Cell-Associated Interleukin-8 in Cord Blood of Term and Preterm Infants

Dembinski, Jörg; Behrendt, Daniela; Heep, Axel; Dorn, Christoph; Reinsberg, Jochen; Bartmann, Peter

doi:10.1128/cdli.9.2.320-323.2002

Cited by 9 publications

(14 citation statements)

References 19 publications

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“…In agreement with observations of Dembinksi et al [28], plasma IL-8 was not influenced by gestational age, in contrast to DLWB IL-8; late preterm neonates had lower DLWB IL-8 concentrations ( fig. 1).…”

Section: Disclosure Statementsupporting

confidence: 81%

“…In our group of spontaneous births (table 2), we also registered the duration of labor and found no correlation between either DLWB or plasma IL-8 concentrations (not shown); however, we did not analyze or standardize labor pain. Dembinski et al [28] found more evident neonatal proinflammatory response to labor stress in concentrations of IL-8 in whole blood than in serum.…”

Section: Influence Of Hematocritmentioning

confidence: 99%

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Influence of Gestational Age, Cesarean Section and Hematocrit on IL-8 Concentrations in Plasma and Detergent-Lysed Whole Blood of Noninfected Newborns

Neunhoeffer

Lipponer

Eichner

et al. 2011

Transfus Med Hemother

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SummaryBackground: Sensitivity of interleukin-8 (IL-8) in detecting early-onset bacterial infection (EOBI) is high. A high percentage is bound to nonspecific receptors on erythrocytes which can be determined via cell lysis. We have shown detergent-lysed whole blood (DLWB) IL-8 to be superior to plasma IL-8 in detecting EOBI. Methods: To evaluate influence of pre-and perinatal factors on plasma and DLWB IL-8 concentrations, IL-8 was determined via ELISA (Immulite) in 146 noninfected newborns with risk factors for EOBI at two different time periods: 0-6 (group I) and 24-30 h (group II) after birth. The influence of gender, mode of delivery, gestational age and hematocrit was evaluated. Results: While we found no influence of gender or gestational age, hematocrit was positively correlated with IL-8 plasma concentration (group I: r = 0.33, p < 0.001; group II: r = 0.30, p <0.01). IL-8 plasma concentrations after primary versus secondary cesarean section were lower (p < 0.05). Gestational age was correlated with DLWB IL-8 concentrations (group I: r = 0.46, p < 0.001; group II: r = 0.28, p < 0.001). Conclusion: Plasma IL-8 concentrations were positively correlated with hematocrit, whereas DLWB IL-8 concentrations increased with gestational age. This may be relevant to the interpretation of IL-8 in preterm infants and infants with anemia, polyglobulia or hematolytic diseases. SchlüsselwörterInterleukin-8 · IL-8 · Lysiertes Vollblut · Hämatokrit · Gestationsalter · Geburtsgewicht Zusammenfassung Hintergrund: Die Sensitivität von Interleukin-8 (IL-8) bei der Diagnose der frühen Form der neonatalen bakteriellen Infektion (early-onset bacterial infection; EOBI) ist hoch. Ein hoher Prozentsatz wird an nichtspezifische Rezeptoren auf Erythrozyten gebunden, welcher nach Zell-Lyse bestimmt werden kann. Wir haben gezeigt, dass Lysat-IL-8 (DLWB) bei der Diagnose der EOBI gegenüber Plasma-IL-8 überlegen ist. Methoden: Um den Einfluss von prä-und perinatalen Faktoren auf Plasma-und Lysat-IL-8 zu untersuchen, wurde bei 146 nichtinfizierten Neugeborenen mit Risikofaktoren für EOBI IL-8 mittels ELISA (Immulite) zu zwei unterschiedlichen Zeitpunkten bestimmt: 0-6 (Gruppe I) und 24-30 h (Gruppe II) nach Geburt. Der Einfluss von Geschlecht, Geburtsmodus, Gestationsalter und Hämatokrit wurde untersucht. Ergebnisse: Wir fanden keinen Einfluss von Geschlecht oder Gestationsalter auf Plasma-IL-8, der Hämato-krit korrelierte positiv mit Plasma-IL-8-Konzentrationen (Gruppe I: r = 0,33, p < 0,001; Gruppe II: r = 0,30, p < 0,01). IL-8-Konzentrationen in Plasma waren primärer niedriger als nach sekundärer Sectio caesarea (p < 0,05). Das Gestationsalter korrelierte positiv mit IL-8-Werten in Lysat: (Gruppe I: r = 0,46, p < 0,001; Gruppe II: r = 0,28. p < 0,001). Schlussfolgerung: Plasma-, jedoch nicht DLWB-IL-8-Konzentrationen, korrelierten positiv mit dem Hämatokrit, wohingegen IL-8 in Lysat mit dem Gestationsalter positiv korrelierte. Dieser Sachverhalt kann bei der Interpretation von IL-8-Werten von Frühgeborenen und von Kindern mit Polyglobul...

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Section: Disclosure Statementsupporting

confidence: 81%

Section: Influence Of Hematocritmentioning

confidence: 99%

Influence of Gestational Age, Cesarean Section and Hematocrit on IL-8 Concentrations in Plasma and Detergent-Lysed Whole Blood of Noninfected Newborns

Neunhoeffer

Lipponer

Eichner

et al. 2011

Transfus Med Hemother

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“…No previous studies have identified increased IL‐12 levels in the plasma of newborns with infection. The present study shows that elevation of this cytokine and IL‐6, IFN‐ γ and IL‐1 β are associated with neonatal infection and may be more sensitive than IL‐8, a cytokine that has reportedly been increased in several studies [2,4]. However, much larger numbers are required to clarify any statistical significance between individual cytokine sensitivity for neonatal infection with other confounding conditions such as inflammatory diseases.…”

Section: Discussionmentioning

confidence: 65%

Rapid simultaneous measurement of multiple cytokines using 100 µl sample volumes − association with neonatal sepsis

Hodge

Haslam³

et al. 2004

Clinical and Experimental Immunology

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SUMMARYEarly diagnosis of neonatal infection has proved problematic due to the inadequacy of currently available laboratory tests. Neonatal sepsis is associated with an increase in plasma-derived cytokine levels, but an increase of a single cytokine cannot identify neonatal sepsis specifically and multiple cytokine levels are required. The time constraints and relatively large volume of plasma required to measure multiple cytokines from newborn infants by conventional enzyme-linked immunosorbent assay (ELISA) techniques is prohibitive. We therefore applied cytometric bead array (CBA) technology for simultaneous measurement of multiple cytokines from a group of 18 term neonates with infection confirmed by culture and a control group. 'Normal' ranges were established for each cytokine from 1-7-, 8-14-and 15-21-day-old newborns. There was no significant change in the levels of cytokines from infants in different control age groups, suggesting that basal cytokine levels are unchanged in the first 3 weeks of life. In the patient groups, however, there was a significant difference in several cytokines between the different age groups. Interleukin (IL)-6, IL-10 and IL-12 were increased significantly in the 1-7-day-old patient group compared to either the 8-14 and 15-21 age group, suggesting that infection in utero is associated with increased levels of these cytokines compared to infection acquired following birth. When individual patient cytokine levels were compared to normal control reference ranges, two patients failed to show significant elevation of any cytokine tested. All other patients showed elevated levels of between one and nine cytokines tested (mean of 4·6). There was no correlation between elevated cytokine levels and types of infective organism or patient age. In conclusion, neonatal sepsis is associated with the elevation of multiple plasma cytokines. The use of CBA kits is a rapid, easy, low sample volume and sensitive method to measure multiple plasma cytokines.Keywords cytokines cytometric bead array flow cytometry inflammatory neonatal sepsis Th1/ Th2

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“…It is well documented that certain chemokines such as CXCL1, CXCL8, and CCL2 mainly present as a cell-bound form in the circulation during various physiological and pathological conditions [34–36]. The cell-bound chemokines function as a reservoir to maintain and adjust their systemic and local level.…”

Section: Discussionmentioning

confidence: 99%

OX40 induces CCL20 expression in the context of antigen stimulation: An expanding role of co-stimulatory molecules in chemotaxis

et al. 2010

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OX40 is an inducible co-stimulatory molecule expressed by activated T cells. It plays an important role in the activation and proliferation of T lymphocytes. Recently, some co-stimulatory molecules have been shown to direct leukocyte trafficking. Chemotaxis is essential for achieving an effective immune response. CCL20 is an important chemoattractant produced by activated T cells. In this study, using DO11.10 mice whose transgenic T cell receptor specifically recognizes ovalbumin, we demonstrate that ovalbumin induces OX40 expression in CD4+ lymphocytes. Further stimulation of OX40 by OX40 activating antibody up-regulates CCL20 production. Both NF-κB dependent and independent signaling pathways are implicated in the induction of CCL20 by OX40. Finally, we primed the DO11.10 splenocytes with or without OX40 activating antibody in the presence of ovalbumin. Intranasal administration of the cell lysates derived from the cells with OX40 stimulation results in more severe leukocyte infiltration in the lung of DO11.10 mice, which is substantially attenuated by CCL20 blocking antibody. Taken together, this study has shown that activation of OX40 induces CCL20 expression in the presence of antigen stimulation. Thus, our results broaden the role of OX40 in chemotaxis, and reveal a novel effect of co-stimulatory molecules in orchestrating both T cell up-regulation and migration.

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Cell-Associated Interleukin-8 in Cord Blood of Term and Preterm Infants

Cited by 9 publications

References 19 publications

Influence of Gestational Age, Cesarean Section and Hematocrit on IL-8 Concentrations in Plasma and Detergent-Lysed Whole Blood of Noninfected Newborns

Influence of Gestational Age, Cesarean Section and Hematocrit on IL-8 Concentrations in Plasma and Detergent-Lysed Whole Blood of Noninfected Newborns

Rapid simultaneous measurement of multiple cytokines using 100 µl sample volumes − association with neonatal sepsis

OX40 induces CCL20 expression in the context of antigen stimulation: An expanding role of co-stimulatory molecules in chemotaxis

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