Mycobacterium tuberculosis: Difference between revisions

Background

• Mycobacterium tuberculosis causes tuberculosis
• Most commonly pulmonary TB but extrapulmonary tuberculosis is possible (including adenitis, gastrointestinal TB, pericarditis, meningitis)
• Standard treatment for susceptible TB is RIPE x2mo then RI x4mo

Microbiology

• Fastidious, aerobic acid-fast bacillus
• Cell wall has high lipid content
• Generation time is very long (15 to 20 hours)
• M. tuberculosis is a complex that comprises seven species:
  • M. tuberculosis sensu stricto: most common causative organism worldwide
  • M. africanum: 50% of cases in West africa
  • M. canetti: rare cause in Eastern African
  • M. bovis: disease in cattle but can infect humans
  • M. caprae: disease in cattle
  • M. microti: disease in rodents
  • M. pinnipdeii: disease in seals, with rare human infection

Epidemiology

• Typically spread via airborne route
  • Droplets are expelled during coughing, sneezing, or talking, and are suspended in the air
  • They can remain for up to 30 minutes
  • Killed by ultraviolet light
  • Not transmitted via fomites
• About a third of the world is infected, mostly as latent tuberculosis
  • This progresses to active tuberculosis at about 3 or 4% in the first year and 5% over the rest of their life
• Reinfection accounts for ~40% of active tuberculosis in endemic countries
• Highest rates in sub-Saharan Africa and south/southeast Asia

Risk Factors

• Source factors, such as sputum smear positivity, cough, cavitations
• Exposure duration, closeness of contact
• Factors in the exposed person, such as immune compromise, HIV status

Clinical Manifestations

Classification

• Primary vs. reactivation vs. reinfection
• Latent vs. active

Primary Tuberculosis

• Primary tuberculosis is usually asymptomatic
• Possible presentations include mild URTI with cough and/or fever
• May be seen on CXR as infiltrate in mid-lung zones with hilar adenopathy
• Ghon complex, especially in children
• May progress in children and the immunocompromised patients
• Immunological phenomena
  • Erythema nodosum
  • Phlyctenular conjunctivitis
  • Erythema induratum

Pulmonary Tuberculosis

• Most common presentation of active tuberculosis
• Refer to separate article on pulmonary tuberculosis

Extra-Pulmonary Tuberculosis

• Pleural tuberculosis is most common extrapulmonary site
• Scrofula (cervical lymph node infection) next-most common
• Tuberculous meningitis
• Tuberculous pericarditis
• Renal tuberculosis
• Abdominal tuberculosis
• Gastrointestinal tuberculosis
• Cutaneous tuberculosis

Latent Tuberculosis

• Refers to chronic latent infection contained within granulomas that may reactivate in the future
• Refer to Latent tuberculosis infection

Other

• Neonatal tuberculosis

Investigations

• Radiography: chest x-ray with or without CT chest
  • Primary TB: consolidation, lymphadenopathy, pleural effusion, Ghon complex
  • Reactivation TB: patchy upper-lobe consolidation, cavitation, fibrosis, pleural disease
  • Miliary TB: uniform 1-3 mm diameter diffuse nodules

Diagnosis

• Latent tuberculosis testing
  • Tuberculin skin test (TST)
  • Interferon-gamma release assay (IGRA)
• Serology or immunologic testing
  • Urine lipoarabinomannan antigen
• Microbiology
  • Samples can include routine or induced sputum (x3 q8h including 1 early AM) or bronchoscopy, or tissue sample
  • Spontaneous sputum should include at least one morning sputum, ideally, but can be done all in a row at least one hour apart if needed
  • Acid-fast bacillus culture of sputum x3 is about 70% sensitive, and PCR (ANTB) x1 is about 75% sensitive
• Molecular testing
  • PCR, including GeneXpert

Management

• Requires at least 2 effective drugs at all times, including at least 3 effective drugs during intensive phase
  • Consider rapid rifampin resistance testing (PCR) in all patients
• Most patients are started on RIPE
  • In cases of increased risk for MDR-TB, still use RIPE while awaiting rapid rifampin testing
  • Typical duration is intensive therapy for 2 months (with at least 3 drugs), then narrowed to at least 2 drugs for the remainder of treatment
  • Rifampin is the most effective agent, and any regimen that excludes rifampin must be extended to 12-18 months
• See also:
  • Management of pulmonary tuberculosis
  • Management of tuberculous meningitis
  • Management of drug-resistant tuberculosis

Antibiotics

Doses by Weight

Duration

Routine Monitoring

Clinical

• Start of treatment: physical examination, weight, visual acuity, colour vision testing
• Follow-up: weight, repeat vision testing monthly while on EMB
• Assess adherence, adverse events, and response to therapy

Radiology

• Chest x-ray at diagnosis (if not already done as part of diagnostic process), at 2 months, and at end of therapy

Laboratory

• Start of treatment: CBC, ALT, bilirubin, creatinine, HIV/HBV/HCV serologies, HbA1c
• Follow-up: monthly CBC, creatinine, ALT, and bilirubin

Microbiology

• Sputum culture twice monthly (~q2wk) until smear negative
  • Repeat susceptibility testing if sputum culture is positive at 3 months
  • Sputum induction not required if unable to produce sputum and smear negative
• Nearing end of therapy, sputum culture 2 months and one month before planned end
  • If sputum remains culture positive at 2 months, repeat sputum cultures should be performed monthly until culture conversion is confirmed

Immune Reconstitution Inflammatory Syndrome (IRIS)

Adverse Drug Reactions

Drug-Induced Liver Injury (DILI)

• Most common complication leading to treatment interruption, with a mortality of 6-12% if drugs are not stopped
• Pyrazinamide, followed by isoniazid, then rifampin, are the most common causes of liver injury12
• Most patients can have the same TB drugs reintroduced without recurrence of DILI, though recurrence can be delayed
• Procedure
  • Hold all medications if ALT >120 (3x ULN) and symptoms, if ALT >200 (5x ULN) even without symptoms, or bili >2x ULN
  • If severe disease and patient needs to continue treatment, immediately start two second-line agents (e.g. a fluoroquinolone and an injectable)
  • Once AST & ALT are less than twice the upper limit of normal, reintroduce the original drugs every 3 to 5 days, trending enzymes
  • Only rechallenge with pyrazinamide if it was a mild case

Dermatologic Reactions

Mild Reactions

• Post-dose flushing or itching with or without rash
  • Mostly face or scalp, and may involve redness or watering of the eyes
  • Usually 2 to 3 hours after drug ingestion
  • Caused by rifampin and pyrazinamide
  • Can use an antihistamine if it is bothersome
• Flushing and/or itching with or without a rash, plus hot flashes, palpitations, headaches, or increased blood pressure
  • Immediately after ingestion of certain foods
  • Usually resolves within 2 hours
  • Caused by isoniazid plus tyramine-containing foods (cheese, red wine) or certain fish (tuna, skipjack)
  • Avoid the causative foods

Moderate-to-Severe Reactions

• Hives with or without fever
• Caused by isoniazid < rifampin < pyrazinamide < ethionamide < cycloserine < ethambutol < PASA < streptomycin
• In children, viral infections may be confused for hives

Management

• Discontinue all drugs until the reaction resolves
• Can consider starting TB background regimen with levofloxacin 15-20 mg daily (max 1 g) plus linezolid 600 mg
  • Substitute amikacin 15 mg/kg daily if one of the above cannot be given
• Every 4 days, add a new drug back in the following order, with a lower challenge dose on the first day:
  • Isoniazid 50 mg challenge on day 1 followed by 300 mg on day 2
  • Rifampin 75 mg challenge on day 1 followed by 300 mg on day 2
  • Pyrazinamide 250 mg challenge on day 1 followed by 1 g on day 2
  • Ethionamide 125 mg challenge on day 1 followed by 375 mg on day 2
  • Cycloserine 125 mg challenge on day 1 followed by 250 mg on day 2
  • Ethambutol 100 mg on day 1 followed by 500 mg on day 2
  • PASA 1 g on day 1 followed by 5 g on day 2
  • Streptomycin 125 mg on day 1 followed by 500 mg on day 2
• If the reaction was severe, use 10% of the day 1 dose (e.g. isoniazid 5 mg)

Adherence to Treatment

• Refer to Let's Talk TB

Special Populations

Liver Disease

• Most of the first-line medications (except ethambutol) can cause drug-induced hepatotoxicity and should be avoided
  • Rifampin may be considered in more extensive disease
• In general, a combination of fluoroquinolone plus ethambutol plus an injectable such as amikacin for the first 2 months, followed by fluoroquinolone and ethambutol alone to complete 18 months total

Prevention

Vaccination

• BCG vaccine given at or shortly after birth in many countries

Infection Prevention and Control

• All cases of suspected tuberculosis should be placed in airborne isolation until three sputum smears are negative for tuberculosis, unless it is still suspected and no other diagnosis is made
  • Sputum samples minimum of 1 hour apart, and at least one early morning sample
  • Three induced sputa are preferable to one bronchoscopy
  • Can accept a single negative PCR test if patient is low probability
  • Can accept two negative PCR tests or 1 negative PCR and 2 negative smears if patient is high probability
• For patients with smear-negative, culture-positive, drug-susceptible respiratory TB:
  • Continue airborne precautions until clinical evidence of improvement and a minimum of 2 weeks of effective therapy
  • Can be discharged home provided there is clinical improvement, drug-resistant TB is not suspected, and there is no contraindication for home isolation
• For patient with smear-positive, culture-positive, drug-susceptible respiratory TB:
  • Continue airborne precautions until clinical evidence of improvement and a minimum of 2 weeks of effective therapy
  • Can be stopped at 4 weeks, or earlier if there are 3 negative smears
  • Can be discharge home as above
• For patients with rifampin- or multidrug-resistant TB:
  • Continue airborne precautions as above, but additionally require three negative sputum cultures to be negative before they are taken out of airborne isolation

Further Reading

• Canadian Tuberculosis Standards, 8th Edition. Can J Respiratory Crit Care Sleep Med. 2022;6:sup1.
  • Chapter 1: Epidemiology of tuberculosis in Canada
  • Chapter 2: Transmission and pathogenesis of tuberculosis
  • Chapter 3: Diagnosis of tuberculosis disease and drug-resistant tuberculosis
  • Chapter 4: Diagnosis of tuberculosis infection
  • Chapter 5: Treatment of tuberculosis disease
  • Chapter 6: Tuberculosis preventive treatment in adults
  • Chapter 7: Extra-pulmonary tuberculosis
  • Chapter 8: Drug-resistant tuberculosis
  • Chapter 9: Pediatric tuberculosis
  • Chapter 10: Treatment of active tuberculosis in special populations
  • Chapter 11: Tuberculosis contact investigation and outbreak management
  • Chapter 12: An introductory guide to tuberculosis care to improve cultural competence for health care workers and public health professionals serving Indigenous Peoples of Canada
  • Chapter 13: Tuberculosis surveillance and tuberculosis infection testing and treatment in migrants
  • Chapter 14: Prevention and control of tuberculosis transmission in healthcare settings
  • Chapter 15: Monitoring tuberculosis program performance