Alternagin-C binding to α2β1 integrin controls matrix metalloprotease-9 and matrix metalloprotease-2 in breast tumor cells and endothelial cells

Moritz, Milene Nóbrega de Oliveira; Eustáquio, Lívia Mara Santos; Micocci, Kelli Cristina; Nunes, Ana Carolina Caetano; Santos, Patty Karina dos; Vieira, Tamires de Castro; Selistre-de-Araújo, Heloísa Sobreiro

doi:10.1186/s40409-018-0150-2

Cited by 10 publications

(4 citation statements)

References 53 publications

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“…As to the primary sequence obtained through Edman degradation and mass spectrometry procedures, Cdc non-RGD disintegrin isolated in this study is absent from the classical RGD motif or any other motif previously observed in this protein family or glutamate-cysteine-aspartate (ECD) motif which characterize disintegrin-like proteins that may inhibit tumor progression [ 47 ]. In the same position of this domain, this toxin presents a triad of amino acids LVN, which was found in disintegrins of C. d. collilineatus by transcriptome techniques [ 48 ], as well as in the disintegrin domains of P-II SVMP of C. d. collilineatus (C0L2T8) and C. atrox (Q2QA03).…”

Section: Discussionmentioning

confidence: 99%

Cell migration inhibition activity of a non-RGD disintegrin from Crotalus durissus collilineatus venom

Oliveira

Manzini

Ferreira

et al. 2018

J Venom Anim Toxins Incl Trop Dis

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BackgroundIn recent decades, snake venom disintegrins have received special attention due to their potential use in anticancer therapy. Disintegrins are small and cysteine-rich proteins present in snake venoms and can interact with specific integrins to inhibit their activities in cell-cell and cell-ECM interactions. These molecules, known to inhibit platelet aggregation, are also capable of interacting with certain cancer-related integrins, and may interfere in important processes involved in carcinogenesis. Therefore, disintegrin from Crotalus durissus collilineatus venom was isolated, structurally characterized and evaluated for its toxicity and ability to interfere with cell proliferation and migration in MDA-MB-231, a human breast cancer cell line.MethodsBased on previous studies, disintegrin was isolated by FPLC, through two chromatographic steps, both on reversed phase C-18 columns. The isolated disintegrin was structurally characterized by Tris-Tricine-SDS-PAGE, mass spectrometry and N-terminal sequencing. For the functional assays, MTT and wound-healing assays were performed in order to investigate cytotoxicity and effect on cell migration in vitro, respectively.ResultsDisintegrin presented a molecular mass of 7287.4 Da and its amino acid sequence shared similarity with the disintegrin domain of P-II metalloproteases. Using functional assays, the disintegrin showed low cytotoxicity (15% and 17%, at 3 and 6 μg/mL, respectively) after 24 h of incubation and in the wound-healing assay, the disintegrin (3 μg/mL) was able to significantly inhibit cell migration (24%, p < 0.05), compared to negative control.ConclusionThus, our results demonstrate that non-RGD disintegrin from C. d. collilineatus induces low cytotoxicity and inhibits migration of human breast cancer cells. Therefore, it may be a very useful molecular tool for understanding ECM-cell interaction cancer-related mechanisms involved in an important integrin family that highlights molecular aspects of tumorigenesis. Also, non-RGD disintegrin has potential to serve as an agent in anticancer therapy or adjuvant component combined with other anticancer drugs.

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Section: Discussionmentioning

confidence: 99%

Cell migration inhibition activity of a non-RGD disintegrin from Crotalus durissus collilineatus venom

Oliveira

Manzini

Ferreira

et al. 2018

J Venom Anim Toxins Incl Trop Dis

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“…In addition, integrins, such as αVβ3 cooperate with MMPs, such as MMP-2 [191], MMP-9 [192] and MMP-14 [193], in regulating migration of metastatic breast cancer cells toward specific substrates in an activation-dependent pathway. Indeed, it has been demonstrated that integrins control MMP-2 and MMP-9 expression regulating angiogenesis in breast tumor cells and endothelial cells [194]. In fact, the inhibition of MMP-9 and α V β 5 -integrin interaction results in a reduced angiogenesis and tumor invasion [195].…”

Section: Intercellular Communication System In the Tumor Microenvimentioning

confidence: 99%

Breast Cancer Tumor Stroma: Cellular Components, Phenotypic Heterogeneity, Intercellular Communication, Prognostic Implications and Therapeutic Opportunities

Eiró

González

Fraile

et al. 2019

Cancers

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Although the mechanisms underlying the genesis and progression of breast cancer are better understood than ever, it is still the most frequent malignant tumor in women and one of the leading causes of cancer death. Therefore, we need to establish new approaches that lead us to better understand the prognosis of this heterogeneous systemic disease and to propose new therapeutic strategies. Cancer is not only a malignant transformation of the epithelial cells merely based on their autonomous or acquired proliferative capacity. Today, data support the concept of cancer as an ecosystem based on a cellular sociology, with diverse components and complex interactions between them. Among the different cell types that make up the stroma, which have a relevant role in the dynamics of tumor/stromal cell interactions, the main ones are cancer associated fibroblasts, endothelial cells, immune cells and mesenchymal stromal cells. Several factors expressed by the stroma of breast carcinomas are associated with the development of metastasis, such as matrix metalloproteases, their tissular inhibitors or some of their regulators like integrins, cytokines or toll-like receptors. Based on the expression of these factors, two types of breast cancer stroma can be proposed with significantly different influence on the prognosis of patients. In addition, there is evidence about the existence of bi-directional signals between cancer cells and tumor stroma cells with prognostic implications, suggesting new therapeutic strategies in breast cancer.

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“…The authors suggest that MDM2 might promote MMP9 driven angiogenesis [41]. Other experiments have indicated that the level of MMPs is modulated by α2β1 integrin in breast cancer and endothelial cells [42]. Webb et al (2017) have indicated that MMP9 and MMP2 promote the process of vascular metastasis and tumour growth in retinoblastoma, an ocular neoplasm described in children.…”

Section: Matrix Metalloproteinases (Mmps)mentioning

confidence: 99%

An update on angiogenesis modulators with a potential therapeutic role

et al. 2018

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Alternagin-C binding to α2β1 integrin controls matrix metalloprotease-9 and matrix metalloprotease-2 in breast tumor cells and endothelial cells

Cited by 10 publications

References 53 publications

Cell migration inhibition activity of a non-RGD disintegrin from Crotalus durissus collilineatus venom

Cell migration inhibition activity of a non-RGD disintegrin from Crotalus durissus collilineatus venom

Breast Cancer Tumor Stroma: Cellular Components, Phenotypic Heterogeneity, Intercellular Communication, Prognostic Implications and Therapeutic Opportunities

An update on angiogenesis modulators with a potential therapeutic role

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