Characterization of mutations in &lt;em&gt;PRNP&lt;/em&gt; (prion) gene and their possible roles in neurodegenerative diseases

Bagyinszky, Eva; Giau, Vo Van; Youn, Young Chul; An, Seong Soo A.; Kim, SangYun

doi:10.2147/ndt.s165445

Cited by 61 publications

(60 citation statements)

References 185 publications

(267 reference statements)

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“…Their clinical phenotype depends on the presence of Met or valine (Val) at codon 129. FFI is correlated to the Met allele [13]. FFI patients with heterozygous (Met-Val) mutation have a longer mean survival time than those with homozygous (Met-Met) [3].…”

Section: Discussionmentioning

confidence: 99%

Clinical features and genetic characteristics of two Chinese pedigrees with fatal family insomnia

Yao

et al. 2019

Prion

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Background : Fatal familial insomnia (FFI) is a rare autosomal-dominant inherited prion disease characterized clinically by severe sleep disorder, motor signs, dysautonomia and abnormal behaviour. FFI is caused by a missense mutation at codon 178 of the prion protein gene (PRNP). Our study is aimed to explore typical clinical and genetic features of two Chinese pedigrees with FFI and review the related literatures. Methods : Two FFI cases with family histories were recruited in our study. The main clinical features, genetic features and possible pathophysiologic mechanisms of these two FFI cases were analysed. Results : The foremost symptoms seemed to be sleep disturbances and psychosis. Progressive sympathetic symptoms, movement disturbances and memory loss were frequently observed as well. Electroencephalography (EEG) showed a minor slowing without periodic triphasic waves. Polysomnography (PSG) showed reduction in total sleep time and disturbance of sleep-related respiratory. Brain magnetic resonance imaging (MRI) did not reveal obvious abnormality. Genetic analysis disclosed the prion protein gene mutation at codon 178 (D178N), with methionine (Met) homozygosity at the polymorphic position 129 (Met129Met). Conclusions : The major clinical features of Chinese FFI are sleep dysfunction, psychiatric symptoms and sympathetic symptoms. Our patients have similar clinical characteristics as that of the typical FFI cases.

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Section: Discussionmentioning

confidence: 99%

Clinical features and genetic characteristics of two Chinese pedigrees with fatal family insomnia

Yao

et al. 2019

Prion

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“…Missense variants in PRNP have been reported in patients with genetic prion disease. The c.628G>A (p.V210I) variant has been reported in many patients with prion disease (Bagyinszky, Giau, Youn, An, & Kim, 2018;Biljan et al.,…”

Section: Genetic Informationmentioning

confidence: 99%

A case report of genetic prion disease with two different PRNP variants

Piazza

Prior

Khalsa

et al. 2020

Molec Gen & Gen Med

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Background Prion diseases are a group of lethal neurodegenerative conditions that occur when the normal, cellular form of the prion protein (PrPC) is converted into an abnormal, scrapie, form of the protein (PrPSc). Disease may be caused by genetic, infectious, or sporadic etiologies. The genetic form of prion disease comprises~10%–15% of all cases. Prion disease is typically inherited in an autosomal dominant manner. The low incidence of disease makes it highly unlikely that a patient would have two different pathogenic variants. However, we recently identified a case in which the patient did have two pathogenic PRNP variants and presented with an atypical phenotype. Methods The patient was evaluated at the Washington Hospital Healthcare System in Fremont, CA. The clinical information for this case report was obtained retrospectively. Variants in the PRNP were identified by polymerase chain reaction (PCR) amplification of exon two of the gene followed by bi‐directional sequence analysis. To determine the phase of the identified variants, a restriction enzyme digestion was utilized, followed by sequence analysis of the products. Cerebral spinal fluid (CSF) was analyzed for surrogate markers of prion disease, 14–3–3 and Tau proteins. CSF real‐time quaking‐induced conversion (RT‐QuIC) assays were also performed. Results The patient was a compound heterozygote for the well‐characterized c.628G>A (p.Val210Ile) variant and the rare octapeptide deletion of two repeats [c.202_249del48 (p.P68_Q83del)]. Clinically, the patient presented with an early onset demyelinating peripheral neuropathy, followed by later onset cognitive symptoms. Conclusion This presentation is reminiscent of prion protein knockout mice whose predominate symptom, due to complete loss of PrP, was late‐onset peripheral neuropathy. To our knowledge this is the first case reported of a patient with prion disease who had two different pathogenic variants in PRNP.

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“…However, the blockage of both canonical endocytic pathways, clathrin- and caveolin-mediated, presented discrepant outcomes according to early or late stages of infection and different PrP Sc variant strains [ 117 ], denoting that there are plenty of unknown mechanisms through which PrP Sc may act. As the PRNP gene is known to show several distinct mutations [ 118 ], it would be relevant to ascertain whether these differences in endocytosis might occur due to these various types of genomic alterations. Interestingly, PrP C mutants at the N-terminal site present a lack of copper-mediated endocytosis, which could lead to neuronal apoptosis and symptoms of prion diseases as if they were infected with PrP Sc , supporting the importance of the endocytic pathway for PrP Sc cell–cell transmission [ 31 ].…”

Section: Cellular Trafficking In Prp Sc Infectimentioning

confidence: 99%

A New Take on Prion Protein Dynamics in Cellular Trafficking

Alves

Iglesia

Prado

et al. 2020

IJMS

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The mobility of cellular prion protein (PrPC) in specific cell membrane domains and among distinct cell compartments dictates its molecular interactions and directs its cell function. PrPC works in concert with several partners to organize signaling platforms implicated in various cellular processes. The scaffold property of PrPC is able to gather a molecular repertoire to create heterogeneous membrane domains that favor endocytic events. Dynamic trafficking of PrPC through multiple pathways, in a well-orchestrated mechanism of intra and extracellular vesicular transport, defines its functional plasticity, and also assists the conversion and spreading of its infectious isoform associated with neurodegenerative diseases. In this review, we highlight how PrPC traffics across intra- and extracellular compartments and the consequences of this dynamic transport in governing cell functions and contributing to prion disease pathogenesis.

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Characterization of mutations in <em>PRNP</em> (prion) gene and their possible roles in neurodegenerative diseases

Cited by 61 publications

References 185 publications

Clinical features and genetic characteristics of two Chinese pedigrees with fatal family insomnia

Clinical features and genetic characteristics of two Chinese pedigrees with fatal family insomnia

A case report of genetic prion disease with two different PRNP variants

A New Take on Prion Protein Dynamics in Cellular Trafficking

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