Clinical Utility of Plasma Microbial Cell-Free DNA Sequencing Among Immunocompromised Patients With Pneumonia

Author:

Madut Deng B1ORCID,Chemaly Roy F2,Dadwal Sanjeet S3,Hill Joshua A45ORCID,Lee Yeon Joo67,Haidar Ghady8,Luk Alfred9ORCID,Drelick Alexander710,Chin-Hong Peter V11,Benamu Esther12,Khawaja Fareed2ORCID,Nanayakkara Deepa3ORCID,Papanicolaou Genovefa A67,Small Catherine Butkus710,Fung Monica11ORCID,Barron Michelle12,Davis Thomas13,McClain Micah T114,Maziarz Eileen K1,Bedoya Armando D1,Gilstrap Daniel L1,Todd Jamie L114,Barkauskas Christina E1,Heldman Madeleine R1,Bigelow Robert14,Leimberger Jeffrey D14,Tsalik Ephraim L11516,Wolf Olivia14,Mughar Mona17,Lau Constance17,Noll Nicholas17,Hollemon Desiree17,Duttagupta Radha17,Lupu Daniel S17,Bercovici Sivan17,Perkins Bradley A17,Blauwkamp Timothy A17,Fowler Vance G114,Holland Thomas L114,Bergin Stephen P114

Affiliation:

1. Duke University School of Medicine , Durham, North Carolina , USA

2. The University of Texas MD Anderson Cancer Center , Houston, Texas , USA

3. City of Hope National Medical Center , Duarte California , USA

4. Fred Hutchinson Cancer Center , Seattle, Washington , USA

5. University of Washington School of Medicine , Seattle, Washington , USA

6. Memorial Sloan Kettering Cancer Center , New York, New York , USA

7. Weill Cornell Medicine , New York, New York , USA

8. University of Pittsburgh Medical Center , Pittsburgh, Pennsylvania , USA

9. Tulane University School of Medicine , New Orleans, Louisiana , USA

10. New York-Presbyterian Hospital , New York, New York , USA

11. University of California San Francisco , San Francisco, California , USA

12. University of Colorado , Aurora, Colorado , USA

13. Indiana University School of Medicine , Indianapolis Indiana , USA

14. Duke Clinical Research Institute , Durham, North Carolina , USA

15. Durham Veterans Affairs Health Care System , Durham, North Carolina , USA

16. Danaher Diagnostics , Washington, DC , USA

17. Karius Inc. , Redwood City, California , USA

Abstract

Abstract Background Plasma microbial cell-free DNA (mcfDNA) sequencing can establish the etiology of multiple infectious syndromes by identifying microbial DNA in plasma. However, data are needed to define the clinical scenarios where this tool offers the highest clinical benefit. Methods We conducted a prospective multicenter observational study that evaluated the impact of plasma mcfDNA sequencing compared with usual care testing among adults with hematologic malignancies. This is a secondary analysis of an expanded cohort that evaluated the clinical utility of plasma mcfDNA sequencing across prespecified and adjudicated outcomes. We examined the percentage of participants for whom plasma mcfDNA sequencing identified a probable cause of pneumonia or clinically relevant nonpneumonia infection. We then assessed potential changes in antimicrobial therapy based on plasma mcfDNA sequencing results and the potential for early mcfDNA testing to avoid bronchoscopy and its associated adverse events. Results Of 223 participants, at least 1 microbial detection by plasma mcfDNA sequencing was adjudicated as a probable cause of pneumonia in 57 (25.6%) and a clinically relevant nonpneumonia infection in 88 (39.5%). A probable cause of pneumonia was exclusively identified by plasma mcfDNA sequencing in 23 (10.3%) participants. Antimicrobial therapy would have changed for 41 (18.4%) participants had plasma mcfDNA results been available in real time. Among the 57 participants with a probable cause of pneumonia identified by plasma mcfDNA sequencing, bronchoscopy identified no additional probable cause of pneumonia in 52 (91.2%). Conclusions Plasma mcfDNA sequencing could improve management of both pneumonia and other concurrent infections in immunocompromised patients with suspected pneumonia.

Funder

Karius Inc.

Publisher

Oxford University Press (OUP)

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