Antimicrobial Prophylaxis in Bone Marrow Transplantation

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	Momin, F.

	Chandrasekar, P. H.

REVIEW

Antimicrobial Prophylaxis in Bone Marrow Transplantation

Feroze Momin and Pranatharthi H. Chandrasekar

1 August 1995 | Volume 123 Issue 3 | Pages 205-215

Objective: To review the efficacy of antimicrobial prophylaxisin bone marrow transplantation.

Data Sources: English-language articles identified througha MEDLINE search (1975 to 1994) and through the bibliographiesof selected articles.

Study Selection: Articles on the use of antimicrobial agentsfor the prevention of infections in bone marrow transplant recipientsand neutropenic patients with cancer.

Data Synthesis: Use of quinolones reduces the incidence ofgram-negative bacillary infections but increases the frequencyof infections caused by streptococci and staphylococci beforemarrow engraftment. Death associated with ${alpha}$ -hemolytic streptococcalbacteremia is of concern and may justify the use of penicillinfor prophylaxis. Conflicting data exist regarding prophylaxiswith vancomycin. Although ganciclovir has diminished the incidenceof infection and disease caused by cytomegalovirus in seropositiverecipients, drug-induced myelotoxicity, emergence of resistantvirus, and cost are major concerns. High-dose acyclovir maysuppress reactivation of cytomegalovirus. Acyclovir preventsherpes simplex virus infection, but its prolonged use to preventreactivation of varicella-zoster virus is not cost-effectiveand remains controversial. Fluconazole prevents colonizationand infection with Candida species other than C. krusei andTorulopsis glabrata before marrow engraftment. Elevation ofcyclosporine concentrations because of interaction between azolesand cyclosporine requires close monitoring of plasma drug levels.Optimal chemoprophylaxis is not available against aspergillusor fungal infections that develop after engraftment. Trimethoprim-sulfamethoxazoledecreases the incidence of Pneumocystis carinii infection and"late" bacterial infections in recipients of allogeneic transplantswho have chronic graft-versus-host disease.

Conclusion: Available antimicrobial agents can prevent commonbacterial, viral, and "early" fungal infections. However, thefew studies that address antimicrobial prophylaxis in bone marrowtransplantation have not always shown a survival benefit. Toxicityand cost-effectiveness of prophylactic strategies should becritically evaluated.

Author and Article Information

From Wayne State University, Detroit, Michigan.
Requests for Reprints: Pranatharthi H. Chandrasekar, MD, Hematology-Oncology/Infectious Diseases Liaison Unit, Division of Infectious Diseases, Wayne State University School of Medicine, 4160 John R, Suite 2140, Detroit, MI 48201.
Acknowledgment: The authors thank Ms. Eileen Surma for expert secretarial assistance.

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