Your search keyword '"Bao Jian, Fan"' showing total 31 results

1. Novel MIP gene mutation causes autosomal-dominant congenital cataract

Author

Jing-Lan Ni, Hua-Ming Wen, Xiao-Sheng Huang, Qian-Wen Li, Jia-Min Cai, Bao-Jian Fan, and Jun Zhao

Subjects

congenital cataract, major intrinsic protein, missense mutation, zebrafish model, Ophthalmology, RE1-994

Abstract

AIM: To identify disease-causative mutations in families with congenital cataract. METHODS: Two Chinese families with autosomal-dominant congenital cataract (ADCC) were recruited and underwent comprehensive eye examinations. Gene panel next-generation sequencing of common pathogenic genes of congenital cataract was performed in the proband of each family. Sanger sequencing was used to valid the candidate gene mutations and sequence the other family members for co-segregation analysis. The effect of sequence changes on protein structure and function was predicted through bioinformatics analysis. Major intrinsic protein (MIP)-wildtype and MIP-G29R plasmids were constructed and microinjected into zebrafish single-cell stage embryos. Zebrafish embryonic lens phenotypes were screened using confocal microscopy. RESULTS: A novel heterozygous mutation (c.85G>A; p.G29R) in the MIP gene was identified in the proband of one family. A known heterozygous mutation (c.97C>T; p.R33C; rs864309693) in MIP was found in the proband of another family. In-silico prediction indicated that the novel mutation might affect the MIP protein function. Zebrafish embryonic lens was uniformly transparent in both wild-type PCS2+MIP and mutant PCS2+MIP. CONCLUSION: Two missense mutations in the MIP gene in Chinese cataract families are identified, and one of which is novel. These findings expand the genetic spectrum of MIP mutations associated with cataracts. The functional studies suggest that the novel MIP mutation might not be a gain-of-function but a loss-of-function mutation.

Published

2024

2. Exome-based investigation of the genetic basis of human pigmentary glaucoma

Author

Carly van der Heide, Wes Goar, Kacie J. Meyer, Wallace L. M. Alward, Erin A. Boese, Nathan C. Sears, Ben R. Roos, Young H. Kwon, Adam P. DeLuca, Owen M. Siggs, Claudia Gonzaga-Jauregui, Val C. Sheffield, Kai Wang, Edwin M. Stone, Robert F. Mullins, Michael G. Anderson, Bao Jian Fan, Robert Ritch, Jamie E. Craig, Janey L. Wiggs, Todd E. Scheetz, and John H. Fingert

Subjects

Pigmentary Glaucoma, Pigment dispersion syndrome, Glaucoma, Exomes, Human genetics, Biotechnology, TP248.13-248.65, Genetics, QH426-470

Abstract

Abstract Background Glaucoma is a leading cause of visual disability and blindness. Release of iris pigment within the eye, pigment dispersion syndrome (PDS), can lead to one type of glaucoma known as pigmentary glaucoma. PDS has a genetic component, however, the genes involved with this condition are largely unknown. We sought to discover genes that cause PDS by testing cohorts of patients and controls for mutations using a tiered analysis of exome data. Results Our primary analysis evaluated melanosome-related genes that cause dispersion of iris pigment in mice (TYRP1, GPNMB, LYST, DCT, and MITF). We identified rare mutations, but they were not statistically enriched in PDS patients. Our secondary analyses examined PMEL (previously linked with PDS), MRAP, and 19 other genes. Four MRAP mutations were identified in PDS cases but not in controls (p = 0.016). Immunohistochemical analysis of human donor eyes revealed abundant MRAP protein in the iris, the source of pigment in PDS. However, analysis of MRAP in additional cohorts (415 cases and 1645 controls) did not support an association with PDS. We also did not confirm a link between PMEL and PDS in our cohorts due to lack of reported mutations and similar frequency of the variants in PDS patients as in control subjects. Conclusions We did not detect a statistical enrichment of mutations in melanosome-related genes in human PDS patients and we found conflicting data about the likely pathogenicity of MRAP mutations. PDS may have a complex genetic basis that is not easily unraveled with exome analyses.

Published

2021

3. Serum Th1 and Th17 related cytokines and autoantibodies in patients with Posner-Schlossman syndrome.

Author

Jun Zhao, Wenchieh Chen, Xiaosheng Huang, Shiming Peng, Tianhui Zhu, Zhihui Deng, Ping Liang, Hui Chang, and Bao Jian Fan

Subjects

Medicine, Science

Abstract

Posner-Schlossman syndrome (PSS) shares some clinical features with uveitis and open angle glaucoma. Cytokines and autoantibodies have been associated with uveitis and open angle glaucoma. However, the role of serum cytokines and autoantibodies in the pathogenesis of PSS remains unknown. This study aimed to evaluate the associations of type 1 T helper (Th1) and Th17 related cytokines and autoantibodies with PSS. Peripheral blood serum samples were collected from 81 patients with PSS and 97 gender- and age-matched healthy blood donors. Th1 and Th17 related cytokines, including interleukin-1β (IL-1β), IL-12, tumor necrosis factor-α (TNF-α), interferon- γ (IFN-γ), IL-6 and IL-17, and glucose-6-phosphate isomerase (GPI) were determined by double antibody sandwich ELISA. Anti-nuclear antibody (ANA), anti-keratin antibody (AKA) and anti-neutrophil cytoplasmic antibody (ANCA) were detected by indirect immunofluorescence assay. Anti-cardiolipin antibody (ACA)-IgG, ACA-IgM, ACA-IgA, anti-double stranded DNA (anti-dsDNA) and anti-cyclic citrullinated peptide antibody (anti-CCP) were detected by indirect ELISA. Serum levels of IL-1β, IL-12 and IL-6 in PSS patients were significantly lower than those in controls (P < 0.003), and these associations survived the Bonferroni correction (Pc < 0.018). There was no significant difference in serum levels of TNF-α, IFN-γ and IL-17 between the PSS and control groups (Pc > 0.12). Positive rate of serum anti-dsDNA in PSS patients was significantly higher than that in the control group (P = 0.002, Pc = 0.018), while positive rates of serum ANA, AKA, ANCA, ACA-IgG, ACA-IgM, ACA-IgA, GPI and anti-CCP in the PSS group were not significantly different from those in the control group (Pc > 0.09). These results suggest that anti-dsDNA may contribute to the pathogenesis of PSS, while Th1 and Th17 related cytokines and other autoantibodies may not be major contributors to PSS.

Published

2017

4. Association of Matrix Metalloproteinase-9 (MMP9) Variants with Primary Angle Closure and Primary Angle Closure Glaucoma.

Author

Xueli Chen, Yuhong Chen, Janey L Wiggs, Louis R Pasquale, Xinghuai Sun, and Bao Jian Fan

Subjects

Medicine, Science

Abstract

Shorter axial length observed in patients with primary angle closure glaucoma (PACG) might be due to altered matrix metalloproteinase-9 (MMP9) activity resulting in ECM remodeling during eye growth and development. This study aimed to evaluate common variants in MMP9 for association with PACG. Six tag SNPs of MMP9 were genotyped in a Chinese sample of 1,030 cases, including 572 PACG and 458 primary angle closure (PAC), and 499 controls. None of 6 SNPs were significantly associated with overall PAC/PACG (P > 0.07) or with PAC/PACG subgroups (Pc > 0.18). Meta-analysis of two non-Chinese studies revealed significant association between rs17576 and PACG (ORs = 0.56, P < 0.0001); however, meta-analysis of our dataset with 4 Chinese datasets did not replicate this association (ORs = 1.23, P = 0.29). Prior significant association for rs3918249 in one Caucasian study (OR = 0.63, P = 0.006) was not replicated in meta-analysis of 3 Chinese studies including this study (ORs = 0.91, P = 0.13). Significant heterogeneity between non-Chinese and Chinese datasets precluded overall meta-analysis for rs17576 and rs3918249 (Q = 0.001 and 0.04 respectively). rs17577 was nominally associated with PACG in one Caucasian study (OR = 1.71, P = 0.02), but not in 3 Chinese studies including our study (ORs = 1.20, P = 0.07). Overall meta-analysis revealed nominal association for rs17577 and PAC/PACG (ORs = 1.26, Pc = 0.05). Meta-analysis did not show significant association between the other SNPs and PAC/PACG (P > 0.47). The largest association study to date did not find significant association between MMP9 and PAC/PACG in Chinese; meta-analysis with other Chinese datasets did not produce significant association. In most instances combination with non-Chinese datasets was not possible except for one variant showing nominally significant association. More work is needed to define the role of MMP9 variants in PACG.

Published

2016

5. Human Leukocyte Antigens-B and -C Loci Associated with Posner-Schlossman Syndrome in a Southern Chinese Population.

Author

Jun Zhao, Tianhui Zhu, Wenjie Chen, Bao Jian Fan, Liumei He, Baocheng Yang, and Zhihui Deng

Subjects

Medicine, Science

Abstract

The etiology of Posner-Schlossman syndrome (PSS) remains unknown. The association of human leukocyte antigens (HLA) allelic diversity with PSS has been poorly investigated. To evaluate the association of allelic polymorphisms of class I HLA-A, -B and -C and class II HLA-DRB1 and -DQB1 with PSS, 100 unrelated patients with PSS and 128 age- and ethnically matched control subjects were recruited from a southern Chinese Han population. Polymorphisms in exons 2-4 for HLA-A, -B, -C loci, exon 2 for HLA-DRB1 and exons 2,3 for HLA-DQB1 were analyzed for association with PSS at allele and haplotype levels. The allele frequency of HLA-C*1402 in PSS patients was significantly higher than that in controls (P = 0.002, OR = 4.12). This association survived the Bonferroni correction (Pc = 0.04). The allele frequency of HLA-B*1301 in PSS patients was lower than that in the control group (P = 0.003, OR = 0.21), although this association did not survive the Bonferroni correction (Pc = 0.16). In PSS patients, the haplotype frequencies of HLA-A*1101~C*1402 and B*5101~C*1402 were higher than that in controls (P = 0.03, OR = 4.44; P = 0.02, OR = 3.20; respectively), while the HLA-B*1301~C*0304 was lower than that in controls (P = 0.007, OR = 0.23), although these associations did not survive the Bonferroni correction (Pc > 0.16). This study for the first time demonstrated that polymorphisms at the HLA-B and HLA-C loci were nominally associated with PSS in the southern Chinese Han population. Our results suggest that HLA-C*1402, A*1101~C*1402 and B*5101~C*1402 might be risk factors for PSS, whereas HLA-B*1301 plus B*1301~C*0304 might be protective factors against PSS, but even larger datasets are required to confirm these findings. Findings from this study provide valuable new clues for investigating the mechanisms and development of new diagnosis and treatment for PSS.

Published

2015

6. The p53 codon 72 PRO/PRO genotype may be associated with initial central visual field defects in caucasians with primary open angle glaucoma.

Author

Janey L Wiggs, Alex W Hewitt, Bao Jian Fan, Dan Yi Wang, Dayse R Figueiredo Sena, Colm O'Brien, Anthony Realini, Jamie E Craig, David P Dimasi, David A Mackey, Jonathan L Haines, and Louis R Pasquale

Subjects

Medicine, Science

Abstract

BACKGROUND:Loss of vision in glaucoma is due to apoptotic retinal ganglion cell loss. While p53 modulates apoptosis, gene association studies between p53 variants and glaucoma have been inconsistent. In this study we evaluate the association between a p53 variant functionally known to influence apoptosis (codon 72 Pro/Arg) and the subset of primary open angle glaucoma (POAG) patients with early loss of central visual field. METHODS:Genotypes for the p53 codon 72 polymorphism (Pro/Arg) were obtained for 264 POAG patients and 400 controls from the U.S. and in replication studies for 308 POAG patients and 178 controls from Australia (GIST). The glaucoma patients were divided into two groups according to location of initial visual field defect (either paracentral or peripheral). All cases and controls were Caucasian with European ancestry. RESULTS:The p53-PRO/PRO genotype was more frequent in the U.S. POAG patients with early visual field defects in the paracentral regions compared with those in the peripheral regions or control group (p=2.7 × 10(-5)). We replicated this finding in the GIST cohort (p =7.3 × 10(-3), and in the pooled sample (p=6.6 × 10(-7)) and in a meta-analysis of both the US and GIST datasets (1.3 × 10(-6), OR 2.17 (1.58-2.98 for the PRO allele). CONCLUSIONS:These results suggest that the p53 codon 72 PRO/PRO genotype is potentially associated with early paracentral visual field defects in primary open-angle glaucoma patients.

Published

2012

7. The influence of detorsion of adnexal torsion on melondialdehyde, peroxidase catalase, and catalase of ovarian tissue in rabbits

Author

Yue-xin YU, Ju LI, Jia CHEN, Bao-jian FAN, and Yu-bo YAN

Subjects

malondialdehyde, lcsh:R5-920, catalase, lcsh:R, adnexa uteri, lcsh:Medicine, glutathione peroxidase catalase, lcsh:Medicine (General)

Abstract

Objective To observe the influence of reperfusion after adnexal torsion (AT) on malondialdehyde (MDA), glutathione peroxidase catalase (GSH-Px) and catalase (CAT) contents of ovarian tissue in rabbits. Methods Forty female Japanese long-eared white rabbits were randomly divided into study group (n=32) and control group (n=8). The left adnexa of rabbits in the study group was clockwise twisted three laps, and then fixed on the left abdominal walls. Adnexal detorsion was then done 24 hours after adnexal torsion in the study group, and then the rabbits were divided into 4 groups (8 each). Both ovaries of each group were removed 24h, 48h, 72h and 96h, respectively, after reperfusion. The rabbits in the control group received sham-operation and both ovaries were removed 96h later. The removed left ovaries were used for biochemical detection of GSH-Px, CAT and MDA. All the right ovaries were used as experimental internal-control. Results The activity of GSH-Px declined significantly 24h to 72h after adnexal detorsion (P0.05). The activity of CAT declined significantly 24h and 48h after adnexal detorsion (P0.05). Conclusions Detorsion after adnexal torsion can affect the degree of oxidative stress injury in rabbits' ovaries as shown by the changes in the activities of GSH-Px, CAT and MDA. With the elongation of detorsion time, ovarian injury will be gradually alleviated.

Published

2013

8. SNP rs1533428 at 2p16.3 as a marker for late-onset primary open-angle glaucoma

Author

Li Jia, Chen, Pancy O S, Tam, Dexter Y L, Leung, Alex H, Fan, Mingzhi, Zhang, Clement C Y, Tham, Sylvia W Y, Chiang, Bao Jian, Fan, Ningli, Wang, and Chi Pui, Pang

Subjects

Adult, Aged, 80 and over, Male, genetic structures, Adolescent, Age Factors, Genes, Recessive, Middle Aged, Polymorphism, Single Nucleotide, eye diseases, Cohort Studies, Toll-Like Receptor 4, Asian People, Genetic Loci, Risk Factors, Chromosomes, Human, Pair 2, Humans, Female, Genetic Predisposition to Disease, Age of Onset, Child, Genetic Association Studies, Glaucoma, Open-Angle, Aged, Research Article

Abstract

Purpose To investigate the associations between gene variants in cholesterol 24S-hydroxylase (CYP46A1), LIM homeobox transcription factor 1-beta (LMX1B), plexin domain containing 2 (PLXDC2), toll-like receptor 4 (TLR4), transmembrane and tetratricopeptide repeat containing 2 (TMTC2), zona pellucida glycoprotein 4 (ZP4), chromosome 2p16.3, and primary open-angle glaucoma (POAG). Methods We studied 462 POAG patients and 577 controls from three cohorts (Hong Kong, Shantou, and Beijing, China). Twelve single-nucleotide polymorphisms (SNPs) were genotyped in the Hong Kong cohort using TaqMan genotyping assay. Significant associations were validated in the Shantou and Beijing cohorts. Results Association of POAG with TLR4 rs7037117, in a recessive model, was identified in the Hong Kong and Shantou cohorts (both southern Chinese, prec=0.0019) but not the Beijing cohort (northern Chinese). rs1533428 at chromosome 2p16.3 showed a consistent trend of age-specific association in all three cohorts. Genotypes TT + CT conferred a 2.16 fold of significantly increased risk to late-onset POAG (pdom=0.00025), but no significant risk to POAG of younger ages of onset in the combined cohort. A joint effect was found between rs7037117 and rs1533428, with carriers of both higher-risk genotypes having a 4.53 fold of increased disease risk (p=0.00028). Conclusions Our study reveals discrepant association patterns of 12 candidate SNPs in 7 genes/loci with POAG in Chinese, provides positive replications for POAG markers rs1533428 at 2p16.3 and TLR4 rs7037117, and suggests that rs1533428 is a putative risk variant for late-onset POAG. The identification of an age-specific association between rs1533428 and late-onset POAG highlights a new genotype-phenotype association in POAG. Further studies are warranted to confirm the age-specific association.

Published

2011

9. Different WDR36 mutation pattern in Chinese patients with primary open-angle glaucoma

Author

Bao Jian, Fan, Dan Yi, Wang, Ching-Yu, Cheng, Wendy Charles, Ko, Shun Chiu, Lam, and Chi Pui, Pang

Subjects

Adult, Aged, 80 and over, Male, China, Adolescent, Middle Aged, Asian People, Haplotypes, Case-Control Studies, Mutation, Humans, Female, Eye Proteins, Glaucoma, Open-Angle, Aged, Demography, Research Article

Abstract

Purpose To determine the distribution of WD repeat domain 36 (WDR36) sequence variants in Chinese patients with primary open-angle glaucoma (POAG). Methods One hundred and thirty-five unrelated POAG patients (82 high tension glaucoma [HTG], 42 normal tension glaucoma [NTG], and 11 juvenile-onset POAG [JOAG] patients) and 77 unrelated controls were recruited. All 23 coding exons and splicing junctions of WDR36 were sequenced using BigDye® Terminator v3.1 cycle sequencing kit. Single nucleotide polymorphism (SNP) and haplotype associations were analyzed using PLINK (version 1.04). Results Nineteen sequence alterations were identified, and eight of them were novel including two novel nonsynonymous SNPs (L240V and I713V). Except the common I264V polymorphism, no other previously reported disease-causing or disease-susceptibility mutations were found. The novel I713V mutation was observed in three (3.7%) patients with HTG. One intronic SNP, IVS5+30C>T (rs10038177), showed significantly higher frequency of minor allele T in HTG patients (16.5%) than in controls (1.3%; Odds ratio [OR]=15.0, p=7.9×10−7, Bonferroni corrected p=1.5×10−5). Haplotype GTA, which is composed of rs13153937, rs10038177, and rs11241095, was significantly associated with HTG (OR=22.5, p=0.002, Bonferroni corrected p=0.013). Neither the individual SNPs nor haplotypes of WDR36 were associated with NTG or JOAG (Bonferroni corrected p>0.05). Conclusions Findings in this study suggest WDR36 to be associated with sporadic HTG but not with NTG or JOAG. Our results also suggest a different mutation pattern of WDR36 in the Chinese population from other ethnic populations.

Published

2009

10. Lack of association of polymorphisms in homocysteine metabolism genes with pseudoexfoliation syndrome and glaucoma

Author

Bao Jian, Fan, Teresa, Chen, Cynthia, Grosskreutz, Louis, Pasquale, Douglas, Rhee, Elizabeth, DelBono, Jonathan L, Haines, and Janey L, Wiggs

Subjects

Male, Humans, Female, Genetic Predisposition to Disease, Glaucoma, Amino Acid Oxidoreductases, Exfoliation Syndrome, Homocysteine, Polymorphism, Single Nucleotide, eye diseases, Aged, Research Article

Abstract

Purpose To evaluate genes involved in homocysteine metabolism as secondary risk factors for pseudoexfoliation syndrome (PXFS) and the associated glaucoma (PXFG). Methods One hundred eighty-six unrelated patients with PXFS, including 140 patients with PXFG and 127 unrelated control subjects were recruited from the Massachusetts Eye and Ear Infirmary. All the patients and controls were Caucasian of European ancestry. Seventeen tag SNPs from 5 genes (methylenetetrahydrofolate reductase [MTHFR], methionine synthase [MTR], methionine synthase reductase [MTRR], methylenetetrahydrofolate dehydrogenase [MTHFD1], and cystathionine β-synthase [CBS]) were genotyped. Single-SNP association was analyzed using Fisher’s exact test (unconditional) or logistic regression after conditioning on the effects of age and three LOXL1 SNPs (rs1048661, rs3825942, and rs2165241). Interaction analysis was performed between the homocysteine and LOXL1 SNPs using logistic regression. Haplotype analysis and the set-based test were used to test for association of individual genes. Multiple comparisons were corrected using the Bonferroni method. Results One SNP (rs8006686) in MTHFD1 showed a nominally significant association with PXFG (p=0.015, OR=2.23). None of the seventeen SNPs tested were significantly associated with PXFS or PXFG after correcting for multiple comparisons (Bonferroni corrected p>0.25). After controlling for the effects of age and three associated LOXL1 SNPs, none of the seventeen tested SNPs were associated with PXFS (p>0.12). No significant interaction effects on PXFS were identified between the homocysteine and LOXL1 SNPs (p>0.06). Haplotype analysis and the set-based test did not find significant association of individual genes with PXFS (p>0.23 and 0.20, respectively). Conclusions Five genes that are critical components of the homocysteine metabolism pathway were evaluated as secondary factors for PXFS and PXFG. Our results suggest that these genes are not significant risk factors for the development of these conditions.

Published

2008

11. EDN1 Lys198Asn is associated with diabetic retinopathy in type 2 diabetes

Author

Haitao, Li, Janice W C, Louey, Kwong Wai, Choy, David T L, Liu, Wai Man, Chan, Yiu Man, Chan, Nicholas S K, Fung, Bao Jian, Fan, Larry, Baum, Juliana C N, Chan, Dennis S C, Lam, and Chi Pui, Pang

Subjects

Male, China, Diabetic Retinopathy, Endothelin-1, Genotype, Lysine, Middle Aged, Polymorphism, Single Nucleotide, Diabetes Mellitus, Type 2, Gene Frequency, Case-Control Studies, Hypertension, Odds Ratio, Humans, Regression Analysis, Female, Genetic Predisposition to Disease, Age of Onset, Asparagine, Aged, Research Article

Abstract

Purpose We tested the hypothesis that genetic variants in vasoactive and angiogenic factors regulating the retina vasculature contribute to the development of diabetic retinopathy (DR). Methods A case-control study was performed to study the genetic association between DR and polymorphic variants of EDN1 (Lys198Asn), LTA (IVS1–80C>A, IVS1–206G>C, IVS1–252A>G), eNOS (Glu298Asp), and ITGA2 (BgI II) in a Chinese population with type 2 diabetes mellitus. A well defined population with type 2 diabetes, consisting of 127 controls and 216 DR patients, was recruited. Results A higher frequency of the Asn/Asn genotype of EDN1 was found in individuals with at least 10 years of diabetes and no retinopathy (controls) compared with DR patients with any duration of diabetes (DR: 2.3%; control: 11.0%; p=0.0002). The Asn allele was also more frequent in controls than DR patients (DR: 16.4%; control: 29.5%; p=0.007). Multiple logistic regression analysis showed that the Asn/Asn genotype was the factor most significantly associated with reduced risk of DR (odds ratio=0.19; 95% CI: 0.07-0.53; p=0.002) and with late onset of diabetes (Asn/Asn: 59 years; Lys/Lys + Lys/Asn: 53 years; p=0.02). Moreover, the Lys/Lys genotype was more common among patients with nonproliferative (75.7%) than proliferative DR (56.9%; p=0.008). The distributions of Lys198Asn alleles in hypertension did not differ from normotensive subjects. No associations between DR and polymorphisms of LTA, eNOS, or ITGA2 were detected, and there were no detectable gene-gene or gene-environmental interactions among the polymorphisms. Conclusions The Asn/Asn genotype of EDN1 was associated with a reduced risk of DR and with delayed onset of type 2 diabetes.

Published

2008

12. Fine mapping of new glaucoma locus GLC1M and exclusion of neuregulin 2 as the causative gene

Author

Bao Jian, Fan, Wendy Charles, Ko, Dan Yi, Wang, Oscar, Canlas, Robert, Ritch, Dennis S C, Lam, and Chi Pui, Pang

Subjects

Aged, 80 and over, Male, Polymorphism, Genetic, Chromosome Mapping, Middle Aged, Telomere, Introns, Cohort Studies, Haplotypes, Case-Control Studies, Humans, Female, Nerve Growth Factors, Glaucoma, Open-Angle, Aged, Genes, Dominant, Research Article

Abstract

Purpose We recently identified a novel glaucoma locus on 5q22.1-q32, designated as GLC1M, in a family from the Philippines with autosomal dominant juvenile-onset primary open angle glaucoma (JOAG). No mutations in myocilin (MYOC), optineurin (OPTN), and WD-repeat protein 36 (WDR36) were found. Neuregulin 2 (NRG2) is an excellent potential functional as well as positional candidate at GLC1M. The goal of the present study was to evaluate the role of the NRG2 gene in this JOAG family and unrelated JOAG patients and to refine the critical interval for GLC1M. Methods Genomic DNA was obtained from 27 family members. All coding exons and splicing sites of NRG2 were screened for sequence alterations by polymerase chain reaction (PCR) and DNA sequencing. A cohort of 92 unrelated JOAG patients and 92 control subjects were genotyped for the three single nucleotide polymorphisms (SNPs) of NRG2 by PCR and DNA sequencing. Haplotype and segregation analyses were performed in the family. Fisher's exact test was used to compare the frequencies of the NRG2 polymorphisms between affected and unaffected subjects in the family and between unrelated JOAG patients and control subjects. Results Three SNPs were identified: c.98G>A (S33N), IVS3+13A>G (rs889022), and c.1976A>G (G659G). None of them segregated with the JOAG phenotype in this family. No association was found between NRG2 and JOAG in the case-control study (p>0.12). However, further inspection of the haplotypes in the family localized the NRG2 gene telomeric to the disease locus. The critical interval of GLC1M was therefore refined to a region of 28 Mb between D5S2051 and NRG2. Conclusions The linkage interval for GLC1M was refined to a smaller region. The NRG2 gene was excluded as the causative gene for JOAG.

Published

2007

13. [Polymorphisms of myocilin and optineurin in primary open angle glaucoma patients]

Author

Hong-yan, Yao, Ching-yu, Cheng, Bao-jian, Fan, Oi-sin, Tam, Chee-yung, Tham, Dan-yi, Wang, Shun-chiu, Lam, and Chi-pui, Pang

Subjects

Aged, 80 and over, Male, Genotype, DNA Mutational Analysis, Membrane Transport Proteins, Cell Cycle Proteins, Middle Aged, Polymorphism, Single Nucleotide, Cytoskeletal Proteins, Gene Frequency, Transcription Factor TFIIIA, Mutation, Humans, Female, Eye Proteins, Glaucoma, Open-Angle, Aged, Glycoproteins

Abstract

To detect the single nucleotide polymorphisms (SNPs) of the myocilin (MYOC) and optineurin (OPTN) genes, and to investigate their associations with high tension glaucoma (HTG) and normal tension glaucoma (NTG).SNPs were detected using polymerase chain reaction (PCR), followed by conformation sensitive gel electrophoresis (CSGE) and fluorescent labeling automated DNA sequencing among 94 unrelated patients with HTG, 48 unrelated patients with NTG, and 77 unrelated control subjects.Fourteen MYOC sequence alterations were identified, five of them: V53A, I304I, T347T, 1-126TC, and IVS2 + 172CA, were novel. Among them, V53A was for the first time found in primary open angle glaucoma (POAG) patient. R76K usually occurred with the promoter polymorphism 1-83GA. No sequence alterations in the MYOC gene showed significant differences among the HTG, NTG and control subjects (all P0.05). A total of 12 sequence alterations were identified in the OPTN gene, and three of them: V161M, I407T and L211L, were novel. Among them, I407T and L211L were found only in the HTG patients. The allele and genotype frequencies of T34T in the NTG patients were significantly higher than those of the controls (P = 0.001 and 0.004 respectively). In HTG, only the allele frequency of T34T was 24% (23/96), significantly higher than those of the NTG group (16.5%, 31/188) and the control group (9.1%, 14/154) (both P0.05). In addition, IVS8 + 20GA was found only in the HTG (3.1%, 3/96) and NTG patients (3.7%, 7/188), and had significantly higher frequencies in the HTG and NTG patients when compared with the controls (P = 0.016 and 0.014, and P = 0.027 and 0.026).Polymorphisms in the MYOC and OPTN genes are associated with POAG in Chinese people. Moreover, sequence alterations not causing amino acid changes may play a role in the pathogenesis of POAG.

Published

2006

14. A genome-wide scan maps a novel juvenile-onset primary open angle glaucoma locus to chromosome 5q

Author

Chi Pui, Pang, Bao Jian, Fan, Oscar, Canlas, Dan Yi, Wang, Stephane, Dubois, Pancy Oi Sin, Tam, Dennis Shun Chiu, Lam, Vincent, Raymond, and Robert, Ritch

Subjects

Adult, Male, Recombination, Genetic, Adolescent, Genome, Human, DNA Mutational Analysis, Chromosome Mapping, Pedigree, Haplotypes, Chromosomes, Human, Pair 5, Humans, Age of Onset, Lod Score, Child, Eye Proteins, Glaucoma, Open-Angle, Genes, Dominant

Abstract

To map the disease-associated locus of a family with autosomal dominant juvenile-onset primary open angle glaucoma (JOAG) and to screen the novel glaucoma gene WD repeat domain 36 (WDR36).Complete ophthalmic examination and genomic DNA were obtained from 27 family members, in which nine were confirmed JOAG patients. Myocilin (MYOC), optineurin (OPTN), and WDR36 were screened for mutations by polymerase chain reaction and direct sequencing. Genome-wide scanning was carried out using the ABI PRISM Linkage Mapping Set MD-10. Two-point and multipoint linkage analyses were performed with the MLINK, ILINK, and LINKMAP programs. For fine mapping, additional markers flanking the most promising region on chromosome 5q were also analyzed. The significance of LOD scores was tested with simulation analyses using FASTLINK. Haplotypes were constructed using Simwalk2.MYOC or OPTN mutations were excluded in all family members. A maximum LOD score value of 4.82 at theta=0.00 was obtained for the marker D5S2011. Markers D5S2065, D5S1384, D5S471, D5S503, D5S2098, and D5S638 had LOD score values over 4.0 at theta=0.00. Haplotype analysis and recombination mapping further confined this region to 5q22.1-q32 within a region of 36 Mb flanked by D5S2051 and D5S2090. Screening of the novel WDR36 glaucoma-associated gene, which lies centromeric to the disease interval, revealed no mutations within any of the 23 coding exons or splicing junctions.Our results provided the mapping of a novel locus for JOAG at 5q and excluded coding or splicing junctions mutations within the WDR36 gene.

Published

2006

15. [Digenic association of RHO and RP1 genes with retinitis pigmentosa among Chinese population in Hong Kong]

Author

Dan-yi, Wang, Bao-jian, Fan, Wai-man, Chan, Oi-sin, Tam, Wai-yee, Chiang, Shun-chiu, Lam, and Chi-pui, Pang

Subjects

Adult, Aged, 80 and over, Male, Rhodopsin, Adolescent, Middle Aged, Pedigree, Asian People, Mutation, Hong Kong, Humans, Female, Child, Eye Proteins, Microtubule-Associated Proteins, Retinitis Pigmentosa, Aged

Abstract

To identify the mutation patterns of RHO and RP1 genes in the Chinese patients with retinitis pigmentosa (RP) and to explore their potential interactions in the pathogenesis of RP.Sequence alterations in the entire coding region and splice sites of RHO and RP1 gene were screened in 151 RP affected probands and 150 unrelated controls who were all Hong Kong Chinese. Additional 46 relatives of 12 RP probands carrying possible mutations in RHO or RP1 were recruited for segregation analysis. Univariate analysis, multivariate analysis and genotype-pedigree disequilibrium test were used to examine the associations of polymorphisms in these two genes with RP.Two mutations in the RHO gene, 5211delC and P347L, were identified each in one proband from the 151 probands, accounting for 1.3% of the RP patients. Two mutations in the RP1 gene, R677X and D984G, were identified each in one proband from the 151 probands, also accounting for 1.3% of the RP patients. In univariate analysis, non-coding sequence variants in the RHO gene, -26GA, was found to increase the risk of RP, while R872H in the RP1 gene was likely to be a protective factor for RP. Multivariable logistic regression analysis and haplotype analysis confirmed these associations.The prevalences of RHO and RP1 mutations among the RP patients in Chinese population are both less than reported in other populations. Besides the disease-causing mutations, non-coding sequence alterations may also be a modifier for RP. The potential interactions between RHO and RP1 suggest a digenic etiology for RP.

Published

2005

16. SNPs and interaction analyses of myocilin, optineurin, and apolipoprotein E in primary open angle glaucoma patients

Author

Bao Jian, Fan, Dan Yi, Wang, Dorothy Shu Ping, Fan, Pancy Oi Sin, Tam, Dennis Shun Chiu, Lam, Clement Chuu Yang, Tham, Ching Yan, Lam, Tung Ching, Lau, and Chi Pui, Pang

Subjects

Adult, Aged, 80 and over, Male, Adolescent, Genotype, Membrane Transport Proteins, Cell Cycle Proteins, Sequence Analysis, DNA, Middle Aged, Polymerase Chain Reaction, Polymorphism, Single Nucleotide, Cytoskeletal Proteins, Apolipoproteins E, Transcription Factor TFIIIA, Mutation, Protein Interaction Mapping, Humans, Female, Child, Eye Proteins, Glaucoma, Open-Angle, Intraocular Pressure, Aged, Glycoproteins

Abstract

To evaluate the association of myocilin (MYOC), optineurin (OPTN), and apolipoprotein E (APOE) genes and their interactions in primary open angle glaucoma (POAG).A cohort of 400 unrelated POAG patients (294 high tension glaucoma, HTG, and 106 normal tension glaucoma, NTG) and 281 unrelated control subjects were recruited. All coding exons and splicing junctions in MYOC and OPTN were screened for sequence alterations. Common polymorphisms in APOE were genotyped. Single genes were investigated by univariate and haplotype analysis, and gene-gene interactions by logistic regression and stratified analysis. Multiple comparisons were corrected by the Bonferroni method. Bioinformatics analysis was performed to assess the conservation of mutation sites across species and to predict putative motifs and secondary structures in mutated proteins.Disease-causing mutations in MYOC and OPTN were identified in 1.75% and 1% of POAG patients, respectively. Most of these mutations were highly conserved across species, many predicted to create new motifs or change protein secondary structures. No individual MYOC polymorphisms significantly contributed to HTG or NTG. A haplotype containing the minor allele of the MYOC IVS2+35AG increased NTG risk (p=0.0001). Three OPTN polymorphisms, T34T, IVS5+38TG, and IVS8-53TC increased NTG risk (p0.0008), while IVS5+38TG increased HTG risk (p=0.0006). One haplotype that contains the minor alleles of 3 OPTN polymorphisms, T34T, IVS5+38TG, and IVS7+24GA, increased NTG risk (p=0.0002). APOE epsilon4 carriers had a decreased NTG risk (p=0.007). Possible gene-gene interactions were found between MYOC, OPTN, and APOE.Disease-causing mutations in MYOC and OPTN accounted for only a small proportion of Chinese POAG patients. Common polymorphisms in MYOC, OPTN, and APOE might interactively contribute to POAG, indicating a polygenic etiology.

Published

2005

17. [Recent progress in molecular genetics and gene therapy for retinitis pigmentosa]

Author

Dan-Yi, Wang, Bao-Jian, Fan, Xiang-Qian, Wu, Wai-Man, Chan, Shun-Chiu, Lam, and Chi-Pui, Pang

Subjects

Mutation, Humans, Genetic Therapy, Retinitis Pigmentosa

Abstract

Retinitis pigmentosa (RP) is a common genetic eye disease affecting about 1 in 3500 people worldwide with pan-ethnic occurrence. So far there is no effective treatment for RP. This paper gives an overview on recent advances in molecular genetics of RP with emphasis on the important gene mutations for diagnosis and prognosis, and a review on gene therapy of RP.

Published

2005

18. Screening of the LTBP2 gene in 214 Chinese sporadic CYP1B1-negative patients with primary congenital glaucoma.

Author

Xueli Chen, Yuhong Chen, Bao Jian Fan, Mingying Xia, Li Wang, and Xinghuai Sun

Published

2016

19. Absence of myocilin and optineurin mutations in a large Philippine family with juvenile onset primary open angle glaucoma

Author

Dan Yi, Wang, Bao Jian, Fan, Oscar, Canlas, Pancy O S, Tam, Robert, Ritch, Dennis S C, Lam, Dorothy S P, Fan, and Chi Pui, Pang

Subjects

Adult, Male, Polymorphism, Genetic, Genetic Linkage, Philippines, DNA Mutational Analysis, Membrane Transport Proteins, Cell Cycle Proteins, Pedigree, Cytoskeletal Proteins, Transcription Factor TFIIIA, Mutation, Humans, Female, Eye Proteins, Glaucoma, Open-Angle, Intraocular Pressure, Genes, Dominant, Glycoproteins, Microsatellite Repeats

Abstract

To analyze the role of the two primary open angle glaucoma (POAG) genes, myocilin (MYOC) and optineurin (OPTN), in a large Philippine family segregating autosomal dominant juvenile onset open angle glaucoma (JOAG).The coding sequences of the MYOC and OPTN genes were screened in 27 family members by polymerase chain reaction and direct sequencing. The specific MYOC promoter polymorphism (MYOC.mtl) was identified by restriction endonuclease assay. All of the ABI MD-10 microsatellite markers on chromosomes 1, 2, 3, 7, 8, and 10, which harbor the six known POAG loci, were analyzed for linkage with POAG.No mutation was identified in this large kindred. Instead, three polymorphisms (-80G-A, -1000G-C, R76K) in MYOC and four polymorphisms (T34T, M98K, R545Q, IVS7+24G-A) in OPTN were found. All markers flanking the six known POAG loci gave LOD scores not more than 1.1. Non-parametric linkage analysis for all these markers resulted in p values more than 0.05.Both mutation testing and linkage analysis provide strong evidence against MYOC and OPTN being the causative gene in this large family. It indicates that unidentified genes will underlie the occurrence of glaucoma in this family.

Published

2004

20. Genetic and environmental risk factors for primary open-angle glaucoma

Author

Bao-jian, Fan, Yuk-fai, Leung, Ning, Wang, Shun-chiu, Lam, Yao, Liu, Oi-sin, Tam, and Chi-pui, Pang

Subjects

Adult, Aged, 80 and over, Male, Alcohol Drinking, Smoking, Middle Aged, Cytoskeletal Proteins, Logistic Models, Risk Factors, Hypertension, Humans, Female, Eye Proteins, Glaucoma, Open-Angle, Aged, Glycoproteins

Abstract

Primary open-angle glaucoma (POAG) is characterized by optic nerve damage and consists of a group of genetically heterogeneous disorders. This study was to investigate the associations of genetic and environmental factors with POAG in a hospital-based Chinese population.Thirty-two adult onset POAG patients and 96 age-sex matched control subjects were studied by multivariable logistic regression analysis for the relationships between POAG and its risk factors including family history, diabetes, hypertension, cardiovascular diseases, cigarette smoking, alcohol consumption and polymorphisms of the myocilin and the optineurin genes.Univariate analysis showed that POAG was related to family history, cardiovascular disease, alcohol consumption and a myocilin sequence alteration (T353I) (P0.04). Multivariable logistic regression analysis confirmed that POAG was significantly associated with family history (OR = 20.2), hypertension (OR = 3.58), cigarette smoking (OR = 10.8), alcohol consumption (OR = 0.028) and T353I (OR = 6.03, all P0.05).Family history, hypertension, cigarette smoking and T353I in the myocilin gene are risk factors for POAG. Alcohol consumption, however, has a protective effect.

Published

2004

21. [Single nucleotide polymorphisms of the myocilin gene in primary open-angle glaucoma patients]

Author

Bao-jian, Fan, Yuk-fai, Leung, Chi-pui, Pang, Larry, Baum, Oi-sin, Tam, Ning, Wang, and Shun-chiu, Lam

Subjects

Adult, Aged, 80 and over, Male, Base Sequence, Genotype, DNA Mutational Analysis, DNA, Middle Aged, Polymorphism, Single Nucleotide, Cytoskeletal Proteins, Amino Acid Substitution, Gene Frequency, Case-Control Studies, Humans, Point Mutation, Female, Eye Proteins, Glaucoma, Open-Angle, Aged, Glycoproteins

Abstract

To detect single nucleotide polymorphisms (SNPs) of the myocilin (MYOC) gene and to investigate their associations with primary open-angle glaucoma (POAG).One hundred and fifty-seven sporadic patients with POAG and 155 unrelated control subjects without POAG were recruited from staff and visitors to the Prince of Wales Hospital between 1998 and 2000. All study subjects are ethnic Chinese living in Hong Kong. The two populations were matched in frequencies of gender and age. The SNPs of the MYOC gene in POAG patients and control subjects were screened and identified by high throughout conformation sensitive gel electrophoresis and fluorescent labeling automated sequencing. The genotype frequencies of each SNP in the two groups were compared by the Chi2 test or Fisher's exact 2-tailed test.A total of seventeen SNPs were identified from 2172 bp long of the MYOC gene, including all 3 exons and adjacent non-coding regions. The identified SNPs were 1-83G --A, G12R, P16L, A17S, R46X, R76K, R91X, T123T, D208E, L215P, 730+35A --G, A260A, I288I, E300K, T353I, Y471C and 1515+73G --C, respectively. Of these, R91X, E300K and Y471C were found only in POAG patients. A significant difference between POAG patients and control subjects was found in the genotype frequencies of 1515+73G --C. The frequency of the heterozygote (CG) was 0.6% in POAG patients, significantly less than the 4.5% in control subjects (Fisher's exact 2-tailed test, P=0.036, OR=0.136, 95%CI=0.022-0.828). No significant difference was found between the two populations in genotype frequencies of all other SNPs.The polymorphisms of the MYOC gene may be related to POAG.

Published

2004

22. The dual role of dexamethasone on anti-inflammation and outflow resistance demonstrated in cultured human trabecular meshwork cells

Author

Yuk Fai, Leung, Pancy Oi Sin, Tam, Wing Shan, Lee, Dennis Shun Chiu, Lam, Hin Fai, Yam, Bao Jian, Fan, Clement Chee Yung, Tham, John Kien Han, Chua, and Chi Pui, Pang

Subjects

Reverse Transcriptase Polymerase Chain Reaction, Gene Expression Profiling, Anti-Inflammatory Agents, Dexamethasone, Up-Regulation, Aqueous Humor, Gene Expression Regulation, Trabecular Meshwork, Humans, Eye Proteins, Endoplasmic Reticulum Chaperone BiP, Glucocorticoids, Cells, Cultured, Oligonucleotide Array Sequence Analysis

Abstract

Dexamethasone (DEX) is a glucocorticoid commonly used in topical eyedrops to treat eye inflammation. It has an undesirable effect of inducing glaucoma in certain patients. In human Trabecular Meshwork (TM) cells DEX regulates a number of genes but its global influence on TM gene expression is still elusive. In the present work, DEX effects on global gene expressions of an established human TM cell line were studied by microarray.The whole experiment of microarray was repeated three times. Differentially expressed genes were identified by an empirical Bayes approach and confirmed by Reverse Transcription Polymerase Chain Reaction.Eight genes (GAS1, CDH4, MT1L, CST3, ATF4, ASNS/TS11, CHOP, HSPA5) were identified that are at least a thousand times more likely to be differentially expressed due to DEX treatment and six genes (TSC22, LDHA, IGFBP2, TAGLN, SCG2, WARS) were identified that are at least a hundred times more likely to be differentially expressed due to DEX treatment. Except for MT1L, ASNS/TS11, IGFBP2, SCG2, and WARS, all the other genes are first reported here to be regulated by DEX in TM. Intriguingly, several of them have overlapping roles in anti-inflammatory response and outflow resistance.The results of our experiments on cultured human TM cells indicate that the increase in outflow resistance and ultimate ocular hypertension may be byproducts of the favorable anti-inflammatory response triggered by DEX.

Published

2003

23. [Antibacterial effect of niaoluqing oral liquid on clinical drug-resistant strains and different serotype strains of Ureaplasma urealyticum in vitro]

Author

Yuan, Lu, Da-Can, Chen, Qiang, Li, Guo-Wei, Xuan, Bao-Jian, Fan, Ji-Wen, Zhao, and Ning, Wang

Subjects

Humans, Microbial Sensitivity Tests, Ureaplasma urealyticum, Anti-Bacterial Agents, Drugs, Chinese Herbal

Abstract

To study the antibacterial effect of Niaoluqing Oral Liquid (NOL) on clinical drug-resistant strains and 14 serotype strains Ureaplasma Urealyticum (UU).Sixty-three clinical strains of UU were detected to determine their serology and antibiotic susceptibilities by the metabolic inhibition test (MIT). Mininum inhibitory concentration (MIC) was used to evaluate the sensitivity of NOL to different serotypes of UU. The sensitivity of NOL, erythromycin and tetracycline to 63 clinical strains of UU was also studied.In 63 clinical strains of UU, the range of MIC to NOL was from 0.48 mg/ml to 15.63 mg/ml, MIC50or = 1.95 mg/ml, MIC90or = 3.91 mg/ml. Among them, 31 strains were resistant to tetracycline and 31 were resistant to erythromycin. No obvious correlation between the sensitivity of NOL to UU clinical strains and that of erythromycin and tetracycline to UU clinical strains (P0.05). Clinical strains of UU in this experiment contains all of its serotypes, also having a higher sensitivity to NOL (MICor = 3.91 mg/ml) except serology 1, 2, 3 and 11 (MICor = 7.81 mg/ml).NOL exerts a strong in vitro antibacterial effect on erythromycin-resistant and tetracycline-resistant clinical strains of UU. All kinds of serotype strains had a higher sensitivity to NOL, too. Chinese medicinal herbs are of momentous significance in the treatment of UU infection.

Published

2002

24. Inherited Optic Neuropathies: Genetics and New Directions for Diagnosis and Therapy.

Author

Bao Jian Fan

Subjects

*GENETICS, *NEUROPATHY, *OPTIC nerve diseases, *GENETIC disorder diagnosis, *GENES

Abstract

The article explores the genetics and future directions for diagnosis and therapy of inherited optic neuropathies. It mentions the treatment options available for inherited optic neuropathies. Information is provided on the epidemiology and molecular genetics of leber hereditary optic neuropathy (LHON) and dominant optic atrophy (DOA), as well as the emerging genetic diagnostic testing and gene therapies for these diseases.

Published

2014

25. The p53 Codon 72 PRO/PRO Genotype May Be Associated with Initial Central Visual Field Defects in Caucasians with Primary Open Angle Glaucoma.

Author

Wiggs, Janey L., Hewitt, Alex W., Bao Jian Fan, Dan Yi Wang, Sena, Dayse R. Figueiredo, O'Brien, Colm, Realini, Anthony, Craig, Jamie E., Dimasi, David P., Mackey, David A., Haines, Jonathan L., Pasquale, Louis R., and Den Hollander, Anneke I.

Subjects

GENETIC code, NUCLEOTIDE sequence, VISUAL fields, VISION research, CAUCASIAN race, WHITE people

Abstract

Background: Loss of vision in glaucoma is due to apoptotic retinal ganglion cell loss. While p53 modulates apoptosis, gene association studies between p53 variants and glaucoma have been inconsistent. In this study we evaluate the association between a p53 variant functionally known to influence apoptosis (codon 72 Pro/Arg) and the subset of primary open angle glaucoma (POAG) patients with early loss of central visual field. Methods: Genotypes for the p53 codon 72 polymorphism (Pro/Arg) were obtained for 264 POAG patients and 400 controls from the U.S. and in replication studies for 308 POAG patients and 178 controls from Australia (GIST). The glaucoma patients were divided into two groups according to location of initial visual field defect (either paracentral or peripheral). All cases and controls were Caucasian with European ancestry. Results: The p53-PRO/PRO genotype was more frequent in the U.S. POAG patients with early visual field defects in the 25 paracentral regions compared with those in the peripheral regions or control group (p = 2.7 x 10-5). We replicated this finding in the GIST cohort (p = 7.3 x 610-3, and in the pooled sample (p = 6.6 x 10-7) and in a meta-analysis of both the US 26 and GIST datasets (1.3 x 10-3, OR 2.17 (1.58-2.98 for the PRO allele). Conclusions: These results suggest that the p53 codon 72 PRO/PRO genotype is potentially associated with early paracentral visual field defects in primary open-angle glaucoma patients. [ABSTRACT FROM AUTHOR]

Published

2012

26. Glaucoma: genes, phenotypes, and new directions for therapy.

Author

Bao Jian Fan, Wiggs, Janey L., and Fan, Bao Jian

Subjects

*GLAUCOMA, *OPTIC nerve diseases, *INTRAOCULAR pressure, *HUMAN genetics, *GENOMICS, *PHENOTYPES, *GENETICS

Abstract

Glaucoma, a leading cause of blindness worldwide, is characterized by progressive optic nerve damage, usually associated with intraocular pressure. Although the clinical progression of the disease is well defined, the molecular events responsible for glaucoma are currently poorly understood and current therapeutic strategies are not curative. This review summarizes the human genetics and genomic approaches that have shed light on the complex inheritance of glaucoma genes and the potential for gene-based and cellular therapies that this research makes possible. [ABSTRACT FROM AUTHOR]

Published

2010

27. DNA sequence variants in the LOXL1 gene are associated with pseudoexfoliation glaucoma in a U.S. clinic-based population with broad ethnic diversity.

Author

Bao Jian Fan, Pasquale, Louis, Grosskreutz, Cynthia L., Rhee, Douglas, Chen, Teresa, DeAngelis, Margaret M., Kim, Ivana, del Bono, Elizabeth, Miller, Joan W., Tiansen Li, Haines, Jonathan L., and Wiggs, Janey L.

Subjects

*GENES, *GLAUCOMA, *CLINICAL trials, *GENETIC research, *GENETIC polymorphisms, *EYE diseases

Abstract

Background: Pseudoexfoliation syndrome is a major risk factor for glaucoma in many populations throughout the world. Using a U.S. clinic-based case control sample with broad ethnic diversity, we show that three common SNPs in LOXL1 previously associated with pseudoexfoliation in Nordic populations are significantly associated with pseudoexfoliation syndrome and pseudoexfoliation glaucoma. Methods: Three LOXL1 SNPs were genotyped in a patient sample (206 pseudoexfoliation, 331 primary open angle glaucoma, and 88 controls) from the Glaucoma Consultation Service at the Massachusetts Eye and Ear Infirmary. The SNPs were evaluation for association with pseudeoexfoliation syndrome, pseudoexfoliation glaucoma, and primary open angle glaucoma. Results: The strongest association was found for the G allele of marker rs3825942 (G153D) with a frequency of 99% in pseudoexfoliation patients (with and without glaucoma) compared with 79% in controls (p = 1.6 x 10-15; OR = 20.93, 95%CI: 8.06, 54.39). The homozygous GG genotype is also associated with pseudoexfoliation when compared to controls (p = 1.2 x 10-12; OR = 23.57, 95%CI: 7.95, 69.85). None of the SNPs were significantly associated with primary open angle glaucoma. Conclusion: The pseudoexfoliation syndrome is a common cause of glaucoma. These results indicate that the G153D LOXL1 variant is significantly associated with an increased risk of pseudoexfoliation and pseudoexfoliation glaucoma in an ethnically diverse patient population from the Northeastern United States. Given the high prevalence of pseudooexfoliation in this geographic region, these results also indicate that the G153D LOXL1 variant is a significant risk factor for adult-onset glaucoma in this clinic based population. [ABSTRACT FROM AUTHOR]

Published

2008

28. Association between promoter - 1607 polymorphism of MMP1 and Lumbar Disc Disease in Southern Chinese.

Author

You-Qiang Song, Ho, Daniel W. H., Karppinen, Jaro, Kao, Patrick Y. P., Bao-Jian Fan, Luk, Keith D. K., Shea-Ping Yip, Leong, John C. Y., Cheah, Kathryn S. E., Pak Sham, Chan, Danny, and Cheung, Kenneth M. C.

Subjects

GENETIC polymorphisms, MEDICAL genetics, LEUCOCYTES, METALLOPROTEINASES, EXTRACELLULAR matrix

Abstract

Background: Matrix metalloproteinases (MMPs) are involved in the degradation of the extracellular matrix of the intervertebral disc. A SNP for guanine insertion/deletion (G/D), the -1607 promoter polymorphism, of the MMP1 gene was found significantly affecting promoter activity and corresponding transcription level. Hence it is a good candidate for genetic studies in DDD. Methods: Southern Chinese volunteers between 18 and 55 years were recruited from the population. DDD in the lumbar spine was defined by MRI using Schneiderman's classification. Genomic DNA was isolated from the leukocytes and genotyping was performed using the Sequenom® platform. Association and Hardy-Weinberg equilibrium checking were assessed by Chi-square test and Mann-Whitney U test. Results: Our results showed substantial evidence of association between -1607 promoter polymorphism of MMP1 and DDD in the Southern Chinese subjects. D allelic was significantly associated with DDD (p value = 0.027, odds ratio = 1.41 with 95% CI = 1.04-1.90) while Genotypic association on the presence of D allele was also significantly associated with DDD (p value = 0.046, odds ratio = 1.50 with 95% CI = 1.01-2.24). Further age stratification showed significant genotypic as well as allelic association in the group of over 40 years (genotypic: p value = 0.035, odds ratio = 1.617 with 95% CI = 1.033-2.529; allelic: p value = 0.033, odds ratio = 1.445 with 95% CI = 1.029-2.029). Disc bulge, annular tears and the Schmorl's nodes were not associated with the D allele. Conclusion: We demonstrated that individuals with the presence of D allele for the -1607 promoter polymorphism of MMP1 are about 1.5 times more susceptible to develop DDD when compared with those having G allele only. Further association was identified in individuals over 40 years of age. Disc bulge, annular tear as well as Schmorl's nodes were not associated with this polymorphism. [ABSTRACT FROM AUTHOR]

Published

2008

29. Novel Myocilin Mutation in a Chinese Family With Juvenile-Onset Open-Angle Glaucoma.

Author

Bao Jian Fan, Leung, Dexter Y. L., Dan Yi Wang, Gobeil, Stéphane, Raymond, Vincent, Tam, Pancy O. S., Lam, Dennis S. C., and Chi Pui Pang

Abstract

Objective: To search for the genetic cause of juvenileonset open-angle glaucoma (JOAG) in a Chinese family. Methods: In a 3-generation glaucoma family affected with JOAG or ocular hypertension, we screened myocilin (MYOC) and optineurin (OPTN) for mutations and investigated apolipoprotein E (APOE) polymorphisms in 6 family members, 2 of them patients with JOAG, 2 patients with ocular hypertension, and 2 patients who were asymptomatic. Normal controls included 200 unrelated Chinese subjects. The COS-7 cell line was transfected with expression vectors encoding wild-type or mutated MYOC complementary DNA. Cellular and secreted MYOC proteins were characterized by Western blotting. Results: One missense MYOC mutation, 734G>A: Cys245Tyr, was identified. It occurred in all 4 family members afflicted with JOAG or ocular hypertension but not in asymptomatic family members. No OPTN variations were observed. APOE polymorphism frequencies were similar to those for controls. The Cys245Tyr MYOC mutation cosegregated with the disorder within the family. It was absent in the 200 control subjects. The Cys245Tyr mutant MYOC protein formed homomultimeric complexes that migrated at molecular weights larger than their wild-type counterparts. These mutant complexes remained sequestered intracellularly in COS-7 cells. Conclusions: The Cys245Tyr MYOC mutation was the genetic cause of JOAG in this Chinese family. This mutation may alter covalent bonds that formed between MYOC cysteines. Clinical Relevance: Genetic tests of MYOC mutations may be beneficial to predict new cases of the disease in families with JOAG. [ABSTRACT FROM AUTHOR]

Published

2006

30. Polymorphisms in the Myocilin Promoter Unrelated to the Risk and Severity of Primary Open-Angle Glaucoma.

Author

Bao-Jian Fan

Published

2004

31. Beginning Microarray Data Analysis.

Author

Bao Jian Fan and Yuk Fai Leung

Subjects

*DNA microarrays, *NONFICTION

Abstract

Reviews the book 'A Biologist's Guide to Analysis of DNA Microarray Data,' by Steen Knudsen.

Published

2003