Your search keyword '"Kelly, Susan J."' showing total 4 results

1. Uric acid is a danger signal of increasing risk for osteoarthritis through inflammasome activation.

Author

Denoble AE, Huffman KM, Stabler TV, Kelly SJ, Hershfield MS, McDaniel GE, Coleman RE, and Kraus VB

Subjects

Aged, Carrier Proteins genetics, Cohort Studies, Female, Humans, Interleukin-1 blood, Interleukin-18 biosynthesis, Male, Middle Aged, NLR Family, Pyrin Domain-Containing 3 Protein, Osteoarthritis genetics, Osteoarthritis immunology, Risk Factors, Severity of Illness Index, Knee pathology, Osteoarthritis blood, Uric Acid blood

Abstract

Uric acid (UA) is known to activate the NLRP3 (Nacht, leucine-rich repeat and pyrin domain containing protein 3) inflammasome. When activated, the NLRP3 (also known as NALP3) inflammasome leads to the production of IL-18 and IL-1β. In this cohort of subjects with knee osteoarthritis (OA), synovial fluid uric acid was strongly correlated with synovial fluid IL-18 and IL-1β. Synovial fluid uric acid and IL-18 were strongly and positively associated with OA severity as measured by both radiograph and bone scintigraphy, and synovial fluid IL-1β was associated with OA severity but only by radiograph. Furthermore, synovial fluid IL-18 was associated with a 3-y change in OA severity, on the basis of the radiograph. We conclude that synovial fluid uric acid is a marker of knee OA severity. The correlation of synovial fluid uric acid with the two cytokines (IL-18 and IL-1β) known to be produced by uric acid-activated inflammasomes and the association of synovial fluid IL-18 with OA progression, lend strong support to the potential involvement of the innate immune system in OA pathology and OA progression.

Published

2011

2. Treating gout with pegloticase, a PEGylated urate oxidase, provides insight into the importance of uric acid as an antioxidant in vivo.

Author

Hershfield MS, Roberts LJ 2nd, Ganson NJ, Kelly SJ, Santisteban I, Scarlett E, Jaggers D, and Sundy JS

Subjects

Cells, Cultured, Erythrocytes cytology, Erythrocytes drug effects, Erythrocytes metabolism, F2-Isoprostanes metabolism, Gout metabolism, Humans, Hydrogen Peroxide metabolism, Oxidation-Reduction, Oxidative Stress, Polyethylene Glycols, Proteins metabolism, Urate Oxidase therapeutic use, Uric Acid blood, Antioxidants metabolism, Gout drug therapy, Urate Oxidase administration & dosage, Uric Acid metabolism

Abstract

A high plasma urate concentration (PUA), related to loss of urate oxidase in evolution, is postulated to protect humans from oxidative injury. This hypothesis has broad clinical relevance, but support rests largely on in vitro data and epidemiologic associations. Pegloticase therapy generates H(2)O(2) while depleting urate, offering an in vivo test of the antioxidant hypothesis. We show that erythrocytes can efficiently eliminate H(2)O(2) derived from urate oxidation to prevent cell injury in vitro; during therapy, disulfide-linked peroxiredoxin 2 dimer did not accumulate in red blood cells, indicating that their peroxidase capacity was not exceeded. To assess oxidative stress, we monitored F2-Isoprostanes (F2-IsoPs) and protein carbonyls (PC), products of arachidonic acid and protein oxidation, in plasma of 26 refractory gout patients receiving up to five infusions of pegloticase at 3-wk intervals. At baseline, PUA was markedly elevated in all patients, and plasma F2-IsoP concentration was elevated in most. Pegloticase infusion rapidly lowered mean PUA to < or = 1 mg/dL in all patients, and PUA remained low in 16 of 21 patients who completed treatment. F2-IsoP levels did not correlate with PUA and did not increase during 15 wk of sustained urate depletion. There also was no significant change in the levels of plasma PC. Because refractory gout is associated with high oxidative stress in spite of high PUA, and profoundly depleting uric acid did not increase lipid or protein oxidation, we conclude that urate is not a major factor controlling oxidative stress in vivo.

Published

2010

3. Development of PEGylated mammalian urate oxidase as a therapy for patients with refractory gout

Author

Hershfield, Michael S., Sundy, John S., Ganson, Nancy J., Kelly, Susan J., Parnham, Michael J., editor, Bruinvels, J., editor, and Veronese, Francesco M., editor

Published

2009

4. Pharmacokinetics and Pharmacodynamics of Intravenous PEGylated Recombinant Mammalian Urate Oxidase in Patients With Refractory Gout.

Author

Sundy, John S., Ganson, Nancy J., Kelly, Susan J., Scarlett, Edna L., Rehrig, Claudia D., Huang, William, and Hershfield, Michael S.

Subjects

OXIDASES, URIC acid, INTRAVENOUS therapy, GOUT treatment, DRUG efficacy, DRUG tolerance, IMMUNOGENETICS, IMMUNE response

Abstract

This article discusses a study that examined the efficacy, immunogenecity and tolerability of intravenous (IV) PEGylated recombinant mammalian urate oxidase for the treatment of severe gout. Patients with symptomatic gout served as study subjects. The common comorbidities associated with gout are cited. Majority of patients had a history of acute gout attacks. The study found a marked reduction in renal uric acid excretion after infusion of PEG-uricase. Information regarding immune response to IV PEG-uricase is given.

Published

2007