Your search keyword '"William A. Gahl"' showing total 2 results

1. Hereditary Inclusion Body Myopathy: Single Patient Response to Intravenous Dosing of GNEGene Lipoplex.

Author

Gregory Nemunaitis, Chris M. Jay, Phillip B. Maples, William A. Gahl, Marjan Huizing, Tal Yardeni, Alex W. Tong, Anagha P. Phadke, Beena O. Pappen, Cynthia Bedell, Henry Allen, Cathy Hernandez, Nancy S. Templeton, Joseph Kuhn, Neil Senzer, and John Nemunaitis

Subjects

*INCLUSION body myositis, *GENE therapy, *QUADRICEPS muscle, *MYALGIA, *TACHYCARDIA

Abstract

AbstractHereditary inclusion body myopathy (HIBM) is an autosomal recessive adult-onset myopathy due to mutations in the GNE(UDP-N-acetylglucosamine 2-epimerase/N-acetylmannosamine kinase) gene. Affected patients have no therapeutic options. We have previously demonstrated in preclinical testing the ability to safely correct GNEgene function through liposomal delivery of the wild-type GNEgene. Results were verified in a single patient treated by intravenous infusion of GNEgene lipoplex. A single patient (patient 001) with severe HIBM treated with a compassionate investigational new drug received seven doses of GNEgene lipoplex via intravenous infusion at the following doses: 0.4, 0.4, 1.0, 4.0, 5.0, 6.0, and 7.0 mg of DNA. GNEtransgene expression, downstream induction of sialic acid, safety, and muscle function were evaluated. Transient low-grade fever, myalgia, tachycardia, transaminase elevation, hyponatremia, and hypotension were observed after infusion of each dose of GNEgene lipoplex. Quadriceps muscle expression of the delivered GNE, plasmid, and RNA was observed 24 hr after the 5.0-mg dose and at significantly greater levels 72 hr after the 7.0-mg infusion in comparison with expression in quadriceps muscle immediately before infusion. Sialic acid-related proteins were increased and stabilization in the decline of muscle strength was observed. We conclude that clinical safety and activity have been demonstrated with intravenous infusion of GNEgene lipoplex. Further assessment will involve a phase I trial of intravenous administration of GNEgene lipoplex in individuals with less advanced HIBM with more muscle function. [ABSTRACT FROM AUTHOR]

Published

2011

2. Minocycline?induced hyperpigmentation masquerading as alkaptonuria in individuals with joint pain.

Author

Pim Suwannarat, Chanika Phornphutkul, Isa Bernardini, Maria Turner, and William A. Gahl

Subjects

*CONNECTIVE tissues, *JOINT diseases, *PIGMENTATION disorders, *URINALYSIS, *TETRACYCLINES

Abstract

Alkaptonuria, a rare autosomal?recessive disorder caused by mutations in the HGD gene and a deficiency of homogentisate 1,2?dioxygenase, is characterized by accumulation of homogentisic acid (HGA), ochronosis, and destruction of connective tissue resulting in joint disease. Certain medications have been reported to cause cutaneous hyperpigmentation resembling that of alkaptonuria. We present 5 such cases. Eighty?eight patients with a possible diagnosis of alkaptonuria were examined at the National Institutes of Health Clinical Center between June 2000 and March 2004. The diagnosis of alkaptonuria was confirmed or ruled out by measurement of HGA in the urine. Five patients with findings consistent with ochronosis, including pigmentary changes of the ear and mild degenerative disease of the spine and large joints, were diagnosed clinically as having alkaptonuria, but the diagnosis was withdrawn based on normal urine HGA levels. All 5 patients were women who had taken minocycline for dermatologic or rheumatologic disorders for extended periods. Minocycline?induced hyperpigmentation should be considered in the differential diagnosis of ochronosis. This could be of increased significance now that minocycline and other tetracyclines have been proposed as therapeutic options for rheumatoid arthritis, bringing a new population of patients with ochronosis and arthritis to medical attention with the potential, but incorrect, diagnosis of alkaptonuria. [ABSTRACT FROM AUTHOR]

Published

2004