An atypical and functionally diverse family of Kunitz-type cysteine serine proteinase inhibitors secreted by the helminth parasite Fasciola hepatica

John Pius Dalton, Krystyna Cwiklinski

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20 Citations (Scopus)

Abstract

Fasciola hepatica is a global parasite of humans and their livestock. Regulation of parasite-secreted cathepsin L-like cysteine proteases associated with virulence is important to fine-tune parasite-host interaction. We uncovered a family of seven Kunitz-type (FhKT) inhibitors dispersed into five phylogenetic groups. The most highly expressed FhKT genes (group FhKT1) are secreted by the newly excysted juveniles (NEJs), the stage responsible for host infection. The FhKT1 inhibitors do not inhibit serine proteases but are potent inhibitors of parasite cathepsins L and host lysosomal cathepsin L, S and K cysteine proteases (inhibition constants10 nM). Their unusual inhibitory properties are due to (a) Leu(15) in the reactive site loop P1 position that sits at the water-exposed interface of the S1 and S1prime subsites of the cathepsin protease, and (b) Arg(19) which forms cation-pi interactions with Trp(291) of the S1 subsite and electrostatic interactions with Asp(125) of the S2 subsite. FhKT1.3 is exceptional, however, as it also inhibits the serine protease trypsin due to replacement of the P1 Leu(15) in the reactive loop with Arg(15). The atypical Kunitz-type inhibitor family likely regulate parasite cathepsin L proteases and or impairs host immune cell activation by blocking lysosomal cathepsin proteases involved in antigen processing and presentation.
Original languageEnglish (Ireland)
Article number20657
JournalScientific Reports
Volume10
Issue number1
DOIs
Publication statusPublished - 1 Nov 2020

Authors (Note for portal: view the doc link for the full list of authors)

  • Authors
  • David Smith, Krystyna Cwiklinski, Heather Jewhurst, Irina G Tikhonova, John P Dalton
  • Smith, D,Cwiklinski, K,Jewhurst, H,Tikhonova, IG,Dalton, JP

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