Abstract

Since the first report of human infection with Pneumocystis carinii in 1942, cases of pneumonia due to this opportunistic pathogen have become increasingly common. Animal studies and clinical observations show that a significant depletion or dysfunction of T helper lymphocytes predisposes to clinical disease. Individuals with damaged T helper cells secondary to malignancies (eg, Hodgkin's lymphoma), drugs (eg, cyclosporine, steroids), or certain infections (eg, human immunodeficiency virus) are at particular risk. Serological studies suggest that disease is most often secondary to the reactivation of an asymptomatic infection, usually acquired during childhood. Increasing shortness of breath, a nonproductive cough and hypoxia often preceded by several weeks of lethargy, fever and weight loss are the classical features of P carinii pneumonia in acquired immune deficiency syndrome. Bronchoalveolar lavage is usually the optimal diagnostic test. Immunofluorescent staining on liquified sputum induced by nebulized saline appears to be a promising and noninvasive test. Early empiric therapy with trimethoprim-sulphamethoxazole (trimethoprim 5 mg-sulphamethoxazole 25 mg/kg/day every 6 h) or intravenous pentamidine (4 mg/kg/day) for 21 days is usually effective, but infection is not eradicated, and clinical disease is likely to recur. Prophylaxis using aerosolized pentamidine reduces the risk of pulmonary disease but can predispose to extrapulmonary infection. Improved in vitro and in vivo models of human pneumocystis infection would significantly increase understanding of the molecular biology of the organism, the pathogenesis of disease, and the optimal therapeutic regimens.

Highlights

  • Chagas [3] originally described P carinii in the lungs of guinea pigs in 1909

  • OVER THE PAST DECADE THE INCIDENCE OF Pneumocystis carinii pneumonia has increased dramatically [1,2]. This changing epidemiology has principally been secondary to the epidemic of human immunodeficiency virus (HIV) infection causing the acquired immune deficiency syndrome (AIDS)

  • By the late 1960s occasional cases of P carinii pneumonia were seen in adults who were immunocompromised from either immunosuppressive therapy or an underlying disease (l)

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Summary

INFECTION AND IMMUNIN SYMPOSIUM

Since the first report of human infection with Pneumocystis carinii in 1942, cases of pneumonia due to this opportunistic pathogen have become increasingly common. Improved in vitro and in vivo models of human pneumocystis infection would significantly increase understanding of the molecular biology of the organism, the pathogenesis of disease. RESUME: Depuis qu'on a rapporte le premier cas d'infection humaine a Pneumocystis carinii en 1942, les cas de pneumonie due a cet agent pathogene opportuniste se sont multiplies. Alberta Correspondence and reprints: Dr MJ Gill. OVER THE PAST DECADE THE INCIDENCE OF Pneumocystis carinii pneumonia has increased dramatically [1,2] This changing epidemiology has principally been secondary to the epidemic of human immunodeficiency virus (HIV) infection causing the acquired immune deficiency syndrome (AIDS). In this review of P carinii infection the authors will outline the current understanding of the host factors related to disease, the biology of the organism, the pathogenesis of infection, the clinical features of disease, and the recent developments in both diagnosis and therapy

BACKGROUND
HOST SUSCEPTIBILITY
CLINICAL FEATURES
LABORATORY INVESTIGATIONS
PROGNOSTIC MARKERS
EXTRAPULMONARY DISEASE
Findings
SUMMARY
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