AI Article Synopsis

  • Proteases are involved in cancer progression by influencing invasion through matrix remodeling and modulating cell behavior, showing both pro- and anti-tumor effects depending on the context.
  • Using a spheroid model of breast cancer, the study highlights the tumor-suppressive role of myoepithelial ADAMTS3, whose loss increases luminal cell invasion through the extracellular matrix.
  • The research demonstrates that ADAMTS3 mediates fibronectin degradation, and its absence leads to elevated fibronectin levels, further promoting cancer cell invasion via integrin activation.

Article Abstract

Proteases have long been associated with cancer progression, due to their ability to facilitate invasion upon matrix remodelling. However, proteases are not simply degraders of the matrix, but also play fundamental roles in modulating cellular behaviour through the proteolytic processing of specific substrates. Indeed, proteases can elicit both pro- and anti- tumorigenic effects depending on context. Using a heterocellular spheroid model of breast cancer progression, we demonstrate the repressive function of myoepithelial ADAMTS3, with its loss directing myoepithelial-led invasion of luminal cells through a physiologically relevant matrix. Degradomic analysis, using terminal amine isotopic labelling of substrates (TAILS), combined with functional assays, implicate ADAMTS3 as a mediator of fibronectin degradation. We show further that loss of ADAMTS3 enhances levels of fibronectin in the microenvironment, promoting invasion through canonical integrin α5β1 activation. Our data highlight a tumour suppressive role for ADAMTS3 in early stage breast cancer, and contribute to the growing evidence that proteases can restrain cancer progression.

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Source
http://dx.doi.org/10.1016/j.matbio.2023.06.005DOI Listing

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