Invasive group B streptococcal infections in Finland: a population-based study. (Research).We analyzed surveillance data on group B streptococcus group B streptococcus Streptococcus agalactiae A streptococcus classified into 7 capsular serotypes, which is the leading cause of sepsis and meningitis in neonates; GBS affects 1. (GBS See GB/sec. ) infection in Finland from 1995 to 2000 and reviewed neonatal cases of early-onset GBS infection in selected hospitals in 1999 to 2000. From 1995 to 2000, 853 cases were reported (annual incidence 2.2-3.0/100,000 population). We found 32-38 neonatal cases of early-onset GBS disease per year (annual incidence 0.6-0.7/1,000 live births). In five hospitals, 35% of 26 neonatal cases of early-onset GBS infection had at least one risk factor: prolonged rupture of membranes Rupture of membranes (ROM) is a term used during pregnancy to describe a rupture of the amniotic sac at the onset of, or during, labor. This is colloquially known as "breaking water". , preterm preterm /pre·term/ (-term´) before completion of the full term; said of pregnancy or of an infant. pre·term adj. delivery, or intrapartum fever. Five of eight mothers screened for GBS were colonized Colonized This occurs when a microorganism is found on or in a person without causing a disease. Mentioned in: Isolation . In one case, disease developed despite intrapartum chemoprophylaxis chemoprophylaxis /che·mo·pro·phy·lax·is/ (-pro?fi-lak´sis) prevention of disease by means of a chemotherapeutic agent. che·mo·pro·phy·lax·is n. Disease prevention by use of chemicals or drugs. . Although the incidence of early-onset. GBS disease in Finland is relatively low, some geographic variation exists, and current prevention practices are suboptimal Suboptimal A solution is called suboptimal if a part of the solution has been optimized without regards to the overall objective. . Establishing national guidelines to prevent perinatal GBS is likely to reduce the incidence of the disease. ********** Group B streptococcus (GBS), a leading cause of invasive bacterial infections in newborns, also affects pregnant women and elderly persons (1-4). 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. , several studies have reported the incidence of GBS infection in different demographic groups, and guidelines were developed and implemented for the prevention of neonatal infection in the 1990s (1-6). In European countries, however, few population-based data on GBS infection are available and no national guidelines have been published (7-10). In the United States, the recommended strategies to prevent perinatal GBS disease include either a risk-based or screening-based approach (5). In the risk-based approach, women in labor who have risk factors for GBS transmission (e.g., fever, prolonged rupture of the membranes, or preterm delivery) are offered intrapartum chemoprophylaxis. In the screening-based approach, vaginal and rectal combined swabs are cultured from all pregnant women and tested for GBS carriage during 35 to 37 weeks' gestation. Those identified as GBS carriers are offered intrapartum chemoprophylaxis. In Finland, laboratory-based surveillance for invasive bacterial infections, including GBS, began in 1995. To identify opportunities for prevention, we analyzed national GBS surveillance data from 1995 to 2000. To assess the proportion of cases that might have been prevented by using the risk-based or screening approaches, we reviewed birth histories of infants with early-onset GBS disease in five hospitals participating in a nosocomial infection Nosocomial infection An infection that can be acquired in a hospital. ABPA is a nosocomial infection. Mentioned in: Allergic Bronchopulmonary Aspergillosis, Hospital-Acquired Infections, Pseudomonas Infections surveillance network from 1999 to 2000. We also conducted two national surveys: one evaluating the microbiologic methods used to screen for GBS cultures in Finnish clinical microbiology Clinical microbiology The adaptation of microbiological techniques to the study of the etiological agents of infectious disease. Clinical microbiologists determine the nature of infectious disease and test the ability of various antibiotics to inhibit or kill laboratories and the other on current practices related to GBS screening and antibiotic use in Finnish hospitals with obstetric ob·stet·ric or ob·stet·ri·cal adj. Of or relating to the profession of obstetrics or the care of women during and after pregnancy. obstetrical, obstetric pertaining to or emanating from obstetrics. services. Methods Surveillance Finnish clinical microbiology laboratories routinely notify the National Infectious Disease Infectious disease A pathological condition spread among biological species. Infectious diseases, although varied in their effects, are always associated with viruses, bacteria, fungi, protozoa, multicellular parasites and aberrant proteins known as prions. Registry of bacterial isolations from blood and 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. . Each report includes the following information: isolation date, birth date, sex, specimen type, and treatment location. Multiple reports of the same case are combined in the database if they are received within 3 months of first isolation. A case is defined as isolation of GBS from blood or cerebrospinal fluid; early-onset neonatal disease is defined as that occurring in infants <7 days old and late-onset disease as that occurring in infants 7-89 days old. Additional Data Collection and Chart Review Neonatal GBS cases that occurred in five hospitals from 1999 to 2000 were identified through hospital wide surveillance of nosocomial nosocomial /noso·co·mi·al/ (nos?o-ko´me-il) pertaining to or originating in a hospital. nos·o·co·mi·al adj. 1. Of or relating to a hospital. 2. bloodstream infections in connection with the Finnish Hospital Infection Program (SIRO). We obtained data on deliveries, local guidelines for perinatal GBS prevention, and microbiologic data (e.g., screening method, number of specimens examined, and number of GBS-positive specimens). In cases of early-onset disease, the following data were abstracted from the medical records: prenatal GBS screening, intrapartum fever >38[degrees]C, prolonged rupture of membranes [greater than or equal to] 18 h before delivery, preterm delivery at <37 weeks of gestation, receipt of intrapartum antibiotics, and outcome of illness. Calculation of Incidence Rates and Statistical Analysis Data from the National Population Registry, including live births, from 1995 to 2000 were used as denominators to calculate age- and sex-specific incidence rates and early-onset and late-onset neonatal disease rates. The average annual incidences during the surveillance period were calculated by using the total number of cases, population, and live births from 1995 to 2000. To evaluate trends, rates of GBS disease in different age and sex groups were calculated for each 6-month period from January 1995 to December 2000. Data were analyzed by using Epi Info Epi Info is a public domain statistical software for epidemiology developed by Centers for Disease Control and Prevention. Developed by the Centers for Disease Control and Prevention (CDC) in Atlanta, Georgia (USA), Epi Info has been in existence for over 20 years and is software, version 6.04 (Centers for Disease Control and Prevention Centers for Disease Control and Prevention (CDC), agency of the U.S. Public Health Service since 1973, with headquarters in Atlanta; it was established in 1946 as the Communicable Disease Center. , Atlanta, GA) 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. software, version 8.2 (SAS Institute SAS Institute Inc., headquartered in Cary, North Carolina, USA, has been a major producer of software since it was founded in 1976 by Anthony Barr, James Goodnight, John Sall and Jane Helwig. , Inc., Cary, NC). A Poisson regression In statistics, the Poisson regression model attributes to a response variable Y a Poisson distribution whose expected value depends on a predictor variable x, typically in the following way: Surveys In February 2002, we sent structured questionnaires by electronic mail to 20 of the 28 Finnish clinical microbiology laboratories and by regular mail to all Finnish hospitals with obstetric services (n=38). The laboratories were asked about their methods for screening cultures for GBS and the hospitals about their GBS prevention policies. Results From 1995 to 2000, a total of 853 cases of invasive GBS disease were identified. Of bacterial isolates, 96% were obtained from blood and 4% from cerebrospinal fluid. The average annual incidence was 2.8 cases per 100,000 population (range by year, 2.2-3.0) and varied from 1.8 to 4.0 by health district. In women aged [greater than or equal to] 65 years of age, the incidence increased significantly, from 1.1 per 100,000 in 1995 to 8.2 per 100,000 in 2000 (p<0.01 by Poisson regression). No trends were identified in other age or sex groups. Infants of <1 year of age had the highest rate and accounted for 272 (32%) of 853 of all GBS infections (Table 1); 211 (78%) of 272 were early-onset disease and 203 (96%) of 211 were identified during the first 2 days of life. The average annual incidence of early-onset infections was 0.6 per 1,000 live births ,(range by year, 0.6-0.7; 32-38 cases/y; Table 2) and varied from 0.1 to 1.3 by health district. In 7 of 20 health districts in the country, the average annual incidence was >0.7 per 1,000 live births. Among 211 early-onset cases, 98% of isolates were obtained from blood and 2% from cerebrospinal fluid. The average annualized annualized Of or relating to a variable that has been mathematically converted to a yearly rate. Inflation and interest rates are generally annualized since it is on this basis that these two variables are ordinarily stated and compared. incidence of late-onset infections was 0.2 per 1,000 live births (range by year, 0.1-0.3; 6-16 cases/y; Table 2) and varied from 0.0 to 0.4 by health district. Among 56 cases of late-onset GBS disease, 59% of isolates were obtained from blood and 41% from cerebrospinal fluid. From 1999 to 2000, a total of 38,687 women delivered babies in the five study hospitals, accounting for one third of all live births in Finland. Of the deliveries, 20% were cesarean sections and 7% preterm deliveries. None of the hospitals had a policy for universal maternal screening of GBS. Their protocol included screening risk groups only and prescribing intrapartum prophylaxis prophylaxis (prō'fĭlăk`sĭs), measures designed to prevent the occurrence of disease or its dissemination. Some examples of prophylaxis are immunization against serious diseases such as smallpox or diphtheria; quarantine to confine for GBS-positive women. Patients who had previously delivered infants with GBS disease and who had tested positive for GBS bacteriuria bacteriuria /bac·te·ri·uria/ (bak-ter?e-u´re-ah) [bacteri- +-uria ] the presence of bacteria in the urine. Bacteriuria The presence of bacteria in the urine. during pregnancy were also screened. Two hospitals prescribed ampicillin ampicillin (ăm'pĭsĭl`ĭn), a penicillin-type antibiotic that is effective against both gram-negative microorganisms and gram-positive microorganisms such as Escherichia coli. , and three hospitals prescribed penicillin. To identify GBS carriers, four hospitals cultured the samples and one used an antigen test. Only vaginal swabs were collected. A total of 9,220 screening specimens were obtained; 12% of them were positive for GBS. The proportion of positive specimens varied from 4% to 21% in the five hospitals. In the study hospitals, 26 cases of early-onset disease (0.7/1,000 live births) and four cases of late-onset disease (0.1/1,000 live births) were identified. One premature neonate neonate /neo·nate/ (ne´o-nat) newborn infant. ne·o·nate n. A neonatal infant. neonate a newborn animal. died. Delivery occurred at 25 weeks of gestation, and the screening result was negative. Of 26 women who had infants with early-onset disease, 1 received intrapartum antibiotics because of prolonged rupture of the membranes and a positive screening result. Of the 25 women who did not receive intrapartum antibiotics, 18 (72%) were not screened. Eight (32%) developed at least one risk factor (six had duration of ruptured membranes [greater than or equal to] 18 hours, two had delivery at <37 weeks of gestation, and one had intrapartum fever). Of the 18 women not screened, 4 (22%) showed risk factors at the time of labor (3 had duration of ruptured membranes [greater than or equal to] 18 hours, and 1 had delivery at <37 weeks of gestation). All 26 isolates from case of early-onset infection and 4 from cases of late-onset infection were evaluated for antibiotic susceptibility. All isolates were susceptible to penicillin; two isolates (8%) were resistant/intermediate to erythromycin erythromycin (ĭrĭth'rōmī`sĭn), any of several related antibiotic drugs produced by bacteria of the genus Streptomyces (see antibiotic). , and one isolate (4%) was resistant to clindamycin. Surveys All 20 microbiology laboratories responded. Of the laboratories, 13 (65%) had a specific laboratory request for GBS culture; 9 laboratories requested cultures from vagina (69%) and 8 (62%) from cervix cervix /cer·vix/ (ser´viks) pl. cer´vices [L.] 1. neck. 2. the front portion of the neck. 3. cervix uteri. . None of the laboratories recommended rectal cultures. One laboratory used selective broth media to culture GBS. All directors of the 38 hospitals with obstetric services responded. Written GBS prevention protocols existed in 30 (79%) hospitals. Most used a combination of risk-based and screening-based strategies; one routinely screened all pregnant women for prenatal GBS carriage. Recommendations for obstetric risk groups include screening patients for GBS when they have one of the following: premature delivery premature delivery n. The birth of a premature baby. Premature delivery The birth of a live baby when a pregnancy ends spontaneously after the twentieth week. Mentioned in: Stillbirth (87%), rupture of membranes without labor (82%), previous delivery of an infant with invasive GBS disease (79%), GBS bacteriuria (66%), and maternal fever during labor (53%). GBS specimens were usually obtained from the vagina (82%) or cervix (45%). No rectal cultures were taken. Culture was used to detect GBS in 82%. of laboratories and antigen test in 34%. In 61% of the hospitals, chemoprophylaxis was given to all identified GBS carriers; the remaining 39% of hospitals required the presence of at least one additional obstetric risk factor before prescribing chemoprophylaxis (Table 3). When screening cultures were not performed or the results were not available at labor, chemoprophylaxis was most often given to risk groups with the following obstetric risks: intrapartum fever, previous delivery of an infant with invasive GBS disease, or prolonged rupture of membranes. Intrapartum chemoprophylaxis was given parenterally par·en·ter·al adj. 1. Physiology Located outside the alimentary canal. 2. Medicine Taken into the body or administered in a manner other than through the digestive tract, as by intravenous or intramuscular in 87% of hospitals and orally in 11%. Penicillin was recommended in 69%, cephalosporins Cephalosporins Definition Cephalosporins are medicines that kill bacteria or prevent their growth. Purpose Cephalosporins are used to treat infections in different parts of the body—the ears, nose, throat, lungs, sinuses, and in 19%, and aminopenicillins in 11% of hospitals. Discussion Compared with rates previously reported from European countries, the incidence of early-onset GBS disease in Finland is relatively low (7-14). However, the incidence is twice as high as rates reported among white infants in the United States (6). Data from the study hospitals in Finland This is a list of hospitals in Finland.
In Europe, most studies documenting the occurrence of early-onset GBS disease during the past decade involved a single hospital (10,12-14). European population-based data from Norway in 2001 showed an incidence of 1 case per 1,000 live births (8). During the period of our surveillance, the incidence of early-onset and late-onset infection in Finland remained unchanged and comparable to rates in a previous nationwide study conducted from 1985 to 1994 (early-onset disease 0.62/1,000 live births; late-onset disease 0.13/1,000 live births) (15). The annual number of cases of early-onset disease appears low, but surveillance is limited to culture-confirmed cases of invasive disease. The number of newborns in whom GBS is treated empirically may therefore be larger. We also identified considerable variation in rates of early-onset infection by health district. In Finland, the need for effective preventive measures was already emphasized during the 1980s, when GBS was identified as the most important etiologic agent of neonatal septicemia septicemia (sĕptĭsē`mēə), invasion of the bloodstream by virulent bacteria that multiply and discharge their toxic products. The disorder, which is serious and sometimes fatal, is commonly known as blood poisoning. (16). The efficacy of intrapartum chemoprophylaxis has also been demonstrated by a Finnish study (17). However, the prophylaxis was only introduced to heavily colonized patients detected by the streptolatex test. In our review of 26 cases of early-onset GBS disease, 1 case-patient received intrapartum antibiotics; 31% were screened prenatally for GBS, and 35% had a risk factor evident at the time of labor. Most case-patients were not screened and had no risk factors at the time of labor; of those not screened, four later developed a risk factor. Screening was performed for those in risk groups; some patients, such as those who had previously delivered infants with GBS disease or who tested positive for GBS bacteriuria during pregnancy, were unnecessarily screened. In addition, the site where cultures were taken and isolation method used differed from those recommended (5,18-22). In the United States, the decline in the incidence of GBS disease in newborns coincided with the implementation of consensus guidelines for the prevention of perinatal GBS disease beginning in 1996 (1). From 1993 to 1998, the incidence of GBS declined 65% from 1.7 to 0.6 per 1,000 live births. Data from 1998 to 1999 indicate a further decline in incidence in selected surveillance areas. Among certain demographic groups, such as white infants, the rate has declined to 0.3 per 1,000 live births (6). A recent review of >300 cases of early-onset infection from the United States also showed missed opportunities for prevention, including cases that would not have been prevented even with perfect implementation of prophylaxis strategies: 21% of cases occurred despite administration of intrapartum antibiotics, 35% of case-patients had been screened perinatally for GBS, and 44% had a risk factor evident at the time labor (2,6). Of case-patients not screened for GBS, 40% showed none of the risk-based criteria for prophylaxis. GBS infection in adults in Finland accounted for 67% of the total cases. The average annualized incidence of invasive GBS infection in adults varied from 1.6 to 5.6 per 100,000 population by age group. Although the incidence among elderly women was slightly lower than in elderly men, this number appears to be increasing. This finding is similar to previous population-based incidence data reported in 1989 to 1990 from metropolitan Atlanta, Georgia, where 48% of the total GBS cases were in adults; the annual incidence was 6.2 per 100,000 (3). Because the Atlanta study focused on nonpregnant adults and our study did not have information on the pregnancy status of the patients, age-specific rates cannot be compared. Recent U.S. data that included pregnant and nonpregnant adults indicate a marked increase in rates among adults, particularly in elderly persons and those with underlying illness, and vary between 2.1 to 21.9 per 100,000 by age group (4). The reasons for differences in rates of GBS disease between countries may include demographic differences, socioeconomic factors, and variations in clinical practices, such as the frequency of taking blood cultures in diagnostic examinations. Another suggested independent risk factor for both early-onset and late-onset GBS infection in neonates is being of black race (3,4). However, the association may also be linked to socioeconomic factors. The increasing prevalence of diabetes mellitus diabetes mellitus Disorder of insufficient production of or reduced sensitivity to insulin. Insulin, synthesized in the islets of Langerhans (see Langerhans, islets of), is necessary to metabolize glucose. In diabetes, blood sugar levels increase (hyperglycemia). and other underlying conditions may contribute to the increasing rates of GBS infection in adults. A common concern in the risk-based prevention approach is that a large number of women would receive unnecessary antibiotics. Widespread use of antibiotics can lead to an increase in allergic reactions, emergence of resistant strains, and cases of antibiotic colitis. The use of intrapartum antibiotics in the United States has doubled from 1996 to 1999, coinciding with GBS prevention implementation (23). We were unable to obtain information on how widely prophylaxis is currently used in Finland because data on type, dose, and time of administration of intrapartum antibiotics are not documented in hospital databases. Unnecessary antibiotic use could be reduced by not offering GBS prophylaxis to women who are not carriers. A recent study suggested that screening may be more effective in prevention than the risk-based approach (23). Screening reaches a broader population, and persons who are screened are more likely to receive prophylactic prophylactic /pro·phy·lac·tic/ (pro?-fi-lak´tik) 1. tending to ward off disease; pertaining to prophylaxis. 2. an agent that tends to ward off disease. pro·phy·lac·tic n. antibiotics. However, wide-scale screening for GBS colonization may be difficult to implement. The results of our study should be used to develop and implement national guidelines for prevention of perinatal GBS. Such guidelines would standardize prevention practices, rationalize the use of intrapartum antibiotics, and reduce the incidence of perinatal GBS disease. Further studies should be done to investigate the reasons for incidence increase among elderly women.
Table 1. Incidence of invasive group B streptococcus infection by age
and sex, Finland, 1995-2000
Men Women Rate
Age group No. of Rate No. of Rate No. of Rate
(y) cases (a) cases (a) cases (a)
<1 143 79.3 129 74.7 272 77.1
1-14 1 0.04 5 0.2 6 0.1
15-64 128 1.2 193 1.9 321 1.6
>64 103 6.0 151 5.4 254 5.6
All 375 2.5 478 3.0 853 2.8
(a) Average annual incidence (cases per 100,000 population).
Table 2. Annual incidence of early-onset and late-onset invasive group
B streptococcus infections, Finland, 1995-2000
1995 1996 1997 1998 1999 2000
Early-onset disease
No. of cases 37 37 34 38 33 32
Incidence (a) 0.6 0.6 0.6 0.7 0.6 0.6
Late-onset disease
No. of cases 8 16 6 10 9 7
Incidence (a) 0.1 0.3 0.1 0.2 0.2 0.1
(a) Cases per 1,000 live births.
Table 3. High risk groups for whom intrapartum antibiotic prophylaxis
is recommended in 38 Finnish hospitals with obstetric services,
2002 (a)
No. of hospitals (%)
GBS specimen
GBS specimen taken not taken (results
Risk group (result positive) (b) unknown)
GBS-positive mothers 23 (61) --
GBS bacteriuria during 15 (39) 15 (39)
current pregnancy
Invasive GBS disease in 25 (66) 25 (66)
previously delivered
child
Delivery <37 wk gestation 18 (47) 9 (24)
Rupture of membranes 26 (68) 19 (50)
[greater than or
equal to] 18 h
Intrapartum fever > 31 (82) 33 (87)
38[degrees]C
(a) GBS, group B streptococcus.
(b) Only one hospital routinely screened all pregnant women for
prenatal GBS carriage.
Acknowledgments We thank the staff at Finnish clinical microbiology laboratories and the following persons for their assistance in the investigation: Marja-Inkeri Tuominen, Ritva Levola, Anne Reiman, Aino Ruponen, Marja Jalkanen, Pirjo Kiiski, Aila Soininen, and Jukka Ollgren. All material published in Emerging Infectious Diseases An emerging infectious disease (EID) is an infectious disease whose incidence has increased in the past 20 years and threatens to increase in the near future. EIDs include diseases caused by a newly identified microorganism or newly identified strain of a known microorganism (e.g. is in the public domain and may be used and reprinted without special permission; proper citation, however, is appreciated. References (1.) Schrag SJ, Zywicki S, Farley MM, Reingold AL, Harrison LH, Lefkowitz LB, et al. Group B streptococcal streptococcal /strep·to·coc·cal/ (-kok´al) pertaining to or caused by a streptococcus. Streptococcal (Streptococcus) Pertaining to any of the Streptococcus bacteria. disease in the era of intrapartum antibiotic prophylaxis. N Engl J Med 2000;342:15-20. (2.) Schuchat A. Group B streptococcal disease from trials and tribulations to triumph and trepidation trepidation /trep·i·da·tion/ (trep?i-da´shun) 1. tremor. 2. nervous anxiety and fear.trep´idant trep·i·da·tion n. 1. An involuntary trembling or quivering. . Clin Infect Dis 2001;33:751-6. (3.) Farley MM, Harvey RC, Stull T, Smith JD, Schuchat A, Wenger JD, et al. A population-based assessment of invasive disease due to group B streptococcus in nonpregnant adults. N Engl J Med 1993;328:1807-11. (4.) Farley MM. Group B streptococcal disease in nonpregnant adults. Clin Infect Dis 2001;33:556-61. (5.) Centers for Disease Control and Prevention. Prevention of perinatal group B streptococcal disease Perinatal Group B Streptococcal Disease a leading infectious cause of morbidity and mortality among newborns. 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Neonatal group B streptococcal infection Infection with Group B Streptococcus (GBS), also known as Streptococcus agalactiae, can cause serious illness and sometimes death, especially in newborn infants and the elderly. in South Bedfordshire See also South Bedfordshire (UK Parliament constituency) South Bedfordshire is a local government district in Bedfordshire, England. Its main towns are Dunstable, Houghton Regis and Leighton Buzzard. 1993-1998. Arch Dis Child Fetal Neonatal Ed 2000;82:F205-7. (11.) Sjoberg I, Hakansson S, Eriksson A, Schollin J, Stjernstedt B, Tessin I. Incidence of early onset group B streptococcal septicemia in Sweden 1973 to 1985. Eur J Clin Microbiol Infect Dis 1990;9:276-8. (12.) Halle E, Halle H, Gunther E, Grauel EL, Schmidt G. Incidence of B streptococcal diseases and colonization--a clinico-epidemiological study [German]. Zentralbl Gynakol 1987;109:830-6. (13.) 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The likelihood that a positive test result indicates disease or that a negative test result excludes disease. predictive value a measure used by clinicians to interpret diagnostic test results. of prenatal cultures. J Infect Dis 1983;148:802-9. (20.) Dillon HC, Gray E, Pass MA, Gray BM. Anorectal a·no·rec·tal adj. Relating to the anus and the rectum. anorectal pertaining to, emanating from or affecting the anorectum. anorectal abscess see perianal fistula. and vaginal carriage of group B streptococci Streptococcus (plural, streptococci) A genus of spherical-shaped anaerobic bacteria occurring in pairs or chains. Sydenham's chorea is considered a complication of a streptococcal throat infection. during pregnancy. J Infect Dis 1982;145:794-9. (21.) Philipson EH, Palermino DA, Robinson A. Enhanced antenatal an·te·na·tal adj. See prenatal. antenatal before parturition. Called also prenatal, antepartal. detection of group B streptococcus colonization. Obstet Gynecol 1995;85:437-9. (22.) Hiller S, Schuchat A. Preventing neonatal group B streptococcal disease: the role of the clinical microbiology laboratory. Clinical Microbiology Newsletter 1997;19:113-6. (23.) Schrag SJ, Arnold KE, Roome A, Lynfield R, Craig A, Gamble M, et al. A. Intrapartum antibiotic exposure in the era of perinatal group B streptococcal (GBS) disease prevention. In: Abstracts of the 41st Interscience Conference on Antibiotic Agents and Chemotherapy; Chicago, Illinois, 22-25 Sept; Abstract G-1824. Washington: American Society for Microbiology The American Society for Microbiology (ASM) is a scientific organization, based in the United States although with over 43,000 members throughout the world. It is the largest single life science professional organization and its members include those whose interests encompass basic ; 2001. Address for correspondence: Outi Lyytikainen, Department of Infectious Disease, Epidemiology, National Public Health Institute, Mannerheimintie 166, FIN-00300 Helsinki, Finland; fax: 358-9-47448468; email: outi.lyytikainen@ktl.fi Outi Lyytikainen, * J. Pekka Nuorti, * Erja Halmesmaki, ([dagger]) Petteri Carlson, ([dagger]) Jukka Uotila, ([double dagger double dagger n. A reference mark (  ) used in printing and writing. Also called diesis.Noun 1. ]) Risto Vuento, ([double dagger]) Tapio Ranta, ([section]) Hannu Sarkkinen, ([section]) Martti Ammala, ([paragraph]) Anja Kostiala, ([paragraph]) and Anna-Liisa Jarvenpaa ([dagger]) * National Public Health Institute, Helsinki, Finland; ([dagger]) Helsinki University Central Hospital Helsinki University Central Hospital (HUCH) (in Finnish, Helsingin yliopistollinen keskussairaala (Hyks), in Swedish, Helsingfors universitets centralsjukhus (HUCS)) is the largest university hospital in Finland. , Helsinki, Finland; ([double dagger]) Tampere University Hospital, Tampere, Finland; ([section]) Paijat-Hame Central Hospital, Lahti, Finland; and ([paragraph]) Jorvi Hospital, Espoo, Finland Dr. Lyytikainen is a graduate of the European Program for Intervention Epidemiology Training assigned to the Robert Koch Institute, Berlin, Germany. She is the project leader of the Finnish National Hospital Infection Program at the Department of Infectious Disease Epidemiology The Department of Infectious Disease Epidemiology[1] is based at Imperial College London and carries out research including the modelling of infectious diseases and molecular epidemiology of pathogens. , National Public Health Institute. Her research interests include nosocomial infections Nosocomial infections Infections that were not present before the patient came to a hospital, but were acquired by a patient while in the hospital. Mentioned in: Enterobacterial Infections, Staphylococcal Infections , invasive bacterial infections, and antibiotic resistance antibiotic resistance, n the ability of certain strains of microorganisms to develop resistance to antibiotics. antibiotic resistance . |
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