Extracellular matrix-specific Caveolin-1 phosphorylation on tyrosine 14 is linked to augmented melanoma metastasis but not tumorigenesis

Ortiz, Rina; Díaz, Jorge; Díaz, Nora; Lobos-González, Lorena; Cárdenas, Areli; Contreras, Pamela; Díaz, María Inés; Otte, E.; Cooper-White, Justin J.; Torres, Vicente A.; Leyton, Lisette; Quest, Andrew F. G.

doi:10.18632/oncotarget.9738

Cited by 45 publications

(60 citation statements)

References 91 publications

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“…Phosphorylation of CAV1 on Y14 is relevant in this context and has been related to increases in anchorageindependent growth, Grb7-dependent cell migration [34], metalloproteinase activation, and cell invasion [35], membrane microdomain internalization regulated by integrins [26] as well as caveolae formation induced by EGF [36]. Also, CAV1 expression is associated with an increase in MDA-MB-231 and B16F10 cell migration [4], which is blocked by inhibition either pharmacologically of Src family kinases with PP2 or using the non-phosphorylatable CAV1(Y14F) mutant [4,7]. Here we show that E-cadherin inhibited Y14-CAV1 Fig.…”

Section: Discussionmentioning

confidence: 99%

“…CAV1 phosphorylation on Y14 is essential to promote migration/invasion and metastatic cells have elevated levels of CAV1 pY14 in comparison to non-metastatic cancer cells [7,33]. Alternatively, the expression of E-cadherin blocks CAV1-enhanced metastasis in vivo [5].…”

Section: E-cadherin Expression Decreases Cav1 Phosphorylation On Tyromentioning

confidence: 99%

“…On the one hand, CAV1 protein and mRNA levels are decreased in transformed fibroblasts, in breast, and colon cancer cell lines [1,2], and re-expression of CAV1 in colon cancer cells reduces subcutaneous tumor formation in immunosuppressed nude mice [3]. On the other hand, CAV1 acts as a promoter of metastasis in later stages of cancer, where enhanced expression of CAV1 favors the malignant phenotype and correlates with an increase in cell migration, metastasis [4][5][6][7][8], and multidrug resistance [9]. The two first mentioned roles of CAV1 are affected by the presence of the glycoprotein E-cadherin, which enhances CAV1 function as a tumor suppressor and blocks the ability of CAV1 to promote metastasis in vivo.…”

Section: Introductionmentioning

confidence: 99%

“…In metastatic breast cancer and melanoma cells, CAV1 phosphorylation on Y14 increases cell migration by promoting focal adhesion turnover, polarization, persistency, speed, and directionality of migration. All these functions of CAV1 are blocked either pharmacologically using Src family kinase inhibitors or by introducing a non-phosphorylatable CAV1 (Y14F) mutation, which also completely blocks the metastasis promoting role of CAV1 [4,7].…”

Section: Introductionmentioning

confidence: 99%

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The non-receptor tyrosine phosphatase type 14 blocks caveolin-1-enhanced cancer cell metastasis

et al. 2020

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Caveolin-1 (CAV1) enhanced migration, invasion, and metastasis of cancer cells is inhibited by co-expression of the glycoprotein E-cadherin. Although the two proteins form a multiprotein complex that includes β-catenin, it remained unclear how this would contribute to blocking the metastasis promoting function of CAV1. Here, we characterized by mass spectrometry the protein composition of CAV1 immunoprecipitates from B16F10 murine melanoma cells expressing or not E-cadherin. The novel protein tyrosine phosphatase PTPN14 was identified by mass spectrometry analysis exclusively in coimmunoprecipitates of CAV1 with E-cadherin. Interestingly, PTPN14 is implicated in controlling metastasis, but only few known PTPN14 substrates exist. We corroborated by western blotting experiments that PTPN14 and CAV1 coinmunoprecipitated in the presence of E-cadherin in B16F10 melanoma and other cancer cells. Moreover, the CAV1(Y14F) mutant protein was shown to co-immunoprecipitate with PTPN14 even in the absence of E-cadherin, and overexpression of PTPN14 reduced CAV1 phosphorylation on tyrosine-14, as well as suppressed CAV1-enhanced cell migration, invasion and Rac-1 activation in B16F10, metastatic colon [HT29(US)] and breast cancer (MDA-MB-231) cell lines. Finally, PTPN14 overexpression in B16F10 cells reduced the ability of CAV1 to induce metastasis in vivo. In summary, we identify here CAV1 as a novel substrate for PTPN14 and show that overexpression of this phosphatase suffices to reduce CAV1-induced metastasis.

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Section: Discussionmentioning

confidence: 99%

Section: E-cadherin Expression Decreases Cav1 Phosphorylation On Tyromentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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The non-receptor tyrosine phosphatase type 14 blocks caveolin-1-enhanced cancer cell metastasis

et al. 2020

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“…[8][9][10] Considering the possibility of physical barriers, or the degradation of physical barriers in relation to metastasis further suggests considering the possibility that abnormal, [11][12][13][14] or abnormally expressed 15,16 cell shape and ECM proteins could facilitate metastasis. [17][18][19] As it turns out, proteins that participate in the formation of the cytoskeleton and extracellular matrix (CECMPs) represent very large coding regions and thereby are frequently mutated in tumorigenesis, 20,21 that is, the random nature of mutagenesis makes it inevitable that many of these coding regions will be mutated. In some cases, particularly in melanoma, these coding regions have been shown to be candidate drivers.…”

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confidence: 99%

Cytoskeleton and ECM tumor mutant peptides: Increased protease sensitivities and potential consequences for the HLA class I mutant epitope reservoir

Callahan¹,

Patel²,

Fawcett

et al. 2017

Intl Journal of Cancer

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Cytoskeleton and extracellular matrix-related proteins (CECMPs) represent the most common class of cancer mutants, owing to the large size of their coding regions and the randomness of mutagenesis. We used a bioinformatics approach to assess the impact of amino acid (AA) substitutions on the sensitivity of CECMPs to proteases relevant to melanoma and on the binding affinities for HLA class I. CECMP peptides with AA substitutions overwhelmingly reflect increased sensitivity to proteases implicated in melanoma development (MME, CTSS, MMP2, CTSD, CTSL) in comparison to the wild-type peptide sequences. Furthermore, peptides with AA substitutions representing increased peptide protease sensitivity also represented relatively high binding affinities for HLA class I allelic variants. These analyses raise the question of whether increased protease sensitivity, of mutant cancer peptides represents a significant increase in the availability of cancer mutant, HLA class I epitopes and a hitherto unappreciated aspect of cancer cell immunogenicity, particularly in the case of melanoma?

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Adhesion‐dependent Caveolin‐1 Tyrosine‐14 phosphorylation is regulated by FAK in response to changing matrix stiffness

et al. 2021

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Integrin‐mediated adhesion regulates cellular responses to changes in the mechanical and biochemical properties of the extracellular matrix. Cell–matrix adhesion regulates caveolar endocytosis, dependent on caveolin 1 (Cav1) Tyr14 phosphorylation (pY14Cav1), to control anchorage‐dependent signaling. We find that cell–matrix adhesion regulates pY14Cav1 levels in mouse fibroblasts. Biochemical fractionation reveals endogenous pY14Cav1 to be present in caveolae and focal adhesions (FA). Adhesion does not affect caveolar pY14Cav1, supporting its regulation at FA, in which PF‐228‐mediated inhibition of focal adhesion kinase (FAK) disrupts. Cell adhesion on 2D polyacrylamide matrices of increasing stiffness stimulates Cav1 phosphorylation, which is comparable to the phosphorylation of FAK. Inhibition of FAK across varying stiffnesses shows it regulates pY14Cav1 more prominently at higher stiffness. Taken together, these studies reveal the presence of FAK–pY14Cav1 crosstalk at FA, which is regulated by cell–matrix adhesion.

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Extracellular matrix-specific Caveolin-1 phosphorylation on tyrosine 14 is linked to augmented melanoma metastasis but not tumorigenesis

Cited by 45 publications

References 91 publications

The non-receptor tyrosine phosphatase type 14 blocks caveolin-1-enhanced cancer cell metastasis

The non-receptor tyrosine phosphatase type 14 blocks caveolin-1-enhanced cancer cell metastasis

Cytoskeleton and ECM tumor mutant peptides: Increased protease sensitivities and potential consequences for the HLA class I mutant epitope reservoir

Adhesion‐dependent Caveolin‐1 Tyrosine‐14 phosphorylation is regulated by FAK in response to changing matrix stiffness

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