EC Number |
Natural Substrates |
---|
3.4.21.B26 | alpha-dystroglycan + H2O |
cleavage site (ANKKPPLPKRVRR312-/-QIHATPTP). Full-length alpha-dystroglycan in the human endometrial epithelium is a barrier for embryo attachment and removal of the N-terminus by proprotein convertase 5/6 regulates receptivity. Removal of alpha-dystroglycan N-terminus is an important posttranslational control of endometrial receptivity and uterine fluid |
3.4.21.B26 | human immunodeficiency virus type 1 Vpr + H2O |
undergoes proteolytic processing at a very well conserved proprotein convertase cleavage site, R85QRR88-/-, proprotein convertases PC5 and PACE4 can efficiently process extracellular Vpr |
3.4.21.B26 | more |
death at birth of the PC5/6-deficient embryos |
3.4.21.B26 | osteopontin + H2O |
Pcsk5/PCSK5 is temporally and spatially expressed with Opn/OPN (Spp1/SPP1) in osteoblasts and osteocytes, indicating that osteopontin could be a physiologically relevant substrate for PC5/6 or PC5/6-activated proteases in bone. Cleavage of osteopontin may modify the function of osteopontin in bone and/or modulate other enzymatic cleavages of osteopontin, leading to alterations in the bone phenotype |
3.4.21.B26 | preprohepcidin + H2O |
key role of the convertases furin, PACE4, PC5 and/or PC7 in the generation and secretion of active hepcidin |
3.4.21.B26 | pro-integrin-alpha5 + H2O |
cleavage of the substrate into its heavy and light chains |
3.4.21.B26 | pro-integrin-alphaV + H2O |
cleavage of the substrate into its heavy and light chains |
3.4.21.B26 | proform bone morphogenetic protein-2 + H2O |
- |
3.4.21.B26 | proform platelet-derived growth factor A + H2O |
activation, the substrate is localized specifically to the apical surface of the luminal and glandular epithelium of uterine endometrium in the receptive phase, but barely detectable in the non-receptive phase |
3.4.21.B26 | protein tyrosine phosphatase kappa + H2O |
the enzyme cleaves the ectodomain of protein tyrosine phosphatase kappa |