SLK-mediated phosphorylation of paxillin is required for focal adhesion turnover and cell migration

Baron

et al. 2012

Oncogene

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“…[30][31][32] Although Smad2/3 signaling is relatively specific to the binding of ligands of the TGFb/activin family to cell surface receptors, investigators are discovering that MAPKs (p42/p44 Erk1/2, JNK, or p38MAPK) phosphorylate specific sites in the middle linker region of Smad2/3, sites that are distinct from the C-terminus that is phosphorylated by the TGFb II receptor (Figure 2). [33][34][35][36] Thus, ligands capable of activating MAPKs potentially modulate Smad signaling induced by TGFb. It has recently been demonstrated that p38MAPK activate phosphorylation of Smad3 in the middle linker region, which enhances Smad3/4 complex formation and nuclear translocation, 37 consistent with our finding of diminished Smad3/4 reporter gene activity in the presence of a p38MAPK inhibitor.…”

Section: Tgfb Signal Transductionmentioning

confidence: 99%

TGFβ pathobiology in the eye

Saika

2006

Laboratory Investigation

236

185

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“…16 The p38 MAP kinase-dependent signal transduction pathway(s) plays a role in serine phosphorylation and disassembly of paxillin. 17 Expression of VEGF, a multifunctional cytokine, is crucial in angiogenesis during the development of cancer and correlates with disease recurrence in patients with early gastric carcinoma. 18 p38 MAP kinase activation by VEGF mediates actin reorganization and cell migration in human endothelial cells.…”

Section: Genes Related To Extracellular Matrixmentioning

confidence: 99%

Expression profiling of gastric adenocarcinoma using cDNA array

et al. 2001

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To investigate the expression profile of gastric adenocarcinoma, cDNA array experiments were performed using Atlas Human Cancer 1.2 K Array (Clontech Laboratories, Palo Alto, CA) on nine xenografted and two primary gastric cancer samples. The expression of the tumor samples was compared to that of two normal gastric epithelial tissues. The expression pattern of the primary tumors was similar to that of xenografted tumors. The up-regulated genes had expression ratios ranging from 2.5 to 16, whereas the down-regulated genes had a range from ؊2.5 to ؊16. No variation in gene expression was detected in the analysis of the xenografted tumors versus the primary tumors, indicating that the xenografts represented the primary tumors well. Thirtyeight genes showed altered gene expression in 5 or more samples (>45%). Thirty-one genes were up-regulated and seven genes were down-regulated. The most abundantly upregulated genes (ratio >5) included genes such as S100A4, CDK4, MMP14 and beta catenin. The GIF was markedly downregulated (ratio < ؊10). To confirm our findings, six genes (three up-and three down-regulated) were selected for semiquantitative RT-PCR analysis. The RT-PCR results were consistent with the array findings. Our approach revealed that several genes are abnormally expressed in gastric cancer and found that genes known to interact in several common molecular pathway(s) were consistently altered. © 2001 Wiley-Liss, Inc. Key words: cDNA arrays; gene expression; xenografts; and gastric adenocarcinomasGastric carcinoma (GC) is one of the most common malignancies worldwide and is the second most common cause of cancerrelated death. 1 Overall relative 5-year survival rates are currently less than 20%. Cytogenetic studies of gastric adenocarcinomas are few in number and have failed to identify any consistent or noteworthy chromosomal abnormalities. 2 Comprehensive studies of DNA copy number changes using comparative genomic hybridization (CGH) have revealed alterations in several chromosomal regions. 3-5 Frequent high-level amplifications were noted at 17q and 20q, whereas DNA copy number losses were frequently seen in 4q, 5q, and 9p. However, there are few data on gene expression in gastric cancer. The recent development of cDNA array technology allows the study of gene expression level and gene activation in thousands of genes and sequences. 6,7 The data obtained from the array analysis are expected to uncover novel genes related to cancer development and its clinical behavior. However, tumor sample contamination with normal cells makes analysis of hundreds of genes more difficult and less sensitive. Xenografting of human tumors has been used to produce optimal samples that are enriched for neoplastic cells for subsequent molecular analyses.

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Serine phosphorylation of paxillin by heregulin-β1: role of p38 mitogen activated protein kinase

Cited by 61 publications

References 50 publications

SLK-mediated phosphorylation of paxillin is required for focal adhesion turnover and cell migration

SLK-mediated phosphorylation of paxillin is required for focal adhesion turnover and cell migration

TGFβ pathobiology in the eye

Expression profiling of gastric adenocarcinoma using cDNA array

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