Nosocomial malaria and saline flush.An investigation of malaria in a US patient without recent travel established Plasmodium falciparum molecular genotype identity in 2 patients who shared a hospital room. P. falciparum can be transmitted in a hospital environment from patient to patient by blood inoculum inoculum /in·oc·u·lum/ (-ok´u-lum) pl. inoc´ula material used in inoculation. in·oc·u·lum n. pl. if standard precautions are breached. ********** Almost all of the 1,400 cases of malaria reported each year in the United States are acquired by mosquito bite during travel in malaria-endemic areas (1). However, mosquito transmission in the United States accounts for a few cases each year (2). Nosocomial nosocomial /noso·co·mi·al/ (nos?o-ko´me-il) pertaining to or originating in a hospital. nos·o·co·mi·al adj. 1. Of or relating to a hospital. 2. malaria represents person-to-person transmission of parasite-infected erythrocytes through blood transfusion, needlestick injury, improper use of blood glucometers, multidose heparin vials, organ transplantation, contaminated catheters that deliver contrast medium, or rarely, open wounds (3-6). Nosocomial transmission of malaria secondary to inpatient nursing practices has never been reported in the United States. We report nosocomial transmission of Plasmodium falciparum, confirmed by molecular genotyping, by improper use of saline flush syringes in a tertiary care hospital in the United States. The Study Abdominal pain, emesis emesis /em·e·sis/ (em´e-sis) vomiting. em·e·sis n. pl. em·e·ses The act or process of vomiting. Emesis The medical term for vomiting. , and a high fever developed in patient 1, a 9-year-old Gambian boy with sickle cell disease sickle cell disease or sickle cell anemia, inherited disorder of the blood in which the oxygen-carrying hemoglobin pigment in erythrocytes (red blood cells) is abnormal. residing in the United States, during the flight home after a month in the Gambia; he had taken no malaria prophylaxis drugs. After diagnosis of P. falciparum malaria fal·cip·a·rum malaria n. Malaria caused by Plasmodium falciparum and characterized by severe malarial paroxysms that recur about every 48 hours and often by acute cerebral, renal, or gastrointestinal manifestations. with 4% parasitemia parasitemia /par·a·si·te·mia/ (par?ah-si-te´me-ah) the presence of parasites, especially malarial forms, in the blood. par·a·si·te·mi·a n. The presence of parasites in the blood. and transfer to unit A of a tertiary care hospital, he responded well to antimalarial antimalarial /an·ti·ma·lar·i·al/ (-mah-lar´e-al) therapeutically effective against malaria, or an agent with this quality. an·ti·ma·lar·i·al adj. Preventing or relieving the symptoms of malaria. therapy and was discharged 2 days later. Seven days before patient 1's admission, patient 2, a 14-year-old girl, with severe developmental delay, was admitted to unit A for placement of a surgical feeding tube. Patients 1 and 2 shared a unit A semiprivate sem·i·pri·vate adj. Shared with usually one to three other hospital patients: a semiprivate room. Adj. 1. room for [approximately equal to] 24 hours. Patient 1 received a continuous quinidine gluconate infusion through a peripheral intravenous line. Chart review and interviews indicated that neither patient had glucose monitoring by glucometer, blood transfusions, common infusions such as contrast material, or a needle-stick injury report, all events that have been previously implicated in nosocomial malaria. Medicine doses given and blood samples drawn were documented with a separation time >50 minutes. A week after discharge and 17 days after sharing the semiprivate room, patient 2 was admitted to another hospital (3-day stay), and a viral illness was diagnosed after all cultures were negative for pathogens. Persistent fever and pancytopenia pancytopenia /pan·cy·to·pe·nia/ (-sit-ah-pe´ne-ah) abnormal depression of all the cellular elements of the blood. pan·cy·to·pe·ni·a n. developed and resulted in her readmission readmission Managed care The admission of a Pt to a health care facility for a condition–eg, stroke, MI, GI bleeding, hip fracture, cancer surgery, shortly after discharge. See nth admission. Cf Admission, Discharge. to unit A of the tertitary care hospital, now 23 days after sharing the room with patient 1. Patient 2 was febrile and pale, with no notable change in her baseline neurologic state. The leukocyte count was 1,890 cells/[mm.sup.3], hematocrit was 35.2%, platelets were 47,000/[mm.sup.3], and total bilirubin was 1.5 mg/dL. Despite administration of antimicrobial drugs for presumed microbial sepsis, the following conditions developed over the next 72 hours: persistent spiking fevers; loose, nonbloody stools; splenomegaly splenomegaly /sple·no·meg·a·ly/ (-meg´ah-le) enlargement of the spleen. congestive splenomegaly Banti's disease; splenomegaly secondary to portal hypertension. ; abdominal distension; and bilateral lower extremity edema. Formal review of her peripheral blood smear by the hematology consultation service showed intraerythrocytic ring forms indicative of P. falciparum malaria, with 12% parasitemia and [approximately equal to] 200 gametocytes/[mm.sup.3]. After 3 blood transfusions and quinidine gluconate and doxycycline therapy, the patient was discharged on hospital day 14, with a stable hematocrit, persistent gametocytemia, and splenomegaly. Initial and follow up tests on patient 2 were negative for viral blood-borne pathogens. The patient lives with her parents in the Baltimore-Washington area [approximately equal to] 12 miles from the nearest international airport. She had no history of recent travel to any areas that are endemic for malaria. No locally acquired cases of malaria had been reported in the regional area. This prompted an investigation to look for a nosocomial route of transmission. Approval for the study was obtained from Johns Hopkins University Johns Hopkins University, mainly at Baltimore, Md. Johns Hopkins in 1867 had a group of his associates incorporated as the trustees of a university and a hospital, endowing each with $3.5 million. Daniel C. Two potential sources of nosocomial transmission in unit A were identified: 1) heparin syringes, which were filled from multidose vials, and 2) factory preloaded 10-mL saline flushes, of which up to 3 mL was used per flush for intravenous lines not in use. Hospital policy had strict guidelines for using multidose devices and did not allow reusing single use devices. However, interviews of 7 nurses, including those who cared for the 2 patients, showed that 2 nurses admitted reusing saline flushes on the same patient, and 4 nurses had observed saline flushes being reused in unit A. Reusing multidose heparin vials was not documented. To determine whether used saline flush syringes that were visibly clear contained blood, we tested saline from 8 used syringes and 2 unused controls. The contents of only 1 used saline flush syringe visibly contained blood. After the contents were centrifuged to concentrate erythrocytes, blood was found in 4 of 8 of the used syringes (Figure 1) by using matrix-assisted laser desorption Desorption A process in which atomic and molecular species residing on the surface of a solid leave the surface and enter the surrounding gas or vacuum. ionization/time-of-flight mass spectrometry (7). No blood was found in the unused syringes. [FIGURE 1 OMITTED] Polymerase chain reaction polymerase chain reaction (pŏl`ĭmərās') (PCR), laboratory process in which a particular DNA segment from a mixture of DNA chains is rapidly replicated, producing a large, readily analyzed sample of a piece of DNA; the process is (PCR PCR polymerase chain reaction. PCR abbr. polymerase chain reaction Polymerase chain reaction (PCR) ) amplification of P. falciparum genomic DNA, isolated with DNAzol (Invitrogen, Carlsbad, CA, USA), was successful from the archived Giemsa blood films from both patients and 2 other patients (not related in time or travel history) infected with P. falciparum malaria seen at our institution in the past year. Figure 2 shows that the PCR product restriction digests for the polymorphic P. falciparum merozoite merozoite /mero·zo·ite/ (mer?o-zo´it) one of the organisms formed by multiple fission (schizogony) of a sporozoite within the body of the host. mer·o·zo·ite n. protein 2 (Pfmsp2) (8) and the P. falciparum chloroquine chloroquine /chlo·ro·quine/ (klor´o-kwin) an antiamebic and anti-inflammatory used in the treatment of malaria, giardiasis, extraintestinal amebiasis, lupus erythematosus, and rheumatoid arthritis; used also as the hydrochloride and resistance transporter (Pfcrt) (9) gene fragments were identical for patients 1 and 2. This identity was also confirmed by sequence analysis. [FIGURE 2 OMITTED] We also examined 4 P. falciparum microsatellite See miniaturized satellite. alleles (TA81, PFPK, C13M30, C4M8) at independent chromosomal loci by a fluorescent-tagged heminested PCR amplification (10). Patients 1 and 2 had identical Plasmodium plasmodium, name for a stage in the life cycle of a slime mold. Also, Plasmodium is the name given to the genus of the protozoan parasite that causes malaria. microsatellite lengths at all 4 loci; each of the positive controls was different as shown in Figure 2, the online Appendix Figure (available at http://www.cdc.gov/ncidod/ EID/volllno07/05-0092_appG.htm), and the Table. With the simplistic sim·plism n. The tendency to oversimplify an issue or a problem by ignoring complexities or complications. [French simplisme, from simple, simple, from Old French; see simple assumption of [greater than or equal to] 10 alleles at each microsatellite loci and Pfmsp2, the chance occurrence of identity is <1:100,000. By using the AmpFLSTR Profiler kit (Applied Biosystems, Foster City, CA, USA), subsequent forensic analysis of the human genomic DNA from leukocytes in the same isolated P. falciparum DNA DNA: see nucleic acid. DNA or deoxyribonucleic acid One of two types of nucleic acid (the other is RNA); a complex organic compound found in all living cells and many viruses. It is the chemical substance of genes. samples from the blood films demonstrated the sex difference between patients 1 and 2. The analysis also demonstrated the differences at 9 human microsatellite loci, which indicated that cross-contamination during processing was not a likely source for the similarities detected. Conclusions Natural transmission of malaria between patients 1 and 2 by a mosquito is not possible within 24 hours; the maturation cycle from ingestion of viable gametocytes in a blood meal to infective sporozoite sporozoite /spo·ro·zo·ite/ (-zo´it) the motile, infective stage of certain protozoa that results from sporogony. spo·ro·zo·ite n. stage in the mosquito salivary glands is 8-35 days (11). Direct mechanical transmission of parasitized blood by an arthropod arthropod Any member of the largest phylum, Arthropoda, in the animal kingdom. Arthropoda consists of more than one million known invertebrate species in four subphyla: Uniramia (five classes, including insects), Chelicerata (three classes, including arachnids and horseshoe vector is a theoretical possibility, but no such transmission has ever been reported, and the female Anopheles Anopheles: see mosquito. mosquito does not regurgitate re·gur·gi·tate v. 1. To rush or surge back. 2. To cause to pour back, especially to cast up partially digested food. re·gur blood upon refeeding. Another remote possibility, luggage malaria, is the introduction of an already infectious mosquito from the Gambia brought into unit A through patient l's luggage (12). If this were the case, a different parasitic genotype would be expected in patients 1 and 2 because the wild mosquito that infected patient 1, from 1 to 2 weeks before onset of symptoms, would have died 2-6 days after delivering the infective bite. Likewise, an asymptomatic traveling companion of patient 1 would have a distinct parasite genotype. In this report, epidemiologic investigation excluded many nosocomial routes of transmission. Potential sources not excluded were multidose heparin vials and saline flush syringes. However, identifying reuse of saline flush syringes in the unit and detecting blood in clear, used saline flush syringes suggested that this was the most likely source. Finally, molecular identity of P. falciparum isolated from patients 1 and 2, as assessed by restriction fragment length polymorphism restriction fragment length polymorphism n. Abbr. RFLP Intraspecies variations in the length of DNA fragments generated by the action of restriction enzymes and caused by mutations that alter the sites at which these enzymes act, changing of Pfmsp2, and forensic microsatellite analysis of P. falciparum genotypes confirmed that contaminated fluid from patient 1 was the source of the infection in patient 2. Together, these data strongly suggest that apparently clear solution in a used saline flush syringe containing infected P. falciparum erythrocytes, was reused on a neighboring patient, leading to nosocomial transmission of malaria. Saline flush vials and bags have been implicated in nosocomial transmission of hepatitis B and microbes, respectively (13,14). Theoretically, a single infected erythrocyte is able to transmit malaria by inoculation. Patient 1 had almost 200 million infected erythrocytes per milliliter of blood based on parasitemia level. Based on our data, apparently clear saline can contain [approximately equal to] 1 million erythrocytes per milliliter. Therefore a single microliter microliter /mi·cro·li·ter/ (µL) (mi´kro-le?ter) one millionth (10-6) of a liter. mi·cro·li·ter n. A unit of volume equal to one-millionth (10-6) of a liter. of patient 1's blood diluted into 5 mL of saline would be almost 40,000 infected erythrocytes per milliliter of an apparently clear solution. Our report illustrates that nosocomial transmission can occur in a tertiary care setting in the United States, despite healthcare workers' access to gloves, disposable needles, intravenous devices, and flushes. The common perception that flushing practices are not associated with the aspiration of minute amounts of blood contributed to this occurrence of nosocomial malaria. Our institution, like many others, has used such episodes to facilitate change and refocus on patient safety. The interventions initiated specifically included retraining of pediatric pediatric /pe·di·at·ric/ (pe?de-at´rik) pertaining to the health of children. pe·di·at·ric adj. Of or relating to pediatrics. staff about 1) no reuse of single use saline flushes, 2) transmission of bloodborne pathogens with an emphasis on nonviral pathogens, and 3) removal of multidose vials, including those with heparin, from pediatric units. Warnings about the potential risks of reusing saline flush syringes have been incorporated into institution-wide safety training. Ongoing rigorous review of healthcare practices and strict adherence to body and fluid precautions are essential for minimizing patient exposure to highly infectious pathogens, even in resource-rich settings. Table. Plasmodium falciparum microsatellite lengths in number of base pairs Patient TA81 PFPK C13M30 C4M8 1 114 178 97 132 2 114 178 97 132 3 111 196 115 138 4 126 178 97 154 HB3 126 190 89 151 Acknowledgments We thank Lirong Shi, Karen Mackie, and the pediatric intensive care unit and hospital epidemiology and infection control staff who assisted in this investigation. We also thank Stephen Dumler for his continued encouragement and support. The AB-Mass Spectrometry Facility at the Johns Hopkins School of Medicine is funded by National Center for Research Resources The National Center for Research Resources or NCRR, is a United States government agency. NCRR provides funding to laboratory scientists and researchers for facilities and tools in the goal of curing and treating diseases. Shared-Instrument Grant 1S10-RR14702. NCCR NCCR National Council of Chain Restaurants NCCR National Coalition for Cancer Research NCCR National Center for Competence in Research (Lausanne, Switzerland) NCCR Network-Controlled Cell Reselection (GSM) grant GPDGCRC RR0052 supported the culture of P. falciparum for control DNA. References (1.) Filler S, Causer LM, Newman RD, Barber AM, Roberts JM, MacArthur J, et al. Malaria surveillance--United States, 2001. MMWR MMWR Morbidity & Mortality Weekly Report Epidemiology A news bulletin published by the CDC, which provides epidemiologic data–eg, statistics on the incidence of AIDS, rabies, rubella, STDs and other communicable diseases, causes of mortality–eg, Surveill Summ. 2003;52:1-14. (2.) Pastor A, Neely J, Goodfriend D, Marr J, Jenkins S, Woolard D, et al. Local transmission of Plasmodium vivax malaria--Virginia, 2002. MMWR Morb Mortal Wkly Rep. 2002;51:921-3. (3.) Lettau LA. Nosocomial transmission and infection control aspects of parasitic and ectoparasitic diseases. Part II. Blood and tissue parasites, infect Control Hosp Epidemiol. 1991;12:111-21. (4.) Arafat R, Long S, Perry M, Marsh S, Wilson M, Avashia S, et al. Probable transfusion-transmitted malaria--Houston, Texas, 2003. MMWR Morb Mortal Wkly Rep. 2003;52:1075-6. (5.) Alweis RL, DiRosario K, Conidi G, Kain KC, Olans R, Tully JL. Serial nosocomial transmission of Plasmodium falciparum malaria from patient to nurse to patient. Infect Control Hosp Epidemiol. 2004;25:55-9. (6.) Abulrahi HA, Bohlega EA, Fontaine RE, al-Seghayer S, Mal-Ruwais AA. Plasmodium falciparum malaria transmitted in hospital through heparin locks. Lancet. 1997;349:23-5. (7.) Jackson PE, Scholl PF, Groopman JD. Mass spectrometry for genotyping: an emerging tool for molecular medicine. Mol Med Today. 2000;6:271-6. (8.) Felger I, Smith T, Edoh D, Kitua A, Alonso P, Tanner M, et al. Multiple Plasmodium falciparum infections in Tanzanian infants. Trans R Soc Trop Med Hyg. 1999;93 Suppl 1:29-34. (9.) Djimde A, Doumbo OK, Cortese JF, Kayentao K, Doumbo S, Diourte Y, et al. A molecular marker for chloroquine-resistant falciparum malaria. N Engl J Med. 2001;344:257-63. (10.) Anderson TJ, Su XZ, Bockarie M, Lagog M, Day KP. Twelve microsatellite markers for characterization of Plasmodium falciparum from finger-prick blood samples. Parasitology. 1999;119 (Pt 2): 113-25. (11.) Do Rosario VE, Vaughan JA, Coleman RE. Analysis of the sporogonic development of Plasmodium falciparum and Plasmodium berghei in anopheline anopheline pertaining to the anopheles genus of mosquitoes. mosquitoes. Parassitologia. 1989;31:101-11. (12.) Guillet P, Germain MC, Giacomini T, Chandre F, Akogbeto M, Faye O, et al. Origin and prevention of airport malaria in France. Trop Med Int Health. 1998;3:700-5. (13.) Oren I, Hershow RC, Ben-Porath E, Krivoy N, Goldstein N, Rishpon S, et al. A common-source outbreak of fulminant hepatitis B in a hospital. Ann Intern Med. 1989;110:691-8. (14.) Chodoff A, Pettis AM, Schoonmaker D, Shelly MA. Polymicrobial gram-negative bacteremia associated with saline solution flush used with a needleless intravenous system. Am J Infect Control. 1995;23:357-63. Sanjay K. Jain, * Deborah Persaud, * Trish M. Perl, * Margaret A. Pass, * Kathleen M. Murphy, * John M. Pisciotta, * Peter F. Scholl, * James F. Casella, * and David J. Sullivan * * Johns Hopkins University, Baltimore, Maryland, USA Dr. Jain is a senior clinical and research fellow in pediatric infectious diseases at Johns Hopkins University. His research interests include tropical diseases and central nervous system tuberculosis. Address for correspondence: David J. Sullivan, W. Harry Feinstone Department of Molecular Microbiology and Immunology, Bloomberg School of Public Health, Johns Hopkins University, 615 North Wolfe St, E5628, Baltimore, MD 21287, USA; fax; 410-955-0105; email: dsulliva@jhsph.edu Use of trade names is for identification only and does not imply endorsement by the Public Health Service or by the U.S. Department of Health and Human Services Noun 1. Department of Health and Human Services - the United States federal department that administers all federal programs dealing with health and welfare; created in 1979 Health and Human Services, HHS . |
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