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Infectious Diseases Case Conference Part II

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CD4 count 10; HIV VL 475K (3/25/4) Begun on FTC/TDF/LPVr w/ in VL to 714 (4/11) ... MOA: virustatic inhibits viral DNA synthesis ... – PowerPoint PPT presentation

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Title: Infectious Diseases Case Conference Part II


1
Infectious Diseases Case ConferencePart II
  • Jason H. Kettler and Asif Zia
  • May 17, 2004
  • Wake Forest University

2
Case Presentation
  • 30 year old Hispanic male
  • Underlying HIV infection
  • CD4 count 10 HIV VL 475K (3/25/4)
  • Begun on FTC/TDF/LPVr w/ ? in VL to 714 (4/11)
  • Intolerant of LPVr ? EFV substituted
  • Most recent CD4 count 30 VL lt50! (5/4/4)
  • Admitted 3/27-4/14 following presentation to the
    ED with N/V/D/RUQ pain

3
Case Presentation
  • Also previously known to have disseminated
    histoplasmosis on the basis of ID consultants
    notations from Concord, NC
  • Clinically manifested by skin ulcerations and
    abnormal chest CT
  • Diagnosis established by positive urine and serum
    antigen at NCBH in 3/2004
  • Txed w/ AmB x ?14d ? itra 200 mg po qD

4
Case Presentation
  • Also of note pt. has a h/o CNS toxoplasmosis
    (again old records) and during March hospzn
    had a cranial MRI demonstrating bilat. basal
    ganglia lesions also known to have () toxo IgG
    on 4/1
  • Upon D/C to Holly Haven ? pyrimethamine
    clindamycin (h/o sulfa hypersensitivity)

5
Case Presentation
  • Also w/ ?history of Hepatitis C
  • HCV Ab negative 3/28/4
  • No transaminitis
  • Isolated elevation of alk. phos. (249) with
    normal bilirubin
  • In light of notion of inability of some to mount
    antibody responses w/ advanced immunosuppression
    ? VL checked ? lt615

6
Case Presentation
  • Owing to GI sxs coupled with finding of anemia
    during last hospitalization ? EGD undertaken 4/13
  • Pathology c/w marked chronic active gastritis
    with ulceration
  • D/Cd on no specific therapy
  • Following discharge

7
Case Presentation
  • Pt. brought back into the hospital through the ED
  • Persistent GI complaints
  • ID consult for recommendations on evaluation and
    treatment of possible CMV gastritis
  • By the way, also colonized with VRE
  • Doesnt speak any English

8
A few questions to answer
  • How is the diagnosis of CMV gastritis
    established?
  • What is the role for any adjunctive testing?
  • PCR, for example
  • What treatment, if any, should be employed?

9
CMV a few basics
  • A large ds-DNA virus of the family Herpesviridae
  • In vivo, CMV-infected cells are found in tissues
    of epithelial and endothelial origin, whereas in
    vitro CMV replication is fully permissive only in
    _________________

10
CMV a few basics
  • A large ds-DNA virus of the family Herpesviridae
  • In vivo, CMV-infected cells are found in tissues
    of epithelial and endothelial origin, whereas in
    vitro CMV replication is fully permissive only in
    human fibroblasts
  • In immunocompetent pts., CMV disease is usually
    associated with a mono-like illness

11
CMV and AIDS
  • Viremia with CMV is common in asymptomatic
    persons w/ low CD4 counts
  • Rare cells containing CMV inclusion bodies may be
    seen on HP specimens even when other pathogens
    are causing organ dysfunction
  • Patients are known to recover with no therapy
    directed at the CMV

12
AIDS-related CMV GI Disease
  • Many studies have suggested that CMV end-organ
    disease results from the hematogenous spread of
    CMV
  • Presence of CMV in the blood is a RF for the
    dvpt. of CMV disease in AIDS patients
  • CD4 T-lymphocyte activity is critical for
    preventing CMV replication and end-organ disease

13
Clinical Manifestations
  • Nearly all patients w/ GI-related CMV disease
    have a CD4 ct. of lt50
  • Sxs determined by location
  • esophagitis? odynophagia/substernal pain
  • pain is persistent and focal in contrast to
    Candida
  • gastritis ? substernal /or epigastric pain
  • small bowel dz? abd. pain /- diarrhea
  • colitis? intractable diarrhea, oft. w/
    hematochezia
  • proctitis ? tenesmus

14
Diagnostic Criteria
  • CMV GI disease is most accurately diagnosed by
    the clinical triad of
  • cardinal symptoms, visualization of mucosal
    ulcers or erosions, histologic evidence of
    tissue destruction caused by CMV
  • Viral culture of mucosal biopsies for CMV does
    not have much clinical utility because mucosal
    CMV shedding is neither sensitive nor specific
    for CMV GI disease

15
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16
Role for PCR testing
  • Data on the use of qualitative CMV PCR on blood
    suggest that it may help to predict eventual
    development of CMV disease
  • Prospective cohort of 97 AIDS pts. (all w/ CD4
    cts. lt50)
  • 16/27 (59) who were CMV PCR () at b/l dvpd. CMV
    dz w/in 12 mos. compared w/ only 3/70 (4) who
    were CMV PCR (-) (AIDS 1997)

17
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18
Treatment
  • HAART ? immune restoration
  • Only 2 randomized trials for CMV GI dz
  • Consensus of clinical experts is that pts. should
    receive 3-6 weeks of BID IV ganciclovir or
    foscarnet
  • Maintenance therapy generally not required
  • Valganciclovir an attractive alternative
  • Only indicated for CMV retinitis, but is likely
    to have similar efficacy to IV GCV

19
VGCV
  • In anecdotal reports, VGCV has been used for
    terminal tx of CMV colitis and esophagitis
  • MOA virustatic inhibits viral DNA synthesis
  • SEs anemia/neutropenia, N/V/D, fever, HA,
    confusion, retinal detachment
  • VGCV at a dose of 900 mg is roughly equivalent to
    IV GCV at a dose of 5 mg/kg

20
Our Patient
  • ? CMV gastritis
  • Dx plausible but not proven
  • Obtain CMV PCR on blood
  • Eye exam
  • Ask path to review slide and perform
    immunoperoxidase stain on gastric bx
  • Begin empiric GCV 5 mg/kg IV q12h
  • Start G-CSF

21
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22
Our Patient
  • PCR ? not done
  • Eye exam ? negative
  • Disposition
  • To Holly Haven on 900 mg po BID of VGCV
  • Completed 12 days of therapy in total
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