Advanced intimal hyperplasia without luminal narrowing of leptomeningeal arteries in CADASIL.

[cadasil]

Leptomeningeal artery abnormalities in Cerebral Autosomal-Dominant Arteriopathy with Subcortical Infarcts and Leukoencephalopathy (CADASIL ) have not been extensively characterized . We quantified substructure and diameter of leptomeningeal arteries in CADASIL compared with age-matched controls and the very old ; in addition , we characterized intimal thickening in CADASIL using immunohistochemistry .Frontal and temporal cortex of 6 genetically proven CADASIL brains (average age , 66 years ), 6 controls without symptoms of cerebrovascular disease , and 6 very old brains (average age , 89 years ) were examined for leptomeningeal artery intimal , medial , and adventitial thickness ; inner diameter ; and sclerotic index and for smooth muscle markers .T he intima of CADASIL arteries was thickened 5 -fold compared with controls and the very aged (P <0 .0001 ). Medial thickness was lower in CADASIL compared with controls and the very old (P <0 .01 ). The adventitia was not significantly increased in CADASIL compared with age-matched controls . Arterial diameters were not smaller in CADASIL compared with controls . Sclerotic index was significantly increased in CADASIL compared with other groups (P <0 .00001 ). Intimal cells in CADASIL expressed smooth muscle actin , S 100 A 4 , and vimentin but not desmin .Principle changes of leptomeningeal arteries in CADASIL include intimal thickening and medial thinning , but not luminal narrowing . Smooth muscle -like cells participate in neointimal thickening of CADASIL arteries .