Biology:Chromobacterium violaceum

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Short description: Species of bacterium

Chromobacterium violaceum
Chromobacterium violaceum blood agar.jpg
Blood agar plate culture of C. violaceum. Image from the CDC.
Scientific classification edit
Domain: Bacteria
Phylum: Pseudomonadota
Class: Betaproteobacteria
Order: Neisseriales
Family: Neisseriaceae
Genus: Chromobacterium
Species:
C. violaceum
Binomial name
Chromobacterium violaceum
(Bergonzini 1880)

Chromobacterium violaceum is a Gram-negative, facultative anaerobic, non-sporing coccobacillus. It is motile with the help of a single flagellum which is located at the pole of the coccobacillus. Usually, there are one or two more lateral flagella as well.[1] It is part of the normal flora of water and soil of tropical and sub-tropical regions of the world. It produces a natural antibiotic called violacein, which may be useful for the treatment of colon and other cancers.[2] It grows readily on nutrient agar, producing distinctive smooth low convex colonies with a characteristic striking dark violet metallic sheen (due to violacein production).[3] Some strains of the bacteria which do not produce this pigment have also been reported.[4] It has the ability to break down tarballs.[5]

Biochemistry

C. violaceum ferments glucose, trehalose, N-acetylglucosamine and gluconate but not L-arabinose, D-galactose, or D-maltose. It is positive for catalase and oxidase reactions.[1] Bacterial isolates in many cases can show high level resistance to a range of antibiotics.[6]

Medical significance

C. violaceum rarely infects humans, but when it does it causes skin lesions, sepsis, and liver abscesses that may be fatal.[7] The first reported case of Chromobacterium violaceum infection in humans in literature is from Malaysia in 1927.[1] Only 150 cases have been reported in literature since then.[8] To date, cases have been reported from Argentina, Australia, Brazil, Canada, Cuba, India, Japan, Nigeria, Singapore, Sri Lanka, Taiwan, United States and Vietnam. The most common mode of entry of the bacteria into the body is through the injured skin coming in contact with soil or water containing the bacteria.[1][9] The disease usually starts as a limited infection of the skin at the point of entry of the bacteria, which progresses to necrotizing metastatic lesions, then multiple abscesses of the liver, lung, spleen, skin, lymph nodes or brain, leading to severe septicaemia, culminating in multiorgan failure which may be fatal.[10] Other reported pathologies include chronic granulomatosis, osteomyelitis, cellulitis, diarrhoea, septic spondylitis, conjunctivitis, periorbital and ocular infection.[1][11][12][13][14] Care must be taken because Burkholderia pseudomallei is commonly misidentified as C. violaceum by many common identification methods.[15][16] The two are readily distinguished because B. pseudomallei produces large wrinkled colonies, whereas C. violaceum produces a distinctive violet pigment.

C. violaceum produces a number of natural antibiotics:

  • Aztreonam is a monobactam antibiotic that is active against gram-negative aerobic bacteria including Pseudomonas aeruginosa. It is marketed as Azactam.
  • Violacein is active against amoebae and trypanosomes;
  • Aerocyanidine is active against Gram-positive organisms;
  • Aerocavin is active against Gram-positive and Gram-negative organisms.

It has been described as a cause of infection in gibbons.[17]

Treatment

Infection caused by C. violaceum is rare, therefore there are no clinical trials evaluating different treatments. Antibiotics that have been used to successfully treat C. violaceum include pefloxacin,[4] ciprofloxacin, amikacin,[1] and co-trimoxazole.[18] Other antibiotics that appear to be effective in vitro include chloramphenicol and tetracycline.[19] For theoretical reasons, infection would not be expected to respond to penicillins, cephalosporins, or aztreonam, although carbapenems like meropenem or imipenem may possibly work.[20] Though the bacteria is reported to be resistant to first generation cephalosporins, susceptibility to the newer cephalosporins is variable.[21]

Genome

The complete genome was sequenced and the results were published in 2003. C. violaceum type strain ATCC 12472 was found to have 4,751,080 base pairs with a G + C content of 64.83% and 4,431 ORFs.[3]

References

  1. 1.0 1.1 1.2 1.3 1.4 1.5 Ray, P; Sharma, J; Marak, SK; Singhi, S; Taneja, N; Garg, RK (2004). "Chromobacterium violaceum septicaemia from North India". Indian J Med Res 120 (6): 523–6. PMID 15654137. 
  2. Kodach, LL; Bos, CL; Durán, N; Peppelenbosch, MP; Ferreira, CV; Hardwick, JC (2006). "Violacein synergistically increases 5-fluorouracil cytotoxicity, induces apoptosis and inhibits Akt-mediated signal transduction in human colorectal cancer cells". Carcinogenesis 27 (3): 508–16. doi:10.1093/carcin/bgi307. PMID 16344270. 
  3. 3.0 3.1 Brazilian National Genome Project Consortium (2003). "The complete genome sequence of Chromobacterium violaceum reveals remarkable and exploitable bacterial adaptability". Proc Natl Acad Sci USA 100 (20): 11660–5. doi:10.1073/pnas.1832124100. PMID 14500782. Bibcode2003PNAS..10011660.. 
  4. 4.0 4.1 Lee, J; Kim, JS; Nahm, CH; Choi, JW; Kim, J; Pai, SH; Moon, KH; Lee, K et al. (1999). "Two Cases of Chromobacterium violaceum Infection after Injury in a Subtropical Region". J Clin Microbiol 37 (6): 2068–2070. doi:10.1128/JCM.37.6.2068-2070.1999. PMID 10325383. 
  5. Itah, A. Y.; Essien, J. P. (2005). "Growth Profile and Hydrocarbonoclastic Potential of Microorganisms Isolated from Tarballs in the Bight of Bonny, Nigeria". World Journal of Microbiology and Biotechnology 21 (6–7): 1317–22. doi:10.1007/s11274-004-6694-z. 
  6. "Chromobacterium violaceum in siblings, Brazil". Emerging Infect. Dis. 11 (9): 1443–5. 2005. doi:10.3201/eid1109.050278. PMID 16229777. 
  7. Sneath, PH; Whelan, JP; Bhagwan Singh, R; Edwards, D (1953). "Fatal infection by Chromobacterium violaceum". Lancet 265 (6780): 276–7. doi:10.1016/S0140-6736(53)91132-5. PMID 13085740. 
  8. M Ravish Kumar. (2012). "Chromobacterium violaceum: A rare bacterium isolated from a wound over the scalp". Int J Appl Basic Med Res 2 (1): 70–2. doi:10.4103/2229-516X.96814. PMID 23776815. 
  9. Duran, N; Menck, FM (2001). "Chromobacterium violaceum: A review of pharmacological and industrial perspectives.". Crit Rev Microbiol 27 (3): 201–22. doi:10.1080/20014091096747. PMID 11596879. 
  10. Slesak, G et al. (2009). "Fatal Chromobacterium violaceum septicaemia in northern Laos, a modified oxidase test and post-mortem forensic family G6PD analysis". Ann Clin Microbiol Antimicrob 8: 24. doi:10.1186/1476-0711-8-24. PMID 19640274. 
  11. Dutta, S; Dutta, SK (2003). "Multidrug resistant chromobacterium violaceum: An unusual bacterium causing long standing wound abscess". Indian J Med Microbiol 21 (3): 217–8. doi:10.1016/S0255-0857(21)03082-6. PMID 17643028. http://www.ijmm.org/text.asp?2003/21/3/217/8025. Retrieved 6 March 2015. 
  12. Chou, YL; Yang ., PY; Huang, CC; Leu, HS; Tsao, TC (2000). "Fatal and non-fatal chromobacterial septicemia: report of two cases". Chang Gung Med J. 23 (8): 492–7. PMID 11039252. 
  13. Shao, PL; Hsueh, PR; Chang, YC; Lu, CY; Lee, PY; Lee, CY; Huang, LM (2002). "Chromobacterium violaceum infection in children: a case of fatal septicemia with nasopharyngeal abscess and literature review". Pediatr Infect Dis J 21 (7): 707–9. doi:10.1097/00006454-200207000-00022. PMID 12237610. 
  14. Chen, CH; Lin, LC; Liu, CE; Young, TG (2003). "Chromobacterium violaceum bacteremia: a case report". J Microbiol Immunol Infect. 36 (2): 141–4. PMID 12886967. 
  15. Inglis, TJ; Chiang, D; Lee, GS; Chor-Kiang, L (1998). "Potential misidentification of Burkholderia pseudomallei by API 20NE". Pathology 30 (1): 62–64. doi:10.1080/00313029800169685. PMID 9534210. 
  16. Lowe, P; Engler, C; Norton, R (2002). "Comparison of Automated and Nonautomated Systems for Identification of Burkholderia pseudomallei". J Clin Microbiol 40 (12): 4625–7. doi:10.1128/JCM.40.12.4625-4627.2002. PMID 12454163. 
  17. Groves, MG; Strauss, JM; Abbas, J; Davis, CE (1969). "Natural infections of gibbons with a bacterium producing violet pigment (Chromobacterium violaceum)". J Infect Dis 120 (5): 605–610. doi:10.1093/infdis/120.5.605. PMID 5388196. 
  18. Moore, C; Lane, J; Stephens, J (2001). "Successful treatment of an infant with Chromobacterium violaceum sepsis". Clin Infect Dis 32 (6): E107–10. doi:10.1086/319356. PMID 11247733. 
  19. Martinez, R; Velludo, MA; Santos, VR; Dinamarco, PV (2000). "Chromobacterium violaceum infection in Brazil. A case report". Rev Inst Med Trop Sao Paulo 42 (2): 111–3. doi:10.1590/s0036-46652000000200008. PMID 10810326. 
  20. Midani, S; Rathore, M (1998). "Chromobacterium violaceum infection". South Med J 91 (5): 464–466. doi:10.1097/00007611-199805000-00011. PMID 9598856. 
  21. Howard, AJ; Ison, CA (1996). "Haemophilus, Gardnerella and other bacilli". in Collee, JG; Fraser, AG; Marmion, BP et al. (in en). Mackie and McCartney Practical Medical Microbiology (14th ed.). New York: Churchill Livingstone. pp. 329–41. 

External links

Wikidata ☰ Q3498295 entry



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