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      Enterovirus 75 and Aseptic Meningitis, Spain, 2005

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          Abstract

          To the Editor: Although most human enterovirus (EV) (genus Enterovirus, family Picornaviridae) infections are asymptomatic, they can cause upper respiratory illness, febrile rash, aseptic meningitis, pleurodynia, encephalitis, acute flaccid paralysis, and neonatal sepsislike disease ( 1 ). Most EVs have been implicated in aseptic meningitis, most notably echovirus (E) 30, 9, 6, and 11 and coxsackie B virus (CBV) type 5 ( 2 ); other serotypes are less frequently associated with neurologic disease. New EV serotypes have come to light, chiefly as a result of molecular typing methods ( 3 – 6 ). EV75 was proposed as a new serotype of the EV genus in 2004 ( 5 ). Retrospective analysis showed that it had circulated sporadically in Asia, the United States, and Africa since at least 1974. Only 8 isolates of this serotype have been reported worldwide, in 1974, 1985, 1986, 1987 (n = 2), 1998, and 2000 (n = 2). Infection in those cases was associated with respiratory disease, acute flaccid paralysis, neonatal jaundice, failure to thrive, or unspecified neurologic disease or was asymptomatic. At the time of writing this manuscript, EV75 had not been linked to aseptic meningitis. From May 2005 through January 2006, 106 EVs were received for typing from Spanish hospital laboratories; 46 of them were from patients with aseptic meningitis, 10 from patients or contacts of patients with acute flaccid paralysis, 27 from patients with fever, 7 from patients with respiratory diseases, and 16 from other patients. Twenty EVs could not be typed by serum neutralization ( 7 ); however, 3´ terminus VP1 gene sequence analysis ( 8 ) showed that they were E18 (n = 7), CBV3 (n = 1), and E16 (n = 2); 2 could not be typed with serologic or molecular methods because the 3´ terminus of VP1 gene amplification was negative. The analysis of the 3´ terminus of VP1 gene of the remaining 5 cerebrospinal fluid (CSF) and 3 nasopharyngeal isolates showed that they were similar to the recently proposed EV75 serotype ( 5 ). These 8 isolates were obtained from samples from children in Bilbao (n = 3), Granada (n = 3), Barcelona (n = 1), and the Canary Islands (n = 1). In 4 patients with aseptic meningitis, EV75 was isolated from CSF. EV75 was isolated from CSF of a fifth patient who had symptoms of fever and irritability. The remaining 3 EV75 isolates were from nasopharyngeal swabs of children who had fever, respiratory disease, or gastroenteritis. All isolates were grown in cell lines (rhabdomyosarcoma, lung adenocarcinoma, and human fetal lung fibroblast) and identified as EV by immunofluorescence with pan-EV antibody assays (Pan Entero Blend Chemicon, Temecula, CA, USA, and Monoclonal Mouse Anti-Enterovirus, Dako, Glostrup, Denmark). Phylogenetic analysis of the isolates from 2005 was performed on the basis of complete VP1 gene sequence (GenBank accession nos. DQ468137–DQ468142). The 5´ terminal domain was obtained by reverse transcriptase–PCR with specific primers EV75_sense: 5´-GAAAGCTTYTTCCAAGGGGA-3´ and EV75_anti: 5´-GAGAAGTGKGACCAWCCATC-3´. Phylogenetic analysis of the Spanish isolates and representatives of all other species B EVs showed that the Spanish isolates clustered (bootstrap value 100, Figure) with strains USA/OK85-10362, ETH74-1341, USA/VA86-10363, USA/CT87-10364-5, OMA98-10366, and BAN00-10367-8 (accession nos. AY556063–AY556070), corresponding to the proposed EV75. The Spanish isolates constitute a subgroup (bootstrap value 100, Figure). The similarity between the Spanish cluster and other EV75 isolates was 82.8%–85.4% at the nucleic acid level. Although the entire VP1 sequence was not available for the isolates from 2006, the VP1 3´ terminal analysis showed the strains belonged to the same cluster. Figure Phylogenetic analysis of complete VP1 sequences of Spanish enterovirus (EV) isolates (GenBank accession nos. DQ468137–DQ468142), the new proposed EV75 sequences (AY556063–AY556070 and AY919545), and prototype EV sequences (echovirus [E] 5, AJ241425; E31, AJ241435; E2, AF081315; E15, AJ241429; E14, AJ241428; E17, AF081330; coxsackie B virus [CBV] 2, AF081312; E26, AJ241433; E27, AF081338; E1, AJ241422; E8, AF081325; E4, AF081319; E21, AF081334; E30, AF081340; E25, AF081336; E29, AJ241434; CBV5, AF114383; CBV6, AF081313; E13, AF081327; EV69, AF081349; E24, AJ241432; E33, AF081346; E3, AF081316; E12, X77708; CBV3, M16572; CBV1, M16560; E6, AF081322; coxsackie A virus [CAV] 9, D00627; E16, AY302542; E9, AF524866; E7, AJ241426; E32, AF081345; E19, AJ241430; E11, AF081326; CBV4, X05690; E18, AF081331; E20, AJ241431; EV70, D17602; CAV6, AF081297; CAV13, AF081303; EV74, AY208118). Phylogenetic trees were constructed with the neighbor-joining method (MEGA version 3.0, available from http://www.megasoftware.net) with Kimura 2-parameter substitution model. Significance of phylogenies was estimated by bootstrap analysis with 1,000 pseudoreplicate datasets. Closed and open circles show Spanish and previously reported EV75 isolates, respectively. To our knowledge, this is the first isolation of EV75 in Spain. Indeed, isolation of EV75 has not been reported in Europe. Given that the European EV75 isolate grows easily in a variety of cell lines, is detected by common EV genus-specific antibodies, and that EV surveillance and typing were performed in Spain since 1988 ( 2 ), EV75 might have begun to circulate in Spain recently. However, because isolates are not obtained from all aseptic meningitis patients and many EVs are detected by PCR but never typed, we cannot rule out the possibility of previous asymptomatic circulation. The European strains of EV75 appear to represent a different evolutionary lineage than those previously described in the United States, Asia, and Africa ( 9 ). Only 1 of those EV75s was obtained from CSF (a nonspecific neurologic syndrome). Thus, EV75 has not been associated with aseptic meningitis, despite the fact that EV infections are a common cause of aseptic meningitis. Most of the Spanish isolates (5 of 8) were associated with aseptic meningitis in children. Although the number of EV75-associated cases was not high (as a percentage of the number of EVs isolated from aseptic meningitis patients, 10.8%), the wide distribution of the cases may indicate wide circulation. To avoid outbreaks of aseptic meningitis caused by previously noncirculating EVs (EV13, 2001 [10]) and to help define the extent of circulation of newly identified EV types, careful surveillance of aseptic meningitis should be undertaken.

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          Most cited references9

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          Enteroviruses 76, 89, 90 and 91 represent a novel group within the species Human enterovirus A.

          Molecular methods have enabled the rapid identification of new enterovirus (EV) serotypes that would have been untypable using existing neutralizing antisera. Nineteen strains of four new EV types termed EV76 (11 isolates), EV89 (two isolates), EV90 (four isolates) and EV91 (two isolates), isolated from clinical specimens from patients in France (one isolate) and Bangladesh (18 isolates), are described. Nucleotide sequences encoding the VP1 capsid protein (882-888 nt) are less than 65 % identical to the homologous sequences of the recognized human EV serotypes, but within each group the sequences are more than 78 % identical. The deduced amino acid sequences of the complete capsid (P1) region are more than 94 % identical within type but less than 76 % identical to those of the recognized serotypes. For both VP1 and P1, the 19 isolates are monophyletic by type with respect to all other EV serotypes. Using the proposed molecular typing scheme, these data support their identification as four new types within the species Human enterovirus A (HEV-A). In almost all cases, the VP1 sequences were more similar to those of some simian EVs than to the human EVs. Partial 3D sequences of all 19 isolates also clustered within HEV-A; they were monophyletic as a group, but not by type, suggesting that recombination has occurred among viruses of these four types. Partial 3D sequences were more closely related to those of simian EVs than to human viruses in HEV-A. These results suggest that the four new types may represent a new subgroup within HEV-A, in addition to the existing human and simian subgroups.
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            Sequencing of 'untypable' enteroviruses reveals two new types, EV-77 and EV-78, within human enterovirus type B and substitutions in the BC loop of the VP1 protein for known types.

            The N-terminal part of VP1 was sequenced for 43 enterovirus isolates that could not initially be neutralized with LBM pools or in-house antisera. Most isolates were found to belong to human enterovirus type A (HEV-A) and HEV-B (18 isolates of each). All HEV-A isolates could be typed by sequencing, with CV (coxsackievirus)-A16 and EV (enterovirus)-71 being dominant (nine and seven isolates, respectively). These types thus seem to have diverged more from their prototypes than the other types. Among the HEV-B isolates, E-18 dominated with five isolates that became typable after filtration. The virus type obtained by molecular typing was verified for 28 of the other patient isolates by neutralization using high-titre monovalent antisera or LBM pools. Twenty-two of the other 30 'untypable' isolates had substitutions in the VP1 protein within or close to the BC loop. Two closely related HEV-B isolates diverged by 19.4 % from E-15, the most similar prototype. Two non-neutralizable HEV-C isolates split off from the CV-A13/CV-A18 branch, from which they diverged by 15.7-18.2 %. Three of the six non-neutralizable isolates, W553-130/99, W543-122/99 and W137-126/99, diverged by >24.2 % from the most similar prototype in the compared region. The complete VP1 was therefore sequenced and found to diverge by >29 % from all prototypes and by >28 % from each other. Strains similar to W553-130/99 that have been identified in the USA are tentatively designated EV-74. The two other isolates fulfil the molecular criterion for being new types. Since strains designated EV-75 and EV-76 have been identified in the USA, we have proposed the tentative designations EV-77 and EV-78 for these two new members of HEV-B.
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              • Record: found
              • Abstract: found
              • Article: not found

              Molecular identification and characterization of two proposed new enterovirus serotypes, EV74 and EV75.

              Sequencing of the gene that encodes the capsid protein VP1 has been used as a surrogate for antigenic typing in order to distinguish enterovirus serotypes; three new serotypes were identified recently by this method. In this study, 14 enterovirus isolates from six countries were characterized as members of two new types within the species Human enterovirus B, based on sequencing of the complete capsid-encoding (P1) region. Isolates within each of these two types differed significantly from one another and from all other known enterovirus serotypes on the basis of sequences that encode either VP1 alone or the entire P1 region. Members of each type were > or =77.2 % identical to one another (89.5 % amino acid identity) in VP1, but members of the two different types differed from one another and from other enteroviruses by > or =31 % in nucleotide sequence (25 % amino acid sequence difference), indicating that the two groups represent separate new candidate enterovirus types. The complete P1 sequences differed from those of all other enterovirus serotypes by > or =31 % (26 % amino acid sequence difference), but were highly conserved within a serotype (<8 % amino acid sequence difference). Phylogenetic analyses demonstrated that isolates of the same serotype were monophyletic in both VP1 and the capsid as a whole, as shown previously for other enterovirus serotypes. This paper proposes that these 14 isolates should be classified as members of two new human enterovirus types, enteroviruses 74 and 75 (EV74 and EV75).
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                Author and article information

                Journal
                Emerg Infect Dis
                EID
                Emerging Infectious Diseases
                Centers for Disease Control and Prevention
                1080-6040
                1080-6059
                October 2006
                : 12
                : 10
                : 1609-1611
                Affiliations
                [* ]Carlos III Institute of Health, Majadahonda, Spain;
                []Cruzes Hospital, Bilbao, Spain;
                []Columbia University, New York, New York, USA;
                [§ ]Sant Pau y Santa Creu Hospital, Barcelona, Spain;
                []Virgen de las Nieves Hospital, Granada, Spain;
                [# ]Doctor Negrín Hospital, Las Palmas de Gran Canaria, Spain
                Author notes
                Address for correspondence: Ana Avellón, Spanish Enterovirus Reference Laboratory, National Center of Microbiology, Carlos III Institute of Health, Carretera de Majadahonda a Pozuelo, Km 2, Majadahonda 28220, Madrid, Spain; email: aavellon@ 123456isciii.es
                Article
                06-0353
                10.3201/eid1210.060353
                3290945
                17176588
                32ee55cf-10c1-4ef6-8a36-7f52c11ec599
                History
                Categories
                Letters to the Editor

                Infectious disease & Microbiology
                aseptic meningitis,enterovirus,letter,ev75,enterovirus type 75
                Infectious disease & Microbiology
                aseptic meningitis, enterovirus, letter, ev75, enterovirus type 75

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