Frequency and clinical characteristics of progranulin mutation carriers in the Manchester frontotemporal lobar degeneration cohort: comparison with patients with MAPT and no known mutations

doi:10.1093/brain/awm331

Brain Advance Access published online on January 11, 2008
Brain, doi:10.1093/brain/awm331

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Frequency and clinical characteristics of progranulin mutation carriers in the Manchester frontotemporal lobar degeneration cohort: comparison with patients with MAPT and no known mutations

Stuart M. Pickering-Brown¹, Sara Rollinson¹, Daniel Du Plessis², Karen E. Morrison³, Anoop Varma¹^,2, Anna M. T. Richardson¹^,2, David Neary¹^,2, Julie S. Snowden¹^,2 and David M. A. Mann¹^,2

¹Clinical Neuroscience Research Group, Faculty of Medical and Human Sciences, University of Manchester, Oxford Rd, Manchester M13 9PT, ²Greater Manchester Neurosciences Centre, Hope Hospital, Salford Royal Hospitals NHS Foundation Trust, Salford M6 8HD and ³Department of Clinical Neurosciences, Division of Neuroscience, The Medical School, University of Birmingham, Edgbaston, Birmingham B15 2TT and Queen Elizabeth Hospital, University Hospitals Birmingham NHS Foundation Trust, Birmingham B15 2TH, UK

Correspondence to: Dr Stuart Pickering-Brown, Clinical Neuroscience Research Group, Faculty of Medical and Human Sciences, University of Manchester, Oxford Rd, Manchester M13 9PT, UK E-mail: SPB{at}Manchester.ac.uk

Two hundred and twenty-three consecutive patients fulfillingclinical diagnostic criteria for frontotemporal lobar degeneration(FTLD), and 259 patients with motor neuron disease (MND), forwhom genomic DNA was available, were investigated for the presenceof mutations in tau (MAPT) and progranulin (PGRN) genes. AllFTLD patients had undergone longitudinal neuropsychologicaland clinical assessment, and in 44 cases, the diagnosis hadbeen pathologically confirmed at post-mortem. Six differentPGRN mutations were found in 13 (6%) patients with FTLD. Fourapparently unrelated patients shared exon Q415X 10 stop codonmutation. However, genotyping data revealed all four patientsshared common alleles of 15 SNPs from rs708386 to rs5848, defininga 45.8-kb haplotype containing the whole PGRN gene, suggestingthey are related. Three patients shared exon 11 R493X stop codonmutation. Four patients shared exon 10 V452WfsX38 frameshiftmutation. Two of these patients were siblings, though not apparentlyrelated to the other patients who in turn appeared unrelated.One patient had exon 1 C31LfsX34 frameshift mutation, one hadexon 4 Q130SfsX130 frameshift mutation and one had exon 10 Q468Xstop codon mutation. In addition, two non-synonymous changeswere detected: G168S change in exon 5 was found in a singlepatient, with no family history, who showed a mixed FTLD/MNDpicture and A324T change in exon 9 was found in two cases; onecase of frontotemporal dementia (FTD) with a sister with FTD+MNDand the other in a case of progressive non-fluent aphasia (PNFA)without any apparent family history. MAPT mutations were foundin 17 (8%) patients. One patient bore exon 10 + 13 splice mutation,and 16 patients bore exon 10 + 16 splice mutation. When PGRNand MAPT mutation carriers were excluded, there were no significantdifferences in either the allele or genotype frequencies, orhaplotype frequencies, between the FTLD cohort as a whole, orfor any clinical diagnostic FTLD subgroup, and 286 controlsor between MND cases and controls. However, possession of theA allele of SNP rs9897526, in intron 4 of PGRN, delayed meanage at onset by $~$ 4 years. Patients with PGRN and MAPT mutationsdid not differ significantly from other FTLD cases in termsof gender distribution or total duration of illness. However,a family history of dementia in a first-degree relative wasinvariably present in MAPT cases, but not always so in PGRNcases. Onset of illness was earlier in MAPT cases compared toPGRN and other FTLD cases. PNFA, combined with limb apraxiawas significantly more common in PGRN mutation cases than otherFTLD cases. By contrast, the behavioural disorder of FTD combinedwith semantic impairment was a strong predictor of MAPT mutations.These findings complement recent clinico-pathological findingsin suggesting identifiable associations between clinical phenotypeand genotype in FTLD.

Key Words: progranulin; tau; MAPT; progressive non-fluent aphasia; apraxia; frontotemporal dementia; genetics

Abbreviations: ALS, amyotrophic lateral sclerosis; CBD, corticobasal degeneration; FTD, frontotemporal dementia; FTLD, frontotemporal lobar degeneration; MND, motoneuron; NCI, neuronal cytoplasmic inclusions; NII, neuronal intranuclear inclusions; NMD, nonsense-mediated decay; PAX, apraxia; PNFA, progressive non-fluent aphasia; SD, semantic dementia.

Received October 3, 2007. Revised December 5, 2007. Accepted December 14, 2007.

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