EM Hadac scite author profile

EM Hadac

3Publications

47Citation Statements Received

20Citation Statements Given

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Mayo Clinic

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Pharmacokinetics of oncolytic measles virotherapy: eventual equilibrium between virus and tumor in an ovarian cancer xenograft model

Hadac

et al. 2006

Cancer Gene Ther

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Because of their ability to replicate, the dose-response relationships of oncolytic viruses cannot easily be predicted. To better understand the pharmacokinetics of virotherapy in relation to viral dose and schedule, we administered MV-CEA intraperitoneally in an orthotopic mouse model of ovarian cancer. MV-CEA is an attenuated oncolytic measles virus engineered to express soluble human carcinoembryonic antigen (CEA), and the virus is currently undergoing phase I clinical testing in patients with ovarian cancer. Plasma CEA levels correlate with numbers of virus-infected tumor cells at a given time, and were used as a surrogate to monitor the profiles of viral gene expression over time. The antineoplastic activity of single-or multiple-dose MV-CEA was apparent over a wide range of virus doses (10 3 -10 8 TCID 50 ), with little reduction in observed antitumor efficacy, even at the lowest tested dose. However, analysis of CEA profiles of treated mice was highly informative, illustrating the variability in virus kinetics at different dose levels. The highest doses of virus were associated with higher initial levels of tumor cell killing, but the final outcome of MV-CEA therapy at all dose levels was a partial equilibrium between virus and tumor, resulting in significant slowing of tumor growth and enhanced survival of the mice.

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B591 Infectious RNA: A Novel Therapeutic Modality for Myeloma

Russell¹,

Hadac²,

Kelly³

2009

Clinical Lymphoma and Myeloma

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B592 Retargeted Coxsackievirus A21 for Myeloma Therapy

Russell¹,

Kelly²,

Hadac³

et al. 2009

Clinical Lymphoma and Myeloma

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EM Hadac

Pharmacokinetics of oncolytic measles virotherapy: eventual equilibrium between virus and tumor in an ovarian cancer xenograft model

B591 Infectious RNA: A Novel Therapeutic Modality for Myeloma

B592 Retargeted Coxsackievirus A21 for Myeloma Therapy

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