Moisture and occlusion

In the past, the mainstay of wound management was to dry the wound bed with absorptive gauzes. A major breakthrough in the management of chronic wounds was the realization that a moist environment is critical for wound healing and occlusive dressings do not increase the risk of infection . Moist retentive wound dressings stimulate collagen synthesis, promote angiogenesis by creating a hypoxic environment, encourage re-epithelialization, and decrease pain. By serving as a barrier against external contamination and by lowering wound pH, occlusive dressings actually decrease wound infection rates .

Dressings should be changed based on their potential for absorbency and the amount of exudate, with attention to the delicate balance between overhydration and excessive dryness. For example, occlusive dressings applied to highly exudative wounds may cause maceration and erosion of the surrounding skin, possibly leading to further deterioration of the wound. In addition, chronic wound fluid can perpetuate cytokine and MMP production (see above), thereby affecting the function of fibroblasts and growth factors and contributing to chronicity. It is therefore important to protect the skin surrounding the wound bed with an ointment in order to preserve barrier integrity .

Debridement

Debridement consists of the removal of necrotic, non-viable, or infected tissue from the wound bed in order to promote healing. In a sense, debridement is an attempt to shift the wound from a chronic state (with a milieu characterized by an abnormal extracellular matrix, an excess of proteolytic enzymes, and senescent cells) into an acute state. Debridement can be surgical (sharp debridement), mechanical (wet-to-dry), autolytic, chemical (enzymatic), and biologic (maggot therapy) .

Sharp debridement with surgical instruments represents the most rapid method for debriding a wound and is most appropriate for large necrotic and/or infected wounds. It also enables the clinician to estimate the extent and severity of a wound. Although damage to viable tissue is possible, sharp debridement performed by a skilled physician is usually highly selective . Caution is advised in the case of arterial ulcers because of the potential risk for tissue desiccation and ulcer enlargement . Sharp debridement may be associated with bleeding and pain and may necessitate analgesia.

Wet-to-dry (mechanical) debridement consists of placing gauze moistened with saline over the wound, allowing the gauze to dry, and then removing the dry gauze along with adherent non-viable tissue. It is relatively fast and easy to perform, but is painful and does not discriminate between viable and non-viable tissue. It is indicated for wounds with large amounts of necrotic tissue.

Autolytic debridement is the process by which the body uses its own proteolytic enzymes and phagocytic cells to clear necrotic debris. The process is enhanced by moist retentive wound dressings and may require weeks to accomplish. Autolytic debridement is selective, painless, and suited primarily for wounds with minimal debris. It is contraindicated if the wound is infected .

Enzymatic (chemical) debridement utilizes topically applied proteolytic enzyme preparations such as papain–urea or collagenase to digest necrotic tissue, collagen, fibrin, and wound exudate. Chemical debridement is a gradual process. The papain–urea preparation contains papain, which is derived from the plant Carica papaya and is a non-selective cysteine protease. It is active over a broad pH range and is associated with an intense inflammatory response and digestion of viable tissue; local pain or a burning sensation is often described. Therefore, the product should be applied only to the wound bed and not to the surrounding intact skin. Collagenase preparations are derived from Clostridium histolyticum ; they specifically target native collagen and are active within a narrow pH range of 6 to 8. These preparations are highly selective and do not harm viable cells . Prior to application, it is advisable to cross-hatch the eschar, if present, in order to increase penetration .

For therapy-resistant, chronic ulcers with marked necrosis and slough, maggot debridement therapy can be considered. Essentially, it exploits the ability of maggots to decompose necrotic tissue (benign myasis), but the debridement is done in a controlled manner so as to avoid undesirable effects on healthy tissues . Degradation via proteinases that are in larval excretory/secretory products is thought to contribute to wound debridement . It is important to select larval strains that feed preferentially on necrotic tissue and to avoid applying too many larvae to a wound. The flies most often employed are facultative calliphorids, in particular the green bottle blowfly, Lucilia sericata .

Maggots are used to treat various types of chronic ulcers, including pressure ulcers, venous ulcers, and neurovascular diabetic ulcers, as well as traumatic and postsurgical wounds. In a multicenter, randomized, open study that compared the clinical effectiveness of larval therapy to a standard debridement technique (hydrogel) for “sloughy” or necrotic leg ulcers, larval therapy did not improve the rate of healing or reduce bacterial load, but it did significantly reduce the time to debridement and increase ulcer pain .

Novel approaches to wound debridement are currently under investigation, including both hydrosurgery and ultrasound- and radiofrequency-based techniques .

Wound dressings

The ideal wound dressing should: (1) provide a moist retentive environment; (2) absorb excess exudate without causing maceration of surrounding skin; (3) protect against bacteria; (4) leave no residual debris but cause no trauma when removed; (5) decrease odor; and (6) relieve pain. In addition, the ideal wound dressing should be cost-effective, easy to handle, and be neither irritating nor allergenic. Obviously, there is no single dressing that can fulfill all these criteria throughout the entire healing process. A vast array of dressings exists and the choice of a dressing depends upon the wound type and its characteristics at a given time ( Table 105.3 ) .

Management of wound infection

The presence of a microbial infection is always detrimental to wound healing. However, all chronic open wounds are colonized with bacteria and it is important, although often difficult, to distinguish true infection from bacterial colonization. Of note, colonization is defined by the presence of replicating bacteria and adherent microorganisms, but without evidence of tissue damage.

Critical colonization is a relatively new concept in which the bacterial burden within a chronic wound does not elicit the typical symptoms or signs of an infection, but does delay healing. The presence of ≥10 ⁶ colony-forming units of bacteria/gram of tissue predicts delayed wound healing and a high risk for developing an infection . More recent studies have demonstrated that in many chronic wounds, bacteria persist in the form of biofilms. The latter represent communities of bacteria, protected by an adhesive polymeric matrix cover, that communicate with each other via water channels. Through these communication channels, bacteria are able to regulate the transcription of genes and protein products in a manner that is beneficial to them, but which can delay healing (quorum sensing) . Biofilms are particularly resistant to antimicrobial therapy.

Wounds become clinically infected when host defenses are overwhelmed. Signs and symptoms of infection include an increased exudate, purulent discharge, pain, and surrounding erythema and swelling. However, sometimes an increase in ulcer size and malodorous or friable granulation tissue are the only clues to the presence of an active infection within a chronic wound. Systemic signs of infection such as fever, chills, tachycardia, and leukocytosis may suggest that the infection has progressed to a bacteremia or septicemia, although the former may be subtle in elderly patients, necessitating a high index of suspicion.

Most chronic wounds have a polymicrobial flora. Bacterial cultures usually grow aerobic Gram-positive cocci, which are often mixed with Gram-negative bacilli and sometimes anaerobes . Clinically infected wounds should be cultured and treated initially with broad-spectrum systemic antibiotics. The antibiotic regimen is then adjusted based on the results of sensitivity testing.

In properly treated, non-healing wounds that demonstrate critical colonization, topical antimicrobials should be considered. Topical antimicrobial agents are divided into two major categories: antiseptics and antibiotics. Antiseptics have a broad antimicrobial spectrum as well as multiple microbial targets, but they are often toxic to host tissues. Topical antibiotics have specific cellular targets and a narrower spectrum of activity; they are not toxic to human cells but are more likely to induce bacterial resistance. Commonly used topical antibiotics include bacitracin, neomycin, mupirocin, retapamulin, gentamicin, and fusidic acid. However, topical antibiotics can cause allergic contact dermatitis, in particular neomycin and bacitracin. It is also preferable to avoid topical antimicrobials that have a systemic counterpart .

Commonly used antiseptics include hydrogen peroxide, chlorhexidine, iodine-based preparations (e.g. povidone-iodine, cadexomer iodine), and silver-releasing agents. Hydrogen peroxide and povidone-iodine have a broad antimicrobial spectrum with minimal resistance but may be cytotoxic. Cadexomer iodine is a complex of 0.9% elemental iodine plus cadexomer microbeads which are composed of a modified starch-based polymer. Upon absorption of exudate, the cadexomer beads swell and slowly release iodine into the wound bed, thus maintaining non-toxic iodine concentrations .

Silver is an effective antiseptic agent with broad-spectrum activity, including against methicillin-resistant Staphylococcus aureus (MRSA), vancomycin-resistant enterococci (VRE), and extended-spectrum β-lactamase producers. Resistance has rarely been reported, primarily with Gram-negative species . Only the ionized form of silver (Ag ⁺ ) has antimicrobial properties, so exposure to wound fluid or exudate is required if the source is metallic silver . Silver ions kill bacteria by damaging bacterial cell walls and intracellular and nuclear membranes as well as denaturing bacterial DNA, RNA, and key enzymes (e.g. respiratory enzymes) . Silver may also promote cellular proliferation and re-epithelialization by inducing the production of metallothionein by epidermal cells. Metallothionein increases zinc- and copper-dependent enzymes required for cellular proliferation and matrix remodeling . Silver has been incorporated into various dressing products (e.g. gauzes, hydrocolloids, alginates, foams) in addition to creams, gels, and barrier protectants which differ in their solubility and the rate at which silver ions are released into the wound bed . Disadvantages of silver products include potential irritation, permanent blue–gray discoloration (localized argyria), and cost. Topical silver sulfadiazine has induced neutropenia in children which was reversible once the cream was discontinued .

Lastly, as chronic wounds may serve as a portal of entry for Clostridium tetani , it is recommended that the tetanus immune status of patients with chronic leg ulcers be assessed .

Adjuncts to wound care

Compression

Compression therapy is a mainstay in the treatment of venous insufficiency. Compression stockings improve venous return, reduce edema, stimulate healthier granulation tissue within venous ulcers , and improve quality of life . A Cochrane meta-analysis of 39 randomized controlled trials concluded that compression therapy increased ulcer healing rates when compared to no compression .

Elastic stockings, preferably with graduated compression, are available in a wide range of compressive pressures (15 to 60 mmHg), lengths, and materials ( Table 105.4 ). Lower levels of compression (20 to 30 mmHg) are sufficient for preventing mild edema, whereas higher levels of compression (30 to 40 mmHg) are required to control stasis dermatitis or lead to the healing of ulcers. Compression stockings also prevent the recurrence of venous ulcers once healed. Therefore, lifelong use of compression is recommended for patients with a history of venous ulcers . In addition to stockings, there are other forms of compression such as bandages and wraps, as outlined in Tables 105.5 and 105.6 . Of note, surgical correction of superficial venous reflux (plus compression) does not improve ulcer healing but does reduce the recurrence of ulcers .

Table 105.4

Classes of compression stockings.

Adapted from Phillips TJ. Current approaches to venous ulcers and compression. Dermatol Surg. 2001;27:611–21.

CLASSES OF COMPRESSION STOCKINGS
Class	Pressure at the ankle	Indication
I	20–30 mmHg	Simple varicose veins
		Mild edema
		Leg fatigue
II	30–40 mmHg	Moderate edema
		Severe varicosities
		Moderate venous insufficiency
III	40–50 mmHg	Severe edema
		Severe venous insufficiency
		Post-thrombotic lymphedema
IV	50–60 mmHg	Elephantiasis

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