Two distinct prions in fatal familial insomnia and its sporadic form

Takeuchi, Atsuko; Mohri, Satoshi; Kai, Hideaki; Tamaoka, Akira; Kobayashi, Atsushi; Mizusawa, Hidehiro; Iwasaki, Yasushi; Yoshida, Mari; Shimizu, Hiroshi; Murayama, Shigeo; Kuroda, Shigetoshi; Morita, Masanori; Parchi, Piero; Kitamoto, Tetsuyuki

doi:10.1093/braincomms/fcz045

Cited by 14 publications

(21 citation statements)

References 43 publications

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“…BvPrP with methionine at codon 109 of Prnp (22). Our work confirmed that also our model is susceptible to FFI.…”

Section: Discussionsupporting

confidence: 89%

“…This has been observed also in transgenic mice expressing BvPrP with isoleucine at codon 109 and the D178 mutation that spontaneously developed prion diseases with the presence of a PrP res with a predominant di-glycosylated band (34). Many other studies showed that this phenomenon occurred also in other transgenic mouse models inoculated with FFI thus suggesting that, regardless of the recipient mice, some biochemical features typical of the FFI are reproduced after inoculation (21,22).…”

Section: Discussionmentioning

confidence: 69%

“…There is a compelling evidence that some human prion strains originally believed to be "pure" are instead composed by a mixture of strains (35)(36)(37)(38). Interestingly, a very recent publication of the group of Kitamoto Tetsuyuki showed that even the FFI D178N-129MM strain might not be pure and that at least two distinct prion strains can be responsible for the disease, one associated with the typical clinical presentation of the disease and the other associated with an atypical phenotype (22). It is therefore conceivable that the mono-glycosylated PrP res observed in one of the animals inoculated with FFI-BH might have emerged either because the FFI propagates as a mixture of prions (as also shown for other sporadic forms of prion diseases) or as a random event due to specific limitations imposed by the animal model used.…”

Section: Discussionmentioning

confidence: 99%

“…The ability of the D178N mutation to promote conversion of PrP C into PrP Sc which results in the generation of spontaneous prion pathology was shown in mice genetically modified to express murine PrP with the D177N mutation (the equivalent to human D178N) where PrP Sc is barely detectable (13,14). The infectious properties of FFI-PrP Sc were extensively investigated by transmission studies in wild-type animals (15,16) and in several lines of mice genetically modified to express human PrP (17,18) as well as primates (15,(19)(20)(21)(22). Results of these studies showed that several factors, including the polymorphisms at codon 129 of the incoming FFI-PrP Sc inoculum, the prion titer of the FFI brain areas used to challenge the animals and the PrP C amino acid sequence of the recipient animals, could significantly influence the transmission efficiency.…”

Section: Introductionmentioning

confidence: 99%

“…Notably, when inoculated in mice expressing a chimeric human-mouse PrP, FFI-PrP Sc is able to promote the generation of prions characterized by similar biochemical features of the original inoculum (21). In a recent report, FFI was efficiently transmitted to knock-in mice expressing the bank vole PrP (BvPrP) with methionine at codon 109 of the PrP C (22). Also in this case, the PrP Sc generated in mice showed the typical biochemical features of FFI-PrP Sc (predominance of the diglycosylated band and migration of the un-glycosylated PrP species at 19kDa).…”

Section: Introductionmentioning

confidence: 99%

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PMCA-generated prions from the olfactory mucosa of patients with Fatal Familial Insomnia cause prion disease in mice

Bistaffa

Marín-Moreno

Espinosa

et al. 2021

eLife

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Background: Fatal Familial Insomnia (FFI) is a genetic prion disease caused by the D178N mutation in the prion protein gene (PRNP) in coupling phase with methionine at PRNP 129. In 2017, we have shown that the olfactory mucosa (OM) collected from FFI patients contained traces of PrPSc detectable by Protein Misfolding Cyclic Amplification (PMCA).Methods In this work, we have challenged PMCA generated products obtained from OM and brain homogenate of FFI patients in BvPrP-Tg407 transgenic mice expressing the bank vole prion protein to test their ability to induce prion pathology.Results: All inoculated mice developed mild spongiform changes, astroglial activation and PrPSc deposition mainly affecting the thalamus. However, their neuropathological alterations were different from those found in the brain of BvPrP-Tg407 mice injected with raw FFI brain homogenate.Conclusions: Although with some experimental constraints, we show that PrPSc present in OM of FFI patients is potentially infectious.Funding: This work was supported in part by the Italian Ministry of Health (GR-2013-02355724 and Ricerca Corrente), MJFF, ALZ, Alzheimer's Research UK and the Weston Brain Institute (BAND2015), and Euronanomed III (Speedy) to FM; by the Spanish Ministerio de Economía y Competitividad [grant AGL2016-78054-R (AEI/FEDER, UE)] to J.M.T. and J.C.E.; A.M.-M. was supported by a fellowship from the INIA (FPI-SGIT-2015-02).

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“…BvPrP with methionine at codon 109 of Prnp (22). Our work confirmed that also our model is susceptible to FFI.…”

Section: Discussionsupporting

confidence: 89%

Section: Discussionmentioning

confidence: 69%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

PMCA-generated prions from the olfactory mucosa of patients with Fatal Familial Insomnia cause prion disease in mice

Bistaffa

Marín-Moreno

Espinosa

et al. 2021

eLife

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Prion Diseases and Hearing Loss

Zirek,

Küçük,

Bayar Muluk

2023

Hearing Loss in Congenital, Neonatal and Childhood Infections

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Phenotypic diversity of genetic Creutzfeldt–Jakob disease: a histo-molecular-based classification

et al. 2021

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The current classification of sporadic Creutzfeldt–Jakob disease (sCJD) includes six major clinicopathological subtypes defined by the physicochemical properties of the protease-resistant core of the pathologic prion protein (PrPSc), defining two major PrPSc types (i.e., 1 and 2), and the methionine (M)/valine (V) polymorphic codon 129 of the prion protein gene (PRNP). How these sCJD subtypes relate to the well-documented phenotypic heterogeneity of genetic CJD (gCJD) is not fully understood. We analyzed molecular and phenotypic features in 208 individuals affected by gCJD, carrying 17 different mutations, and compared them with those of a large series of sCJD cases. We identified six major groups of gCJD based on the combination PrPSc type and codon 129 genotype on PRNP mutated allele, each showing distinctive histopathological characteristics, irrespectively of the PRNP associated mutation. Five gCJD groups, named M1, M2C, M2T, V1, and V2, largely reproduced those previously described in sCJD subtypes. The sixth group shared phenotypic traits with the V2 group and was only detected in patients carrying the E200K-129M haplotype in association with a PrPSc type of intermediate size (“i”) between type 1 and type 2. Additional mutation-specific effects involved the pattern of PrP deposition (e.g., a “thickened” synaptic pattern in E200K carriers, cerebellar “stripe-like linear granular deposits” in those with insertion mutations, and intraneuronal globular dots in E200K-V2 or -M”i”). A few isolated cases linked to rare PRNP haplotypes (e.g., T183A-129M), showed atypical phenotypic features, which prevented their classification into the six major groups. The phenotypic variability of gCJD is mostly consistent with that previously found in sCJD. As in sCJD, the codon 129 genotype and physicochemical properties of PrPSc significantly correlated with the phenotypic variability of gCJD. The most common mutations linked to CJD appear to have a variable and overall less significant effect on the disease phenotype, but they significantly influence disease susceptibility often in a strain-specific manner. The criteria currently used for sCJD subtypes can be expanded and adapted to gCJD to provide an updated classification of the disease with a molecular basis.

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Two distinct prions in fatal familial insomnia and its sporadic form

Cited by 14 publications

References 43 publications

PMCA-generated prions from the olfactory mucosa of patients with Fatal Familial Insomnia cause prion disease in mice

PMCA-generated prions from the olfactory mucosa of patients with Fatal Familial Insomnia cause prion disease in mice

Prion Diseases and Hearing Loss

Phenotypic diversity of genetic Creutzfeldt–Jakob disease: a histo-molecular-based classification

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