Your search keyword '"Pangburn MK"' showing total 27 results

1. Mechanistic understanding for the greater sensitivity of monkeys to antisense oligonucleotide-mediated complement activation compared with humans.

Author

Shen L, Frazer-Abel A, Reynolds PR, Giclas PC, Chappell A, Pangburn MK, Younis H, and Henry SP

Subjects

Adolescent, Adult, Amino Acid Sequence, Animals, Dose-Response Relationship, Drug, Double-Blind Method, Female, Humans, Macaca fascicularis, Male, Middle Aged, Molecular Sequence Data, Oligonucleotides, Oligonucleotides, Antisense genetics, Oligoribonucleotides genetics, Young Adult, Complement Activation drug effects, Complement Activation physiology, Complement Factor H genetics, Comprehension, Oligonucleotides, Antisense pharmacology, Oligoribonucleotides pharmacology

Abstract

Differences in sensitivity of monkeys and humans to antisense oligonucleotide (ASO)-induced complement alternative pathway (AP) activation were evaluated in monkeys, humans, and in serum using biochemical assays. Transient AP activation was evident in monkeys at higher doses of two 2'-O-methoxyethyl (2'-MOE) ASOs (ISIS 426115 and ISIS 183750). No evidence of AP activation was observed in humans for either ASO, even with plasma ASO concentrations that reached the threshold for activation in monkeys. The absence of complement activation in humans is consistent with a query of the Isis Clinical Safety Database containing 767 subjects. The in vivo difference in sensitivity was confirmed in vitro, as monkey and human serum exposed to increasing concentrations of ASO indicated that monkeys were more sensitive to AP activation with this class of compounds. The mechanistic basis for the greater sensitivity of monkeys to AP activation by 2'-MOE ASO was evaluated using purified human or monkey factor H protein. The binding affinities between a representative 2'-MOE ASO and either purified protein are similar. However, the IC50 of fluid-phase complement inhibition for monkey factor H is about 3-fold greater than that for human protein using either monkey serum or factor H-depleted human serum. Interestingly, there is a sequence variant in the monkey complement factor H gene similar to a single nucleotide polymorphism in humans that is correlated with decreased factor H protein function. These findings show that monkeys are more sensitive to 2'-MOE ASO-mediated complement activation than humans likely because of differences in factor H inhibitory capacity., (Copyright © 2014 by The American Society for Pharmacology and Experimental Therapeutics.)

Published

2014

2. Essential role of surface-bound complement factor H in controlling immune complex-induced arthritis.

Author

Banda NK, Mehta G, Ferreira VP, Cortes C, Pickering MC, Pangburn MK, Arend WP, and Holers VM

Subjects

Animals, Arthritis, Experimental genetics, Cartilage immunology, Cartilage metabolism, Complement Activation immunology, Complement C3 genetics, Complement C3 immunology, Complement C3 metabolism, Complement C5 immunology, Complement C5 metabolism, Complement Factor H genetics, Complement Factor H metabolism, Joints immunology, Joints pathology, Male, Mice, Mice, Knockout, Peptides immunology, Peptides metabolism, Protein Binding, Antigen-Antibody Complex immunology, Arthritis, Experimental immunology, Complement Factor H immunology

Abstract

Factor H (fH) is an endogenous negative regulator of the alternative pathway (AP) that binds polyanions as well as complement activation fragments C3b and C3d. The AP is both necessary and sufficient to develop collagen Ab-induced arthritis (CAIA) in mice; the mechanisms whereby normal control of the AP is overcome and injury develops are unknown. Although primarily a soluble circulating protein, fH can also bind to tissues in a manner dependent on the carboxyl-terminal domain containing short consensus repeats 19 and 20. We examined the role of fH in CAIA by blocking its binding to tissues through administration of a recombinant negative inhibitor containing short consensus repeats 19 and 20 (rfH19-20), which impairs fH function and amplifies surface AP activation in vitro. Administration of rfH19-20, but not control rfH3-5, significantly worsened clinical disease activity, histopathologic injury, and C3 deposition in the synovium and cartilage in wild-type and fH(+/-) mice. In vitro studies demonstrated that rfH19-20 increased complement activation on cartilage extracts and injured fibroblast-like synoviocytes, two major targets of complement deposition in the joint. We conclude that endogenous fH makes a significant contribution to inhibition of the AP in CAIA through binding to sites of immune complex formation and complement activation.

Published

2013

3. The critical role of complement alternative pathway regulator factor H in allergen-induced airway hyperresponsiveness and inflammation.

Author

Takeda K, Thurman JM, Tomlinson S, Okamoto M, Shiraishi Y, Ferreira VP, Cortes C, Pangburn MK, Holers VM, and Gelfand EW

Subjects

Allergens immunology, Animals, Asthma immunology, Asthma metabolism, Asthma pathology, Bronchial Hyperreactivity metabolism, Female, Inflammation immunology, Inflammation metabolism, Inflammation pathology, Mice, Mice, Inbred C57BL, Ovalbumin administration & dosage, Ovalbumin immunology, Allergens administration & dosage, Bronchial Hyperreactivity immunology, Bronchial Hyperreactivity pathology, Complement Factor H physiology, Complement Pathway, Alternative immunology, Inflammation Mediators physiology

Abstract

Activation of the alternative pathway of complement plays a critical role in the development of allergen-induced airway hyperresponsiveness (AHR) and inflammation in mice. Endogenous factor H, a potent inhibitor of the alternative pathway, is increased in the airways of sensitized and challenged mice, but its role in regulating inflammation or AHR has been unknown. We found that blocking the tissue-binding function of factor H with a competitive antagonist increased complement activation and tissue inflammation after allergen challenge of sensitized mice. Conversely, administration of a fusion protein that contains the iC3b/C3d binding region of complement receptor 2 linked to the inhibitory region of factor H, a molecule directly targeting complement-activating surfaces, protected mice in both primary and secondary challenge models of AHR and lung inflammation. Thus, although endogenous factor H does play a role in limiting the development of AHR, strategies to deliver the complement-regulatory region of factor H specifically to the site of inflammation provide greater protection than that afforded by endogenous regulators. Such an agent may be an effective therapy for the treatment of asthma.

Published

2012

4. Binding of factor H to tubular epithelial cells limits interstitial complement activation in ischemic injury.

Author

Renner B, Ferreira VP, Cortes C, Goldberg R, Ljubanovic D, Pangburn MK, Pickering MC, Tomlinson S, Holland-Neidermyer A, Strassheim D, Holers VM, and Thurman JM

Subjects

Animals, Complement Pathway, Alternative, Extracellular Fluid immunology, Mice, Protein Binding, Complement Activation, Complement Factor H metabolism, Epithelial Cells metabolism, Kidney Tubules pathology, Reperfusion Injury immunology

Abstract

Factor H is a regulator of the alternative pathway of complement, and genetic studies have shown that patients with mutations in factor H are at increased risk for several types of renal disease. Pathogenic activation of the alternative pathway in acquired diseases, such as ischemic acute kidney injury, suggests that native factor H has a limited capacity to control the alternative pathway in the kidney. Here we found that an absolute deficiency of factor H produced by gene deletion prevented complement activation on tubulointerstitial cells after ischemia/reperfusion (I/R) injury, likely because alternative pathway proteins were consumed in the fluid phase. In contrast, when fluid-phase regulation by factor H was maintained while the interaction of factor H with cell surfaces was blocked by a recombinant inhibitor protein, complement activation after renal I/R increased. Finally, a recombinant form of factor H, specifically targeted to sites of C3 deposition, reduced complement activation in the tubulointerstitium after ischemic injury. Thus, although factor H does not fully prevent activation of the alternative pathway of complement on ischemic tubules, its interaction with the tubule epithelial cell surface is critical for limiting complement activation and attenuating renal injury after ischemia.

Published

2011

5. The complement inhibitors Crry and factor H are critical for preventing autologous complement activation on renal tubular epithelial cells.

Author

Renner B, Coleman K, Goldberg R, Amura C, Holland-Neidermyer A, Pierce K, Orth HN, Molina H, Ferreira VP, Cortes C, Pangburn MK, Holers VM, and Thurman JM

Subjects

Animals, Cells, Cultured, Complement Factor H biosynthesis, Complement Factor H deficiency, Complement Inactivator Proteins deficiency, Complement Pathway, Alternative immunology, Epithelial Cells cytology, Epithelial Cells metabolism, Female, Kidney Tubules cytology, Kidney Tubules metabolism, Membrane Proteins biosynthesis, Membrane Proteins deficiency, Membrane Proteins physiology, Mice, Mice, Inbred C57BL, Mice, Knockout, Protein Binding immunology, Receptors, Complement biosynthesis, Receptors, Complement deficiency, Receptors, Complement 3b, Complement Factor H physiology, Complement Inactivator Proteins physiology, Epithelial Cells immunology, Kidney Tubules immunology, Receptors, Complement physiology

Abstract

Congenital and acquired deficiencies of complement regulatory proteins are associated with pathologic complement activation in several renal diseases. To elucidate the mechanisms by which renal tubular epithelial cells (TECs) control the complement system, we examined the expression of complement regulatory proteins by the cells. We found that Crry is the only membrane-bound complement regulator expressed by murine TECs, and its expression is concentrated on the basolateral surface. Consistent with the polarized localization of Crry, less complement activation was observed when the basolateral surface of TECs was exposed to serum than when the apical surface was exposed. Furthermore, greater complement activation occurred when the basolateral surface of TECs from Crry(-/-)fB(-/-) mice was exposed to normal serum compared with TECs from wild-type mice. Complement activation on the apical and basolateral surfaces was also greater when factor H, an alternative pathway regulatory protein found in serum, was blocked from interacting with the cells. Finally, we injected Crry(-/-)fB(-/-) and Crry(+/+)fB(-/-) mice with purified factor B (an essential protein of the alternative pathway). Spontaneous complement activation was seen on the tubules of Crry(-/-)fB(-/-) mice after injection with factor B, and the mice developed acute tubular injury. These studies indicate that factor H and Crry regulate complement activation on the basolateral surface of TECs and that factor H regulates complement activation on the apical surface. However, congenital deficiency of Crry or reduced expression of the protein on the basolateral surface of injured cells permits spontaneous complement activation and tubular injury.

Published

2010

6. Complement control protein factor H: the good, the bad, and the inadequate.

Author

Ferreira VP, Pangburn MK, and Cortés C

Subjects

Animals, Complement C3b immunology, Complement C3b metabolism, Complement C3d immunology, Complement C3d metabolism, Complement Factor H genetics, Complement Factor H metabolism, Humans, Models, Immunological, Protein Binding, Complement Factor H immunology, Complement Pathway, Alternative immunology, Immune Evasion immunology

Abstract

The complement system is an essential component of the innate immune system that participates in elimination of pathogens and altered host cells and comprises an essential link between the innate and adaptive immune system. Soluble and membrane-bound complement regulators protect cells and tissues from unintended complement-mediated injury. Complement factor H is a soluble complement regulator essential for controlling the alternative pathway in blood and on cell surfaces. Normal recognition of self-cell markers (i.e. polyanions) and C3b/C3d fragments is necessary for factor H function. Inadequate recognition of host cell surfaces by factor H due to mutations and polymorphisms have been associated with complement-mediated tissue damage and disease. On the other hand, unwanted recognition of pathogens and altered self-cells (i.e. cancer) by factor H is used as an immune evasion strategy. This review will focus on the current knowledge related to these versatile recognition properties of factor H., (Copyright 2010 Elsevier Ltd. All rights reserved.)

Published

2010

7. The binding of factor H to a complex of physiological polyanions and C3b on cells is impaired in atypical hemolytic uremic syndrome.

Author

Ferreira VP, Herbert AP, Cortés C, McKee KA, Blaum BS, Esswein ST, Uhrín D, Barlow PN, Pangburn MK, and Kavanagh D

Subjects

Animals, Cells, Cultured, Complement Factor H genetics, Erythrocytes pathology, Genetic Predisposition to Disease, Hemolytic-Uremic Syndrome immunology, Hemolytic-Uremic Syndrome pathology, Humans, Polyelectrolytes, Polymers metabolism, Protein Binding genetics, Sheep, Complement C3b metabolism, Complement Factor H metabolism, Erythrocytes immunology, Hemolytic-Uremic Syndrome genetics, Heparin metabolism, Mutation

Abstract

Factor H (fH) is essential for complement homeostasis in fluid-phase and on surfaces. Its two C-terminal domains (CCP 19-20) anchor fH to self-surfaces where it prevents C3b amplification in a process requiring its N-terminal four domains. In atypical hemolytic uremic syndrome (aHUS), mutations clustering toward the C terminus of fH may disrupt interactions with surface-associated C3b or polyanions and thereby diminish the ability of fH to regulate complement. To test this, we compared a recombinant protein encompassing CCP 19-20 with 16 mutants. The mutations had only very limited and localized effects on protein structure. Although we found four aHUS-linked fH mutations that decreased binding to C3b and/or to heparin (a model compound for cell surface polyanionic carbohydrates), we identified five aHUS-associated mutants with increased affinity for either or both ligands. Strikingly, these variable affinities for the individual ligands did not correlate with the extent to which all the aHUS-associated mutants were found to be impaired in a more physiological assay that measured their ability to inhibit cell surface complement functions of full-length fH. Taken together, our data suggest that disruption of a complex fH-self-surface recognition process, involving a balance of affinities for protein and physiological carbohydrate ligands, predisposes to aHUS.

Published

2009

8. Factor H mediated cell surface protection from complement is critical for the survival of PNH erythrocytes.

Author

Ferreira VP and Pangburn MK

Subjects

Adult, CD55 Antigens metabolism, CD59 Antigens metabolism, Case-Control Studies, Complement Factor H antagonists & inhibitors, Erythrocyte Aging, Flow Cytometry, Humans, Blood Proteins physiology, Cell Survival, Complement Factor H metabolism, Complement System Proteins metabolism, Erythrocyte Membrane metabolism, Erythrocytes physiology, Hemoglobinuria, Paroxysmal blood, Hemolysis

Abstract

Paroxysmal nocturnal hemoglobinuria (PNH) cells are partially (type II) or completely (type III) deficient in GPI-linked complement regulatory proteins CD59 and CD55. PNH III erythrocytes circulate 6 to 60 days in vivo. Why these cells are not lysed as rapidly by complement as unprotected foreign cells, which normally lyse within minutes, remains undetermined. Factor H plays a key role in the homeostasis of complement in fluid phase and on cell surfaces. We have recently shown that a recombinant protein encompassing the C-terminus of factor H (rH19-20) specifically blocks cell-surface complement regulatory functions of factor H without affecting fluid-phase control of complement. Here we show that PNH II and III cells become highly susceptible to complement-mediated lysis by nonacidified normal human serum in vitro, when the cell surface complement-regulatory functions of factor H are blocked. The results indicate that cells deficient in surface-bound regulators are protected for extended periods of time by factor H.

Published

2007

9. Structure shows that a glycosaminoglycan and protein recognition site in factor H is perturbed by age-related macular degeneration-linked single nucleotide polymorphism.

Author

Herbert AP, Deakin JA, Schmidt CQ, Blaum BS, Egan C, Ferreira VP, Pangburn MK, Lyon M, Uhrín D, and Barlow PN

Subjects

Aging genetics, Aging pathology, Anticoagulants metabolism, Anticoagulants pharmacology, Apoptosis physiology, Binding Sites physiology, Complement Factor H chemistry, Heparin metabolism, Heparin pharmacology, Histidine genetics, Humans, Macular Degeneration metabolism, Protein Structure, Quaternary, Protein Structure, Tertiary, Surface Plasmon Resonance, Tyrosine genetics, Complement Factor H genetics, Complement Factor H metabolism, Glycosaminoglycans metabolism, Macular Degeneration genetics, Macular Degeneration pathology, Polymorphism, Single Nucleotide

Abstract

A common single nucleotide polymorphism in the factor H gene predisposes to age-related macular degeneration. Factor H blocks the alternative pathway of complement on self-surfaces bearing specific polyanions, including the glycosaminoglycan chains of proteoglycans. Factor H also binds C-reactive protein, potentially contributing to noninflammatory apoptotic processes. The at risk sequence contains His (rather than Tyr) at position 402 (384 in the mature protein), in the seventh of the 20 complement control protein (CCP) modules (CCP7) of factor H. We expressed both His(402) and Tyr(402) variants of CCP7, CCP7,8, and CCP6-8. We determined structures of His(402) and Tyr(402) CCP7 and showed them to be nearly identical. The side chains of His/Tyr(402) have similar, solvent-exposed orientations far from interfaces with CCP6 and -8. Tyr(402) CCP7 bound significantly more tightly than His(402) CCP7 to a heparin affinity column as well as to defined-length sulfated heparin oligosaccharides employed in gel mobility shift assays. This observation is consistent with the position of the 402 side chain on the edge of one of two glycosaminoglycan-binding surface patches on CCP7 that we inferred on the basis of chemical shift perturbation studies with a sulfated heparin tetrasaccharide. According to surface plasmon resonance measurements, Tyr(402) CCP6-8 binds significantly more tightly than His(402) CCP6-8 to immobilized C-reactive protein. The data support a causal link between H402Y and age-related macular degeneration in which variation at position 402 modulates the response of factor H to age-related changes in the glycosaminoglycan composition and apoptotic activity of the macula.

Published

2007

10. Critical role of the C-terminal domains of factor H in regulating complement activation at cell surfaces.

Author

Ferreira VP, Herbert AP, Hocking HG, Barlow PN, and Pangburn MK

Subjects

Animals, Binding Sites, Binding, Competitive, Complement Factor H genetics, Erythrocytes immunology, Hemolysis immunology, Humans, Protein Structure, Tertiary genetics, Protein Structure, Tertiary physiology, Recombinant Proteins genetics, Recombinant Proteins metabolism, Complement Activation, Complement C3b metabolism, Complement Factor H metabolism, Erythrocyte Membrane immunology

Abstract

The plasma protein factor H primarily controls the activation of the alternative pathway of complement. The C-terminal of factor H is known to be involved in protection of host cells from complement attack. In the present study, we show that domains 19-20 alone are capable of discriminating between host-like and complement-activating cells. Furthermore, although factor H possesses three binding sites for C3b, binding to cell-bound C3b can be almost completely inhibited by the single site located in domains 19-20. All of the regulatory activities of factor H are expressed by the N-terminal four domains, but these activities toward cell-bound C3b are inhibited by isolated recombinant domains 19-20 (rH 19-20). Direct competition with the N-terminal site is unlikely to explain this because regulation of fluid phase C3b is unaffected by domains 19-20. Finally, we show that addition of isolated rH 19-20 to normal human serum leads to aggressive complement-mediated lysis of normally nonactivating sheep erythrocytes and moderate lysis of human erythrocytes, which possess membrane-bound regulators of complement. Taken together, the results highlight the importance of the cell surface protective functions exhibited by factor H compared with other complement regulatory proteins. The results may also explain why atypical hemolytic uremic syndrome patients with mutations affecting domains 19-20 can maintain complement homeostasis in plasma while their complement system attacks erythrocytes, platelets, endothelial cells, and kidney tissue.

Published

2006

11. Disease-associated sequence variations congregate in a polyanion recognition patch on human factor H revealed in three-dimensional structure.

Author

Herbert AP, Uhrín D, Lyon M, Pangburn MK, and Barlow PN

Subjects

Amino Acid Sequence, Complement C3d chemistry, Heparin chemistry, Humans, Magnetic Resonance Spectroscopy methods, Molecular Sequence Data, Pichia metabolism, Polymorphism, Genetic, Protein Conformation, Saccharomyces cerevisiae metabolism, Sequence Homology, Amino Acid, Anions chemistry, Complement Factor H chemistry

Abstract

Mutations and polymorphisms in the regulator of complement activation, factor H, have been linked to atypical hemolytic uremic syndrome (aHUS), membranoproliferative glomerulonephritis, and age-related macular degeneration. Many aHUS patients carry mutations in the two C-terminal modules of factor H, which normally confer upon this abundant 155-kDa plasma glycoprotein its ability to selectively bind self-surfaces and prevent them from inappropriately triggering the complement cascade via the alternative pathway. In the current study, the three-dimensional solution structure of the C-terminal module pair of factor H has been determined. A binding site for a fully sulfated heparin-derived tetrasaccharide has been delineated using chemical shift mapping and the C3d/C3b-binding site inferred from sequence comparisons and computational docking. The resultant information allows assessment of the likely consequences of aHUS-associated amino acid substitutions in this critical region of factor H. It is striking that, excepting those likely to perturb the three-dimensional structure, aHUS-associated missense mutations congregate in the polyanion-binding site delineated in this study, thus potentially disrupting a vital mechanism for control of complement on self-surfaces in the microvasculature of the kidney. It is intriguing that a single nucleotide polymorphism predisposing to age-related macular degeneration occupies another region of factor H that harbors a polyanion-binding site.

Published

2006

12. Disease-associated sequence variations in factor H: a structural biology approach.

Author

Herbert AP, Soares DC, Pangburn MK, and Barlow PN

Subjects

Aging physiology, Animals, Complement Activation, Hemolytic-Uremic Syndrome immunology, Hemolytic-Uremic Syndrome pathology, Humans, Macular Degeneration immunology, Macular Degeneration pathology, Models, Molecular, Molecular Sequence Data, Protein Isoforms chemistry, Protein Isoforms genetics, Protein Isoforms metabolism, Amino Acid Sequence, Complement Factor H chemistry, Complement Factor H genetics, Complement Factor H metabolism, Complement Inactivating Agents chemistry, Complement Inactivating Agents metabolism, Polymorphism, Genetic, Protein Conformation

Published

2006

13. In vivo binding of complement regulator factor H by Streptococcus pneumoniae.

Author

Quin LR, Carmicle S, Dave S, Pangburn MK, Evenhuis JP, and McDaniel LS

Subjects

Animals, Bacteremia microbiology, Bacterial Proteins genetics, Flow Cytometry, Humans, Mice, Mice, Inbred CBA, Pneumococcal Infections microbiology, RNA, Messenger genetics, RNA, Messenger metabolism, Bacterial Proteins metabolism, Complement Factor H metabolism, Streptococcus pneumoniae metabolism, Streptococcus pneumoniae pathogenicity

Abstract

Pneumococcal surface protein C (PspC) binds to the complement regulatory protein factor H (FH), which inhibits alternative pathway activation. In the present study, using a mouse model of systemic infection and flow-cytometric analyses, we demonstrated an in vivo interaction between FH and pneumococci and showed differential FH binding during bacteremia. Flow-cytometric analyses of pneumococci harvested after intraperitoneal (ip) challenge demonstrated increased binding of FH, compared with that after intravenous (iv) challenge. Real-time polymerase chain reaction analyses of PspC mRNA showed that, relative to pneumococci grown in vitro, those recovered from the blood of mice 24 h after iv challenge exhibited 23-fold higher mRNA levels; however, after ip challenge, PspC mRNA induction was increased 870-fold. A subsequent increase in PspC expression was detected by flow cytometry using a monoclonal antibody against PspC. Furthermore, pneumococci with FH bound to complement before exposure had increased proliferation, compared with pneumococci not pretreated with FH. These results suggest that the interaction between PspC and FH contributes to pneumococcal virulence.

Published

2005

14. Dual roles of PspC, a surface protein of Streptococcus pneumoniae, in binding human secretory IgA and factor H.

Author

Dave S, Carmicle S, Hammerschmidt S, Pangburn MK, and McDaniel LS

Subjects

Bacterial Proteins chemistry, Binding Sites, Blotting, Western, Humans, Surface Plasmon Resonance, Bacterial Proteins physiology, Complement Factor H metabolism, Immunoglobulin A, Secretory metabolism

Abstract

Streptococcus pneumoniae, also known as the pneumococcus, contains several surface proteins that along with the polysaccharide capsule function in antiphagocytic activities and evasion of the host immune system. These pneumococcal proteins interact with the host immune system in various ways and possess a wide range of biological activities that suggests that they may be involved at different stages of pneumococcal infection. PspC, also known as CbpA and SpsA, is one of several pneumococcal surface proteins that binds host proteins, including factor H (FH) and secretory IgA (sIgA) via the secretory component. Previous work by our laboratory has demonstrated that PspC on the surface of live pneumococcal cells binds FH. This paper provides evidence that FH activity is maintained in the presence of PspC and that the PspC binding site is located in the short consensus repeat 6-10 region of FH. We also report for the first time that although both FH and sIgA binding has been localized to the alpha-helical domain of PspC, the binding of FH to PspC is not inhibited by sIgA. ELISA, surface plasmon resonance, and flow cytometry indicate that the two host proteins do not compete for binding with PspC and likely do not share the same binding sites. We confirmed by Western analysis that the binding sites are separate using recombinant PspC proteins. These PspC variants bind FH yet fail to bind sIgA. Thus, we conclude that FH and sIgA can bind concurrently to the alpha-helical region of PspC.

Published

2004

15. Interaction of human factor H with PspC of Streptococcus pneumoniae.

Author

Dave S, Pangburn MK, Pruitt C, and McDaniel LS

Subjects

Base Sequence, Binding Sites, DNA Primers, Flow Cytometry, Humans, Bacterial Proteins metabolism, Complement Factor H metabolism, Streptococcus pneumoniae metabolism

Abstract

Background & Objectives: Streptococcus pneumoniae has acquired virulence factors such as the polysaccharide capsule and various surface proteins, which prevent opsonization mediated by the complement system. PspC is one of the multi-functional pneumococcal surface proteins capable of eliciting an antibody response in mice. Our study further explores the role of pneumococcal surface proteins in resistance to complement mediated opsonophagocytosis by providing evidence that PspC binds human Factor H (FH), a regulatory protein of the alternative complement pathway. The present study was carried out to map the binding regions on PspC and FH, and to assess the functional activity of FH upon binding to PspC., Methods: FH binding to D39 and other pneumococcal strains was observed by flow cytometry. A series of FH truncated and deletion mutants and PspC mutants were used to localize binding regions within these molecules. The functional activity of FH upon binding to PspC was measured by a haemolysis assay., Results: FH binding to D39 and not to TRE108 (PspC-) cells was demonstrated by flow cytometry. Pneumococcal isolates of 14 different strains varied in their ability to bind FH. The binding region of FH within PspC to the first 225 amino acids of the alpha-helical domain was localized. The corresponding binding site for PspC is located within the SCR 6-10 region of FH. Haemolysis of rabbit red blood cells was inhibited by FH even in the presence of PspC., Interpretation & Conclusion: FH binding is specific to PspC on the pneumococcal cell surface. The binding region on PspC mapped to the non-conserved N-terminal region of the alpha-helical domain. The binding site on FH to PspC is different from the active site that functions in degradation of C3b. A haemolysis assay provided evidence that the functional activity of FH was maintained upon binding to PspC. Thus, binding of FH to PspC might be an important mechanism by which S. pneumoniae resist complement activation and opsonophagocytosis.

Published

2004

16. Cutting edge: localization of the host recognition functions of complement factor H at the carboxyl-terminal: implications for hemolytic uremic syndrome.

Author

Pangburn MK

Subjects

Animals, Complement Factor H genetics, Complement Factor H physiology, Complement Pathway, Alternative genetics, Complement Pathway, Alternative immunology, Hemolysis genetics, Hemolysis immunology, Hemolytic-Uremic Syndrome genetics, Humans, Mutagenesis, Site-Directed, Peptide Fragments genetics, Peptide Fragments physiology, Polyelectrolytes, Polymers metabolism, Protein Structure, Tertiary genetics, Rabbits, Recombinant Proteins genetics, Recombinant Proteins metabolism, Recombinant Proteins pharmacology, Sequence Deletion immunology, Sheep, Complement Factor H metabolism, Hemolytic-Uremic Syndrome immunology, Peptide Fragments metabolism

Abstract

Incidents of hemolytic uremic syndrome (HUS) include a subset of patients that exhibit mutations in C factor H. These mutations cluster in the C-terminal domains of factor H where previous reports have identified polyanion and C3b-binding sites. In this study, we show that recombinant human factor H with deletions at the C-terminal end of the protein loses the ability to control the spontaneous activation of the alternative C pathway on host-like surfaces. For the pathology of HUS, the findings imply that mutations that disrupt the normal functions of the C-terminal domains prevent host polyanion recognition. The resulting uncontrolled activation of complement on susceptible host tissues appears to be the initiating event behind the acute renal failure of familial HUS patients.

Published

2002

17. PspC, a pneumococcal surface protein, binds human factor H.

Author

Dave S, Brooks-Walter A, Pangburn MK, and McDaniel LS

Subjects

Blotting, Western, Humans, Bacterial Proteins metabolism, Calcium-Binding Proteins metabolism, Complement Factor H metabolism, Protozoan Proteins

Abstract

PspC was found to bind human complement factor H (FH) by Western blot analysis of D39 (pspC(+)) and an isogenic mutant TRE108 (pspC). We confirmed that PspA does not bind FH, while purified PspC binds FH very strongly. The binding of FH to exponentially growing pneumococci varied among different isolates when analyzed by fluorescence activated cell sorting analysis.

Published

2001

18. Host recognition and target differentiation by factor H, a regulator of the alternative pathway of complement.

Author

Pangburn MK

Subjects

Animals, Binding Sites, Complement Factor H chemistry, Humans, Infections immunology, Protein Structure, Tertiary, Complement Factor H physiology, Complement Pathway, Alternative physiology

Abstract

Factor H is responsible for recognition of host cells and tissues and mediates discrimination among microbial pathogens during activation of the alternative pathway of complement (AP). Its unique structure of 20 SCR domains arranged in a flexible chain permits a variety of functional sites to interact with complement proteins and surface markers in a biological example of single-molecule combinatorial chemistry. In addition to the complement regulatory site located in the N-terminal four SCR domains, two other sites bind complement protein C3b and three sites appear to recognize a variety of polyanions that serve as host markers. Recent studies indicate that cooperativity among several C3b- and polyanion-binding sites influences the biological functions of factor H and that the degree of influence of each site varies on different cells. The engagement of one or more of the host marker recognition sites enables factor H to control activation of the AP. The absence of host-like markers allows AP activation, but many common pathogens have developed receptors for factor H or mimics of host markers of varying degrees of authenticity allowing them to escape detection by this innate defense system. Organisms using one or more of these evasive techniques include Neisseria gonorrhoeae, Streptococcus pyogenes, Yersinia enterocolitica, Trypanosoma cruzi, and the HIV virus.

Published

2000

19. Molecular mechanisms of target recognition in an innate immune system: interactions among factor H, C3b, and target in the alternative pathway of human complement.

Author

Pangburn MK, Pangburn KL, Koistinen V, Meri S, and Sharma AK

Subjects

Animals, CD55 Antigens metabolism, Complement C3-C5 Convertases metabolism, Complement Factor H genetics, Complement Pathway, Alternative genetics, Erythrocyte Membrane immunology, Erythrocyte Membrane metabolism, Humans, Immunity, Innate, Mutagenesis, Site-Directed, Protein Binding immunology, Protein Structure, Tertiary, Rabbits, Recombinant Proteins immunology, Recombinant Proteins metabolism, Sequence Deletion, Sheep, Complement C3b metabolism, Complement Factor H metabolism, Complement Pathway, Alternative immunology

Abstract

In the alternative pathway of complement (APC) factor H is the primary control factor involved in discrimination between potential pathogens. The APC deposits C3b on possible Ags, and the interaction with factor H determines whether the initial C3b activates the APC. Factor H is composed of a linear array of 20 homologous short consensus repeats (SCR) domains with many functional sites. Three of these sites are involved in binding C3b and regulating complement activation; others bind to sialic acid and/or heparin and are responsible for host recognition. Using site-directed mutations we have examined the contributions of each of these sites to target discrimination and to functional activities of factor H. Decay acceleration by SCR1-4 of C3/C5 convertases bound to nonactivators was strongly dependent on SCR domains 11-15 and 16-20. Loss of these regions caused a 97% loss of activity, with SCR16-20 being the most critical (>90% loss). On APC activators the pattern of site usage was different and unique on each. On yeast, deletion of the 10 C-terminal domains (SCR11-20) had no effect on specific activity. On rabbit erythrocytes, this deletion caused loss of 75% of the specific activity. An examination of binding affinity to C3b on the four cell types demonstrated that factor H exhibits a unique pattern of SCR involvement on each cell. The results reveal a complex molecular mechanism of discrimination between microbes and host in this ancient innate defense system and help explain the different rates and intensities of APC activation on different biological particles.

Published

2000

20. Nephritogenic lambda light chain dimer: a unique human miniautoantibody against complement factor H.

Author

Jokiranta TS, Solomon A, Pangburn MK, Zipfel PF, and Meri S

Subjects

Amino Acid Sequence, Autoantibodies metabolism, Autoantibodies physiology, Binding Sites, Antibody, Complement Factor H antagonists & inhibitors, Complement Factor H metabolism, Complement Inactivator Proteins physiology, Complement Pathway, Alternative immunology, Crystallography, X-Ray, Dimerization, Female, Glomerulonephritis, Membranoproliferative metabolism, Humans, Immunoglobulin lambda-Chains metabolism, Immunoglobulin lambda-Chains physiology, Middle Aged, Models, Molecular, Molecular Sequence Data, Structure-Activity Relationship, Autoantibodies chemistry, Complement Factor H immunology, Glomerulonephritis, Membranoproliferative immunology, Immunoglobulin lambda-Chains chemistry

Abstract

A unique monoclonal Ig lambda light chain dimer (protein LOI) was isolated from the serum and urine of a patient with hypocomplementemic membranoproliferative glomerulonephritis. In vitro the lambda light chain dimer efficiently activated the alternative pathway of complement (AP). When added to normal human serum, LOI temporarily enhanced AP hemolytic activity, but during a prolonged incubation the hemolytic activity was depleted. Protein LOI was found to bind to factor H, the main regulator molecule of AP. By binding to the short consensus repeat domain 3 of factor H, the dimer LOI blocked one of three interaction sites between H and C3b and thus inhibited the activity of H and induced an uncontrolled activation of the AP. Structural analysis showed that LOI belonged to the Vlambda3a subgroup of lambda light chains. The variable (V) region of LOI was most closely related to the predicted product of the Vlambda3 germline gene Iglv3s2, although it contained several unique residues that in a tertiary homology model structure form an unusual ring of charged residues around a hydrophobic groove in the putative Ag binding site. This site fitted considerably well with a putative binding site in the molecular model of domain 3 of factor H containing a reciprocal ring of charged amino acids around a hydrophobic area. Apparently, functional blocking of factor H by the Ab fragment-like lambda light chain dimer had initiated the development of a severe form of membranoproliferative glomerulonephritis. Thus, the lambda light chain dimer LOI represents the first described pathogenic miniautoantibody in human disease.

Published

1999

21. Binding of complement factor H to loop 5 of porin protein 1A: a molecular mechanism of serum resistance of nonsialylated Neisseria gonorrhoeae.

Author

Ram S, McQuillen DP, Gulati S, Elkins C, Pangburn MK, and Rice PA

Subjects

Amino Acid Sequence, Animals, Binding Sites, Blood Bactericidal Activity, Complement Factor H immunology, Humans, Molecular Sequence Data, Porins immunology, Rabbits, Sialic Acids metabolism, Complement Factor H metabolism, Neisseria gonorrhoeae immunology, Porins metabolism

Abstract

Neisseria gonorrhoeae isolated from patients with disseminated infection are often of the porin (Por1A) serotype and resist killing by nonimmune normal human serum. The molecular basis of this resistance (termed stable serum resistance) in these strains has not been fully defined but is not related to sialylation of lipooligosaccharide. Here we demonstrate that Por1A bearing gonococcal strains bind more factor H, a critical downregulator of the alternative complement pathway, than their Por1B counterparts. This results in a sevenfold reduction in C3b, which is >75% converted to iC3b. Factor H binding to isogenic gonococcal strains that differed only in their porin serotype, confirmed that Por1A was the acceptor molecule for factor H. We identified a surface exposed region on the Por1A molecule that served as the binding site for factor H. We used gonococcal strains with hybrid Por1A/B molecules that differed in their surface exposed domains to localize the factor H binding site to loop 5 of Por1A. This was confirmed by inhibition of factor H binding using synthetic peptides corresponding to the putative exposed regions of the porin loops. The addition of Por1A loop 5 peptide in a serum bactericidal assay, which inhibited binding of factor H to the bacterial surface, permitted 50% killing of an otherwise completely serum resistant gonococcal strain. Collectively, these data provide a molecular basis to explain serum resistance of Por1A strains of N. gonorrhoeae.

Published

1998

22. A novel sialic acid binding site on factor H mediates serum resistance of sialylated Neisseria gonorrhoeae.

Author

Ram S, Sharma AK, Simpson SD, Gulati S, McQuillen DP, Pangburn MK, and Rice PA

Subjects

Antigens, Bacterial chemistry, Gonorrhea blood, Humans, Neisseria gonorrhoeae immunology, Neisseria gonorrhoeae metabolism, Neuraminidase pharmacology, Repetitive Sequences, Nucleic Acid, Antigens, Bacterial immunology, Complement C3b immunology, Complement C3b metabolism, Complement Factor H physiology, Gonorrhea immunology, Lipopolysaccharides metabolism, Neisseria gonorrhoeae pathogenicity, Sialic Acids metabolism

Abstract

Factor H (fH), a key alternative complement pathway regulator, is a cofactor for factor I-mediated cleavage of C3b. fH consists of 20 short consensus repeat (SCR) domains. Sialic acid binding domains have previously been localized to fH SCRs 6-10 and 13. To examine fH binding on a sialylated microbial surface, we grew Neisseria gonorrhoeae in the presence of 5'-cytidinemonophospho-N-acetylneuraminic acid, which sialylates lipooligosaccharide and converts to serum resistance gonococci previously sensitive to nonimmune serum killing. fH domains necessary for binding sialylated gonococci were determined by incubating organisms with recombinant human fH (rH) and nine mutant rH molecules (deletions spanning the entire fH molecule). rH and all mutant rH molecules that contained SCRs 16-20 bound to the sialylated strain; no mutant molecule bound to serum-sensitive nonsialylated organisms. Sialic acid was demonstrated to be the fH target by flow cytometry that showed a fourfold increase in fH binding that was reversed by neuraminidase-mediated cleavage of sialic acid off gonococci. Functional specificity of fH was confirmed by decreased total C3 binding and almost complete conversion to iC3b on sialylated gonococci. Sialic acid can therefore bind fH uniquely through SCRs 16-20. This blocks complement pathway activation for N. gonorrhoeae at the level of C3.

Published

1998

23. Localization by site-directed mutagenesis of the site in human complement factor H that binds to Streptococcus pyogenes M protein.

Author

Sharma AK and Pangburn MK

Subjects

Animals, Bacterial Proteins genetics, Complement Factor H genetics, Mutagenesis, Site-Directed, Protein Binding genetics, Protein Binding immunology, Recombinant Proteins metabolism, Spodoptera, Streptococcus pyogenes genetics, Antigens, Bacterial, Bacterial Outer Membrane Proteins, Bacterial Proteins immunology, Bacterial Proteins metabolism, Carrier Proteins, Complement Factor H metabolism, Streptococcus pyogenes immunology, Streptococcus pyogenes metabolism

Abstract

M-protein receptors located on Streptococcus pyogenes cells are known to bind human plasma protein factor H. Human factor H is composed of 20 short consensus repeat (SCR) domains containing approximately 60 amino acids each. Factor H controls the activation of the alternative pathway of complement in plasma. We have scanned the entire human factor H molecule by site-directed deletion mutagenesis, expressed the recombinant proteins in insect cells using the baculovirus system, and measured the binding of different purified mutant proteins to three strains of S. pyogenes. These studies have revealed that recombinant factor H lacking SCR domains 6 to 10 does not bind to wild-type M+ S. pyogenes JRS4. Experiments performed with S. pyogenes JRS251, in which both C-repeat domains of M protein were deleted, demonstrated that all of the factor H mutant proteins bound weakly to these cells except those lacking the SCR region from domains 6 to 10. Neither human factor H nor any of the recombinant proteins bound to the M- strain JRS145. Our results indicate that the only binding site on human factor H that interacts with streptococcus M protein is located in SCR domains 6 to 10 of factor H and that regions of M protein outside the C-repeat domains are involved in binding factor H.

Published

1997

24. Identification of three physically and functionally distinct binding sites for C3b in human complement factor H by deletion mutagenesis.

Author

Sharma AK and Pangburn MK

Subjects

Animals, Binding Sites, Fibrinogen metabolism, Heparin metabolism, Humans, Mutagenesis, Site-Directed, Nucleopolyhedroviruses, Protein Binding, Sequence Deletion, Spodoptera, Structure-Activity Relationship, Complement C3b metabolism, Complement Factor H metabolism

Abstract

Human complement factor H controls spontaneous activation of complement in plasma and appears to play a role in distinguishing host cells from activators of the alternative pathway of complement. In both mice and humans, the protein is composed of 20 homologous short consensus repeat (SCR) domains. The size of the protein suggests that portions of the structure outside the known C3b binding site (SCR 1-4) possess a significant biological role. We have expressed the full-length cDNA of factor H in the baculovirus system and have shown the recombinant protein to be fully active. Mutants of this full-length protein have now been prepared, purified, and examined for cofactor activity and binding to C3b and heparin. The results demonstrate (i) that factor H has at least three sites that bind C3b, (ii) that one of these sites is located in SCR domains 1-4, as has been shown by others, (iii) that a second site exists in the domain 6-10 region, (iv) that a third site resides in the SCR 16-20 region, and (v) that two heparin binding sites exist in factor H, one near SCR 13 and another in the SCR 6-10 region. Functional assays demonstrated that only the first C3b site located in SCR 1-4 expresses factor I cofactor activity. Mutant proteins lacking any one of the three C3b binding sites exhibited 6- to 8-fold reductions in affinity for C3b on sheep erythrocytes, indicating that all three sites contribute to the control of complement activation on erythrocytes. The identification of multiple functionally distinct sites on factor H clarifies many of the heretofore unexplainable behaviors of this protein, including the heterogeneous binding of factor H to surface-bound C3b, the effects of trypsin cleavage, and the differential control of complement activation on activators and nonactivators of the alternative pathway of complement.

Published

1996

25. Analysis of the recognition mechanism of the alternative pathway of complement by monoclonal anti-factor H antibodies: evidence for multiple interactions between H and surface bound C3b.

Author

Jokiranta TS, Zipfel PF, Hakulinen J, Kühn S, Pangburn MK, Tamerius JD, and Meri S

Subjects

Animals, Antibodies, Monoclonal, Antibody Specificity, Binding Sites, Antibody, Blotting, Western, Complement C3b analysis, Complement C3b immunology, Complement Factor H analysis, Complement Factor H immunology, Cross-Linking Reagents, Humans, Mice, Mice, Inbred BALB C, Peptide Mapping, Radioimmunoassay, Recombinant Proteins analysis, Recombinant Proteins immunology, Recombinant Proteins metabolism, Trypsin, Complement C3b metabolism, Complement Factor H metabolism, Complement Pathway, Alternative

Abstract

The ability of the alternative pathway of complement to discriminate targets as either activators or non-activators is mediated by different binding properties of factor H to surface-associated C3b molecules. In the present study we have probed the interaction between H and C3b using five anti-H mAb. The binding sites of the mAb were mapped by Western blotting using both recombinant and trypsin-generated H fragments. Two mAb bound to CCP1 (90X, 196X), two to CCP5 (MRC OX24, 86X) and one to CCP8-15a (131X). At a molar ratio 2:1 of 125I-H:mAb all tested mAb enhanced binding of H to both activator- and non-activator-bound C3b. At higher concentrations two mAb had an inhibitory effect on H binding to surface-associated C3b (OX24, 131X). Thus the mAb 131X inhibits H binding to surface-bound C3b but unlike OX24 it does not bind to the previously described C3b binding site within or near CCP4-5. These results indicate that there is an additional interaction site on factor H for surface-bound C3b.

Published

1996

26. Biologically active recombinant human complement factor H: synthesis and secretion by the baculovirus system.

Author

Sharma AK and Pangburn MK

Subjects

Animals, Baculoviridae, Complement C3b metabolism, Complement Factor H metabolism, Genetic Vectors, Humans, Moths, Recombinant Proteins metabolism, Complement Factor H biosynthesis, Recombinant Proteins biosynthesis

Abstract

A complete cDNA clone (4.3 kb) encoding human complement factor H (hCFH; 155 kDa) has been cloned into the pVL1393 baculovirus expression vector and transfected into Spodoptera frugiperda Sf9 insect cells. A biologically active (92 +/- 15%) 140-kDa protein was secreted into the medium with a yield of more than 5 mg/liter. This is the first report of synthesis of biologically active recombinant hCFH in a heterologous system.

Published

1994

27. Regulation of alternative pathway complement activation by glycosaminoglycans: specificity of the polyanion binding site on factor H.

Author

Meri S and Pangburn MK

Subjects

Anions, Binding Sites, Carrageenan pharmacology, Chondroitin Sulfates pharmacology, Complement C3 metabolism, Complement C3b metabolism, Dextran Sulfate pharmacology, Glycoconjugates pharmacology, Heparin pharmacology, Heparitin Sulfate pharmacology, Humans, Hyaluronic Acid pharmacology, Keratan Sulfate pharmacology, Kinetics, Complement Factor H metabolism, Complement Pathway, Alternative drug effects, Glycosaminoglycans pharmacology

Abstract

The discrimination between activators and nonactivators of the alternative pathway of complement depends on the affinity of the control factor H for C3b molecules covalently associated with the target. The affinity of factor H for the C3b-target complex is regulated by a positively charged site at or near the 13th short consensus repeat (SCR) domain of factor H. In this study we have analyzed the ability of different glycosaminoglycans and other negatively charged macromolecules to interact with the factor H polyanion recognition site and to enhance binding of H to the C3b-target complex. Strongest enhancement of factor H binding to zymosan-C3b was observed by the highly sulphated glycoconjugates dextran sulphate (m.w. = 5,000), heparin, chondroitin sulphate A and carrageenan (types III and IV). DNA also enhanced H binding. Removal of N-linked sulphates or reduction of the size of heparin decreased its enhancing effect on H binding. Little or no effect was seen with chondroitin sulphate C, keratan sulphate, hyaluronic acid, colominic acid (bacterial polysialic acid) or negatively charged polypeptides. The results show that the interaction of the polyanion binding site on factor H with glycosaminoglycans depends upon the number, orientation and polymeric arrangement of sulphate groups and suggest that most, but not all, sulphated glycosaminoglycans participate in the protection of host tissues from complement damage by promoting inactivation of tissue-bound C3b.

Published

1994