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1,193 results on '"AVILA, A. C."'

1. Entomological survey and 'Leishmania 'Leishmania) mexicana' prevalence in sand fly species during an outbreak of cutaneous leishmaniasis in Quintana Roo State, Mexico

Author

Caneda-Guzman, Isabel C, de Oca-Aguilar, Ana C Montes, Miranda-Caballero, Carlos I, Grostieta, Estefania, Correa-Morales, Fabian, Romero-Perez, Raquel, Romero-Contreras, Francisco E, Rodriguez-Atanacio, Jose A, Ruiz-Tovar, Karina, Huerta, Heron, Mis-Avila, Pedro C, Quintanilla-Cedillo, Marco R, Lammoglia-Villagomez, Miguel A, Blum-Dominguez, Selene, Tamay-Segovia, Paulino, Rojas-Ronquillo, Rebeca, Sanchez-Montes, Sokani, and Becker, Ingeborg

Published
2023

3. Numerical modeling of the influence of randomly macroscopic inhomogeneities on the magnetic induction and temperature dynamics of a high-T$_c$ superconducting slab

Author

Romero-Salazar, C., Valdés-Negrin, P. L., Ávila-Crisóstomo, C. E., Hernández-Flores, O. A., Cortés-Maldonado, R., Chabanenko, V., and Pérez-Rodríguez, F.

Subjects
Condensed Matter - Superconductivity, Physics - Applied Physics
Abstract

In this study we perform numerical calculations of the spatial and time variation of the magnetic induction, current density and temperature in an infinite superconducting slab with macroscopic inhomogeneities. We also modeled an homogeneuos superconductor as a referential material, considering characteristic magnetothermal properties of a high-T$_c$ single crystal. The theoretical formalism is enclosed in the dynamical regime and a continuum electrodynamic approach. In particular, we studied the correlation between the magnetic jumps and temperature rise occurrence with the presence of macroscopical inhomogeneities, modeled through an stochastic current-carrying ability spatial profile.

Published
2022

5. Association between particulate air pollution and hypertensive disorders in pregnancy: A retrospective cohort study

Author

Sun, Yi, Bhuyan, Rashmi, Jiao, Anqi, Avila, Chantal C., Chiu, Vicki Y., Slezak, Jeff M., Sacks, David A., Molitor, John, Benmarhnia, Tarik, Chen, Jiu-Chiuan, Getahun, Darios, and Wu, Jun

Subjects
United States. Environmental Protection Agency -- Analysis, Health maintenance organizations -- Analysis -- Research, Pollutants -- Analysis -- Research, Pregnancy -- Research -- Analysis, Pregnant women -- Analysis -- Research, Sulfates -- Analysis -- Research, Air pollution -- Research -- Analysis, Hypertension -- Research, African Americans -- Analysis -- Research, Biological sciences, World Health Organization, Kaiser Permanente
Abstract

Background Epidemiological findings regarding the association of particulate matter [less than or equal to]2.5 [mu]m (PM.sub.2.5) exposure with hypertensive disorders in pregnancy (HDP) are inconsistent; evidence for HDP risk related to PM.sub.2.5 components, mixture effects, and windows of susceptibility is limited. We aimed to investigate the relationships between HDP and exposure to PM.sub.2.5 during pregnancy. Methods and findings A large retrospective cohort study was conducted among mothers with singleton pregnancies in Kaiser Permanente Southern California from 2008 to 2017. HDP were defined by International Classification of Diseases-9/10 (ICD-9/10) diagnostic codes and were classified into 2 subcategories based on the severity of HDP: gestational hypertension (GH) and preeclampsia and eclampsia (PE-E). Monthly averages of PM.sub.2.5 total mass and its constituents (i.e., sulfate, nitrate, ammonium, organic matter, and black carbon) were estimated using outputs from a fine-resolution geoscience-derived model. Multilevel Cox proportional hazard models were used to fit single-pollutant models; quantile g-computation approach was applied to estimate the joint effect of PM.sub.2.5 constituents. The distributed lag model was applied to estimate the association between monthly exposure and HDP risk. This study included 386,361 participants (30.3 ± 6.1 years) with 4.8% (17,977/373,905) GH and 5.0% (19,381/386,361) PE-E cases, respectively. In single-pollutant models, we observed increased relative risks for PE-E associated with exposures to PM.sub.2.5 total mass [adjusted hazard ratio (HR) per interquartile range: 1.07, 95% confidence interval (CI) [1.04, 1.10] p < 0.001], black carbon [HR = 1.12 (95% CI [1.08, 1.16] p < 0.001)] and organic matter [HR = 1.06 (95% CI [1.03, 1.09] p < 0.001)], but not for GH. The population attributable fraction for PE-E corresponding to the standards of the US Environmental Protection Agency (9 [mu]g/m.sup.3) was 6.37%. In multi-pollutant models, the PM.sub.2.5 mixture was associated with an increased relative risk of PE-E ([HR = 1.05 (95% CI [1.03, 1.07] p < 0.001)], simultaneous increase in PM.sub.2.5 constituents of interest by a quartile) and PM.sub.2.5 black carbon gave the greatest contribution of the overall mixture effects (71%) among all individual constituents. The susceptible window is the late first trimester and second trimester. Furthermore, the risks of PE-E associated with PM.sub.2.5 exposure were significantly higher among Hispanic and African American mothers and mothers who live in low- to middle-income neighborhoods (p < 0.05 for Cochran's Q test). Study limitations include potential exposure misclassification solely based on residential outdoor air pollution, misclassification of disease status defined by ICD codes, the date of diagnosis not reflecting the actual time of onset, and lack of information on potential covariates and unmeasured factors for HDP. Conclusions Our findings add to the literature on associations between air pollution exposure and HDP. To our knowledge, this is the first study reporting that specific air pollution components, mixture effects, and susceptible windows of PM.sub.2.5 may affect GH and PE-E differently., Author(s): Yi Sun 1,2, Rashmi Bhuyan 2,3,4, Anqi Jiao 2, Chantal C. Avila 5, Vicki Y. Chiu 5, Jeff M. Slezak 5, David A. Sacks 5,6, John Molitor 7, Tarik [...]

Published
2024
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11. Anti-PLA2R Antibody Levels and Clinical Risk Factors for Treatment Nonresponse in Membranous Nephropathy

Author

Barbour, Sean J., Fervenza, Fernando C., Induruwage, Dilshani, Brenchley, Paul E., Rovin, Brad, Hladunewich, Michelle A., Reich, Heather N., Lafayette, Richard, Aslam, Nabeel, Appel, Gerald B., Zand, Ladan, Kiryluk, Krzysztof, Liu, Lili, Cattran, Daniel C., Fervenza, F.C., Cattran, D.C., Appel, J., Gipson, D., Kretzler, M., Rovin, B., Fervenza, F.C., Lieske, J.C., Leung, N., Erickson, S.B., Radhakrishnan, J., Bomback, A., Hogan, J., Canetta, P., Ahn, W., Lafayette, R., Arora, N., Nargund, P., Rovin, B., Alvarado, A., Parikh, S., Hebert, L.A., Aslam, N., Gipson, P., Kretzler, M., Plattner, B., Gipson, D., Mariani, L., Garg, P., Rao, P., Sedor, J., O’Toole, J., Jefferson, J.A., Nelson, P.J., McCarthy, E., Yarlagadda, S., Jain, N., Rizk, D., Simon, J., Gebreselassie, S., Blumenthal, S., Beara-Lasic, L., Zhdanova, O., Thomas, L., Cohen, I., Keddis, M., Sussman, A., Thajudeen, B., Fulop, T., Craici, I., Wagner, S., Dreisbach, A., Monga, D., Green, D., Mattiazzi, A., Nayer, A., Thomas, D., Barisoni, L., Li, T., Vijayan, A., Juncos, L., Cattran, D.C., Reich, H., Hladunewich, M., Barbour, S., Levin, A., Philibert, D., Mac-Way, F., Desmeules, S., Ankawi, G., Sethi, S., Avila-Casado, C., and Brenchley, P.

Published
2023
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14. Author Correction: Association study in African-admixed populations across the Americas recapitulates asthma risk loci in non-African populations.

Author

Daya, Michelle, Rafaels, Nicholas, Brunetti, Tonya M, Chavan, Sameer, Levin, Albert M, Shetty, Aniket, Gignoux, Christopher R, Boorgula, Meher Preethi, Wojcik, Genevieve, Campbell, Monica, Vergara, Candelaria, Torgerson, Dara G, Ortega, Victor E, Doumatey, Ayo, Johnston, Henry Richard, Acevedo, Nathalie, Araujo, Maria Ilma, Avila, Pedro C, Belbin, Gillian, Bleecker, Eugene, Bustamante, Carlos, Caraballo, Luis, Cruz, Alvaro, Dunston, Georgia M, Eng, Celeste, Faruque, Mezbah U, Ferguson, Trevor S, Figueiredo, Camila, Ford, Jean G, Gan, Weiniu, Gourraud, Pierre-Antoine, Hansel, Nadia N, Hernandez, Ryan D, Herrera-Paz, Edwin Francisco, Jiménez, Silvia, Kenny, Eimear E, Knight-Madden, Jennifer, Kumar, Rajesh, Lange, Leslie A, Lange, Ethan M, Lizee, Antoine, Maul, Pissamai, Maul, Trevor, Mayorga, Alvaro, Meyers, Deborah, Nicolae, Dan L, O'Connor, Timothy D, Oliveira, Ricardo Riccio, Olopade, Christopher O, Olopade, Olufunmilayo, Qin, Zhaohui S, Rotimi, Charles, Vince, Nicolas, Watson, Harold, Wilks, Rainford J, Wilson, James G, Salzberg, Steven, Ober, Carole, Burchard, Esteban G, Williams, L Keoki, Beaty, Terri H, Taub, Margaret A, Ruczinski, Ingo, Mathias, Rasika A, Barnes, Kathleen C, and CAAPA

Subjects
CAAPA
Abstract

An amendment to this paper has been published and can be accessed via a link at the top of the paper.

Published
2019

15. Genome‐wide association study of inhaled corticosteroid response in admixed children with asthma

Author

Hernandez‐Pacheco, Natalia, Farzan, Niloufar, Francis, Ben, Karimi, Leila, Repnik, Katja, Vijverberg, Susanne J, Soares, Patricia, Schieck, Maximilian, Gorenjak, Mario, Forno, Erick, Eng, Celeste, Oh, Sam S, Pérez‐Méndez, Lina, Berce, Vojko, Tavendale, Roger, Samedy, Lesly‐Anne, Hunstman, Scott, Hu, Donglei, Meade, Kelley, Farber, Harold J, Avila, Pedro C, Serebrisky, Denise, Thyne, Shannon M, Brigino‐Buenaventura, Emerita, Rodriguez‐Cintron, William, Sen, Saunak, Kumar, Rajesh, Lenoir, Michael, Rodriguez‐Santana, Jose R, Celedón, Juan C, Mukhopadhyay, Somnath, Potočnik, Uroš, Pirmohamed, Munir, Verhamme, Katia M, Kabesch, Michael, Palmer, Colin NA, Hawcutt, Daniel B, Flores, Carlos, der Zee, Anke H Maitland‐van, Burchard, Esteban G, and Pino‐Yanes, Maria

Subjects
Biomedical and Clinical Sciences, Immunology, Human Genome, Asthma, Genetics, Clinical Research, Lung, Respiratory, Administration, Inhalation, Adolescent, Adrenal Cortex Hormones, Child, Cytidine Deaminase, DNA-Binding Proteins, Female, GTPase-Activating Proteins, Genome-Wide Association Study, Humans, Male, Minor Histocompatibility Antigens, African American, childhood asthma, exacerbations, Latino, pharmacogenomics, Nutrition and Dietetics, Public Health and Health Services, Allergy
Abstract

BackgroundInhaled corticosteroids (ICS) are the most widely prescribed and effective medication to control asthma symptoms and exacerbations. However, many children still have asthma exacerbations despite treatment, particularly in admixed populations, such as Puerto Ricans and African Americans. A few genome-wide association studies (GWAS) have been performed in European and Asian populations, and they have demonstrated the importance of the genetic component in ICS response.ObjectiveWe aimed to identify genetic variants associated with asthma exacerbations in admixed children treated with ICS and to validate previous GWAS findings.MethodsA meta-analysis of two GWAS of asthma exacerbations was performed in 1347 admixed children treated with ICS (Hispanics/Latinos and African Americans), analysing 8.7 million genetic variants. Those with P ≤ 5 × 10-6 were followed up for replication in 1697 asthmatic patients from six European studies. Associations of ICS response described in published GWAS were followed up for replication in the admixed populations.ResultsA total of 15 independent variants were suggestively associated with asthma exacerbations in admixed populations (P ≤ 5 × 10-6 ). One of them, located in the intergenic region of APOBEC3B and APOBEC3C, showed evidence of replication in Europeans (rs5995653, P = 7.52 × 10-3 ) and was also associated with change in lung function after treatment with ICS (P = 4.91 × 10-3 ). Additionally, the reported association of the L3MBTL4-ARHGAP28 genomic region was confirmed in admixed populations, although a different variant was identified.Conclusions and clinical relevanceThis study revealed the novel association of APOBEC3B and APOBEC3C with asthma exacerbations in children treated with ICS and replicated previously identified genomic regions. This contributes to the current knowledge about the multiple genetic markers determining responsiveness to ICS which could lead in the future the clinical identification of those asthma patients who are not able to respond to such treatment.

Published
2019

16. A genome-wide association and admixture mapping study of bronchodilator drug response in African Americans with asthma

Author

Spear, Melissa L, Hu, Donglei, Pino-Yanes, Maria, Huntsman, Scott, Eng, Celeste, Levin, Albert M, Ortega, Victor E, White, Marquitta J, McGarry, Meghan E, Thakur, Neeta, Galanter, Joshua, Mak, Angel CY, Oh, Sam S, Ampleford, Elizabeth, Peters, Stephen P, Davis, Adam, Kumar, Rajesh, Farber, Harold J, Meade, Kelley, Avila, Pedro C, Serebrisky, Denise, Lenoir, Michael A, Brigino-Buenaventura, Emerita, Cintron, William Rodriguez, Thyne, Shannon M, Rodriguez-Santana, Jose R, Ford, Jean G, Chapela, Rocio, Estrada, Andrés Moreno, Sandoval, Karla, Seibold, Max A, Winkler, Cheryl A, Bleecker, Eugene R, Myers, Deborah A, Williams, L Keoki, Hernandez, Ryan D, Torgerson, Dara G, and Burchard, Esteban G

Subjects
Pharmacology and Pharmaceutical Sciences, Biomedical and Clinical Sciences, Lung, Genetics, Asthma, Human Genome, Respiratory, Pharmacology & Pharmacy, Pharmacology and pharmaceutical sciences
Abstract

Short-acting β2-adrenergic receptor agonists (SABAs) are the most commonly prescribed asthma medications worldwide. Response to SABAs is measured as bronchodilator drug response (BDR), which varies among racial/ethnic groups in the United States. However, the genetic variation that contributes to BDR is largely undefined in African Americans with asthma. To identify genetic variants that may contribute to differences in BDR in African Americans with asthma, we performed a genome-wide association study (GWAS) of BDR in 949 African-American children with asthma, genotyped with the Axiom World Array 4 (Affymetrix, Santa Clara, CA) followed by imputation using 1000 Genomes phase III genotypes. We used linear regression models adjusting for age, sex, body mass index (BMI) and genetic ancestry to test for an association between BDR and genotype at single-nucleotide polymorphisms (SNPs). To increase power and distinguish between shared vs. population-specific associations with BDR in children with asthma, we performed a meta-analysis across 949 African Americans and 1830 Latinos (total = 2779). Finally, we performed genome-wide admixture mapping to identify regions whereby local African or European ancestry is associated with BDR in African Americans. We identified a population-specific association with an intergenic SNP on chromosome 9q21 that was significantly associated with BDR (rs73650726, p = 7.69 × 10-9). A trans-ethnic meta-analysis across African Americans and Latinos identified three additional SNPs within the intron of PRKG1 that were significantly associated with BDR (rs7903366, rs7070958 and rs7081864, p ≤ 5 × 10-8). Our results failed to replicate in three additional populations of 416 Latinos and 1615 African Americans. Our findings indicate that both population-specific and shared genetic variation contributes to differences in BDR in minority children with asthma, and that the genetic underpinnings of BDR may differ between racial/ethnic groups.

Published
2019

17. Acculturation is associated with asthma burden and pulmonary function in Latino youth: The GALA II study

Author

Thakur, Neeta, Borrell, Luisa N, Ye, Morgan, Oh, Sam S, Eng, Celeste, Meade, Kelley, Avila, Pedro C, Farber, Harold J, Serebrisky, Denise, Brigino-Buenaventura, Emerita, Rodriguez-Cintron, William, Kumar, Rajesh, Bibbins-Domingo, Kirsten, Thyne, Shannon, Sen, Saunak, Rodriguez-Santana, Jose R, and Burchard, Esteban G

Subjects
Biomedical and Clinical Sciences, Immunology, Asthma, Behavioral and Social Science, Basic Behavioral and Social Science, Pediatric, Lung, Clinical Research, Respiratory, Acculturation, Adolescent, Adult, Case-Control Studies, Child, Female, Forced Expiratory Volume, Hispanic or Latino, Humans, Male, Young Adult, Latino, asthma, acculturation, pediatric, health disparities, social determinants of health, Allergy
Abstract

BackgroundAcculturation is an important predictor of asthma in Latino youth, specifically Mexican Americans. Less is known about acculturation and pulmonary function measures.ObjectiveWe sought to estimate the association of acculturation measures with asthma and pulmonary function in Latino youth and determine whether this association varies across Latino subgroups.MethodsWe included 1849 Latinos (302 Caribbean Spanish, 193 Central or South Americans, 1136 Mexican Americans, and 218 other Latino children) aged 8 to 21 years from 4 urban regions in the United States. Acculturation measures include nativity status, age of immigration, language of preference, and generation in the United States. We used multivariable logistic and linear regression models to quantify the association of acculturation factors with the presence of asthma (case-control study) and pulmonary function (case-only study), adjusting for demographic, socioenvironmental, and clinical variables.ResultsFor all acculturation measures (nativity status, age of immigration, language of preference, and generation in the United States), greater levels of acculturation were associated with greater odds of asthma. Among cases, high (English preference) and medium (equal preference for Spanish and English) levels of language acculturation were associated with decreased bronchodilator response compared with low (Spanish preference) levels (P = .009 and .02, respectively). Similarly, high language acculturation was associated with increased FEV1 compared with low language acculturation (P = .02). There was insufficient evidence of heterogeneity for associations across Latino subgroups.ConclusionsAcculturation was associated with diagnosed asthma and pulmonary function in Latino children and is an important factor to consider in the management of Latino youth with asthma.

Published
2019

18. Association study in African-admixed populations across the Americas recapitulates asthma risk loci in non-African populations.

Author

Daya, Michelle, Rafaels, Nicholas, Brunetti, Tonya M, Chavan, Sameer, Levin, Albert M, Shetty, Aniket, Gignoux, Christopher R, Boorgula, Meher Preethi, Wojcik, Genevieve, Campbell, Monica, Vergara, Candelaria, Torgerson, Dara G, Ortega, Victor E, Doumatey, Ayo, Johnston, Henry Richard, Acevedo, Nathalie, Araujo, Maria Ilma, Avila, Pedro C, Belbin, Gillian, Bleecker, Eugene, Bustamante, Carlos, Caraballo, Luis, Cruz, Alvaro, Dunston, Georgia M, Eng, Celeste, Faruque, Mezbah U, Ferguson, Trevor S, Figueiredo, Camila, Ford, Jean G, Gan, Weiniu, Gourraud, Pierre-Antoine, Hansel, Nadia N, Hernandez, Ryan D, Herrera-Paz, Edwin Francisco, Jiménez, Silvia, Kenny, Eimear E, Knight-Madden, Jennifer, Kumar, Rajesh, Lange, Leslie A, Lange, Ethan M, Lizee, Antoine, Maul, Pissamai, Maul, Trevor, Mayorga, Alvaro, Meyers, Deborah, Nicolae, Dan L, O'Connor, Timothy D, Oliveira, Ricardo Riccio, Olopade, Christopher O, Olopade, Olufunmilayo, Qin, Zhaohui S, Rotimi, Charles, Vince, Nicolas, Watson, Harold, Wilks, Rainford J, Wilson, James G, Salzberg, Steven, Ober, Carole, Burchard, Esteban G, Williams, L Keoki, Beaty, Terri H, Taub, Margaret A, Ruczinski, Ingo, Mathias, Rasika A, Barnes, Kathleen C, and CAAPA

Subjects
CAAPA, Chromosomes, Human, Pair 8, Chromosomes, Human, Pair 12, Chromosomes, Human, Pair 17, Humans, Asthma, Genetic Predisposition to Disease, Polymorphism, Single Nucleotide, African Americans, Hispanic Americans, United States, Genome-Wide Association Study, Genetic Loci, Chromosomes, Human, Pair 12, Pair 17, Pair 8, Polymorphism, Single Nucleotide
Abstract

Asthma is a complex disease with striking disparities across racial and ethnic groups. Despite its relatively high burden, representation of individuals of African ancestry in asthma genome-wide association studies (GWAS) has been inadequate, and true associations in these underrepresented minority groups have been inconclusive. We report the results of a genome-wide meta-analysis from the Consortium on Asthma among African Ancestry Populations (CAAPA; 7009 asthma cases, 7645 controls). We find strong evidence for association at four previously reported asthma loci whose discovery was driven largely by non-African populations, including the chromosome 17q12-q21 locus and the chr12q13 region, a novel (and not previously replicated) asthma locus recently identified by the Trans-National Asthma Genetic Consortium (TAGC). An additional seven loci reported by TAGC show marginal evidence for association in CAAPA. We also identify two novel loci (8p23 and 8q24) that may be specific to asthma risk in African ancestry populations.

Published
2019

20. A new flow path: eDNA connecting hydrology and biology.

Author

URycki, Dawn R., Kirtane, Anish A., Aronoff, Rachel, Avila, Colton C., Blackman, Rosetta C., Carraro, Luca, Evrard, Olivier, Good, Stephen P., Hoyos J., Diana C., López‐Rodríguez, Nieves, Mora, Demetrio, Schadewell, Yvonne, Schilling, Oliver S., and Ceperley, Natalie C.

Subjects
HYDROLOGICAL surveys, DNA analysis, TRACERS (Biology), ENDANGERED species, WATER distribution
Abstract

Environmental DNA (eDNA) has revolutionized ecological research, particularly for biodiversity assessment in various environments, most notably aquatic media. Environmental DNA analysis allows for non‐invasive and rapid species detection across multiple taxonomic groups within a single sample, making it especially useful for identifying rare or invasive species. Due to dynamic hydrological processes, eDNA samples from running waters may represent biodiversity from broad contributing areas, which is convenient from a biomonitoring perspective but also challenging, as hydrological knowledge is required for meaningful biological interpretation. Hydrologists could also benefit from eDNA to address unsolved questions, particularly concerning water movement through catchments. While naturally occurring abiotic tracers have advanced our understanding of water age distribution in catchments, for example, current geochemical tracers cannot fully elucidate the timing and flow paths of water through landscapes. Conversely, biological tracers, owing to their immense diversity and interactions with the environment, could offer more detailed information on the sources and flow paths of water to the stream. The informational capacity of eDNA as a tracer, however, is determined by the ability to interpret the complex biological heterogeneity at a study site, which arguably requires both biological and hydrological expertise. As eDNA data has become increasingly available as part of biomonitoring campaigns, we argue that accompanying eDNA surveys with hydrological observations could enhance our understanding of both biological and hydrological processes; we identify opportunities, challenges, and needs for further interdisciplinary collaboration; and we highlight eDNA's potential as a bridge between hydrology and biology, which could foster both domains. This article is categorized under:Science of Water > Hydrological ProcessesScience of Water > MethodsWater and Life > Nature of Freshwater Ecosystems [ABSTRACT FROM AUTHOR]

Published
2024
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21. Using Pod Based e-Cigarettes and Nicotine Pouches to Reduce Harm for Adults With Low Socioeconomic Status Who Smoke: A Pilot Randomized Controlled Trial.

Author

Avila, Jaqueline C, Maglalang, Dale Dagar, Nollen, Nicole L, Lee, Sangah Clara, Suh, Riley, Malone, Mona, Binjrajka, Urvi, and Ahluwalia, Jasjit S

Subjects
*ELECTRONIC cigarettes, *CAREER development, *SMOKING cessation, *SMOKING, *NICOTINE, *NICOTINE replacement therapy
Abstract

Introduction Alternative Nicotine Delivery Systems (ANDS) such as e-cigarettes (EC) and oral nicotine pouches (ONP) may facilitate the substitution of smoking for those unwilling to quit. This pilot study assesses the harm-reduction potential of EC and ONP among smokers with low socioeconomic status (SES). Aims and Methods Adults who smoked daily in the past 6 months, had a household income < 250% federal poverty level and had no intention of quitting smoking in the next 30 days were randomized 2:2:1 to 8 weeks of 5% nicotine EC; 4 mg ONP or assessment-only control (CC). The primary outcome was a within-group change in cigarettes per day (CPD) from Baseline to week 8. Results Forty-five individuals were randomized (EC: N  = 18; ONP: N  = 18; CC: N  = 9). Analyses included 33 participants who completed the week 8 visit. The mean age was 50.1 years (SD: 10.7) and the average CPD at baseline was 13.9 (SD: 10.1). For those randomized to EC, the average CPD decreased from 14.7 (95% CI: 10.3 to 19.1) at the Baseline to 2.9 (95% CI:.1 to 5.8) at week 8 (p -value < .001). For those randomized to ONP, average CPD decreased from 15.0 (95% CI: 5.0 to 24.9) to 8.3 (95% CI: 1.3 to 15.2) by week 8 (p -value = .01). In the EC and ONP groups, respectively, 4 (28.6%) and 1 (8.3%) participant fully switched from smoking to the ANDS product by week 8. Conclusions Individuals with low SES who smoke had lower CPD after switching to EC or ONP. These findings show the potential of ANDS in helping smokers switch to less harmful devices. Implications This study provides novel evidence that e-cigarettes and nicotine pouches can be a harm-reduction tool for individuals with lower SES who smoke and are not willing to quit smoking, contributing to reducing tobacco-related disparities in this population. Clinical Trials Identifier: NCT05327439 [ABSTRACT FROM AUTHOR]

Published
2024
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22. Effects of combination treatment with tezepelumab and allergen immunotherapy on nasal responses to allergen: A randomized controlled trial

Author

Corren, Jonathan, Larson, David, Altman, Matthew C., Segnitz, R. Max, Avila, Pedro C., Greenberger, Paul A., Baroody, Fuad, Moss, Mark H., Nelson, Harold, Burbank, Allison J., Hernandez, Michelle L., Peden, David, Saini, Sarbjit, Tilles, Stephen, Hussain, Iftikhar, Whitehouse, Don, Qin, Tielin, Villarreal, Miguel, Sever, Michelle, Wheatley, Lisa M., Nepom, Gerald T., and Sanda, Srinath

Published
2022
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23. Secondhand smoke exposure and asthma outcomes among African-American and Latino children with asthma

Author

Neophytou, Andreas M, Oh, Sam S, White, Marquitta J, Mak, Angel CY, Hu, Donglei, Huntsman, Scott, Eng, Celeste, Serebrisky, Denise, Borrell, Luisa N, Farber, Harold J, Meade, Kelley, Davis, Adam, Avila, Pedro C, Thyne, Shannon M, Rodríguez-Cintrón, William, Rodríguez-Santana, José R, Kumar, Rajesh, Brigino-Buenaventura, Emerita, Sen, Saunak, Lenoir, Michael A, Williams, L Keoki, Benowitz, Neal L, Balmes, John R, Eisen, Ellen A, and Burchard, Esteban G

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Social Determinants of Health, Tobacco, Tobacco Smoke and Health, Health Disparities, Lung, Women's Health, Minority Health, Pediatric, Asthma, Health Effects of Indoor Air Pollution, Respiratory, Adolescent, Black or African American, Child, Female, Hispanic or Latino, Humans, Incidence, Male, Risk Assessment, Risk Factors, Tobacco Smoke Pollution, United States, Young Adult, asthma epidemiology, tobacco and the lung, Respiratory System, Cardiovascular medicine and haematology, Clinical sciences
Abstract

BackgroundSecondhand smoke (SHS) exposures have been linked to asthma-related outcomes but quantitative dose-responses using biomarkers of exposure have not been widely reported.ObjectivesAssess dose-response relationships between plasma cotinine-determined SHS exposure and asthma outcomes in minority children, a vulnerable population exposed to higher levels of SHS and under-represented in the literature.MethodsWe performed analyses in 1172 Latino and African-American children with asthma from the mainland USA and Puerto Rico. We used logistic regression to assess relationships of cotinine levels ≥0.05 ng/mL with asthma exacerbations (defined as asthma-related hospitalisations, emergency room visits or oral steroid prescription) in the previous year and asthma control. The shape of dose-response relationships was assessed using a continuous exposure variable in generalised additive logistic models with penalised splines.ResultsThe OR for experiencing asthma exacerbations in the previous year for cotinine levels ≥0.05 ng/mL, compared with

Published
2018

24. Whole-Genome Sequencing of Pharmacogenetic Drug Response in Racially Diverse Children with Asthma

Author

Mak, Angel CY, White, Marquitta J, Eckalbar, Walter L, Szpiech, Zachary A, Oh, Sam S, Pino-Yanes, Maria, Hu, Donglei, Goddard, Pagé, Huntsman, Scott, Galanter, Joshua, Wu, Ann Chen, Himes, Blanca E, Germer, Soren, Vogel, Julia M, Bunting, Karen L, Eng, Celeste, Salazar, Sandra, Keys, Kevin L, Liberto, Jennifer, Nuckton, Thomas J, Nguyen, Thomas A, Torgerson, Dara G, Kwok, Pui-Yan, Levin, Albert M, Celedón, Juan C, Forno, Erick, Hakonarson, Hakon, Sleiman, Patrick M, Dahlin, Amber, Tantisira, Kelan G, Weiss, Scott T, Serebrisky, Denise, Brigino-Buenaventura, Emerita, Farber, Harold J, Meade, Kelley, Lenoir, Michael A, Avila, Pedro C, Sen, Saunak, Thyne, Shannon M, Rodriguez-Cintron, William, Winkler, Cheryl A, Moreno-Estrada, Andrés, Sandoval, Karla, Rodriguez-Santana, Jose R, Kumar, Rajesh, Williams, L Keoki, Ahituv, Nadav, Ziv, Elad, Seibold, Max A, Darnell, Robert B, Zaitlen, Noah, Hernandez, Ryan D, and Burchard, Esteban G

Subjects
Pharmacology and Pharmaceutical Sciences, Biomedical and Clinical Sciences, Health Disparities, Precision Medicine, Lung, Genetics, Asthma, Human Genome, Pediatric, Minority Health, Biotechnology, 2.1 Biological and endogenous factors, Respiratory, Good Health and Well Being, Adolescent, Black or African American, Albuterol, Bronchodilator Agents, Child, Female, Genome-Wide Association Study, Hispanic or Latino, Humans, Male, Mexican Americans, Pharmacogenomic Variants, Polymorphism, Single Nucleotide, Race Factors, United States, albuterol, asthma, minority, NFKB1, Latinos, NHLBI Trans-Omics for Precision Medicine (TOPMed) Consortium, Medical and Health Sciences, Respiratory System, Cardiovascular medicine and haematology, Clinical sciences
Abstract

RationaleAlbuterol, a bronchodilator medication, is the first-line therapy for asthma worldwide. There are significant racial/ethnic differences in albuterol drug response.ObjectivesTo identify genetic variants important for bronchodilator drug response (BDR) in racially diverse children.MethodsWe performed the first whole-genome sequencing pharmacogenetics study from 1,441 children with asthma from the tails of the BDR distribution to identify genetic association with BDR.Measurements and main resultsWe identified population-specific and shared genetic variants associated with BDR, including genome-wide significant (P

Published
2018

25. Management, Utilization, and Outcomes of Preterm Labor in an Integrated Health Care System

Author

Getahun, Darios, additional, Sacks, David A., additional, Shi, Jiaxiao, additional, Xie, Fagen, additional, Khadka, Nehaa, additional, Chiu, Vicki Y., additional, Mensah, Nana A., additional, Avila, Chantal C., additional, Yeh, Meiyu, additional, Kawatkar, Aniket A., additional, Ruma, Michael S., additional, Joyce, Derek, additional, and Fassett, Michael J., additional

Published
2024
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28. Features of the bronchial bacterial microbiome associated with atopy, asthma, and responsiveness to inhaled corticosteroid treatment.

Author

Durack, Juliana, Lynch, Susan V, Nariya, Snehal, Bhakta, Nirav R, Beigelman, Avraham, Castro, Mario, Dyer, Anne-Marie, Israel, Elliot, Kraft, Monica, Martin, Richard J, Mauger, David T, Rosenberg, Sharon R, Sharp-King, Tonya, White, Steven R, Woodruff, Prescott G, Avila, Pedro C, Denlinger, Loren C, Holguin, Fernando, Lazarus, Stephen C, Lugogo, Njira, Moore, Wendy C, Peters, Stephen P, Que, Loretta, Smith, Lewis J, Sorkness, Christine A, Wechsler, Michael E, Wenzel, Sally E, Boushey, Homer A, Huang, Yvonne J, and National Heart, Lung and Blood Institute's “AsthmaNet”

Subjects
National Heart, Lung and Blood Institute's “AsthmaNet”, Bronchi, Humans, Bacteria, Asthma, Hypersensitivity, Immediate, Adrenal Cortex Hormones, RNA, Bacterial, RNA, Ribosomal, 16S, Administration, Inhalation, Adult, Middle Aged, Female, Male, Young Adult, Microbiota, Fluticasone, 16S ribosomal RNA, T(H)2 inflammation, atopy, bacteria, corticosteroids, metabolic pathways, microbiome, short-chain fatty acids, three-gene mean, Genetics, Lung, Clinical Research, 2.1 Biological and endogenous factors, Aetiology, Respiratory, Immunology, Allergy
Abstract

BackgroundCompositional differences in the bronchial bacterial microbiota have been associated with asthma, but it remains unclear whether the findings are attributable to asthma, to aeroallergen sensitization, or to inhaled corticosteroid treatment.ObjectivesWe sought to compare the bronchial bacterial microbiota in adults with steroid-naive atopic asthma, subjects with atopy but no asthma, and nonatopic healthy control subjects and to determine relationships of the bronchial microbiota to phenotypic features of asthma.MethodsBacterial communities in protected bronchial brushings from 42 atopic asthmatic subjects, 21 subjects with atopy but no asthma, and 21 healthy control subjects were profiled by using 16S rRNA gene sequencing. Bacterial composition and community-level functions inferred from sequence profiles were analyzed for between-group differences. Associations with clinical and inflammatory variables were examined, including markers of type 2-related inflammation and change in airway hyperresponsiveness after 6 weeks of fluticasone treatment.ResultsThe bronchial microbiome differed significantly among the 3 groups. Asthmatic subjects were uniquely enriched in members of the Haemophilus, Neisseria, Fusobacterium, and Porphyromonas species and the Sphingomonodaceae family and depleted in members of the Mogibacteriaceae family and Lactobacillales order. Asthma-associated differences in predicted bacterial functions included involvement of amino acid and short-chain fatty acid metabolism pathways. Subjects with type 2-high asthma harbored significantly lower bronchial bacterial burden. Distinct changes in specific microbiota members were seen after fluticasone treatment. Steroid responsiveness was linked to differences in baseline compositional and functional features of the bacterial microbiome.ConclusionEven in subjects with mild steroid-naive asthma, differences in the bronchial microbiome are associated with immunologic and clinical features of the disease. The specific differences identified suggest possible microbiome targets for future approaches to asthma treatment or prevention.

Published
2017

29. Perceived Discrimination Associated With Asthma and Related Outcomes in Minority Youth The GALA II and SAGE II Studies

Author

Thakur, Neeta, Barcelo, Nicolas E, Borrell, Luisa N, Singh, Smriti, Eng, Celeste, Davis, Adam, Meade, Kelley, LeNoir, Michael A, Avila, Pedro C, Farber, Harold J, Serebrisky, Denise, Brigino-Buenaventura, Emerita, Rodriguez-Cintron, William, Thyne, Shannon, Rodriguez-Santana, Jose R, Sen, Saunak, Bibbins-Domingo, Kirsten, and Burchard, Esteban Gonzalez

Subjects
Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Clinical Sciences, Behavioral and Social Science, Clinical Research, Pediatric, Lung, Asthma, Respiratory, Adolescent, Black or African American, Case-Control Studies, Child, Female, Health Status Disparities, Hispanic or Latino, Humans, Male, Racism, Risk Factors, Social Class, Stress, Psychological, Surveys and Questionnaires, United States, Young Adult, children, health status disparity, psychosocial stress, race, socioeconomic status, Respiratory System, Cardiovascular medicine and haematology, Clinical sciences
Abstract

BackgroundAsthma disproportionately affects minority populations and is associated with psychosocial stress such as racial/ethnic discrimination. We aimed to examine the association of perceived discrimination with asthma and poor asthma control in African American and Latino youth.MethodsWe included African American (n = 954), Mexican American (n = 1,086), other Latino (n = 522), and Puerto Rican Islander (n = 1,025) youth aged 8 to 21 years from the Genes-Environments and Admixture in Latino Americans study and the Study of African Americans, Asthma, Genes, and Environments. Asthma was defined by physician diagnosis, and asthma control was defined based on the National Heart, Lung, and Blood Institute guidelines. Perceived racial/ethnic discrimination was assessed by the Experiences of Discrimination questionnaire, with a focus on school, medical, and public settings. We examined the associations of perceived discrimination with each outcome and whether socioeconomic status (SES) and global African ancestry modified these associations.ResultsAfrican American children reporting any discrimination had a 78% greater odds of experiencing asthma (OR, 1.78; 95% CI, 1.33-2.39) than did those not reporting discrimination. Similarly, African American children faced increased odds of poor asthma control with any experience of discrimination (OR, 1.97; 95% CI, 1.42-2.76) over their counterparts not reporting discrimination. These associations were not observed among Latino children. We observed heterogeneity of the association between reports of discrimination and asthma according to SES, with reports of discrimination increasing the odds of having asthma among low-SES Mexican American youth (interaction P = .01) and among high-SES other Latino youth (interaction P = .04).ConclusionsPerceived discrimination is associated with increased odds of asthma and poorer control among African American youth. SES exacerbates the effect of perceived discrimination on having asthma among Mexican American and other Latino youth.

Published
2017

30. Identification of a novel locus associated with skin colour in African-admixed populations.

Author

Hernandez-Pacheco, Natalia, Flores, Carlos, Alonso, Santos, Eng, Celeste, Mak, Angel CY, Hunstman, Scott, Hu, Donglei, White, Marquitta J, Oh, Sam S, Meade, Kelley, Farber, Harold J, Avila, Pedro C, Serebrisky, Denise, Thyne, Shannon M, Brigino-Buenaventura, Emerita, Rodriguez-Cintron, William, Sen, Saunak, Kumar, Rajesh, Lenoir, Michael, Rodriguez-Santana, Jose R, Burchard, Esteban G, and Pino-Yanes, Maria

Subjects
Humans, Proteins, Membrane Transport Proteins, Antiporters, DNA, Intergenic, Antigens, Neoplasm, Skin Pigmentation, Genotype, Phenotype, Polymorphism, Single Nucleotide, African Americans, Asian Continental Ancestry Group, European Continental Ancestry Group, Hispanic Americans, Female, Male, Genome-Wide Association Study, Genetic Loci, RNA Splicing Factors, Antigens, Neoplasm, DNA, Intergenic, Polymorphism, Single Nucleotide
Abstract

Skin pigmentation is a complex trait that varies largely among populations. Most genome-wide association studies of this trait have been performed in Europeans and Asians. We aimed to uncover genes influencing skin colour in African-admixed individuals. We performed a genome-wide association study of melanin levels in 285 Hispanic/Latino individuals from Puerto Rico, analyzing 14 million genetic variants. A total of 82 variants with p-value ≤1 × 10-5 were followed up in 373 African Americans. Fourteen single nucleotide polymorphisms were replicated, of which nine were associated with skin colour at genome-wide significance in a meta-analysis across the two studies. These results validated the association of two previously known skin pigmentation genes, SLC24A5 (minimum p = 2.62 × 10-14, rs1426654) and SLC45A2 (minimum p = 9.71 × 10-10, rs16891982), and revealed the intergenic region of BEND7 and PRPF18 as a novel locus associated with this trait (minimum p = 4.58 × 10-9, rs6602666). The most significant variant within this region is common among African-descent populations but not among Europeans or Native Americans. Our findings support the advantages of analyzing African-admixed populations to discover new genes influencing skin pigmentation.

Published
2017

31. Differential methylation between ethnic sub-groups reflects the effect of genetic ancestry and environmental exposures.

Author

Galanter, Joshua M, Gignoux, Christopher R, Oh, Sam S, Torgerson, Dara, Pino-Yanes, Maria, Thakur, Neeta, Eng, Celeste, Hu, Donglei, Huntsman, Scott, Farber, Harold J, Avila, Pedro C, Brigino-Buenaventura, Emerita, LeNoir, Michael A, Meade, Kelly, Serebrisky, Denise, Rodríguez-Cintrón, William, Kumar, Rajesh, Rodríguez-Santana, Jose R, Seibold, Max A, Borrell, Luisa N, Burchard, Esteban G, and Zaitlen, Noah

Subjects
Humans, Environmental Exposure, DNA Methylation, Epigenesis, Genetic, Ethnic Groups, Hispanic Americans, Latinos, chromosomes, epigenetics, ethnicity, genes, human, human biology, medicine, methylation, Human Genome, Genetics, Prevention, Biochemistry and Cell Biology
Abstract

Populations are often divided categorically into distinct racial/ethnic groups based on social rather than biological constructs. Genetic ancestry has been suggested as an alternative to this categorization. Herein, we typed over 450,000 CpG sites in whole blood of 573 individuals of diverse Hispanic origin who also had high-density genotype data. We found that both self-identified ethnicity and genetically determined ancestry were each significantly associated with methylation levels at 916 and 194 CpGs, respectively, and that shared genomic ancestry accounted for a median of 75.7% (IQR 45.8% to 92%) of the variance in methylation associated with ethnicity. There was a significant enrichment (p=4.2×10-64) of ethnicity-associated sites amongst loci previously associated environmental exposures, particularly maternal smoking during pregnancy. We conclude that differential methylation between ethnic groups is partially explained by the shared genetic ancestry but that environmental factors not captured by ancestry significantly contribute to variation in methylation.

Published
2017

32. Histologic and Clinical Factors Associated with Kidney Outcomes in IgA Vasculitis Nephritis

Author

Barbour, S, Coppo, R, Er, L, Pillebout, E, Russo, M, Alpers, C, Fogo, A, Ferrario, F, Jennette, J, Roberts, I, Cook, H, Ding, J, Su, B, Zhong, X, Fervenza, F, Zand, L, Peruzzi, L, Lucchetti, L, Katafuchi, R, Shima, Y, Yoshikawa, N, Ichikawa, D, Suzuki, Y, Murer, L, Wyatt, R, Nelson, R, Narus, J, Wenderfer, S, Geetha, D, Daugas, E, Monteiro, R, Nakatani, S, Mastrangelo, A, Nuutinen, M, Koskela, M, Weber, L, Hackl, A, Pohl, M, Pecoraro, C, Tsuboi, N, Yokoo, T, Takafumi, I, Fujimoto, S, Conti, G, Santoro, D, Materassi, M, Zhang, H, Shi, S, Liu, Z, Tesar, V, Maixnerova, D, Avila-Casado, C, Bajema, I, Barreca, A, Becker, J, Comstock, J, Cornea, V, Eldin, K, Hernandez, L, Hou, J, Joh, K, Lin, M, Messias, N, Muda, A, Pagni, F, Diomedi-Camassei, F, Tokola, H, D’Armiento, M, Seidl, M, Rosenberg, A, Sannier, A, Soares, M, Wang, S, Zeng, C, Haas, M, Barbour, Sean J., Coppo, Rosanna, Er, Lee, Pillebout, Evangeline, Russo, Maria Luisa, Alpers, Charles E., Fogo, Agnes B., Ferrario, Franco, Jennette, J. Charles, Roberts, Ian S. D., Cook, H. Terence, Ding, Jie, Su, Baige, Zhong, Xuhui, Fervenza, Fernando C., Zand, Ladan, Peruzzi, Licia, Lucchetti, Laura, Katafuchi, Ritsuko, Shima, Yuko, Yoshikawa, Norishige, Ichikawa, Daisuke, Suzuki, Yusuke, Murer, Luisa, Wyatt, Robert J., Nelson, Raoul D., Narus, JoAnn H., Wenderfer, Scott, Geetha, Duvuru, Daugas, Eric, Monteiro, Renato C., Nakatani, Shinya, Mastrangelo, Antonio, Nuutinen, Matti, Koskela, Mikael, Weber, Lutz T, Hackl, Agnes, Pohl, Martin, Pecoraro, Carmine, Tsuboi, Nobuo, Yokoo, Takashi, Takafumi, Ito, Fujimoto, Shouichi, Conti, Giovanni, Santoro, Domenico, Materassi, Marco, Zhang, Hong, Shi, Sufang, Liu, Zhi-Hong, Tesar, Vladimir, Maixnerova, Dita, Avila-Casado, Carmen, Bajema, Ingeborg, Barreca, Antonella, Becker, Jan U., Comstock, Jessica M., Cornea, Virgilius, Eldin, Karen, Hernandez, Loren Herrera, Hou, Jean, Joh, Kensuke, Lin, Mercury, Messias, Nidia, Muda, Andrea Onetti, Pagni, Fabio, Diomedi-Camassei, Francesca, Tokola, Heikki, D’Armiento, Maria, Seidl, Maximilian, Rosenberg, Avi, Sannier, Aurélie, Soares, Maria Fernanda, Wang, Suxia, Zeng, Caihong, Haas, Mark, Barbour, S, Coppo, R, Er, L, Pillebout, E, Russo, M, Alpers, C, Fogo, A, Ferrario, F, Jennette, J, Roberts, I, Cook, H, Ding, J, Su, B, Zhong, X, Fervenza, F, Zand, L, Peruzzi, L, Lucchetti, L, Katafuchi, R, Shima, Y, Yoshikawa, N, Ichikawa, D, Suzuki, Y, Murer, L, Wyatt, R, Nelson, R, Narus, J, Wenderfer, S, Geetha, D, Daugas, E, Monteiro, R, Nakatani, S, Mastrangelo, A, Nuutinen, M, Koskela, M, Weber, L, Hackl, A, Pohl, M, Pecoraro, C, Tsuboi, N, Yokoo, T, Takafumi, I, Fujimoto, S, Conti, G, Santoro, D, Materassi, M, Zhang, H, Shi, S, Liu, Z, Tesar, V, Maixnerova, D, Avila-Casado, C, Bajema, I, Barreca, A, Becker, J, Comstock, J, Cornea, V, Eldin, K, Hernandez, L, Hou, J, Joh, K, Lin, M, Messias, N, Muda, A, Pagni, F, Diomedi-Camassei, F, Tokola, H, D’Armiento, M, Seidl, M, Rosenberg, A, Sannier, A, Soares, M, Wang, S, Zeng, C, Haas, M, Barbour, Sean J., Coppo, Rosanna, Er, Lee, Pillebout, Evangeline, Russo, Maria Luisa, Alpers, Charles E., Fogo, Agnes B., Ferrario, Franco, Jennette, J. Charles, Roberts, Ian S. D., Cook, H. Terence, Ding, Jie, Su, Baige, Zhong, Xuhui, Fervenza, Fernando C., Zand, Ladan, Peruzzi, Licia, Lucchetti, Laura, Katafuchi, Ritsuko, Shima, Yuko, Yoshikawa, Norishige, Ichikawa, Daisuke, Suzuki, Yusuke, Murer, Luisa, Wyatt, Robert J., Nelson, Raoul D., Narus, JoAnn H., Wenderfer, Scott, Geetha, Duvuru, Daugas, Eric, Monteiro, Renato C., Nakatani, Shinya, Mastrangelo, Antonio, Nuutinen, Matti, Koskela, Mikael, Weber, Lutz T, Hackl, Agnes, Pohl, Martin, Pecoraro, Carmine, Tsuboi, Nobuo, Yokoo, Takashi, Takafumi, Ito, Fujimoto, Shouichi, Conti, Giovanni, Santoro, Domenico, Materassi, Marco, Zhang, Hong, Shi, Sufang, Liu, Zhi-Hong, Tesar, Vladimir, Maixnerova, Dita, Avila-Casado, Carmen, Bajema, Ingeborg, Barreca, Antonella, Becker, Jan U., Comstock, Jessica M., Cornea, Virgilius, Eldin, Karen, Hernandez, Loren Herrera, Hou, Jean, Joh, Kensuke, Lin, Mercury, Messias, Nidia, Muda, Andrea Onetti, Pagni, Fabio, Diomedi-Camassei, Francesca, Tokola, Heikki, D’Armiento, Maria, Seidl, Maximilian, Rosenberg, Avi, Sannier, Aurélie, Soares, Maria Fernanda, Wang, Suxia, Zeng, Caihong, and Haas, Mark

Abstract

BACKGROUND: Nephritis is a common manifestation of IgA vasculitis and is morphologically indistinguishable from IgA nephropathy. While MEST-C scores are predictive of kidney outcomes in IgA nephropathy, their value in IgA vasculitis nephritis has not been investigated in large multiethnic cohorts. METHODS: Biopsies from 262 children and 99 adults with IgA vasculitis nephritis ( N =361) from 23 centers in North America, Europe, and Asia were independently scored by three pathologists. MEST-C scores were assessed for correlation with eGFR/proteinuria at biopsy. Because most patients ( N =309, 86%) received immunosuppression, risk factors for outcomes were evaluated in this group using latent class mixed models to identify classes of eGFR trajectories over a median follow-up of 2.7 years (interquartile range, 1.2-5.1). Clinical and histologic parameters associated with each class were determined using logistic regression. RESULTS: M, E, T, and C scores were correlated with either eGFR or proteinuria at biopsy. Two classes were identified by latent class mixed model, one with initial improvement in eGFR followed by a late decline (class 1, N =91) and another with stable eGFR (class 2, N =218). Class 1 was associated with a higher risk of an established kidney outcome (time to ≥30% decline in eGFR or kidney failure; hazard ratio, 5.84; 95% confidence interval, 2.37 to 14.4). Among MEST-C scores, only E1 was associated with class 1 by multivariable analysis. Other factors associated with class 1 were age 18 years and younger, male sex, lower eGFR at biopsy, and extrarenal noncutaneous disease. Fibrous crescents without active changes were associated with class 2. CONCLUSIONS: Kidney outcome in patients with biopsied IgA vasculitis nephritis treated with immunosuppression was determined by clinical risk factors and endocapillary hypercellularity (E1) and fibrous crescents, which are features that are not part of the International Study of Diseases of Children classificatio

Published
2024

33. 5-HTP inhibits eosinophilia via intracellular endothelial 5-HTRs; SNPs in 5-HTRs associate with asthmatic lung function.

Author

Walker, Matthew T., Bloodworth, Jeffrey C., Kountz, Timothy S., McCarty, Samantha L., Green, Jeremy E., Ferrie, Ryan P., Campbell, Jackson A., Averill, Samantha H., Beckman, Kenneth B., Grammer, Leslie C., Eng, Celeste, Avila, Pedro C., Farber, Harold J., Rodriguez-Cintron, William, Rodriguez-Santana, Jose R., Serebrisky, Denise, Thyne, Shannon M., Seibold, Max A., Burchard, Esteban G., and Kumar, Rajesh

Published
2024
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34. Inclusive Human-Centered Design: Experiences and Challenges to Teaching Design Engineering Students

Author

Landa-Avila, Irma C., Aceves-Gonzalez, Carlos, Kacprzyk, Janusz, Series Editor, Pal, Nikhil R., Advisory Editor, Bello Perez, Rafael, Advisory Editor, Corchado, Emilio S., Advisory Editor, Hagras, Hani, Advisory Editor, Kóczy, László T., Advisory Editor, Kreinovich, Vladik, Advisory Editor, Lin, Chin-Teng, Advisory Editor, Lu, Jie, Advisory Editor, Melin, Patricia, Advisory Editor, Nedjah, Nadia, Advisory Editor, Nguyen, Ngoc Thanh, Advisory Editor, Wang, Jun, Advisory Editor, Bagnara, Sebastiano, editor, Tartaglia, Riccardo, editor, Albolino, Sara, editor, Alexander, Thomas, editor, and Fujita, Yushi, editor

Published
2019
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35. Usability Assessment of a Portable Corneal Topography Device

Author

Aceves-González, Carlos, Galindo-Estupiñan, Zuli T., Landa-Avila, Irma C., Díaz-Gutiérrez, Citlali, Prado-Jiménez, Stephanie Daphne, Kacprzyk, Janusz, Series Editor, Pal, Nikhil R., Advisory Editor, Bello Perez, Rafael, Advisory Editor, Corchado, Emilio S., Advisory Editor, Hagras, Hani, Advisory Editor, Kóczy, László T., Advisory Editor, Kreinovich, Vladik, Advisory Editor, Lin, Chin-Teng, Advisory Editor, Lu, Jie, Advisory Editor, Melin, Patricia, Advisory Editor, Nedjah, Nadia, Advisory Editor, Nguyen, Ngoc Thanh, Advisory Editor, Wang, Jun, Advisory Editor, Ahram, Tareq Z., editor, and Falcão, Christianne, editor

Published
2019
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37. Air Pollution and Lung Function in Minority Youth with Asthma in the GALA II (Genes–Environments and Admixture in Latino Americans) and SAGE II (Study of African Americans, Asthma, Genes, and Environments) Studies

Author

Neophytou, Andreas M, White, Marquitta J, Oh, Sam S, Thakur, Neeta, Galanter, Joshua M, Nishimura, Katherine K, Pino-Yanes, Maria, Torgerson, Dara G, Gignoux, Christopher R, Eng, Celeste, Nguyen, Elizabeth A, Hu, Donglei, Mak, Angel C, Kumar, Rajesh, Seibold, Max A, Davis, Adam, Farber, Harold J, Meade, Kelley, Avila, Pedro C, Serebrisky, Denise, Lenoir, Michael A, Brigino-Buenaventura, Emerita, Rodriguez-Cintron, William, Bibbins-Domingo, Kirsten, Thyne, Shannon M, Williams, L Keoki, Sen, Saunak, Gilliland, Frank D, Gauderman, W James, Rodriguez-Santana, Jose R, Lurmann, Fred, Balmes, John R, Eisen, Ellen A, and Burchard, Esteban G

Subjects
Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Clinical Sciences, Climate-Related Exposures and Conditions, Asthma, Genetics, Clinical Research, Lung, Pediatric, Aetiology, 2.2 Factors relating to the physical environment, Respiratory, Adolescent, Black or African American, Air Pollutants, Air Pollution, Child, Environmental Exposure, Female, Hispanic or Latino, Humans, Male, Minority Groups, Puerto Rico, United States, air pollution, minority, children, lung function, ancestry, Medical and Health Sciences, Respiratory System, Cardiovascular medicine and haematology, Clinical sciences
Abstract

RationaleAdverse effects of exposures to ambient air pollution on lung function are well documented, but evidence in racial/ethnic minority children is lacking.ObjectivesTo assess the relationship between air pollution and lung function in minority children with asthma and possible modification by global genetic ancestry.MethodsThe study population consisted of 1,449 Latino and 519 African American children with asthma from five different geographical regions in the mainland United States and Puerto Rico. We examined five pollutants (particulate matter ≤10 μm and ≤2.5 μm in diameter, ozone, nitrogen dioxide, and sulfur dioxide), derived from participant residential history and ambient air monitoring data, and assessed over several time windows. We fit generalized additive models for associations between pollutant exposures and lung function parameters and tested for interaction terms between exposures and genetic ancestry.Measurements and main resultsA 5 μg/m(3) increase in average lifetime particulate matter less than or equal to 2.5 μm in diameter exposure was associated with a 7.7% decrease in FEV1 (95% confidence interval = -11.8 to -3.5%) in the overall study population. Global genetic ancestry did not appear to significantly modify these associations, but percent African ancestry was a significant predictor of lung function.ConclusionsEarly-life particulate exposures were associated with reduced lung function in Latino and African American children with asthma. This is the first study to report an association between exposure to particulates and reduced lung function in minority children in which racial/ethnic status was measured by ancestry-informative markers.

Published
2016

38. Association of a PAI-1 Gene Polymorphism and Early Life Infections with Asthma Risk, Exacerbations, and Reduced Lung Function.

Author

Cho, Seong H, Min, Jin-Young, Kim, Dong Young, Oh, Sam S, Torgerson, Dara R, Pino-Yanes, Maria, Hu, Donglei, Sen, Saunak, Huntsman, Scott, Eng, Celeste, Farber, Harold J, Rodriguez-Cintron, William, Rodriguez-Santana, Jose R, Serebrisky, Denise, Thyne, Shannon M, Borrell, Luisa N, Williams, L Keoki, DuPont, William, Seibold, Max A, Burchard, Esteban G, Avila, Pedro C, and Kumar, Rajesh

Subjects
Humans, Respiratory Tract Infections, Asthma, Disease Progression, Genetic Predisposition to Disease, Plasminogen Activator Inhibitor 1, Respiratory Function Tests, Odds Ratio, Risk Assessment, Risk Factors, Case-Control Studies, Genotype, Polymorphism, Genetic, Alleles, Socioeconomic Factors, Adolescent, Adult, Child, Ethnic Groups, United States, Female, Male, Young Adult, Genetic Association Studies, Polymorphism, Genetic, General Science & Technology
Abstract

BackgroundPlasminogen activator inhibitor-1 (PAI-1) is induced in airways by virus and may mediate asthmatic airway remodeling. We sought to evaluate if genetic variants and early life lower respiratory infections jointly affect asthma risk.MethodsWe included Latino children, adolescents, and young adults aged 8-21 years (1736 subjects with physician-diagnosed asthma and 1747 healthy controls) from five U.S. centers and Puerto Rico after excluding subjects with incomplete clinical or genetic data. We evaluated the independent and joint effects of a PAI-1 gain of function polymorphism and bronchiolitis / Respiratory Syncytial Virus (RSV) or other lower respiratory infections (LRI) within the first 2 years of life on asthma risk, asthma exacerbations and lung function.ResultsRSV infection (OR 9.9, 95%CI 4.9-20.2) and other LRI (OR 9.1, 95%CI 7.2-11.5) were independently associated with asthma, but PAI-1 genotype was not. There were joint effects on asthma risk for both genotype-RSV (OR 17.7, 95% CI 6.3-50.2) and genotype-LRI (OR 11.7, 95% CI 8.8-16.4). A joint effect of genotype-RSV resulted in a 3.1-fold increased risk for recurrent asthma hospitalizations. In genotype-respiratory infection joint effect analysis, FEV1% predicted and FEV1/FVC % predicted were further reduced in the genotype-LRI group (β -2.1, 95% CI -4.0 to -0.2; β -2.0, 95% CI -3.1 to -0.8 respectively). Similarly, lower FEV1% predicted was noted in genotype-RSV group (β -3.1, 95% CI -6.1 to -0.2) with a trend for lower FEV1/FVC % predicted.ConclusionsA genetic variant of PAI-1 together with early life LRI such as RSV bronchiolitis is associated with an increased risk of asthma, morbidity, and reduced lung function in this Latino population.

Published
2016

42. The Southern Ocean Exchange: porous boundaries between humpback whale breeding populations in southern polar waters

Author

Marcondes, M. C. C., Cheeseman, T., Jackson, J. A., Friedlaender, A. S., Pallin, L., Olio, M., Wedekin, L. L., Daura-Jorge, F. G., Cardoso, J., Santos, J. D. F., Fortes, R. C., Araújo, M. F., Bassoi, M., Beaver, V., Bombosch, A., Clark, C. W., Denkinger, J., Boyle, A., Rasmussen, K., Savenko, O., Avila, I. C., Palacios, D. M., Kennedy, A. S., and Sousa-Lima, R. S.

Published
2021
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46. Genome-wide association study and admixture mapping reveal new loci associated with total IgE levels in Latinos

Author

Pino-Yanes, Maria, Gignoux, Christopher R, Galanter, Joshua M, Levin, Albert M, Campbell, Catarina D, Eng, Celeste, Huntsman, Scott, Nishimura, Katherine K, Gourraud, Pierre-Antoine, Mohajeri, Kiana, O'Roak, Brian J, Hu, Donglei, Mathias, Rasika A, Nguyen, Elizabeth A, Roth, Lindsey A, Padhukasahasram, Badri, Moreno-Estrada, Andres, Sandoval, Karla, Winkler, Cheryl A, Lurmann, Fred, Davis, Adam, Farber, Harold J, Meade, Kelley, Avila, Pedro C, Serebrisky, Denise, Chapela, Rocio, Ford, Jean G, Lenoir, Michael A, Thyne, Shannon M, Brigino-Buenaventura, Emerita, Borrell, Luisa N, Rodriguez-Cintron, William, Sen, Saunak, Kumar, Rajesh, Rodriguez-Santana, Jose R, Bustamante, Carlos D, Martinez, Fernando D, Raby, Benjamin A, Weiss, Scott T, Nicolae, Dan L, Ober, Carole, Meyers, Deborah A, Bleecker, Eugene R, Mack, Steven J, Hernandez, Ryan D, Eichler, Evan E, Barnes, Kathleen C, Williams, L Keoki, Torgerson, Dara G, and Burchard, Esteban G

Subjects
Biomedical and Clinical Sciences, Immunology, Clinical Research, Human Genome, Genetics, 2.1 Biological and endogenous factors, Aetiology, Inflammatory and immune system, Adolescent, Adult, Black or African American, Child, Chromosome Mapping, Chromosomes, Human, Pair 14, DNA-Binding Proteins, Female, Genetic Loci, Genome, Human, Genome-Wide Association Study, Genotype, HLA-DQ alpha-Chains, Hispanic or Latino, Humans, Immunoglobulin E, Male, Polymorphism, Single Nucleotide, Transcription Factors, White People, IgE, genome-wide association study, admixture mapping, allergy, asthma, next-generation sequencing, Latinos, Hispanics, minority populations, Allergy
Abstract

BackgroundIgE is a key mediator of allergic inflammation, and its levels are frequently increased in patients with allergic disorders.ObjectiveWe sought to identify genetic variants associated with IgE levels in Latinos.MethodsWe performed a genome-wide association study and admixture mapping of total IgE levels in 3334 Latinos from the Genes-environments & Admixture in Latino Americans (GALA II) study. Replication was evaluated in 454 Latinos, 1564 European Americans, and 3187 African Americans from independent studies.ResultsWe confirmed associations of 6 genes identified by means of previous genome-wide association studies and identified a novel genome-wide significant association of a polymorphism in the zinc finger protein 365 gene (ZNF365) with total IgE levels (rs200076616, P = 2.3 × 10(-8)). We next identified 4 admixture mapping peaks (6p21.32-p22.1, 13p22-31, 14q23.2, and 22q13.1) at which local African, European, and/or Native American ancestry was significantly associated with IgE levels. The most significant peak was 6p21.32-p22.1, where Native American ancestry was associated with lower IgE levels (P = 4.95 × 10(-8)). All but 22q13.1 were replicated in an independent sample of Latinos, and 2 of the peaks were replicated in African Americans (6p21.32-p22.1 and 14q23.2). Fine mapping of 6p21.32-p22.1 identified 6 genome-wide significant single nucleotide polymorphisms in Latinos, 2 of which replicated in European Americans. Another single nucleotide polymorphism was peak-wide significant within 14q23.2 in African Americans (rs1741099, P = 3.7 × 10(-6)) and replicated in non-African American samples (P = .011).ConclusionWe confirmed genetic associations at 6 genes and identified novel associations within ZNF365, HLA-DQA1, and 14q23.2. Our results highlight the importance of studying diverse multiethnic populations to uncover novel loci associated with total IgE levels.

Published
2015

47. Obesity and Bronchodilator Response in Black and Hispanic Children and Adolescents With Asthma

Author

McGarry, Meghan E, Castellanos, Elizabeth, Thakur, Neeta, Oh, Sam S, Eng, Celeste, Davis, Adam, Meade, Kelley, LeNoir, Michael A, Avila, Pedro C, Farber, Harold J, Serebrisky, Denise, Brigino-Buenaventura, Emerita, Rodriguez-Cintron, William, Kumar, Rajesh, Bibbins-Domingo, Kirsten, Thyne, Shannon M, Sen, Saunak, Rodriguez-Santana, Jose R, Borrell, Luisa N, and Burchard, Esteban G

Subjects
Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Clinical Sciences, Pediatric, Clinical Research, Obesity, Asthma, Nutrition, Lung, Respiratory, Administration, Inhalation, Adolescent, Adrenal Cortex Hormones, Albuterol, Black People, Bronchodilator Agents, Case-Control Studies, Child, Cross-Sectional Studies, Female, Hispanic or Latino, Humans, Leukotriene Antagonists, Logistic Models, Male, Retrospective Studies, Treatment Outcome, Respiratory System, Cardiovascular medicine and haematology, Clinical sciences
Abstract

BackgroundObesity is associated with poor asthma control, increased asthma morbidity, and decreased response to inhaled corticosteroids. We hypothesized that obesity would be associated with decreased bronchodilator responsiveness in children and adolescents with asthma. In addition, we hypothesized that subjects who were obese and unresponsive to bronchodilator would have worse asthma control and would require more asthma controller medications.MethodsIn the Study of African Americans, Asthma, Genes, and Environments (SAGE II) and the Genes-environments and Admixture in Latino Americans (GALA II) study, two identical, parallel, case-control studies of asthma, we examined the association between obesity and bronchodilator response in 2,963 black and Latino subjects enrolled from 2008 to 2013 using multivariable logistic regression. Using bronchodilator responsiveness, we compared asthma symptoms, controller medication usage, and asthma exacerbations between nonobese (< 95th% BMI) and obese (≥ 95th% BMI) subjects.ResultsThe odds of being bronchodilator unresponsive were 24% (OR, 1.24; 95% CI, 1.03-1.49) higher among obese children and adolescents compared with their not obese counterparts after adjustment for age, race/ethnicity, sex, recruitment site, baseline lung function (FEV1/FVC), and controller medication. Bronchodilator-unresponsive obese subjects were more likely to report wheezing (OR, 1.38; 95% CI, 1.13-1.70), being awakened at night (OR, 1.34; 95% CI, 1.09-1.65), using leukotriene receptor inhibitors (OR, 1.33; 95% CI, 1.05-1.70), and using inhaled corticosteroid with long-acting β2-agonist (OR, 1.37; 95% CI, 1.05-1.78) than were their nonobese counterpart. These associations were not seen in the bronchodilator-responsive group.ConclusionsObesity is associated with bronchodilator unresponsiveness among black and Latino children and adolescents with asthma. The findings on obesity and bronchodilator unresponsiveness represent a unique opportunity to identify factors affecting asthma control in blacks and Latinos.

Published
2015

48. Genetic ancestry influences asthma susceptibility and lung function among Latinos

Author

Pino-Yanes, Maria, Thakur, Neeta, Gignoux, Christopher R, Galanter, Joshua M, Roth, Lindsey A, Eng, Celeste, Nishimura, Katherine K, Oh, Sam S, Vora, Hita, Huntsman, Scott, Nguyen, Elizabeth A, Hu, Donglei, Drake, Katherine A, Conti, David V, Moreno-Estrada, Andres, Sandoval, Karla, Winkler, Cheryl A, Borrell, Luisa N, Lurmann, Fred, Islam, Talat S, Davis, Adam, Farber, Harold J, Meade, Kelley, Avila, Pedro C, Serebrisky, Denise, Bibbins-Domingo, Kirsten, Lenoir, Michael A, Ford, Jean G, Brigino-Buenaventura, Emerita, Rodriguez-Cintron, William, Thyne, Shannon M, Sen, Saunak, Rodriguez-Santana, Jose R, Bustamante, Carlos D, Williams, L Keoki, Gilliland, Frank D, Gauderman, W James, Kumar, Rajesh, Torgerson, Dara G, and Burchard, Esteban G

Subjects
Biomedical and Clinical Sciences, Immunology, Asthma, Genetics, Human Genome, Lung, Clinical Research, Respiratory, Adolescent, Adult, Child, Female, Genetic Predisposition to Disease, Hispanic or Latino, Humans, Male, Odds Ratio, Racial Groups, United States, Young Adult, Genetic admixture, Hispanics, childhood asthma, minority, pulmonary function, Childhood asthma, Minority, Pulmonary function, Allergy
Abstract

BackgroundChildhood asthma prevalence and morbidity varies among Latinos in the United States, with Puerto Ricans having the highest and Mexicans the lowest.ObjectiveTo determine whether genetic ancestry is associated with the odds of asthma among Latinos, and secondarily whether genetic ancestry is associated with lung function among Latino children.MethodsWe analyzed 5493 Latinos with and without asthma from 3 independent studies. For each participant, we estimated the proportion of African, European, and Native American ancestry using genome-wide data. We tested whether genetic ancestry was associated with the presence of asthma and lung function among subjects with and without asthma. Odds ratios (OR) and effect sizes were assessed for every 20% increase in each ancestry.ResultsNative American ancestry was associated with lower odds of asthma (OR = 0.72, 95% CI: 0.66-0.78, P = 8.0 × 10(-15)), while African ancestry was associated with higher odds of asthma (OR = 1.40, 95% CI: 1.14-1.72, P = .001). These associations were robust to adjustment for covariates related to early life exposures, air pollution, and socioeconomic status. Among children with asthma, African ancestry was associated with lower lung function, including both pre- and post-bronchodilator measures of FEV1 (-77 ± 19 mL; P = 5.8 × 10(-5) and -83 ± 19 mL; P = 1.1 x 10(-5), respectively) and forced vital capacity (-100 ± 21 mL; P = 2.7 × 10(-6) and -107 ± 22 mL; P = 1.0 x 10(-6), respectively).ConclusionDifferences in the proportions of genetic ancestry can partially explain disparities in asthma susceptibility and lung function among Latinos.

Published
2015

50. Design Requirements to Enhance the Postural Control in Patients with Severe Spastic Quadriplegia

Author

Manzano-Hernandez, Paulina, Vidana-Zavala, David, Landa-Avila, Irma C., Aceves-Gonzalez, Carlos, Kacprzyk, Janusz, Series editor, Pal, Nikhil R., Advisory editor, Bello Perez, Rafael, Advisory editor, Corchado, Emilio S., Advisory editor, Hagras, Hani, Advisory editor, Kóczy, László T., Advisory editor, Kreinovich, Vladik, Advisory editor, Lin, Chin-Teng, Advisory editor, Lu, Jie, Advisory editor, Melin, Patricia, Advisory editor, Nedjah, Nadia, Advisory editor, Nguyen, Ngoc Thanh, Advisory editor, Wang, Jun, Advisory editor, Rebelo, Francisco, editor, and Soares, Marcelo, editor

Published
2018
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