Diferencia entre revisiones de «Necrotizing fasciitis»

Revisión actual - 09:55 22 mar 2026

Background

Rapidly progressive, life-threatening infection involving fascia and subcutaneous tissue
Mortality: 20-40% even with treatment; increases with delayed diagnosis^[1]
Early surgical exploration and debridement are the most important prognostic factors
Gas formation is NOT required for diagnosis; absence of gas on imaging does NOT rule out NF^[2]

Types

Type I (Polymicrobial): mixed aerobic/anaerobic organisms; most common overall
- Typically in diabetics, immunocompromised, post-surgical patients
- Abdominal wall, perineum (Fournier gangrene)
Type II (Monomicrobial): Group A Streptococcus (most common) or Staphylococcus aureus
- Can occur in young, healthy patients
- Extremities most common site
Type III (Gas gangrene): Clostridium perfringens (myonecrosis)
- Extremely rapid progression; crepitus common
Type IV: Fungal (immunocompromised, trauma)

Risk Factors

Diabetes (most common comorbidity), IV drug use, obesity
Immunosuppression (HIV, malignancy, chronic steroids)
Recent surgery or traumatic wounds
Peripheral vascular disease, chronic renal failure, cirrhosis
NSAIDs (may mask early symptoms and promote GAS virulence)

Clinical Features

Pain out of proportion to exam (most important early clinical clue)
- However: some patients present with "la belle indifference" (painless) — ischemic insensate tissue^[3]
Erythema without sharp margins (unlike erysipelas)
Rapidly progressive swelling and induration
Hemorrhagic bullae (violaceous/dusky bullae)
Skin anesthesia (destruction of superficial cutaneous nerves — late but specific)
Crepitus (type I infections; absent in many cases)
Skip lesions (areas of normal-appearing skin between involved areas)
Lymphangitis and lymphadenopathy are ABSENT (fascia lacks lymphatic drainage)^[4]
Systemic toxicity: fever, tachycardia, shock, DIC

Differential Diagnosis

Cellulitis (most common misdiagnosis — cellulitis improves with antibiotics; NF does not)
DVT
Compartment syndrome
Pyomyositis
Gas gangrene without fasciitis
Erysipelas

Template:Skin and soft tissue infection DDX

Evaluation

Labs

CBC: leukocytosis (or leukopenia in severe sepsis)
BMP: creatinine (AKI), sodium <135 (associated with NF)
CRP: >150 mg/L
Lactate: elevated (tissue ischemia)
CK: may be elevated (myonecrosis)
Blood cultures, wound cultures
Coagulation studies (DIC screening)

LRINEC Score^[5]

Has NOT been prospectively validated
Score ≥6: PPV 92% for NF
10% of patients with score <6 still had NF — low score does NOT rule out NF
CRP ≥150 (+4), WBC 15-25 (+1) / >25 (+2), Hgb 11-13.5 (+1) / <11 (+2), Na <135 (+2), Cr >1.6 (+2), Glucose >180 (+1)

HUCLA Criteria^[6]

WBC >15.4 OR Na <135: associated with NF
PPV 26%, NPV 99% — useful to rule out NF, not confirm it

Imaging

Should NOT delay surgical exploration if clinical suspicion is high
CT (study of choice if imaging obtained): soft tissue gas, fascial thickening, fluid collections, fat stranding
MRI: T2 fascial/subcutaneous edema (very sensitive but time-consuming)
Bedside US: thickened fascia, subcutaneous fluid, subcutaneous emphysema; limited by gas artifact^[7]
Absence of gas on imaging does NOT exclude NF

Definitive Diagnosis

Surgical exploration is the ONLY way to definitively diagnose NF
Findings: grayish necrotic fascia, lack of tissue resistance to blunt dissection, "dishwater" pus, thrombosed vessels

Management

Surgical

Emergent surgical exploration and debridement — the single most important intervention
Indicated if: severe pain, systemic toxicity, elevated CK, clinical suspicion with or without imaging findings
Repeat debridement (planned "second look") typically at 24-48 hours
Average: 3-4 debridements before wound management
Delay in surgery increases mortality by approximately 9x

Antibiotics

Must cover gram-positives (including MRSA), gram-negatives, AND anaerobes
Empiric regimen:
- Piperacillin-tazobactam 4.5g IV q6h (or meropenem 1g IV q8h)
- + Vancomycin 25-30 mg/kg IV loading dose (or linezolid 600 mg IV q12h) — MRSA coverage
- + Clindamycin 900 mg IV q8h — suppresses toxin production (especially GAS exotoxins)^[8]
Clindamycin should be included in all regimens regardless of other antibiotics

Supportive Care

Aggressive IV fluid resuscitation
Vasopressors for septic shock
Serial lactate monitoring
Blood products for DIC
ICU admission

IVIG

Consider for streptococcal toxic shock syndrome associated with NF (controversial)

Disposition

ICU admission for all patients
Surgery consult in ED for any suspected case
Serial debridements as needed
Wound management: VAC therapy, skin grafting after infection controlled

Calculators

LRINEC Score

LRINEC Score — Necrotizing Soft Tissue Infection
Lab Value	Select
CRP (mg/L)	1 <150 (0) ≥150 (+4)
WBC (×10³/μL)	1 <15 (0) 15–25 (+1) >25 (+2)
Hemoglobin (g/dL)	1 >13.5 (0) 11–13.5 (+1) <11 (+2)
Sodium (mEq/L)	1 ≥135 (0) <135 (+2)
Creatinine (mg/dL)	1 ≤1.6 (0) >1.6 (+2)
Glucose (mg/dL)	1 ≤180 (0) >180 (+1)
LRINEC Score	/ 13

Interpretation
<6	Low risk — <50% probability of necrotizing fasciitis. Consider other diagnoses but maintain clinical suspicion.
6–7	Moderate risk — 50–75% probability. Consider surgical consultation and advanced imaging.
≥8	High risk — >75% probability of necrotizing fasciitis. Urgent surgical consultation for exploration.

References
Wong CH, Khin LW, Heng KS, et al. The LRINEC (Laboratory Risk Indicator for Necrotizing Fasciitis) score: a tool for distinguishing necrotizing fasciitis from other soft tissue infections. Crit Care Med. 2004;32(7):1535-1541. PMID 15241098. Caution: LRINEC has limited sensitivity (~80%). A low score does NOT rule out necrotizing fasciitis. Clinical suspicion should always guide management.

Template:LRINEC Score Calculator

References

↑ Hakkarainen TW et al. Necrotizing soft tissue infections: review and current concepts. Curr Probl Surg. 2014;51(8):344-72. PMID 25069713
↑ Misiakos EP et al. Current concepts in the management of necrotizing fasciitis. Front Surg. 2014;1:36. PMID 25593960
↑ TheHealthScience. Emergent Management of Necrotizing Soft Tissue Skin Infections. 2013.
↑ Seal DV. Necrotizing fasciitis. Curr Opin Infect Dis. 2001;14(2):127-32. PMID 11979122
↑ Wong CH, et al. The LRINEC score: a tool for distinguishing necrotizing fasciitis from other soft tissue infections. Crit Care Med. 2004;32(7):1535-1541. PMID 15241098
↑ Wall DB et al. A simple model to help distinguish NF from non-NF soft tissue infection. J Am Coll Surg. 2000;191(3):227-31. PMID 10989895
↑ Core Ultrasound: Soft Tissue. https://www.coreultrasound.com/sti/
↑ Stevens DL, et al. Practice guidelines for the diagnosis and management of SSTI: 2014 update by IDSA. Clin Infect Dis. 2014;59(2):e10-e52. PMID 24973422

Golger A, et al. Mortality in patients with necrotizing fasciitis. Plast Reconstr Surg. 2007;119(6):1803-7. PMID 17440360
Puvanendran R et al. Necrotizing fasciitis. Can Fam Physician. 2009;55(10):981-987. PMID 19826154
Anaya DA, Dellinger EP. Necrotizing soft-tissue infection: diagnosis and management. Clin Infect Dis. 2007;44(5):705-710. PMID 17278065

Authors:

[1] Hakkarainen TW et al. Necrotizing soft tissue infections: review and current concepts. Curr Probl Surg. 2014;51(8):344-72. PMID 25069713

[2] Misiakos EP et al. Current concepts in the management of necrotizing fasciitis. Front Surg. 2014;1:36. PMID 25593960

[3] TheHealthScience. Emergent Management of Necrotizing Soft Tissue Skin Infections. 2013.

[4] Seal DV. Necrotizing fasciitis. Curr Opin Infect Dis. 2001;14(2):127-32. PMID 11979122

[5] Wong CH, et al. The LRINEC score: a tool for distinguishing necrotizing fasciitis from other soft tissue infections. Crit Care Med. 2004;32(7):1535-1541. PMID 15241098

[6] Wall DB et al. A simple model to help distinguish NF from non-NF soft tissue infection. J Am Coll Surg. 2000;191(3):227-31. PMID 10989895

[7] Core Ultrasound: Soft Tissue. https://www.coreultrasound.com/sti/

[8] Stevens DL, et al. Practice guidelines for the diagnosis and management of SSTI: 2014 update by IDSA. Clin Infect Dis. 2014;59(2):e10-e52. PMID 24973422

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@@ Línea 1: / Línea 1: @@
 ==Background==
-*A rare, rapidly progressive infection primarily involving the fascia and subcutaneous tissue
+*'''Rapidly progressive, life-threatening infection''' involving fascia and subcutaneous tissue
-*Most severe form of soft tissue infection and potentially limb and life threatening
+*Mortality: 20-40% even with treatment; increases with delayed diagnosis<ref>Hakkarainen TW et al. Necrotizing soft tissue infections: review and current concepts. ''Curr Probl Surg''. 2014;51(8):344-72. PMID 25069713</ref>
-*Early recognition and aggressive debridement are major prognostic determinants and delay increases mortality<ref>Wong CH, Khin LW, Heng KS, Tan KC, Low CO (2004). "The LRINEC Laboratory Rother soft tissue infections". Critical Care Medicine 32 (7): 1535–1541. doi:10.1097/01.CCM.0000129486.35458.7D. PMID 15241098</ref>
+*Early surgical exploration and debridement are the most important prognostic factors
+*Gas formation is NOT required for diagnosis; absence of gas on imaging does NOT rule out NF<ref>Misiakos EP et al. Current concepts in the management of necrotizing fasciitis. ''Front Surg''. 2014;1:36. PMID 25593960</ref>
+===Types===
+*Type I (Polymicrobial): mixed aerobic/anaerobic organisms; most common overall
+**Typically in diabetics, immunocompromised, post-surgical patients
+**Abdominal wall, perineum ([[Fournier gangrene]])
+*Type II (Monomicrobial): Group A Streptococcus (most common) or ''Staphylococcus aureus''
+**Can occur in young, healthy patients
+**Extremities most common site
+*Type III (Gas gangrene): ''Clostridium perfringens'' (myonecrosis)
+**Extremely rapid progression; crepitus common
+*Type IV: Fungal (immunocompromised, trauma)
 ===Risk Factors===
-*[[DM]]
+*[[Diabetes]] (most common comorbidity), IV drug use, obesity
-*Drug use
+*Immunosuppression ([[HIV]], malignancy, chronic steroids)
-*Obesity
+*Recent surgery or traumatic wounds
-*Immunosuppression
+*Peripheral vascular disease, chronic [[renal failure]], [[cirrhosis]]
-*Recent surgery
+*NSAIDs (may mask early symptoms and promote GAS virulence)
-*Traumatic wounds
 ==Clinical Features==
-[[File:NectrotizingFasciitis.jpeg|thumbnail|Nectrotizing fasciitis]]
+*Pain out of proportion to exam (most important early clinical clue)
-*Skin exam
+**However: some patients present with "la belle indifference" (painless) — ischemic insensate tissue<ref>TheHealthScience. Emergent Management of Necrotizing Soft Tissue Skin Infections. 2013.</ref>
-**Erythema (without sharp margins)
+*Erythema without sharp margins (unlike [[erysipelas]])
-**Exquisitely tender (pain out of proportion to exam)
+*Rapidly progressive swelling and induration
-**Skip lesions
+*Hemorrhagic bullae (violaceous/dusky bullae)
-**Hemorrhagic bullae (violaceous bullae)
+*Skin anesthesia (destruction of superficial cutaneous nerves — late but specific)
-***May be preceded by skin anesthesia (destruction of superficial nerves)
+*Crepitus (type I infections; absent in many cases)
-**Crepitus (in type I infections)
+*Skip lesions (areas of normal-appearing skin between involved areas)
-*Swelling/edema may produce compartment syndrome
+*Lymphangitis and lymphadenopathy are ABSENT (fascia lacks lymphatic drainage)<ref>Seal DV. Necrotizing fasciitis. ''Curr Opin Infect Dis''. 2001;14(2):127-32. PMID 11979122</ref>
-*Constitutional
+*Systemic toxicity: fever, tachycardia, [[shock]], [[DIC]]
-**Fever
-**Tachycardia
-**Systemic toxicity
 ==Differential Diagnosis==
-{{Template:SSTI DDX}}
+*[[Cellulitis]] (most common misdiagnosis — cellulitis improves with antibiotics; NF does not)
+*[[DVT]]
+*[[Compartment syndrome]]
+*Pyomyositis
+*Gas gangrene without fasciitis
+*[[Erysipelas]]
+{{Skin and soft tissue infection DDX}}
-==Diagnosis==
+==Evaluation==
-===Work-Up===
+===Labs===
-*CBC
+*CBC: leukocytosis (or leukopenia in severe sepsis)
-*Chem
+*BMP: creatinine (AKI), sodium <135 (associated with NF)
-*PT/PTT/INR
+*CRP: >150 mg/L
-*CK
+*Lactate: elevated (tissue ischemia)
-*Lactate
+*CK: may be elevated (myonecrosis)
+*Blood cultures, wound cultures
+*Coagulation studies (DIC screening)
-===Evaluation===
+===LRINEC Score<ref>Wong CH, et al. The LRINEC score: a tool for distinguishing necrotizing fasciitis from other soft tissue infections. ''Crit Care Med''. 2004;32(7):1535-1541. PMID 15241098</ref>===
-[[File:CTNecrotizingFasciitis.png|thumbnail|CT of necrotizing fasciitis]]
+*Has NOT been prospectively validated
-*Surgical exploration is the ONLY way to definitively establish the diagnosis of necrotizing infection
+*Score ≥6: PPV 92% for NF
-*Imaging
+*10% of patients with score <6 still had NF — low score does NOT rule out NF
-**Should not delay surgical exploration
+*CRP ≥150 (+4), WBC 15-25 (+1) / >25 (+2), Hgb 11-13.5 (+1) / <11 (+2), Na <135 (+2), Cr >1.6 (+2), Glucose >180 (+1)
-**CT is study of choice
-===HUCLA NF vs Non-NF Criteria (Wall et al)===
+===HUCLA Criteria<ref>Wall DB et al. A simple model to help distinguish NF from non-NF soft tissue infection. ''J Am Coll Surg''. 2000;191(3):227-31. PMID 10989895</ref>===
-*Retrospective study discovered:<ref>Wall DB et al. A simple model to help distinguish necrotizing fasciitis from nonnecrotizing soft tissue infection. J Am Coll Surg. 2000 Sep;191(3):227-31.</ref>
+*WBC >15.4 OR Na <135: associated with NF
-**'''WBC count''' '''>15.4'''(x10<sup>3</sup>/mm<sup>3</sup>) OR '''Na''' '''<135'''(mmol/L)
+*PPV 26%, NPV 99% — useful to rule out NF, not confirm it
-**Associated with NF and combo of both increased likelihood of NF
-**PPV 26%/NPV 99%
-*Useful tool to rule out NF, not a good tool for confirming presence of NF
-**Helps distinguish NF from non-NF infection, when classic 'hard' signs of NF are absent however clinical judgment should still be used in patient with high suspicion of the disease
-===[[EBQ:LRINEC Score|Laboratory Risk Indicator for Necrotizing Fasciitis (LRINEC) Score (Wong et al)]]===
+===Imaging===
-{{LRINEC SCORE}}
+*Should NOT delay surgical exploration if clinical suspicion is high
+*CT (study of choice if imaging obtained): soft tissue gas, fascial thickening, fluid collections, fat stranding
+*MRI: T2 fascial/subcutaneous edema (very sensitive but time-consuming)
+*Bedside US: thickened fascia, subcutaneous fluid, subcutaneous emphysema; limited by gas artifact<ref>Core Ultrasound: Soft Tissue. https://www.coreultrasound.com/sti/</ref>
+*Absence of gas on imaging does NOT exclude NF
+===Definitive Diagnosis===
+*Surgical exploration is the ONLY way to definitively diagnose NF
+*Findings: grayish necrotic fascia, lack of tissue resistance to blunt dissection, "dishwater" pus, thrombosed vessels
 ==Management==
-#Surgical exploration and debridement is both the definitive diagnostic modality and the definitive treatment
+===Surgical===
-#*Indicated in setting of severe pain, toxicity, fever, elevated CK (with or without radiographic evidence)
+*Emergent surgical exploration and debridement — the single most important intervention
-#[[Antibiotics]]
+*Indicated if: severe pain, systemic toxicity, elevated CK, clinical suspicion with or without imaging findings
-#*Must cover [[gram positives]], [[gram negatives]], and [[anaerobes]] (especially [[GAS]] and [[clostridium]])
+*Repeat debridement (planned "second look") typically at 24-48 hours
-#*[[Piperacillin-Tazobactam]] 3.375-4.5g q6hr AND [[clindamycin]] 600-900mg q8hr AND [[vancomycin]] 1gm IV q12hr
+*Average: 3-4 debridements before wound management
+*Delay in surgery increases mortality by approximately 9x
-===Diabetics===
+===Antibiotics===
-*IVFs and IV Insulin (with high POCT glucose) for glycemic control (after paging surgery)
+*Must cover '''gram-positives (including MRSA), gram-negatives, AND anaerobes'''
+*Empiric regimen:
+**Piperacillin-tazobactam 4.5g IV q6h (or meropenem 1g IV q8h)
+**+ Vancomycin 25-30 mg/kg IV loading dose (or linezolid 600 mg IV q12h) — MRSA coverage
+**+ Clindamycin 900 mg IV q8h — suppresses toxin production (especially GAS exotoxins)<ref>Stevens DL, et al. Practice guidelines for the diagnosis and management of SSTI: 2014 update by IDSA. ''Clin Infect Dis''. 2014;59(2):e10-e52. PMID 24973422</ref>
+*Clindamycin should be included in all regimens regardless of other antibiotics
+===Supportive Care===
+*Aggressive IV fluid resuscitation
+*Vasopressors for [[septic shock]]
+*Serial lactate monitoring
+*Blood products for DIC
+*ICU admission
+===IVIG===
+*Consider for streptococcal toxic shock syndrome associated with NF (controversial)
 ==Disposition==
-*Admit/OR
+*ICU admission for all patients
+*Surgery consult in ED for any suspected case
+*Serial debridements as needed
+*Wound management: VAC therapy, skin grafting after infection controlled
+==Calculators==
+{{LRINEC Calculator}}
+{{LRINEC Score Calculator}}
 ==See Also==
-*[[Necrotizing Soft Tissue Infections]]
+*[[Necrotizing soft tissue infections]]
-*[[EBQ:LRINEC Score]]
+*[[Fournier gangrene]]
+*[[Cellulitis]]
+*[[Gas gangrene]]
+*[[Sepsis]]
 ==References==
 <references/>
+*Golger A, et al. Mortality in patients with necrotizing fasciitis. ''Plast Reconstr Surg''. 2007;119(6):1803-7. PMID 17440360
+*Puvanendran R et al. Necrotizing fasciitis. ''Can Fam Physician''. 2009;55(10):981-987. PMID 19826154
+*Anaya DA, Dellinger EP. Necrotizing soft-tissue infection: diagnosis and management. ''Clin Infect Dis''. 2007;44(5):705-710. PMID 17278065
-[[Category:ID]]
+[[Category:Infectious Disease]]
+[[Category:Surgery]]

Diferencia entre revisiones de «Necrotizing fasciitis»

Revisión actual - 09:55 22 mar 2026

Background

Types

Risk Factors

Clinical Features

Differential Diagnosis

Evaluation

Labs

LRINEC Score[5]

HUCLA Criteria[6]

Imaging

Definitive Diagnosis

Management

Surgical

Antibiotics

Supportive Care

IVIG

Disposition

Calculators

LRINEC Score

See Also

References

LRINEC Score^[5]

HUCLA Criteria^[6]