NYUHSL Faculty Bibliography

Searched for:

person:silveg03

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143

Journal of clinical rheumatology. JCR. 2015:21(5):231-8.DOI: 10.1097/RHU.0000000000000276

Efficacy and Safety of Tabalumab, an Anti-B-Cell-Activating Factor Monoclonal Antibody, in a Heterogeneous Rheumatoid Arthritis Population: Results From a Randomized, Placebo-Controlled, Phase 3 Trial (FLEX-O)

Genovese, Mark C; Silverman, Gregg J; Emery, Paul; Gupta, Ramesh C; Gill, Anne; Veenhuizen, Melissa; Xie, Li; Komocsar, Wendy J; Berclaz, Pierre-Yves; Lee, Chin

OBJECTIVES: The efficacy and safety of 2 different dosing regimens of tabalumab, a monoclonal antibody that neutralizes membrane-bound and soluble B-cell-activating factor (BAFF), were evaluated in patients with rheumatoid arthritis. METHODS: In this phase 3, multicenter, randomized study, 1004 patients (intention-to-treat population) received subcutaneous 120 mg tabalumab every 4 weeks (120/Q4W), 90 mg tabalumab every 2 weeks (90/Q2W), or placebo over 24 weeks. At baseline, a loading dose double the planned dose (ie, 240 mg, 180 mg, or placebo) was administered. Efficacy analyses were based on a prespecified subset of patients with 5 or more of 68 tender and 5 or more of 66 swollen joints at baseline (efficacy population, n = 849). The primary efficacy end point was ACR20 (20% improvement in American College of Rheumatology criteria) response at week 24. RESULTS: At week 24, there were no differences in ACR20 response rates (120/Q4W = 34.4%, 90/Q2W = 33.5%, placebo = 31.5%) or any other measures of efficacy across the treatment groups. Discontinuations due to adverse events (AE) were 3.4%, 2.7%, and 4.0%; incidence of treatment-emergent AEs were 64.1%, 58.2%, and 58.8%, with 23.2%, 25.9%, and 22.0% treatment-emergent infections; and incidence rates of serious AEs were 3.7%, 2.2%, and 2.8% with 1.1%, 0.3%, and 0.7% serious infections in the 120/Q4W, 90/Q2W, and placebo groups, respectively. Three deaths were reported (120/Q4W, n = 2; 90/Q2W, n = 1). Each tabalumab group had significant decreases versus placebo in CD3-CD20 B cells (P

PMID: 26203826

ISSN: 1536-7355

CID: 1698212

Discovery medicine. 2015:19(103):117-25.DOI:

T cell chemokine receptor patterns as pathogenic signatures in autoimmunity

Strazza, Marianne; Azoulay-Alfaguter, Inbar; Silverman, Gregg J; Mor, Adam

Autoimmune diseases arise from aberrant activation of immune cells directed against endogenous autoantigens expressed throughout the human body. While the initiating triggers remain poorly understood, the self-perpetuating phase of these diseases is directly linked to the ongoing recruitment of inflammatory cells that traffic to the affected anatomical sites. T lymphocytes are prominent drivers of many autoimmune diseases and the targeted trafficking of these cells to infiltrate the affected organs is often a common denominator. The regulation of T cell trafficking involves the coordinated expression of specific patterns of chemokines and the reciprocal expression of cognate chemokine receptors on T cell membranes. Thereby, chemokines direct the specific trafficking of a wide array of responsive activated immune cells. Specific patterns of chemokine receptor expression can correlate with disease activity in an autoimmune disease, confirming the importance of further characterizing the T cells that infiltrate specific sites of autoimmunity. Herein, we will review our current understanding of the roles of chemokines in two common autoimmune diseases: rheumatoid arthritis and multiple sclerosis. We also discuss the implications for chemokine receptor signatures in autoimmune pathogenesis, and how these may provide novel targets for therapeutic intervention.

PMID: 25725226

ISSN: 1539-6509

CID: 1474182

Arthritis & rheumatology. 2015:67.DOI:

Does Dysbiosis within the Intestinal Microbiome Contribute to SLE Pathogenesis? [Meeting Abstract]

Silverman, Gregg J; Getu, Lelise; Niu, Haitao; El Bannoudi, Hanane; Heguy, Adriana; Alekseyenko, Alexander; Buyon, Jill P; Azzouz, Doua

ISI:000370860203483

ISSN: 2326-5205

CID: 2029162

Arthritis & rheumatology. 2014:66:S191-S191.DOI:

Citrulline-Specific Autoimmunity Resides in Quiescent Circulating Memory B Cells in Rheumatoid Arthritis. [Meeting Abstract]

Pelzek, Adam; Groenwall, Caroline; Greenberg, Jeffrey D; Silverman, Gregg J

ISI:000344384900447

ISSN: 2326-5205

CID: 1443962

Arthritis & rheumatology. 2014:66:S584-S584.DOI:

Modulation of Natural IgM-Autoantibodies to Oxidative Stress-Related Neo-Epitopes on Apoptotic Cells in Newborns of Mothers with Anti-Ro Autoimmunity [Meeting Abstract]

Groenwall, Caroline; Clancy, Robert M; Getu, Lelise; Siegel, Don L; Reed, Joanne; Buyon, Jill P; Silverman, Gregg J

ISI:000344384902432

ISSN: 2326-5205

CID: 1444002

Arthritis & rheumatology. 2014:66:S165-S165.DOI:

Levels of IgG Autoantibodies to Oxidation-Associated MDA Neo-Determinants Are a Biomarker for Systemic Inflammation and Disease Activity in SLE and RA [Meeting Abstract]

Groenwall, Caroline; Getu, Lelise; Greenberg, Jeffrey D; Clancy, Robert M; Silverman, Gregg J

ISI:000344384900386

ISSN: 2326-5205

CID: 1443952

Journal of clinical immunology. 2014:34 Suppl 1:S12-21.DOI: 10.1007/s10875-014-0025-4

Natural IgM: beneficial autoantibodies for the control of inflammatory and autoimmune disease

Gronwall, Caroline; Silverman, Gregg J

Natural IgM are highly represented in the circulation at birth, and these often autoreactive antibodies have been postulated to have innate-like properties and play crucial roles in apoptotic cell clearance, tissue homeostasis, and immune modulation. This review summarizes the known properties of these IgM autoantibodies, and the evidence that these anti-apoptotic cell IgM natural antibodies can regulate inflammatory responses through ancient pathways of the innate immune system that first arose long before the initial emergence of the adaptive immune system. While the regulatory contributions of these natural IgM autoantibodies are certainly not an essential and fundamental component of host defenses, these provide an additional layer to further protect the host. More importantly, these IgM antibody responses are highly inducible and their up-regulation can be a powerful means for the host to survive in a setting of chronic inflammation. The observed beneficial clinical associations for cardiovascular disease and autoimmunity, as well as opportunities for potential therapeutic implications are discussed.

PMCID:4354681

PMID: 24691998

ISSN: 0271-9142

CID: 1153342

Clinical immunology. 2014:153(1):1-7.DOI: 10.1016/j.clim.2014.03.017

Relation of carotid plaque with natural IgM antibodies in patients with systemic lupus erythematosus

Gronwall, Caroline; Reynolds, Harmony; Kim, June K; Buyon, Jill; Goldberg, Judith D; Clancy, Robert M; Silverman, Gregg J

Noninvasive carotid measurements have proven value in the estimation of future cardiovascular (CV) outcomes in systemic lupus erythematosus (SLE). Natural IgM-antibodies to phosphorylcholine (PC) epitopes can enhance apoptotic-cell clearance and induce anti-inflammatory pathways. Herein, we show that subclinical CV disease, as detected by carotid ultrasound, in a cross-sectional SLE cohort was associated with lower levels of IgM anti-PC, as well as lower levels of the ratio of IgM anti-PC/total IgM, compared to patients without plaque (p=0.004 and p=0.02, respectively). The IgM anti-PC/total IgM association remained significant after adjusting for age, cholesterol and hypertension. Adiponectin and sE-selectin were significantly elevated in patients with plaque, and statistical models showed that combining adiponectin, sE-selectin and IgM anti-PC/total IgM was better for predicting plaque than either test alone. These results support the hypothesis that IgM-natural autoantibodies may inhibit atherogenesis, and confirm the utility of IgM anti-PC levels as a biomarker for subclinical CV disease.

PMCID:4068957

PMID: 24704464

ISSN: 1521-6616

CID: 960172

Clinical immunology. 2014:153(1):145-52.DOI: 10.1016/j.clim.2014.04.010

Programmed death-1 pathway in cancer and autoimmunity

Pedoeem, Ariel; Azoulay-Alfaguter, Inbar; Strazza, Marianne; Silverman, Gregg J; Mor, Adam

Programmed death-1 (PD-1) is a co-receptor that is expressed predominantly by T cells. The binding of PD-1 to its ligands, PD-L1 or PD-L2, is vital for the physiologic regulation of the immune system. A major functional role of the PD-1 signaling pathway is the inhibition of self-reactive T cells, which serve to protect against autoimmune disease. Elimination of the PD-1 pathway can therefore result in the breakdown of immune tolerance that can ultimately lead to the development of pathogenic autoimmunity. Conversely, tumor cells can at times co-opt the PD-1 pathway to escape from immunosurveillance mechanisms. Therefore, blockade of the PD-1 pathway has become an attractive target in cancer therapy. Recent clinical trials have shown that anti-PD-1 agents have profound effects on solid tumor regression. Current approaches include six agents that are either PD-1 and PD-L1 targeted neutralizing antibodies or fusion proteins. More than forty clinical trials are underway to better define the role of PD-1 blockade in variety of tumor types. In this review we will highlight the basic biology of the PD-1 system and discuss its potential roles in both autoimmunity and cancer. We propose that future research on PD-1 may lead to the translation of fundamental regulatory pathways into the development of practical new approaches for the treatment of autoimmune diseases and cancer.

PMID: 24780173

ISSN: 1521-6616

CID: 940352

Annals of the rheumatic diseases. 2014:73:595-595.DOI: 10.1136/annrheumdis-2014-eular.4322

CORRELATION OF CAROTID INTIMAL PLAQUE IN SLE WITH NON-TRADITIONAL SERUM BIOMARKERS [Meeting Abstract]

Groenwall, C; Reynolds, HR; Buyon, J; Kim, J; Goldberg, JD; Silverman, GJ; Clancy, RM

ISI:000346919803214

ISSN: 1468-2060

CID: 1599012