Selective Impairment of TLR-Mediated Innate Immunity in Human Newborns: Neonatal Blood Plasma Reduces Monocyte TNF-α Induction by Bacterial Lipopeptides, Lipopolysaccharide, and Imiquimod, but Preserves the Response to R-848

Levy, Ofer; Zarember, Kol A.; Roy, René; Cywes, Colette; Godowski, Paul J.; Wessels, Michael R.

doi:10.4049/jimmunol.173.7.4627

Cited by 338 publications

(376 citation statements)

References 28 publications

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“…TLR4 was expressed on a smaller subset of monocytes in preterm infants, but the expression was also equivalent across groups. Similar levels of mRNA and of protein expressions of TLR2 and TLR4 are reported in neonatal cells of term infants and in adult cells (35), whereas another study found that TLR4 expression increased with increasing GA (36). We conclude that differences in responses to SE in preterm infants are unlikely to result from GA-related increases in TLR2 expression.…”

Section: Monocyte Response To Staphylococcus Epidermidissupporting

confidence: 80%

Responsiveness of human monocytes to the commensal bacterium Staphylococcus epidermidis develops late in gestation

et al. 2012

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Section: Monocyte Response To Staphylococcus Epidermidissupporting

confidence: 80%

Responsiveness of human monocytes to the commensal bacterium Staphylococcus epidermidis develops late in gestation

et al. 2012

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“…The measure of responses on whole blood provides a more global determination of anti-microbial responses. Indeed, previous studies have demonstrated that neonatal plasma suppresses TLR-mediated cytokine production, indicating that both cellular and soluble humeral factors are important in the functional determination of immune responsiveness (13,14).Our data are consistent with previous studies that have measured a low surface expression of TLRs on blood mononuclear cells of preterm neonates, with TLR2 and TLR4 expression increasing during the first 2 mo of age (15). However, because TLR-dependent cytokine responses generally correlate poorly with their corresponding receptor gene or protein expression, it is important to validate the impact of a reduced expression of PRR at the functional level by examining relevant cytokine responses (6).…”

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confidence: 83%

Attenuated innate immune defenses in very premature neonates during the neonatal period

et al. 2015

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Background: Antimicrobial responses have been shown to be profoundly attenuated in very preterm neonates when examined on cord blood. However, we lack data on these responses at the time these neonates are most vulnerable to infections. Methods: Multiple cytokine responses to two prototypic Toll-like receptor (TLR) agonists: lipopolysaccharide (LPS) (TLR4) and R848 (TLR7/8) were prospectively measured in preterm neonates born ≤30 wk of gestation (n = 50) during the first 28 d of age using whole blood and single-cell multiparameter flow cytometry assays. Results were compared to term neonates (n = 30) and adult controls (n = 25). results: In preterm neonates, LPS and R848 responses remained attenuated in both cord blood and in the first 28 d of age. These responses showed significant maturation over time after adjusting for gestational age and were confirmed in monocytes and dendritic cells on a per-cell basis. We detected no major contribution of chorioamnionitis, maternal antenatal corticosteroids or magnesium sulfate treatment, labor, or mode of delivery to the maturation of cytokine responses. conclusion: Innate immune antimicrobial defenses are profoundly attenuated developmentally in very preterm neonates during the neonatal period, suggesting that exogenous factors drive the sustained systemic inflammation that has been linked to increased morbidities in these infants.d espite improvements in neonatal health care, mortality from infections has continued to increase in very preterm neonates over the last two decades, owing to the improved survival of smaller and more vulnerable infants (1). However, the underlying immunological basis of their high morbidities and high vulnerability to sepsis remains poorly understood (2). To defend themselves against infection, neonates rely on first-line, innate immune defense mechanisms. These mechanisms include the detection of specific microbial molecular structures called pathogenassociated molecular patterns through specialized receptors termed pattern recognition receptors (PRR), but also other defense mechanisms such as phagocytosis and antigen presentation to the adaptive immune system.It is widely stated that the high risk of neonatal sepsis observed in these infants is due to immature immune defense mechanisms. However, data are lacking on the development of immune functions beyond measures performed on umbilical cord blood. Recent studies have reported reduced antigen-presenting receptor expression during the first week of age in infants born below 33 wk of gestation (3,4). In contrast, phagocytic functions in these infants are more comparable to term infants (5). Toll-like receptors (TLRs) play a predominant role as a major family of PRR that act as essential "detectors" in the recognition of microbial pathogens by the innate immune system. We and others have shown that TLR-induced cytokine immune reactivity are profoundly attenuated in cord blood of very preterm neonates and develops asynchronously over the last trimester of gestation (6-10). These infants als...

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“…Based on published work (5,13,14), we usually tested cultures with R-848 at 1 g/ml to investigate its effects on HIV replication. Titrating R-848 from 10 -0.01 g/ml revealed a clear dose dependency: R-848 gradually lost its anti-HIV activity at concentrations Ͻ 0.1 g/ml (Fig.…”

Section: Dose-and Time-dependent Inhibition Of Hiv Replicationmentioning

confidence: 99%

“…The B cell line Namalwa was cultivated in RPMI 1640, 15% FCS, 1 mM sodium pyruvate, 1 mM nonessential amino acids, and 1% P/S. R-848 (InvivoGen) was used mainly at 1 g/ml (5,13,14), polyinosic: polycytidylic acid (poly(I:C); Amersham Biosciences) at 20 g/ml, flagellin from Salmonella typhimurium (provided by J. C. Sirard (Institut de Biologie de Lille, Université E0364 1, Lille, France)) at 100 g/ml, peptidoglycan from Staphylococcus aureus (Fluka) at 10 g/ml and LPS (Escherichia coli K-235; Sigma-Aldrich) at 20 g/ml. Sequences of phosphothioate-modified ssRNA (i.e., ssRNA40, 41, and 42) were identical to those published by Heil et al (6); in particular the RNA40 is a 20 mer identical to the U5 region from 108 to 127; RNA41 and 42 are 20 mer where all U or G nucleotides were replaced with adenosine, respectively (IBA).…”

Section: Cells Cell Lines and Reagentsmentioning

confidence: 99%

TLR7/8 Triggering Exerts Opposing Effects in Acute versus Latent HIV Infection

Schlaepfer¹,

Audigé²,

Joller

et al. 2006

The Journal of Immunology

105

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TLRs trigger innate immunity by recognizing conserved motifs of microorganisms. Recently, ssRNAs from HIV and influenza virus were shown to trigger TLR7 and 8. Thus, we hypothesized that HIV ssRNA, by triggering TLR7/8, affects HIV pathogenesis. Indeed, HIV ssRNA rendered human lymphoid tissue of tonsillar origin or PBMC barely permissive to HIV replication. The synthetic compound R-848, which also triggers TLR7/8, showed similar anti-HIV activity. Loss of R-848’s activity in lymphoid tissue depleted of B cells suggested a role for B cells in innate immunity. TLR7/8 triggering appears to exert antiviral effects through soluble factors: conditioned medium reduced HIV replication in indicator cells. Although a number of cytokines and chemokines were increased upon adding R-848 to lymphoid tissue, blocking those cytokines/chemokines (i.e., IFN-α receptor, IFN-γ, MIP-1α, -1β, RANTES, and stromal cell-derived factor-1) did not result in the reversal of R-848’s anti-HIV activity. Thus, the nature of this soluble factor(s) remains unknown. Unlike lymphoid tissue acutely infected with HIV, triggering latently infected promonocytic cells induced the release of HIV virions. The anti-HIV effects of triggering TLR7/8 may inhibit rapid killing, while pro-HIV effects may guarantee a certain replication level. Compounds triggering TLR7/8 may be attractive drug candidates to purge latent HIV while preventing new infections.

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Selective Impairment of TLR-Mediated Innate Immunity in Human Newborns: Neonatal Blood Plasma Reduces Monocyte TNF-α Induction by Bacterial Lipopeptides, Lipopolysaccharide, and Imiquimod, but Preserves the Response to R-848

Cited by 338 publications

References 28 publications

Responsiveness of human monocytes to the commensal bacterium Staphylococcus epidermidis develops late in gestation

Responsiveness of human monocytes to the commensal bacterium Staphylococcus epidermidis develops late in gestation

Attenuated innate immune defenses in very premature neonates during the neonatal period

TLR7/8 Triggering Exerts Opposing Effects in Acute versus Latent HIV Infection

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