The murine complement regulator Crry: new insights into the immunobiology of complement regulation

Abstract Mutations in the gene encoding for complement regulator factor H (FH) severely disrupt its normal function to protect human cells from unwanted complement activation, resulting in diseases such as atypical hemolytic uremic syndrome (aHUS). aHUS presents with severe hemolytic anemia, thrombocytopenia, and renal disease, leading to end-stage renal failure. Treatment of severe complement-mediated disease, such as aHUS, by inhibiting the terminal complement pathway, has proven to be successful but at the same time fails to preserve the protective role of complement against pathogens. To improve complement regulation on human cells without interfering with antimicrobial activity, we identified an anti-FH monoclonal antibody (mAb) that induced increased FH-mediated protection of primary human endothelial cells from complement, while preserving the complement-mediated killing of bacteria. Moreover, this FH-activating mAb restored complement regulation in sera from aHUS patients carrying various heterozygous mutations in FH known to impair FH function and dysregulate complement activation. Our data suggest that FH normally circulates in a less active conformation and can become more active, allowing enhanced complement regulation on human cells. Antibody-mediated potentiation of FH may serve as a highly effective approach to inhibit unwanted complement activation on human cells in a wide range of hematological diseases while preserving the protective role of complement against pathogens.

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CD46 Plays a Key Role in Tailoring Innate Immune Recognition of Apoptotic and Necrotic Cells

Journal of Biological Chemistry ◽

10.1074/jbc.m506579200 ◽

2005 ◽

Vol 280 (43) ◽

pp. 36342-36354 ◽

Cited By ~ 104

Author(s):

Kristina Elward ◽

Mark Griffiths ◽

Masashi Mizuno ◽

Claire L. Harris ◽

Jim W. Neal ◽

...

Keyword(s):

Immune System ◽

Innate Immune System ◽

Apoptotic Cell ◽

Membrane Attack Complex ◽

Factor H ◽

Innate Immune ◽

Immune Recognition ◽

Alternative Pathways ◽

Complement Regulator ◽

Complement C1q

Complement is the canonical innate immune system involved in host defense and tissue repair with the clearance of cell debris. In contrast to the robust armory mounted against microbial nonself-pathogens, complement is selectively activated on altered self (i.e. apoptotic and necrotic cells) to instruct the safe demise by poorly characterized mechanisms. Our data shed new light on the role of complement C1q in sensing nucleic acids (NA) rapidly exposed on apoptotic Jurkat T cell membranes and in driving C3 opsonization but without the lytic membrane attack complex. DNA/RNase-treated apoptotic cells failed to activate complement. We found that several other apoptotic cell models, including senescent keratinocytes, ionophore-treated sperm cells, and CMK-derived platelets, stained for cleaved caspase 3 were rapidly losing the key complement regulator CD46. CD46 from nuclear and membrane stores was found to cluster into blebs and shed into microparticles together with NA, phosphatidylserine, C1q, and factor H. Classical and alternative pathways of complement were involved in the recognition of H2O2-treated necrotic cells. Membrane attack complex was detected on necrotic cells possibly as a result of CD46 and CD59 shedding into soluble forms. Our data highlight a novel and universal paradigm whereby the complement innate immune system is using two synergistic strategies with the recognition of altered self-NA and missing self-CD46 signals to instruct and tailor the efficient removal of apoptotic and necrotic cells in immunoprivileged sites.

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Rapid Degradation of the Complement Regulator, CD59, by a Novel Inhibitor

Journal of Biological Chemistry ◽

10.1074/jbc.m113.547083 ◽

2014 ◽

Vol 289 (17) ◽

pp. 12109-12125 ◽

Cited By ~ 9

Author(s):

Bishuang Cai ◽

Shuwei Xie ◽

Fengming Liu ◽

Laura C. Simone ◽

Steve Caplan ◽

...

Keyword(s):

Rapid Degradation ◽

Complement Regulator

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Borrelia burgdorferi Complement Regulator-Acquiring Surface Protein 2 Does Not Contribute to Complement Resistance or Host Infectivity

PLoS ONE ◽

10.1371/journal.pone.0003010 ◽

2008 ◽

Vol 3 (8) ◽

pp. 3010e ◽

Cited By ~ 40

Author(s):

Adam S. Coleman ◽

Xiuli Yang ◽

Manish Kumar ◽

Xinyue Zhang ◽

Kamoltip Promnares ◽

...

Keyword(s):

Borrelia Burgdorferi ◽

Surface Protein ◽

Complement Resistance ◽

Complement Regulator

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Complement regulation in tenocytes under the influence of leukocytes in an indirect co-culture model

Inflammation Research ◽

10.1007/s00011-021-01451-4 ◽

2021 ◽

Author(s):

Sandeep Silawal ◽

Benjamin Kohl ◽

Georg Girke ◽

Tobias Schneider ◽

Gundula Schulze-Tanzil

Keyword(s):

Complement Regulation ◽

Culture Model

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Mechanism of complement regulator Factor H mediated pneumococcal uptake by human cells

Molecular Immunology ◽

10.1016/j.molimm.2010.05.138 ◽

2010 ◽

Vol 47 (13) ◽

pp. 2242-2242

Author(s):

Vaibhav Agarwal ◽

Tauseef Asmat ◽

Shanshan Luo ◽

Peter F. Zipfel ◽

Sven Hammerschmidt

Keyword(s):

Human Cells ◽

Factor H ◽

Complement Regulator

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Anatomical-spatial dissection of single-cell retinal transcriptomics yields new insights in complement regulation

Molecular Immunology ◽

10.1016/j.molimm.2018.06.017 ◽

2018 ◽

Vol 102 ◽

pp. 129

Author(s):

Divyansh Agarwal ◽

Dwight Stambolian ◽

Avneesh Gautam ◽

Mingyao Li ◽

Nancy Zhang

Keyword(s):

Single Cell ◽

Complement Regulation

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Aseptic Injury to Epithelial Cells Alters Cell Surface Complement Regulation in a Tissue Specific Fashion

Retinal Degenerative Diseases - Advances in Experimental Medicine and Biology ◽

10.1007/978-1-4419-1399-9_18 ◽

2009 ◽

pp. 151-158 ◽

Cited By ~ 4

Author(s):

Joshua M. Thurman ◽

Brandon Renner ◽

Kannan Kunchithapautham ◽

V. Michael Holers ◽

Bärbel Rohrer

Keyword(s):

Epithelial Cells ◽

Cell Surface ◽

Complement Regulation ◽

Tissue Specific

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Dapagliflozin Ameliorates Diabetic Kidney Disease via Upregulating Crry and Alleviating Complement Over-activation in db/db Mice

Frontiers in Pharmacology ◽

10.3389/fphar.2021.729334 ◽

2021 ◽

Vol 12 ◽

Author(s):

Dong-Yuan Chang ◽

Xiao-Qian Li ◽

Min Chen ◽

Ming-Hui Zhao

Keyword(s):

Kidney Disease ◽

Protective Effect ◽

High Glucose ◽

Diabetic Kidney Disease ◽

Membrane Attack Complex ◽

Sglt2 Inhibitors ◽

Tubulointerstitial Injury ◽

Diabetic Kidney ◽

Proximal Tubular Epithelial Cells ◽

Complement Regulator

Sodium-glucose cotransporter 2(SGLT2) inhibitors show prominent renal protective effect in diabetic kidney disease (DKD), anti-inflammatory effect being one of its key mechanisms. Over-activation of the complement system, a crucial part of innate immunity, plays an important role in DKD. We aimed to investigate the effect of SGLT2 inhibitors on alleviating complement over-activation in DKD. Db/db mice were randomly divided into two groups, with 7 mice in each group treated with dapagliflozin and vehicle respectively, and 7 mice in m/m mice group. Laboratory and renal pathological parameters were evaluated. Mouse proximal tubular epithelial cells (MPTECs) were cultured and treated with high glucose. Dapagliflozin and dimethyloxallyl glycine (DMOG) were added as conditional treatment. Dapagliflozin-treated db/db mice showed significantly lower urinary albumin than vehicle-treated ones. Besides typical glomerular and tubulointerstitial injury, both C3b and membrane attack complex (MAC) depositions were significantly attenuated in dapagliflozin-treated db/db mice. The expression of complement receptor type 1-related protein y (Crry), a key complement regulator which inhibits complement over-activation, was significantly upregulated by dapagliflozin. Dapagliflozin-mediated Crry upregulation was associated with inhibition of HIF-1α accumulation under high glucose. When HIF-1α expression was stabilized by DMOG, the protective effect of dapagliflozin via upregulating Crry was blocked. In conclusion, dapagliflozin could attenuate complement over-activation in diabetic mice via upregulating Crry, which is associated with the suppression of HIF-1α accumulation in MPTECs.

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Deregulation of Factor H by Factor H-Related Protein 1 Depends on Sialylation of Host Surfaces

Frontiers in Immunology ◽

10.3389/fimmu.2021.615748 ◽

2021 ◽

Vol 12 ◽

Author(s):

Arthur Dopler ◽

Selina Stibitzky ◽

Rachel Hevey ◽

Marco Mannes ◽

Mara Guariento ◽

...

Keyword(s):

Sialic Acid ◽

Atypical Hemolytic Uremic Syndrome ◽

Immune Surveillance ◽

Factor H ◽

Sialic Acid Binding ◽

Uremic Syndrome ◽

High Concentrations ◽

Complement Regulator ◽

Physiological Impact ◽

The Complement System

To discriminate between self and non-self surfaces and facilitate immune surveillance, the complement system relies on the interplay between surface-directed activators and regulators. The dimeric modulator FHR-1 is hypothesized to competitively remove the complement regulator FH from surfaces that strongly fix opsonic C3b molecules—a process known as “deregulation.” The C-terminal regions of FH and FHR-1 provide the basis of this competition. They contain binding sites for C3b and host surface markers and are identical except for two substitutions: S1191L and V1197A (i.e., FH “SV”; FHR-1 “LA”). Intriguingly, an FHR-1 variant featuring the “SV” combination of FH predisposes to atypical hemolytic uremic syndrome (aHUS). The functional impact of these mutations on complement (de)regulation, and their pathophysiological consequences, have largely remained elusive. We have addressed these questions using recombinantly expressed wildtype, mutated, and truncated versions of FHR-1 and FH. The “SV” to “LA” substitutions did not affect glycosaminoglycan recognition and had only a small effect on C3b binding. In contrast, the two amino acids substantially affected the binding of FH and FHR-1 to α2,3-linked sialic acids as host surfaces markers, with the S-to-L substitution causing an almost complete loss of recognition. Even with sialic acid-binding constructs, notable deregulation was only detected on host and not foreign cells. The aHUS-associated “SV” mutation converts FHR-1 into a sialic acid binder which, supported by its dimeric nature, enables excessive FH deregulation and, thus, complement activation on host surfaces. While we also observed inhibitory activities of FHR-1 on C3 and C5 convertases, the high concentrations required render the physiological impact uncertain. In conclusion, the SV-to-LA substitution in the C-terminal regions of FH and FHR-1 diminishes its sialic acid-binding ability and results in an FHR-1 molecule that only moderately deregulates FH. Such FH deregulation by FHR-1 only occurs on host/host-like surfaces that recruit FH. Conversion of FHR-1 into a sialic acid binder potentiates the deregulatory capacity of FHR-1 and thus explains the pathophysiology of the aHUS-associated FHR-1 “SV” variant.

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