Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Rim Halaby, M.D. [2]
Synonyms and keywords: Febrile neutropenia
Definition
Neutropenic fever is defined as one oral temperature of ≥38.3°C (101°F) or a temperature of ≥38.0°C (100.4°F) for over one hour. Neutropenia is defined as an absolute neutrophil count (ANC) <500 cells/mm3 or an ANC that is expected to become less than 500 cells/mm3 over the next 48 hours. Profound neutropenia is defined as an ANC <100 cells/mm3. Patients with functional neutropenia have a qualitative abnormality of neutrophil functions despite a normal or elevated ANC, as seen in hematological malignancy, and are at increased risk of infections similarly to patients with low ANC.[1]
Causes
Life Threatening Causes
Life-threatening causes include conditions which may result in death or permanent disability within 24 hours if left untreated.
Common Causes
Management
Day 1: Initial Management of Patients With Neutropenic Fever
| | | | | | Characterize the symptoms:
Symptom suggestive of neutropenic fever:
❑ Fever in cancer patients who are on chemotherapy
- ❑ Single oral temperature ≥38.3° C (101° F)
or
- ❑ Temperature ≥38° C (100.4°F) sustained for over one hour
with
❑ Reduced absolute neutrophil count (ANC)
- ❑ ANC <500 cells/mm3
or
- ❑ ANC that is expected to decrease to <500 cells/mm3 in the next 48 hours
| | | | | |
| | | | | | | | | | | | | | | |
| | | | | | Consider the diagnosis of neutropenic fever POTENTIALLY LIFE THREATENING | | | | | |
| | | | | | | | | | | | | | | |
| | | | | | Obtain a detailed history:
❑ History of any symptom of infections and inflammation of
- ❑ Skin and soft-tissues
- ❑ Respiratory system
- ❑ Central nervous system
- ❑ Urinary tract
❑ History of any co-morbid conditions
- ❑ Diabetes mellitus
- ❑ Chronic obstructive lung disease
❑ History of any recent exposure to infections
❑ History of any current antibiotic prophylaxis
❑ History of non infectious causes of fever (example: administration of blood products)
❑ History of recent surgical procedures
❑ History of prior documentation of infections or pathogen colonization | | | | | |
| | | | | | | | | | | | | | | |
| | | | | | Examine the patient:
❑ Search for signs of infections at
- ❑ Entry and exit sites of catheters in skin
- ❑ Sites of previous procedures in skin (example: bone marrow aspiration site)
- ❑ Oropharynx (including perioduntum)
- ❑ Lungs
- ❑ Alimentary tract
- ❑ Perineum
| | | | | |
| | | | | | | | | | | | | | | |
| | | | | | Order laboratory tests (routine):
❑ CBC with
- ❑ Differential leukocyte count
- ❑ Platelet count
❑ BMP
❑ AST
❑ ALT
❑ Total bilirubin
❑ Blood cultures (at least 2 sets)
Central catheter | 1st set | 2nd set |
❑ Present | ❑ From each lumen of existing central catheters | ❑ From a peripheral vein site |
❑ Absent | ❑ From one separate venipuncture | ❑ From another separate venipuncture |
❑ Urinalysis
Order additional tests (not routine and order if clinically indicated):
Tests | Clinical indications |
❑ Urine culture | ❑ Urinary tract infection ❑ Urinary catheter in place ❑ Abnormal findings on urinalysis |
❑ Chest X-ray | ❑ Respiratory tract infection |
❑ CT head | ❑ CNS infection |
❑ CT sinuses | ❑ Sinus infection |
❑ CT abdomen | ❑ Infection of abdominal organs |
❑ CT pelvis | ❑ Infection of pelvic organs |
❑ Stool for clostridium difficile toxin assay | ❑ Diarrhea |
❑ Stool for bacterial pathogen cultures or for ova and parasite | ❑ Diarrhea following a history of recent travel |
❑ CSF analysis and culture | ❑ Meningitis |
❑ Skin aspiration or biopsy for cytological testing, gram staining, and culture | ❑ Skin infection |
❑ Sputum analysis | ❑ Productive cough |
❑ Bronchoalveolar lavage and analysis | ❑ Infiltrations on chest imaging with an uncertain etiology |
❑ Nasal wash or bronchoalveolar lavage and assays for viral detection | ❑ Respiratory infection during an outbreak or during winter |
| | | | | |
| | | | | | | | | | | | | | | |
| | | | | | Do a risk assessment using MASCC risk Index: (MANDATORY)
Characteristic | Score |
❑ No or mild symptoms in patients following an episode of febrile neutropenia | ❑ 5 |
❑ Absence of hypotension with a systolic blood pressure >90 mmHg | ❑ 5 |
❑ No chronic obstructive pulmonary disease (active chronic bronchitis, emphysema, decrease in forced expiratory volumes, need for oxygen therapy and/or steroids and/or bronchodilators) | ❑ 4 |
❑ Solid tumor or hematologic malignancy with no previously demonstrated fungal infection or empirically treated suspected fungal infection | ❑ 4 |
❑ Absence of dehydration that requires parenteral fluids | ❑ 3 |
❑ Moderate symptoms in patients following an episode of febrile neutropenia | ❑ 3 |
❑ Outpatient status | ❑ 3 |
❑ Age <60 years | ❑ 2 |
| | | | | |
| | | | | | | | | | | | | | | | | |
| | | | | |
| | | | Low risk patients:
❑ MASCC score ≥21
or
❑ Expected brief neutropenia (≤7 days) and/or
❑ Clinically stable and/or
❑ Absence of comorbidities (neurological changes, gastrointestinal symptoms, underlying chronic lung disease, intravascular catheter infection, hemodynamic instability, hepatic insufficiency, or renal insufficiency) | | High risk patients:
❑ MASCC score <21
or
❑ Expected prolonged neutropenia (>7 days) and
❑ Profound neutropenia (ANC≤100 cells mm3) and/or
❑ Clinically unstable (unbearable pain, altered mental status, or hypotension) and/or
❑ Presence of comorbidities (neurological changes, gastrointestinal symptoms, underlying chronic lung disease, intravascular catheter infection, hemodynamic instability, hepatic insufficiency, or renal insufficiency)
Patients who do not strictly fulfill the criteria for being at low risk
Afebrile neutropenic patients with new signs or symptoms suggestive of infection | | |
| | | | | | | | | | | | | | | | |
| | | | Administer oral or IV empirical broad-spectrum antibiotic therapy (URGENT):
❑ Ciprofloxacin + Amoxicillin-clavulanate
❑ In clinic or hospital setting
❑ Observe for 4-24 hours after drug administration | | Hospitalize the patient | | | |
| | | | | | | | | | | | | | | | | | |
| | | |
| | | | | Consider continuing with inpatient IV broad-spectrum antibiotics:
❑ Inability to tolerate oral medications
❑ Unavailabilty of telephone, transportation to hospital, caregiver
❑ Identified infections requiring IV antibiotics
❑ Patient is clinically unstable
❑ Patient and physician decision | | | | |
| | | | | | | | | | | | | | | | | |
| | | | | | | | Inpatient monitoring:
Monitor for recovery, adverse drug effects, secondary infections and development of drug-resistance with
❑ Daily review of systems
❑ Daily physical examination
❑ Cultures of specimens from suspicious sites
❑ Focused imaging studies | | | | | | | |
| | |
| | | | | | | | | | | | | | | | | | | | |
| | | Consider discharge with outpatient oral broad-spectrum antibiotics:
❑ Ability to tolerate oral medications
❑ Availabilty of telephone, transportation to hospital, caregiver
❑ Fulminant infections are excluded
❑ Patient is clinically stable
❑ Patient and physician decision | | | Add vancomycin to the initial empirical antibiotic monotherapy for:
❑ Suspected Catheter related infection ❑ Suspected skin and soft tissue infection ❑ Suspected pneumonia ❑ Hemodynamic instability ❑ Positive gram-positive bacterial blood culture (that is available before the final identification and susceptibility test) ❑ Colonization with MRSA, VRE, or penicillin-resistant streptococcus pneumoniae ❑ Severe mucositis (following fluoroquinolone prophylaxis and use of ceftazidime as empirical therapy)
Consider modifying the initial empirical antibiotic monotherapy for:
❑ Suspected antimicrobial resistance:
- ❑ Patient is unstable
- ❑ Patient's positive blood culture is suspicious for a resistant bacteria
- ❑ Patient has/had treatment in a hospital with high rates of endemicity
- ❑ Patient had previous history of any infection or colonization with an organism
or
❑ Proven antimicrobial resistance where the blood cultures are positive for resistant bacteria
| | | | | | |
| | | | | | | | | | | | | | | | | | |
| | | Outpatient monitoring:
❑ Monitor for recovery, adverse drug effects, secondary infections and development of drug-resistance with
- ❑ Daily review of systems
- ❑ Daily physical examination
- ❑ Cultures of specimens from suspicious sites
- ❑ Focused imaging studies
❑ Ensure 24 hours a day and 7 days a week access to the appropriate medical care
❑ Consider re-admission for IV broad-spectrum antibiotics in case of
- ❑ Persisting fever
- ❑ Recurrent fever
- ❑ New signs of infection
- ❑ Decreasing neutrophil counts
| | | | | | | | | | | |
Days 2 to 4: Management of Low Risk Patients With Neutropenic Fever After Day 1 Management
| | | | | | Low risk patients | | | | | | |
| | | | | | | | | | | | | | | | | | |
| | | | | | | |
| | | Unexplained fever after day 1 | | | | Clinically or microbiologically documented infection during day 1 | | | |
| | | | | | | | | | | | | | | | | | | |
| | | | | |
| ❑ Persistent or recurrent fever and/or ❑ Clinically unstable | | ❑ Responding to initial empirical therapy and/or ❑ Cultures negative | | Modify antibiotics according to culture results and/or infection site:
Culture results and/or infection site | Modified regimen |
❑ Gram-negative bacteremia | ❑ Administer a combination of
- ❑ Beta-lactam
or
- ❑ Carbapenem
plus
- ❑ Aminoglycosides
or
- ❑ Fluoroquinolones
and
❑ Switch to a monotherapy with a beta-lactam agent once the susceptibilities are known |
❑ Gram-positive bacteremia or skin and soft-tissue infections | ❑ Administer
- ❑ Vancomycin
or
- ❑ Linezolid
or
- ❑ Daptomycin
and
❑ Adjust regimen based on susceptibility of pathogen |
❑ Pneumonia | ❑ Administer a combination of
- ❑ Beta-lactam
or
- ❑ Carbapenem
plus
- ❑ Aminoglycosides
or
- ❑ Antipseudomonal fluoroquinolones
and
❑ If MRSA suspected add
- ❑ Vancomycin
or
- ❑ Linezolid
and
❑ Adjust regimen based on susceptibility of pathogens and clinical progress |
❑ HSV or candida esophagitis | ❑ Administer acyclovir and/or fluconazole |
❑ Neutropenic enterocolitis | ❑ Adminsiter
- ❑ Monotherapy: Piperacillin-tazobactam or carbapenem
or
- ❑ Combination therapy: Anti-pseudomonal cephalosporin plus metronidazole
|
| | | |
| | | | | | | | | | | | | | | | | | |
|
Inpatient management:
❑ Hospitalize the patients who are on outpatient broad-spectrum antibiotics
❑ Continue the patients who are on inpatient IV broad-spectrum antibiotics with inpatient management
Order:
❑ A new set of blood cultures
❑ Stool sample for C. difficile antigen and toxin assay (if diarrhea is present)
❑ Abdominal CT (if abdominal pain and diarrhea is present)
❑ Other symptom related diagnostic tests
Consider noninfectious causess:
❑ Drug related fever
❑ Thrombophlebitis
❑ Underlying cancer
❑ Resorption of blood from a large hematoma | | Continue the initial oral or IV broad-spectrum antibiotics until:
❑ ANC is >500 cells/mm3 and rising
Outpatient management:
❑ Consider discharging patients with oral broad-spectrum antibiotics
- ❑ Ability to tolerate oral medications
- ❑ Availabilty of telephone, transportation to hospital, caregiver
- ❑ Fulminant infections are excluded
- ❑ Patient is clinically stable
- ❑ Patient and physician decision
❑ Monitor the patients for recovery, adverse drug effects, secondary infections and development of drug-resistance with
- ❑ Daily review of systems
- ❑ Daily physical examination
- ❑ Cultures of specimens from suspicious sites
- ❑ Focused imaging studies
❑ Ensure 24 hours a day and 7 days a week access to the appropriate medical care
❑ Consider re-admission of patients in case of
- ❑ Persisting fever
- ❑ Recurrent fever
- ❑ New signs of infection
- ❑ Decreasing neutrophil counts
| | | | | | | | |
| | | | | | | | | | | | | | | | | |
| | | | | | | | | | | | | | | | | | | |
| | | | | |
| Modify antibiotics according to culture results and/or infection site:
Culture results and/or infection site | Modified regimen |
❑ Drug-resistant gram-negative bacteria
❑ Drug-resistant gram-positive bacteria
❑ Drug-resistant anaerobes | ❑ Change from initial cephalosporin to
- ❑ Imipenem
or
- ❑ Meropenem
❑ If initially on vancomycin add
- ❑ Aminoglycoside
or
- ❑ Ciprofloxacin
or
- ❑ Aztreonam
|
❑ Suspected systemic inflammatory response syndrome | ❑ Add fluconazole |
❑ Clostridium difficile | ❑ Add
- ❑ Oral vancomycin
or
- ❑ Oral metronidazole
|
❑ Neutropenic enterocolitis | ❑ Adminsiter
- ❑ Monotherapy: Piperacillin-tazobactam or carbapenem
or
- ❑ Combination therapy: Anti-pseudomonal cephalosporin plus metronidazole
|
| | | | | Responding | | Not responding | |
| | | |
| | | | | | | | | | | | | | | | | | |
| |
❑ Continue antibiotics
- ❑ For 7-14 days as appropriate for documented infection
or
- ❑ Until ANC >500 cells/mm3 and rising
and
❑ Consider resuming oral fluoroquinolone prophylaxis until ANC >500 cells/mm3 and rising in patients
- ❑ Who remain neutropenic after completion of appropriate treatment
- ❑ Who's signs and symptoms of a documented infection has resolved
| | | | | | | ❑ Consider re-examination and re-imaging studies (CT, MRI) for new or worsening sites of infection ❑ Consider culturing, biopsy, or draining sites of worsening infection ❑ Consider reviewing antibiotic coverage for adequacy of dosing and spectrum ❑ Consider adding empirical antifungal therapy ❑ Broaden antimicrobial coverage for hemodynamic instability | |
Days 2 to 4: Management of High Risk Patients With Neutropenic Fever After Day 1 Management
| | | | | | High risk patients | | | | | | |
| | | | | | | | | | | | | | | | | | |
| | | | | | | |
| | | Unexplained fever after day 1 | | | | Clinically or microbiologically documented infection during day 1 | | | |
| | | | | | | | | | | | | | | | | | | |
| | | | | |
| ❑ Persistent or recurrent fever and/or ❑ Clinically stable | | ❑ Responding to initial empirical therapy and/or ❑ Cultures negative | | Modify antibiotics according to culture results and/or infection site:
Culture results and/or infection site | Modified regimen |
❑ Gram-negative bacteremia | ❑ Administer a combination of
- ❑ Beta-lactam
or
- ❑ Carbapenem
plus
- ❑ Aminoglycosides
or
- ❑ Fluoroquinolones
and
❑ Switch to a monotherapy with a beta-lactam agent once the susceptibilities are known |
❑ Gram-positive bacteremia or skin and soft-tissue infections | ❑ Administer
- ❑ Vancomycin
or
- ❑ Linezolid
or
- ❑ Daptomycin
and
❑ Adjust regimen based on susceptibility of pathogen |
❑ Pneumonia | ❑ Administer a combination of
- ❑ Beta-lactam
or
- ❑ Carbapenem
plus
- ❑ Aminoglycosides
or
- ❑ Antipseudomonal fluoroquinolones
and
❑ If MRSA suspected add
- ❑ Vancomycin
or
- ❑ Linezolid
and
❑ Adjust regimen based on susceptibility of pathogens and clinical progress |
❑ HSV or candida esophagitis | ❑ Administer acyclovir and/or fluconazole |
❑ Neutropenic enterocolitis | ❑ Adminsiter
- ❑ Monotherapy: Piperacillin-tazobactam or carbapenem
or
- ❑ Combination therapy: Anti-pseudomonal cephalosporin plus metronidazole
|
| | | |
| | | | | | | | | | | | | | | | | | |
| ❑ Assess for infection sites ❑ Include CT of the chest
and sinuses to assess for invasive fungal infection | | Continue antibiotics until ANC >500 cells/mm3 and rising | | | | | | | | |
| | | | | | | | | | | | | | | | | | |
| ❑ No changes in empirical antibiotics ❑ Consider continuing the empirical antibiotic therapy until ANC >500 cells/mm3 and rising ❑ Consider modifying the empirical antibiotic coverage based on the clinical or microbiologic evidence of infections (including anti-fungal agents) ❑ Consider switching back to fluoroquinolone prophylaxis for the remaining duration of neutropenia if afebrile for 4-5 days ❑ Consider switching from inpatient to outpatient oral or IV antibiotic regimens if the patients fever has subsided, combined with careful daily follow up | | Recurrent fever during persistent neutropenia | | | | | | | | |
| | | | | | | | | | | | | | | | | | |
| | | | | |
| | | | | | | Responding | | Not responding | |
| | | | | | | | | | | | | | | | | |
| | | | | | |
❑ Continue antibiotics
- ❑ For 7-14 days as appropriate for documented infection
or
- ❑ Until ANC >500 cells/mm3 and rising
and
❑ Consider resuming oral fluoroquinolone prophylaxis until ANC >500 cells/mm3 and rising in patients
- ❑ Who remain neutropenic after completion of appropriate treatment
- ❑ Who's signs and symptoms of a documented infection has resolved
| | ❑ Consider re-examination and re-imaging studies (CT, MRI) for new or worsening sites of infection ❑ Consider culturing, biopsy, or draining sites of worsening infection ❑ Consider reviewing antibiotic coverage for adequacy of dosing and spectrum ❑ Consider adding empirical antifungal therapy ❑ Broaden antimicrobial coverage for hemodynamic instability | |
After Day 4: Management of High Risk Patients With Neutropenic Fever
Do's
- Modify the antibiotic regimens depending on the clinical picture and the epidemiology of infections in the area and the hospital where the patient is being treated at.
Don'ts
- Don't measure the temperature of the patient in the axillary area because it is not as specific as if it was taken orally.
- Don't measure the temperature of the patient rectally to avoid contaminating the skin and soft tissues of the rectal area.
References
- ↑ Freifeld, AG.; Bow, EJ.; Sepkowitz, KA.; Boeckh, MJ.; Ito, JI.; Mullen, CA.; Raad, II.; Rolston, KV.; Young, JA. (2011). "Clinical practice guideline for the use of antimicrobial agents in neutropenic patients with cancer: 2010 update by the infectious diseases society of america". Clin Infect Dis. 52 (4): e56–93. doi:10.1093/cid/cir073. PMID 21258094.
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