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==Overview==
==Overview==


'''Nontuberculous mycobacteria''' (NTM), or '''atypical mycobacteria''' or '''mycobacteria other than tuberculosis''' (MOTT), are mycobacteria which do not cause [[tuberculosis]] or [[Leprosy|Hansen's disease]] (leprosy).
'''Nontuberculous mycobacteria''' (NTM), also known as '''environmental mycobacteria''', '''atypical mycobacteria'''<ref>{{MeshName|Atypical+Mycobacteria}}</ref> and '''mycobacteria other than tuberculosis''' (MOTT), are [[mycobacteria]] which do not cause [[tuberculosis]] or [[Leprosy|Hansen's disease]] (also known as leprosy).


==Introduction==
Mycobacteria are a family of small, rod-shaped bacilli that can be classified into 3 main groups for the purpose of diagnosis and treatment:
* ''[[Mycobacterium tuberculosis]]'' complex which can cause [[tuberculosis]]: ''[[Mycobacterium tuberculosis|M. tuberculosis]]'', ''[[Mycobacterium bovis|M. bovis]]'', ''[[M. africanum]]'', ''[[M. microti]]'' and ''[[Mycobacterium canetti|M. canetti]]''.
* ''[[Mycobacterium leprae|M. leprae]]'' and ''[[Mycobacterium lepromatosis|M. lepromatosis]]''  which cause [[Leprosy|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.
 
==Taxonomy==
 
{{Main|Runyon classification}}
 
In 1959, botanist Ernest Runyon put these human disease-associated bacteria into four groups ([[Runyon classification]]):<ref name="G221">Grange, p. 221</ref>


Over the past 25 years, there has been a dramatic increase in the number of NTM cases seen by clinicians across the United States and Canada.
*Photochromogens, which develop pigments in or after being exposed to light. Examples include ''[[M. kansasii]]'', ''[[M. simiae]]'' and ''[[M. marinum]]''.<ref name="G221"/>
*Scotochromogens, which become pigmented in darkness. Examples include ''[[Mycobacterium scrofulaceum|M. scrofulaceum]]'' and ''[[M. szulgai]]''.<ref name="G221"/>
*Non-chromogens, which includes a group of prevalent opportunistic pathogens called [[Mycobacterium avium complex|''M. avium'' complex]] (MAC). Other examples are ''[[M. ulcerans]]'', ''[[M. xenopi]]'', ''[[M. malmoense]]'', ''[[M. terrae]]'', ''[[M. haemophilum]]'' and ''[[M. genavense]]''.<ref name="G222">Grange, p. 222</ref>
*Rapid growers include four well recognized pathogenic rapidly growing non-chromogenic species: ''[[M. chelonae]]'', ''[[M. abscessus]]'', ''[[M. fortuitum]]'' and ''[[M. peregrinum]]''. Other examples cause disease rarely, such as ''[[M. smegmatis]]'' and ''[[M. flavescens]]''.<ref name="G222"/>


The correct name of NTM is "nontuberculous mycobacteria."  There is no such bacteria called "nontuberculosis microbacteria."
The number of identified and cataloged NTM species has been increasing rapidly, from about 50 in 1997 to over 125 by January 2007. The surge is mainly due to improved isolation and identification technique.<ref>American Thoracic Society, p.369</ref>


See ''[[Mycobacterium]]'' for more information about this [[genus]] and a list of species.
However, even with these new techniques, the Runyon classification is still sometimes used to organize the mycobacteria into categories.<ref name="pmid12692101">{{cite journal |author=Tortoli E |title=Impact of genotypic studies on mycobacterial taxonomy: the new mycobacteria of the 1990s |journal=Clinical Microbiology Reviews |volume=16 |issue=2 |pages=319–54 |date=April 2003 |pmid=12692101 |pmc=153139 |doi= 10.1128/CMR.16.2.319-354.2003|url=http://cmr.asm.org/cgi/pmidlookup?view=long&pmid=12692101}}</ref>


==Medical classification==
==Epidemiology==


Mycobacteria are a family of small, rod-shaped bacilli that can be classified into 3 main groups for the purpose of diagnosis and treatment:
NTM are widely distributed in the environment, particularly in wet soil, marshland, streams, rivers and estuaries. Different species of NTM prefer different types of environment.<ref name="Grange, p. 226">Grange, p. 226</ref> Human disease is believed to be acquired from environmental exposures, and unlike tuberculosis and leprosy, there has been no evidence of animal-to-human or human-to-human transmission of NTM, hence the alternative label "environmental bacteria".<ref name="ATS370">American Thoracic Society, p. 370</ref>
* ''Mycobacterium tuberculosis'' complex which can cause [[tuberculosis]]: ''[[Mycobacterium tuberculosis|M. tuberculosis]]'', ''[[Mycobacterium bovis|M. bovis]]'', ''M. africanum'', , ''M. microti'' and ''[[M. canetti]]''.
 
* ''[[Mycobacterium leprae|M. leprae]]'' which causes [[Leprosy|Hansen's disease]] or leprosy.
NTM diseases have been seen in most industrialized countries, where incidence rates vary from 1.0 to 1.8 cases per 100,000 persons. Recent studies, including one done in Ontario, Canada, suggest that incidence is much higher.  Pulmonary NTM is estimated by some experts in the field to be at least ten times more common than TB in the U.S., with at least 150,000 cases per year.
* Nontuberculous mycobacteria (NTM) are all the other mycobacteria which can cause pulmonary disease resembling tuberculosis, lymphadenitis, skin disease, or disseminated disease. Pulmonary NTM infections include: MAC (mycobacterium avian complex), which includes M. avium and M. intracellulare; faster-growing M. abscessus, M. chelonae, and M. fortuitum; and less common strains such as M. kansasii and M. xenopi.
 
Most NTM disease cases involve the species MAC, ''M. abscessus'', ''M. fortuitum'' and ''M. kansasii''. ''M. abscessus'' is being seen with increasing frequency and is particularly difficult to treat.<ref name="ATS370"/>
 
Mayo Clinic researchers found a three-fold increased incidence of cutaneous NTM infection between 1980 to 2009 in a population-based study of residents of Olmsted County, Minnesota. The most common species were ''M. marinum'', accounting for 45% of cases and ''M. chelonae'' and ''M. abscessus'', together accounting for 32% of patients.<ref name=Mayo>{{cite journal|last=Wentworth|first=A.B.|coauthors=Drage L.A., Wengenack N.L., Wilson J.W., Lohse C.M.|title=Increased Incidence of Cutaneous Nontuberculous Mycobacterial Infection, 1980 to 2009: A Population-Based Study.|journal=Mayo Clinic Proceedings|date=4 December 2012|doi=10.1016/j.mayocp.2012.06.029|pmid=23218797|url=http://www.ncbi.nlm.nih.gov/pubmed/23218797|accessdate=13 December 2012|volume=88|issue=1|pages=38–45}}</ref> ''M. chelonae'' infection outbreaks, as a consequence of tattooing with infected ink, have been reported in the United Kingdom<ref name=Sergeant>{{cite journal|last=Sergeant|first=A.|coauthors=Conaglen P., Laurenson I.F., Claxton P., Mathers M.E., Kavanagh G.M., Tidman M.J.|title=Mycobacterium chelonae infection: a complication of tattooing.|journal=Clinical and Experimental Dermatology|date=25 July 2012|doi=10.1111/j.1365-2230.2012.04421.x|pmid=22831709|url=http://www.ncbi.nlm.nih.gov/pubmed/22831709|accessdate=13 December 2012|volume=38|issue=2|pages=140–2}}</ref> and the United States.<ref name=CDC>{{cite journal|last=Centers for Disease Control and Prevention (CDC)|title=Tattoo-associated nontuberculous mycobacterial skin infections--multiple states, 2011-2012.|journal=CDC - Morbidity and Mortality Weekly Report (MMWR)|date=24 August 2012|volume=61|issue=33|pages=635–6|pmid=22914227|url=http://www.ncbi.nlm.nih.gov/pubmed/22914227|accessdate=13 December 2012}}</ref>
 
Rapidly growing NTMs are implicated in catheter infections, post-LASIK, skin and soft tissue (especially post-cosmetic surgery) and pulmonary infections.<ref>De Groote, MA and Huitt G. Infections due to Rapidly Growing Mycobacteria. ''Clinical Infectious Diseases'' 2006;42:1756–1763.</ref>
 
==Pathogenesis==
 
The most common clinical manifestation of NTM disease is lung disease, but lymphatic, skin/soft tissue, and disseminated disease are also important.<ref name="ATS370"/>
 
Pulmonary disease caused by NTM is most often seen in post-menopausal women. It is not uncommon for cystic fibrosis, Alpha-1 Antitrypsin Deficiency, Marfan's and Primary Ciliary Dyskenesia patients to have pulmonary NTM colonization and/or infection. Pulmonary NTM can also be found in individuals with [[AIDS]] and malignant disease. It can be caused by many NTM species which depends on region, but most frequently MAC and ''M. kansasii''.<ref name="G225">Grange, p. 225</ref>


Unlike TB and leprosy, which are primarily spread by human-to-human contact, NTM is believed to be contracted from the environment, hence its alternative label, "environmental bacteria." NTM is believed to exist naturally in soil and water.  
[[Lymphadenitis]] can be caused by various species that is different from one place to another; but again, MAC is the main cause worldwide. Most patient are aged less than 5 years, but the incidence is rare for children having [[BCG vaccine]]. The disease has a high curability.<ref name="G223">Grange, p. 223</ref>


==Diagnosis==
Soft tissue disease due to NTM infection include post-traumatic abscesses (caused by rapid growers), [[swimming pool granuloma]] (caused by ''M. marinum'') and [[Buruli ulcer]] (caused by ''M. ulcerans'' or ''M. shinshuense''). Post-traumatic abscesses most commonly occur after injection.<ref name="G223"/>


'''Epidemiology:''' typical NTM patient is female, over age 50, caucasian, slender body habitus, negligible history of smoking.
Disseminated mycobacterial disease was common in US and European AIDS patients in the 1980s and early 1990s, though the incidence has declined in developed nations since the introduction of highly active antiretroviral therapy. It can also occur in individuals after having renal transplantation.<ref name="G225"/>


'''Symptoms:''' Dry cough which becomes very wet, sometimes blood is coughed up; fever, chills, night sweats; recurrent bronchitis or pneumonia; vague malaise and diminished energy.
==Diagnosis==


'''Tests:''' NTM diagnosis requires a high-resolution CT scan of the lungs and Acid Fast Bacilli test of sputum (growth of NTM bacteria will take several weeks or more to occur and sample must be in a cultural media specific to mycobacteria). NTM do not take up a Gram stain (Gram neutral).
Diagnosis of opportunistic mycobacteria is made by repeated isolation and identification of the pathogen with compatible clinical and radiological features. Similar to ''M. tuberculosis'', most nontuberculous mycobacteria can be detected microscopically and grow on [[Löwenstein-Jensen medium]].<ref name="G225"/> Many reference centres now use a nucleic acid-based method such as sequence differences detection in the gene coding for 16S ribosomal RNA to identify the species.<ref name="Grange, p. 226"/>


'''Possible Predisposing or Co-existing Conditions:''' Cystic Fibrosis (including adult onset); Alpha-1 Antitrypsin Deficiency; Primary ciliary diskinesia (Kartagener's Syndrome); GERD; scoliosis; allergies.
Pulmonary NTM disease diagnosis requires both identification of the mycobacterium in the patient's lung(s) as well as a high resolution CT scan of the lungs.


==References==
==Research==
Virginia Tech is conducting a home water supply and patient sputum comparison study to determine source of infection in pulmonary NTM cases.  This study was funded by NTM Info & Research and results will be available by mid-2009.  http://www.ntminfo.org/default_aspx/p/research.aspx {{dead link|date=May 2013}}


* American Thoracic Society Guidelines: Diagnosis, Treatment and Prevention of Nontuberculous Mycobacterial Diseases. Am. J. Respiratory and Critical Care Medicine, Vol. 175, pp. 367-417, 2007[http://www.thoracic.org/sections/publications/statements/pages/mtpi/nontuberculous-mycobacterial-diseases.html]
An epidemiology study on pulmonary NTM is currently being conducted by National Institute of Allergy & Infectious Disease and Kaiser Permanente in southern California. Results will be available by mid-2009This study was funded by NTM Info & Research.


* eMedicine Radiology © - pictures of [[X-ray]] and [[CT scan]] of various findings of NTM disease:
French researchers finalized the genome sequence of ''M. abscessus'' in March 2008.  The genome is available at http://www.ncbi.nlm.nih.gov/sites/entrez?db=genome&cmd=search&term=abscessus.
**[http://www.emedicine.com/radio/topic413.htm Lung, Nontuberculous Mycobacterial Infections] - cavity, volume loss, fibrosis, nodule, bronchiectasis, atelectasis, lymphadenopathy


==External links==
McGill University in Montreal, Canada is conducting a study to determine the genome sequence (type strain) of M. avium intracellulare.  This study is partially funded by NTM Info & Research and results will be available by late 2009.


*[http://www.ntmhandbook.com/ The NTM Handbook: A Guide for Patients with Nontuberculosis Mycobacterial Infections Including MAC] 
==References==
* [http://www.nationaljewish.org/disease-info/diseases/nts-mycobac/progs/index.aspx National Jewish Medical and Research Center]
* [http://www.uthct.edu/research/microbiology/forthepatient.asp University of Texas, Tyler Health Center]
*[http://www.stopntmnow.com/ Stop NonTuberculosis Mycobacterium Now] informational website.


===Organizations===
{{reflist|2}}


*'''NTM Info & Research''' [http://www.ntminfo.org]  
==External Links==
: "ntminfo.org" is the most comprehensive website explaining Nontuberculous Mycobacterial pulmonary disease. NTM (Nontuberculous Mycobacterial) is also known as Atypical TB or MOTT (Mycobacteria Other Than TB),or MAC (Mycobacteria Avium Complex).
*[http://www.ntmhandbook.com/ The NTM Handbook: A Guide for Patients with Nontuberculous Mycobacterial Infections Including MAC]
*[http://www.ntminfo.org/ NTM Info & Research, a nonprofit research and patient support organization]
*[http://www.stopntmnow.com/ Stop NTM Now]
*[http://www.nationaljewish.org/disease-info/diseases/nts-mycobac/progs/index.aspx National Jewish Medical and Research Center]
*[http://www.uthct.edu/research/microbiology/forthepatient.asp University of Texas, Tyler Health Center]


[[Category:Tuberculosis]]
[[Category:Bacterial diseases]]
[[Category:Bacterial diseases]]
[[Category:Bacteriology]]
[[Category:Bacteriology]]
[[Category:Bacterial diseases]]
[[Category:Infectious disease]]
[[Category:Pulmonology]]
[[Category:Pulmonology]]
[[Category:Needs content]]
[[Category:Tuberculosis]]

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Template:Seealso Template:Seealso

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]

Synonyms and keywords: MOTT, NTM

Overview

Nontuberculous mycobacteria (NTM), also known as environmental mycobacteria, atypical mycobacteria[1] and mycobacteria other than tuberculosis (MOTT), are mycobacteria which do not cause tuberculosis or Hansen's disease (also known as leprosy).

Mycobacteria are a family of small, rod-shaped bacilli that can be classified into 3 main groups for the purpose of diagnosis and treatment:

Taxonomy

In 1959, botanist Ernest Runyon put these human disease-associated bacteria into four groups (Runyon classification):[2]

The number of identified and cataloged NTM species has been increasing rapidly, from about 50 in 1997 to over 125 by January 2007. The surge is mainly due to improved isolation and identification technique.[4]

However, even with these new techniques, the Runyon classification is still sometimes used to organize the mycobacteria into categories.[5]

Epidemiology

NTM are widely distributed in the environment, particularly in wet soil, marshland, streams, rivers and estuaries. Different species of NTM prefer different types of environment.[6] Human disease is believed to be acquired from environmental exposures, and unlike tuberculosis and leprosy, there has been no evidence of animal-to-human or human-to-human transmission of NTM, hence the alternative label "environmental bacteria".[7]

NTM diseases have been seen in most industrialized countries, where incidence rates vary from 1.0 to 1.8 cases per 100,000 persons. Recent studies, including one done in Ontario, Canada, suggest that incidence is much higher. Pulmonary NTM is estimated by some experts in the field to be at least ten times more common than TB in the U.S., with at least 150,000 cases per year.

Most NTM disease cases involve the species MAC, M. abscessus, M. fortuitum and M. kansasii. M. abscessus is being seen with increasing frequency and is particularly difficult to treat.[7]

Mayo Clinic researchers found a three-fold increased incidence of cutaneous NTM infection between 1980 to 2009 in a population-based study of residents of Olmsted County, Minnesota. The most common species were M. marinum, accounting for 45% of cases and M. chelonae and M. abscessus, together accounting for 32% of patients.[8] M. chelonae infection outbreaks, as a consequence of tattooing with infected ink, have been reported in the United Kingdom[9] and the United States.[10]

Rapidly growing NTMs are implicated in catheter infections, post-LASIK, skin and soft tissue (especially post-cosmetic surgery) and pulmonary infections.[11]

Pathogenesis

The most common clinical manifestation of NTM disease is lung disease, but lymphatic, skin/soft tissue, and disseminated disease are also important.[7]

Pulmonary disease caused by NTM is most often seen in post-menopausal women. It is not uncommon for cystic fibrosis, Alpha-1 Antitrypsin Deficiency, Marfan's and Primary Ciliary Dyskenesia patients to have pulmonary NTM colonization and/or infection. Pulmonary NTM can also be found in individuals with AIDS and malignant disease. It can be caused by many NTM species which depends on region, but most frequently MAC and M. kansasii.[12]

Lymphadenitis can be caused by various species that is different from one place to another; but again, MAC is the main cause worldwide. Most patient are aged less than 5 years, but the incidence is rare for children having BCG vaccine. The disease has a high curability.[13]

Soft tissue disease due to NTM infection include post-traumatic abscesses (caused by rapid growers), swimming pool granuloma (caused by M. marinum) and Buruli ulcer (caused by M. ulcerans or M. shinshuense). Post-traumatic abscesses most commonly occur after injection.[13]

Disseminated mycobacterial disease was common in US and European AIDS patients in the 1980s and early 1990s, though the incidence has declined in developed nations since the introduction of highly active antiretroviral therapy. It can also occur in individuals after having renal transplantation.[12]

Diagnosis

Diagnosis of opportunistic mycobacteria is made by repeated isolation and identification of the pathogen with compatible clinical and radiological features. Similar to M. tuberculosis, most nontuberculous mycobacteria can be detected microscopically and grow on Löwenstein-Jensen medium.[12] Many reference centres now use a nucleic acid-based method such as sequence differences detection in the gene coding for 16S ribosomal RNA to identify the species.[6]

Pulmonary NTM disease diagnosis requires both identification of the mycobacterium in the patient's lung(s) as well as a high resolution CT scan of the lungs.

Research

Virginia Tech is conducting a home water supply and patient sputum comparison study to determine source of infection in pulmonary NTM cases. This study was funded by NTM Info & Research and results will be available by mid-2009. http://www.ntminfo.org/default_aspx/p/research.aspx[dead link]

An epidemiology study on pulmonary NTM is currently being conducted by National Institute of Allergy & Infectious Disease and Kaiser Permanente in southern California. Results will be available by mid-2009. This study was funded by NTM Info & Research.

French researchers finalized the genome sequence of M. abscessus in March 2008. The genome is available at http://www.ncbi.nlm.nih.gov/sites/entrez?db=genome&cmd=search&term=abscessus.

McGill University in Montreal, Canada is conducting a study to determine the genome sequence (type strain) of M. avium intracellulare. This study is partially funded by NTM Info & Research and results will be available by late 2009.

References

  1. Atypical+Mycobacteria at the US National Library of Medicine Medical Subject Headings (MeSH)
  2. 2.0 2.1 2.2 Grange, p. 221
  3. 3.0 3.1 Grange, p. 222
  4. American Thoracic Society, p.369
  5. Tortoli E (April 2003). "Impact of genotypic studies on mycobacterial taxonomy: the new mycobacteria of the 1990s". Clinical Microbiology Reviews. 16 (2): 319–54. doi:10.1128/CMR.16.2.319-354.2003. PMC 153139. PMID 12692101.
  6. 6.0 6.1 Grange, p. 226
  7. 7.0 7.1 7.2 American Thoracic Society, p. 370
  8. Wentworth, A.B. (4 December 2012). "Increased Incidence of Cutaneous Nontuberculous Mycobacterial Infection, 1980 to 2009: A Population-Based Study". Mayo Clinic Proceedings. 88 (1): 38–45. doi:10.1016/j.mayocp.2012.06.029. PMID 23218797. Retrieved 13 December 2012. Unknown parameter |coauthors= ignored (help)
  9. Sergeant, A. (25 July 2012). "Mycobacterium chelonae infection: a complication of tattooing". Clinical and Experimental Dermatology. 38 (2): 140–2. doi:10.1111/j.1365-2230.2012.04421.x. PMID 22831709. Retrieved 13 December 2012. Unknown parameter |coauthors= ignored (help)
  10. Centers for Disease Control and Prevention (CDC) (24 August 2012). "Tattoo-associated nontuberculous mycobacterial skin infections--multiple states, 2011-2012". CDC - Morbidity and Mortality Weekly Report (MMWR). 61 (33): 635–6. PMID 22914227. Retrieved 13 December 2012.
  11. De Groote, MA and Huitt G. Infections due to Rapidly Growing Mycobacteria. Clinical Infectious Diseases 2006;42:1756–1763.
  12. 12.0 12.1 12.2 Grange, p. 225
  13. 13.0 13.1 Grange, p. 223

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