Clinical Trial: Caspofungin or Micafungin as Empiric Antifungal Therapy for Persistent Fever and Neutropenia

Study Status: Completed
Recruit Status: Completed
Study Type: Observational

Official Title: Evaluation of Caspofungin or Micafungin as Empiric Antifungal Therapy in Adult Patients With Persistent Febrile Neutropenia: A Retrospective, Observational, Sequential Coh

Brief Summary: Invasive fungal infections are an important cause of morbidity and mortality in patients with neutropenia who are receiving chemotherapy for cancer. Early diagnosis of these infections is difficult and fever may be the only sign. A delay in treatment while a diagnosis is pursued may lead to increased morbidity and mortality. There are now several echinocandins available with similar in vitro spectrum of activity. Caspofungin is the only echinocandin Food and Drug Administration (FDA) approved for empiric antifungal therapy in febrile neutropenia. Although all echinocandin antifungal agents have similar spectrum of activity, there are limited data on the use of micafungin in patients with persistent fever and neutropenia (FN). In November 2006 the Pharmacy and Therapeutics Committee at Brigham & Women's Hospital / Dana Farber Cancer Institute (BWH/DFCI) switched from caspofungin to micafungin as our formulary echinocandin. Given the limited clinical data on the use of micafungin as empiric antifungal therapy in patients with FN, we sought to evaluate the safety and effectiveness of micafungin, compared with caspofungin, for this indication using a sequential cohort analysis of patients treated before and after the formulary change at Brigham and Women's Hospital.

Detailed Summary:

Objectives

This retrospective cohort analysis of converting from caspofungin to micafungin as empiric antifungal therapy for cancer patients who are persistently febrile and neutropenic after receiving broad spectrum antibiotics at Brigham & Women's Hospital / Dana Farber Cancer Institute (BWH/DFCI) is designed to evaluate the following objectives:

  • Safety of micafungin in this patient population
  • Effective dose of 100 mg daily of micafungin compared to 70mg x1, then 50 mg daily of caspofungin
  • Economic impact of converting or formulary echinocandin from micafungin to caspofungin

Study Design

  • Retrospective cohort analysis - limited to medical records

  • Data to be collected include the following:

    • Demographic information: including: gender, age, race
    • Past medical history and admitting diagnoses
    • Laboratory results: Liver function tests (LFTs), Including alanine aminotransferase (ALT), aspartate aminotransferase (AST), Total bilirubin, as well as serum fungal assays: Serum Galactomannan assay, 1.3-BD Glucan assay
    • Concomitant medications and duration of therapy for all systemic: antibiotics and antifungals
    • All invasive breakthrough fungal infection details, including speciation and outcomes during echinocandin therapy
    • Dosing, duration, and adverse events assoc
      Sponsor: Brigham and Women's Hospital

      Current Primary Outcome:

      • Composite Primary Endpoint: Number of Participants With an Overall Favorable Response to Echinocandin Therapy for Empiric Antifungal Therapy for Persistent Febrile Neutropenia (FN) [ Time Frame: 11/1/2005 - 10/31/2007 ]
        Overall favorable response was defined as achievement of successful treatment of baseline fungal infections, survival to hospital discharge, absence of breakthrough Ivasive fungal disese (IFD), and lack of advserse events (AE) attributable to treatment that led to discontinuation of echinocandin therapy.
      • Successful Treatment of Any Baseline Invasive Fungal Disease (IFD) [ Time Frame: 11/1/2005 - 10/31/2007 ]
        Possible or proven baseline invasive fungal disease were defined as were diagnosed within the 2 days of initiating echinocandin therapy for persistent febrile neutropenia
      • Mortality at Hospital Discharge [ Time Frame: 11/1/2005 - 10/31/2007 ]
        We assessed all patients in the study cohort who dischaged from the hospital alive
      • Absence of Any Breakthrough Invasive Fungal Disease (IFD) [ Time Frame: 11/1/2005 - 10/31/2007 ]
        a breakthrough invasive fungal disesase was defined as any fungal infection that was diagnosed > 3 days on or during therapy or within 7 days after completion of therapy with an echinocandin
      • Lack of an Adverse Drug Event (ADE) Attributable to Echinocandin (EC) Therapy That Led to Discontinuation of Therapy [ Time Frame: 11/1/2005 - 10/31/2007 ]
        Defined as any advsere event directly attr

        Original Primary Outcome: Percentage of breakthrough invasive fungal infections in each arm [ Time Frame: 11/1/2005 - 10/31/2007 ]

        Current Secondary Outcome:

        • Duration of Echinocadin Therapy for Persistent Febrile Neutropenia (FN) [ Time Frame: 11/1/2005 - 10/31/2007 ]
          median duration of therapy with an echinocandin (caspofungin or micafungin) for persistent febrile neutropenia (FN)
        • Liver Function Tests (LFTs) Elevated During or After Echinocandin Therapy [ Time Frame: 11/1/2005 - 10/31/2007 ]
          aspartate aminotransferase (AST) or alanine aminotransferase (ALT)> 5x the upper limit of normal (ULN) or total bilirubin > 3x the upper limit of normal (ULN)
        • Specific Type of Adverse Event That Resulted in Echinocandin (EC) Therapy Discontinuation [ Time Frame: 11/1/2005 - 10/31/2007 ]
          The description of the adverse event that resulted in discontinuation of echinocandin (EC) therapy
        • Duration of Hospitization [ Time Frame: 11/1/2005 - 10/31/2007 ]
          Median number of days patients were hospitalized during the study period
        • Duration of Neutropenia [ Time Frame: 11/1/2005 - 10/31/2007 ]
          Median number of days patients were neutropenic during the study period


        Original Secondary Outcome:

        • Mortality at discharge [ Time Frame: 11/1/2005 - 10/31/2007 ]
        • Neutrophil recovery at discharge [ Time Frame: 11/1/2005 - 10/31/2007 ]
        • Duration of therapy with an echinocandin (caspofungin and micafungin) for febrile neutropenia [ Time Frame: 11/1/2005 - 10/31/2007 ]
        • Hepatotoxicity measure by LFT abnormalities during and after therapy [ Time Frame: 11/1/2005 - 10/31/2007 ]


        Information By: Brigham and Women's Hospital

        Dates:
        Date Received: July 24, 2008
        Date Started: January 2008
        Date Completion:
        Last Updated: August 25, 2010
        Last Verified: August 2010