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Literature DB >> 12031126

Correction of the nonlinear dose response improves the viability of adenoviral vectors for gene therapy of Fabry disease.

Robin J Ziegler¹, Chester Li, Maribeth Cherry, Yunxiang Zhu, Donna Hempel, Nico van Rooijen, Yiannis A Ioannou, Robert J Desnick, Mark A Goldberg, Nelson S Yew, Seng H Cheng.

Abstract

Systemic administration of recombinant adenoviral vectors for gene therapy of chronic diseases such as Fabry disease can be limited by dose-dependent toxicity. Because administration of a high dose of Ad2/CMVHI-alpha gal encoding human alpha-galactosidase A results in expression of supraphysiological levels of the enzyme, we sought to determine whether lower doses would suffice to correct the enzyme deficiency and lysosomal storage abnormality observed in Fabry mice. Reducing the dose of Ad2/CMVHI-alpha gal by 10-fold (from 10(11) to 10(10) particles/mouse) resulted in a greater than 200-fold loss in transgene expression. In Fabry mice, the reduced expression of alpha-galactosidase A, using the lower dose of Ad2/CMVHI-alpha gal, was associated with less than optimal clearance of the accumulated glycosphingolipid (GL-3) from the affected lysosomes. It was determined that this lack of linearity in dose response was not due to an inability to deliver the recombinant viral vectors to the liver but rather to sequestration, at least in part, of the viral vectors by the Kupffer cells. This lack of correlation between dose and expression levels could be obviated by supplementing the low dose of Ad2/CMVHI-alpha gal with an unrelated adenoviral vector or by depleting the Kupffer cells before administration of Ad2/CMVHI-alpha gal. Prior removal of the Kupffer cells, using clodronate liposomes, facilitated the use of a 100-fold lower dose of Ad2/CMVHI-alpha gal (10(9) particles/mouse) to effect the nearly complete clearance of GL-3 from the affected organs of Fabry mice. These results suggest that practical strategies that minimize the interaction between the recombinant adenoviral vectors and the reticuloendothelial system (RES) may improve the therapeutic window of this vector system. In this regard, we showed that pretreatment of mice with gamma globulins also resulted in significantly enhanced adenovirus-mediated transduction and expression of alpha-galactosidase A in the liver.

Entities: Chemical Disease Gene Species

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Year: 2002 PMID： 12031126 DOI： 10.1089/10430340252939041

Source DB: PubMed Journal: Hum Gene Ther ISSN： 1043-0342 Impact factor: 5.695

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Cited

15 in total

1. Anderson-Fabry disease in Austria.

Authors: Matthias Lorenz; Anna-Christina Hauser; Margot Püspök-Schwarz; Peter Kotanko; Ingrid Arias; Herbert Zodl; Reinhard Kramar; Eduard Paschke; Till Voigtländer; Gere Sunder-Plassmann
Journal: Wien Klin Wochenschr Date: 2003-04-30 Impact factor: 1.704

Review 2. Adenovirus vector induced innate immune responses: impact upon efficacy and toxicity in gene therapy and vaccine applications.

Authors: Zachary C Hartman; Daniel M Appledorn; Andrea Amalfitano
Journal: Virus Res Date: 2007-11-26 Impact factor: 3.303

3. Long-term correction of globotriaosylceramide storage in Fabry mice by recombinant adeno-associated virus-mediated gene transfer.

Authors: Jinhee Park; Gary J Murray; Advait Limaye; Jane M Quirk; Monique P Gelderman; Roscoe O Brady; Pankaj Qasba
Journal: Proc Natl Acad Sci U S A Date: 2003-03-06 Impact factor: 11.205

4. Sustained phenotypic correction in a mouse model of hypoalphalipoproteinemia with a helper-dependent adenovirus vector.

Authors: K Oka; L M Belalcazar; C Dieker; E A Nour; P Nuno-Gonzalez; A Paul; S Cormier; J-K Shin; M Finegold; L Chan
Journal: Gene Ther Date: 2006-09-07 Impact factor: 5.250

5. Modifications of adenovirus hexon allow for either hepatocyte detargeting or targeting with potential evasion from Kupffer cells.

Authors: Jan-Michael Prill; Sigrid Espenlaub; Ulrike Samen; Tatjana Engler; Erika Schmidt; Francesco Vetrini; Amanda Rosewell; Nathan Grove; Donna Palmer; Philip Ng; Stefan Kochanek; Florian Kreppel
Journal: Mol Ther Date: 2010-10-19 Impact factor: 11.454

6. Naked plasmid DNA-based alpha-galactosidase A gene transfer partially reduces systemic accumulation of globotriaosylceramide in Fabry mice.

Authors: Gen Nakamura; Hiroki Maruyama; Satoshi Ishii; Masaaki Shimotori; Shigemi Kameda; Toru Kono; Jun-ichi Miyazaki; Ashok B Kulkarni; Fumitake Gejyo
Journal: Mol Biotechnol Date: 2007-10-13 Impact factor: 2.695

Correction of the nonlinear dose response improves the viability of adenoviral vectors for gene therapy of Fabry disease.

1. Anderson-Fabry disease in Austria.

Review 2. Adenovirus vector induced innate immune responses: impact upon efficacy and toxicity in gene therapy and vaccine applications.

3. Long-term correction of globotriaosylceramide storage in Fabry mice by recombinant adeno-associated virus-mediated gene transfer.

4. Sustained phenotypic correction in a mouse model of hypoalphalipoproteinemia with a helper-dependent adenovirus vector.

5. Modifications of adenovirus hexon allow for either hepatocyte detargeting or targeting with potential evasion from Kupffer cells.

6. Naked plasmid DNA-based alpha-galactosidase A gene transfer partially reduces systemic accumulation of globotriaosylceramide in Fabry mice.

7. Redundant and synergistic mechanisms control the sequestration of blood-born adenovirus in the liver.

Review 8. Sphingolipid lysosomal storage disorders.

Review 9. Gene therapy approaches for lysosomal storage disease: next-generation treatment.

10. A new model for CD8+ T cell memory inflation based upon a recombinant adenoviral vector.