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DNDi and the Open Synthesis Network

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Presentation on theme: "DNDi and the Open Synthesis Network"— Presentation transcript:

1 DNDi and the Open Synthesis Network
Benjamin Perry PhD (excerpts from original presentation) Logo

2 Today’s talks 1. Background to DNDi (BP) 2. Leishmaniasis (BP)
3. DNDi discovery process (BP) 4. Open Synthesis Network (BP)

3 1. Background to DNDi

4 Creation of DNDi 2003 Endemic Country Founders Founding Partners
Institut Pasteur, France Indian Council of Medical Research, India Kenya Medical Research Institute, Kenya Médecins Sans Frontières Ministry of Health, Malaysia Oswaldo Cruz Foundation/Fiocruz, Brazil WHO –TDR (Special Programme for Research and Training in Tropical Diseases) as a permanent observer Intro slide – why we were created / history/ Bernard wants to modify wording MARTA: I suggest several photos that illustrate the ‘problem’ – but they are not aligned etc.

5 DNDi’s PRIORITY: Neglected Patients
Responding to the Needs of Patients Suffering from Neglected Diseases… © Sa'adia Khan-MSF Hepatitis C Sleeping sickness DNDi’s PRIORITY: Neglected Patients Malaria Mycetoma Chagas disease Paediatric HIV Filarial diseases Leishmaniasis …from Bench to Bedside

6 Treatment Limitations For Neglected Diseases Safe, Effective, Easy-to-Use Drugs Are Needed
Toxic Painful injections Difficult to use Cause side effects Sometimes high death rate with drug therapy Expensive Not registered in endemic regions Poorly effective - parasites build resistance

7 7 new treatments delivered, recommended, implemented
30 projects, 8 diseases areas 13 entirely new chemical entities (NCEs) Over 160 partnerships, most in endemic countries 160 staff, half in endemic countries & 700 people working on DNDi projects EUR 400 million raised equally from public and private sources 4 regional disease-specific clinical trial platforms/ networks and several technology transfers 2016 SUPERBOOSTER THERAPY P aediatric HIV/TB HI V /TB Easy to use Affordable Field-adapted Non-patented

8 DNDi’s Strategy Address Immediate Patient Needs And Deliver Innovative Medicines New formulations New indications for existing drugs Completing registration dossier Geographical extension New chemical entities (NCEs) Long- term projects Medium- term projects Short-term projects Research Translation Development Implementation Development > 5 years 3-5 years 1-2 years

9 Universities & Research Institutes
DNDi’s success is possible through innovative partnerships PDPs Int. Org. & NGOs Universities & Research Institutes Biotechs Pharmaceutical companies CROs Over 160 partnerships worldwide CRITERIA FOR SUCCESS Share the same vision Mutual understanding Involvement throughout the whole process

10 Some of DNDi’s Open Innovation Projects
NTD Drug Discovery Booster Est. 2015 Open Synthesis Network Est. 2016 Open Source Mycetoma Est. 2015 Anybody & Everybody!

11 2. Leishmaniasis

12 Leishmaniasis 350 million at risk worldwide in 98 countries
Life-threatening disease transmitted by Sandflies 2 types Visceral (VL) fatal without treatment Cutaneous (CL) Skin lesions Symptoms prolonged fever, enlarged spleen & liver, large weight loss, progressive anemia Elimination <1 in 10000, elimination goal for 2020 Treatment needs Oral, safe, effective, low-cost and short-course treatment (in combo)

13 Two Major Forms of Leishmaniasis
VISCERAL FORM 400,000 cases per year CUTANEOUS / MUCOCUTANEOUS FORMS 1.2 million cases per year Localized cutaneous Diffuse cutaneous Muco-cutaneous Fatal if untreated Emerging more Complicated Disease Forms HIV/VL coinfection Post-Kala Azar Dermal Leishmaniasis Patients with chemo-immunosupression .. And Asymptomatic Carriers

14 Leishmaniasis Visceral Leishmaniasis Cutaneous Leishmaniasis
L. donovani L. infantum Cutaneous Leishmaniasis L. major L. tropica L. braziliensis Elimination <1 in 10000, elimination goal for 2020

15 Drugs for Leishmaniasis - the good, the bad & the ugly
Variable efficacy, serious toxicities, only one is oral & rest are painful iv/im

16 DNDi efforts in Leishmaniasis
From Poor drugs to Effective drugs to Oral drugs

17 3. DNDi Discovery

18 Drug Discovery Process
5-7 years + 5-7 years = 10-15 years>

19 Drug Discovery Process
5-7 years + 5-7 years = 10-15 years>

20 Drug Discovery Process
Screen Hit to Lead Lead Optimization Preclinical Output Output Output «Hit» Compound -Single compound demonstrating low-moderate anti-parasitic activity «Hit» Series -Collection of similar compounds, some with improved potency «Lead» Series - Large collection of compounds - Optimized for Potency, PK, Pd, Tox… 1 Compound >100 Compounds >1000 Compounds

21 DNDi compounds in the evolving drug landscape for leishmaniasis
Lead Optimisation Preclinical Phase 1 Discovery Preclinical Phase I DNDI-0690 (nitroimidazole) 2017 DNDI-6148 (oxaborole) Aminopyrazole series CGH VL series 1 GSK /DDD (BA05 series) GNF-6702 (proteasome inhibitor) Candidate from DNDi discovery project Candidate from DNDi discovery project DNDi/Takeda discovery project DNDi/Celgene discovery project

22 4. Open Synthesis Network

23 Open Synthesis Network – Opportunity
Can DNDi benfit from the synthetic firepower of university training to further DNDi projects? and Can DNDi help and enable undergraduate and postgraduate medicinal chemistry training through exposure to active projects Open Synthesis Network

24 DNDi - Centralised biological and physicochemical screening
Open Synthesis Network – The Idea DNDi Medicinal Chemistry Challenge e.g. Improve metabolic stability of a drug hit University Partners Synthetic Chemistry Exercise Select one or more compounds to synthesise as under/post graduate exercise Small Team of Medicinal Chemists Propose a number of compounds to test different hypotheses. Medicinal Chemistry Exercise Option to design and synthesise additional compounds DNDi - Centralised biological and physicochemical screening DNDi Combined data posted in public domain Medicinal Chemistry Teaching Resource DNDi Incorporate data into research Contribution to public health initiative Open Synthesis Network

25 Open Synthesis Network – 2016-2017

26 Open Synthesis Network – Project 1
Based around Aminopyrazole series Annotating SAR avenues previously put on hold Started Oct 2016 Building chemical probes for use in MoA studies Starting Jan 2017 Open Synthesis Network

27 Open Synthesis Network – Web Portal
Access to Web Portal to be provided for Imperial College collaborators in coming weeks Open Synthesis Network

28 Questions ? Open Synthesis Network

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