Mutations in progranulin are a major cause of ubiquitin-positive frontotemporal lobar degeneration

Jennifer Gass; Ashley Cannon; Ian R. Mackenzie; Bradley Boeve; Matt Baker; Jennifer Adamson; Richard Crook; Stacey Melquist; Karen Kuntz; Ron Petersen; Keith Josephs; Stuart M. Pickering-Brown; Neill Graff-Radford; Ryan Uitti; Dennis Dickson; Zbigniew Wszolek; John Gonzalez; Thomas G. Beach; Eileen Bigio; Nancy Johnson; Sandra Weintraub; Marsel Mesulam; Charles L. White; Bryan Woodruff; Richard Caselli; Ging Yuek Hsiung; Howard Feldman; Dave Knopman; Mike Hutton; Rosa Rademakers

doi:10.1093/hmg/ddl241

Mutations in progranulin are a major cause of ubiquitin-positive frontotemporal lobar degeneration

Jennifer Gass, Ashley Cannon, Ian R. Mackenzie, Bradley Boeve, Matt Baker, Jennifer Adamson, Richard Crook, Stacey Melquist, Karen Kuntz, Ron Petersen, Keith Josephs, Stuart M. Pickering-Brown, Neill Graff-Radford, Ryan Uitti, Dennis Dickson, Zbigniew Wszolek, John Gonzalez, Thomas G. Beach, Eileen Bigio, Nancy JohnsonSandra Weintraub, Marsel Mesulam, Charles L. White, Bryan Woodruff, Richard Caselli, Ging Yuek Hsiung, Howard Feldman, Dave Knopman, Mike Hutton, Rosa Rademakers

Research output: Contribution to journal › Article › peer-review

499 Scopus citations

Abstract

Null mutations in the progranulin gene (PGRN) were recently reported to cause tau-negative frontotemporal dementia linked to chromosome 17. We assessed the genetic contribution of PGRN mutations in an extended population of patients with frontotemporal lobar degeneration (FTLD) (N = 378). Mutations were identified in 10% of the total FTLD population and 23% of patients with a positive family history. This mutation frequency dropped to 5% when analysis was restricted to an unbiased FTLD subpopulation (N = 167) derived from patients referred to Alzheimer's Disease Research Centers (ADRC). Among the ADRC patients, PGRN mutations were equally frequent as mutations in the tau gene (MAPT). We identified 23 different pathogenic PGRN mutations, including a total of 21 nonsense, frameshift and splice-site mutations that cause premature termination of the coding sequence and degradation of the mutant RNA by nonsense-mediated decay. We also observed an unusual splice-site mutation in the exon 1 5′ splice site, which leads to loss of the Kozac sequence, and a missense mutation in the hydrophobic core of the PGRN signal peptide. Both mutations revealed novel mechanisms that result in loss of functional PGRN. One mutation, c.1477C>T (p.Arg493X), was detected in eight independently ascertained familial FTLD patients who were shown to share a common extended haplotype over the PGRN genomic region. Clinical examination of patients with PGRN mutations revealed highly variable onset ages with language dysfunction as a common presenting symptom. Neuropathological examination showed FTLD with ubiquitin-positive cytoplasmic and intranuclear inclusions in all PGRN mutation carriers.

Original language	English (US)
Pages (from-to)	2988-3001
Number of pages	14
Journal	Human molecular genetics
Volume	15
Issue number	20
DOIs	https://doi.org/10.1093/hmg/ddl241
State	Published - Oct 15 2006

ASJC Scopus subject areas

Molecular Biology
Genetics
Genetics(clinical)

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10.1093/hmg/ddl241

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Gass, J., Cannon, A., Mackenzie, I. R., Boeve, B., Baker, M., Adamson, J., Crook, R., Melquist, S., Kuntz, K., Petersen, R., Josephs, K., Pickering-Brown, S. M., Graff-Radford, N., Uitti, R., Dickson, D., Wszolek, Z., Gonzalez, J., Beach, T. G., Bigio, E., ... Rademakers, R. (2006). Mutations in progranulin are a major cause of ubiquitin-positive frontotemporal lobar degeneration. Human molecular genetics, 15(20), 2988-3001. https://doi.org/10.1093/hmg/ddl241

Gass, J, Cannon, A, Mackenzie, IR, Boeve, B, Baker, M, Adamson, J, Crook, R, Melquist, S, Kuntz, K, Petersen, R, Josephs, K, Pickering-Brown, SM, Graff-Radford, N, Uitti, R, Dickson, D, Wszolek, Z, Gonzalez, J, Beach, TG, Bigio, E, Johnson, N, Weintraub, S, Mesulam, M, White, CL, Woodruff, B, Caselli, R, Hsiung, GY, Feldman, H, Knopman, D, Hutton, M & Rademakers, R 2006, 'Mutations in progranulin are a major cause of ubiquitin-positive frontotemporal lobar degeneration', Human molecular genetics, vol. 15, no. 20, pp. 2988-3001. https://doi.org/10.1093/hmg/ddl241

@article{b24c55d43da14451bf0b773a02ecb020,

title = "Mutations in progranulin are a major cause of ubiquitin-positive frontotemporal lobar degeneration",

abstract = "Null mutations in the progranulin gene (PGRN) were recently reported to cause tau-negative frontotemporal dementia linked to chromosome 17. We assessed the genetic contribution of PGRN mutations in an extended population of patients with frontotemporal lobar degeneration (FTLD) (N = 378). Mutations were identified in 10% of the total FTLD population and 23% of patients with a positive family history. This mutation frequency dropped to 5% when analysis was restricted to an unbiased FTLD subpopulation (N = 167) derived from patients referred to Alzheimer's Disease Research Centers (ADRC). Among the ADRC patients, PGRN mutations were equally frequent as mutations in the tau gene (MAPT). We identified 23 different pathogenic PGRN mutations, including a total of 21 nonsense, frameshift and splice-site mutations that cause premature termination of the coding sequence and degradation of the mutant RNA by nonsense-mediated decay. We also observed an unusual splice-site mutation in the exon 1 5′ splice site, which leads to loss of the Kozac sequence, and a missense mutation in the hydrophobic core of the PGRN signal peptide. Both mutations revealed novel mechanisms that result in loss of functional PGRN. One mutation, c.1477C>T (p.Arg493X), was detected in eight independently ascertained familial FTLD patients who were shown to share a common extended haplotype over the PGRN genomic region. Clinical examination of patients with PGRN mutations revealed highly variable onset ages with language dysfunction as a common presenting symptom. Neuropathological examination showed FTLD with ubiquitin-positive cytoplasmic and intranuclear inclusions in all PGRN mutation carriers.",

author = "Jennifer Gass and Ashley Cannon and Mackenzie, {Ian R.} and Bradley Boeve and Matt Baker and Jennifer Adamson and Richard Crook and Stacey Melquist and Karen Kuntz and Ron Petersen and Keith Josephs and Pickering-Brown, {Stuart M.} and Neill Graff-Radford and Ryan Uitti and Dennis Dickson and Zbigniew Wszolek and John Gonzalez and Beach, {Thomas G.} and Eileen Bigio and Nancy Johnson and Sandra Weintraub and Marsel Mesulam and White, {Charles L.} and Bryan Woodruff and Richard Caselli and Hsiung, {Ging Yuek} and Howard Feldman and Dave Knopman and Mike Hutton and Rosa Rademakers",

year = "2006",

month = oct,

day = "15",

doi = "10.1093/hmg/ddl241",

language = "English (US)",

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T1 - Mutations in progranulin are a major cause of ubiquitin-positive frontotemporal lobar degeneration

AU - Gass, Jennifer

AU - Cannon, Ashley

AU - Mackenzie, Ian R.

AU - Boeve, Bradley

AU - Baker, Matt

AU - Adamson, Jennifer

AU - Crook, Richard

AU - Melquist, Stacey

AU - Kuntz, Karen

AU - Petersen, Ron

AU - Josephs, Keith

AU - Pickering-Brown, Stuart M.

AU - Graff-Radford, Neill

AU - Uitti, Ryan

AU - Dickson, Dennis

AU - Wszolek, Zbigniew

AU - Gonzalez, John

AU - Beach, Thomas G.

AU - Bigio, Eileen

AU - Johnson, Nancy

AU - Weintraub, Sandra

AU - Mesulam, Marsel

AU - White, Charles L.

AU - Woodruff, Bryan

AU - Caselli, Richard

AU - Hsiung, Ging Yuek

AU - Feldman, Howard

AU - Knopman, Dave

AU - Hutton, Mike

AU - Rademakers, Rosa

PY - 2006/10/15

Y1 - 2006/10/15

N2 - Null mutations in the progranulin gene (PGRN) were recently reported to cause tau-negative frontotemporal dementia linked to chromosome 17. We assessed the genetic contribution of PGRN mutations in an extended population of patients with frontotemporal lobar degeneration (FTLD) (N = 378). Mutations were identified in 10% of the total FTLD population and 23% of patients with a positive family history. This mutation frequency dropped to 5% when analysis was restricted to an unbiased FTLD subpopulation (N = 167) derived from patients referred to Alzheimer's Disease Research Centers (ADRC). Among the ADRC patients, PGRN mutations were equally frequent as mutations in the tau gene (MAPT). We identified 23 different pathogenic PGRN mutations, including a total of 21 nonsense, frameshift and splice-site mutations that cause premature termination of the coding sequence and degradation of the mutant RNA by nonsense-mediated decay. We also observed an unusual splice-site mutation in the exon 1 5′ splice site, which leads to loss of the Kozac sequence, and a missense mutation in the hydrophobic core of the PGRN signal peptide. Both mutations revealed novel mechanisms that result in loss of functional PGRN. One mutation, c.1477C>T (p.Arg493X), was detected in eight independently ascertained familial FTLD patients who were shown to share a common extended haplotype over the PGRN genomic region. Clinical examination of patients with PGRN mutations revealed highly variable onset ages with language dysfunction as a common presenting symptom. Neuropathological examination showed FTLD with ubiquitin-positive cytoplasmic and intranuclear inclusions in all PGRN mutation carriers.

AB - Null mutations in the progranulin gene (PGRN) were recently reported to cause tau-negative frontotemporal dementia linked to chromosome 17. We assessed the genetic contribution of PGRN mutations in an extended population of patients with frontotemporal lobar degeneration (FTLD) (N = 378). Mutations were identified in 10% of the total FTLD population and 23% of patients with a positive family history. This mutation frequency dropped to 5% when analysis was restricted to an unbiased FTLD subpopulation (N = 167) derived from patients referred to Alzheimer's Disease Research Centers (ADRC). Among the ADRC patients, PGRN mutations were equally frequent as mutations in the tau gene (MAPT). We identified 23 different pathogenic PGRN mutations, including a total of 21 nonsense, frameshift and splice-site mutations that cause premature termination of the coding sequence and degradation of the mutant RNA by nonsense-mediated decay. We also observed an unusual splice-site mutation in the exon 1 5′ splice site, which leads to loss of the Kozac sequence, and a missense mutation in the hydrophobic core of the PGRN signal peptide. Both mutations revealed novel mechanisms that result in loss of functional PGRN. One mutation, c.1477C>T (p.Arg493X), was detected in eight independently ascertained familial FTLD patients who were shown to share a common extended haplotype over the PGRN genomic region. Clinical examination of patients with PGRN mutations revealed highly variable onset ages with language dysfunction as a common presenting symptom. Neuropathological examination showed FTLD with ubiquitin-positive cytoplasmic and intranuclear inclusions in all PGRN mutation carriers.

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Mutations in progranulin are a major cause of ubiquitin-positive frontotemporal lobar degeneration

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