4.6 Article

Desmoglein 3-Influence on oral carcinoma cell migration and invasion

Journal

EXPERIMENTAL CELL RESEARCH
Volume 370, Issue 2, Pages 353-364

Publisher

ELSEVIER INC
DOI: 10.1016/j.yexcr.2018.06.037

Keywords

Desmoglein 3; 3D in vitro model; Co-culture; Myogel; Migration; Invasion; Live cell imaging; Cell tracking; Image analysis; Monoclonal antibody testing

Funding

  1. Sigrid Juselius Foundation
  2. Finnish Cancer Foundation
  3. Medical Faculty of the University of Oulu
  4. Medical Faculty of Oulu University Hospital special state support for research
  5. Finnish Doctoral Programme in Oral Sciences (FINDOS)
  6. Tyyni Tani Foundation
  7. Oulu University Research Foundation
  8. Centre for International Mobility (CIMO) [TM-15-9587]
  9. Medical Research Center Oulu

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Desmoglein 3 (Dsg3) is an adhesion receptor in desmosomes, but its role in carcinoma cell migration and invasion is mostly unknown. Our aim was to quantitatively analyse the motion of Dsg3-modified carcinoma cells in 2D settings and in 3D within tumour microenvironment mimicking (TMEM) matrices. We tested mutant constructs of C-terminally truncated Dsg3 (Delta 238 and Delta 560), overexpressed full-length (FL) Dsg3, and empty vector control (Ct) of buccal mucosa squamous cell carcinoma (SqCC/Y1) cells. We captured live cell images and analysed migration velocities and accumulated and Euclidean distances. We compared rodent collagen and Matrigel. with human Myogel TMEM matrices for these parameters in 3D sandwich, in which we also tested the effects of monoclonal antibody AK23, which targets the EC1 domain of Dsg3. In monolayer culture, FL and both truncated constructs migrated faster and had higher accumulated distances than Ct cells. However, in the 3D assays, only the mutants invaded faster relative to Ct cells. Of the mutants, the shorter form (Delta 238) exhibited faster migration and invasion than Delta 560 cells. In the Transwell, all of the cells invaded faster through Myogel than Matrigel coated wells. In 3D sandwich, AK23 antibody inhibited only the invasion of FL cells. We conclude that different experimental 2D and 3D settings can markedly influence the movement of oral carcinoma cells with various Dsg3 modifications.

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