MELIOIDOSIS: PATHOGENESIS AND IMMUNITY IN MICE AND HAMSTERS: I. STUDIES WITH STRAINS OF MALLEOMYCES PSEUDOMALLEI

doi:10.1084/jem.107.1.153

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The Journal of Experimental Medicine, Vol 107, 153-166, Copyright, 1958, by The Rockefeller Institute for Medical Research New York

ARTICLE

MELIOIDOSIS: PATHOGENESIS AND IMMUNITY IN MICE AND HAMSTERS : I. STUDIES WITH STRAINS OF MALLEOMYCES PSEUDOMALLEI

Arthur M. Dannenberg Jr. M.D.¹ and Eva M. Scott ¹

¹ From the Naval Medical Research Unit No. 1 and the Naval Biological Laboratory Department of Bacteriology, University of California, Berkeley

The pathogenesis of acute respiratory melioidosis mice andhamsters is described. Inhaled organisms giving rise to lesionsseemed to be first engulfed by the mononuclear alveolar phagocytes,but in less than 1 day polymorphonuclear cells made their appearance.In spite of this defense reaction, the bacteria continued tomultiply and their products caused focal necrosis. These focienlarged and gave rise to septicemia, toxemia, and eventuallydeath, which usually occurred in 3 to 10 days depending on thedose. Melioidosis, is, therefore, an acute septicotoxemic diseaseresembling plague and anthrax in this respect.

In hamsters thedisease process developed more rapidly than in mice and deathoccurred sooner. The course of the disease in hamsters was sometimescomplicated by intraglomerular deposits resembling "fibrinoid,"which were similar to those of the generalized Shwartzman phenomenon.This phenomenon may have been an indirect cause of both theperifocal hemorrhage and the extremely large number of bacteriain some of the hamster lesions.

When low infecting doses oforganisms were employed, mice, but not hamsters, developed achronic type of disease, lasting 2 to 8 weeks. This was characterizedby large abscesses in the spleen or lung, marked proliferationof mononuclear phagocytes and plasma cells, and increased immunityagainst reinfection (about 40-fold against respiratory challenge).

Whenmice and hamsters inhaled high infecting doses of organisms,a peracute disease resulted with death in 1 to 3 days. Increasednumbers of bacteria were observed in the lesions, and the histologicalchanges in the spleen resembled those following the intravenousinjection of Malleomyces pseudomallei toxin or the intramuscularinjection of large doses of cortisone. These changes were characterizedby a swelling of the phagocytes of the white pulp with nucleardebris.

The peracute, the acute, and the chronic forms of melioidosisin mice are similar to analogous clinical forms found in man.

Submitted on June 7, 1957

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