DDI-2015 18th International Conference on Drug-Drug Interactions: NDA and Literature Update; Novel DDI Experimental Approach: Human Hepatocytes Cultured in Human Plasma; Physiologically-Mediated Drug Interactions; Transporters and IVIVE: Quantitative Proteomics to PET Imaging Tissue Concentrations; Biotherapeutics Disposition & DDI June 29 – July 1, 2015 Husky Union Building, University of Washington; Seattle, WA, USA 4001 NE Stevens Way, Seattle, WA 98195 (206) 543-8131 REGISTRATION DISCOUNT UNTIL MAY 29, 2015 ISC, INC. 9221 Rumsey Road, Suite # 8 Columbia, Maryland 21045 USA DDI-2015 MEDIA PARTNER Featuring the Following Experts: Albert P. Li; Ken Thummel; Chuang Lu; Yuichi Sugiyama; Jash Unadkat; Jan Wahlstrom; Eugenia Kraynov; Isabelle Ragueneau-Majlessi; JIngjing Yu; Wen Lin; Joe Ware; Jialin Mao; Sophie Argon; Stephen Wang; Maciej J. Zamek-Gliszczynski; Yang Xu; Ken-ichi Umehara; Yang Xu; Anup Zutshi DDI-2015 is a yearly event providing a comprehensive update on the status of the science of drug-drug interactions and its relevance to drug development. Presentations will be given by experts from industry and academia. Topics covered will include literature and NDA reviews, mechanism and in vitro-in vivo extrapolation of DDI via enzyme and transporter inhibition and induction. The conference will also include a review on the current status of DDI potential of biologics and industrial perspectives. PLEASE VISIT US ONLINE AT WWW.IFSCOMM.ORG 1 Organizing Chairs: Albert P. Li, APSciences/In Vitro ADMET Laboratories, LLC Isabelle Ragueneau-Majlessi, University of Washington Jashvant Unadkat, University of Washington Jan Wahlstrom, Amgen Inc. Stephen Wang, Pfizer, Inc. DDI-2015 18 International Conference on Drug-Drug Interactions th MONDAY, JUNE 29, 2015 DDI-2015 – DAY 1 8:00 AM – 9:00 AM – REGISTRATION 9:00 AM – 9:15 AM Welcome Remarks: Albert P. Li, APSciences/IVAL 9:15 AM – 9:45 AM Opening Remarks: Ken Thummel, University of Washington; Seattle, WA Session 1: NDA and Literature Update (Chair: Isabelle Ragueneau-Majlessi) 9:45 AM – 10:30 AM Critical Review of the 2014-2015 Literature (Sophie Argon, University of Washington, Seattle, WA) 2014 and 2015 drugdrug interactions publications in 2014 and 2015 will be reviewed and analyzed with particular focus on new findings on drug-enzyme, drug-transporter interactions, and clinically significant drug-drug interactions 10:30 AM – 11:00 AM – BREAK 11:00 AM – 11:45 AM New Molecular Entities approved by FDA in 2014: review of in vitro and in vivo DDI data (Jingjing Yu , University of Washington; Seattle, WA) This presentation will focus on the in vitro and clinical findings on drug-drug interactions of new drugs approved by U.S. FDA in 2014. 11:45 PM – 2:00 PM – LUNCH BREAK 2:00 PM – 2:45 PM Is BCRP Relevant to Human Drug PK, and What are the Best Practices in Clinical BCRP DDI Study Design?: A Literature Review (Maciej J. Zamek-Gliszczynski, GlaxoSmithKline; Research Triangle Park, NC) BCRP limits intestinal absorption of low-permeability substrate drugs and mediates biliary excretion of drugs and metabolites. Based on clinical evidence of BCRP-mediated drug-drug interactions (DDIs) and the c.421C>A functional polymorphism affecting drug efficacy and safety, both the FDA and EMA recommend preclinical evaluation, and when appropriate, clinical evaluation of BCRP-mediated DDIs. Although many BCRP substrates and inhibitors have been identified in vitro, clinical translation has been confounded by overlap with other transporters and metabolic enzymes. Thus, mechanistic attribution of clinical DDIs to BCRP has been equivocal. Regulatory recommendations for BCRP-mediated clinical DDI studies are challenging, as consensus is lacking on the choice of the most robust and specific human BCRP substrates and inhibitors and optimal study design. This presentation proposes a path forward based on a comprehensive analysis of available data. Oral sulfasalazine (1000 mg, IR tablet) is the best available clinical substrate for intestinal BCRP, oral rosuvastatin (20 mg) for both intestinal and hepatic BCRP, and intravenous rosuvastatin (4 mg) for hepatic BCRP. Oral curcumin (2000 mg) and lapatinib (250 mg) are the best available clinical BCRP inhibitors. To interrogate the worst-case clinical BCRP DDI scenario, study subjects harboring the BCRP c.421C/C reference genotype are recommended. In addition, if sulfasalazine is selected as the substrate, subjects having the rapid acetylator phenotype are recommended, whereas if rosuvastatin is selected, subjects harboring the OATP1B1 c.521T/T reference genotype are recommended. A proof-ofconcept clinical study is being planned by a collaborative consortium. 2:45 PM – 3:15 PM – SESSION 1 PANEL DISCUSSION Session 2: Novel DDI Experimental Approach: Human Hepatocytes Cultured in Human Plasma (Chair: A.P. Li) 3:15 PM – 4:00 PM Culture Hepatocytes in Human Plasma to Count the Free Concentration of Drugs in Evaluation of Drug-drug Interactions (Chuang Lu, Takeda; Cambridge, MA) Determination of free fraction of a drug (fu) in plasma and in an in vitro test system (fu, mic) are essential for evaluation and prediction of drug-drug interactions. However, accurate determination of those values is often test system dependent. This is especially challenge for high bound compounds. In this presentation, a hepatocyte culture method using suspension of human hepatocytes in human plasma will be presented. In this system, determination of the free fraction can be avoided. Further, in the present of an inhibitor for DDI evaluation, the CYP activity remaining in this system can be extrapolated to the [I]/ki ratio which is an important factor for prediction of drugdrug interaction. 4:00 PM – 4:45 PM Human Hepatocytes Suspended in Human Plasma: Application in Clearance Prediction and Drug-Drug Interactions (DDI) Prediction Involved Inhibitory Metabolites (Jialin Mao, Genentech, A Member of the Roche; South San Francisco, CA) Prediction of human hepatic clearance with in vitro metabolism assays is important in drug discovery and development. Meanwhile, as recent EMA (final) and FDA (draft) drug interaction guidances proposed that human circulating metabolites should be investigated in vitro for their drug-drug interaction (DDI) potential if present at ≥ 25% of parent AUC (FDA) or ≥ 25% parent and ≥10% of total drugrelated AUC (EMA), more attention has been paid to how the inhibitory metabolite(s) can be identified earlier in the drug discovery and development. Therefore, cryopreserved human hepatocytes suspended in human plasma has been explored as one of the in vitro systems to predict human hepatic clearance and DDIs involved the inhibitory metabolite. The findings will be reviewed and discussed in details. 4:45 PM – 5:15 PM – BREAK 2 5:15 PM – 6:00 PM Long Term Culturing of Human Hepatocytes in Human Plasma for DDI Studies (Albert Li, In Vitro ADMET Laboratories, LLC; Columbia, MD) Extrapolation of in vitro DDI results to clinical effects is complicated by plasma protein binding that occurs in vivo but often is lacking during in vitro experimentation. Adjustment of results based on fraction unbound (fu) does not always lead to accurate prediction of in vivo effects. In this study, human hepatocytes are cultured for multiple days in human plasma. The properties of the hepatocytes after prolonged culturing and the application of the human hepatocyte/human plasma cultures in DDI studies will be discussed. Transient Versus Chronic Cytokine Elevation (Yang Xu, Amgen; Thousand Oaks, CA) Immunotherapy is an emerging area of cancer treatment. Transient cytokine elevation was observed during treatment of bispecific T-cell engager antibody constructs as an initial immune response. The presentation will discuss the potential DDI mediated by the transient cytokine elevation and quantification of the DDI risk with a PBPK model. The results will be compared with the DDI mediated by inflammation based chronic cytokine elevation. The key determinants of cytokine mediated DDI and its clinical implication will be presented. 6:00 PM – 6:30 PM – SESSION 2 PANEL DISCUSSION 2:30 PM – 3:00 PM – SESSION 3 PANEL DISCUSSION 12:30 PM – 2:30 PM – LUNCH BREAK END OF DAY 1 Session 4: Transporters and IVIVE: Quantitative Proteomics to PET Imaging Tissue Concentrations (Chair: Jashvant Unadkat ) TUESDAY, JUNE 30, 2015 DDI-2015 - Day 2 8:00 AM – 9:00 AM – REGISTRATION Session 3: Physiologically-Mediated Drug Interactions (Chair: Jan Wahlstrom) 9:00 AM – 9:45 AM Physiology, Biopharmaceutics and PharmacodynamicsMediated DDIs (Jan Wahlstrom, Amgen, Thousand Oaks, CA) Physicochemical and biopharmaceutic properties may markedly impact drug formulation and exposure. These properties may also indicate susceptibility to drug interactions due to diseasebased changes in physiology or pharmacodynamics. This talk will cover case examples outlining the potential for drug interactions based on fundamental drug properties. 9:45 AM – 10:30 AM Predicting Food Effects and Bioavailability Using Preclinical Models with Physiologically Based Pharmacokinetics (PBPK) Modeling (Wen Lin, Tycho Heimbach, Jin Zhang, Fan Wu, Handan He, DMPK; Novartis Institutes for Biomedical Research; East Hanover, NJ) Physiologically based pharmacokinetic (PBPK) models are now routinely employed at Novartis and the Industry (e.g. http://www.orbitoproject.eu/) to provide quantitative, integrated analyses of drug absorption, bioavailability and disposition both in preclinical species and humans. Case studies demonstrating PBPK impacts from early through late development will be shared covering topics such as e.g.: a) PBPK modelling for BCSII/IV drugs to predict human absorption and bioavailability, b) food effect assessments across BCS/BDDCS classes, c) anticipating negative food effects, d) trouble-shooting and using parameter sensitivity analyses for poorly soluble drugs, e) regional absorption studies for formulation and modified release assessments 10:30 AM – 11:00 - BREAK 11:00 AM – 11:45 AM Joe Ware, Genentech-TBD 11:45 AM – 12:30 PM Cytokine Mediated DDI: Perspectives on Impact of 3:00 PM – 3:45 PM Predicting Transporter-Based Drug Disposition and DDI using Quantitative Proteomics: Methodological Issue and Challenges (Jashvant (Jash) D. Unadkat, Department of Pharmaceutics, University of Washington, Seattle, WA) The next frontier in drug disposition is predicting transporter-based drug disposition (including tissue concentrations) and DDI. This is now becoming possible as data on transporter protein expression are available through proteomics by quantifying surrogate peptides using LC-MS/MS. However, like any other approach, this approach to quantify transporter protein expression has its limitations. My presentation will discuss these limitations and methods to either overcome or avoid these limitations. Supported by UWRAPT which is sponsored by Genentech, Merck and Biogen Idec. 3:45 PM – 4:30 PM Predicting Human Hepatic Clearance from In Vitro Metabolism and Transport Data (Ken-ichi Umehara, Birk Poller, Annett Kunze, Gian Camenisch; Novartis Institutes of BioMedical Research (NIBR); Novartis Pharma AG; Basel, SWITZERLAND) Membrane transporters and metabolism are major determinants of the hepatobiliary elimination of drugs. The presentation will give answer to the question which drugs demonstrate transporter-based clearance in the clinic, based on the in vitro data measured using human liver microsomes and hepatocytes. Considering all four physiological processes driving hepatic drug elimination (sinusoidal influx and efflux, metabolism and biliary secretion), a mechanism-based hepatobiliary clearance prediction model will be presented determining the individual intrinsic clearance for compounds with various physicochemical and pharmacokinetic properties. Furthermore, analysis of the contribution of the individual uptake transporters to total hepatic uptake will be presented. 4:30 PM – 5:00 PM – BREAK 5:00 PM – 5:45 PM Imaging Hepatic Concentration and Biliary Excretion of Drugs (Yuichi Sugiyama, Sugiyama Laboratory, RIKEN Innovation Center, RIKEN, Yokohama, Japan) PET is a promising approach to determine the functional change of transporters associated with genetic polymorphisms or drugdrug interactions. Labeled PET probes are being developed for 3 specific transporters. For example, the effects of changes in uptake and efflux transporters activity on systemic and hepatic exposure of statins were determined. Here in this presentation, I will share will you our recent progress in the use of the analysis of plasma clearance of drugs and PET imaging to evaluate the transporter function in vivo including PET probes for hepatic uptake transporters (OATP1B1, OATP1B3) and biliary excretion transporters (MRP2, BCRP)) both in experimental animals and in human. About Institute for Scientific Communications, Inc. The Institute for Scientific Communication is a not-forprofit organization with the mission to distribute scientific knowledge via effective communications. ISC sponsors conferences and workshops to allow exchange of scientific observations and ideas, with the ultimate goal being timely application of the latest scientific discoveries to better human lives. Please visit our web site at www.ifscomm.org. 5:45 PM – 6:15 PM – SESSION 4 PANEL DISCUSSION POSTER PRESENTATIONS: WEDNESDAY, JULY 1, 2015 DDI-2015 - Day 3 8:00 AM – 9:00 AM – REGISTRATION SESSION 5: Biotherapeutics Disposition & DDI (Chair: Stephen Wang) 9:00 AM – 9:45 AM Recommendations from the IQ-sponsored ADC ADME Working Group on the Strategy for Assessing DDI of Antibody-Drug Conjugates (Eugenia Kranov, Pfizer, Inc.; La Jolla, CA) This presentation will discuss recommended strategy for assessing DDI potential of Antibody-Drug Conjugates generated by a cross-company working group . The talk will address selection as well as pros and cons of available experimental systems, translation of preclinical results to the clinical situation, and clinical implications. 9:45 AM – 10:30 AM (Stephen Wang, Pfizer, Inc.; Cambridge, MA)-TBD 10:30 AM – 11:00 AM 11:00 AM – 11:45 AM Site-of-Action Models: A Systems Modeling Approach to Quantifying Pharmacology (Anup Zutshi., Pfizer Andover/Cambridge Laboratories; Cambridge) The basic tenets of establishing pharmacology require that 1) the drug gets to the site-of-action, following which 2) the drug binds to its intended target with high affinity and the binding 3) results in the anticipated effects for which the drug was intended and designed. Using a combination of pharmacokinetic and equilibrium binding models called ‘Site-of-Action’ models, we have attempted to quantitatively understand the drug related as well as the physiological system related factors that impact the desired pharmacological outcomes. Case studies will be presented to depict the impact of this approach to decision making in early discovery. 11:45 AM – 12:15 PM – FINAL REMARKS – ALBERT P. LI (IVAL) Poster Presentations are always encouraged. Please submit your poster abstract for approval by the organizing th board by May 30 . Poster size should be no larger than 3 feet high by 6 feet long. Abstracts of posters will be included in the conference materials and will be available on the ISC website. The conference materials will be posted on the basis of availability from the author or presenter. There is no formal poster presentation scheduled. All posters will remain displayed throughout the conference. Please be prepared to display your poster th during registration on Sunday, June 28 or before the th first session begins on Monday, June 29 . Poster presenters will have ample time for discussion during breaks and Panel discussions. Submit posters abstracts for approval to Nola Mahaney, ISC; 9221 Rumsey Road, Suite # 8; Columbia, MD 21045 or email files attachment to nola@ifscomm.org. Approved poster applicants are responsible for completing a conference attendance registration form and payment of fee - visit www.ifscomm.org - and for the shipping of the poster itself. Please contact Nola Mahaney for any questions or comments. Please refer to “Travel Information” for hotel address and shipping information. The conference will be held at Husky Union Building, University of Washington; 4001 NE Stevens Way, Seattle, WA 98195 (206) 543-8131 TRAVEL INFORMATION: http://www.ifscomm.org/index.php?main_page=page&id=4 Watertown Hotel is conveniently located just four blocks from the University of Washington. There's no better home base if you're checking out campus, visiting a nearby medical facility, hosting a business event or simply want to see everything that makes Seattle a world-class city. Here you'll enjoy the kind of service that only a boutique hotel can offer including 102 smoke-free rooms, complimentary breakfast bar and a warm, inviting staff at your service 24 hours a day. Amenities: Complimentary Shuttle Service; Bicycle Checkout Program; Dog Friendly Seattle Hotel; Earth-Friendly Seattle Hotel. Please click on www.watertownseattle.com for more details. END OF DAY 3 END OF CONFERENCE 4242 Roosevelt Way NE Seattle, WA 98105 4 Guest Room Rates: Studio Double Queen Suite (SDQS) and Board Room Suite (BRS) $159.00 +tax, single/double occupancy. Add $20.00 per each additional adult per room. Check in time is 3 pm. Check out time is 12 Noon. Rates do not include applicable tax, currently 15.6% Rates applicable 3 days pre and post contracted room block, based upon availability. Rates include wireless internet service and overnight guest parking. Please note that parking is limited and not guaranteed. Reservation Method: Individuals are responsible for making their own reservations. They may go online at www.watertownseattle.com and enter Group Code: 150627ISCD in the Group Code window. In addition, they may call toll free, 1.866.866.7977, or by email request, reservations@staypineapple.com. All reservations must be guaranteed with a credit card number. Room Block Release Date: Friday, 05/29/2015 All remaining guest rooms which have not been reserved may be released for sale to the public. Hotel may continue to accept new reservations, based upon availability and at the Best Available Rate. Hotel guests have access to each property’s amenities. Watertown guests may use the pool at University Inn and University Inn guests may use the fitness room and free road bikes offered at Watertown. Both hotels offer complimentary guest laundry facilities. Conference Registration Payment Payment may be made by check or credit card. Checks should be made in US $, payable to Institute for Scientific Communications, Inc. Mail to: ISC, Inc., 9221 Rumsey Road, Suite # 8, Columbia, MD 21045, USA Cancellation Policy All cancellations are subjected to a $250.00 cancellation fee. Longer than 30 days, 100% refund (less cancellation fee). Less than 30 days, no refund but registration may be transferred to another person. All refund requests must be in writing. All refunds will be issued after the meeting has occurred. No refunds requests will be accepted after May 29, 2015. Please submit cancellation and refund requests including transferring of registration to: Fax: 410-869-9560; E-mail: nola@ifscomm.org; Cancel Deadline: May 29, 2015 Registration Form AVAILABLE ONLINE AT WWW.IFSCOMM.ORG Email to nola@ifscomm.org with remittance to: ISC, Inc. 9221 Rumsey Road, Suite # 8; Columbia, MD 21045, USA; FAX No: (410) 869-9560. Payment may be made by check in US$, payable to Institute for Scientific Communications, Inc. or by credit card. Academic/Government participants will receive a 50% discount. Contact Nola Mahaney for Exhibitor or Sponsorship Opportunities at nola@ifscomm.org or phone (410) 869-9166); or visit http://www.ifscomm.org. 5 REGISTRATION FORM: DDI-2015 Or please register online at: http://www.ifscomm.org/ A. Credit Card Information: B. Registrant Information: *Required fields to be completed *American Express VISA MC *Cardholder Name: Dr.________ Mr.________ Ms._________ Please type your name as you wish it to appear on your name badge PLEASE PRINT *Cardholder Billing Address: Last Name First Name Mid. 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