Table 1.
Members of the microbiome have both beneficial and detrimental effects on cutaneous homeostasis, which dictates their role as a commensal microorganism or pathogen in uninjured skin or a wound microenvironment
| Bacteria | Good | Bad | Effects of Stress Mediators |
|---|---|---|---|
| Staphylococcus epidermidis | Stimulates keratinocyte production of host AMPs, such as hBD2 and hBD3, and produces its own AMPs, including PSMγ and PSMδ.10,18 | Causative agent of hospital-acquired infections associate with medical devices.3,53 | Glucocorticoids decrease the effects of super antigen activated T cells and inhibit staphylococcal exotoxin-induced T-cell proliferation, cytokine release.3 |
| Propionibacterium acnes | Fatty acids generated by lipase activities may slow/inhibit growth of other microorganisms.49,67 | Associated with pathogenesis of acne and a number of other opportunistic infections.67 | Cortisol and steroids significantly exacerbate inflammation associated with P. acnes via TLR2 stimulation.2,49 |
| Pseudomonas aeruginosa | Produces pseudomonic acid A, which kills staphylococcal and streptococcal pathogens.2 | Most common cause of chronic and acute burn wound infections.6 | Norepinephrine increases expression of the attachment factor PA-1 of P. aeruginosa and increases biofilm formation.2,7 |
| Accelerates epithelialization and neovascularization in acute wounds.6,36 | |||
| Staphylococcus aureus | Produces bacteriocins such as staphylococcin 462, which can inhibit growth of other. | Commonly associated with infectious skin conditions, such as folliculitis and abscesses. | Norepinephrine increases ability to steal iron from host and therefore increases ability to form biofilms.2,55 |
| S. aureus strains.67 | Produces superantigen toxins that can trigger staphylococcal toxic shock syndrome.67 | ||
| Corynebacterium jeikeium | Manganese acquisition inhibits Mg-dependent superoxide dismutase, which may function to prevent oxidative damage to epidermal tissue.68 | Causes infections in immune-compromised patients, in conjunction with underlying malignancies, on implanted medical devices and in skin-barrier defects.68 | Reduced expression of transcriptional regulators involved in C. jeikeium carbohydrate metabolism due to a less versatile sugar metabolism; variations in the number of metalloregulatory sensors such that pathogenic C. jeikeium predominantly import metal ions directly from host during hypoglycemic or ionic stress responses.2,68 |
| Group A Streptococcus | Surface-expressed streptokinase sequesters and activates host plasminogen in the epidermis, which leads to keratinocyte chemotaxis, suppression of cell proliferation, and potential re-epithelialization of wounds.68 | Associated with numerous infections, such as “strep throat,” impetigo, cellulitis, erysipelas, and necrotizing fasciitis.59 | Catecholamines enhance growth likely by increasing iron availability.2,68 |
Stress mediators can alter bacterial physiology and increase virulence. This shift from a nonpathogenic to a pathogenic state can result in delayed or stalled wound healing responses and infection.
AMP, antimicrobial peptide; hBD, human β-defensin; PSM, phenol-soluble modulin; TLRs, toll-like receptors.