Streptococcus pneumoniae serotype 19A in children, South Korea.Despite the concern of replacement disease, notably by serotype serotype /se·ro·type/ (ser´o-tip) the type of a microorganism determined by its constituent antigens; a taxonomic subdivision based thereon. se·ro·type n. See serovar. v. 19A after 7-valent conjugate vaccine A conjugate vaccine is created by covalently attaching a poor antigen to a carrier protein, thereby conferring the immunological attributes of the carrier on the attached antigen. (PCV PCV packed-cell volume. PCV packed-cell volume, the volume of packed red cells in milliliters per 100 ml of blood. 7) use, serotype 19A was increasingly recognized in Korean children before the introduction of PCV7. To understand the dynamics of serogroup 19 prevalence from 1991-2006, we serotyped 538 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. pneumococcal pneumococcal /pneu·mo·coc·cal/ (-kok´al) pertaining to or caused by pneumococci. isolates. Serogroup 19 isolates (n = 126) were characterized by antimicrobial drug susceptibility, presence of mefA/ermB, and multilocus sequence typing Multilocus sequence typing (MLST) is a technique in molecular biology for the typing of multiple loci. The procedure characterizes isolates of bacterial species using the DNA sequences of internal fragments of multiple (usually seven) housekeeping genes. . Overall, the proportion of serotype 19A isolates increased but serotype 19F decreased. Among children <5 years of age, the proportion of serotype 19A isolates in invasive pneumococcal disease increased from 0% in 1991-1994 to 8%-10% in 1995-2000, reached 26% in 2001-2003, and remained at 20% in 2004-2006 when vaccine coverage did not exceed 25% (p = 0.005 for trend). This study demonstrates that the expansion of multidrug-resistant ST320 was responsible for the increase in serotype 19A before PCV7 use. ********** Streptococcus pneumoniae Streptococcus pneu·mo·ni·ae n. Pneumococcus. Streptococcus pneumoniae Microbiology A pathogenic streptococcus with 90 serotypes associated with pneumonia, bacteremia, meningitis Transmission Person to person Incidence is a major cause of invasive infections in young infants and children. Among >90 serotypes, only a limited number account for pneumococcal diseases. Serotype incidence can vary by patient age, geographic region, and time of surveillance. Since the introduction of 7-valent conjugate vaccine (PCV7) in the United States United States, officially United States of America, republic (2005 est. pop. 295,734,000), 3,539,227 sq mi (9,166,598 sq km), North America. The United States is the world's third largest country in population and the fourth largest country in area. , a decrease in the incidence of invasive pneumococcal disease (IPD IPD Institut für Programmstrukturen und Datenorganisation IPD Investment Property Databank (UK) IPD Integrated Product Development IPD Intellectual Property Department IPD Invasive Pneumococcal Disease IPD Implicit Price Deflator ) caused by vaccine serotypes has been observed in pediatric and nonpediatric age groups (1,2). However, the incidence of IPD caused by nonvaccine serotypes (including serotype 19A) increased 1.5-fold in 2002 compared to that in 1999 (2,3). To date, replacement for IPD has been observed for serotypes 3, 15, 19A, 22F, 33F, and 35, with the increase in 19A being the most prevalent. (2-7). Recently, Singleton et al. reported that serotype 19A was responsible for 28.3% of IPD in rural Alaska Native children <2 years of age during 2004-2006 (8). In addition, recent studies from Massachusetts and Texas showed that a multidrug-resistant sequence type of serotype 19A has emerged as an important cause of IPD (9,10). The direct effects of PCV7 in serotype distribution changes and genetic structures of pneumococcal isolates are not clear. However, capsular cap·su·lar adj. Of, relating to, or resembling a capsule. Adj. 1. capsular - resembling a capsule; "the capsular ligament is a sac surrounding the articular cavity of a freely movable joint and attached to the bones" switching of vaccine serotypes under selective pressure by PCV7 is one of the mechanisms underlying the expansion of serotype 19A (4,11-13). As part of this surveillance implemented in a tertiary referral center in South Korea, all pneumococcal isolates obtained from sterile body fluids and from various clinical specimens were subjected to serotype and antimicrobial drug susceptibility pattern determinations (14). Surveillance since 1991 shows that serotype 19A isolates were increasingly recognized among clinical isolates before PCV7 was introduced in South Korea in November 2003. We describe S. pneumoniae serotype distribution changes in Korean children during 1991-2006 with an emphasis on serogroup 19. Methods Patients and Pneumococcal Isolates Hospital-wide surveillance was continued to monitor pneumococcal diseases as a part of routine clinical care at Seoul National University Not to be confused with the University of Seoul. Seoul National University (SNU) is a national research university in Seoul, South Korea. Founded in 1946, SNU was the first national university in South Korea, and served as a model for the many national and public Children's Hospital from 1991 through 2006. Only initial isolates were included in the study; repeated isolates from the same patient were excluded. Isolates were classified as invasive (e.g., blood, pleural fluid pleural fluid n. The thin film of serous fluid between the visceral and parietal pleurae. , cerebrospinal fluid cerebrospinal fluid (CSF) Clear, colourless liquid that surrounds the brain and spinal cord and fills the spaces in them. It helps support the brain, acts as a lubricant, maintains pressure in the skull, and cushions shocks. , joint fluid) and noninvasive (pharynx pharynx (fâr`ĭngks), area of the gastrointestinal and respiratory tracts which lies between the mouth and the esophagus. In humans, the pharynx is a cone-shaped tube about 4 1-2 in. (11.43 cm) long. , middle ear fluid, sputum sputum /spu·tum/ (spu´tum) [L.] expectoration; matter ejected from the trachea, bronchi, and lungs through the mouth. sputum cruen´tum bloody sputum. ). Methods of surveillance and of obtaining blood cultures did not change during the study period. Analysis of Serotype Distributions and Classifications All isolates were serotyped by the Quellung reaction quel·lung reaction n. See Neufeld capsular swelling. using antiserum antiserum /an·ti·se·rum/ (an´ti-se?rum) a serum containing antibody(ies), obtained from an animal immunized either by injection of antigen or by infection with microorganisms containing antigen. (Statens Serum Institute, Copenhagen, Denmark). The study period was divided into five 3- or 4-year-periods: 1991-1994 (period 1), 1995-1997 (period 2), 1998-2000 (period 3), 2001-2003 (period 4), and 2004-2006 (period 5). The PCV7 serotypes were 4, 6B, 9V, 14, 18C, 19F, and 23F. Serotypes considered to be PCV7 related included those not directly targeted by PCV7 but of the same serogroups (6A, 9A, 9N, 18B, 18F, and 23A); serotype 19A was analyzed separately. Non-PCV7 serotypes included all other serotypes. Multilocus Squence Typing Analysis Multilocus sequence typing (MLST MLST Multi Locus Sequence Typing MLST Medical Logistics Support Team MLST Mini Losi Super Truck (1/18th scale radio control vehicle) ) was performed on all serotype 19A isolates (n = 58) and serotype 19F isolates (n = 68) obtained from children <5 years of age (15-17). New alleles were verified by resequencing gene fragments of both strands. When sequence types (STs) that had not been associated with a particular serotype in the past were identified, serotyping and sequencing typing were confirmed by repeating the reactions. STs were divided into sets using eBURST software (Imperial College, London, UK) (18), which is available at the MLST database. eBURST sets meet the requirement that all STs must be single-locus variants (SLVs) of at least 1 other ST within the group. Founder STs were defined as described previously (18). Clonal complexes (CCs) consisted of eBURST sets or eBURST sets plus related STs that shared 5 of 7 allelic al·lele n. One member of a pair or series of genes that occupy a specific position on a specific chromosome. [German Allel, short for Allelomorph, allelomorph, from English identities with most other STs included within an eBURST set. Antimicrobial Drug Susceptibility Testing and Detection of ermB/mefA Genes MICs of serogroup 19 were determined for 6 antimicrobial drugs (penicillin, cefotaxime, chloramphenicol chloramphenicol (klōr'ămfĕn`əkŏl'), antibiotic effective against a wide range of gram-negative and gram-positive bacteria (see Gram's stain). It was originally isolated from a species of Streptomyces bacteria. , tetracycline tetracycline (tĕ'trəsī`klēn), any of a group of antibiotics produced by bacteria of the genus Streptomyces. They are effective against a wide range of Gram positive and Gram negative bacteria, interfering with protein , clindamycin, and erythromycin erythromycin (ĭrĭth'rōmī`sĭn), any of several related antibiotic drugs produced by bacteria of the genus Streptomyces (see antibiotic). ) by E-test (AB Biodisk, Solna, Sweden) (19). Susceptibilities to vancomycin vancomycin (văn'kōmī`sĭn), antibiotic resembling penicillin in the way it acts. It is derived from the bacterium Streptomyces orientalis, which was isolated from soil of India and Indonesia. and trimethoprim-sulfamethoxazole were determined by disk diffusion test. Multidrug resistance multidrug resistance, n the adaptation of tumor cells or infectious agents to resist chemotherapeutic agents. was defined as nonsusceptibility to [greater than or equal to] 3 antimicrobial drug classes. The mefA and ermB genes were detected by PCR PCR polymerase chain reaction. PCR abbr. polymerase chain reaction Polymerase chain reaction (PCR) using the primers mefA (forward, 5'-AGT ATC ATC Air Traffic Control ATC Average Total Cost ATC Certified Athletic Trainer ATC At the Center (Hartford, Maine retreat center) ATC Applied Technology Council ATC All Things Considered ATT ATT ammonia tolerance test. AAT Alpha-1-antitrypsin (AAT) A blood component that breaks down infection-fighting enzymes such as elastase. Mentioned in: Chronic Obstructive Lung Disease CAC See Consumer Advisory Council. TAG TGC TGC The Golf Channel TGC The Game Creators (forum) TGC Trading Card Game TGC Time-Gain Compensation TGC The Gungan Council TGC The Golden Compass (Phillip Pullman book) TGC Take Good Care 3'; reverse, 5'-TTC TTC TTC Trying To Conceive TTC Toronto Transit Commission TTC Trans Texas Corridor TTC Toutes Taxes Comprises (French) TTC Trident Technical College (North Charleston, SC) TTC Temporary Traffic Control TGG TGG The Great Gatsby (novel F. Scott Fitzgerald; movie) TGG Kuala Terengganu, Malaysia - Sultan Mahmood (Airport Code) TGG Temporary Geographic Grid TGG Third Generation Gyro TGG Triple Graph Grammar TAC 1. TAC - Translator Assembler-Compiler. For Philco 2000. 2. TAC - Terminal Access Controller. TAA TAA - Track Average Amplitude AAG AAG Association of American Geographers (Washington, DC) AAG Assistant Attorney General AAG Asociación Argentina de Golf AAG Anti-Aircraft Gun AAG Assistant Adjutant General AAG Australian Association of Gerontology TGG-3') and ermB (forward, 5'-GAA AAG GTA GTA Grand Theft Auto (legal) GTA Grand Theft Auto (video game) GTA Greater Toronto Area (Canada) GTA Graduate Teaching Assistant CTC CTC - Cornell Theory Center AAC (Advanced Audio Coding) An audio compression technology that is part of the MPEG-2 and MPEG-4 standards. AAC, especially MPEG-4 AAC, provides greater compression and better sound quality than MP3, which also came out of the MPEG standard. CAA Caa See CCC. ATA-3'; reverse, 5'-GTA ACG ACG American College of Gastroenterology; angiocardiography; apexcardiogram. AcG accelerator globulin (coagulation factor V). AcG accelerator globulin (clotting factor V). GTA CTT CTT Correios (Portuguese Postal Service) CTT Certified Technical Trainer CTT Charity Technology Trust CTT Cholesterol Treatment Trialists' (collaboration) CTT Common Task Training AAA AAA: see American Automobile Association. (Triple A) A common single-cell battery used in a myriad of electronic devices of all variety. Like its double A (AA) cousin, it provides 1.5 volts of DC power. When used in series, the voltage is multiplied. TTG tTG Tissue Transglutaminase TTG Telltale Games (website) TTG TiVo To Go TTG Time-To-Go TTG Tonalite-Trondhjemite-Granodiorite TTG Tea Tree Gully (South Australia) TTG Tom Tom Go TTT "Thought that too." See digispeak. AC-3') (20). PCRs were performed with 35 amplification cycles: 30 s at 94[degrees]C, 30 s at 50[degrees]C, and 1 min 30 s at 72[degrees]C, followed by a final extension at 72[degrees]C for 10 min. Statistical Analysis Statistical analysis was performed by using SPSS A statistical package from SPSS, Inc., Chicago (www.spss.com) that runs on PCs, most mainframes and minis and is used extensively in marketing research. It provides over 50 statistical processes, including regression analysis, correlation and analysis of variance. software version 13.0 (SPSS, Chicago, IL, USA). Serotype proportion in each period was compared using the [chi square chi square (kī), n a nonparametric statistic used with discrete data in the form of frequency count (nominal data) or percentages or proportions that can be reduced to frequencies. ] or Fisher exact test, as appropriate. The Mantel-Haenszel [chi square] test was used for trend analysis. Results Changes in Serotype Distributions From 1991 through 2006, 538 strains of S. pneumoniae were obtained from various clinical specimens. Of these, 158 (29%) were from invasive isolates; 124 blood, 15 cerebrospinal fluid, 6 pleural fluid, 5 ascites Ascites Definition Ascites is an abnormal accumulation of fluid in the abdomen. Description Rapidly developing (acute) ascites can occur as a complication of trauma, perforated ulcer, appendicitis, or inflammation of the colon or other , and 8 other sterile deep-seated tissues (e.g., bone and joint fluid). The remaining 380 (71%) were from noninvasive isolates; 110 (pharyngeal pharyngeal /pha·ryn·ge·al/ (fah-rin´je-al) pertaining to the pharynx. pha·ryn·geal or pha·ryn·gal adj. Of, relating to, located in, or coming from the pharynx. swab), 91 (transtracheal aspirate as·pi·rate v. To take in or remove by aspiration. n. A substance removed by aspiration. Aspirate The removal by suction of a fluid from a body cavity using a needle. ), 81 (sputum), 69 (middle ear fluid), 15 (urine), and 14 (open pus pus, thick white or yellowish fluid that forms in areas of infection such as wounds and abscesses. It is constituted of decomposed body tissue, bacteria (or other micro-organisms that cause the infection), and certain white blood cells. ). The most common serotypes were 19F (113, 21%), 23F (96, 17.8%), 19A (58, 10.8%), 6B (50, 9.3%), 6A (43, 8%), 14 (40, 7.4%), and 9V (24, 4.5%); these 7 serotypes accounted for 79% of the total isolates. Overall, PCV7 serotypes accounted for 64.1% of total isolates and 62.7% of invasive isolates. Table 1 shows the serotype distributions of invasive and noninvasive isolates by age group. For invasive isolates, PCV7 serotype coverage was 67% among children <60 months of age and 47% among children [greater than or equal to] 60 months (Table 1). During 2001-2003, just before PCV7 was introduced in South Korea, overall PCV7 coverage rates for PCV7 serotypes and PCV7-related serotypes were 54% and 10% among the 138 invasive isolates and 57% and 13% among the 380 noninvasive isolates. The proportion of serotype 19A isolates increased from 0% (0/40) during 1991-1994 to 18% (7/39) during 2001-2003 among the 138 invasive isolates. Similarly, from 1995-1997 to 1998-2000, the proportion of serotype 19A isolates increased from 3% (1/33) to 17% (14/81) among noninvasive isolates (Figure 1). Among the 107 invasive isolates from children <5 years of age (Figure 2), serotype 19F decreased from 31% (8/26) in period 1 to 13% (3/24) in period 2 and to 5% (1/20) in periods 3 and 4 (p = 0.008 for trend). The proportion of 19A increased from 0% (0/26) in period 1 to 8% (2/24) in period 2 and reached 26% (7/27) in period 4 (p = 0.005 for trend). There were no significant trends for the remaining serotypes: 23F (p = 0.58), 14 (p = 0.28), 9V (p = 0.23), 6A (p = 0.38), and 6B (p = 0.23). During period 5, after vaccine introduction, the proportion of 19A isolates was 20% (2/10). During 2001-2003, 19A was the most common serotype among IPD isolates from South Korean children <5 years of age. During 2004-2006, the postvaccine period, when PCV7 uptake reached [approximately equal to] 20%-25% of South Korean children <2 years of age (21), the distribution of serotypes was unaltered compared with distribution during the prevaccine 2001-2003 period. There was no major change in antimicrobial drug treatment policy or pressure to use antimicrobial drugs in the local pediatric practice during the study period. MLST Analysis of Serogroup 19 MLST analysis showed 4 STs among the 58 serotype 19A isolates: ST320 (52 isolates), ST 1374 (4), ST1451 (1), and ST2394 (1). Eighteen STs were found among the 68 serotype 19F isolates: ST271 (14 isolates), ST320 (6), ST236 (14), ST283 (7), ST1464 (10), ST2395 (3), ST2695 (3), and 1 isolate each of ST1203, ST1412, ST1417, ST2396, ST2397, ST2398, ST2399, ST2694, ST2696, ST2697, and ST2698. Through the course of this study, 11 new STs (ST2394-ST2399 and ST2694-ST2698) were identified among the serogroup 19 isolates, and 8 of these were SLVs or double-locus variants of ST271. According to eBURST analysis, 1 major CC (CC271) accounted for most of the isolates (n = 116, 92% of serotypes 19A and 19F). CC271 comprised 16 SYs, where ST271 was predicted as the founder, and ST320 was the predominant allelic profile. The 5 ST lineages that were unrelated to CC271 were nonlinked singlets (ST1203, ST1374, ST2394, ST2395, and ST2399) (Figure 3). ST320 was the only ST found among serotypes 19A and 19F; ST320 was the most common ST (n = 52, 90% of total 19A isolates) among serotype 19A. ST320 was observed in only 9% (n = 6) of serotype 19F isolates. The genetic structure of serotype 19A comprised primarily ST1374 during periods 1 and 2 (1991-1997), but ST1374 isolates were not recovered after 2001. In contrast, ST320 was the most common sequence type from 1998, and all 19A isolates from 2002-2006 were of ST320. The numbers of 19A isolates increased consistently from 1996 through 2003, which suggests that single clonal expansion of ST320 was responsible for the increase of serotype 19A isolates during this period (Figure 4). Unlike serotype 19A, serotype 19F comprises diverse STs grouped within CC271 (16 STs) and 5 different singlets. All STs, except ST1203, were associated with multidrug-resistant mef/erm-containing isolates. The distributions of predominant STs among serotype 19F isolates varied during each study period (Figure 4). For example, ST2395 predominated in period 1 (1991-1994), but ST1464 (an SLV SLV abbr. standard launch vehicle of ST271) predominated in periods 4 and 5 (2001-2006). Association of ST with Antimicrobial Drug Susceptibility and mef/erm Prevalence Antimicrobial drug susceptibilities were tested for 126 of 171 serogroup 19 isolates. Degrees of resistance to penicillin and cefotaxime differed among isolates containing different STs. In addition, a distinct correlation was found between mef/erm prevalence and STs (Table 2). All CC271 isolates (n = 116, 16 different STs) were not susceptible to penicillin and cefotaxime and showed multidrug resistance to [greater than or equal to] 3 antimicrobial drug classes. Erythromycin MICs of CC271 isolates were [greater than or equal to] 256 [micro]g/mL and were all positive for mef and erm. However, 5 singlets that were unrelated to CC271 showed different patterns of antimicrobial drug susceptibility and presence of mef/erm determinants (Table 2). Four serotype 19A isolates representing ST1374 appeared to be less resistant to 2 [beta]-1actam antimicrobial drugs than CC271 isolates. ST 1374 strains were also highly resistant to erythromycin (MIC [greater than or equal to] 256 [micro]g/mL) and were positive for ermB only. Strains of ST2394, ST2395, and ST2399 showed a lower degree of erythromycin resistance (MIC = 2-8 [micro]g/mL) than CC271 and ST1374 and contained mefA only. One serotype, 19F strain of ST1203, did not express mef or erm. Serotypes 19A and 19F strains with CC271 were shown to be closely related to the internationally established clone, [Taiwan.sup.19F]-14, which is multidrug resistant and carries mefA/ermB macrolide-resistance determinants defined by the pneumococcal molecular epidemiology molecular epidemiology Molecular medicine An evolving field that combines the tools of standard epidemiology–case studies, questionnaires and monitoring of exposure to external factors with the tools of molecular biology–eg, restriction endonucleases, network (22). [FIGURE 1 OMITTED] [FIGURE 2 OMITTED] Discussion We found that before PCV7 introduction in South Korea, the proportion of serotype 19A isolates increased from 0% in 1991 to 26% in 2003 but 19F isolates decreased during the same period. Our study also demonstrated that multidrug-resistant ST320 isolates containing mef/erm determinants were responsible for the expansion of serotype 19A. In the United States, serotype 19A is now the most important cause of IPD by replacement serotypes (4,8,23,24). Contrary to what we report for South Korea, the increase in the United States was documented after widespread use of PCV7 (4-6). Increase in non-PCV7 serotypes, i.e., serotype replacement, has been noted in carriage studies and the pre-licensure clinical trials (11,25,26). After widespread use of PCV7 in young children, replacement of serotypes for IPD has been described for several serotypes in previous studies (4-6). Of these, an increase in the incidence of IPD cases caused by serotype 19A was quite high. Therefore, the increasing prevalence of IPDs caused by serotype 19A among the vaccine target group is of considerable concern. Our findings of an increase in serotype 19A disease before conjugate vaccine introduction calls into question the role vaccine may play in the emergence of serotype 19A disease and suggests that other factors are important. Of the factors contributing to the increase in serotype 19A, the MLST findings in our study point to a homogeneous pattern of ST320. ST320 of serotype 19A might have originated from ST271 or ST236 strains that have been prevalent among serotype 19F since 1993 (20) or could have been introduced from other countries. Thus, single clonal expansion of ST320, related to a multidrug-resistant internationally prevalent clone, [Taiwan.sup.19F]-14 (that also carries mefA/ermB determinants), was most likely responsible for the prevaccine increase observed for serotype 19A. Antimicrobial drug use may provide selective pressure that would give this highly resistant strain an advantage over other strains. A study in the United States demonstrated an increasing prevalence of mefA/ermB; 17% percent of 221 children had been colonized Colonized This occurs when a microorganism is found on or in a person without causing a disease. Mentioned in: Isolation by mefA/ermB containing serogroup 19 pneumococci strains after receiving at least 1 dose of PCV7; the major clonal type was related to [Taiwan.sup.19F]-14 (27). In Alaska, the increase observed in 19A colonization and IPD seems to be related to CC172 clonal expansion (8). In contrast, recent genetic analysis of 19A strains isolated after PCV7 use in the United States showed that diverse mechanisms were involved in the expansion of 19A strains, expansion of preexisting pre·ex·ist or pre-ex·ist v. pre·ex·ist·ed, pre·ex·ist·ing, pre·ex·ists v.tr. To exist before (something); precede: Dinosaurs preexisted humans. v.intr. predominant CC 199, capsular switching of PCV7 types (4, 6, 14, and 9V), and appearance of multiple unrelated multidrug-resistant CCs among serotype 19A strains (CC271, including ST1451 and ST320, CC156, and CC1296) (4). Capsular switching of PCV7 serotypes under selective pressure by vaccine use is one of the mechanisms underlying the expansion of serotype 19A (4,11-13,28). However, there is no evidence of capsular switching as a contributing factor to the increase in serotype 19A in our study. [FIGURE 3 OMITTED] We also found that serotype 19F gradually decreased in proportion and diversified to include several newer descendants that differ from the founder by only 1 or 2 of 7 alleles but ST320 was not a major genetic structure among serotype 19F strains (18). Thus, it appears that ST320 has a selective advantage in serotype 19A strains, whereas ST320 did not seem to have expansion merit in the close serotype 19F strains. This finding suggests that the properties of particular clonal or capsular types are likely important determining factors of the potential of pneumococci to influence disease type and severity (29,30). Further studies are necessary to explain why certain sequence types exhibit different selective pressures according to serotype, even for close serotypes such as 19A and 19F. This study has several limitations. First, pneumococcal isolates were collected at a single center, and thus, may not represent the national situation. However, no surveillance system has been established for IPD in South Korea. Nevertheless, at least 2 studies have demonstrated a recent increase in serotype 19A isolates among children in daycare centers (3% in 2002 and 11% in 2004) (14,31). In addition, the number of serotype 19A isolates from children and adults at another tertiary South Korean hospital showed an increase over the same period (32). Second, the number of 19A isolates was relatively small, and it is possible that uncommon strains possessing minor clones were not detected. Thus, our finding of a clonal expansion of ST320 among serotype 19A strains may be an overstatement o·ver·state tr.v. o·ver·stat·ed, o·ver·stat·ing, o·ver·states To state in exaggerated terms. See Synonyms at exaggerate. o . However, MLST analysis showed that all 7 of the 19A strains from colonized children who were identified from a previous study (14) were of ST320 (H.J. Lee, unpub. data). The present study has implications for future pneumococcal immunization programs In the 1950s, medical breakthroughs resulted in new vaccines to combat such diseases as polio and measles. States responded by requiring mandatory immunization for schoolchildren. One result was the near eradication of diseases that had previously been crippling or fatal. . In particular, the demonstration of an increase in 19A before the use of PCV7 suggests that PCV7 vaccination may not be entirely responsible for the observed increase of serotype 19A. Had the vaccine been introduced in 2000, as in the United States, the increase of serotype 19A would have been attributed to serotype replacement after PCV7 introduction. Nevertheless, whether minor multidrug-resistant clones of serotype 19A (appearing after the introduction of PCV7 in the United States) possess an advantage to increase with time is a concern (23,29). We demonstrated that multidrug-resistant ST320 strains among serotype 19A have selective advantage in terms of expansion over ST 1374, which were less resistant to [beta]-1actams in a country where antimicrobial drug therapy is frequently used. Reports on PCV7 efficacy indicate negligible cross-protection for serotype 19A (11). In addition, a recent increase in the antimicrobial drug resistance of invasive 19A isolates and the increase in colonization by serogroup 19 strains carrying mef/erm determinants raise the possibility of potential increases in the prevalence of this clone. Thus, potential for colonization because of widespread antimicrobial drug use and resistance may interact and provide the selective advantage necessary for serotype expansion, which may be the situation in South Korea. Similarly, the influence of population characteristic dynamics, i.e., HIV HIV (Human Immunodeficiency Virus), either of two closely related retroviruses that invade T-helper lymphocytes and are responsible for AIDS. There are two types of HIV: HIV-1 and HIV-2. HIV-1 is responsible for the vast majority of AIDS in the United States. infection or poverty and overcrowding overcrowding overcrowding of animal accommodation. Many countries now publish codes of practice which define what the appropriate volumetric allowances should be for each species of animal when they are housed indoors. Breaches of these codes is overcrowding. , as well as PCV7 introduction, may combine with the necessary factor for serotype replacement and play an important role in serotype expansion, which may be the situation in Alaska. It is too early to determine the effect of PCV7 on expansion of serotype 19A in South Korea. PCV7 was introduced in South Korea in November 2003 when PCV7 serotype coverage was 56% among invasive isolates in children <5 years of age. In 2007, PCV7 coverage is [approximately equal to] 30% of the target group (21). At this time it is difficult to predict the effect of low vaccination coverage on serotype expansion/replacement. Therefore, surveillance is essential to monitor antimicrobial drug resistance, serotype expansion, and serotype replacement as early indications of an increase in pneumococcal disease by non-PCV7 or PCV7-related serotypes. [FIGURE 4 OMITTED] Acknowledgments We thank Sue Kyung Park for her critical comments on the statistical analysis. This study was supported in part by Seoul National University Hospital grant (no. 06-2006-203-0), which was underwritten by Wyeth Research. Dr Choi is a pediatric infectious diseases specialist at Seoul National University Bundang Hospital Seoul National University Bundang Hospital (분당 서울대병원) is located in Gumi-dong, Bundang, Seongnam, Gyeonggi-do, South Korea. It began its first treatment on 10 May 2003. in South Korea and an assistant professor at Seoul National University College of Medicine. Her research interests are pediatric respiratory infections and pneumococcal diseases. References (1.) Black S, Shinefield H, Baxter R, Austrian R, Bracken L, Hansen J, et al. Postlicensure surveillance for pneumococcal invasive disease after use of heptavalent Hep`tav´a`lent a. 1. (Chem.) Having seven units of attractive force or affinity; - said of heptad elements or radicals. pneumococcal conjugate vaccine Pneumococcal conjugate vaccine is a vaccine used to protect infants and young children against disease caused by the bacterium Streptococcus pneumoniae (pneumococcus). in Northern California Kaiser Permanente. Pediatr infect Dis J. 2004;23:485-9. (2.) Whitney CG, Farley MM, Hadler J, Harrison LH, Bennett NM, Lynfield R, et al. Decline in invasive pneumococcal disease after the introduction of protein-polysaccharide conjugate vaccine. N Engl J Med. 2003;348:1737-46. (3.) Kaplan SL, Mason EO, Wald ER, Schutze GE, Bradley JS, Tan TO, et al. Decrease of invasive pneumococcal infections in children among 8 children's hospitals in the United States after the introduction of the 7-valent pneumococcal conjugate vaccine. Pediatrics. 2004;113:443-9. (4.) Pai R, Moore MR, Pilishvili T, Gertz RE, Whitney CG, Beall B. Active Bacterial Core Surveillance Team. Postvaccine genetic structure of Streptococcus pneumoniae serotype 19A from children in the United States. J Infect Dis. 2005;192:1988-95. (5.) Schutze GE, Tucker NC, Mason EO. Impact of the conjugate conjugate /con·ju·gate/ (kon´jdbobr-gat) 1. paired, or equally coupled; working in unison. 2. a conjugate diameter of the pelvic inlet; used alone usually to denote the true conjugate diameter; see pneumococcal vaccine pneu·mo·coc·cal vaccine n. A vaccine containing purified capsular polysaccharide antigen from the most common infectious types of Streptococcus pneumoniae, used to immunize against pneumonococcal disease. in Arkansas. Pediatr Infect Dis J. 2004;23: 1125-9. (6.) Byington CL, Samore MH, Stoddard GJ, Barlow S, Daly J, Korgenski K, et al. Temporal trends of invasive disease due to Streptococcus pneumoniae among children in the intermountain west: emergence of nonvaccine serogroups. Clin Infect Dis. 2005;41:21-9. (7.) Albrich WC, Baughman W, Schmotzer B, Farley MM. Changing characteristics of invasive pneumococcal disease in metropolitan Atlanta, Georgia, after introduction of a 7-valent pneumococcal conjugate vaccine. Clin Infect Dis. 2007;44:1569-76. (8.) Singleton RJ, Hennessy TW, Bulkow LR, Hammitt LL, Zulz T, Hurlburt DA, et al. Invasive pneumococcal disease caused by nonvaccine serotypes among Alaska native children with high levels of 7-valent pneumococcal conjugate vaccine coverage. JAMA JAMA abbr. Journal of the American Medical Association . 2007;297: 1784-92. (9.) Pelton SI, Huot H, Finkelstein JA, Bishop CJ, Hsu KK, Kellenberg J, et al. Emergence of 19A as virulent and multidrug resistant pneumococcus pneumococcus Spheroidal bacterium (Streptococcus pneumoniae) that causes human diseases including pneumonia, sinusitis, ear infection, and meningitis. Usually occurring in the upper respiratory tract, this gram-positive (see in Massachusetts following universal immunization immunization: see immunity; vaccination. of infants with pneumococcal conjugate vaccine. Pediatr Infect Dis J. 2007;26:468-72. (10.) Messina AF, Katz-Gaynor K, Barton T, Ahmad N, Ghaffar F, Rasko D, et al. Impact of the pneumococcal conjugate vaccine on serotype distribution and antimicrobial resistance of invasive Streptococcus pneumoniae isolates in Dallas, TX, children from 1999 through 2005. Pediatr Infect Dis J. 2007;26:461-7. (11.) Eskola J, Kilpi T, Palmu A, Jokinen J, Haapakoski J, Herva E, et al. Efficacy of a pneumococcal conjugate vaccine against acute otitis media Acute otitis media Inflammation of the middle ear with signs of infection lasting less than three months. Mentioned in: Myringotomy and Ear Tubes acute otitis media . N Engl J Med. 2001;344:403-9. (12.) Huang SS, Platt R, Rifas-Shiman SL, Pelton SI, Goldmann D, Finkelstein JA. Post-PCV7 changes in colonizing pneumococcal serotypes in 16 Massachusetts communities, 2001 and 2004. Pediatrics. 2005;116:e408-13. (13.) Kilpi T, Ahman H, Jokinen J, Lankinen KS, Palmu A, Savolainen H, et al. Protective efficacy of a second pneumococcal conjugate vaccine against pneumococcal acute otitis media in infants and children: 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. , controlled trial controlled trial Clinical research A clinical study in which one group of participants receives an experimental drug while the other receives either a placebo or an approved–'gold standard' therapy. See Blinding, Double-blinded. of a 7-valent pneumococcal polysaccharide-meningococcal outer membrane protein complex conjugate vaccine in 1666 children. Clin Infect Dis. 2003;37:1155-64. (14.) Lee JA, Kim NH, Kim DH, Park KW, Kim YK, Kim KH, et al. Serotypes and penicillin susceptibility of Streptococcus pneumoniae isolated from clinical specimens and healthy carriers of Korean children. Korean Journal of Pediatrics. 2003;46:846-53. (15.) Enright MC, Spratt BG. A multilocus sequence typing scheme for Streptococcus pneumoniae: identification of clones associated with serious invasive disease. Microbiology. 1998;144:3049-60. (16.) Gertz RE, McEllistrem MC, Boxrud DJ, Li Z, Sakota V, Thompson TA, et al. Clonal distribution of invasive pneumococcal isolates from children and selected adults in the United States prior to 7-valent conjugate vaccine introduction. J Clin Microbiol. 2003;41: 4194-216. (17.) Multi Locus Sequence Typing Web Site. Streptococcus pneumoniae database [cited 12 Feb 2007]. Available from http//spneumoniae. mist.net (18.) Feil EJ, Li BC, Aanensen DM, Hanage WP, Spratt BG. eBURST: inferring patterns of evolutionary descent among clusters of related bacterial genotypes from multilocus sequence typing data. J. Bacteriol. 2004;186:1518-30. (19.) The National Committee for Clinical Standards. Performance standards for antimicrobial susceptibility testing. 8th information supplement, NCCLS NCCLS National Committee for Clinical Laboratory Standards document M100-S14. Wayne (PA): The Committee; 2004. (20.) Ko KS, Song JH. Evolution of erythromycin-resistant Streptococcus pneumoniae from Asian countries that contains erm(B) and mef(A) genes. J Infect Dis. 2004;190:739-47. (21.) Lee HJ, Choi EH, Kim MJ, Cheon BC. Change of etiologic agents in invasive infections among immunocompetent im·mu·no·com·pe·tent adj. Having the normal bodily capacity to develop an immune response following exposure to an antigen. im children from the multicentered study and distribution of serotype of Streptococcus pneumoniae during the period, 2003-2006. Seoul: Korea Center for Disease Control and Prevention Noun 1. Center for Disease Control and Prevention - a federal agency in the Department of Health and Human Services; located in Atlanta; investigates and diagnoses and tries to control or prevent diseases (especially new and unusual diseases) CDC ; 2006. (22.) McGee L, McDougal L, Zhou J, Spratt BG, Tenover FC, George R, et al. Nomenclature of major antimicrobial-resistant clones of Streptococcus pneumoniae defined by the pneumococcal molecular epidemiology network. J Clin Microbiol. 2001;39:2565-71. (23.) Kyaw MH, Lynfield R, Schaffner W, Craig AS, Hadler J, Reingold A, et al. Effect of introduction of the pneumococcal conjugate vaccine on drug-resistant Streptococcus pneumoniae. N Engl J Med. 2006;354:1455-63. (24.) Flannery B, Schrag S, Bennett NM, Lynfield R, Harrison LH, Reingold A, et al. Impact of childhood vaccination on racial disparities in invasive Streptococcus pneumoniae infections. JAMA. 2004;291:2197-203. (25.) McEllistrem MC, Pass M, Elliott JA, Whitney CG, Harrison LH. Clonal groups of penicillin-nonsusceptible Streptococcus pneumoniae in Baltimore, Maryland: a population-based, molecular epidemiologic study epidemiologic study A study that compares 2 groups of people who are alike except for one factor, such as exposure to a chemical or the presence of a health effect; the investigators try to determine if any factor is associated with the health effect . J Clin Microbiol. 2000;38:4367-72. (26.) Ghaffar F, Barton T, Lozano J, Muniz LS, Hicks P, Gan V, et al. Effect of the 7-valent pneumococcal conjugate vaccine on nasopharyngeal nasopharyngeal pertaining to the nasal and pharyngeal cavities. nasopharyngeal meatus see nasopharyngeal meatus. nasopharyngeal spasm see reverse sneeze. colonization by Streptococcus pneumoniae in the first 2 years of life. Clin Infect Dis. 2004;39:930-8. (27.) Toltzis P, Dul M, O'Riordan MA, Jacobs MR, Blumer J. Serogroup 19 pneumococci containing both reef and erm macrolide resistance determinants in an American city. Pediatr Infect Dis J. 2006;25: 19-24. (28.) Porat N, Arguedas A, Spratt BG, Trefler R, Brilla E, Loaiza C, et al. Emergence of penicillin-nonsusceptible Streptococcus pneumoniae clones expressing serotypes not present in the antipneumococcal conjugate vaccine. J Infect Dis. 2004;190:2154-61. (29.) Sandgren A, Sjostrom K, Olsson-Liljequist B, Christensson B, Samuelsson A, Kronvall G, et al. Effect of clonal and serotype-specific properties on the invasive capacity of Streptococcus pneumoniae. J Infect Dis. 2004;189:785-96. (30.) Hanage WP, Kaijalainen TH, Syrjanen RK, Auranen K, Leinonen M, Makela PH, et al. Invasiveness of serotypes and clones of Streptococcus pneumoniae among children in Finland. Infect Immun. 2005;73:431-5. (31.) Cho KY, Lee JA, Cho SE, Kim NH, Lee JA, Hong KS, et al. A study of serotyping of Streptococcus pneumoniae by multibead assay. Korean Journal of Pediatrics. 2007;50:151-6. (32.) Lee TJ, Chun JK, Choi KM, Yong DE, Lee KW, Kim DS. Trends in serotype distribution of clinical isolates of Streptococcus pneumoniae: a single center experience from 2001 to 2006. Korean Journal of Pediatric Infectious Diseases. 2006;13:115-23. Address for correspondence: Hoan Jong Lee, Seoul National University College of Medicine, 28 Yeongeon-dong, Jongno-gu, Seoul 110-744, South Korea; email: hoanlee@snu.ac.kr Eun Hwa Choi, * ([dagger]) So Hee Kim, * Byung Wook Eun, * Sun Jung Kim, ([dagger]) Nam Hee Kim, ([double dagger]) Jina Lee, ([section]) and Hoan Jong Lee * ([paragraph]) * Seoul National University College of Medicine, Seoul, South Korea; ([dagger]) Seoul National University Bundang Hospital, Seongnam, South Korea; ([double dagger]) Inje University College of Medicine, Goyang, South Korea; ([section]) Seoul National University Boramae Hospital, Seoul, South Korea; and ([paragraph]) Seoul National University Hospital, Seoul, South Korea
Table 1. Distributions of serotypes among 538 isolates from children in
South Korea, by age group, 1991-2006 *
No. (%) invasive isolates ([dagger])
[greater
than or
equal
Serotype <24 mo 24-59 mo to] 60 mo Total
PCV7 serotypes 44 (67) 28 (68) 24 (47) 96 (61)
19F 8 (12) 6 (15) 4 (8) 18 (11)
23F 16 (24) 6 (15) 4 (8) 26 (16)
6B 8 (12) 3 (7) 7 (14) 18 (11)
14 7 (11) 10 (24) 5 (10) 22 (14)
9V 4 (6) 3 (7) 3 (6) 10 (6)
4 0 (0) 0 (0) 0 (0) 0 (0)
18C 1 (2) 0 (0) 1 (2) 2 (1)
PCV7-related 3 (5) 6 (15) 7 (14) 16 (10)
serotypes
6A 3 (5) 5 (12) 6 (12) 14 (9)
23A 0 (0) 1 (2) 1 (2) 2 (1)
9N 0 (0) 0 (0) 0 (0) 0 (0)
19A 11 (16) 2 (5) 0 (0) 13 (8)
Non-PCV7 8 (12) 5 (12) 20 (39) 33 (21) ([double
serotypes dagger])
Total 66 (100) 41 (100) 51 (100) 158 (100)
No. (%) noninvasive isolates ([dagger])
[greater than or
Serotype <24 mo 24-59 mo equal to] 60 mo Total
PCV7 serotypes 113 (65) 81 (71) 42 (45) 236 (62)
19F 50 (29) 33 (29) 12 (13) 95 (25)
23F 32 (18) 20 (18) 18 (19) 70 (18)
6B 19 (18) 10 (9) 3 (3) 32 (8)
14 8 (5) 7 (6) 3 (3) 18 (5)
9V 4 (2) 8 (7) 2 (2) 14 (4)
4 0 (0) 2 (2) 4 (4) 6 (2)
18C 0 (0) 1 (1) 0 (0) 1 (0)
PCV7-related 15 (9) 14 (12) 9 (9) 38 (10)
serotypes
6A 12 (7) 10 (9) 7 (7) 29 (8)
23A 3 (2) 4 (4) 0 (0) 7 (2)
9N 0 (0) 0 (0) 2 (2) 2 (1)
19A 27 (16) 8 (7) 10 (11) 45 (12)
Non-PCV7 18 (11) 11 (10) 32 (35) 61 (16)
serotypes
Total 173 (100) 114 (100) 93 (100) 380 (100)
* PVC7, 7-valent conjugate vaccine.
([dagger]) Percentages have been rounded.
([double dagger]) Thirteen serogroups were included among 33 invasive
isolates as follows: 15 (6 strains), 24F (6), 10 (4), 34 (3), 35 (3),
1 (2), 3 (2), 12F (2), 5 (1), 11A (1), 13 (1), 20 (1), an d 27 (1).
Table 2. Antimicrobial susceptibility and mef and erm prevalence of
serogroup 19 pneumococcal isolates from children in South Korea,
1991-2006, according to sequence type
Multidrug
CC or ST * (no. strains) Serotypes resistance ([dagger])
CC271-related ([double 19A, 19F Yes
dagger]) (116)
ST1203 (1) 19F No
ST1374 (4) 19A Yes
ST2394 (1) 19A Yes
ST2395 (3) 19F Yes
ST2399 (1) 19F Yes
[MIC.sub.50] (range) in [micro]g/mL
for each antimicrobial drug
CC or ST * (no. strains) Penicillin Cefotaxime
CC271-related ([double 1.5 (1.0-3.0) 1.0 (0.75-4.0)
dagger]) (116)
ST1203 (1) 0.5 0.25
ST1374 (4) 0.06 (0.04-0.06) 0.12 (0.09-0.12)
ST2394 (1) 1.0 0.5
ST2395 (3) 4.0 (4.0) 2.0 (1.0-2.0)
ST2399 (1) 0.12 0.25
[MIC.sub.50] (range) in [micro]g/mL
for each antimicrobial drug
mef/erm,
CC or ST * (no. strains) Erythromycin determinants
CC271-related ([double [less than or equal to] 256 mef+, erm+
dagger]) (116) ([less than or equal to] 256)
ST1203 (1) 0.5 mef-, erm-
ST1374 (4) [less than or equal to] 256 mef-, erm+
([less than or equal to] 256)
ST2394 (1) 2.0 mef+, erm,
ST2395 (3) 2.0 (2.0) mef+, erm,
ST2399 (1) 8.0 mef+, erm,
* C, clonal complex; ST, sequence type.
([dagger]) resistant to at least 3 antimicrobial drug classes.
([double dagger]) CC271-related sequence types: ST320 (59 isolates),
ST271 (14), ST236 (14), ST283 (7), ST1451 (1), ST1464 (10), ST2395 (3),
ST2695 (3), and 1 isolate of each of ST1412, ST1417, ST2396, ST2397,
ST2398, ST2694, ST2696, ST2697, and ST2698.
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