Proteomic profiling of tumour tissue‐derived extracellular vesicles in colon cancer

Author:

Cvjetkovic Aleksander1ORCID,Karimi Nasibeh1,Crescitelli Rossella123ORCID,Thorsell Annika4,Taflin Helena5,Lässer Cecilia1,Lötvall Jan1ORCID

Affiliation:

1. Krefting Research Centre, Institute of Medicine at Sahlgrenska Academy University of Gothenburg Gothenburg Sweden

2. Sahlgrenska Center for Cancer Research and Wallenberg Centre for Molecular and Translational Medicine, Department of Surgery, Institute of Clinical Sciences, Sahlgrenska Academy University of Gothenburg Gothenburg Sweden

3. Department of Surgery Sahlgrenska University Hospital Gothenburg Sweden

4. Proteomics Core Facility, Sahlgrenska Academy University of Gothenburg Gothenburg Sweden

5. Transplant Institute at Sahlgrenska University Hospital, Institute of Clinical Sciences Sahlgrenska Academy at University of Gothenburg Gothenburg Sweden

Abstract

AbstractColon cancer is one of the most commonly occurring tumours among both women and men, and over the past decades the incidence has been on the rise. As such, the need for biomarker identification as well as an understanding of the underlying disease mechanism has never been greater. Extracellular vesicles are integral mediators of cell‐to‐cell communication and offer a unique opportunity to study the machinery that drives disease progression, and they also function as vectors for potential biomarkers. Tumour tissue and healthy mucosal tissue from the colons of ten patients were used to isolate tissue‐resident EVs that were subsequently subjected to global quantitative proteomic analysis through LC‐MS/MS. In total, more than 2000 proteins were identified, with most of the common EV markers being among them. Bioinformatics revealed a clear underrepresentation of proteins involved in energy production and cellular adhesion in tumour EVs, while proteins involved in protein biosynthesis were overrepresented. Additionally, 53 membrane proteins were found to be significantly upregulated in tumour EVs. Among them were several proteins with enzymatic functions that degrade the extracellular matrix, and three of these, Fibroblast activating factor (FAP), Cell surface hyaluronidase (CEMIP2), as well as Ephrin receptor B3 (EPHB3), were validated and found to be consistent with the global quantitative results. These stark differences in the proteomes between healthy and cancerous tissue emphasise the importance of the interstitial vesicle secretome as a major player of disease development.

Funder

Swedish Cancer Foundation

Publisher

Wiley

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