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392 WEDNESDAY • MAY 18 12:15 Update on Current Pulmonary Issues at the FDA L.I. Gilbert-McClain, MD, Silver Spring, MD 12:33 Old Drug New Use: Anticholinergics and Asthma S.J. Chin, MD, Silver Spring, MD 12:51 Targeted Therapy for Asthma: Lessons from the IL-5 Pathway K.M. Donohue, MD, Silver Spring, MD 1:09 Questions and Answers L.I. Gilbert-McClain, MD, Silver Spring, MD L24 VARIOUS ORGANIZATIONS RESEARCH FUNDING OPPORTUNITIES 12:15 p.m. - 1:15 p.m. MOSCONE CENTER Room 2001/2003 (West Building, Level 2) Target Audience Any ATS member who conducts research and is seeking funding. Objectives At the conclusion of this session, the participant will be able to: • describe the research priorities of each funding agency represented on the panel; • discuss practical steps that researchers take to improve quality of grant applications; • identify a funding agency that is most closely aligned with the attendee’s research interests. This session will introduce programs and research grant opportunities offered from major funding agencies. Speakers will present current research priorities and mechanisms of research funding available from each agency. Chairing: J. Yorke, PhD, RN, Manchester, United Kingdom J. Choi, PhD, RN, Pittsburgh, PA 12:15 National Institute of Nursing Research N. Redeker, PhD, RN, West Haven, CT 12:25 National Heart, Lung, and Blood Institute L. Reineck, MD, Bethesda, MD 12:35 Department of Veterans Affairs E.G. Collins, PhD, RN, Chicago, IL 12:45 American Lung Association S. Rappaport, MPH, New York, NY 12:55 ATS <strong>Program</strong> of Research Speaker To Be Announced 1:05 Panel Discussion J. Yorke, PhD, RN, Manchester, United Kingdom L25 NATIONAL HEART, LUNG, AND BLOOD INSTITUTE, DIVISION OF LUNG DISEASES, NIH NEW RESULTS FROM THE COPDGENE STUDY 12:15 p.m. - 1:15 p.m. MOSCONE CENTER Target Audience Those with clinical or research responsibilities. Room 2002/2004 (West Building, Level 2) Objectives At the conclusion of this session, the participant will be able to: • learn about imaging in the COPDGene study; • understand and learn about subtypes identified by the COPDGene study; • learn about longitudinal follow-up in the COPDGene study. Chronic obstructive pulmonary disease (COPD), the third leading cause of death in the United States, is a heterologous syndrome. The COPDGene study has created the largest cohort of well-characterized current and former smokers for respiratory disease research. The primary goals of COPDGene are: 1) to identify new genetic loci that influence the development of COPD and COPD-related phenotypes and 2) to reclassify COPD into subtypes that can ultimately be used to develop effective therapies. This session will describe the progress and future plans of the COPDGene study. Chairing: E.K. Silverman, MD, PhD, Boston, MA J.D. Crapo, MD, Denver, CO L. Postow, PhD, Bethesda, MD 12:15 Overview of COPDGene J.D. Crapo, MD, Denver, CO 12:27 Longitudinal Follow-Up of COPDGene Subjects: Clinical Epidemiology M.K. Han, MD, MS, Ann Arbor, MI 12:39 Advances in Quantitative Lung Imaging and Visual CT Assessment D.A. Lynch, MD, Denver, CO 12:51 COPD Genetics: From GWAS to Sequencing E.K. Silverman, MD, PhD, Boston, MA 1:03 Defining Subtypes of COPD M.H. Cho, MD, MPH, Boston, MA L26 NATIONAL HEART, LUNG, AND BLOOD INSTITUTE, DIVISION OF LUNG DISEASES, NIH ENHANCED PHENOTYPING OF PULMONARY VASCULAR DISEASES 12:15 p.m. - 1:15 p.m. MOSCONE CENTER Target Audience Health providers, trainees, and researchers. Room 2006/2008 (West Building, Level 2) ATS 2016 • San Francisco
WEDNESDAY • MAY 18 393 Objectives At the conclusion of this session, the participant will be able to: • learn about current deep-phenotyping of PH; • understand and learn pediatrics PH registry; • learn about the national biorepository of PH patient samples for PH research. Pulmonary hypertension (PH) currently has no cure, thus PH research remains a high priority for NHLBI. Recently, NHLBI launched several major multi-center clinical studies of PH including: Redefining Pulmonary Hypertension through Pulmonary Vascular Disease Phenomics (PVDOMICS); and Pulmonary Hypertension Breakthrough Initiative (PHBI), which will help us understand the molecular mechanisms of PH in adult patients, and provide phenotypic data and biomarkers for future clinical trials and measures of disease severity. Data Fusion: A Sustainable, Scalable, Open Source Registry Advancing PVD Research using a novel biomedical informatics approach will develop computable phenotypes of pediatric pulmonary vascular diseases. This session will introduce these programs and present data from these studies Chairing: L. Xiao, MD, PhD, Bethesda, MD C.J. Blaisdell, MD, Bethesda, MD 12:15 NHLBI PVDOMICS <strong>Program</strong> Overview S.C. Erzurum, MD, Cleveland, OH 12:25 PVDOMICS Study Design and Update J.H. Newman, MD, Nashville, TN 12:35 Data Fusion: A Sustainable, Open Source Registry Advancing Pediatric Pulmonary Vascular Disease Research - Part I S.H. Abman, MD, Aurora, CO 12:45 Data Fusion: A Sustainable, Open Source Registry Advancing Pediatric Pulmonary Vascular Disease Research - Part II K. Mandl, MD, MPH, Boston, MA 12:55 Pulmonary Hypertension Breakthrough Initiative (PHBI) Update M. Geraci, MD, Indianapolis, IN 1:05 National Biological Sample and Data Repository for Pulmonary Arterial Hypertension W. Nichols, PhD, Cincinnati, OH L27 NATIONAL HEART, LUNG, AND BLOOD INSTITUTE, DIVISION OF LUNG DISEASES, NIH OXIDANT STRESS IN HIV-RELATED CHRONIC LUNG DISEASE 12:15 p.m. - 1:15 p.m. MOSCONE CENTER Room 2016/2018 (West Building, Level 2) Target Audience Providers of lung health; medical fellows in training; graduate post-doctoral fellows; established scientists in basic research on lung biology, HIV pathogenesis and infection disease. Objectives At the conclusion of this session, the participant will be able to: • understand the role of oxidative stress in the onset of lung diseases associated with HIV infection in the HAART era; • improve target possibilities for treating lung inflammatory diseases such as pulmonary hypertension in HAART treated HIV patients; • learn new findings about the role of oxidative stress in the onset of lung complications in HIV (+) patients undergoing ART. HIV-infected patients on antiretroviral therapy (ART) have now a longer life expectancy, but as a consequence chronic diseases are increasingly becoming a major cause of morbidity and death. Many pulmonary conditions, including PAH, and COPD are more prevalent in HIV infected individuals under treatment but the mechanisms by which HIV and ART induce cellular dysfunction that may trigger these pathologies are largely unknown. One such pathway is oxidative stress (OS), which results from excessive free radical production, and exceeding endogenous antioxidant defense mechanisms, which can damage a wide variety of cellular components. The session will address current research and results in this area and will give an overview of current HIV research on the oxidative stress role in HIV infection. Presenters will delineate current knowledge of lung complications in relationship to OS, and describe latest results and techniques utilized in their projects. Chairing: H.L. Twigg, MD, Indianapolis, IN E. Caler, PhD, Bethesda, MD 12:15 HIV Proteins and Pulmonary Hypertension S. Flores, PhD, Aurora, CO 12:30 Oxidative Stress in HIV Associated COPD B.D. Medoff, MD, Boston, MA 12:45 Redox Stress and Chronic Lung Disease in HIV J. Roman, MD, Louisville, KY 1:00 HIV+ Alveolar Macrophage Oxidant-Mediated Apoptosis of Pulmonary Endothelium M.R. Staudt, PhD, New York, NY NATIONAL HEART, LUNG, AND BLOOD INSTITUTE, DIVISION OF LUNG DISEASES, NIH L28 NHLBI PETAL CLINICAL TRIAL NETWORK: PREVENTION AND EARLY TREATMENT OF ACUTE LUNG INJURY 12:15 p.m. - 1:15 p.m. MOSCONE CENTER Room 2020/2022 (West Building, Level 2) Target Audience Practicing critical care and emergency medicine clinicians and clinical researchers would benefit from this session. This includes fellows, students, nurses, and other medical professionals. Persons interested in clinical trial design and conduct would also benefit from this session. Objectives At the conclusion of this session, the participant will be able to: • understand the goals and structure of the PETAL network • understand the questions being addressed in PETAL and outreach efforts of the network • have a better understanding of PETAL trial design and conduct including utilization of a central IRB WEDNESDAY MID-DAY ATS 2016 • San Francisco
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American Thoracic Society Internati
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TABLE OF CONTENTS ATS 2016 INTERNAT
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2 FRIDAY • MAY 13 PG2A CLINICAL P
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4 FRIDAY • MAY 13 Target Audience
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6 FRIDAY • MAY 13 11:15 Case Disc
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8 FRIDAY • MAY 13 Chairing: H.B.
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10 FRIDAY • MAY 13 10:25 Advanced
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12 FRIDAY • MAY 13 Objectives At
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14 SATURDAY • MAY 14 Abdominal Ul
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16 SATURDAY • MAY 14 PG17 BASIC
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18 SATURDAY • MAY 14 1:05 In What
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20 SATURDAY • MAY 14 10:30 Practi
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22 SATURDAY • MAY 14 Objectives A
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24 SATURDAY • MAY 14 10:10 Is My
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26 SUNDAY • MAY 15 Chairing: D.M.
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28 SUNDAY • MAY 15 Chronic Cough:
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30 SUNDAY • MAY 15 • understand
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32 SUNDAY • MAY 15 Target Audienc
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34 SUNDAY • MAY 15 Oral Presentat
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36 SUNDAY • MAY 15 9:15 Hyperpola
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38 SUNDAY • MAY 15 310 A Smartpho
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40 SUNDAY • MAY 15 103 Immunosupp
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42 SUNDAY • MAY 15 A26 POSTER DIS
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44 SUNDAY • MAY 15 822 Incidence
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46 SUNDAY • MAY 15 519 Maternal H
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114 SUNDAY • MAY 15 A86 BASIC •
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126 SUNDAY • MAY 15 1014 Determin
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130 SUNDAY • MAY 15 412 Daytime S
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132 SUNDAY • MAY 15 6:30 p.m. - 8
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134 MONDAY • MAY 16 SS111 SS112 S
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136 MONDAY • MAY 16 Target Audien
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138 MONDAY • MAY 16 9:40 Empoweri
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142 MONDAY • MAY 16 10:15 Adaptiv
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146 MONDAY • MAY 16 624 Neonatal
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234 TUESDAY • MAY 17 Chairing: D.
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244 TUESDAY • MAY 17 C18 MINI SYM
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246 TUESDAY • MAY 17 415 Investig
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248 TUESDAY • MAY 17 207 Survival
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334 WEDNESDAY • MAY 18 6:45 Acute
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Page 418: Where today’s science meets tomor
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