Journal of Enzyme Inhibition and Medicinal Chemistry (Jan 2019)

Aberrant regulation favours matriptase proteolysis in neoplastic B-cells that co-express HAI-2

  • Yi-Lin Chiu,
  • Yi-Ying Wu,
  • Robert B. Barndt,
  • Yee Hui Yeo,
  • Yu-Wen Lin,
  • Hou-Ping Sytwo,
  • Huan-Cheng Liu,
  • Yuan Xu,
  • Bailing Jia,
  • Jehng-Kang Wang,
  • Michael D. Johnson,
  • Chen-Yong Lin

DOI
https://doi.org/10.1080/14756366.2019.1577831
Journal volume & issue
Vol. 34, no. 1
pp. 692 – 702

Abstract

Read online

Matriptase is ectopically expressed in neoplastic B-cells, in which matriptase activity is enhanced by negligible expression of its endogenous inhibitor, hepatocyte growth factor activator inhibitor (HAI)-1. HAI-1, however, is also involved in matriptase synthesis and intracellular trafficking. The lack of HAI-1 indicates that other related inhibitor, such as HAI-2, might be expressed. Here, we show that HAI-2 is commonly co-expressed in matriptase-expressing neoplastic B-cells. The level of active matriptase shed after induction of matriptase zymogen activation in 7 different neoplastic B-cells was next determined and characterised. Our data reveal that active matriptase can only be generated and shed by those cells able to activate matriptase and in a rough correlation with the levels of matriptase protein. While HAI-2 can potently inhibit matriptase, the levels of active matriptase are not proportionally suppressed in those cells with high HAI-2. Our survey suggests that matriptase proteolysis might aberrantly remain high in neoplastic B-cells regardless of the levels of HAI-2.

Keywords