Molecular characterization of novel progranulin (<i>GRN</i>) mutations in frontotemporal dementia

Mukherjee, Odity; Wang, Jun; Gitcho, Michael A.; Chakraverty, Sumi; Taylor‐Reinwald, Lisa; Shears, Shantia; Kauwe, John; Norton, Joanne; Levitch, Denise; Bigio, Eileen H.; Hatanpaa, Kimmo J.; White, Charles L.; Morris, John C.; Cairns, Nigel J.; Goate, Alison M.

doi:10.1002/humu.20681

Cited by 74 publications

(63 citation statements)

References 25 publications

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“…A total of 27 other mutations were observed more than once (Table 2). For nine of these mutations (p.A9D, p.C31LfsX35, p.G35EfsX19, p.T52HfsX2, p.G79DfsX39, p.S226WfsX28, p.V200GfsX18, p.Q415X, and p.R418X) haplotype sharing analysis supported a common genetic origin for each of them (Table 2) Le Ber et al, 2007;Mukherjee et al, 2008;Beck et al, 2008]. The 34 remaining mutations were reported in a single family.…”

Section: Grn Mutation Spectrum Null Mutationsmentioning

confidence: 83%

“…Families Dutch-III, Brescia-F071, Biv, and Seattle B segregated a frameshift mutation resulting in a PTC [Benussi et al, 2008;Bronner et al, 2007;Leverenz et al, 2007;Bruni et al, 2007]. In Family HDDD2, the disease was caused by a missense mutation (p.A9D) introducing a charged amino acid in the signal peptide, resulting in the mislocalization of the protein [Mukherjee et al, 2006[Mukherjee et al, , 2008, which was shown to lead to a decrease in secreted GRN protein [Mukherjee et al, 2008]. In the Kertesz family, GRN mutations were excluded [Bruni et al, 2007].…”

Section: Grn Mutation Spectrum Null Mutationsmentioning

confidence: 99%

“…The loss of functional protein is mainly the result of loss of GRN transcript caused by NMD of transcripts containing PTCs (n 5 52) or by nuclear degradation of transcripts retaining the first intron due to splice-site mutations in intron 1 (n 5 2) Le Ber et al, 2007]. PTCs can be the result from nonsense mutations (n 5 12), splice-site mutations (n 5 10), and small insertions/deletions (n 5 30) Baker et al, 2006;Huey et al, 2006;Pickering-Brown et al, 2006Boeve et al, 2006;Masellis et al, 2006;Gass et al, 2006;Benussi et al, 2008;Bronner et al, 2007;Mesulam et al, 2007;Behrens et al, 2007;Leverenz et al, 2007;Bruni et al, 2007;Van Deerlin et al, 2007;Brouwers et al, 2007;Rademakers et al, 2007;Llado et al, 2007;Le Ber et al, 2007;Davion et al, 2007;Kelley et al, in press;Spina et al, 2007a;Mukherjee et al, 2008;Beck et al, 2008;Le Ber et al, 2008]. Second, loss of translation as a result of mutations affecting the Kozak sequence (n 5 4) Baker et al, 2006;Pickering-Brown et al, 2006;Boeve et al, 2006;Gass et al, 2006;Le Ber et al, 2008] and reduction of secreted protein due to missense mutations affecting the signal sequence (n 5 2) [Mukherjee et al, 2006;Gass et al, 2006;Kelley et al, in press;Mukherjee et al, 2008;Le Ber et al, 2008], results in reduced GRN.…”

Section: Grn Mutation Spectrum Null Mutationsmentioning

confidence: 99%

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Granulin mutations associated with frontotemporal lobar degeneration and related disorders: An update

2008

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Communicated by Mark H. PaalmanMutations in the gene encoding granulin (HUGO gene symbol GRN, also referred to as progranulin, PGRN), located at chromosome 17q21, were recently linked to tau-negative ubiquitin-positive frontotemporal lobar degeneration (FTLDU). Since then, 63 heterozygous mutations were identified in 163 families worldwide, all leading to loss of functional GRN, implicating a haploinsufficiency mechanism. Together, these mutations explained 5 to 10% of FTLD. The high mutation frequency, however, might still be an underestimation because not all patient samples were examined for all types of loss-of-function mutations and because several variants, including missense mutations, have a yet uncertain pathogenic significance. Although the complete phenotypic spectrum associated with GRN mutations is not yet fully characterized, it was shown that it is highly heterogeneous, suggesting the influence of modifying factors. A role of GRN in neuronal survival was suggested but the exact mechanism by which neurodegeneration and deposition of pathologic brain inclusions occur still has to be clarified. Hum Mutat 29(12), [1373][1374][1375][1376][1377][1378][1379][1380][1381][1382][1383][1384][1385][1386] 2008.

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Section: Grn Mutation Spectrum Null Mutationsmentioning

confidence: 83%

Section: Grn Mutation Spectrum Null Mutationsmentioning

confidence: 99%

Section: Grn Mutation Spectrum Null Mutationsmentioning

confidence: 99%

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Granulin mutations associated with frontotemporal lobar degeneration and related disorders: An update

2008

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“…However, a number of FTD-linked mutations that specifically lead to deficiencies in PGRN secretion have also been identified (Mukherjee et al, 2008;Shankaran et al, 2008;Wang et al, 2010). A further understanding of the regulation of PGRN secretion is therefore warranted.…”

Section: Introductionmentioning

confidence: 99%

Activity-dependent secretion of progranulin from synapses

Petoukhov¹,

Fernando²,

Mills³

et al. 2013

Journal of Cell Science

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SummaryThe secreted growth factor progranulin (PGRN) has been shown to be important for regulating neuronal survival and outgrowth, as well as synapse formation and function. Mutations in the PGRN gene that result in PGRN haploinsufficiency have been identified as a major cause of frontotemporal dementia (FTD). Here we demonstrate that PGRN is colocalized with dense-core vesicle markers and is cotransported with brain-derived neurotrophic factor (BDNF) within axons and dendrites of cultured hippocampal neurons in both anterograde and retrograde directions. We also show that PGRN is secreted in an activity-dependent manner from synaptic and extrasynaptic sites, and that the temporal profiles of secretion are distinct in axons and dendrites. Neuronal activity is also shown to increase the recruitment of PGRN to synapses and to enhance the density of PGRN clusters along axons. Finally, treatment of neurons with recombinant PGRN is shown to increase synapse density, while decreasing the size of the presynaptic compartment and specifically the number of synaptic vesicles per synapse. Together, this indicates that activity-dependent secretion of PGRN can regulate synapse number and structure.

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“…Of the mutations reported to date (http:// www.molgen.vib-ua.be/FTDMutations/), most are loss-offunction mutations leading to GRN haploinsufficiency , which results in a severe reduction of GRN levels in tissues and biological fluids of patients (Ghidoni et al, 2008;Finch et al, 2009;Sleegers et al, 2009). Additionally, missense mutations (Schymick et al, 2007; Brouwers et al, 2008) lead to cytoplasmic missorting and degradation of GRN (Mukherjee et al, 2008;Shankaran et al, 2008) or to reduced secretion probably attributable to misfolding (Shanka- BafA1 but none of the tested protease inhibitors increase intracellular and secreted GRN levels. A, B, HeLa and SH-SY5Y cells were treated for 16 h with DMSO, BafA1 (50 nM), phenanthroline (10 mM), EDTA (15 mM), MG132 (10 M), epoxomicin (1 M), pepstatin A (1 M), E64 (10 M), antipain (5 M), ALLN (5 M), mix 1 (E64, leupeptin, and antipain), and mix 2 (mix 1 plus pepstatin A and ALLN).…”

Section: Introductionmentioning

confidence: 99%

Rescue of Progranulin Deficiency Associated with Frontotemporal Lobar Degeneration by Alkalizing Reagents and Inhibition of Vacuolar ATPase

Capell¹,

Liebscher²,

Fellerer³

et al. 2011

J. Neurosci.

121

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Numerous loss-of-function mutations in the progranulin (GRN) gene cause frontotemporal lobar degeneration with ubiquitin and TAR–DNA binding protein 43-positive inclusions by reduced production and secretion of GRN. Consistent with the observation that GRN has neurotrophic properties, pharmacological stimulation of GRN production is a promising approach to rescueGRNhaploinsufficiency and prevent disease progression. We therefore searched for compounds capable of selectively increasing GRN levels. Here, we demonstrate that four independent and highly selective inhibitors of vacuolar ATPase (bafilomycin A1, concanamycin A, archazolid B, and apicularen A) significantly elevate intracellular and secreted GRN. Furthermore, clinically used alkalizing drugs, including chloroquine, bepridil, and amiodarone, similarly stimulate GRN production. Elevation of GRN levels occurs via a translational mechanism independent of lysosomal degradation, autophagy, or endocytosis. Importantly, alkalizing reagents rescue GRN deficiency in organotypic cortical slice cultures from a mouse model for GRN deficiency and in primary cells derived from human patients withGRNloss-of-function mutations. Thus, alkalizing reagents, specifically those already used in humans for other applications, and vacuolar ATPase inhibitors may be therapeutically used to prevent GRN-dependent neurodegeneration.

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Molecular characterization of novel progranulin (GRN) mutations in frontotemporal dementia

Cited by 74 publications

References 25 publications

Granulin mutations associated with frontotemporal lobar degeneration and related disorders: An update

Granulin mutations associated with frontotemporal lobar degeneration and related disorders: An update

Activity-dependent secretion of progranulin from synapses

Rescue of Progranulin Deficiency Associated with Frontotemporal Lobar Degeneration by Alkalizing Reagents and Inhibition of Vacuolar ATPase

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