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Dive into the research topics where Stuart Friedrich is active.

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Featured researches published by Stuart Friedrich.


Transplantation | 2001

Coadministration of either cyclosporine or steroids with humanized monoclonal antibodies against CD80 and CD86 successfully prolong allograft survival after life supporting renal transplantation in cynomolgus monkeys.

Bernard Hausen; Jochen Klupp; U. Christians; John P. Higgins; Roxanne E. Baumgartner; L. Hook; Stuart Friedrich; Abbie Celnicker; Randall E. Morris

BACKGROUND Recent studies have shown some efficacy using monotherapy with monoclonal antibodies (mAb) against CD80 and CD86 receptors after life-supporting renal transplantation in non-human primates. Our study was designed to evaluate the efficacy of combinations of the same mAbs with either microemulsion cyclosporine (CsA) or steroids. METHODS Unilateral renal transplantation was performed in 16 blood group-matched and MLR-mismatched cynomolgus monkeys that were assigned to four different treatment groups. All monkeys in groups I, II, and IV were treated with the combination of a CD80 (h1F1) and CD86 (h3D1) mAb given at 20 mg/kg each preoperatively, then 5 mg/kg at weekly intervals starting postoperative (po) day 0 until poday 56 (9 doses). In group I the animals (n=4) were treated with mAbs only. In group II (n=4) mAbs were combined with a CsA regimen adjusted daily to maintain target 24 hr trough levels of 150-300 ng/ml CsA for poday 0 to poday 56. In group III (n=4) the animals received CsA monotherapy according to the same regimen as group II. In group IV methylprednisone was administered at 2 mg/kg IV on poday 0-2, then at 0.5 mg/kg/day prednisone per gavage that was and tapered to 0.2 mg/kg/day on which they were maintained until poday 56. All animals were off all immunosuppressive treatment after poday 56 and were then followed until poday 119. RESULTS The mean survival of groups I-IV was 74 (range 9-119 days), 113 (96-119 days), 39 (22-71 days), and 79 days (6 to 119), respectively. All animals in group I showed clinical evidence of acute severe rejection (fever, creatinine increase, anuria) within the first week posttransplant, including those that retained renal function until poday 119. Only one animal in group II had a moderate clinical rejection during the treatment period and three of four animals survived the intended follow-up period. All animals in group III had multiple biopsy proven or severe clinical rejection episodes within the first 21 days and only one animal survived beyond poday 40. Moderate or severe acute rejection was diagnosed in three of four animals of group IV within the first 28 days post transplant and only one animal survived until poday 119. CONCLUSION Our data show that combining a calcineurin inhibitor or prednisone with mAbs designed to block costimulatory signals does not antagonize the immunosuppressive efficacy of these mAbs. In addition, combining CsA with mAbs directed against the CD80 and CD86 receptors significantly prolongs graft survival when compared to CsA monotherapy. Therefore clinical trials of humanized mAbs to CD80 and CD86 used in combination with conventional immunosuppression can be considered.


Transplantation | 2003

Treatment with humanized monoclonal antibodies against CD80 and CD86 combined with sirolimus prolongs renal allograft survival in cynomolgus monkeys.

Tudor B rsan; Bernard Hausen; John P. Higgins; Richard W. Hubble; Jochen Klupp; Mario Stalder; Abbie Cheryl Celniker; Stuart Friedrich; Richard M. O Hara; Randall E. Morris

Background. Co-stimulatory blockade has been shown to prolong allograft survival in different transplant models. We investigated the effect of combining humanized anti-CD80 and anti-CD86 monoclonal antibodies (mAb) with sirolimus in cynomolgus monkey renal transplant recipients. Methods. After renal transplantation, groups of four animals were treated daily with sirolimus, sirolimus and nine weekly doses of mAb, two weekly doses of mAb, or sirolimus and two weekly doses of mAb. Results. Survival was significantly better in monkeys treated with the combination of sirolimus and mAb when compared with treatment with either agent alone (P =0.0067 by log-rank analysis). When combined with sirolimus, nine weekly doses of mAb did not result in an additional survival benefit compared with only two mAb doses (P =0.74). None of the treatment regimens used in this study resulted in development of transplantation tolerance. Conclusions. Sirolimus can be successfully combined with humanized mAb against CD80 and CD86. Induction with a short course of mAb is effective in prolonging allograft survival in combination with sirolimus.


Archive | 2000

Human antibodies that bind human il-12 and methods for producing

Jochen G. Salfeld; Michael Roguska; Michael Paskind; Subhashis Banerjee; Daniel Edward Tracey; Michael White; Zehra Kaymakcalan; Boris Labkovsky; Paul Sakorafas; Geertruida M. Veldman; Amy Venturini; Angela Widom; Stuart Friedrich; Nicholas W. Warne; Angela Myles; John Gawain Elvin; Alexander Robert Duncan; Elaine J. Derbyshire; Sara Carmen; Thor Las Holtet; Sarah Leila Du Fou; Stephen Smith


Archive | 2006

Methods for inhibiting the activity of the P40 subunit of human IL-12

Jochen G. Salfeld; Michael Roguska; Michael Paskind; Subhashis Banerjee; Daniel Edward Tracey; Michael White; Zehra Kaymakcalan; Boris Labkovsky; Paul Sakorafas; Geertruida M. Veldman; Amy Venturini; Angela Widom; Stuart Friedrich; Nicholas W. Warne; Angela Kantor; John Gawain Elvin; Alexander Robert Duncan; Elaine J. Derbyshire; Sara Carmen; Stephen Smith; Thor Las Holtet; Sarah Leila Du Fou


Archive | 2004

Human antibodies that bind human IL-12

Jochen G. Salfeld; Michael Roguska; Michael Paskind; Subhashis Banerjee; Daniel Edward Tracey; Michael White; Zehra Kaymakcalan; Boris Labkovsky; Paul Sakorafas; Geertruida M. Veldman; Amy Venturini; Angela Widom; Stuart Friedrich; Nicholas W. Warne; Angela Myles; John Gawain Elvin; Alexander Robert Duncan; Elaine J. Derbyshire; Sara Carmen; Stephen Smith; Thor Las Holtet; Sarah Leila Du Fou


Archive | 2002

Therapies that improve graft survival

Abbie Celnicker; Gary S. Gray; Stuart Friedrich; Allan D. Kirk; Garvin Warner; Bernard Hausen; Randall E. Morris


Archive | 2015

ANTICUERPO AISLADO ANTI IL-12

Michael Roguska; Zehra Kaymakcalan; Paul Sakorafas; Nicholas W. Warne; Angela Widom; John Gawain Elvin; Alexander Robert Duncan; Elaine J. Derbyshire; Sara Carmen; Stephen Smith; Thor Las Holtet; Sarah Leila Du Fou; Subhashis Banerjee; Daniel Edward Tracey; Amy Venturini; Boris Labkovsky; Jochen G. Salfeld; Michael White; Geertruida M. Veldman; Stuart Friedrich; Angela Myles; Michael Paskind


Archive | 2012

Human antibodies that bind human interleukin-12

Jochen G. Salfeld; Michael Roguska; Michael Paskind; Subhashis Banerjee; Daniel Edward Tracey; Michael White; Zehra Kaymakcalan; Boris Labkovsky; Paul Sakorafas; Geertruida M. Veldman; Amy Venturini; Angela Widom; Stuart Friedrich; Nicholas W. Warne; Angela Myles; John Gawain Elvin; Alexander Robert Duncan; Elaine J. Derbyshire; Sara Carmen; Stephen Smith; Thor Las Holtet; Sarah Leila Du Fou


Archive | 2012

Human antibodies that bind the P40 subunit of human IL-12 and methods for using the same

Jochen G. Salfeld; Michael Roguska; Michael Paskind; Subhashis Banerjee; Daniel Edward Tracey; Michael White; Zehra Kaymakcalan; Boris Labkovsky; Paul Sakorafas; Geertruida M. Veldman; Amy Venturini; Angela Widom; Stuart Friedrich; Nicholas W. Warne; Angela Myles; John Gawain Elvin; Alexander Robert Duncan; Elaine J. Derbyshire; Sara Carmen; Stephen Smith; Thor Las Holtet; Sarah Leila Du Fou


Archive | 2012

Methods of treatment using human antibodies that bind IL-12

Jochen G. Salfeld; Michael Roguska; Michael Paskind; Subhashis Banerjee; Daniel Edward Tracey; Michael White; Zehra Kaymakcalan; Boris Labkovsky; Paul Sakorafas; Geertruida M. Veldman; Amy Venturini; Angela Widom; Stuart Friedrich; Nicholas W. Warne; Angela Kantor; John Gawain Elvin; Alexander Robert Duncan; Elaine J. Derbyshire; Sara Carmen; Stephen Smith; Thor Las Holtet; Sarah Leila Du Fou

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Michael Paskind

Massachusetts Institute of Technology

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Michael White

Carnegie Mellon University

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