Cerebral amyloid angiopathy.

To cite: Sharma N, Vyas S. BMJ Case Rep Published online: [please include Day Month Year] doi:10.1136/ bcr-2013-201558 DESCRIPTION A 72-year-old man presented with headache, vomiting and diminution of vision. There was no history of smoking, diabetes mellitus, hypertension or use of aspirin or recreational drugs. The general physical examination, pulse, blood pressure, chest and cardiovascular examination were normal. On central nervous system examination, the visual acuity was reduced to perception of light at 6 m and pupils were 3 mm and reacting to light. Tests for cerebellar functions showed dysdiadochokinesia and impaired tandem walking. Blood investigations were normal and the axial MRI of the head disclosed a right occipital haematoma (figure 1) and other changes of probable cerebral amyloid angiopathy (figures 2 and 3). Cerebral amyloid angiopathy (CAA) accounts for 15% of all non-traumatic intracerebral haemorrhage in persons greater than 60 years. 2 In people above 70 years, it accounts for 50% of all lobar haematomas. CAA and CAA-related intracranial haemorrhage are also common in elderly individuals with Alzheimer’s disease and Down syndrome. Histopathologically, the deposition of β-amyloid material occurs in the walls of medium and small arteries mainly in the parietal and occipital lobes. 2 The amyloid deposit in the media can be extensive as to cause necrosis of the vessel wall, microaneurysm formation and lobar haemorrhage. The Boston Criteria were proposed in 1990 to standardise the definition of CAA. They comprise of clinical, imaging and pathological criteria. According to these criteria, probable CAA is diagnosed in patients older than 55 years with appropriate clinical history and MRI findings demonstrating multiple haemorrhages limited to lobar, cortical, corticosubcortical region of varying sizes and ages (cerebellar haemorrhages allowed) with no other explanation. Patients of CAA may present with neuroimaging evidence of small subclinical bleed called microbleeds. Gradient-echo (GRE) MRI sequences can demonstrate small haemorrhagic lesions which are not seen on T1-weighted and T2-weighted images. 2 GRE sequences are broadly divided into coherent and incoherent or spoiled sequences. For detecting microbleeds, T2 GRE images and SWI (susceptibility weighted imaging) are used. SWI are high-resolution, three-dimensional, fully velocity compensated GRE sequences and are currently the gold standard for the evaluation of haemorrhagic lesions. Cerebral microbleeds are not pathognomonic of CAA and can also be detected in 5–23% of older individuals in population-based studies. 4 In the Rotterdam cohort, microbleeds were more prevalent among those on antiplatelet therapy. Another study has suggested that microbleeds arise from amyloid-based pathology. Microbleeds also occur in hypertensive microangiopathy in the basal ganglia and thalamus and infective endocarditis generally in anatomic locations different from CAA. In patients of CAAwith primary lobar haematoma, the