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Respiratory Pathophysiology: Pulmonary Infections (Krell) PNEUMONIA: Definition: inflammation of gas exchanging areas of the lungs/lower respiratory tract Epidemiology: 10% of all hospitalizations Complicates hospital course in 5% of all patients 5th leading cause of death in US Leading cause of death from infectious disease in US Normal Host Defenses: Mechanical: o Curved shape of upper airway o Vibrissae (nose hair) Reflexes: o Coughing/sneezing (expel material) Mucociliary Escalator: o Unidirectional beating of airway cilia to move blanket of mucus upward o Brings trapped material to be swallowed or expectorated Cellular: o Alveolar Macrophages: phagocytosis and chemotacxin release o Immunologic Reactions: T Cells: cell mediated immunity B Cells: Ab production Alterations in Host Defenses Predisposing to Pneumonia: Age: o Very young (immature immune system) o Very old (depressed immune function due to debilitation or disease) Debilitation or malnutrition Depressed level of consciousness: o Neurologic illness or injury o Seizures o Drug overdose o Anesthesia Airway abnormalities: o Trauma o Inhalant injury o Obstruction Problems with mucociliary function: o Abnormal mucus (CF) o Poor ciliary function Inhibition of ciliary motion (cigarette smoke, pollutants, alcohol, anesthesia, viral infections, COPD, some drugs) Immotile or dysfunctional cilia syndromes Other Diseases: o Cancer (depressed immunity, obstruction, debilitation) o CHF o Diabetes (altered upper airway flora, decreased immune cell function) o Viral infections (affects mucociliary function, depresses PMN function) o Alcoholism (debility, malnutrition, depressed level of consciousness, poor ciliary function) Immunosuppression o Primary: congenital defect in any system component o Secondary: Neutropenia: drug induced, irradiation, malignancy Defective PMN Function: malignancy, uremia, burns, diabetes, steroids Depressed Cell Mediated Immunity: AIDS, steroids, uremia, cancers, chemotherapy Depressed Humoral Immunity: splenectomy, sickle cell disease, malignancy, irradiation, chemotherapy, malnutrition Modes of Transmissions: Aspiration of Oropharyngeal Organisms: most common* o Pneumococcus: most common bacterial pneumonia (part of normal oral flora) o Anaerobes: live in gingival crevices o Altered upper airway flora: Colonization with pathogens (gram negatives) in hospitals and nursing homes People using needles (IV drug abusers, diabetics, dialysis patients) o Predisposition: Altered state of consciousness Neuromuscular illness Inhalation of Airborne Organisms: o Organisms: Mycoplasma TB Legionella Fungi o Important Factors: Size of inoculums State of host defenses Hematogenous Spread: not very common o Bloodborne infections: spread from elsewhere in the body (ie. IV drug users, infected IV lines) Lymphatic Spread: uncommon o Lymph borne infection: from another body site CLASSIFICATION OF PNEUMONIAS: By Organism: bacterial, viral, fungal etc. By Host Factors: this classification is important because it suggests the potential organisms (start empiric therapy with antibiotics based on these likely organisms while cultures are pending) Community Acquired: seen in normal population (ie. nursing home) Nosocomial: acquired due to hospital environment o Colonization of upper airway by pathogens o Medications, anesthesia may lead to aspiration o Invasive devices can become colonized o Lack of handwashing o Contaminated respiratory equipment Immunocompromised Patients: o Due to underlying disease (cancer, AIDS) o Due to therapy (chemotherapy, radiation, steroids, immunosuppressants) o See infections with unusual pathogens and common bacteria Unusual pathogens include: Fungi Atypical TB Protozoans (Pneumocystis) By Radiographic Appearance: may be distinctive and may help determining potential causative organisms (only a rough guide, not a diagnostic tool) Lobar Pneumonia: o Consolidation (alveolar filling process) o Homogenous white area following anatomic segments (lobes) o Air bronchogram shows air filled airway outlined by consolidated lung o Classic presentation of pneumococcal pneumonia Bronchopneumonia Interstitial Pneumonia Cavitary Lesions Pleural Effusions BACTERIAL PNEUMONIAS: Classic Clinical Picture: Acutely ill with fever Shaking and chills at onset Cough with sputum production Chest pain, chest tightness, and dyspnea may be present Patient History: Rapid onset and course (may be helpful) Determine if CAP, HAP, or immunocompromised Determine if risk factors for aspiration exist Determine patient contacts Recent travel, occupational or environmental exposures Exam: General: fever, tachycardia, tachypnea Lobar Pneumonia: o Percussion dullness o Bronchial breath sounds o Increased tactile/vocal fremitus Patchy/Interstitial Pattern: o Rales or crackles Effusion: o Percussion dullness o Decreased transmission of sounds and fremitus Chest X-Ray: may assist in differential diagnosis (see above) Sputum: Color/Consistency: o Rusty (pneumococcal) o “Currant jelly” (Klebsiella) o Creamy yellow (Staphylococcus) o Foul odor (anaerobes) o Lots of PMNs Gram Stain: o Need adequate specimen: <10 epithelial cells/LPF >25 PMNs/LPF Ratio of PMNs:Epithelial cells ~5:1 o In the ideal situation, identify one single or one prominent organism o Certain pathogens cannot be seen with Gram stain Mycoplasma Legionella TB Viruses Sputum Culture: o Difficult to sort out contaminants from pathogens o Organism may not grow on routine media Other Means: o Cultures from blood or pleural fluid o Serology or skin testing o Invasive diagnostics (bronchoscopy, surgical biopsy) Specific Bacterial Pneumonias: Pneumococcal Pneumonia: o Epidemiology: Most common cause of bacterial pneumonia Can colonize oropharynx of healthy people o Clinical Picture: Acute onset of shaking chills (may follow URI) Fever, dyspnea, pleuritic chest pain Cough with rusty colored sputum Leukocytosis (increased WBC count) Signs of consolidation on exam (chest XR shows lobar consolidation) Gram stain shows G+ lancet shaped diplococci (intracellular) o - - Treatment: Antibiotics: macrolide + 3rd generation cephalosporin (some resistant strains exist) Vaccine: pneumovax o Signs Indicating Poor Outcome: Bacteremia (greater burden of infection) Hematogenous spread (meningitis, endocarditis, arthritis) More than 1 lobe involved Type 3 serotype (more virulent than others) Very young or very old age Mycoplasma Pneumonia (“Walking Pneumonia”): o Epidemiology: Common cause in otherwise healthy young people Outbreaks (family, school, military) Most common in fall and winter Spread by inhalation of infected aerosol o Clinical Picture: Insidious onset of fever, headache, chills, malaise and other systemic manigestations Non-productive cough No leukocytosis Bullous myringitis (blisters on eardrum) Usually bronchopneumonia with patchy rales/crackles heard on exam (rarely consolidates) Patchy bronchopneumonia on chest X-ray Diagnosis by serology Organism does not gram stain well or grow on routine media (3 layered membrane with no cell wll) Positive cold agglutinins test (not all patients) o Treatment: Macrolide OR tetracycline May resolve spontaneously if milder illness Legionella spp.: o Epidemiology: Presents as epidemics or as a nosocomial infection Common source of infection is contaminated water supply or air conditioning units Risk factors: Immunosuppression Smoking COPD Advanced age Male Cardiac disease o Clinical Picture: High fever, recurrent chills, cough, diarrhea (GI involvement) Relative bradycardia (for degree of fever; normally, increase HR by 10bpm per degree of fever increase) Electrolyte disturbances: Hyponatremia Hypophosphatemia Diagnosis: Chest X-ray shows varied patterns (no typical patterns) Does not stain by Gram stain (need silver or DFA stain) Serology Culture on selective media Course may be fulminant and systemic o Treatment: Macrolides OR rifampin - - Aerobic Bacterial Pneumonias: o Hemophilus influenzae: Risk Factors: COPD Alcoholics Sickle cell (asplenia) Immunodeficiency Clinical Picture: Large amounts of sputum Low grade fever Dyspnea and pleuritis Diagnosis: Sputum shows G- coccobacilli (intracellular) Treatment is fairly easy (cephalosporins, sulfa drugs, ampicillin) o Klebsiella pneumoniae: Risk Factors: Alcoholics Diabetes Debilitation Clinical Picture: Abrupt onset of high fevers Diagnosis: Bulging fissure on CXR (lobar pneumonia) Sputum shows plump G- rod Treatment includes cephalosporins or AMGs o Other Gram Negative Pneumonias: Cause mostly HAP (rare cause of CAPs) Nosocomial infections often caused by Pseudomonas Risk Factors: Alcoholics Diabetics Debilitation Immunocompromise Cause necrotizing and destructive infections with very high mortality rate o Staphylococcus aureus: CAP (IV drug users, people with colonization of nasopharynx) Elderly (often follows the flu) Nosocomial infections (IV devices) Sputum shows G+ cocci in clusters (easily cultured) Clinical course involves multiple cavitary lesions , lung destruction and pleural complications Anaerobic Pulmonary Infections: o Mechanism: aspiration o Predisposing Factors: Alcoholism Impaired level of consciousness (drugs, seizures, CNS insult) Dysphagia NM disease Poor oral hygiene (ie. dental caries) o Organisms: usually mixed flora (Fusobacterium, Bacteroides, Peptostreptococcus) o Clinical Picture: Foul smelling sputum Subacute/chronic course History suggestive of aspiration Sweats, malaise, weight loss, leukocytosis o Spectrum: Lung Abscess: occur about 12 days after aspiration (necrosis/liquefaction of tissue) CXR shows cavity with air-fluid level 1/3 extend into pleural space (forming an empyema) Necrotizing Pneumonia: multiple small cavities Patient very ill with high fever and leukocytosis Empyema: infection in the pleural space o Treatment: Antibiotics (penicillin, clindamycin- Abx require long course) Drainage (chest clapping, cough, postural drainage, chest tube) Effusion Related Infections: Parapneumonic: o Occur in relation to pneumonias o Sterile exudates on culture o Treating pneumonia treats the effusion Empyema: o Direct or other spread of infection to pleural space o Organisms seen and cultured from exudates Fluid also contains a lot of PMNs, with low glucose and low pH o Treatment involves antibiotics and pleural space drainage FUNGAL PNEUMONIAS: Coccidiodomycosis: Epidemiology: o Endemic Areas: SW USA, northern border of Mexico, San Joaquin Valley (California) o Life Cycle: Germinates as arthrospore in the soil (infectious to humans) Tissue form in spherule (contains endospores) Immunology: o Skin Testing: coccidiodin (produces induration) Negative to positive skin test means new infections Will be positive between 3 days-3 weeks of illness Positive to negative skin test means severe or disseminated disease o IgM Testing: tube precipitin or latex particle agglutination Positive 2-4 weeks into illness o IgG Testing: complement fixation Positive ~ 8 weeks after infection (results are diagnostic and prognostic) Very high titers result in high chance of disseminated disease o Culture: dangerous (airborne infection via arthrospores) Clinical Patterns: o Asymptomatic: ~60% of cases (only evidence of infection is immunologic) o Primary Coccidiodomycosis: Low grade fever, cough, chest pain, headaches, malaise, joint aches Valley Fever is a specific subtype most often seen in young women Skin lesions (particularly erythema nodosum) Clinical Course: Milder than bacterial pneumonia Most recover without therapy in ~8 weeks Risk Factors for Dissemination: Age (over 50 or under 5) Immunosuppression Race (African Americans, Native Americans, Mexicans and Filipinos higher risk) o Persistent Chronic Infection: uncommon Infection lasting greater than 8 weeks May require anti-fungal therapy o Disseminated Disease: can affect any organ system Often see change in skin test from positive to negative Skin is the most common system effected Worst outcome is meningitis (fatal without treatment) Therapy IV anti-fungals Same risk factors as above Histoplasmosis: Epidemiology: o Endemic Areas: worldwide distribution with centers around Mississippi, Ohio, Missouri and Tennessee River Valleys o Life Cycle: Infectious microconidia (spore) lives in soil Fowl and bat droppings increase growth of fungus Tissue form is narrow necked budding yeast Immunology: o Skin Testing: not useful for making diagnosis because too many people have + reactions Can also cause false positive serologic tests o Serologic Testing: detection of Ab by immunodiffusion Helpful diagnostically but not prognostically o Culture: difficult to grow Clinical Patterns: o Asymptomatic: majority of cases CXR may show calcifications from old infections o Symptomatic: Non-specific malaise, headache, fever, nonproductive cough, pain on swallowing May recover without treatment o Chronic Histoplasmosis: Seen in patients with severe underlying disease (ie. COPD) May need antifungal therapy if pulmonary status deteriorates o Disseminated Histoplasmosis: Rare opportunistic infection that is fatal if untreated Occurs in patients with decreased CMI Sites of dissemination include bone marrow, LNs, GI tract, and oropharynx High dose IV antifungal treatment is required Blastomycosis: Epidemiology: o Endemic Areas: not well known (may be similar to histo) Outbreaks reported in south and south-central US and in regions around Great Lakes o Life Cycle: Dumbbell shaped spores become airborne from soil Reproduce in tissue as broad necked budding yeast Immunology: o Skin Testing: not useful (more likely to indicate histoplasma) o Serologic Testing: not useful (high titer may suggest illness in someone whom the infection is not suspected) o Culture: definitive diagnosis (fast growing and easy to culture) Clinical Patterns: o Asymptomatic: we presume that the majority of infections are asymptomatic OR patients recover without therapy o Acute: Abrupt onset high fever, and productive cough Most recover spontaneously (in about 4 weeks) o Chronic: requires antifungal therapy o Disseminated: Infects lungs, skin (ulcerated lesions), bone (destructive lesions) May also cause prostatitis and epididymitis in males Treatment with IV antifungals Aspergillus: Epidemiology: o Ubiquitous o Type of disease it causes in humans related to status of the patient Immunology: o Skin Testing: valuable in acute forms of aspergillosis (immediate type I hypersensitivity) o Serology: IgE Abs found in patient with acute illness or fungus balls (may also see IgG) - Clinical Patterns: o Hypersensitivity Pneumonitis/Extrinsic Allergic Alveolitis: Cough, dyspnea, fever and chills within 4-6 hours of exposure to spores Responds well to corticosteroids o Allergic Bronchopulmonary Aspergillosis (ABPA): Occurs in patients with longstanding asthma Manifestations: Worsened airflow obstruction Eosinophilia Positive skin test and serology Elevated serum IgE Migratory chest XR infiltrates Cough up brown mucus plugs Treatment with corticosteroids o Aspergilloma (Fungus Ball): Colonization of PRE-EXISTING cavity (ie. old TB) Can cause bleeding and erosion May need to remove surgically o Invasive Aspergillosis: Only seen in immunocompromised patients Immunologic testing is not of value (culture for diagnosis) Treat with more than 1 IV antifungal (very high mortality) COMMUNITY ACQUIRED PNEUMONIA: General: Grouping these patients by age, presence of other medical illnesses and severity of pneumonia helps with determining initial therapy and prognosis Streptococcus pneumoniae is the most common organism in all four groups of CAP Group 1: Classification: o Outpatient pneumonia o No co-morbidity o Age <60 years old Mortality: <5% Organisms: o Streptococcus pneumoniae o Mycoplasma pneumoniae Group 2: Classification: o Outpatient pneumonia o Comorbidity and/or age >60 years old Mortality: <5% Organisms: o Streptococcus penumoniae o Respiratory viruses o Hemophilus influenzae Group 3: Classification: hospitalized with CAP Mortality: 5-25% Organisms: o Streptococcus pneumoniae o Hemophilus infleunzae o Polymicrobial (including anaerobes) o Gram negative bacilli o Legionella o Staphylococcus aureus Group 4: Classification: severe pneumonia (hospitalized, ICU) - Mortality: up to 50% Organisms: o Streptococcus pneumoniae o Legionella o Gram negative bacilli o Respiratory viruses NOSOCOMIAL PNEUMONIAS: Epidemiology: 15% of all pneumonias (high cost, morbidity and mortality) Mechanisms of Infection: Altered upper airway flora (colonized with G- and others) Aspiration of pathogens Organisms from hospital environment are likely to be resistant to therapy Patients have one or more risk factors decreasing normal host defenses Organisms: Enteric Gram Negative Bacilli: 60% o E.coli, Klebsiella, Enterobacter, Pseudomonas, Serratia, Prosteus Staphylococcus aureus: 10% Legionella Others Goals: Prevention Recognition of patients at high risk Prompt recognition and treatment of infections IMMUNOCOMPROMISED HOSTS: Organisms: General: o Most infections are routine G+ and G- bacteria May have atypical presentations Prophylactic Abx often used in these patients Opportunistic Infections: o Definition: organisms that are not pathogenic in a normal host cause disease in immunocompromise o Fungal Infections: Aspergillus (esp. in hematologic malignancies) Candida Dissemination of normally self-limited infections (Histoplasma, Coccidiomycosis) o Viral Infections: Example Scenarios: AIDs or post transplant CMV: most commonly seen Source: o Donor blood or organ o Reactivation of dormant infection in host Clinical: fever and interstitial pneumonia Diagnosis: o Viral inclusions in cells o Cultures o Monoclonal Abs Treatment: supportive care, immune replacement or antivirals o Protozoan Infections: Pneumocystis carinii: AIDS: slowly progressive infection (fever, cough, dyspnea, infiltrative CXR) Leukemia (Kids): more fulminant downhill course Diagnosis: organisms in secretions or tissue Treatment: TMP/SMX (first line); IV pentamidine if can’t tolerate
