1 / 58

CLINICAL APPROACH TO THE DRUG-INDUCED LUNG TOXICITY

CLINICAL APPROACH TO THE DRUG-INDUCED LUNG TOXICITY. Demet KARNAK, MD Ankara University Sc h o o l of Medicine Department of Chest Disease Interstitial Lung Dis e ase Subdivision. DRUG-INDUCED LUNG TOXICITY. First mentioned in 1972 , Rosenow EC 19 drug s, pulmonary toxicity

soren
Download Presentation

CLINICAL APPROACH TO THE DRUG-INDUCED LUNG TOXICITY

An Image/Link below is provided (as is) to download presentation Download Policy: Content on the Website is provided to you AS IS for your information and personal use and may not be sold / licensed / shared on other websites without getting consent from its author. Content is provided to you AS IS for your information and personal use only. Download presentation by click this link. While downloading, if for some reason you are not able to download a presentation, the publisher may have deleted the file from their server. During download, if you can't get a presentation, the file might be deleted by the publisher.

E N D

Presentation Transcript

  1. CLINICAL APPROACH TO THE DRUG-INDUCED LUNG TOXICITY Demet KARNAK, MD Ankara University School of Medicine Department of Chest Disease Interstitial Lung Disease Subdivision

  2. DRUG-INDUCED LUNG TOXICITY • First mentioned in1972,Rosenow EC 19 drugs, pulmonary toxicity • > 350 drugs • First runner of iatrogenic injury • Various types of injury • Mortality and morbidity↑ • Rosenow EC: Dis Mon 40:253-310, 1972 • Aronchick JM, Gefter WB: Semin Roentgenol 30:18-34, 1995

  3. DRUG-INDUCED LUNG TOXICITY • 5% of side effects • 0,03% of hospital deaths • Discontinuation (toxicity and death↓) • Past clinical and drug history in detail • Knowledge about the drugs on the market

  4. DRUG-INDUCED LUNG TOXICITY • Airway involvement (larynx edema, cough, bronchospasm) • Parenchymal involvement (ILD) • Pulmonary circulation (PHT, permeability ↑, vasculitis) • Pleural involvement (effusion, thickening) • Lupus syndrome • Neuromuscular disease(respiratory insufficiency) • Lymphadenopathy

  5. RISK FACTORS • Genetic predisposition • Basic pulmonary functions • Underlying disease • Environmental factors • Activation and detoxification mechanisms • Therapy interactions and other drug toxicity • Dose

  6. DIAGNOSTIC CRITERIA • History of drug exposure • Appropriate clinical picture • Exclusion of other diagnoses • Improvement after therapy cessation • Recurrence after re-administration

  7. TYPES OF INJURY • Interstitial • Alveolar (diffuse lung injury, alveolar hemorrhage, edema) • Vascular

  8. MECHANISMS OF INJURY • Oxidative • Direct toxicity • Phospholipid accumulation induced • Immune system induced

  9. TYPES OF INVOLVEMENT • Asthma • BOOP • Hypersensitivity infiltrates • Interstitial pneumonitis-fibrosis • Non-cardiogenic pulmonary edema • Pleural effusion • Eosinophilia and pulmonary infiltrates • Pulmonary vascular disease

  10. CLINICAL PRESENTATIONS

  11. RADIOGRAPHIC PATTERNS

  12. Bleomycin - ARDS

  13. Bisulphan, cyclophosphamide - BOOP

  14. Amiodarone - BOOP

  15. Amiodarone-BOOP

  16. DRUG INDUCED LUPUS (DIL) • Underlying lupus may become manifest • Activation can occur if predisposition exists • Drug can cause lupus by itself • Fever, myalgia, rash, arthralgia, arthritis, serositis • Parenchymal and pleural involvement, 50% and 75% respectively • Pleural effusion, pleurodynia, diffuse interstitial pneumonitis, alveolar infiltrates • Should be distinguished from spontaneous lupus (SL) (F/M:1 in DIL, F/M:9/1in SL)

  17. DRUG INDUCED LUPUS(DIL) • Discoid lesion or CNS involvement can not be seen, malar rash 2%, renal involvement 5% • Complements ve immune complexes DIL-Normal (vs. SL-↑) • antihistone ab (+) in 95% of cases but other ab (anti-ds DNA) (-) • In 90% of cases, responsible drugs are diphenilhydantoin, hydralazine, procainamide, isoniazid

  18. Sulphonamide Hydralazine İsoniazid Procainamide Amiodarone ACEİ Beta-blocking agents Carbamazepine Gold Simvastatin Etanercept Phenytoin Tetracycline SYSTEMIC LUPUS ERYTHEMATOSUS AND LUPUS-LIKE SYNDROME

  19. DRUG INDUCED BRONCHOSPASM • Propranolol or other beta-adrenergic antagonistsCan increase airway resistance in normal or asemptomatic asthma cases, should not be used in COPD or asthma • Thymolol Can increase airway resistance in asthmatic glocoma cases • Aspirin Causes bronchospasm in 4% of asthma cases • Other non-steroid anti-inflammatory agents Can cause similar symptoms

  20. AMIODARONE • Primary drug causing pulmonary toxicity • Suppresses ventricular and/or supraventricular beats • ILD, OP, ARDS, solitary pulmonary nodule • High concentration oxygen along with amiodarone may lead to ARDS • Immunological mechanisms, direct toxicity or free radicals • Interstitial pneumonitis - 400mg/d • ILD - Incidental beginning, dry cough, dyspnea, weight loss and widespread patchy infiltrates

  21. AMIODARONE • İnfiltrates are not pathognomonic • FOB and BAL excludes infections • Foamy alveolar macrophages, type 2 cell hyperplasia and fibrosis • These features can also be seen in patients without toxicity

  22. AMIODARONE • OP- Dry cough, pleuritic type pain, fever, dyspnea, patchy infiltrates 25% • Pneumonitis, CHF, PTE should be excluded • No specific test • Galium scintigraphy is positive

  23. Amiodarone - high attenuation areas

  24. ACE INHIBITORS • 3-20 % of cases • Persistant, dry cough, increasing cough at night • A couple of months or a year later (after first dose?) • Symptoms decrease in 3 days and disappear in 10 days after cessation • Pathogenesis is not clear - kinins?, substance P? • Arachidonic acid pathway activation by ACE inhibition • Thromboxan A2 elevation and bronchoconstruction • Thromboxan inhibition - stop cough

  25. ACE INHIBITORS

  26. ASPIRIN • Samter syndrome (Aspirin triad) Asthma, nasal poliposis, drug sensitivity - 4% of asthma cases • Vasomotor rhinitis- clear rhinorrhea • Nasal polyps and asthma symptoms in middle ages • Aspirin sensitivity 3rd – 4th decades • Wheezing, flushing, angioedema, gastrointestinal symptoms - 30 min or 2 hrs later

  27. ASPIRIN • Aspirin blocks cyclo-oxigenase 1 pathway which forms thromboxanes and prostoglandins from arachidonic acid. • Alternate way activates by this inhibition. • 5-lipo-oxigenase enzyme converts arachidonic acid to potent bronchoconstrictor compounds (LTC4, LTD4, LTE4)

  28. ANALGESIC AND ANTI-INFLAMMATORY DRUGS: ASPIRIN • High doses (>30-40mg/dl, uncertain) can cause acute pulmonary edema; smoking is a risk factor? • Dyspnea, tachypnea, letargy and confusion, hypoxemia • Obvious cardiomegaly or perihilar alveolar infiltration without pleural fluid • Increased alveolocapillary permeability • 1-2% mortality in youngs, 25% in elder cases

  29. TRANSFUSION LUNG INJURY (TRALI) • Develops a few hours later from tx • Donor originated ab can cause the disease • These antibodies are HLA (Class I or II) or granulocyte-specific • These antibodies appear to act as mediators, which result in granulocyte aggregation, activation, and microvascular pulmonary injury • In a retrospective study, these antibodies were detected in 85% of donors • 80% of patients recover within 96 hours of the original insult • No permanent pulmonary sequelae • Diagnosis can be established by detecting donor originated ab in donor circulation Kopko PM, et al: JAMA 287:1968-71, 2002

  30. ALVEOLAR HEMORRHAGE • After diffuse hemorrhage in pulmonary capillary bed, rare • Incidental BAL diagnosis, subclinic pulmonary infiltrates, hemociderin laden macrophages, ARDS • Unexplained anemia or transient hypoxemia attacks

  31. MICROSCOPIC POLYANGITIS • Anti-thyroid drugs - PTU and thiamazol (methimazol) • Mimics Wegener granulamatosis • Antimyeloperoxidase ab (p-ANCA) positivity • After discontinuation, clinical and immunological symptoms improve

  32. Alveolar hemoraji • Interstitial and alveolar infiltrates causing dyspnea in advanced cases • Increased DLCO, anemia • Hemorrhage or hemociderin laden macrophages in BAL • Otoimmune disease can be excluded by detecting otoantibodies

  33. PTU- Alveolar Hemorrhage

  34. LEUKOTRIENE ANTAGONISTS • Steroid cessation and LTA administration can lead to Churg-Strauss syndrome in asthma cases • Pulmonary infiltrates, cardiomyopathy and eosinophilia can relieve after discontinuation of LTA and commencing steroids Limper AH, Rosenow EC.In Murray JF,Nadel JA. Textbook of Respiratory Medicine, 2000 1971-94

  35. PULMONARY VENO-OCCLUSIVE DISEASE • Iatrogenic disease is extremely rare • Bleomycin, carmustine, gemcytabine, mitomycin, vinca alcoloids, radiation and bone marrow tx • Dyspnea, irregular interstitial changes, Kerley-B lines • PHT and right heart failure

  36. L-TRYPTOPHAN AND EOSINOPHILIA MYALGIA SYNDROME • High doses of L-tryptophan causes EMS • Insidious/rapid onset myalgia, skin changes, and cardiac-neurologic constitutional symptoms can occur • Pulmonary infiltrates, PHT, pleural effusion and acute respiratory insufficiency • Histology; eosinophilic infiltration and angitis • Symptoms relieve by cessation or sometimes be permanent • May be mortal

  37. Pathology

  38. CHEMOTHERAPY RELATED LUNG INJURY • Generaly 2 months after discontinuation . • Main picture - “pulmonary fibrosis” Lacework honey-combing Irregular septal thickening Intralobular lining Marked bronchioles Raugh honey-combing Alteration in anatomy Fibrosis

  39. Agents causing early onset pulmonary injury

  40. VINCA ALCALOIDS • Combination therapy can cause the injury • 387 cases; 25 cases developed acute dyspnea and 87% of cases had focal interstitial infiltrates and reduced DLCO • 60% of cases have chronic respiratory insufficiency • Bronchospasm • Progressive interstitial fibrosis following radiation Luedke D, et al: Cancer 55:542-545, 1985 Rivera MP, et al: Am J Clin Oncol 18:245-250, 1995 Davies AM, et al: Invest New Drugs Apr 18; 2007 (in press)

  41. Methotrexate

  42. Carbo + Vinorelbine

  43. Carbo + Paclitaxel

  44. Agents causing late onset lung injury

  45. Alkylating drugs • Low molecular weight compounds produce direct toxic effect when they pass through pulmonary circulation and they cause interstitial pneumonitis and consequently fibrosis • Bisulphan • Cyclophosphamide • Melphalan • Chlorambusil • BCNU (carmustine)

  46. Bleomycin • Binds Fe+2 and forms Fe+3 • Fe+3 + O2 complex produces free radicals • PG + LTx activation • IL-1, MIP-1, MCP-1, TGF-b, TNF-a areincreased • Redox reaction and fatty acid oxidation • Membrane instabilization • Capillary endothelium damage and apoptosis • Interstitial edema • Type 1 pneumocyte necrosis • Type 2 pneumocyte metaplasia and fibrosis • Bleomycin hydrolase • Liver, spleen, bone marrow, GİS (+) • Lung and skin (-)

More Related