Minimal hepatic toxicity of Onyx-015: spatial restriction of coxsackie-adenoviral receptor in normal liver

We administered an adenoviral vector, Onyx-015, into the hepatic artery of patients with metastatic colorectal cancer involving the liver. Thirty-five patients enrolled in this multi-institutional phase I/II trial received up to eight arterial infusions of up to 2 × 10(12) viral particles. Hepatic t...

Descripción completa

Detalles Bibliográficos
Autores principales: Au, T, Thorne, S, Korn, W M, Sze, D, Kirn, D, Reid, T R
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group US 2006
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7091580/
https://www.ncbi.nlm.nih.gov/pubmed/17139321
http://dx.doi.org/10.1038/sj.cgt.7700988
_version_ 1783510034256232448
author Au, T
Thorne, S
Korn, W M
Sze, D
Kirn, D
Reid, T R
author_facet Au, T
Thorne, S
Korn, W M
Sze, D
Kirn, D
Reid, T R
author_sort Au, T
collection PubMed
description We administered an adenoviral vector, Onyx-015, into the hepatic artery of patients with metastatic colorectal cancer involving the liver. Thirty-five patients enrolled in this multi-institutional phase I/II trial received up to eight arterial infusions of up to 2 × 10(12) viral particles. Hepatic toxicity was the primary dose-limiting toxicity observed in preclinical models. However, nearly 200 infusions of this adenoviral vector were administered directly into the hepatic artery without significant toxicity. Therefore, we undertook this analysis to determine the impact of repeated adenoviral exposure on hepatic function. Seventeen patients were treated at our institution, providing a detailed data set on the changes in hepatic function following repeated exposure to adenovirus. No changes in hepatic function occurred with the first treatment of Onyx-015 among these patients. Transient increases in transaminase levels occurred in one patient starting with the second infusion and transient increases in bilirubin was observed in two patients starting with the fifth treatment. These changes occurred too early to be explained by viral-mediated lysis of hepatocytes. In addition, viremia was observed starting 3–5 days after the viral infusion in half of the patient, but was not associated with hepatic toxicity. To further understand the basis for the minimal hepatic toxicity of adenoviral vectors, we evaluated the replication of adenovirus in primary hepatocytes and tumor cells in culture and the expression of the coxsackie-adenoviral receptor (CAR) in normal liver and colon cancer metastatic to the liver. We found that adenovirus replicates poorly in primary hepatocytes but replicates efficiently in tumors including tumors derived from hepatocytes. In addition, we found that CAR is localized at junctions between hepatocytes and is inaccessible to hepatic blood flow. CAR is not expressed on tumor vasculature but is expressed on tumor cells. Spatial restriction of CAR to the intercellular space in normal liver and diminished replication of adenovirus in hepatocytes may explain the minimal toxicity observed following repeated hepatic artery infusions with Onyx-015.
format Online
Article
Text
id pubmed-7091580
institution National Center for Biotechnology Information
language English
publishDate 2006
publisher Nature Publishing Group US
record_format MEDLINE/PubMed
spelling pubmed-70915802020-03-24 Minimal hepatic toxicity of Onyx-015: spatial restriction of coxsackie-adenoviral receptor in normal liver Au, T Thorne, S Korn, W M Sze, D Kirn, D Reid, T R Cancer Gene Ther Article We administered an adenoviral vector, Onyx-015, into the hepatic artery of patients with metastatic colorectal cancer involving the liver. Thirty-five patients enrolled in this multi-institutional phase I/II trial received up to eight arterial infusions of up to 2 × 10(12) viral particles. Hepatic toxicity was the primary dose-limiting toxicity observed in preclinical models. However, nearly 200 infusions of this adenoviral vector were administered directly into the hepatic artery without significant toxicity. Therefore, we undertook this analysis to determine the impact of repeated adenoviral exposure on hepatic function. Seventeen patients were treated at our institution, providing a detailed data set on the changes in hepatic function following repeated exposure to adenovirus. No changes in hepatic function occurred with the first treatment of Onyx-015 among these patients. Transient increases in transaminase levels occurred in one patient starting with the second infusion and transient increases in bilirubin was observed in two patients starting with the fifth treatment. These changes occurred too early to be explained by viral-mediated lysis of hepatocytes. In addition, viremia was observed starting 3–5 days after the viral infusion in half of the patient, but was not associated with hepatic toxicity. To further understand the basis for the minimal hepatic toxicity of adenoviral vectors, we evaluated the replication of adenovirus in primary hepatocytes and tumor cells in culture and the expression of the coxsackie-adenoviral receptor (CAR) in normal liver and colon cancer metastatic to the liver. We found that adenovirus replicates poorly in primary hepatocytes but replicates efficiently in tumors including tumors derived from hepatocytes. In addition, we found that CAR is localized at junctions between hepatocytes and is inaccessible to hepatic blood flow. CAR is not expressed on tumor vasculature but is expressed on tumor cells. Spatial restriction of CAR to the intercellular space in normal liver and diminished replication of adenovirus in hepatocytes may explain the minimal toxicity observed following repeated hepatic artery infusions with Onyx-015. Nature Publishing Group US 2006-12-01 2007 /pmc/articles/PMC7091580/ /pubmed/17139321 http://dx.doi.org/10.1038/sj.cgt.7700988 Text en © Nature Publishing Group 2007 This article is made available via the PMC Open Access Subset for unrestricted research re-use and secondary analysis in any form or by any means with acknowledgement of the original source. These permissions are granted for the duration of the World Health Organization (WHO) declaration of COVID-19 as a global pandemic.
spellingShingle Article
Au, T
Thorne, S
Korn, W M
Sze, D
Kirn, D
Reid, T R
Minimal hepatic toxicity of Onyx-015: spatial restriction of coxsackie-adenoviral receptor in normal liver
title Minimal hepatic toxicity of Onyx-015: spatial restriction of coxsackie-adenoviral receptor in normal liver
title_full Minimal hepatic toxicity of Onyx-015: spatial restriction of coxsackie-adenoviral receptor in normal liver
title_fullStr Minimal hepatic toxicity of Onyx-015: spatial restriction of coxsackie-adenoviral receptor in normal liver
title_full_unstemmed Minimal hepatic toxicity of Onyx-015: spatial restriction of coxsackie-adenoviral receptor in normal liver
title_short Minimal hepatic toxicity of Onyx-015: spatial restriction of coxsackie-adenoviral receptor in normal liver
title_sort minimal hepatic toxicity of onyx-015: spatial restriction of coxsackie-adenoviral receptor in normal liver
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7091580/
https://www.ncbi.nlm.nih.gov/pubmed/17139321
http://dx.doi.org/10.1038/sj.cgt.7700988
work_keys_str_mv AT aut minimalhepatictoxicityofonyx015spatialrestrictionofcoxsackieadenoviralreceptorinnormalliver
AT thornes minimalhepatictoxicityofonyx015spatialrestrictionofcoxsackieadenoviralreceptorinnormalliver
AT kornwm minimalhepatictoxicityofonyx015spatialrestrictionofcoxsackieadenoviralreceptorinnormalliver
AT szed minimalhepatictoxicityofonyx015spatialrestrictionofcoxsackieadenoviralreceptorinnormalliver
AT kirnd minimalhepatictoxicityofonyx015spatialrestrictionofcoxsackieadenoviralreceptorinnormalliver
AT reidtr minimalhepatictoxicityofonyx015spatialrestrictionofcoxsackieadenoviralreceptorinnormalliver

Ejemplares similares