Abstract

We have concluded that ornithine transcarbamylase deficiency (OTCD) is a well suited disease for the development of both acute and long-term gene therapy. Current treatment of OTCD has failed to avert a high mortality or morbidity rate; Given the relative frequency of OTCD, an adequate population is available for study; The OTC gene has been sequenced and preliminary studies of gene therapy in animal models have been promising; The OTC gene is not rate-limiting for ureagenesis, so excessive activity should not have adverse consequences; The disorder is X-linked and hemizygous males have virtually absent enzyme activity; and Restoration of enzyme activity in the liver, should suffice to normalize metabolism without the need to introduce the gene into the central nervous system. We propose to study in vivo gene therapy for OTCD with a recombinant adenovirus in order to control acute, life-threatening hyperammonemic crises. We also propose to use ex vivo transfer of the OTC gene with a recombinant retrovirus to provide long-term management of patients who are clinically stable at the time of gene therapy, but who remain at high risk of sustaining brain damage or of dying because of a future hyperammonemic episode. Stable transduction will also be tested in children using a second generation recombinant adenovirus. Studies will focus on duration of metabolic, neurochemical, toxicologic, and immunologic consequences, and neurodevelopmental outcome. There are three specific aims to this project: (I) We hypothesize that a recombinant adenovirus containing the OTC gene will be effective and safe for the short-term treatment of neonates and older children with OTCD who are in hyperammonemic crisis. To establish the effective and safe dose we will initially test various doses of the construct in adult asymptomatic OTCD heterozygotes. We will subsequently treat neonates in hyperammonemic coma and infants, children and adults with symptomatic OTCD using the recombinant adenovirus. Efficacy will be measured by normalization of plasma ammonium, urea cycle intermediates, and urinary orotate excretion, rate of flux through the urea cycle, and OTC correction in liver. (II) We hypothesize that long-term correction of OTCD can be achieved either by ex vivo or in vivo gene therapy using a recombinant retrovirus or a second generation temperature sensitive recombinant adenovirus. (III) Finally, we hypothesize that immune activation following gene therapy may affect safety, efficacy and duration of gene therapy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Program Projects (P01)
Project #
5P01HD032649-04
Application #
6272338
Study Section
Project Start
1997-12-01
Project End
1998-11-30
Budget Start
1997-10-01
Budget End
1998-09-30
Support Year
4
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
Children's Hospital of Philadelphia
Department
Type
DUNS #
073757627
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Raper, Steven E; Chirmule, Narendra; Lee, Frank S et al. (2003) Fatal systemic inflammatory response syndrome in a ornithine transcarbamylase deficient patient following adenoviral gene transfer. Mol Genet Metab 80:148-58
Raper, Steven E; Yudkoff, Marc; Chirmule, Narendra et al. (2002) A pilot study of in vivo liver-directed gene transfer with an adenoviral vector in partial ornithine transcarbamylase deficiency. Hum Gene Ther 13:163-75
Ye, X; Zimmer, K P; Brown, R et al. (2001) Differences in the human and mouse amino-terminal leader peptides of ornithine transcarbamylase affect mitochondrial import and efficacy of adenoviral vectors. Hum Gene Ther 12:1035-46
Chen, S J; Tazelaar, J; Wilson, J M (2001) Selective repopulation of normal mouse liver by hepatocytes transduced in vivo with recombinant adeno-associated virus. Hum Gene Ther 12:45-50
Chen, S J; Tazelaar, J; Moscioni, A D et al. (2000) In vivo selection of hepatocytes transduced with adeno-associated viral vectors. Mol Ther 1:414-22
Ye, X; Whiteman, B; Jerebtsova, M et al. (2000) Correction of argininosuccinate synthetase (AS) deficiency in a murine model of citrullinemia with recombinant adenovirus carrying human AS cDNA. Gene Ther 7:1777-82
Xiao, W; Chirmule, N; Schnell, M A et al. (2000) Route of administration determines induction of T-cell-independent humoral responses to adeno-associated virus vectors. Mol Ther 1:323-9
Ye, X; Robinson, M B; Pabin, C et al. (2000) Transient depletion of CD4 lymphocyte improves efficacy of repeated administration of recombinant adenovirus in the ornithine transcarbamylase deficient sparse fur mouse. Gene Ther 7:1761-7
Mitchell, M; Jerebtsova, M; Batshaw, M L et al. (2000) Long-term gene transfer to mouse fetuses with recombinant adenovirus and adeno-associated virus (AAV) vectors. Gene Ther 7:1986-92
Chirmule, N; Moscioni, A D; Qian, Y et al. (1999) Fas-Fas ligand interactions play a major role in effector functions of cytotoxic T lymphocytes after adenovirus vector-mediated gene transfer. Hum Gene Ther 10:259-69

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