Mycoplasma

	Mycoplasmosis
	Classification and external resources
ICD-10	A49.3
ICD-9	041.81

Mycoplasma
Scientific classification
Kingdom:	Bacteria;
Phylum:	Tenericutes or; Firmicutes;
Class:	Mollicutes;
Order:	Mycoplasmatales;
Family:	Mycoplasmataceae;
Genus:	Mycoplasma; Nowak 1929
Species
	M. gallisepticum; M. genitalium; M. hominis; M. hyopneumoniae; M. laboratorium; M. ovipneumoniae; M. pneumoniae; etc.

From Wikipedia, the free encyclopedia

Jump to: navigation, search

Not to be confused with Mycobacteria.

Mycoplasma is a genus of bacteria which lack a cell wall.^[1] Without a cell wall, they are unaffected by many common antibiotics such as penicillin or other beta-lactam antibiotics that target cell wall synthesis. They can be parasitic or saprotrophic. Several species are pathogenic in humans, including M. pneumoniae, which is an important cause of atypical pneumonia and other respiratory disorders, and M. genitalium, which is believed to be involved in pelvic inflammatory diseases.

[edit] Origin of the name

The name Mycoplasma, from the Greek mykes (fungus) and plasma (formed), was first used by A. B. Frank in 1889. He thought it was a fungus, due to fungus-like characteristics ^[2].

An older name for Mycoplasma was PleuroPneumonia-Like Organisms (PPLO), referring to organisms similar to the causative agent of contagious bovine pleuropneumonia (CBPP).^[3] It was later found that the fungus-like growth pattern of M. mycoides is unique to that species.

[edit] Characteristics

There are over 100 recognized species of the genus Mycoplasma, one of several genera within the bacterial class Mollicutes. Mollicutes are parasites or commensals of humans, other animals (including insects), and plants; the genus Mycoplasma is by definition restricted to vertebrate hosts. Cholesterol is required for the growth of species of the genus Mycoplasma as well as certain other genera of mollicutes. Their optimum growth temperature is often the temperature of their host if warmbodied (e. g. 37° C in humans) or ambient temperature if the host is unable to regulate its own internal temperature. Analysis of 16S ribosomal RNA sequences as well as gene content strongly suggest that the mollicutes, including the mycoplasmas, are closely related to either the Lactobacillus or the Clostridium branch of the phylogenetic tree (Firmicutes sensu stricto).

[edit] Cell wall structure

The bacteria of the genus Mycoplasma (trivial name: mycoplasmas) and their close relatives are characterized by lack of a cell wall. Despite this, the cells often present a certain shape. These cell shapes presumably contribute to the ability of mycoplasmas to thrive in their respective environments.
For example, the members of the genus Spiroplasma assume an elongated helical shape without the aid of a rigid structural cell envelope. M. pneumoniae cells possess an extension, the so-called 'tip-structure', protruding from the coccoid cell body. This structure is involved in adhesion to host cells, in movement along solid surfaces (gliding motility), and in cell division. M. pneumoniae cells are of small size and pleomorphic, but with a rough shape in longitudinal cross-section resembling that of a round-bottomed flask.

Mycoplasmas are unusual among bacteria in that most require sterols for the stability of their cytoplasmic membrane. Sterols are acquired from the environment, usually as cholesterol from the animal host. Mycoplasmas generally possess a relatively small genome of 0.58-1.38 megabases, which results in drastically reduced biosynthetic capabilities and explains their dependence on a host. Additionally they use an alternate genetic code where the codon UGA is encoding for the amino acid tryptophan instead of the usual opal stop codon. They have a low GC-content (23-40 mol %)

[edit] First isolation

In 1898 Nocard and Roux reported the cultivation of the causative agent of CBPP, which was at that time a grave and widespread disease in cattle herds. ^[4] ^[5] The disease is caused by M. mycoides subsp. mycoides SC (small-colony type), and the work of Nocard and Roux represented the first isolation of a mycoplasma species. Cultivation was, and still is difficult because of the complex growth requirements.

These researchers succeeded by inoculating a semi-permeable pouch of sterile medium with pulmonary fluid from an infected animal and depositing this pouch intraperitoneally into a live rabbit. After fifteen to twenty days, the fluid inside of the recovered pouch was opaque, indicating the growth of a microorganism. Opacity of the fluid was not seen in the control. This turbid broth could then be used to inoculate a second and third round and subsequently introduced into a healthy animal, causing disease. However, this did not work if the material was heated, indicating a biological agent at work. Uninoculated media in the pouch, after removal from the rabbit, could be used to grow the organism in vitro, demonstrating the possibility of cell-free cultivation and ruling out viral causes, although this was not fully appreciated at the time (Nocard and Roux, 1890).

[edit] Small genome

Recent advances in molecular biology and genomics have brought the genetically simple mycoplasmas, particularly M. pneumoniae and its close relative M. genitalium, to a larger audience. The second published complete bacterial genome sequence was that of M. genitalium, which has one of the smallest genomes of free-living organisms.^[6] The M. pneumoniae genome sequence was published soon afterwards and was the first genome sequence determined by primer walking of a cosmid library instead of the whole-genome shotgun method.^[7] Mycoplasma genomics and proteomics continue in efforts to understand the so-called minimal cell,^[8] catalog the entire protein content of a cell,^[9] and generally continue to take advantage of the small genome of these organisms to understand broad biological concepts.

[edit] Taxonomy

The medical and agricultural importance of members of the genus Mycoplasma and related genera has led to the extensive cataloging of many of these organisms by culture, serology, and small subunit rRNA gene and whole genome sequencing. A recent focus in the sub-discipline of molecular phylogenetics has both clarified and confused certain aspects of the organization of the class Mollicutes.^[10]

Originally the trivial name "mycoplasmas" has commonly denoted all members of the class Mollicutes. The name "Mollicutes" is derived from the Latin mollis (soft) and cutes (skin), and all of these bacteria do lack a cell wall and the genetic capability to synthesize peptidoglycan. Now Mycoplasma is a genus in Mollicutes. Despite the lack of a cell wall, many taxonomists have classified Mycoplasma and relatives in the phylum Firmicutes, consisting of low G+C Gram-positive bacteria such as Clostridium, Lactobacillus, and Streptococcus based on 16S rRNA gene analysis. The order Mycoplasmatales contains a single family, Mycoplasmataceae, comprising two genera: Mycoplasma and Ureaplasma.

Historically, the description of a bacterium lacking a cell wall was sufficient to classify it to the genus Mycoplasma and as such it is the oldest and largest genus of the class with about half of the class' species (107 validly described), each usually limited to a specific host and with many hosts harboring more than one species, some pathogenic and some commensal. In later studies, many of these species were found to be phylogenetically distributed among at least three separate orders.

A limiting criterion for inclusion within the genus Mycoplasma is that the organism have a vertebrate host. In fact, the type species, M. mycoides, along with other significant mycoplasma species like M. capricolum, is evolutionarily more closely related to the genus Spiroplasma in the order Entomoplasmatales than to the other members of the Mycoplasma genus. This and other discrepancies will likely remain unresolved because of the extreme confusion that change could engender among the medical and agricultural communities.

The remaining species in the genus Mycoplasma are divided into three non-taxonomic groups, hominis, pneumoniae and fermentans, based on 16S rRNA gene sequences.
The hominis group contains the phylogenetic clusters of M. bovis, M. pulmonis, and M. hominis, among others.
The pneumoniae group contains the clusters of M. muris, M. fastidiosum, U. urealyticum, the currently unculturable haemotrophic mollicutes, informally referred to as haemoplasmas (recently transferred from the genera Haemobartonella and Eperythrozoon), and the M. pneumoniae cluster. This cluster contains the species (and the usual or likely host) M. alvi (bovine), M. amphoriforme (human), M. gallisepticum (avian), M. genitalium (human), M. imitans (avian), M. pirum (uncertain/human), M. testudinis (tortoises), and M. pneumoniae (human). Most if not all of these species share some otherwise unique characteristics including an attachment organelle, homologs of the M. pneumoniae cytadherence-accessory proteins, and specialized modifications of the cell-division apparatus. Mycoplasma hyopneumoniae is a primary bacterial agent of the Porcine Respiratory Disease Complex.

[edit] Early evolution of Mollicutes

A detailed analysis of the 16S rRNA genes from the order Mollicutes has given rise to a view of the evolution of these bacteria that includes an estimate of the time-scale for the emergence of some groups or features.^[11] This analysis suggests that about 600 million years ago (MYA), late in the Proterozoic era, Mollicutes branched away from the low G+C Gram-positive ancestor of the streptococci, losing their cell wall. At this time on Earth, molecular oxygen was present in the atmosphere at 1%, and the fossil record shows that multicellular marine animals had recently spread in the Cambrian explosion. One hundred million years later the requirement for sterols in the cytoplasmic membrane evolved along with the change to the alternate genetic code. Also, the ancestor of the genera Spiroplasma and Entomoplasma (primarily plant and insect pathogens) and Mycoplasma emerged at this time and would itself diverge into the Spiroplasma-Entomoplasma and Mycoplasma lineages approximately 100 million years after that. This diversity coincided with the origin of land plants 500 MYA. It appears that the calculated rate of evolution for the Mycoplasma group increased several fold about 190 MYA, soon after the appearance of vertebrates, while the Spiroplasma-Entomoplasma ancestor continued to evolve at the previously shared slower rate until about 100 MYA, when angiosperms and their associated pollinating insects appeared. Then the evolution rate of these bacteria appears to have also increased significantly. This is an attractive hypothesis, but while it tracks the emergence of several of the unusual characteristics of Mycoplasma and related organisms, it does not address the selective pressures driving their evolution, except perhaps the widespread close association of a parasite with a specific host. The advantages of a reduced genome, cell wall-less structure, and alternate genetic code remain murky.

[edit] Laboratory contaminant

Mycoplasma species are often found in research laboratories as contaminants in cell culture. Mycoplasmal cell culture contamination occurs due to contamination from individuals or contaminated cell culture medium ingredients. Mycoplasma cells are physically small – less than 1 µm – and they are therefore difficult to detect with a conventional microscope. Mycoplasmas may induce cellular changes, including chromosome aberrations, changes in metabolism and cell growth. Severe Mycoplasma infections may destroy a cell line. Detection techniques include PCR, plating on sensitive agar and staining with a DNA stain including DAPI or Hoechst.

[edit] External links

Compare the size of these small bacteria to the sizes of other cells and viruses.
MedPix(r)Images Mycoplasma Pneumonia

[edit] References

^ Ryan KJ, Ray CG (editors) (2004). Sherris Medical Microbiology (4th ed. ed.). McGraw Hill. pp. 409–12. ISBN 0838585299.
^ Conrad J. Krass and Max W. Gardner Etymology of the Term Mycoplasma Int. J. of Syst. Bact.; Jan 1973, p. 62-64; Vol. 23, No. 1
^ Edward DG, Freundt EA (February 1956). "The classification and nomenclature of organisms of the pleuropneumonia group". J. Gen. Microbiol. 14 (1): 197–207. PMID 13306904. pdf [1]
^ Nocard, E.I.E. & Roux, E.; Le microbe de la péripneumonie. Ann Inst Pasteur 12, 240-262. (Translated as ‘The microbe of pleuropneumonia’ in Rev Infect Dis 12, 354-358 (1990))
^ Hayflick L. & Chanock, R.M. (1965). "Mycoplasma Species of Man". Bacteriol. Reviews 29 (2): 185-221. http://mmbr.asm.org/cgi/reprint/29/2/185.pdf.
^ Fraser CM, Gocayne JD, White O, et al. (October 1995). "The minimal gene complement of Mycoplasma genitalium". Science (journal) 270 (5235): 397–403. PMID 7569993. http://www.sciencemag.org/cgi/pmidlookup?view=long&pmid=7569993.
^ Himmelreich R, Hilbert H, Plagens H, Pirkl E, Li BC, Herrmann R (November 1996). "pmid=8948633 Complete sequence analysis of the genome of the bacterium Mycoplasma pneumoniae". Nucleic Acids Res. 24 (22): 4420–49. PMID 8948633. PMC: 146264. http://nar.oxfordjournals.org/cgi/pmidlookup?view=long& pmid=8948633.
^ Hutchison CA, Montague MG (2002). "Mycoplasmas and the minimal genome concept". Molecular Biology and Pathogenicity of Mycoplasmas (Razin S, Herrmann R, eds.). New York: Kluwer Academic/Plenum. pp. 221–54. ISBN 0306472872.
^ Regula JT, Ueberle B, Boguth G, et al. (November 2000). "Towards a two-dimensional proteome map of Mycoplasma pneumoniae". Electrophoresis 21 (17): 3765–80. doi:10.1002/1522-2683(200011)21:17<3765::AID-ELPS3765>3.0.CO;2-6. PMID 11271496.
^ Johansson K-E, Pettersson B (2002). "Taxonomy of Mollicutes". Molecular Biology and Pathogenicity of Mycoplasmas (Razin S, Herrmann R, eds.). New York: Kluwer Academic/Plenum. pp. 1–30. ISBN 0306472872.
^ Maniloff J (2002). "Phylogeny and Evolution". Molecular Biology and Pathogenicity of Mycoplasmas (Razin S, Herrmann R, eds.). New York: Kluwer Academic/Plenum. pp. 31–44. ISBN 0306472872.

[Sherris-0] Ryan KJ, Ray CG (editors) (2004). Sherris Medical Microbiology (4th ed. ed.). McGraw Hill. pp. 409–12. ISBN 0838585299.

[1] Conrad J. Krass and Max W. Gardner Etymology of the Term Mycoplasma Int. J. of Syst. Bact.; Jan 1973, p. 62-64; Vol. 23, No. 1

[Edward-2] Edward DG, Freundt EA (February 1956). "The classification and nomenclature of organisms of the pleuropneumonia group". J. Gen. Microbiol. 14 (1): 197–207. PMID 13306904. pdf [1]

[3] Nocard, E.I.E. & Roux, E.; Le microbe de la péripneumonie. Ann Inst Pasteur 12, 240-262. (Translated as ‘The microbe of pleuropneumonia’ in Rev Infect Dis 12, 354-358 (1990))

[Hayflick-4] Hayflick L. & Chanock, R.M. (1965). "Mycoplasma Species of Man". Bacteriol. Reviews 29 (2): 185-221. http://mmbr.asm.org/cgi/reprint/29/2/185.pdf.

[Fraser-5] Fraser CM, Gocayne JD, White O, et al. (October 1995). "The minimal gene complement of Mycoplasma genitalium". Science (journal) 270 (5235): 397–403. PMID 7569993. http://www.sciencemag.org/cgi/pmidlookup?view=long&pmid=7569993.

[6] Himmelreich R, Hilbert H, Plagens H, Pirkl E, Li BC, Herrmann R (November 1996). "pmid=8948633 Complete sequence analysis of the genome of the bacterium Mycoplasma pneumoniae". Nucleic Acids Res. 24 (22): 4420–49. PMID 8948633. PMC: 146264. http://nar.oxfordjournals.org/cgi/pmidlookup?view=long& pmid=8948633.

[7] Hutchison CA, Montague MG (2002). "Mycoplasmas and the minimal genome concept". Molecular Biology and Pathogenicity of Mycoplasmas (Razin S, Herrmann R, eds.). New York: Kluwer Academic/Plenum. pp. 221–54. ISBN 0306472872.

[8] Regula JT, Ueberle B, Boguth G, et al. (November 2000). "Towards a two-dimensional proteome map of Mycoplasma pneumoniae". Electrophoresis 21 (17): 3765–80. doi:10.1002/1522-2683(200011)21:17<3765::AID-ELPS3765>3.0.CO;2-6. PMID 11271496.

[9] Johansson K-E, Pettersson B (2002). "Taxonomy of Mollicutes". Molecular Biology and Pathogenicity of Mycoplasmas (Razin S, Herrmann R, eds.). New York: Kluwer Academic/Plenum. pp. 1–30. ISBN 0306472872.

[10] Maniloff J (2002). "Phylogeny and Evolution". Molecular Biology and Pathogenicity of Mycoplasmas (Razin S, Herrmann R, eds.). New York: Kluwer Academic/Plenum. pp. 31–44. ISBN 0306472872.

[1]

[2]

[3]

[4]

[5]

[6]

[7]

[8]

[9]

[10]

[11]

Mycoplasma

From Wikipedia, the free encyclopedia

Contents

[edit] Origin of the name

[edit] Characteristics

[edit] Cell wall structure

[edit] First isolation

[edit] Small genome

[edit] Taxonomy

[edit] Early evolution of Mollicutes

[edit] Laboratory contaminant

[edit] See also

[edit] External links

[edit] References

Views

Personal tools

Navigation

Search

Interaction

Toolbox

Languages

Mycoplasmosis
Classification and external resources
ICD-10	A49.3
ICD-9	041.81