Your search keyword '"Complement factor I"' showing total 2,121 results

1. Functional evaluation of rare variants in complement factor I using a minigene assay.

Author

Donelson, Cobey J. H., Borsa, Nicolo Ghiringhelli, Taylor, Amanda O., Smith, Richard J. H., and Yuzhou Zhang

Subjects

ALTERNATIVE RNA splicing, MISSENSE mutation, GENE frequency, GENETIC variation, SERINE

Abstract

The regulatory serine protease, complement factor I (FI), in conjunction with one of its cofactors (FH, C4BP, MCP, or CR1), plays an essential role in controlling complement activity through inactivation of C3b and C4b. The functional impact by missense variants in the CFI gene, particularly those with minor allele frequencies of 0.01% to 0.1%, is infrequently studied. As such, these variants are typically classified as variants of uncertain significance (VUS) when they are identified by clinical testing. Herein, we utilized a minigene splicing assay to assess the functional impact of 36 ultra-rare variants of CFI. These variants were selected based on their minor allele frequencies (MAF) and their association with low-normal FI levels. Four variants lead to aberrant splicing-one 5' consensus splice site (NM_000204.5: c.1429G>C, p. Asp477His) and three exonic changes (c.355G>A, p.Gly119Arg; c.472G>A, p.Gly158Arg; and c.950G>A, p.Arg317Gln)- enabling their reclassification to likely pathogenic (LP) or pathogenic (P) based on ACMG guidelines. These findings underscore the value of functional assays, such as the minigene assay, in assessing the clinical relevance of rare variants in CFI. [ABSTRACT FROM AUTHOR]

Published

2024

2. Complement Factor I Gene Variant as a Treatable Cause of Recurrent Aseptic Neutrophilic Meningitis: A Case Report.

Author

Rolfes, Mary, Harroud, Adil, Zorn, Kelsey C, Tubati, Asritha, Omura, Charles, Kurtz, Kenneth, Matloubian, Mehrdad, Berger, Amy, Chiu, Charles Y, Wilson, Michael R, and Ramachandran, Prashanth S

Subjects

Humans, Meningitis, Aseptic, Inflammation, Complement Factor I, Antibodies, Monoclonal, Mutation, Adult, Male, Neurosciences, Genetics, Biotechnology, Aetiology, 2.1 Biological and endogenous factors

Abstract

Mutations in the complement factor I (CFI) gene have previously been identified as causes of recurrent CNS inflammation. We present a case of a 26-year-old man with 18 episodes of recurrent meningitis, who had a variant in CFI(c.859G>A,p.Gly287Arg) not previously associated with neurologic manifestations. He achieved remission with canakinumab, a human monoclonal antibody targeted at interleukin-1 beta.

Published

2023

3. C3 glomerulopathy is highly prevalent in French Polynesia

Author

Nelly Candela, Nicolas Benichou, Mathilde Lefebvre, Lorraine Gueguen, Paula Vieira-Martins, Carine El Sissy, Hervé Sartelet, Pascale Testevuide, Ronan Delaval, and Stanislas Faguer

Subjects

C3 glomerulonephritis, Acute post-infectious glomerulopathy, Complement alternative pathway, Complement factor I, Immunologic diseases. Allergy, RC581-607

Abstract

Objective: To compare the natural history of C3 glomerulopathy (C3G) to acute post-infectious glomerulonephritis (APIGN) in a cohort of patients with a relative homogeneity of environment conditions and genetic background. Methods: We retrospectively reviewed the characteristics of all patients with biopsy proven C3G or APIGN referred in 2013–2019 to the only renal unit in French Polynesia. Results: Point prevalence of C3G is ∼23 cases per 100,000 inhabitants. A recurrent variation of CFI (p.Arg406His) was identified at the heterozygous state in 4/8 (50 %) patients with C3G but its pathogenicity remain elusive. Characteristics at presentation and kidney outcomes were roughly similar between C3G (n = 16) and APIGN (n = 20), excepted for the presence of humps on kidney biopsy. Conclusions: C3G is highly prevalent in French Polynesia suggesting specific genetic or environmental susceptibility factors. Systematic diagnosis workflow should be proposed to all patients with C3 predominant glomerulonephritis.

Published

2024

4. Functional evaluation of rare variants in complement factor I using a minigene assay

Author

Cobey J. H. Donelson, Nicolo Ghiringhelli Borsa, Amanda O. Taylor, Richard J. H. Smith, and Yuzhou Zhang

Subjects

complement, alternative pathway, complement factor I, complement-mediated diseases, haploinsufficiency, RNA splicing, Immunologic diseases. Allergy, RC581-607

Abstract

The regulatory serine protease, complement factor I (FI), in conjunction with one of its cofactors (FH, C4BP, MCP, or CR1), plays an essential role in controlling complement activity through inactivation of C3b and C4b. The functional impact by missense variants in the CFI gene, particularly those with minor allele frequencies of 0.01% to 0.1%, is infrequently studied. As such, these variants are typically classified as variants of uncertain significance (VUS) when they are identified by clinical testing. Herein, we utilized a minigene splicing assay to assess the functional impact of 36 ultra-rare variants of CFI. These variants were selected based on their minor allele frequencies (MAF) and their association with low-normal FI levels. Four variants lead to aberrant splicing–one 5’ consensus splice site (NM_000204.5: c.1429G>C, p.Asp477His) and three exonic changes (c.355G>A, p.Gly119Arg; c.472G>A, p.Gly158Arg; and c.950G>A, p.Arg317Gln)–enabling their reclassification to likely pathogenic (LP) or pathogenic (P) based on ACMG guidelines. These findings underscore the value of functional assays, such as the minigene assay, in assessing the clinical relevance of rare variants in CFI.

Published

2024

5. Thrombotic microangiopathy due to acquired complement factor I deficiency in a male receiving interferon‐beta treatment for multiple sclerosis.

Author

Mrabet, Sanda, Dahmane, Rihem, Raja, Boukadida, Fradi, Asma, Aicha, Narjess Ben, Sahtout, Wissal, Azzabi, Awatef, Guedri, Yosra, Zellama, Dorsaf, Achour, Abdellatif, Sfar, Imen, Goucha, Rim, Abdessayed, Nihed, and Mokni, Moncef

Subjects

*ECULIZUMAB, *INTERFERON beta 1b, *MULTIPLE sclerosis, *HEMOLYTIC anemia, *HEMOLYTIC-uremic syndrome, *COMPLEMENT activation, *KIDNEY failure

Abstract

Aims: Interferon‐beta (IFNβ), the most widely prescribed medication for multiple sclerosis, is generally considered safe. Nevertheless, rare serious and/or life‐threatening side effects have been reported such as thrombotic microangiopathy. A few mechanisms have been proposed to explain how interferon causes thrombotic microangiopathy, but immunological studies have been unable to pin this phenomenon down to a single pathophysiologic pathway. The aim of this article was to report a new mechanism explaining Interferon beta related thrombotic microangiopathy. Methods: We report thrombotic microangiopathy in a 28‐year‐old male receiving interferon‐beta treatment for multiple sclerosis. Results: After three years of starting interferon beta therapy, the patient presented with malignant hypertension causing seizures, rapidly progressive renal failure requiring haemodialysis and haemolytic anaemia. Corticosteroid and plasma exchange sessions permitted haemolysis control. Nonetheless, the patient remained hemodialysis‐dependent. Exploration of the complement system found a complement factor I deficiency whose activity normalized at the control carried out after 2 years. Conclusion: IFNβ treatment may cause complement factor I deficit, which can lead to thrombotic microangiopathy and severe renal failure. [ABSTRACT FROM AUTHOR]

Published

2023

6. Rare Dysfunctional Complement Factor I Genetic Variants and Progression to Advanced Age-Related Macular Degeneration

Author

Johanna M. Seddon, MD, Bernard Rosner, PhD, Dikha De, MPH, Tianxiao Huan, PhD, Anuja Java, MD, and John Atkinson, MD

Subjects

Advanced age-related macular degeneration, Complement factor I, Genetic variants, Geographic atrophy, Neovascular disease, Ophthalmology, RE1-994

Abstract

Purpose: To evaluate associations between rare dysfunctional complement factor I (CFI) genetic variant status and progression to advanced age-related macular degeneration (AAMD), geographic atrophy (GA), and neovascular disease (NV). Design: Prospective, longitudinal study Participants: Patients aged 55 to 80 years at baseline identifying as White with non-AAMD in 1 or both eyes at baseline were included. Follow-up grades were assigned as early, intermediate, or AAMD (GA or NV). CFI variants were categorized using genotyping and sequencing platforms. Methods: Analyses were performed using the Seddon Longitudinal Cohort Study (N = 2116 subjects, 3901 eyes, and mean follow-up of 8.3 years) and the Age-Related Eye Disease Study (N = 2837 subjects, 5200 eyes, and mean follow-up of 9.2 years). CFI rare variants associated with low serum factor I (FI) protein levels and decreased FI function (type 1), other AMD genetic variants, and demographic, behavioral, and ocular factors were evaluated. Generalized estimating equations methods were used to assess the association between CFI rare variants and progression, independent of other genetic variants and covariates. Main Outcome Measures: Progression to AAMD, GA, or NV. Results: In the prospective cohort of 4953 subjects (9101 eyes with non-AAMD at baseline), 1% were type 1 rare CFI carriers. Over 12 years, progression to AAMD was 44% for carriers and 20% for noncarriers (P < 0.001), 30% of carriers versus 10% of noncarriers progressed to GA (P

Published

2023

7. An Infant Case of Streptococcus Pneumoniae-Associated Thrombotic Microangiopathy with Heterozygous CFI Mutation and CFHR3-CFHR1 Deletion.

Author

Yuji Matsumoto, Yohei Ikezumi, Tomomi Kondoh, Katsuyuki Yokoi, Yoko Nakajima, Naonori Kumagai, Takema Kato, Hiroki Kurahashi, and Tetsuya Ito

Abstract

Thrombotic microangiopathy (TMA) is a disease that causes organ damage due to microvascular hemolytic anemia, thrombocytopenia, and microvascular platelet thrombosis. Streptococcus pneumoniae-associated TMA (spTMA) is a rare complication of invasive pneumococcal infection. In addition, atypical hemolytic uremic syndrome (aHUS) is TMA associated with congenital or acquired dysregulation of complement activation. We report the case of a nine-month-old boy with refractory nephrotic syndrome complicated by spTMA in the setting of heterozygous complement factor-I (CFI) gene mutation and CFHR3-CFHR1 deletion. He repeatedly developed thrombocytopenia, anemia with schistocytes, hypocomplementemia, and abnormal coagulation triggered by infection, which manifested clinically with convulsions and an intraperitoneal hematoma. Eculizumab (a monoclonal humanized anti-C5 antibody) provided transient symptomatic benefit including improvement in thrombocytopenia; however, he developed unexplained cardiac arrest and was declared brain dead a few days later. In this report, we highlight the diagnostic challenges of this case and the causal relationship between spTMA and complement abnormalities and consider the contribution of heterozygous mutation of CFI and CFHR3-CFHR1 deletion. [ABSTRACT FROM AUTHOR]

Published

2022

8. Functional and Expressional Analyses Reveal the Distinct Role of Complement Factor I in Regulating Complement System Activation during GCRV Infection in Ctenopharyngodon idella.

Author

Liu, Yi, Lv, Zhao, Xiao, Tiaoyi, Zhang, Xuewen, Ding, Chunhua, Qin, Beibei, Xu, Baohong, and Liu, Qiaolin

Subjects

*CTENOPHARYNGODON idella, *COMPLEMENT activation, *FUNCTIONAL analysis, *BLOOD proteins, *CRUCIAN carp, *COMPLEMENT inhibition

Abstract

Complement factor I (CFI), a complement inhibitor, is well known for regulating the complement system activation by degrading complement component 3b (C3b) in animal serum, thus becoming involved in innate defense. Nevertheless, the functional mechanisms of CFI in the complement system and in host-pathogen interactions are far from being clarified in teleost fish. In the present study, we cloned and characterized the CFI gene, CiCFI, from grass carp (Ctenopharyngodon idella) and analyzed its function in degrading serum C3b and expression changes after grass carp reovirus (GCRV) infection. The open reading frame of CiCFI was found to be 2121 bp, encoding 706 amino acids with a molecular mass of 79.06 kDa. The pairwise alignments showed that CiCFI shared the highest identity (66.9%) with CFI from Carassius gibelio and the highest similarity (78.7%) with CFI from Danio rerio. The CiCFI protein was characterized by a conserved functional core Tryp_SPc domain with the catalytic triad and substrate binding sites. Phylogenetic analysis indicated that CiCFI and the homologs CFIs from other teleost fish formed a distinct evolutionary branch. Similar with the CFIs reported in mammals, the recombinant CiCFI protein could significantly reduce the C3b content in the serum, demonstrating the conserved function of CiCFI in the complement system in the grass carp. CiCFI mRNA and protein showed the highest expression level in the liver. After GCRV infection, the mRNA expressions of CiCFI were first down-regulated, then up-regulated, and then down-regulated to the initial level, while the protein expression levels maintained an overall downward trend to the late stage of infection in the liver of grass carps. Unexpectedly, the protein levels of CiCFI were also continuously down-regulated in the serum of grass carps during GCRV infection, while the content of serum C3b proteins first increases and then returns to the initial level, suggesting a distinct role of CiCFI in regulating complement activation and fish-virus interaction. Combining our previous results that complement factor D, a complement enhancer, shows continuously up-regulated expression levels in grass carps during GCRV infection, and this study may provide the further essential data for the full picture of complex complement regulation mechanism mediated by Df and CFI of the grass carp during pathogen infection. [ABSTRACT FROM AUTHOR]

Published

2022

9. Circulating levels of endogenous complement inhibitors correlate inversely with complement consumption in systemic lupus erythematosus.

Author

van der Meulen S, Monahan RC, Gelderman KA, van Kooten C, Teng YKO, Huizinga TWJ, Steup-Beekman GM, and Trouw LA

Subjects

Humans, Female, Adult, Male, Middle Aged, Complement Activation immunology, Complement Factor I, Lupus Vasculitis, Central Nervous System blood, Lupus Vasculitis, Central Nervous System immunology, Complement C4 metabolism, Complement C3 metabolism, Aged, Lupus Erythematosus, Systemic blood, Lupus Erythematosus, Systemic immunology, Complement C1 Inhibitor Protein metabolism, Biomarkers blood, Complement Factor H metabolism, Complement Factor H immunology, Complement C4b-Binding Protein

Abstract

Systemic lupus erythematosus (SLE) is marked by excessive complement activation, contributing to tissue damage. Complement activation can be detected in many organs including the skin, kidney, and brain. The involvement of the central nervous system is particularly relevant to understanding neuropsychiatric SLE (NPSLE), one of the poorest understood manifestations of SLE for which no biomarkers are available. We studied the levels of complement inhibitors in SLE in relation to disease activity and as possible biomarkers to identify NPSLE. Serum levels of complement inhibitors C1-inhibitor (C1-INH), C4b-binding protein (C4BP), Factor I, and Factor H were measured in 345 SLE patients (including 102 with NPSLE) and 108 healthy controls. Compared with controls, SLE patients had higher C1-INH and C4BP but lower Factor I and H levels. All inhibitors positively correlated with total C3 and C4 levels. While correlating with the SLE Disease Activity Index (SLEDAI), no distinction in inhibitor levels was found between SLE and NPSLE patients. Over time, C1-INH and Factor H levels normalized, but no significant changes were observed for C4BP and Factor I. In SLE the levels of circulating complement inhibitors are inversely correlated to complement consumption but do not serve as biomarkers for NPSLE., (© 2024 The Author(s). European Journal of Immunology published by Wiley‐VCH GmbH.)

Published

2024

10. C3 glomerulopathy is highly prevalent in French Polynesia.

Author

Candela N, Benichou N, Lefebvre M, Gueguen L, Vieira-Martins P, El Sissy C, Sartelet H, Testevuide P, Delaval R, and Faguer S

Abstract

Objective: To compare the natural history of C3 glomerulopathy (C3G) to acute post-infectious glomerulonephritis (APIGN) in a cohort of patients with a relative homogeneity of environment conditions and genetic background., Methods: We retrospectively reviewed the characteristics of all patients with biopsy proven C3G or APIGN referred in 2013-2019 to the only renal unit in French Polynesia., Results: Point prevalence of C3G is ∼23 cases per 100,000 inhabitants. A recurrent variation of CFI (p.Arg406His) was identified at the heterozygous state in 4/8 (50 %) patients with C3G but its pathogenicity remain elusive. Characteristics at presentation and kidney outcomes were roughly similar between C3G (n = 16) and APIGN (n = 20), excepted for the presence of humps on kidney biopsy., Conclusions: C3G is highly prevalent in French Polynesia suggesting specific genetic or environmental susceptibility factors. Systematic diagnosis workflow should be proposed to all patients with C3 predominant glomerulonephritis., Competing Interests: The authors declare the following financial interests/personal relationships which may be considered as potential competing interests:SF received personal fees for consultancy from Abionyx Pharma, CSL-VIFOR and 10.13039/100004336Novartis SA, for scientific advisory boards from CSL-Vifor, Sanofi-Genzyme, Alexion-AstraZeneca, and for lecture from 10.13039/100004702Baxter and CSL-Vifor. Other authors declared no conflict of interest., (© 2024 The Authors.)

Published

2024

11. Does Complement Factor I Correlate with Complement Component 4b in HIV Infected Patients with Preeclampsia?

Author

Govender, Rowen, Govender, Nalini, and Naicker, Thajasvarie

Subjects

*DIASTOLIC blood pressure, *PREECLAMPSIA, *SYSTOLIC blood pressure, *HIV-positive persons, *HIV

Abstract

Objective: This study aims to determine the concentration of complement factor I (CFI) and complement component 4b (C4b) in normotensive (N) pregnant women compared to women with preeclampsia (PE) and human immunodeficiency virus (HIV). Materials and Methods: The study population consisted of preeclamptic (n=38) and normotensive (n=38) pregnant women, who were further stratified by HIV status into HIV-positive (n=19) and HIV-negative (n=19) groups. Serum levels of CFI and C4b were determined using the Bio-Plex multiplex immunoassays. Data analysis was conducted using Stata (version 12) and Graphpad Prism (8.0.1). Results: A statistically significant downregulation of C4b was noted in the N+ve vs. N-ve, PE+ve in comparison with the N+ve group (p=0.0001) and in PE+ve compared to the PE-ve pregnancies. CFI levels were significantly upregulated in the N+ve vs. N-ve groups (p=0.004) and downregulated in PE+ve compared to N+ve and in PE+ve vs. PE-ve groups (p=0.004). Significant positive associations were noted for C4b with parity, between the PE-ve and N+ve groups (r=0.47; p=0.04), and for CFI in the PE+ve group (r=0.68; p=0.0001). Negative significant associations were noted between C4b and systolic blood pressure (r=-0.53, p=0.01) and C4b and diastolic blood pressure (r=-0.78, p=0.0001). CFI also showed negative association with parity (r=-0.48, p=0.03). Conclusion: This innovative study demonstrates a decline of C4b and CFI levels in PE+ve, compared to N+ve pregnancies. It is plausible that the downregulation may be attributed to complement mediated virolysis emanating from C3 convertase dysregulation in PE comorbidity with HIV infection [ABSTRACT FROM AUTHOR]

Published

2022

12. Ocular biomarker profiling after complement factor I gene therapy in geographic atrophy secondary to age-related macular degeneration (Updated November 4, 2024).

Published

2024

13. Patent Issued for Complement factor I-related compositions and methods (USPTO 12116606).

Subjects

COMPLEMENT (Immunology), BLOOD proteins, LOW density lipoprotein receptors, PEPTIDES, PROTEOLYTIC enzymes

Abstract

A patent has been issued for complement factor I-related compositions and methods by Vertex Pharmaceuticals Incorporated. The patent discusses the role of Complement Factor I (CFI) in regulating the complement system by cleaving C4b and C3b proteins. The invention provides variants of CFI capable of modulating the complement system with improved characteristics compared to wild type CFI, such as increased activity or substrate specificity. The patent also describes fusion constructs involving CFI and half-life extenders for pharmaceutical compositions. [Extracted from the article]

Published

2024

14. Uppsala University Reports Findings in Complement C3b Inactivator Proteins (Model-based Interspecies Scaling for Predicting Human Pharmacokinetics of Cb 4332, a Complement Factor I Protein).

Abstract

A study conducted by Uppsala University in Sweden examined the pharmacokinetics of CB 4332, a complement factor I protein, using traditional and model-based approaches. The study found species-specific differences in elimination and observed the formation of anti-drug antibodies in rats and nonhuman primates. The researchers concluded that a once-weekly subcutaneous dose of 5 mg/kg would reach the efficacy target range for CB 4332 in humans. This research has been peer-reviewed and published in the Journal of Pharmaceutical Sciences. [Extracted from the article]

Published

2024

15. Post-Transplant Thrombotic Microangiopathy due to a Pathogenic Mutation in Complement Factor I in a Patient With Membranous Nephropathy: Case Report and Review of Literature

Author

Maryam Saleem, Sana Shaikh, Zheng Hu, Nicola Pozzi, and Anuja Java

Subjects

thrombotic microangiopathy, kidney transplantation, complement factor I, membranous nephropathy, atypical hemolytic uremic syndrome, complement functional analysis, Immunologic diseases. Allergy, RC581-607

Abstract

Thrombotic microangiopathy (TMA) is characterized by microangiopathic hemolytic anemia, thrombocytopenia and organ injury occurring due to endothelial cell damage and microthrombi formation in small vessels. TMA is primary when a genetic or acquired defect is identified, as in atypical hemolytic uremic syndrome (aHUS) or secondary when occurring in the context of another disease process such as infection, autoimmune disease, malignancy or drugs. Differentiating between a primary complement-mediated process and one triggered by secondary factors is critical to initiate timely treatment but can be challenging for clinicians, especially after a kidney transplant due to presence of multiple confounding factors. Similarly, primary membranous nephropathy is an immune-mediated glomerular disease associated with circulating autoantibodies (directed against the M-type phospholipase A2 receptor (PLA2R) in 70% cases) while secondary membranous nephropathy is associated with infections, drugs, cancer, or other autoimmune diseases. Complement activation has also been proposed as a possible mechanism in the etiopathogenesis of primary membranous nephropathy; however, despite complement being a potentially common link, aHUS and primary membranous nephropathy have not been reported together. Herein we describe a case of aHUS due to a pathogenic mutation in complement factor I that developed after a kidney transplant in a patient with an underlying diagnosis of PLA2R antibody associated-membranous nephropathy. We highlight how a systematic and comprehensive analysis helped to define the etiology of aHUS, establish mechanism of disease, and facilitated timely treatment with eculizumab that led to recovery of his kidney function. Nonetheless, ongoing anti-complement therapy did not prevent recurrence of membranous nephropathy in the allograft. To our knowledge, this is the first report of a patient with primary membranous nephropathy and aHUS after a kidney transplant.

Published

2022

16. Functional Analysis of Variants in Complement Factor I Identified in Age-Related Macular Degeneration and Atypical Hemolytic Uremic Syndrome.

Author

de Jong, Sarah, de Breuk, Anita, Bakker, Bjorn, Katti, Suresh, Hoyng, Carel B., Nilsson, Sara C., Blom, Anna M., van den Heuvel, Lambert P., den Hollander, Anneke I., and Volokhina, Elena B.

Subjects

HEMOLYTIC-uremic syndrome, MACULAR degeneration, FUNCTIONAL analysis, THROMBOTIC thrombocytopenic purpura, COMPLEMENT inhibition, GENETIC variation

Abstract

Complement factor I (FI) is a central inhibitor of the complement system, and impaired FI function increases complement activation, contributing to diseases such as age-related macular degeneration (AMD) and atypical hemolytic uremic syndrome (aHUS). Genetic variation in complement factor I (CFI) has been identified in both AMD and aHUS, with more than half of these variants leading to reduced FI secretion levels. For many of the variants with normal FI secretion, however, functional implications are not yet known. Here we studied 11 rare missense variants, with FI secretion levels comparable to wildtype, but a predicted damaging effects based on the Combined Annotation Dependent Depletion (CADD) score. Three variants (p.Pro50Ala, p.Arg339Gln, and p.Ser570Thr) were analyzed in plasma and serum samples of carriers affected by AMD. All 11 variants (nine for the first time in this study) were recombinantly expressed and the ability to degrade C3b was studied with the C3b degradation assay. The amount of degradation was determined by measuring the degradation product iC3b with ELISA. Eight of 11 (73%) mutant proteins (p.Pro50Ala, p.Arg339Gln, p.Ile340Thr, p.Gly342Glu, p.Gly349Arg, p.Arg474Gln, p.Gly487Cys, and p.Gly512Ser) showed significantly impaired C3b degradation, and were therefore classified as likely pathogenic. Our data indicate that genetic variants in CFI with a CADD score >20 are likely to affect FI function, and that monitoring iC3b in a degradation assay is a useful tool to establish the pathogenicity of CFI variants in functional studies. [ABSTRACT FROM AUTHOR]

Published

2022

17. Functional Analysis of Variants in Complement Factor I Identified in Age-Related Macular Degeneration and Atypical Hemolytic Uremic Syndrome

Author

Sarah de Jong, Anita de Breuk, Bjorn Bakker, Suresh Katti, Carel B. Hoyng, Sara C. Nilsson, Anna M. Blom, Lambert P. van den Heuvel, Anneke I. den Hollander, and Elena B. Volokhina

Subjects

complement factor I, genetic variants, age-related macular degeneration, atypical hemolytic uremic syndrome, functional analysis, Immunologic diseases. Allergy, RC581-607

Abstract

Complement factor I (FI) is a central inhibitor of the complement system, and impaired FI function increases complement activation, contributing to diseases such as age-related macular degeneration (AMD) and atypical hemolytic uremic syndrome (aHUS). Genetic variation in complement factor I (CFI) has been identified in both AMD and aHUS, with more than half of these variants leading to reduced FI secretion levels. For many of the variants with normal FI secretion, however, functional implications are not yet known. Here we studied 11 rare missense variants, with FI secretion levels comparable to wildtype, but a predicted damaging effects based on the Combined Annotation Dependent Depletion (CADD) score. Three variants (p.Pro50Ala, p.Arg339Gln, and p.Ser570Thr) were analyzed in plasma and serum samples of carriers affected by AMD. All 11 variants (nine for the first time in this study) were recombinantly expressed and the ability to degrade C3b was studied with the C3b degradation assay. The amount of degradation was determined by measuring the degradation product iC3b with ELISA. Eight of 11 (73%) mutant proteins (p.Pro50Ala, p.Arg339Gln, p.Ile340Thr, p.Gly342Glu, p.Gly349Arg, p.Arg474Gln, p.Gly487Cys, and p.Gly512Ser) showed significantly impaired C3b degradation, and were therefore classified as likely pathogenic. Our data indicate that genetic variants in CFI with a CADD score >20 are likely to affect FI function, and that monitoring iC3b in a degradation assay is a useful tool to establish the pathogenicity of CFI variants in functional studies.

Published

2022

18. Genetic Risk in Families with Age-Related Macular Degeneration

Author

Anita de Breuk, MD, Yara T.E. Lechanteur, MD, PhD, Thomas J. Heesterbeek, MD, PhD, Sascha Fauser, MD, PhD, Caroline C.W. Klaver, MD, PhD, Carel B. Hoyng, MD, PhD, and Anneke I. den Hollander, PhD

Subjects

Age-related macular degeneration, Complement factor H, Complement factor I, Complement system, Genetic risk score, Ophthalmology, RE1-994

Abstract

Purpose: To determine the contribution of common and rare genetic risk variants in families with age-related macular degeneration (AMD). Design: Case-control study. Participants: A family cohort (355 affected and 342 unaffected family members from 144 families with AMD) and an unrelated case-control cohort (1078 patients, 952 controls), recruited from the European Genetic Database. Methods: Genetic data of both cohorts were filtered for carriership of rare genetic variants in the coding and splice-site regions of the complement factor H (CFH) and complement factor I (CFI) genes, and 52 AMD-associated variants were extracted for calculation of genetic risk scores (GRS). To compare GRSs between familial and nonfamilial rare CFH and CFI variant carriers and noncarriers and between AMD disease stages, we performed a 2-way analysis of variance, with Bonferroni correction for multiple testing. Within families with AMD carrying rare CFH and CFI variants, we analyzed segregation patterns by calculating the proportion of affected among carriers. Main Outcome Measures: GRSs and segregation of rare CFH and CFI variants. Results: We observed higher GRSs in familial versus nonfamilial individuals without rare CFH and CFI variants: mean GRS, 1.76 (standard error [SE], 0.08) versus 0.83 (SE, 0.03; P < 0.001). In 51 of 144 families (35.4%), rare CFH and CFI variants were identified. Within the AMD family cohort, carriers of rare CFH and CFI variants showed lower GRSs compared with noncarriers (mean GRS, 1.05 [SE, 0.23] vs. 1.76 [SE, 0.08]; P = 0.02). The proportion of affected family members with a high GRS was 57.3% (176/307). Of the affected family members with a low or intermediate GRS, 40.0% carried rare CFH or CFI variants. Among carriers of 11 rare CFH or CFI variants, the proportion affected by AMD was more than 75%. Conclusions: Genetic risk in families with AMD often is attributed to high GRSs based on common variants. However, in part of the families with a low or intermediate GRS, rare CFH and CFI variants contributed to disease development. We recommend computing GRSs and sequencing the CFH and CFI genes in families with AMD, in particular in the light of ongoing gene-specific clinical trials.

Published

2021

19. Hot Spot of Complement Factor I Rare Variant p.Ile357Met in Patients With Hemolytic Uremic Syndrome.

Author

Schwotzer N, Fakhouri F, Martins PV, Delmas Y, Caillard S, Zuber J, Moranne O, Mesnard L, Frémeaux-Bacchi V, and El-Sissy C

Subjects

Adult, Child, Female, Humans, Male, Middle Aged, Young Adult, Mutation, Missense, Retrospective Studies, Atypical Hemolytic Uremic Syndrome genetics, Complement Factor I genetics

Abstract

Atypical hemolytic uremic syndrome (aHUS) is a rare kidney disease due to a dysregulation of the complement alternative pathway. Complement factor I (CFI) negatively regulates the alternative pathway and CFI gene rare variants have been associated to aHUS with a low disease penetrance. We report 10 unrelated cases of HUS associated to a rare CFI variant, p.Ile357Met (c.1071T>G). All patients with isolated p.Ile357Met CFI missense variant were retrospectively identified among patients included between January 2007 and January 2022 in the French HUS Registry. We identified 10 unrelated patients (70% women; median age at HUS diagnosis, 36.5 years) who carry the same rare variant p.Ile357Met in the CFI gene. Seven patients (cases 1-7) presented with aHUS in the native kidney associated with malignant hypertension in 5 patients. None received a C5 inhibitor. Two of these cases occurred in the peripartum period with complete recovery of kidney function, while 5 of these patients reached kidney failure requiring replacement therapy (KFRT). Four patients with KFRT subsequently underwent kidney transplantation. Three later developed C3 glomerulopathy in their kidney graft, but none had aHUS recurrence. Three other patients (cases 8-10) experienced de novo thrombotic microangiopathy after kidney transplantation, precipitated by various triggers. The rare CFI variant p.Ile357Met appears to be a facilitating genetic factor for HUS and for some forms of secondary HUS., (Copyright © 2024 National Kidney Foundation, Inc. Published by Elsevier Inc. All rights reserved.)

Published

2024

20. Comprehensive functional characterization of complement factor I rare variant genotypes identified in the SCOPE geographic atrophy cohort.

Author

Hallam TM, Andreadi A, Sharp SJ, Brocklebank V, Gardenal E, Dreismann A, Lotery AJ, Marchbank KJ, Harris CL, Jones AV, and Kavanagh D

Subjects

Humans, Female, Male, Aged, Cohort Studies, Macular Degeneration genetics, Macular Degeneration metabolism, Middle Aged, Complement Factor I genetics, Complement Factor I metabolism, Geographic Atrophy genetics, Geographic Atrophy blood, Geographic Atrophy metabolism, Genotype, Complement C3b metabolism, Complement C3b genetics

Abstract

Rare variants (RVs) in the gene encoding the regulatory enzyme complement factor I (CFI; FI) that reduce protein function or levels increase age-related macular degeneration risk. A total of 3357 subjects underwent screening in the SCOPE natural history study for geographic atrophy secondary to age-related macular degeneration, including CFI sequencing and serum FI measurement. Eleven CFI RV genotypes that were challenging to categorize as type I (low serum level) or type II (normal serum level, reduced enzymatic function) were characterized in the context of pure FI protein in C3b and C4b fluid phase cleavage assays and a novel bead-based functional assay (BBFA) of C3b cleavage. Four variants predicted or previously characterized as benign were analyzed by BBFA for comparison. In all, three variants (W51S, C67R, and I370T) resulted in low expression. Furthermore, four variants (P64L, R339Q, G527V, and P528T) were identified as being highly deleterious with IC50s for C3b breakdown >1 log increased versus the WT protein, while two variants (K476E and R474Q) were ∼1 log reduced in function. Meanwhile, six variants (P50A, T203I, K441R, E548Q, P553S, and S570T) had IC50s similar to WT. Odds ratios and BBFA IC50s were positively correlated (r = 0.76, p < 0.01), while odds ratios versus combined annotation dependent depletion (CADD) scores were not (r = 0.43, p = 0.16). Overall, 15 CFI RVs were functionally characterized which may aid future patient stratification for complement-targeted therapies. Pure protein in vitro analysis remains the gold standard for determining the functional consequence of CFI RVs., Competing Interests: Conflict of interest D. K.: Gyroscope Therapeutics (consultancy, equity, grant income), Novartis (consultancy), Alexion Pharmaceuticals (consultancy), Apellis (consultancy); Sarepta (consultancy), Chemocentryx (Consultancy), Sobi (consultancy), Samsung (consultancy), Purespring (consultancy), Roche (consultancy); C. L. H: Q32 Bio (consultancy), Gyroscope Therapeutics (Consultancy), Novartis (employee), Ra Pharmaceuticals (Grant income), Biocryst (consultancy); K. J. M: Qualasept (consultancy), Freeline Therapeutics (consultancy), Catalyst Biosciences (grant income, consultancy), Idorsia Pharmaceuticals (grant income), Gemini Therapeutics (grant income, consultancy), Alexion Pharmaceuticals (grant income, consultancy); T. M. H.: Gyroscope Therapeutics, Novartis (employee); S. J. S.: Gyroscope Therapeutics, Novartis (employee); E. G.: Gyroscope Therapeutics, Novartis (employee); A. D.: Gyroscope Therapeutics, Novartis, Beacon Therapeutics (employee); A. V. J.: Gyroscope Therapeutics, Novartis (employee); A. L.: Gyroscope Therapeutics (consultancy, equity), Roche (consultancy), Apellis (consultancy), Novartis (consultancy)., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024

21. Complement factor I knockdown inhibits colon cancer development by affecting Wnt/β-catenin/c-Myc signaling pathway and glycolysis.

Author

Du YJ, Jiang Y, Hou YM, and Shi YB

Abstract

Background: Colon cancer (CC) occurrence and progression are considerably influenced by the tumor microenvironment. However, the exact underlying regulatory mechanisms remain unclear., Aim: To investigate immune infiltration-related differentially expressed genes (DEGs) in CC and specifically explored the role and potential molecular mechanisms of complement factor I (CFI)., Methods: Immune infiltration-associated DEGs were screened for CC using bioinformatics. Quantitative reverse transcription polymerase chain reaction was used to examine hub DEGs expression in the CC cell lines. Stable CFI-knockdown HT29 and HCT116 cell lines were constructed, and the diverse roles of CFI in vitro were assessed using CCK-8, 5-ethynyl-2'-deoxyuridine, wound healing, and transwell assays. Hematoxylin and eosin staining and immunohistochemistry staining were employed to evaluate the influence of CFI on the tumorigenesis of CC xenograft models constructed using BALB/c male nude mice. Key proteins associated with glycolysis and the Wnt pathway were measured using western blotting., Results: Six key immune infiltration-related DEGs were screened, among which the expression of CFI, complement factor B, lymphoid enhancer binding factor 1, and SRY-related high-mobility-group box 4 was upregulated, whereas that of fatty acid-binding protein 1, and bone morphogenic protein-2 was downregulated. Furthermore, CFI could be used as a diagnostic biomarker for CC. Functionally, CFI silencing inhibited CC cell proliferation, migration, invasion, and tumor growth. Mechanistically, CFI knockdown downregulated the expression of key glycolysis-related proteins (glucose transporter type 1, hexokinase 2, lactate dehydrogenase A, and pyruvate kinase M2) and the Wnt pathway-related proteins (β-catenin and c-Myc). Further investigation indicated that CFI knockdown inhibited glycolysis in CC by blocking the Wnt/β-catenin/c-Myc pathway., Conclusion: The findings of the present study demonstrate that CFI plays a crucial role in CC development by influencing glycolysis and the Wnt/β-catenin/c-Myc pathway, indicating that it could serve as a promising target for therapeutic intervention in CC., Competing Interests: Conflict-of-interest statement: All the authors report no relevant conflicts of interest for this article., (©The Author(s) 2024. Published by Baishideng Publishing Group Inc. All rights reserved.)

Published

2024

22. Complement factor I upregulates expression of matrix metalloproteinase‐13 and ‐2 and promotes invasion of cutaneous squamous carcinoma cells.

Author

Rahmati Nezhad, Pegah, Riihilä, Pilvi, Piipponen, Minna, Kallajoki, Markku, Meri, Seppo, Nissinen, Liisa, and Kähäri, Veli‐Matti

Subjects

*SQUAMOUS cell carcinoma, *EXTRACELLULAR matrix, *CELL growth, *CANCER cells, *CELL proliferation, *COLLAGEN

Abstract

The incidence of cutaneous squamous cell carcinoma (cSCC) is increasing globally. Here, we have studied the functional role of complement factor I (CFI) in the progression of cSCC. CFI was knocked down in cSCC cells, and RNA‐seq analysis was performed. Significant downregulation of genes in IPA biofunction categories Proliferation of cells and Growth of malignant tumor, in Gene Ontology (GO) terms Metallopeptidase activity and Extracellular matrix component, as well as Reactome Degradation of extracellular matrix was detected after CFI knockdown. Further analysis of the latter three networks, revealed downregulation of several genes coding for invasion‐associated matrix metalloproteinases (MMPs) after CFI knockdown. The downregulation of MMP‐13 and MMP‐2 was confirmed at mRNA, protein and tissue levels by qRT‐qPCR, Western blot and immunohistochemistry, respectively. Knockdown of CFI decreased the invasion of cSCC cells through type I collagen. Overexpression of CFI in cSCC cells resulted in enhanced production of MMP‐13 and MMP‐2 and increased invasion through type I collagen and Matrigel, and in increased ERK1/2 activation and cell proliferation. Altogether, these findings identify a novel mechanism of action of CFI in upregulation of MMP‐13 and MMP‐2 expression and cSCC invasion. These results identify CFI as a prospective molecular marker for invasion and metastasis of cSCC. [ABSTRACT FROM AUTHOR]

Published

2021

23. Prevalence and phenotype associations of complement factor I mutations in geographic atrophy.

Author

Khan, Adnan H., Sutton, Janice, Cree, Angela J., Khandhadia, Samir, De Salvo, Gabriella, Tobin, John, Prakash, Priya, Arora, Rashi, Amoaku, Winfried, Charbel Issa, Peter, MacLaren, Robert E., Bishop, Paul N., Peto, Tunde, Mohamed, Quresh, Steel, David H., Sivaprasad, Sobha, Bailey, Clare, Menon, Geeta, Kavanagh, David, and Lotery, Andrew J.

Abstract

Rare variants in the complement factor I (CFI) gene, associated with low serum factor I (FI) levels, are strong risk factors for developing the advanced stages of age‐related macular degeneration (AMD). No studies have been undertaken on the prevalence of disease‐causing CFI mutations in patients with geographic atrophy (GA) secondary to AMD. A multicenter, cross‐sectional, noninterventional study was undertaken to identify the prevalence of pathogenic rare CFI gene variants in an unselected cohort of patients with GA and low FI levels. A genotype‐phenotype study was performed. Four hundred and sixty‐eight patients with GA secondary to AMD were recruited to the study, and 19.4% (n = 91) demonstrated a low serum FI concentration (below 15.6 μg/ml). CFI gene sequencing on these patients resulted in the detection of rare CFI variants in 4.7% (n = 22) of recruited patients. The prevalence of CFI variants in patients with low serum FI levels and GA was 25%. Of the total patients recruited, 3.2% (n = 15) expressed a CFI variant classified as pathogenic or likely pathogenic. The presence of reticular pseudodrusen was detected in all patients with pathogenic CFI gene variants. Patients with pathogenic CFI gene variants and low serum FI levels might be suitable for FI supplementation in therapeutic trials. [ABSTRACT FROM AUTHOR]

Published

2021

24. Researchers' Work from University of Gdansk Focuses on Lung Cancer (Elevated Expression of Complement Factor I In Lung Cancer Cells Associates With Shorter Survival-potentially Via Non-canonical Mechanism).

Abstract

A study conducted by researchers at the University of Gdansk in Poland focused on the expression of complement factor I (FI) in lung cancer cells and its association with patient outcomes. The researchers found that the intensity of FI expression did not correlate with various clinicopathological characteristics, but it was associated with progression-free survival, overall survival, and disease-specific survival. The study also revealed that FI may have a non-canonical role in lung cancer cells, influencing cellular physiology and contributing to poor prognosis. Further research is needed to understand the mechanisms behind this association. [Extracted from the article]

Published

2024

25. Ocular biomarker profiling after complement factor I gene therapy in geographic atrophy secondary to age-related macular degeneration (Updated June 15, 2024).

Abstract

A recent preprint abstract discusses the use of gene therapy in treating geographic atrophy (GA) secondary to age-related macular degeneration (AMD). The study evaluated the effects of subretinal AAV2 complement factor I (CFI) gene therapy on complement biomarkers in ocular fluid samples from 28 subjects in a Phase I/II clinical trial. The results showed an increase in intact complement factor I (FI) levels post-treatment, but minimal changes in other complement proteins. The study suggests that the gene therapy may not have provided sufficient FI protein to effectively slow GA growth. Further research is needed to determine the optimal dose for future clinical development. [Extracted from the article]

Published

2024

26. Generation and Characterization of Mouse Models of C3 Glomerulonephritis With CFI D288G and P467S Mutations

Author

Hui Song, Mingchao Zhang, Xue Li, Feng Xu, Difei Zhang, Xiaodong Zhu, Jiong Zhang, Weisong Qin, Shaolin Shi, and Jiqiu Wen

Subjects

complement factor I, amino acid variations, C3 glomerulopathy, mouse model, lipopolysaccharides, Physiology, QP1-981

Abstract

C3 glomerulopathy (C3GP) is a disease entity caused by abnormality of the complement alternative pathway (AP) and characterized by C3 deposition in glomeruli. Many variations or mutations of complement factors are believed to underlie the susceptibility to C3GP, but there is a lack of experimental evidence. We have recently reported a patient with C3 glomerulonephritis (C3GN) and compound heterozygosity of two novel variations in the complement factor (CFI). Here, we generated a mouse model to mimic the CFI variations for studying pathogenicity of CFI variations in C3GN development. We used the CRISPR/Cas9 system to make mutant mouse lines that carried D288G and P467S mutations in CFI, respectively, and crossed them to generate mice with compound heterozygosity of CFI D288G and P467S. The mice were all normal in either SPF (specific pathogen free) or regular environment. When treated with lipopolysaccharides (LPS), a bacterial endotoxin that mimics infection and sepsis, the mice developed albuminuria, kidney function impairment, and C3 glomerular deposition at levels comparable with the wild-type mice. The mice with other genotypes concerning CFI D288G and P467S were also tested in parallel. Unexpectedly, we found that the D288G homozygotes all developed severe mesangial deposition of C3 in the LPS model, indicating that CFI D288G variation was involved in the C3 deposition, a key feature of C3GN. The mouse lines generated in the present study can be used to further study the role of CFI variations in C3GN development; in addition, they may be used to screen and test infections and environmental factors capable of triggering C3GN.

Published

2021

27. A rare cause of recurrent acute kidney injury in a 3-year-old girl: Answers.

Author

Kar, Shrutiprajna, Krishnamurthy, Sriram, Karunakar, Pediredla, Maya, Malini, Thangaraj, Abarna, and Agarwal, Yamini

Subjects

*HYPERTENSION, *PLASMA exchange (Therapeutics), *DISEASE relapse, *HEMOLYTIC-uremic syndrome, *RARE diseases, *ACUTE kidney failure, *CHILDREN

Abstract

The article presents answers to a clinical quiz about a rare cause of recurrent acute kidney injury in a three-year-old girl.

Published

2021

28. Generation and Characterization of Mouse Models of C3 Glomerulonephritis With CFI D288G and P467S Mutations.

Author

Song, Hui, Zhang, Mingchao, Li, Xue, Xu, Feng, Zhang, Difei, Zhu, Xiaodong, Zhang, Jiong, Qin, Weisong, Shi, Shaolin, and Wen, Jiqiu

Subjects

LABORATORY mice, ANIMAL disease models, GLOMERULONEPHRITIS, LIPOPOLYSACCHARIDES, KIDNEY physiology, KIDNEY diseases, IGA glomerulonephritis

Abstract

C3 glomerulopathy (C3GP) is a disease entity caused by abnormality of the complement alternative pathway (AP) and characterized by C3 deposition in glomeruli. Many variations or mutations of complement factors are believed to underlie the susceptibility to C3GP, but there is a lack of experimental evidence. We have recently reported a patient with C3 glomerulonephritis (C3GN) and compound heterozygosity of two novel variations in the complement factor (CFI). Here, we generated a mouse model to mimic the CFI variations for studying pathogenicity of CFI variations in C3GN development. We used the CRISPR/Cas9 system to make mutant mouse lines that carried D288G and P467S mutations in CFI, respectively, and crossed them to generate mice with compound heterozygosity of CFI D288G and P467S. The mice were all normal in either SPF (specific pathogen free) or regular environment. When treated with lipopolysaccharides (LPS), a bacterial endotoxin that mimics infection and sepsis, the mice developed albuminuria, kidney function impairment, and C3 glomerular deposition at levels comparable with the wild-type mice. The mice with other genotypes concerning CFI D288G and P467S were also tested in parallel. Unexpectedly, we found that the D288G homozygotes all developed severe mesangial deposition of C3 in the LPS model, indicating that CFI D288G variation was involved in the C3 deposition, a key feature of C3GN. The mouse lines generated in the present study can be used to further study the role of CFI variations in C3GN development; in addition, they may be used to screen and test infections and environmental factors capable of triggering C3GN. [ABSTRACT FROM AUTHOR]

Published

2021

29. 120 Treatable Acute Neuroinflammatory Disease Associated with Complement Factor I Loss-of-function in the Plain Community.

Author

Reid, Whitney, Carson, Vincent, Krieger, Portia, Stiegler, Amy, Boggon, Titus, Sullivan, Kathleen, Heuvel, Lambertus van den, and Romberg, Neil

Subjects

*ACUTE diseases, *PLAINS

Published

2024

30. A complement factor I (CFI) gene mediates innate immune responses in yellow catfish Pelteobagrus fulvidraco.

Author

Tang, Ying-Yu, Li, Yue-Tian, Zha, Xiao-Han, Zhang, Dai-Zhen, Tang, Bo-Ping, Liu, Qiu-Ning, Jiang, Sen-Hao, and Dai, Li-Shang

Subjects

*FLATHEAD catfish, *GENES, *CHANNEL catfish, *IMMUNE response, *ANTISENSE DNA, *AMINO acids

Abstract

This study isolated CFI gene from Pelteobagrus fulvidraco and named it PfCFI. The cDNA of PfCFI is 2374 bp long, including a 52 bp 5′ untranslated sequence, a 222 bp 3′ untranslated sequence, and an open reading frame (ORF) of 2100 bp encoding polypeptide consisting of 699 amino acids. Phylogenetic analysis revealed that the PfCFI was closely related to CFI of Ictalurus punctatus. Real-time quantitative reverse transcription-PCR (qRT-PCR) analysis indicate that there is the PfCFI gene which expressed in all the rest of tested tissues in varied levels, and mainly distributed in liver and least in heart. The reseachers induce the expressions level of PfCFI gene in liver, spleen, head kidney and blood at different points in time after challenged with lipopolysaccharide (LPS), and polyriboinosinic polyribocytidylic acid (poly I:C), respectively. Together these results suggested that CFI gene plays an important role in resistance to pathogens in yellow catfish immunity. • A complement factor I gene was characterized from yellow catfish Pelteobagrus fulvidraco. • The expression profiles of PfCFI in various tissues were investigated. • The mRNA expression levels of PfCFI were performed in response to Poly I:C or LPS challenge. [ABSTRACT FROM AUTHOR]

Published

2021

31. C3 glomerulonephritis and thrombotic microangiopathy of renal allograft after pulmonary infection in a male with concomitant two complement factor I gene variations: a case report

Author

Jiqiu Wen, Wei Wang, Feng Xu, Jun Sun, Jinsong Chen, and Xuefeng Ni

Subjects

Kidney allograft, Complement factor I, Mutation, Diseases of the genitourinary system. Urology, RC870-923

Abstract

Abstract Background It has been suggested that C3 glomerulonephritis (C3GN) and atypical hemolytic-uremic syndrome (a stereotypical phenotype of thrombotic microangiopathy), two rare entities caused by complement alternative pathway dysregulation share overlapping genetic origin and can be triggered by infections. Case presentation We report a case of concomitant C3GN and thrombotic microangiopathy (TMA) after pulmonary infection in a young male receiving kidney transplantation. Genetic assessment revealed two missense variations in compound heterozygous form in CFI gene (complement factor I). These two variations are segregated with disease in the core family member of this patient. Plasma CFI levels of the patient and family members were all in normal range. We considered that these two variations only impair CFI function rather than its quantity in the serum. Conclusion Our case supports that C3GN and TMA shared overlapping genetic variations and might be triggered by infection in genetically susceptible patients after kidney transplantation.

Published

2018

32. Patent Application Titled "Fluorescence Detection of Circulating Cell Free DNA Including Within Extracellular Vesicles in Biospecimens and Liquid Biopsies" Published Online (USPTO 20240102995).

Abstract

The patent application titled "Fluorescence Detection of Circulating Cell Free DNA Including Within Extracellular Vesicles in Biospecimens and Liquid Biopsies" outlines a method for detecting circulating cell-free DNA (ccf-DNA) in liquid biopsies. By staining extracellular vesicles (EVs) in a biological sample with a DNA staining dye, the presence of DNA, including mitochondrial DNA (mtDNA), can be detected. This method has potential applications in assessing tissue/organ injury severity, monitoring disease progression, and evaluating the response to therapeutic interventions. It can be used in various settings, such as emergency rooms, critical care settings, or at home, and has the potential to diagnose lung adenocarcinoma, traumatic brain injury, brain trauma, concussion, diseases of oxidative stress, and viral infections. The patent application provides a comprehensive list of proteins that can be measured and used in an algorithm to determine the presence and severity of traumatic brain injury. [Extracted from the article]

Published

2024

33. Complement Factor I Gene Polymorphism in a Turkish Age-Related Macular Degeneration Population.

Author

Bezci Aygun, Figen, Kadayıfcılar, Sibel, Ozgul, Rıza Koksal, and Eldem, Bora

Subjects

*RETINAL degeneration, *GENETIC polymorphisms, *PROLIFERATIVE vitreoretinopathy, *OPTICAL coherence tomography, *RHODOPSIN, *FLUORESCENCE angiography

Abstract

Objective: Evaluation of Complement Factor I (CFI) rs10033900 and rs2285714 polymorphism frequencies in patients with age-related macular degeneration (AMD) and healthy controls in a Turkish population. Methods: A total of 111 eyes of 111 AMD patients and 96 eyes of 96 healthy controls, only one eye of individuals, were included in the study; however, 2 patients' and 4 controls' samples were excluded as analyses could not be performed for rs10033900 polymorphism. The AMD patients and control group (>50 years) lacked corneal, lenticular, vitreal opacity. However, these patients did not have any retinal diseases apart from AMD. Venous blood samples of patients were collected. Central macular thickness, subfoveal choroidal thickness (SCT), presence of reticular drusen, epiretinal membrane, and pigment epithelial detachment were investigated using Spectral-Domain Optical Coherence Tomography, and the largest diameter of atrophic areas measured. Drusen properties were documented from fundus photographs. The lesion width was calculated by using fundus fluorescein angiography. Results: There was no difference between patient and control groups and polymorphism distributions. The frequency of the CT allele was higher in patients with dry-type AMD with retinal pigment epithelial abnormality (p = 0.041). SCT was significantly thinner in TT allele carriers with rs2285714 polymorphism (p = 0.030). No significant relationship was found between the other parameters and polymorphism distributions. Con-clusion:CFIrs10033900 and rs2285714 polymorphisms in a Turkish population were not associated with AMD. [ABSTRACT FROM AUTHOR]

Published

2020

34. A novel complement factor I involving in the complement system immune response from Lampetra morii.

Author

Lv, Wanrong, Ma, Anqi, Chi, Xiaoyuan, Li, Qingwei, Pang, Yue, and Su, Peng

Subjects

*IMMUNE response, *LIPOPROTEIN receptors, *IMMUNE system, *VIBRIO anguillarum, *CELL membranes, *COMPLEMENT receptors, *HELA cells, *TRYPSIN

Abstract

Complement factor I (CFI) is a serine protease which plays a key role in the modulation of complement system and the induced-fit factor responsible for controlling the complement-mediated processes. In this study, a CFI gene was cloned and characterized from Lampetra morii (designated as L-CFI) at molecular and cellular levels. The L-CFI protein included a factor I membrane attack complex domain (FIMAC), a scavenger receptor cysteine-rich domain (SRCR), a trypsin-like serine protease domain (Tryp_SPc) and 2 low-density lipoprotein receptor class A domains (LDLa) which would exhibit functional similarities to CFI superfamily proteins. Tissue expression profile analysis showed that L-CFI mRNA constitutively expressed in all tested tissues except erythrocytes, with the predominant expression in liver. The mRNA expression level of L-CFI increased significantly after Vibrio anguillarum and Staphylocccus aureus stimulation. It is demonstrated that L-CFI interacted with L-C3 protein and affected the deposition of L-C3 on the cell surface. Furthermore, lamprey serum after deplete L-CFI and L-C3 reduced the cytotoxic activity against HeLa cells. These findings suggest that L-CFI plays an important role in lamprey immunity and involved in the lamprey complement system. • The expression of L-CFI increased after challenged with S. aureus and V. anguillarum in the adult lamprey leukocytes. • L-CFI could be associated with the function of L-C3 to kill HeLa cells and reduce the biological activity of L-C3. • L-CFI affected the activity of L-C3 depositing on the cell surface. [ABSTRACT FROM AUTHOR]

Published

2020

35. Classical and Non-classical Presentations of Complement Factor I Deficiency: Two Contrasting Cases Diagnosed via Genetic and Genomic Methods

Author

Adrian M. Shields, Alistair T. Pagnamenta, Andrew J. Pollard, OxClinWGS, Jenny C. Taylor, Holger Allroggen, Smita Y. Patel, Samantha J. L. Knight, Niko Popitsch, Carme Camps, Melissa M. Pentony, Erika M. Kvikstad, Lukas Lange, Mona Hashim, Steve Harris, Mark Tilley, Dimitris Vavoulis, Pamela Kaisaki, Vassilis Ragoussis, and Matteo Feral

Subjects

complement factor I, primary immunodeficiency, genomic medicine, pneumococcal infection, neuroinflammation, complement deficiency, Immunologic diseases. Allergy, RC581-607

Abstract

Deficiency of complement factor I is a rare immunodeficiency that typically presents with increased susceptibility to encapsulated bacterial infections. However, non-infectious presentations including rheumatological, dermatological and neurological disease are increasingly recognized and require a high-index of suspicion to reach a timely diagnosis. Herein, we present two contrasting cases of complement factor I deficiency: one presenting in childhood with invasive pneumococcal disease, diagnosed using conventional immunoassays and genetics and the second presenting in adolescence with recurrent sterile neuroinflammation, diagnosed via a genomic approach. Our report and review of the literature highlight the wide spectrum of clinical presentations associated with CFI deficiency and the power of genomic medicine to inform rare disease diagnoses.

Published

2019

36. Classical and Non-classical Presentations of Complement Factor I Deficiency: Two Contrasting Cases Diagnosed via Genetic and Genomic Methods.

Author

Shields, Adrian M., Pagnamenta, Alistair T., Pollard, Andrew J., Taylor, Jenny C., Allroggen, Holger, Patel, Smita Y., Knight, Samantha J. L., Popitsch, Niko, Camps, Carme, Pentony, Melissa M., Kvikstad, Erika M., Lange, Lukas, Hashim, Mona, Harris, Steve, Tilley, Mark, Vavoulis, Dimitris, Kaisaki, Pamela, Ragoussis, Vassilis, Feral, Matteo, and Schuh, Anna H.

Subjects

NEUROLOGICAL disorders, DIAGNOSIS, BACTERIAL diseases, GENETICS, RARE diseases

Abstract

Deficiency of complement factor I is a rare immunodeficiency that typically presents with increased susceptibility to encapsulated bacterial infections. However, non-infectious presentations including rheumatological, dermatological and neurological disease are increasingly recognized and require a high-index of suspicion to reach a timely diagnosis. Herein, we present two contrasting cases of complement factor I deficiency: one presenting in childhood with invasive pneumococcal disease, diagnosed using conventional immunoassays and genetics and the second presenting in adolescence with recurrent sterile neuroinflammation, diagnosed via a genomic approach. Our report and review of the literature highlight the wide spectrum of clinical presentations associated with CFI deficiency and the power of genomic medicine to inform rare disease diagnoses. [ABSTRACT FROM AUTHOR]

Published

2019

37. Rare complement factor I variants associated with reduced macular thickness and age-related macular degeneration in the UK Biobank

Author

Nikolaos Tzoumas, David Kavanagh, Heather J Cordell, Andrew J Lotery, Praveen J Patel, and David H Steel

Subjects

Genotype, Fibrinogen, General Medicine, Polymorphism, Single Nucleotide, United Kingdom, eye diseases, Macular Degeneration, Complement Factor I, Complement Factor H, Genetics, Humans, sense organs, Molecular Biology, Genetics (clinical), Biological Specimen Banks

Abstract

To evaluate potential diagnostic and therapeutic biomarkers for age-related macular degeneration (AMD), we identified 8433 UK Biobank participants with rare complement Factor I gene (CFI) variants, 579 with optical coherence tomography-derived macular thickness data. We stratified these variants by predicted gene expression and measured their association with retinal pigment epithelium-Bruch’s membrane (RPE-BM) complex and retinal thicknesses at nine macular subfields, as well as AMD risk, using multivariable regression models adjusted for the common complement Factor H gene (CFH) p.Y402H and age-related maculopathy susceptibility protein 2 gene (ARMS2) p.A69S risk genotypes. CFI variants associated with low Factor I levels predicted a thinner mean RPE-BM (95% confidence interval [CI] −1.66 to −0.37 μm, P = 0.002) and retina (95% CI −5.88 to −0.13 μm, P = 0.04) and a higher AMD risk (odds ratio [OR] = 2.26, 95% CI 1.56 to 3.27, P

Published

2022

38. Complement factor I: Regulatory nexus, driver of immunopathology, and therapeutic.

Author

Hallam, T.M., Sharp, S.J., Andreadi, A., and Kavanagh, D.

Subjects

*IMMUNOPATHOLOGY, *MACULAR degeneration, *HEMOLYTIC-uremic syndrome, *BLOOD proteins, *DISEASE relapse, *PROTEIN S

Abstract

Complement factor I (FI) is the nexus for classical, lectin and alternative pathway complement regulation. FI is an 88 kDa plasma protein that circulates in an inactive configuration until it forms a trimolecular complex with its cofactor and substrate whereupon a structural reorganization allows the catalytic triad to cleave its substrates, C3b and C4b. In keeping with its role as the master complement regulatory enzyme, deficiency has been linked to immunopathology. In the setting of complete FI deficiency, a consumptive C3 deficiency results in recurrent infections with encapsulated microorganisms. Aseptic cerebral inflammation and vasculitic presentations are also less commonly observed. Heterozygous mutations in the factor I gene (CFI) have been demonstrated to be enriched in atypical haemolytic uraemic syndrome, albeit with a very low penetrance. Haploinsufficiency of CFI has also been associated with decreased retinal thickness and is a strong risk factor for the development of age-related macular degeneration. Supplementation of FI using plasma purified or recombinant protein has long been postulated, however, technical difficulties prevented progression into clinical trials. It is only using gene therapy that CFI supplementation has reached the clinic with GT005 in phase I/II clinical trials for geographic atrophy. [ABSTRACT FROM AUTHOR]

Published

2023

39. Cutaneous Vasculitis and Recurrent Infection Caused by Deficiency in Complement Factor I

Author

Sira Nanthapisal, Despina Eleftheriou, Kimberly Gilmour, Valentina Leone, Radhika Ramnath, Ebun Omoyinmi, Ying Hong, Nigel Klein, and Paul A. Brogan

Subjects

complement factor I, vasculitis, infection, complement deficiency, autoinflammation, Immunologic diseases. Allergy, RC581-607

Abstract

Cutaneous leukocytoclastic vasculitis arises from immune complex deposition and dysregulated complement activation in small blood vessels. There are many causes, including dysregulated host response to infection, drug reactions, and various autoimmune conditions. It is increasingly recognised that some monogenic autoinflammatory diseases cause vasculitis, although genetic causes of vasculitis are extremely rare. We describe a child of consanguineous parents who presented with chronic cutaneous leukocytoclastic vasculitis, recurrent upper respiratory tract infection, and hypocomplementaemia. A homozygous p.His380Arg mutation in the complement factor I (CFI) gene CFI was identified as the cause, resulting in complete absence of alternative complement pathway activity, decreased classical complement activity, and low levels of serum factor I, C3, and factor H. C4 and C2 levels were normal. The same homozygous mutation and immunological defects were also identified in an asymptomatic sibling. CFI deficiency is thus now added to the growing list of monogenic causes of vasculitis and should always be considered in vasculitis patients found to have persistently low levels of C3 with normal C4.

Published

2018

40. High level of complement factor Ba within first prenatal test of gestation increases the risk of subsequent gestational diabetes: a propensity score-matched study

Author

Junxi Lu, Junxian Li, Fang Liu, Ying Shen, Huijuan Lu, Ye Ji, Bo Liu, Hairong Tian, and Ziyun Li

Subjects

Blood Glucose, medicine.medical_specialty, endocrine system diseases, Endocrinology, Diabetes and Metabolism, Perinatal outcome, Complement factor I, Endocrinology, Pregnancy, Prenatal Diagnosis, Humans, Medicine, Propensity Score, business.industry, Obstetrics, nutritional and metabolic diseases, Obstetrics and Gynecology, Glucose Tolerance Test, medicine.disease, Test (assessment), Gestational diabetes, Diabetes, Gestational, Propensity score matching, Gestation, Female, business, Complement Factor B

Abstract

This study was to assess the alteration of circulating complement factor Ba (CFBa) within 11 to 17 weeks of gestation and its association with subsequent gestational diabetes mellitus (GDM) and its delivery outcome.Biochemical parameters and blood samples were collected from 399 pregnant women within 11 to 17 weeks of gestation. At 24 to 28 weeks of gestation, all participants underwent 75-g oral glucose tolerance test and were assigned to GDM group (Two groups of 74 well-matched patients who maintained balance in terms of baseline characteristics. The levels of CFBa in pregnant women who later developed GDM were significantly higher than those in healthy pregnant women [0.4(0.1-0.8)High level of the CFBa within 11 to 17 weeks of gestation increases the risk of subsequent GDM, and maybe a biomarker for predicting GDM.

Published

2021

41. Membrane cofactor protein (MCP; CD46): deficiency states and pathogen connections

Author

John P. Atkinson and M. Kathryn Liszewski

Subjects

0301 basic medicine, COVID-19 Vaccines, T-Lymphocytes, viruses, T cell, Immunology, Complement factor I, Lymphocyte Activation, medicine.disease_cause, Article, Membrane Cofactor Protein, 03 medical and health sciences, 0302 clinical medicine, Autophagy, medicine, Animals, Humans, Immunology and Allergy, Receptor, Complement Activation, ComputingMethodologies_COMPUTERGRAPHICS, Coronavirus, Oncolytic Virotherapy, Serine protease, Polymorphism, Genetic, biology, SARS-CoV-2, CD46, Reproduction, COVID-19, female genital diseases and pregnancy complications, Complement system, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Host-Pathogen Interactions, biology.protein, 030215 immunology

Abstract

Graphical abstract, Membrane cofactor protein (MCP; CD46), a ubiquitously expressed complement regulatory protein, serves as a cofactor for serine protease factor I to cleave and inactivate C3b and C4b deposited on host cells. However, CD46 also plays roles in human reproduction, autophagy, modulating T cell activation and effector functions and is a member of the newly identified intracellular complement system (complosome). CD46 also is a receptor for 11 pathogens (‘pathogen magnet’). While CD46 deficiencies contribute to inflammatory disorders, its overexpression in cancers and role as a receptor for some adenoviruses has led to its targeting by oncolytic agents and adenoviral-based therapeutic vectors, including coronavirus disease of 2019 (COVID-19) vaccines. This review focuses on recent advances in identifying disease-causing CD46 variants and its pathogen connections.

Published

2021

42. Anti-Factor H Antibody-Associated Atypical Hemolytic Uremic Syndrome: A Case Report

Author

Emilija Sahpazova, Nora Abazi-Emini, Jovana Putnik, and Velibor Tasic

Subjects

medicine.medical_specialty, Thrombotic microangiopathy, 030232 urology & nephrology, Complement factor I, 030204 cardiovascular system & hematology, Neutropenia, Gastroenterology, 03 medical and health sciences, 0302 clinical medicine, Maintenance therapy, Internal medicine, Atypical hemolytic uremic syndrome, medicine, Humans, Cyclophosphamide, Atypical Hemolytic Uremic Syndrome, Autoantibodies, Proteinuria, business.industry, Autoantibody, Complement System Proteins, medicine.disease, 3. Good health, Child, Preschool, Complement Factor H, Alternative complement pathway, Female, medicine.symptom, business

Abstract

Introduction: Atypical hemolytic uremic syndrome (aHUS) is a rare form of thrombotic microangiopathy, caused by dysregulation of the complement alternative pathway. Deletion of the complement factor H–related genes, CFHR1 and CFHR3, together with the presence of CFH autoantibodies are reported in aHUS patients, representing 10% of cases of patients with aHUS. Case presentation: We report here on a case of 4-year-old girl with anti-CFH antibody-associated aHUS. The measurement of complement factors and anti-factor H antibodies, was the main guideline for making an accurate diagnosis and providing the appropriate therapy, with the patient responding positively to plasma exchanges (PEs) and cyclophosphamide pulses. We then, one year after disease onset, continued with glucocorticoids and mycophenolate mofetil (MMF), as maintenance therapy. There were no complications during the therapy other than neutropenia. Now, one year after the cessation of the immune suppression therapy, she is in remission with normal kidney function, no signs of hemolysis, normal C3 levels, and normal range proteinuria. The anti-factor H autoantibody titer decreased but still remained positive, the factor H antigen values remained low all throughout. Close follow-up is applied with frequent urine testing and complete blood count with an intention for early detection of relapse of the disease. Conclusion: The purpose of this case report is to emphasize the value of complement factor measurements and also to separate anti-CFH antibody-associated aHUS as an entity, because immunosuppressive therapy provides an excellent response..

Published

2021

43. Functional and Expressional Analyses Reveal the Distinct Role of Complement Factor I in Regulating Complement System Activation during GCRV Infection in Ctenopharyngodon idella

Author

Yi Liu, Zhao Lv, Tiaoyi Xiao, Xuewen Zhang, Chunhua Ding, Beibei Qin, Baohong Xu, and Qiaolin Liu

Subjects

Inorganic Chemistry, grass carp, complement factor I, complement component 3b, grass carp reovirus infection, complement regulation mechanism, Organic Chemistry, General Medicine, Physical and Theoretical Chemistry, Molecular Biology, Spectroscopy, Catalysis, Computer Science Applications

Abstract

Complement factor I (CFI), a complement inhibitor, is well known for regulating the complement system activation by degrading complement component 3b (C3b) in animal serum, thus becoming involved in innate defense. Nevertheless, the functional mechanisms of CFI in the complement system and in host-pathogen interactions are far from being clarified in teleost fish. In the present study, we cloned and characterized the CFI gene, CiCFI, from grass carp (Ctenopharyngodon idella) and analyzed its function in degrading serum C3b and expression changes after grass carp reovirus (GCRV) infection. The open reading frame of CiCFI was found to be 2121 bp, encoding 706 amino acids with a molecular mass of 79.06 kDa. The pairwise alignments showed that CiCFI shared the highest identity (66.9%) with CFI from Carassius gibelio and the highest similarity (78.7%) with CFI from Danio rerio. The CiCFI protein was characterized by a conserved functional core Tryp_SPc domain with the catalytic triad and substrate binding sites. Phylogenetic analysis indicated that CiCFI and the homologs CFIs from other teleost fish formed a distinct evolutionary branch. Similar with the CFIs reported in mammals, the recombinant CiCFI protein could significantly reduce the C3b content in the serum, demonstrating the conserved function of CiCFI in the complement system in the grass carp. CiCFI mRNA and protein showed the highest expression level in the liver. After GCRV infection, the mRNA expressions of CiCFI were first down-regulated, then up-regulated, and then down-regulated to the initial level, while the protein expression levels maintained an overall downward trend to the late stage of infection in the liver of grass carps. Unexpectedly, the protein levels of CiCFI were also continuously down-regulated in the serum of grass carps during GCRV infection, while the content of serum C3b proteins first increases and then returns to the initial level, suggesting a distinct role of CiCFI in regulating complement activation and fish-virus interaction. Combining our previous results that complement factor D, a complement enhancer, shows continuously up-regulated expression levels in grass carps during GCRV infection, and this study may provide the further essential data for the full picture of complex complement regulation mechanism mediated by Df and CFI of the grass carp during pathogen infection.

Published

2022

44. Molecular characterization and expression of complement factor I in Pelteobagrus vachellii during Aeromonas hydrophila infection.

Author

Qin, Chuanjie, Gong, Quan, Wen, Zhengyong, and Yuan, Dengyue

Subjects

*SERINE proteinases, *PROTEIN expression, *CATFISHES, *AEROMONAS hydrophila, *BACTERIAL diseases in fishes

Abstract

Complement factor I (CFI) is a novel regulatory serine protease that plays an important role in resistance to pathogen infection. In this study, the CFI gene of Pelteobagrus vachellii ( Pv-CFI ) was sequenced and characterized. The full-length cDNA of 2320 bp includes a 155 bp 5′-untranslated region (UTR), a 164 bp 3′-UTR, and a 2001 bp open reading frame (ORF) encoding a 667 amino acids. Multiple sequence alignment revealed five highly conserved domains with a typical modular architecture and identical active sites in vertebrates, indicating a conserved function. Pv-CFI mRNA was constitutively expressed in all examined tissues and most abundant in liver. During infection with Aeromonas hydrophila , Pv-CFI mRNA expression was significantly up-regulated in liver at 3–24 h, spleen at 3–48 h and head kidney at 3–48 h. The results suggest Pv-CFI plays an important role in resistance to pathogenic bacteria in P. vachellii . [ABSTRACT FROM AUTHOR]

Published

2018

45. Cutaneous Vasculitis and Recurrent Infection Caused by Deficiency in Complement Factor I.

Author

Nanthapisal, Sira, Eleftheriou, Despina, Gilmour, Kimberly, Leone, Valentina, Ramnath, Radhika, Omoyinmi, Ebun, Hong, Ying, Klein, Nigel, and Brogan, Paul A.

Subjects

LEUKOCYTOCLASTIC vasculitis, RESPIRATORY infections

Abstract

Cutaneous leukocytoclastic vasculitis arises from immune complex deposition and dysregulated complement activation in small blood vessels. There are many causes, including dysregulated host response to infection, drug reactions, and various autoimmune conditions. It is increasingly recognised that some monogenic autoinflammatory diseases cause vasculitis, although genetic causes of vasculitis are extremely rare. We describe a child of consanguineous parents who presented with chronic cutaneous leukocytoclastic vasculitis, recurrent upper respiratory tract infection, and hypocomplementaemia. A homozygous p.His380Arg mutation in the complement factor I (CFI) gene CFI was identified as the cause, resulting in complete absence of alternative complement pathway activity, decreased classical complement activity, and low levels of serum factor I, C3, and factor H. C4 and C2 levels were normal. The same homozygous mutation and immunological defects were also identified in an asymptomatic sibling. CFI deficiency is thus now added to the growing list of monogenic causes of vasculitis and should always be considered in vasculitis patients found to have persistently low levels of C3 with normal C4. [ABSTRACT FROM AUTHOR]

Published

2018

46. Cloning of the full-length cDNA of the gene encoding complement C5 from grass carp (Ctenopharyngodon idella) and its expression in different tissues by following grass carp reovirus infection

Author

Tiaoyi Xiao, Hang Su, Baohong Xu, Qiaolin Liu, Jiajia Ni, Ligang Lv, and Yi Liu

Subjects

Signal peptide, Cloning, biology, Complement factor I, Aquatic Science, biology.organism_classification, Grass carp, Complement system, Microbiology, Rapid amplification of cDNA ends, Complementary DNA, sense organs, Agronomy and Crop Science, Gene

Abstract

Grass carp (Ctenopharyngodon idella) is the most widely produced freshwater aquaculture product worldwide. However, its susceptibility to microbial infections during its cultivation restricts its development. The complement system plays an important role in immune defence. To investigate the transcription of the complement factor C5 and production of its cleavage product C5a in grass carp infected with grass carp reovirus (GCRV), the full-length C5 gene sequence was cloned and sequenced using the rapid amplification of cDNA ends method, and C5 transcription and C5a production in different grass carp tissues at different GCRV infection stages were determined by RT-qPCR and western blotting, respectively. Our results showed that the full-length cDNA of the C5 gene was 5365-bp long, encoding 1687 amino acids. Signal peptide prediction showed that C5 had a secretory signal peptide. After artificial infection with GCRV, C5 transcription in grass carp liver increased significantly before the appearance of symptoms. C5a generation in the liver increased significantly from the onset of disease symptoms, and continued to increase until recovery. GCRV induced C5 cleavage in grass carp, with C5a production.

Published

2021

47. Vaccinia-related kinase 2 drives pancreatic cancer progression by protecting Plk1 from Chfr-mediated degradation

Author

Hengqing Zhu, Qing Li, Hong Peng, Bin Xu, Zhaoxia Zeng, Zi Jiang, Liangyun Guo, Sisi Chen, Yulan Zhao, and Jing Zhu

Subjects

0301 basic medicine, Cancer Research, biology, Kinase, Complement factor I, PLK1, Ubiquitin ligase, Cell biology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Ubiquitin, 030220 oncology & carcinogenesis, CHFR, Genetics, biology.protein, Phosphorylation, Threonine, Molecular Biology

Abstract

As a key cell cycle regulator, polo-like kinase 1 (Plk1) has been recognized as a crucial factor involved in the progression of pancreatic cancer (PC). However, its regulatory mechanism is poorly understood. Here, we present evidence that Plk1 is a novel substrate of vaccinia-related kinase 2 (VRK2), a serine-threonine kinase that is highly expressed and predicts poor prognosis in PC. VRK2 phosphorylates Plk1 at threonine 210 and protects it from ubiquitin-dependent proteasomal degradation. We showed that mechanistically complement factor H-related protein (CFHR), as a major E3 ligase, promotes Plk1 degradation by ubiquitinating it at lysine 209. Phosphorylation of Plk1 at threonine 210 by VRK2 interferes with the interaction of Chfr with Plk1 and antagonizes Plk1 ubiquitination, thereby stabilizing the Plk1 protein. Taken together, our data reveal a mechanism of Plk1 overexpression in PC and provide evidence for targeting VRK2 as a potential therapeutic strategy.

Published

2021

48. Inflammatory immune response in recipients of transcatheter aortic valves

Author

Christian Nitsche, Dominika Polak, Cecilia Veraar, Hendrik Jan Ankersmit, Matthias Koschutnik, Andreas Mangold, Barbara Bohle, Maria Laggner, Julia Mascherbauer, and Bernhard Moser

Subjects

medicine.medical_specialty, biology, business.industry, MitraClip, Inflammation, Complement factor I, medicine.disease, Systemic inflammation, Immune system, Internal medicine, Aortic valve stenosis, medicine, biology.protein, Cardiology, medicine.symptom, Antibody, Mitral valve regurgitation, business

Abstract

Objective Transcatheter aortic valve implantation (TAVI) is rapidly replacing cardiac surgery due to its minimal invasiveness and practicality. Midterm immunological studies on the biocompatibility of galactose-alpha-1,3-galactose (α-Gal)–carrying bioprosthetic heart valves for TAVI are not available. In this study we investigated whether bioprosthetic heart valves employed for TAVI augment an α-Gal–specific antibody-dependent and antibody-independent immune response 3 months after TAVI implantation. Methods This prospective observational study included 27 patients with severe aortic valve stenosis undergoing TAVI and 10 patients with severe mitral valve regurgitation treated with a transcatheter MitraClip (Abbott Laboratories, Abbott Park, Ill) procedure. Blood samples were drawn before and 90 days after treatment at a routine checkup. Serum samples were analyzed using enzyme-linked immunosorbent assay. Serum concentrations of α-Gal–specific immunoglobulin (Ig) G, IgG subclasses and IgE, complement factor 3a, NETosis-specific citrullinated H3, and the systemic inflammation markers soluble suppression of tumorigenicity and interleukin 33 were evaluated. Results Three months after TAVI, we found significantly increased serum concentrations of α-Gal–specific IgG3, complement factor complement factor 3a, citrullinated H3 levels, and soluble suppression of tumorigenicity (P = .002, P = .001, P = .025, and P = .039, respectively). Sensitization of α-Gal–specific IgE antibodies occurred in 55% of all patients after TAVI. Conclusions Our results indicate that TAVI elicits a midterm, specific humoral immune response against α-Gal and causes an unspecific humoral inflammation compared with patients undergoing MitraClip implantation. This observation will lead to a better understanding of postintervention morbidity and the long-term durability of bioprostheses and indicates that caution is appropriate when designing implantation strategies for younger patients.

Published

2021

49. Research from Linnaeus University Provides New Data on Complement C3b Inactivator Proteins (Functional evaluation of complement factor I variants by immunoassays and SDS-PAGE).

Abstract

A recent study conducted at Linnaeus University in Kalmar, Sweden, focused on complement C3b inactivator proteins, which play a crucial role in regulating the complement system. The researchers evaluated eight genetic variants of complement factor I (FI) found in patients and assessed their co-factor activity using various analytical assays. The study found that mutations in certain domains of FI led to reduced protease activity, while others did not significantly affect its function. The results highlight the importance of using multiple methods and co-factors to accurately assess the impact of mutations in FI and provide new insights for diagnostic tools in evaluating these mutations. [Extracted from the article]

Published

2023

50. Researchers at Newcastle University Release New Data on Age-Related Macular Degeneration (Rare Complement Factor I Variants Associated With Reduced Macular Thickness and Age-related Macular Degeneration In the Uk Biobank).

Abstract

Newcastle upon Tyne, United Kingdom, Europe, Age-Related Macular Degeneration, Biological Factors, Biological Pigments, Blood Proteins, Complement Factor I, Complement C3b Inactivator Proteins, Enzymes and Coenzymes, Eye Diseases and Conditions, Genetics, Health and Medicine, Immunology, Immunoproteins, Macular Degeneration, Peptide Hydrolases, Retinal Degeneration, Retinal Diseases and Conditions, Retinal Pigments, Risk and Prevention, Serine Endopeptidases, Complement System Proteins Keywords: Newcastle upon Tyne; United Kingdom; Europe; Age-Related Macular Degeneration; Biological Factors; Biological Pigments; Blood Proteins; Complement C3b Inactivator Proteins; Complement Factor I; Complement System Proteins; Enzymes and Coenzymes; Eye Diseases and Conditions; Genetics; Health and Medicine; Immunology; Immunoproteins; Macular Degeneration; Peptide Hydrolases; Retinal Degeneration; Retinal Diseases and Conditions; Retinal Pigments; Risk and Prevention; Serine Endopeptidases EN Newcastle upon Tyne United Kingdom Europe Age-Related Macular Degeneration Biological Factors Biological Pigments Blood Proteins Complement C3b Inactivator Proteins Complement Factor I Complement System Proteins Enzymes and Coenzymes Eye Diseases and Conditions Genetics Health and Medicine Immunology Immunoproteins Macular Degeneration Peptide Hydrolases Retinal Degeneration Retinal Diseases and Conditions Retinal Pigments Risk and Prevention Serine Endopeptidases 1823 1823 1 10/30/23 20231103 NES 231103 2023 NOV 3 (NewsRx) -- By a News Reporter-Staff News Editor at Genomics & Genetics Weekly -- Investigators publish new report on Eye Diseases and Conditions - Age-Related Macular Degeneration. [Extracted from the article]

Published

2023