Mycobacteria

1. Mycobacteria Ziad Elnasser, MD, Ph.D

3. Mycobacteria • Structurally is gram positive rod, characteristic of acid fastness. • M. tuberculosis is the leading cause of infectious disease deaths in the world. • M. leprae and leprosy. • Atypical mycobacteria and immunecompromised conditions. • 0.2-0.4 x 2-10 μ, nonmotile, obligate aerobes, nonspore former, N-glycolyl muramic acid instead of N-acetyl muramic acid.

4. Structure • Polysaccharides, proteins and lipids in the cell wall. • Mycolic acids are long chain fatty acids >60% of the cell wall. • Mycosides, sulfolipids, Lipoarabinomannan (LAM) analogous to LPS of g- bacteria. • Porins and others.

7. Structure • Hydrophobic cell wall → no regular stains. • Acid fastness. • Enhanced growth with 10% CO2, PH 6.5 to 6.8). • Classification is based on phenotypic, nutritional, growth rate, pigmentation of colonies in light or dark, biochemical tests, fatty acids, rRNA and DNA sequences → Probes.

8. Diseases • Many pathogenic species, M. tuberculosis in humans only, others in special cases. • Chronic course, granulomas no disease to follow. • No exotoxins, or endotoxins. • DTH response leads to destruction of macrophages having the organisms, CMI activates macrophages.

9. M. tuberculosis • AFB, irregular beads, 37C, Complexed media, CO2 ehancement, 12-24 hours generation time. • Lowenstein-Jensen media, Dry rough, buff-colored colonies in 3-6 weeks. • Cording, Niacin production, hydrophobic so it is resistant. • PPD.

11. Tuberculosis • Systemic, immune response, chronic pneumonia with fever, cough, bloody sputum and wt loss. • Chronic wasting then death (consumption) • 200-700/100,000 deaths, white plague. • Poverty, ignorance and low socioeconomic status, developed countries. • Aerosol, milk, 10 bacilli is enough, the closer the area the more infectivity. • Very low in developed countries, old age, AIDS→ reactivation. • 30 millions globally, 8 mil new cases 2-3 mil die.

12. Pathogenesis • Primary is the initial infection. • Bacilli in alveoli, then macrophages. • Hilar LNs drainage, systemic any where. • Tubercle → multinucleated giant cells, epitheliod cells, lymphocytes, caseous necrosis in the center. • Fibrosis healing, sub apical area of lungs, organism die. • Kidneys. • Reactivation. • Virulence related to structure.

15. Immunity • Lubeck disaster, genetic effect. • DTH and CMI in 2-6 weeks. • DTH destroys nonactivated macrophages. • CMI destroys activated macrophages. • Both T helper and T cytotoxic participates. • If CMI is impaired lots of bacilli seen with less epitheloid cells accumulation.

18. Clinical Aspects • Primary could be asymptomatic or fever, malaise, large LNs, infiltrates in the lung, fibrosis, calcify (ghon focus), could dissaminate (milliary). • Reactivation TB: 10% recover from primary, old age, immunesuppression, malnutrition, alcoholism, DM, loss of spouse, pregnancy, AIDS. • Bloody cough, fever, malaise, fatigue, wt loss, granulomas, 2-5 years death.

19. Diagnosis • Tuberculin: PPD, measures DTH, standardized, 5 TU. • Intradermal injection. • Interpretation. • Laboratory Dx: ZN staining, sputum, urine, • N-acetyl-cystein role and NaOH. • Media. • Automated systems. • DNA probes.

28. Treatment • Isoniazid. Para-aminosalicylic acid • Ethambutol. Ethionamide. • Rifampin. Cycloserine. • Pyrazinamide. Fluoroquinolones. • Strepotomycin. Kanamycin, etc. • Multiple drug combination! • Multi drug resistance. • Failure of therapy?

29. Prevention • Prophylactic antibiotics. • BCG vaccine, only in PPD negative individulas. • Contraindications to the vaccine.

30. Mycobacteria other than Tuberculosis (MOTT) • M.kansasi, M.avium-intracellulare complex M. scrofulaceum. In lungs. • In tissue: M. fortuitum, M. marinum, M. ucerans. • No case to case transmission. • Grow more rapidly, colored colonies, dark, or light. • More resistant to antimicrobial agents.