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Anatoli Chkaroubo

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Anatoli Chkaroubo. Jessica Fitzgerald. Alison Hulme. Naomi Steenhof ... Incidence: predicted that out of all ADRs 20% are idiosyncratic ... – PowerPoint PPT presentation

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Title: Anatoli Chkaroubo


1
Chemically Induced AutoimmunityIdiosyncratic
Drug Reactions
  • Anatoli Chkaroubo
  • Jessica Fitzgerald
  • Alison Hulme
  • Naomi Steenhof

2
Idiosyncratic Drug Reactions
3
Clinical Characteristics
  • Incidence predicted that out of all ADRs 20 are
    idiosyncratic
  • Time to onset in almost all cases there is a
    delay between starting the drug and the onset of
    the adverse reaction
  • Dose dependence Drugs given at low doses are
    less likely to cause an IDR.
  • Adaptation In many cases the initial reaction
    will resolve despite continued treatment.
  • Clinical Features highly variable being
    dependent on both the drug and the patient. There
    are non-specific manifestations such as fever,
    rash, arthralgia and eosinophilia.

4
Immunology simplified
  • Both Signal 1 and Signal 2 are required for an
    immune response
  • Signal 1 - recognition of drug-modified peptide
    fragments presented in the MHC groove of the APCs
    by T cells
  • Signal 2 co-stimulation of T-cells by APCs

5
Mechanism Hypotheses
  • Hapten Hypothesis
  • PI Hypothesis
  • Danger Hypothesis

6
The Hapten Hypothesis
  • Studies by Landstiner (1935) small molecules
    cannot induce immune response unless they are
    chemically reactive, and bound to protein.
  • Led to Hapten Hypothesis a small molecule
    (called hapten) binds to cellular protein, this
    modified protein is what induces an immune
    response
  • Drug-modified protein is seen as foreign
    immune response

7
Hapten Pathway
  • 1.Reactive drug/metabolites bind to protein
  • 2. Taken up by APC
  • 3. Processsed
  • 4. Presented in MHC groove to T cells
  • 5. Gives immune response

8
  • Evidence for Hapten
  • Penicillin-induced anaphylaxis
  • Penicillin chemically reactive because of
    beta-lactam ring
  • Reacts irreversibly with free amino and
    sulfhydryl groups on proteins
  • Generates immune response against
    penicillin-protein adduct
  • If sufficient IgE antibodies produced severe
    allergic reaction can result (anaphylaxis)
  • Studies in support Most antibodies associated
    with penicillin allergies are directed against
    penicillin-modified proteins

9
Pharmacological Interaction Hypothesis
  • Studies by Pichler (2002) T cell clones from
    patients with IDR history proliferated in the
    presence of drug, in the absence of metabolism
  • Led to PI Hypothesis Drugs bind reversibly to
    MHC complex, induces immune response can lead
    to IDR
  • Drug binds to MHC immune response

10
PI Pathway
  • 1.Drug binds reversibly to MHC complex
  • 2. Presented in MHC groove to T cells
  • 3. Gives immune response

11
Evidence for PI
  • Sulfamethoxazole
  • major drug in original studies
  • primary aromatic amine
  • associated with significant IDR incidence (if
    given 10mg/day)
  • Undergoes oxidation to reactive metabolites
  • controversy What is binding and causing immune
    response? Is it the parent drug, or reactive
    metabolites??
  • Ximegalatran
  • does not form reactive metabolites
  • structurally similar to a small peptide
  • evidence that it binds directly and reversibly to
    MHC

12
The Danger Hypothesis
  • Proposed by Polly Matzinger (1994)
  • challenges the classical self-nonself hypothesis
    of immunology
  • responding to something unless it was causing
    injury or was dangerous to an organism is
    inefficient
  • in general, foreign proteins do not generate a
    significant immune response, unless an adjuvant
    stimulates APCs
  • Damage to cells causes them to release danger
    signals
  • The danger signals up-regulate Signal 2 and cause
    the immune response.
  • No Signal 2 is immune tolerance

13
Danger Pathway
  • In IDRs, it may be that some reactive metabolites
    cause cell damage, which generates a danger
    signal
  • The metabolites themselves could act as danger
    signals rather than as haptens
  • Or they could do both
  • Some drugs may form reactive metabolites but do
    not cause IDRs because the metabolites dont
    cause/dont signal danger

14
Evidence for Danger Hypothesis
  • Therefore, other types of injuries or infections
    could increase the incidence of IDRs.
  • In fact, some viral infections do increase the
    risk of IDRs, as do episodes of inflammation.

A. Roth et al. JPET 307 (2003) 1-8
15
  • danger signals are not all known but are likely
    different for different types of cell stress and
    different types of cells.

M. Pirmohamed et al. / Toxicology 181182 (2002)
5563
16
Drug Induced Lupus Erythematosus
  • A classic IDR

17
Drug Induced Lupus Erythematosus (DILE)
  • an autoimmune disease that can affect skin,
    joints, heart, lungs, kidneys and brain.
  • presents with similar symptoms to idiopathic
    systemic lupus erythematosus (SLE) but resolves
    when causative drug removed
  • as many as 10 of SLE cases could actually be
    DILE
  • DILE is equally probable in males and females
    while SLE is more common in women than in men
    (ratio of 91)
  • must be cautious during diagnosis to confirm that
    it is DILE and not a drug-associated exacerbation
    of SLE or another underlying autoimmune disease.

18
DILE - Causes
  • Generally caused by continuous drug exposure
    ranging from one month to as long as a decade and
    can begin anytime from 3 weeks to 2 years after
    exposure.
  • Physical and clinical problems resolve within
    days to months of withdrawing the causative drug
  • Drugs that can cause DILE hydralazine,
    procainamide, quinidine, isoniazid, diltiazem
    (over 80 confirmed medications that can cause
    DILE)
  • 20 incidence of DILE in procainamide patients at
    normal doses for one year.
  • People who have deficiencies of the
    N-acetyltranserase enzyme are predisposed to
    experiencing DILE

19
DILE - Diagnosis and Treatment
  • no standard diagnostic criteria but generally
    patients have arthritis, serositis, anti-nuclear
    and antihistone antibodies .
  • patients frequently present with arthalgia (often
    the only symptom). Can also have myalgia, fever
    and pericarditis.
  • changes of the skin are less common with DILE
    than SLE
  • NSAIDS to control the symptoms.
  • Corticosteroids and immunosuppressive agents
    should
  • be reserved for patients with organ damage.
  • should not rechallenge because will result in
    recurrence.

20
Strategies to decrease the risk of ADRs
  • Decreasing Reactive Metabolites
  • Developing biomarkers to Predict IDR risk
  • Personalized drug therapy
  • Developing a better understanding of IDR
    mechanism

21
References
  • Kauffman, C. Lisa Lupus Erythematosus,
    Drug-Induced, 2007. http//emedicine.medscape.com
    /article/1065086-overview
  • Matzinger, P. Annu. Rev. lmmunol. 12 (1994)
    991-1045
  • Pirmohamed, M. et al. Toxicology 181182 (2002)
    5563
  • Roth, A. et al. JPET 307 (2003) 1-8
  • Uetrecht , J., Annu. Rev. Pharmacol. Toxicol. 47
    (2007) 51339
  • Uetrecht, J. Autoimmunity Reviews 4 (2005)
    309314
  • Vedove CD. Archives of Dermatological Research,
    Drug Induced lupus erythematosus
  • 2009 Jan 301 (1) 99-105
  • Images (accessed March 3 2009)
  • http//www.eorthopod.com/public/patient_education/
    6590/systemic_lupus_erythematosus.html
  • http//www.flickr.com/photos/listsanddiagrams/2389
    358590/
  • http//users.rcn.com/jkimball.ma.ultranet/BiologyP
    ages/T/Tolerance.html
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