The clinical impact of bacterial biofilms.
- Author:
Niels HØIBY
1
;
Oana CIOFU
;
Helle Krogh JOHANSEN
;
Zhi-jun SONG
;
Claus MOSER
;
Peter Østrup JENSEN
;
Søren MOLIN
;
Michael GIVSKOV
;
Tim TOLKER-NIELSEN
;
Thomas BJARNSHOLT
Author Information
- Publication Type:Journal Article
- MeSH: Animals; Antibiotic Prophylaxis; Biofilms; drug effects; growth & development; Chronic Disease; Cystic Fibrosis; microbiology; Drug Resistance, Microbial; physiology; Foreign Bodies; microbiology; Humans; Microbial Consortia; drug effects; genetics; immunology; Phagocytosis; Pseudomonas Infections; microbiology; Pseudomonas aeruginosa; drug effects; genetics; physiology; Quorum Sensing; drug effects; genetics
- From: International Journal of Oral Science 2011;3(2):55-65
- CountryChina
- Language:English
- Abstract: Bacteria survive in nature by forming biofilms on surfaces and probably most, if not all, bacteria (and fungi) are capable of forming biofilms. A biofilm is a structured consortium of bacteria embedded in a self-produced polymer matrix consisting of polysaccharide, protein and extracellular DNA. Bacterial biofilms are resistant to antibiotics, disinfectant chemicals and to phagocytosis and other components of the innate and adaptive inflammatory defense system of the body. It is known, for example, that persistence of staphylococcal infections related to foreign bodies is due to biofilm formation. Likewise, chronic Pseudomonas aeruginosa lung infections in cystic fibrosis patients are caused by biofilm growing mucoid strains. Gradients of nutrients and oxygen exist from the top to the bottom of biofilms and the bacterial cells located in nutrient poor areas have decreased metabolic activity and increased doubling times. These more or less dormant cells are therefore responsible for some of the tolerance to antibiotics. Biofilm growth is associated with an increased level of mutations. Bacteria in biofilms communicate by means of molecules, which activates certain genes responsible for production of virulence factors and, to some extent, biofilm structure. This phenomenon is called quorum sensing and depends upon the concentration of the quorum sensing molecules in a certain niche, which depends on the number of the bacteria. Biofilms can be prevented by antibiotic prophylaxis or early aggressive antibiotic therapy and they can be treated by chronic suppressive antibiotic therapy. Promising strategies may include the use of compounds which can dissolve the biofilm matrix and quorum sensing inhibitors, which increases biofilm susceptibility to antibiotics and phagocytosis.
