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See detailIn-line characterization of hetero bipolar transistor base layers and pMOS devices with embedded SiGe by high-resolution x-ray diffraction
Hikavyy, A.; Nguyen, Ngoc Duy ULg; Loo, R. et al

Poster (2008)

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See detailIn-line characterization of heterojunction bipolar transistor base layers by high-resolution x-ray diffraction
Nguyen, Ngoc Duy ULg; Loo, R.; Hikavyy, A. et al

in ECS Transactions (2007), 10

The suitability of high-resolution X-ray diffraction (HRXRD) as an in-line measurement tool for the characterization of heterojunction bipolar transistor SiGe base layers and Si cap layers was ... [more ▼]

The suitability of high-resolution X-ray diffraction (HRXRD) as an in-line measurement tool for the characterization of heterojunction bipolar transistor SiGe base layers and Si cap layers was investigated. We showed that despite of polycrystalline Si on the mask material of patterned wafers, HRXRD measurements performed on an array of small windows yield results which are comparable to those that were obtained on a window which is larger than the size of the source beam, regarding the thickness and the Ge content of the SiGe layers. The possibility to extract layer parameters for active device windows of different sizes was therefore demonstrated. The suitability of HRXRD for in-line measurement of the Si cap thickness was also assessed and the sensitivity of this technique for determining the substitutional boron concentration in SiGe was studied. The detection limit in the monitoring of the active dopant concentration was about 2.7 × 1019 cm-3. [less ▲]

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See detailIn-line characterization of heterojunction bipolar transistor base layers by high-resolution x-ray diffraction
Nguyen, Ngoc Duy ULg; Loo, R.; Hikavyy, A. et al

Poster (2007)

Detailed reference viewed: 6 (0 ULg)
Peer Reviewed
See detailIn-line characterization of heterojunction bipolar transistor base layers by high-resolution x-ray diffraction
Nguyen, Ngoc Duy ULg; Loo, R.; Hikavyy, A. et al

Conference (2007)

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See detailHuman platelet glycoprotein VI function is antagonized by monoclonal antibody-derived Fab fragments.
Lecut, Christelle ULg; Feeney, L. A.; Kingsbury, G. et al

in Journal of Thrombosis and Haemostasis [=JTH] (2003), 1(12), 2653-62

Platelet interactions with adhesive ligands exposed at sites of vascular injury initiate the normal hemostatic response but may also lead to arterial thrombosis. Platelet membrane glycoprotein (GP)VI is a ... [more ▼]

Platelet interactions with adhesive ligands exposed at sites of vascular injury initiate the normal hemostatic response but may also lead to arterial thrombosis. Platelet membrane glycoprotein (GP)VI is a key receptor for collagen. Impairment of GPVI function in mice results in a long-term antithrombotic protection and prevents neointimal hyperplasia following arterial injury. On the other hand, GPVI deficiency in humans or mice does not result in serious bleeding tendencies. Blocking GPVI function may thus represent a new and safe antithrombotic approach, but no specific, potent anti-GPVI directed at the human receptor is yet available. Our aim was to produce accessible antagonists of human GPVI to evaluate the consequences of GPVI blockade. Amongst several monoclonal antibodies to the extracellular domain of human GPVI, one, 9O12.2, was selected for its capacity to disrupt the interaction of GPVI with collagen in a purified system and to prevent the adhesion of cells expressing recombinant GPVI to collagen and collagen-related peptides (CRP). While 9O12.2 IgGs induced platelet activation by a mechanism involving GPVI and Fc gamma RIIA, 9O12.2 Fab fragments completely blocked collagen-induced platelet aggregation and secretion from 5 microg mL-1 and fully prevented CRP-induced activation from 1.5 microg mL-1. 9O12.2 Fabs also inhibited the procoagulant activity of collagen-stimulated platelets and platelet adhesion to collagen in static conditions. Furthermore, 9O12.2 Fabs impaired platelet adhesion, and prevented thrombi formation under arterial flow conditions. We thus describe here for the first time a functional monoclonal antibody to human GPVI and demonstrate its effect on collagen-induced platelet aggregation and procoagulant activity, and on thrombus growth. [less ▲]

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