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3. Subjective and Objective Screening Tests for Hydroxychloroquine Toxicity

Author

Cukras, Catherine, Huynh, Nancy, Vitale, Susan, Wong, Wai T, Ferris, Fredrick L, and Sieving, Paul A

Subjects
Biomedical and Clinical Sciences, Ophthalmology and Optometry, Biomedical Imaging, Eye Disease and Disorders of Vision, Neurosciences, Rare Diseases, Clinical Research, Detection, screening and diagnosis, 4.2 Evaluation of markers and technologies, Eye, Adult, Aged, Antirheumatic Agents, Arthritis, Rheumatoid, Case-Control Studies, Diagnostic Techniques, Ophthalmological, Electroretinography, Female, Fluorescein Angiography, Humans, Hydroxychloroquine, Lupus Erythematosus, Systemic, Male, Middle Aged, Prospective Studies, Retina, Retinal Diseases, Sensitivity and Specificity, Tomography, Optical Coherence, Visual Acuity, Visual Fields, Clinical Sciences, Opthalmology and Optometry, Public Health and Health Services, Ophthalmology & Optometry, Ophthalmology and optometry
Abstract

ObjectiveTo compare subjective and objective clinical tests used in the screening for hydroxychloroquine retinal toxicity to multifocal electroretinography (mfERG) reference testing.DesignProspective, single-center, case control study.ParticipantsFifty-seven patients with a previous or current history of hydroxychloroquine treatment of more than 5 years' duration.MethodsParticipants were evaluated with a detailed medical history, dilated ophthalmologic examination, color fundus photography, fundus autofluorescence (FAF) imaging, spectral-domain (SD) optical coherence tomography (OCT), automated visual field testing (10-2 visual field mean deviation [VFMD]), and mfERG testing. We used mfERG test parameters as a gold standard to divide participants into 2 groups: those affected by hydroxychloroquine-induced retinal toxicity and those unaffected.Main outcome measuresWe assessed the association of various imaging and psychophysical variables in the affected versus the unaffected group.ResultsFifty-seven study participants (91.2% female; mean age, 55.7±10.4 years; mean duration of hydroxychloroquine treatment, 15.0±7.5 years) were divided into affected (n = 19) and unaffected (n = 38) groups based on mfERG criteria. Mean age and duration of hydroxychloroquine treatment did not differ statistically between groups. Mean OCT retinal thickness measurements in all 9 macular subfields were significantly lower (

Published
2015

4. Sorting out Co-occurrence of Rare Monogenic Retinopathies: Stargardt Disease Co-existing with Congenital Stationary Night Blindness

Author

Huynh, Nancy, Jeffrey, Brett G, Turriff, Amy, Sieving, Paul A, and Cukras, Catherine A

Subjects
Genetics, Genetic Testing, Neurosciences, Macular Degeneration, Rare Diseases, Neurodegenerative, Clinical Research, Eye Disease and Disorders of Vision, Eye, ATP-Binding Cassette Transporters, Color Vision, Electroretinography, Eye Diseases, Hereditary, Female, Genetic Diseases, X-Linked, Humans, Middle Aged, Mutation, Missense, Myopia, Night Blindness, Open Reading Frames, Polymerase Chain Reaction, Receptors, Glutamate, Stargardt Disease, Tomography, Optical Coherence, Visual Acuity, Visual Fields, ABCA4, congenital stationary night blindness, electronegative ERG, GRM6, Stargardt disease, Opthalmology and Optometry, Ophthalmology & Optometry
Abstract

BackgroundInherited retinal diseases are uncommon, and the likelihood of having more than one hereditary disorder is rare. Here, we report a case of Stargardt disease and congenital stationary night blindness (CSNB) in the same patient, and the identification of two novel in-frame deletions in the GRM6 gene.Materials and methodsThe patient underwent an ophthalmic exam and visual function testing including: visual acuity, color vision, Goldmann visual field, and electroretinography (ERG). Imaging of the retina included fundus photography, spectral-domain optical coherence tomography (OCT), and fundus autofluorescence. Genomic DNA was PCR-amplified for analysis of all coding exons and flanking splice sites of both the ABCA4 and GRM6 genes.ResultsA 46-year-old woman presented with recently reduced central vision and clinical findings of characteristic yellow flecks consistent with Stargardt disease. However, ERG testing revealed an ERG phenotype unusual for Stargardt disease but consistent with CSNB1. Genetic testing revealed two previously reported mutations in the ABCA4 gene and two novel deletions in the GRM6 gene.ConclusionsDiagnosis of concurrent Stargardt disease and CSNB was made on the ophthalmic history, clinical examination, ERG, and genetic testing. This case highlights that clinical tests need to be taken in context, and that co-existing retinal dystrophies and degenerations should be considered when clinical impressions and objective data do not correlate.

Published
2014

7. Generation of LexA enhancer-trap lines in Drosophila by an international scholastic network

Author

Kim, Ella S, primary, Rajan, Arjun, additional, Chang, Kathleen, additional, Govindarajan, Sanath, additional, Gulick, Clara, additional, English, Eva, additional, Rodriguez, Bianca, additional, Bloomfield, Orion, additional, Nakada, Stella, additional, Beard, Charlotte, additional, O’Connor, Sarah, additional, Mastroianni, Sophia, additional, Downey, Emma, additional, Feigenbaum, Matthew, additional, Tolentino, Caitlin, additional, Pace, Abigail, additional, Khan, Marina, additional, Moon, Soyoun, additional, DiPrima, Jordan, additional, Syed, Amber, additional, Lin, Flora, additional, Abukhadra, Yasmina, additional, Bacon, Isabella, additional, Beckerle, John, additional, Cho, Sophia, additional, Donkor, Nana Esi, additional, Garberg, Lucy, additional, Harrington, Ava, additional, Hoang, Mai, additional, Lawani, Nosa, additional, Noori, Ayush, additional, Park, Euwie, additional, Parsons, Ella, additional, Oravitan, Philip, additional, Chen, Matthew, additional, Molina, Cristian, additional, Richmond, Caleb, additional, Reddi, Adith, additional, Huang, Jason, additional, Shugrue, Cooper, additional, Coviello, Rose, additional, Unver, Selma, additional, Indelicarto, Matthew, additional, Islamovic, Emir, additional, McIlroy, Rosemary, additional, Yang, Alana, additional, Hamad, Mahdi, additional, Griffin, Elizabeth, additional, Ahmed, Zara, additional, Alla, Asha, additional, Fitzgerald, Patricia, additional, Choi, Audrey, additional, Das, Tanya, additional, Cheng, Yuchen, additional, Yu, Joshua, additional, Roderiques, Tabor, additional, Lee, Ethan, additional, Liu, Longchao, additional, Harper, Jaekeb, additional, Wang, Jason, additional, Suhr, Chris, additional, Tan, Max, additional, Luque, Jacqueline, additional, Tam, A Russell, additional, Chen, Emma, additional, Triff, Max, additional, Zimmermann, Lyric, additional, Zhang, Eric, additional, Wood, Jackie, additional, Clark, Kaitlin, additional, Kpodonu, Nat, additional, Dey, Antar, additional, Ecker, Alexander, additional, Chuang, Maximilian, additional, López, Ramón Kodi Suzuki, additional, Sun, Harry, additional, Wei, Zijing, additional, Stone, Henry, additional, Chi, Chia Yu Joy, additional, Silvestri, Aiden, additional, Orloff, Petra, additional, Nedumaran, Neha, additional, Zou, Aletheia, additional, Ünver, Leyla, additional, Page, Oscair, additional, Kim, Minseo, additional, Chan, Terence Yan Tao, additional, Tulloch, Akili, additional, Hernandez, Andrea, additional, Pillai, Aruli, additional, Chen, Caitlyn, additional, Chowdhury, Neil, additional, Huang, Lina, additional, Mudide, Anish, additional, Paik, Garrett, additional, Wingate, Alexandra, additional, Quinn, Lily, additional, Conybere, Chris, additional, Baumgardt, Luca Laiza, additional, Buckley, Rollo, additional, Kolberg, Zara, additional, Pattison, Ruth, additional, Shazli, Ashlyn Ahmad, additional, Ganske, Pia, additional, Sfragara, Luca, additional, Strub, Annina, additional, Collier, Barney, additional, Tamana, Hari, additional, Ravindran, Dylan, additional, Howden, James, additional, Stewart, Madeleine, additional, Shimizu, Sakura, additional, Braniff, Julia, additional, Fong, Melanie, additional, Gutman, Lucy, additional, Irvine, Danny, additional, Malholtra, Sahil, additional, Medina, Jillian, additional, Park, John, additional, Yin, Alicia, additional, Abromavage, Harrison, additional, Barrett, Breanna, additional, Chen, Jacqueline, additional, Cho, Rachelle, additional, Dilatush, Mac, additional, Gaw, Gabriel, additional, Gu, Caitlin, additional, Huang, Jupiter, additional, Kilby, Houston, additional, Markel, Ethan, additional, McClure, Katie, additional, Phillips, William, additional, Polaski, Benjamin, additional, Roselli, Amelia, additional, Saint-Cyr, Soleil, additional, Shin, Ellie, additional, Tatum, Kylan, additional, Tumpunyawat, Tai, additional, Wetherill, Lucia, additional, Ptaszynska, Sara, additional, Zeleznik, Maddie, additional, Pesendorfer, Alexander, additional, Nolan, Anna, additional, Tao, Jeffrey, additional, Sammeta, Divya, additional, Nicholson, Laney, additional, Dinh, Giao Vu, additional, Foltz, Merrin, additional, Vo, An, additional, Ross, Maggie, additional, Tokarski, Andrew, additional, Hariharan, Samika, additional, Wang, Elaine, additional, Baziuk, Martha, additional, Tay, Ashley, additional, Wong, Yuk Hung Maximus, additional, Floyd, Jax, additional, Cui, Aileen, additional, Pierre, Kieran, additional, Coppisetti, Nikita, additional, Kutam, Matthew, additional, Khurjekar, Dhruv, additional, Gadzi, Anthony, additional, Gubbay, Ben, additional, Pedretti, Sophia, additional, Belovich, Sofiya, additional, Yeung, Tiffany, additional, Fey, Mercy, additional, Shaffer, Layla, additional, Li, Arthur, additional, Beritela, Giancarlo, additional, Huyghue, Kyle, additional, Foster, Greg, additional, Durso-Finley, Garrett, additional, Thierfelder, Quinn, additional, Kiernan, Holly, additional, Lenkowsky, Andrew, additional, Thomas, Tesia, additional, Cheng, Nicole, additional, Chao, Olivia, additional, L’Etoile-Goga, Pia, additional, King, Alexa, additional, McKinley, Paris, additional, Read, Nicole, additional, Milberg, David, additional, Lin, Leila, additional, Wong, Melinda, additional, Gilman, Io, additional, Brown, Samantha, additional, Chen, Lila, additional, Kosai, Jordyn, additional, Verbinsky, Mark, additional, Belshaw-Hood, Alice, additional, Lee, Honon, additional, Zhou, Cathy, additional, Lobo, Maya, additional, Tse, Asia, additional, Tran, Kyle, additional, Lewis, Kira, additional, Sonawane, Pratmesh, additional, Ngo, Jonathan, additional, Zuzga, Sophia, additional, Chow, Lillian, additional, Huynh, Vianne, additional, Yang, Wenyi, additional, Lim, Samantha, additional, Stites, Brandon, additional, Chang, Shannon, additional, Cruz-Balleza, Raenalyn, additional, Pelta, Michaela, additional, Kujawski, Stella, additional, Yuan, Christopher, additional, Standen-Bloom, Elio, additional, Witt, Oliver, additional, Anders, Karina, additional, Duane, Audrey, additional, Huynh, Nancy, additional, Lester, Benjamin, additional, Fung-Lee, Samantha, additional, Fung, Melanie, additional, Situ, Mandy, additional, Canigiula, Paolo, additional, Dijkgraaf, Matijs, additional, Romero, Wilbert, additional, Baula, Samantha Karmela, additional, Wong, Kimberly, additional, Xu, Ivana, additional, Martinez, Benjamin, additional, Nuygen, Reena, additional, Norris, Lucy, additional, Nijensohn, Noah, additional, Altman, Naomi, additional, Maajid, Elise, additional, Burkhardt, Olivia, additional, Chanda, Jullian, additional, Doscher, Catherine, additional, Gopal, Alex, additional, Good, Aaron, additional, Good, Jonah, additional, Herrera, Nate, additional, Lanting, Lucas, additional, Liem, Sophia, additional, Marks, Anila, additional, McLaughlin, Emma, additional, Lee, Audrey, additional, Mohr, Collin, additional, Patton, Emma, additional, Pyarali, Naima, additional, Oczon, Claire, additional, Richards, Daniel, additional, Good, Nathan, additional, Goss, Spencer, additional, Khan, Adeeb, additional, Madonia, Reagan, additional, Mitchell, Vivian, additional, Sun, Natasha, additional, Vranka, Tarik, additional, Garcia, Diogo, additional, Arroyo, Frida, additional, Morales, Eric, additional, Camey, Steven, additional, Cano, Giovanni, additional, Bernabe, Angelica, additional, Arroyo, Jennifer, additional, Lopez, Yadira, additional, Gonzalez, Emily, additional, Zumba, Bryan, additional, Garcia, Josue, additional, Vargas, Esmeralda, additional, Trinidad, Allen, additional, Candelaria, Noel, additional, Valdez, Vanessa, additional, Campuzano, Faith, additional, Pereznegron, Emily, additional, Medrano, Jenifer, additional, Gutierrez, Jonathan, additional, Gutierrez, Evelyn, additional, Abrego, Ericka Taboada, additional, Gutierrez, Dayanara, additional, Ortiz, Cristian, additional, Barnes, Angelica, additional, Arms, Eleanor, additional, Mitchell, Leo, additional, Balanzá, Ciara, additional, Bradford, Jake, additional, Detroy, Harrison, additional, Ferguson, Devin, additional, Guillermo, Ethel, additional, Manapragada, Anusha, additional, Nanula, Daniella, additional, Serna, Brigitte, additional, Singh, Khushi, additional, Sramaty, Emily, additional, Wells, Brian, additional, Wiggins, Matthew, additional, Dowling, Melissa, additional, Schmadeke, Geraldine, additional, Cafferky, Samantha, additional, Good, Stephanie, additional, Reese, Margaret, additional, Fleig, Miranda, additional, Gannett, Alex, additional, Cain, Cory, additional, Lee, Melody, additional, Oberto, Paul, additional, Rinehart, Jennifer, additional, Pan, Elaine, additional, Mathis, Sallie Anne, additional, Joiner, Jessica, additional, Barr, Leslie, additional, Evans, Cory J, additional, Baena-Lopez, Alberto, additional, Beatty, Andrea, additional, Collette, Jeanette, additional, Smullen, Robert, additional, Suttie, Jeanne, additional, Chisholm, Townley, additional, Rotondo, Cheryl, additional, Lewis, Gareth, additional, Turner, Victoria, additional, Stark, Lloyd, additional, Fox, Elizabeth, additional, Amirapu, Anjana, additional, Park, Sangbin, additional, Lantz, Nicole, additional, Rankin, Anne E, additional, Kim, Seung K, additional, and Kockel, Lutz, additional

Published
2023
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8. Ka-band High-Rate Downlink System for the NISAR Mission

Author

Kobayashi, M. Michael, Pugh, Michael, Kuperman, Igor, Bell, David, Stocklin, Frank, El-Nimri, Salem, Johnson, Brad, Huynh, Nancy, Kelly, Shane, Nessel, James, Svitak, Andy, Williams, Tim, Linton, Nancy, Arciaga, Meghan, and Dissanayake, Asoka

Published
2018

9. Ka-band High-Rate Downlink System for the NISAR Mission

Author

Dissanayake, Asoka, Arciaga, Meghan, Linton, Nancy, Williams, Tim, Svitak, Andy, Nessel, James, Kelly, Shane, Huynh, Nancy, Johnson, Brad, El-Nimri, Salem, Stocklin, Frank, Bell, David, Kuperman, Igor, Pugh, Michael, and Kobayashi, M. Michael

Abstract

This paper provides a description and analyses of the high-rate Ka-band telecom system for the upcoming NISAR (NASA-ISRO Synthetic Aperture Radar) mission. NISAR is a collaborative Earth-Science mission between National Aeronautics and Space Administration (NASA) and Indian Space Research Organization (ISRO), which features an L-band SAR instrument and an S-band SAR instrument. The simultaneous dual-frequency radar system at peak rates will produce data at gigabit-per-second speeds, which drives the data-volume requirements. The key driving requirement for the payload communication subsystem is to provide a minimum of 26 Terabits per day of radar science data to the ground. The high-rate transmitter on the flight system is a software-defined radio developed at the Jet Propulsion Laboratory (JPL), based on the Universal Space Transponder platform, providing an offset quadrature phase shift key modulated waveform with Low-Density Parity-Check encoding of the data transfer frames. Two transmitters used in a dual-polarization configuration with each transmitter providing two giga-symbols per second (Gsps) of coded data provides an aggregate rate of four Gsps. In this system, only one watt of signal power is necessary on each polarization to overcome propagation losses and achieve a successful RF link. Several Near Earth Network (NEN) ground station sites (Alaska in the United States, Svalbard in Norway, and Punta Arenas in Chile) are baselined for the space-to-Earth communications link. Each ground station will also feature multiple upgrades to support NISAR’s transmission starting with new Ka-band antennas, wideband downconverters and high-rate receivers. In addition, a baseband data processor called Data Acquisition Processor and Handling Network Environment (DAPHNE), newly developed by the NEN, provides data storage and connectivity to backhaul networks. With NISAR’s large quantities of data (over 3.5 Petabytes over the mission), the processing of science data will be primarily performed on a cloud system to reduce the overall cost to the mission. The system described herein will be the first operational use of Gsps-class downlink rates on an Earth-Science mission.

Published
2018

10. Ka-band High-Rate Downlink System for the NISAR Mission

Author

Stocklin, Frank, Pugh, Michael, Kuperman, Igor, Bell, David, El-Nimri, Salem, Johnson, Brad, Huynh, Nancy, Kelly, Shane, Nessel, James, Svitak, Andy, Williams, Tim, Linton, Nancy, Arciaga, Meghan, and Dissanayake, Asoka

Published
2018

11. Systems biology-based analysis implicates a novel role for vitamin D metabolism in the pathogenesis of age-related macular degeneration

Author

Morrison Margaux A, Silveira Alexandra C, Huynh Nancy, Jun Gyungah, Smith Silvia E, Zacharaki Fani, Sato Hajime, Loomis Stephanie, Andreoli Michael T, Adams Scott M, Radeke Monte J, Jelcick Austin S, Yuan Yang, Tsiloulis Aristoteles N, Chatzoulis Dimitrios Z, Silvestri Giuliana, Kotoula Maria G, Tsironi Evangelia E, Hollis Bruce W, Chen Rui, Haider Neena B, Miller Joan W, Farrer Lindsay A, Hageman Gregory S, Kim Ivana K, Schaumberg Debra A, and DeAngelis Margaret M

Subjects
vitamin D, age-related macular degeneration, Medicine, Genetics, QH426-470
Abstract

Abstract Vitamin D has been shown to have anti-angiogenic properties and to play a protective role in several types of cancer, including breast, prostate and cutaneous melanoma. Similarly, vitamin D levels have been shown to be protective for risk of a number of conditions, including cardiovascular disease and chronic kidney disease, as well as numerous autoimmune disorders such as multiple sclerosis, inflammatory bowel diseases and type 1 diabetes mellitus. A study performed by Parekh et al. was the first to suggest a role for vitamin D in age-related macular degeneration (AMD) and showed a correlation between reduced serum vitamin D levels and risk for early AMD. Based on this study and the protective role of vitamin D in diseases with similar pathophysiology to AMD, we examined the role of vitamin D in a family-based cohort of 481 sibling pairs. Using extremely phenotypically discordant sibling pairs, initially we evaluated the association of neovascular AMD and vitamin D/sunlight-related epidemiological factors. After controlling for established AMD risk factors, including polymorphisms of the genes encoding complement factor H (CFH) and age-related maculopathy susceptibility 2/HtrA serine peptidase (ARMS2/HTRA1), and smoking history, we found that ultraviolet irradiance was protective for the development of neovascular AMD (p = 0.001). Although evaluation of serum vitamin D levels (25-hydroxyvitamin D [25(OH)D]) was higher in unaffected individuals than in their affected siblings, this finding did not reach statistical significance. Based on the relationship between ultraviolet irradiance and vitamin D production, we employed a candidate gene approach for evaluating common variation in key vitamin D pathway genes (the genes encoding the vitamin D receptor [VDR]; cytochrome P450, family 27, subfamily B, polypeptide 1 [CYP27B1]; cytochrome P450, family 24, subfamily A, polypeptide 1 [CYP24A1]; and CYP27A1) in this same family-based cohort. Initial findings were then validated and replicated in the extended family cohort, an unrelated case-control cohort from central Greece and a prospective nested case-control population from the Nurse's Health Study and Health Professionals Follow-Up Studies, which included patients with all subtypes of AMD for a total of 2,528 individuals. Single point variants in CYP24A1 (the gene encoding the catabolising enzyme of the vitamin D pathway) were demonstrated to influence AMD risk after controlling for smoking history, sex and age in all populations, both separately and, more importantly, in a meta-analysis. This is the first report demonstrating a genetic association between vitamin D metabolism and AMD risk. These findings were also supplemented with expression data from human donor eyes and human retinal cell lines. These data not only extend previous biological studies in the AMD field, but further emphasise common antecedents between several disorders with an inflammatory/immunogenic component such as cardiovascular disease, cancer and AMD.

Published
2011
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12. Ruthenium-Catalyzed Cycloadditions to Form 5-, 6- and 7-Membered Rings

Author

Doerksen, Rosalie S., Hodík, Tomáš, Hu, Guanyu, Huynh, Nancy O., Shuler, William G., and Krische, Michael J.

Subjects
Cyclization, Heterocyclic Compounds, Organometallic Compounds, Polycyclic Compounds, Stereoisomerism, Photochemical Processes, Oxidation-Reduction, Article, Catalysis, Ruthenium
Abstract

Ruthenium-catalyzed cycloadditions to form five-, six-, and seven-membered rings are summarized, including applications in natural product total synthesis. Content is organized by ring size and reaction type. Coverage is limited to processes that involve formation of at least one C-C bond. Processes that are stoichiometric in ruthenium or exploit ruthenium as a Lewis acid (without intervention of organometallic intermediates), ring formations that occur through dehydrogenative condensation-reduction, σ-bond activation-initiated annulations that do not result in net reduction of bond multiplicity, and photochemically promoted ruthenium-catalyzed cycloadditions are not covered.

Published
2021

13. Digital pins

Author

Huynh, Nancy Danh and Huynh, Nancy Danh

Abstract

Joan Flasch Artists' Book Collection

Published
2021

16. From Skin Infections to Ebola: Practice, Policy, and Beyond

Author

Mirza, Fatima N., Mirza, Humza N., Horien, Corey, and Huynh, Nancy

Subjects
Disease Detective, Health Security, The Centers for Disease Control (CDC), infectious disease, public health, Ebola, Field Epidemiology, Interview, Global Health, policy, skin infections
Published
2017

18. The NEI/NCBI dbGAP database: Genotypes and haplotypes that may specifically predispose to risk of neovascular age-related macular degeneration

Author

Miller Joan W, Brown Alison, Regan Maureen, Huynh Nancy, Andreoli Michael, Adams Scott, DeWan Andy, Morrison Margaux A, Zhang Hong, Kim Ivana K, Hoh Josephine, and DeAngelis Margaret M

Subjects
Internal medicine, RC31-1245, Genetics, QH426-470
Abstract

Abstract Background To examine if the significantly associated SNPs derived from the genome wide allelic association study on the AREDS cohort at the NEI (dbGAP) specifically confer risk for neovascular age-related macular degeneration (AMD). We ascertained 134 unrelated patients with AMD who had one sibling with an AREDS classification 1 or less and was past the age at which the affected sibling was diagnosed (268 subjects). Genotyping was performed by both direct sequencing and Sequenom iPLEX system technology. Single SNP analyses were conducted with McNemar's Test (both 2 × 2 and 3 × 3 tests) and likelihood ratio tests (LRT). Conditional logistic regression was used to determine significant gene-gene interactions. LRT was used to determine the best fit for each genotypic model tested (additive, dominant or recessive). Results Before release of individual data, p-value information was obtained directly from the AREDS dbGAP website. Of the 35 variants with P < 10-6 examined, 23 significantly modified risk of neovascular AMD. Many variants located in tandem on 1q32-q22 including those in CFH, CFHR4, CFHR2, CFHR5, F13B, ASPM and ZBTB were significantly associated with AMD risk. Of these variants, single SNP analysis revealed that CFH rs572515 was the most significantly associated with AMD risk (P < 10-6). Haplotype analysis supported our findings of single SNP association, demonstrating that the most significant haplotype, GATAGTTCTC, spanning CFH, CFHR4, and CFHR2 was associated with the greatest risk of developing neovascular AMD (P < 10-6). Other than variants on 1q32-q22, only two SNPs, rs9288410 (MAP2) on 2q34-q35 and rs2014307 (PLEKHA1/HTRA1) on 10q26 were significantly associated with AMD status (P = .03 and P < 10-6 respectively). After controlling for smoking history, gender and age, the most significant gene-gene interaction appears to be between rs10801575 (CFH) and rs2014307 (PLEKHA1/HTRA1) (P < 10-11). The best genotypic fit for rs10801575 and rs2014307 was an additive model based on LRT. After applying a Bonferonni correction, no other significant interactions were identified between any other SNPs. Conclusion This is the first replication study on the NEI dbGAP SNPs, demonstrating that alleles on 1q, 2q and 10q may predispose an individual to AMD.

Published
2008
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19. Reply

Author

Huynh, Nancy, primary, Fares, Wassim H., additional, Lee, Alfred I., additional, Dardik, Alan, additional, Sarac, Timur, additional, and Ochoa Chaar, Cassius Iyad, additional

Published
2018
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21. Visual Acuity after Cataract Surgery in Patients with Age-Related Macular Degeneration. Age-Related Eye Disease Study 2 Report No. 5

Author

Huynh, Nancy, Nicholson, Benjamin P., Agrón, Elvira, Clemons, Traci E., Bressler, Susan B., Rosenfeld, Philip J., and Chew, Emily Y.

Subjects
Aged, 80 and over, Male, Phacoemulsification, Pseudophakia, Lutein, Visual Acuity, Vitamins, Middle Aged, Xanthophylls, Severity of Illness Index, Article, Cataract, Cohort Studies, Macular Degeneration, Lens Implantation, Intraocular, Zeaxanthins, Dietary Supplements, Fatty Acids, Omega-3, Humans, Female, Prospective Studies, Aged
Abstract

To evaluate visual acuity outcomes after cataract surgery in persons with varying degrees of severity of age-related macular degeneration (AMD).Cohort study.A total of 1232 eyes of 793 participants who underwent cataract surgery during the Age-Related Eye Disease Study 2, a prospective, multicenter, randomized controlled trial of nutritional supplements for treatment of AMD.Preoperative and postoperative characteristics of participants who underwent cataract extraction during the 5-year trial were analyzed. Both clinical data and standardized red-reflex lens and fundus photographs were obtained at baseline and annually. Photographs were graded by a centralized reading center for cortical and posterior subcapsular lens opacities and for AMD severity. Cataract surgery was documented at annual study visits or by history during the 6-month telephone calls. Analyses were conducted using multivariate repeated-measures regression.Change in best-corrected visual acuity (BCVA) after cataract surgery compared with preoperative BCVA.Adjusting for age at time of surgery, gender, interval between preoperative and postoperative visits, and type and severity of cataract, the mean changes in visual acuity were as follows: eyes with mild AMD (n = 30) gained 11.2 letters (95% confidence interval [CI], 6.9-15.5), eyes with moderate AMD (n = 346) gained 11.1 letters (95% CI, 9.1-13.2), eyes with severe AMD (n = 462) gained 8.7 letters (95% CI, 6.7-10.7), eyes with noncentral geographic atrophy (n = 70) gained 8.9 letters (95% CI, 5.8-12.1), and eyes with advanced AMD (central geographic atrophy, neovascular disease, or both; n = 324) gained 6.8 letters (95% CI, 4.9-8.8). The visual acuity gain across all AMD severity groups was statistically significant from preoperative values (P 0.0001).Mean visual acuities improved significantly after cataract surgery across varying degrees of AMD severity.

Published
2014

27. Mechanisms controlling vacuolar H+-adenosine triphosphatase activity: targets for the development of new therapeutic agents for the management of osteoporosis

Author

Holliday,L Shannon, Huynh,Nancy, Zuo,Jian, Toro,Edgardo J, Holliday,L Shannon, Huynh,Nancy, Zuo,Jian, and Toro,Edgardo J

Abstract

L Shannon Holliday,1,2 Nancy Huynh,1 Jian Zuo,1 Edgardo J Toro1,31Department of Orthodontics, University of Florida College of Dentistry, Gainesville, FL, USA; 2Department of Anatomy and Cell Biology, University of Florida College of Medicine, Gainesville, FL, USA; 3Department of Advanced Graduate Dental Education, University of Puerto Rico School of Dental Medicine, San Juan, Puerto RicoAbstract: Recent genetic studies show that mutations in vacuolar H+-adenosine triphosphatase (V-ATPase) subunit isoforms that are selectively expressed in osteoclasts (a3 and d2) lead to both reduced bone resorption and increased bone formation. This implies that pharmaceuticals targeting these subunits or activities that are linked to these subunits might prove to be bone anabolic. The fact that V-ATPase is a ubiquitous "housekeeping" enzyme has made it challenging to directly target the enzymatic activity of the subset of V-ATPases involved in bone resorption; however, the unique mechanisms that control the V-ATPases involved in bone resorption have begun to emerge. These include binding interactions with the cytoskeleton and with proteins involved in regulating the cytoskeleton and membrane trafficking, links to glycolysis, and surprising ties to the renin–angiotensin signaling network. Links between controlling mechanisms and subunit a3 have been identified, suggesting that it may be possible to develop agents that disrupt bone resorptive V-ATPase activity while leaving the housekeeping activities unhindered. The first steps toward using this new information to rationally design novel classes of therapeutic agents have been taken. Such agents might selectively act against osteoclasts both to prevent the initiation of osteoporosis and to restore already-compromised bone.Keywords: vacuolar H+-ATPase, enoxacin, luteolin, computational chemistry, microfilaments, ARF6

Published
2013

29. The NEI/NCBI dbGAP database: Genotypes and haplotypes that may specifically predispose to risk of neovascular age-related macular degeneration

Author

Zhang, Hong, primary, Morrison, Margaux A, additional, DeWan, Andy, additional, Adams, Scott, additional, Andreoli, Michael, additional, Huynh, Nancy, additional, Regan, Maureen, additional, Brown, Alison, additional, Miller, Joan W, additional, Kim, Ivana K, additional, Hoh, Josephine, additional, and DeAngelis, Margaret M, additional

Published
2008
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31. Mechanisms controlling vacuolar H+-adenosine triphosphatase activity: targets for the development of new therapeutic agents for the management of osteoporosis.

Author

Holliday, L. Shannon, Huynh, Nancy, Zuo, Jian, and Toro, Edgardo J.

Subjects
GENETIC mutation, ADENOSINE triphosphatase, OSTEOCLASTS, BONE resorption, CYTOSKELETON, CELLULAR control mechanisms
Abstract

Recent genetic studies show that mutations in vacuolar H+-adenosine triphosphatase (V-ATPase) subunit isoforms that are selectively expressed in osteoclasts (a3 and d2) lead to both reduced bone resorption and increased bone formation. This implies that pharmaceuticals targeting these subunits or activities that are linked to these subunits might prove to be bone anabolic. The fact that V-ATPase is a ubiquitous "housekeeping" enzyme has made it challenging to directly target the enzymatic activity of the subset of V-ATPases involved in bone resorption; however, the unique mechanisms that control the V-ATPases involved in bone resorption have begun to emerge. These include binding interactions with the cytoskeleton and with proteins involved in regulating the cytoskeleton and membrane trafficking, links to glycolysis, and surprising ties to the renin--angiotensin signaling network. Links between controlling mechanisms and subunit a3 have been identified, suggesting that it may be possible to develop agents that disrupt bone resorptive V-ATPase activity while leaving the housekeeping activities unhindered. The first steps toward using this new information to rationally design novel classes of therapeutic agents have been taken. Such agents might selectively act against osteoclasts both to prevent the initiation of osteoporosis and to restore already-compromised bone. [ABSTRACT FROM AUTHOR]

Published
2013
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32. The NEI/NCBI dbGAP database: Genotypes and haplotypes that may specifically predispose to risk of neovascular age-related macular degeneration.

Author

Hong Zhang, Morrison, Margaux A., DeWan, Andy, Adams, Scott, Andreoli, Michael, Huynh, Nancy, Regan, Maureen, Brown, Alison, Miller, Joan W., Kim, Ivana K., Hoh, Josephine, and DeAngelis, Margaret M.

Subjects
GENOMES, DISEASE risk factors, RETINAL degeneration, DISEASES in older people, GENES, MEDICAL genetics
Abstract

Background: To examine if the significantly associated SNPs derived from the genome wide allelic association study on the AREDS cohort at the NEI (dbGAP) specifically confer risk for neovascular age-related macular degeneration (AMD). We ascertained 134 unrelated patients with AMD who had one sibling with an AREDS classification 1 or less and was past the age at which the affected sibling was diagnosed (268 subjects). Genotyping was performed by both direct sequencing and Sequenom iPLEX system technology. Single SNP analyses were conducted with McNemar's Test (both 2 x 2 and 3 x 3 tests) and likelihood ratio tests (LRT). Conditional logistic regression was used to determine significant gene-gene interactions. LRT was used to determine the best fit for each genotypic model tested (additive, dominant or recessive). Results: Before release of individual data, p-value information was obtained directly from the AREDS dbGAP website. Of the 35 variants with P < 10-6 examined, 23 significantly modified risk of neovascular AMD. Many variants located in tandem on 1q32-q22 including those in CFH, CFHR4, CFHR2, CFHR5, F13B, ASPM and ZBTB were significantly associated with AMD risk. Of these variants, single SNP analysis revealed that CFH rs572515 was the most significantly associated with AMD risk (P < 10-6). Haplotype analysis supported our findings of single SNP association, demonstrating that the most significant haplotype, GATAGTTCTC, spanning CFH, CFHR4, and CFHR2 was associated with the greatest risk of developing neovascular AMD (P < 10-6). Other than variants on 1q32-q22, only two SNPs, rs9288410 (MAP2) on 2q34-q35 and rs2014307 (PLEKHA1/HTRA1) on 10q26 were significantly associated with AMD status (P = .03 and P < 10-6 respectively). After controlling for smoking history, gender and age, the most significant gene-gene interaction appears to be between rs10801575 (CFH) and rs2014307 (PLEKHA1/HTRA1) (P < 10-11). The best genotypic fit for rs10801575 and rs2014307 was an additive model based on LRT. After applying a Bonferonni correction, no other significant interactions were identified between any other SNPs. Conclusion: This is the first replication study on the NEI dbGAP SNPs, demonstrating that alleles on 1q, 2q and 10q may predispose an individual to AMD. [ABSTRACT FROM AUTHOR]

Published
2008
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33. Dilated fundus exam and associated findings in spontaneous subconjunctival haemorrhage.

Author

Huynh, Nancy, Wang, Jay, and Vavvas, Demetrios

Subjects
*TREATMENT of eye diseases, *RETINAL diseases, *HEMORRHAGE treatment, *WARFARIN, *DRUG therapy, *ANTIHISTAMINES, *PATIENTS, *THERAPEUTICS
Abstract

The article focuses on a study for investigating the yield of a dilated fundus exam in patients with spontaneous non-traumatic subconjunctival haemorrhage (SCH) and associated risk factor. It mentions biilateral SCH has been associated with more serious pathology such as scurvy, haematological dyscrasia and ocular or systemic malignancy. It also mentions use of warfarin and antihistamine for treatment of SCH.

Published
2017
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34. Generation of LexA enhancer-trap lines in Drosophila by an international scholastic network.

Author

Kim ES, Rajan A, Chang K, Govindarajan S, Gulick C, English E, Rodriguez B, Bloomfield O, Nakada S, Beard C, O'Connor S, Mastroianni S, Downey E, Feigenbaum M, Tolentino C, Pace A, Khan M, Moon S, DiPrima J, Syed A, Lin F, Abukhadra Y, Bacon I, Beckerle J, Cho S, Donkor NE, Garberg L, Harrington A, Hoang M, Lawani N, Noori A, Park E, Parsons E, Oravitan P, Chen M, Molina C, Richmond C, Reddi A, Huang J, Shugrue C, Coviello R, Unver S, Indelicarto M, Islamovic E, McIlroy R, Yang A, Hamad M, Griffin E, Ahmed Z, Alla A, Fitzgerald P, Choi A, Das T, Cheng Y, Yu J, Roderiques T, Lee E, Liu L, Harper J, Wang J, Suhr C, Tan M, Luque J, Tam AR, Chen E, Triff M, Zimmermann L, Zhang E, Wood J, Clark K, Kpodonu N, Dey A, Ecker A, Chuang M, López RKS, Sun H, Wei Z, Stone H, Chi CYJ, Silvestri A, Orloff P, Nedumaran N, Zou A, Ünver L, Page O, Kim M, Chan TYT, Tulloch A, Hernandez A, Pillai A, Chen C, Chowdhury N, Huang L, Mudide A, Paik G, Wingate A, Quinn L, Conybere C, Baumgardt LL, Buckley R, Kolberg Z, Pattison R, Shazli AA, Ganske P, Sfragara L, Strub A, Collier B, Tamana H, Ravindran D, Howden J, Stewart M, Shimizu S, Braniff J, Fong M, Gutman L, Irvine D, Malholtra S, Medina J, Park J, Yin A, Abromavage H, Barrett B, Chen J, Cho R, Dilatush M, Gaw G, Gu C, Huang J, Kilby H, Markel E, McClure K, Phillips W, Polaski B, Roselli A, Saint-Cyr S, Shin E, Tatum K, Tumpunyawat T, Wetherill L, Ptaszynska S, Zeleznik M, Pesendorfer A, Nolan A, Tao J, Sammeta D, Nicholson L, Dinh GV, Foltz M, Vo A, Ross M, Tokarski A, Hariharan S, Wang E, Baziuk M, Tay A, Wong YHM, Floyd J, Cui A, Pierre K, Coppisetti N, Kutam M, Khurjekar D, Gadzi A, Gubbay B, Pedretti S, Belovich S, Yeung T, Fey M, Shaffer L, Li A, Beritela G, Huyghue K, Foster G, Durso-Finley G, Thierfelder Q, Kiernan H, Lenkowsky A, Thomas T, Cheng N, Chao O, L'Etoile-Goga P, King A, McKinley P, Read N, Milberg D, Lin L, Wong M, Gilman I, Brown S, Chen L, Kosai J, Verbinsky M, Belshaw-Hood A, Lee H, Zhou C, Lobo M, Tse A, Tran K, Lewis K, Sonawane P, Ngo J, Zuzga S, Chow L, Huynh V, Yang W, Lim S, Stites B, Chang S, Cruz-Balleza R, Pelta M, Kujawski S, Yuan C, Standen-Bloom E, Witt O, Anders K, Duane A, Huynh N, Lester B, Fung-Lee S, Fung M, Situ M, Canigiula P, Dijkgraaf M, Romero W, Baula SK, Wong K, Xu I, Martinez B, Nuygen R, Norris L, Nijensohn N, Altman N, Maajid E, Burkhardt O, Chanda J, Doscher C, Gopal A, Good A, Good J, Herrera N, Lanting L, Liem S, Marks A, McLaughlin E, Lee A, Mohr C, Patton E, Pyarali N, Oczon C, Richards D, Good N, Goss S, Khan A, Madonia R, Mitchell V, Sun N, Vranka T, Garcia D, Arroyo F, Morales E, Camey S, Cano G, Bernabe A, Arroyo J, Lopez Y, Gonzalez E, Zumba B, Garcia J, Vargas E, Trinidad A, Candelaria N, Valdez V, Campuzano F, Pereznegron E, Medrano J, Gutierrez J, Gutierrez E, Abrego ET, Gutierrez D, Ortiz C, Barnes A, Arms E, Mitchell L, Balanzá C, Bradford J, Detroy H, Ferguson D, Guillermo E, Manapragada A, Nanula D, Serna B, Singh K, Sramaty E, Wells B, Wiggins M, Dowling M, Schmadeke G, Cafferky S, Good S, Reese M, Fleig M, Gannett A, Cain C, Lee M, Oberto P, Rinehart J, Pan E, Mathis SA, Joiner J, Barr L, Evans CJ, Baena-Lopez A, Beatty A, Collette J, Smullen R, Suttie J, Chisholm T, Rotondo C, Lewis G, Turner V, Stark L, Fox E, Amirapu A, Park S, Lantz N, Rankin AE, Kim SK, and Kockel L

Subjects
Animals, Gene Expression Regulation, Enhancer Elements, Genetic, Drosophila genetics, Drosophila metabolism, Drosophila Proteins genetics, Drosophila Proteins metabolism
Abstract

Conditional gene regulation in Drosophila through binary expression systems like the LexA-LexAop system provides a superb tool for investigating gene and tissue function. To increase the availability of defined LexA enhancer trap insertions, we present molecular, genetic, and tissue expression studies of 301 novel Stan-X LexA enhancer traps derived from mobilization of the index SX4 line. This includes insertions into distinct loci on the X, II, and III chromosomes that were not previously associated with enhancer traps or targeted LexA constructs, an insertion into ptc, and seventeen insertions into natural transposons. A subset of enhancer traps was expressed in CNS neurons known to produce and secrete insulin, an essential regulator of growth, development, and metabolism. Fly lines described here were generated and characterized through studies by students and teachers in an international network of genetics classes at public, independent high schools, and universities serving a diversity of students, including those underrepresented in science. Thus, a unique partnership between secondary schools and university-based programs has produced and characterized novel resources in Drosophila, establishing instructional paradigms devoted to unscripted experimental science., Competing Interests: Conflicts of interest statement The author(s) declare no conflict of interest., (© The Author(s) 2023. Published by Oxford University Press on behalf of The Genetics Society of America.)

Published
2023
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