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126 results on '"Di Narzo, Antonio"'

1. A mechanistic framework for cardiometabolic and coronary artery diseases

Author

Koplev, Simon, Seldin, Marcus, Sukhavasi, Katyayani, Ermel, Raili, Pang, Shichao, Zeng, Lingyao, Bankier, Sean, Di Narzo, Antonio, Cheng, Haoxiang, Meda, Vamsidhar, Ma, Angela, Talukdar, Husain, Cohain, Ariella, Amadori, Letizia, Argmann, Carmen, Houten, Sander M, Franzén, Oscar, Mocci, Giuseppe, Meelu, Omar A, Ishikawa, Kiyotake, Whatling, Carl, Jain, Anamika, Jain, Rajeev Kumar, Gan, Li-Ming, Giannarelli, Chiara, Roussos, Panos, Hao, Ke, Schunkert, Heribert, Michoel, Tom, Ruusalepp, Arno, Schadt, Eric E, Kovacic, Jason C, Lusis, Aldon J, and Björkegren, Johan LM

Subjects
Biological Sciences, Bioinformatics and Computational Biology, Biomedical and Clinical Sciences, Heart Disease - Coronary Heart Disease, Genetics, Heart Disease, Human Genome, Cardiovascular, Atherosclerosis, 2.1 Biological and endogenous factors, Coronary Artery Disease, Animals, Humans, Gene Regulatory Networks, Cardiometabolic Risk Factors, Female, Genetic Predisposition to Disease, Mice, Male, Middle Aged, Mice, Inbred C57BL, Disease Models, Animal, Databases, Genetic, Blood Glucose, Phenotype, Case-Control Studies, Adipose Tissue, Adipokines
Abstract

Coronary atherosclerosis results from the delicate interplay of genetic and exogenous risk factors, principally taking place in metabolic organs and the arterial wall. Here we show that 224 gene-regulatory coexpression networks (GRNs) identified by integrating genetic and clinical data from patients with (n = 600) and without (n = 250) coronary artery disease (CAD) with RNA-seq data from seven disease-relevant tissues in the Stockholm-Tartu Atherosclerosis Reverse Network Engineering Task (STARNET) study largely capture this delicate interplay, explaining >54% of CAD heritability. Within 89 cross-tissue GRNs associated with clinical severity of CAD, 374 endocrine factors facilitated inter-organ interactions, primarily along an axis from adipose tissue to the liver (n = 152). This axis was independently replicated in genetically diverse mouse strains and by injection of recombinant forms of adipose endocrine factors (EPDR1, FCN2, FSTL3 and LBP) that markedly altered blood lipid and glucose levels in mice. Altogether, the STARNET database and the associated GRN browser (http://starnet.mssm.edu) provide a multiorgan framework for exploration of the molecular interplay between cardiometabolic disorders and CAD.

Published
2022

4. Prediction of Causal Candidate Genes in Coronary Artery Disease Loci

Author

Brænne, Ingrid, Civelek, Mete, Vilne, Baiba, Di Narzo, Antonio, Johnson, Andrew D, Zhao, Yuqi, Reiz, Benedikt, Codoni, Veronica, Webb, Thomas R, Foroughi Asl, Hassan, Hamby, Stephen E, Zeng, Lingyao, Trégouët, David-Alexandre, Hao, Ke, Topol, Eric J, Schadt, Eric E, Yang, Xia, Samani, Nilesh J, Björkegren, Johan LM, Erdmann, Jeanette, Schunkert, Heribert, and Lusis, Aldons J

Subjects
Heart Disease, Cardiovascular, Atherosclerosis, Biotechnology, Heart Disease - Coronary Heart Disease, Human Genome, Genetics, Aetiology, 2.1 Biological and endogenous factors, Coronary Artery Disease, Female, Genetic Loci, Genetic Predisposition to Disease, Genetic Variation, Genome-Wide Association Study, Humans, Male, MicroRNAs, Polymorphism, Single Nucleotide, Predictive Value of Tests, Promoter Regions, Genetic, coronary artery disease, genome-wide association study, microRNAs, single-nucleotide polymorphism, systems biology, Leducq Consortium CAD Genomics‡, Cardiorespiratory Medicine and Haematology, Clinical Sciences, Cardiovascular System & Hematology
Abstract

ObjectiveGenome-wide association studies have to date identified 159 significant and suggestive loci for coronary artery disease (CAD). We now report comprehensive bioinformatics analyses of sequence variation in these loci to predict candidate causal genes.Approach and resultsAll annotated genes in the loci were evaluated with respect to protein-coding single-nucleotide polymorphism and gene expression parameters. The latter included expression quantitative trait loci, tissue specificity, and miRNA binding. High priority candidate genes were further identified based on literature searches and our experimental data. We conclude that the great majority of causal variations affecting CAD risk occur in noncoding regions, with 41% affecting gene expression robustly versus 6% leading to amino acid changes. Many of these genes differed from the traditionally annotated genes, which was usually based on proximity to the lead single-nucleotide polymorphism. Indeed, we obtained evidence that genetic variants at CAD loci affect 98 genes which had not been linked to CAD previously.ConclusionsOur results substantially revise the list of likely candidates for CAD and suggest that genome-wide association studies efforts in other diseases may benefit from similar bioinformatics analyses.

Published
2015

6. Cardiometabolic risk loci share downstream cis- and trans-gene regulation across tissues and diseases

Author

Franzén, Oscar, Ermel, Raili, Cohain, Ariella, Akers, Nicholas K., Di Narzo, Antonio, Talukdar, Husain A., Foroughi-Asl, Hassan, Giambartolomei, Claudia, Fullard, John F., Sukhavasi, Katyayani, Köks, Sulev, Gan, Li-Ming, Giannarelli, Chiara, Kovacic, Jason C., Betsholtz, Christer, Losic, Bojan, Michoel, Tom, Hao, Ke, Roussos, Panos, Skogsberg, Josefin, Ruusalepp, Arno, Schadt, Eric E., and Björkegren, Johan L. M.

Published
2016

8. Pericytes impair capillary blood flow and motor function after chronic spinal cord injury

Author

Li, Yaqing, Lucas-Osma, Ana M, Black, Sophie, Bandet, Mischa V, Stephens, Marilee J, Vavrek, Romana, Sanelli, Leo, Fenrich, Keith K, Di Narzo, Antonio F, Dracheva, Stella, Winship, Ian R, Fouad, Karim, and Bennett, David J

Subjects
Norepinephrine -- Dosage and administration, Blood flow -- Analysis, Spinal cord injuries -- Care and treatment -- Drug therapy, Tryptophan -- Health aspects, Enzymes -- Health aspects, Biological sciences, Health
Abstract

Blood vessels in the central nervous system (CNS) are controlled by neuronal activity. For example, widespread vessel constriction (vessel tone) is induced by brainstem neurons that release the monoamines serotonin and noradrenaline, and local vessel dilation is induced by glutamatergic neuron activity. Here we examined how vessel tone adapts to the loss of neuron-derived monoamines after spinal cord injury (SCI) in rats. We find that, months after the imposition of SCI, the spinal cord below the site of injury is in a chronic state of hypoxia owing to paradoxical excess activity of monoamine receptors (5-HT[sub.1]) on pericytes, despite the absence of monoamines. This monoamine-receptor activity causes pericytes to locally constrict capillaries, which reduces blood flow to ischemic levels. Receptor activation in the absence of monoamines results from the production of trace amines (such as tryptamine) by pericytes that ectopically express the enzyme aromatic L-amino acid decarboxylase (AADC), which synthesizes trace amines directly from dietary amino acids (such as tryptophan). Inhibition of monoamine receptors or of AADC, or even an increase in inhaled oxygen, produces substantial relief from hypoxia and improves motoneuron and locomotor function after SCI., Author(s): Yaqing Li [1]; Ana M Lucas-Osma [1]; Sophie Black [1]; Mischa V Bandet [2]; Marilee J Stephens [1]; Romana Vavrek [1]; Leo Sanelli [1]; Keith K Fenrich [1]; Antonio [...]

Published
2017
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9. Genome-wide association study identifies four novel loci associated with Alzheimer’s endophenotypes and disease modifiers

Author

Deming, Yuetiva, Li, Zeran, Kapoor, Manav, Harari, Oscar, Del-Aguila, Jorge L., Black, Kathleen, Carrell, David, Cai, Yefei, Fernandez, Maria Victoria, Budde, John, Ma, Shengmei, Saef, Benjamin, Howells, Bill, Huang, Kuan-lin, Bertelsen, Sarah, Fagan, Anne M., Holtzman, David M., Morris, John C., Kim, Sungeun, Saykin, Andrew J., De Jager, Philip L., Albert, Marilyn, Moghekar, Abhay, O’Brien, Richard, Riemenschneider, Matthias, Petersen, Ronald C., Blennow, Kaj, Zetterberg, Henrik, Minthon, Lennart, Van Deerlin, Vivianna M., Lee, Virginia Man-Yee, Shaw, Leslie M., Trojanowski, John Q., Schellenberg, Gerard, Haines, Jonathan L., Mayeux, Richard, Pericak-Vance, Margaret A., Farrer, Lindsay A., Peskind, Elaine R., Li, Ge, Di Narzo, Antonio F., Kauwe, John S. K., Goate, Alison M., Cruchaga, Carlos, Alzheimer’s Disease Neuroimaging Initiative (ADNI), and The Alzheimer Disease Genetic Consortium (ADGC)

Published
2017
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10. The HDAC9-associated risk locus promotes coronary artery disease by governing TWIST1

Author

Ma, Lijiang, primary, Bryce, Nicole S., additional, Turner, Adam W., additional, Di Narzo, Antonio F., additional, Rahman, Karishma, additional, Xu, Yang, additional, Ermel, Raili, additional, Sukhavasi, Katyayani, additional, d’Escamard, Valentina, additional, Chandel, Nirupama, additional, V’Gangula, Bhargavi, additional, Wolhuter, Kathryn, additional, Kadian-Dodov, Daniella, additional, Franzen, Oscar, additional, Ruusalepp, Arno, additional, Hao, Ke, additional, Miller, Clint L., additional, Björkegren, Johan L. M., additional, and Kovacic, Jason C., additional

Published
2022
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14. Genome-wide approach identifies a novel gene-maternal pre-pregnancy BMI interaction on preterm birth

Author

Hong, Xiumei, Hao, Ke, Ji, Hongkai, Peng, Shouneng, Sherwood, Ben, Di Narzo, Antonio, Tsai, Hui-Ju, Liu, Xin, Burd, Irina, Wang, Guoying, Ji, Yuelong, Caruso, Deanna, Mao, Guangyun, Bartell, Tami R., Zhang, Zhongyang, Pearson, Colleen, Heffner, Linda, Cerda, Sandra, Beaty, Terri H., Fallin, M. Daniele, Lee-Parritz, Aviva, Zuckerman, Barry, Weeks, Daniel E., and Wang, Xiaobin

Published
2017
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17. Profiling Microbiota from Multiple Sites in the Respiratory Tract to Identify a Biomarker for PM2.5Nitrate Exposure-Induced Pulmonary Damages

Author

Zhang, Jushan, Cheng, Haoxiang, Di Narzo, Antonio, Zhu, Yujie, Xie, Shuanshuan, Shao, Xiaowen, Zhang, Zhongyang, Chung, Sookja Kim, and Hao, Ke

Abstract

The microbiota present in the respiratory tract (RT) responds to environmental stimuli and engages in a continuous interaction with the host immune system to maintain homeostasis. A total of 40 C57BL/6 mice were divided into four groups and exposed to varying concentrations of PM2.5nitrate aerosol and clean air. After 10 weeks of exposure, assessments were conducted on the lung and airway microbiome, lung functions, and pulmonary inflammation. Additionally, we analyzed data from both mouse and human respiratory tract (RT) microbiomes to identify possible biomarkers for PM2.5exposure-induced pulmonary damages. On average, 1.5 and 13.5% inter-individual microbiome variations in the lung and airway were explained by exposure, respectively. In the airway, among the 60 bacterial OTUs (operational taxonomic units) > 0.05% proportion, 40 OTUs were significantly affected by PM2.5exposure (FDR ≤ 10%). Further, the airway microbiome was associated with peak expiratory flow (PEF) (p= 0.003), pulmonary neutrophil counts (p= 0.01), and alveolar 8-OHdG oxidative lesions (p= 0.0078). The Clostridialesorder bacteria showed the strongest signals. For example, the o_Clostridiales;f_;g_OTU was elevated by PM2.5nitrate exposure (p= 4.98 × 10–5) and negatively correlated with PEF (r= −0.585 and p= 2.4 × 10–4). It was also associated with the higher pulmonary neutrophil count (p= 8.47 × 10–5) and oxidative lesion (p= 7.17 × 10–3). In human data, we confirmed the association of airway Clostridialesorder bacteria with PM2.5exposure and lung function. For the first time, this study characterizes the impact of PM2.5exposure on the microbiome of multiple sites in the respiratory tract (RT) and its relevance to airflow obstructive diseases. By analyzing data from both humans and mice, we have identified bacteria belonging to the Clostridialesorder as a promising biomarker for PM2.5exposure-induced decline in pulmonary function and inflammation.

Published
2023
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18. Polygenic risk score for alcohol drinking behavior improves prediction of inflammatory bowel disease risk

Author

Di Narzo, Antonio F, primary, Hart, Amy, additional, Kosoy, Roman, additional, Peters, Lauren, additional, Stojmirovic, Aleksandar, additional, Cheng, Haoxiang, additional, Zhang, Zhongyang, additional, Shan, Mingxu, additional, Cho, Judy, additional, Kasarskis, Andrew, additional, Argmann, Carmen, additional, Peter, Inga, additional, Schadt, Eric E, additional, and Hao, Ke, additional

Published
2021
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19. Prenatal exposure to ambient air multi-pollutants significantly impairs intrauterine fetal development trajectory

Author

Shao, Xiaowen, primary, Cheng, Haoxiang, additional, Zhou, Jonathan, additional, Zhang, Jushan, additional, Zhu, Yujie, additional, Yang, Chun, additional, Di Narzo, Antonio, additional, Yu, Jing, additional, Shen, Yuan, additional, Li, Yuanyuan, additional, Xu, Shunqing, additional, Zhang, Zhongyang, additional, Chen, Jia, additional, Cheng, Jiajing, additional, and Hao, Ke, additional

Published
2020
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20. Rare loss-of-function mutations of PTGIR are enriched in fibromuscular dysplasia

Author

Georges, Adrien, primary, Albuisson, Juliette, additional, Berrandou, Takiy, additional, Dupré, Délia, additional, Lorthioir, Aurélien, additional, D’Escamard, Valentina, additional, Di Narzo, Antonio F, additional, Kadian-Dodov, Daniella, additional, Olin, Jeffrey W, additional, Warchol-Celinska, Ewa, additional, Prejbisz, Aleksander, additional, Januszewicz, Andrzej, additional, Bruneval, Patrick, additional, Baranowska, Anna A, additional, Webb, Tom R, additional, Hamby, Stephen E, additional, Samani, Nilesh J, additional, Adlam, David, additional, Fendrikova-Mahlay, Natalia, additional, Hazen, Stanley, additional, Wang, Yu, additional, Yang, Min-Lee, additional, Hunker, Kristina, additional, Combaret, Nicolas, additional, Motreff, Pascal, additional, Chédid, Antoine, additional, Fiquet, Béatrice, additional, Plouin, Pierre-François, additional, Mousseaux, Elie, additional, Azarine, Arshid, additional, Amar, Laurence, additional, Azizi, Michel, additional, Gornik, Heather L, additional, Ganesh, Santhi K, additional, Kovacic, Jason C, additional, Jeunemaitre, Xavier, additional, and Bouatia-Naji, Nabila, additional

Published
2020
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21. 620 A MOLECULAR NETWORK SURVEY PREDICTS NICKEL EXPOSURE AS A POTENTIAL ENVIRONMENTAL TRIGGER OF INFLAMMATORY BOWEL DISEASE

Author

Wei, Gabrielle, primary, Huang, Ruiqi, additional, Kosoy, Roman, additional, Di Narzo, Antonio F., additional, Hao, Ke, additional, Zhu, Jun, additional, Dubinsky, Marla, additional, Sands, Bruce E., additional, Schadt, Eric E., additional, Colombel, Jean Frederic, additional, Cho, Judy H., additional, Kasarskis, Andrew, additional, Suarez-Farinas, Mayte, additional, and Argmann, Carmen A., additional

Published
2020
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22. Rare Loss-of-function Mutations ofPTGIRIdentified in Fibromuscular Dysplasia and Spontaneous Coronary Artery Dissection

Author

Georges, Adrien, primary, Albuisson, Juliette, additional, Berrandou, Takiy, additional, Dupré, Délia, additional, Lorthioir, Aurélien, additional, D’Escamard, Valentina, additional, Di Narzo, Antonio F, additional, Kadian-Dodov, Daniella, additional, Olin, Jeffrey W, additional, Warchol-Celinska, Ewa, additional, Prejbisz, Aleksander, additional, Januszewicz, Andrzej, additional, Bruneval, Patrick, additional, Baranowska, Anna A., additional, Webb, Tom R., additional, Hamby, Stephen E., additional, Samani, Nilesh J., additional, Adlam, David, additional, Fendrikova-Mahlay, Natalia, additional, Hazen, Stanley, additional, Wang, Yu, additional, Yang, Min-Lee, additional, Hunker, Kristina, additional, Combaret, Nicolas, additional, Motreff, Pascal, additional, Chédid, Antoine, additional, Fiquet, Béatrice, additional, Plouin, Pierre-François, additional, Mousseaux, Elie, additional, Azarine, Arshid, additional, Amar, Laurence, additional, Azizi, Michel, additional, Gornik, Heather L., additional, Ganesh, Santhi K., additional, Kovacic, Jason C., additional, Jeunemaitre, Xavier, additional, and Bouatia-Naji, Nabila, additional

Published
2019
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23. A plasma proteogenomic signature for fibromuscular dysplasia

Author

Olin, Jeffrey W, primary, Di Narzo, Antonio F, additional, d’Escamard, Valentina, additional, Kadian-Dodov, Daniella, additional, Cheng, Haoxiang, additional, Georges, Adrien, additional, King, Annette, additional, Thomas, Allison, additional, Barwari, Temo, additional, Michelis, Katherine C, additional, Bouchareb, Rihab, additional, Bander, Emir, additional, Anyanwu, Anelechi, additional, Stelzer, Paul, additional, Filsoufi, Farzan, additional, Florman, Sander, additional, Civelek, Mete, additional, Debette, Stephanie, additional, Jeunemaitre, Xavier, additional, Björkegren, Johan L M, additional, Mayr, Manuel, additional, Bouatia-Naji, Nabila, additional, Hao, Ke, additional, and Kovacic, Jason C, additional

Published
2019
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24. Bio3Air, an integrative system for monitoring individual-level air pollutant exposure with high time and spatial resolution

Author

Cheng, Haoxiang, primary, Wang, Liping, additional, Wang, Dongbin, additional, Zhang, Jushan, additional, Cheng, Long, additional, Yao, Pengfei, additional, Zhang, Zhongyang, additional, Di Narzo, Antonio, additional, Shen, Yuan, additional, Yu, Jing, additional, Wang, Changhui, additional, Fan, Lihong, additional, Lu, Jianwei, additional, Jiang, Jingkun, additional, and Hao, Ke, additional

Published
2019
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26. Gut microbiota density influences host physiology and is shaped by host and microbial factors

Author

Contijoch, Eduardo J, primary, Britton, Graham J, additional, Yang, Chao, additional, Mogno, Ilaria, additional, Li, Zhihua, additional, Ng, Ruby, additional, Llewellyn, Sean R, additional, Hira, Sheela, additional, Johnson, Crystal, additional, Rabinowitz, Keren M, additional, Barkan, Revital, additional, Dotan, Iris, additional, Hirten, Robert P, additional, Fu, Shih-Chen, additional, Luo, Yuying, additional, Yang, Nancy, additional, Luong, Tramy, additional, Labrias, Philippe R, additional, Lira, Sergio, additional, Peter, Inga, additional, Grinspan, Ari, additional, Clemente, Jose C, additional, Kosoy, Roman, additional, Kim-Schulze, Seunghee, additional, Qin, Xiaochen, additional, Castillo, Anabella, additional, Hurley, Amanda, additional, Atreja, Ashish, additional, Rogers, Jason, additional, Fasihuddin, Farah, additional, Saliaj, Merjona, additional, Nolan, Amy, additional, Reyes-Mercedes, Pamela, additional, Rodriguez, Carina, additional, Aly, Sarah, additional, Santa-Cruz, Kenneth, additional, Peters, Lauren, additional, Suárez-Fariñas, Mayte, additional, Huang, Ruiqi, additional, Hao, Ke, additional, Zhu, Jun, additional, Zhang, Bin, additional, Losic, Bojan, additional, Irizar, Haritz, additional, Song, Won-Min, additional, Di Narzo, Antonio, additional, Wang, Wenhui, additional, Cohen, Benjamin L, additional, DiMaio, Christopher, additional, Greenwald, David, additional, Itzkowitz, Steven, additional, Lucas, Aimee, additional, Marion, James, additional, Maser, Elana, additional, Ungaro, Ryan, additional, Naymagon, Steven, additional, Novak, Joshua, additional, Shah, Brijen, additional, Ullman, Thomas, additional, Rubin, Peter, additional, George, James, additional, Legnani, Peter, additional, Telesco, Shannon E, additional, Friedman, Joshua R, additional, Brodmerkel, Carrie, additional, Plevy, Scott, additional, Cho, Judy H, additional, Colombel, Jean-Frederic, additional, Schadt, Eric E, additional, Argmann, Carmen, additional, Dubinsky, Marla, additional, Kasarskis, Andrew, additional, Sands, Bruce, additional, and Faith, Jeremiah J, additional

Published
2019
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27. Airway microbiome is associated with respiratory functions and responses to ambient particulate matter exposure

Author

Wang, Liping, primary, Cheng, Haoxiang, additional, Wang, Dongbin, additional, Zhao, Bo, additional, Zhang, Jushan, additional, Cheng, Long, additional, Yao, Pengfei, additional, Di Narzo, Antonio, additional, Shen, Yuan, additional, Yu, Jing, additional, Li, Yuanyuan, additional, Xu, Shunqing, additional, Chen, Jia, additional, Fan, Lihong, additional, Lu, Jianwei, additional, Jiang, Jingkun, additional, Zhou, Yang, additional, Wang, Changhui, additional, Zhang, Zhongyang, additional, and Hao, Ke, additional

Published
2019
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28. Genetic regulation of the placental transcriptome underlies birth weight and risk of childhood obesity

Author

Peng, Shouneng, primary, Deyssenroth, Maya A., additional, Di Narzo, Antonio F., additional, Cheng, Haoxiang, additional, Zhang, Zhongyang, additional, Lambertini, Luca, additional, Ruusalepp, Arno, additional, Kovacic, Jason C., additional, Bjorkegren, Johan L. M., additional, Marsit, Carmen J., additional, Chen, Jia, additional, and Hao, Ke, additional

Published
2018
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29. Author response: Gut microbiota density influences host physiology and is shaped by host and microbial factors

Author

Contijoch, Eduardo J, primary, Britton, Graham J, additional, Yang, Chao, additional, Mogno, Ilaria, additional, Li, Zhihua, additional, Ng, Ruby, additional, Llewellyn, Sean R, additional, Hira, Sheela, additional, Johnson, Crystal, additional, Rabinowitz, Keren M, additional, Barkan, Revital, additional, Dotan, Iris, additional, Hirten, Robert P, additional, Fu, Shih-Chen, additional, Luo, Yuying, additional, Yang, Nancy, additional, Luong, Tramy, additional, Labrias, Philippe R, additional, Lira, Sergio, additional, Peter, Inga, additional, Grinspan, Ari, additional, Clemente, Jose C, additional, Kosoy, Roman, additional, Kim-Schulze, Seunghee, additional, Qin, Xiaochen, additional, Castillo, Anabella, additional, Hurley, Amanda, additional, Atreja, Ashish, additional, Rogers, Jason, additional, Fasihuddin, Farah, additional, Saliaj, Merjona, additional, Nolan, Amy, additional, Reyes-Mercedes, Pamela, additional, Rodriguez, Carina, additional, Aly, Sarah, additional, Santa-Cruz, Kenneth, additional, Peters, Lauren, additional, Suárez-Fariñas, Mayte, additional, Huang, Ruiqi, additional, Hao, Ke, additional, Zhu, Jun, additional, Zhang, Bin, additional, Losic, Bojan, additional, Irizar, Haritz, additional, Song, Won-Min, additional, Di Narzo, Antonio, additional, Wang, Wenhui, additional, Cohen, Benjamin L, additional, DiMaio, Christopher, additional, Greenwald, David, additional, Itzkowitz, Steven, additional, Lucas, Aimee, additional, Marion, James, additional, Maser, Elana, additional, Ungaro, Ryan, additional, Naymagon, Steven, additional, Novak, Joshua, additional, Shah, Brijen, additional, Ullman, Thomas, additional, Rubin, Peter, additional, George, James, additional, Legnani, Peter, additional, Telesco, Shannon E, additional, Friedman, Joshua R, additional, Brodmerkel, Carrie, additional, Plevy, Scott, additional, Cho, Judy H, additional, Colombel, Jean-Frederic, additional, Schadt, Eric E, additional, Argmann, Carmen, additional, Dubinsky, Marla, additional, Kasarskis, Andrew, additional, Sands, Bruce, additional, and Faith, Jeremiah J, additional

Published
2018
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30. Radiogenomics Consortium Genome-Wide Association Study Meta-Analysis of Late Toxicity After Prostate Cancer Radiotherapy

Author

L. Kerns, Sarah, Fachal, Laura, Dorling, Leila, C. Barnett, Gillian, Baran, Andrea, R. Peterson, Derick, Hollenberg, Michelle, Hao, Ke, Di Narzo, Antonio, Eren Ahsen, Mehmet, Pandey, Gaurav, Søren, M. Bentzen, Janelsins, Michelle, M. Elliott, Rebecca, D. P. Pharoah, Paul, G. Burnet, Neil, P. Dearnaley, David, L. Gulliford, Sarah, Hall, Emma, R. Sydes, Matthew, Miguel, E. Aguado-Barrera, Antonio, Gomez-Caamano, M. Carballo, Ana, Peleteiro, Paula, Ramon, Lobato-Busto, Stock, Richard, N. Stone, Nelson, Ostrer, Harry, Usmani, Nawaid, Singhal, Sandeep, Tsuji, Hiroshi, Imai, Takashi, Saito, Shiro, Eeles, Rosalind, DeRuyck, Kim, Parliament, Matthew, M. Dunning, Alison, Vega, Ana, S. Rosenstein, Barry, and M. L.West, Catharine

Abstract

Background: A total of 10%–20% of patients develop long-term toxicity following radiotherapy for prostate cancer. Identification of common genetic variants associated with susceptibility to radiotoxicity might improve risk prediction and inform functional mechanistic studies. Methods: We conducted an individual patient data meta-analysis of six genome-wide association studies (n=3871) in men of European ancestry who underwent radiotherapy for prostate cancer. Radiotoxicities (increased urinary frequency, decreased urinary stream, hematuria, rectal bleeding) were graded prospectively. We used grouped relative risk models to test associations with approximately 6 million genotyped or imputed variants (time to first grade 2 or higher toxicity event). Variants with two-sided Pmeta less than 5 X E-8 were considered statistically significant. Bayesian false discovery probability provided an additional measure of confidence. Statistically significant variants were evaluated in three Japanese cohorts (n=962). All statistical tests were two-sided. Results: Meta-analysis of the European ancestry cohorts identified three genomic signals: single nucleotide polymorphism rs17055178 with rectal bleeding (Pmeta = 6.2 X E-10), rs10969913 with decreased urinary stream (Pmeta = 2.9 X E-10), and rs11122573 with hematuria (Pmeta = 1.8 X E-8). Fine-scale mapping of these three regions was used to identify another independent signal (rs147121532) associated with hematuria (Pconditional = 4.7 X E-6). Credible causal variants at these four signals lie in gene-regulatory regions, some modulating expression of nearby genes. Previously identified variants showed consistent.

Published
2019

31. High-Throughput Identification of the Plasma Proteomic Signature of Inflammatory Bowel Disease

Author

Di Narzo, Antonio F, primary, Brodmerkel, Carrie, additional, Telesco, Shannon E, additional, Argmann, Carmen, additional, Peters, Lauren A, additional, Li, Katherine, additional, Kidd, Brian, additional, Dudley, Joel, additional, Cho, Judy, additional, Schadt, Eric E, additional, Kasarskis, Andrew, additional, Dobrin, Radu, additional, and Hao, Ke, additional

Published
2018
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32. Tu1802 - Disease Demarcation in Ulcerative Colitis is Associated with Different Patterns of Gene Expression

Author

Suarez-Farinas, Mayte, primary, Huang, Ruiqi, additional, Kosoy, Roman, additional, Irizar, Aritz, additional, Losic, Bojan, additional, Wei, Gabrielle, additional, Peters, Lauren A., additional, Song, Won-min, additional, Di Narzo, Antonio F., additional, Wang, Wenhui, additional, Perrigoue, Jacqueline, additional, Castillo, Anabella, additional, Rogers, Jason, additional, Atreja, Ashish, additional, Hurley, Amanda, additional, Mahajan, Milind, additional, Zhang, Bin, additional, Stojmirović, Aleksandar, additional, Curran, Mark, additional, Dobrin, Radu, additional, Dubinsky, Marla, additional, Hao, Ke, additional, Zhu, Jun, additional, Schadt, Eric E., additional, Plevy, Scott, additional, Friedman, Joshua R., additional, Brodmerkel, Carrie, additional, Sands, Bruce E., additional, Kasarskis, Andrew, additional, Ungaro, Ryan C., additional, Colombel, Jean Frederic, additional, and Argmann, Carmen A., additional

Published
2018
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33. Gut microbiota density influences host physiology and is shaped by host and microbial factors

Author

Contijoch, Eduardo J., primary, Britton, Graham J., additional, Yang, Chao, additional, Mogno, Ilaria, additional, Li, Zhihua, additional, Ng, Ruby, additional, Llewellyn, Sean R., additional, Hira, Sheela, additional, Johnson, Crystal, additional, Rabinowitz, Keren M., additional, Barkan, Revital, additional, Dotan, Iris, additional, Hirten, Robert P., additional, Fu, Shih-Chen, additional, Luo, Yuying, additional, Yang, Nancy, additional, Luong, Tramy, additional, Labrias, Philippe R., additional, Lira, Sergio A., additional, Peter, Inga, additional, Grinspan, Ari, additional, Clemente, Jose C., additional, Kosoy, Roman, additional, Kim-Schulze, Seunghee, additional, Qin, Xiaochen, additional, Castillo, Anabella, additional, Hurley, Amanda, additional, Atreja, Ashish, additional, Rogers, Jason, additional, Fasihuddin, Farah, additional, Saliaj, Merjona, additional, Nolan, Amy, additional, Reyes-Mercedes, Pamela, additional, Rodriguez, Carina, additional, Aly, Sarah, additional, Santa-Cruz, Kenneth, additional, Peters, Lauren A., additional, Suárez-Fariñas, Mayte, additional, Huang, Ruiqi, additional, Hao, Ke, additional, Zhu, Jun, additional, Zhang, Bin, additional, Losic, Bojan, additional, Irizar, Haritz, additional, Song, Won-Min, additional, Di Narzo, Antonio, additional, Wang, Wenhui, additional, Cohen, Benjamin L., additional, DiMaio, Christopher, additional, Greenwald, David, additional, Itzkowitz, Steven, additional, Lucas, Aimee, additional, Marion, James, additional, Maser, Elana, additional, Ungaro, Ryan, additional, Naymagon, Steven, additional, Novak, Joshua, additional, Shah, Brijen, additional, Ullman, Thomas, additional, Rubin, Peter, additional, George, James, additional, Legnani, Peter, additional, Telesco, Shannon E, additional, Friedman, Joshua R., additional, Brodmerkel, Carrie, additional, Plevy, Scott, additional, Cho, Judy, additional, Colombel, Jean-Frederic, additional, Schadt, Eric, additional, Argmann, Carmen, additional, Dubinsky, Marla, additional, Kasarskis, Andrew, additional, Sands, Bruce, additional, and Faith, Jeremiah J., additional

Published
2018
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36. Test of Four Colon Cancer Risk-Scores in Formalin Fixed Paraffin Embedded Microarray Gene Expression Data

Author

Di Narzo, Antonio F., Tejpar, Sabine, Rossi, Simona, Yan, Pu, Popovici, Vlad, Wirapati, Pratyaksha, Budinska, Eva, Xie, Tao, Estrella, Heather, Pavlicek, Adam, Mao, Mao, Martin, Eric, Scott, Weinrich, Bosman, Fred T., Roth, Arnaud, Delorenzi, Mauro, Di Narzo, Antonio F., Tejpar, Sabine, Rossi, Simona, Yan, Pu, Popovici, Vlad, Wirapati, Pratyaksha, Budinska, Eva, Xie, Tao, Estrella, Heather, Pavlicek, Adam, Mao, Mao, Martin, Eric, Scott, Weinrich, Bosman, Fred T., Roth, Arnaud, and Delorenzi, Mauro

Abstract

Background Prognosis prediction for resected primary colon cancer is based on the T-stage Node Metastasis (TNM) staging system. We investigated if four well-documented gene expression risk scores can improve patient stratification. Methods Microarray-based versions of risk-scores were applied to a large independent cohort of 688 stage II/III tumors from the PETACC-3 trial. Prognostic value for relapse-free survival (RFS), survival after relapse (SAR), and overall survival (OS) was assessed by regression analysis. To assess improvement over a reference, prognostic model was assessed with the area under curve (AUC) of receiver operating characteristic (ROC) curves. All statistical tests were two-sided, except the AUC increase. Results All four risk scores (RSs) showed a statistically significant association (single-test, P < .0167) with OS or RFS in univariate models, but with HRs below 1.38 per interquartile range. Three scores were predictors of shorter RFS, one of shorter SAR. Each RS could only marginally improve an RFS or OS model with the known factors T-stage, N-stage, and microsatellite instability (MSI) status (AUC gains < 0.025 units). The pairwise interscore discordance was never high (maximal Spearman correlation = 0.563) A combined score showed a trend to higher prognostic value and higher AUC increase for OS (HR = 1.74, 95% confidence interval [CI] = 1.44 to 2.10, P < .001, AUC from 0.6918 to 0.7321) and RFS (HR = 1.56, 95% CI = 1.33 to 1.84, P < .001, AUC from 0.6723 to 0.6945) than any single score. Conclusions The four tested gene expression-based risk scores provide prognostic information but contribute only marginally to improving models based on established risk factors. A combination of the risk scores might provide more robust information. Predictors of RFS and SAR might need to be different

Published
2017

37. A functional genomics predictive network model identifies regulators of inflammatory bowel disease

Author

Peters, Lauren A, primary, Perrigoue, Jacqueline, additional, Mortha, Arthur, additional, Iuga, Alina, additional, Song, Won-min, additional, Neiman, Eric M, additional, Llewellyn, Sean R, additional, Di Narzo, Antonio, additional, Kidd, Brian A, additional, Telesco, Shannon E, additional, Zhao, Yongzhong, additional, Stojmirovic, Aleksandar, additional, Sendecki, Jocelyn, additional, Shameer, Khader, additional, Miotto, Riccardo, additional, Losic, Bojan, additional, Shah, Hardik, additional, Lee, Eunjee, additional, Wang, Minghui, additional, Faith, Jeremiah J, additional, Kasarskis, Andrew, additional, Brodmerkel, Carrie, additional, Curran, Mark, additional, Das, Anuk, additional, Friedman, Joshua R, additional, Fukui, Yoshinori, additional, Humphrey, Mary Beth, additional, Iritani, Brian M, additional, Sibinga, Nicholas, additional, Tarrant, Teresa K, additional, Argmann, Carmen, additional, Hao, Ke, additional, Roussos, Panos, additional, Zhu, Jun, additional, Zhang, Bin, additional, Dobrin, Radu, additional, Mayer, Lloyd F, additional, and Schadt, Eric E, additional

Published
2017
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38. CEREBROSPINAL FLUID ENDOPHENOTYPES PROVIDE INSIGHT INTO BIOLOGY UNDERLYING ALZHEIMER'S DISEASE

Author

Deming, Yuetiva, primary, Kapoor, Manav, additional, Li, Zeran, additional, Harari, Oscar, additional, Black, Kathleen, additional, Del-Aguila, Jorge L., additional, Carrell, David, additional, Cai, Yefei, additional, Fernandez, Maria Victoria, additional, Budde, John P., additional, Ma, Shengmei, additional, Saef, Benjamin, additional, Howells, Bill, additional, Huang, Kuan-lin, additional, Bertelsen, Sarah, additional, Fagan, Anne M., additional, Holtzman, David M., additional, Morris, John C., additional, Kim, Sungeun, additional, Saykin, Andrew J., additional, De Jager, Philip L., additional, Albert, Marilyn S., additional, Moghekar, Abhay, additional, o'Brien, Richard, additional, Riemenschneider, Matthias, additional, Petersen, Ronald C., additional, Blennow, Kaj, additional, Zetterberg, Henrik, additional, Minthon, Lennart, additional, Van Deerlin, Vivianna M., additional, M-Y Lee, Virginia, additional, Shaw, Leslie M., additional, Trojanowski, John Q., additional, Schellenberg, Gerard D., additional, Haines, Jonathan L., additional, Mayeux, Richard, additional, Pericak-Vance, Margaret A., additional, Farrer, Lindsay A., additional, Peskind, Elaine R., additional, Li, Ge, additional, Molinuevo, José Luis, additional, Lleó, Alberto, additional, Clarimon, Jordi, additional, Pastor, Pau, additional, Di Narzo, Antonio, additional, Piccio, Laura, additional, Kauwe, John, additional, Goate, Alison M., additional, and Cruchaga, Carlos, additional

Published
2017
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39. High-Throughput Characterization of Blood Serum Proteomics of IBD Patients with Respect to Aging and Genetic Factors

Author

Di Narzo, Antonio F., primary, Telesco, Shannon E., additional, Brodmerkel, Carrie, additional, Argmann, Carmen, additional, Peters, Lauren A., additional, Li, Katherine, additional, Kidd, Brian, additional, Dudley, Joel, additional, Cho, Judy, additional, Schadt, Eric E., additional, Kasarskis, Andrew, additional, Dobrin, Radu, additional, and Hao, Ke, additional

Published
2017
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40. Su1858 Integrative Networks Identify Novel Regulators of Susceptibility and Pathogenesis of Inflammatory Bowel Disease

Author

Peters, Lauren, primary, Perrigoue, Jacqueline, additional, Mortha, Arthur, additional, Stojmirovic, Aleksandar, additional, Neiman, Eric M., additional, Iuga, Alina, additional, Song, Won-min, additional, Kidd, Brian A., additional, Losic, Bojan, additional, Llewellyn, Sean, additional, Miotto, Riccardo, additional, Shameer, Khader, additional, Zhao, Yongzhong, additional, Di Narzo, Antonio, additional, Shah, Hardik, additional, Cohain, Ariella, additional, Dudley, Joel T., additional, Faith, Jeremiah, additional, Merad, Miriam, additional, Fukui, Fumiyuki, additional, Iritani, Brian, additional, Sibinga, Nicholas, additional, Tarrant, Teresa, additional, Argmann, Carmen, additional, Kasarskis, Andrew, additional, Curran, Mark, additional, Das, Anuk, additional, Dobrin, Radu, additional, Hao, Ke, additional, Roussos, Panos, additional, Zhang, Bin, additional, Zhu, Jun, additional, Mayer, Lloyd F., additional, Friedman, Joshua, additional, and Schadt, Eric E., additional

Published
2016
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42. Meta-analysis of 65,734 Individuals Identifies TSPAN15 and SLC44A2 as Two Susceptibility Loci for Venous Thromboembolism

Author

Germain, Marine, primary, Chasman, Daniel I., additional, de Haan, Hugoline, additional, Tang, Weihong, additional, Lindström, Sara, additional, Weng, Lu-Chen, additional, de Andrade, Mariza, additional, de Visser, Marieke C.H., additional, Wiggins, Kerri L., additional, Suchon, Pierre, additional, Saut, Noémie, additional, Smadja, David M., additional, Le Gal, Grégoire, additional, van Hylckama Vlieg, Astrid, additional, Di Narzo, Antonio, additional, Hao, Ke, additional, Nelson, Christopher P., additional, Rocanin-Arjo, Ares, additional, Folkersen, Lasse, additional, Monajemi, Ramin, additional, Rose, Lynda M., additional, Brody, Jennifer A., additional, Slagboom, Eline, additional, Aïssi, Dylan, additional, Gagnon, France, additional, Deleuze, Jean-Francois, additional, Deloukas, Panos, additional, Tzourio, Christophe, additional, Dartigues, Jean-Francois, additional, Berr, Claudine, additional, Taylor, Kent D., additional, Civelek, Mete, additional, Eriksson, Per, additional, Psaty, Bruce M., additional, Houwing-Duitermaat, Jeanine, additional, Goodall, Alison H., additional, Cambien, François, additional, Kraft, Peter, additional, Amouyel, Philippe, additional, Samani, Nilesh J., additional, Basu, Saonli, additional, Ridker, Paul M., additional, Rosendaal, Frits R., additional, Kabrhel, Christopher, additional, Folsom, Aaron R., additional, Heit, John, additional, Reitsma, Pieter H., additional, Trégouët, David-Alexandre, additional, Smith, Nicholas L., additional, and Morange, Pierre-Emmanuel, additional

Published
2015
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43. Genome-wide approach identifies a novel gene-maternal pre-pregnancy BMI interaction on preterm birth.

Author

Xiumei Hong, Ke Hao, Hongkai Ji, Shouneng Peng, Sherwood, Ben, Di Narzo, Antonio, Hui-Ju Tsai, Xin Liu, Irina Burd, Guoying Wang, Yuelong Ji, Deanna Caruso, Guangyun Mao, Tami R. Bartell, Zhongyang Zhang, Pearson, Colleen, Heffner, Linda, Cerda, Sandra, Beaty, Terri H., and Fallin, M. Daniele

Abstract

Preterm birth (PTB) contributes significantly to infant mortality and morbidity with lifelong impact. Few robust genetic factors of PTB have been identified. Such 'missing heritability' may be partly due to gene × environment interactions (G × E), which is largely unexplored. Here we conduct genome-wide G × E analyses of PTB in 1,733 African-American women (698 mothers of PTB; 1,035 of term birth) from the Boston Birth Cohort. We show that maternal COL24A1 variants have a significant genome-wide interaction with maternal pre-pregnancy overweight/obesity on PTB risk, with rs11161721 (PG × E=1.8 × 10-8; empirical PG × E=1.2 × 10-8) as the top hit. This interaction is replicated in African-American mothers (PG × E=0.01) from an independent cohort and in meta-analysis (PG × E=3.6 × 10-9), but is not replicated in Caucasians. In adipose tissue, rs11161721 is significantly associated with altered COL24A1 expression. Our findings may provide new insight into the aetiology of PTB and improve our ability to predict and prevent PTB. [ABSTRACT FROM AUTHOR]

Published
2017
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47. A common haplotype lowers PU.1 expression in myeloid cells and delays onset of Alzheimer's disease

Author

Huang, Kuan-lin, Marcora, Edoardo, Pimenova, Anna A, Di Narzo, Antonio F, Kapoor, Manav, Jin, Sheng Chih, Harari, Oscar, Bertelsen, Sarah, Fairfax, Benjamin P, Czajkowski, Jake, Chouraki, Vincent, Grenier-Boley, Benjamin, Bellenguez, Céline, Deming, Yuetiva, McKenzie, Andrew, Raj, Towfique, Renton, Alan E, Budde, John, Smith, Albert, Fitzpatrick, Annette, Bis, Joshua C, DeStefano, Anita, Adams, Hieab H H, Ikram, M Arfan, van der Lee, Sven, Del-Aguila, Jorge L, Fernandez, Maria Victoria, Ibañez, Laura, Sims, Rebecca, Escott-Price, Valentina, Mayeux, Richard, Haines, Jonathan L, Farrer, Lindsay A, Pericak-Vance, Margaret A, Lambert, Jean Charles, van Duijn, Cornelia, Launer, Lenore, Seshadri, Sudha, Williams, Julie, Amouyel, Philippe, Schellenberg, Gerard D, Zhang, Bin, Borecki, Ingrid, Kauwe, John S K, Cruchaga, Carlos, Hao, Ke, and Goate, Alison M

Abstract

A genome-wide survival analysis of 14,406 Alzheimer's disease (AD) cases and 25,849 controls identified eight previously reported AD risk loci and 14 novel loci associated with age at onset. Linkage disequilibrium score regression of 220 cell types implicated the regulation of myeloid gene expression in AD risk. The minor allele of rs1057233 (G), within the previously reported CELF1 AD risk locus, showed association with delayed AD onset and lower expression of SPI1 in monocytes and macrophages. SPI1 encodes PU.1, a transcription factor critical for myeloid cell development and function. AD heritability was enriched within the PU.1 cistrome, implicating a myeloid PU.1 target gene network in AD. Finally, experimentally altered PU.1 levels affected the expression of mouse orthologs of many AD risk genes and the phagocytic activity of mouse microglial cells. Our results suggest that lower SPI1 expression reduces AD risk by regulating myeloid gene expression and cell function.

Published
2017
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48. Estimating accruals models in Europe: industry-based approaches versus a data-driven approach

Author

Marco Maria Mattei, Antonio Fabio Di Narzo, Marzia Freo, Di Narzo, Antonio F., Freo, Marzia, and Mattei, Marco Maria

Subjects
Estimation, Economics and Econometrics, 050208 finance, Actuarial science, Earnings management, accruals models, abnormal accruals (AA), small capital markets, mixture model (MIX), Accrual, 05 social sciences, 050201 accounting, Variety (cybernetics), Data-driven, Earnings management, 0502 economics and business, Economics, accruals models, abnormal accruals (AA), small capital markets, mixture model (MIX)
Abstract

Accruals models have been estimated using a variety of approaches, but the industry-based cross-sectional approach currently seems to be the standard method. This estimation approach cannot be easily used in the vast majority of European countries where several industry groups do not have sufficient yearly observations. Using data from France, Germany, Italy and the UK, we artificially induce earnings manipulations to investigate how the ability to detect those manipulations through accruals models is affected by the use of different industry classifications. Moreover, we propose an alternative estimation approach based on a data-driven statistical procedure that provides an optimal choice of estimation samples. Our analyses show that enlarging the industry classification and/or pooling observations across years reduces the probability of discovering earnings manipulations but allows for the estimation of abnormal accruals (AA) for more firms. The data-driven approach, however, in most cases outperforms the industry-based estimation approaches without sample attrition. This result suggests that there is still ample room for improving the accruals model estimation process for capital markets of European countries. Furthermore, the analysis documents which accruals model outperforms the others in each of the four countries and the probabilities to detect earning management in a high variety of circumstances.

Published
2018

49. Profiling Microbiota from Multiple Sites in the Respiratory Tract to Identify a Biomarker for PM 2.5 Nitrate Exposure-Induced Pulmonary Damages.

Author

Zhang J, Cheng H, Di Narzo A, Zhu Y, Xie S, Shao X, Zhang Z, Chung SK, and Hao K

Subjects
Humans, Mice, Animals, Nitrates, Particulate Matter toxicity, Particulate Matter analysis, Mice, Inbred C57BL, Lung, Biomarkers, Organic Chemicals, Environmental Exposure analysis, Air Pollutants toxicity, Air Pollutants analysis, Microbiota
Abstract

The microbiota present in the respiratory tract (RT) responds to environmental stimuli and engages in a continuous interaction with the host immune system to maintain homeostasis. A total of 40 C57BL/6 mice were divided into four groups and exposed to varying concentrations of PM 2.5 nitrate aerosol and clean air. After 10 weeks of exposure, assessments were conducted on the lung and airway microbiome, lung functions, and pulmonary inflammation. Additionally, we analyzed data from both mouse and human respiratory tract (RT) microbiomes to identify possible biomarkers for PM 2.5 exposure-induced pulmonary damages. On average, 1.5 and 13.5% inter-individual microbiome variations in the lung and airway were explained by exposure, respectively. In the airway, among the 60 bacterial OTUs (operational taxonomic units) > 0.05% proportion, 40 OTUs were significantly affected by PM 2.5 exposure (FDR ≤ 10%). Further, the airway microbiome was associated with peak expiratory flow (PEF) ( p = 0.003), pulmonary neutrophil counts ( p = 0.01), and alveolar 8-OHdG oxidative lesions ( p = 0.0078). The Clostridiales order bacteria showed the strongest signals. For example, the o&#95;Clostridiales;f&#95;;g&#95; OTU was elevated by PM 2.5 nitrate exposure ( p = 4.98 × 10 -5 ) and negatively correlated with PEF ( r = -0.585 and p = 2.4 × 10 -4 ). It was also associated with the higher pulmonary neutrophil count ( p = 8.47 × 10 -5 ) and oxidative lesion ( p = 7.17 × 10 -3 ). In human data, we confirmed the association of airway Clostridiales order bacteria with PM 2.5 exposure and lung function. For the first time, this study characterizes the impact of PM 2.5 exposure on the microbiome of multiple sites in the respiratory tract (RT) and its relevance to airflow obstructive diseases. By analyzing data from both humans and mice, we have identified bacteria belonging to the Clostridiales order as a promising biomarker for PM 2.5 exposure-induced decline in pulmonary function and inflammation.

Published
2023
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50. Within- and cross-tissue gene regulations were disrupted by PM 2.5 nitrate exposure and associated with respiratory functions.

Author

Zhang J, Cheng H, Di Narzo A, Zhu Y, Shan M, Zhang Z, Shao X, Chen J, Wang C, and Hao K

Subjects
Animals, Environmental Exposure analysis, Lung, Mice, Mice, Inbred C57BL, Nitrates pharmacology, Nitrogen Oxides, Organic Chemicals, Particulate Matter analysis, Particulate Matter toxicity, Air Pollutants analysis, Air Pollutants toxicity, Air Pollution analysis
Abstract

Background: Pathogenesis of complex diseases often involves multiple organs/tissue-types. To date, the PM 2.5 exposure's toxic effects and induced disease risks were not studied at multi-tissue level., Methods: C57BL/6 mice (n = 40) were exposed to PM 2.5 NO 3 - and clean air, respectively, and afterwards assessed respiratory functions and transcriptome in relevant tissues: blood and lung. We constructed within- and cross-tissue gene regulation networks and identified network modules associated with exposure and respiratory functions., Results: PM 2.5 NO 3 - exposure elevated naïve B cells proportion in blood (p = 0.0028). Among the 6000 highest expressed genes in blood, 18.8 % (1133 genes) were altered by exposure at p ≤ 0.05 level, among which 763 genes were also associated with respiratory function (enrichment folds = 7.63, p = 2.7E-189). The exposure disrupted blood genes were primarily in the immunoregulation pathways. Both within- and cross-tissue gene network modules were perturbed by exposure and associated with respiratory function. An immunodeficiency related cross-tissue module of 555 genes was affected by exposure (p = 0.0023) and strongly correlated with FEV 0.05 /FVC (r = 0.61 and p = 3E-5)., Conclusions: This study aims to fill in a major knowledge gap and investigated the effect of PM 2.5 exposure simultaneously in multiple tissues. We provided novel evidence that PM 2.5 NO 3 - exposure profoundly perturbed within- and cross-tissue gene regulations, and highlighted their roles in the etiology of respiratory decline., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2022 The Authors. Published by Elsevier B.V. All rights reserved.)

Published
2022
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