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Aug 2012, Vol 69, No. 8 >

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Original Contribution | Aug 2012

Frontotemporal Dementia in Elderly Individuals

Atik Baborie, MD; Tim D. Griffiths, DM; Evelyn Jaros, PhD; Parastoo Momeni, PhD; Ian G. McKeith, MD; David J. Burn, MD; G. Keir, PhD; Andrew J. Larner, MD; David M. Mann, PhD; Robert Perry, MD
Arch Neurol. 2012;69(8):1052-1060. doi:10.1001/archneurol.2011.3323.
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Objective  To determine whether cases of frontotemporal lobar degeneration (FTLD) do exist in elderly individuals and have clinical and neuropathological features distinct from those with presenile onset.

Design  Retrospective matched cohort study.

Setting  Regional Neuroscience Centre, North East England.

Patients  We compared clinicopathological features of 11 cases of FTLD in elderly individuals with 19 cases of presenile-onset FTLD.

Results  Retrospective case note analysis showed that most elderly patients with FTLD had behavioral features consistent with orbitofrontal and basofrontal involvement, similar to presenile-onset FTLD, though symptomatic memory loss was present in 91% (10 of 11) of elderly patients with FTLD compared with only 36% (7 of 19) of patients with presenile-onset FTLD. Neuropathologically, the group of elderly patients with FTLD comprised 7 with FTLD–TDP-43, 1 with ubiquitin-positive FTLD, 2 with FTLD-tau/Pick disease, and 1 with FTLD-tau/neurofibrillary tangle–predominant dementia with TDP-43, a composition similar to presenile-onset FTLD. However, hippocampal sclerosis was more common in elderly patients with FTLD than patients with presenile-onset FTLD (82% vs 37%) and more severe in elderly patients with FTLD (P < .05). By contrast, severe atrophy of the frontal and temporal lobes was less common in elderly patients with FTLD (frontal: 45%; temporal: 27%) than patients with presenile-onset FTLD (frontal: 63%; temporal: 78%). Elderly patients with FTLD represented 3.2% of all elderly patients with dementia autopsied at Newcastle General Hospital.

Conclusions  Frontotemporal lobar degeneration in elderly patients does exist as a separate entity from presenile-onset FTLD. Its main features include (1) clinically frequent memory loss and behavioral change predominating over language and semantic dysfunction and (2) neuropathologically prominent hippocampal sclerosis but less pronounced cortical lobar atrophy. Clinically, FTLD in elderly patients is underrecognized and should be considered in the elderly subjects presenting with an “atypical Alzheimer disease” phenotype.
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Figure 1. Frequency distributions of severity of macroscopic atrophy in the frontal and temporal lobes of patients with presenile-onset frontotemporal lobar degeneration (FTLDp) and elderly patients with frontotemporal lobar degeneration (FTLDe). Severity of atrophy: 0 = not visible, 1 = mild, 2 = moderate, 3 = moderately severe, 4 = very severe. n = number of cases where data available. *Statistically significant difference in temporal lobe atrophy between FTLDe and FTLDp (χ2 = 5.86; P < .02).

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Figure 2. Frequency distributions of severity of microscopic atrophy (neuronal loss) in the frontal and temporal lobes and hippocampal sclerosis (HS) of patients with presenile-onset frontotemporal lobar degeneration (FTLDp) and elderly patients with frontotemporal lobar degeneration (FTLDe). Severity of atrophy: 0 = not visible, 1 = mild, 2 = moderate, 3 = moderately severe, 4 = very severe. n = number of cases where data available. *Hippocampal sclerosis was significantly different between FTLDe and FTLDp (χ2 = 4.63; P < .05). LMB indicates lower midbrain; SN, substantia nigra; UMB, upper midbrain.

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Country-Specific Mortality and Growth Failure in Infancy and Yound Children and Association With Material Stature

Use interactive graphics and maps to view and sort country-specific infant and early dhildhood mortality and growth failure data and their association with maternal

References

Correspondence

Submit a Letter
March 1, 2013
Elderly Individuals With FTLD
Kurt A. Jellinger, MD
JAMA Neurol. 2013;70(3):412-413. doi:10.1001/2013.jamaneurol.552.
March 1, 2013
Elderly Individuals With FTLD
Atik Baborie, MD; Tim D. Griffiths, DM; Evelyn Jaros, PhD; Parastoo Momeni, PhD; Ian G. McKeith, MD; David J. Burn, MD; G. Keir, PhD; Andrew J. Larner, MD; David M. Mann, PhD; Robert Perry, MD
JAMA Neurol. 2013;70(3):412-413. doi:10.1001/jamaneurol.2013.1649.
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