Your search keyword '"Ayyagari, R."' showing total 13 results

1. Biogeographic Ancestry in the African Descent and Glaucoma Evaluation Study (ADAGES): Association With Corneal and Optic Nerve Structure

Author

Girkin, CA, Nievergelt, CM, Kuo, JZ, Maihofer, AX, Huisingh, C, Liebmann, JM, Ayyagari, R, Weinreb, RN, Ritch, R, Zangwill, LM, and Grp, ADAGESS

Subjects

Retinal Ganglion Cells, Male, Aging, genetic structures, Optic Disk, Black People, Eye, Ophthalmology & Optometry, optic disc, Medical and Health Sciences, Cornea, Cohort Studies, Nerve Fibers, biogeographic ancestry, Genetics, Humans, race, Eye Disease and Disorders of Vision, African Continental Ancestry Group, Aged, Neurosciences, retinal nerve fiber layer, Glaucoma, Middle Aged, Blacks, Biological Sciences, corneal thickness, eye diseases, Open-Angle, Regression Analysis, Female, sense organs, ADAGES Study Group

Abstract

PurposeWe determined if quantitative measurements of biogeographic ancestry (BGA) correlate with variations in optic disc area, corneal thickness (CCT), and retinal nerve fiber layer (RNFL) thickness.MethodsData were obtained from 656 participants in the African Descent and Glaucoma Evaluation Study (ADAGES) cohort who consented to BGA testing. Data for CCT, optic disc area, and RNFL thickness were obtained from subjects in the ADAGES study who also had participated in the current substudy. A total of 31 ancestry informative markers (AIMs) with large allele frequencies differences between populations was used to calculate admixture proportion (implemented in STRUCTURE). Correlations with BGA adjusted for diagnosis, age, and sex for CCT and optic disc area using the whole group and RNFL thickness adjusted for age and sex for the normal study participants were determined.ResultsThe mean percentage of African admixture was 79.6% in the self-described African Descent (AD) group and 3.5% in the European Descent (ED) group. Percent African ancestry was significantly correlated with CCT (ρ = -0.27, P < 0.0001) and disc area (ρ = 0.15, P < 0.0001), but only marginally associated with RNFL thickness (ρ = 0.20, P = 0.092) in adjusted models.ConclusionsThe BGA correlates with variation in ocular features that significantly differ across racial groups and that have been associated with the development of glaucoma. While BGA can provide an objective measurement of the biologic component of self-described race for ocular research, for most nongenetic epidemiologic studies, self-described race may adequately describe the associations with these ocular characteristics. (ClinicalTrials.gov number, NCT00221923.).

Published

2015

2. An analytical framework for analysis and design of networked control systems with random delays and packet losses

Author

Vallabhan, M., Seshadhri, S., Ashok, S., Ramaswmay, S., and Ayyagari, R.

Subjects

Computer Science - Networking and Internet Architecture, Networking and Internet Architecture (cs.NI), FOS: Computer and information sciences, FOS: Electrical engineering, electronic engineering, information engineering, Computer Science - Systems and Control, Systems and Control (eess.SY)

Abstract

Delays and data losses are undesirable from a control system perspective as they tend to adversely affect performance Networked Control Systems (NCSs) are a class of control systems wherein control components exchange information using a shared communication channel. Delays and packet losses in the communication channels are usually random, thereby making the analysis and design of control loops more complex. The usual assumptions in classical control theory, such as delay free sensing and synchronous actuation, assume lesser significance when it comes to NCSs. Hence, this necessitates a reformulation/relook into the existing models used for NCS control loop analysis and design. In this paper, we study and present the reformulations required for NCSs to include random delays and packet loss in the channel. This paper thereby gives a complete overview of what has been accomplished thus far in NCS research and puts forth a unified framework for analyzing a host of problems that can be captured as NCSs subjected to random delays and packet losses., Comment: Proceedings of the 25th IEEE Canadian Conference on Electrical and Computer Engineering (CCECE)

Published

2015

3. Evaluation of the ELOVL4 gene in patients with autosomal recessive retinitis pigmentosa and Leber congenital amaurosis

Author

Carlo Rivolta, Ayyagari R, Pa, Sieving, El, Berson, and Tp, Dryja

Subjects

Open Reading Frames, DNA Mutational Analysis, Mutation, Missense, Humans, Membrane Proteins, Optic Atrophy, Hereditary, Leber, Sequence Analysis, DNA, Blindness, Eye Proteins, Polymerase Chain Reaction, Polymorphism, Single-Stranded Conformational, Retinitis Pigmentosa, DNA Primers

Abstract

To determine whether pathogenic mutations exist in the ELOVL4 gene in patients with inherited retinal degenerations other than Stargardt-like macular dystrophy or other hereditary macular degenerations.All six exons comprising the open reading frame of the ELOVL4 gene were evaluated by single-strand conformation analysis, direct nucleotide sequencing, or both methods.No pathogenic mutations were found among 84 patients with autosomal recessive retinitis pigmentosa or among 51 patients with Leber congenital amaurosis (congenital retinal blindness).These data support the conclusion that recessive retinitis pigmentosa and Leber congenital amaurosis are rarely if ever associated with changes in the ELOVL4 gene.

Published

2003

4. Genetic studies of age-related macular degeneration

Author

Yashar, BM, Swaroop, A, Hiriyanna, S, Ayyagari, R, Elner, S, Johnson, MW, Kurtz, R, Sieving, PA, and Vine, AK

Subjects

Biological Sciences, Ophthalmology & Optometry, Medical and Health Sciences

Published

1999

5. Association of severity of primary open-angle glaucoma with serum vitamin D levels in patients of African descent

Author

Ayyagari, R., Chen, Y. -D I., Zangwill, L. M., Holman, M., Dirkes, K., Hai, Y., Arzumanyan, Z., Slight, R., Hammel, N., Girkin, C. A., Liebmann, J. M., Robert Feldman, Taylor, K. D., Rotter, J. I., Guo, X., and Weinreb, R. N.

6. A missense mutation in ASRGL1 is involved in causing autosomal recessive retinal degeneration

Author

Biswas, P., Chavali, V. R., Agnello, G., Stone, E., Chakarova, C., Duncan, J. L., Kannabiran, C., Homsher, M., Bhattacharya, S. S., Muhammad Asif Naeem, Kimchi, A., Sharon, D., Iwata, T., Riazuddin, S., Reddy, G. B., Hejtmancik, J. F., Georgiou, G., Riazuddin, S. A., and Ayyagari, R.

7. Novel mutations in ltbp2 identified in familial cases of primary congenital glaucoma

Author

Rauf, B., Irum, B., Khan, S. Y., Kabir, F., Muhammad Asif Naeem, Riazuddin, S., Ayyagari, R., and Amer Riazuddin, S.

Subjects

Male, Adolescent, Evolution, Genetic Linkage, DNA Mutational Analysis, Ophthalmology & Optometry, Chromosomes, Evolution, Molecular, Clinical Research, Opthalmology and Optometry, Genetics, Humans, 2.1 Biological and endogenous factors, Pakistan, Aetiology, Child, Preschool, Alleles, Chromosomes, Human, Pair 14, Pediatric, Pair 14, Human Genome, Molecular, Glaucoma, Sequence Analysis, DNA, DNA, Exons, Pedigree, Latent TGF-beta Binding Proteins, Child, Preschool, Mutation, Female, Sequence Analysis, Research Article, Human

Abstract

Purpose Primary congenital glaucoma (PCG) is a genetically heterogeneous disorder caused by developmental defects in the anterior chamber and trabecular meshwork. This disease is an important cause of childhood blindness. In this study, we aim to identify the genetic determinants of PCG in three consanguineous families of Pakistani descent. Methods Affected members of all three families underwent detailed ophthalmological examination including slit-lamp biomicroscopy. Blood samples were collected from affected and healthy members of all three families, and genomic DNA was extracted. Linkage analysis was performed for the known or reported loci of PCG to localize the disease interval, and logarithm of odds (LOD) scores were calculated. All protein-coding exons of the candidate gene, latent transforming growth factor-beta binding protein 2 (LTBP2), were bidirectionally sequenced to identify the disease-causing mutation. Results Short tandem repeat (STR) marker-based linkage analysis localized the critical interval to chromosome 14q with a maximum two-point LOD score of 2.86 (PKGL076), 2.8 (PKGL015), and 2.92 (PKGL042). Bidirectional Sanger sequencing of LTBP2 revealed three novel pathogenic variants, i.e., c.3028G>A (p.Asp1010Asn), c.3427delC (p.Gln1143Argfs*35), and c.5270G>A (p.Cys1757Tyr) in PKGL076, PKGL015, and PKGL042, respectively. All three mutations segregated with the disease phenotype in their respective families and were absent in 200 ethnically matched normal chromosomes. Conclusions We identified three novel mutations, p.D1010N, p.Q1143Rfs*35, and p.C1757Y, in LTBP2 responsible for PCG.

8. Loss of function mutations in RP1 are responsible for retinitis pigmentosa in consanguineous familial cases

Author

Kabir, F., Ullah, I., Ali, S., Gottsch, A. D. H., Muhammad Asif Naeem, Assir, M. Z., Khan, S. N., Akram, J., Riazuddin, S., Ayyagari, R., Fielding Hejtmancik, J., and Amer Riazuddin, S.

Subjects

Male, Base Sequence, Genetic Linkage, DNA Mutational Analysis, Exons, Ophthalmology & Optometry, Polymerase Chain Reaction, eye diseases, Pedigree, Consanguinity, Young Adult, Loss of Function Mutation, Opthalmology and Optometry, Mutation, Electroretinography, Humans, Female, sense organs, Lod Score, Eye Proteins, Microtubule-Associated Proteins, Retinitis Pigmentosa, Genome-Wide Association Study

Abstract

PurposeThis study was undertaken to identify causal mutations responsible for autosomal recessive retinitis pigmentosa (arRP) in consanguineous families.MethodsLarge consanguineous families were ascertained from the Punjab province of Pakistan. An ophthalmic examination consisting of a fundus evaluation and electroretinography (ERG) was completed, and small aliquots of blood were collected from all participating individuals. Genomic DNA was extracted from white blood cells, and a genome-wide linkage or a locus-specific exclusion analysis was completed with polymorphic short tandem repeats (STRs). Two-point logarithm of odds (LOD) scores were calculated, and all coding exons and exon-intron boundaries of RP1 were sequenced to identify the causal mutation.ResultsThe ophthalmic examination showed that affected individuals in all families manifest cardinal symptoms of RP. Genome-wide scans localized the disease phenotype to chromosome 8q, a region harboring RP1, a gene previously implicated in the pathogenesis of RP. Sanger sequencing identified a homozygous single base deletion in exon 4: c.3697delT (p.S1233Pfs22*), a single base substitution in intron 3: c.787+1G>A (p.I263Nfs8*), a 2 bp duplication in exon 2: c.551_552dupTA (p.Q185Yfs4*) and an 11,117 bp deletion that removes all three coding exons of RP1. These variations segregated with the disease phenotype within the respective families and were not present in ethnically matched control samples.ConclusionsThese results strongly suggest that these mutations in RP1 are responsible for the retinal phenotype in affected individuals of all four consanguineous families.

9. Molecular and phenotypic analysis of a family with autosomal recessive cone-rod dystrophy and Stargardt disease

Author

Yzer, S., Den Born, L. I., Zonneveld, M. N., Lopez, I., Ayyagari, R., Teye-Botchway, L., Luisa Mota-Vieira, Cremers, F. P. M., and Koenekoop, R. K.

Subjects

Genetics and epigenetic pathways of disease [NCMLS 6], Genetic defects of metabolism [UMCN 5.1], genetic structures

Abstract

Contains fulltext : 52433.pdf (Publisher’s version ) (Open Access) PURPOSE: To identify the causative gene mutations in three siblings with severe progressive autosomal recessive cone-rod dystrophy (arCRD) and their fifth paternal cousin with Stargardt disease (STGD1) and to specify the phenotypes. METHODS: We evaluated eight sibs of one family, three family members displayed arCRD, and one STGD1. All of them were screened for mutations using a new microarray for autosomal recessive retinitis pigmentosa. RESULTS: We found a new pathologic ATP-binding cassette transporter (ABCA4) splice-site mutation, c.3523-2A>T and the previously reported c.5327C>T (p.P1776L) missense mutation in the arCRD patients. The three siblings shared these two ABCA4 mutations and showed similar phenotypes. An unusual aspect was nystagmus which presented in one of the arCRD patients. In the STGD1 patient we found the c.5327C>T (p.P1776L) missense mutation and a novel c.868C>T (p.R290W) missense mutation. CONCLUSIONS: Two new ABCA4 mutations were identified in a family with arCRD and STGD1. A new finding was nystagmus associated with arCRD in one of the patients.

10. Is intrinsic motivation as important in utilitarian systems as it is in hedonic systems? A preliminary meta-analysis

Author

Gerow, J. E., Ayyagari, R., Jason Thatcher, and Roth, P. L.

11. Erythrocyte aldose reductase activity and sorbitol levels in diabetic retinopathy

Author

G. Bhanuprakash Reddy, Satyanarayana, A., Balakrishna, N., Ayyagari, R., Padma, M., Viswanath, K., and Petrash, J. M.

Subjects

Blood Glucose, Male, Erythrocytes, Glycated Hemoglobin A, endocrine system diseases, Fundus Oculi, Glycosylated, Eye, Ophthalmology & Optometry, Clinical Research, Aldehyde Reductase, Opthalmology and Optometry, Diabetes Mellitus, 2.1 Biological and endogenous factors, Humans, Sorbitol, Prospective Studies, Aetiology, Eye Disease and Disorders of Vision, Metabolic and endocrine, Glycated Hemoglobin, Diabetic Retinopathy, Diabetes, nutritional and metabolic diseases, Hemoglobin A, Middle Aged, Diabetes Mellitus, Type 2, Case-Control Studies, Female, Type 2, Research Article

Abstract

Purpose Activation of polyol pathway due to increased aldose reductase (ALR2) activity has been implicated in the development of diabetic complications including diabetic retinopathy (DR), a leading cause of blindness. However, the relationship between hyperglycemia-induced activation of polyol pathway in retina and DR is still uncertain. We investigated the relationship between ALR2 levels and human DR by measuring ALR2 activity and its product, sorbitol, in erythrocytes. Methods We enrolled 362 type 2 diabetic subjects (T2D) with and without DR and 66 normal subjects in this clinical case-control study. Clinical evaluation of DR in T2D patients was done by fundus examination. ALR2 activity and sorbitol levels along with glucose and glycosylated hemoglobin (HbA1C) levels in erythrocytes were determined. Results T2D patients with DR showed significantly higher specific activity of ALR2 as compared to T2D patients without DR. Elevated levels of sorbitol in T2D patients with DR, as compared to T2D patients without DR, corroborated the increased ALR2 activity in erythrocytes of DR patients. However, the increased ALR2 activity was not significantly associated with diabetes duration, age, and HbA1C in both the DR group and total T2D subjects. Conclusions Levels of ALR2 activity as well as sorbitol in erythrocytes may have value as a quantitative trait to be included among other markers to establish a risk profile for development of DR.

12. Impact of obesity with impaired glucose tolerance on retinal degeneration in a rat model of metabolic syndrome

Author

Godisela, K. K., Reddy, S. S., Kumar, C. U., Saravanan, N., Reddy, P. Y., Jablonski, M. M., Ayyagari, R., and Reddy, G. B.

13. Retinal Phenotypes in Patients Homozygous for the G1961E Mutation in the ABCA4 Gene

Author

Tomas R. Burke, Robert K. Koenekoop, Caroline C W Klaver, Alfonso Baldi, F. P. M. Cremers, Jana Zernant, Alessandro Iannaccone, Radha Ayyagari, Carl Schubert, Allison C. Umfress, R. T. Smith, Rando Allikmets, Maria Laura Ciccarelli, Stephen H. Tsang, Gerald A. Fishman, Burke, Tr, Fishman, Ga, Zernant, J, Shubert, C, Tsang, Sh, Smith, Rt, Ayyagari, R, Koenekoop, Rk, Umfress, A, Ciccarelli, Ml, Baldi, Alfonso, Iannaccone, A, Cremers, Fp, Klaver, Cc, Allikmets, R., and Ophthalmology

Subjects

Pathology, medicine.medical_specialty, medicine.diagnostic_test, biology, Genetics and epigenetic pathways of disease [NCMLS 6], Fundus photography, ABCA4, Articles, Macular degeneration, Fundus (eye), medicine.disease, Fluorescein angiography, eye diseases, Stargardt disease, Mutation (genetic algorithm), medicine, biology.protein, Age of onset

Abstract

PURPOSE. We evaluated the pathogenicity of the G1961E mutation in the ABCA4 gene, and present the range of retinal phenotypes associated with this mutation in homozygosity in a patient cohort with ABCA4-associated phenotypes. METHODS. Patients were enrolled from the ABCA4 disease database at Columbia University or by inquiry from collaborating physicians. Only patients homozygous for the G1961E mutation were enrolled. The entire ABCA4 gene open reading frame, including all exons and flanking intronic sequences, was sequenced in all patients. Phenotype data were obtained from clinical history and examination, fundus photography, infrared imaging, fundus autofluorescence, fluorescein angiography, and spectral domain-optical coherence tomography. Additional functional data were obtained using the full-field electroretinogram, and static or kinetic perimetry. RESULTS. We evaluated 12 patients homozygous for the G1961E mutation. All patients had evidence of retinal pathology consistent with the range of phenotypes observed in ABCA4 disease. The latest age of onset was recorded at 64 years, in a patient diagnosed initially with age-related macular degeneration (AMD). Of 6 patients in whom severe structural (with/ without functional) fundus changes were detected, 5 had additional, heterozygous or homozygous, variants detected in the ABCA4 gene. CONCLUSIONS. Homozygous G1961E mutation in ABCA4 results in a range of retinal pathology. The phenotype usually is at the milder end of the disease spectrum, with severe phenotypes linked to the presence of additional ABCA4 variants. Our report also highlights that milder, late-onset Stargardt disease may be confused with AMD. (Invest Ophthalmol Vis Sci. 2012; 53:4458–4467) DOI:10.1167/iovs.11-9166

Published

2012