An invasion-related complex of cortactin, paxillin and PKCμ associates with invadopodia at sites of extracellular matrix degradation

Bowden, Emma T.; Barth, Mara; Thomas, D. A.; Glazer, Robert I.; Mueller, Susette C.

doi:10.1038/sj.onc.1202827

Cited by 338 publications

(362 citation statements)

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“…Additionally, recent studies have shown the overexpression of cortactin in NIH3T3 cells to result in increased cell invasion/migration in vitro (Patel et al, 1998;Huang et al, 1998). Moreover, cortactin takes part in formation and function of invadopodias in (Bowden et al, 1999) supporting the hypothesis of direct involvement of cortactin in metastasis.…”

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confidence: 73%

Human cortactin as putative cancer antigen

et al. 2000

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Humoral immune response against overexpressed oncogenic or tumor supressor proteins has been demonstrated for many types of cancer. In this study we report on the detection of the autologous antibody response to putative oncogene, human cortactin using serological analysis of breast carcinoma expression library. Cortactin maps to chromosome 11q13, the region ampli®ed in about 15% of primary breast carcinomas and 30% of head and neck squamous cell carcinomas. Cortactin overexpression due to such ampli®cation might a ect adhesive properties of human cancer cells and is associated with poor disease prognosis. Accordingly, we detected overexpression of cortactin transcript in autologous tumor and ampli®ca-tion/overexpression of cortactin in tumors of breast cancer patients serologically positive for this marker. We demonstrate that 15% of breast cancer patients elicit humoral immune response against human cortactin. Oncogene (2000) 19, 5204 ± 5207.Keywords: breast cancer; cortactin; cancer antigen; tumor markerThe development of cancer vaccines requires the identi®cation and characterization of tumor antigens. In the past decade many tumor antigens have been de®ned (reviewed by Old and Chen, 1998;Rosenberg, 1999).In 1991 T Boon and colleagues discovered the ®rst antigen recognized by cytotoxic T-lymphocytes (CTL) in human melanoma (van der Bruggen et al., 1991). In their study tumor antigens have been identi®ed by the transfection of cDNA libraries into cells expressing the appropriate MHC molecule followed by the identi®ca-tion of transfectant using cytokine release or lysis by human T cells with speci®c antitumor reactivity (Boon et al., 1994).An alternative technique for the identi®cation of tumor antigens has been reported by Sahin et al. (1995). This approach of serological analysis of cDNA expression libraries (SEREX), was based on previously described molecular screening techniques (D'Arpa et al., 1988) and exploited patient's B-cell repertoire for the identi®cation of human tumor antigens that show immunogenicity in the autologous host. Many antigens have been isolated by this technique, demonstrating that most, if not all, human cancers express multiple antigens including ampli®ed/overexpressed proteins with known cancer association (reviewed by Old and Chen, 1998;Disis and Cheever, 1996;Brass et al., 1999).In this study we applied the SEREX method to isolate and characterize candidate tumor antigens expressed in breast carcinoma. A cDNA library in phage expression vector (lambda ZAP Express) was prepared from a surgical tumor specimen of a 56-yearold woman with ER-positive breast carcinoma (T 1 M 0 N 0 ). The library was plated and screened with autologous patient's serum diluted 1 : 200 as previously described (Scanlan et al., 1998). Screening of 3610 5 primary recombinant phage clones yielded a total of 70Oncogene (2000) 19, 5204 ± 5207 ã 2000 Macmillan Publishers Ltd All rights reserved 0950 ± 9232/00 $15.00 www.nature.com/onc The deduced amino acid sequence of MOBr-140 represents human cortactin from a...

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confidence: 73%

Human cortactin as putative cancer antigen

et al. 2000

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“…Invasive tumor cells form actin-rich protrusions, called invadopodia, that degrade and extend into ECMs (Bowden et al, 1999;Onodera et al, 2005;Weaver, 2006;Cortesio et al, 2008). To evaluate the ability of invadopodia formation during in vitro invasion of SaOS-2 cells, Alexa-labeled gelatin (red) was utilized as ECM (see Materials and Methods).…”

Section: Ror2 Has Important Functions In Ecm Degradation and Invadopomentioning

confidence: 99%

“…Fluorescent images were obtained using a laser scanning confocal imaging system (LSM510, Carl Zeiss, Go¨ttingen, Germany). For ECM degradation assay, glass-bottom dishes were coated with gelatin (Type A with 300 Bloom; Sigma) conjugated with Alexa 594 (Invitrogen) (Alexa-gelatin) and then treated with 0.5% glutaraldehyde, as described earlier (Bowden et al, 1999;Onodera et al, 2005). Cells were cultured on these glassbottom dishes in DMEM, fixed and stained with anti-cortactin antibody or Alexa 488-phalloidin.…”

Section: Reporter Assaymentioning

confidence: 99%

Autonomous regulation of osteosarcoma cell invasiveness by Wnt5a/Ror2 signaling

et al. 2009

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The receptor tyrosine kinase Ror2 regulates cell migration by acting as a receptor or co-receptor for Wnt5a. Although Wnt5a has been implicated in the invasiveness of several types of tumors, the role of Ror2 in tumor invasion remains elusive. Here we show that osteosarcoma cell lines SaOS-2 and U2OS show invasive properties in vitro by activating Wnt5a/Ror2 signaling in a cell-autonomous manner. The suppressed expression of either Wnt5a or Ror2 in osteosarcoma cells inhibits cell invasiveness accompanying decreased invadopodia formation. Gene-expression profiling identified matrix metalloproteinase 13 (MMP-13) as one of the genes whose expression is downregulated in SaOS-2 cells following suppression of Ror2 expression. Reduced expression or activity of MMP-13 suppresses invasiveness of SaOS-2 cells. Moreover, expression of MMP-13 and cell invasiveness by Wnt5a/Ror2 signaling can be abrogated by an inhibitor of the Src-family protein tyrosine kinases (SFKs), suggesting the role of the SFKs in MMP-13 expression through Wnt5a/Ror2 signaling. We further show that activation of an SFK is inhibited by the suppressed expression of Ror2. Collectively, these results indicate that Wnt5a/Ror2 signaling involves the activation of a SFK, leading to MMP-13 expression, and that constitutively active Wnt5a/Ror2 signaling confers invasive properties on osteosarcoma cells in a cell-autonomous manner.

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“…Fluorescently-labeled gelatin-coated coverslips were prepared as described by Berdeaux et al (2004), as originally described by Bowden et al (1999). In brief, coverslips were coated with Oregon green 488-conjugated gelatin (Chemicon, Temecula, CA), cross-linked 15 min in 0.5% glutaraldehyde in phosphate-buffered saline (PBS), and incubated for 3 min with 5 mg/ml NaBH 4 in PBS.…”

Section: Extracellular Matrix Degradation Assay and Fluorescence Micrmentioning

confidence: 99%

“…They are regulated by various proteins, including the Arp2/3 complex, N-WASp, WAVE1, Cdc42, ASAP1, cortactin, gelsolin, and cofilin (Bowden et al, 1999(Bowden et al, , 2006Baldassarre et al, 2003;Yamaguchi et al, 2005;Artym et al, 2006;Chellaiah, 2006;Bharti et al, 2007;Clark et al, 2007). Podosomes/invadopodia are found in various mammalian cells such as macrophages, osteoclasts and vascular smooth muscle cells (Linder and Aepfelbacher, 2003).…”

Section: Introductionmentioning

confidence: 99%

A role for the podosome/invadopodia scaffold protein Tks5 in tumor growth in vivo

Blouw

Seals

Pass

et al. 2008

European Journal of Cell Biology

105

112

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Podosomes and invadopodia are electron-dense, actin-rich protrusions located on the ventral side of the cellular membrane. They are detected in various types of normal cells, but also in human cancer cells and in Src-transformed fibroblasts. Previously we have shown that the scaffold protein Tks5 (tyrosine kinase substrate 5) co-localizes to podosomes/invadopodia in different human cancer cells and in Src-transformed NIH-3T3 cells. Upon reduced expression of Tks5 podosome formation is decreased, which leads to diminished gelatin degradation in vitro in various human cancer cell lines. It is unclear, however, whether cancer cells need podosomes for tumor growth and metastasis in vivo. To test this idea, we evaluated the ability of Srctransformed NIH-3T3 cells, showing stable reduced expression of Tks5 and podosome formation (Tks5 KD), to form subcutaneous tumors in mice. We demonstrate that decreased expression of Tks5 correlated with reduced tumor growth at this site. In addition, we generated lung metastases from these cells following tail vein injection. The lungs of mice injected i.v. with the Tks5 KD showed smaller-sized metastases, but there was no difference in the number of lesions compared to the controls, indicating that podosomes may not be required for extravasation from the blood stream into the lung parenchyma. Independent of the microenvironment however, the reduced tumor growth correlated with decreased tumor vascularization. Our data potentially implicate a novel role of podosomes as mediators of tumor angiogenesis and support further exploration of how podosome formation and Tks5 expression contribute to tumor progression.

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An invasion-related complex of cortactin, paxillin and PKCμ associates with invadopodia at sites of extracellular matrix degradation

Cited by 338 publications

References 35 publications

Human cortactin as putative cancer antigen

Human cortactin as putative cancer antigen

Autonomous regulation of osteosarcoma cell invasiveness by Wnt5a/Ror2 signaling

A role for the podosome/invadopodia scaffold protein Tks5 in tumor growth in vivo

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