Human Siglec-5 Inhibitory Receptor and Immunoglobulin A (IgA) Have Separate Binding Sites in Streptococcal β Protein

Nordström, Therése; Movert, Elin; Olin, Anders I.; Ali, Shariq; Nizet, Victor; Varki, Ajit; Areschoug, Thomas

doi:10.1074/jbc.m111.251728

Cited by 26 publications

(43 citation statements)

References 37 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…The IgA-binding M4 and non-IgA-binding M4Δ451 were diluted in 10 mM sodium acetate (pH 4) (Merck, Darmstadt, Germany) and immobilized via amine coupling on separate CM5 sensor chip chambers (GE Healthcare, Uppsala, Sweden) at moderate response levels (1500 response units) as previously described (44). A flow chamber subjected to the immobilization conditions but without addition of protein was used as a control (blank) for each experiment.…”

Section: Methodsmentioning

confidence: 99%

The Combined Role of Galactose-Deficient IgA1 and Streptococcal IgA–Binding M Protein in Inducing IL-6 and C3 Secretion from Human Mesangial Cells: Implications for IgA Nephropathy

Schmitt

Ståhl

Olin

et al. 2014

The Journal of Immunology

Self Cite

View full text Add to dashboard Cite

IgA nephropathy is characterized by mesangial cell proliferation and extracellular matrix expansion associated with immune deposits consisting of galactose-deficient polymeric IgA1 and C3. We have previously shown that IgA-binding regions of streptococcal M proteins co-localize with IgA in mesangial immune deposits in patients with IgA nephropathy. In the current study, the IgA-binding M4 protein from group A streptococcus was found to bind to galactose-deficient polymeric IgA1 with higher affinity than to other forms of IgA1, as shown by surface plasmon resonance and solid-phase immunoassay. The M4 protein was demonstrated to bind to mesangial cells not via the IgA-binding region but rather via the C-terminal region, as demonstrated by flow cytometry. IgA1 enhanced binding of M4 to mesangial cells, but not vice versa. Co-stimulation of human mesangial cells with M4 and galactose-deficient polymeric IgA1 resulted in a significant increase in IL-6 secretion compared to each stimulant alone. Galactose-deficient polymeric IgA1 alone, but not M4, induced C3 secretion from the cells and co-stimulation enhanced this effect. In addition, co-stimulation enhanced mesangial cell proliferation compared to each stimulant alone. These results indicate that IgA-binding M4 protein binds preferentially to galactose-deficient polymeric IgA1 and that these proteins together induce excessive pro-inflammatory responses and proliferation of human mesangial cells. Thus, tissue deposition of streptococcal IgA-binding M proteins may contribute to the pathogenesis of IgA nephropathy.

show abstract

Section: Methodsmentioning

confidence: 99%

The Combined Role of Galactose-Deficient IgA1 and Streptococcal IgA–Binding M Protein in Inducing IL-6 and C3 Secretion from Human Mesangial Cells: Implications for IgA Nephropathy

Schmitt

Ståhl

Olin

et al. 2014

The Journal of Immunology

Self Cite

View full text Add to dashboard Cite

show abstract

“…Several serotypes of the group B Streptococci (serotypes Ia, Ib, II and V) are known to produce the Streptococcus β protein [13], which binds SHP-2 directly. SHP-2 binds to the Nterminal part of Streptococcus β protein (AA 1-152, called B6N region); this region is sufficient to trigger recruitment of SHP-2 to Siglec-5 (tested using the human monocyte cell line U937) [14]. Exact role of SHP-2 in the Streptococcus β protein signaling is poorly understood; use of the isogenic β-negative group B Streptococcus mutant revealed that the Streptococcus β protein interaction with host Siglec-5 recruits SHP-2 to Siglec-5 in U937 cells, inhibits phagocytosis of group B Streptococci by U937 cells, inhibits the IL-8 secretion of primary human neutrophils, and suppresses also the oxidative burst of primary human neutrophils and formation of neutrophil extracellular traps in response to the group B Streptococci [14].…”

Section: Streptococcal β Protein Recruits Shp-2mentioning

confidence: 99%

“…Selected inhibitors of non-metazoan PTPs:(12) benzanilide scaffold-based compound,(13) isoxazole carboxylic acid isostere 433 Da analogue,(14) brunsvicamide B, (15) brunsvicamide C,(16) iodoacetamide, (17) N-ethylmaleimide,(18)(19) isothiazolidinone derivatives, (20) nitrophenylphosphate derivative, (21) bidentate α-ketoacid-based compound, (22) salicylic acid derivative, (23) homotyrosine-based selenic acid.…”

mentioning

confidence: 99%

Finding the Smoking Gun: Protein Tyrosine Phosphatases as Tools and Targets of Unicellular Microorganisms and Viruses

Heneberg

2012

CMC

View full text Add to dashboard Cite

Protein tyrosine phosphatases (PTPs) are increasingly recognized as important effectors of host-pathogen interactions. Since Guan and Dixon reported in 1990 that phosphatase YopH serves as an essential virulence determinant of Yersinia, the field shifted significantly forward, and dozens of PTPs were identified in various microorganisms and even in viruses. The discovery of extensive tyrosine signaling networks in non-metazoan organisms refuted the moth-eaten paradigm claiming that these organisms rely exclusively on phosphoserine/phosphothreonine signaling. Similarly to humans, phosphotyrosine signaling is thought to comprise a small fraction of total protein phosphorylation, but plays a disproportionately important role in cell-cycle control, differentiation, and invasiveness. Here we summarize the state-of-art knowledge on PTPs of important non-metazoan pathogens (Listeria monocytogenes, Staphylococcus aureus, Porphyromonas gingivalis, Caulobacter crescentus, Yersinia, Synechocystis, Leishmania, Plasmodium falciparum, Entamoeba histolytica, etc.), and focus also at the microbial proteins affecting directly or indirectly the PTPs of the host (Mycobacterium tuberculosis MTSA-10, Bacillus anthracis anthrax toxin, streptococcal β protein, Helicobacter pylori CagA and VacA, Leishmania GP63 and EF-1α, Plasmodium hemozoin, etc.). This is the first review summarizing the knowledge on biological activity and pharmacological inhibition of non-metazoan PTPs, with the emphasis of those important in host-pathogen interactions. Targeting of numerous non-metazoan PTPs is simplified by the fact that they act either as ectophosphatases or are secreted outside of the pathogen. Interfering with tyrosine phosphorylation represents a powerful pharmacologic approach, and even though the PTP inhibitors are difficult to develop, lifting the fog of phosphatase inhibition is of the great market potential and further clinical impact.

show abstract

“…GBS MVs contained multiple virulence factors, including: 1) HylB, 2) CAMP factor (Christine, Atkins, Munch-Peterson factor [85]), a secreted pore-forming protein [86] that may amplify [87], but is not essential for GBS virulence [88], 3) IgA binding protein, with the ability to bind human IgA [89] for host immune evasion [90] and 4) multiple enzymes that may regulate ECM degradation [84]. Intra-amniotic administration of GBS MVs in pregnant mice caused significant damage to choriodecidual tissues and stimulated leukocytic infiltration and inflammation, leading to membrane weakening [84].…”

Section: Bacterial Factors That Promote Gbs Vaginal Colonization Ascmentioning

confidence: 99%

Perinatal Group B Streptococcal Infections: Virulence Factors, Immunity, and Prevention Strategies

Vornhagen

Waldorf

Rajagopal

2017

Trends in Microbiology

115

112

View full text Add to dashboard Cite

Summary Group B Streptococcus (GBS) or Streptococcus agalactiae are β-hemolytic, Gram-positive bacteria that are a leading cause of neonatal infections. GBS commonly colonize the lower gastrointestinal and genital tracts and during pregnancy, neonates are at risk for infection. Although intrapartum antibiotic prophylaxis during labor and delivery has decreased the incidence of early onset neonatal infection, these measures do not prevent ascending infection that can occur earlier in pregnancy leading to preterm births, stillbirths, or late onset neonatal infections. Prevention of GBS infection in pregnancy is complex and likely influenced by multiple factors including pathogenicity, host factors, vaginal microbiome, false negative screening, and/or changes in antibiotic resistance. A deeper understanding of mechanisms of GBS infections during pregnancy will facilitate the development of novel therapeutics and vaccines. Here, we summarize and discuss important advancements in our understanding of GBS vaginal colonization, ascending infection and preterm birth.

show abstract

Human Siglec-5 Inhibitory Receptor and Immunoglobulin A (IgA) Have Separate Binding Sites in Streptococcal β Protein

Cited by 26 publications

References 37 publications

The Combined Role of Galactose-Deficient IgA1 and Streptococcal IgA–Binding M Protein in Inducing IL-6 and C3 Secretion from Human Mesangial Cells: Implications for IgA Nephropathy

The Combined Role of Galactose-Deficient IgA1 and Streptococcal IgA–Binding M Protein in Inducing IL-6 and C3 Secretion from Human Mesangial Cells: Implications for IgA Nephropathy

Finding the Smoking Gun: Protein Tyrosine Phosphatases as Tools and Targets of Unicellular Microorganisms and Viruses

Perinatal Group B Streptococcal Infections: Virulence Factors, Immunity, and Prevention Strategies

Contact Info

Product

Resources

About