Targeted Deletion of HAI-1 Increases Prostasin Proteolysis but Decreases Matriptase Proteolysis in Human Keratinocytes

Overview

Journal Hum Cell

Publisher Springer

Specialty Cell Biology

Date 2021 Jan 24

PMID 33486722

Citations 2

Authors

Dajun D Lu

Yayun Gu

Sheng-Wen A Li

Robert J Barndt

Shih-Ming Huang

Jehng-Kang Wang

Hui Chen Su

Michael D Johnson

Chen-Yong Lin

Affiliations

Soon will be listed here.

Abstract

Epidermal differentiation and barrier function require well-controlled matriptase and prostasin proteolysis, in which the Kunitz-type serine protease inhibitor HAI-1 represents the primary enzymatic inhibitor for both proteases. HAI-1, however, also functions as a chaperone-like protein necessary for normal matriptase synthesis and intracellular trafficking. Furthermore, other protease inhibitors, such as antithrombin and HAI-2, can also inhibit matriptase and prostasin in solution or in keratinocytes. It remains unclear, therefore, whether aberrant increases in matriptase and prostasin enzymatic activity would be the consequence of targeted deletion of HAI-1 and so subsequently contribute to the epidermal defects observed in HAI-1 knockout mice. The impact of HAI-1 deficiency on matriptase and prostasin proteolysis was, here, investigated in HaCaT human keratinocytes. Our results show that HAI-1 deficiency causes an increase in prostasin proteolysis via increased protein expression and zymogen activation. It remains unclear, however, whether HAI-1 deficiency increases "net" prostasin enzymatic activity because all of the activated prostasin was detected in complexes with HAI-2, suggesting that prostasin enzymatic activity is still under tight control in HAI-1-deficient keratinocytes. Matriptase proteolysis is, however, unexpectedly suppressed by HAI-1 deficiency, as manifested by decreases in zymogen activation, shedding of active matriptase, and matriptase-dependent prostasin zymogen activation. This suppressed proteolysis results mainly from the reduced ability of HAI-1-deficient HaCaT cells to activate matriptase and the rapid inhibition of nascent active matriptase by HAI-2 and other yet-to-be-identified protease inhibitors. Our study provides novel insights with opposite impacts by HAI-1 deficiency on matriptase versus prostasin proteolysis in keratinocytes.

Citing Articles

N-glycosylation on Asn-57 is required for the correct HAI-2 protein folding and protease inhibitory activity.

Huang N, Wang Q, Chen C, Hu J, Wang J, Chang P Glycobiology. 2023; 33(3):203-214.

PMID: 36637420 PMC: 10114645. DOI: 10.1093/glycob/cwad002.

Understanding HAIs: Ally proteins in the fight against cancer.

Nonboe A, Bald Z, Vogel L FEBS J. 2022; 289(12):3416-3418.

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