Activation and enzymatic characterization of recombinant human kallikrein 8

Kishi, Tadaaki; Cloutier, Sylvain M.; Kündig, Christoph; Deperthes, David; Diamandis, Eleftherios P.

doi:10.1515/bc.2006.091

Cited by 29 publications

(41 citation statements)

References 55 publications

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“…The consensus site for KLK8 has not been elucidated in full detail. However, based on sequence prediction and in vitro peptide proteolysis analysis, it is clear that KLK8 has a trypsin-like specificity (66,68,74,75). The P1 position contains a positively charged amino acid, with Arg preferable over Lys (68,74).…”

Section: Discussionmentioning

confidence: 99%

“…However, based on sequence prediction and in vitro peptide proteolysis analysis, it is clear that KLK8 has a trypsin-like specificity (66,68,74,75). The P1 position contains a positively charged amino acid, with Arg preferable over Lys (68,74). In addition, a binding site of four amino acids in the substrate confers specificity with hydrophobic residues in P2 and P3 and preferably Ser/Thr or Phe/Tyr at P1= (64).…”

Section: Discussionmentioning

confidence: 99%

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Kallikrein-8 Proteolytically Processes Human Papillomaviruses in the Extracellular Space To Facilitate Entry into Host Cells

Cerqueira

Ventayol

Vogeley

et al. 2015

J Virol

104

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The entry of human papillomaviruses into host cells is a complex process. It involves conformational changes at the cell surface, receptor switching, internalization by a novel endocytic mechanism, uncoating in endosomes, trafficking of a subviral complex to the Golgi complex, and nuclear entry during mitosis. Here, we addressed how the stabilizing contacts in the capsid of human papillomavirus 16 (HPV16) may be reversed to allow uncoating of the viral genome. Using biochemical and cell-biological analyses, we determined that the major capsid protein L1 underwent proteolytic cleavage during entry. In addition to a dispensable cathepsin-mediated proteolysis that occurred likely after removal of capsomers from the subviral complex in endosomes, at least two further proteolytic cleavages of L1 were observed, one of which was independent of the low-pH environment of endosomes. This cleavage occurred extracellularly. Further analysis showed that the responsible protease was the secreted trypsin-like serine protease kallikrein-8 (KLK8) involved in epidermal homeostasis and wound healing. Required for infection, the cleavage was facilitated by prior interaction of viral particles with heparan sulfate proteoglycans. KLK8-mediated cleavage was crucial for further conformational changes exposing an important epitope of the minor capsid protein L2. Occurring independently of cyclophilins and of furin that mediate L2 exposure, KLK8-mediated cleavage of L1 likely facilitated access to L2, located in the capsid lumen, and potentially uncoating. Since HPV6 and HPV18 also required KLK8 for entry, we propose that the KLK8-dependent entry step is conserved. IMPORTANCEOur analysis of the proteolytic processing of incoming HPV16, an etiological agent of cervical cancer, demonstrated that the capsid is cleaved extracellularly by a serine protease active during wound healing and that this cleavage was crucial for infection. The cleavage of L1 is one of at least four structural alterations that prime the virus extracellularly for receptor switching, internalization, and possibly uncoating. This step was also important for HPV6 and HPV18, which may suggest that it is conserved among the papillomaviruses. This study advances the understanding of how HPV16 initially infects cells, strengthens the notion that wounding facilitates infection of epidermal tissue, and may help the development of antiviral measures. Human papillomaviruses (HPVs) comprise a large family of small, nonenveloped DNA viruses with transforming potential. HPVs selectively infect basal keratinocytes of stratified skin and mucosal epithelia and persist, mostly without clinical symptoms, in virtually every part of the human skin. The biological costs of HPV persistence range from benign papilloma and genital warts over preneoplastic lesions to anogenital or oropharyngeal cancers (1). In fact, infection by the so-called "high-risk" HPV causes about 5% of all human cancers (2). Of these, cervical cancers are the most prevalent. However, HPV-associated oropharyngea...

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Kallikrein-8 Proteolytically Processes Human Papillomaviruses in the Extracellular Space To Facilitate Entry into Host Cells

Cerqueira

Ventayol

Vogeley

et al. 2015

J Virol

104

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“…Its activity is inhibited by typical serine protease inhibitors [6,27]. This suggests that it is implicated in extracellular matrix protein degradation in the areas surrounding KLK8-producing cells [6].…”

Section: Discussionmentioning

confidence: 99%

Human Kallikrein 8 Expression in Salivary Gland Tumors

Darling

Tsai

Jackson-Boeters

et al. 2008

Head and Neck Pathol

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The human kallikrein 8 protein (KLK8) is expressed in many normal tissues including esophagus, skin, testis, tonsil, kidney, breast, and salivary gland, and is found in biological fluids including breast milk, amniotic fluid, seminal fluid and serum. It has also been shown to be a biomarker and prognostic factor for breast cancer. The aim of this study was to determine whether KLK8 is expressed in salivary gland tissues and salivary gland tumors (both benign and malignant), in order to compare normal with tumor tissues. Pleomorphic adenomas, adenoid cystic carcinomas, polymorphous low grade adenocarcinomas, acinic cell carcinomas, mucoepidermoid carcinomas, and adenocarcinomas NOS of both minor and major salivary glands were examined. The results of this study indicate that most salivary gland tumors show high levels of expression of KLK8.

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“…Not detected ND (Rajapakse et al, 2005;Kishi et al, 2006;Stefansson et al, 2008) 9 (Luo et al, 2001a;Petraki et al, 2002Petraki et al, , 2003a 11 Tryptic Arg SF; N; B Up c (Mitsui et al, 2000;) Nakamura et al, 2003; Brought to you by | University of Queensland -UQ Library Authenticated Download Date | 9/14/15 3:38 AM (Memari et al, 2007a; 13 Tryptic Arg)Lys SF; N; B; C Down Kapadia et al, 2004;(Kapadia et al, 2003;Petraki et al, 2003a,b;Borgono et al, 2007a) Shaw and 14 Tryptic Arg)Lys, Tyr, Phe, Tyr, Gly, Leu SF; N Up c (Brattsand et al, 2005;Felber et al, 2005;(Borgono et al, 2007c;Diamandis, 2007) Oikonomopoulou et al, 2006;Borgono et al, 2007a,b,c;Stefansson et al, 2008) …”

Section: Arg Lysmentioning

confidence: 99%

“…In prostate cancer, as in other diseases, this dysregulation is mediated by changes in levels of various factors including metal ions (e.g., Zn 2q ) and proteinaceous inhibitors. For example, in prostate and other tissues, Zn 2q ions provide an effective means of regulating the action of several KLK and other trypsin-like enzymes including KLK2 (Lovgren et al, 1999a), KLK4 (Debela et al, 2006a), KLK5 Debela et al, 2007), KLK8 (Kishi et al, 2006), KLK12 (Memari et al, 2007a) and KLK14 (Borgono et al, 2007c), as well as prostasin (Shipway et al, 2004) and uPA (Ishii et al, 2001). Of relevance to normal prostate physiology as well as prostate cancer, Zn 2q levels are up to 10-fold higher in normal prostate than in other tissues (Kavanagh, 1985), while there is a 10-to 20-fold decrease in these levels in patients with advanced prostate cancer (Zaichick et al, 1996(Zaichick et al, , 1997.…”

Section: Dysregulated Tryptic Proteolytic Activitymentioning

confidence: 99%

Prostatic trypsin-like kallikrein-related peptidases (KLKs) and other prostate-expressed tryptic proteinases as regulators of signalling via proteinase-activated receptors (PARs)

Ramsay

Reid

Adams

et al. 2008

BCHM

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The prostate is a site of high expression of serine proteinases including members of the kallikrein-related peptidase (KLK) family, as well as other secreted and membrane-anchored serine proteinases. It has been known for some time that members of this enzyme family elicit cellular responses by acting directly on cells. More recently, it has been recognised that for serine proteinases with specificity for cleavage after arginine and lysine residues (trypsin-like or tryptic enzymes) these cellular responses are often mediated by cleavage of members of the proteinase-activated receptor (PAR) family -a four member sub-family of G protein-coupled receptors. Here, we review the expression of PARs in prostate, the ability of prostatic trypsin-like KLKs and other prostateexpressed tryptic enzymes to cleave PARs, as well as the prostate cancer-associated consequences of PAR activation. In addition, we explore the dysregulation of trypsin-like serine proteinase activity through the loss of normal inhibitory mechanisms and potential interactions between these dysregulated enzymes leading to aberrant PAR activation, intracellular signalling and cancer-promoting cellular changes.

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Activation and enzymatic characterization of recombinant human kallikrein 8

Cited by 29 publications

References 55 publications

Kallikrein-8 Proteolytically Processes Human Papillomaviruses in the Extracellular Space To Facilitate Entry into Host Cells

Kallikrein-8 Proteolytically Processes Human Papillomaviruses in the Extracellular Space To Facilitate Entry into Host Cells

Human Kallikrein 8 Expression in Salivary Gland Tumors

Prostatic trypsin-like kallikrein-related peptidases (KLKs) and other prostate-expressed tryptic proteinases as regulators of signalling via proteinase-activated receptors (PARs)

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