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Putative lipoproteins of Streptococcus agalactiae identified by bioinformatic genome analysisSutcliffe, I.C., Harrington, Dean J. 05 1900 (has links)
No / Streptococcus agalactiae is a significant pathogen causing invasive disease in neonates and thus an understanding of the molecular basis of the pathogenicity of this organism is of importance. N-terminal lipidation is a major mechanism by which bacteria can tether proteins to membranes. Lipidation is directed by the presence of a cysteine-containing 'lipobox' within specific signal peptides and this feature has greatly facilitated the bioinformatic identification of putative lipoproteins. We have designed previously a taxon-specific pattern (G+LPP) for the identification of Gram-positive bacterial lipoproteins, based on the signal peptides of experimentally verified lipoproteins (Sutcliffe I.C. and Harrington D.J. Microbiology 148: 2065-2077). Patterns searches with this pattern and other bioinformatic methods have been used to identify putative lipoproteins in the recently published genomes of S. agalactiae strains 2603/V and NEM316. A core of 39 common putative lipoproteins was identified, along with 5 putative lipoproteins unique to strain 2603/V and 2 putative lipoproteins unique to strain NEM316. Thus putative lipoproteins represent ca. 2% of the S. agalactiae proteome. As in other Gram-positive bacteria, the largest functional category of S. agalactiae lipoproteins is that predicted to comprise of substrate binding proteins of ABC transport systems. Other roles include lipoproteins that appear to participate in adhesion (including the previously characterised Lmb protein), protein export and folding, enzymes and several species-specific proteins of unknown function. These data suggest lipoproteins may have significant roles that influence the virulence of this important pathogen.
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Effet du dépistage universel du streptocoque B[bêta]-hémolytique du groupe B sur l'incidence de la chorioamnioniteJohnson, Carolyne January 2007 (has links)
Mémoire numérisé par la Division de la gestion de documents et des archives de l'Université de Montréal.
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Streptococcus agalactiae - Distribuição sorotípica e relação com fatores de virulência e resistência antimicrobiana / Streptococcus agalactiae - Serotype distriburion and correlation with virulence factors and antibiotic resistanceNascimento, Cilícia Silverio 02 April 2019 (has links)
Streptococcus agalactiae, ou Estreptococo do Grupo B, é um microrganismo que encontrado na microbiota intestinal, vaginal e/ou geniturinária de 10-30% de mulheres saudáveis. A principal infecção causada por S. agalactiae é a sepse neonatal. O bebê pode adquirir o microrganismo durante o parto ao passar pelo canal vaginal, ou até mesmo durante a gestação, caso haja ascensão de S. agalactiae para o útero. Existem diversos fatores associados à infecção do feto por S. agalactiae quando a mãe é colonizada, tais como fator CAMP, cápsula de polissacarídeos, hialuronidase, β-citolisina/hemolisina e pili. Não existe consenso ou recomendação técnica sobre o tema no Brasil. Segundo o Caderno de Atenção Básica ao Pré-Natal, não existem estudos que levem à recomendação da antibioticoterapia intraparto. É necessário elucidar as características genotípicas de cepas de S. agalactiae isoladas no Brasil para alinhar as práticas clínicas às características fenotípicas do microrganismo. Desta forma, os objetivos deste projeto são: i) classificar cepas de S. agalactiae isoladas de gestantes e não gestantes quanto ao sorotipo capsular, por PCR Multiplex, ii) avaliar a presença e distribuição de fatores de virulência, por PCR e iii) avaliar o perfil de resistência antimicrobiana, pelo método de disco difusão e teste D. Os achados de virulência e resistência a antimicrobianos foram comparados com os sorotipos, gestação, localização geográfica e sítio de isolamento. Foram analisadas 292 cepas isoladas de gestantes e não gestantes em São Paulo, São José dos Campos e Rio de Janeiro. O sorotipo Ia foi o mais prevalente entre as cepas. Na cidade de São José dos Campos não houve diferença significativa entre a prevalência dos sorotipos Ia e V, sendo que o sorotipo V foi mais abundante do que nas cidades de São Paulo e Rio de Janeiro. O sorotipo II foi mais abundante em mulheres não gestantes do que gestantes. Não foram encontradas cepas resistentes à Penicilina e vancomicina; contudo a resistência a Cefepima, Eritromicina e Clindamicina ficou em torno de 22%. Foram encontradas diferenças entre os sorotipos quanto à resistência, genes de virulência e sítio de isolamento das cepas. Portanto essas diferenças podem se refletir no perfil epidemiológico da infecção por S. agalactiae quanto à localização geográfica também quanto à gestação. A incidência de sepse causada por S. agalactiae diminuiu muito nas últimas décadas, contudo o monitoramento constante é necessário para alinhar as práticas clínicas às características fenotípicas do microrganismo. / Streptococcus agalactiae, or Group B Streptococcus, is a microorganism found in intestinal, vaginal and/or genitourinary microbiota from about 10-30% of all healthy women. The main infection caused by S. agalactiae is neonatal sepsis. The baby can contract the infection during labor when passing through the vaginal canal, or even during pregnancy, if S. agalactiae ascends from the vaginal canal to the uterus. There are several factors associated to the infection of the fetus by S. agalactiae when the mother is colonized, such as the CAMP factor, polysaccharide capsule, hyaluronidase, β-cytolysin/hemolysin and pili. There is no consensus or technical recommendation regarding this theme in Brazil. According to the Brazilian guidelines to prenatal care, there is no research that justifies the implementation of intrapartum antibiotic therapy. There is a need to clarify genotype characteristics of S. agalactiae strains isolated in Brazil in order to align clinical practices to phenotypical characteristics of this microorganism. This way, the goals of this project are: i) to classify S. agalactiae strains isolated from pregnant and nonpregnant women according to their capsular serotype, using PCR Multiplex, ii) to evaluate the presence and distribution of virulence factors, using PCR and iii) to evaluate their antibiotic resistance profile, using disk-diffusion and D-zone tests. The findings regarding virulence and resistance were compared to serotypes, pregnancy, geographic localization and the site where the sample was isolated. A total of 292 strains from pregnant and nonpregnant women from the cities of São Paulo, São José dos Campos and Rio de Janeiro were analyzed. Serotype Ia was the most prevalent among the strains. In São José dos Campos there was no significate difference in the prevalence of serotypes Ia and V. Serotype V was the most abundant in São Paulo and Rio de Janeiro. Serotype II was most prevalent in nonpregnant women when compared to pregnant women. No resistance to Penicillin nor Vancomycin was found. However, resistance to Cefepime, Erythromycin or Clindamycin was found in around 22% of strains. There were differences among serotypes regarding resistance, virulence genes and site where the strain was isolated. Therefore these differences can reflect into the epidemiologic profile of S. agalactiae infection in regards to geographic localization and pregnancy. The incidence of sepsis caused by S. agalactiae has decrease in the last few decades, however constant monitoring is necessary in order to align clinical practice to the microorganisms phenotypical characteristics.
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Effet du dépistage universel du streptocoque B[bêta]-hémolytique du groupe B sur l'incidence de la chorioamnioniteJohnson, Carolyne January 2007 (has links)
Mémoire numérisé par la Division de la gestion de documents et des archives de l'Université de Montréal
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A study of group B streptococcus in Brisbane : the epidemiology, detection by PCR assay and serovar prevalenceTaylor, Karen Leigh January 2006 (has links)
The neonate is still at risk of acquiring Group B Streptococcus (GBS) infection upon delivery even with the implementation of early onset GBS neonatal disease preventative protocols. GBS was reported as the most prevalent organism causing neonatal morbidity and mortality in the USA and Australia in the 1990s. GBS is also known to cause disease in children, women, the immunocompromised adult and the elderly, but it is the preterm neonates who are at greatest risk of GBS neonatal disease. The aim of this study was to determine the prevalence of lower genital tract (LGT) colonisation with GBS in Brisbane women of child bearing age. We also aimed: (i) to compare the GBS LGT prevalence rate of Indigenous and non Indigenous women; (ii) to determine whether previously reported risk factors for LGT colonisation with GBS were also risk factors associated with GBS colonisation of women in this study; (iii) to further develop and optimise a rapid PCR assay that could detect maternal LGT GBS colonisation; and (iv) to serotype the GBS strains that were isolated from pregnant and non pregnant women who participated in this study. This study recruited 374 women of childbearing age attending public medical providers and found an overall GBS prevalence of 98/374 (26.2%) for these Brisbane women, a rate higher than previously reported in Australia. When the GBS prevalence for pregnant women (25.6%) was compared to non pregnant women (27.2%) they were similar. We also compared the GBS LGT colonisation rate of women attending different medical providers. The GBS LGT prevalence rate for pregnant women attending the Mater was 36/118 (30.5%), whilst those women attending the Redlands Hospital antenatal clinic had a LGT GBS prevalence rate of only 7/53 (13.2%). By comparison, the LGT GBS prevalence rate for non pregnant women attending Biala Sexual Health clinic was 21/69 (30.4%) and 34/127 (26.8%) of women attending the Brisbane Family Planning Queensland were also GBS positive. The seven women recruited from Inala community centre tested negative for GBS LGT colonisation. The LGT GBS prevalence of Australian Aboriginal women was 5/22 (22.7%), a rate which was not significantly different from non-Aboriginal women 78/288 (27.1%). Established early onset GBS neonatal disease preventative policies have been recently revised. The CDC now recommends that all pregnant women are screened for LGT GBS colonisation during late gestation, and that any GBS isolates be tested for resistance to antibiotics if the GBS positive women have an allergy to penicillin. Queensland's Department of Health recommend that Queensland medical agencies implement a non screening based preventative protocol, where clinicians monitor: women prior to labour for reported risk factors associated with maternal GBS colonisation: women in labour for 'obstetric risk factors'. A number of risk factors have previously been reported in association with GBS LGT colonisation. However, in this current study we found that only one risk factor was significantly associated with current GBS: previous reported LGT GBS colonisation was significantly associated with maternal LGT GBS colonisation reported in this study. Women who previously tested positive for GBS were significantly more likely to be GBS positive in subsequent tests (OR 4.7; 95%CI, 1.8-12.5) compared to women with no previous history of GBS colonisation. An assessment of adverse pregnancy outcomes, preterm deliveries, and GBS colonisation data was made. It was established that 30 women had previously given birth to one or more preterm neonates and of these 30 women, nine (30%) of them tested positive for GBS in this current study. Of the 71 women who had given birth to neonates and who had suffered an adverse pregnancy outcome 25.3% also tested positive for GBS in this current study. GBS was identified in up to 30% of all mothers who had delivered their neonate preterm, 27.4% of women who had previously suffered miscarriages and 16.7% of women who had previously had stillbirths. In this study we found that Australian Aboriginal women also had a greater risk of delivering neonates who suffered from an adverse pregnancy outcome in comparison to all other women. Twenty one of the 22 Aboriginal women had previously been pregnant at least once, and nine (42.9%) of these women had at least one prior adverse pregnancy outcome while seven (33.3%) of these women had previously delivered at least one neonate preterm. Of the 21 Aboriginal women who had a previous pregnancy more than half the total number of Aboriginal women (11/21) had either delivered one or more neonates preterm or had suffered from one or more adverse pregnancy outcomes. When the incidence of adverse pregnancy outcomes was compared for Aboriginal and all other women the results were surprising. Overall, this study found 216 women including Aboriginal women had previously been pregnant and of these women 71 (32.8%) of them suffered an adverse pregnancy outcome. By comparison, only 62 of 195 (31.8%) non Aboriginal women but nine out of 21 (41.9%) Australian Aboriginal women suffered from a previous adverse pregnancy outcome. The clinical LGT GBS isolates found in this study of Brisbane women were typed and all nine GBS serotypes plus non typeable GBS serotypes were detected. Seventy women tested GBS culture positive and vaginal and/or perianal samples obtained from these women were evaluated. GBS serotype III was the serotype most frequently isolated from this total population, from 47.4% of pregnant women and 51.7% of non pregnant women. From some women only a single GBS serotype was isolated: in these women we found that GBS serotype III (50%) was the predominant isolate, followed by GBS serotype Ia isolated from 16.7% women. In addition 4.2% of women were colonised with GBS serotypes; Ib, II and V, whilst GBS serotypes IV and VII were isolated from 2.1% women. Non typeable GBS strains confirmed by latex agglutination tests accounted for 11.9% of all strains isolated from these Brisbane women. This study identified multiple serovars in 15 clinical samples and found that 22 (31.4%) women were colonised with mixed GBS serotypes in samples collected from both vaginal and perianal regions. In five women the combination of serotypes III/Ia were identified and in other women combinations of serotypes III/II, III/IV, III/V, III/VIII, Ia/IV and Ib/NT were also detected. In two instances three serotype combinations were detected in samples from one woman and these included serotypes III/Ib/II and III/Ia/Ib. Isolates were also typed for women who were colonised in both vaginal and perianal regions and it was found that only 10 participants had identical isolates in both regions. GBS serotype III was the predominant serotype detected in women tested in this study and this is the serotype that has previously been associated with invasive infections in neonates. GBS neonatal disease is a world wide economic, health and social burden affecting different ethnic groups and is preventable. Currently no vaccine technology is available for the prevention of GBS neonatal disease and the most effective EOGND preventative protocol would be to test for maternal GBS colonisation during labour, or screen women for GBS at >36 weeks' gestation and administer intrapartum antibiotic prophylaxis (IAP) to all women who tested positive for GBS. In this current study we utilised a rapid bsp PCR assay to detect LGT GBS colonisation in women of child bearing age. The PCR assay identified 62.5% of all vaginal and perianal positive culture GBS samples. The specificity of the PCR assay was 89% while the positive and negative predictive values were 56.8% and 91.1% respectively. This PCR assay using the current parameters is not an effective GBS detection assay but could be further optimised in the near future. This PCR assay could be an effective test in the future with the development of an alternative DNA extraction method to InstaGene (BioRad). However, this PCR assay if used in conjunction with the current culture method is able to detect a further 8.9% of women colonised with asymptomatic GBS. Brisbane women aged between 26 to 35 years who are pregnant and who are attending public health care agencies are at greatest risk of being colonised with GBS. No disparity was identified when ethnicity or social standing were assessed. The overall results of this study demonstrate that the LGT GBS prevalence rate in Brisbane women is 26.2% but this rate was higher at 30.5% for women attending a Brisbane sexual health clinic and for pregnant women attending the Mater Mothers' antenatal clinic. GBS serovar III has been identified as the dominant serovar in our population group and this strain has been reported as the major cause of GBS disease in neonates and infants aged to three months. Disparity (11.1%) was reported when the incidence of adverse pregnancy outcomes amongst Aboriginal women was compared to non Aboriginal women. From the outcomes of this study it has been suggested that Queensland adopt a screening based GBS preventative protocol. It has also been suggested that an Australian wide GBS prevention strategy may further reduce the incidence of neonatal disease.
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Inflammation gestationnelle induite par le streptocoque de groupe B inactivé : rôle de l'interleukine-1 / Gestational inflammation induced by inactivated group B streptococcus : role of interleukin-1Bergeron, Julie January 2017 (has links)
Depuis les dernières décennies, plusieurs études épidémiologiques montrent des associations entre l’infection/inflammation durant la grossesse, les accouchements prématurés, les lésions cérébrales périnatales et les troubles neuro-développementaux ultérieurs tels que l’autisme. Le pathogène le plus fréquemment rencontré durant la grossesse est le streptocoque de groupe B (SGB). Le SGB colonise le tractus gastro-intestinal et/ou vaginal de 10 à 30% des femmes enceintes et provoque une combinaison d’infection et d’inflammation dont la cible la plus fréquente est le placenta (chorioamnionite). Nous avions précédemment montré, à l’aide d’un modèle animal pré-clinique (rat), que l’exposition systémique au SGB inactivé en fin de gestation induit une chorioamnionite, des lésions cérébrales ainsi que des traits comportementaux de type autistique dans la progéniture mâle.
Dans le cadre de ce travail, nous avons précisé la nature de la réaction inflammatoire sous-jacente à l’exposition maternelle au SGB inactivé en fin de gestation. Cette réaction inflammatoire est caractérisée par une surexpression d’IL-1β à la fois dans le plasma maternel, le placenta et le plasma foetal. Les placentas présentent une chorioamnionite sévère, principalement caractérisée par des infiltrations de cellules inflammatoires (majoritairement des cellules polymorphonucléaires neutrophiles (PMN), s’étendant jusqu’au versant foetal placentaire. De manière générale, les tissus associés aux foetus mâles présentent des niveaux d’inflammation supérieurs, autant par le profil d’expression des cytokines pro-inflammatoires (IL-1β, IL-6 et TNF-α) que par les infiltrations de PMN.
Puisque l’IL-1 est une cytokine pro-inflammatoire associée au travail préterme, aux lésions cérébrales ainsi qu’à l’autisme, nous avons tenté de valider son rôle dans la genèse des troubles neuro-développementaux SGB-induits dans notre modèle. Toutefois, le rôle de l’IL-1 n’a pu être élucidé.
Ces résultats supportent les évidences croissantes que le sexe foetal impacte la susceptibilité du foetus face aux agressions inflammatoires. Ces résultats ouvrent plusieurs nouvelles avenues de recherche, notamment sur l’identification de joueurs clés dans la réaction inflammatoire materno-foetale suivant l’exposition au SGB et ainsi développer de nouvelles mesures pour protéger le placenta et le cerveau du foetus en développement. / Abstract : For the last decades, epidemiological studies have associated preterm birth, cerebral lesions and neurodevelopmental disorders to infection and/or inflammation during pregnancy. One of the most common pathogen encountered during gestation is Group B Streptococcus (GBS), which colonizes 10 to 30% of pregnant women’s gastro-intestinal and/or vaginal tracts. We have previously shown - with a preclinical rat model - that exposure to killed GBS at the end of gestation leads to placental and cerebral lesions. Moreover, only male offspring from mothers who experienced GBS-induced gestational inflammation displayed autistic-like behavior.
In this work, we analyzed the inflammatory response to maternal inactivated GBS exposure at the end of gestation. This inflammatory response involves IL-1β, which is over expressed in maternal plasma, placenta and fetal plasma. Placentas displayed acute signs of histological chorioamnionitis, with polymorphonuclear cells (PMN) infiltrations even on the fetal side of placenta. Following GBS-induced inflammation, tissues associated to male fetuses generally showed increased inflammatory response as compared to females (IL-1β, IL-6 and TNF-α) and higher PMN placental infiltrations.
Because IL-1β is associated to preterm birth, cerebral damage and autism, we wanted to validate the role of IL-1 in the onset of GBS-induced autism-like behavior in our animal model. However, at this stage, we have not been able to demonstrate this role.
These results support the evidences that fetal sex matters for fetal susceptibility to inflammatory aggressions during pregnancy. These results pave the way toward the identification of key molecules in chorioamnionitis, brain damage and subsequent neurobehavioral disorders. This will help to find new strategies to protect the placenta and the fetal brain.
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A proteomic investigation of Streptococcus agalactiae reveals that human serum induces the C protein β antigen and arginine deiminaseYang, Q., Zhang, M., Harrington, Dean J., Black, G.W., Sutcliffe, I.C. 2011 March 1931 (has links)
No / Streptococcus agalactiae is a major neonatal pathogen. Disease progression is characterised by bacterial adaptation from commensal maternal vaginal colonisation to environments associated with neonatal disease, including exposure to blood. To explore this adaptation in vitro, we have used proteomics to identify proteins differentially expressed following growth on Todd Hewitt agar in the presence or absence of 10% v/v human serum. Twelve differentially expressed proteins were identified. Notably, the C protein β antigen and arginine deiminase proteins were upregulated following growth in the presence of human serum, consistent with previous studies implicating these two proteins in the pathogenesis of S. agalactiae disease.
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A proteomic investigation of Streptococcus agalactiae grown under conditions associated with neonatal exposure reveals the upregulation of the putative virulence factor C protein β antigenYang, Q., Zhang, M., Harrington, Dean J., Black, G.W., Sutcliffe, I.C. 04 February 2010 (has links)
No / Streptococcus agalactiae is a major neonatal pathogen that is able to adapt to a variety of host environments, including both rectal and vaginal maternal carriage, growth in amniotic fluid and at various neonatal body sites. As such it is important to elucidate the patterns of protein expression that are associated with S. agalactiae growth under these different in vivo conditions. To this end, we have grown S. agalactiae strain A909 under in vitro conditions reflecting those associated with maternal vaginal carriage (low pH, low oxygen, nutrient stress) and those associated with exposure to body fluids during invasive disease (neutral pH, aeration, nutrient sufficient). The protein profiles of bacterial cells grown under each of these conditions were compared using a proteome approach. A total of 76 proteins were reproducibly identified 16 of which were shown to be differentially expressed. The putative virulence factor C protein β and several proteins linked to resistance to oxidative stress were found to be upregulated under the conditions hypothesised to reflect those associated with foetal exposure to S. agalactiae. Thus, these data add to the currently limited understanding of the molecular basis of S. agalactiae GBS adaptation to different environmental conditions.
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Epidemiology of invasive group B streptococcal disease in infants from urban area of South China, 2011–2014Guan, X., Mu, X., Ji, W., Yuan, C., He, P., Zhang, L., Huang, Y., Li, J., Chen, J., Zhong, H., Pang, S., Tan, N., Deng, Q., Gao, K., Huang, Y., Chang, Chien-Yi, Liu, H. 01 August 2018 (has links)
Yes / Background: Group B Streptococcus (GBS) is a leading cause of morbidity and mortality in infants in both
developed and developing countries. To our knowledge, only a few studies have been reported the clinical
features, treatment and outcomes of the GBS disease in China. The severity of neonatal GBS disease in China
remains unclear. Population-based surveillance in China is therefore required.
Methods: We retrospectively collected data of <3 months old infants with culture-positive GBS in sterile samples
from three large urban tertiary hospitals in South China from Jan 2011 to Dec 2014. The GBS isolates and their
antibiotic susceptibility were routinely identified in clinical laboratories in participating hospitals. Serotyping and
multi-locus sequence typing (MLST) were also conducted for further analysis of the neonatal GBS disease.
Results: Total 70 cases of culture-confirmed invasive GBS infection were identified from 127,206 live births born in
studying hospitals, giving an overall incidence of 0.55 per 1000 live births (95% confidence interval [CI] 0.44–0.69).
They consisted of 49 with early-onset disease (EOD, 0.39 per 1000 live births (95% CI 0.29–0.51)) and 21 with
late-onset disease (LOD, 0.17 per 1000 live births (95% CI 0.11–0.25)). The incidence of EOD increased significantly over
the studying period. Five infants (4 EOD and 1 LOD) died before discharge giving a mortality rate of 7.1% and five
infants (7.1%, 2 EOD and 3 LOD) had neurological sequelae. Within 68 GBS isolates from GBS cases who born in the
studying hospitals or elsewhere, serotype III accounted for 77.9%, followed by Ib (14.7%), V (4.4%), and Ia (2.9%). MLST
analysis revealed the presence of 13 different sequence types among the 68 GBS isolates and ST-17 was the most
frequent sequence type (63.2%). All isolates were susceptible to penicillin, ceftriaxone, vancomycin and linezolid, while
57.4% and 51.5% were resistant to erythromycin and clindamycin, respectively.
Conclusions: This study gains the insight into the spectrum of GBS infection in south China which will facilitate the
development of the guidance for reasonable antibiotics usage and will provide evidence for the implementation of
potential GBS vaccines in the future. / Supported by medical and health science and technology projects of Health and Family Planning Commission of Guangzhou Municipality (grant number 20151A010034) and Guangdong provincial science and technology planning projects (grant number 2014A020212520).
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Nėščiųjų B grupės beta hemolizinio streptokoko ir Escherichia coli nešiojimo dažnumo nustatymas bei įtakos naujagimių ankstyvam infekciniam sergamumui vertinimas / Group B streptococcus and Escherichia coli colonization in pregnant women and the impact of colonization on early onset neonatal infectionsBarčaitė, Eglė 08 December 2008 (has links)
Tyrimo tikslas – nustatyti nėščių moterų B grupės β hemolizinio streptokoko (BGS) ir Escherichia coli (E.coli) nešiojimo bei naujagimių kolonizacijos dažnumą ir įvertinti šių mikroorganizmų įtaką naujagimių ankstyvai infekcijai atsirasti.
Metodika. Perspektyvinis momentinis stebėjimo tyrimas vykdytas Kauno medicinos universiteto Akušerijos ir ginekologijos bei Neonatologijos klinikose. Moterims du atskiri pasėliai iš makšties apatinio trečdalio ir išangės buvo paimti 35-37 nėštumo savaitę arba gimdymo metu, o naujagimiams - iš ausies išorinės landos bei nosiaryklės per 5 – 15 min. po gimimo. Išskirtų BGS serotipavimas atliktas naudojant 9 specifinius antiserumus, o jautrumas antibiotikams nustatytas diskų difuzijos metodu pagal klinikinių laboratorijų standartus nustatančio komiteto (NCCLS) rekomendacijas.
Rezultatai. Šimtas keturiasdešimt aštuonioms moterims iš 970 (15,3 proc.) buvo nustatytas BGS nešiojimas, o 193 moterims (19,9 proc.) - E.coli nešiojimas. Naujagimių BGS ir E.coli kolonizacijos dažnumas buvo 6,4 proc. ir 14,4 proc., o vertikalaus pernešimo – atitinkamai 28,4 ir 24,4 procentai. Moterims ir naujagimiams dažniausiai identifikuotas III ir Ia serotipo BGS. Bendras naujagimių įgimtos infekcijos dažnumas buvo 37,5 atvejai iš 1000 naujagimių, o BGS sukeltos infekcijos dažnumas - 3,6 atvejai iš 1000 naujagimių. Nebuvo nė vieno E.coli sukeltos ankstyvos naujagimių infekcijos atvejo. Klinikinis sepsis diagnozuotas 5 kartus dažniau nei mikrobiologiniais tyrimais... [toliau žr. visą tekstą] / Objective - to examine the prevalence of maternal and neonatal colonization of group B streptococcus (GBS) and Escherichia coli (E.coli) in our area, and to evaluate the colonization impact on early onset neonatal infections as a whole.
Methods. A prospective cross-sectional study carried out at the Department of Obstetrics and Gynaecology and the Department of Neonatology of Kaunas University Hospital. Samples were collected from the lower vagina and the anorectum of pregnant women at 35-37 weeks of gestation or at delivery and the ear canal as well as throat of the neonates within 5 – 15 min of their lives. The distribution of serotypes of the GBS identified was determined using specific antisera and antimicrobial susceptibility was investigated by disc-diffusion method as described by National Committee for Clinical Laboratory Standards (NCCLS).
Results. GBS carriage was detected in 148 (15.3%) of 970 women screened whereas E.coli colonisation was found in 193 (19.9%) of the women studied. The overall GBS and E.coli neonatal colonization rates were 6.4% and 14.4%; vertical transmission rates - 28.4% and 24.4%, respectively. The most common GBS serotypes were III and Ia. The overall incidence of early onset neonatal infection was estimated to be 37.5 per 1000 live birth and the incidence of early onset GBS disease in newborns – 3.6 per 1000 live birth. There was no case of early neonatal E. coli infection. The incidence of clinical sepsis in neonates was 5 fold higher that... [to full text]
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