Adenovirus-mediated blockade of tumor necrosis factor in mice protects against endotoxic shock yet impairs pulmonary host defense

Jay K. Kolls; Dinghua Lei; Steve Nelson; Warren R. Summer; Stanley Greenberg; Bruce Beutler

doi:10.1093/infdis/171.3.570

Adenovirus-mediated blockade of tumor necrosis factor in mice protects against endotoxic shock yet impairs pulmonary host defense

Jay K. Kolls, Dinghua Lei, Steve Nelson, Warren R. Summer, Stanley Greenberg, Bruce Beutler

Research output: Contribution to journal › Article › peer-review

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Abstract

A replication-deficient recombinant adenovirus encoding a chimeric protein capable of binding tumor necrosis factor (TNF) and lymphotoxin was given to mice. Administration of this virus (l09 pfu intravenously) yielded high levels of the recombinant protein in plasma and afforded significant protection to a lethal challenge with lipopolysaccharide with or without D-galactosamine. However, this protein inhibitor was readily detectable in the lung and was associated with decreased neutrophil recruitment and bacterial killing after intratracheal LPS or Pseudomonas aeruginosa, respectively. These data reflect the dual role of many proinflammatory cytokines. This model of TNF inhibition is similar to the homozygous SS-kDa TNF receptor deletion; thus, adenovirus-mediated gene transfer of cytokine inhibitors in vivo is a useful tool to abrogate the function of single or multiple cytokines for investigational or therapeutic purposes.

Original language	English (US)
Pages (from-to)	570-575
Number of pages	6
Journal	Journal of Infectious Diseases
Volume	171
Issue number	3
DOIs	https://doi.org/10.1093/infdis/171.3.570
State	Published - Mar 1995

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Medicine(all)

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title = "Adenovirus-mediated blockade of tumor necrosis factor in mice protects against endotoxic shock yet impairs pulmonary host defense",

abstract = "A replication-deficient recombinant adenovirus encoding a chimeric protein capable of binding tumor necrosis factor (TNF) and lymphotoxin was given to mice. Administration of this virus (l09 pfu intravenously) yielded high levels of the recombinant protein in plasma and afforded significant protection to a lethal challenge with lipopolysaccharide with or without D-galactosamine. However, this protein inhibitor was readily detectable in the lung and was associated with decreased neutrophil recruitment and bacterial killing after intratracheal LPS or Pseudomonas aeruginosa, respectively. These data reflect the dual role of many proinflammatory cytokines. This model of TNF inhibition is similar to the homozygous SS-kDa TNF receptor deletion; thus, adenovirus-mediated gene transfer of cytokine inhibitors in vivo is a useful tool to abrogate the function of single or multiple cytokines for investigational or therapeutic purposes.",

author = "Kolls, {Jay K.} and Dinghua Lei and Steve Nelson and Summer, {Warren R.} and Stanley Greenberg and Bruce Beutler",

note = "Funding Information: Received 3 August 1994; revised 19 October 1994. Grant support: Parker 8. Francis Pulmonary Research Fellowship (J.K.K.); National Institutes of Health (AA-077 10 to S.N .. AA-09816 to S.G.. and DK-42582 to 8.8.). All studies were carried out in accordance with requirements of the LSU Institutional Animal Care and Use Committee. Reprints or correspondence: Dr. Jay K. Kolls, LSU Section of Pulmonary/Critical Care Medicine. LSU Section of Pediatric Pulmonology. 190 I Perdido si., Room 3205. New Orleans. LA 70 I 12.",

year = "1995",

month = mar,

doi = "10.1093/infdis/171.3.570",

language = "English (US)",

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AU - Kolls, Jay K.

AU - Lei, Dinghua

AU - Nelson, Steve

AU - Summer, Warren R.

AU - Greenberg, Stanley

AU - Beutler, Bruce

N1 - Funding Information: Received 3 August 1994; revised 19 October 1994. Grant support: Parker 8. Francis Pulmonary Research Fellowship (J.K.K.); National Institutes of Health (AA-077 10 to S.N .. AA-09816 to S.G.. and DK-42582 to 8.8.). All studies were carried out in accordance with requirements of the LSU Institutional Animal Care and Use Committee. Reprints or correspondence: Dr. Jay K. Kolls, LSU Section of Pulmonary/Critical Care Medicine. LSU Section of Pediatric Pulmonology. 190 I Perdido si., Room 3205. New Orleans. LA 70 I 12.

PY - 1995/3

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AB - A replication-deficient recombinant adenovirus encoding a chimeric protein capable of binding tumor necrosis factor (TNF) and lymphotoxin was given to mice. Administration of this virus (l09 pfu intravenously) yielded high levels of the recombinant protein in plasma and afforded significant protection to a lethal challenge with lipopolysaccharide with or without D-galactosamine. However, this protein inhibitor was readily detectable in the lung and was associated with decreased neutrophil recruitment and bacterial killing after intratracheal LPS or Pseudomonas aeruginosa, respectively. These data reflect the dual role of many proinflammatory cytokines. This model of TNF inhibition is similar to the homozygous SS-kDa TNF receptor deletion; thus, adenovirus-mediated gene transfer of cytokine inhibitors in vivo is a useful tool to abrogate the function of single or multiple cytokines for investigational or therapeutic purposes.

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Adenovirus-mediated blockade of tumor necrosis factor in mice protects against endotoxic shock yet impairs pulmonary host defense

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