| Literature DB >> 23628320 |
Patricia Ferrieri1, Ruth Lynfield, Roberta Creti, Aurea E Flores.
Abstract
Group B Streptococcus (GBS) is a major cause of invasive disease in neonates in the United States. Surveillance of invasive GBS disease in Minnesota, USA, during 2000-2010 yielded 449 isolates from 449 infants; 257 had early-onset (EO) disease (by age 6 days) and 192 late-onset (LO) disease (180 at age 7-89 days, 12 at age 90-180 days). Isolates were characterized by capsular polysaccharide serotype and surface-protein profile; types III and Ia predominated. However, because previously uncommon serotype IV constitutes 5/31 EO isolates in 2010, twelve type IV isolates collected during 2000-2010 were studied further. By pulsed-field gel electrophoresis, they were classified into 3 profiles; by multilocus sequence typing, representative isolates included new sequence type 468. Resistance to clindamycin or erythromycin was detected in 4/5 serotype IV isolates. Emergence of serotype IV GBS in Minnesota highlights the need for serotype prevalence monitoring to detect trends that could affect prevention strategies.Entities:
Keywords: CPS; GBS; Minnesota; United States; antimicrobial resistance; bacteria; capsular polysaccharide; clindamycin resistance; early-onset GBS disease; group B Streptococcus; invasive GBS disease; late-onset GBS disease; neonatal GBS disease; neonates; prophylaxis; serotype; serotype IV; streptococci
Mesh:
Substances:
Year: 2013 PMID: 23628320 PMCID: PMC3647718 DOI: 10.3201/eid1904.121572
Source DB: PubMed Journal: Emerg Infect Dis ISSN: 1080-6040 Impact factor: 6.883
Distribution of GBS invasive disease in infants by isolate source and age of infant at time of culture, Minnesota, USA, 2000–2010*
| Culture source | No. infants with GBS invasive disease† | Total | |||
|---|---|---|---|---|---|
| Early onset | Late onset | ||||
| 7–89 | 90–180 | >181 | |||
| Blood | 251 | 142 | 10 | 3 | 406 |
| Cerebrospinal fluid | 4 | 37 | 1 | 1 | 43 |
| Other sites‡ | 2 | 1 | 1 | 0 | 4 |
| All | 257 | 180 | 12 | 4 | 453 |
*GBS, group B Streptococcus. †No. isolates studied were 1 per infant (n = 453). Early-onset is birth–6 days. Late-onset categories (age in days at time of culture): classical (7–89); delayed (90–180); ultra (>181; not included in analyses). ‡Other sites, normally sterile: 1 bone, 1 joint, 2 tissues (1 liver, 1 lung).
Serotype distribution of invasive GBS isolates for cultures collected from infants, Minnesota, USA, January 2000–December 2010*
| CPS type | No. (%) patients† | ||
|---|---|---|---|
| Early onset | Late onset | Total | |
| Ia | 79 (30.7) | 57 (29.7) | 136 (30.3) |
| Ib | 25 (9.7) | 12 (6.2) | 37 (8.2) |
| II | 43 (16.7) | 5 (2.6) | 48 (10.7) |
| III | 57 (22.2) | 95 (49.5) | 152 (33.9) |
| IV | 8 (3.1) | 4 (2.1) | 12 (2.7) |
| V | 39 (15.2) | 18 (9.4) | 57 (12.7) |
| VII | 2 (0.8) | 0 (0.0) | 2 (0.4) |
| Nontypeable | 4 (1.6) | 1 (0.5) | 5 (1.1) |
| Total | 257 (100.0) | 192 (100.0) | 449 (100.0) |
*GBS, group B Streptococcus; CPS, capsular polysaccharide serotype. †Early-onset, patient age birth–6 days; late-onset, patient age 7–180 days.
Figure 1Distribution of early-onset and late-onset invasive group B Streptococcus disease in infants, by year, Minnesota, USA, 2000–2010. Bars indicate isolates of all capsular polysaccharide serotypes (CPS); line indicates all serotype IV isolates. A total of 257 infants had early-onset and 192 infants late-onset disease; 12 infants had type IV infection.
Figure 2Incidence of early-onset and late-onset group B Streptococcus disease per 1,000 live births, by year, Minnesota, USA, 2000–2010.
Patient characteristics of and clinical data for serotype IV GBS isolates from infants with invasive GBS disease, Minnesota, USA, January 2000–December 2010*
| Period | Disease type† | Patient age at diagnosis | Patient outcome | Culture source | Clindamycin susceptibility‡ | Isolate protein profile | Isolate PFGE profile |
|---|---|---|---|---|---|---|---|
| 2001–2009 | Late-onset | 98 d | Survived | Joint fluid | S | C-α and BPS | 37a |
| Late-onset | 30 d | Survived | Blood | S | C-α and BPS | 37 | |
| Late-onset | 9 d | Died | Blood | S | BPS | 37a | |
| Early-onset | 1 d | Survived | Blood | S | None | 40 | |
| Late-onset | 9 d | Survived | Blood | S | BPS | 37a | |
| Early-onset | 2 d | Survived | Blood | S | BPS | 37a | |
| Early-onset | 1 d | Survived | Blood | S | BPS | 37a | |
| 2010 | Early-onset | 1 d | Survived | Blood | R | C-α | 39a |
| Early-onset | Newborn | Survived | Blood | R | C-α | 39c | |
| Early-onset | Newborn | Survived | Blood | R | C-α | 39a | |
| Early-onset | Newborn | Survived | Blood | R | C-α | 39a | |
| Early-onset | Newborn | Survived | Blood | S | BPS | 37a |
*GBS, group B Streptococcus; PFGE, pulsed-field gel electrophoresis; C-α, C-protein α; BPS, group B protective surface protein. †Early-onset, patient age birth–6 days; late-onset, patient age 7–180 days. ‡S, susceptible, MIC <0.25 μg/mL; R, resistant, MIC >1 μg/mL.
Clindamycin susceptibility profiles of GBS isolates from 45 infants with invasive GBS disease, Minnesota, USA, 2010*
| Antimicrobial susceptibility profile† | CPS serotype | Total | ||||||||
|---|---|---|---|---|---|---|---|---|---|---|
| Clindamycin | Erythromycin | D-test | Ia | Ib | II | III | IV | V | ||
| S | S | Not done | 7 | 1 | 0 | 13 | 1 | 2 | 24 | |
| S | R | Negative | 4 | 0 | 0 | 3 | 0 | 0 | 7 | |
| S→R | R | Positive | 1 | 1 | 0 | 2 | 0 | 0 | 4 | |
| R | R | Not done |
| 0 | 2 | 1 | 0 | 4 | 3 | 10 |
| Total no. | 12 | 4 | 1 | 18 | 5 | 5 | 45 | |||
| No. (%) resistant | 1 (8.3) | 3 (75.0) | 1 | 2 (11.1) | 4 (80.0) | 3 (60.0) | 14 (31.1) | |||
*GBS, group B Streptococcus; CPS, capsular polysaccharide serotype. †S, susceptible, MIC <0.25 μg/mL; R, resistant, MIC >1 μg/mL; S→R, inducible resistance to clindamycin indicated by positive D-zone test (double-disk diffusion test).
Figure 3DNA macrorestriction profiles for serotype IV isolates from invasive group B Streptococcus (GBS) disease in infants, Minnesota. Isolates were studied by SmaI digestion and pulsed-field gel electrophoresis (PFGE) analysis and were designated as expressing C-protein α (C-α) or group B protective surface protein (BPS). Lane number is at the top and PFGE profile number at the bottom of each lane. A) Lane 2, λ molecular size standard; lanes 3 and 4, serotype IV/C-α GBS isolates from early-onset disease; lanes 5–7, prototypes of PFGE profile groups 39 (IV/C-α), 38 (IV/C-α), and 37 (IV/C-α and BPS); lane 8, internal standard 89-022 (Ib/C-α and C-β). B) Lane 1, λ molecular size standard; lane 2, PFGE profile 37 prototype (IV/C-α and BPS); lanes 3–6, isolates from late-onset disease; lanes 7–9, isolates from early-onset disease; lane 10, internal standard 89-022. Protein profile of isolates in lanes 2–4, C-α and BPS; lanes 5–8, BPS only. The isolate in lane 9 did not express any of the proteins studied.
Molecular characteristics of serotype IV GBS isolates causing invasive disease in infants and adults, Minnesota*
| Isolate source† | PFGE profile† | Allelic profile‡ | Sequence type§ | Clonal complex¶ |
|---|---|---|---|---|
| Mother, early-onset | 38d | 1,1,3,1,1,12,2 | 196 | 1 |
| Infant, early-onset | 40 | 1,1,3,1,1,12,2 | 196 | 1 |
| Nonpregnant adult | 39a | 1,1,3,1,41,12,2 | 459 | 1 |
| Mother, early-onset | 36c | 2,25,1,2,1,1,1 | 291 | 17 |
| Nonpregnant adult | 36d | 2,25,1,2,1,1,1 | 291 | 17 |
| Infant, late-onset | 37 | 5,25,4,3,2,3,3 | 452 | 23 |
| Infant, late-onset | 37a | 5,25,4,3,2,3,3 | 452 | 23 |
| Infant, early-onset | 37a | 5,25,4,3,2,3,1 | 468 | 23 |
*GBS, group B Streptococcus; PFGE, pulsed-field gel electrophoresis. †Early-onset, patient age birth–6 days or mother during peripartum period; late-onset, patient age 7–180 days. ‡Multilocus sequence type of 7 housekeeping genes (adhP, pheS, atr, glnA, sdhA, glcK, tkt). §From http://pubmlst.org/sagalactiae database. ¶Determined by eBurst analysis ().
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