Table 1.
Patient data for brain samples.
| Case | Group | Sex | Age at death | PMI (hours) | Clinical Diagnosis | Primary Path Diagnosis* | Other Path Diagnosis** |
|---|---|---|---|---|---|---|---|
| 1 | Ctrl | F | 86 | 6.4 | Control | N/A | AGD, limbic; VBI |
| 2 | Ctrl | F | 81 | 30.3 | MCI, amnestic | PART | None |
| 3 | Ctrl | M | 76 | 8.2 | Control | N/A | AGD, limbic |
| 4 | Ctrl | M | 77 | 4.9 | MCI, executive | AGD | VBI, microinfarct in cerebellar folia |
| 5 | Ctrl | F | 86 | 7.8 | Control | N/A | VBI, microinfarcts in claustrum and angular gyrus; AGD |
| 6 | GRN | M | 66 | 10.1 | DLB, ?bvFTD | LBD | Incipient FTLD‐TDP‐A |
| 7 | GRN | M | 72 | 23.8 | PPA‐mixed | FTLD‐TDP‐A | Subdural hematoma |
| 8 | GRN | M | 74 | 30.9 | nfvPPA, CBS | FTLD‐TDP‐A | None |
| 9 | GRN | F | 73 | 20.7 | nfvPPA, CBS | FTLD‐TDP‐A | None |
| 10 | GRN | F | 66 | 7.4 | bvFTD | FTLD‐TDP‐A | None |
| 11 | GRN | M | 64 | 7.2 | bvFTD | FTLD‐TDP‐A | None |
| 12 | GRN | F | 70 | 9.1 | PPA, unspecified | FTLD‐TDP‐A | Hippocampal Sclerosis, VBI, ischemic infarct |
| 13 | GRN | F | 56 | 7.6 | bvFTD | FTLD‐TDP‐A | None |
| 14 | GRN | F | 78 | 19 | mixed FTD | FTLD‐TDP‐A | None |
| 15 | GRN | F | 66 | 17.1 | bvFTD | FTLD‐TDP‐A | None |
| 16 | GRN | F | 64 | 10.5 | CBS | FTLD‐TDP‐A | None |
| 17 | GRN | M | 72 | 7.2 | AD | AD, FTLD‐TDP‐A? | Hippocampal Sclerosis |
| 18 | GRN | F | 69 | 11 | bvFTD | FTLD‐TDP‐A | Pre‐Hippocampal Sclerosis |
AGD, argyrophilic grain disease; CAA, Cerebral amyloid angiopathy; CBS, Corticobasal syndrome; DLB, dementia with Lewy bodies; LBD, Lewy body disease; MCI, Mild cognitive impairment; nfv, nonfluent variant; PART, Primary age‐related tauopathy; PMI, post mortem interval, PPA, Primary progressive aphasia; VBI, Vascular brain injury.
*
Disease considered most likely to explain the clinical syndrome.
**
No control subject had limbic TDP‐43 proteinopathy.