Sandbox carlos: Difference between revisions

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::* '''3. Meningitis:'''
::* '''3. Meningitis:'''


:::* '''Adult:'''
:::* '''3.1 Adult:'''
::::* Preferred regimen: [[Fluconazole]] 400–1,000 mg PO q24h indefinitely.
::::* Preferred regimen: [[Fluconazole]] 400–1,000 mg PO q24h indefinitely.
::::* Alternative regimen: [[Amphotericin B]] 3-5 mg/kg IV q24 hrs {{plus}} 0.1–0.3 mg qd intrathecal (intraventricular) via reservoir device {{OR}} [[Itraconazole]] 400–800 mg q24h {{OR}} [[Voriconazole]]
::::* Alternative regimen: [[Amphotericin B]] 3-5 mg/kg IV q24 hrs {{plus}} 0.1–0.3 mg qd intrathecal (intraventricular) via reservoir device {{OR}} [[Itraconazole]] 400–800 mg q24h {{OR}} [[Voriconazole]]
::::* Note (1): Some use combination of [[Amphotericin B]] and [[Fluconazole]] for progressive severe disease; controlled series lacking.
::::* Note: Some use combination of [[Amphotericin B]] and [[Fluconazole]] for progressive severe disease; controlled series lacking.


:::*'''Child:'''
:::*'''3.2 Child:'''
::::* Preferred regimen: [[Fluconazole]] PO (Pediatric dose not established, 6 mg per kg q24h used)
::::* Preferred regimen: [[Fluconazole]] PO (Pediatric dose not established, 6 mg per kg q24h used)
::::* Alternative regimen: [[Amphotericin B]] 3-5 mg/kg IV q24 hrs {{plus}} 0.1–0.3 mg daily intrathecal (intraventricular) via reservoir device {{OR}} itra 400–800 mg q24h {{OR}} [[Voriconazole]]
::::* Alternative regimen: [[Amphotericin B]] 3-5 mg/kg IV q24 hrs {{plus}} 0.1–0.3 mg daily intrathecal (intraventricular) via reservoir device {{OR}} itra 400–800 mg q24h {{OR}} [[Voriconazole]]




::* '''3.Special considerations for HIV/AIDS patients'''
::* '''4.Special considerations for HIV/AIDS patients'''
:::* '''3.1 Focal Pneumonia'''
:::* '''4.1 Focal Pneumonia'''
:::* 3.1.1 Preferred regimen in mild Infections: [[Fluconazole]] 400 mg PO daily {{or}} [[Itraconazole]] 200 mg PO bid
:::* 4.1.1 Preferred regimen in mild Infections: [[Fluconazole]] 400 mg PO daily {{or}} [[Itraconazole]] 200 mg PO bid
:::* 3.1.2 Alternative regimen in mild infections for patients who failed to respond to [[Fluconazole]] {{or}} [[Itraconazole]]: [[Posaconazole]] 200 mg PO bid {{or}} [[Voriconazole]] 200 mg PO bid
:::* 4.1.2 Alternative regimen in mild infections for patients who failed to respond to [[Fluconazole]] {{or}} [[Itraconazole]]: [[Posaconazole]] 200 mg PO bid {{or}} [[Voriconazole]] 200 mg PO bid
:::* Note: Itraconazole, posaconazole, and voriconazole may have significant interactions with certain antiretro viral agents. These interactions are complex and can be bi-directional
:::* Note: Itraconazole, posaconazole, and voriconazole may have significant interactions with certain antiretro viral agents. These interactions are complex and can be bi-directional
:::* '''3.2 Severe, Non-Meningeal Infection'''
:::* '''4.2 Severe, Non-Meningeal Infection'''
:::* 3.2.1 Preferred regimen in severe, Non-Meningeal Infection (Diffuse pulmonary infection or severely ill patients with extrathoracic, disseminated disease): [[Amphotericin B deoxycholate]] 0.7–1.0 mg/kg IV q12hrs {{or}} Lipid formulation [[Amphotericin B]] 4–6 mg/kg IV q24hrs. Duration of therapy: continue until clinical improvement, then switch to an azole.
:::* 4.2.1 Preferred regimen in severe, Non-Meningeal Infection (Diffuse pulmonary infection or severely ill patients with extrathoracic, disseminated disease): [[Amphotericin B deoxycholate]] 0.7–1.0 mg/kg IV q12hrs {{or}} Lipid formulation [[Amphotericin B]] 4–6 mg/kg IV q24hrs. Duration of therapy: continue until clinical improvement, then switch to an azole.
:::* 3.2.2 Alternative regimen in severe, Non-Meningeal Infection (Diffuse pulmonary infection or severely ill Patients with extrathoracic, disseminated disease): Some specialists will add a triazole ([[Fluconazole]] or [[Itraconazole]], with [[Itraconazole]] (preferred for bone disease) 400 mg per day to [[Amphotericin B]] therapy and continue triazole once [[Amphotericin B]] is stopped
:::* 4.2.2 Alternative regimen in severe, Non-Meningeal Infection (Diffuse pulmonary infection or severely ill Patients with extrathoracic, disseminated disease): Some specialists will add a triazole ([[Fluconazole]] or [[Itraconazole]], with [[Itraconazole]] (preferred for bone disease) 400 mg per day to [[Amphotericin B]] therapy and continue triazole once [[Amphotericin B]] is stopped
:::* Note (1): Therapeutic drug monitoring and dosage adjustment may be necessary to ensure triazole antifungal and antiretroviral efficacy and reduce concentration-related toxicities.
:::* Note (1): Therapeutic drug monitoring and dosage adjustment may be necessary to ensure triazole antifungal and antiretroviral efficacy and reduce concentration-related toxicities.
:::* Note (2): Therapy should be continued indefinitely in patients with diffuse pulmonary or disseminated diseases because relapse can occur in 25%–33% of HIV-negative patients. It can also occur in HIV-infected patients with CD4 counts >250 cells/μL
:::* Note (2): Therapy should be continued indefinitely in patients with diffuse pulmonary or disseminated diseases because relapse can occur in 25%–33% of HIV-negative patients. It can also occur in HIV-infected patients with CD4 counts >250 cells/μL
:::* '''3.3 Meningeal Infections'''
:::* '''4.3 Meningeal Infections'''
:::* Preferred regimen: [[Fluconazole]] 400–800 mg IV or PO daily
:::* Preferred regimen: [[Fluconazole]] 400–800 mg IV or PO daily
:::* Alternative regimen: [[Itraconazole]] 200 mg PO tid for 3 days {{then}} 200 mg PO bid {{or}} [[Posaconazole]] 200 mg PO bid {{or}} [[Voriconazole]] 200–400 mg PO bid {{or}} Intrathecal [[Amphotericin B deoxycholate]] when triazole antifungals are ineffective.
:::* Alternative regimen: [[Itraconazole]] 200 mg PO tid for 3 days {{then}} 200 mg PO bid {{or}} [[Posaconazole]] 200 mg PO bid {{or}} [[Voriconazole]] 200–400 mg PO bid {{or}} Intrathecal [[Amphotericin B deoxycholate]] when triazole antifungals are ineffective.
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:::* Note (2): Some patients with meningitis may develop hydrocephalus and require CSF shunting
:::* Note (2): Some patients with meningitis may develop hydrocephalus and require CSF shunting
:::* Note (3): Therapy should be lifelong in patients with meningeal infections because relapse occurs in 80% of HIV-infected patients after discontinuation of triazole therapy
:::* Note (3): Therapy should be lifelong in patients with meningeal infections because relapse occurs in 80% of HIV-infected patients after discontinuation of triazole therapy
:::* '''3.4 Chronic Suppressive Therapy:''' 
:::* '''4.4 Chronic Suppressive Therapy:''' 
:::* Preferred regimen: Fluconazole 400 mg PO daily (AII), or Itraconazole 200 mg PO BID
:::* Preferred regimen: Fluconazole 400 mg PO daily (AII), or Itraconazole 200 mg PO BID
:::* Alternative regimen: Posaconazole 200 mg PO BID or Voriconazole 200 mg PO BID
:::* Alternative regimen: Posaconazole 200 mg PO BID or Voriconazole 200 mg PO BID

Revision as of 19:42, 22 July 2015

  • 1. Primary pulmonary infection in patients low risk persistence/complication: Antifungal treatment not generally recommended. Treat fever weight loss and/or fatigue.
  • 1.1 Uncomplicated acute coccidioidal pneumonia
  • 1.1.1 For many (if not most) patients, management may rely on periodic reassessment of symptoms and radiographic findings to assure resolution without antifungal treatment.
  • 1.1.2 Indications for antifungal therapy:
  • Immunosupression (AIDS,therapy with high dose corticosteroids, receiptients of TNF-alpha, receiptients of an organ transplant)
  • Diabetes
  • Preexisting cardiomyopathy
  • Pregnancy (third trimester)
  • Filipino or african
  • Weight loss of 110%
  • Intense night sweats persisting longer than 3 weeks
  • Infiltrates involving more than one-half of one lung or portions of both lungs
  • Prominent or persistent hilar adenopathy
  • Anticoccidiodial complement-fixing antibody concentrations in excess of 1:16
  • 1.1.3 Antifungal regimenes
  • Preferred regimen: Oral azole antifungal agents at dosages of 200–400 mg qd. Courses of typically recommended treatment range from 3 to 6 months.


  • 2. Primary pulmonary infection in patients with increased risk of complications or dissemination:
  • 2.1 Preferred regimen in mild to moderate disease: Itraconazole solution 200 mg PO bid or IV q12h Template:OR Fluconazole 400 mg PO q24h for 3–12 months
  • 2.2 Preferred regimen in locally severe or disseminated disease: Amphotericin B 0.6–1 mg/kg PO qd every 7 days THEN 0.8 mg/kg PO every other day OR Liposomal Amphotericin B 3-5 mg/kg IV q24 hrs or Amphotericin B lipid complex 5 mg/kg IV q24 hrs until clinical improvement (usually several weaks or longer in disseminated disease) followed by Itraconazole OR Fluconazole for at least 1 year.
  • Note (1): Some use combination of Amphotericin B and Fluconazole for progressive severe disease; controlled series lacking.
  • Note (2): Consultation with specialist recommendation, surgery may be required.
  • 3. Meningitis:
  • 3.1 Adult:
  • 3.2 Child:


  • 4.Special considerations for HIV/AIDS patients
  • 4.1 Focal Pneumonia
  • 4.1.1 Preferred regimen in mild Infections: Fluconazole 400 mg PO daily OR Itraconazole 200 mg PO bid
  • 4.1.2 Alternative regimen in mild infections for patients who failed to respond to Fluconazole OR Itraconazole: Posaconazole 200 mg PO bid OR Voriconazole 200 mg PO bid
  • Note: Itraconazole, posaconazole, and voriconazole may have significant interactions with certain antiretro viral agents. These interactions are complex and can be bi-directional
  • 4.2 Severe, Non-Meningeal Infection
  • 4.2.1 Preferred regimen in severe, Non-Meningeal Infection (Diffuse pulmonary infection or severely ill patients with extrathoracic, disseminated disease): Amphotericin B deoxycholate 0.7–1.0 mg/kg IV q12hrs OR Lipid formulation Amphotericin B 4–6 mg/kg IV q24hrs. Duration of therapy: continue until clinical improvement, then switch to an azole.
  • 4.2.2 Alternative regimen in severe, Non-Meningeal Infection (Diffuse pulmonary infection or severely ill Patients with extrathoracic, disseminated disease): Some specialists will add a triazole (Fluconazole or Itraconazole, with Itraconazole (preferred for bone disease) 400 mg per day to Amphotericin B therapy and continue triazole once Amphotericin B is stopped
  • Note (1): Therapeutic drug monitoring and dosage adjustment may be necessary to ensure triazole antifungal and antiretroviral efficacy and reduce concentration-related toxicities.
  • Note (2): Therapy should be continued indefinitely in patients with diffuse pulmonary or disseminated diseases because relapse can occur in 25%–33% of HIV-negative patients. It can also occur in HIV-infected patients with CD4 counts >250 cells/μL
  • 4.3 Meningeal Infections
  • Preferred regimen: Fluconazole 400–800 mg IV or PO daily
  • Alternative regimen: Itraconazole 200 mg PO tid for 3 days THEN 200 mg PO bid OR Posaconazole 200 mg PO bid OR Voriconazole 200–400 mg PO bid OR Intrathecal Amphotericin B deoxycholate when triazole antifungals are ineffective.
  • Note (1): Intrathecal amphotericin B should only be given in consultation with a specialist and administered by an individual with experience with the technique.
  • Note (2): Some patients with meningitis may develop hydrocephalus and require CSF shunting
  • Note (3): Therapy should be lifelong in patients with meningeal infections because relapse occurs in 80% of HIV-infected patients after discontinuation of triazole therapy
  • 4.4 Chronic Suppressive Therapy:
  • Preferred regimen: Fluconazole 400 mg PO daily (AII), or Itraconazole 200 mg PO BID
  • Alternative regimen: Posaconazole 200 mg PO BID or Voriconazole 200 mg PO BID




References

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