JC Virus Infection of the Brain

Typical infratentorial cPML in another HIV-positive patient classically involving the middle cerebellar peduncle (left). A and B, This lesion also has diffusion restriction at the anterolateral advancing edge (high DWI signal intensity and low ADC value, arrows) and diffusion facilitation at the center as evidenced by the DWI (A) and the ADC map (B). C and D, The lesion shows typical hypointensity on the T1-weighted sequence (C) and hyperintensity on FLAIR (D). Note, there are no mass effect. There is no enhancement in the postcontrast T1-weighted sequence (E).

There is an incomplete rim of T1 hyperintensity (arrows) at the advancing edges of the supratentorial (A) and infratentorial (B) cPML lesions.

Progression of cPML. A and B, These FLAIR images, 4 months apart, from an HIV-positive patient with cPML demonstrate typical progression of the supratentorial white matter FLAIR hyperintensity.

A, Intralesional microcyst on T2-weighted sequence on the left parietal cPML lesion in an HIV-positive patient, zoomed up in the inset. The arrow points to a microcyst. B, There are 2 intralesional microcysts (arrows) in this right fronto-parietal cPML lesion in another HIV-positive patient.

Typical disease course of cPML in an HIV-positive patient receiving HAART. Top panel, a set of images at presentation with focal diffusion restriction (A and B) and very subtle but typical hypointensity on T1 (C) and hyperintensity on FLAIR (D). This initial study was confused with acute subcortical infarction. Middle panel, a set of images 1 month after the initial presentation. No HAART was administered before this scanning. Now the lesion has enlarged in size with typical diffusion restriction (arrows) at the medial and posterior advancing edges (E and F). Now the T1 hypointensity is more obvious (G). The adjacent cortex is not involved (arrows). Typically the lesion is hyperintense on FLAIR (H). Bottom panel, a set of images 19 months after initial presentation. The patient received HAART for 18 months. Now there is no diffusion restriction (I). On the T1-weighted sequence (J), there is profound T1 hypointensity associated with new/progressive atrophy. There is FLAIR hyperintensity in the adjacent areas. However, the main lesion is not hyperintense on FLAIR (K). On T2 (L), the lesion itself is very hyperintense compared with the adjacent white matter, suggesting cystic encephalomalacia. Note that the adjacent cortical architecture is preserved.