Literature DB >> 29588430

An Engineered Complement Factor H Construct for Treatment of C3 Glomerulopathy.

Yi Yang1, Harriet Denton1, Owen R Davies2, Kate Smith-Jackson1, Heather Kerr3, Andrew P Herbert3, Paul N Barlow3, Matthew C Pickering4, Kevin J Marchbank5.   

Abstract

Background C3 glomerulopathy (C3G) is associated with dysregulation of the alternative pathway of complement activation, and treatment options for C3G remain limited. Complement factor H (FH) is a potent regulator of the alternative pathway and might offer a solution, but the mass and complexity of FH makes generation of full-length FH far from trivial. We previously generated a mini-FH construct, with FH short consensus repeats 1-5 linked to repeats 18-20 (FH1-5^18-20), that was effective in experimental C3G. However, the serum t1/2 of FH1-5^18-20 was significantly shorter than that of serum-purified FH.Methods We introduced the oligomerization domain of human FH-related protein 1 (denoted by R1-2) at the carboxy or amino terminus of human FH1-5^18-20 to generate two homodimeric mini-FH constructs (FHR1-2^1-5^18-20 and FH1-5^18-20^R1-2, respectively) in Chinese hamster ovary cells and tested these constructs using binding, fluid-phase, and erythrocyte lysis assays, followed by experiments in FH-deficient Cfh-/- mice.Results FHR1-2^1-5^18-20 and FH1-5^18-20^R1-2 homodimerized in solution and displayed avid binding profiles on clustered C3b surfaces, particularly FHR1-2^1-5^18-20 Each construct was >10-fold more effective than FH at inhibiting cell surface complement activity in vitro and restricted glomerular basement membrane C3 deposition in vivo significantly better than FH or FH1-5^18-20 FH1-5^18-20^R1-2 had a C3 breakdown fragment binding profile similar to that of FH, a >5-fold increase in serum t1/2 compared with that of FH1-5^18-20, and significantly better retention in the kidney than FH or FH1-5^18-20Conclusions FH1-5^18-20^R1-2 may have utility as a treatment option for C3G or other complement-mediated diseases.
Copyright © 2018 by the American Society of Nephrology.

Entities:  

Keywords:  Immunology and pathology; complement; glomerulopathy; membranoproliferative glomerulonephritis (MPGN)

Mesh:

Substances:

Year:  2018        PMID: 29588430      PMCID: PMC6054357          DOI: 10.1681/ASN.2017091006

Source DB:  PubMed          Journal:  J Am Soc Nephrol        ISSN: 1046-6673            Impact factor:   10.121


  73 in total

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8.  Structural basis for engagement by complement factor H of C3b on a self surface.

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Authors:  Peter F Zipfel; Thorsten Wiech; Emma D Stea; Christine Skerka
Journal:  J Am Soc Nephrol       Date:  2020-01-24       Impact factor: 10.121

2.  Novel Approaches to Control of the Alternative Complement Pathway for the Treatment of C3 Glomerulopathies.

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10.  Utilization of Staphylococcal Immune Evasion Protein Sbi as a Novel Vaccine Adjuvant.

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