Bio21 - Research Publications

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Author: Ang, Ching-Seng × Author: Keerthikumar, Shivakumar ×

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    Proteomic Profiling of Exosomes Secreted by Breast Cancer Cells with Varying Metastatic Potential
    Gangoda, L ; Liem, M ; Ang, C-S ; Keerthikumar, S ; Adda, CG ; Parker, BS ; Mathivanan, S (WILEY, 2017-12)
    Cancer cells actively release extracellular vesicles, including exosomes, into the surrounding microenvironment. Exosomes play pleiotropic roles in cancer progression and metastasis, including invasion, angiogenesis, and immune modulation. However, the proteome profile of exosomes isolated from cells with different metastatic potential and the role of these exosomes in driving metastasis remains unclear. Here, we conduct a comparative proteomic analysis of exosomes isolated from several genetically related mouse breast tumor lines with different metastatic propensity. The amount of exosomes produced and the extent of cancer-associated protein cargo vary significantly between nonmetastatic and metastatic cell-derived exosomes. Metastatic cell-derived exosomes contain proteins that promote migration, proliferation, invasion, and angiogenesis while the nonmetastatic cell-derived exosomes contain proteins involved in cell-cell/cell-matrix adhesion and polarity maintenance. The metastatic exosomes contain a distinct set of membrane proteins including Ceruloplasmin and Metadherin which could presumably aid in targeting the primary cancer cells to specific metastatic sites. Hence, it can be concluded that the exosomes contain different protein cargo based on the host cells metastatic properties and can facilitate in the dissemination of the primary tumors to distant sites.
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    Oral administration of bovine milk-derived extracellular vesicles induces senescence in the primary tumor but accelerates cancer metastasis
    Samuel, M ; Fonseka, P ; Sanwlani, R ; Gangoda, L ; Chee, SH ; Keerthikumar, S ; Spurling, A ; Chitti, SV ; Zanker, D ; Ang, C-S ; Atukorala, I ; Kang, T ; Shahi, S ; Marzan, AL ; Nedeva, C ; Vennin, C ; Lucas, MC ; Cheng, L ; Herrmann, D ; Pathan, M ; Chisanga, D ; Warren, SC ; Zhao, K ; Abraham, N ; Anand, S ; Boukouris, S ; Adda, CG ; Jiang, L ; Shekhar, TM ; Baschuk, N ; Hawkins, CJ ; Johnston, AJ ; Orian, JM ; Hoogenraad, NJ ; Poon, IK ; Hill, AF ; Jois, M ; Timpson, P ; Parker, BS ; Mathivanan, S (NATURE RESEARCH, 2021-06-24)
    The concept that extracellular vesicles (EVs) from the diet can be absorbed by the intestinal tract of the consuming organism, be bioavailable in various organs, and in-turn exert phenotypic changes is highly debatable. Here, we isolate EVs from both raw and commercial bovine milk and characterize them by electron microscopy, nanoparticle tracking analysis, western blotting, quantitative proteomics and small RNA sequencing analysis. Orally administered bovine milk-derived EVs survive the harsh degrading conditions of the gut, in mice, and is subsequently detected in multiple organs. Milk-derived EVs orally administered to mice implanted with colorectal and breast cancer cells reduce the primary tumor burden. Intriguingly, despite the reduction in primary tumor growth, milk-derived EVs accelerate metastasis in breast and pancreatic cancer mouse models. Proteomic and biochemical analysis reveal the induction of senescence and epithelial-to-mesenchymal transition in cancer cells upon treatment with milk-derived EVs. Timing of EV administration is critical as oral administration after resection of the primary tumor reverses the pro-metastatic effects of milk-derived EVs in breast cancer models. Taken together, our study provides context-based and opposing roles of milk-derived EVs as metastasis inducers and suppressors.
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    Arrestin-Domain Containing Protein 1 (Arrdc1) Regulates the Protein Cargo and Release of Extracellular Vesicles
    Anand, S ; Foot, N ; Ang, C-S ; Gembus, KM ; Keerthikumar, S ; Adda, CG ; Mathivanan, S ; Kumar, S (WILEY, 2018-09)
    Extracellular vesicles (EVs) are lipid-bilayered vesicles that are released by multiple cell types and contain nucleic acids and proteins. Very little is known about how the cargo is packaged into EVs. Ubiquitination of proteins is a key posttranslational modification that regulates protein stability and trafficking to subcellular compartments including EVs. Recently, arrestin-domain containing protein 1 (Arrdc1), an adaptor for the Nedd4 family of ubiquitin ligases, has been implicated in the release of ectosomes, a subtype of EV that buds from the plasma membrane. However, it is currently unknown whether Arrdc1 can regulate the release of exosomes, a class of EVs that are derived endocytically. Furthermore, it is unclear whether Arrdc1 can regulate the sorting of protein cargo into the EVs. Exosomes and ectosomes are isolated from mouse embryonic fibroblasts isolated from wild type and Arrdc1-deficient (Arrdc1-/- ) mice. Nanoparticle tracking analysis-based EV quantitation shows that Arrdc1 regulates the release of both exosomes and ectosomes. Proteomic analysis highlights the change in protein cargo in EVs upon deletion of Arrdc1. Functional enrichment analysis reveals the enrichment of mitochondrial proteins in ectosomes, while proteins implicated in apoptotic cleavage of cell adhesion proteins and formation of cornified envelope are significantly depleted in exosomes upon knockout of Arrdc1.
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    A novel community driven software for functional enrichment analysis of extracellular vesicles data
    Pathan, M ; Keerthikumar, S ; Chisanga, D ; Alessandro, R ; Ang, C-S ; Askenase, P ; Batagov, AO ; Benito-Martin, A ; Camussi, G ; Clayton, A ; Collino, F ; Di Vizio, D ; Falcon-Perez, J ; Fonseca, P ; Fonseka, P ; Fontana, S ; Gho, YS ; Hendrix, A ; Nolte-'t Hoen, E ; Iraci, N ; Kastaniegaard, K ; Kislinger, T ; Kowal, J ; Kurochkin, IV ; Leonardi, T ; Liang, Y ; Llorente, A ; Lunavat, TR ; Maji, S ; Monteleone, F ; Overbye, A ; Panaretakis, T ; Patel, T ; Peinado, H ; Pluchino, S ; Principe, S ; Ronquist, G ; Royo, F ; Sahoo, S ; Spinelli, C ; Stensballe, A ; Thery, C ; van Herwijnen, MJC ; Wauben, M ; Welton, JL ; Zhao, K ; Mathivanan, S (TAYLOR & FRANCIS LTD, 2017-05-26)
    Bioinformatics tools are imperative for the in depth analysis of heterogeneous high-throughput data. Most of the software tools are developed by specific laboratories or groups or companies wherein they are designed to perform the required analysis for the group. However, such software tools may fail to capture "what the community needs in a tool". Here, we describe a novel community-driven approach to build a comprehensive functional enrichment analysis tool. Using the existing FunRich tool as a template, we invited researchers to request additional features and/or changes. Remarkably, with the enthusiastic participation of the community, we were able to implement 90% of the requested features. FunRich enables plugin for extracellular vesicles wherein users can download and analyse data from Vesiclepedia database. By involving researchers early through community needs software development, we believe that comprehensive analysis tools can be developed in various scientific disciplines.
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    Bovine milk-derived exosomes from colostrum are enriched with proteins implicated in immune response and growth
    Samuel, M ; Chisanga, D ; Liem, M ; Keerthikumar, S ; Anand, S ; Ang, C-S ; Adda, CG ; Versteegen, E ; Jois, M ; Mathivanan, S (NATURE PORTFOLIO, 2017-07-19)
    Exosomes are extracellular vesicles secreted by multiple cell types into the extracellular space. They contain cell-state specific cargos which often reflects the (patho)physiological condition of the cells/organism. Milk contains high amounts of exosomes and it is unclear whether their cargo is altered based on the lactation stage of the organism. Here, we isolated exosomes from bovine milk that were obtained at various stages of lactation and examined the content by quantitative proteomics. Exosomes were isolated by OptiPrep density gradient centrifugation from milk obtained from cow after 24, 48 and 72 h post calving. As control, exosomes were also isolated from cows during mid-lactation period which has been referred to as mature milk (MM). Biochemical and biophysical characterization of exosomes revealed the high abundance of exosomes in colostrum and MM samples. Quantitative proteomics analysis highlighted the change in the proteomic cargo of exosomes based on the lactation state of the cow. Functional enrichment analysis revealed that exosomes from colostrum are significantly enriched with proteins that can potentially regulate the immune response and growth. This study highlights the importance of exosomes in colostrum and hence opens up new avenues to exploit these vesicles in the regulation of the immune response and growth.
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    Extracellular vesicles containing oncogenic mutant β-catenin activate Wnt signalling pathway in the recipient cells
    Kalra, H ; Gangoda, L ; Fonseka, P ; Chitti, S ; Liem, M ; Keerthikumar, S ; Samuel, M ; Boukouris, S ; Al Saffar, H ; Collins, C ; Adda, CG ; Ang, C-S ; Mathivanan, S (TAYLOR & FRANCIS LTD, 2019-12-01)
    Mutations in β-catenin, especially at the residues critical for its degradation, render it constitutively active. Here, we show that mutant β-catenin can be transported via extracellular vesicles (EVs) and activate Wnt signalling pathway in the recipient cells. An integrative proteogenomic analysis identified the presence of mutated β-catenin in EVs secreted by colorectal cancer (CRC) cells. Follow-up experiments established that EVs released from LIM1215 CRC cells stimulated Wnt signalling pathway in the recipient cells with wild-type β-catenin. SILAC-based quantitative proteomics analysis confirmed the transfer of mutant β-catenin to the nucleus of the recipient cells. In vivo tracking of DiR-labelled EVs in mouse implanted with RKO CRC cells revealed its bio-distribution, confirmed the activation of Wnt signalling pathway in tumour cells and increased the tumour burden. Overall, for the first time, this study reveals that EVs can transfer mutant β-catenin to the recipient cells and promote cancer progression.
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    Extracellular vesicles secreted by Saccharomyces cerevisiae are involved in cell wall remodelling
    Zhao, K ; Bleackley, M ; Chisanga, D ; Gangoda, L ; Fonseka, P ; Liem, M ; Kalra, H ; Al Saffar, H ; Keerthikumar, S ; Ang, C-S ; Adda, CG ; Jiang, L ; Yap, K ; Poon, IK ; Lock, P ; Bulone, V ; Anderson, M ; Mathivanan, S (NATURE PUBLISHING GROUP, 2019-08-09)
    Extracellular vesicles (EVs) are membranous vesicles that are released by cells. In this study, the role of the Endosomal Sorting Complex Required for Transport (ESCRT) machinery in the biogenesis of yeast EVs was examined. Knockout of components of the ESCRT machinery altered the morphology and size of EVs as well as decreased the abundance of EVs. In contrast, strains with deletions in cell wall biosynthesis genes, produced more EVs than wildtype. Proteomic analysis highlighted the depletion of ESCRT components and enrichment of cell wall remodelling enzymes, glucan synthase subunit Fks1 and chitin synthase Chs3, in yeast EVs. Interestingly, EVs containing Fks1 and Chs3 rescued the yeast cells from antifungal molecules. However, EVs from fks1∆ or chs3∆ or the vps23∆chs3∆ double knockout strain were unable to rescue the yeast cells as compared to vps23∆ EVs. Overall, we have identified a potential role for yeast EVs in cell wall remodelling.