Blackwater fever in children, Burundi.Blackwater fever black·wa·ter fever n. A serious, often fatal complication of falciparum malaria, characterized by the passage of bloody, dark red, or black urine. blackwater fever see babesiosis. is characterized by acute intravascular intravascular /in·tra·vas·cu·lar/ (in?trah-vas´ku-lar) within a vessel. in·tra·vas·cu·lar adj. Within one or more blood vessels. hemolysis hemolysis (hĭmŏl`ĭsĭs), destruction of red blood cells in the bloodstream. Although new red blood cells, or erythrocytes, are continuously created and old ones destroyed, an excessive rate of destruction sometimes occurs. with hemoglobinuria hemoglobinuria /he·mo·glo·bin·uria/ (he?mo-glo?bi-nu´re-ah) free hemoglobin in the urine.hemoglobinu´ric march hemoglobinuria that seen after prolonged exercise. in patients with Plasmodium falciparum Plasmodium fal·cip·a·rum n. A protozoan that causes falciparum malaria. malaria. Its pathogenesis and management are still debated. Nine cases of this syndrome occurred in 2003 at Kiremba Hospital in Burundi in children receiving multiple quinine quinine (kwī`nīn', kwĭnēn`), white crystalline alkaloid with a bitter taste. Before the development of more effective synthetic drugs such as quinacrine, chloroquine, and primaquine, quinine was the specific agent in the treatment of treatments. ********** Blackwater fever (BWF BWF Badminton World Federation BWF British Woodworking Federation (London, UK) BWF Broadcast WAV Format BWF British Walking Federation BWF Babilonia Wilner Foundation (Manila, Philippines) ) is a clinical entity well known only in long-term residents in 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. falciparum-endemic areas who take quinine irregularly. This syndrome became less frequent when 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 was the drug of choice for malaria from 1950 until the 1990s (1). Glucose-6-phosphate dehydrogenase glucose-6-phosphate dehydrogenase /glu·cose-6-phos·phate de·hy·dro·gen·ase/ (G6PD) (-fos´fat de-hi´dro-jen-as) an enzyme of the pentose phosphate pathway which, with NADP+ as coenzyme, catalyzes the oxidation of glucose 6-phosphate to a (G6PD G6PD glucose-6-phosphate dehydrogenase. G6PD glucose-6-phosphate dehydrogenase. ) deficiency is also frequently associated with the syndrome; however, its role is not determinant, as BWF is frequently described in patients with normal erythrocyte erythrocyte (ĭrĭth`rəsīt'): see blood. erythrocyte or red blood cell or red blood corpuscle Blood cell that carries oxygen from the lungs to the body tissues. G6PD levels who are receiving quinine for severe malaria (2). Isolated cases have also been described with other antimalarials, such as halofantrine and mefloquine mefloquine /mef·lo·quine/ (mef´lo-kwin) an antimalarial effective against chloroquine-resistant strains of Plasmodium falciparum and P. vivax; used as the hydrochloride salt. , which belong to the amino-alcohol drug family (3 5). The pathogenesis of BWF thus remains unclear (4,6,7). Its management changed with the introduction of artemisinin Artemisinin (IPA: [artɛˈmɪsɪnən]) is a drug used to treat multi-drug resistant strains of falciparum malaria. derivates but is still debated. White and other researchers (2,8) state that parenteral parenteral /pa·ren·ter·al/ (pah-ren´ter-al) not through the alimentary canal, but rather by injection through some other route, as subcutaneous, intramuscular, etc. par·en·ter·al adj. 1. quinine can be stopped when artemisinin derivatives are available because they seem to be safe and well tolerated. Clinical features defining BWF are well established (2,9). The syndrome is characterized by severe intravascular hemolysis and anemia producing dark urine in patients with severe malaria. Abdominal pain, jaundice jaundice (jôn`dĭs, jän`–), abnormal condition in which the body fluids and tissues, particularly the skin and eyes, take on a yellowish color as a result of an excess of bilirubin. , hepatosplenomegaly, vomiting, and renal failure (especially in adults) have also been reported. As P. falciparum resistance to chloroquine developed, quinine was increasingly used in clinical practice for treating intermittent malaria infections. BWF seemed to reappear at the end of the 1990s, according to descriptions in several European clinics of imported diseases (3-5). It particularly affected European missionaries with years of previous residence in malarious areas. In fact, some of the classical definitions of the syndrome described it in expatriate populations only (9). Cases of BWF in autochthonous autochthonous /au·toch·tho·nous/ (aw-tok´thah-nus) 1. originating in the same area in which it is found. 2. denoting a tissue graft to a new site on the same individual. populations have recently been described in the literature from Southeast Asia (10) and in African children in Senegal (7). We describe a large number of BWF cases in the 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. ward of a hospital in the Burundi highlands, where no case has been observed in the previous 10-year period (1992 2002). The Study Since January 1992, a hospital-based survey of malaria has been conducted at Kiremba Hospital in Ngozi Province. This 140-bed facility is located 1,540 m above sea level in the Burundi highlands; it serves a population of 75,000 (11). For each case of malaria, laboratory data and clinical findings are recorded. Rising illness and death rates are being reported throughout Burundi, where P. falciparum accounts for most cases (12). According to the Kiremba Hospital registry, a 2-fold increase in admissions for malaria in the pediatric ward (children [less than or equal to] 14 years of age) was recorded from 1997 (658 cases) to 2002 (1,343 cases). From February to December 2003, a period when 1,039 malaria patients were hospitalized, we observed 9 cases of severe intravascular hemolysis with dark urine in pediatric patients who had been treated with quinine. These children were all male with a mean age of 8.2 years (range 3-14 years). According to patients' health cards, all had been previously treated with quinine, either parenterally par·en·ter·al adj. 1. Physiology Located outside the alimentary canal. 2. Medicine Taken into the body or administered in a manner other than through the digestive tract, as by intravenous or intramuscular or orally according to Burundi's national policy for treating severe malaria (10 mg/kg 3x/day for 7 days). Clinical and laboratory data are presented in the Table. When BWF occurred, quinine was stopped and artemether (3.2 mg/kg on day 1, then 1.6 mg/kg from day 2 to day 5), was administered intramuscularly in·tra·mus·cu·lar adj. Within a muscle: an intramuscular injection. in in association with 3 days of corticosteroid corticosteroid /cor·ti·co·ster·oid/ (-ster´oid) any of the steroids elaborated by the adrenal cortex (excluding the sex hormones) or any synthetic equivalents; divided into two major groups, the glucocorticoids and therapy. All patients had severe anemia requiring blood transfusion according to hospital policy (hemoglobin <4.5 g/dL or <6 g/dL with accompanying dyspnea dyspnea /dysp·nea/ (disp-ne´ah) labored or difficult breathing.dyspne´ic paroxysmal nocturnal dyspnea ). Four patients needed 1 U of blood; 5 other patients needed >1 U. No deaths were recorded, and clinical outcome on discharge was satisfactory: thick smears were negative and hemoglobin levels had improved in all patients. Conclusions In Burundi, chloroquine was replaced by sulfadoxine-pyrimethamine (SP) alone as firstline treatment for uncomplicated malaria in 2001. However, the rapid development of resistance to SP brought back the use of oral quinine, a drug still available in health centers as well as in hospital settings. Since November 2003, artesunate and amodiaquine have replaced SP as firstline treatment in Burundi (13). The result of the new treatment guidelines was a considerable reduction in the number of hospitalized malaria cases in 2004 (671 cases from January 1 to October 31, 2004). No cases of BWF were observed in this period. Despite changes in policy for the use of firstline antimalarial drugs, however, parenteral quinine continued to be the drug of choice for severe cases throughout this period. All 9 patients with BWF seen in 2003 (with 1 exception) lived in the area served by Kiremba Hospital and were recorded during an 11-month period. This number represents an incidence of 11.5 cases/100.000 population/ year. In reviewing recent literature, we found only 1 publication on BWF involving an African population (7). The study was carried out at the Dielmo village in Senegal, where 3 cases were detected in a 10-year prospective study in a small population (315 inhabitants
The game is based loosely on the concepts from SameGame. ). All 3 cases were in children who suffered several malaria attacks and were treated with oral or parenteral quinine, depending on the severity of the case. As a consequence, quinine was withdrawn as the drug of firstline therapy for uncomplicated cases of malaria. No more cases of BWF were recorded during the subsequent 6-year follow-up period. In our study, patients were all boys admitted to the pediatric ward. No cases of oligoanuria were seen, which is not surprising in pediatric patients (14). At the onset of severe intravascular hemolysis, the blood smears of 2 children were negative for malaria; 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. was low in the others. These findings agree with the definition of BWF as being characterized by scanty or absent parasitemia (4,6,9). We were unable to determine G6PD levels in our patients, which is a major limitation of our study. However, in view of the overlap between malaria, quinine administration, and G6PD deficiency, the hemoglobinuria triggered by this deficiency should not be seen as a separate syndrome (10). The management of our cases included 3 components: First, treatment with parenteral (intramuscular intramuscular /in·tra·mus·cu·lar/ (-mus´ku-ler) within the muscular substance. in·tra·mus·cu·lar adj. Abbr. IM Within a muscle. ) artemether (3.2 mg/kg on day 1, then 1.6 mg/kg from days 2 to 5) after stopping quinine, according to recent trends in the literature (3-5). Artemisinin derivates have not been implicated im·pli·cate tr.v. im·pli·cat·ed, im·pli·cat·ing, im·pli·cates 1. To involve or connect intimately or incriminatingly: evidence that implicates others in the plot. 2. in BWF episodes unless given in combination with mefloquine (8). Second, blood transfusion for severe anemia was performed according to the above described hospital policy. And finally, a short course of corticosteroid therapy was administered. Our experience suggests the need to review the definition of BWF since the syndrome affects not only adult expatriates but also African children. All reported African children with cases of BWF had frequently received oral quinine therapy. African adults seem to be only occasionally affected. This finding suggests that BWF occurs in nonimmune persons or those who have not yet gained immunity. This statement is supported by the lack of cases in adults cured in the same hospital. To reduce hemolysis, we treated BWF with corticosteroids Corticosteroids Definition Corticosteroids are group of natural and synthetic analogues of the hormones secreted by the hypothalamic-anterior pituitary-adrenocortical (HPA) axis, more commonly referred to as the pituitary gland. , even though this step is not recommended by the World Health Organization. Our reasoning was that the phenomenon could be related to immune mechanisms in quinine-sensitized erythrocytes Erythrocytes Red blood cells. Mentioned in: Bartonellosis erythrocytes (ē·rithˑ·rō·sīts), n.pl red blood cells. (14). The influence of quinine seems to be an important factor in the pathogenesis of BWF. Other amino-alcohol drugs such as mefloquine or halofantrine have never been used intensively in Africa, principally because they are expensive. When policy changes lead to less use of oral quinine, BWF syndrome tends to disappear. Further similar reports from other areas in the African continent that would confirm our findings could have important implications on national policies for treating malaria in African children. Table. Clinical data from children at the onset of blackwater fever Data Case 1 Case 2 Case 3 Case 4 Age 13 3 5 14 Hemoglobin (g/dL) 4.2 3.8 2.2 4.6 Parasites/[micro]L 4,700 6,800 8,100 1,680 Fever * + + + - Jaundice ([dagger]) + - + + Hepatomegaly ([double dagger]) - + - - Splenomegaly ([double dagger]) - + + - Vomiting - - + + Oligoanuria - - - - Abdominal pain + - - + Data Case 5 Case 6 Case 7 Case 8 Age 7 12 14 3 Hemoglobin (g/dL) 5.8 4.3 2.5 2.5 Parasites/[micro]L 0 7,600 11,480 5,450 Fever * + + + + Jaundice ([dagger]) - - - - Hepatomegaly ([double dagger]) - - - + Splenomegaly ([double dagger]) - + + + Vomiting + + - - Oligoanuria - - - - Abdominal pain - - - + Data Case 9 Age 3 Hemoglobin (g/dL) 3.1 Parasites/[micro]L 0 Fever * + Jaundice ([dagger]) - Hepatomegaly ([double dagger]) + Splenomegaly ([double dagger]) + Vomiting - Oligoanuria - Abdominal pain - * Axillary temperature >37.5[degrees]C. ([dagger]) Total bilirubinemia >1.5 mg/dL. ([double dagger]) Manually assessed, >2 cm by costal margin. Acknowledgments We thank Mr. Bernard and the entire staff of the pediatric ward of Kiremba Hospital. References (1.) Bruce-Chwatt LJ. Quinine and the mystery of blackwater fever. Acta Leiden. 1987;55:181-96. (2.) White NJ. Malaria. In: Cook GC, Zumla AI, editors. Manson's tropical diseases. XXI ed. Philadelphia: W.B. Saunders; 2003. p. 1205-95. (3.) Bruncel F, Gachot B, Wolff M, Regnier B, Danis M, Vachon F, et al. Resurgence of blackwater fever in long-term European expatriates in Africa: report of 21 cases and review. Clin Infect Dis. 2001;32: 1133-40. (4.) Van den Ende J, Coppens G, Verstraeten T, Van Haeghenborgh T, Depraetere K, Van Gompel A, et al. Recurrence of blackwater fever: triggering of relapses by different antimalarials. Trop Med Int Health. 1998;3:632-9. (5.) Bisoffi Z, Marocco S, Montero G, Marsiaj M. Acute intravascular haemolysis Hae`mol´y`sis n. 1. (Physiol.) Same as Hæmatolysis, Hæmatolytic. hemolysis, haemolysis the breaking down of erythrocytes with liberation of hemoglobin in the blood. (blackwater fever) after malarial treatment. Trop Med Int Health. 1999;4:72-3. (6.) Bruneel F, Gachot B, Wolff M, Bedos JR Regnier B, Danis M, et al. Blackwater fever. Presse Med. 2002;31:1329-34. (7.) Rogier C, Imbert P, Tall A, Sokhna C, Spiegel A, Trape JF. Epidemiological and clinical aspects of blackwater fever among African children suffering frequent malaria attacks. Trans R Soc Trop Med Hyg. 2003;97:193-7. (8.) Price R, Van Vugt M, Phaipun L, Luxemburger C, Simpson J, McGready R, et al. Adverse effects in patients with acute 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. treated with artemisinin derivatives. Am J Trop Med Hyg. 1999;60:547-55. (9.) World Health Organization. Severe falciparum malaria. Trans R Soc Trop Med Hyg. 2000;94(Suppl1):S1-74. (10.) Tran TH, Day NR Ly VC, Nguyen TH, Pham PL, Nguyen HP, et al. Blackwater fever in southern Vietnam: a prospective descriptive study of 50 cases. Clin Infect Dis. 1996;23:1274-81. (11.) Bonora S, De Rosa FG, Boffito M, Rossati A, Di Perri G. Rising temperature and the malaria epidemic in Burundi. Trends Parasitol. 2001;17:572-3. (12.) Etchegorry MG, Matthys F, Galinski M, White NJ, Nosten F. Malaria epidemic in Burundi. Lancet. 2001;357:1046-7. (13.) Ndayiragije A, Niyungeko D, Karenzo J, Niyungeko E, Barutwanayo M, Ciza A, et al. Efficacy of therapeutic combinations with artemisinin derivatives in the treatment of non complicated malaria in Burundi. Trop Med Int Health. 2004;9:673-9. (14.) Warrel DA. Clinical features of malaria, In: Warrel DA, Gilles HM, editors. Essential malariology malariology Rare. the study of malaria. — malariologist, n. See also: Disease and Illness . Fourth ed. London: Arnold; 2002. p. 191-205. Federico Gobbi, * Sabrina Audagnotto, * Laura Trentini, * Innocent Nkurunziza, ([dagger]) Manuel Corachan, ([double dagger]) and Giovanni Di Perri * * Clinica Universitaria Malattie Infettive, Turin, Italy; ([dagger]) Hopital de Kiremba, Ngozi, Burundi; and ([double dagger]) University Hospital, Barcelona, Spain Dr. Gobbi is a specialist in infectious diseases at Turin University in Italy. Much of his research has been conducted in African countries (Burundi, Kenya, Democratic Republic of Congo, Uganda, Mozambique). His primary research interests are tropical diseases, in particular, malaria. Address for correspondence: Federico Gobbi, Clinica Universitaria Malattie Infettive, Ospedale Amedeo di Savoia, Corso Svizzera 164, 10149, Torino, Italy; fax: 39-01-1439-3972: email: fedgobbi@tin.it |
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