Creutzfeldt-Jakob dementia

1. Instituto Estadual do Cerebro Paulo Niemeyer, Rio de Janeiro, RJ,Brazil. 2. Hospital Casa de Portugal / 3D Diagnostico por Imagem, Riode Janeiro, RJ, Brazil. 3. Universidade Federal do Rio de Janeiro (UFRJ),Rio de Janeiro, RJ, Brazil. Mailing Address: Dr. Bruno Niemeyer deFreitas Ribeiro. Instituto Estadual do Cerebro Paulo Niemeyer – Ser-vico de Radiologia. Rua do Rezende, 156, Centro. Rio de Janeiro, RJ,Brazil, 20231-092. E-mail: bruno.niemeyer@hotmail.com.


Dear Editor,
A 72-year-old woman with rapidly progressive dementia, behavioral changes and apraxia of gait for seven months, extrapyramidal signs and diffuse myoclonus. Electroencephalography dem-onstrated periodic electric activity with high amplitude acute phase waves diffusely distributed over the cortex. The cerebrospinal fluid was normal. Magnetic resonance imaging (MRI) was performed ( Figure 1).
The association of clinical, radiological, electroencephalic or cerebrospinal fluid findings (presence of 14-3-3 brain protein in diseased patient for less than two years -absent in this case), Figure 1. A: Axial magnetic resonance imaging of the skull demonstrating foci of hypersignal at diffusion-weighted sequences in the heads of the caudate nuclei, putamina, thalami and medial occipitotemporal gyri. B: At the ADC mapping, the low signal intensity in the same region confirms the diffusion restriction.

A B
allows for a probable diagnosis of Creutzfeldt-Jakob dementia (CJD). The differential diagnosis is made with other diseases associated with dementias, as follows: a) Alzheimer's disease, that does not present with alterations observed at diffusion-weighted images; b) vascular dementia, with multiple infarcts, but with abnormalities at diffusion-weighted images only in cases of recent infarcts, and without diffuse cortical involvement; c) other encephalopathies that present alterations restricted to the cortex at diffusion-weighted images (such as MELAS -mitochondrial myopathy, encephalopathy, lactic acidosis and stroke-like episodes -a genetic metabolic disease occurring in younger patients); venous hypertensive encephalopathy and chronic herpes simplex encephalitis. CJD is a subacute spongiform encephalopathy that presents with rapidly progressive dementia, and is the most frequent among rare prion diseases. Myoclonus, pyramidal, extrapyramidal and cerebellar signs are associated. Psychiatric symptoms are observed at the first six months; and progressive immobility, cortical blindness, dysphagia and mutism constitute late signs of the disease. Death generally occurs one year after the symptoms onset, since there is no therapy to prevent a fatal outcome (1) . The disease is subdivided into sporadic (85% of cases), familial, iatrogenic and a less common, recently described variant related to epidemic bovine spongiform encephalopathy (2) .
Like in other acute encephalopathies, the 14-3-3 brain protein may be present in the cerebrospinal fluid. Encephalography may demonstrate periodic activity composed of three-phase highfrequency waves over attenuated background activity.
At MRI, hyperintense signal is observed in the basal ganglia, putamen and later in the cerebral cortex on T2-weighted and FLAIR sequences (1,3) . Such alterations suggest CJD, more than any other dementia disorder (4) .
At early stages of the disease, however, conventional imaging studies may present normal results. Diffusion-weighted sequences may favor an early diagnosis, demonstrating abnormal hyperintense foci even before the appearance of electroencephalographic alterations, and should be performed in case of suspicion of CJD (1,4,5) . Diffusion restriction is observed, probably in association with the cytotoxic edema secondary to spongiform degeneration and to accumulation of abnormal cytoplasmic vacuoles. As the disease progresses, global atrophy is observed and, in general, this is the only alteration depicted at computed tomography (1,4,6) .
Histopathological analysis (Figure 2A) demonstrated spongiform alterations with variable intensity in the neuropil, markedly in the caudate nucleus, putamen, and in the region CA1 of the hippocampus, moderately in the frontal and temporal cortices, and slightly in the parietal and occipital cortices. Immunohistochemical analysis demonstrated gliosis ( Figure 2B). Such results are compatible with a definite diagnosis of CJD. The lesions distribution, the absence of similar cases in the family, and the absence of a known infectious source are compatible com the sporadic presentation of the disease (4,7) . Such a diagnosis is relevant for controlling the transmission and to rule out treatable causes of dementia (1,8) .