Diabetic foot medical therapy: Difference between revisions

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Revision as of 03:58, 4 June 2014

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Alonso Alvarado, M.D. [2]

Overview

Appropriate wound care is essential for the management of all diabetic foot ulcers. Uninfected diabetic ulcers do not require antibiotic therapy. For acutely infected wounds, empiric antibiotic with efficacy against Gram-positive cocci should be initiated after obtaining a post-debridement specimen for aerobic and anaerobic culture. Infections with antibiotic-resistant organisms and those that are chronic, previously treated, or severe usually require broader spectrum regimens.

Diabetic Foot Infection

Principles of Therapy Adapted from Diabetes Care. 2013;36(9):2862-71.^[1] and Clin Infect Dis. 2012;54(12):e132-73.^[2]

Diagnosis of Diabetic Foot Infection

Diabetic foot infection (DFI) is diagnosed clinically by the presence of at least two signs or symptoms of inflammation:

Local swelling or induration
Erythema
Local tenderness or pain
Local warmth
Purulent discharge (thick, opaque to white or sanguineous secretion)

Indications for Hospitalization

Hospitalization is appropriate for the following conditions:

Severe (grade 4) infections
Moderate (grade 3) infections with complicating features

Severe peripheral arterial disease or limb ischemia
Lack of home support

Patients unable to comply with the required outpatient treatment regimen for psychological or social reasons
Patients not responding to outpatient treatment

Obtaining Specimens

Properly obtained specimens for culture prior to initiating empiric therapy provide useful information for guiding antibiotic selection, particularly in those with chronic or previously treated infections which are commonly caused by Gram-negative bacilli or obligate anaerobic organisms.

Infected wounds should be cultured by obtaining tissue samples during any surgical procedure or by tissue biopsy or wound base curettage.
Bone cultures are optimal for detecting the pathogen in osteomyelitis, but blood cultures are only necessary for those with a severe (grade 4) infection.
Cultures may be unnecessary for mild infections in patients who have not recently received antibiotic therapy and who are at low risk for methicillin-resistant Staphylococcus aureus (MRSA) infection; these infections are predictably caused solely by staphylococci and streptococci.
Cultures may yield organisms that are commonly considered to be contaminants (eg, coagulase-negative staphylococci, corynebacteria), but these may be true pathogens in DFIs and are often resistant to the empiric antibiotics.

Consultation

Conditions to request consultation from specialists:

Urgent surgical intervention should be sought for DFIs accompanied by gas in the deeper tissues, an abscess, or necrotizing fasciitis, and less urgent surgery for DFIs with substantial nonviable tissue or extensive bone or joint involvement.
Consult a vascular surgeon to consider revascularization if ischemia complicates a DFI.
Infectious diseases specialists should be consulted when cultures yield multiple or antibiotic-resistant organisms, the patient has substantial renal impairment, or the infection does not respond to appropriate medical or surgical therapy in a timely manner.

Adjunctive Therapy

No adjunctive therapy has been proven to improve resolution of infection, but for selected diabetic foot wounds that are slow to heal, clinicians might consider using bioengineered skin equivalents, growth factors, granulocyte colony-stimulating factors, hyperbaric oxygen therapy, or negative pressure wound therapy.

Selection of Antibiotic Regimen

Clinically uninfected wounds should not be treated with antibiotic therapy. For all infected wounds, antibiotic therapy combined with appropriate wound care is recommended.

For clinically infected wounds, consider the questions below:

1. Is there high risk of MRSA?

Methicillin-resistant Staphylococcus auerus (MRSA) coverage should be considered in the following conditions:

Prior history of MRSA infection or colonization within the past year
High local prevalence of MRSA infection or colonization (50% for a mild and 30% for a moderate soft tissue infection)
Clinically severe diabetic foot infection

2. Is the infected wound chronic or treated with antibiotics in the past month?

If so, include agents active against aerobic gram-negative bacilli in regimen.
If not, agents targeted against just aerobic Gram-positive cocci may be sufficient.

Aerobic gram-negative bacilli are frequently copathogens in infections that are chronic or follow antibiotic treatment
Obligate anaerobes may be copathogens in ischemic or necrotic wounds.

3. Are there risk factors for infection with Pseudomonas aeruginosa or extended-spectrum β-lactamase (ESBL)–producing organisms?

Anti-pseudomonal agent is usually unnecessary except for patients with risk factors:

High local prevalence of Pseudomonas aeruginosa infection
Frequent exposure of the foot to water
Warm climate

Coverage of ESBL-producing gram-negative organisms should be considered in countries in which they are relatively common.

4. What is the severity status?

DFI is classified based on its severity according to the Infectious Diseases Society of America (IDSA) guideline or the PEDIS grade developed by International Working Group on the Diabetic Foot (IWGDF). (see Table below)
Selection of empiric antimicrobial regimen should be determined by the severity of DFI and the likely etiologic agents.

Mild (grade 2) to moderate (grade 3) DFI without recent antibiotic treatment:

Highly bioavailable oral antibiotics against aerobic Gram-positive cocci may be sufficient.

Severe (grade 4) DFI:

Broad-spectrum antibiotics are recommended while culture results and susceptibility data are pending.

Clinical Manifestation	PEDIS Grade	IDSA Severity
No symptoms or signs of infection	1	Uninfected
Local infection involving only the skin and the subcutaneous tissue without involvement of deeper tissues and without signs of SIRS If erythema, must be >0.5 cm to ≤2 cm around the ulcer. Exclude other causes of an inflammatory response of the skin (eg, trauma, gout, acute Charcot neuro-osteoarthropathy, fracture, thrombosis, venous stasis).	2	Mild
Local infection with erythema >2 cm or involving structures deeper than skin and subcutaneous tissues (eg, abscess, osteomyelitis, septic arthritis, fasciitis) without signs of SIRS	3	Moderate
Local infection with the signs of SIRS, as manifested by ≥2 of the following: Temperature >38 °C or <36 °C Heart rate >90 beats/min Respiratory rate >20 breaths/min or PaCO2 <32 mm Hg White blood cell count >12,000 or <4,000 cells/μL or ≥10% immature (band) forms	4	Severe

5. What is the appropriate route, setting, and duration of antibiotic therapy?

The table below describes the recommended route, setting, and duration of antibiotic therapy based on the extent and severity of DFI.

Site of Infection, by Severity or Extent		Route of Administration	Setting	Duration of Therapy
Soft-tissue only	Mild (Grade 2)	Oral (or topical for superficial infections)	Outpatient	1–2 wk
	Moderate (Grade 3)	Oral (or initial parenteral)	Outpatient (or inpatient)	1–3 wk
	Severe (Grade 4)	Initial parenteral, switch to oral when possible	Inpatient, then outpatient	2–4 wk
Bone or joint	No residual infected tissue	Parenteral or oral	Inpatient, then outpatient	2–5 d
	Residual infected soft tissue	Parenteral or oral	Inpatient, then outpatient	1–3 wk
	Residual infected, viable bone	Initial parenteral, switch to oral when possible	Inpatient, then outpatient	4–6 wk
	Residual dead bone or no surgery	Initial parenteral, switch to oral when possible	Inpatient, then outpatient	≥3 mo

Empiric Therapy

▸ Click on the following categories to expand treatment regimens.

Uninfected (Grade 1)

▸ No Evidence of Infection

Mild (Grade 2)

▸ Acute Infection Without Recent Antibiotic Use

▸ High Risk for MRSA

Moderate to Severe (Grade 3–4)

▸ Chronic Infection or Recent Antibiotic Use