Designed to attract experts working in all areas of medicinal chemistry and molecular pharmacology the summit has five tracks focusing on key issues such as optimising hit to lead quality and timescale, protein degradation, DNA Encoded libraries, GPCR’s, small molecule Immuno-oncology research, FBDD, SBDD, CADD as well as best strategies for partnerships, collaborations, outsourcing and integration of research. The Summit will provide a forum to network, learn and engage with senior representatives of leading pharmaceutical and biotech companies worldwide. It is a gathering not to be missed!
This document provides an agenda for the Global Medicinal Chemistry & GPCR Leaders Summit Europe 2017 conference happening on November 27-28, 2017 in London, UK. The two-day conference will feature expert speakers from pharmaceutical and biotech companies discussing topics related to medicinal chemistry strategies, enabling technologies like protein degradation and DNA encoded libraries, integrating medicinal chemistry in the drug discovery process, and GPCR targets. Some of the expert speakers listed include representatives from Merck, GSK, AstraZeneca, Sanofi, and Celgene. The agenda outlines the schedule of talks and panel discussions taking place across three tracks on both days of the conference.
Target identification and validation in drug discoverySpringer
This document discusses the SELEX (Systematic Evolution of Ligands by EXponential enrichment) process for identifying aptamers (nucleic acid molecules) that bind to specific targets. It provides details on how SELEX has been used to produce aptamers that bind to membrane-bound receptors and whole cells/organisms. The document also describes a protocol for selecting RNA aptamers that act as allosteric modulators of nicotinic acetylcholine receptors.
Aptamer Technology in the Targeted Delivery of Doxorubicin | Crimson PublishersCrimsonpublishersCancer
This review aims at giving an insight at some of the recent approaches in using the aptamer technology in formulating the chemotherapeutic agent, doxorubicin, so as to achieve its targeted delivery and reduce its non-specific cytotoxicity.
Discovery on Target 2014 - The Industry's Preeminent Event on Novel Drug TargetsJaime Hodges
Cambridge Healthtech Institute's 12th Annual Discovery on Target will showcase current and emerging “hot” targets for the pharmaceutical industry, October 8 – 10, 2014 in Boston, MA. Spanning three days, the meeting will bring together more than 900 global attendees, including scientists/technologists, executives, directors, and managers from biopharma, academic, and healthcare organizations. In 2014 the event is comprised of 14 conference tracks which include Epigenetic Readers, Ubiquitin Proteasome, Big Data Discovery, GPCR Drug Discovery, RNAi-Screens-Functional-Genomics, PPI Targets, Protein-Targets, Histone-Methyltransferases-Demethylases, Drug Transporters, Maximizing Efficiency, GPCR Therapeutics, Genomics Screening, Cancer Metabolism and Membrane Production. The 2014 event will offer 200+ scientific presentations across 14 conference tracks, 1 Symposium and 15 conference short courses, 40+ interactive breakout discussion groups, an exhibit hall of 40+ companies, and dedicated poster viewing and networking sessions.
Precision Medicine & Biomarkers Leaders Summit - Boston USA - 7th & 8th MayTony Couch
This expanding series attracts the leading authorities worldwide working in companion diagnostics, biomarkers, immuno-oncology, liquid biopsies, AI and other facets of precision medicine. It has been praised for its stimulating, interactive and engaging environment where it brings together a multi-disciplined community of researchers, leaders and innovators whose aim is to develop groundbreaking and impactful treatments for patients.
Srinivas Maddi CV _ Prinicipal scientist_ DMPK_ 2015Srinivas Maddi
This cover letter summarizes an applicant's 8+ years of experience in drug metabolism, pharmacokinetics, and preclinical formulation research. They established a DMPK lab and led due diligence programs that resulted in out-licensing of new chemical entities. The applicant has expertise in designing and interpreting in vitro and in vivo pharmacokinetic studies for small molecules and experience with PK-PD modeling.
1) Researchers have created a new online resource called the IUPHAR/MMV Guide to Malaria Pharmacology (GtoMPdb) to curate information on antimalarial compounds and their molecular targets in Plasmodium.
2) The database currently contains 25 Plasmodium molecular targets and 57 antimalarial ligands that were manually curated from scientific literature.
3) A new customized online portal provides open access to the antimalarial data and allows browsing by parasite lifecycle stage, target species, and other features to help malaria research.
This document provides an agenda for the Global Medicinal Chemistry & GPCR Leaders Summit Europe 2017 conference happening on November 27-28, 2017 in London, UK. The two-day conference will feature expert speakers from pharmaceutical and biotech companies discussing topics related to medicinal chemistry strategies, enabling technologies like protein degradation and DNA encoded libraries, integrating medicinal chemistry in the drug discovery process, and GPCR targets. Some of the expert speakers listed include representatives from Merck, GSK, AstraZeneca, Sanofi, and Celgene. The agenda outlines the schedule of talks and panel discussions taking place across three tracks on both days of the conference.
Target identification and validation in drug discoverySpringer
This document discusses the SELEX (Systematic Evolution of Ligands by EXponential enrichment) process for identifying aptamers (nucleic acid molecules) that bind to specific targets. It provides details on how SELEX has been used to produce aptamers that bind to membrane-bound receptors and whole cells/organisms. The document also describes a protocol for selecting RNA aptamers that act as allosteric modulators of nicotinic acetylcholine receptors.
Aptamer Technology in the Targeted Delivery of Doxorubicin | Crimson PublishersCrimsonpublishersCancer
This review aims at giving an insight at some of the recent approaches in using the aptamer technology in formulating the chemotherapeutic agent, doxorubicin, so as to achieve its targeted delivery and reduce its non-specific cytotoxicity.
Discovery on Target 2014 - The Industry's Preeminent Event on Novel Drug TargetsJaime Hodges
Cambridge Healthtech Institute's 12th Annual Discovery on Target will showcase current and emerging “hot” targets for the pharmaceutical industry, October 8 – 10, 2014 in Boston, MA. Spanning three days, the meeting will bring together more than 900 global attendees, including scientists/technologists, executives, directors, and managers from biopharma, academic, and healthcare organizations. In 2014 the event is comprised of 14 conference tracks which include Epigenetic Readers, Ubiquitin Proteasome, Big Data Discovery, GPCR Drug Discovery, RNAi-Screens-Functional-Genomics, PPI Targets, Protein-Targets, Histone-Methyltransferases-Demethylases, Drug Transporters, Maximizing Efficiency, GPCR Therapeutics, Genomics Screening, Cancer Metabolism and Membrane Production. The 2014 event will offer 200+ scientific presentations across 14 conference tracks, 1 Symposium and 15 conference short courses, 40+ interactive breakout discussion groups, an exhibit hall of 40+ companies, and dedicated poster viewing and networking sessions.
Precision Medicine & Biomarkers Leaders Summit - Boston USA - 7th & 8th MayTony Couch
This expanding series attracts the leading authorities worldwide working in companion diagnostics, biomarkers, immuno-oncology, liquid biopsies, AI and other facets of precision medicine. It has been praised for its stimulating, interactive and engaging environment where it brings together a multi-disciplined community of researchers, leaders and innovators whose aim is to develop groundbreaking and impactful treatments for patients.
Srinivas Maddi CV _ Prinicipal scientist_ DMPK_ 2015Srinivas Maddi
This cover letter summarizes an applicant's 8+ years of experience in drug metabolism, pharmacokinetics, and preclinical formulation research. They established a DMPK lab and led due diligence programs that resulted in out-licensing of new chemical entities. The applicant has expertise in designing and interpreting in vitro and in vivo pharmacokinetic studies for small molecules and experience with PK-PD modeling.
1) Researchers have created a new online resource called the IUPHAR/MMV Guide to Malaria Pharmacology (GtoMPdb) to curate information on antimalarial compounds and their molecular targets in Plasmodium.
2) The database currently contains 25 Plasmodium molecular targets and 57 antimalarial ligands that were manually curated from scientific literature.
3) A new customized online portal provides open access to the antimalarial data and allows browsing by parasite lifecycle stage, target species, and other features to help malaria research.
The document discusses drug design, development, and delivery. It covers rational drug design using molecular properties and receptor modeling. Computer-assisted drug design uses molecular docking and QSAR methods. Neural networks are also used in drug design. Drug discovery involves identifying candidates and screening for efficacy. Drug development evaluates ADME, toxicity, and safety through preclinical and clinical studies. Drug delivery methods aim to effectively administer pharmaceutical compounds and improve drug release profiles.
This document provides information about the 10th Annual Conference on RNA Therapeutics taking place on February 20-21, 2019 in London. It outlines the chairs, guest speakers, and key speakers at the conference, as well as featured highlights and topics to be discussed. Some of the topics to be covered include the clinical progress of spherical nucleic acids with Exicure, Sanofi's strategies for oligonucleotide delivery, ProQR's plans for oligonucleotide supply, and the development of self-amplifying mRNA vaccines at GSK. The document provides an agenda and schedule for the two-day conference.
Therapeutic peptides and their trends in the pharmaceutical market. Peptide drugs generated $25.4 billion in sales in 2018. Phage display technology has produced several FDA-approved antibody drugs. Macrocyclization of peptides discovered by phage display can enhance binding affinity, selectivity, permeability and proteolytic stability. The speaker's lab uses phage display and chemical modification to discover novel peptide ligands for protein targets.
This document provides an agenda for the 10th annual conference on Mitigating Drug Toxicities and Developing New Tools to Model Drug Metabolism to Strengthen Human Relevant Results (ADMET), taking place on June 29-30, 2015 in London. The conference will focus on topics such as in vitro models for detecting cardiotoxicity and hepatotoxicity, analyzing the performance of different in vitro models to detect hepatotoxic drugs, regulatory guidance on drug transporters, mitigating errors in early human dose predictions, and setting criteria for ADME endpoints. Speakers will discuss opportunities for modeling kidney disease and general toxicology studies, optimizing pre-clinical approaches and human relevance, population pharmacokinetics prediction and PK/PD
This document discusses the use of single nucleotide polymorphisms (SNPs) in pharmacogenomic studies. It begins by introducing personalized medicine and pharmacogenetics/pharmacogenomics. SNPs are described as the most common type of human genetic variation and are important in pharmacogenomic studies as they can affect drug metabolism and response. Methods for detecting SNPs like DNA sequencing and microarrays are presented. Examples are given of how SNPs in genes like TPMT, CYP2D6, and UGT1A1 can affect drug metabolism and dosing for medications like 6-mercaptopurine, codeine, and irinotecan. The SNP Consortium is summarized as a public effort to map SNPs to aid pharmacogen
MOLECULAR DOCKING AND RELATED DRUG DESIGN ACHIEVEMENTS santosh Kumbhar
Molecular docking is a computational method used in structure-based drug design to predict how biological macromolecules interact with other molecules. It attempts to predict the preferred orientation of one molecule to another when bound to each other to form a stable complex. Docking is useful for predicting the binding orientation of small molecule drug candidates to their protein targets in order to predict their interaction and to design effective inhibitors. There are various types of docking software available that implement different algorithms to predict the binding orientation and affinity between molecules rapidly and accurately to help identify potential lead compounds for drug development. Molecular docking has contributed to the discovery of several new drug classes and is playing an increasingly important role in modern computer-aided drug design and virtual
Specialized in custom synthesis of organic molecules. Broad experience of working on multiple business models - FTEs, FFS, Milestone services of pharmaceutical industry.
Commited to deliver highest quality products in a timely manner and value to the customers.
2015 11-26 ODDP2015 Course Oncology Drug Development, Amsterdam, Alain van GoolAlain van Gool
This document describes the development of biomarkers to support targeted cancer therapies, using the case study of biomarkers for BRAF inhibitors in melanoma. Key points:
- The BRAFV600E mutation causes constitutive activation of the ERK pathway and is prevalent in melanoma, making it a promising drug target.
- siRNA and RAF inhibitor compounds were shown to inhibit the ERK pathway and cell proliferation in BRAF mutant cell lines but not wildtype lines, validating BRAF mutation as a predictive biomarker.
- Further optimization of RAF inhibitors focused on potency, selectivity against other kinases, and efficacy in mouse models to support clinical development.
- There remains a need to identify soluble protein biomarkers in blood
Introducing VSPGx: Pharmacogenomics Testing in VarSeqGolden Helix
Inter-individual variability in drug response poses a significant challenge for clinicians, with much of this variability resulting from inherited genetic differences. While the field of pharmacogenomics (PGx) can provide powerful insights into how genomic factors affect drug response, the implementation of PGx testing in the clinic is hampered by the difficulty of translating genetic test results into actionable recommendations. In this webcast, we will discuss VarSeq’s new PGx testing capabilities, including the ability to identify actionable pharmacogenomic diplotypes and generate clinical reports.
In this webcast you will learn:
-How to identify pharmacogenomic diplotypes and drug recommendations from NGS data.
-How to incorporate externally called CNVs and SVs into your PGx annotations.
-How to generate customizable PGx reports from these annotations.
2014 11-27 ODDP 2014 course, Amsterdam, Alain van GoolAlain van Gool
Presentation as part of a comprehensive oncology drug development course, to discuss a pharmaceutical approach to identify, validate and develop biomarkers for personalized medicine for melanoma.
MRCT's Centre for Therapeutics Discoverywarwick_amr
The MRCT Centre for Therapeutics Discovery provides early stage drug discovery capabilities to academic and industry partners. It has over 140 staff with expertise in small molecule drug discovery, antibody engineering, and target validation. The Centre aims to progress early scientific discoveries into marketable healthcare products through partnerships. It has a track record of success, with 4 drugs on the market and 7 in clinical trials from past projects. The Centre is seeking new academic and industry partnerships to build its pipeline of around 20 ongoing projects focused on areas of high unmet medical need.
This document provides information about the 9th annual conference on ADMET (Absorption, Distribution, Metabolism, Excretion and Toxicity) enhancing drug quality by ADMET optimisation in discovery that will take place from June 30th to July 2nd 2014 at the Marriott Regents Park Hotel in London. Key information includes:
- Discounts are available for booking by March 31st (save £300) and April 30th (save £100).
- The conference will focus on integrating ADMET and toxicity data to enhance drug safety prediction, drug transporters, predictive toxicology, and computational/in vitro ADMET approaches.
- There will be presentations from industry leaders at companies like
2nd CRISPR Congress Boston, 23-25 February 2016 Diane McKenna
The 2nd Annual CRISPR Congress will enhance the basic research, drug discovery and therapeutic applications of CRISPR technology by overcoming key specificity, efficiency and delivery challenges needed to improve the precise editing and repair of the genome.
This document provides an agenda and details for the 6th annual RNA Therapeutics conference taking place on February 16-17, 2015 in London. The conference will focus on RNA interference therapeutics, antisense oligonucleotides, microRNA, and CRISPR-Cas technologies. Over the two days, there will be keynote speeches from industry leaders at Roche, AstraZeneca, and Sarepta Therapeutics, as well as academic speakers from institutions like the University of Southern Denmark and University of Oxford. Panel discussions will address collaborative models between academia and pharmaceutical companies. Business attendees will learn about maximizing returns on investment in oligonucleotide R&D. A half-day post-conference workshop
This document provides information about the 5th International Conference and Exhibition on World Metabolomics 2016 that will take place from May 16-18, 2016 in Osaka, Japan. It discusses the conference themes, sessions, speakers and highlights. It also lists the conference secretariat contact information and invites industrial and academic researchers to participate.
This document provides information about the 11th Annual Conference and Exhibition on ADMET (Absorption, Distribution, Metabolism, Excretion and Toxicity) taking place on June 13-14, 2016 in London. The conference will focus on linking ADME and pharmacokinetic properties with safety for drug assessment. It will include sessions on optimizing drug design/discovery, translating non-clinical ADME data to clinical use, linking pharmacokinetics with safety, and improving drug-drug interaction assessment. Speakers will discuss topics like physiologically-based pharmacokinetic modeling, in vitro transporter assays, predicting and avoiding drug-induced liver injury, and assessing human plasma concentrations using in silico ADMET models.
Updated Agenda- CRISPR Congress in Berlin, 24-26 October 2016Diane McKenna
This document summarizes an upcoming conference on harnessing precision genome editing using CRISPR/Cas9 technology. The 3-day conference in Berlin will feature presentations and workshops on optimizing CRISPR workflows for applications in biomedical research and therapeutic development. Speakers will discuss improving genome editing efficiency, developing screening methods and disease models, and navigating regulatory environments. Attendees can learn how both academic institutions and companies are advancing the use of CRISPR in areas like target identification, disease modeling, and developing new cell and gene therapies.
This document provides information about the 3rd Annual Conference on Drug Discovery Chemistry hosted by SMi Group. The conference will take place on March 18-19, 2019 in London, UK, with a half-day workshop on March 20. Key speakers will discuss topics such as novel drug modalities, targeting difficult proteins, using artificial intelligence in drug discovery, and optimizing drug discovery techniques. Attendees can learn about recent advances, network with industry leaders, and explore strategic partnerships. Discounts are available for early registration.
Precision Medicine & Biomarkers Leaders Summit - Boston USA - 7th & 8th MayTony Couch
Global Engage is pleased to announce the 2018 Precision Medicine & Biomarkers Leaders Summit USA taking place on May 7-8th in Boston, MA. The event is part of our highly successful Drug Discovery Series which includes conferences on Biologics, Medicinal Chemistry, NASH, Pharmaceutical R&D IT and the Human Microbiome amongst others. It is also the sister meeting of the European Precision Medicine Summit which has run successfully since 2013.
Biomaterials & Tissue engineering - London - AgendaTony Couch
Designed for experts in academia and industry working in this exciting field, this conference will examine cutting-edge
research in several key areas across four dedicated tracks. Talks will look to cover the development of scaffold
technology for both soft and hard tissues, and the novel biomaterials used in their construction, new platforms for
Biofabrication, tissue culture techniques, advances in hydrogels in regenerative medicine, and recent developments in
stem cell research. There will also be a track dedicated to the exciting developing field of organ fabrication, reviewing
recent advances and challenges to be overcome.
Precision Medicine & Biomarkers Leaders Summit - Boston USA - 7th & 8th MayTony Couch
Tracks focus on R&D strategies, Biomarker development, Immuno-oncology, CDx development, AI and Big data analysis and approaches – Attending this Summit will provide you with the opportunity to mix and interact with experts working in all facets of Precision Medicine through the individual, panel and roundtable discussions on offer.
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This document provides information about the 10th Annual Conference on RNA Therapeutics taking place on February 20-21, 2019 in London. It outlines the chairs, guest speakers, and key speakers at the conference, as well as featured highlights and topics to be discussed. Some of the topics to be covered include the clinical progress of spherical nucleic acids with Exicure, Sanofi's strategies for oligonucleotide delivery, ProQR's plans for oligonucleotide supply, and the development of self-amplifying mRNA vaccines at GSK. The document provides an agenda and schedule for the two-day conference.
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This document discusses the use of single nucleotide polymorphisms (SNPs) in pharmacogenomic studies. It begins by introducing personalized medicine and pharmacogenetics/pharmacogenomics. SNPs are described as the most common type of human genetic variation and are important in pharmacogenomic studies as they can affect drug metabolism and response. Methods for detecting SNPs like DNA sequencing and microarrays are presented. Examples are given of how SNPs in genes like TPMT, CYP2D6, and UGT1A1 can affect drug metabolism and dosing for medications like 6-mercaptopurine, codeine, and irinotecan. The SNP Consortium is summarized as a public effort to map SNPs to aid pharmacogen
MOLECULAR DOCKING AND RELATED DRUG DESIGN ACHIEVEMENTS santosh Kumbhar
Molecular docking is a computational method used in structure-based drug design to predict how biological macromolecules interact with other molecules. It attempts to predict the preferred orientation of one molecule to another when bound to each other to form a stable complex. Docking is useful for predicting the binding orientation of small molecule drug candidates to their protein targets in order to predict their interaction and to design effective inhibitors. There are various types of docking software available that implement different algorithms to predict the binding orientation and affinity between molecules rapidly and accurately to help identify potential lead compounds for drug development. Molecular docking has contributed to the discovery of several new drug classes and is playing an increasingly important role in modern computer-aided drug design and virtual
Specialized in custom synthesis of organic molecules. Broad experience of working on multiple business models - FTEs, FFS, Milestone services of pharmaceutical industry.
Commited to deliver highest quality products in a timely manner and value to the customers.
2015 11-26 ODDP2015 Course Oncology Drug Development, Amsterdam, Alain van GoolAlain van Gool
This document describes the development of biomarkers to support targeted cancer therapies, using the case study of biomarkers for BRAF inhibitors in melanoma. Key points:
- The BRAFV600E mutation causes constitutive activation of the ERK pathway and is prevalent in melanoma, making it a promising drug target.
- siRNA and RAF inhibitor compounds were shown to inhibit the ERK pathway and cell proliferation in BRAF mutant cell lines but not wildtype lines, validating BRAF mutation as a predictive biomarker.
- Further optimization of RAF inhibitors focused on potency, selectivity against other kinases, and efficacy in mouse models to support clinical development.
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Introducing VSPGx: Pharmacogenomics Testing in VarSeqGolden Helix
Inter-individual variability in drug response poses a significant challenge for clinicians, with much of this variability resulting from inherited genetic differences. While the field of pharmacogenomics (PGx) can provide powerful insights into how genomic factors affect drug response, the implementation of PGx testing in the clinic is hampered by the difficulty of translating genetic test results into actionable recommendations. In this webcast, we will discuss VarSeq’s new PGx testing capabilities, including the ability to identify actionable pharmacogenomic diplotypes and generate clinical reports.
In this webcast you will learn:
-How to identify pharmacogenomic diplotypes and drug recommendations from NGS data.
-How to incorporate externally called CNVs and SVs into your PGx annotations.
-How to generate customizable PGx reports from these annotations.
2014 11-27 ODDP 2014 course, Amsterdam, Alain van GoolAlain van Gool
Presentation as part of a comprehensive oncology drug development course, to discuss a pharmaceutical approach to identify, validate and develop biomarkers for personalized medicine for melanoma.
MRCT's Centre for Therapeutics Discoverywarwick_amr
The MRCT Centre for Therapeutics Discovery provides early stage drug discovery capabilities to academic and industry partners. It has over 140 staff with expertise in small molecule drug discovery, antibody engineering, and target validation. The Centre aims to progress early scientific discoveries into marketable healthcare products through partnerships. It has a track record of success, with 4 drugs on the market and 7 in clinical trials from past projects. The Centre is seeking new academic and industry partnerships to build its pipeline of around 20 ongoing projects focused on areas of high unmet medical need.
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- Discounts are available for booking by March 31st (save £300) and April 30th (save £100).
- The conference will focus on integrating ADMET and toxicity data to enhance drug safety prediction, drug transporters, predictive toxicology, and computational/in vitro ADMET approaches.
- There will be presentations from industry leaders at companies like
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The UK is currently facing a Adhd Medication Shortage Uk, which has left many patients and their families grappling with uncertainty and frustration. ADHD, or Attention Deficit Hyperactivity Disorder, is a chronic condition that requires consistent medication to manage effectively. This shortage has highlighted the critical role these medications play in the daily lives of those affected by ADHD. Contact : +1 (747) 209 – 3649 E-mail : sales@trinexpharmacy.com
TEST BANK For Community Health Nursing A Canadian Perspective, 5th Edition by...Donc Test
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Local Advanced Lung Cancer: Artificial Intelligence, Synergetics, Complex Sys...Oleg Kshivets
Overall life span (LS) was 1671.7±1721.6 days and cumulative 5YS reached 62.4%, 10 years – 50.4%, 20 years – 44.6%. 94 LCP lived more than 5 years without cancer (LS=2958.6±1723.6 days), 22 – more than 10 years (LS=5571±1841.8 days). 67 LCP died because of LC (LS=471.9±344 days). AT significantly improved 5YS (68% vs. 53.7%) (P=0.028 by log-rank test). Cox modeling displayed that 5YS of LCP significantly depended on: N0-N12, T3-4, blood cell circuit, cell ratio factors (ratio between cancer cells-CC and blood cells subpopulations), LC cell dynamics, recalcification time, heparin tolerance, prothrombin index, protein, AT, procedure type (P=0.000-0.031). Neural networks, genetic algorithm selection and bootstrap simulation revealed relationships between 5YS and N0-12 (rank=1), thrombocytes/CC (rank=2), segmented neutrophils/CC (3), eosinophils/CC (4), erythrocytes/CC (5), healthy cells/CC (6), lymphocytes/CC (7), stick neutrophils/CC (8), leucocytes/CC (9), monocytes/CC (10). Correct prediction of 5YS was 100% by neural networks computing (error=0.000; area under ROC curve=1.0).
Title: Sense of Smell
Presenter: Dr. Faiza, Assistant Professor of Physiology
Qualifications:
MBBS (Best Graduate, AIMC Lahore)
FCPS Physiology
ICMT, CHPE, DHPE (STMU)
MPH (GC University, Faisalabad)
MBA (Virtual University of Pakistan)
Learning Objectives:
Describe the primary categories of smells and the concept of odor blindness.
Explain the structure and location of the olfactory membrane and mucosa, including the types and roles of cells involved in olfaction.
Describe the pathway and mechanisms of olfactory signal transmission from the olfactory receptors to the brain.
Illustrate the biochemical cascade triggered by odorant binding to olfactory receptors, including the role of G-proteins and second messengers in generating an action potential.
Identify different types of olfactory disorders such as anosmia, hyposmia, hyperosmia, and dysosmia, including their potential causes.
Key Topics:
Olfactory Genes:
3% of the human genome accounts for olfactory genes.
400 genes for odorant receptors.
Olfactory Membrane:
Located in the superior part of the nasal cavity.
Medially: Folds downward along the superior septum.
Laterally: Folds over the superior turbinate and upper surface of the middle turbinate.
Total surface area: 5-10 square centimeters.
Olfactory Mucosa:
Olfactory Cells: Bipolar nerve cells derived from the CNS (100 million), with 4-25 olfactory cilia per cell.
Sustentacular Cells: Produce mucus and maintain ionic and molecular environment.
Basal Cells: Replace worn-out olfactory cells with an average lifespan of 1-2 months.
Bowman’s Gland: Secretes mucus.
Stimulation of Olfactory Cells:
Odorant dissolves in mucus and attaches to receptors on olfactory cilia.
Involves a cascade effect through G-proteins and second messengers, leading to depolarization and action potential generation in the olfactory nerve.
Quality of a Good Odorant:
Small (3-20 Carbon atoms), volatile, water-soluble, and lipid-soluble.
Facilitated by odorant-binding proteins in mucus.
Membrane Potential and Action Potential:
Resting membrane potential: -55mV.
Action potential frequency in the olfactory nerve increases with odorant strength.
Adaptation Towards the Sense of Smell:
Rapid adaptation within the first second, with further slow adaptation.
Psychological adaptation greater than receptor adaptation, involving feedback inhibition from the central nervous system.
Primary Sensations of Smell:
Camphoraceous, Musky, Floral, Pepperminty, Ethereal, Pungent, Putrid.
Odor Detection Threshold:
Examples: Hydrogen sulfide (0.0005 ppm), Methyl-mercaptan (0.002 ppm).
Some toxic substances are odorless at lethal concentrations.
Characteristics of Smell:
Odor blindness for single substances due to lack of appropriate receptor protein.
Behavioral and emotional influences of smell.
Transmission of Olfactory Signals:
From olfactory cells to glomeruli in the olfactory bulb, involving lateral inhibition.
Primitive, less old, and new olfactory systems with different path
Here is the updated list of Top Best Ayurvedic medicine for Gas and Indigestion and those are Gas-O-Go Syp for Dyspepsia | Lavizyme Syrup for Acidity | Yumzyme Hepatoprotective Capsules etc
Muktapishti is a traditional Ayurvedic preparation made from Shoditha Mukta (Purified Pearl), is believed to help regulate thyroid function and reduce symptoms of hyperthyroidism due to its cooling and balancing properties. Clinical evidence on its efficacy remains limited, necessitating further research to validate its therapeutic benefits.
Ear and its clinical correlations By Dr. Rabia Inam Gandapore.pptx
Global Medicinal Chemistry & GPCR Leaders summit 2017 - Agenda
1. 27-28 November 2017
LONDON, UK
www.global-engage.com
GLOBAL MEDICINAL
CHEMISTRY & GPCR
LEADERS SUMMIT: EUROPE
#GEDD17
Exhibitors & Content Sponsors
Platinum Sponsors
2. WARM WELCOME
GLOBAL MEDICINAL CHEMISTRY & GPCR LEADERS SUMMIT EUROPE 2017
Global Engage are pleased to announce as part of their Drug Discovery Series of events, the
Global Medicinal Chemistry & GPCR Leaders Summit which will be held on November 27-28
2017 in London, UK.
Designed to attract experts working in all areas of medicinal chemistry and molecular pharmacology the summit
has five tracks focusing on key issues such as optimising hit to lead quality and timescale, protein degradation,
DNA Encoded libraries, GPCR’s, small molecule Immuno-oncology research, FBDD, SBDD, CADD as well as best
strategies for partnerships, collaborations, outsourcing and integration of research. The Summit will provide a
forum to network, learn and engage with senior representatives of leading pharmaceutical and biotech companies
worldwide. It is a gathering not to be missed!
LAURENT SCHIO
Head of France Medicinal Chemistry,
Lead Optimization, Sanofi
EMMA PARMEE
Associate VP, Head of Chemistry
Capabilities and Screening,
Merck Sharp & Dohme
EXPERT SPEAKERS Include:
IAN CHURCHER
Head, Protein Degradation
Discovery Performance Unit, GSK
GARRY PAIRAUDEAU
Head of External Sciences,
AstraZeneca
FIONA MARSHALL
Founder, Director & CSO,
Heptares Therapeutics
JULIE SELKIRK
Associate Director,
Biology, Celgene
3. DAY 1 – TRACK 1
Medicinal Chemistry Strategies
• Drug Discovery Chemistry – where are we heading
• Artificial Intelligence for medicinal chemistry
• Target (In)validation using medicinal chemistry tools
• Optimising hit to lead optimization quality and timescale
▶ Best Practice Case Studies
▶ CADD / Cheminformatics
▶ Data for decision making
▶ Virtual screening for identifying hits
• Panel Discussion – Future of Medicinal Chemistry
DAY 1 – TRACK 2
Enabling Technologies - Degraded Chemistry & DNA Encoded Libraries
• Targeted protein degradation / PROTACs
• DNA encoded libraries
• Integrated synthesis platforms
• Oher enabling technologies
• Panel Discussion – Protein Degradation – the possibilities
CONFERENCE SYNOPSIS
DAY 2 – TRACK 1
Integrating Medicinal Chemistry into the drug discovery process
• ADCs – Targeted delivery
• Small molecule Immuno-oncology research
• Methods to Reducing Toxicity
• Molecules with predictable in vivo and safety profiles
• Phenotypic screening
Fragment Based Drug Discovery
• When FBDD should be used
• Best practice case studies
Structure Based Drug Design
• SBDD Case studies
• GPCR targets
• Macrocyclic compounds
DAY 2 – TRACK 2
Partnerships, Collaborations & Outsourcing
• Identifying & choosing a partner for a productive partnership
▶ CRO v partnership
▶ True benefits to outsourcing
▶ Risk sharing business models
▶ Managing the partnership – communication, data exchange,
measuring quality & success
• What and when to outsource
▶ Integrating outsourced research to internal products
▶ Keeping to budget – Optimizing ROI
▶ Risk and rewards
• What worked well and what didn’t – Lessons learned and tips for success
• Open Innovation / Pre-competitive activity
• Panel Discussion – Best methods to identify, choose and manage your
partnership
PANEL & ROUNDTABLE DISCUSSIONS
Panel Discussions
1. Future of Medicinal Chemistry
2. Targeted Protein Degradation
3. Best methods to identify, choose and manage
your outsourcing partner
One Hour Roundtable Discussions
1. Targeted Protein Degradation
2. Optimising hit to lead optimization
3. Optimising Outsourcing activities
4. DNA Encoded Libraries
5. Fragment Based Drug Discovery
6. GPCR – Biased Signalling
DAY 1 – TRACK 3
GPCR - Addressing complex pharmacology and signalling
• Allosteric Modulation approaches and development
• Signalling / Biased signalling
• Drug Discovery case studies
4. CONFIRMED SPEAKERS
EMMA PARMEE
Associate VP, Head of Chemistry
Capabilities and Screening,
Merck Sharp & Dohme
DAVID WILSON
Senior Director and Head,
Global Oncology Chemistry,
IMED Oncology, AstraZeneca
STEVAN DJURIC
Distinguished Research Fellow,
Senior Director Discovery
Chemistry and Technology,
Abbvie
LAURENT SCHIO
Head of France Medicinal
Chemistry, Lead Optimization,
Sanofi
THOMAS FRANCH
CSO Nuevolution A/S
ANDREAS LERCHNER
Senior Investigator, Project
Team Leader, Novartis Institutes
for Biomedical Research
ANDREAS
BRUNSCHWEIGER
Independent Group Leader, TU
Dortmund
MARK BOYS
Principal Research Investigator,
Array BioPharma
FIONA MARSHALL
Founder, Director & CSO,
Heptares Therapeutics
NICK TERRETT
Scientific Associate Vice
President, European Chemistry
Lead, Merck Sharp and Dohme
IAN CHURCHER
Head, Protein Degradation
Discovery Performance Unit,
GSK
GEORGE BURSLEM
Research Fellow, Crews Lab, Yale
University
DARREN GREEN
Director Molecular Design,
GSK
GARRY PAIRAUDEAU
Head of External Sciences,
AstraZeneca
ALLEYN PLOWRIGHT
Head of Integrated Drug
Discovery Germany, Sanofi
TAKASHI ICHIKAWA
Senior Director, Head of
Drug Discovery Chemistry
Laboratories, CNS Drug
Discovery Unit, Research, Takeda
Pharmaceutical Company
LAWRENCE HAMANN
Vice President, Chemistry,
Celgene
GISBERT SCHNEIDER
Professor, Computer-Assisted
Drug Design at the Institute of
Pharmaceutical Sciences in the
Department of Chemistry and
Applied Biosciences, ETH Zurich
ALESSIO CIULLI
Professor of Chemical &
Structural Biology, Division
of Biological Chemistry and
Drug Discovery, School of Life
Sciences, University of Dundee
ALEXANDER ALANINE
Chief Operating Officer, Bactevo
XIAOPENG BAI
Investigator, GSK
STEPHEN
SHUTTLEWORTH
Chief Operating Officer &
Chief Scientific Officer, Karus
Therapeutics Ltd
NICHOLAS
CARRUTHERS
Senior Director, Neuroscience,
Janssen, Pharmaceutical
Companies of Johnson and
Johnson
EDUARD FELDER
Director, Head of Chemical
Core Technologies, Oncology
Research, Nerviano Medical
Sciences
DAVID POWELL
Director, Chemistry, Inception
Sciences Canada
DARREN
MCKERRECHER
Director Medicinal Chemistry,
AstraZeneca
MATTHIAS ZENTGRAF
Head of Computational
Chemistry, Boehringer-Ingelheim
JONATHAN MASON
Senior Research Fellow & Head
of CADD, Heptares Therapeutics
(UK)
CRAIG JOHNSTONE
Executive Vice President, Head
of Chemistry and Directeur
General, Evotec (France) SAS
CRAIG JOHNSTONE
Executive Vice President, Head
of Chemistry and Directeur
General, Evotec (France) SAS
HONG SHEN
Head of Medicinal Chemistry
and Head of External Innovation
Therapeutic Modalities, Roche
Innovation Center Shanghai
JEFF REAGAN
Scientific Director,
CardioMetabolic Disorders,
Amgen
ANDREW ALT
Associate Director, Biology,
Arvinas
AYLIN HANYALOGLU
Senior Lecturer, Institute of
Reproductive and Developmental
Biology, Department of Surgery
and Cancer, Faculty of Medicine,
Imperial College London
METTE ROSENKILDE
Professor, Laboratory for Molecular
Pharmacology, Department of
Biomedical Sciences, Faculty of
Health and Medical Sciences,
University of Copenhagen
ADAM WEINGLASS
Director, Screening & Compound
Profiling, MSD
GLOBAL MEDICINAL CHEMISTRY & GPCR LEADERS SUMMIT EUROPE 2017
5. CONGRESS SCHEDULE DAY 1 MONDAY 27TH
NOVEMBER 2017
GLOBAL MEDICINAL CHEMISTRY & GPCR LEADERS SUMMIT EUROPE 2017
Morning Refreshments / Poster Presentations / One-to-One Networking Meetings10:45-11:55 Room: Lindbergh & Aviators Lobby
Registration & Refreshments08:00-08:50
08:50-09:00 Global Engage Welcome Address and Morning Chair’s Opening Remarks
KEYNOTE ADDRESS:
EMMA PARMEE
Associate VP, Head of Chemistry Capabilities and Screening, Merck Sharp & Dohme
Novel Strategies for Design Cycle Enhancement in Medicinal Chemistry
This presentation will highlight several strategic elements adopted at Merck aimed at accelerating the molecular optimization “design cycle” used by medicinal chemists. The talk will describe our efforts
to capitalize on advances in structure based drug design and our ability to integrate datasets and leverage predictive tools. Most importantly, recent breakthroughs in high throughput experimentation
technology pioneered at Merck will be described. This latter topic is also part of our strategy to ensure a continued focus on the crucial role synthetic chemistry plays in enabling and inspiring design in Drug Discovery.
Room: Lindbergh & Aviators Lobby
Room: Lindbergh 2&3
09:00-09:35
KEYNOTE ADDRESS:
NICHOLAS CARRUTHERS
Senior Director, Neuroscience, Janssen, Pharmaceutical Companies of Johnson and Johnson
Targeting Protein-Protein Interactions of AMPA Channels
Glutamate mediates the majority of fast synaptic transmission in the central nervous system (CNS) via activation of ionotropic α-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid (AMPA) receptors.
Although AMPA receptors (AMPARs) are widely expressed throughout the CNS, their activity can be modulated by numerous auxiliary proteins including transmembrane regulatory proteins (TARPs),
which are often localized in distinct brain regions. In particular, TARP-ƴ8 is expressed primarily in the hippocampus, a key component of the limbic system. By selectively inhibiting neurotransmission within this brain
region, negative modulators of TARP-ƴ8 dependent AMPARs exhibit strong anticonvulsant effects in rodent seizure models without the motor impairment associated with nonselective AMPAR antagonists. The preclinical
pharmacology for JNJ-55511118 an AMPA receptor negative modulator with exquisite selectivity for TARP-ƴ8 together with a second-generation series of 5-pyridyloxindoles will be presented.
09:35-10:15
SOLUTION PROVIDER PRESENTATION:
SENIOR REPRESENTATIVE
WuXi AppTec
10:15-10:45
6. CONGRESS SCHEDULE DAY 1 MONDAY 27TH
NOVEMBER 2017
GLOBAL MEDICINAL CHEMISTRY & GPCR LEADERS SUMMIT EUROPE 2017
ENABLING TECHNOLOGIES - DEGRADED CHEMISTRY & DNA ENCODED LIBRARIES MEDICINAL CHEMISTRY STRATEGIES
Room: Lindbergh 2&3 Room: Lindbergh 1
DAVID WILSON
Senior Director and Head, Global Oncology
Chemistry, IMED Oncology, AstraZeneca
Successful strategies to drug protein-protein
interactions: Discovery of AZD5991, a potent
and selective inhibitor of Mcl-1
This presentation will highlight the challenges faced by medicinal
chemists in successfully ‘drugging’ protein-protein interactions (PPIs)
and will focus on how macrocyclization has been used successfully as
a strategy in lead optimization. Mcl-1, a member of the Bcl/Mcl family,
is a key protein involved in evasion of apoptosis in a wide variety of
tumors. Its amplification and overexpression have also been implicated
in innate and acquired resistance to anticancer drugs. AZD5991 is a
rationally designed macrocycle with sub-nanomolar affinity for Mcl-1. It
demonstrates all the hallmarks of a true Mcl-1 inhibitor and is active in
vivo, with complete (100%) tumor regression demonstrated in several
mouse xenograft models after a single tolerated dose.
STEVAN DJURIC
Distinguished Research Fellow, Senior Director
Discovery Chemistry and Technology, Abbvie
Enabling Chemistry Technologies –
Accelerators of Drug Discovery
Drug Discovery has recently been described as
a race by diMasi et al. As such, it is imperative to develop chemistry
related technology that can reduce cycle time, cost of goods and
improve PoS. To this end, we will describe our efforts in the chemistry
technology area with a focus on integrated synthesis-purification-
bioassay, photochemistry and high temperature chemistry platforms.
11:55-12:25
11:55-12:2512:25-12:55
GPCR: ADDRESSING COMPLEX PHARMACOLOGY AND SIGNALLING
Bleriot Suite
JULIE SELKIRK
Associate Director, Biology, Celgene
Ozanimod: A novel sphingosine 1 phosphate
receptor modulator for the treatment of
relapsing and remitting multiple sclerosis
Ozanimod is a novel sphingosine 1 phosphate
receptor (S1PR) modulator with demonstrated selectivity for
S1PR1 and S1PR5. Ozanimod was specifically developed to treat
relapsing and remitting multiple sclerosis by targeting multiple
critical control points in the progression of the disease, acting both
peripherally to reduce lymphocyte exit from the lymph nodes and
centrally vial S1PR1/5 expressed on neural cells. Ozanimod was
developed in an expedited manner and has demonstrated clinical
efficacy in Phase III clinical trials in patients with relapsing and
remitting multiple sclerosis. The presentation will highlight the
project flow scheme, pharmacological characterization, and clinical
data of this efficacious modulator.
11:55-12:25
12:25-12:55
12:25-12:55
For sponsorship opportunities please contact Tony Couch/
Faizel Ismail at Sponsorship@Globalengage.co.uk
SOLUTION PROVIDER PRESENTATION
LAURENT SCHIO
Head of France Medicinal Chemistry, Lead
Optimization, Sanofi
Drug Design: Beyond a Static Vision
3D structures elucidation of target-ligand complexes
has often provided valuable information in the way
to design more potent inhibitors or agonists. However the comparison of
apo vs natural substrate and ligand binding structures usually highlights
protein segments shifts, so called induced fits and transient pockets
formation which weaken the standard and rigid lock-key model. Over
the last years several reports have pointed out the productive effect
of considering the role of water molecules located in the binding site
regarding ligand affinity improvement. Long run molecular dynamics
simulations as well as free energy perturbation calculations are
methodologies that are now accessible and could be applied to better
predict new compound affinity or to rationalize observed structure
activities relationships. Several case studies will be shown.
THOMAS FRANCH
CSO Nuevolution A/S
DNA-encoded Library Technology: From Hits
to clinical Candidate
Identification of attractive hit matter is imperative
as starting point for small molecule lead discovery
efforts. The recent advancement of DNA-encoding technologies has
enabled the encoding of fragments and combinatorial chemistry
libraries at a massive scale comprising billions of compounds to aid
the screening of drug targets supporting lead discovery. The principle
of the DNA encoding technology will be illustrated including library
designs and properties as well as screening data from multiple
targets across epigenetic targets, proteases and “tough-to-drug”
protein-protein interactions. Case stories on the BET bromodomains
and the RORуt NHR will be presented showing the application of
the technology and program data from initial hit finding through lead
optimization to preclinical candidate identification.
12:55-13:25
12:55-13:25
JEFF REAGAN
Scientific Director, CardioMetabolic Disorders,
Amgen
Allosteric Modulation of the Calcium Sensing
Receptor: A History of Calcimimetics
Calcimimetics are positive allosteric modulators
to the calcium sensing receptor (CaSR) which are used clinically to
treat primary and secondary hyperparathyroidism. This presentation
will discuss.
• Brief history of cinacalcet, a first generation calcimimetic
• Application of an operational model of allosteric modulation to
aid in the design of second generation calcimimetics
• Evaluation of calcimimetics to treat patients suffering from
hypercalcemia as a consequence of inactivating mutations in
the CaSR.
12:55-13:25
SOLUTION PROVIDER PRESENTATION:
SENIOR REPRESENTATIVE
Hitgen
SOLUTION PROVIDER
PRESENTATION:
CRAIG JOHNSTONE
Executive Vice President, Head of Chemistry
and Directeur General,
Evotec (France) SAS
7. CONGRESS SCHEDULE DAY 1 MONDAY 27TH
NOVEMBER 2017
GLOBAL MEDICINAL CHEMISTRY & GPCR LEADERS SUMMIT EUROPE 2017
Lunch / One-to-One Networking Meetings13:25-14:20 Room: Lindbergh & Aviators Lobby
ANDREAS LERCHNER
Senior Investigator, Project Team Leader,
Novartis Institutes for Biomedical Research
Is CLK a valid target for Phelan-McDermid
syndrome?
SHANK3 haploinsufficiency is causative for
Phelan-McDermid syndrome (PMDS), a neurodevelopmental
condition leading to Autism Spectrum Disorder. Recent results
demonstrated that down-regulation of Akt/mTORC1 signaling
resulted from enhanced phosphorylation and activation of PP2A
regulatory subunit, B56β, due to increased steady-state levels
of its kinase, Cdc2-like kinase 2 (CLK2) (Bidinosti et al. Science
2016). Based on this evidence, a 30k biochemical CLK2 HTS was
performed, and a very potent and selective CLK inhibitor series
was identified via SAR by archive. Efficacy of the most advanced
CLK inhibitors was shown in a Shank3 kd mouse brain slice assay
on synaptogenesis and assessment of the best tool compounds in
a human primary lymphocytes MNT was performed to judge the
suitability of CLK as a possible target for PMDS.
ANDREAS BRUNSCHWEIGER
Independent Group Leader, TU Dortmund
Accessing genetically tagged heterocycle
libraries via a chemoresistant DNA sequence
DNA-encoded compound libraries (DELs) have
found widespread use in drug research as
screening technology. Tagging compounds with genetic information
allows for handling them as complex mixtures. Bioactive compounds
are efficiently identified from these mixtures by selection and
DNA-sequencing. However, the chemical space of DELs is biased
by the requirement to employ DNA-compatible synthesis methods
in library synthesis. We observed that a hexathymidine DNA
oligonucleotide “hexT” tolerated a surprisingly broad spectrum
of catalysts, thus we use it as an adapter in the initial step of DEL
synthesis. Testimony of the remarkable chemoresistance of the hexT
sequence was the synthesis of hexT-pyrazole conjugates through a
Au(I)-mediated three-component reaction in glacial acetic acid. The
hexT-heterocycle conjugates were readily ligated to coding DNA
sequences giving rise to encoded libraries.
13:10-13:35
14:20-14:50
ANDREW ALT
Associate Director, Biology, Arvinas
Positive Allosteric Modulators of Opioid
Receptors: A Novel Approach for Future Pain
Medications
• Positive Allosteric Modulators (PAMs)
of opioid receptors block pain by amplifying the activity of
endogenous opioid agonists which are naturally released in pain
states
• Opioid PAMs do not directly activate opioid receptors, and have
no effect in tissues where agonists are not present
• Therefore, opioid PAMs may exhibit significantly improved side
effect and abuse liability profiles compared to current opioid
medications
• The current preclinical data supporting a rationale for developing
opioid receptor PAMs as novel pain medications will be presented
13:10-13:35
14:50-15:20
14:50-15:20 For sponsorship opportunities please contact Tony Couch/
Faizel Ismail at Sponsorship@Globalengage.co.uk
SOLUTION PROVIDER PRESENTATION
14:50-15:20
For sponsorship opportunities please contact Tony Couch/
Faizel Ismail at Sponsorship@Globalengage.co.uk
SOLUTION PROVIDER PRESENTATION
SOLUTION PROVIDER PRESENTATION:
SENIOR REPRESENTATIVE
X-Chem Pharmaceuticals
8. CONGRESS SCHEDULE DAY 1 MONDAY 27TH
NOVEMBER 2017
GLOBAL MEDICINAL CHEMISTRY & GPCR LEADERS SUMMIT EUROPE 2017
15:20-15:45
50 MINUTE EXECUTIVE PANEL DISCUSSION:
Future of Medicinal Chemistry
TAKASHI ICHIKAWA
Senior Director, Head of Drug Discovery Chemistry
Laboratories, CNS Drug Discovery Unit, Research,
Takeda Pharmaceutical Company
DAVID POWELL
Director, Chemistry, Inception Sciences Canada
DARREN MCKERRECHER
Director Medicinal Chemistry, AstraZeneca
Reserved:
Giles Brown
Director of Medicinal Chemistry, Heptares
Nick Carruthers
Senior Director, Janssen, Pharmaceutical Companies of Johnson
and Johnson
15:20-16:10
ADAM WEINGLASS
Director, Screening & Compound Profiling, MSD
Structural basis for the cooperative allosteric
activation of the free fatty acid receptor GPR40
Agonists of GPR40 enhance glucose-
dependent insulin secretion and represent a
potential mechanism for the treatment of type-2 diabetes mellitus.
Pharmacologic studies indicate that partial and full allosteric
agonists (AgoPAM’s) bind distinct sites on GPR40 eliciting
differentiated pre-clinical efficacy. Here, we present the path to a
ternary complex structure with partial and full allosteric agonists
bound, and evidence supporting an identified novel, lipid-facing
AgoPAM binding pocket.
15:20-15:45
XIAOPENG BAI
Investigator, GSK
DNA-encoded Library Technology (ELT) at
GSK: Hit Identification and Beyond
DNA-encoded Library Technologies (ELT) has
evolved into important screening platforms
in pharmaceutical industry. The recent advancement in the ELT
platform at GSK will be discussed together with several case studies
on how the technology has impacted the drug discovery programs.
In addition, the application of ELT on parallel screening of large sets
of proteins will also be presented to demonstrate its potential on the
identification and prioritization of therapeutic targets.
15:45-16:10
AYLIN HANYALOGLU
Senior Lecturer, Institute of Reproductive and
Developmental Biology, Department of Surgery
and Cancer, Faculty of Medicine, Imperial
College London
Multi-dimensional programming of GPCR
signalling via the endocytic pathway; functional and therapeutic
applications
• Recent studies have not only demonstrated that membrane
trafficking of GPCRs is critical for temporal control of cell surface
signalling, but that signalling can also be reactivated or continue to
signal from highly distinct endocytic compartments.
• GPCRs are divergently organized within the endocytic system
and our recent work demonstrates that compartmental bias in
signalling occurs is tightly regulated by location
• across a complex inter-endosomal communication system.
• Examples of how spatially encoded GPCR signalling is critical for
physiological function and potentially perturbed in disease
15:45-16:10
Afternoon Refreshments / Poster Presentations / One-to-One Networking Meetings16:10-17:00 Room: Lindbergh & Aviators Lobby
IAN CHURCHER
Head, Protein Degradation Discovery
Performance Unit, GSK
Protein degradation in drug discovery –
where next?
In this presentation I will introduce the concepts
around using targeted protein degradation in drug discovery and
briefly review some of the key published progress. The talk will go
on to highlight opportunities where protein degradation approaches
could give unique ways to identify new medicines and will also
discuss outstanding challenges in the area
17:00-17:30
NICK TERRETT
Scientific Associate Vice President, European
Chemistry Lead, Merck Sharp and Dohme
Cell permeability with beyond ‘Rule of 5’
modalities – do we understand how this works?
• The talk will describe the considerable growth
in interest in beyond ‘Rule of 5’ drug molecules, but there are
significant challenges in achieving cell penetration
• We are beginning to understand the factors that can influence
cell permeability but the picture is still complex with multiple
mechanisms in play
• The talk will describe the need to distinguish between classes of
molecules that can enter cells by passive permeation vs. endocytosis
17:00-17:30
JEAN-LUC GALZI (Reserved)
Research Director, School of Biotechnology,
CNRS, University of Strasbourg
Biased Signalling – Title TBC
15:45-16:10
FREDERIC BERST (Reserved)
Senior Investigator, Program Team Leader, Head
DNA Encoded Library Chemistry Team, Novartis
Institutes for Biomedical Research
DNA Encoded Libraries – Title TBC
9. CONGRESS SCHEDULE DAY 1 MONDAY 27TH
NOVEMBER 2017
GLOBAL MEDICINAL CHEMISTRY & GPCR LEADERS SUMMIT EUROPE 2017
GEORGE BURSLEM
Research Fellow, Crews Lab, Yale University
PROTACs: Inducing Protein Degradation as a
Therapeutic Strategy
For the last 15 years, the Crews lab has focused
on developing Proteolysis Targeting Chimera
(PROTAC), a technology that overcomes the limitations of the
current inhibitor pharmacological paradigm. PROTACs offer a
mechanism to irreversibly inhibit protein function by destruction
of the target proteins. This approach employs heterobifunctional
molecules to recruit target proteins to the cellular quality control
machinery, thus leading to their degradation. We have demonstrated
the ability to degrade a wide variety of targets. This talk will highlight
some of our key findings in the field of protein degradation and
demonstrate the advantages of degradation over inhibition.
17:30-18:00
ALEXANDER ALANINE
Chief Operating Officer, Bactevo
Next generation drug discovery: T.I.M.E. an
integrated micro-droplet based platform’
Bactevo has developed a tightly integrated set of
game-changing proprietary technologies which
radically disrupt current methods of creating new medicines. Our
Totally Integrated Medicines Engine (T.I.M.E.) has been devised to
address the needs of drug discovery and development scientists.
Integrating the latest generation of microfluidics enabling ultra-fast
phenotypic assaying, next-generation encoded synthetic libraries,
natural products, in vitro profiling and in silico machine learning
to create new therapeutics, TIME provides a paradigm shift in the
speed, efficiency and quality of drug discovery. Bactevo is applying
its TIME platform to create a portfolio of therapeutics for the
treatment of diseases involving defects in mitochondrial function,
with an internal focus on rare diseases.
17:30-18:00
METTE ROSENKILDE
Professor, Laboratory for Molecular
Pharmacology, Department of Biomedical
Sciences, Faculty of Health and Medical
Sciences, University of Copenhagen
Development of GIP receptor antagonists to
reveal the role of GIP in normal physiology and
during diseases like obesity and T2D
Family B has the conserved 7TM domain and is distinguished from
other families by the large N-terminal extracellular domain (ECD)
for which structural information is available. Recently, increased
interest for the structure of the 7TM domain of family B GPCRs
has resulted in novel crystal structures. Glucose-dependent
insulinotropic polypeptide (GIP) is an incretin hormone secreted
from enteroendocrine K-cells in the postprandial state in parallel
with GLP1, secreted from L-cells. Both stimulate insulin secretion
when blood glucose is high. Yet only GIP stimulates glucagon
secretion during hypoglycemia and also inhibits bone resorption and
stimulates fat deposition. I present the discovery of the first GIPR
antagonist with efficacy in humans designed to reveal the role of
GIP in pathophysiological conditions like obesity and T2D.
17:30-18:00
ALESSIO CIULLI
Professor of Chemical & Structural Biology, Division
of Biological Chemistry and Drug Discovery, School
of Life Sciences, University of Dundee
Targeted protein degradation with small
molecules: How PROTACs work.
Targeted protein degradation is a new modality of pharmacological
intervention onto biological systems with therapeutic potential.
One approach is to design bivalent degrader molecules (also called
PROTACs) that comprise of a ligand for the target protein, and a
ligand for an E3 ubiquitin ligase, joined by a linker. Formation of a
ternary complex between the degrader, the ligase and the target
triggers target polyubiquitylation and subsequent degradation by
the proteasome. I will describe research that led to the structure-
guided design of VH298, a potent and selective ligand for the E3
ligase VHL, a discovery that opened the door to the development
of increasingly ‘drug-like’ molecules. Our first crystal structure of a
PROTAC bound to its ligase and target protein has shone new light
into how PROTACs work.
18:00-18:30
HORST HEMMERLE (Reserved)
Executive Director, Lead Generation, Novartis
Lead generation Strategies17:30-18:00
ROCHDI BOUHELAL (Reserved)
Senior Investigator, Novartis
Title TBC
17:30-18:00
Chair's Closing Remarks / End of Day One18:25
Networking Drinks Reception18:25-19:25 Room: Lindbergh & Aviators Lobby
10. CONGRESS SCHEDULE DAY 2 TUESDAY 28TH
NOVEMBER 2017
Refreshments / One-to-One Partnering Meetings08:00-08:40
INTEGRATING MEDICINAL CHEMISTRY INTO THE DRUG DISCOVERY PROCESS PARTNERSHIPS, COLLABORATIONS & OUTSOURCING
Room: Lindbergh 2&3 Room: Lindbergh 1
08:40-09:15
KEYNOTE ADDRESS:
FIONA MARSHALL
Founder, Director & CSO, Heptares Therapeutics
Structure based drug design applied to allosteric modulators of GPCRs
• Heptares Therapeutics have applied it’s StaR® technology platform to generate over 150 GPCR ligand co-structures
• Many of these structures have revealed a diverse range of unexpected allosteric binding sites throughout the GPCR protein
• These novel allosteric binding sites may be exploited for the design of novel drugs targeting the GPCR superfamily
GISBERT SCHNEIDER
Professor, Computer-Assisted Drug Design at
the Institute of Pharmaceutical Sciences in the
Department of Chemistry and Applied Biosciences,
ETH Zurich
Automating drug discovery
• Artificial intelligence methods for molecular design
• Target prediction and hit de-orphaning
• Robotic synthesis and testing
GARRY PAIRAUDEAU
Head of External Sciences, AstraZeneca
Open Innovation at Astrazeneca - Title TBC
09:15-09:45
09:15-09:45
09:45-10:15
09:45-10:15
For sponsorship opportunities please contact
Faizel Ismail at faizel@globalengage.co.uk
SOLUTION PROVIDER PRESENTATION
Morning Refreshments / Poster Presentation Sessions / One-to-One Partnering Meetings10:15-11:25
DARREN GREEN
Director Molecular Design, GSK
Automation, Analytics and AI: what is and what
should never be
This presentation will describe how data-driven
chemoinformatics methods may automate much of
what has historically been done by a medicinal chemist. It will explore
what is reasonable to expect “AI” approaches might achieve, and what
is best left with a human expert.
MARK BOYS
Principal Research Investigator, Array BioPharma
Partnering and outsourcing, experiences from a
small company perspective
Throughout its almost 20 years of existence Array
BioPharma has a rich history of partnerships.
Many IND’s have been generated for partners, a significant number
of these experimental drugs are still active in various stages of clinical
development. Some of these partnerships will be discussed with reference
to the deal structure, what worked well and what were important learnings
or pitfalls. More recently Array has moved to a flexible business model with
more impetus behind strategic outsourcing and contingency resources.
Key learnings from these endeavours will be discussed.
11:25-11:55
11:25-11:55
11:55-12:25
11:55-12:25
For sponsorship opportunities please contact
Faizel Ismail at faizel@globalengage.co.uk
SOLUTION PROVIDER PRESENTATION
GLOBAL MEDICINAL CHEMISTRY & GPCR LEADERS SUMMIT EUROPE 2017
Room: Lindbergh & Aviators Lobby
Room: Lindbergh & Aviators Lobby
SOLUTION PROVIDER PRESENTATION:
SENIOR REPRESENTATIVE
Jubilant Biosys
SOLUTION PROVIDER
PRESENTATION:
HONG SHEN
Head of Medicinal Chemistry and Head of
External Innovation Therapeutic Modalities,
Roche Innovation Center Shanghai
Structure-based Drug Design (SBDD) in Medicinal Chemistry-
Enabled Drug Discovery
Structure-based drug design (SBDD) allows medicinal chemists
to develop deep insight in establishing the structure activity
relationship (SAR) of chemical series. This powerful drug
discovery approach enables precise modifications to fine tune
molecular properties while maintaining target binding affinity. In
addition, SBDD may play a vital role in achieving target selectivity
if an X-ray co-crystal structure or a homology model is available
for the pharmaceutical target as well as the off-target. In this
presentation, several in-house examples will illustrate the power
of SBDD leading to remarkable progress in potency improvement,
particularly with respect to challenging PPI targets, key issue
resolution, or extraordinary target selectivity.
11. CONGRESS SCHEDULE DAY 2 TUESDAY 28TH
NOVEMBER 2017
GLOBAL MEDICINAL CHEMISTRY & GPCR LEADERS SUMMIT EUROPE 2017
ALLEYN PLOWRIGHT
Head of Integrated Drug Discovery Germany, Sanofi
Applications of New Synthetic Modalities in
Drug Discovery
• Opportunities and applications with New
Modalities in Drug Discovery
• Natural peptidic frameworks for peptide therapeutics
• Mixed modalities for half-life extension and tissue targeting
• Optimization of physicochemical and biophysical properties
12:25-12:50
50 MINUTE EXECUTIVE PANEL DISCUSSION:
Best methods to identify, choose and manage your partner
GARRY PAIRAUDEAU
Head of External Sciences, AstraZeneca
CRAIG JOHNSTONE
Executive Vice President, Head of Chemistry and
Directeur General, Evotec (France) SAS
Senior Representatives x2
12:25-13:15
12:50-13:15
MATTHIAS ZENTGRAF
Head of Computational Chemistry, Boehringer-
Ingelheim
eDesign – The next generation molecular
design platform
Excellence in molecular design is a key business
capability of every research driven Pharma Company. Boehringer
Ingelheim has recently implemented a molecular design platform
to provide scientists live access to contextual experimental data
and in-silico predictions during their molecular design sessions
and idea prioritization discussions. It facilitates molecular designs
of an even higher quality and a more stringent prioritization of
compounds for synthesis.
JONATHAN MASON
Senior Research Fellow & Head of CADD,
Heptares Therapeutics (UK)
High End GPCR SBDD: The Revolution in GPCR
Ligand Design from Multiple Co-Crystal X-Ray
Structures
• Unexpected binding modes of ligands for GPCR targets revealed
from new X-ray structures
• Key role of water molecules in ligand binding and selectivity
• Implications of these new experimental findings for all ligand
identification & design/optimisation
TAKASHI ICHIKAWA
Senior Director, Head of Drug Discovery Chemistry
Laboratories, CNS Drug Discovery Unit, Research,
Takeda Pharmaceutical Company Limited
Driving External Chemistry Optimization at
Takeda - Management of Chemistry CRO
The exploration of new business models to effectively utilize contract
research organizations (CROs) would be common topic in the Pharma
Industries. Especially in the synthetic chemistry arena, the Pharma
industries can increasingly leverage external synthetic execution
capabilities as long as the management effort to conduct daily research
activities can be streamlined to maximize efficiency and output. Takeda
has developed an interface with IT for this purpose, which we call
Takeda Outsourcing Management Interface (TOMi). TOMi has the
following IT functions without email; communication board, compound
shipping tracking, individual and team productivity data, final report
posting, and sharing document. I will show you detail about that. In
addition, I would like to discuss how to manage CRO's productivity.
14:15-14:45
14:15-14:45
DON KYLE (Reserved)
Vice President, Discovery Research and Non-
Clinical Development, Purdue Pharma
IP Analysis – Title TBC
14:45-15:15
14:40-15:10
STEPHEN SHUTTLEWORTH
Chief Operating Officer & Chief Scientific Officer,
Karus Therapeutics Ltd
Small Molecule Immuno-oncology – Title TBC
Lunch / One-to-One Partnering Meetings13:15-14:15 Room: Lindbergh & Aviators Lobby
12. CONGRESS SCHEDULE DAY 2 TUESDAY 28TH
NOVEMBER 2017
GLOBAL MEDICINAL CHEMISTRY & GPCR LEADERS SUMMIT EUROPE 2017
EDUARD FELDER
Director, Head of Chemical Core Technologies,
Oncology Research, Nerviano Medical Sciences
The systematic use of highly profiled antitumor
agents in probing the sensitivity contexts
of cancer cells and assessing the validity of
target combinations
A diligently assembled panel of annotated chemical probes, broadly
profiled antitumor agents, including active ingredients of oncology drugs,
is used recurrently for the identification of targets and target combinations
associated with specific cancer sensitivity contexts. This cell-based
screening approach is part of our purinome platform developed in house,
addressing structurally diverse ATP-binding targets such as kinases and
ATPases. Cellular inhibitory activity is cross-referenced with biochemical
data to identify candidate targets. Our results on six different Chordoma
cell lines show Afatinib, an FDA approved EGFR inhibitor, being broadly
active across all lines, unlike other biochemically equipotent EGFR
inhibitors. Other applications range from the characterization of MELK as a
novel survival marker in particular carcinomas to the documentation of the
polypharmacology effects of clinically relevant kinase inhibitors.
15:45-16:15
ONE HOUR ROUNDTABLE DISCUSSIONS:
1) Targeted Protein Degradation
LAWRENCE HAMANN
Vice President, Chemistry, Celgene
2) Optimising hit to lead optimization
DARREN MCKERRECHER
Director Medicinal Chemistry, AstraZeneca
3) Optimising Outsourcing activities
4) DNA Encoded Libraries
5) Fragment Based Drug Discovery
6) GPCR – Biased Signalling
15:15-16:15
Conference Close16:15
BRADLEY MORGAN (Reserved)
Vice President, Cytokinetics
Modulation of Muscle Contractility
Overview of over 15 years of discovery efforts that
have resulted in two compounds currently in phase
3 clinical trials, omecamtive mercarbil for heart
failure and tirsemtiv for ALS
15:15-15:45
13. MAKING A POSTER PRESENTATION
Poster presentation sessions will take place in breaks and alongside the other bkout sessions of the conference. Your presentation will be
displayed in a dedicated area, with the other accepted posters from industry and academic presenters. We also issue a poster eBook to all
attendees with your full abstract in and can share your poster as a PDF after the meeting if you desire (optional). Whether looking for funding,
employment opportunities or simply wanting to share your work with a like-minded and focused group, these are an excellent way to join the
heart of this congress.
In order to present a poster at the congress you need to be registered as a delegate. Please note that there is limited space available and poster
space is assigned on a first come first served basis (subject to checks and successful registration). We charge an admin fee of £100 to industry
delegates to present, that goes towards the shared cost of providing the poster presentation area and display boards, guides etc. This fee is
waived for those representing academic institutions and not for profit organisations.
POSTER PRESENTATIONS
14. VENUE INFORMATION
London Heathrow Marriott Hotel,
Bath Road, Hayes,
UB3 5AN, United Kingdom
The London Heathrow Marriott Hotel provides a welcoming home
away from home for business and leisure guests and is conveniently
located half a mile from the airport. Stretch out in one of our beautiful
guest rooms, which boast soundproof windows, pillowtop bedding
and high-speed Internet access. Treat yourself to delicious dining
at one of our several hotel restaurants and bars, including Tuscany
Ristorante, Cast Iron Grill and THE SEVENS. Additional perks include
on-site parking & free Wi-Fi in the lobby and public areas of the hotel.
Staying fit here in London is easy, thanks to our modern Leisure Club
and heated indoor pool. Our award winning, interactive meeting
venues provide the flexibility you need to host a truly successful event.
Winners of the London Venue Awards and the European Hotel Design
Awards for Best Hotel Event Space.
GLOBAL MEDICINAL CHEMISTRY & GPCR LEADERS SUMMIT EUROPE 2017
15. T: +44 (0) 1865 849841
E: info@globalengage.co.uk
www.global-engage.com
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For more details contact Faizel Ismail/Tony Couch at
sponsorship@globalengage.co.uk or call +44 (0) 1865 849841
DON’T DELAY, BOOK YOUR PLACE TODAY!
Places are limited and are based on a first come, first served basis so to avoid disappointment contact us today to reserve
your place at Global Engage’s Global Medicinal Chemistry Leaders Summit Europe 2017 on the 27th
– 28th
November 2017.
PHONE BOOKING
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Our conference team will make all the necessary arrangements.
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Visit the website to book your place
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THE CONGRESS PACKAGE INCLUDES:
All Conference Sessions
Lunches and Refreshments
Access to Exhibition Room
Networking Drinks Reception
Conference Workbook
E-Document Pack
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Hotel accommodation will be available at a group rate.
FREE NEWSLETTER
For updates on the Global Medicinal Chemistry Leaders Summit Europe 2017, plus free resources
and reports, as and when our speakers authorise their release dates, check for updates at:
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