Abstract

Liver directed gene therapy with recombinant AAV vectors has had recent success in human patients with hemophilia B. However, several problems remain to be solved before gene therapy can be broadly applied to the majority of inborn errors affecting the liver. First, hepatocytes turn over - albeit slowly - in both humans an rodents even without injury. Since rAAV remains mostly episomal and is lost with cell replication it is predictable that transgenes introduced by current generation rAAVs will not persist indefinitely. Second, the limited size capacity of AAV makes it poorly suited for disorders caused by mutations in large genes - for example hemophilia A. Third, the vector doses required to achieve efficient in vivo transduction in human are high and lower doses would be desirable from a manufacturing/cost as well as safety perspective. Finally, the currently used minigene cDNA expression cassettes result in unregulated and non-physiologic levels of transgene expression, which may prove to be problematic for the treatment of some disorders. Here we propose to further develop 3 distinct approaches to enhance transgene persistence in liver gene therapy.
In aim 1, we will work on gene rAAV mediated gene repair in hepatocytes.
Aim 2 is focused on rAAV vectors that can integrate into ribosomal DNA as a safe harbor.
In aim 3 we will refine the components of a system designed to achieve in vivo selection of genetically modified hepatocytes using a small molecule inhibitor of fumarylacetoacetate hydrolase (Fah).

Public Health Relevance

Liver directed gene therapy using recombinant adeno-associated virus (rAAV) vectors is a very promising approach for the treatment of hepatic enzyme deficiencies. However, rAAV vectors do not permanently integrate into the chromosomes of liver cells and therefore the effects of current generation gene therapies are predicted to be only transient. The relevance of the proposed studies is that they may lead to the development of new approaches to enhance transgene persistence in human liver cells and successful implementation could result in a life-long cure of metabolic liver diseases.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK048252-21
Application #
8787101
Study Section
Special Emphasis Panel (ZRG1-GGG-T (02))
Program Officer
Leschek, Ellen W
Project Start
1993-12-01
Project End
2017-12-31
Budget Start
2015-01-01
Budget End
2015-12-31
Support Year
21
Fiscal Year
2015
Total Cost
$369,057
Indirect Cost
$120,940

  Institution

Name
Oregon Health and Science University
Department
Genetics
Type
Schools of Medicine
DUNS #
096997515
City
Portland
State
OR
Country
United States
Zip Code
97239

  Publications

Paulk, Nicole K; Pekrun, Katja; Zhu, Erhua et al. (2018) Bioengineered AAV Capsids with Combined High Human Liver Transduction In Vivo and Unique Humoral Seroreactivity. Mol Ther 26:289-303
Nygaard, Sean; Barzel, Adi; Haft, Annelise et al. (2016) A universal system to select gene-modified hepatocytes in vivo. Sci Transl Med 8:342ra79
Hickey, Raymond D; Mao, Shennen A; Glorioso, Jaime et al. (2014) Fumarylacetoacetate hydrolase deficient pigs are a novel large animal model of metabolic liver disease. Stem Cell Res 13:144-53
Yin, Hao; Xue, Wen; Chen, Sidi et al. (2014) Genome editing with Cas9 in adult mice corrects a disease mutation and phenotype. Nat Biotechnol 32:551-3
Harding, Cary O; Winn, Shelley R; Gibson, K Michael et al. (2014) Pharmacologic inhibition of L-tyrosine degradation ameliorates cerebral dopamine deficiency in murine phenylketonuria (PKU). J Inherit Metab Dis 37:735-43
Lisowski, Leszek; Dane, Allison P; Chu, Kirk et al. (2014) Selection and evaluation of clinically relevant AAV variants in a xenograft liver model. Nature 506:382-6
Dorrell, Craig; Tarlow, Branden; Wang, Yuhan et al. (2014) The organoid-initiating cells in mouse pancreas and liver are phenotypically and functionally similar. Stem Cell Res 13:275-83
Gramignoli, Roberto; Tahan, Veysel; Dorko, Kenneth et al. (2013) New potential cell source for hepatocyte transplantation: discarded livers from metabolic disease liver transplants. Stem Cell Res 11:563-73
Grompe, Markus; Strom, Stephen (2013) Mice with human livers. Gastroenterology 145:1209-14
Taylor, A M; Preston, A J; Paulk, N K et al. (2012) Ochronosis in a murine model of alkaptonuria is synonymous to that in the human condition. Osteoarthritis Cartilage 20:880-6

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