Mycobacterium is a genus of Actinobacteria, given its own family, the Mycobacteriaceae. Over 190 species are recognized in this genus. This genus includes pathogens known to cause serious diseases in mammals, including tuberculosis (Mycobacterium tuberculosis) and leprosy (Mycobacterium leprae) in humans. The Greek prefix myco- means "fungus," alluding to the way mycobacteria have been observed to grow in a mold-like fashion on the surface of cultures. It is acid fast and cannot be stained by the Gram stain procedure.
|TEM micrograph of M. tuberculosis.|
Lehmann & Neumann 1896
- 1 Microbiologic characteristics
- 2 Ecology
- 3 Pathogenicity
- 4 Mycosides
- 5 Genomics
- 6 Evolution
- 7 Species
- 7.1 Slowly growing
- 7.2 Intermediate growth rate
- 7.3 Rapidly growing
- 7.4 Ungrouped
- 7.5 Proposed division of the genus
- 8 Mycobacteriophage
- 9 References
- 10 Further reading
- 11 External links
Metabolism and morphologyEdit
Mycobacteria are aerobic. They are bacillary in form, at least in most phases that have attracted human microbiological attention to date; they are straight or slightly curved rods between 0.2 and 0.6 µm wide and between 1.0 and 10 µm long. They are generally nonmotile bacteria, except for the species Mycobacterium marinum, which has been shown to be motile within macrophages. They are characteristically acid-fast. Mycobacteria have an outer membrane. They possess capsules, and most do not form endospores. M. marinum and perhaps M. bovis have been shown to sporulate; however, this has been contested by further research. The distinguishing characteristic of all Mycobacterium species is that the cell wall is thicker than in many other bacteria, being hydrophobic, waxy, and rich in mycolic acids/mycolates. The cell wall consists of the hydrophobic mycolate layer and a peptidoglycan layer held together by a polysaccharide, arabinogalactan. The cell wall makes a substantial contribution to the hardiness of this genus. The biosynthetic pathways of cell wall components are potential targets for new drugs for tuberculosis.
Many Mycobacterium species adapt readily to growth on very simple substrates, using ammonia or amino acids as nitrogen sources and glycerol as a carbon source in the presence of mineral salts. Optimum growth temperatures vary widely according to the species and range from 25 °C to over 50 °C.
Most Mycobacterium species, including most clinically relevant species, can be cultured in blood agar. However, some species grow very slowly due to extremely long reproductive cycles—M. leprae, may take more than 20 days to proceed through one division cycle (for comparison, some E. coli strains take only 20 minutes), making laboratory culture a slow process. In addition, the availability of genetic manipulation techniques still lags far behind that of other bacterial species.
A natural division occurs between slowly- and rapidly-growing species. Mycobacteria that form colonies clearly visible to the naked eye within 7 days on subculture are termed rapid growers, while those requiring longer periods are termed slow growers.
Some mycobacteria produce carotenoid pigments without light. Others require photoactivation for pigment production.
- Photochromogens (Group I)
- Produce nonpigmented colonies when grown in the dark and pigmented colonies only after exposure to light and reincubation.
- Ex: M. kansasii, M. marinum, M. simiae.
- Scotochromogens (Group II)
- Produce deep yellow to orange colonies when grown in the presence of either the light or the dark.
- Ex: M. scrofulaceum, M. gordonae, M. szulgai.
- Non-chromogens (Groups III and IV)
- Nonpigmented in the light and dark or have only a pale yellow, buff or tan pigment that does not intensify after light exposure.
- Ex: M. tuberculosis, M. avium-intra-cellulare, M. bovis, M. ulcerans, M. xenopi
- Ex: M. fortuitum, M. chelonae
Mycobacteria are widespread organisms, typically living in water (including tap water treated with chlorine) and food sources. Some, however, including the tuberculosis and the leprosy organisms, appear to be obligate parasites and are not found as free-living members of the genus.
Mycobacteria can colonize their hosts without the hosts showing any adverse signs. For example, billions of people around the world have asymptomatic infections of M. tuberculosis (citation needed).
Mycobacterial infections are notoriously difficult to treat. The organisms are hardy due to their cell wall, which is neither truly Gram negative nor positive. In addition, they are naturally resistant to a number of antibiotics that disrupt cell-wall biosynthesis, such as penicillin. Due to their unique cell wall, they can survive long exposure to acids, alkalis, detergents, oxidative bursts, lysis by complement, and many antibiotics. Most mycobacteria are susceptible to the antibiotics clarithromycin and rifamycin, but antibiotic-resistant strains have emerged.
As with other bacterial pathogens, M. tuberculosis produces a number of surface and secreted proteins that contribute to its virulence. However, the mechanism by which these proteins contribute to virulence remains unknown.
Mycobacteria can be classified into several major groups for purpose of diagnosis and treatment: M. tuberculosis complex, which can cause tuberculosis: M. tuberculosis, M. bovis, M. africanum, and M. microti; M. leprae, which causes Hansen's disease or leprosy; nontuberculous mycobacteria (NTM) are all the other mycobacteria, which can cause pulmonary disease resembling tuberculosis, lymphadenitis, skin disease, or disseminated disease.
Mycosides are phenolic alcohols (such as phenolphthiocerol) that were shown to be components of Mycobacterium glycolipids that are termed glycosides of phenolphthiocerol dimycocerosate. Mycosides A and B have 18 and 20 carbon atoms, respectively.
Comparative analyses of mycobacterial genomes have identified several conserved indels and signature proteins that are uniquely found in all sequenced species from the genus Mycobacterium. Additionally, 14 proteins are found only in the species from the genera Mycobacterium and Nocardia, suggesting that these two genera are closely related.
The genomes of some mycobacteria are quite large when compared to other bacteria. For instance, the genome of M. vulneris encodes 6,653 proteins, which is larger than that of small eukaryotes such as yeast (which encodes only ~6,000 proteins).
M. ulcerans evolved from M. marinum.
Phenotypic tests can be used to identify and distinguish different mycobacteria species and strains. In older systems, mycobacteria are grouped based upon their appearance and rate of growth. However, these are symplesiomorphies, and more recent classification is based upon cladistics. Over 100 species are currently recognised.
Runyon's group I, II and III
Mycobacterium tuberculosis complexEdit
- Mycobacterium tuberculosis complex (MTBC) members are causative agents of human and animal tuberculosis. Species in this complex include:
Mycobacterium avium complexEdit
- Mycobacterium avium complex (MAC) is a group of species that, in a disseminated infection but not lung infection, used to be a significant cause of death in AIDS patients. The species M. indicus pranii appears to be basal in this complex. Species in this complex include:
Mycobacterium gordonae cladeEdit
Mycobacterium kansasii cladeEdit
Mycobacterium nonchromogenicum/terrae cladeEdit
Mycobacterium simiae cladeEdit
- M. florentinum
- M. genavense
- M. heidelbergense
- M. interjectum
- M. kubicae
- M. lentiflavum
- M. montefiorense
- M. palustre
- M. parascrofulaceum
- M. simiae
- M. triplex
- M. arabiense
- M. aromaticivorans
- M. aquaticum
- M. bacteremicum
- M. bohemicum
- M. botniense
- M. branderi
- M. celatum
- M. chimaera
- M. conspicuum
- M. cookii
- M. doricum
- M. farcinogenes
- M. haemophilum
- M. heckeshornense
- M. intracellulare
- M. lacus
- M. leprae, which causes leprosy
- M. lepraemurium
- M. lepromatosis, another (less significant) cause of leprosy, described in 2008
- M. liflandii
- M. llatzerense
- M. malmoense
- M. marinum, causes a rare disease called Aquarium granuloma.
- M. neoaurum
- M. monacense
- M. murale
- M. nebraskense
- M. saskatchewanense
- M. sediminis
- M. scrofulaceum
- M. shimoidei
- M. szulgai
- Mycobacterium talmoniae
- M. tusciae
- M. xenopi
- M. yongonense
Intermediate growth rateEdit
Mycobacterium abscessus cladeEdit
Together they are known as the M. abscessus complex
Mycobacterium chelonae cladeEdit
Mycobacterium fortuitum cladeEdit
- M. boenickei
- M. brisbanense
- M. cosmeticum
- M. fortuitum
- M. fortuitum subsp. acetamidolyticum
- M. houstonense
- M. mageritense
- M. neworleansense
- M. peregrinum
- M. porcinum
- M. senegalense
- M. septicum
Mycobacterium mucogenicum cladeEdit
Mycobacterium parafortuitum cladeEdit
Mycobacterium vaccae cladeEdit
- M. agri
- M. aichiense
- M. alvei
- M. arupense
- M. barrassiae
- M. brumae
- M. canariasense
- M. chubuense
- M. conceptionense
- M. confluentis
- M. duvalii
- M. elephantis
- M. flavescens
- M. gadium
- M. gilvum
- M. hassiacum
- M. holsaticum
- M. iranicum
- M. komossense
- M. madagascariense
- M. massilipolynesiensis
- M. moriokaense
- M. obuense
- M. phlei
- M. psychrotolerans
- M. pulveris
- M. pyrenivorans
- M. smegmatis
- M. sphagni
- M. thermoresistibile
- M. vanbaalenii
- M. arosiense
- M. aubagnense
- M. chlorophenolicum
- M. fluoroanthenivorans
- M. kumamotonense
- M. novocastrense
- M. parmense
- M. poriferae
- M. rhodesiae
- M. seoulense
- M. tokaiense
Proposed division of the genusEdit
Gupta et al. have, based on the analysis of 150 species in the genus, proposed dividing Mycobacterium into five genera. The proposed new genera are:
- Mycobacterium based on the Tuberculosis-Simiae clade
- Mycolicibacterium based on the Fortuitum-Vaccae clade
- Mycolicibacter based on the Terrae clade
- Mycolicibacillus based on the Triviale clade
- Mycobacteroides based on the Abscessus-Chelonae clade
Wider acceptance of this proposal is awaited.
Mycobacteria can be infected by mycobacteriophages, bacterial viruses that may be used in the future to treat tuberculosis and related diseases by phage therapy. The procedure may not go into practice in the case of Mtb for some time, as bacteriophage particles cannot penetrate into the tuberculosis bacilli, or clumps.
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