A CD99-related antigen on endothelial cells mediates neutrophil but not lymphocyte extravasation in vivo

Bixel, M. Gabriele; Petri, Bjӧrn; Khandoga, Alexander G.; Khandoga, Andrej; Wolburg‐Buchholz, Karen; Wolburg, Hartwig; März, Sigrid; Krombach, Fritz; Vestweber, Dietmar

doi:10.1182/blood-2006-08-043109

Cited by 93 publications

(110 citation statements)

References 37 publications

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“…57 Specifically, although both molecules mediate neutrophil transendothelial cell migration in vitro and in vivo, CD99L2, in contrast to CD99, but similar to another endothelial cell junctional molecule ESAM, does not mediate lymphocyte transmigration in a model of delayed type hypersensitivity. 57,58 Furthermore, as found with PECAM-1, CD99L2 appears to block neutrophil transmigration in vivo at the level of the perivascular basement membrane, though the mechanism by which it can achieve this is at present unclear. 57 Studies from our group have also compared the functional role and potential additive effects of PECAM-1 with JAM-A and ICAM-2.…”

Section: Comparative and Potential Cooperative Roles Of Pecam-1 With mentioning

confidence: 99%

PECAM-1: A Multi-Functional Molecule in Inflammation and Vascular Biology

Woodfin

Voisin

Nourshargh

2007

ATVB

491

345

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Abstract-Platelet endothelial cell adhesion molecule-1 (PECAM-1 or CD31) is a molecule expressed on all cells within the vascular compartment, being expressed to different degrees on most leukocyte sub-types, platelets, and on endothelial cells where its expression is largely concentrated at junctions between adjacent cells. As well as exhibiting adhesive properties, PECAM-1 is an efficient signaling molecule and is now known to have diverse roles in vascular biology including roles in angiogenesis, platelet function, and thrombosis, mechanosensing of endothelial cell response to fluid shear stress, and regulation of multiple stages of leukocyte migration through venular walls. This review will focus on some new developments with respect to the role of PECAM-1 in inflammation and vascular biology, highlighting the emerging complexities associated with the functions of this unique molecule. (Arterioscler Thromb Vasc

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Section: Comparative and Potential Cooperative Roles Of Pecam-1 With mentioning

confidence: 99%

PECAM-1: A Multi-Functional Molecule in Inflammation and Vascular Biology

Woodfin

Voisin

Nourshargh

2007

ATVB

491

345

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“…23,24 All animal procedures were performed in accordance with national and regional laws and regulations and were approved by animal ethics committees. All efforts were made to minimize suffering of the mice.…”

Section: In Vivo Permeability and Inflammation Assaysmentioning

confidence: 99%

Esm1 Modulates Endothelial Tip Cell Behavior and Vascular Permeability by Enhancing VEGF Bioavailability

Rocha¹,

Schiller

Ding

et al. 2014

Circulation Research

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198

178

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Rationale: Endothelial cell–specific molecule 1 (Esm1) is a secreted protein thought to play a role in angiogenesis and inflammation. However, there is currently no direct in vivo evidence supporting a function of Esm1 in either of these processes. Objective: To determine the role of Esm1 in vivo and the underlying molecular mechanisms. Methods and Results: We generated and analyzed Esm1 knockout ( Esm1 KO ) mice to study its role in angiogenesis and inflammation. Esm1 expression is induced by the vascular endothelial growth factor A (VEGF-A) in endothelial tip cells of the mouse retina. Esm1 KO mice showed delayed vascular outgrowth and reduced filopodia extension, which are both VEGF-A–dependent processes. Impairment of Esm1 function led to a decrease in phosphorylated Erk1/2 (extracellular-signal regulated kinases 1/2) in sprouting vessels. We also found that Esm1 KO mice displayed a 40% decrease in leukocyte transmigration. Moreover, VEGF-induced vascular permeability was decreased by 30% in Esm1 KO mice and specifically on stimulation with VEGF-A 165 but not VEGF-A 121 . Accordingly, cerebral edema attributable to ischemic stroke–induced vascular permeability was reduced by 50% in the absence of Esm1. Mechanistically, we show that Esm1 binds directly to fibronectin and thereby displaces fibronectin-bound VEGF-A 165 leading to increased bioavailability of VEGF-A 165 and subsequently enhanced levels of VEGF-A signaling. Conclusions: Esm1 is simultaneously a target and modulator of VEGF signaling in endothelial cells, playing a role in angiogenesis, inflammation, and vascular permeability, which might be of potential interest for therapeutic applications.

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“…The crucial biologic processes involving CD99 include lymphocyte development, cell adhesion and monocyte diapedesis, and expression of TCR, MHC class I and II as well as of some adhesion molecules (i.e., ELAM-1, VCAM-1, ICAM-1) by mobilization of these molecules from the Golgi to the plasma membrane (7)(8)(9)(10)(11)(12)(13)(14). In pathology, CD99 is found on the cell surface of EWS, acute lymphoblastic leukemia, thymic tumors, some spindle cell tumors (e.g., synovial sarcoma), hemangiopericytoma, meningioma, and malignant glioma, in which it confers high invasiveness and low survival rates (13,(15)(16)(17)(18).…”

Section: Introductionmentioning

confidence: 99%

CD99 Triggering in Ewing Sarcoma Delivers a Lethal Signal through p53 Pathway Reactivation and Cooperates with Doxorubicin

Guerzoni

Fiori²,

Terracciano

et al. 2015

Clinical Cancer Research

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Purpose: The paucity of new drugs for the treatment of Ewing sarcoma (EWS) limits the cure of these patients. CD99 has a strong membranous expression in EWS cells and, being also necessary for tumor survival, is a suitable target to aim at. In this article, we described a novel human monospecific bivalent single-chain fragment variable diabody (dAbd C7) directed against CD99 of potential clinical application.Experimental Design: In vitro and in vivo evaluation of cell death and of the molecular mechanisms triggered by anti-CD99 agents were performed alone or in combination with doxorubicin to demonstrate efficacy and selectivity of the new dAbd C7.Results: The dAbd C7 induced rapid and massive EWS cell death through Mdm2 degradation and p53 reactivation. Mdm2 overexpression as well as silencing of p53 in p53wt EWS cells decreased CD99-induced EWS cell death, whereas treatment with nutlin-3 enhanced it. Furthermore, cell death was associated with induction of p21, bax, and mitochondrial depolarization together with substantial inhibition of tumor cell proliferation. Combined treatment of anti-CD99 dAbd C7 with doxorubicin was additive both in vitro and in vivo against EWS xenografts. Normal mesenchymal stem cells showed no p53 activation and were resistant to cell death, unless transformed by EWS-FLI, the oncogenic driver of EWS.Conclusions: These results indicate that dAbd C7 is a suitable candidate tool to target CD99 in patients with EWS able to spare normal stem cells from death as it needs an aberrant genetic context for the efficient delivery of CD99-triggered cell death.

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A CD99-related antigen on endothelial cells mediates neutrophil but not lymphocyte extravasation in vivo

Cited by 93 publications

References 37 publications

PECAM-1: A Multi-Functional Molecule in Inflammation and Vascular Biology

PECAM-1: A Multi-Functional Molecule in Inflammation and Vascular Biology

Esm1 Modulates Endothelial Tip Cell Behavior and Vascular Permeability by Enhancing VEGF Bioavailability

CD99 Triggering in Ewing Sarcoma Delivers a Lethal Signal through p53 Pathway Reactivation and Cooperates with Doxorubicin

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