| Literature DB >> 28099644 |
Vanessa Soares Lanziotti1,2, Pedro Póvoa3,4, Márcio Soares1, José Roberto Lapa E Silva2, Arnaldo Prata Barbosa1,4, Jorge Ibrain Figueira Salluh1.
Abstract
Despite advances in recent years, sepsis is still a leading cause of hospitalization and mortality in infants and children. The presence of biomarkers during the response to an infectious insult makes it possible to use such biomarkers in screening, diagnosis, prognosis (risk stratification), monitoring of therapeutic response, and rational use of antibiotics (for example, the determination of adequate treatment length). Studies of biomarkers in sepsis in children are still relatively scarce. This review addresses the use of biomarkers in sepsis in pediatric patients with emphasis on C-reactive protein, procalcitonin, interleukins 6, 8, and 18, human neutrophil gelatinase, and proadrenomedullin. Assessment of these biomarkers may be useful in the management of pediatric sepsis.Entities:
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Year: 2016 PMID: 28099644 PMCID: PMC5225923 DOI: 10.5935/0103-507X.20160080
Source DB: PubMed Journal: Rev Bras Ter Intensiva ISSN: 0103-507X
Figure 1Biomarkers in pediatric sepsis.
CRP - C-reactive protein; PCT - procalcitonin; IL-6 - interleukin 6; IL-8 - interleukin 8; NGAL - human neutrophil gelatinase.
Main biomarkers in pediatric sepsis
| Biomarker | Why use? | Limitations |
|---|---|---|
| CRP | Easily available and low cost | Variable sensitivity and specificity for
detecting bacterial infection (lower when a single measurement is
performed) |
| PCT | Peaks 24 - 36 hours after an inflammatory
trigger | Variable sensitivity and specificity
|
| IL-6 and IL-8 | Increased accuracy when combined with
other biomarkers | Few studies in the pediatric population |
| Adrenomedullin (proADM) | Correlation with severity and potential
use as a risk stratifier | Studies in the pediatric population are
still scarce |
| NGAL | Promising biomarker of acute kidney injury
(organ dysfunction) | Lacks validation in pediatric patients
with septic shock (low specificity as a kidney injury predictor)
|
CRP - C-reactive protein; PCT - procalcitonin; IL-6 - interleukin 6; IL-8 - interleukin 8; NGAL - human neutrophil gelatinase.
Main publications on the use of C-reactive protein in pediatric infection/sepsis
| Authors | Type of publication | Main results | Conclusion |
|---|---|---|---|
| McWilliam et al.( | Narrative review | Single measurement of CRP is not
sensitive or specific enough to identify severe bacterial
infection | Serial measurements of CRP are useful
in assessing the response to antimicrobial treatment |
| Sanders et al.( | Systemic review | Diagnostic accuracy of CRP for
bacterial infection in non-hospitalized children with fever has
77% sensitivity and 79% specificity | CRP is useful (moderately and
independently) for the diagnosis and exclusion of severe
bacterial infection |
| Santolaya et al.( | Prospective cohort | 447 episodes of high-risk febrile
neutropenia - 17% with diagnosis of severe sepsis | Validation of the predictive risk
model for severe sepsis in patients with high-risk febrile
neutropenia in the first 24 hours of admission |
| Kitanovski et al.( | Prospective cohort - 47 children | 18 of 90 episodes of febrile
neutropenia were classified as bacteremia/sepsis | On admission and 24 hours later, the diagnostic accuracy of CRP alone for severe sepsis in children with febrile neutropenia was lower than that of PCT and IL-6 |
| Lanziotti et al.( | Prospective cohort (preliminary results) - 57 children | 50 of 57 patients were classified
according to a CRP response pattern in the first week of
antibiotic therapy in pediatric sepsis | Sequential CRP assessment (CRP ratio)
is useful in the early identification of patients with poor
prognosis |
CRP - C-reactive protein; IL-8 - interleukin-8; RR - relative risk; IL-6 - interleukin-6; PCT - procalcitonin; ICU - intensive care unit.
Main publications of the use of procalcitonin in pediatric infection/sepsis
| Authors | Type of publication | Methods and main results | Conclusion |
|---|---|---|---|
| Rey et al.( | Observational prospective cohort | 359 patient-days included in the study
| PCT is a better diagnostic marker for
sepsis in critically ill patients than CRP |
| Fioretto et al.( | Prospective cohort | 87 patients (46 patients diagnosed
with sepsis and 41 patients diagnosed with septic shock)
| PCT was better than CRP for the diagnosis of sepsis and septic shock, particularly on admission, and was related to disease severity |
| England et al.( | Systematic review | 7 studies of 2,317 patients | PCT values < 0.3ng/mL may be useful in the exclusion of severe bacterial infection, as an additional test to clinical prediction, remaining as a key factor to guide the therapeutic approach in these patients |
| Arkader et al.( | Observational prospective cohort | PCT and CRP kinetics studied in
patients undergoing heart surgery with cardiopulmonary bypass
(Group 1 - SRIS) and in patients with confirmed bacterial sepsis
(Group 2) | PCT was able to differentiate patients
with SRIS and sepsis, and CRP was not |
| Han et al.( | Prospective cohort | 87 patients with sepsis and septic
shock | PCT is persistently elevated in children with bacterial sepsis and poor prognosis |
| Hu et al.( | Prospective cohort | Investigation of the relationship
between the PCT SL and prognosis in children with bacterial
meningitis | PCT SL are related to disease severity
in children with bacterial meningitis |
| Henry et al.( | Systematic review | 8 studies were included (616 patients)
| PCT SL are highly accurate in differentiating bacterial meningitis from viral meningitis in children |
| Hatzistilianou et al.( | Prospective cohort | Assessment of PCT, CRP, TNF-alpha,
IL-1b, IL-8 and TNF-receptor II values in the rapid and early
diagnosis of infection in patients with acute lymphocytic
leukemia and febrile neutropenia and differentiation between
bacterial and viral infection | Serial PCT measurements may be useful in predicting severe sepsis in patients with acute lymphoid leukemia and febrile neutropenia |
| Zurek et al.( | Prospective cohort | 62 patients (0 - 19 years) with SRIS
or sepsis were included | PCT SL from day 1 to day 5 of pediatric ICU admission are related to severity and multiple organ dysfunction in children with SRIS/sepsis |
PCT - procalcitonin; CRP - C-reactive protein; SRIS - systemic inflammatory response syndrome; RR - relative risk; SL - serum levels; TNF-alpha - Tumor necrosis factor alpha; IL-1b-interleukin 1 beta; IL-8 interleukin 8; TNF-receptor II - tumor necrosis factor receptor II; PELOD - Pediatric Logistic Organ Dysfunction score.