HMB440H1 Lecture Notes - Lecture 8: C9Orf72, Alternative Splicing, Wound Healing

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12 Apr 2019
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Lecture 8: genetics of frontotemporal dementia (ftd) and. The strongest risk factor for ftd and als is increasing age and family history (10-20% of cases are familial) Ftd and als are linked by common pathogenic pathways: ftd behavioral problems (e. g. social disinhibition), speech problems, and shrinkage of the frontal & temporal lobes, als voluntary movement problems (e. g. talking, walking, breathing, etc. ) & the loss of motor neurons in the: m1, brain stem & spinal cord. 50% of als cases have frontal cognitive impairment and tdp-43 inclusions detected in most als & ftd cases (i. e. overlapping genes and symptoms) There are 3 ftd loci detected by linkage studies on chromosome 17, 3, and 9 this is microtubule associated protein tau (mapt) gene: contributes to 10% of familial ftd, correlated with tau +ve inclusions. The tau/mapt gene generates six main isoforms as result of the alternative spicing of exons 2, 3, & 10.

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