1 / 15

Neutropenic sepsis

Neutropenic sepsis. Jackie Thomson. OBJECTIVE AND OUTCOME. Apporoach to a patient with neutropenic fever DEFINITION/ABBREVIATION NF = neutropenic fever Fever = Fever is defined as a single oral temperature measurement of >38.0  C 30 minutes apart.

darby
Download Presentation

Neutropenic sepsis

An Image/Link below is provided (as is) to download presentation Download Policy: Content on the Website is provided to you AS IS for your information and personal use and may not be sold / licensed / shared on other websites without getting consent from its author. Content is provided to you AS IS for your information and personal use only. Download presentation by click this link. While downloading, if for some reason you are not able to download a presentation, the publisher may have deleted the file from their server. During download, if you can't get a presentation, the file might be deleted by the publisher.

E N D

Presentation Transcript


  1. Neutropenic sepsis Jackie Thomson

  2. OBJECTIVE AND OUTCOME • Apporoach to a patient with neutropenic fever • DEFINITION/ABBREVIATION • NF = neutropenic fever • Fever = Fever is defined as a single oral temperature measurement of >38.0C 30 minutes apart. • Neutropenia = Neutropenia is defined as an ANC of <500 cells/mm3 or an ANC that is expected to decrease to <500 cells/mm3 during the next 3 days

  3. approach • The host • The bugs • The tests • The drugs

  4. Risk assesment • When dealing with a patient with neutropenic sepsis please always consider the host first. • RISK FACTORS FOR COMPLICATION OF SEVERE INFECTION IN NEUTROPENIC FEVER • HIGH RISK • Anticipated brief (<7 days duration) neutropenic periods • or no or few comorbidities • Such patients are candidates for oral empirical therapy (A-II) on an outpatient basis • Anticipated prolonged (>7 days duration) • Profound neutropenia (absolute neutrophil count [ANC] <100 cells/mm3 following cytotoxic chemotherapy)

  5. Comorbid disease • Presence of any co-morbid medical problems including but not limited to: • Hemodynamic instability • Oral or gastrointestinal mucositis that interferes with swallowing or causes severe diarrhoea • Gastrointestinal symptoms, including abdominal pain, nausea and vomiting, or diarrhoea • Neurologic or mental-status changes of new onset • Intravascular catheter infection, especially catheter tunnel infection • New pulmonary infiltrate or hypoxemia, or underlying chronic lung disease • Evidence of hepatic insufficiency (defined as aminotransferase levels .5 3 normal values) or renal insufficiency (defined as a creatinine clearance of <30 mL/min). • Such patients should be initially admitted to the hospital for IV empirical therapy (A-II).

  6. Low risk patients • Not high dose chemotherapy • No comorbid disease • No hemodynamic instability • Expected neutropenia 3-4 days

  7. The bugs • Know your environment • Get surveillance from the microbiologist

  8. Lab test • FBC ; UKE; LFT, CRP AND PCT. (A-III). • Blood culture • At least 2 sets of blood cultures are recommended, with a set collected simultaneously from each lumen of an existing CVC, if present, and from a peripheral vein site; 2 blood culture sets from separate venepunctures should be sent if no central catheter is present (A-III). • Blood culture volumes should be limited to <1% of total blood volume (usually 70 mL/kg) in patients weighing <40 kg (C-III). (a ‘‘set’’ consists of 1 venepuncture or catheter access draw of 20 mL of blood divided into 1 aerobic and 1 anaerobic blood culture bottle) • Culture specimens from other sites of suspected infection should be obtained as clinically indicated (A-III). • Stool • A stool specimen in a patient with diarrhoea should be evaluated with a Clostridium difficile toxin assay. There is limited value in sending a stool specimen for bacterial pathogen cultures or for ova and parasite examination for most patients treated in US hospitals unless there has been recent travel to or residence in areas of endemicity.

  9. test • Respiratory • Sputum samples for routine bacterial culture should be sent if the patient has a productive cough. Lower respiratory tract specimens obtained by bronchoalveolar • lavage (BAL) are recommended for patients with an infiltrate of uncertain etiology visible on chest imaging. Nasal wash or BAL specimens are recommended to evaluate for symptoms of respiratory virus infection, particularly during an outbreak or during winter. Assays should be sent for detection of adenovirus, influenza A and B virus, RSV, and parainfluenza virus. • Radiography • A chest radiograph is indicated for patients with respiratory signs or symptoms (A-III). CT of other areas (head, sinuses, abdomen, and pelvis) should be performed as clinically indicated. If no abnormality on CXR order CT Chest

  10. tests • Rectal swab • Weekly surveillance • Urine • Culture of urine samples is indicated if signs or symptoms of urinary tract infection exist, a urinary catheter is in place, or the findings of urinalysis are abnormal. • CSF • Examination and culture of spinal fluid is indicated if meningitis is suspected. Platelet transfusion should be given prior to lumbar puncture if thrombocytopenia is a concern. • Skin • Aspiration or biopsy of skin lesions suspected of being infected should be performed for cytological testing, Gram staining, and culture.

  11. Risk assessment • Low Risk Patients: • Oral antibiotic therapy on an outpatient basis if possible, according to sensitivity and/or previous antibiotic history. • Selected hospitalized patients who meet criteria for being at low risk may be transitioned to the outpatient setting to receive either IV or oral antibiotics, as long as adequate daily follow-up is ensured (B-III). • If fever persists or recurs within 48 h in outpatients, hospital re-admission is recommended, with management as for high-risk patients (A-III). • In low-risk patients, the risk of invasive fungal infection is low, and therefore routine use of empirical antifungal therapy is not recommended (A-III).

  12. General rules DESCRIPTION • Neutropenic Prophylaxis • Levofloxacin 500mg od • Posaconazole 5ml tds only for patients with AML induction and SCT • Fluconazole 200 mg bd for all other patients • No ALL or NHL patient receiving vincristine should NOT be on any azole prophylaxis – use amphotericinB deoxycholate 15 mg daily or Ambisome 50 mg 3x/week or amphotericinB deoxycholate 50mg po • Outpatient treatment • Amoxycillin clavulanate 1g bd po • Levofloxacin 500 mg bd po • No Comorbidities, see patients every 24 hrs

  13. Appropriate Antibiotic Therapy – IMPORTANT Considerations • High-risk patients require hospitalization for IV empirical antibiotic therapy; • Monotherapy with an anti-pseudomonal b-lactam agent, such as cefepime, a carbapenem (meropenem or imipenem-cilastatin), or piperacillin-tazobactam, is recommended (A-I). • Other antimicrobials aminoglycosides, fluoroquinolones, and/or vancomycin) may be added to the initial regimen for management of complications (eg, hypotension and pneumonia) or if antimicrobial resistance is suspected or proven (B-III). • Vancomycin (or other agents active against aerobic gram positive cocci) is not recommended as a standard part of the initial antibiotic regimen for fever and neutropenia (A-I). • These agents should be considered for specific clinical indications, including suspected catheter-related infection, skin and soft-tissue infection, pneumonia, or hemodynamic instability. • Modifications to initial empirical therapy may be considered for patients at risk for infection with the following antibiotic resistant organisms, particularly if the patient’s condition is unstable or if the patient has positive blood culture results suspicious for resistant bacteria (B-III). • These include MRSA, VRE, ESBL-producing gram-negative bacteria, and carbapenemase-producing organisms, including KPC. • Risk factors include previous infection or colonization with the organism and treatment in a hospital with high rates of endemicity. • MRSA: Consider early addition of vancomycin, linezolid. (B-III). • VRE: Consider early addition of linezolid. (B-III). • ESBLs: Consider early use of a carbapenems. (B-III). • KPCs: Consider early use of polymyxin-colistin or tigecycline (C-III). • Afebrile neutropenic patients who have new signs or symptoms suggestive of infection should be evaluated and treated as high-risk patients (B-III).

More Related