Lung injury in vivax malaria: pathophysiological evidence for pulmonary vascular sequestration and posttreatment alveolar-capillary inflammation

Nicholas M Anstey; Tjandra Handojo; Michael C F Pain; Enny Kenangalem; Emiliana Tjitra; Ric N Price; Graeme P Maguire

doi:10.1086/510756

Lung injury in vivax malaria: pathophysiological evidence for pulmonary vascular sequestration and posttreatment alveolar-capillary inflammation

J Infect Dis. 2007 Feb 15;195(4):589-96. doi: 10.1086/510756. Epub 2007 Jan 4.

Authors

Nicholas M Anstey¹, Tjandra Handojo, Michael C F Pain, Enny Kenangalem, Emiliana Tjitra, Ric N Price, Graeme P Maguire

Affiliation

¹ International Health Program, Infectious Diseases Division, Menzies School of Health Research and Charles Darwin University, Darwin, NT 0811, Australia. anstey@menzies.edu.au

PMID: 17230420
PMCID: PMC2532499
DOI: 10.1086/510756

Abstract

Background: The mechanisms underlying lung injury in vivax malaria are not well understood. Inflammatory responses to Plasmodium falciparum and P. vivax, to our knowledge, have not previously been compared at an organ level.

Methods: Respiratory symptoms and physiological aspects were measured longitudinally in Indonesian adults with uncomplicated vivax (n=50) and falciparum (n=50) malaria. Normal values were derived from 109 control subjects. Gas transfer was partitioned into its alveolar-capillary membrane (D(M)) and pulmonary capillary vascular (V(C)) components, to characterize the site and timing of impaired gas transfer.

Results: Mean baseline V(C) volume was significantly reduced in vivax and falciparum malaria, improving with treatment in each species. Baseline D(M) function was not impaired in either species. The progressive deterioration in D(M) function after treatment was statistically significant in vivax malaria but not in uncomplicated falciparum malaria. Oxygen saturation deteriorated after treatment in vivax but improved in falciparum malaria.

Conclusions: The baseline reduction in V(C) volume but not in D(M) function suggests encroachment on V(C) volume by parasitized erythrocytes and suggests that P. vivax-infected erythrocytes may sequester within the pulmonary microvasculature. Progressive alveolar-capillary dysfunction after treatment of vivax malaria is consistent with a greater inflammatory response to a given parasite burden in P. vivax relative to that in P. falciparum.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adolescent
Adult
Animals
Blood Gas Analysis
Capillaries / parasitology*
Erythrocytes / parasitology
Female
Humans
Indonesia
Longitudinal Studies
Lung / blood supply
Lung / parasitology
Lung / pathology
Lung / physiopathology*
Malaria, Falciparum / drug therapy
Malaria, Falciparum / parasitology
Malaria, Falciparum / pathology
Malaria, Falciparum / physiopathology*
Malaria, Vivax / drug therapy
Malaria, Vivax / parasitology
Malaria, Vivax / pathology
Malaria, Vivax / physiopathology*
Male
Middle Aged
Oxygen / analysis
Parasitemia
Plasmodium vivax / physiology
Pulmonary Alveoli / pathology
Pulmonary Gas Exchange
Respiratory Function Tests
Respiratory Mechanics*

Substances

Oxygen

Abstract

Publication types

MeSH terms

Substances

Grants and funding