CADASIL and CARASIL.

[cadasil]

CADASIL and CARASIL are hereditary small vessel diseases leading to vascular dementia . CADASIL commonly begins with migraine followed by minor strokes in mid-adulthood . Dominantly inherited CADASIL is caused by mutations (n â€‰>â€‰230 ) in NOTCH 3 gene , which encodes Notch 3 receptor expressed in vascular smooth muscle cells (VSMC ). Notch 3 extracellular domain (N 3 ECD ) accumulates in arterial walls followed by VSMC degeneration and subsequent fibrosis and stenosis of arterioles , predominantly in cerebral white matter , where characteristic ischemic MRI changes and lacunar infarcts emerge . The likely pathogenesis of CADASIL is toxic gain of function related to mutation -induced unpaired cysteine in N 3 ECD . Definite diagnosis is made by molecular genetics but is also possible by electron microscopic demonstration of pathognomonic granular osmiophilic material at VSMCs or by positive immunohistochemistry for N 3 ECD in dermal arteries . In rare , recessively inherited CARASIL the clinical picture and white matter changes are similar as in CADASIL , but cognitive decline begins earlier . In addition , gait disturbance , low back pain and alopecia are characteristic features . CARASIL is caused by mutations (presently n â€‰=â€‰10 ) in high -temperature requirement . A serine peptidase 1 (HTRA 1 ) gene , which result in reduced function of HTRA 1 as repressor of transforming growth factor -Î² (TGF Î² ) -signaling . Cerebral arteries show loss of VSMCs and marked hyalinosis , but not stenosis .