The objective of this treatment protocol is to provide guidance to Treating Physicians who seek access to pegunigalsidase alfa for Fabry patients whose clinical condition, in the opinion of the Treating Physician, requires treatment with enzyme replacement therapy (ERT) with pegunigalsidase alfa and a) cannot be adequately treated with currently approved FDA products and/or b) are not able or willing to participate in any of the on-going clinical trials in the United States.
Drug: Pegunigalsidase Alfa
Pengunigalsidase alfa is a recombinant ERT (enzyme replacement therapy) used to treat Fabry disease (dosage: 1 mg/kg body weight every 2 weeks).
Inclusion Criteria: - In the opinion of the Treating Physician, the patient cannot be adequately treated with any FDA approved drugs for Fabry and is not able to enroll in any current clinical trial for Fabry disease. - Patient (or legal guardian) is able to sign an informed consent prior to treatment. - A documented diagnosis of Fabry disease. - Preferably two, but at minimum 1, historical serum creatinine evaluations in the last 2 years with the latest value within the last 6 months. - Female patients and male patients whose co-partners are of child-bearing potential agree to use a medically acceptable method of contraception, not including the rhythm method. Acceptable methods of contraception include hormonal products, intrauterine device, or male or female condoms. Contraception should be used for 90 days after treatment discontinuation.
Exclusion Criteria: - Patients enrolled and currently treated in Study PB-102-F20, and patients enrolled and currently treated in Extension Study PB-102-F60 - Patients who currently are on treatment under any other ongoing clinical trials of PRX-102 - History of Type 1 (anaphylaxis or anaphylactoid like) life-threatening hypersensitivity during previous exposure to other ERTs which could not be handled with medication - Women who are breastfeeding may not participate unless they agree to stop breastfeeding. - Women who are currently pregnant.
University of Alabama-Birmingham
Birmingham, Alabama, 35294
Investigator: Eric Wallace
Phoenix Children's Hospital, Inc.
Phoenix, Arizona, 85006
Investigator: Jasmine Knoll
University of California Irvine
Orange, California, 92868
Investigator: Virginia Kimonis
Central Coas Nephrology
Salinas, California, 93901
Investigator: Barbara Rever
University of Florida, Division of Pediatric Genetics
Jacksonville, Florida, 32207
Investigator: Estella Mellin
Emory University School of Medicine
Atlanta, Georgia, 30322
Investigator: William Wilcox
University of Iowa
Iowa City, Iowa, 52242
Investigator: John Bernat
Infusion Associates
Grand Rapids, Michigan, 49525
Investigator: Khan Nedd
Dallas Nephrology Associates
Dallas, Texas, 75235-2208
Investigator: Ankit Mehta
University of Utah
Salt Lake City, Utah, 84108
Investigator: Nicola Longo
Lysosomal & Rare Disorder Research & Treatment Center (LRDRTC)
Fairfax, Virginia, 22030
Investigator: Ozlem Goker-Alpan
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