Platelet Membrane Receptor Proteolysis: Implications for Platelet Function

J.Y. Wu; J.W.M. Heemskerk; C.C.F.M.J. Baaten

doi:10.3389/fcvm.2020.608391

Platelet Membrane Receptor Proteolysis: Implications for Platelet Function

J.Y. Wu, J.W.M. Heemskerk^*, C.C.F.M.J. Baaten

^*Corresponding author for this work

Research output: Contribution to journal › (Systematic) Review article › peer-review

Abstract

The activities of adhesion and signaling receptors in platelets are controlled by several mechanisms. An important way of regulation is provided by proteolytic cleavage of several of these receptors, leading to either a gain or a loss of platelet function. The proteases involved are of different origins and types: (i) present as precursor in plasma, (ii) secreted into the plasma by activated platelets or other blood cells, or (iii) intracellularly activated and cleaving cytosolic receptor domains. We provide a comprehensive overview of the proteases acting on the platelet membrane. We describe how these are activated, which are their target proteins, and how their proteolytic activity modulates platelet functions. The review focuses on coagulation-related proteases, plasmin, matrix metalloproteinases, ADAM(TS) isoforms, cathepsins, caspases, and calpains. We also describe how the proteolytic activities are determined by different platelet populations in a thrombus and conversely how proteolysis contributes to the formation of such populations.

Original language	English
Article number	608391
Number of pages	13
Journal	Frontiers in Cardiovascular Medicine
Volume	7
DOIs	https://doi.org/10.3389/fcvm.2020.608391
Publication status	Published - 8 Jan 2021

Keywords

adam
calpain
calpain cleavage
caspase
coagulation factors
factor-va
glycoprotein ib-ix
hemostatic function
in-vitro
integrin alpha(iib)beta(3)
matrix metalloproteinases
mmp
platelets
procoagulant activity
protease-activated receptor-1
receptor proteolysis
thrombin
INTEGRIN ALPHA(IIB)BETA(3)
HEMOSTATIC FUNCTION
ADAM
IN-VITRO
FACTOR-VA
CALPAIN CLEAVAGE
PROTEASE-ACTIVATED RECEPTOR-1
PROCOAGULANT ACTIVITY
THROMBIN
GLYCOPROTEIN IB-IX
MMP
MATRIX METALLOPROTEINASES

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10.3389/fcvm.2020.608391Licence: CC BY

Cite this

@article{cfcef696a98644cf83b6be1b953b40aa,

title = "Platelet Membrane Receptor Proteolysis: Implications for Platelet Function",

abstract = "The activities of adhesion and signaling receptors in platelets are controlled by several mechanisms. An important way of regulation is provided by proteolytic cleavage of several of these receptors, leading to either a gain or a loss of platelet function. The proteases involved are of different origins and types: (i) present as precursor in plasma, (ii) secreted into the plasma by activated platelets or other blood cells, or (iii) intracellularly activated and cleaving cytosolic receptor domains. We provide a comprehensive overview of the proteases acting on the platelet membrane. We describe how these are activated, which are their target proteins, and how their proteolytic activity modulates platelet functions. The review focuses on coagulation-related proteases, plasmin, matrix metalloproteinases, ADAM(TS) isoforms, cathepsins, caspases, and calpains. We also describe how the proteolytic activities are determined by different platelet populations in a thrombus and conversely how proteolysis contributes to the formation of such populations.",

keywords = "adam, calpain, calpain cleavage, caspase, coagulation factors, factor-va, glycoprotein ib-ix, hemostatic function, in-vitro, integrin alpha(iib)beta(3), matrix metalloproteinases, mmp, platelets, procoagulant activity, protease-activated receptor-1, receptor proteolysis, thrombin, INTEGRIN ALPHA(IIB)BETA(3), HEMOSTATIC FUNCTION, ADAM, IN-VITRO, FACTOR-VA, CALPAIN CLEAVAGE, PROTEASE-ACTIVATED RECEPTOR-1, PROCOAGULANT ACTIVITY, THROMBIN, GLYCOPROTEIN IB-IX, MMP, MATRIX METALLOPROTEINASES",

author = "J.Y. Wu and J.W.M. Heemskerk and C.C.F.M.J. Baaten",

note = "Funding Information: Funding. JW was supported by the China Scholarship Council (Grant No. 201908440512). CB was supported by the Alexander von Humboldt Foundation. Publisher Copyright: Copyright {\textcopyright} 2021 Wu, Heemskerk and Baaten.",

year = "2021",

month = jan,

day = "8",

doi = "10.3389/fcvm.2020.608391",

language = "English",

volume = "7",

journal = "Frontiers in Cardiovascular Medicine",

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T1 - Platelet Membrane Receptor Proteolysis: Implications for Platelet Function

AU - Wu, J.Y.

AU - Heemskerk, J.W.M.

AU - Baaten, C.C.F.M.J.

N1 - Funding Information: Funding. JW was supported by the China Scholarship Council (Grant No. 201908440512). CB was supported by the Alexander von Humboldt Foundation. Publisher Copyright: Copyright © 2021 Wu, Heemskerk and Baaten.

PY - 2021/1/8

Y1 - 2021/1/8

N2 - The activities of adhesion and signaling receptors in platelets are controlled by several mechanisms. An important way of regulation is provided by proteolytic cleavage of several of these receptors, leading to either a gain or a loss of platelet function. The proteases involved are of different origins and types: (i) present as precursor in plasma, (ii) secreted into the plasma by activated platelets or other blood cells, or (iii) intracellularly activated and cleaving cytosolic receptor domains. We provide a comprehensive overview of the proteases acting on the platelet membrane. We describe how these are activated, which are their target proteins, and how their proteolytic activity modulates platelet functions. The review focuses on coagulation-related proteases, plasmin, matrix metalloproteinases, ADAM(TS) isoforms, cathepsins, caspases, and calpains. We also describe how the proteolytic activities are determined by different platelet populations in a thrombus and conversely how proteolysis contributes to the formation of such populations.

AB - The activities of adhesion and signaling receptors in platelets are controlled by several mechanisms. An important way of regulation is provided by proteolytic cleavage of several of these receptors, leading to either a gain or a loss of platelet function. The proteases involved are of different origins and types: (i) present as precursor in plasma, (ii) secreted into the plasma by activated platelets or other blood cells, or (iii) intracellularly activated and cleaving cytosolic receptor domains. We provide a comprehensive overview of the proteases acting on the platelet membrane. We describe how these are activated, which are their target proteins, and how their proteolytic activity modulates platelet functions. The review focuses on coagulation-related proteases, plasmin, matrix metalloproteinases, ADAM(TS) isoforms, cathepsins, caspases, and calpains. We also describe how the proteolytic activities are determined by different platelet populations in a thrombus and conversely how proteolysis contributes to the formation of such populations.

KW - adam

KW - calpain

KW - calpain cleavage

KW - caspase

KW - coagulation factors

KW - factor-va

KW - glycoprotein ib-ix

KW - hemostatic function

KW - in-vitro

KW - integrin alpha(iib)beta(3)

KW - matrix metalloproteinases

KW - mmp

KW - platelets

KW - procoagulant activity

KW - protease-activated receptor-1

KW - receptor proteolysis

KW - thrombin

KW - INTEGRIN ALPHA(IIB)BETA(3)

KW - HEMOSTATIC FUNCTION

KW - ADAM

KW - IN-VITRO

KW - FACTOR-VA

KW - CALPAIN CLEAVAGE

KW - PROTEASE-ACTIVATED RECEPTOR-1

KW - PROCOAGULANT ACTIVITY

KW - THROMBIN

KW - GLYCOPROTEIN IB-IX

KW - MMP

KW - MATRIX METALLOPROTEINASES

U2 - 10.3389/fcvm.2020.608391

DO - 10.3389/fcvm.2020.608391

M3 - (Systematic) Review article

C2 - 33490118

SN - 2297-055X

VL - 7

JO - Frontiers in Cardiovascular Medicine

JF - Frontiers in Cardiovascular Medicine

M1 - 608391

ER -