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Targeted Inflammation During Oncolytic Virus Therapy Severely Compromises Tumor Blood Flow
by
McGuire, Allison
, Falls, Theresa J
, Parato, Kelley A
, McCart, J Andrea
, Daneshmand, Manijeh
, Speth, Kelly
, Kirn, David
, Atkins, Harold
, Bell, John C
, Breitbach, Caroline J
, Paterson, Jennifer M
, Lemay, Chantal G
, Stojdl, David F
in
Animals
/ Apoptosis
/ Apoptosis - physiology
/ Blood Flow Velocity
/ Cancer
/ Cell Line, Tumor
/ Compromises
/ Fluorescent Antibody Technique
/ Gene therapy
/ Humans
/ Immunohistochemistry
/ In Situ Nick-End Labeling
/ In Vitro Techniques
/ Infections
/ Inflammation - genetics
/ Inflammation - pathology
/ Inflammation - therapy
/ Liver
/ Medical research
/ Mice
/ Mice, Inbred BALB C
/ Neoplasms - genetics
/ Neoplasms - pathology
/ Neoplasms - therapy
/ Neutrophils
/ Neutrophils - metabolism
/ Neutrophils - pathology
/ Oligonucleotide Array Sequence Analysis
/ Oncolytic Virotherapy - methods
/ Oncolytic Viruses - physiology
/ Research centers
/ Reverse Transcriptase Polymerase Chain Reaction
/ Tumors
/ Vesicular stomatitis Indiana virus - physiology
/ Viral infections
/ Virus Replication
/ Viruses
/ Xenograft Model Antitumor Assays
2007
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Targeted Inflammation During Oncolytic Virus Therapy Severely Compromises Tumor Blood Flow
by
McGuire, Allison
, Falls, Theresa J
, Parato, Kelley A
, McCart, J Andrea
, Daneshmand, Manijeh
, Speth, Kelly
, Kirn, David
, Atkins, Harold
, Bell, John C
, Breitbach, Caroline J
, Paterson, Jennifer M
, Lemay, Chantal G
, Stojdl, David F
in
Animals
/ Apoptosis
/ Apoptosis - physiology
/ Blood Flow Velocity
/ Cancer
/ Cell Line, Tumor
/ Compromises
/ Fluorescent Antibody Technique
/ Gene therapy
/ Humans
/ Immunohistochemistry
/ In Situ Nick-End Labeling
/ In Vitro Techniques
/ Infections
/ Inflammation - genetics
/ Inflammation - pathology
/ Inflammation - therapy
/ Liver
/ Medical research
/ Mice
/ Mice, Inbred BALB C
/ Neoplasms - genetics
/ Neoplasms - pathology
/ Neoplasms - therapy
/ Neutrophils
/ Neutrophils - metabolism
/ Neutrophils - pathology
/ Oligonucleotide Array Sequence Analysis
/ Oncolytic Virotherapy - methods
/ Oncolytic Viruses - physiology
/ Research centers
/ Reverse Transcriptase Polymerase Chain Reaction
/ Tumors
/ Vesicular stomatitis Indiana virus - physiology
/ Viral infections
/ Virus Replication
/ Viruses
/ Xenograft Model Antitumor Assays
2007
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Targeted Inflammation During Oncolytic Virus Therapy Severely Compromises Tumor Blood Flow
by
McGuire, Allison
, Falls, Theresa J
, Parato, Kelley A
, McCart, J Andrea
, Daneshmand, Manijeh
, Speth, Kelly
, Kirn, David
, Atkins, Harold
, Bell, John C
, Breitbach, Caroline J
, Paterson, Jennifer M
, Lemay, Chantal G
, Stojdl, David F
in
Animals
/ Apoptosis
/ Apoptosis - physiology
/ Blood Flow Velocity
/ Cancer
/ Cell Line, Tumor
/ Compromises
/ Fluorescent Antibody Technique
/ Gene therapy
/ Humans
/ Immunohistochemistry
/ In Situ Nick-End Labeling
/ In Vitro Techniques
/ Infections
/ Inflammation - genetics
/ Inflammation - pathology
/ Inflammation - therapy
/ Liver
/ Medical research
/ Mice
/ Mice, Inbred BALB C
/ Neoplasms - genetics
/ Neoplasms - pathology
/ Neoplasms - therapy
/ Neutrophils
/ Neutrophils - metabolism
/ Neutrophils - pathology
/ Oligonucleotide Array Sequence Analysis
/ Oncolytic Virotherapy - methods
/ Oncolytic Viruses - physiology
/ Research centers
/ Reverse Transcriptase Polymerase Chain Reaction
/ Tumors
/ Vesicular stomatitis Indiana virus - physiology
/ Viral infections
/ Virus Replication
/ Viruses
/ Xenograft Model Antitumor Assays
2007
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Targeted Inflammation During Oncolytic Virus Therapy Severely Compromises Tumor Blood Flow
Journal Article
Targeted Inflammation During Oncolytic Virus Therapy Severely Compromises Tumor Blood Flow
2007
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Overview
Oncolytic viruses (OVs) are selected or designed to eliminate malignancies by direct infection and lysis of cancer cells. In contrast to this concept of direct tumor lysis by viral infection, we observed that a significant portion of the in vivo tumor killing activity of two OVs, vesicular stomatitis virus (VSV) and vaccinia virus is caused by indirect killing of uninfected tumor cells. Shortly after administering the oncolytic virus we observed limited virus infection, coincident with a loss of blood flow to the interior of the tumor that correlated with induction of apoptosis in tumor cells. Transcript profiling of tumors showed that virus infection resulted in a dramatic transcriptional activation of pro-inflammatory genes including the neutrophil chemoattractants CXCL1 and CXCL5. Immunohistochemical examination of infected tumors revealed infiltration by neutrophils correlating with chemokine induction. Depletion of neutrophils in animals prior to VSV administration eliminated uninfected tumor cell apoptosis and permitted more extensive replication and spreading of the virus throughout the tumor. Taken all together, these results indicate that targeted recruitment of neutrophils to infected tumor beds enhances the killing of malignant cells. We propose that activation of inflammatory cells can be used for enhancing the effectiveness of oncolytic virus therapeutics, and that this approach should influence the planning of therapeutic doses.
Publisher
Elsevier Inc,Elsevier Limited
Subject
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