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Ariel - Volume 2 Number 3

Author: Ager Steve
Bergman Donald
Blecker Michael J.
Case Jr., Delvyn C.
Claflin William
Dorand Rod
Doyle Harry A.
Edwards Lin Set
Edwards Robin
Fernhoff Deborah
Flynn Steve P.
Forsyte Jolian
Graitzer Phil
Guralnik Jack
Miller Eugenia
Williams Tom
Zeligman Harvey
Publication venue: 'Thomas Jefferson University'
Publication date: 01/11/1969
Field of study

Editors Delvyn C. Case, Jr. Paul M. Fernhoff News Editors Richard Bonanno Daniel B. Gould Robin A. Edwards Lay-Out Editor Carol Dolinskas Sports Editor James J. Nocon Contributing Editors Michael J. Blecker Lin Sey Edwards Jack Guralnik W. Cherry Light Features Editor Steven A. Ager Donald A. Bergman Stephen P. Flynn Business Manager Nick Greg

Jefferson Digital Commons

700: Jewish genetic diseases: larger screening panel increases the aggregate carrier rate in the Ashkenazi Jewish population

Author: Barbouth Deborah
Cohen Arnold
Fernhoff Paul
Grinzaid Karen
Hoffman Jodi
Rosen Shoshana
Schneider Adele
Shapiro Faye
Wasserman Debra
Publication venue: Mosby, Inc
Publication date: 01/01/2012
Field of study

Crossref

University of Miami: Scholarship Miami

Safety and efficacy of velaglucerase alfa in Gaucher disease type 1 patients previously treated with imiglucerase

Author: Charrow Joel
Crombez Eric
Elstein Deborah
Eng Christine
Fernhoff Paul
Giraldo Pilar
Grabowski Gregory A
Harmatz Paul
Heisel‐Kurth Margaret
Hughes Derralynn A
Longo Nicola
Mardach Rebecca
Pastores Gregory M
Rhead William
Ruiz Juan A
Smith Laurie
Tylki‐Szymanska Anna
Zahrieh David
Zimran Ari
Publication venue: eScholarship, University of California
Publication date: 19/12/2012
Field of study

Velaglucerase alfa is a glucocerebrosidase produced by gene activation technology in a human fibroblast cell line (HT-1080), and it is indicated as an enzyme replacement therapy (ERT) for the treatment of Gaucher disease type 1 (GD1). This multicenter, open-label, 12-month study examined the safety and efficacy of velaglucerase alfa in patients with GD1 previously receiving imiglucerase. Eligible patients, ≥2 years old and clinically stable on imiglucerase therapy, were switched to velaglucerase alfa at a dose equal to their prior imiglucerase dose. Infusion durations were 1 hr every other week. Forty patients received velaglucerase alfa (18 male, 22 female; four previously splenectomized; age range 9-71 years). Velaglucerase alfa was generally well tolerated with most adverse events (AEs) of mild or moderate severity. The three most frequently reported AEs were headache (12 of 40 patients), arthralgia (9 of 40 patients), and nasopharyngitis (8 of 40 patients). No patients developed antibodies to velaglucerase alfa. There was one serious AE considered treatment-related: a grade 2 anaphylactoid reaction within 30 min of the first infusion. The patient withdrew; this was the only AE-related withdrawal. Hemoglobin concentrations, platelet counts, and spleen and liver volumes remained stable through 12 months. In conclusion, adult and pediatric patients with GD1, previously treated with imiglucerase, successfully transitioned to velaglucerase alfa, which was generally well tolerated and demonstrated efficacy over 12 months' treatment consistent with that observed in the velaglucerase alfa phase 3 clinical trial program

UCL Discovery

PubMed Central

eScholarship - University of California