Abstract

An ideal cancer therapeutic agent would specifically target malignant cells to kill these cells while avoiding normal tissues. Oncolytic viruses are viruses developed to selectively kill tumor cells by infecting, replicating, and ultimately killing these cells. These agents have the appeal of being """"""""self-amplifying"""""""" drugs, because each infected tumor cell produces 10,000 more viruses to amplify the number of killed tumor cells. Oncolytic viruses have shown promise in preclinical and clinical trials where they have proved most useful when applied by direct intratumoral injection. While this may be useful for debulking tumors, this approach cannot address distant metastases. Adenoviruses have been engineered to achieve cancer specificity by taking advantage of specific traits of certain cancer cell types or by taking advantage of molecular changes intrinsic to oncogenesis. While these viruses have higher cancer specificity, loss of 90% of the intravenously injected dose to liver reduces the amount of virus available to kill tumor metastases. This loss also produces dose-limiting and sometimes lethal liver damage. In addition to these pharmacologic problems, another significant hurdle to clinical translation is the presence or high levels of neutralizing antibodies against Ad5 in patients. These antibodies deplete most of an injected dose markedly reducing efficacy. Given these problems, this project will apply clinically-relevant interventions to attempt to improve both the pharmacology and immunogenicity of adenoviral oncolytics for systemic cancer therapy. This project will detarget oncolytic viruses from the liver and shield them from the immune system by genetic and chemical engineering. The Molecular Medicine Program at Mayo Clinic has previously translated other oncolytic viruses into the clinic for cancer applications. If this project is successful, it will therefore lay the groundwork for translating these adenovirus oncolytics for the treatment of cancer patients at Mayo Clinic and other sites.

Public Health Relevance

Successful pursuit of this project will enable more specific and less dangerous oncolytic adenoviruses for cancer therapy. This project will work to improve the ability of these cancer killing viruses to be used for systemic therapy to find and kill distant tumor sites in metastatic disease. This work will lay the foundation for future testing in humans.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA136945-02
Application #
8035883
Study Section
Developmental Therapeutics Study Section (DT)
Program Officer
Muszynski, Karen
Project Start
2010-03-01
Project End
2014-12-31
Budget Start
2011-01-01
Budget End
2011-12-31
Support Year
2
Fiscal Year
2011
Total Cost
$304,127
Indirect Cost

  Institution

Name
Mayo Clinic, Rochester
Department
Type
DUNS #
006471700
City
Rochester
State
MN
Country
United States
Zip Code
55905

  Publications

Dorta-Estremera, Stephanie; Nehete, Pramod N; Yang, Guojun et al. (2017) Minimally invasive monitoring of CD4 T cells at multiple mucosal tissues after intranasal vaccination in rhesus macaques. PLoS One 12:e0188807
Crosby, Catherine M; Barry, Michael A (2017) Transgene Expression and Host Cell Responses to Replication-Defective, Single-Cycle, and Replication-Competent Adenovirus Vectors. Genes (Basel) 8:
Nguyen, Tien V; Heller, Greg J; Barry, Mary E et al. (2016) Evaluation of polymer shielding for adenovirus serotype 6 (Ad6) for systemic virotherapy against human prostate cancers. Mol Ther Oncolytics 3:
Crosby, Catherine M; Nehete, Pramod; Sastry, K Jagannadha et al. (2015) Amplified and persistent immune responses generated by single-cycle replicating adenovirus vaccines. J Virol 89:669-75
Turner, Mallory A; Middha, Sumit; Hofherr, Sean E et al. (2015) Comparison of the Life Cycles of Genetically Distant Species C and Species D Human Adenoviruses Ad6 and Ad26 in Human Cells. J Virol 89:12401-17
Crosby, Catherine M; Barry, Michael A (2014) IIIa deleted adenovirus as a single-cycle genome replicating vector. Virology 462-463:158-65
Khare, Reeti; Hillestad, Matthew L; Xu, Zhili et al. (2013) Circulating antibodies and macrophages as modulators of adenovirus pharmacology. J Virol 87:3678-86
Khare, Reeti; Reddy, Vijay S; Nemerow, Glen R et al. (2012) Identification of adenovirus serotype 5 hexon regions that interact with scavenger receptors. J Virol 86:2293-301
Hillestad, Matthew L; Guenzel, Adam J; Nath, Karl A et al. (2012) A vector-host system to fingerprint virus tropism. Hum Gene Ther 23:1116-26
Barry, Michael A; May, Shannon; Weaver, Eric A (2012) Imaging luciferase-expressing viruses. Methods Mol Biol 797:79-87

Showing the most recent 10 out of 15 publications