Natural History of Opportunistic Disease in an HIV-Infected Urban Clinical Cohort

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	Moore, R. D.

	Chaisson, R. E.

ARTICLE

Natural History of Opportunistic Disease in an HIV-Infected Urban Clinical Cohort

Richard D. Moore, MD, MHSc, and Richard E. Chaisson, MD

1 April 1996 | Volume 124 Issue 7 | Pages 633-642

Objective: To determine the effect of contemporary clinicalcare on the natural history of opportunistic disease in an urbanpopulation infected with the human immunodeficiency virus (HIV).

Setting: Urban university HIV clinic.

Design: Retrospective and prospective observational study.

Patients: 1246 HIV-infected patients with CD4⁺ counts of 300cells/mm³ or less.

Measurements: Incidence rates and Kaplan-Meier estimates ofthe probability of developing opportunistic disease with time,distribution of the CD4⁺ counts at which opportunistic diseasedevelops, survival after the development of opportunistic disease,and the association between preventive drug therapies and theoccurrence of opportunistic infection.

Results: The most common opportunistic disease was Candidaesophagitis, which had an incidence of 13.3 events per 100 person-yearsand a 3-year Kaplan-Meier probability of 0.30. Pneumocystiscarinii pneumonia, Mycobacterium avium complex bacteremia, cytomegalovirus,and the acquired immunodeficiency syndrome dementia complexoccurred at rates of 5 to 9 events per 100 person-years and3-year Kaplan-Meier probabilities of 0.15 to 0.22. Toxoplasmosis,cryptococcal meningitis, herpes zoster, the wasting syndrome,and Kaposi sarcoma occurred at rates of about 2 to 4 eventsper 100 person-years and with 3-year Kaplan-Meier probabilitiesof 0.05 to 0.10. Non-Hodgkin lymphoma, M. tuberculosis infection,progressive multifocal leukoencephalopathy, and cryptosporidiosiswere the least common disorders, with an incidence of about1 to 2 events per 100 person-years and a 3-year Kaplan-Meierprobability less than 0.05. Only the incidences of cryptococcalmeningitis, secondary P. carinii pneumonia, and herpes zosterdecreased (P < 0.05) between 1989-1992 and 1993-1995. Fluconazoleuse was associated with a decreased relative rate of 0.49 (P= 0.06) for cryptococcal meningitis and a decreased relativerate of 0.61 (P = 0.005) for esophageal candidiasis. Rifabutinuse was associated with a decreased relative rate of 0.37 (P= 0.002) for M. avium complex bacteremia, and trimethoprim-sulfamethoxazoleuse was associated with decreased relative rates of 0.33 (P= 0.02) for secondary P. carinii pneumonia and 0.55 (P = 0.08)for primary P. carinii pneumonia. Candidiasis, herpes zoster,and M. tuberculosis infection first occurred at a median CD4⁺count greater than 100 cells/mm³, but all other opportunisticdiseases first occurred at a median CD4⁺ count less than 50cells/mm³. Median survival after diagnosis varied from 35 daysfor non-Hodgkin lymphoma to 680 days for herpes zoster.

Conclusions: In the patients studied, the incidences of secondaryP. carinii pneumonia, cryptococcal meningitis, and herpes zosterhave declined in the past 5 years. The incidences of primaryP. carinii pneumonia and Kaposi sarcoma appear to be decliningcompared with historical estimates. However, although theseand other opportunistic diseases continue to be relatively frequentcomplications of HIV infection, they are first occurring atmore advanced immunosuppression than in the past. Continuedefforts are needed to develop effective strategies for preventingopportunistic disease in very advanced HIV infection.

Author and Article Information

From Johns Hopkins University School of Medicine, Baltimore, Maryland.
Acknowledgments: The authors thank Jeanne Keruly, Darrell Forney, Joel Gibson, Lisa-Marie Castro, Cathy Riggin, Shelia Kasey, and Kim Veney for technical support.
Grant Support: By grant RO1 HS07809 from the Agency for Health Care Policy and Research.
Requests for Reprints: Richard D. Moore, MD, Johns Hopkins University School of Medicine, 1830 East Monument Street, Room 8059, Baltimore, MD 21205.
Current Author Addresses: Dr. Moore: Johns Hopkins University School of Medicine, 1830 East Monument Street, Room 8059, Baltimore, MD 21205.

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