Brief Communication: Fatal Human Metapneumovirus Infection in Stem-Cell Transplant Recipients

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	Englund, J. A.

	Corey, L.

ARTICLE

Brief Communication: Fatal Human Metapneumovirus Infection in Stem-Cell Transplant Recipients

Janet A. Englund, MD; Michael Boeckh, MD; Jane Kuypers, PhD; W. Garrett Nichols, MD, MS; Robert C. Hackman, MD; Rhoda A. Morrow, PhD; David N. Fredricks, MD; and Lawrence Corey, MD

7 March 2006 | Volume 144 Issue 5 | Pages 344-349

Background: Human metapneumovirus (hMPV), a recently discoveredrespiratory virus, is associated with clinical disease in youngand elderly persons.

Objective: To determine the importance of hMPV in hematopoieticstem-cell transplant recipients.

Design: Retrospective survey of patients with consecutive residualbronchoalveolar lavage (BAL) samples.

Setting: Referral cancer center.

Patients: Hematopoietic stem-cell transplant recipients whounderwent BAL because of lower respiratory tract disease.

Measurements: Bronchoalveolar lavage specimens were assayedby quantitative real-time polymerase chain reaction methods.

Results: Human metapneumovirus was detected in BAL specimensfrom 5 of 163 patients (3.0%). Persistent viral infection wasnoted in 3 patients with several samples, and hMPV was detectedin 1 of 2 lung specimens tested. Infected patients became symptomaticwithin the first 40 days after transplantation. Initial symptomsincluded fever, cough, nasal congestion, and sore throat. Clinicalfindings included respiratory failure, pulmonary hemorrhage,and culture-negative septic shock. Four of 5 patients died withacute respiratory failure.

Limitations: This retrospective study did not evaluate asymptomaticpatients or those with mild disease.

Conclusion: Human metapneumovirus infection in the lower respiratorytract is associated with respiratory failure in immunocompromisedadults who were previously considered to have "idiopathic pneumonia."The infection may result in fulminant respiratory decompensationand shock after transplantation.

Editors' Notes

Context

Human metapneumovirus (hMPV) is a newly discoveredrespiratory virus.

Contribution

This study from a cancerreferral center retrospectively examined bronchoalveolar lavagesamples collected from 1995 to 1999 from hematopoietic celltransplant recipients with new or changing pulmonary infiltrates.The authors cultured hMPV in 5 of 163 symptomatic patients whowere thought to have had the idiopathic pneumonia syndrome.Clinical findings included fever, cough, nasal congestion, respiratoryfailure, pulmonary hemorrhage, and culture-negative sepsis.Four of the patients died.

Cautions

All patients had moderateto severe symptoms.

Implications

Human metapneumovirus maycause respiratory failure in immunocompromised adults.

—TheEditors

Author and Article Information

From the Children's Hospital and Regional Medical Center, University of Washington, and Fred Hutchinson Cancer Research Center, Seattle, Washington.

The paper was presented in part at the American Society of Hematology46th Annual Meeting, San Diego, California, 4–7 December2004.

Note: Drs. Englund and Boeckh contributed equally to the manuscript.

Acknowledgments: The authors acknowledge the immunohistochemicalstudies in lung tissue performed by Dr. Thijs Kuiken, ErasmusUniversity. They thank Kristen White for specimen processingand Nancy Wright for laboratory assistance with PCR testing.

Grant Support: In part by National Institutes of Health (grantsCA 18029, CA 15704, and PO1 AI 30731), the Fred Hutchinson CancerResearch Center (support grant P30 CA015704), and Adult LeukemiaResearch Center (grant P01 CA18029).

Potential Financial Conflicts of Interest: Consultancies: J.A.Englund (MedImmune Inc., Wyeth Vaccines); Grants received: J.A.Englund (MedImmune Inc.), R.A. Morrow (GlaxoSmithKline); Grantspending: J.A. Englund (National Institutes of Health).

Requests for Single Reprints: Janet A. Englund, MD, Children'sHospital and Regional Medical Center, 4800 Sand Point Way NE,Mail Stop W-8851, Seattle, WA 98105; e-mail, janet.englund{at}seattlechildrens.org.

Current Author Addresses: Dr. Englund: Children's Hospital andRegional Medical Center, 4800 Sand Point Way NE, Mail Stop W-8851,Seattle, WA 98105.

Drs. Boeckh, Fredricks, and Corey: Program in Infectious Diseases,D3-100, Fred Hutchinson Cancer Research Center, 1100 FairviewAvenue North, P.O. Box 19024, Seattle, WA 98109-1024.

Dr. Kuypers: Department of Laboratory Medicine, University ofWashington Clinical Virology Laboratory, Children's Hospitaland Regional Medical Center, 4800 Sand Point Way NE, Mailstop8G-3, Seattle, WA 98105.

Dr. Nichols: 5 Moore Drive, 17.1354B, Research Triangle Park,NC 27709.

Dr. Hackman: Department of Pathology, Fred Hutchinson CancerResearch Center, 1100 Fairview Avenue North, P.O. Box 19024,Seattle, WA 98109-1024.

Dr. Morrow: Department of Laboratory Medicine, University ofWashington Clinical Virology Laboratory, Children's Hospitaland Regional Medical Center, 4800 Sand Point Way NE, Mail StopG 815, Seattle, WA 98105.

Author Contributions: Conception and design: J.A. Englund, M.Boeckh, W.G. Nichols, L. Corey.

Analysis and interpretation of the data: J.A. Englund, M. Boeckh,J. Kuypers, W.G. Nichols, R.C. Hackman, R.A. Morrow, D.N. Fredricks,L. Corey.

Drafting of the article: J.A. Englund, M. Boeckh, W.G. Nichols,R.C. Hackman, R.A. Morrow, L. Corey.

Critical revision of the article for important intellectualcontent: J.A. Englund, M. Boeckh, J. Kuypers, W.G. Nichols,L. Corey.

Final approval of the article: J.A. Englund, M. Boeckh, W.G.Nichols, R.A. Morrow, D.N. Fredricks, L. Corey.

Provision of study materials or patients: J.A. Englund, M. Boeckh,R.C. Hackman, L. Corey.

Obtaining of funding: M. Boeckh, L. Corey.

Administrative, technical, or logistic support: R.A. Morrow,L. Corey.

Collection and assembly of data: J.A. Englund, M. Boeckh, W.G.Nichols, R.C. Hackman, R.A. Morrow, D.N. Fredricks.

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