| Literature DB >> 24716014 |
Tom Wingfield1, Jo Baxter2, Amit Herwadkar3, Daniel du Plessis4, Tom J Blanchard2, F Javier Vilar2, Anoop Varma5.
Abstract
Background. HIV-positive people starting combined antiretroviral therapy may develop immune reconstitution to latent or treated opportunistic infections. Immune reconstitution to cerebral Cryptococcus is poorly understood and can be fatal. Case Presentation. A 33-year-old Zimbabwean female presented with cryptococcal meningitis and newly diagnosed HIV with a CD4 count of 51 cells/ μ L (4%). She was treated with amphotericin and flucytosine. Combined antiretroviral therapy was started four weeks later and she showed early improvement. However, over the ensuing 18 months, her clinical course was marked by periodic worsening with symptoms resembling cryptococcal meningitis despite having achieved CD4 counts ≥400 cells/ μ L. Although initially treated for relapsing cryptococcal immune reconstitution syndrome, a brain biopsy taken 17 months after initial presentation showed budding Cryptococci. Conclusion. This unusually protracted case highlights the difficulties in differentiating relapsing cryptococcal meningitis from immune reconstitution and raises questions concerning the optimum timing of initiation of combined antiretroviral therapy in such patients.Entities:
Year: 2014 PMID: 24716014 PMCID: PMC3970336 DOI: 10.1155/2014/164826
Source DB: PubMed Journal: Case Rep Neurol Med ISSN: 2090-6676
Figure 1(a) MRI brain 5 days into admission in August 2005 showing right-sided occipitoparietal leptomeningeal inflammation. (b) MRI brain on readmission December 2005, 4 months after initial presentation showing worsening right-sided occipitoparietal leptomeningeal inflammation. (c) T2-weighted MRI brain in December 2006, 16 months after initial presentation showing large clusters of ring-enhancing lesions and leptomeningeal inflammation in the right occipitoparietal area with oedema and midline shift. Also seen but not shown on this cross-section were smaller clustered ring-enhancing lesions in the right thalamus and left frontal and temporal lobes.
The patient's relapsing clinical course with setting, symptoms, signs, investigations, imaging, and treatment choices.
| Months after 1st presentation | Presenting complaint and potential precipitant | LP results | HIV parameters | MRI results | Brain biopsy | Treatment and length of stay |
|---|---|---|---|---|---|---|
| 3 | Fever and meningism | ↑OP/lymphocytes/protein | CD4 76 cells/ | — | — | Fluconazole changed to itraconazole due to MIC |
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| 4 | Two focal seizures with secondary generalization. New neurological signs: RUL spastic catch, BL lower limb spasticity and ↑right plantar | ↑OP/lymphocytes/protein | CD4 67 cells/ | Worsening right occipito-parietal focal meningeal inflammation ( | Reactive gliosis and focally distended perivascular spaces containing cryptococcus ( | Itraconazole dose increased and prednisolone reinstated |
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| 8 | Asymptomatic | — | CD4 190 cells/ | — | — | Itraconazole changed to fluconazole |
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| 15 | Non-attendance at clinic | — | CD4 473 cells/ | — | — | Fluconazole not restarted at this point |
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| 16 | Left-sided focal motor seizures with secondary generalization | — | — | — | — | Lamotrigine increased and clobazam added to anti-epileptic regimen |
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| 17 | Headache, nausea and increasing unsteadiness | First: ↑lymphocyte count (88/cu mm)/↑protein | CD4 560 cells/ | Large clusters of ring-enhancing lesions and leptomeningeal inflammation in R occipito-parietal area with oedema and midline shift. Smaller clustered ring-enhancing lesions in R thalamus and L frontal and temporal lobes ( | Brain biopsy showed cryptococcal, encapsulated, budding yeast forms, scattered singly with some surrounding necrosis and moderate chronic inflammation | Ambisome 3 mg/kg once daily, flucytosine and high dose dexamethasone commenced |
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| 40 | Full resolution of neurological symptoms | — | — | Resolution of MRI features | — | Self-discontinued fluconazole. Since discharge developed steroid-induced DM and avascular necrosis |
Abbreviations: VL: viral load; L: left; R: right; BL: bilateral; ↑: raised above normal values; CNS: entral nervous system; DM: diabetes mellitus; CRAG: cryptococcal antigen; —: not performed.
Figure 2(a) Brain biopsy taken in December 2005, 4 months after initial presentation showing reactive gliosis and focally distended perivascular spaces containing Cryptococcus. (b) Brain biopsy taken in December 2006, 16 months after initial presentation showing encapsulated, budding yeast forms, scattered singly with some surrounding necrosis and moderate chronic inflammation. No granulomata were seen.