Literature DB >> 4430713

Increased sheep lung vascular permeability caused by pseudomonas bacteremia.

K L Brigham, W C Woolverton, L H Blake, N C Staub.   

Abstract

In awake sheep, we compared the responses of lung lymph flow and lymph and plasma protein concentrations to steady state elevations of pulmonary vascular pressures made by inflating a left atrial balloon with those after an intravenous infusion of 10(5)-10(10)Pseudomonas aeruginosa. Lymph flow increased when pressure was increased, but lymph-plasma protein concentration ratios always fell and lymph protein flow (lymph flow x lymph protein concentration) increased only slightly. After Pseudomonas, sheep had transient chills, fever, leukopenia, hypoxemia, increased pulmonary artery pressure and lymph flow and decreased left atrial pressure and lymph protein concentration, 3-5 h after Pseudomonas, when vascular pressures and lymph protein concentrations had returned to near base line, lymph flow increased further to 3-10 times base line and remained at a steady level for many hours. During this steady state period, lymph-plasma protein concentration ratios were similar to base line and lymph protein flow was higher than in the increased pressure studies. Two sheep died of pulmonary edema 7 and 9 h after Pseudomonas, but in 16 studies, five other sheep appeared well during the period of highest lymph flow and all variables returned to base line in 24-72 h. Six serial indicator dilution lung water studies in five sheep changed insignificantly from base line after Pseudomonas. Postmortem lung water was high in the two sheep dead of pulmonary edema and one other, but six sheep killed 1-6 h after Pseudomonas had normal lung water. Because of the clear difference between the effects of increased pressure and Pseudomonas on lymphplasma protein concentration ratios and lymph protein flow, we conclude that Pseudomonas causes a prolonged increase in lung vessel permeability to protein. Because we saw lung lymph flow as high as 10 times base line without pulmonary edema, we conclude that lung lymphatics are a sensitive high-capacity mechanism for removing excess filtered fluid. An equivalent pore model of sheep lung vessels suggests that the changes we saw after Pseudomonas could result from small changes in the structure of exchanging vessel walls.

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Year:  1974        PMID: 4430713      PMCID: PMC301619          DOI: 10.1172/JCI107819

Source DB:  PubMed          Journal:  J Clin Invest        ISSN: 0021-9738            Impact factor:   14.808


  31 in total

1.  Effect of elevated left atrial pressure and decreased plasma protein concentration on the development of pulmonary edema.

Authors:  A C GUYTON; A W LINDSEY
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2.  Pulmonary oedema in bacterial shock.

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3.  Pulmonary hypertension caused by minute amounts of endotoxin in calves.

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4.  Histamine and interstitial pulmonary edema in the dog.

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5.  Pulmonary edema as a result of endotoxemia.

Authors:  J D Snell; L H Ramsey
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6.  Interstitial fluid pressure changes in endotoxin shock.

Authors:  P Anas; W A Neely; J D Hardy
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7.  Increase in capillary filtration rate resulting from reduction in the intravascular calcium ion-concentration.

Authors:  G Nicolaysen
Journal:  Acta Physiol Scand       Date:  1971-04

8.  Pulmonary capillary pressure and filtration coefficient in the isolated perfused lung.

Authors:  K A Gaar; A E Taylor; L J Owens; A C Guyton
Journal:  Am J Physiol       Date:  1967-10

9.  On the mechanism of vascular leakage caused by histaminetype mediators. A microscopic study in vivo.

Authors:  G Majno; V Gilmore; M Leventhal
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Authors:  R D Body; J R Hill; P W Humphreys; I C Normand; E O Reynolds; L B Strang
Journal:  J Physiol       Date:  1969-05       Impact factor: 5.182

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7.  Pulmonary edema after aneurysm surgery is modified by mannitol.

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8.  Cecal ligation and puncture-induced murine sepsis does not cause lung injury.

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9.  Effects of asphyxia on lung fluid balance in baby lambs.

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10.  Pulmonary vascular effects of fat emulsion infusion in unanesthetized sheep. Prevention by indomethacin.

Authors:  C R McKeen; K L Brigham; R E Bowers; T R Harris
Journal:  J Clin Invest       Date:  1978-05       Impact factor: 14.808

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