Your search keyword '"CFH"' showing total 344 results

1. Complement proteins and complement regulatory proteins are associated with age-related macular degeneration stage and treatment response.

Author

Thomsen, Alexander Kai, Steffensen, Maria Abildgaard, Villarruel Hinnerskov, Jenni Martinez, Nielsen, Amalie Thomsen, Vorum, Henrik, Honoré, Bent, Nissen, Mogens Holst, and Sørensen, Torben Lykke

Abstract

Background: Dysregulation of the complement system is involved in development of age-related macular degeneration (AMD). The complement cascade is regulated by membrane bound complement regulatory proteins (Cregs) on mononuclear leukocytes among others. This study aims to investigate systemic complement proteins and Cregs in AMD stages and their association with treatment response in neovascular AMD (nAMD). Methods: In this clinical prospective study, treatment-naïve patients with nAMD, intermediate AMD (iAMD) and healthy controls were recruited and systemic complement proteins C3, C3a and C5a were investigated with electrochemiluminescence immunoassays, and Creg expression (CD35, CD46 and CD59) on T cells (CD4 + and CD8+) and monocytes (classical, intermediate and non-classical) investigated with flow cytometry. Treatment response in nAMD patients was evaluated after loading dose and after one year, and categorized as good, partial or poor. Complement proteins and Creg expression levels were compared between healthy controls, iAMD and nAMD, as well as between good, partial and poor nAMD treatment response groups. Polymorphisms in the CFH and ARMS2 genes were analyzed and compared to complement proteins and Creg expression levels in nAMD patients. Results: One hundred patients with nAMD, 34 patients with iAMD and 61 healthy controls were included. 94 nAMD patients completed the 1-year follow-up. Distribution of treatment response in nAMD was 61 (65%) good, 26 (28%) partial, and 7 (7%) poor responders. The distribution of 1-year treatment response was 50 (53%) good, 33 (36%) partial, and 11 (11%) poor responders. The concentrations of systemic C3, C3a, and the C3a/C3-ratio were significantly increased in patients with nAMD compared to healthy controls (P < 0.001, P = 0.002, and P = 0.035, respectively). Systemic C3 was also increased in iAMD compared to healthy controls (P = 0.031). The proportion of CD46 + CD4 + T cells and CD59 + intermediate monocytes were significantly decreased in patients with nAMD compared to healthy controls (P = 0.018 and P = 0.042, respectively). The post-loading dose partial treatment response group had significantly lower concentrations of C3a and C5a compared to the good response group (P = 0.005 and P = 0.042, respectively). The proportion of CD35 + monocytes was significantly lower in the 1-year partial response group compared to the 1-year good response group (P = 0.039). High-risk CFH genotypes in nAMD patients was associated with increased C3a, C3a/C3-ratio, and expression levels of CD35 + CD8 + T cells and CD46 + classical monocytes, while expression level of CD46 + non-classical monocytes was decreased. Conclusion: Elevated concentrations of systemic complement proteins were found in patients with iAMD and nAMD. Decreased Creg expression levels were found in patients with nAMD. Partially responding nAMD patients had a dysregulated complement system and Cregs compared to good responders. [ABSTRACT FROM AUTHOR]

Published

2024

2. Impact of genomic and epigenomic alterations of multigene on a multicancer pedigree.

Author

Gao, Jinyu, Wu, Yongzhang, Yu, Jieming, Qiu, Yinbin, Yi, Tiantian, Luo, Chaochao, Zhang, Junxiao, Lu, Gary, Li, Xu, Xiong, Fu, Wu, Xuedong, and Pan, Xinghua

Subjects

*HEREDITARY cancer syndromes, *WHOLE genome sequencing, *SOMATIC mutation, *MONOZYGOTIC twins, *TWINS, *EPIGENOMICS, BONE marrow cancer

Abstract

Background: Germline mutations have been identified in a small number of hereditary cancers, but the genetic predisposition for many familial cancers remains to be elucidated. Methods: This study identified a Chinese pedigree that presented different cancers (breast cancer, BRCA; adenocarcinoma of the esophagogastric junction, AEG; and B‐cell acute lymphoblastic leukemia, B‐ALL) in each of the three generations. Whole‐genome sequencing and whole‐exome sequencing were performed on peripheral blood or bone marrow and cancer biopsy samples. Whole‐genome bisulfite sequencing was conducted on the monozygotic twin brothers, one of whom developed B‐ALL. Results: According to the ACMG guidelines, bioinformatic analysis of the genome sequencing revealed 20 germline mutations, particularly mutations in the DNAH11 (c.9463G > A) and CFH (c.2314G > A) genes that were documented in the COSMIC database and validated by Sanger sequencing. Forty‐one common somatic mutated genes were identified in the cancer samples, displaying the same type of single nucleotide substitution Signature 5. Meanwhile, hypomethylation of PLEK2, MRAS, and RXRA as well as hypermethylation of CpG island associated with WT1 was shown in the twin with B‐ALL. Conclusions: These findings reveal genomic alterations in a pedigree with multiple cancers. Mutations found in the DNAH11, CFH genes, and other genes predispose to malignancies in this family. Dysregulated methylation of WT1, PLEK2, MRAS, and RXRA in the twin with B‐ALL increases cancer susceptibility. The similarity of the somatic genetic changes among the three cancers indicates a hereditary impact on the pedigree. These familial cancers with germline and somatic mutations, as well as epigenomic alterations, represent a common molecular basis for many multiple cancer pedigrees. [ABSTRACT FROM AUTHOR]

Published

2024

3. Genetic Insights into Age-Related Macular Degeneration.

Author

Bhumika, Bora, Nalini S., and Bora, Puran S.

Subjects

MACULAR degeneration, EXTRACELLULAR matrix proteins, COMPLEMENT factor H, VISION disorders, GENETIC variation

Abstract

One of the major causes of vision impairment among elderly people in developed nations is age-related macular degeneration (AMD). The distinctive features of AMD are the accumulation of extracellular deposits called drusen and the gradual deterioration of photoreceptors and nearby tissues in the macula. AMD is a complex and multifaceted disease influenced by several factors such as aging, environmental risk factors, and a person's genetic susceptibility to the condition. The interaction among these factors leads to the initiation and advancement of AMD, where genetic predisposition plays a crucial role. With the advent of high-throughput genotyping technologies, many novel genetic loci associated with AMD have been identified, enhancing our knowledge of its genetic architecture. The common genetic variants linked to AMD are found on chromosome 1q32 (in the complement factor H gene) and 10q26 (age-related maculopathy susceptibility 2 and high-temperature requirement A serine peptidase 1 genes) loci, along with several other risk variants. This review summarizes the common genetic variants of complement pathways, lipid metabolism, and extracellular matrix proteins associated with AMD risk, highlighting the intricate pathways contributing to AMD pathogenesis. Knowledge of the genetic underpinnings of AMD will allow for the future development of personalized diagnostics and targeted therapeutic interventions, paving the way for more effective management of AMD and improved outcomes for affected individuals. [ABSTRACT FROM AUTHOR]

Published

2024

4. Association between circulatory complement activation and hypertensive renal damage: a case–control study

Author

Zhongli Wang, Tingting Zhang, Xinyu Wang, Jianlong Zhai, Lili He, Sai Ma, Qingjuan Zuo, Guorui Zhang, and Yifang Guo

Subjects

Complement system, hypertensive renal damage, complement C3, alternative complement pathway (AP), CFH, Diseases of the genitourinary system. Urology, RC870-923

Abstract

Objective The aim of this study was to investigate the potential importance of complement system activation, with particular emphasis on the complement alternative pathway (AP), in the pathogenesis of hypertensive renal damage.Methods Serum complement C3, complement Factor H (CFH) and AP activation were assessed in 66 participants with established essential hypertension with renal damage (RD). Fifty-nine patients with age- and sex-matched essential hypertension without renal damage (NRD) and 58 healthy participants (normal) were selected.Results Our study revealed that C3 and AP50 continuously increased from normal to NRD to RD (p

Published

2024

5. Moss-produced human complement factor H with modified glycans has an extended half-life and improved biological activity.

Author

Tschongov, Todor, Konwar, Swagata, Busch, Andreas, Sievert, Christian, Hartmann, Andrea, Noris, Marina, Gastoldi, Sara, Aiello, Sistiana, Schaaf, Andreas, Panse, Jens, Zipfel, Peter F., Dabrowska-Schlepp, Paulina, and Häffner, Karsten

Subjects

COMPLEMENT factor H, HEMOLYTIC-uremic syndrome, GLYCANS, COMPLEMENT activation, INDUSTRIAL costs

Abstract

Most drugs that target the complement system are designed to inhibit the complement pathway at either the proximal or terminal levels. The use of a natural complement regulator such as factor H (FH) could provide a superior treatment option by restoring the balance of an overactive complement system while preserving its normal physiological functions. Until now, the systemic treatment of complement-associated disorders with FH has been deemed unfeasible, primarily due to high production costs, risks related to FH purified from donors' blood, and the challenging expression of recombinant FH in different host systems. We recently demonstrated that a moss-based expression system can produce high yields of properly folded, fully functional, recombinant FH. However, the half-life of the initial variant (CPV-101) was relatively short. Here we show that the same polypeptide with modified glycosylation (CPV-104) achieves a pharmacokinetic profile comparable to that of native FH derived from human serum. The treatment of FH-deficient mice with CPV-104 significantly improved important efficacy parameters such as the normalization of serum C3 levels and the rapid degradation of C3 deposits in the kidney compared to treatment with CPV-101. Furthermore, CPV-104 showed comparable functionality to serum-derived FH in vitro, as well as similar performance in ex vivo assays involving samples from patients with atypical hemolytic uremic syndrome, C3 glomerulopathy and paroxysomal nocturnal hematuria. CPV-104 - the human FH analog expressed in moss - will therefore allow the treatment of complement-associated human diseases by rebalancing instead of inhibiting the complement cascade. [ABSTRACT FROM AUTHOR]

Published

2024

6. CFH (rs1061170, rs1410996), KDR (rs2071559, rs1870377) and KDR and CFH Serum Levels in AMD Development and Treatment Efficacy.

Author

Cebatoriene, Dzastina, Vilkeviciute, Alvita, Gedvilaite, Greta, Bruzaite, Akvile, Kriauciuniene, Loresa, Zaliuniene, Dalia, and Liutkeviciene, Rasa

Subjects

MACULAR degeneration, ENDOTHELIAL growth factors, TREATMENT effectiveness, CYTOTOXIC T lymphocyte-associated molecule-4, OLDER people

Abstract

Background: Age-related macular degeneration (AMD) is a major global health problem as it is the leading cause of irreversible loss of central vision in the aging population. Av-vascular endothelial growth factor (anti-VEGF) therapies have been shown to be effective, but they do not respond optimally to all patients. Objective. This study investigates the genetic factors associated with susceptibility to AMD and response to treatment, focusing on key polymorphisms in the CFH (rs1061170, rs1410996) and KDR (rs2071559, rs1870377) genes and the association of CFH and KDR serum levels in patients with AMD. Results. A cohort of 255 patients with early AMD, 252 patients with exudative AMD, and 349 healthy controls underwent genotyping analysis, which revealed significant associations between CFH polymorphisms and the risk of exudative AMD. The CFH rs1061170 CC genotype was associated with an increased risk of early AMD (p = 0.046). For exudative AMD, the CFH rs1061170 TC + CC genotype increased odds (p < 0.001), while the rs1410996 GA + AA genotype decreased odds (p < 0.001). Haplotypes of CFH SNPs were associated with decreased odds of AMD. In terms of response to treatment, none of the SNPs were associated with the response to anti-VEGF treatment. We also found that both early and exudative AMD patients had lower CFH serum levels compared to the control group (p = 0.038 and p = 0.006, respectively). Exudative AMD patients with the CT genotype of CFH rs1061170 had lower CFH serum levels compared to the control group (p = 0.035). Exudative AMD patients with the GG genotype of CFH rs1410996 also had lower CFH serum levels compared to the control group (p = 0.021). Conclusions. CFH polymorphisms influence susceptibility to AMD but do not correlate with a response to anti-VEGF therapy. Further research is imperative to fully evaluate the developmental significance, treatment efficacy, and predictive role in influencing susceptibility to anti-VEGF therapy for KDR and CFH. [ABSTRACT FROM AUTHOR]

Published

2024

7. Impact of genomic and epigenomic alterations of multigene on a multicancer pedigree

Author

Jingyu Gao, Yongzhang Wu, Jieming Yu, Yinbin Qiu, Tiantian Yi, Chaochao Luo, Junxiao Zhang, Gary Lu, Xu Li, Fu Xiong, Xuedong Wu, and Xinghua Pan

Subjects

CFH, DNA methylation, DNAH11, familial cancer syndromes, germline mutations, somatic mutation, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Germline mutations have been identified in a small number of hereditary cancers, but the genetic predisposition for many familial cancers remains to be elucidated. Methods This study identified a Chinese pedigree that presented different cancers (breast cancer, BRCA; adenocarcinoma of the esophagogastric junction, AEG; and B‐cell acute lymphoblastic leukemia, B‐ALL) in each of the three generations. Whole‐genome sequencing and whole‐exome sequencing were performed on peripheral blood or bone marrow and cancer biopsy samples. Whole‐genome bisulfite sequencing was conducted on the monozygotic twin brothers, one of whom developed B‐ALL. Results According to the ACMG guidelines, bioinformatic analysis of the genome sequencing revealed 20 germline mutations, particularly mutations in the DNAH11 (c.9463G > A) and CFH (c.2314G > A) genes that were documented in the COSMIC database and validated by Sanger sequencing. Forty‐one common somatic mutated genes were identified in the cancer samples, displaying the same type of single nucleotide substitution Signature 5. Meanwhile, hypomethylation of PLEK2, MRAS, and RXRA as well as hypermethylation of CpG island associated with WT1 was shown in the twin with B‐ALL. Conclusions These findings reveal genomic alterations in a pedigree with multiple cancers. Mutations found in the DNAH11, CFH genes, and other genes predispose to malignancies in this family. Dysregulated methylation of WT1, PLEK2, MRAS, and RXRA in the twin with B‐ALL increases cancer susceptibility. The similarity of the somatic genetic changes among the three cancers indicates a hereditary impact on the pedigree. These familial cancers with germline and somatic mutations, as well as epigenomic alterations, represent a common molecular basis for many multiple cancer pedigrees.

Published

2024

8. Association of KDR (rs2071559, rs1870377), CFH (rs1061170, rs1410996) genes variants and serum levels with pituitary adenoma.

Author

Bruzaite, Akvile, Gedvilaite, Greta, Kriauciuniene, Loresa, and Liutkeviciene, Rasa

Subjects

*PITUITARY tumors, *GENETIC variation, *TUMOR growth, *BENIGN tumors, *ORGANS (Anatomy)

Abstract

Introduction: Pituitary adenomas (PA) are slow‐growing, benign tumors that usually do not metastasize to other body organs. Although they are referred to as benign, tumor growth can eventually put pressure on nearby structures, spread to surrounding tissues, and cause symptoms. The exact cause of PA is unknown, and the pathogenesis is multifactorial. Methods: Our study included PA patients and healthy volunteers. Genomic DNA was extracted using the DNA salting‐out method. All participants were genotyped for the KDR rs2071559, rs1870377, CFH rs1061170, and rs1410996 polymorphisms. Serum levels of KDR and CFH were examined using the ELISA method. Results: The results of the present study showed that KDR rs2071559 A allele was associated with the occurrence of PA, hormonally active PA, invasive PA, and PA without recurrence development. KDR rs1870377 increased the probability of invasive PA and PA recurrence. CFH rs1061170 C allele was associated with hormonally active PA and the T allele was associated with non‐invasive PA development. Conclusion: KDR rs2071559, rs1870377, and CFH rs1061170 could be potential biomarkers associated with PA. [ABSTRACT FROM AUTHOR]

Published

2024

9. Moss-produced human complement factor H with modified glycans has an extended half-life and improved biological activity

Author

Todor Tschongov, Swagata Konwar, Andreas Busch, Christian Sievert, Andrea Hartmann, Marina Noris, Sara Gastoldi, Sistiana Aiello, Andreas Schaaf, Jens Panse, Peter F. Zipfel, Paulina Dabrowska-Schlepp, and Karsten Häffner

Subjects

recombinant factor H, C3 glomerulopathy, complement-associated disease, CPV-104, CFH, complement, Immunologic diseases. Allergy, RC581-607

Abstract

Most drugs that target the complement system are designed to inhibit the complement pathway at either the proximal or terminal levels. The use of a natural complement regulator such as factor H (FH) could provide a superior treatment option by restoring the balance of an overactive complement system while preserving its normal physiological functions. Until now, the systemic treatment of complement-associated disorders with FH has been deemed unfeasible, primarily due to high production costs, risks related to FH purified from donors’ blood, and the challenging expression of recombinant FH in different host systems. We recently demonstrated that a moss-based expression system can produce high yields of properly folded, fully functional, recombinant FH. However, the half-life of the initial variant (CPV-101) was relatively short. Here we show that the same polypeptide with modified glycosylation (CPV-104) achieves a pharmacokinetic profile comparable to that of native FH derived from human serum. The treatment of FH-deficient mice with CPV-104 significantly improved important efficacy parameters such as the normalization of serum C3 levels and the rapid degradation of C3 deposits in the kidney compared to treatment with CPV-101. Furthermore, CPV-104 showed comparable functionality to serum-derived FH in vitro, as well as similar performance in ex vivo assays involving samples from patients with atypical hemolytic uremic syndrome, C3 glomerulopathy and paroxysomal nocturnal hematuria. CPV-104 – the human FH analog expressed in moss – will therefore allow the treatment of complement-associated human diseases by rebalancing instead of inhibiting the complement cascade.

Published

2024

10. Identification of CFH and FHL2 as biomarkers for idiopathic pulmonary fibrosis

Author

Xingchen Liu, Meng Yang, Jiayu Li, Hangxu Liu, Yuchao Dong, Jianming Zheng, and Yi Huang

Subjects

CFH, FHL2, biomarker, IPF, machine-learning strategies, Medicine (General), R5-920

Abstract

BackgroundIdiopathic pulmonary fibrosis (IPF) is a fatal disease of unknown etiology with a poor prognosis, characterized by a lack of effective diagnostic and therapeutic interventions. The role of immunity in the pathogenesis of IPF is significant, yet remains inadequately understood. This study aimed to identify potential key genes in IPF and their relationship with immune cells by integrated bioinformatics analysis and verify by in vivo and in vitro experiments.MethodsGene microarray data were obtained from the Gene Expression Omnibus (GEO) for differential expression analysis. The differentially expressed genes (DEGs) were identified and subjected to functional enrichment analysis. By utilizing a combination of three machine learning algorithms, specific genes associated with idiopathic pulmonary fibrosis (IPF) were pinpointed. Then their diagnostic significance and potential co-regulators were elucidated. We further analyzed the correlation between key genes and immune infiltrating cells via single-sample gene set enrichment analysis (ssGSEA). Subsequently, a single-cell RNA sequencing data (scRNA-seq) was used to explore which cell types expressed key genes in IPF samples. Finally, a series of in vivo and in vitro experiments were conducted to validate the expression of candidate genes by western blot (WB), quantitative real-time PCR (qRT-PCR), and immunohistochemistry (IHC) analysis.ResultsA total of 647 DEGs of IPF were identified based on two datasets, including 225 downregulated genes and 422 upregulated genes. They are closely related to biological functions such as cell migration, structural organization, immune cell chemotaxis, and extracellular matrix. CFH and FHL2 were identified as key genes with diagnostic accuracy for IPF by three machine learning algorithms. Analysis using ssGSEA revealed a significant association of both CFH and FHL2 with diverse immune cells, such as B cells and NK cells. Further scRNA-seq analysis indicated CFH and FHL2 were specifically upregulated in human IPF tissues, which was confirmed by in vitro and in vivo experiments.ConclusionIn this study, CFH and FHL2 have been identified as novel potential biomarkers for IPF, with potential diagnostic utility in future clinical applications. Subsequent investigations into the functions of these genes in IPF and their interactions with immune cells may enhance comprehension of the disease’s pathogenesis and facilitate the identification of therapeutic targets.

Published

2024

11. Underlying Genetics of aHUS: Which Connection with Outcome and Treatment Discontinuation?

Author

Spasiano, Andrea, Palazzetti, Daniela, Dimartino, Lucrezia, Bruno, Francesca, Baccaro, Rocco, Pesce, Francesco, and Grandaliano, Giuseppe

Subjects

*HEMOLYTIC-uremic syndrome, *GENETICS, *TERMINATION of treatment, *THROMBOTIC microangiopathies, *CHRONIC kidney failure, *POLYCYSTIC kidney disease

Abstract

Atypical hemolytic uremic syndrome (aHUS) is a rare disease caused by a genetic dysregulation of the alternative complement pathway, characterized by thrombocytopenia, hemolytic anemia, and acute kidney injury, and included in the group of thrombotic microangiopathies. With the introduction of humanized monoclonal antibodies that inhibit C5 activation, the natural history of aHUS completely changed, with a better prognosis, a quick recovery of renal function, and a significant reduction of end-stage renal disease incidence. Nowadays, there is an increasing interest in the molecular and genetic bases of this severe disease. The aim of this narrative review is to provide readers with a practical guide about different possible involved genes, elucidating the specific role of each transcribed protein in the pathogenesis of aHUS. Moreover, we analyzed the main current evidence about the relationship among genetic mutations, outcomes, and the risk of recurrence of this manifold disease. [ABSTRACT FROM AUTHOR]

Published

2023

12. On the signatures of local and regional dynamics in the distribution of lower stratospheric water vapour over Indian region using balloon-borne and satellite observations.

Author

Emmanuel, Maria, Sunilkumar, S. V., Satheesh Chandran, P. R., and Muhsin, M.

Subjects

*WATER vapor, *ATMOSPHERIC water vapor measurement, *MAGNETIC recorders & recording, *TROPOPAUSE, *STRATOSPHERE, *MONSOONS

Abstract

Balloon-borne cryogenic frost-point hygrometer (CFH) observations over two tropical stations Trivandrum (8.53° N, 76.87° E) and Hyderabad (17.47° N, 78.58° E) [2014–2017] along with Microwave Limb Sounder (MLS) observations [2011–2017] are used to examine the signatures of local and regional dynamics in the distribution of lower stratospheric water vapour over the Indian region. The column-integrated water vapour in the lower stratosphere (IWVLS) varies in the range 2.5–5 g/m2 with low values during winter and high values during summer monsoon and post monsoon seasons. About 50–75% of IWVLS lies in the lower regime of the lower stratosphere, the region from cold point tropopause (CPT) to 21 km (LS1). Hygropause is very near to the CPT in winter and pre-monsoon and 2–3 km above the CPT in summer-monsoon and post-monsoon. The CPT and the minimum in saturated mixing ratio (SMRmin) altitudes show a positive correlation, with SMRmin mostly occurring below the CPT. Though water vapour mixing ratio (WVMR) at CPT increases with increase in SMRmin, it is mostly less than the corresponding SMRmin value. CFH observations showed that the tape recorder signal in the LS1 is disturbed by the local/regional dynamics. While the amount of water vapour entering the lower stratosphere is higher over Hyderabad in winter and summer monsoon, it is higher over Trivandrum in the other two seasons. Hydration at the tropopause level is mainly determined by the overshooting/deep convection, monsoon dynamics and horizontal transport and dehydration is determined by temperature variations in the tropical tropopause layer (TTL). [ABSTRACT FROM AUTHOR]

Published

2023

13. CFH (rs1061170, rs1410996), KDR (rs2071559, rs1870377) and KDR and CFH Serum Levels in AMD Development and Treatment Efficacy

Author

Dzastina Cebatoriene, Alvita Vilkeviciute, Greta Gedvilaite, Akvile Bruzaite, Loresa Kriauciuniene, Dalia Zaliuniene, and Rasa Liutkeviciene

Subjects

age-related macular degeneration, gene polymorphisms KDR, CFH, ELISA, anti-VEGF therapy, Biology (General), QH301-705.5

Abstract

Background: Age-related macular degeneration (AMD) is a major global health problem as it is the leading cause of irreversible loss of central vision in the aging population. Av-vascular endothelial growth factor (anti-VEGF) therapies have been shown to be effective, but they do not respond optimally to all patients. Objective. This study investigates the genetic factors associated with susceptibility to AMD and response to treatment, focusing on key polymorphisms in the CFH (rs1061170, rs1410996) and KDR (rs2071559, rs1870377) genes and the association of CFH and KDR serum levels in patients with AMD. Results. A cohort of 255 patients with early AMD, 252 patients with exudative AMD, and 349 healthy controls underwent genotyping analysis, which revealed significant associations between CFH polymorphisms and the risk of exudative AMD. The CFH rs1061170 CC genotype was associated with an increased risk of early AMD (p = 0.046). For exudative AMD, the CFH rs1061170 TC + CC genotype increased odds (p < 0.001), while the rs1410996 GA + AA genotype decreased odds (p < 0.001). Haplotypes of CFH SNPs were associated with decreased odds of AMD. In terms of response to treatment, none of the SNPs were associated with the response to anti-VEGF treatment. We also found that both early and exudative AMD patients had lower CFH serum levels compared to the control group (p = 0.038 and p = 0.006, respectively). Exudative AMD patients with the CT genotype of CFH rs1061170 had lower CFH serum levels compared to the control group (p = 0.035). Exudative AMD patients with the GG genotype of CFH rs1410996 also had lower CFH serum levels compared to the control group (p = 0.021). Conclusions. CFH polymorphisms influence susceptibility to AMD but do not correlate with a response to anti-VEGF therapy. Further research is imperative to fully evaluate the developmental significance, treatment efficacy, and predictive role in influencing susceptibility to anti-VEGF therapy for KDR and CFH.

Published

2024

14. Exogenous CFH Modulates Levels of Pro-Inflammatory Mediators to Prevent Oxidative Damage of Retinal Pigment Epithelial Cells with the At-Risk CFH Y402H Variant.

Author

Velazquez-Soto, Henry, Groman-Lupa, Sergio, Cruz-Aguilar, Marisa, Salazar, Alberto L., Zenteno, Juan C., and Jimenez-Martinez, Maria C.

Subjects

RHODOPSIN, CHROMATOPHORES, MACULAR degeneration, COMPLEMENT factor H, EPITHELIAL cells, OXIDATIVE stress

Abstract

Age-related macular degeneration (AMD) is a complex, progressive degenerative retinal disease. Retinal pigment epithelial (RPE) cells play an important role in the immune defense of the eye and their dysfunction leads to the progressive irreversible degeneration of photoreceptors. Genetic factors, chronic inflammation, and oxidative stress have been implicated in AMD pathogenesis. Oxidative stress causes RPE injury, resulting in a chronic inflammatory response and cell death. The Y402H polymorphism in the complement factor H (CFH) protein is an important risk factor for AMD. However, the functional significance of CFH Y402H polymorphism remains unclear. In the present study, we investigated the role of CFH in the pro-inflammatory response using an in vitro model of oxidative stress in the RPE with the at-risk CFH Y402H variant. ARPE-19 cells with the at-risk CFH Y402H variant were highly susceptible to damage caused by oxidative stress, with increased levels of inflammatory mediators and pro-apoptotic factors that lead to cell death. Pretreatment of the ARPE-19 cell cultures with exogenous CFH prior to the induction of oxidative stress prevented damage and cell death. This protective effect may be related to the negative regulation of pro-inflammatory cytokines. CFH contributes to cell homeostasis and is required to modulate the pro-inflammatory cytokine response under oxidative stress in the ARPE-19 cells with the at-risk CFH Y402H variant. [ABSTRACT FROM AUTHOR]

Published

2023

15. Complement biomarkers reflect the pathological status of neuromyelitis optica spectrum disorders.

Author

Katsuichi Miyamoto, Mai Minamino, Motoi Kuwahara, Hiroshi Tsujimoto, Katsuki Ohtani, Nobutaka Wakamiya, Kei-ichi Katayama, Norimitsu Inoue, and Hidefumi Ito

Subjects

NEUROMYELITIS optica, COMPLEMENT factor H, MYASTHENIA gravis, GUILLAIN-Barre syndrome, BIOMARKERS, COMPLEMENT activation

Abstract

Complement is involved in the pathogenesis of neuroimmune disease, but the detailed pathological roles of the complement pathway remain incompletely understood. Recently, eculizumab, a humanized anti-C5 monoclonal antibody, has been clinically applied against neuroimmune diseases such as myasthenia gravis and neuromyelitis optica spectrum disorders (NMOSD). Clinical application of eculizumab is also being investigated for another neuroimmune disease, Guillain-Barre' syndrome (GBS). However, while the effectiveness of eculizumab for NMOSD is extremely high in many cases, there are some cases of myasthenia gravis and GBS in which eculizumab has little or no efficacy. Development of effective biomarkers that reflect complement activation in these diseases is therefore important. To identify biomarkers that could predict disease status, we retrospectively analyzed serum levels of complement factors in 21 patients with NMOSD and 25 patients with GBS. Ba, an activation marker of the alternative complement pathway, was elevated in the acute phases of both NMOSD and GBS. Meanwhile, sC5b-9, an activation marker generated by the terminal complement pathway, was elevated in NMOSD but not in GBS. Complement factor H (CFH), a complement regulatory factor, was decreased in the acute phase as well as in the remission phase of NMOSD, but not in any phases of GBS. Together, these findings suggest that complement biomarkers, such as Ba, sC5b-9 and CFH in peripheral blood, have potential utility in understanding the pathological status of NMOSD. [ABSTRACT FROM AUTHOR]

Published

2023

16. Two Different Presentation of C3 Glomerulonephritis Treated with Eculizumab: Two Cases and Brief Overview.

Author

Öztürk, Yasin, Özer, Hakan, Baloğlu, İsmail, and Türkmen, Kültigin

Subjects

*COMPLEMENT factor H, *ECULIZUMAB, *GLOMERULONEPHRITIS, *KIDNEY glomerulus diseases, *KIDNEY failure

Abstract

C3 glomerulopathy is a newly defined glomerular disease dominated by C3 complement storage and uncertain C1, C4, and immunoglobin accumulations. Hereditary mutations associated with Complement Factor H (CFH) causing hyperactivation of the alternative complement pathway were identified. Most mutations associated with C3 glomerulopathy are associated with the N-terminal end. Whether mutations are pathogenic or not will direct diagnosis and treatment. We present 2 cases, one 61-year-old and one 24-year-old attending our clinic at different times with hematuria, proteinuria, edema, and kidney failure. Both patients had C3 glomerulopathy diagnosed based on the results of kidney biopsy and were treated with eculizumab. Both cases had CFH-associated mutations. [ABSTRACT FROM AUTHOR]

Published

2023

17. Underlying Genetics of aHUS: Which Connection with Outcome and Treatment Discontinuation?

Author

Andrea Spasiano, Daniela Palazzetti, Lucrezia Dimartino, Francesca Bruno, Rocco Baccaro, Francesco Pesce, and Giuseppe Grandaliano

Subjects

atypical hemolytic uremic syndrome, genetics, aHUS, CFH, MCP, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Atypical hemolytic uremic syndrome (aHUS) is a rare disease caused by a genetic dysregulation of the alternative complement pathway, characterized by thrombocytopenia, hemolytic anemia, and acute kidney injury, and included in the group of thrombotic microangiopathies. With the introduction of humanized monoclonal antibodies that inhibit C5 activation, the natural history of aHUS completely changed, with a better prognosis, a quick recovery of renal function, and a significant reduction of end-stage renal disease incidence. Nowadays, there is an increasing interest in the molecular and genetic bases of this severe disease. The aim of this narrative review is to provide readers with a practical guide about different possible involved genes, elucidating the specific role of each transcribed protein in the pathogenesis of aHUS. Moreover, we analyzed the main current evidence about the relationship among genetic mutations, outcomes, and the risk of recurrence of this manifold disease.

Published

2023

18. Genetic analysis of CFH and MCP in Egyptian patients with immune-complex proliferative glomerulonephritis.

Author

Gouda, Heba R., Talaat, Iman M., Bouzid, Amal, El-Assi, Hoda, Nabil, Amira, Venkatachalam, Thenmozhi, Bhamidimarri, Poorna Manasa, Wohlers, Inken, Mahdami, Amena, EL-Gendi, Saba, ElKoraie, Ahmed, Busch, Hauke, Saber-Ayad, Maha, Hamoudi, Rifat, and Baddour, Nahed

Subjects

EGYPTIANS, GLOMERULONEPHRITIS, LUPUS nephritis, GENETIC variation, DNA sequencing, NEPHRITIS, AUTOIMMUNE diseases

Abstract

Glomerulonephritis (GN) is a complex disease with intricate underlying pathogenic mechanisms. The possible role of underlying complement dysregulation is not fully elucidated in some GN subsets, especially in the setting of autoimmunity or infection. In the current study, diagnosed cases of lupus nephritis (LN) and post-infectious GN (PIGN) were recruited for molecular genetic analysis and targeted next-generation DNA sequencing was performed for two main complement regulating genes: in the fluid phase; CFH, and on tissue surfaces; MCP. Three heterozygous pathogenic variants in CFH (Q172*, W701*, and W1096*) and one likely pathogenic heterozygous variant in MCP (C223R) have been identified in four of the studied LN cases. Additionally, among the several detected variants of uncertain significance, one novel variant (CFH:F614S) was identified in 74% of the studied LN cases and in 65% of the studied PIGN cases. This variant was detected for the first time in the Egyptian population. These findings suggest that subtle mutations may be present in complement regulating genes in patients with immune-complex mediated category of GN that may add to the disease pathogenesis. These findings also call for further studies to delineate the impact of these gene variants on the protein function, the disease course, and outcome. [ABSTRACT FROM AUTHOR]

Published

2022

19. Variation in CFHR3 determines susceptibility to meningococcal disease by controlling factor H concentrations.

Author

Kumar, Vikrant, Pouw, Richard B., Autio, Matias I., Sagmeister, Manfred G., Phua, Zai Yang, Borghini, Lisa, Wright, Victoria J., Hoggart, Clive, Pan, Bangfen, Tan, Antson Kiat Yee, Binder, Alexander, Brouwer, Mieke C., Pinnock, Ellie, De Groot, Ronald, Hazelzet, Jan, Emonts, Marieke, Van Der Flier, Michiel, Reiter, Karl, Nöthen, Markus M., and Hoffmann, Per

Subjects

*DISEASE susceptibility, *COMPLEMENT factor H, *MENINGOCOCCAL infections, *NEISSERIA meningitidis, *PREVENTIVE medicine, *GENETIC variation

Abstract

Neisseria meningitidis protects itself from complement-mediated killing by binding complement factor H (FH). Previous studies associated susceptibility to meningococcal disease (MD) with variation in CFH , but the causal variants and underlying mechanism remained unknown. Here we attempted to define the association more accurately by sequencing the CFH - CFHR locus and imputing missing genotypes in previously obtained GWAS datasets of MD-affected individuals of European ancestry and matched controls. We identified a CFHR3 SNP that provides protection from MD (rs75703017, p value = 1.1 × 10−16) by decreasing the concentration of FH in the blood (p value = 1.4 × 10−11). We subsequently used dual-luciferase studies and CRISPR gene editing to establish that deletion of rs75703017 increased FH expression in hepatocyte by preventing promotor inhibition. Our data suggest that reduced concentrations of FH in the blood confer protection from MD; with reduced access to FH, N. meningitidis is less able to shield itself from complement-mediated killing. Neisseria meningitidis evades complement-mediated clearance by hijacking host complement regulator factor H (FH). Kumar et al. investigate the genetic variations in the CFH locus associating with meningococcal disease. A regulatory region in the adjacent CFHR3 gene controls CFH expression, thereby determining FH plasma amounts and susceptibility towards meningococcal disease. [ABSTRACT FROM AUTHOR]

Published

2022

20. Complement or insult: the emerging link between complement cascade deficiencies and pathology of myeloid malignancies.

Author

Oakes A, Liu Y, and Dubielecka PM

Subjects

Humans, Animals, Hematologic Neoplasms pathology, Hematologic Neoplasms immunology, Inflammation pathology, Inflammation immunology, Myeloproliferative Disorders immunology, Myeloproliferative Disorders pathology, Myeloproliferative Disorders etiology, Complement System Proteins immunology, Complement System Proteins metabolism, Complement Activation immunology

Abstract

The complement cascade is an ancient and highly conserved arm of the immune system. The accumulating evidence highlights elevated activity of the complement cascade in cancer microenvironment and emphasizes its effects on the immune, cancer, and cancer stroma cells, pointing to a role in inflammation-mediated etiology of neoplasms. The role the cascade plays in development, progression, and relapse of solid tumors is increasingly recognized, however its role in hematological malignancies, especially those of myeloid origin, has not been thoroughly assessed and remains obscure. As the role of inflammation and autoimmunity in development of myeloid malignancies is becoming recognized, in this review we focus on summarizing the links that have been identified so far for complement cascade involvement in the pathobiology of myeloid malignancies. Complement deficiencies are primary immunodeficiencies that cause an array of clinical outcomes including an increased risk of a range of infectious as well as local or systemic inflammatory and thrombotic conditions. Here, we discuss the impact that deficiencies in complement cascade initiators, mid- and terminal-components and inhibitors have on the biology of myeloid neoplasms. The emergent conclusions indicate that the links between complement cascade, inflammatory signaling, and the homeostasis of hematopoietic system exist, and efforts should continue to detail the mechanistic involvement of complement cascade in the development and progression of myeloid cancers., Competing Interests: Conflict of interest statement. None declared., (© The Author(s) 2024. Published by Oxford University Press on behalf of Society for Leukocyte Biology. All rights reserved. For commercial re-use, please contact reprints@oup.com for reprints and translation rights for reprints. All other permissions can be obtained through our RightsLink service via the Permissions link on the article page on our site—for further information please contact journals.permissions@oup.com.)

Published

2024

21. Genetic analysis of CFH and MCP in Egyptian patients with immune-complex proliferative glomerulonephritis

Author

Heba R. Gouda, Iman M. Talaat, Amal Bouzid, Hoda El-Assi, Amira Nabil, Thenmozhi Venkatachalam, Poorna Manasa Bhamidimarri, Inken Wohlers, Amena Mahdami, Saba EL-Gendi, Ahmed ElKoraie, Hauke Busch, Maha Saber-Ayad, Rifat Hamoudi, and Nahed Baddour

Subjects

complement system, glomerulonephritis, CFH, MCP, lupus nephritis, post-infectious glomerulonephritis, Immunologic diseases. Allergy, RC581-607

Abstract

Glomerulonephritis (GN) is a complex disease with intricate underlying pathogenic mechanisms. The possible role of underlying complement dysregulation is not fully elucidated in some GN subsets, especially in the setting of autoimmunity or infection. In the current study, diagnosed cases of lupus nephritis (LN) and post-infectious GN (PIGN) were recruited for molecular genetic analysis and targeted next-generation DNA sequencing was performed for two main complement regulating genes: in the fluid phase; CFH, and on tissue surfaces; MCP. Three heterozygous pathogenic variants in CFH (Q172*, W701*, and W1096*) and one likely pathogenic heterozygous variant in MCP (C223R) have been identified in four of the studied LN cases. Additionally, among the several detected variants of uncertain significance, one novel variant (CFH:F614S) was identified in 74% of the studied LN cases and in 65% of the studied PIGN cases. This variant was detected for the first time in the Egyptian population. These findings suggest that subtle mutations may be present in complement regulating genes in patients with immune-complex mediated category of GN that may add to the disease pathogenesis. These findings also call for further studies to delineate the impact of these gene variants on the protein function, the disease course, and outcome.

Published

2022

22. Exogenous CFH Modulates Levels of Pro-Inflammatory Mediators to Prevent Oxidative Damage of Retinal Pigment Epithelial Cells with the At-Risk CFH Y402H Variant

Author

Henry Velazquez-Soto, Sergio Groman-Lupa, Marisa Cruz-Aguilar, Alberto L. Salazar, Juan C. Zenteno, and Maria C. Jimenez-Martinez

Subjects

CFH, RPE, oxidative stress, AMD, cytokines, cell death, Therapeutics. Pharmacology, RM1-950

Abstract

Age-related macular degeneration (AMD) is a complex, progressive degenerative retinal disease. Retinal pigment epithelial (RPE) cells play an important role in the immune defense of the eye and their dysfunction leads to the progressive irreversible degeneration of photoreceptors. Genetic factors, chronic inflammation, and oxidative stress have been implicated in AMD pathogenesis. Oxidative stress causes RPE injury, resulting in a chronic inflammatory response and cell death. The Y402H polymorphism in the complement factor H (CFH) protein is an important risk factor for AMD. However, the functional significance of CFH Y402H polymorphism remains unclear. In the present study, we investigated the role of CFH in the pro-inflammatory response using an in vitro model of oxidative stress in the RPE with the at-risk CFH Y402H variant. ARPE-19 cells with the at-risk CFH Y402H variant were highly susceptible to damage caused by oxidative stress, with increased levels of inflammatory mediators and pro-apoptotic factors that lead to cell death. Pretreatment of the ARPE-19 cell cultures with exogenous CFH prior to the induction of oxidative stress prevented damage and cell death. This protective effect may be related to the negative regulation of pro-inflammatory cytokines. CFH contributes to cell homeostasis and is required to modulate the pro-inflammatory cytokine response under oxidative stress in the ARPE-19 cells with the at-risk CFH Y402H variant.

Published

2023

23. Molecular Genetic Mechanisms in Age-Related Macular Degeneration.

Author

Shughoury, Aumer, Sevgi, Duriye Damla, and Ciulla, Thomas A.

Subjects

*MACULAR degeneration, *MOLECULAR genetics, *LIPID metabolism, *GENETIC variation, *TOBACCO use, *LOCUS (Genetics), *COMPLEMENT activation

Abstract

Age-related macular degeneration (AMD) is among the leading causes of irreversible blindness worldwide. In addition to environmental risk factors, such as tobacco use and diet, genetic background has long been established as a major risk factor for the development of AMD. However, our ability to predict disease risk and personalize treatment remains limited by our nascent understanding of the molecular mechanisms underlying AMD pathogenesis. Research into the molecular genetics of AMD over the past two decades has uncovered 52 independent gene variants and 34 independent loci that are implicated in the development of AMD, accounting for over half of the genetic risk. This research has helped delineate at least five major pathways that may be disrupted in the pathogenesis of AMD: the complement system, extracellular matrix remodeling, lipid metabolism, angiogenesis, and oxidative stress response. This review surveys our current understanding of each of these disease mechanisms, in turn, along with their associated pathogenic gene variants. Continued research into the molecular genetics of AMD holds great promise for the development of precision-targeted, personalized therapies that bring us closer to a cure for this debilitating disease. [ABSTRACT FROM AUTHOR]

Published

2022

24. Age-Related Maculopathy Susceptibility 2 and Complement Factor H Polymorphism and Intraocular Complement Activation in Neovascular Age-Related Macular Degeneration

Author

Yutaka Kato, MD, Yasuharu Oguchi, MD, PhD, Tomoko Omori, PhD, Akihito Kasai, MD, Masashi Ogasawara, MD, Yukinori Sugano, MD, PhD, Kanako Itagaki, MD, Akira Ojima, MD, PhD, Yumi Ishida, Takeshi Machida, PhD, Hideharu Sekine, MD, PhD, and Tetsuju Sekiryu, MD, PhD

Subjects

Aqueous humor, ARMS2, CFH, C3a, C4a, C5a, Ophthalmology, RE1-994

Abstract

Purpose: To investigate the association of risk alleles in complement factor H (CFH) and age-related maculopathy susceptibility 2 (ARMS2) with complement activation products in the aqueous humor in eyes with neovascular age-related macular degeneration (nAMD) including polypoidal choroidal vasculopathy (PCV), retinal angiomatous proliferation (RAP), and pachychoroid neovasculopathy (PNV). Design: Prospective, comparative, observational study. Participants: Treatment-naïve patients with nAMD and cataract patients as controls. Methods: The study included 236 eyes of 236 patients with nAMD and 49 control eyes of 49 patients. Aqueous humor samples were collected from 67 eyes with drusen-associated nAMD, 72 eyes with PCV, 26 eyes with RAP, and 71 eyes with PNV before intravitreal anti-VEGF injection and cataract surgery in the 49 control eyes. Clinical samples were measured for complement component 3a (C3a), C4a, and C5a using a bead-based immunoassay. Genotyping of the ARMS2 A69S (rs10490924), CFH I62V (rs800292), and CFH Y402H (rs1061170) was performed using TaqMan genotyping. Main Outcome Measures: The levels of complement activation products (C3a, C4a, and C5a) in the aqueous humor in each genotype of ARMS2 and CFH. Results: The C3a level in the aqueous humor was significantly elevated (P = 0.006) in patients with nAMD and the ARMS2 A69S risk allele, whereas the levels of the complement activation products were not associated with CFH I62V and Y402H genotypes. Among the control eyes, no significant differences were seen in any complement activation products for all genetic polymorphisms. The levels of the complement activation products in the aqueous humor of eyes with the nAMD subtypes for each genetic polymorphism did not show significant differences. Conclusions: The C3a concentration in the aqueous humor was significantly higher in Japanese nAMD patients with the ARMS2 A69S risk allele, whereas it was not elevated in the patients with CFH I62V. Age-related maculopathy susceptibility 2 A69S polymorphism is strongly associated with local complement activation in nAMD patients.

Published

2022

25. Associations of ARMS2 and CFH Gene Polymorphisms with Neovascular Age-Related Macular Degeneration

Author

Supanji S, Romdhoniyyah DF, Sasongko MB, Agni AN, Wardhana FS, Widayanti TW, Prayogo ME, Perdamaian ABI, Dianratri A, Kawaichi M, and Oka C

Subjects

age-related macular degeneration, arms2, cfh, polymorphism, Ophthalmology, RE1-994

Abstract

Supanji Supanji,1– 4 Dewi Fathin Romdhoniyyah,1,2 Muhammad Bayu Sasongko,1,2,4 Angela Nurini Agni,1,2,4 Firman Setya Wardhana,1,2,4 Tri Wahyu Widayanti,1,2,4 Muhammad Eko Prayogo,1,2,4 Ayudha Bahana Ilham Perdamaian,1,2 Aninditta Dianratri,1,2 Masashi Kawaichi,5 Chio Oka5 1Department of Ophthalmology, Faculty of Medicine, Public Health and Nursing, Universitas Gadjah Mada, Yogyakarta, Indonesia; 2Department of Ophthalmology, Dr. Sardjito General Hospital, Yogyakarta, Indonesia; 3Ophthalmology Clinic, Military Air Force Central Hospital Dr. Suhardi Hardjolukito, Yogyakarta, Indonesia; 4Ophthalmology Clinic, Dr YAP Eye Hospital, Yogyakarta, Indonesia; 5Laboratory of Gene Function in Animals, Nara Institute of Science and Technology, Ikoma, Nara, JapanCorrespondence: Supanji SupanjiDepartment of Ophthalmology, Faculty of Medicine, Public Health and Nursing, Universitas Gadjah Mada, Jalan Farmako Sekip Utara, Yogyakarta, 55281, IndonesiaTel +62 274 560300Fax +62 274 581 876Email supanji@ugm.ac.idPurpose: This study aimed to determine the association of ARMS2 A69S, ARMS2 del443ins54, and CFH Y402H polymorphisms with neovascular age-related macular degeneration (nAMD) for the first time in an Indonesian population.Patients and Methods: Our case–control study involved 104 nAMD and 100 control subjects. AMD diagnosis was evaluated by retinal specialists based on color fundus photography and optical coherence tomography. The polymorphisms on CFH Y402H and ARMS2 A69S were analyzed by PCR-restriction fragment length polymorphism (PCR-RFLP), whereas ARMS2 del443ins54 was evaluated by PCR-based assay.Results: Significant allelic associations with nAMD were detected on all polymorphisms (P< 0.05), with stronger association with the ARMS2 A69S (OR 3.13; 95% CI 2.08– 4.71; P< 0.001) and ARMS2 del443ins54 (OR 3.28; 95% CI 2.17– 4.95; P< 0.001) polymorphisms than with CFH Y402H (OR 2.08; 95% CI 1.08– 3.99; P=0.028). Genotype analysis showed a statistical difference between nAMD and the control group for all polymorphisms (P< 0.05). However, the association with nAMD was weaker for CFH Y402H (P=0.043) than for ARMS2 A69S and ARMS2 del443ins54 (P< 0.001). A significant interaction between ARMS2 A69S and hypertension was documented (OR 9.53; 95% CI 3.61– 25.1; P< 0.001).Conclusion: Our findings indicate that ARMS2 A69S and ARMS2 del443ins54 polymorphisms are strongly associated with the risk of nAMD for the first time in an Indonesian population. The risk of nAMD increased when the presence of risk alleles from ARMS2 A69S was combined with the presence of hypertension.Keywords: age-related macular degeneration, ARMS2, CFH, polymorphism

Published

2021

26. Bioinformatic identification of differentially expressed genes regulated by DNA‐methylation in glioblastoma.

Author

Guan, Sizhong, Jian, Linge, He, Ye, Su, Yanna, and Zhou, Liping

Subjects

*GENE ontology, *GLIOBLASTOMA multiforme, *GENE expression profiling, *PROGNOSIS, *GENES, *DRUG target

Abstract

DNA methylation‐driven differentially expressed genes (DEGs) play potentially important roles in glioblastoma (GBM). In the present study, we applied bioinformatic analyses to identify key methylation‐regulated DEGs (MeDEGs) in glioblastoma and elucidate their functions. Gene expression and methylation profile data from glioblastoma samples along with clinical information were obtained from GEO and TCGA databases. A total of 65 genes were identified as MeDEGs from the aforementioned data. Subsequently, gene ontology and kyoto encyclopaedia of genes and genomes enrichment analyses of these MeDEGs exhibited that MeDEGs were mostly enriched in several tumour‐related terms such as 'activation of cysteine‐type endopeptidase activity involved in apoptotic process' and 'phospholipid scrambling'. Kaplan–Meier survival analysis demonstrated significant correlation of CASP1, CFH and TTLL7 hyper‐methylation with patient prognosis. Finally, CASP1 protein could indirectly interact with CFH protein, but interaction of TTLL7 protein with CASP1 or CFH protein was not evident. Based on gene set enrichment analysis, hyper‐methylation of CASP1, CFH and TTLL7 were found enriched in tumour‐related KEGG terms, such as 'RNA degradation', 'apyruvate metabolism' and 'nitrogen metabolism'. Methylation levels of CASP1, CFH and TTLL7 were addressed to negatively correlate with their mRNA levels in GBM cell lines. In sum, the present identification of MeDEGs associated with overall survival put forth potential molecular targets for translation towards improved diagnosis and treatment of GBM, and specifically, methylation levels of CASP1, CFH and TTLL7 genes could serve as key prognostic biomarkers in GBM. [ABSTRACT FROM AUTHOR]

Published

2022

27. Susceptible Single Nucleotide Polymorphisms in Exon 10 and Intron 9 of Complement Factor H Gene in Patients With Age-related Macular Degeneration

Author

Zahrasoheila Soheili, Hamid Ahmadieh, Siamak Moradian, Shahram Samiee, Narsis Daftarian, Samira Kheitan, Shamila D.Alipoor, Abouzar Bagheri, and Seyed Ghader Azizi

Subjects

amd, cfh, snp, exon10, intron 9, Medicine (General), R5-920

Abstract

Background: Age-related macular degeneration (AMD) is the leading cause of vision loss in the elderly. Although it has been shown that Y402H polymorphism in the CFH gene was strongly associated with AMD in the Iranian population, there were no data on other single nucleotide polymorphisms (SNPs), which have the most significant association with AMD. This study aimed to investigate hot point regions in exon 10 and intron 9. Materials and Methods: One hundred and sixty-six AMD patients and 69 controls were recruited. Their blood was collected in the tubes containing EDTA. Then, DNA was extracted from the blood, and its quality was evaluated. Primers were designed for intron 9 and exon10 sequencing. A viral polymorphisms analysis software named CEQ was used for the analysis of putative polymorphisms. Results: We noticed three polymorphisms in study cases: rs7535263 and C66379A in intron 9 and rs2274700 in exon 10. Based on the McNamara’s test (rs7535263 and rs2274700) and the Phi and Cramer’s test (C66379A), a significant difference was found between the control and patient groups regarding rs7535263 and rs2274700 polymorphisms. Conclusion: We found a synonymous or silent mutation, A473A, rs2274700 in exon 10 in 85% of patients. From two intronic SNPs, just rs7535263 showed association with the disease in studied patients living in Gilan Province, Iran. Although no significant relationship was found between controls and patients regarding the C66379A allele, it would be important that no other sources have reported C66379A polymorphism in AMD yet.

Published

2021

28. Association between circulatory complement activation and hypertensive renal damage: a case-control study.

Author

Wang Z, Zhang T, Wang X, Zhai J, He L, Ma S, Zuo Q, Zhang G, and Guo Y

Subjects

Humans, Male, Female, Middle Aged, Case-Control Studies, Risk Factors, Aged, Adult, Hypertension complications, Hypertension blood, Complement Activation, Essential Hypertension blood, Essential Hypertension complications, Essential Hypertension physiopathology, Logistic Models, Complement Pathway, Alternative, Disease Progression, Complement C3 metabolism, Complement C3 analysis, Complement Factor H

Abstract

Objective: The aim of this study was to investigate the potential importance of complement system activation, with particular emphasis on the complement alternative pathway (AP), in the pathogenesis of hypertensive renal damage., Methods: Serum complement C3, complement Factor H (CFH) and AP activation were assessed in 66 participants with established essential hypertension with renal damage (RD). Fifty-nine patients with age- and sex-matched essential hypertension without renal damage (NRD) and 58 healthy participants (normal) were selected., Results: Our study revealed that C3 and AP50 continuously increased from normal to NRD to RD ( p  < 0.05, respectively), while CFH was significantly lower than that in NRD and healthy participants ( p  < 0.05, respectively). After multifactorial logistic regression analysis corrected for confounders, elevated serum C3 ( p  = 0.001) and decreased CFH ( p  < 0.001) were found to be independent risk factors for hypertension in healthy participants; elevated serum C3 ( p  = 0.034), elevated AP50 ( p  < 0.001), decreased CFH ( p  < 0.001), increased age ( p  = 0.011) and increased BMI ( p  = 0.013) were found to be independent risk factors for the progression of hypertension to hypertensive renal damage; elevated serum C3 ( p  = 0.017), elevated AP50 ( p  = 0.023), decreased CFH ( p  = 0.005) and increased age ( p  = 0.041) were found to be independent risk factors for the development of hypertensive renal damage in healthy participants., Conclusion: Abnormal activation of complement, particularly complement AP, may be a risk factor for the development and progression of hypertensive renal damage.

Published

2024

29. Genetic factors associated with age‐related macular degeneration: identification of a novel PRPH2 single nucleotide polymorphism associated with increased risk of the disease.

Author

Ulańczyk, Zofia, Grabowicz, Aleksandra, Mozolewska‐Piotrowska, Katarzyna, Safranow, Krzysztof, Kawa, Miłosz Piotr, Pałucha, Andrzej, Krawczyk, Mariusz, Sikora, Piotr, Matczyńska, Ewa, Machaliński, Bogusław, and Machalińska, Anna

Subjects

*SINGLE nucleotide polymorphisms, *EYE diseases, *MACULAR degeneration, *NUCLEOTIDE sequencing, *PROTEIN structure

Abstract

Purpose: Age‐related macular degeneration (AMD) is associated with multiple environmental and genetic risk factors. Two main risk factors for AMD are variants in the CFH and ARMS2/HTRA1 genes. We investigated over 2000 variants in AMD patients and controls using high‐throughput sequencing methods to search for variants associated with AMD. Methods: A total of 296 AMD patients and 100 controls were enrolled in this study. Genetic analysis was performed with the Illumina NextSeq 500 system. Results: Multivariate analysis of patients and controls, adjusted for age, sex and smoking status (pack‐years), revealed that three SNPs were strong risk factors independently associated with AMD: CFH Y402H, ARMS A69S and PRPH2 c.582‐67T>A (rs3818086). The TC genotype in CFH Y402H was associated with 1.90‐fold higher odds, and the CC genotype was associated with 5.66‐fold higher odds of AMD compared with the TT genotype. The GT genotype in ARMS A69S was associated with 2.40‐fold higher odds, and the TT genotype was associated with 6.75‐fold higher odds of disease compared with the GG genotype. In the case of rs3818086, the A allele could be considered a 'risk' allele, since AA + TA genotypes were associated with 2.33‐fold higher odds of AMD compared with the TT genotype. Conclusions: Although PRPH2 mutations have been previously implicated in various forms of retinal degeneration, to the best of our knowledge, this study is the first to show that the rs3818086 variant increases the risk for AMD more than two times. Further studies on larger cohorts are required to elucidate how this variant affects protein structure. [ABSTRACT FROM AUTHOR]

Published

2021

30. Common haplotypes at the CFH locus and low-frequency variants in CFHR2 and CFHR5 associate with systemic FHR concentrations and age-related macular degeneration.

Author

Lorés-Motta, Laura, van Beek, Anna E., Willems, Esther, Zandstra, Judith, van Mierlo, Gerard, Einhaus, Alfred, Mary, Jean-Luc, Stucki, Corinne, Bakker, Bjorn, Hoyng, Carel B., Fauser, Sascha, Clark, Simon J., de Jonge, Marien I., Nogoceke, Everson, Koertvely, Elod, Jongerius, Ilse, Kuijpers, Taco W., and den Hollander, Anneke I.

Subjects

*MACULAR degeneration, *COMPLEMENT factor H, *GENOME-wide association studies, *GENETIC variation, *HAPLOTYPES

Abstract

Age-related macular degeneration (AMD) is the principal cause of blindness in the elderly population. A strong effect on AMD risk has been reported for genetic variants at the CFH locus, encompassing complement factor H (CFH) and the complement-factor-H-related (CFHR) genes, but the underlying mechanisms are not fully understood. We aimed to dissect the role of factor H (FH) and FH-related (FHR) proteins in AMD in a cohort of 202 controls and 216 individuals with AMD. We detected elevated systemic levels of FHR-1 (p = 1.84 × 10−6), FHR-2 (p = 1.47 × 10−4), FHR-3 (p = 1.05 × 10−5) and FHR-4A (p = 1.22 × 10−2) in AMD, whereas FH concentrations remained unchanged. Common AMD genetic variants and haplotypes at the CFH locus strongly associated with FHR protein concentrations (e.g., FH p.Tyr402His and FHR-2 concentrations, p = 3.68 × 10−17), whereas the association with FH concentrations was limited. Furthermore, in an International AMD Genomics Consortium cohort of 17,596 controls and 15,894 individuals with AMD, we found that low-frequency and rare protein-altering CFHR2 and CFHR5 variants associated with AMD independently of all previously reported genome-wide association study (GWAS) signals (p = 5.03 × 10−3 and p = 2.81 × 10−6, respectively). Low-frequency variants in CFHR2 and CFHR5 led to reduced or absent FHR-2 and FHR-5 concentrations (e.g., p.Cys72Tyr in CFHR2 and FHR-2, p = 2.46 × 10−16). Finally, we showed localization of FHR-2 and FHR-5 in the choriocapillaris and in drusen. Our study identifies FHR proteins as key proteins in the AMD disease mechanism. Consequently, therapies that modulate FHR proteins might be effective for treating or preventing progression of AMD. Such therapies could target specific individuals with AMD on the basis of their genotypes at the CFH locus. [ABSTRACT FROM AUTHOR]

Published

2021

31. Molecular and bioenergetic differences between cells with African versus European inherited mitochondrial DNA haplogroups: implications for population susceptibility to diseases.

Author

Chwa, Marilyn, Falatoonzadeh, Payam, Ramirez, Claudio, Malik, Deepika, Tarek, Mohamed, Del Carpio, Javier, Nesburn, Anthony, Boyer, David, Vawter, Marquis, Jazwinski, S, Miceli, Michael, Wallace, Douglas, Udar, Nitin, Kuppermann, Baruch, Kenney, Maria, and Atilano, Shari

Subjects

ABI, ARPE-19, ATP, Adenosine triphosphate, Applied Biosystems, C1s, C3, C4B, CFH, Carbonyl Cyanide 4-trifluoromethoxy-phenylhydrazone, Complement activation, Complement component 1, s subcomponent, Complement component 3, Complement component 4B, Complement factor H, Cybrid, DMEM, DNA, Deoxyribonucleic acid, Dulbeccos modified Eagles medium, ECAR, EDTA, ETC, Electron transport chain, Ethylenediaminetetracetic acid, Extracellular acidification rate, FCCP, Haplogroup, Innate immunity, MT-CO1, MT-CO2, MT-CO3, MT-CYB, MT-ND1, MT-ND3, MT-ND5, Maximal oxygen uptake, MicroMolar, Mitochondria encoded NADH dehydrogenase 1, Mitochondria encoded NADH dehydrogenase 3, Mitochondria encoded NADH dehydrogenase 5, Mitochondria encoded cytochrome B, Mitochondria encoded cytochrome oxidase 1, Mitochondria encoded cytochrome oxidase 2, Mitochondria encoded cytochrome oxidase 3, Mitochondrion, OCR, OXPHOS, Oxidative phosphorylation, Oxygen consumption rate, Q-PCR, Quantitative polymerase chain reaction, Retina, Retinal pigmented epithelium cell line, SEM, SNPs, Single nucleotide polymorphisms, Standard error mean, UCLA, University of California, Los Angeles, VO2(max), μM, Adenosine Triphosphate, Adult, Black People, Cell Line, Cell Proliferation, DNA, Mitochondrial, Energy Metabolism, Gene Dosage, Gene Expression Profiling, Genes, Mitochondrial, Genetic Predisposition to Disease, Haplotypes, Humans, Hybrid Cells, Lactates, Middle Aged, Oligonucleotide Array Sequence Analysis, Polymorphism, Single Nucleotide, Reactive Oxygen Species, Reverse Transcriptase Polymerase Chain Reaction, White People

Abstract

The geographic origins of populations can be identified by their maternally inherited mitochondrial DNA (mtDNA) haplogroups. This study compared human cybrids (cytoplasmic hybrids), which are cell lines with identical nuclei but mitochondria from different individuals with mtDNA from either the H haplogroup or L haplogroup backgrounds. The most common European haplogroup is H while individuals of maternal African origin are of the L haplogroup. Despite lower mtDNA copy numbers, L cybrids had higher expression levels for nine mtDNA-encoded respiratory complex genes, decreased ATP (adenosine triphosphate) turnover rates and lower levels of reactive oxygen species production, parameters which are consistent with more efficient oxidative phosphorylation. Surprisingly, GeneChip arrays showed that the L and H cybrids had major differences in expression of genes of the canonical complement system (5 genes), dermatan/chondroitin sulfate biosynthesis (5 genes) and CCR3 (chemokine, CC motif, receptor 3) signaling (9 genes). Quantitative nuclear gene expression studies confirmed that L cybrids had (a) lower expression levels of complement pathway and innate immunity genes and (b) increased levels of inflammation-related signaling genes, which are critical in human diseases. Our data support the hypothesis that mtDNA haplogroups representing populations from different geographic origins may play a role in differential susceptibilities to diseases.

Published

2014

32. Molecular and bioenergetic differences between cells with African versus European inherited mitochondrial DNA haplogroups: Implications for population susceptibility to diseases

Author

Kenney, M Cristina, Chwa, Marilyn, Atilano, Shari R, Falatoonzadeh, Payam, Ramirez, Claudio, Malik, Deepika, Tarek, Mohamed, Del Carpio, Javier Cáceres, Nesburn, Anthony B, Boyer, David S, Kuppermann, Baruch D, Vawter, Marquis P, Jazwinski, S Michal, Miceli, Michael V, Wallace, Douglas C, and Udar, Nitin

Subjects

Genetics, Aetiology, 1.1 Normal biological development and functioning, 2.1 Biological and endogenous factors, Underpinning research, Generic health relevance, Adenosine Triphosphate, Adult, Blacks, Cell Line, Cell Proliferation, DNA, Mitochondrial, Energy Metabolism, Gene Dosage, Gene Expression Profiling, Genes, Mitochondrial, Genetic Predisposition to Disease, Haplotypes, Humans, Hybrid Cells, Lactates, Middle Aged, Oligonucleotide Array Sequence Analysis, Polymorphism, Single Nucleotide, Reactive Oxygen Species, Reverse Transcriptase Polymerase Chain Reaction, Whites, Mitochondrion, Complement activation, Innate immunity, Haplogroup, Cybrid, Retina, White People, Black People, ABI, ARPE-19, ATP, Adenosine triphosphate, Applied Biosystems, C1s, C3, C4B, CFH, Carbonyl Cyanide 4-trifluoromethoxy-phenylhydrazone, Complement component 1, s subcomponent, Complement component 3, Complement component 4B, Complement factor H, DMEM, DNA, Deoxyribonucleic acid, Dulbecco's modified Eagle's medium, ECAR, EDTA, ETC, Electron transport chain, Ethylenediaminetetracetic acid, Extracellular acidification rate, FCCP, MT-CO1, MT-CO2, MT-CO3, MT-CYB, MT-ND1, MT-ND3, MT-ND5, Maximal oxygen uptake, MicroMolar, Mitochondria encoded NADH dehydrogenase 1, Mitochondria encoded NADH dehydrogenase 3, Mitochondria encoded NADH dehydrogenase 5, Mitochondria encoded cytochrome B, Mitochondria encoded cytochrome oxidase 1, Mitochondria encoded cytochrome oxidase 2, Mitochondria encoded cytochrome oxidase 3, OCR, OXPHOS, Oxidative phosphorylation, Oxygen consumption rate, Q-PCR, Quantitative polymerase chain reaction, Retinal pigmented epithelium cell line, SEM, SNPs, Single nucleotide polymorphisms, Standard error mean, UCLA, University of California, Los Angeles, VO2(max), μM, Physical Sciences, Biological Sciences

Abstract

The geographic origins of populations can be identified by their maternally inherited mitochondrial DNA (mtDNA) haplogroups. This study compared human cybrids (cytoplasmic hybrids), which are cell lines with identical nuclei but mitochondria from different individuals with mtDNA from either the H haplogroup or L haplogroup backgrounds. The most common European haplogroup is H while individuals of maternal African origin are of the L haplogroup. Despite lower mtDNA copy numbers, L cybrids had higher expression levels for nine mtDNA-encoded respiratory complex genes, decreased ATP (adenosine triphosphate) turnover rates and lower levels of reactive oxygen species production, parameters which are consistent with more efficient oxidative phosphorylation. Surprisingly, GeneChip arrays showed that the L and H cybrids had major differences in expression of genes of the canonical complement system (5 genes), dermatan/chondroitin sulfate biosynthesis (5 genes) and CCR3 (chemokine, CC motif, receptor 3) signaling (9 genes). Quantitative nuclear gene expression studies confirmed that L cybrids had (a) lower expression levels of complement pathway and innate immunity genes and (b) increased levels of inflammation-related signaling genes, which are critical in human diseases. Our data support the hypothesis that mtDNA haplogroups representing populations from different geographic origins may play a role in differential susceptibilities to diseases.

Published

2014

33. Case Report: A Rare Truncating Variant of the CFHR5 Gene in IgA Nephropathy

Author

Gabriella Guzzo, Salima Sadallah, Heidi Fodstad, Jean-Pierre Venetz, Samuel Rotman, Daniel Teta, Thierry Gauthier, Giuseppe Pantaleo, Andrea Superti-Furga, and Manuel Pascual

Subjects

IgA nephropathy, complement, CFHR5, CFH, eculizumab, atypical hemolytic uremic syndrome, Genetics, QH426-470

Abstract

IgA nephropathy (IgAN) is the most common primary glomerulonephritis worldwide. Despite appropriate therapy, 20–40% of affected-patients evolve toward end-stage kidney disease (ESKD). Mesangial IgA deposits are the hallmark of IgAN, and complement deposition (C3) seems to differentiate latent IgA mesangial deposits from active IgAN. Atypical hemolytic uremic syndrome (aHUS), another disease in which complement plays an important role, is caused by inherited or acquired deregulation of the alternative pathway (AP) of complement. A subgroup of IgAN shows thrombotic microangiopathy (TMA) lesions in kidney biopsies, the histological characteristic of aHUS. Genetic variants of complement Factor H (CFH), known to be present in aHUS, have been associated with rapidly progressive forms of IgAN and a clinical pattern of aHUS. Genome-wide association studies (GWAS) have confirmed that the 1q32 region, encoding for CFH and its related proteins, is an IgAN susceptibility locus. A 30 year-old man was admitted for seizures and malignant hypertension. The kidney biopsy showed IgAN associated with features of TMA. Despite five plasma exchanges, the patient remained dialysis-dependent, and ESKD was diagnosed. Functional and genetic complement analysis were performed. A monoallelic protein-truncating, likely loss-of-function variant was identified in the CFHR5 gene. Eculizumab is the treatment of aHUS. As it has been successfully used in a few cases of rapidly progressive IgAN, it was decided to administer eculizumab over a period of 12 months in addition to the usual immunosuppression for renal transplantation. After a follow-up of 3 years, there was no clinical disease recurrence. Systematic biologic and genetic screening of complement in individuals with IgAN might be useful to better delineate the role of the AP of complement in renal disease progression, and this may have therapeutic implications.

Published

2021

34. Case Report: A Rare Truncating Variant of the CFHR5 Gene in IgA Nephropathy.

Author

Guzzo, Gabriella, Sadallah, Salima, Fodstad, Heidi, Venetz, Jean-Pierre, Rotman, Samuel, Teta, Daniel, Gauthier, Thierry, Pantaleo, Giuseppe, Superti-Furga, Andrea, and Pascual, Manuel

Subjects

IGA glomerulonephritis, COMPLEMENT factor H, HEMOLYTIC-uremic syndrome, GENOME-wide association studies, CHRONIC kidney failure, COMPLEMENT receptors

Abstract

IgA nephropathy (IgAN) is the most common primary glomerulonephritis worldwide. Despite appropriate therapy, 20–40% of affected-patients evolve toward end-stage kidney disease (ESKD). Mesangial IgA deposits are the hallmark of IgAN, and complement deposition (C3) seems to differentiate latent IgA mesangial deposits from active IgAN. Atypical hemolytic uremic syndrome (aHUS), another disease in which complement plays an important role, is caused by inherited or acquired deregulation of the alternative pathway (AP) of complement. A subgroup of IgAN shows thrombotic microangiopathy (TMA) lesions in kidney biopsies, the histological characteristic of aHUS. Genetic variants of complement Factor H (CFH), known to be present in aHUS, have been associated with rapidly progressive forms of IgAN and a clinical pattern of aHUS. Genome-wide association studies (GWAS) have confirmed that the 1q32 region, encoding for CFH and its related proteins, is an IgAN susceptibility locus. A 30 year-old man was admitted for seizures and malignant hypertension. The kidney biopsy showed IgAN associated with features of TMA. Despite five plasma exchanges, the patient remained dialysis-dependent, and ESKD was diagnosed. Functional and genetic complement analysis were performed. A monoallelic protein-truncating, likely loss-of-function variant was identified in the CFHR5 gene. Eculizumab is the treatment of aHUS. As it has been successfully used in a few cases of rapidly progressive IgAN, it was decided to administer eculizumab over a period of 12 months in addition to the usual immunosuppression for renal transplantation. After a follow-up of 3 years, there was no clinical disease recurrence. Systematic biologic and genetic screening of complement in individuals with IgAN might be useful to better delineate the role of the AP of complement in renal disease progression, and this may have therapeutic implications. [ABSTRACT FROM AUTHOR]

Published

2021

35. Association of HTRA1 and CFH gene polymorphisms with age-related macular degeneration in Ningbo, China.

Author

Gong, Yan, Zhan, Yu, Yuan, Tao, Liao, Yanhong, Zhang, Lingyi, Liu, Xiaotian, Zheng, Yuanhao, and Bao, Yongbo

Abstract

Background: Age-related macular degeneration (AMD) is one of the major causes of blindness, and the incidence of this disease has been increasing in recent years. Objective: To investigate the association between the single nucleotide polymorphisms (SNPs) of the high temperature requirement factor A-1 (HTRA1) and complement factor H (CFH) genes and susceptibility to AMD in Ningbo, China. Methods: Ninety-eight patients with AMD and seventy-three controls were recruited at the Sixth Hospital of Ningbo from August 2017 to April 2019 in China. Genomic DNA was extracted from the venous blood provided by the hospital, and the genotypes of the AMD susceptibility genes CFH and HTAR1 were detected by polymerase chain reaction and sequenced directly. The SNPs rs11200638 on the HTRA1 gene and rs3753394 on the CFH gene were selected for genotype and association analysis. The correlations between the different genotypes of HTRA1 and CFH and AMD were analysed by the Chi-squared test. Results: All the genotypes adhered to the Hardy–Weinberg equilibrium. There were three genotypes (AA, AG and GG) in HTRA1 (rs11200638). The differences in genotypes and allele frequency between the AMD group and the control group were statistically significant (P < 0.05). The A allele was a risk allele (OR: 4.19, 95% Cl: 2.28 ~ 7.70, P < 0.05), with a frequency of 61.7% in patients versus 43.8% in controls. However, the rs3753394 SNP in CFH was not associated with AMD in our study (P > 0.05). Conclusions: The rs11200638 SNP of the HTRA1 gene is associated with AMD, and the AA genotype is a risk factor for AMD in the Ningbo population. There is no significant correlation between the rs3753394 SNP of the CFH gene and AMD. [ABSTRACT FROM AUTHOR]

Published

2021

36. Mitochondrial DNA haplogroups confer differences in risk for age-related macular degeneration: a case control study

Author

Kenney, MC, Hertzog, D, Chak, G, Atilano, SR, Khatibi, N, Soe, K, Nobe, A, Yang, E, Chwa, M, Zhu, F, Memarzadeh, M, King, J, Langberg, J, Small, K, Nesburn, AB, Boyer, DS, and Udar, N

Subjects

Age-related macular degeneration, Mitochondrial haplogroups, mtDNA, CFH, ARMS2

Published

2013

37. Role of carbonate electrolytes on interaction of quinolone drug with anionic surfactant at various temperatures: A conductometric study.

Author

Mahbub, Shamim, Islam, Mohayminul, Masum, Abuzayed, Akter, Parul, Hoque, Md. Anamul, Kumar, Dileep, Khan, Farah, Rub, Malik Abdul, Alfaifi, Sulaiman Y.M., and Asiri, Abdullah M.

Subjects

*DRUG interactions, *CRITICAL micelle concentration, *ELECTROLYTES, *RESPIRATORY infections, *CARBONATES, *BACTERIAL diseases, *SODIUM dodecyl sulfate, *ANIONIC surfactants

Abstract

The role of different carbonate salts on the interaction of anionic surfactant sodium dodecyl sulfate (SDS) with employed quinolone antibiotic drug (ciprofloxacin hydrochloride [CFH]) was explosively inspected through measuring specific conductivity (κ) of the investigated system. The drug, CFH, is an excellent antibiotic for the treatment of different bacterial infections like skin, urinary tract, and respiratory infections. The estimated critical micelle concentrations (cmc) of SDS were observed to be dwindled in the attendance of electrolytes and cmc reduction continues with the escalation of the electrolyte's concentration. The magnitudes of cmc for the SDS + CFH mixture were reduced with the elevation of temperature in K2CO3 and CaCO3 medium while increased with the rise of the temperature in the Na2CO3 medium. The magnitudes of counterion binding to micelles (β) were increased with the increase of the concentration of Na2CO3 and K2CO3 up to definite value and then reduced with the increase of successive rise of concentration of both salts at all temperatures while decreased monotonically with the rise of electrolyte concentration in CaCO3 medium. The values of standard free energy (∆Gmo) were achieved to be negative in each case suggesting spontaneous self‐assembly formation. The standard entropy change (∆Smo) along with enthalpy change (∆Hmo) was also assessed and discussed elaborately. [ABSTRACT FROM AUTHOR]

Published

2021

38. Identification of CFH and FHL2 as biomarkers for idiopathic pulmonary fibrosis.

Author

Liu X, Yang M, Li J, Liu H, Dong Y, Zheng J, and Huang Y

Abstract

Background: Idiopathic pulmonary fibrosis (IPF) is a fatal disease of unknown etiology with a poor prognosis, characterized by a lack of effective diagnostic and therapeutic interventions. The role of immunity in the pathogenesis of IPF is significant, yet remains inadequately understood. This study aimed to identify potential key genes in IPF and their relationship with immune cells by integrated bioinformatics analysis and verify by in vivo and in vitro experiments., Methods: Gene microarray data were obtained from the Gene Expression Omnibus (GEO) for differential expression analysis. The differentially expressed genes (DEGs) were identified and subjected to functional enrichment analysis. By utilizing a combination of three machine learning algorithms, specific genes associated with idiopathic pulmonary fibrosis (IPF) were pinpointed. Then their diagnostic significance and potential co-regulators were elucidated. We further analyzed the correlation between key genes and immune infiltrating cells via single-sample gene set enrichment analysis (ssGSEA). Subsequently, a single-cell RNA sequencing data (scRNA-seq) was used to explore which cell types expressed key genes in IPF samples. Finally, a series of in vivo and in vitro experiments were conducted to validate the expression of candidate genes by western blot (WB), quantitative real-time PCR (qRT-PCR), and immunohistochemistry (IHC) analysis., Results: A total of 647 DEGs of IPF were identified based on two datasets, including 225 downregulated genes and 422 upregulated genes. They are closely related to biological functions such as cell migration, structural organization, immune cell chemotaxis, and extracellular matrix. CFH and FHL2 were identified as key genes with diagnostic accuracy for IPF by three machine learning algorithms. Analysis using ssGSEA revealed a significant association of both CFH and FHL2 with diverse immune cells, such as B cells and NK cells. Further scRNA-seq analysis indicated CFH and FHL2 were specifically upregulated in human IPF tissues, which was confirmed by in vitro and in vivo experiments., Conclusion: In this study, CFH and FHL2 have been identified as novel potential biomarkers for IPF, with potential diagnostic utility in future clinical applications. Subsequent investigations into the functions of these genes in IPF and their interactions with immune cells may enhance comprehension of the disease's pathogenesis and facilitate the identification of therapeutic targets., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2024 Liu, Yang, Li, Liu, Dong, Zheng and Huang.)

Published

2024

39. Alternative complement pathway is activated in the brains of scrapie-infected rodents.

Author

Chen, Cao, Lv, Yan, Hu, Chao, Xu, Xiao-Feng, Zhang, Ren-Qing, Xiao, Kang, Ma, Yue, Gao, Li-Ping, Li, Jian-Le, Shi, Qiang, Wang, Jing, Shi, Qi, and Dong, Xiao-Ping

Subjects

*SCRAPIE, *CENTRAL nervous system, *ANIMAL disease models, *PRION diseases, *RODENTS, *COMPLEMENT activation

Abstract

Activation of complement system in central nervous system (CNS) of the patients suffering from prion diseases or animal models infected with prion agents experimentally is reported repeatedly, but which pathways are involved in the complement system during prion infection is not well documented. Here, we evaluated the level of complement factor B (CFB), which is the key factor that triggers alterative pathway (AP) of complement in the brain tissues of scrapie-infected mice with various methodologies. We found that the levels of mRNA and protein of CFB significantly increased in the brain tissues of scrapie-infected mice. Morphologically, the increased CFB-specific signal overlapped with the elevated C3 signal in brain sections of scrapie-infected mice, meanwhile overlapped with damaged neurons and activated microglia, but not with the proliferative astrocytes. Additionally, the level of complement factor P (CFP), the key positive regulator of AP, also increased remarkably in the brain tissues of infected mice. The transcriptional levels of CD55 and CD46, two negative regulators of AP, decreased without significance in brain tissues of scrapie-infected mice at the terminal stage. However, the mRNA and protein levels of CFH, another negative regulator of AP, increased. Through the dynamic analyses of the expressions of CFB, CFP, and CFH in brain sections of 139A-infected mice, which were collected at different time-points during incubation period, illustrated time-dependent increase levels of each factor during the incubation period of scrapie infection. Taken together, our data here demonstrate that the AP of complement cascade is activated in the CNS microenvironment during prion infection. [ABSTRACT FROM AUTHOR]

Published

2020

40. Gene-Diet Interactions in Age-Related Macular Degeneration

Author

Rowan, Sheldon, Taylor, Allen, Bowes Rickman, Catherine, editor, LaVail, Matthew M., editor, Anderson, Robert E., editor, Grimm, Christian, editor, Hollyfield, Joe, editor, and Ash, John, editor

Published

2016

41. Downregulation of complement factor H attenuates the stemness of MDA‑MB‑231 breast cancer cells via modulation of the ERK and p38 signaling pathways.

Author

Park, Soon Yong, Eum, Da-Young, Jin, Yunho, Lee, Chae Young, Shim, Jae Woong, Choi, Si Ho, Park, Seong-Joon, Heo, Kyu, and Choi, Yoo Jin

Subjects

*COMPLEMENT factor H, *CANCER cells, *BREAST cancer, *CANCER stem cells, *CELLULAR signal transduction

Abstract

The complement system is a powerful innate immune system deployed in the immediate response to pathogens and cancer cells. Complement factor H (CFH), one of the regulators involved in the complement cascade, can interrupt the death of target cells. Certain types of cancer, such as breast cancer, can adopt an aggressive phenotype, such as breast cancer stem cells (BCSCs), through enhancement of the defense system against complement attack by amplifying various complement regulators. However, little is known about the association between CFH and BCSCs. In the present study, the roles of CFH in the CSC characteristics and radioresistance of MDA-MB-231 human breast cancer cells were investigated. CFH knockdown in MDA-MB-231 cells decreased the viability of the cells upon complement cascade activation. Notably, CFH knockdown also decreased cell survival and suppressed mammosphere formation, cell migration and cell invasion by attenuating radioresistance. Additionally, CFH knockdown further enhanced irradiation-induced apoptosis through G2/M cell cycle arrest. It was also discovered that CFH knockdown attenuated the aggressive phenotypes of cancer cells by regulating CSC-associated gene expression. Finally, by microarray analysis, it was found that the expression of erythrocyte membrane protein band 4.1-like 3 (EPB41L3) was markedly increased following CFH knockdown. EPB41L3 inhibited ERK and activated the p38 MAPK signaling pathway. Taken together, these results indicated that CFH knockdown attenuated CSC properties and radioresistance in human breast cancer cells via controlling MAPK signaling and through upregulation of the tumor suppressor, EPB41L3. [ABSTRACT FROM AUTHOR]

Published

2023

42. Deleterious Impact of a Novel CFH Splice Site Variant in Atypical Hemolytic Uremic Syndrome

Author

Ria Schönauer, Anna Seidel, Maik Grohmann, Tom H. Lindner, Carsten Bergmann, and Jan Halbritter

Subjects

complement factor H, atypical hemolytic uremic syndrome, splice site variant, short consensus repeat 18, eculizumab, CFH, Genetics, QH426-470

Abstract

Atypical hemolytic uremic syndrome (aHUS) is a heterogeneous disorder characterized by microangiopathic hemolytic anemia (MAHA), thrombocytopenia, and acute kidney injury (AKI). In about 50% of cases, pathogenic variants in genes involved in the innate immune response including complement factors complement factor H (CFH), CFI, CFB, C3, and membrane co-factor protein (MCP/CD46) put patients at risk for uncontrolled activation of the alternative complement pathway. As aHUS is characterized by incomplete penetrance and presence of additional triggers for disease manifestation, genetic variant interpretation is challenging and streamlined functional variant evaluation is urgently needed. Here, we report the case of a 27-year-old female without previous medical and family history who presented with confusion, petechial bleeding, and anuric AKI. Kidney biopsy revealed glomerular thrombotic microangiopathy (TMA). Targeted next generation sequencing identified a paternally transmitted novel heterozygous splice site variant in the CFH gene [c.3134-2A>G; p.Asp1045_Thr1053del] which resulted in a partial in-frame deletion of exon 20 transcript as determined by cDNA analysis. On the protein level, the concomitant loss of 9 amino acids in the short consensus repeat (SCR) domains 17 and 18 of CFH includes a highly conserved cysteine residue, which is assumed to be essential for proper structural folding and protein function. Treatment with steroids, plasmapheresis, and the complement inhibitor eculizumab led to complete hematological and clinical remission after several months and stable renal function up to 6 years later. In conclusion, genetic investigation for pathogenic variants and evaluation of their functional impact, in particular in the case of splice site variants, is clinically relevant and enables not only better molecular understanding but helps to guide therapy with complement inhibitors.

Published

2019

43. Genetic associations of central serous chorioretinopathy subtypes, neovascular age-related macular degeneration, and polypoidal choroidal vasculopathy.

Author

Chen ZJ, Ng DS, Ho M, Lu SY, Tam POS, Young AL, Brelen ME, Yam JC, Tham CC, Pang CP, and Chen LJ

Subjects

Humans, Genotype, Polypoidal Choroidal Vasculopathy, Polymorphism, Single Nucleotide, Fluorescein Angiography, Central Serous Chorioretinopathy genetics, Macular Degeneration genetics, Choroidal Neovascularization genetics

Abstract

Purpose: To evaluate the genetic associations of different subtypes of central serous chorioretinopathy (CSCR), neovascular age-related macular degeneration (nAMD), and polypoidal choroidal vasculopathy (PCV)., Design: A case-control genetic association study., Methods: This study enrolled 217 CSCR, 341 nAMD, 288 PCV patients, and 1380 controls. The CSCR patients were classified into those with focal or diffuse leakage, with or without pigment epithelial detachment (PED), and with or without macular neovascularization (MNV). Associations between 11 variants from 8 genes, ADAMTS9, ANGPT2, ARMS2, CFH, NR3C2, PGF, TNFRSF10A and VIPR2, and diseases/subtypes were analyzed by logistic regression analysis adjusted for age and sex, and inter-phenotype comparison by heterogeneity test., Results: The CFH rs800292-A conferred a protective effect for CSCR with MNV (OR=0.44, P = 0.002) and a risk effect for CSCR without MNV (OR=1.31, P = 0.023). CSCR patients carrying rs800292-G had a 3.23-fold of increased risk towards developing secondary MNV (P = 1.45 ×10 -4 ). CFH rs3753394, rs800292 and rs1329428 showed similar effects among CSCR with MNV, nAMD and PCV, but opposite effects on CSCR without MNV. TNFRSF10A rs13278062-T was associated with overall CSCR but not with CSCR subtypes, nAMD or PCV. Moreover, CFH and ARMS2 SNPs showed heterogeneous effects in CSCR without MNV against CSCR with MNV, nAMD and PCV., Conclusions: Genetic associations of CSCR with MNV resembled nAMD and PCV compared to CSCR without MNV, indicating differential genetic effects on neovascularization and choroidopathy. Further investigation of the functional roles of CFH, ARMS2, and TNFRSF10A in CSCR, nAMD and PCV should help elucidate the mechanisms of these maculopathies., Competing Interests: Declaration of Competing Interest No conflicting relationship exists for any author., (Copyright © 2023. Published by Elsevier Inc.)

Published

2024

44. Association of the Complement Factor H Y402H Polymorphism and Response to Anti-Vascular Endothelial Growth Factor Treatment in Age-Related Macular Degeneration: An Updated Meta-Analysis.

Author

Roshanshad A, Moosavi SA, and Arevalo JF

Subjects

Humans, Genotype, Complement Factor H genetics, Vascular Endothelial Growth Factor A antagonists & inhibitors, Vascular Endothelial Growth Factor A genetics, Angiogenesis Inhibitors therapeutic use, Polymorphism, Single Nucleotide, Macular Degeneration genetics, Macular Degeneration drug therapy

Abstract

Introduction: Anti-vascular endothelial growth factor (anti-VEGF) agents have a variable effect on patients with age-related macular degeneration (AMD) that has been attributed to several causes, including genetic factors. We evaluated the effects of Complement Factor H (CFH) rs1061170/Y402H polymorphism on the response to anti-VEGF therapy among AMD patients., Methods: PubMed, Scopus, EMBASE, Web of Science, and Google Scholar were used for a literature search. Pooled odds ratios (ORs) and their 95% confidence intervals (CIs) were estimated to assess the effects of CFH Y402H polymorphism on the response to anti-VEGF therapy in AMD. I2 was used to present the amount of heterogeneity. We used STATA version 14.0 software., Results: Twenty-five papers reporting data for 4,681 patients were included in this study. Better response to anti-VEGF therapy was seen in T over C (OR = 1.25, 95% CI = 1.04-1.50), TT over CC (OR = 1.60, 95% CI = 1.06-2.4), and TT + TC over CC (OR = 1.68, 95% CI = 1.23-2.28) genotypes. There was no significant difference in the three other genetic models (TT vs. TC, TT vs. TC + CC, TC vs. TT + CC). In Asians, no significant difference was observed in all six genetic models. Ranibizumab and bevacizumab had similar efficacy; however, conbercept was more effective in homozygous genotypes. The literature indicated that TT and TC genotypes and T allele were associated with a better functional response, while the CC genotype and C alleles had a better anatomical response. The combination of risk alleles in ARMS2 A69S (rs10490924), VEGF-A (rs699947), and VEGF-A (rs833069) with Y420H is a predictor of non-respondents., Conclusion: In patients with AMD, the CFH Y402H is a predictor of the response to anti-VEGF agents and should be considered in the treatment plan., (© 2024 The Author(s). Published by S. Karger AG, Basel.)

Published

2024

45. Drusenoid Pigment Epithelial Detachment: Genetic and Clinical Characteristics

Author

Taiyo Shijo, Yoichi Sakurada, Koji Tanaka, Akiko Miki, Seigo Yoneyama, Yumiko Machida, Aya Chubachi, Yu Wakatsuki, Atsushi Sugiyama, Hajime Onoe, Wataru Kikushima, Ryusaburo Mori, and Kenji Kashiwagi

Subjects

drusenoid pigment epithelial detachment, ARMS2, CFH, reticular pseudodrusen, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Few studies report drusenoid pigment epithelial detachment (DPED) in Asians. In this multicenter study, we report the clinical and genetic characteristics of 76 patients with DPED, and, for comparison, 861 patients with exudative age-related macular degeneration (AMD) were included. On the initial presentation, the mean best-corrected visual acuity was 0.087 ± 0.17 (logMAR unit), and mean DPED height and width were 210 ± 132 and 1633 ± 1114 µm, respectively. Fifty-one (67%) patients showed macular neovascularization in the contralateral eye. The risk allele frequency of both ARMS2 A69S and CFH I62V was significantly higher in DPED than in typical AMD and polypoidal choroidal vasculopathy (PCV) (ARMS2 A69S risk allele frequency: DPED 77% vs. typical AMD 66% vs. PCV 57%, CFH I62V risk allele frequency: DPED 87% vs. typical AMD 73% vs. PCV 73%), although the risk allele frequency of both genes was similar between the DPED group and retinal angiomatous proliferation (RAP) group (ARMS2 A69S: p = 0.32, CFH I62V, p = 0.11). The prevalence of reticular pseudodrusen (RPD) was highest in RAP (60%), followed by DPED (22%), typical AMD (20%), and PCV (2%). Although the prevalence of RPD differs between DPED and RAP, these entities share a similar genetic background in terms of ARMS2 and CFH genes.

Published

2021

46. Association of rs10490924 in ARMS2/HTRA1 with age‐related macular degeneration in the Pakistani population.

Author

Ayub, Humaira, Shafique, Sobia, Azam, Aisha, Muslim, Irfan, Qazi, Nauman A, Akhtar, Farah, Khan, Muhammad Asim, Ayub, Adil, Bashir, Shaheena, Bakker, Bjorn, Ahmed, Shakil, Azam, Maleeha, Hollander, Anneke I., and Qamar, Raheel

Subjects

*RETINAL degeneration, *SINGLE nucleotide polymorphisms, *POPULATION, *DISTRIBUTION (Probability theory), *GENE frequency, *GENOTYPES

Abstract

Age‐related macular degeneration (AMD) is a disease of the elderly in which central vision is lost because of degenerative changes of the macula. The current study investigated the association of single‐nucleotide polymorphisms (SNPs) with AMD in the Pakistani population. Four SNPs were analyzed in this study: rs1061170 in the CFH, rs429608 near CFB, rs2230199 in the C3, and rs10490924 in ARMS2/HTRA1. This case‐control association study was conducted on 300 AMD patients (125 wet AMD and 175 dry AMD) and 200 unaffected age‐ and gender‐matched control individuals. The association of the SNP genotypes and allele frequency distributions were compared between patients and healthy controls, keeping age, gender, and smoking status as covariates. A significant genotype and variant allele association was found of rs10490924 in ARMS2/HTRA1 with wet AMD, while the SNPs in CFH, CFB, and C3 were not associated with AMD in the current Pakistani cohort. The lack of association of CFH, CFB, and C3 may be attributed to limited sample size. This study demonstrates that genetic causative factors of AMD differ among populations and supports the need for genetic association studies among cohorts from various populations to increase our global understanding of the disease pathogenesis. [ABSTRACT FROM AUTHOR]

Published

2019

47. Immunological features and functional analysis of anti-CFH autoantibodies in patients with atypical hemolytic uremic syndrome.

Author

Guo, Wei-yi, Song, Di, Liu, Xiao-rong, Chen, Zhi, Xiao, Hui-jie, Ding, Jie, Sun, Shu-zhen, Liu, Hong-yan, Wang, Su-xia, Yu, Feng, Zhao, Ming-hui, and On behalf of the Chinese Renal-TMA Network

Subjects

*HEMOLYTIC-uremic syndrome diagnosis, *ERYTHROCYTES, *AUTOANTIBODIES, *DISEASE susceptibility, *ENZYME-linked immunosorbent assay, *EPITHELIAL cells, *HEMOLYTIC-uremic syndrome, *IMMUNOGLOBULINS, *IMMUNOLOGY technique, *LONGITUDINAL method, *ACUTE diseases

Abstract

Objective: Atypical hemolytic uremic syndrome (aHUS) is associated with defective complement regulation. Anti-complement factor H (CFH) antibodies were thought to participate in the pathogenesis of aHUS. The aim of this study was to address the functions and properties of CFH autoantibodies in a Chinese Han cohort of aHUS patients.Methods: Thirty-six anti-CFH antibody-positive aHUS patients at the acute phase of the disease were involved in this study. Clinical data of the patients were collected. Anti-CFH immunoglobulin G (IgG) subclasses and antibody isotypes were detected by ELISA. Epitope mapping was performed using recombinant CFH fragments (SCRs 1-4, SCR 7, SCRs 11-14, and SCRs 19-20). Purified IgG from plasma from seven patients were used for functional analyses.Results: All patients presented with the classic triad of HUS. The anti-CFH autoantibodies mostly bound to the SCRs 19-20 domains of CFH but not the SCRs 1-4 domains. CFI cofactor activity was not disturbed by the anti-CFH antibody in any of the seven patients. Purified IgG interfered with the binding of CFH to C3b and CFH-mediated sheep erythrocyte protection in all seven patients. IgG from 4/5 (80%) patients tested inhibited the binding of CFH to glomerular endothelial cells.Conclusions: Our study suggests that the properties of CFH antibodies from patients with aHUS, including the recognition of SCRs and IgG subclasses, can influence and impair the biological role of CFH and therefore contribute to aHUS susceptibility. [ABSTRACT FROM AUTHOR]

Published

2019

48. Association between Polygenic Risk Score and One-Year Outcomes Following As-Needed Aflibercept Therapy for Exudative Age-Related Macular Degeneration

Author

Taiyo Shijo, Yoichi Sakurada, Seigo Yoneyama, Wataru Kikushima, Atsushi Sugiyama, Mio Matsubara, Yoshiko Fukuda, Fumihiko Mabuchi, and Kenji Kashiwagi

Subjects

age-related macular degeneration, polygenic risk score, aflibercept therapy, treatment outcomes, ARMS2, CFH, Medicine, Pharmacy and materia medica, RS1-441

Abstract

We investigated whether polygenic risk score (PRS) was associated with one-year outcome of as-needed aflibercept therapy for exudative age-related macular degeneration (AMD), including AMD (n = 129) and polypoidal choroidal vasculopathy (n = 132). A total of 261 patients were treated with as-needed intravitreal aflibercept injection (IAI) after three monthly IAIs and the completion of a one-year follow-up. One hundred and seventy-two healthy volunteers served as controls. Genotyping of ARMS2 A69S (rs10490924), CFH I62V (rs800292), SKIV2L-C2-CFB (rs429608), C3 (rs2241394), ADAMTS-9 (rs6795735) and CETP (rs3764261) was performed for all participants. A total of 63 PRSs were quantified. There was a positive association between the PRS involving ARMS2, CFH, C3, and ADAMTS-9 and best-corrected visual acuity at twelve months (p = 0.046, multiple regression analysis). When comparing PRSs of patients requiring retreatment and of patients without retreatment, 35 PRSs were significantly greater in patients requiring retreatment than in patients without requiring retreatment, with the PRS involving ARMS2 and CFH being most significantly associated (p = 1.6 × 10−4). The number of additional injections was significantly associated with 40 PRSs and the PRS involving ARMS2 and CFH showed a most significant p-value (p = 2.42 × 10−6). Constructing a PRS using a combination with high-risk variants might be informative for predicting the response to IAI for exudative AMD.

Published

2020

49. Analysis of the association between CFH Y402H polymorphism and response to intravitreal ranibizumab in patients with neovascular age-related macular degeneration (nAMD)

Author

Nur Afiqah Mohamad, Vasudevan Ramachandran, Patimah Ismail, Hazlita Mohd Isa, Yoke Mun Chan, Nor Fariza Ngah, Norshakimah Md Bakri, Siew Mooi Ching, Fan Kee Hoo, Wan Aliaa Wan Sulaiman, Liyana Najwa Inche Mat, and Mohd Hazmi Mohamed

Subjects

Age-related macular degeneration, AMD, complement factor H, CFH, ranibizumab, Y402H, Biology (General), QH301-705.5

Abstract

Pharmacogenetic studies indicate that a variable response to anti-vascular endothelial growth factor (VEGF) therapy in patients with neovascular form of AMD (nAMD) may be due to polymorphisms in the complement factor H gene (CFH). This study is the first to investigate the association between CFH Y402H polymorphism and the response to ranibizumab therapy in Malaysian patients with nAMD. We included 134 patients with nAMD, examined between September 2014 and February 2016. The diagnosis of nAMD was confirmed by ophthalmologic examination, before ranibizumab therapy was started. Each patient received an intravitreal injection of 0.5 mg/0.05 ml ranibizumab following a treat-and-extend (TE) regimen. Best-corrected visual acuity (BCVA) and central retinal thickness (CRT) were recorded after 3 and 6 months following the first injection and compared with the baseline values. Genotyping of Y402H (rs1061170) polymorphism was performed using PCR-RFLP and the amplified product was digested with MluCI restriction enzyme. Association between the Y402H genotypes and response to treatment was determined by a logistic regression analysis of responder (n = 49) and non-responder (n = 84) group. Significantly worse mean BCVA was observed for the CC genotype compared to the TT + CT genotype in the total sample after 6-month follow-up (p = 0.018). Comparing the baseline and 6-month point measurements, improved mean BCVA was observed in responder group, while worse mean BCVA was recorded for non-responder group. However, our regression analysis, adjusted for confounding factors, showed no significant association between the Y402H genotypes and response to treatment in nAMD patients under the recessive model (p > 0.05). Overall, our results suggest that factors other than Y402H polymorphism may be involved in the progression of nAMD after treatment with anti-VEGF agents, in Malaysian population.

Published

2018

50. Common Mechanisms for Separate Maculopathies?

Author

Kortvely, Elod, Ueffing, Marius, LaVail, Matthew M., editor, Ash, John D., editor, Anderson, Robert E., editor, Hollyfield, Joe G., editor, and Grimm, Christian, editor

Published

2012