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HEMOSTASIS, THROMBOSIS, AND VASCULAR BIOLOGY
From the Blood Research Institute, The Blood
Center of Southeastern Wisconsin, and the Departments of Microbiology
and Molecular Genetics, Pharmacology, and Cellular Biology, Medical
College of Wisconsin, Milwaukee, WI.
Platelet responses to collagen are mediated by the combined
actions of the integrin Platelet endothelial cell adhesion molecule-1
(PECAM-1, CD31) is a 130-kd member of the immunoglobulin (Ig)
superfamily that is expressed on the surface of circulating platelets,
endothelial cells, neutrophils, monocytes, and certain T-lymphocyte
subsets. The extracellular domain of PECAM-1 is composed of 6 extracellular Ig-like homology units,1 the amino-terminal
2 of which mediates PECAM-1-PECAM-1 homophilic
interactions.2,3 Antibodies to the extracellular domain
have been shown to have profound physiologic and cell biologic effects,
including delaying leukocyte transendothelial migration4-6
and inhibiting angiogenesis.7 The extracellular domain of
PECAM-1 also serves as a portal for entry into endothelial cells of
certain strains of Plasmodium falciparum-infected
erythrocytes.8,9
The PECAM-1 cytoplasmic domain also plays a key biologic role because a
large number of extracellular stimuli (reviewed in Newman10) have been shown to result in the phosphorylation
of 2 key tyrosine residues, located at positions 663 and 686 of the cytoplasmic domain.11 The sequence surrounding each of
these 2 tyrosine residues conforms to an immunoreceptor tyrosine-based inhibitory motif (ITIM) that, when phosphorylated, provides a major
docking site for the src homology 2 (SH2) domain-containing protein
tyrosine phosphatase (PTP), SHP-2.11-14 Based on the
presence of its highly conserved ITIM and the similarity in its genomic organization to that of other ITIM-bearing transmembrane receptors, we
have recently proposed10 that PECAM-1 is a member of a
growing family of transmembrane PTP-binding proteins collectively known as inhibitory receptors.
There are good examples at the cell biological level that
support a role for inhibitory receptors in attenuating the action of
agonist receptors that contain one or more immunoreceptor
tyrosine-based activation motifs (ITAMs).15,16
Human platelets express 2 such ITAM-bearing
receptors Materials
Preparation of mouse platelets
Adhesion assays Immulon-2 microtiter 96-well plates were coated with varying concentrations of fibrillar collagen without Mg2+ or with a constant concentration of poly L-lysine (0.01%) overnight at 4°C. Washed wild-type and PECAM-1 / platelets, prepared as
described above, were loaded with calcine AM (5 µmol/L)
for 30 minutes at 37°C. The loaded wild-type and PECAM-1/ platelets were rewashed in modified
Tyrode-HEPES buffer and suspended at a concentration of
1.2 × 108 platelets/mL. Calcine AM-loaded
platelets (100 µL) were added to the matrix-coated wells and
incubated for the indicated amount of time at 37°C. Nonadherent
platelets were removed by washing, and the extent of platelet adherence
was determined by measuring the fluorescence emitted by adhered
platelets at 520 nm after excitation at 490 nm. The assay was performed
in triplicate, and each data point represented the mean ± SD of
triplicate measurements.
Platelet aggregation and secretion Platelets were suspended in 200 µL at a final concentration of 2.5 × 108 platelets/mL, and aggregometry was performed at 37°C in a Bio/Data PAP-4 channel aggregometer (Horsham, PA) with continuous stirring (1000 rpm). ATP release was determined by removing 10-µL aliquots at selected time points, centrifuging them at 500g for 1 minute at room temperature in the presence of 1 mM EDTA to prevent further platelet activation, and adding the supernatant to a 100-µL reaction mixture containing luciferase (0.5 mM) and luciferin (1.25 µg/mL). The luminescence generated in the presence of platelet-released ATP was read in a luminometer (TD-20e; Turner, Sunnyvale, CA) and compared to an ATP standard curve to determine the amount of ATP released.
Platelets derived from PECAM-1-deficient mice exhibit exaggerated GPVI-mediated adhesion and aggregation responses Platelet activation by collagen is thought to proceed by a 2-step mechanism involving the initial attachment of collagen fibrils to surface-expressed integrin 2 1,
followed by an obligatory signal transduction cascade mediated, at
least in part, by the GPVI/FcR -chain complex.19 The
latter operates through tyrosine-phosphorylated ITAMs within the
cytoplasmic domain of the FcR-chain dimer.23 Despite
much progress in identifying components of the signaling pathway
responsible for initiating and sustaining collagen-induced platelet
activation,24-30 virtually nothing is known about
the regulatory elements that modulate this important hemostatic event. Others and we have recently found that PECAM-1 becomes strongly tyrosine phosphorylated on its ITIM after exposure of platelets to
collagen,31,32 leading us to speculate that agonist
induction simultaneously activates a feedback inhibitory pathway
mediated by PECAM-1.
To test the hypothesis that PECAM-1 normally functions to attenuate
GPVI-mediated platelet activation, we first compared the ability of
platelets derived from wild-type versus PECAM-1-deficient mice to bind
to immobilized fibrillar collagen in the absence of
Mg2+
There is growing support for the notion that ITAM- and ITIM-bearing receptors act antagonistically when expressed in the same cell, possibly because of the potential for ITIM-associated PTPs to dephosphorylate ITAM-bearing receptors or their tyrosine-phosphorylated substrates.16,34 To determine whether the observed exaggerated platelet adhesion to immobilized collagen was specific for ITAM-bearing agonist receptors, we compared platelet aggregation responses to GPVI-specific agonists22 with those obtained using thrombin, which acts through a heterotrimeric G-protein-coupled receptor.35 Relative to wild-type platelets, PECAM-1-deficient platelets
exhibited strikingly hyper-aggregation responses to subthreshold doses
of fibrillar collagen (Figure 2A) or CRP
(Figure 2C), though the aggregation responses were equivalent at higher
concentrations of either agonist (Figure 2B,D). In contrast, platelet
activation by either low-dose (Figure 2E) or high-dose (Figure 2F)
thrombin was identical in wild-type and PECAM-1
Effect of PECAM-1 deficiency on dense granule secretion We have recently shown that co-ligation of PECAM-1 with the ITAM-bearing T-cell receptor on the surface of Jurkat T cells attenuates calcium mobilization from intracellular stores.20 The physiological consequences of this inhibition, however, have not been examined. Because platelet alpha and dense granule secretion also require the elevation of cytosolic calcium and because the GPVI-FcR-chain-mediated signaling acts through
phospholipase C2 (PLC2) to mobilize intracellular calcium ion
stores,36 we hypothesized that, like adhesion and
aggregation, the platelet release reaction should also be accentuated
in PECAM-1-deficient platelets stimulated with GPVI-specific agonists.
To determine whether PECAM-1 deficiency has an effect on granule
release, we compared the ability of wild-type and
PECAM-1
After injury to the vascular endothelium, platelets adhere to and
become activated by collagen fibers in the exposed subendothelium. Among the numerous platelet receptors for collagen that have been reported, the integrin GPVI is associated within the plane of the plasma membrane with the
Fc-receptor We could not, a priori, have predicted whether PECAM-1 deficiency would have a stimulatory or an inhibitory effect on collagen-induced, GPVI-mediated signal transduction. This is because the ability of an immunoglobulin-ITIM-bearing membrane receptor to have a positive rather than a negative regulatory effect is influenced by a number of factors, including the target specificity of the phosphatase recruited and the identity of the phosphatase substrates that are proximal to the receptor-PTP complex. The situation with PECAM-1 is complicated by the observations that, although the PECAM-1 ITIM clearly provides a docking site for the cytoplasmic PTP SHP-2,11-14,49-51 tyrosine-phosphorylated PECAM-1 has also been reported to associate with SHP-113,49-51 and with the 5'-inositol phosphatase SHIP.51 The situation is further complicated by the observations that, depending on whether the pathway is regulated, SHP-1 and SHP-2 appear to be capable of conveying either positive or negative regulatory signals.20,52-59 Because the identity of the phosphatase recruited by PECAM-1 in response to GPVI signaling, the target substrates for SHP-1 and SHP-2 in general, and the subcellular location of these substrates relative to that of PECAM-1 are completely unknown, there was no way to predict the physiological consequences of PECAM-1 deficiency. Interestingly, Pasquet et al60 have recently found that SHP-1 becomes tyrosine phosphorylated after platelet activation by GPVI and associates with other tyrosine-phosphorylated proteins of 28, 32, 50, 70, and 130 kd, and they suggested that SHP-1 plays a functional role in platelet responses to collagen. The 130-kd co-precipitating band was not, however, identified as PECAM-1. The identity of the receptor(s) that recruit and activate SHP-1 under these conditions remains to be determined. The observation that PECAM-1 Our finding that platelets from PECAM-1 Despite the rapid formation of the PECAM-1/SHP-2 signaling complex
during platelet aggregation,12 virtually nothing is known about the physiologic consequences of this association. One potential mechanism by which a PECAM-1/PTP signaling complex might interfere with
GPVI-dependent platelet activation may involve dephosphorylation of
PTKs and PTK substrates that become recruited to the nearby ITAM-bearing GPVI-FcR
We thank Drs Gordon S. Duncan and Tak W. Mak (Amgen Institute, Toronto, ON, Canada) for providing PECAM-1-deficient mice.
Submitted September 14, 2000; accepted November 16, 2000.
Supported by National Institutes of Health grant P01 HL44612 (D.K.N., P.J.N.). S.P. is a recipient of a Northwestern Mutual Life Fellowship in Biomedicine awarded to the Medical College of Wisconsin.
The publication costs of this article were defrayed in part by page charge payment. Therefore, and solely to indicate this fact, this article is hereby marked "advertisement" in accordance with 18 U.S.C. section 1734.
Reprints: Peter J. Newman, Blood Research Institute, The Blood Center of Southeastern Wisconsin, 638 N. 18th St, PO Box 2178, Milwaukee, WI 53233; e-mail: pjnewman{at}bcsew.edu.
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P. J. Newman New role for the GPVI/FcR{gamma} chain complex Blood, February 15, 2006; 107(4): 1248 - 1249. [Full Text] [PDF]
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S. Falati, S. Patil, P. L. Gross, M. Stapleton, G. Merrill-Skoloff, N. E. Barrett, K. L. Pixton, H. Weiler, B. Cooley, D. K. Newman, et al. Platelet PECAM-1 inhibits thrombus formation in vivo Blood, January 15, 2006; 107(2): 535 - 541. [Abstract] [Full Text] [PDF]
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J. L. Wee and D. E. Jackson The Ig-ITIM superfamily member PECAM-1 regulates the "outside-in" signaling properties of integrin {alpha}IIb{beta}3 in platelets Blood, December 1, 2005; 106(12): 3816 - 3823. [Abstract] [Full Text] [PDF]
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S. J.A. Korporaal, G. Gorter, H. J.M. van Rijn, and J.-W. N. Akkerman Effect of Oxidation on the Platelet-Activating Properties of Low-Density Lipoprotein Arterioscler Thromb Vasc Biol, April 1, 2005; 25(4): 867 - 872. [Abstract] [Full Text] [PDF]
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 M. Maas, M. Stapleton, C. Bergom, D. L. Mattson, D. K. Newman, and P. J. Newman Endothelial cell PECAM-1 confers protection against endotoxic shock Am J Physiol Heart Circ Physiol, January 1, 2005; 288(1): H159 - H164. [Abstract] [Full Text] [PDF]
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 C. D. O'Brien, G. Cao, A. Makrigiannakis, and H. M. DeLisser Role of immunoreceptor tyrosine-based inhibitory motifs of PECAM-1 in PECAM-1-dependent cell migration Am J Physiol Cell Physiol, October 1, 2004; 287(4): C1103 - C1113. [Abstract] [Full Text] [PDF]
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S. J. Shattil and P. J. Newman Integrins: dynamic scaffolds for adhesion and signaling in platelets Blood, September 15, 2004; 104(6): 1606 - 1615. [Abstract] [Full Text] [PDF]
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 S. M. Albelda, K. C. Lau, P. Chien, Z.-Y. Huang, E. Arguiris, A. Bohen, J. Sun, J. A. Billet, M. Christofidou-Solomidou, Z. K. Indik, et al. Role for Platelet-Endothelial Cell Adhesion Molecule-1 in Macrophage Fc{gamma} Receptor Function Am. J. Respir. Cell Mol. Biol., August 1, 2004; 31(2): 246 - 255. [Abstract] [Full Text] [PDF]
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J. M. Gibbins Platelet adhesion signalling and the regulation of thrombus formation J. Cell Sci., July 15, 2004; 117(16): 3415 - 3425. [Abstract] [Full Text] [PDF]
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J. A. Lopez A tale of 2 (or more) tails: PECAM-1 regulation of GPIb-IX-V signaling Blood, November 15, 2003; 102(10): 3463 - 3464. [Full Text] [PDF]
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L. M. Thai, L. K. Ashman, S. N. Harbour, P. M. Hogarth, and D. E. Jackson Physical proximity and functional interplay of PECAM-1 with the Fc receptor Fc{gamma}RIIa on the platelet plasma membrane Blood, November 15, 2003; 102(10): 3637 - 3645. [Abstract] [Full Text] [PDF]
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V. Rathore, M. A. Stapleton, C. A. Hillery, R. R. Montgomery, T. C. Nichols, E. P. Merricks, D. K. Newman, and P. J. Newman PECAM-1 negatively regulates GPIb/V/IX signaling in murine platelets Blood, November 15, 2003; 102(10): 3658 - 3664. [Abstract] [Full Text] [PDF]
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I. A. M. Relou, G. Gorter, I. A. Ferreira, H. J. M. van Rijn, and J.-W. N. Akkerman Platelet Endothelial Cell Adhesion Molecule-1 (PECAM-1) Inhibits Low Density Lipoprotein-induced Signaling in Platelets J. Biol. Chem., August 29, 2003; 278(35): 32638 - 32644. [Abstract] [Full Text] [PDF]
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C. Gao, W. Sun, M. Christofidou-Solomidou, M. Sawada, D. K. Newman, C. Bergom, S. M. Albelda, S. Matsuyama, and P. J. Newman PECAM-1 functions as a specific and potent inhibitor of mitochondrial-dependent apoptosis Blood, July 1, 2003; 102(1): 169 - 179. [Abstract] [Full Text] [PDF]
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P. J. Newman and D. K. Newman Signal Transduction Pathways Mediated by PECAM-1: New Roles for an Old Molecule in Platelet and Vascular Cell Biology Arterioscler Thromb Vasc Biol, June 1, 2003; 23(6): 953 - 964. [Abstract] [Full Text] [PDF]
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T. R. Kyriakides, P. Rojnuckarin, M. A. Reidy, K. D. Hankenson, T. Papayannopoulou, K. Kaushansky, and P. Bornstein Megakaryocytes require thrombospondin-2 for normal platelet formation and function Blood, May 15, 2003; 101(10): 3915 - 3923. [Abstract] [Full Text] [PDF]
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 K. Eto, R. Murphy, S. W. Kerrigan, A. Bertoni, H. Stuhlmann, T. Nakano, A. D. Leavitt, and S. J. Shattil Megakaryocytes derived from embryonic stem cells implicate CalDAG-GEFI in integrin signaling PNAS, October 1, 2002; 99(20): 12819 - 12824. [Abstract] [Full Text] [PDF]
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R. Wiewrodt, A. P. Thomas, L. Cipelletti, M. Christofidou-Solomidou, D. A. Weitz, S. I. Feinstein, D. Schaffer, S. M. Albelda, M. Koval, and V. R. Muzykantov Size-dependent intracellular immunotargeting of therapeutic cargoes into endothelial cells Blood, February 1, 2002; 99(3): 912 - 922. [Abstract] [Full Text] [PDF]
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M. Cicmil, J. M. Thomas, M. Leduc, C. Bon, and J. M. Gibbins Platelet endothelial cell adhesion molecule-1 signaling inhibits the activation of human platelets Blood, January 1, 2002; 99(1): 137 - 144. [Abstract] [Full Text] [PDF]
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K. L. Jones, S. C. Hughan, S. M. Dopheide, R. W. Farndale, S. P. Jackson, and D. E. Jackson Platelet endothelial cell adhesion molecule-1 is a negative regulator of platelet-collagen interactions Blood, September 1, 2001; 98(5): 1456 - 1463. [Abstract] [Full Text] [PDF]
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G. Cao, C. D. O'Brien, Z. Zhou, S. M. Sanders, J. N. Greenbaum, A. Makrigiannakis, and H. M. DeLisser Involvement of human PECAM-1 in angiogenesis and in vitro endothelial cell migration Am J Physiol Cell Physiol, May 1, 2002; 282(5): C1181 - C1190. [Abstract] [Full Text] [PDF]
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Top
Abstract
Introduction
Fc
