Nocardia asteroides (yellow colonies).
Scientific classification
Kingdom: Bacteria
Phylum: Actinobacteria
Class: Actinobacteria
Order: Actinomycetales
Suborder: Corynebacterineae
Family: Nocardiaceae
Genus: Nocardia
Trevisan 1889

N. aerocolonigenes
N. africana
N. argentinensis
N. asteroides
N. blackwellii
N. brasiliensis
N. brevicatena
N. carnea
N. caviae
N. cerradoensis
N. corallina
N. cyriacigeorgica
N. dassonvillei
N. elegans
N. farcinica
N. nigiitansis
N. nova
N. opaca
N. otitidis-cavarium
N. paucivorans
N. pseudobrasiliensis
N. rubra
N. transvelencesis
N. uniformis
N. vaccinii
N. veterana

Nocardia as found on a brain biopsy.

Nocardia is a genus of weakly staining Gram-positive, catalase-positive, rod-shaped bacteria. It forms partially acid-fast beaded branching filaments (acting as fungi, but being truly bacteria). It has a total of 85 species. Some species are non-pathogenic while others are responsible for nocardiosis.[1] Nocardia are found worldwide in soil that is rich with organic matter. In addition, Nocardia are oral microflora found in healthy gingiva as well as periodontal pockets. Most Nocardia infections are acquired by inhalation of the bacteria or through traumatic introduction.


Culture and Staining

Nocardia colonies have a variable appearance, but most species appear to have aerial hyphae when viewed with a dissecting microscope, particularly when they have been grown on nutritionally limiting media. Nocardia grow slowly on non-selective culture media, and are strict aerobes with the ability to grow in a wide temperature range. Some species are partially acid fast (meaning that a less concentrated solution of sulfuric or hydrochloric acid should be used during the staining procedure) due to the presence of intermediate-length mycolic acids in their cell wall. Majority of strains possess the cord factor (trehalose 6-6' dimycolate) an important virulence factor.

They are catalase positive and can grow easily on the most commonly used media with colonies becoming evident in 3–5 days. However sometimes prolonged incubation periods (2–3 weeks) are needed.

The genus includes at least 30 different species with ten of them isolated from humans.


The various species of Nocardia are pathogenic bacteria with low virulence; therefore clinically significant disease most frequently occurs as an opportunistic infection in those with a weak immune system, such as small children, the elderly, and the immunocompromised (most typically, HIV). Nocardial virulence factors are the enzymes catalase and superoxide dismutase (which inactivate reactive oxygen species that would otherwise prove toxic to the bacteria), as well as a "cord factor" (which interferes with phagocytosis by macrophages by preventing the fusion of the phagosome with the lysosome).

Clinical disease and microbiological diagnosis

Nocardia asteroides is the species of Nocardia most frequently infecting humans, and most cases occur as an opportunistic infection in immunocompromised patients. Other species of medical interest are N. brasiliensis and N. caviae. Because it is acid-fast to some degree, it stains only weakly gram positive.

The most common form of human nocardial disease is a slowly progressive pneumonia, whose common symptoms include cough, dyspnea (shortness of breath), and fever. It is not uncommon for this infection to spread to the pleura or to chest wall. Pre-existing pulmonary disease, especially pulmonary alveolar proteinosis, increases the risk of contracting a Nocardia pneumonia. Every organ can be affected if a systemic spread takes place.

Nocardia spp are deeply involved in the process of endocarditis as one of its main pathogenic effects.

In about 25-33% of people Nocardia infection will take the form of encephalitis and/or brain abscess formation.

Nocardia may also cause a variety of cutaneous infections such as actinomycetoma (especially Nocardia brasiliensis), lymphocutaneous disease, cellulitis and subcutaneous abscesses.

Nocardia isolation from biological specimens can be performed using agar medium enriched with yeast extract and activated charcoal (BCYE), the same utilized for Legionella spp. Selective media for Mycobacteria or fungi can also be inoculated. The most suitable specimens are the sputum or, when clinically necessary, bronchoalveolar lavage or biopsy. Further biochemical tests for species identification are not routinely performed. Serological or cutaneous tests are not available.


Antibiotic therapy with a sulfonamide, most commonly trimethoprim-sulfamethoxazole, is the treatment of choice.[2] People who take trimethoprim-sulfamethoxazole for other reasons, such as prevention of Pneumocystis jirovecii infection, appear to have fewer Nocardia infections,[3] although this protective effect has been considered unreliable[4] and some studies have disputed it altogether.[5] Minocycline is usually substituted when a sulfa cannot be given; high-dose imipenem and amikacin have also been used in severe or refractory cases.[2] Linezolid appears to be highly effective against Nocardia, but it is very expensive and may cause severe adverse effects.[6]

Antibiotic therapy is continued for six months (in immunocompetent people) to a year (in immunosuppression), and may need to be continued indefinitely.[2] Proper wound care is also critical.


Although Nocardia has interesting and important features such as production of antibiotics and aromatic compound-degrading or converting enzymes, the genetic study of this organism has been hampered by the lack of genetic tools. However, practical NocardiaE. coli shuttle vectors have been developed recently.[7]


  1. ^ Ryan KJ; Ray CG (editors) (2004). Sherris Medical Microbiology (4th ed.). McGraw Hill. pp. 460–2. ISBN 0838585299. 
  2. ^ a b c Bartlett JG (October 5, 2007). "Nocardia". Point-of-Care Information Technology ABX Guide. Johns Hopkins University.  Retrieved on January 3, 2009. Freely available with registration.
  3. ^ Muñoz P, Muñoz RM, Palomo J, Rodríguez-Creixéms M, Muñoz R, Bouza E (November 1997). "Pneumocystis carinii infection in heart transplant recipients. Efficacy of a weekend prophylaxis schedule". Medicine (Baltimore) 76 (6): 415–22. doi:10.1097/00005792-199711000-00004. PMID 9413427. 
  4. ^ Peleg AY, Husain S, Qureshi ZA, et al. (May 2007). "Risk factors, clinical characteristics, and outcome of Nocardia infection in organ transplant recipients: a matched case-control study". Clin Infect Dis 44 (10): 1307–14. doi:10.1086/514340. PMID 17443467. Lay summary – Doctor's Guide. 
  5. ^ Khan BA, Duncan M, Reynolds J, Wilkes DS (2008). "Nocardia infection in lung transplant recipients". Clin Transplant 22 (5): 562–6. doi:10.1111/j.1399-0012.2008.00824.x. PMID 18435787. 
  6. ^ Jodlowski TZ, Melnychuk I, Conry J (October 2007). "Linezolid for the treatment of Nocardia spp. infections". Ann Pharmacother 41 (10): 1694–9. doi:10.1345/aph.1K196. PMID 17785610. 
  7. ^ Chiba K, Hoshino Y, Ishino K, Kogure T, Mikami Y, Uehara Y, Ishikawa J (2007). "Construction of a Pair of Practical Nocardia-Escherichia coli Shuttle Vectors". Jpn J Infect Dis 60 (1): 45–7. PMID 17314425. 

Further reading

External links

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