Your search keyword '"Lavin, Peter"' showing total 5 results

1. Arhgap24 inactivates Rac1 in mouse podocytes, and a mutant form is associated with familial focal segmental glomeruosclerosis

Author

Akilesh, Shreeram, Suleiman, Hani, Yu, Haiyang, Stander, M. Christine, Lavin, Peter, Gbadegesin, Rasheed, Antignac, Corinne, Pollak, Martin, Kopp, Jeffrey B., Winn, Michelle P., and Shaw, Andrey S.

Subjects

Gene mutations -- Health aspects -- Research, Epithelial cells -- Physiological aspects -- Research, Kidney diseases -- Genetic aspects -- Research -- Risk factors, Health care industry

Abstract

The specialized epithelial cell of the kidney, the podocyte, has a complex actinbased cytoskeleton. Dynamic regulation of this cytoskeleton is required for efficient barrier function of the kidney. Podocytes are a useful cell type to study the control of the actin cytoskeleton in vivo, because disruption of components of the cytoskeleton results in podocyte damage, cell loss, and a prototypic injury response called focal segmental glomerulosclerosis (FSGS). Searching for actin regulatory proteins that are expressed in podocytes, we identified a RhoA-activated Rac1 GTPase-activating protein (Rac1-GAP), Arhgap24, that was upregulated in podocytes as they differentiated, both in vitro and in vivo. Increased levels of active Rac1 and Cdc42 were measured in Arhgap24 knockdown experiments, which influenced podocyte cell shape and membrane dynamics. Consistent with a role for Arhgap24 in normal podocyte functioning in vivo, sequencing of the ARHGAP24 gene in patients with FSGS identified a mutation that impaired its Rac1-GAP activity and was associated with disease in a family with FSGS. Thus, Arhgap24 contributes to the careful balancing of RhoA and Rac1 signaling in podocytes, the disruption of which may lead to kidney disease., Introduction The kidneys filter plasma and reabsorb solutes and nutrients to maintain the appropriate extracellular environment. The proximal component of the nephron, the glomerulus, is the primary filtration barrier that [...]

Published

2011

2. Pathogenesis and therapy of focal segmental glomerulosclerosis: an update

Author

Gbadegesin, Rasheed, Lavin, Peter, Foreman, John, and Winn, Michelle

Subjects

Glomerulonephritis -- Development and progression -- Care and treatment, Pediatric research, Health

Abstract

Focal and segmental glomerulosclerosis (FSGS) is an important cause of steroid-resistant nephrotic syndrome in adults and children. It is responsible for 5-20% of all cases of end-stage kidney disease (ESKD) in the United States. The pathogenesis of FSGS has not been fully elucidated; however, data from molecular studies of familial cases in the last two decades suggest that FSGS is a defect of the podocyte. The therapeutic agents available for treatment of FSGS are not very effective and only a small percentage of affected individuals will achieve complete remission. Recent data from molecular biology and molecular genetics has provided insight into the mechanisms of action of old agents and also identification of other novel therapeutic targets. This review focuses on recent advances in the molecular pathogenesis of FSGS and currently available therapeutic agents as well as potential novel therapies., Author(s): Rasheed Gbadegesin [sup.1] , Peter Lavin [sup.2] , John Foreman [sup.1] , Michelle Winn [sup.2] Author Affiliations: (1) grid.189509.c, 0000000100241216, Department of Pediatrics, Duke University Medical Center, , 27710, [...]

Published

2011

3. Pathogenesis and therapy of focal segmental glomerulosclerosis: an update

Author

Gbadegesin, Rasheed, Lavin, Peter, Foreman, John, and Winn, Michelle

Subjects

Molecular genetics -- Health aspects, Chronic kidney failure -- Health aspects, Health

Abstract

Focal and segmental glomerulosclerosis (FSGS) is an important cause of steroid-resistant nephrotic syndrome in adults and children. It is responsible for 5-20% of all cases of end-stage kidney disease (ESKD) in the United States. The pathogenesis of FSGS has not been fully elucidated; however, data from molecular studies of familial cases in the last two decades suggest that FSGS is a defect of the podocyte. The therapeutic agents available for treatment of FSGS are not very effective and only a small percentage of affected individuals will achieve complete remission. Recent data from molecular biology and molecular genetics has provided insight into the mechanisms of action of old agents and also identification of other novel therapeutic targets. This review focuses on recent advances in the molecular pathogenesis of FSGS and currently available therapeutic agents as well as potential novel therapies. Keywords Focal and segmental glomerulosclerosis * Podocyte * Molecular pathogenesis * Therapy, Introduction Focal segmental glomerulosclerosis (FSGS) was first described in kidney biopsy of adults with nephrotic syndrome by Fahr in 1925 (cited in [1, 2]). About 32 years later, Rich made [...]

Published

2011

4. Madonna Expiratory Respiratory Trainer (MERT): a self-practice device for improving the control of alveolar pressure (technical note)

Author

Hakel, Mark, Beukelman, David, Perez, Lance C., Lavin, Peter, and Kavan, Paul

Subjects

Speech disorders -- Care and treatment, Respiratory therapy -- Equipment and supplies, Health, Care and treatment, Product introduction

Abstract

Reduced respiratory drive for speech occurs in conjunction with a range of neurological conditions. Traditional interventions to increase respiratory drive may include laryngeal aerodynamic instrumentation, manometers, or use of a [...]

Published

2008

5. Cover story

Author

Lavin, Peter

Subjects

Company acquisition/merger, Mitsubishi Electric Corp. -- Mergers, acquisitions and divestments, Apricot Computers Ltd. -- Mergers, acquisitions and divestments

Abstract

COVER STORY Q Will there still be Apricots in the UK? In other markets will they be Mitsubishi's? A We're looking at it market by market but in general the […]

Published

1990