In Vivo Detection of c-MET Expression in a Rat Hepatocarcinogenesis Model Using Molecularly Targeted Magnetic Resonance Imaging

The multifunctional growth factor scatter factor/hepatocyte growth factor and its tyrosine kinase receptor, c-MET, have been implicated in the genesis and malignant progression of numerous human malignancies, including hepatocellular carcinomas. The incidence of hepatocellular carcinomas in the Unit...

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Main Authors: Rheal A. Towner, Nataliya Smith, Yasvir A. Tesiram, Andrew Abbott, Debbie Saunders, Rebecca Blindauer, Oana Herlea, Robert Silasi-Mansat, Florea Lupu
Format: Article
Language:English
Published: Hindawi - SAGE Publishing 2007-01-01
Series:Molecular Imaging
Online Access:https://doi.org/10.2310/7290.2006.00031
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spelling doaj-7a359e16acc6497694a0e4300c215b992021-04-02T11:42:29ZengHindawi - SAGE PublishingMolecular Imaging1536-01212007-01-01610.2310/7290.2006.0003110.2310_7290.2006.00031In Vivo Detection of c-MET Expression in a Rat Hepatocarcinogenesis Model Using Molecularly Targeted Magnetic Resonance ImagingRheal A. TownerNataliya SmithYasvir A. TesiramAndrew AbbottDebbie SaundersRebecca BlindauerOana HerleaRobert Silasi-MansatFlorea LupuThe multifunctional growth factor scatter factor/hepatocyte growth factor and its tyrosine kinase receptor, c-MET, have been implicated in the genesis and malignant progression of numerous human malignancies, including hepatocellular carcinomas. The incidence of hepatocellular carcinomas in the United States has increased noticeably over the past two decades and is listed as the fifth major cancer in men worldwide. In this study, we used a choline-deficient l -amino acid (CDAA)-defined rat hepatocarcinogenesis model to visualize increased in vivo expression of the c-MET antigen in neoplastic lesion formation with the use of a super paramagnetic iron oxide (SPIO)–anti-c-MET molecularly targeted magnetic resonance imaging (MRI) contrast agent. SPIO–anti-c-MET was used for the first time to detect overexpression of c-MET in neoplastic nodules and tumors within the livers of CDAA-treated rats, as determined by a decrease in MRI signal intensity and a decrease in regional T 2 values. Specificity for the binding of the molecularly targeted anti-c-MET contrast agent was determined using rat hepatoma (H4-II-E-C3) cell cultures and immunofluorescence microscopic imaging of the targeting agents within neoplastic liver tissue 1 to 2 hours following intravenous administration of SPIO–anti-c-MET and MRI investigation. This method has the ability to visualize in vivo the overexpression of c-MET at early developmental stages of tumor formation.https://doi.org/10.2310/7290.2006.00031
collection DOAJ
language English
format Article
sources DOAJ
author Rheal A. Towner
Nataliya Smith
Yasvir A. Tesiram
Andrew Abbott
Debbie Saunders
Rebecca Blindauer
Oana Herlea
Robert Silasi-Mansat
Florea Lupu
spellingShingle Rheal A. Towner
Nataliya Smith
Yasvir A. Tesiram
Andrew Abbott
Debbie Saunders
Rebecca Blindauer
Oana Herlea
Robert Silasi-Mansat
Florea Lupu
In Vivo Detection of c-MET Expression in a Rat Hepatocarcinogenesis Model Using Molecularly Targeted Magnetic Resonance Imaging
Molecular Imaging
author_facet Rheal A. Towner
Nataliya Smith
Yasvir A. Tesiram
Andrew Abbott
Debbie Saunders
Rebecca Blindauer
Oana Herlea
Robert Silasi-Mansat
Florea Lupu
author_sort Rheal A. Towner
title In Vivo Detection of c-MET Expression in a Rat Hepatocarcinogenesis Model Using Molecularly Targeted Magnetic Resonance Imaging
title_short In Vivo Detection of c-MET Expression in a Rat Hepatocarcinogenesis Model Using Molecularly Targeted Magnetic Resonance Imaging
title_full In Vivo Detection of c-MET Expression in a Rat Hepatocarcinogenesis Model Using Molecularly Targeted Magnetic Resonance Imaging
title_fullStr In Vivo Detection of c-MET Expression in a Rat Hepatocarcinogenesis Model Using Molecularly Targeted Magnetic Resonance Imaging
title_full_unstemmed In Vivo Detection of c-MET Expression in a Rat Hepatocarcinogenesis Model Using Molecularly Targeted Magnetic Resonance Imaging
title_sort in vivo detection of c-met expression in a rat hepatocarcinogenesis model using molecularly targeted magnetic resonance imaging
publisher Hindawi - SAGE Publishing
series Molecular Imaging
issn 1536-0121
publishDate 2007-01-01
description The multifunctional growth factor scatter factor/hepatocyte growth factor and its tyrosine kinase receptor, c-MET, have been implicated in the genesis and malignant progression of numerous human malignancies, including hepatocellular carcinomas. The incidence of hepatocellular carcinomas in the United States has increased noticeably over the past two decades and is listed as the fifth major cancer in men worldwide. In this study, we used a choline-deficient l -amino acid (CDAA)-defined rat hepatocarcinogenesis model to visualize increased in vivo expression of the c-MET antigen in neoplastic lesion formation with the use of a super paramagnetic iron oxide (SPIO)–anti-c-MET molecularly targeted magnetic resonance imaging (MRI) contrast agent. SPIO–anti-c-MET was used for the first time to detect overexpression of c-MET in neoplastic nodules and tumors within the livers of CDAA-treated rats, as determined by a decrease in MRI signal intensity and a decrease in regional T 2 values. Specificity for the binding of the molecularly targeted anti-c-MET contrast agent was determined using rat hepatoma (H4-II-E-C3) cell cultures and immunofluorescence microscopic imaging of the targeting agents within neoplastic liver tissue 1 to 2 hours following intravenous administration of SPIO–anti-c-MET and MRI investigation. This method has the ability to visualize in vivo the overexpression of c-MET at early developmental stages of tumor formation.
url https://doi.org/10.2310/7290.2006.00031
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