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Immunology of Asthma through Biologics Private Practice & St Michael’s Hospital Lecturer, Division of Clinical Immunology & Allergy Department of Medicine,

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Presentation on theme: "Immunology of Asthma through Biologics Private Practice & St Michael’s Hospital Lecturer, Division of Clinical Immunology & Allergy Department of Medicine,"— Presentation transcript:

1 Immunology of Asthma through Biologics Private Practice & St Michael’s Hospital Lecturer, Division of Clinical Immunology & Allergy Department of Medicine, University of Toronto Jason Lee, MD, FRCPC

2 Learning Objectives To understand the pathophysiologic basis of biologics in asthma To become familiar with various biologics that have been tried for asthma and the rationale behind these t reatment approaches  learn the immunology

3 Why the need for Biologics? Patients with severe asthma who are uncontrolled with maximum doses of inhaled “conventional” therapies Although only 5% of all asthmatic patients are severe and these patients represent ~50% of health care spending Biologics and asthma is a fascinating topic with a lot of exciting new advances Barnes, JACI. 2012

4 Biologics are the future Current monoclonal antibodies are the fastest growing segment of the pharmaceutical industry Produced based on understanding the underlying immunology: -Cytokines -Monoclonal antibodies -Fusion proteins Albrecht H, Radosevich JA, Babich M. Fundamentals of antibody-related therapy and diagnostics. Drugs Today (Barc) 2009

5 Why use Biologics? Easiest way to form a customized target medication Reduce the number of “collateral damage” thereby limiting side effects 12

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11 What is happening?

12 Healthy airway Smooth muscle

13 Cells have no reaction to allergens Healthy airway

14 With asthma Constricted airway during a n asthma attack Mucus

15 Cells see allergens as pathogens = With asthma

16 Major Inflammatory Cells Mast CellEosinophil 12

17 Mast Cell Activation

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27 Role of IgE in Asthma Initially controversial IgE cross-linking leads to : - More IL4 - More CD40L on T cells - Induction of Eosinophilic inflammation In some asthma patients non-IgE mediated pathways that enhance Th2 cytokines = Even more IgE production

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29 - IgE not acting in Isolation. - Expression of FcεRI receptor has been reported to be increased in fatal asthma Fatal asthm a (n=10) Non-pulmonary d eaths (n=9) Mild-intermittent a sthma † (n=16) *p<0.05 vs other groups; † biopsy Fregonese L, et al. Am J Respir Crit Care Med 2004 (abstract) 1,200 1,000 800 600 400 200 0 FceRI receptor expression in lamina propria (+ cells/mm 2 ) 1,085 *

30 Eosinophil Activation

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34 Biologics used for asthma OmalizumabAnti-il-5 mAbs 12

35 Omalizumab

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42 Omalizumab (n=209) Placebo (n=210) 0.6 0.5 0.4 0.3 0.2 0.1 0 ∆ –50.0% p=0.002 Omalizumab (n=209) Placebo (n=210) 0.6 0.5 0.4 0.3 0.2 0.1 0 ∆ –43.9% p=0.038 Severe exacerbation rateTotal emergency visit rate Humbert M, et al. Allergy 2005 Omalizumab significantly reduces severe exacerbation s and emergency visits

43 Omalizumab significantly reduces the need for systemic corticosteroid bursts Steroid bursts (mean) Omalizumab (n=2,511) Control (n=1,797)) 0.8 0.6 0.4 0.2 0 Relative risk: –43.0% p<0.001 Maykut R, et al. J Allergy Clin Immunol 2006 (abstract) Busse W, et al. Curr Med Res Opin 2007;2379-2386

44 OCS is reduced or stopped in 79% of patients following omalizumab therapy * Steroid bursts (mean) 60 50 40 30 20 10 0 78.8% ReducedStoppedNot reduced/stopped Patients (%) 54.5 Niven R, et al. Thorax 2007 (abstract)

45 Anti-IL-5 mAbs

46 Mepolizumab - Has been shown to reduce bronchial mucosa eosinophilia - In a subgroup: has clinical improvement or FEV1, B HR, peak flows - Reduces some extracellular matrix protein remodeling - 100% reduction in sputum eosinophils and airway eosinophils by 55%

47 Future Therapies - TGF-B - Anti-IL-4 - Anti-IL-5 - Anti-IL-9 - Anti-IL-13 - Inhibition of Th2 cytokines - Inhaled anti-inflammatories targeting neutrophils - Novel classes of bronchodilators (Ro 25-1553, Rho kinase inhibitors - Targeting neutrophilic inflammatory mediators - Masitinib -> a tyrosine kinase inhibitor that blocks c-Kit - Cytokine receptor antagonists - TLR 4 and 9 agonists - Syk Kinase inhibitors - GATA3 antagonists

48 Thank you! Q&A

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