A new antivirulence approach against pathogenic bacteria

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A new antivirulence approach A new antivirulence approach against pathogenic bacteria against pathogenic bacteria May 2005 Sonia Escaich - President & CSO

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A new antivirulence approach against pathogenic bacteria. May 2005 Sonia Escaich - President & CSO. Corporate overview. Biopharmaceutical company specialized in antibacterial drug discovery for prevention of severe infections especially nosocomial Portfolio of intellectual property - PowerPoint PPT Presentation

Transcript of A new antivirulence approach against pathogenic bacteria

Page 1: A new antivirulence approach  against pathogenic bacteria

A new antivirulence approach A new antivirulence approach against pathogenic bacteriaagainst pathogenic bacteria

May 2005Sonia Escaich - President & CSO

Page 2: A new antivirulence approach  against pathogenic bacteria

Corporate overviewCorporate overviewCorporate overviewCorporate overview

• Biopharmaceutical company specialized in antibacterial drug discovery for prevention of severe infections especially nosocomial

• Portfolio of intellectual property

• Virulence validated targets – Preclinical development of inhibitors small molecules

• Experienced management and R&D team - Prestigious academic partnerships - 3 R&D grants (ANVAR, Genhomme,

BioSecurity)

• 20 Employees:– 1 CEO/CSO, 1 director MedChem, 9 biologists/biochemists, 7

medicinal chemists (8 Ph.D,10 RAs)– 2 G&As

• Incorporated mid-2001 - Located at Biocitech Parc, Paris (France)

• EUR 10.2M (USD 13M) raised since 2002 - Investors: BioAm, Axa PE, Auriga, Credit Agricole PE.

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MUTABILIS’ research objectivesMUTABILIS’ research objectivesMUTABILIS’ research objectivesMUTABILIS’ research objectives

Discovery of innovative anti-virulence treatments for nosocomial infections

– Therapeutic molecules : Inhibition of virulence factors.

– Therapeutic vaccines and antibodies

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Background: Medical need for new Background: Medical need for new anti-infective therapiesanti-infective therapiesBackground: Medical need for new Background: Medical need for new anti-infective therapiesanti-infective therapies

• Nosocomial infections (NI) occur in 2-10% of hospitalized patients (ICU, Surgery, internal medicine…)

• Three types of pathogens: Gram+ bacteria: 45%. Gram- bacteria: 35%. Others: 20%.

• Complications of nosocomial infections generate extensive hospitalization, and intensive care costs. Severe infections and sepsis can be lethal (30% cases)

• The increasing number of invasive procedures and the emergence of antibiotic resistance are causing a real public health problem

• Antibiotics-based treatments result in the destruction of commensal bacteria and drug resistance

• Newer antibiotics are kept as last resort therapy

• Nosocomial infections (NI) occur in 2-10% of hospitalized patients (ICU, Surgery, internal medicine…)

• Three types of pathogens: Gram+ bacteria: 45%. Gram- bacteria: 35%. Others: 20%.

• Complications of nosocomial infections generate extensive hospitalization, and intensive care costs. Severe infections and sepsis can be lethal (30% cases)

• The increasing number of invasive procedures and the emergence of antibiotic resistance are causing a real public health problem

• Antibiotics-based treatments result in the destruction of commensal bacteria and drug resistance

• Newer antibiotics are kept as last resort therapy

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Pathogenic bacteria use a range of Pathogenic bacteria use a range of virulence factors to establish infectionvirulence factors to establish infectionPathogenic bacteria use a range of Pathogenic bacteria use a range of virulence factors to establish infectionvirulence factors to establish infection

Pathogenic bacteriaSpecific

ImmunityInnate

Immunity

Colonization

Invasion

Shield to immune system

Toxins

Virulence mechanismsHost defenses

Environment adaptation

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MUTABILIS’MUTABILIS’ approach to virulenceapproach to virulenceMUTABILIS’MUTABILIS’ approach to virulenceapproach to virulence

Gut

Blood

Systemic infection

Selective inhibition of the virulence factors required for systemic dissemination in the host.

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• Drug approach:

– Selective inhibition of pathogenic bacteria by targeting virulence factors necessary for bacterial spreading in blood

– Virulence inhibitors do not perturb development of commensal bacteria

– Diminished risk of developing resistant mutants because of lower selective pressure

This lead to the discovery of new classes of antibacterial molecules that are not classical antibiotics

• Vaccine approach: Inhibition of specific pathogens in a bacterial species

Preventive vaccine/passive immunity for nosocomial infections

Scientific strategy:Scientific strategy:Scientific strategy:Scientific strategy:

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THERAPEUTIC APPROACH: THERAPEUTIC APPROACH: AntibioticsAntibiotics versus virulence versus virulence inhibitors inhibitors THERAPEUTIC APPROACH: THERAPEUTIC APPROACH: AntibioticsAntibiotics versus virulence versus virulence inhibitors inhibitors

• Common ground in both approaches:

– Infections are treated through eradication of bacteria in the blood.

• Advantages of virulence inhibitors:

– Virulence inhibitors do not perturb development of commensal bacteria.– Diminished risk of developing resistant mutants because of lower selective

pressure.

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Anti-virulence product profile opens Anti-virulence product profile opens preventive therapypreventive therapyAnti-virulence product profile opens Anti-virulence product profile opens preventive therapypreventive therapy

• Product profile: – Anti-infective agent (not an antibiotic) which eradicates bacteria from the blood

and leaves the commensal flora untouched.

• Product characteristics:– No induction of bacterial resistance.– No cross resistance with existing antibiotics. – Large gram- spectrum.– Large gram+ spectrum.– Gram- and gram+ combination.

• Product positioning:– Preventive therapy: compound will be used on its own.

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Virulence inhibition: Virulence inhibition: planplanVirulence inhibition: Virulence inhibition: planplan

• Mutagenesis of every coding sequence in the genome of a model bacteria.

• Identification of pathogen genes which are essential for producing systemic infection.

• Validation of these genes as therapeutic targets in experimental models of infection.

• Drug development based on molecules which inhibit these targets.

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Drug discoveryDrug discoveryDrug discoveryDrug discovery

Objective: Discovery of new class of antibacterial molecules for selective inhibition of pathogenic bacteria

Discovery process:Discovery process:•Target identification (complete Tn mutagenesis of pathogenic Gram+ and Gram- pathogenic bacteria) and validation (KO mutants phenotype, protein function, consevation…)

•Rational drug design, virtual screening, hit identification

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Anti-virulence product profile Anti-virulence product profile opens preventive therapy markets.opens preventive therapy markets.Anti-virulence product profile Anti-virulence product profile opens preventive therapy markets.opens preventive therapy markets.

Healthy individuals Patients at risk of infections Infected patients

VACCINATION ANTIVIRULENCE ANTIBIOTICS

Specific to the risk of infection

•Haemophilus•Meningococcus•Pneumococcus•E. Coli•Streptococcus B

Broad spectrum therapy

•Transplantees (kidney, bone marrow, liver, etc.)•Intensive care patients•Cancer patients undergoing treatment•Kidney failure•Corticoid treatment

Pathogenic strainsPrevention

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MUTABILIS targets: conserved, required for virulence and systemic infection but not for commensalism.

MUTABILIS developed assays needed for pharmacological studies.

Efficacy prediction through animal model: targets functions are conserved in animal species and man.

MUTABILIS using rational approaches did identify inhibitors molecules.

Conclusions: virulence projectsConclusions: virulence projects Conclusions: virulence projectsConclusions: virulence projects

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Research area of interest:Research area of interest:Research area of interest:Research area of interest:

• Comparative genomics + physiopathology of infectious diseases Interactions bacteria/host Metabolic pathways common to pathogenic

bacteriaconserved targets

• Bacterial membranes and pharmacology : why some drugs get through or not?