[beta]-herpesviruses in febrile children with cancer.We conducted a cross-sectional study cross-sectional study n. See synchronic study. cross-sectional study, n the scientific method for the analysis of data gathered from two or more samples at one point in time. of [beta]-herpesviruses in febrile febrile /feb·rile/ (feb´ril) pertaining to or characterized by fever. feb·rile adj. Of, relating to, or characterized by fever; feverish. 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. oncology patients (n = 30), with a reference group of febrile pediatric solid-organ transplant recipients (n = 9). One (3.3%) of 30 cancer patients and 3 (33%) of 9 organ recipients were PCR PCR polymerase chain reaction. PCR abbr. polymerase chain reaction Polymerase chain reaction (PCR) positive for cytomegalovirus cytomegalovirus (sī'təmĕg'əlōvī`rəs), member of the herpesvirus family that can cause serious complications in persons with weakened immune systems. . Four (13%) of 30 cancer patients and 3 (33%) of 9 transplant recipients had human herpesvirus herpesvirus, any of the family (Herpesviridae) of common DNA-containing viruses, many of which are associated with human disease. See cytomegalovirus; Epstein-Barr virus; herpes simplex; herpes zoster. 6B (HHV HHV Human Herpes Virus HHV Higher Heating Value HHV Hilton Hawaiian Village HHV High Heating Value HHV Help Hospitalized Veterans (Winchester, CA) HHV Heavy HMMWV HHV Hydraulic Hybrid Vehicle 6B) DNAemia, which was more common within 6 months of initiation of immune suppression (4 of 16 vs. 0 of 14 cancer patients; p = 0.050). HHV-6A and HHV-7 were not detected. No other cause was identified in children with HHV-6B or cytomegalovirus DNAemia. One HHV-6B-positive cancer patient had febrile disease with concomitant hepatitis. Other HHV-6B-positive children had mild "viral" illnesses, as did a child with primary cytomegalovirus infection Cytomegalovirus infection A common asymptomatic infection caused by cytomegalovirus, which can produce life-threatening illnesses in the immature fetus and in immunologically deficient subjects. . Cytomegalovirus and HHV-6B should be included in the differential diagnosis differential diagnosis n. Determination of which one of two or more diseases with similar symptoms is the one from which the patient is suffering. Also called differentiation. of febrile disease in children with cancer. ********** Much remains to be learned about the pathogenic role of [beta]-herpesviruses (cytomegalovirus [CMV CMV cytomegalovirus. CMV abbr. 1. controlled mechanical ventilation 2. cytomegalovirus Cytomegalovirus (CMV) ], human herpesvirus 6 variants A and B [HHV-6A and HHV-6B], and human herpesvirus 7 [HHV-7]) in immune-compromised children. Most persons are infected with CMV, HHV-6B, and HHV-7 during childhood; the age of acquisition and clinical spectrum of HHV-6A have not been defined. In immune-competent children, CMV is associated with heterophile-negative mononucleosis mononucleosis /mono·nu·cle·o·sis/ (-noo?kle-o´sis) excess of mononuclear leukocytes (monocytes) in the blood. chronic mononucleosis chronic fatigue syndrome. , HHV-6B with roseola infantum roseola in·fan·tum n. See exanthema subitum. roseola infantum Exanthem subitum, see there (exanthem exanthem /ex·an·them/ (eg-zan´them) 1. any eruptive disease or fever. 2. an eruption characterizing an eruptive fever. subitum or sixth disease), and HHV-7 with a small percentage of clinically recognized cases of roseola Roseola Definition Roseola is a common disease of babies or young children, in which several days of very high fever are followed by a rash. Description Roseola is an extraordinarily common infection, caused by a virus. . However, most primary infections with these viruses are either asymptomatic or involve a nonspecific nonspecific /non·spe·cif·ic/ (non?spi-sif´ik) 1. not due to any single known cause. 2. not directed against a particular agent, but rather having a general effect. nonspecific 1. mild illness that can include fever, malaise, and abnormal liver function or hepatosplenomegaly (1-4). After primary infection, these viruses establish life-long residency in the host, seldom causing disease unless the immune system immune system Cells, cell products, organs, and structures of the body involved in the detection and destruction of foreign invaders, such as bacteria, viruses, and cancer cells. Immunity is based on the system's ability to launch a defense against such invaders. is weakened, as occurs after treatment for solid-organ and stem cell transplantation Stem Cell Transplantation Definition Stem cells are basic human cells that reproduce (replicate) easily, providing a continuous source of new, sometimes different types of cells. . In these patients, each of the [beta]-herpesviruses can reactivate re·ac·ti·vate v. 1. To make active again. 2. To restore the ability to function or the effectiveness of. re·ac , manifesting as febrile and sometimes life-threatening illness including pneumonitis pneumonitis /pneu·mo·ni·tis/ (noo?mo-ni´tis) inflammation of the lung; see also pneumonia. hypersensitivity pneumonitis , encephalitis encephalitis (ĕnsĕf'əlī`təs), general term used to describe a diffuse inflammation of the brain and spinal cord, usually of viral origin, often transmitted by mosquitoes, in contrast to a bacterial infection of the meninges , bone marrow suppression Bone marrow suppression A decrease in cells responsible for providing immunity, carrying oxygen, and those responsible for normal blood clotting. Mentioned in: Cancer Therapy, Definitive bone marrow suppression , graft-versus-host disease graft-versus-host disease n. A type of incompatibility reaction of transplanted cells against host tissues that possess an antigen not possessed by the donor. Also called graft-versus-host reaction. , and organ rejection (5-7). In addition to having independent pathologic effects, [beta]-herpesviruses may have additive or synergistic effects, as well as interactions with other infectious agents (e.g., fungal infections) (8,9). Immune suppression caused by cancer treatment has many forms, often as pulses of cytotoxic agents that kill rapidly dividing cells, including lymphocytes. The risk for infections in pediatric cancer patients is well recognized, and much effort has been devoted to identifying and treating bacterial and fungal infections associated with fever and neutropenia Neutropenia Definition Neutropenia is an abnormally low level of neutrophils in the blood. Neutrophils are white blood cells (WBCs) produced in the bone marrow that ingest bacteria. (10-14). This effort usually involves hospitalization for empiric administration of intravenous antimicrobial drugs, even though most bacterial blood cultures remain negative; 40%-70% of such febrile episodes have no identifiable source (15,16). Some viral infections, such as those with herpes simplex herpes simplex (hûr`pēz), an acute viral infection of the skin characterized by one or more painful, itching blisters filled with clear fluid. or varicella varicella: see chicken pox. zoster zoster /zos·ter/ (zos?ter) herpes zoster. zos·ter n. See shingles. zoster, See herpes zoster. viruses, are associated with disease that can be serious and even fatal in pediatric oncology patients (17,18). Most episodes of fever are unexplained and assumed to be viral in nature (19). Little attention has been paid to the possible contribution of [beta]-herpesvirnses as a cause of febrile illness in children with cancer, despite recognition that these viruses cause disease after organ transplantation The transfer of organs such as the kidneys, heart, or liver from one body to another. The transplantation of human organs has become a common medical procedure. Typical organs transplanted are the kidneys, heart, liver, pancreas, cornea, skin, bones, and lungs. . In studies that preceded application of PCR, CMV detection was associated with fever and hepatitis in children with malignancy (20,21). HHV-6 seroprevalence seroprevalence Immunology The proportion of a population that is seropositive–ie, has been exposed to a particular pathogen or immunogen; the seropositivity of a population is calculated as the number of individuals who produce a particular antibody divided is similar in pediatric cancer patients and controls (22,23), but virus has been detected less frequently in saliva of children with cancer than that of healthy controls (24). In children from the Czech Republic, Michalek et al. detected both primary and reactivated HHV-6 and CMV infections during cytotoxic chemotherapy by using serologic se·rol·o·gy n. pl. se·rol·o·gies 1. The science that deals with the properties and reactions of serums, especially blood serum. 2. analysis and PCR (23,25). Some HHV-6 infections were associated with severe disease, including pneumonitis, bone marrow aplasia aplasia /apla·sia/ (ah-pla´zhah) lack of development of an organ or tissue.aplas´tic aplasia axia´lis extracortica´lis conge´nita familial centrolobar sclerosis. , and persisting fever. Because of the biologic plausibility of [beta]-herpesvirus involvement in febrile illness in pediatric cancer patients and the paucity of PCR-era literature in this area, we conducted a cross-sectional study of the activity of these viruses in pediatric cancer patients and other immune-compromised children. The purpose of this study was to determine whether there is sufficient viral activity in these populations to warrant in-depth study and clinical consideration. Materials and Methods Patients The study was reviewed and approved by the Cleveland Clinic Institutional Review Board. Informed consent was obtained from a parent or guardian of each person <18 years of age, or directly from persons [greater than or equal to] 18 years of age; assent was obtained from children 7-17 years of age. Patients were enrolled from August 2004 through April 2005. Enrolled children were receiving treatment for a malignancy or were receiving immunosuppressive therapy Immunosuppressive therapy Medical treatment in which the immune system is purposefully thwarted. Such treatment is necessary, for example, to prevent organ rejection in transplant cases. after solid-organ transplantation (SOT). Inclusion criteria were an age of newborn to 21 years and new onset of fever with an oral or rectal temperature [greater than or equal to] 38[degrees]C or an axillary ax·il·lar·y n. Relating to the axilla. Axillary Located in or near the armpit. Mentioned in: Mastectomy axillary of or pertaining to the armpit. temperature [greater than or equal to] 37.5[degrees]C. At enrollment, we collected a blood specimen and information on age, sex, underlying illness and diagnosis, acute symptoms accompanying fever, and details about immune suppression (chemotherapy regimen, radiation therapy, immune modulators immune modulators, n.pl chemicals that influence the immune system. Also called cytokines. , and steroids). Gastrointestinal symptoms were defined as either vomiting or diarrhea. Clinical laboratory data collected included complete blood counts, renal and liver function test results, bacterial blood cultures, as well as results of testing conducted for evaluation of fever, such as respiratory virus analysis, stool studies, chest radiographs, and computed tomography scans Computed Tomography Scans Definition Computed tomography (CT) scans are completed with the use of a 360-degree x-ray beam and computer production of images. These scans allow for cross-sectional views of body organs and tissues. . Specimens and Storage Whole blood was collected in EDTA EDTA: see chelating agents. tubes and stored at 4[degrees]C until processed. A leukocyte leukocyte (l  `kəsīt'): see blood. leukocyte or white blood cell or white corpuscle pellet was collected from 1 mL of whole blood; 400 [micro]L of plasma was preserved, 200 [micro]L for PCR and 200 [micro]L for serologic analysis. Pelleted leukocytes were added to MagnaPure LC lysis buffer (Roche Diagnostics, Indianapolis, 1N, USA) and stored at -20[degrees]C. Virus Culture CMV culture was conducted with pelleted leukocytes by using conventional MRC-5 cell shell vial cultures (Diagnostic Hybrids, Athens, OH, USA). Immune fluorescence testing was conducted after 48 hours by using a monoclonal antibody directed against the CMV immediate early protein (Chemicon, Temecula, CA, USA). Shell vial cultures were obtained for the first 11 patients enrolled; all cultures were negative. Because shell vial culture uses a large number of leukocytes and we were studying a neutropenic population, this procedure was discontinued to preserve cells for more sensitive PCR analysis (26). Purified lymphocytes were cultured to detect HHV-6 or HHV-7 infections as described (27,28). Cytopathic effect was recognized as enlarged and refractile cells, with confirmatory testing by PCR. 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 Template 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. was extracted by using the MagnaPure automated extraction method (Roche Diagnostics) and eluted into 50 [micro]L of buffer. A total of 5 [micro]L of eluted DNA was used in each PCR. The PCRs contained DNA extracted from the equivalent of [approximately equal to] 20 [micro]L of plasma, leukocytes present in 100 [micro]L of whole blood, and 20 [micro]L of whole blood. For detection of CMV and HHV-6 variants A and B, the Artus CMV RG PCR ASWReal Art/Qiagen RealArt CMV LC Assay and the RealArt/Qiagen HHV-6 A/B A/B Airborne A/B Afterburner (jet engines) A/B Air Blast A/B Answerback A/B Auto-brake A/B Air Bus A/B Afterburning LC Assay (QIAGEN, Hamburg, Germany) were used. A co-amplified internal control was used to identify PCR inhibition. To differentiate between HHV-6 variants, the system uses the specific melting temperatures of the probes. Detection of HHV-7 was conducted by using previously described primers and hybridization probes (29). Real-time PCR was performed on a LightCycler system (Roche Diagnostics). Serologic Analysis CMV serologic analysis was performed by using the VIDAS CMV IgG Assay (bioMerieux, Durham, NC, USA) in an automated instrument, according to the manufacturer's protocol. Analyses for HHV-6 (using HHV-6A--infected cells) and HHV-7 were conducted by using conventional indirect immunofluorescence with commercial slides (Panbio Ltd, Columbia, MD, USA). Avidity avidity /avid·i·ty/ (ah-vid´i-te) 1. the strength of an acid or base. 2. in immunology, an imprecise measure of the strength of antigen-antibody binding based on the rate at which the complex is formed. Cf. of antibody to HHV-6 was tested as described by Ward et al. (30). Statistical Analysis and Clinical Associations The exact unconditional test was used to compare groups on viral activity (31). All tests were 2-tailed and performed at a significance level of 0.05. Analyses were performed by using StatXact PROCs version 6.3 (Cytel Software Corp., Cambridge, MA, USA) and SAS (1) (SAS Institute Inc., Cary, NC, www.sas.com) A software company that specializes in data warehousing and decision support software based on the SAS System. Founded in 1976, SAS is one of the world's largest privately held software companies. See SAS System. version 9.1 (SAS Institute Inc., Cary, NC, USA). Clinical associations with [beta]-herpesvirus infection were based on symptoms and concomitant laboratory findings in patients who had no other identifiable cause for their febrile illness. Results Patient Characteristics Forty-one children were enrolled, from whom 39 evaluable specimens were available (Table 1). Thirty of the 39 children had a malignancy (our primary interest) and 9 were organ transplant recipients who were included for comparison. All cancer patients were receiving active therapy, except for 1 child who was included in the study because she had been receiving chemotherapy for 2.5 years, which ended 3 months before study enrollment. Several patients had symptoms in addition to fever, mostly upper respiratory or gastrointestinal. A source of fever was identified for 5 (17%) of 30 cancer patients and 2 (22%) of 9 organ transplant recipients. Two cancer patients had bacteremia bacteremia: see septicemia. bacteremia Presence of bacteria in the blood. Short-term bacteremia follows dental or surgical procedures, especially if local infection or very high-risk surgery releases bacteria from isolated sites. (Escherichia coli, coagulase-negative staphylococci); no fungal infections were detected. Three cancer patients and 2 organ transplant recipients had respiratory viral infections diagnosed by symptoms and positive direct fluorescent antibody Direct fluorescent antibody (DFA or dFA) is a laboratory test that uses antibodies tagged with fluorescent dye to detect the presence of microorganisms. This is the main test used to detect rabies in animals and requires the examination of brain tissue. test results. Of the 39 children, levels of liver enzymes were obtained for 28 as part of routine care. Of these children, 6 had abnormal values; 2 of these 6 also had virus detected (HHV-6B in 1 patient and influenza A in the other). The other 4 patients with increased levels of liver enzymes had longstanding abnormalities; review of their records suggested that the abnormal results were caused by underlying disease in 1 liver transplant patient and chemotherapy in 3 cancer patients. Six patients have died since completion of our study, none from infectious causes. Laboratory Results Of the 11 specimens tested in the shell vial assay, none was positive for CMV. CMV DNA was detected by PCR in lymphocytes of 1 (3.3%) of 30 cancer patients and 3 (33%) of 9 organ transplant recipients (Table 2). Lymphocyte cultures for HHV-6 and HHV-7 were obtained for 34 of the 39 children. Of these, 15 cultures showed cytopathic effects similar to those commonly reported for HHV-6, but none of these were positive for HHV-6 by PCR. Cultured cells from 1 patient with leukemia (study participant 19) were positive for HHV-6B by PCR, in the absence of a cytopathic effect. Four (13%) of 30 cancer patients and 3 (33%) of 9 transplant recipients (p = 0.19) had HHV-6B DNAemia; HHV-6A was not detected. Viral loads ranged from 50 to 500,000 DNA copies/mL. Of 7 PCR-positive patients, 3 also showed positive results in peripheral blood mononuclear mononuclear /mono·nu·cle·ar/ (-noo´kle-er) 1. having but one nucleus. 2. a cell having a single nucleus, especially a monocyte of the blood or tissues. mon·o·nu·cle·ar adj. cells (PBMC PBMC Peripheral Blood Mononuclear Cell ) and whole blood specimens, 2 in only PBMC, and 1 only in a lymphocyte culture. Patient 40, a transplant recipient, had positive results in all specimens tested including PBMC, whole blood, and plasma, with the highest viral load (>5 x [10.sup.5] genomes/mL) in PBMC. These results are consistent with either severe acute infection or the child having germline integrated HHV-6B (32,33). PCR positivity was more common in children whose blood was collected within 6 months of initiation of immune suppression compared with children sampled >6 months after initiation of immune suppression (cancer patients: 4 of 16 vs. 0 of 14 after 6 months, p = 0.050; transplant recipients: 2 of 3 vs. 1 of 6, p = 0.26) (Figure). Solid-tumor patients were less likely to be positive for HHV-6B than either leukemic (1 of 20 vs. 3 of 9, p = 0.046) or SOT patients (1 of 20 vs. 3 of 9, p = 0.046). Two of the HHV-6B-positive SOT patients had concurrent CMV DNAemia. HHV-7 DNA was not detected in any patients. Lymphocyte cultures were not tested for HHV-7 by PCR because none of the plasma, whole blood, or leukocyte pellets were positive for the virus. Possible Associations between [beta]-Herpesvirus Activity and Disease Patients who were positive for [beta]-herpesviruses and those who were negative for these viruses did not differ in their average fever temperature (38.5[degrees]C vs. 38.6[degrees]C). In SOT recipients, the prevalence of HHV-6B and CMV and the spectrum of their associated illnesses were concordant with prior reports. Thus, we will focus on the cancer patients. The only cancer patient with CMV DNAemia appeared to have primary CMV infection on the basis of negative results for immunoglobulin (Ig) G to CMV, negative bacterial blood culture, and age (online Appendix Table, available from www.cdc.gov/EID/content/14/4/579-appT.htm). This patient was a 5.4-year-old child (study participant 29) with acute lymphoblastic leukemia acute lymphoblastic leukemia n. Abbr. ALL Lymphoblastic leukemia occurring mainly in older adults, characterized by rapid onset and progression of symptoms. Also called acute lymphocytic leukemia. (ALL) in remission; he had upper respiratory symptoms and fever but otherwise appeared well. He was treated with an antimicrobial drug (ceftriaxone ceftriaxone /cef·tri·ax·one/ (cef?tri-ak´son) a semisynthetic, ß–resistant, third-generation cephalosporin effective against a wide range of gram-positive and gram-negative bacteria, used as the sodium salt. ) on an outpatient basis, but his blood culture was negative for bacteria and no other source for his fever and illness was found. This child began cancer chemotherapy 36 months before the febrile event. Four patients appeared to have reactivated HHV-6B infection on the basis of positive results for virus DNA, high-avidity IgG, and clinical symptoms. The first patient (study participant 19) was a 2-year-old boy with ALL in remission for the first time. In the second month of chemotherapy; he was hospitalized for fever and ill appearance, but he was not neutropenic or lymphopenic. He had marked hepatomegaly hepatomegaly /hep·a·to·meg·a·ly/ (hep?ah-to-meg´ah-le) enlargement of the liver. hep·a·to·meg·a·ly n. The abnormal enlargement of the liver. Also called megalohepatia. ([approximately equal to] 10 cm below the right costal margin) and abnormal results in liver function tests Liver Function Tests Definition Liver function tests, or LFTs, include tests for bilirubin, a breakdown product of hemoglobin, and ammonia, a protein byproduct that is normally converted into urea by the liver before being excreted by the kidneys. . He was receiving fluconazole fluconazole /flu·con·a·zole/ (floo-kon´ah-zol) a triazoleantifungal used in the systemic treatment of candidiasis and cryptococcal meningitis. flu·con·a·zole n. for oral thrush, and his liver enzyme levels were mildly increased before the febrile illness. However, at admission he had an aspartate aminotransferase (AST (AST Computer, Irvine, CA) A PC manufacturer founded in 1980 by Albert Wong, Safi Quershey and Tom Yuen (A, S and T). It offered a complete line of PCs that sold through its dealer channel. ) level of 2,356 U/L U/L Upload U/L Uplink U/L Universal/Local U/L Units/Litre and an alanine aminotransferase (ALT) level of 2,410 U/L. HHV-6 and HHV-7 IgM and IgG titers were obtained (Specialty Laboratories, Valencia, CA, USA) as part of his ALL treatment protocol. His HHV-6 IgM titer was negative (<40), and his IgG titer was positive (320) and high-avidity antibodies were detected. Results for HHV-7 IgM were negative, and those for IgG were weakly positive (titer 20). Other studies conducted by the primary medical team included tests for acute hepatitis and a CMV PCR; all results were negative. Four days later, his AST level was 84 U/L and his ALT level was 314 U/L. On follow up 7 days after admission, both values were near normal. The hepatitis was attributed to methotrexate methotrexate, drug used in halting the growth of actively proliferating tissues. Introduced in the 1950s, it is used in the treatment of leukemia, psoriasis, and non-Hodgkin's lymphoma. , which was therefore withheld until the levels of liver enzymes returned to nonnal. On the basis of the positive culture for HHV-6B and hepatitis in the setting of febrile illness without other identified infections, we suspect that reactivated HHV-6B infection caused the fever and exacerbated the hepatitis. A 5-year-old girl with relapsed acute myeloid leukemia (study participant 23) was intermittently febrile while hospitalized for 1 month during chemotherapy. She was treated with broad-spectrum antibacterial drugs and anti-fungal drugs. At study enrollment on day 12 of hospitalization, she had an absolute neutrophil count Absolute neutrophil count (ANC) is a measure of the number of neutrophil granulocytes (also known as polymorphonuclear cells, PMN's, polys, granulocytes, segmented neutrophils or segs) present in the blood. Neutrophils are a type of white blood cell that fights against infection. of 0 and an absolute lymphocyte count of 560 cells/[micro]L. Daily blood cultures and sporadic respiratory viral studies did not reveal a cause for her fever, but her whole blood and PBMC were positive for HHV-6B by PCR. [FIGURE OMITTED] HHV-6B was detected in a 2-year-old girl with ALL in remission (study participant 25) and in a 22-month-old boy with stage 3 Wilms tumor (study participant 38). Both of these patients were lymphopenic and had nonspecific febrile illnesses; neither had other identified sources of fever. We suspect primary CMV infection in 1 patient and reactivated HHV-6B infection in 4 cancer patients as likely causes of the febrile episodes. This conclusion is based on a combination of clinical data, positive PCR findings, and lack of other identified sources for fever. Discussion [beta]-Herpesviruses are known pathogens in immunocompromised immunocompromised /im·mu·no·com·pro·mised/ (-kom´pro-mizd) having the immune response attenuated by administration of immunosuppressive drugs, by irradiation, by malnutrition, or by certain disease processes (e.g., cancer). patients, but they have not been extensively studied in children with malignancies. In this study of children who had fever, signs of infection, and had samples taken at 1 time point, we detected [beta]-herpesviruses in 5 of 25 cancer patients who had no other source of fever identified: 4 had HHV-6B DNA and 1 had CMV DNA detected by PCR. [beta]-Herpesviruses were detected in 4 of 7 SOT patients who had no other source of fever identified: 1 had HHV-6B, 1 had CMV, and 2 had both virus (Figure). One of these children was ill and had a high fever and pleuritis with no other pathogens identified. HHV-6A and HHV-7 were not detected in any of the cancer or SOT patients. In our study, frequencies of HHV-6B were similar in transplant recipients and cancer patients (3 of 9 vs. 4 of 30, p = 0.19). HHV-6B was detected more frequently in children with leukemia and solid-organ transplants than in children with other cancers. This finding may be the result of similarities in the degree and type of immune suppression. Children with leukemia and SOT patients generally receive intense initial immune suppression followed by a constant lower level of suppression. In contrast, solid-tumor patients generally receive monthly immune-suppressive treatments and seldom have prolonged lymphopenia. HHV-6B DNAemia was more frequent in children sampled during the first 6 months of immune suppression when immune suppression is most intense, which is consistent with findings for pediatric bone marrow and solid-organ transplant recipients (34). Detection of HHV-6B early after initiation of therapy in patients with cancer (Figure) suggests that the presence of virus DNA may be related to intense immune suppression and not to random occurrence, which would not have clustered early in therapy. Our observations of possible clinical associations with [beta]-herpesvirus infection concur with those of Michalek et al. (23,25) of a cohort dating from 1993 to 1999. Our population included 1 child with suspected HHV-6 disease and hepatitis, which has been seen in association with HHV-6 activity after liver (35), renal (36), and stem cell transplantation (37). In contrast to laboratory detection for CMV, testing for HHV-6 and HHV-7 DNA is often conducted by using in-house assays, which makes comparison across studies difficult. We used an assay for detecting HHV-6 DNA that is commercially available in Europe. This test was concordant with our in-house assay in detecting previously characterized HHV-6 isolates (D. Kohn et al., unpub, data). In addition to standardization of molecular testing, various methods for detecting HHV-6 during febrile episodes should be evaluated because some investigators have suggested that viral isolation by culture may be more useful in correlating active infection with clinical disease (38). Furthermore, reverse transcription--PCR can distinguish active replication from latency (39,40). Several limitations are inherent to our cross-sectional study design. First, capturing data at single time points limits the ability to assess the temporality tem·po·ral·i·ty n. pl. tem·po·ral·i·ties 1. The condition of being temporal or bounded in time. 2. temporalities Temporal possessions, especially of the Church or clergy. Noun 1. of the virologic burden in relation to disease. Second, although we found HHV-6B positivity during febrile events in 18% of our population, we do not have data during periods without fever and therefore cannot be certain that viremia viremia /vi·re·mia/ (vi-re´me-ah) the presence of viruses in the blood. vi·re·mi·a n. The presence of viruses in the bloodstream. is specifically associated with disease. The studies by Michalek et al. also included treatment-phase blood specimens that were obtained only during febrile illness or other clinical events suggestive of viral infection (23,25). Thus, activity of HHV-6 and other lymphotropic viruses during nonfebrile periods in this patient population remains unknown. We studied a heterogeneous patient population that included several types of cancer; the level of immune suppression varied widely. Finally, identification of possible causes of febrile episodes was limited by the assays we performed and the tests ordered by the primary medical team. Thus, we cannot exclude other viral pathogens such as human metapneumovirus or Epstein-Barr virus for which no testing was conducted. Evidence for our suspected associations between HHV-6B and the febrile events includes 1) our use of relatively small volumes of blood in the PCR analyses, which reduces the chance of detecting sporadic latently infected lymphocytes; 2) the temporal association of detection of HHV-6B with initiation of chemotherapy; and 3) a lack of other identified sources for the fever. With the exception of the transplant recipient with possible HHV-6B germline integration, HHV-6B or CMV are plausible causes of the febrile episode in every instance in which they were detected. Our study differs from prior studies in that we assayed for all 4 [beta]-herpesviruses and considered the timing of viral activity relative to the onset of immune suppression. We included solid-organ transplant patients as a reference for cancer patients, and excluded stem cell transplant patients, a population in whom reactivation reactivation to become active after a period of quiescence or, as in bacterial and viral infections, latency. cross reactivation of CMV and HHV-6 has been studied. By enrolling children with a variety of malignancies, we surveyed a diverse cancer population. Although the number of patients we studied was small, CMV and HHV-6B are clearly active in pediatric cancer patients. The lack of other identified agents coincident with fever suggests that these viruses may cause febrile illness in this population. Our observations, combined with those of Michalek et al. (23,25), suggest that HHV-6B and CMV should be included in the differential diagnoses of febrile disease in children with cancer. Further investigation in this patient population is needed to clarify the role of [beta]-herpesviruses in these febrile illnesses. Acknowledgments We thank the patients and their families and physicians and nursing staff in Pediatric Hematology and Oncology for their participation in and support of this project. Dr Yee-Guardino is a consultant in pediatrics at the Cleveland Clinic. Her research interests include herpesvirus disease in immunocompromised children. References (1. Hall CB, Long CE, Schnabel KC, Caserta MY, McIntyre KM, Costanzo MA, et al. Human herpesvirus-6 infection in children. A prospective study of complications and reactivation. N Engl J Med. 1994;331:432-8. (2.) Hall CB, Caserta MT, Schnabel KC, McDermott MP, Lofthus GK, Camahan JA, et al. 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Cytomegaloviruses. In: Knipe DM. Howley PM, Griffin DE, Lamb RA, Martin MA, Roizman B, et al., editors. Fields virology. Philadelphia: Lippincott Williams and Wilkins; 2007. p.2701-72. (8.) Wang FZ, Pellett PE. Human herpesviruses 6A, 6B, and 7: immunobiology and host response. In: Arvin A, Campadelli-Fiume G, Mocarski ES, Roizman B, Whitley RJ, Yamanishi K, editors. Human herpesviruses: biology, therapy, and immunoprophylaxis. Cambridge (UK): Cambridge University Press Cambridge University Press (known colloquially as CUP) is a publisher given a Royal Charter by Henry VIII in 1534, and one of the two privileged presses (the other being Oxford University Press). ; 2006. p. 850-74. (9.) Singh N. Human herpesviruses-6, -7 and -8 in organ transplant recipients. Clin Microbiol Infect. 2000;6:453-9. (10.) Quezada G, Sunderland T, Chan KW, Rolston K, Mullen CA. Medical and non-medical barriers to outpatient treatment of fever and neutropenia in children with cancer. Pediatr Blood Cancer. 2007;48:273-7. (11.) Ozkaynak ME Krailo M, Chen Z, Feusner J. Randomized ran·dom·ize tr.v. ran·dom·ized, ran·dom·iz·ing, ran·dom·iz·es To make random in arrangement, especially in order to control the variables in an experiment. comparison of antibiotics with and without granulocyte colony-stimulating factor granulocyte colony-stimulating factor See G-CSF. in children with chemotherapy-induced febrile neutropenia: a report from the Children's Oncology Group. Pediatr Blood Cancer. 2005;45:274-80. (12.) Sung L, Feldman BM, Schwamborn G, Paczesny D, Cochrane A, Greenberg ML, et al. Inpatient versus outpatient management of low risk pediatric febrile neutropenia: measuring parents' and healthcare professionals' preferences. J Clin Oncol. 2004;22:3922-9. (13.) Alexander SW, Wade KC, Hibberd PL, Parsons SK. Evaluation of risk prediction criteria for episodes of febrile neutropenia in children with cancer. J Pediatr Hematol Oncol. 2002;24:38-42. (14.) 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Pediatr Blood Cancer. 2005;45:945-51. (19.) Wood MJ. Viral infections in neutropenia--current problems and chemotherapeutic control. J Antimicrob Chemother 1998;41Suppl D:81-93. (20.) Furukawa T, Funamoto Y, Ishida S, Kamiya H. The importance of primary cytomcgalovirus infection in childhood cancer. Eur J Pediatr. 1987;146:34-7. (21.) Rokicka-Milewska R, Pacholska J, Lukowska K, Paciorkiewicz W, Jastrzebska M. Cytomegalovirus infection in children with blood diseases. Acta Haematol Pol. 1992;23:191-5. (22.) Lyall EG. Serological serological pertaining to or emanating from serology. serological test one involving examination of blood serum usually for antibody. response of paediatric Adj. 1. paediatric - of or relating to the medical care of children; "pediatric dentist" pediatric oncology patients to human herpesvirus-6. J Med Virol. 1994;43:373-9. (23.) Michalek J, Horvath R, Benedik J, Hrstkova H. Human herpes virus-6 infection in children with cancer. Pediatr Hematol Oncol. 1999; 16:423-30. (24.) Lyall EG, Cubic HA. Human herpesvirus-6 DNA in the saliva of paediatric oncology patients and controls. J Med Virol. 1995;47:317-22. (25.) Michalek J, Horvath R. High incidence of Epstein-Barr virus, cytomegalovirus and human herpesvirus 6 infections in children with cancer. BMC (BMC Software, Inc., Houston, TX, www.bmc.com) A leading supplier of software that supports and improves the availability, performance, and recovery of applications in complex computing environments. Pediatr. 2002;2:1. (26.) Caliendo AM, Yen-Lieberman B, Baptista J, Andersen J, Crumpacker C, Schuurman R, et al. Comparison of molecular tests for detection and quantification of cell-associated cytomegalovirus DNA. J Clin Microbiol. 2003;41:3509-13. (27.) Black JB, Burns DA, Goldsmith CS, Feorino PM, Kite-Powell K, Schinazi RF, et al. Biologic properties of human herpesvirus 7 strain SB. Virus Res. 1997;52:25-41. (28.) 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Human herpesviruses 6 and 7 as potential pathogens after liver transplant: prospective comparison with the effect of cytomegalovirus. J Med Virol. 1999;59:496-501. (36.) Ratnamohan VM, Chapman J, Howse H, Bovington K, Robertson P, Byth K, et al. Cytomegalovirus and human herpesvirus 6 both cause viral disease after renal transplantation. Transplantation. 1998;66:877-82. (37.) Ljungman P, Wang FZ, Clark DA, Emery VC, Remberger M, Ringden O, et al. High levels of human herpesvirus 6 DNA in peripheral blood leucocytes are correlated to platelet engraftment engraftment /en·graft·ment/ (en-graft´ment) incorporation of grafted tissue into the body of the host. Engraftment The process of transplanted stem cells reproducing new cells. and disease in allogeneic allogeneic /al·lo·ge·ne·ic/ (-je-ne´ik) 1. having cell types that are antigenically distinct. 2. in transplantation biology, denoting individuals (or tissues) that are of the same species but antigenically stem cell transplant patients. Br J Haematol. 2000;111:774-81. (38.) Yoshikawa T, Asano Y, Ihira M, Suzuki K, Ohashi M, Suga S, et al. Human herpesvirus 6 viremia in bone marrow transplant bone marrow transplant: see bone marrow. recipients: clinical features and risk factors. J Infect Dis. 2002;185:847-53. (39.) Norton RA, Caserta MT, Hall CB, Schnabel K, Hocknell P, Dewburst S. Detection of human herpesvirus 6 by reverse transcription-PCR. J Clin Microbiol. 1999;37:3672-5. (40.) Yoshikawa T, Akimoto S, Nishimura N, Ozaki T, Ihira M, Ohashi M, et al. Evaluation of active human herpesvirus 6 infection by reverse transcription-PCR. J Med Virol. 2003;70:267-72. Address for correspondence: Philip E. Pellett, Department of Immunology and Microbiology, Wayne State University School of Medicine The Wayne State University School of Medicine (WSUSOM) is the largest single-campus medical school in the United States with more than 1,000 medical students. In addition to undergraduate medical education, the school offers master’s degree, Ph.D. and M.D.-Ph.D. , 540 E Canfield Ave, 6225 Scott Hall, Detroit, M148202, USA; email: ppellett@ med.wayne.edu Stephanie Yee-Guardino, * Kate Gowans, * Belinda Yen-Lieberman, ([dagger]) Pamela Berk, ([dagger]) Debra Kohn, ([dagger]) Fu-Zhang Wang, ([dagger]) (1) Lara Danziger-Isakov, * ([dagger]) Camille Sabella, * ([dagger]) Sarah Worley, ([dagger]) Philip E. Pellett, ([dagger]) (2) and Johanna Goldfarb * ([dagger]) * Cleveland Clinic Children's Hospital, Cleveland, Ohio, USA; and ([dagger]) Cleveland Clinic, Cleveland, Ohio, USA (1) Current affiliation: University of North Carolina, Chapel Hill, North Carolina Chapel Hill is a town in North Carolina and the home of the University of North Carolina at Chapel Hill (UNC-CH), the oldest state-supported university in the United States. As of the 2000 census, it had a population of 48,715. As of 2004 its estimated population was 52,440. , USA (2) Current affiliation: Wayne State University School of Medicine, Detroit, Michigan, USA
Table 1. Characteristics of febrile immune-suppressed children *
Cancer SOT
Characteristic (n = 30) (n = 9)
Age, y; mean, median, range 6.1, 5.0, 11.8, 13.3,
0.4-17 4.3-20.6
Sex
F 14 7
M 16 2
Basis of immune suppression
Cancer 30 (77%) --
Solid tumor 20 --
Leukemia 9 --
Lymphoma 1 --
Solid-organ transplant -- 9 (23%)
Heart -- 5
Lung -- 2
Liver -- 2
Immune suppressants 29 9
Cytotoxic chemotherapy 28 --
Radiation 6 --
Chemotherapy and radiation 6 --
Immune modulators ([dagger]) -- 9
Steroids (past 6 months) 14 7
Signs and symptoms
III appearance 7 1
Upper respiratory 17 1
Gastrointestinal 10 7
Headache 3 3
Rash 0 0
Seizure 0 0
Hepatitis 1 1
Blood products (past 6 months)
([double dagger]) 20 5
Laboratory parameters
Neutropenic (<500 cells/[micro]L) 14 2
Lymphopenic (<500 cells/[micro]L) 13 4
Established source for fever
Bacteremia 2 0
Positive respiratory DFA test 3 2
result ([section])
* SOT, solid-organ transplantation; -, not applicable; DFA, direct
fluorescence antigen.
([dagger]) Immune modulators included tacrolimus in 4, tacrolimus
and azathioprine in 2, cyclosporine and mycophenolate mofetil in 2,
sirolimus in 1, and tacrolimus, mycophenolate mofetil, antithymocyte
globulin (rabbit), and corticosteroids in 1.
([double dagger]) Blood products recorded included packed
erythrocytes or platelets.
([section]) Of the 5 patients with positive respiratory DFA test
results, 2 were positive for parainfluenza 3, 2 for influenza A,
and 1 for respiratory syncytial virus.
Table 2. Detection of [beta]-herpesviruses in cancer patients and
solid-organ transplant recipients *
Cancer patients, no.
positive/no. tested (%)
Transplant patients
Leukemia Solid tumor (n = 9), no. positive/
Characteristic (n = 9) (n = 20) no. tested (%)
CMV PCR
Whole blood 1/6 (17) 0/5 3/7 (43)
PBMC 1/7 (14) 0/16 2/8 (25)
Plasma 0/9 0/20 2/9 (22)
All tests 1/9 (11) 0//20 (0) 3/9 (33)
HHV-6 PCR
Whole blood 2/6 (33) 0/5 2/7 (29)
PBMC 1/7 (14) 1/16 (6) 3/8 (38)
Plasma 0/9 0/19 1/9 (11)
Lymphocyte culture 1/8 (13) 0/16 0/9
All tests 3/9 (33) 1/20 (5) 3/9 (33)
HHV-7 PCR
Whole blood 0/6 0/5 0/7
PBMC 0/7 0/16 0/8
Plasma 0/9 0/20 0/9
All tests 0/9 0/20 0/9
* Data are not shown for study participant 23, a patient with lymphoma
who did not have [beta]-herpesviruses detected in whole blood, PBMC,
or plasma. CMV, cytomegalovirus; PBMC, peripheral blood mononuclear
cells; HHV-6, human herinesvirus 6.
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