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Preferential targeting of disseminated liver tumors using a recombinant adeno-associated viral vector.


ABSTRACT: A novel selectively targeting gene delivery approach has been developed for advanced hepatocellular carcinoma (HCC), a leading cause of cancer mortality whose prognosis remains poor. We combine the strong liver tropism of serotype-8 capsid-pseudotyped adeno-associated viral vectors (AAV8) with a liver-specific promoter (HLP) and microRNA-122a (miR-122a)-mediated posttranscriptional regulation. Systemic administration of our AAV8 construct resulted in preferential transduction of the liver and encouragingly of HCC at heterotopic sites, a finding that could be exploited to target disseminated disease. Tumor selectivity was enhanced by inclusion of miR-122a-binding sequences (ssAAV8-HLP-TK-122aT4) in the expression cassette, resulting in abrogation of transgene expression in normal murine liver but not in HCC. Systemic administration of our tumor-selective vector encoding herpes simplex virus-thymidine kinase (TK) suicide gene resulted in a sevenfold reduction in HCC growth in a syngeneic murine model without toxicity. In summary, we have developed a systemically deliverable gene transfer approach that enables high-level expression of therapeutic genes in HCC but not normal tissues, thus improving the prospects of safe and effective treatment for advanced HCC.

SUBMITTER: Della Peruta M 

PROVIDER: S-EPMC4326028 | biostudies-literature | 2015 Feb

REPOSITORIES: biostudies-literature

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Preferential targeting of disseminated liver tumors using a recombinant adeno-associated viral vector.

Della Peruta Marco M   Badar Adam A   Rosales Cecilia C   Chokshi Shilpa S   Kia Azadeh A   Nathwani Devhrut D   Galante Eva E   Yan Ran R   Arstad Erik E   Davidoff Andrew M AM   Williams Roger R   Lythgoe Mark F MF   Nathwani Amit C AC  

Human gene therapy 20150201 2


A novel selectively targeting gene delivery approach has been developed for advanced hepatocellular carcinoma (HCC), a leading cause of cancer mortality whose prognosis remains poor. We combine the strong liver tropism of serotype-8 capsid-pseudotyped adeno-associated viral vectors (AAV8) with a liver-specific promoter (HLP) and microRNA-122a (miR-122a)-mediated posttranscriptional regulation. Systemic administration of our AAV8 construct resulted in preferential transduction of the liver and en  ...[more]

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