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136 MONDAY • MAY 16 Target Audience Pulmonologists, post graduate fellows and trainees, advanced practice nurses. Objectives At the conclusion of this session, the participant will be able to: • identify clinical features from a patient’s history that can help distinguish among the non-IPF ILDs in a patients with newly recognized ILD; • identify radiographic features from a patient’s HCRT that can help distinguish among the non-IPF ILDs in a patients with newly recognized ILD; • identify pathologic features from a patient’s biopsy that can help distinguish among the non-IPF ILDs in patients with newly recognized ILD. Distinguishing among the non-IPF interstitial lung diseases can be very challenging for the clinician. This symposium will seek to review the evidence for the best discriminating clinical, pathologic and radiologic features that can be used to differentiate among the non IPF ILDs. Following a review of these characteristics, 3 ILD clinicians will discuss real life cases that they will have been given ahead of time (without the diagnosis) to demonstrate how best to work thorough these challenging cases. Chairing: M. Kreider, MD, Philadelphia, PA G. Tino, MD, Philadelphia, PA A. Olson, MD, MSPH, Denver, CO 9:00 Introduction G. Tino, MD, Philadelphia, PA 9:10 Top 5 Clinical Features to Differentiate Among Non-IPF ILD K.K. Brown, MD, Denver, CO 9:30 Top 5 Radiographic Features to Differentiate Among Non-IPF ILD D. Hansell, MD, London, United Kingdom 9:45 Top 5 Pathologic Features to Differentiate Among Non-IPF ILD W.D. Travis, MD, New York, NY 10:00 Case I T.M. Maher, MD, MSc, PhD, London, United Kingdom A. Olson, MD, MSPH, Denver, CO 10:15 Case II C.D. Fell, MD, MSc, Calgary, Canada M. Kreider, MD, Philadelphia, PA 10:30 Case III G. Tino, MD, Philadelphia, PA J.S. Lee, MD, Aurora, CO 10:45 Questions and Answers M. Kreider, MD, Philadelphia, PA This session and the International Conference are supported by an educational grant from Boehringer Ingelheim Pharmaceuticals, Inc. All CME sessions have been planned and implemented in accordance with the Essential Areas and Policies of the Accreditation Council for Continuing Medical Education (ACCME) and are free of the control of commercial interests. B4 BASIC • CLINICAL • TRANSLATIONAL CRITICAL CARE TRACK CME Credits Available: 2.0 MECHANISMS OF ORGAN FAILURE IN SEPSIS Assemblies on Critical Care; Respiratory Cell and Molecular Biology; Respiratory Structure and Function 9:00 a.m. - 11:00 a.m. MOSCONE CENTER Room 3000/3002/3004 (West Building, Level 3) Target Audience Pulmonary and critical care researchers (undergraduates, graduates, post graduates and postdoctoral), clinicians (adults and peds), and trainees interested in understanding the athophysiology and pathogenesis of organ failure in sepsis. Objectives At the conclusion of this session, the participant will be able to: • learn new paradigms about sepsis-induced organ failure; • recognize risk and development of sepsis-induced organ failure; • translate new advancements in basic research with current and future clinical practice. This session will review seminal concepts in sepsis-induced organ failure as well as present novel and cutting edge research in the field. The aim is to translate cutting-edge advancements in molecular physiology and functional genomics of organ failure in the septic patient to a broad clinical and translational audience. The session will engage/stimulate and enhanced understanding of the leading concepts regarding the relative contributions of over-inflammation, immunosuppression, the microbiome, epithelium and endothelium as critical target(s) of organ failure that ultimately determine (lung, kidney, liver, heart, muscle, gut and brain) dysfunction and clinical outcomes in the critically ill. The session will have broad appeal to physicians and scientists at any level of training who work on diverse problems in the critically ill, and it will draw a diverse international audience because of the generalizability of the topics. Chairing: C.C. Dos Santos, MD, Toronto, Canada I.S. Douglas, MD, Denver, CO J. Chiche, MD, PhD, Paris, France 9:00 Mechanisms of Organ Failure in Sepsis R. Hotchkiss, MD, St. Louis, MO 9:15 Innate Immune Training in Sepsis? M. Netea, MD, PhD, Nijmegen, Netherlands 9:30 Liver Dysfunction in Sepsis M. Bauer, MD, Jena, Germany 9:45 Is the Microbiome an “Organ” that Fails in Septic Patients? J. Alverdy, MD, Chicago, IL 10:00 Is All Organ Failure Created Equal? C.C. Dos Santos, MD, Toronto, Canada 10:15 Sepsis Induced Immunosuppression Shift in Therapeutic Paradigm J. Chiche, MD, PhD, Paris, France ATS 2016 • San Francisco
MONDAY • MAY 16 137 B5 BASIC • TRANSLATIONAL BASIC SCIENCE CORE CME Credits Available: 2.0 HARNESSING BREAKTHROUGHS IN CRISPR GENE EDITING TECHNOLOGY FOR RESEARCH AND THERAPY Assemblies on Respiratory Cell and Molecular Biology; Allergy, Immunology and Inflammation; Microbiology, Tuberculosis and Pulmonary Infections; Respiratory Structure and Function; Thoracic Oncology 9:00 a.m. - 11:00 a.m. MOSCONE CENTER Room 2009/2011 (West Building, Level 2) Target Audience Basic and translational researchers seeking to understand the most important advance in biotechnology in the last decade and clinical investigators and clinicians interested in learning more about this technology that is poised to move into clinical application in the coming decade. Objectives At the conclusion of this session, the participant will be able to: • learn new findings about the CRISPR system functions and how it can be adapted to edit human and other animal genomes; • improve lung research by learning new strategies for selectively turning genes on and off, creating lung cancer models, performing genome-wide screens, and imaging the genome; • contribute to conversations that will shape scientific and ethical approaches to the use of CRISPR technology to treat human disease. The development of the CRISPR system for efficient and selective editing of the human genome represents the most important scientific breakthrough of the past decade. CRISPR-based systems are already being widely used for inactivating or repairing individual genes in human cells and animal models and for genome-wide studies of the functions of coding and non-coding RNAs. This session will introduce the basic CRISPR/Cas9 system, explain how this technology is being modified to allow selective inactivation, activation, and live imaging of the genome, and illustrate how the technology can be applied to study and treat lung diseases, including cancer. Chairing: D. Erle, MD, San Francisco, CA S. Albelda, MD, Philadephia, PA N. Chandel, PhD, Chicago, IL 9:00 CRISPR: From Biology to Transformative Technology J. Corn, PhD, Berkeley, CA 9:30 Genome-Scale CRISPR-Mediated Control of Gene Repression and Activation J. Weissman, PhD, San Francisco, CA 10:00 Dissecting the Role of Oxidative Homeostasis in Lung Cancer Using CRISPR/Cas9 Genome Engineering T. Papagiannakopoulos, PhD, New York, NY 10:30 CRISPR Tools for Complex Transcription Control and Functional Study S. Qi, PhD, Stanford, CA This session and the International Conference are supported by an educational grant from AstraZeneca LP. All CME sessions have been planned and implemented in accordance with the Essential Areas and Policies of the Accreditation Council for Continuing Medical Education (ACCME) and are free of the control of commercial interests. B6 BEHAVIORAL • CLINICAL SCIENTIFIC SYMPOSIUM CME Credits Available: 2.0 BUILDING E-BRIDGES: TOOLS AT OUR FINGERTIPS FOR ENHANCING COLLABORATIVE CARE Assemblies on Behavioral Science and Health Services Research; Clinical Problems; Critical Care; Nursing; Thoracic Oncology 9:00 a.m. - 11:00 a.m. MOSCONE CENTER Room 303/305 (South Building, Esplanade Level) Target Audience Clinicians and scientists seeking to understand developments in shared decision-making and to explore cutting edge tools aimed at advancing interdisciplinary, patient centered collaboration across pulmonary and critical care. Objectives At the conclusion of this session, the participant will be able to: • present new findings about the complexity of shared decision-making to enhance patient-centered care; • apply novel, innovative tools to enrich risk communication and improve the quality of life and health of patients; • evaluate future directions in and barriers to collaborative, personalized care. For most medical decisions, multiple options are available with each choice having its own list of benefits and harms. Decisions inconsistent with patient preferences may have unintended consequences to both patients and the health system. Shared decision-making provides a model for personalized medicine to enhance patient-centered care. This session will allow leading experts to discuss: (1) how traditional communication has failed and why shared decision-making has evolved; (2) the complexity of the decision-making process; (3) what tools are available, across pulmonary and critical care, to enhance communication; (4) what future directions and barriers may lie ahead in patient-centered risk communication. Chairing: T.S. Valley, MD, Ann Arbor, MI R.S. Wiener, MD, MPH, Boston, MA C.E. Cox, MD, MPH, Durham, NC 9:00 A Patient’s Perspective K. Erickson, Coral Gables, FL 9:05 Helping Me Help You: Making the Right Decision for Different Patients T.S. Valley, MD, Ann Arbor, MI 9:23 So You’re Telling Me There’s a Chance? Theories to Improve Risk Communication J.L. Hart, MD, Philadelphia, PA MONDAY MORNING 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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48 SUNDAY • MAY 15 P14 P15 P16 P1
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50 SUNDAY • MAY 15 P1545 P1546 Fa
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52 SUNDAY • MAY 15 P60 P61 Facili
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54 SUNDAY • MAY 15 P149 P150 Faci
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56 SUNDAY • MAY 15 P749 P750 P751
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58 SUNDAY • MAY 15 Facilitator: P
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60 SUNDAY • MAY 15 P1243 P1244 P1
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62 SUNDAY • MAY 15 P1295 P1296 P1
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64 SUNDAY • MAY 15 P1358 P1359 P1
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66 SUNDAY • MAY 15 P91 Facilitato
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68 SUNDAY • MAY 15 P616 P617 P618
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70 SUNDAY • MAY 15 P914 P915 P916
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72 SUNDAY • MAY 15 P556 P557 P558
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74 SUNDAY • MAY 15 Facilitators:
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76 SUNDAY • MAY 15 P997 P998 P999
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78 SUNDAY • MAY 15 P256 P257 P258
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80 SUNDAY • MAY 15 A61 THEMATIC P
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82 SUNDAY • MAY 15 P824 Facilitat
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84 SUNDAY • MAY 15 P1055 P1056 P1
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Page 138 and 139: 134 MONDAY • MAY 16 SS111 SS112 S
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186 MONDAY • MAY 16 P15 P16 P17 P
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188 MONDAY • MAY 16 Facilitator:
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190 MONDAY • MAY 16 P114 P115 P11
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192 MONDAY • MAY 16 P1408 Enhance
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194 MONDAY • MAY 16 P1455 P1456 P
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196 MONDAY • MAY 16 P1487 P1488 P
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198 MONDAY • MAY 16 P1514 P1515 P
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200 MONDAY • MAY 16 Facilitator:
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202 MONDAY • MAY 16 P559 P560 P56
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204 MONDAY • MAY 16 WS3 CLINICAL
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206 MONDAY • MAY 16 Satellite ear
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208 MONDAY • MAY 16 Objectives At
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210 MONDAY • MAY 16 encourage tra
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212 MONDAY • MAY 16 B82 BEHAVIORA
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214 MONDAY • MAY 16 B86 BASIC •
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216 MONDAY • MAY 16 and a number
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218 MONDAY • MAY 16 2:30 Mortalit
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220 MONDAY • MAY 16 3:00 Simultan
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222 MONDAY • MAY 16 525 Clinical
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224 MONDAY • MAY 16 320 Sensitivi
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226 MONDAY • MAY 16 113 COPD Subt
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228 MONDAY • MAY 16 1004 Health C
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230 MONDAY • MAY 16 609 Skeletal
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232 MONDAY • MAY 16 5:00 p.m. - 7
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234 TUESDAY • MAY 17 Chairing: D.
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236 TUESDAY • MAY 17 CLINICAL YEA
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238 TUESDAY • MAY 17 This session
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240 TUESDAY • MAY 17 bronchiectas
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242 TUESDAY • MAY 17 Target Audie
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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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250 TUESDAY • MAY 17 906 Phenotyp
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252 TUESDAY • MAY 17 807 The Vali
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254 TUESDAY • MAY 17 515 Roles of
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258 TUESDAY • MAY 17 Facilitator:
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260 TUESDAY • MAY 17 P199 P200 P2
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262 TUESDAY • MAY 17 P620 Facilit
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264 TUESDAY • MAY 17 P428 P429 P4
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268 TUESDAY • MAY 17 P318 P319 P3
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270 TUESDAY • MAY 17 P474 P475 Fa
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278 TUESDAY • MAY 17 C53 THEMATIC
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282 TUESDAY • MAY 17 P1095 P1096
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284 TUESDAY • MAY 17 P1167 P1168
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286 TUESDAY • MAY 17 P632 P633 P6
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300 TUESDAY • MAY 17 P1363 P1364
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302 TUESDAY • MAY 17 P928 P929 P9
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310 TUESDAY • MAY 17 P98 P99 P100
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312 TUESDAY • MAY 17 • become a
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314 TUESDAY • MAY 17 The topics a
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316 TUESDAY • MAY 17 C85 BASIC
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318 TUESDAY • MAY 17 C89 BASIC
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320 TUESDAY • MAY 17 3:20 Pediatr
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322 TUESDAY • MAY 17 2:45 Long-Te
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324 TUESDAY • MAY 17 918 Sarcoido
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326 TUESDAY • MAY 17 410 Effectiv
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328 TUESDAY • MAY 17 710 Follista
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330 TUESDAY • MAY 17 509 A Mechan
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332 TUESDAY • MAY 17 806 Upper Ai
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334 WEDNESDAY • MAY 18 6:45 Acute
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336 WEDNESDAY • MAY 18 CLINICAL Y
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338 WEDNESDAY • MAY 18 Objectives
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340 WEDNESDAY • MAY 18 D9 BASIC
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342 WEDNESDAY • MAY 18 Oral Prese
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344 WEDNESDAY • MAY 18 10:15 Plas
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346 WEDNESDAY • MAY 18 419 A Nove
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348 WEDNESDAY • MAY 18 216 Simpli
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350 WEDNESDAY • MAY 18 815 Multip
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352 WEDNESDAY • MAY 18 D28 POSTER
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354 WEDNESDAY • MAY 18 720 Repeat
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356 WEDNESDAY • MAY 18 P389 Facil
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358 WEDNESDAY • MAY 18 P439 P440
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360 WEDNESDAY • MAY 18 P10 P11 P1
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362 WEDNESDAY • MAY 18 P52 P53 Fa
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364 WEDNESDAY • MAY 18 P95 P96 P9
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368 WEDNESDAY • MAY 18 D42 THEMAT
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370 WEDNESDAY • MAY 18 P748 Funge
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376 WEDNESDAY • MAY 18 P808 Facil
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390 WEDNESDAY • MAY 18 11:45 Intr
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392 WEDNESDAY • MAY 18 12:15 Upda
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394 WEDNESDAY • MAY 18 This sessi
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396 WEDNESDAY • MAY 18 1:30 The B
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398 WEDNESDAY • MAY 18 D88 BEHAVI
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400 WEDNESDAY • MAY 18 3:00 Accel
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402 WEDNESDAY • MAY 18 D96 MINI S
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404 WEDNESDAY • MAY 18 604 CARMA3
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406 WEDNESDAY • MAY 18 702 Potent
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408 WEDNESDAY • MAY 18 803 ICU Ac
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410 WEDNESDAY • MAY 18 Chairing:
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412 WEDNESDAY • MAY 18 404 Interm
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Where today’s science meets tomor
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Final Program

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