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Infectious Diseases Case Conference

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Title: Infectious Diseases Case Conference


1
Infectious Diseases Case Conference
  • Jason Kettler
  • Wake Forest University
  • February 10, 2003

2
Case Presentation
  • 68 year old BM with underlying DM/htn
  • HgbA1C 13.2
  • To dentist on 11/12/2 c/o tooth pain which
    resulted in an extraction, followed by a 6-day
    course of amoxicillin
  • Pt. then presented to an OSH on 4 separate
    occasions w/ various c/o including facial
    swelling, h/a, ?ed facial sensation

3
Case Presentation
  • Hospitalized elsewhere from 12/7/2 12/12/2
    after having X-rays, CTs, bloodwork
  • Apparently still symptomatic at the time of d/c
    reports he was still having h/a, facial swelling,
    ?ed visual acuity, ?ed facial sensation
  • Seen by a dentist the day after d/c from the
    hospital ? full mouth extraction

4
Case Presentation
  • Multiple courses of antibiotics throughout the
    hospitalization
  • Seen by a neurologist who ordered an MRI per the
    family but no specific dx was provided
  • Also referred to an ophthalmologist but to no
    avail
  • Due to persistence of h/a, worsened visual
    acuity, ?ed facial sensation, inability to
    entirely open his mouth - pt. went to DHP ?
    admitted to undergo MRI and ENT evaluation

5
  • Poorly-controlled diabetic man who has a symptom
    complex of facial swelling, headache, diminished
    visual acuity, diminished facial sensation,
    evidence of dental caries
  • Knowing only that much, are you inclined toward a
    particular diagnosis?

6
  • MUCORMYCOSIS

7
  • MUCORMYCOSIS
  • Principal other diagnosis in the differential
    would be aspergillosis
  • Less likely considerations might include
    actinomycosis, botryomycosis

8
Case Presentation
  • PMH DM x 3-4 yrs., recently dxed htn
  • Meds SSI, amiloride, amphotericin b 40 mg x 1
    dose
  • All codeine, hydrocodone
  • SH Remote EtOH use smoker x 30 yrs
  • FH 2 daughters on dialysis 2o GN
  • ROS Ff/c/wt. loss appetite good
    FN/V/D/CP/SOB/rhinorrhea/sneezing /-
    congestion h/a x 1-1/2 mos.,?ed visual acuity
    ?ed facial sensation

9
Physical Exam
  • tcur tmax 99.9 p89 bp143/73 r20 sat92 in
    RA
  • gen pleasant, appears well
  • heent perrla, eomi L eyelid swollen, eye
    closed could not appreciate light in L eye
    nares patent F obvious eschar or lesion o/p
    edentulous w/ sinus tract in mid-portion of soft
    palate, ?ed oral aperture

10
Physical Exam
  • neck supple, soft tissue swelling on posterior
    neck (old) FLAD
  • cv regular rhythm II/VI systolic murmur
  • lungs soft bibasilar crackles, F wheeze
  • abd soft, nt, nd, nabs
  • extrem Fc/c/e Fskin breakdown on feet
  • skin hyperpigmented macules/papules on abdomen
  • neuro ?ed facial sensation B, CN o/w intact
    F obvious focal weakness DTRs 2 in U/LE

11
Lab data
  • WBC 13.3 hgb 9.9 plt 700
  • CMP entirely WNL except nf glc of 162
  • CRP 4.4
  • ESR 98
  • Gram stain of sinuses 1 WBC, 1 GNR
  • Blood cx NG

12
MRI brain
13
Assessment
  • Elderly diabetic gentleman who now presents w/
    extensive bilateral sinusitis w/ accompanying
    tissue destruction. Statistically, the most
    likely causes would be mucormycosis,
    aspergillosis. Organisms are distinguishable
    pathologically and that specimen is pending. ENT
    feels surgery potentially not feasible, though
    therapy for invasive disease such as this is
    typically a combined medical and surgical
    approach. Cannot r/o concomitant bacterial
    sinusitis.

14
Our Suggestions
  • Abelcet 10mg/kg/d
  • Cefepime 2 g IV q12
  • Await further culture / pathologic data

15
Path Specimen
16
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17
Hospital Course
  • Initially treated with 10/kg Abelcet but dose
    diminished 2o renal insufficiency
  • Ultimately infusion extended over 11 hours

18
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19
Hospital Course
  • Initially treated with 10/kg Abelcet but dose
    diminished 2o renal insufficiency
  • Ultimately infusion extended over 11 hours
  • Rifampin 600 mg BID
  • Briefly treated w/ Cefepime
  • S/P B max antrotomies, B ethmoidectomies,
    septectomy, inf. middle turbinate resections
    AND 2 subsequent debridements

20
MUCORMYCOSIS
  • Salient points of interest and management issues

21
Classification
  • Mucormycosis refers to a group of mycoses caused
    by one of the ubiquitous, saprophytic fungi of
    the ORDER Mucorales
  • The names of the fungi have changed over the
    years
  • The term Zygomycosis refers to the class
    Zygomycetes, which contains the Mucorales as well
    as the Entomophthorales, agents that cause
    completely different diseases than the Mucorcales
  • Rhizopus, Rhizomucor, Absidia are most commonly
    isolated pathogens but diseases are virtually
    identical
  • I. Zygomycotina
  • A. Zygomycetes
  • a. Mucorales
  • 1. Mucoraceae
  • i. Absidia
  • (a) A. corymbifera
  • (b) A. ramosa
  • ii. Mucor
  • (a) M. circinelloides
  • iii. Rhizomucor
  • (a) R. pusillus
  • iv. Rhizopus
  • (a) R. oryzae ( R. arrhizus)
  • (c) R. rhizopodiformis
  • 2. Cunninghamellacaeae
  • i. Cunninghamella
  • (a) C. bertholletiae
  • 3. Mortierellaceae
  • i. Mortierella

22
Characteristics of Mucorales
  • NOT fastidious organisms and grow at a range of
    temperatures
  • The organisms are aerobic and typically grow
    within 2-5 days of incubation
  • Ubiquitous organisms which initiate and
    facilitate decay of organic material
  • Exposure to spores of these fungi is unavoidable
    and hence the rarity of infections caused by
    Mucorales is indicative of their relative
    avirulence
  • Infection caused by one of these organisms
    suggests a serious underlying predisposition
  • Can colonize the respiratory and GI tracts of
    healthy humans

23
Pathogenesis
  • Infection occurs after inhalation of spores into
    the respiratory tract
  • Spores may be deposited into the nasal turbinates
    or may pass through to the pulmonary alveoli
  • It is thought that impaired function of
    macrophages in diabetic pts. predisposes them to
    invasive disease (CID 1992)
  • Most characteristic feature of mucormycosis is
    hyphal invasion of blood vessels, leading to
    hemorrhage, thrombosis, infarction necrosis
  • This can lead to cavernous sinus and internal
    carotid artery thrombosis

24
Clinical Manifestations
  • Six separate syndromes rhinocerebral,
    pulmonary, cutaneous, GI, CNS, disseminated
  • Most common is rhinocerebral
  • Most common complaints are facial pain, h/a,
    fever can extend to orbit via the nasal
    turbinates and cause visual disturbances can
    also extend to the brain, esp. the frontal lobes
  • When the disease invades into the mouth, a black
    necrotic eschar can be seen on the palate, a
    finding which is highly suggestive of invasive
    mucormycosis (though perhaps overemphasized,
    occurring 19-40 of the time in one case series)

25
At-risk populations
  • Diabetics, especially with poor glycemic control,
    /or who are in ketoacidosis
  • Other immunocompromised individuals, especially
    organ transplant pts., hematologic malignancies,
    severe burns, ESRD
  • These pts. are more likely to present with
    pulmonary or disseminated disease
  • Rarely reported in pts. w/ AIDS
  • Pts. receiving deferoxamine as a chelating agent

26
Diagnosis
  • Since invasion of blood vessels is a major
    manifestation of mucor, areas of vasculitis w/
    thrombosis, hemorrhage, etc. are important clues
  • Aggressive progression (hours to days) w/ assoc.
    tissue damage esp. in the resp. tree CNS is
    characteristic
  • Pts. w/ aspergillosis can present w/ cutaneous
    and respiratory findings that are similar to mucor

27
Diagnosis
  • Culture of, and pathologic examination of bx
    specimens is, thus, the only way to definitively
    dx mucormycosis
  • Mucorales appear in tissue as irregularly shaped,
    broad, nonseptate hyphae with right-angle
    branching
  • Cultures are infrequently positive
  • CT/MR may reveal orbital involvement, extent of
    soft tissue/vascular invasion by fungi
  • In pts. w/ intracranial involvement, CSF sampling
    is nonspecific and unhelpful

28
Treatment
  • Historically has involved three fundamental
    components 1) systemic antifungal treatment
    with amphotericin B, 2) debridement and excision
    of all necrotic tissue, 3) reversal of underlying
    predispositions
  • With the combined approach, mortality rates have
    fallen below 20
  • Mortality higher in pts. w/o DM, but with other
    predisposing risk factors or underlying diseases

29
Amphotericin B
  • No definitive recommended dosing of amphotericin
    therapy usually has required the maximum
    recommended dosage of 1.5 mg/kg/d
  • The lipid formulations offer an attractive
    treatment option
  • substantially reduced renal toxicity
  • the lethal dose of lipid-based AmB is approx.
    10-15x higher than conventional ampho
  • may exhibit better diffusion into the CNS

30
  • Mondy, K, B Haughey et al. Rhinocerebral
    Mucormycosis in the Era of Lipid-Based
    Amphotericin B Case Report and Literature
    Review. Pharmacotherapy 200222519-26.
  • Lipid formulations of AmB are ideally suited for
    therapy against infections such as RCM, which
    require large doses of drug given for long
    periods of time (CID 1998)
  • Of 24 immunocompromised pts. w/ various forms of
    mucor prior nephrotoxicity or therapeutic
    failure while on conventional AmB, 17 (71) were
    cured or improved after switching to ABLC

31
Mondy et al
  • A study of AmB lipid complex administered to pts.
    w/ DM revealed that of four patients treated for
    RCM, all were either cured or improved w/ this
    drug, despite prior nephrotoxicity or poor
    response to conventional AmB (Infect Dis in Clin
    Practice 1997)

32
Medical therapy only?
  • 3 case reports in the literature of pts. cured w/
    medical therapy alone
  • 2 are similar diabetic, advanced rhinoorbital
    involvement w/ intracranial extension cavernous
    sinus involvement both treated w/ ABLC
  • 1 an IVDA w/ a basal ganglia abscess received
    conventional AmB only but had no rhinoorbital
    involvement that could serve as a persistent
    source for spread of infection no underlying
    illness

33
Other experimental therapies
  • Hyperbaric oxygen
  • Nebulized or local irrigation w/ AmB
  • Topical H2O2
  • Combo of AmB w/ either flucytosine, rifampin, or
    fluconazole
  • None of these agents has shown consistent in vivo
    or in vitro activity

34
Prolonging ABLC infusion
  • Eriksson U et al. Comparison of effects of
    amphotericin B deoxycholate infused over 4 or 24
    hours randomised controlled trial. BMJ 2001.
  • Continuous infusions of AmB reduce nephrotoxicity
    and SEs related to infusion w/o increasing
    mortality
  • At WFUBMC, we have extrapolated these findings to
    pts. being treated with ABLC therapy with
    favorable results
  • Not yet reported
  • At least 3 clinical observations of success
  • We, the ID people of Wake Forest, are pioneers!

35
Take-home points regarding therapy
  • Best outcomes are achievable with combined
    surgical medical approaches, w/ reversal of
    underlying illness if possible
  • Lipid-based ampho appears to be the best medical
    option considering length of therapy and need for
    very high doses
  • Other adjunctive therapies, e.g. rifampin, may or
    may not be of benefit
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