Keratinization (Homo sapiens)

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2916363, 12, 22, 3517, 5048811434, 43, 5311, 18, 44, 564, 109, 27, 547, 13, 412, 2557555924, 5832, 3649311352844, 46638, 42, 4715, 3920, 284836, 56553545cytosolcornified envelopecytosolCDSN TGM1 KLK13LCE3C RCOOHDSC1 CDSN RPTN CASP14DSC3 LCE6A IVL PPL LCE1A LCE5A Keratin type I, hair specific SPRR2D Keratin type II, hair follicle specific TGM1 LCE1D CDSN LCE2D Cell surface LCE1A LELP1 TCHH CDSNKRTAP29-1 DSG3 DSG4 DSG4 Keratin unit lengthfilamentLCE3C CHOL ST14SPRR2D LCE1E Keratin type II, epithelial TAGsH2OTCHH CASP14(153-242) LCE1D Keratin type I, epithelial Keratin tonofilament:Desmosome network LCE1C ceramide PPL LCE1D ceramide Mature cornifiedenvelopeLCE1F DSG4 PI3(61-117) LCE1E EVPL PKP1 SPINK6 LCE1D ceramide Lamellar bodyKLK5:SPINK5RPTN SPINK6 PKP1 KRTAP5s CSTA DSG4 PPL LCE3D IVL LCE2C TGM1 SPRR2F LCE3E fatty acid Cell surface Keratin type II, hair follicle specific SPRR2D IVL PPL SPRR1A SPRR2B DSG3 SPRR2B H2OKRTAP21s KLK14:SPINK6SPRR3 Cell surface SPINK6KLK5 SPRR2E DSG1 LCE3B DSG3 CELA2A propeptideSPRR1B Cornified envelopeKRTAP25-1 LCE2A SPINK6KLK5LCE4A EVPL SPRsproKLK5FLG(?-?) LCE3A TGM1EVPL LCE2C PPL SPRR2B ceramide SPRR2F fatty acid SPRR2A KRTAP8-1 DSG2 LIPK CELA2ASPRR3 LCE2B SPRR1A LCE1A KLK5:SPINK9Keratin type I, hair specific DesmosomeTGM1 LCE3E PCSK6 SPRR3 PPL SPRR1A LCE5A DSG2 EVPL LCE6A LCE1B CHOL KLK12 EVPL:PPL:CellsurfaceH2OKeratin type II, epithelial PI3(61-117) Late envelopeproteinsSPRR2A LOR CHOL CSTA SPRR3 FLG-Keratin filamentnetworkCytoplasmicprofilaggrinprocessingproteasesKeratin type I, hair specific Keratin type II, hair specific SPRR2E SPRR3 TGM5 Keratin type II, epithelial TCHH CHOL Cornifiedenvelope:CDSNSPRR1B IVL DSC2 SPRR2G SPRR2A SPRR3 proCELA2APKP4 IVL:TGM1:CellsurfaceCell surface EVPL:PPLSPRR2B KLK5 CAPNS1 LCE3D KAZNLCE4A LCE1B TGM1 LCE2A Late cornifiedenvelopeSPRR1A FLG(?-?):Keratintonofilament:DesmosomeCASP14(6-146) PKP4 KLK13 CSTA PKP1 PKP2 CDSN KLK14 KLK13:SPINK6KRTAP17-1 SPRR2B Keratin tonofilamentDSC2 LOR JUP PI3(61-117) SPINK6 KRTAP12s fatty acid SPRR1A KRTAP2s DSG1 SPRR3 LCE3A Keratin type IISPRR2E SPRR2A Keratin type I, hair specific SPRR2G SPINK5(490-624)SPRR2F DSC1 LCE4A EVPL:PPL:IVL:TGM1:Cell surfaceSPRR2G SPRR1B LCE3C Minor CE proteinsLCE1B KLK8RPTN RPTN LCE2B SPRR2G PKP1 JUP FLG(1-4061)TCHH SPRR2A Keratin type I, hair follicle specific Keratin type IKRTAP4s KRTAP13s FLG-Keratin filament network KLK5 SPRR2E SPRR2G Keratin type II, hair specific SPRR1B SPRR1B SPRR2F LCE1F SPRR2D SPINK6 SPRR2E LCE1F Keratin associatedproteinsCell surface PKP2 SPRR1B PKP4 PPL LOR PRSS8(45-322) LCE2A PPLKLK5 propeptideLCE1A TGM1 CASP14(153-242) DSG3 SPRR2G EVPL H+LCE2D SPINK5(490-624) SPRR2D SPRR2F Mature cornifiedenvelopeSPINK9LCE5A Keratin tonofilament JUP PKP3 FLG(?-?)DSG1 Keratin type II, hair follicle specific LCE3B LCE2B PI3(61-117) Keratin type I, hair specific keratinocyte LIPsLCE2D LCE2D PKP3 FLG-Keratin filament network Keratin type II, hair follicle specific DSP DSC2 Keratin type I, epithelial DSC1 Keratin type I, epithelial CSTA SPINK5(490-624)IVL KRTAP9s FURIN proKLK8TGM1 LCE5A SPRR2A LCE3B Keratin type I, epithelial IVL LCE3C SPRR2D LCE2B SPINK9 Keratintonofilament:DesmosomeDSG2 Keratin type I, hair follicle specific LCE1C DSG1 Cell surface PKP3 PERP KRTAP16-1 KRTAP27-1 EVPL Keratin tonofilament LCE1C LCE1F Keratin type II, hair follicle specific CSTA SPRR2E CSTA LCE3D DSG2 Keratin tonofilament:Desmosome network LCE3D PKP4 DSC1 KRTAP19s EVPL PERPKeratin type II, hair specific DSP Cell surfaceLOR DAGsPPL LCE3A Cell surface KRTAP11-1 CASP14(6-146) LIPN DSC2 CSTA LCE2C KLK12PKP2 SPRR1A LOR Keratin type I, hair follicle specific DSP SPRR2G KLK8 propeptideKeratin type I, hair follicle specific DSC3 DSC3 FLG-Keratin filament network Keratin type I, hair follicle specific EVPLKeratin tetramerPI3(61-117) Keratin type II, hair specific MembraneprofilaggrinprocessingproteasesSPRR2E ceramide LCE1E PI3(61-117) KLK5:SPINK6KLK12:SPINK6TCHH Ca2+ Cell surface KRTAP24-1 JUP PPL LCE1E SPRR2F LIPJ RPTN H2OLCE6A KLK5IVL LCE1C Early cornifiedenvelopeSPRR2D DSP TGM1:Ca2+, TGM5:Ca2+fatty acid KRTAP3s KAZN Keratin type I, epithelial TCHH CELA2A LCE4A Keratintonofilament:Keratin associated proteins polymerEVPL Desmosome:PERPDSC3 fatty acid RPTN CHOL Keratin type II, epithelial LIPM KRTAP1s PKP2 Keratin type II, epithelial KRTAP26-1 PI3(61-117) LCE3E LCE3A CAPN1 Keratin filamentunitsKeratin heterodimerLCE2C LELP1 IVL EVPL RPTN KLK5 KLK14SPRR2B ceramide Ca2+ LCE2A FLG-Keratin filament network Keratin filamentPPL TCHH PRSS8(33-44) CHOL SPRR2B KAZN:PPLTGM1 LOR SPRR2F LCE3E LELP1 Keratin type II, hair specific ST14 LCE1B LCE6A SPRR1B IVLKRTAP20s KRTAP10s KRTAP6s TGM1 PKP3 LORSPRR1A LELP1 fatty acid SPRR2A LCE3B 5523, 40485526, 5215, 393023, 40372126, 52444815, 395, 193348364823, 4023, 4033374851305, 1923, 404823, 4015, 394848430


Description

Keratins are the major structural protein of vertebrate epidermis, constituting up to 85% of a fully differentiated keratinocyte (Fuchs 1995). Keratins belong to a superfamily of intermediate filament (IF) proteins that form alpha-helical coiled-coil dimers, which associate laterally and end-to-end to form approximately 10 nm diameter filaments. Keratin filaments are heteropolymeric, formed from equal amounts of acidic type I and basic /neutral type 2 keratins. Humans have 54 keratin genes (Schweitzer et al. 2006). They have highly specific expression patterns, related to the epithelial type and stage of differentiation. Roughly half of human keratins are specific to hair follicles (Langbein & Schweizer 2005). Keratin filaments bundle into tonofilaments that span the cytoplasm and bind to desmosomes and other cell membrane structures (Waschke 2008). This reflects their primary function, maintaining the mechanical stability of individual cells and epithelial tissues (Moll et al. 2008). View original pathway at:Reactome.

Comments

Reactome-Converter 
Pathway is converted from Reactome ID: 6805567
Reactome-version 
Reactome version: 63
Reactome Author 
Reactome Author: Jupe, Steve

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Bibliography

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History

View all...
CompareRevisionActionTimeUserComment
114957view16:48, 25 January 2021ReactomeTeamReactome version 75
113401view11:47, 2 November 2020ReactomeTeamReactome version 74
112605view15:58, 9 October 2020ReactomeTeamReactome version 73
101521view11:38, 1 November 2018ReactomeTeamreactome version 66
101057view21:20, 31 October 2018ReactomeTeamreactome version 65
100588view19:54, 31 October 2018ReactomeTeamreactome version 64
100137view16:40, 31 October 2018ReactomeTeamreactome version 63
99687view15:09, 31 October 2018ReactomeTeamreactome version 62 (2nd attempt)
99277view12:45, 31 October 2018ReactomeTeamreactome version 62
93483view11:24, 9 August 2017ReactomeTeamNew pathway

External references

DataNodes

View all...
NameTypeDatabase referenceComment
CAPN1 ProteinP07384 (Uniprot-TrEMBL)
CAPNS1 ProteinP04632 (Uniprot-TrEMBL)
CASP14(153-242) ProteinP31944 (Uniprot-TrEMBL)
CASP14(6-146) ProteinP31944 (Uniprot-TrEMBL)
CASP14ComplexR-HSA-8847680 (Reactome)
CDSN ProteinQ15517 (Uniprot-TrEMBL)
CDSNProteinQ15517 (Uniprot-TrEMBL)
CELA2A ProteinP08217 (Uniprot-TrEMBL)
CELA2A propeptideProteinP08217 (Uniprot-TrEMBL)
CELA2AProteinP08217 (Uniprot-TrEMBL)
CHOL MetaboliteCHEBI:16113 (ChEBI)
CSTA ProteinP01040 (Uniprot-TrEMBL)
Ca2+ MetaboliteCHEBI:29108 (ChEBI)
Cell surface R-ALL-983438 (Reactome) This entity is intended to represent any molecule that might be at the outer cell surface of any cell, host or microbial.
Cell surfaceR-ALL-983438 (Reactome) This entity is intended to represent any molecule that might be at the outer cell surface of any cell, host or microbial.
Cornified envelope:CDSNComplexR-HSA-6814723 (Reactome)
Cornified envelopeComplexR-HSA-6814278 (Reactome)
Cytoplasmic

profilaggrin processing

proteases
ComplexR-HSA-8934797 (Reactome)
DAGsMetaboliteCHEBI:18035 (ChEBI)
DSC1 ProteinQ08554 (Uniprot-TrEMBL)
DSC2 ProteinQ02487 (Uniprot-TrEMBL)
DSC3 ProteinQ14574 (Uniprot-TrEMBL)
DSG1 ProteinQ02413 (Uniprot-TrEMBL)
DSG2 ProteinQ14126 (Uniprot-TrEMBL)
DSG3 ProteinP32926 (Uniprot-TrEMBL)
DSG4 ProteinQ86SJ6 (Uniprot-TrEMBL)
DSP ProteinP15924 (Uniprot-TrEMBL)
Desmosome:PERPComplexR-HSA-8848046 (Reactome)
DesmosomeComplexR-HSA-6814388 (Reactome)
EVPL ProteinQ92817 (Uniprot-TrEMBL)
EVPL:PPL:Cell surfaceComplexR-HSA-6814188 (Reactome)
EVPL:PPL:IVL:TGM1:Cell surfaceComplexR-HSA-6814177 (Reactome)
EVPL:PPLComplexR-HSA-6814178 (Reactome)
EVPLProteinQ92817 (Uniprot-TrEMBL)
Early cornified envelopeComplexR-HSA-6814285 (Reactome)
FLG(1-4061)ProteinP20930 (Uniprot-TrEMBL)
FLG(?-?) ProteinP20930 (Uniprot-TrEMBL)
FLG(?-?):Keratin tonofilament:DesmosomeComplexR-HSA-8942225 (Reactome)
FLG(?-?)ProteinP20930 (Uniprot-TrEMBL)
FLG-Keratin filament networkR-HSA-6814323 (Reactome)
FLG-Keratin filament network R-HSA-6814323 (Reactome)
FURIN ProteinP09958 (Uniprot-TrEMBL)
H+MetaboliteCHEBI:15378 (ChEBI)
H2OMetaboliteCHEBI:15377 (ChEBI)
IVL ProteinP07476 (Uniprot-TrEMBL)
IVL:TGM1:Cell surfaceComplexR-HSA-6814746 (Reactome)
IVLProteinP07476 (Uniprot-TrEMBL)
JUP ProteinP14923 (Uniprot-TrEMBL)
KAZN ProteinQ674X7 (Uniprot-TrEMBL)
KAZN:PPLComplexR-HSA-6814328 (Reactome)
KAZNProteinQ674X7 (Uniprot-TrEMBL)
KLK12 ProteinQ9UKR0 (Uniprot-TrEMBL)
KLK12:SPINK6ComplexR-HSA-8850791 (Reactome)
KLK12ProteinQ9UKR0 (Uniprot-TrEMBL)
KLK13 ProteinQ9UKR3 (Uniprot-TrEMBL)
KLK13:SPINK6ComplexR-HSA-8850785 (Reactome)
KLK13ProteinQ9UKR3 (Uniprot-TrEMBL)
KLK14 ProteinQ9P0G3 (Uniprot-TrEMBL)
KLK14:SPINK6ComplexR-HSA-8850790 (Reactome)
KLK14ProteinQ9P0G3 (Uniprot-TrEMBL)
KLK5 ProteinQ9Y337 (Uniprot-TrEMBL)
KLK5 propeptideProteinQ9Y337 (Uniprot-TrEMBL)
KLK5:SPINK5ComplexR-HSA-8849656 (Reactome)
KLK5:SPINK6ComplexR-HSA-8850796 (Reactome)
KLK5:SPINK9ComplexR-HSA-8850817 (Reactome)
KLK5ProteinQ9Y337 (Uniprot-TrEMBL)
KLK8 propeptideProteinO60259 (Uniprot-TrEMBL)
KLK8ProteinO60259 (Uniprot-TrEMBL)
KRTAP10s R-HSA-6810289 (Reactome)
KRTAP11-1 ProteinQ8IUC1 (Uniprot-TrEMBL)
KRTAP12s R-HSA-6810253 (Reactome)
KRTAP13s R-HSA-6810256 (Reactome)
KRTAP16-1 ProteinA8MUX0 (Uniprot-TrEMBL)
KRTAP17-1 ProteinQ9BYP8 (Uniprot-TrEMBL)
KRTAP19s R-HSA-6810257 (Reactome)
KRTAP1s R-HSA-6809848 (Reactome)
KRTAP20s R-HSA-6810282 (Reactome)
KRTAP21s R-HSA-6810272 (Reactome)
KRTAP24-1 ProteinQ3LI83 (Uniprot-TrEMBL)
KRTAP25-1 ProteinQ3LHN0 (Uniprot-TrEMBL)
KRTAP26-1 ProteinQ6PEX3 (Uniprot-TrEMBL)
KRTAP27-1 ProteinQ3LI81 (Uniprot-TrEMBL)
KRTAP29-1 ProteinA8MX34 (Uniprot-TrEMBL)
KRTAP2s R-HSA-6809961 (Reactome)
KRTAP3s R-HSA-6809847 (Reactome)
KRTAP4s R-HSA-6809956 (Reactome)
KRTAP5s R-HSA-6810283 (Reactome)
KRTAP6s R-HSA-6810263 (Reactome)
KRTAP8-1 ProteinQ8IUC2 (Uniprot-TrEMBL)
KRTAP9s R-HSA-6809972 (Reactome)
Keratin tonofilament:DesmosomeComplexR-HSA-6814735 (Reactome)
Keratin tonofilament:Keratin associated proteins polymerR-HSA-8848101 (Reactome)
Keratin associated proteinsComplexR-HSA-6809850 (Reactome)
Keratin filament unitsComplexR-HSA-6809659 (Reactome)
Keratin filamentR-HSA-6809669 (Reactome)
Keratin heterodimerComplexR-HSA-6809611 (Reactome)
Keratin tetramerComplexR-HSA-6809664 (Reactome)
Keratin tonofilament R-HSA-6809668 (Reactome)
Keratin tonofilament:Desmosome network R-HSA-6814760 (Reactome)
Keratin tonofilament:Desmosome network R-HSA-8847708 (Reactome)
Keratin tonofilamentR-HSA-6809668 (Reactome)
Keratin type I, epithelial R-HSA-6809602 (Reactome)
Keratin type I, hair follicle specific R-HSA-6809609 (Reactome)
Keratin type I, hair specific R-HSA-6809597 (Reactome)
Keratin type II, epithelial R-HSA-6809639 (Reactome)
Keratin type II, hair follicle specific R-HSA-6809641 (Reactome)
Keratin type II, hair specific R-HSA-6809629 (Reactome)
Keratin type IIComplexR-HSA-6809612 (Reactome)
Keratin type IComplexR-HSA-6809600 (Reactome)
Keratin unit length filamentComplexR-HSA-6809673 (Reactome)
LCE1A ProteinQ5T7P2 (Uniprot-TrEMBL)
LCE1B ProteinQ5T7P3 (Uniprot-TrEMBL)
LCE1C ProteinQ5T751 (Uniprot-TrEMBL)
LCE1D ProteinQ5T752 (Uniprot-TrEMBL)
LCE1E ProteinQ5T753 (Uniprot-TrEMBL)
LCE1F ProteinQ5T754 (Uniprot-TrEMBL)
LCE2A ProteinQ5TA79 (Uniprot-TrEMBL)
LCE2B ProteinO14633 (Uniprot-TrEMBL)
LCE2C ProteinQ5TA81 (Uniprot-TrEMBL)
LCE2D ProteinQ5TA82 (Uniprot-TrEMBL)
LCE3A ProteinQ5TA76 (Uniprot-TrEMBL)
LCE3B ProteinQ5TA77 (Uniprot-TrEMBL)
LCE3C ProteinQ5T5A8 (Uniprot-TrEMBL)
LCE3D ProteinQ9BYE3 (Uniprot-TrEMBL)
LCE3E ProteinQ5T5B0 (Uniprot-TrEMBL)
LCE4A ProteinQ5TA78 (Uniprot-TrEMBL)
LCE5A ProteinQ5TCM9 (Uniprot-TrEMBL)
LCE6A ProteinA0A183 (Uniprot-TrEMBL)
LELP1 ProteinQ5T871 (Uniprot-TrEMBL)
LIPJ ProteinQ5W064 (Uniprot-TrEMBL)
LIPK ProteinQ5VXJ0 (Uniprot-TrEMBL)
LIPM ProteinQ5VYY2 (Uniprot-TrEMBL)
LIPN ProteinQ5VXI9 (Uniprot-TrEMBL)
LOR ProteinP23490 (Uniprot-TrEMBL)
LORProteinP23490 (Uniprot-TrEMBL)
Lamellar bodyComplexR-ALL-6814274 (Reactome)
Late cornified envelopeComplexR-HSA-6814275 (Reactome)
Late envelope proteinsComplexR-HSA-6814261 (Reactome)
Mature cornified envelopeComplexR-HSA-6814763 (Reactome)
Mature cornified envelopeComplexR-HSA-8847742 (Reactome)
Membrane

profilaggrin processing

proteases
ComplexR-HSA-8849785 (Reactome)
Minor CE proteinsComplexR-HSA-6814197 (Reactome)
PCSK6 ProteinP29122 (Uniprot-TrEMBL)
PERP ProteinQ96FX8 (Uniprot-TrEMBL)
PERPProteinQ96FX8 (Uniprot-TrEMBL)
PI3(61-117) ProteinP19957 (Uniprot-TrEMBL)
PKP1 ProteinQ13835 (Uniprot-TrEMBL)
PKP2 ProteinQ99959 (Uniprot-TrEMBL)
PKP3 ProteinQ9Y446 (Uniprot-TrEMBL)
PKP4 ProteinQ99569 (Uniprot-TrEMBL)
PPL ProteinO60437 (Uniprot-TrEMBL)
PPLProteinO60437 (Uniprot-TrEMBL)
PRSS8(33-44) ProteinQ16651 (Uniprot-TrEMBL)
PRSS8(45-322) ProteinQ16651 (Uniprot-TrEMBL)
RCOOHMetaboliteCHEBI:33575 (ChEBI)
RPTN ProteinQ6XPR3 (Uniprot-TrEMBL)
SPINK5(490-624) ProteinQ9NQ38 (Uniprot-TrEMBL)
SPINK5(490-624)ProteinQ9NQ38 (Uniprot-TrEMBL)
SPINK6 ProteinQ6UWN8 (Uniprot-TrEMBL)
SPINK6ProteinQ6UWN8 (Uniprot-TrEMBL)
SPINK9 ProteinQ5DT21 (Uniprot-TrEMBL)
SPINK9ProteinQ5DT21 (Uniprot-TrEMBL)
SPRR1A ProteinP35321 (Uniprot-TrEMBL)
SPRR1B ProteinP22528 (Uniprot-TrEMBL)
SPRR2A ProteinP35326 (Uniprot-TrEMBL)
SPRR2B ProteinP35325 (Uniprot-TrEMBL)
SPRR2D ProteinP22532 (Uniprot-TrEMBL)
SPRR2E ProteinP22531 (Uniprot-TrEMBL)
SPRR2F ProteinQ96RM1 (Uniprot-TrEMBL)
SPRR2G ProteinQ9BYE4 (Uniprot-TrEMBL)
SPRR3 ProteinQ9UBC9 (Uniprot-TrEMBL)
SPRsComplexR-HSA-6810840 (Reactome)
ST14 ProteinQ9Y5Y6 (Uniprot-TrEMBL)
ST14ProteinQ9Y5Y6 (Uniprot-TrEMBL)
TAGsMetaboliteCHEBI:17855 (ChEBI)
TCHH ProteinQ07283 (Uniprot-TrEMBL)
TGM1 ProteinP22735 (Uniprot-TrEMBL)
TGM1:Ca2+, TGM5:Ca2+ComplexR-HSA-6814175 (Reactome)
TGM1ProteinP22735 (Uniprot-TrEMBL)
TGM5 ProteinO43548 (Uniprot-TrEMBL)
ceramide MetaboliteCHEBI:17761 (ChEBI)
fatty acid MetaboliteCHEBI:35366 (ChEBI)
keratinocyte LIPsComplexR-HSA-6789317 (Reactome)
proCELA2AProteinP08217 (Uniprot-TrEMBL)
proKLK5ProteinQ9Y337 (Uniprot-TrEMBL)
proKLK8ProteinO60259 (Uniprot-TrEMBL)

Annotated Interactions

View all...
SourceTargetTypeDatabase referenceComment
CASP14mim-catalysisR-HSA-6814387 (Reactome)
CDSNR-HSA-6814734 (Reactome)
CELA2A propeptideArrowR-HSA-8849857 (Reactome)
CELA2AArrowR-HSA-8849857 (Reactome)
Cell surfaceR-HSA-6810899 (Reactome)
Cell surfaceR-HSA-6814187 (Reactome)
Cornified envelope:CDSNArrowR-HSA-6814734 (Reactome)
Cornified envelope:CDSNR-HSA-6814298 (Reactome)
Cornified envelopeArrowR-HSA-6810937 (Reactome)
Cornified envelopeR-HSA-6814734 (Reactome)
Cytoplasmic

profilaggrin processing

proteases
mim-catalysisR-HSA-8934819 (Reactome)
DAGsArrowR-HSA-6789310 (Reactome)
Desmosome:PERPArrowR-HSA-6814695 (Reactome)
DesmosomeR-HSA-6809393 (Reactome)
DesmosomeR-HSA-6814695 (Reactome)
EVPL:PPL:Cell surfaceArrowR-HSA-6814187 (Reactome)
EVPL:PPL:Cell surfaceR-HSA-6810894 (Reactome)
EVPL:PPL:IVL:TGM1:Cell surfaceArrowR-HSA-6810894 (Reactome)
EVPL:PPL:IVL:TGM1:Cell surfaceR-HSA-6811539 (Reactome)
EVPL:PPLArrowR-HSA-6810843 (Reactome)
EVPL:PPLR-HSA-6814187 (Reactome)
EVPLR-HSA-6810843 (Reactome)
Early cornified envelopeArrowR-HSA-6811539 (Reactome)
Early cornified envelopeR-HSA-6810937 (Reactome)
FLG(1-4061)R-HSA-8849797 (Reactome)
FLG(1-4061)R-HSA-8934819 (Reactome)
FLG(?-?):Keratin tonofilament:DesmosomeArrowR-HSA-8942224 (Reactome)
FLG(?-?):Keratin tonofilament:DesmosomeR-HSA-6810357 (Reactome)
FLG(?-?)ArrowR-HSA-8849797 (Reactome)
FLG(?-?)ArrowR-HSA-8934819 (Reactome)
FLG(?-?)R-HSA-8942224 (Reactome)
FLG-Keratin filament networkArrowR-HSA-6810357 (Reactome)
FLG-Keratin filament networkR-HSA-6811539 (Reactome)
H+ArrowR-HSA-8849638 (Reactome)
H2OR-HSA-6789310 (Reactome)
H2OR-HSA-8849826 (Reactome)
H2OR-HSA-8849857 (Reactome)
H2OR-HSA-8850831 (Reactome)
IVL:TGM1:Cell surfaceArrowR-HSA-6810899 (Reactome)
IVL:TGM1:Cell surfaceR-HSA-6810894 (Reactome)
IVLR-HSA-6810899 (Reactome)
KAZN:PPLArrowR-HSA-6814374 (Reactome)
KAZNR-HSA-6814374 (Reactome)
KLK12:SPINK6ArrowR-HSA-8850786 (Reactome)
KLK12R-HSA-8850786 (Reactome)
KLK13:SPINK6ArrowR-HSA-8850797 (Reactome)
KLK13R-HSA-8850797 (Reactome)
KLK14:SPINK6ArrowR-HSA-8850777 (Reactome)
KLK14R-HSA-8850777 (Reactome)
KLK5 propeptideArrowR-HSA-8849826 (Reactome)
KLK5:SPINK5ArrowR-HSA-8849646 (Reactome)
KLK5:SPINK5R-HSA-8849638 (Reactome)
KLK5:SPINK6ArrowR-HSA-8850794 (Reactome)
KLK5:SPINK9ArrowR-HSA-8850818 (Reactome)
KLK5ArrowR-HSA-8849638 (Reactome)
KLK5ArrowR-HSA-8849826 (Reactome)
KLK5R-HSA-8849646 (Reactome)
KLK5R-HSA-8850794 (Reactome)
KLK5R-HSA-8850818 (Reactome)
KLK5mim-catalysisR-HSA-8849857 (Reactome)
KLK5mim-catalysisR-HSA-8850831 (Reactome)
KLK8 propeptideArrowR-HSA-8850831 (Reactome)
KLK8ArrowR-HSA-8850831 (Reactome)
Keratin tonofilament:DesmosomeArrowR-HSA-6809393 (Reactome)
Keratin tonofilament:DesmosomeR-HSA-8942224 (Reactome)
Keratin tonofilament:Keratin associated proteins polymerArrowR-HSA-6809663 (Reactome)
Keratin associated proteinsR-HSA-6809663 (Reactome)
Keratin filament unitsR-HSA-6806610 (Reactome)
Keratin filamentArrowR-HSA-6806610 (Reactome)
Keratin filamentR-HSA-6806629 (Reactome)
Keratin heterodimerArrowR-HSA-6805546 (Reactome)
Keratin heterodimerR-HSA-6805573 (Reactome)
Keratin tetramerArrowR-HSA-6805573 (Reactome)
Keratin tetramerR-HSA-6806613 (Reactome)
Keratin tonofilamentArrowR-HSA-6806629 (Reactome)
Keratin tonofilamentR-HSA-6809393 (Reactome)
Keratin tonofilamentR-HSA-6809663 (Reactome)
Keratin type IIR-HSA-6805546 (Reactome)
Keratin type IR-HSA-6805546 (Reactome)
Keratin unit length filamentArrowR-HSA-6806613 (Reactome)
LORR-HSA-6811539 (Reactome)
Lamellar bodyR-HSA-6810937 (Reactome)
Late cornified envelopeArrowR-HSA-6814298 (Reactome)
Late cornified envelopeR-HSA-6814387 (Reactome)
Late envelope proteinsR-HSA-6814298 (Reactome)
Mature cornified envelopeArrowR-HSA-6814387 (Reactome)
Mature cornified envelopeArrowR-HSA-6814764 (Reactome)
Mature cornified envelopeR-HSA-6814764 (Reactome)
Membrane

profilaggrin processing

proteases
mim-catalysisR-HSA-8849797 (Reactome)
Minor CE proteinsR-HSA-6811539 (Reactome)
PERPR-HSA-6814695 (Reactome)
PPLR-HSA-6810843 (Reactome)
PPLR-HSA-6814374 (Reactome)
R-HSA-6789310 (Reactome) Lipases are enzymes that hydrolyse dietary lipids such as fats, oils and triglycerides. The majority of human lipases are secreted by the pancreas and function mainly in the digestive system. Lipase members K, M and N (LIPK, M and N), however, all appear to play a role in the last step of keratinocyte differentiation where they are proposed to hydrolyse triglycerides to free fatty acids and glycerol which is essential to stratum corneum hydration (Toulza et al. 2007).
R-HSA-6805546 (Reactome) The first step in keratin assembly is the formation of coiled-coil heterodimers consisting of an acidic type I keratin and a basic or neutral type II keratin (Coulombe & Fuchs 1990, Hatzfeld & Webber 1990, Steinert 1990). In humans, the type I keratins are K9-24, K25-28, which are specific to the inner root sheath of hair, and the hair-specific keratins K31-K38. The type II keratins are K1-8, K71-80 and K81-86 (Bragula & Homberger 2009). Binding between dimer pairs is remarkably strong and can form even in 9M urea (Coulombe & Fuchs 1990). The ~50 nm long middle rod region of keratin protein aligns with its partner in a parallel orientation (Pauling & Corey 1953, Hanukoglu & Fuchs 1983, Parry et al. 1985, Steinert et al. 1994). The rod region is sufficient to form a heterodimer and subsequent tetramers, but the assembly of keratin filaments requires the non-helical head and tail regions (Wilson et al. 1992). The assembly of rod domain heterodimers has asymmetric salt bridges, hydrogen bonds and hydrophobic contacts, and surface of the heterodimer interface exhibits a notable charge polarization (Lee et al. 2012).

In vitro, virtually any type I keratin can dimerize with any type II keratin, leading to the formation of 10-nm long filaments (Franke et al. 1983, Hatzfeld et al. 1987). In vivo, the composition of keratin heterodimers is probably determined by expression. Differing keratin combinations are not characteristic of entire tissues, but probably confer particular functional properties to cells and tissue regions (Bragulla & Homberger 2009). Certain combinations are characteristic of a cell type, e.g. K18/K8 in simple epithelia. At least some keratins can be replaced with no loss of functionality of the keratin filament, e.g. K1/K10, K1/K9, K2/K9, K2/K10 in epithelia (Coulombe & Omary 2002). Suprabasal cells of stratified epithelia express different keratin pairs in different tissues, e.g. skin epidermis predominantly expresses K1/K10, the anterior corneal epithelium produces K3/K12, esophageal epithelium produces K4/K13 (Eichner & Kahn 1990) while hyperproliferative suprabasal cells are characterized by K6/K16 (Sun 2006).
R-HSA-6805573 (Reactome) Keratin dimers associate in antiparallel orientation to form tetramers (Wood & Inglis 1984, Quinlan et al. 1984). The rod regions of heterodimers align, but alignment of the head and tail regions differs between keratin types. Soft-keratinizing-cornifying cell keratins are slightly out of phase, by 7-8 amino acids, while keratin heterodimers of hard-keratinizing-cornifying cells are in register and consequently there is no overlap between the head and tail domains when a tetramer is formed (Jones et al. 1997). Protofilament tetramers have a diameter of about 2 nm (Aebi et al. 1983, Eicher & Kahn 1990). Heterodimers and tetramers represent the stable building blocks of larger octamers (Herrmann & Abei 2004) and Unit Length Filaments (ULFs), which have a diameter of 20 nm (Parry et al. 2001, Hermann et al. 2007). The tetramers are stabilized by a hydrophobic stripe exposed at the surface of coiled-coil keratin heterodimers (Bernot et al. 2005).
R-HSA-6806610 (Reactome) Mammalian keratin filaments are produced by the lateral and longitudinal aggregation of subunits, such as tetrameric protofilaments and octameric protofibrils (Aebi et al. 1983). The extent of aggregation depends on the pH and osmolarity of the surrounding cytoplasm (Yamada et al. 2002, Magin et al. 2007). Filaments have a cross-section of 32 keratin molecules (Jones et al. 1997).
R-HSA-6806613 (Reactome) Mammalian keratins form soluble short full-width filaments called unit length full-width particles (Parry et al. 2007), unit length filaments (ULFs) (Herrmann et al. 2002) or intermediate filament-like particles (Steinert 1991). These are formed by the lateral association of tetramers. ULFs are ~ 70 nm long, with a diameter of ~20 nm. The diameter shrinks during formation of filaments (Parry et al. 2001). X-ray diffraction suggests that ULFs are tube-like structures formed from eight tetramers in non-cornified cells (Parry et al. 2007). In cornified hair cells, the tetramers are thought to be arranged in a seven-member ring, with an eighth in the centre (Parry et al. 2007).
R-HSA-6806629 (Reactome) Keratin filaments are packed into bundles of varying diameter, called tonofilament bundles. These are the building blocks of the cytoskeleton in epithelial cells. Each bundle is surrounded by polyribosomes and multivesicular or folded membrane complexes that form a branched, tubular network (Norlen et al. 2003). In the stratum corneum, keratin bundles are thought to pack in a cubic rod pattern (Norlen & Al-Amoudi 2004). In living cells, X-ray diffraction studies of keratin intermediate filaments indicate a filament radius of 5 nm, hexagonal geometric arrangement with an interfilament distance of 14 nm and bundle diameters of 70 nm (Hémonnot et al. 2016).

Keratin filaments can rapidly disassemble and reassemble, allowing flexibility for the cytoskeleton. Keratin building blocks accumulate at the cell periphery near focal adhesions. Polymerization is regulated by signaling molecules, e.g. heat shock proteins, 14-3-3 proteins, kinases and phosphatases (Magin et al. 2007, Kayser et al. 2003).
R-HSA-6809393 (Reactome) Keratin filaments bind cell-cell adhesion complexes such as desmosomes and hemidesmosomes, transferring mechanical forces between cells and maintaining cytoskeletal integrity (Hanakawa et al. 2002). The stability of the tonofilament-desmosome interaction depends, in part, on the type of keratin present in the cell (Loschke et al. 2016).

At the ultrastructural level, desmosomes appear as electron dense discs approximately 0.2-0.5 μm in diameter, which assemble in a mirror-image arrangement at cell-cell interfaces (North et al. 1999, Al-Amoudi et al. 2011, Kowalczyk & Green 2013). Large bundles of filaments extend from the nuclear surface and cell interior out towards the plasma membrane, where they attach to desmosomes by interweaving with the cytoplasmic plaque of the adhesive complex. The head domains of keratins bind the tail domains of desmosomal cadherin molecules such as plakoglobin (Dusek et al. 2007), plectin, periplakin, envoplakin and desmoplakin (Bornslaeger et al. 1996, Kazerounian et al. 2002), thereby anchoring the cytoskeleton to the cell membrane.

The five major desmosomal components are the desmosomal cadherins, represented by desmogleins (DSG1-4) and desmocollins (DSC1-3), the armadillo family members, plakoglobin (PG) and the plakophilins (PKP1-3), and the plakin linker protein desmoplakin (DSP), which anchors the intermediate keratin filaments.

Certain adhesion complex proteins are expressed only when cornification commences. These include desmoglein-1, desmocollin-1, envoplakin, periplakin, plakophilin-1 and corneodesmosin (Candi et al. 2005). This expression is associated with changes in desmosome mophology whereby the cytoplasmic plaque integrates with the cornified envelope (Serre et al. 1991, Simon et al. 2001). Deregulation of desmosome formation can lead to degenerative cutaneous diseases (Brooke et al. 2012, Cirillo 2014).
R-HSA-6809663 (Reactome) Hair consists of three major structural components: the cuticle, the cortex and the central medulla. Approximately 90% of cortical cells contain longitudinally arrayed keratin filaments. These filaments have a surrounding matrix that contains keratin-associated proteins (KAPs) that are involved in the formation of cornified, resilient hair shafts (Shimomura & Ito 2005, Lee et al. 2006, Harland et al., 2010, Gong et al. 2016). KAPs forming extensive disulfide cross-links with keratin filaments (Marshall et al. 1991).

The proliferative cells that give rise to hair fibres are located in the bulb at the base of the hair follicle. As they leave the germinative compartment, trichocytic differentiation begins and in matrix, cuticular, and cortical cells, the genes for keratins and KAPs (KRTAPs) are expressed. In the lower and middle cortex, keratin filaments are embedded in a matrix that consists of KAPs. Based on amino acid composition, three classes of KAPs have been described, the high sulfur KAPs (<30 mol % cysteine content), the ultrahigh sulfur KAPs (>30 mol % cysteine content), and the high tyrosine/glycine KAPs (Rogers et al. 2001). KAPs can be divided into subfamilies based on amino acid composition and phylogenetic relationships (Wu et al. 2008). Humans have approximately 100 KAP genes (Wu et al. 2008). Compared to the conserved structure and modality of keratins within mammals, KAP genes differ significantly between species and are likely to explain the variety of characteristics seen in hard keratin appendages such as feathers, claws, scales and hair (Wu et al. 2008, Khan et al. 2014). KAPs are crucial for the assembly of keratin intermediate filaments into arrays and likely to affect attributes of hair such as strength, rigidity and chemical inertness (Parry & Steinert 1999, Koster et al. 2015).
R-HSA-6810357 (Reactome) During cornification a network of keratin intermediate filaments (KIF) and filaggrin (FLG) becomes crosslinked to the cornified envelope (CE). This facilitates the collapse and flattening of cells in the outermost stratum corneum to produce squames (Dale et al. 1978, Mack et al. 1993, Candi et al. 2005, Gruber et al. 2011).
R-HSA-6810843 (Reactome) Envoplakin (EVPL) is insoluble under physiological conditions but soluble as a heterodimer with periplakin (PPL) (Kalinin et al. 2004). The heterodimers provide a firm but flexible structures (Al-Jassar et al. 2013). EVPL and PPL deposition and crosslinking are amongst the earliest events of cornification (Kalinin et al. 2002, Candi et al. 2005). They partially colocalize with desmosomal proteins and keratin intermediate filaments (Ruhrberg et al. 1996, DiColandrea et al. 2000), linking the cornified envelope to desmosomes and keratin filaments (Ruhrberg et al. 1996, 1997). PPL also associates with cortical actin at the interdesmosomal plasma membrane (DiColandrea et al. 2000, Groot et al. 2004).
R-HSA-6810894 (Reactome) The current model of cornified envelope (CE) formation suggests that crosslinking between envoplakin (EVPL), periplakin (PPL), involucrin (IVL) and small proline-rich proteins (SPRs) results in the formation of a layer along the entire inner surface of the plasma membrane, including desmosomes, forming a scaffold to which other precursors are added to form the mature CE (Steinert & Marekov 1999, Kalinin et al. 2002, Candi et al. 2001).

Transglutaminases (TGs) are believed to mediate the intramolecular bonds involved in CE formation. They catalyze inter-protein bond formation by forming a thiolester acyl-enzyme intermediate and subsequently transferring the acyl residue to a primary amine (Folk & Finlayson 1977, Folk 1980). The amine acceptor is generally provided by the epsilon-amino group of a protein-bound lysine and the link formed is an N6-(gamma-glutamyl)lysine isopeptide bond.

CE assembly is thought to be initiated on the inner face of the plasma membrane between desmosomes by the cross-linking of involucrin to itself, to envoplakin and perhaps to periplakin (Steinert & Marekov 1999). The extent of homo- and heterologous cross-linking varies as the CE matures. In the immature CE, EVPL, IVL, SPR1, and SPR2 are largely cross-linked to themselves; EVPL-IVL and IVL-SPR crosslinks are common while cross-links between desmoplakin (DSP) and IVL or DSP and EVPL are not. Later there are many more cross-links between DSP and IVL, DSP and EVL, or IVL and type II keratins. Loricrin (LOR) cross-linking to other protein partners appears later.

Transglutaminase-1 (TGM1) can crosslink IVL (Simon & Green 1988, Nemes et al. 1999), LOR (Candi et al. 2001), SPR3 (Steinert et al. 1999) and is thought to be responsible for EVPL crosslinking to itself and to IVL (Steinert & Marekov 1999). TGM5 can catalyse homo-crosslinking in LOR, SPR1, SPR2, and IVL, and hetero-crosslinks between LOR-SPR3 (Candi et al. 2001).
R-HSA-6810899 (Reactome) Transglutaminase-1 (TGM1) and involucrin (IVL) are expressed shortly after envoplakin and periplakin. TGM1 associates with the plasma membrane via C14-16 fatty-acid adducts on its C-terminus (Steinert et al. 1996). IVL deposition precedes that of most other cornified envelope proteins (Nemes & Steinert 1999). It can bind the plasma membrane in a calcium and phosphatidyl-serine dependent manner, where it becomes a substrate for membrane-bound TGM1 and TGM5 (Nemes et al. 1999, Candi et al. 2001).
R-HSA-6810937 (Reactome) Lamellar bodies (LBs) ) are lipid-rich organelles produced by keratinocytes and secreted to form an impermeable water barrier (Feingold & Elias 2014). The lipids in LBs contain phospholipids, glucosylceramides, sphingomyelin and cholesterol (Feingold 2007). These lipids, some of which are keratinization specific, are synthesized and accumulate in the trans Golgi apparatus, budding off as LBs that accumulate in the granular layer (Wertz & van den Bergh 1998). ). LB lipids also organize into characteristic intercellular lamellae (Kalinin et al. 2002). LBs fuse with the plasma membrane (Schmitz & Muller 1991, Chattopadhyay et al. 2003) delivering lipids which become ester-linked to involucrin and probably other cornified envelope proteins by TG1 (Nemes et al. 1991) and possibly TG5 (Candi et al. 2005), forming a monomolecular layer termed the lipid envelope. Eventually these lipids replace the plasma membrane lipid bilayer, which is reabsorbed. Extracellularly, the LB lipids are further metabolized to have a unique composition and are 50% ceramides, 25% cholesterol, and 15% free fatty acids (Feingold 2007).
R-HSA-6811539 (Reactome) The inital scaffold of the cornified envelope (CE) is reinforced by the inclusion of loricrin (LOR) and small proline-rich proteins (SPRs), which together comprise about 75% of the total mass of the CE. Other proteins include filaggrin (FLG) (8%), elafin (6%), cystatin A (5%), involucrin (IVL) and keratin intermediate filaments (KIFs) (about 2% each) (Steinert & Marekov 1995). Other minor proteins include repetin (RPTN), trichohyalin (TCHH) and elafin (PI3) (Steinert & Marekov 1997, Steinert et al. 1998).

LOR is poorly soluble in vivo, while SPRs are very soluble. Both are preferred substrates of cytosolic transglutaminase-3 (TGM3) (Candi et al. 1999, Steinert et al. 1999, Tarcsa et al. 1999), which suggests that TGM3 may cross-link LOR and SPRs to create soluble complexes that are more easily translocated to the cell periphery (Kalinin et al. 2002). These cross-linked oligomers are good substrates for TGM1 (Candi et al. 1999, Steinert et al. 1999) which may link the LOR-SPR complexes to the CE scaffold. LOR can also be crosslinked by TGM5 (Candi et al. 2001). SPR content varies in epithelia from different body sites and increasing SPR content correlates with mechanical requirements of the tissue (Steinert et al. 1998). In humans LOR is initially deposited in the granular layer of the epidermis in keratohyalin granules, intermixed with profilaggrin (Yoneda & Steinert 1993). These are encoded in a linked 'Epidermal Differentiation Complex.' (Kypriotou et al. 2012, Niehues et al. 2016).

As the main component of the CE (Steinert & Marekov 1995), LOR is thought to function as the main reinforcement protein. LOR proteins are extensively crosslinked through isopeptide bonds but also crosslinked to SPRs, which may function as bridging proteins between LOR molecules (Candi et al. 2005). LOR can also form crosslinks with keratin and filaggrin (Steinert & Marekov 1995). CE crosslinking involves TGM1, TGM3 and TGM5 (Lorand & Graham 2003). The type-II keratin chains (K1, K2e and K5) are crosslinked at a specific Lys residue that is located in a conserved region of the V1 subdomain of the head domain (Steinert & Marekov 1995). IVL can be crosslinked by TGM1, which preferentially crosslinks Gln495 and Gln496 (Simon & Green 1998). In vitro, LOR is a substrate for TGM1-3 and 5 (Candi et al. 1995). In the epidermis, TGM1, TGM5 and TGM3 are believed to crosslink LOR sequentially; an initial attachment by TGM1 and 5 forms interchain crosslinks followed by a compaction process that involves TGM3 (Candi et al. 2005). SPRs are also TGM substrates, particularly TGM3 (Candi et al. 1999, Tarcsa et al. 1998, Steinert et al. 1999).

FLG binds KIFs, aggregating them into tight bundles. As a component of the CE, FLG 'glues' KIFs to the CE and coordinates the structure of cornifying cells (Steinert & Marekov 1995, Candi et al. 2005).
R-HSA-6814187 (Reactome) Envoplakin:periplakin heterodimers (EVPL:PPL) bind the plasma membrane. In vitro, EVPL:PPL can bind lipid vesicles in response to increasing Ca2+, suggesting that translocation and binding to the plasma membrane is regulated by elevation of intracellular Ca2+ (Kalinin et al. 2004).
R-HSA-6814298 (Reactome) Late envelope proteins or late cornified envelope proteins (LCEs) are a family of 18 proteins that are expressed after assembly of the cornified envelope (CE) is advanced (Marshall et al. 2000, Kypriotou et al. 2012). They are incorporated into the CE late in the process of envelope maturation during epidermal differentiation. They are probable substrates for epidermal transglutaminases and proposed to link CE proteins and mediate differences in barrier quality, perhaps through interaction with cytoplasmic components of the cornified cell (Marshall et al. 2001).

Human LCEs fall into distinct structural groups, encoded by genes which form clusters on the genome at 1q21 (Marshall et al. 2001, Niehues et al. 2016). Group 1 are expressed predominantly in epidermis. Group 4 (LEP 13-17) have highest expression in internal epithelia (Wang et al. 2001, Marshall et al. 2001).
R-HSA-6814374 (Reactome) Kazrin (KAZN) is an evolutionarily-conserved cytoplasmic and nuclear protein that was identified as a binding partner of periplakin (PPL), a component of epidermal desmosomes (DS) and the cornified envelope (CE) (Groot et al. 2004).

Kazrin has at least 5 different isoforms. Overexpression of the short isoform kazrinE stimulates the terminal differentiation of cultured human keratinocytes and is associated with a reduction in F-actin content, disruption of DS assembly, and changes in cell shape. Overexpression of activated RhoA rescues the effects on cell shape and adhesion. Conversely, knockdown of the longest isoform kazrinA impairs terminal differentiation, independently of RhoA activity (Sevilla et al. 2008a). KazrinE colocalizes with stabilized microtubules in differentiating keratinocytes (Nachat et al. 2009). All KAZN isoforms can form complexes with one another (Nachat et al. 2009), suggesting that like periplakin and envoplakin, it may form part of the cortical scaffold that integrates the actin cytoskeleton with DS (Ruhrberg et al. 1997, Kalinin et al. 2001, Groot et al. 2004). In Xenopus embryos, depletion of endogenous KAZN results in striking defects in axial elongation, muscle and notochord differentiation, and epidermal morphogenesis. These effects are believed to be due to disruption of cell-cell junctions (Sevilla et al. 2008b, Cho et al. 2010). However, mice with a knockout that removes exons 5-15 of KAZN had normal epidermal morphogenesis and homeostasis (Chhatriwala et al. 2012).
R-HSA-6814387 (Reactome) In fully cornified cells, filaggrin is degraded into free amino acids. This high concentration of hydrophillic amino acids is essential for water retention and contributes to the osmolarity, and consequently the flexibility of the cornified layer (Candi et al. 2005). Filaggrin monomers are a direct target for cleavage by the aspartate-specific protease caspase 14 (Denecker et al. 2007, 2008, Hoste et al. 2011, Eckhart & Tschachler 2011). Proteases able to process profilaggrin into fillagrin in vitro include microbial ST14 (Profillagrin endopeptidase 1, PEP1), CAPN1 (mu-calpain), furin, PACE4 and matriptase MT-SP1 (Reising et al. 1995, Yamazaki et al. 1997, Pearton et al. 2001, List et al. 2003, Candi et al. 2005), but these proteases do not appear to have a role in the degradation of filaggrin that occurs at a late stage in keratinization.
R-HSA-6814695 (Reactome) PERP (p53 effector related to PMP-22) is a p53/p63 target gene involved in DNA damage-induced apoptosis (Flores et al. 2002). It is a tetraspan membrane protein,distantly related to members of the claudin/PMP-22/EMP family of four-pass membrane proteins (Attardi et al. 2000). It has an epithelial-specific expression pattern during embryogenesis and localizes to desmosomes. Perp -/- knockout mice exhibit numerous desmosomal structural defects, suggesting a role for Perp in promoting the stable assembly of desmosomal adhesive complexes (Ihrie et al. 2005).
R-HSA-6814734 (Reactome) Corneodesmosomes (CDS) are an ultrastructurally modified form of desmosomes (DS) (Chapman & Walsh 1990). When DS are transformed into CDS between the stratum granulosum and the stratum corneum, the desmoglea loses its trilamellar structure and becomes homogeneously electron dense. On the cytoplasmic side, the attachment plaque (desmosomal plaque) becomes incorporated into the cornified cell envelope (CE). Keratin filaments are connected to the attachment plaque in DS; this association is no longer visible in CDS.

Like DS, desmoglein and desmocollin constitute the extracellular parts of CDS (Simon et al. 1997), but there is an additional unique extracellular component known as corneodesmosin (CDSN). CDSN is a 52- to 56-kDa glycoprotein produced by keratinocytes that is incorporated into the desmoglea of DS shortly before their transformation into CDS during cornification (Serre et al. 1991). It is stored and secreted by Lamellar bodies. After secretion CDSN localizes to the extracellular structures of CDS and covalently cross-links to the CE. This step coincides with the morphological transformation of DS into CDS. In vitro studies suggest that CDSN mediates homophilic binding to counterparts on adjacent corneocytes (Ishida-Yamamoto & Kishibe 2011). Cleavage of desmoglein, desmocollin and CDSN is a key step in desquamation.
R-HSA-6814764 (Reactome) In differentiating keratinocytes, fusion of lamellar body (LB) membranes with the plasma membrane enriches the plasma membrane with lipids including omega-OH-ceramides. Their fatty acid chains are long enough to span the lipid bilayer, so that the omega-OH projects into the cell. In vitro data have shown that the membrane-anchored transglutaminase 1 enzyme can covalently esterify these ceramides onto glutamine residues of cornified envelope scaffold proteins (Nemes et al. 1999). Eventually, the ceramides replace the bilayer plasma membrane and are thought to serve to interdigitate with and organize the extracellular lipids into characteristic lamellae (Kalinin et al. 2001).
R-HSA-8849638 (Reactome) At low pH, the complex of the D8D9 fragment of SPINK5 (Serine protease inhibitor Kazal-type 5, also known as LEKTI, Lympho-epithelial Kazal-type-related inhibitor), consisting of residues 490 - 624 of the full-length protein, and KLK5 (Kallikrein-5) dissociates, releasing active KLK5 protease. In normal skin, this event occurs extracellularly in upper layers of the skin (Deraison et al. 2007).
R-HSA-8849646 (Reactome) The D8D9 fragment of SPINK5 (Serine protease inhibitor Kazal-type 5, also known as LEKTI, Lympho-epithelial Kazal-type-related inhibitor), consisting of residues 490 - 624 of the full-length protein, binds to KLK5 (Kallikrein-5), inactivating the latter. At neutral pH, complex formation is effectively irreversible. In normal skin, this event occurs extracellularly in the stratum corneum of the skin. As the complex is carried into layers nearer the surface of the skin, falling pH triggers its dissociation and release of active KLK5. Mutations that inactivate SPINK5 are associated with a severe skin disorder, Netherton syndrome (NS, MIM 256500), whose symptoms include premature desquamation (Deraison et al, 2007; Fortugno et al. 2011). Consistent with the hypothesis that SPINK5-mediated inhibition of KLK5 activity is a key feature of regulating normal desquamation, the NS-like phenotype of mice whose SPINK5-homologous gene has been knocked out is reversed in mice missing both SPINK5 and KLK5 activitiies (Furio et al. 2015).
R-HSA-8849797 (Reactome) Filaggrin is initially synthesized as a large, insoluble, highly phosphorylated precursor containing many tandem copies of 324 residues. This precursor is dephosphorylated and proteolytically cleaved by several proteases, including the undefined protease PEP1 (Resing et al. 1996), mu-calpain (Yamazaki et al. 1997), furin, PCSK6 (PACE4) (Pearton et al. 2001), PRSS8 (cap1) (Leyvraz et al. 2005), ST14 (matriptase) (List et al. 2003), CELA2 (Bonnart et al. 2010), CASP14 (Denecker et al. 2007) and Kallikrein-related peptidase 5 (KLK5) (Sakabe et al. 2013). Filaggrin is further processed and proteolytically degraded by CASP14 (Eckhart & Tschachler 2011).
R-HSA-8849826 (Reactome) ST14 (Suppressor of tumorigenicity 14, also known as matriptase) associated with the plasma membrane catalyzes the hydrolytic cleavage of proKLK5 (pro-Kallekrein-5) to yield active KLK5 enzyme. The activity of human ST14 enzyme is inferred from that of its well-characterized mouse homolog (Sales et al. 2010). Consistent with this inference, deficiencies of the human enzyme are associated with an ichthyosis syndrome (MIM 602400) as is a knockout mutation of mouse St14 (Alef et al. 2009).
R-HSA-8849857 (Reactome) In the low-pH environment of the upper layers of the stratum corneum, KLK5 (Kallikrein 5) dissociates from its complex with SPINK5 (Serine protease inhibitor kazal-type 5) (Deraison et al. 2007) and is free to cleave proCELA2 (Elastase 2), activating it (Bonnart et al. 2010).
R-HSA-8850777 (Reactome) Extracellular SPINK6 (Serine protease inhibitor Kazal-type 6) binds KLK14 (kallekrein-related peptidase 14), inactivating the latter. KLK14 activity contributes to the process of desquamation, and SPINK6 binding may play a role in the regulation of that process (Meyer-Hoffert et al. 2010).
R-HSA-8850786 (Reactome) Extracellular SPINK6 (Serine protease inhibitor Kazal-type 6) binds KLK12 (kallekrein-related peptidase 12), inactivating the latter (Kantyka et al. 2011).
R-HSA-8850794 (Reactome) Extracellular SPINK6 (Serine protease inhibitor Kazal-type 6) binds KLK5 (kallekrein-related peptidase 5), inactivating the latter. KLK5 activity contributes to the process of desquamation, and SPINK6 binding may play a role in the regulation of that process (Meyer-Hoffert et al. 2010).
R-HSA-8850797 (Reactome) Extracellular SPINK6 (Serine protease inhibitor Kazal-type 6) binds KLK13 (kallekrein-related peptidase 13), inactivating the latter (Kantyka et al. 2011).
R-HSA-8850818 (Reactome) Extracellular SPINK9 (Serine protease inhibitor Kazal-type 6) binds KLK5 (kallekrein-related peptidase 5), inactivating the latter. KLK5 activity contributes to the process of desquamation, and SPINK9 binding may play a role in the regulation of that process (Brattsand et al. 2009; Meyer-Hoffert et al. 2009).
R-HSA-8850831 (Reactome) In vitro, KLK5 (Kallikrein 5) catalyzes the slow cleavage of a four-residue aminoterminal propeptide from proKLK8 (pro-Kallekrein 8), to generate active KLK8. The abundance of KLK8 in the stratum corneum and its serine endopeptidase activity are consistent with a role for KLK8 in formation of the stratum corneum, desquamation, or both. Physiological substrates for KLK8 remains to be identified, however, as do possible additional activators of it (Eissa et al. 2011). A possible pathogenic role for KLK8 is suggested by the recent demonstration that it can mediate the extracellular cleavage of the L1 capsid protein of human papilloma viruses, facilitating their infection of human host cells (Cerqueira et al. 2015).
R-HSA-8934819 (Reactome) Filaggrin is initially synthesized as a large, insoluble, highly phosphorylated precursor containing many tandem copies of 324 residues. This precursor is dephosphorylated and proteolytically cleaved by several proteases, including the undefined protease PEP1 (Resing et al. 1996), mu-calpain (Yamazaki et al. 1997), furin, PCSK6 (PACE4) (Pearton et al. 2001), PRSS8 (cap1) (Leyvraz et al. 2005), ST14 (matriptase) (List et al. 2003), CELA2 (Bonnart et al. 2010), CASP14 (Denecker et al. 2007) and Kallikrein-related peptidase 5 (KLK5) (Sakabe et al. 2013). Filaggrin is further processed and proteolytically degraded by CASP14 (Eckhart & Tschachler 2011).
R-HSA-8942224 (Reactome) During cornification, a network of keratin intermediate filaments (KIF) and filaggrin (FLG) becomes crosslinked to the cornified envelope (CE). The FLG-KIF linkage occurs primarily through a specific lysine residue on the head domain of type II keratin chains, which can crosslink with several CE proteins including loricrin, SPRs, envoplakin and involucrin (Dale et al. 1978, Manabe et al. 1991, Mack et al. 1993, Steinert et al. 1995, Candi et al. 1998). This FLG-KIF crosslinking is believed to organise intermediate filaments into bundles, which stabilize the keratin network (Steinert et al. 1981, Candi et al. 2005) and facilitate the collapse and flattening of cells in the outermost stratum corneum to produce squames. Cell flattening can occur in the absence of FLG, but at the ultrastructural level loss-of-function mutations in FLG are associated with disorganized keratin filaments, impaired lamellar body loading and abnormal architecture of the lamellar bilayer (Gruber et al. 2011).
RCOOHArrowR-HSA-6789310 (Reactome)
SPINK5(490-624)ArrowR-HSA-8849638 (Reactome)
SPINK5(490-624)R-HSA-8849646 (Reactome)
SPINK6R-HSA-8850777 (Reactome)
SPINK6R-HSA-8850786 (Reactome)
SPINK6R-HSA-8850794 (Reactome)
SPINK6R-HSA-8850797 (Reactome)
SPINK9R-HSA-8850818 (Reactome)
SPRsR-HSA-6811539 (Reactome)
ST14mim-catalysisR-HSA-8849826 (Reactome)
TAGsR-HSA-6789310 (Reactome)
TGM1:Ca2+, TGM5:Ca2+mim-catalysisR-HSA-6810894 (Reactome)
TGM1R-HSA-6810899 (Reactome)
keratinocyte LIPsmim-catalysisR-HSA-6789310 (Reactome)
proCELA2AR-HSA-8849857 (Reactome)
proKLK5R-HSA-8849826 (Reactome)
proKLK8R-HSA-8850831 (Reactome)
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