Genetic and Epidemiologic Analyses of an Outbreak of Pneumocystis jirovecii Pneumonia Among Kidney Transplant Recipients in the United States

Author:

Azar Marwan M1ORCID,Cohen Elizabeth2,Ma Liang3,Cissé Ousmane H3,Gan Geliang4,Deng Yanhong4,Belfield Kristen5,Asch William25,Grant Matthew1,Gleeson Shana1,Koff Alan6,Gaston David C7,Topal Jeffrey1,Curran Shelly3,Kulkarni Sanjay28,Kovacs Joseph A3,Malinis Maricar18

Affiliation:

1. Department of Internal Medicine, Section of Infectious Diseases, Yale School of Medicine, New Haven, Connecticut,USA

2. Kidney Transplantation Program, Yale-New Haven Hospital, New Haven, Connecticut, USA

3. Critical Care Medicine Department, NIH Clinical Center, Bethesda, Maryland, USA

4. Yale Center for Analytical Sciences, Yale School of Public Health, New Haven, Connecticut, USA

5. Department of Internal Medicine, Section of Nephrology, Yale School of Medicine, New Haven, Connecticut, USA

6. Department of Internal Medicine, Section of Infectious Diseases, UC Davis School of Medicine, Sacramento, California, USA

7. Department of Pathology, Division of Medical Microbiology, Johns Hopkins School of Medicine, Baltimore, Maryland, USA

8. Department of Surgery, Yale School of Medicine, New Haven, Connecticut, USA

Abstract

Abstract Background Pneumocystis jirovecii is an opportunistic fungus that causes Pneumocystis pneumonia (PCP) in immunocompromised hosts. Over an 11-month period, we observed a rise in cases of PCP among kidney-transplant recipients (KTR), prompting an outbreak investigation. Methods Clinical and epidemiologic data were collected for KTR diagnosed with PCP between July 2019 and May 2020. Pneumocystis strain typing was performed using restriction fragment length polymorphism analyses and multilocus sequence typing in combination with next-generation sequencing. A transmission map was drawn, and a case-control analysis was performed to determine risk factors associated with PCP. Results Nineteen cases of PCP in KTR were diagnosed at a median of 79 months post-transplantation; 8 received monthly belatacept infusions. Baseline characteristics were similar for KTR on belatacept versus other regimens; the number of clinic visits was numerically higher for the belatacept group during the study period (median 7.5 vs 3). Molecular typing of respiratory specimens from 9 patients revealed coinfection with up to 7 P. jirovecii strains per patient. A transmission map suggested multiple clusters of interhuman transmission. In a case-control univariate analysis, belatacept, lower absolute lymphocyte count, non-White race, and more transplant clinic visits were associated with an increased risk of PCP. In multivariate and prediction power estimate analyses, frequent clinic visits was the strongest risk factor for PCP. Conclusions Increased clinic exposure appeared to facilitate multiple clusters of nosocomial PCP transmission among KTR. Belatacept was a risk factor for PCP, possibly by increasing clinic exposure through the need for frequent visits for monthly infusions.

Funder

National Institute of Health Clinical Center

Publisher

Oxford University Press (OUP)

Subject

Infectious Diseases,Microbiology (medical)

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