Knockdown of prion protein (PrP) by RNA interference weakens the protective activity of wild-type PrP against copper ion and antagonizes the cytotoxicity of fCJD-associated PrP mutants in cultured cells

Dong, Xiao‐Ping

doi:10.3892/ijmm.2011.688

Int J Mol Med

2011

DOI: 10.3892/ijmm.2011.688

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Knockdown of prion protein (PrP) by RNA interference weakens the protective activity of wild-type PrP against copper ion and antagonizes the cytotoxicity of fCJD-associated PrP mutants in cultured cells

Xiao‐Ping Dong

Abstract: Abstract. development of the pathogenesis of transmissible spongiform encephalopathies (tSes) requires the presence of both the normal host prion protein (PrP c ) and the abnormal pathological proteinase-K resistant isoform (PrP Sc ). reduction of PrP c levels has been shown to extend survival time after prion infection. in this report, based on analysis of the known sequences of human PrP, we constructed two small interfering rna (sirna) duplexes targeting the segments of amino acids (aa) 108-114 (ri2) and aa… Show more

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Cited by 2 publications

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El silenciamiento de la proteína priónica celular (PrPC) mediante RNA de interferencia (siRNA) reduce la infección por HSV-1 y HSV-2 en células SK-SY5Y

Ortega-Soto¹,

Arellano-Anaya²,

Castañeda-Colín³

et al. 2018

Rev. Mex. Cienc. Pecu.

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RESUMENLas encefalopatías espongiformes transmisibles (EETs) son enfermedades neurodegenerativas fatales que afectan a humanos y ciertas especies animales. La hipótesis más aceptada indica que el agente infeccioso, denotado como prion y compuesto principalmente por la Proteína Priónica Scrapie (PrP Sc ), corresponde a una conformación anormal de una proteína codificada por el huésped denominada Proteína Priónica Celular (PrP C ), cuya función es aún desconocida; sin embargo, la expresión ubicua de PrP C así como su elevado grado de conservación entre especies, sugieren un papel importante para esta proteína. En este trabajo se detectó a la PrP C en diferentes tipos celulares incluyendo un cultivo primario de células de peces (Tilapia, Oreochromis spp.). Además, basándonos en la secuencia de la PrP C humana, se diseñó un RNA de interferencia (siRNA) con el fin de silenciar el gen PRNP en células neuronales SK-SY5Y. El siRNA diseñado inhibió la expresión de PrP C a lo largo de las 96 h post-transfección y las células silenciadas fueron menos susceptibles a la infección por HSV-1 y HSV-2, en comparación con células no transfectadas con el siRNA. PALABRAS CLAVE: Proteína Priónica, PrP C , siRNA, HSV-1, HSV-2. ABSTRACTThe transmissible spongiform encephalopathies (TSEs) are neurodegenerative and fatal diseases, affecting humans and some other animal species. The most accepted hypothesis suggests that the infectious agent, named "prion", is composed mainly by the prion protein scrapie (PrP Sc ) and it corresponds to an abnormal conformation of a host encoded protein, the cellular prion protein (PrP C ), which function is still unknown. However, the ubiquitous expression of PrP C and its highly conserved presence among different species suggests it has a very important role in cell functions. In this work, the PrP C in different cell types, including a primary fish cell culture (Oreochromis spp.), was detected. In addition, based on the human PrP C sequence, we designed a short interfering RNA (siRNA) to silence the PRNP gen in neuronal SK-SY5Y cells. The designed siRNA inhibited the PrP C expression along 96 hours posttransfection and the silenced cells were less susceptible to HSV-1 and HSV-2 infections, in comparison to non siRNA-transfected cells.

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El silenciamiento de la proteína priónica celular (PrPC) mediante RNA de interferencia (siRNA) reduce la infección por HSV-1 y HSV-2 en células SK-SY5Y

Ortega-Soto¹,

Arellano-Anaya²,

Castañeda-Colín³

et al. 2018

Rev. Mex. Cienc. Pecu.

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Different Aberrant Changes of mGluR5 and Its Downstream Signaling Pathways in the Scrapie-Infected Cell Line and the Brains of Scrapie-Infected Experimental Rodents

Chen

Xia

et al. 2022

Front. Cell Dev. Biol.

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Metabotropic glutamate receptor subtype 5 (mGluR5) is a G-protein-coupled receptor found widely in the central nervous system. It has been involved in the development and progression of some neurodegenerative diseases, but its role in prion diseases is rarely described. In this study, the changes of mGluR5 and its downstream signaling pathways in prion-infected cell line SMB-S15 and the brains of scrapie-infected experimental rodents were evaluated by various methodologies. We found the levels of mGluR5 were significantly increased in a prion-infected cell line SMB-S15 and the cultured cells transiently express an abnormal form PrP (Cyto-PrP). Using immunoprecipitation tests and immunofluorescent assays (IFA), molecular interaction and morphological colocalization between PrP and mGluR5 were observed in the cultured cells. We identified that the (GPCRs)-IP3-IP3R-Ca2+ pathway was activated and the levels of the downstream kinases p38, ERK, and JNK were increased in SMB-S15 cells. After treated with mGluR5 antagonist (MTEP) or the removal of prion replication by resveratrol in SMB-S15 cells, the upregulations of mGluR5 and the downstream kinases were restored in a certain degree. Moreover, increased mGluR5 contributes to the cell damage in prion-infected cells. Contrarily, the levels of mGluR5 in the brains of several scrapie-infected rodent models were decreased at terminal stage. IFA of the brain sections of scrapie-infected rodents demonstrated that the signals of mGluR5 were preferentially colocalized with the NeuN-positive cells, accompanying with severe neuron losses in Nissl staining, which might be a reason for the decrease of mGluR5. Our data indicate the different aberrant alterations of mGluR5 and the downstream signaling pathways during prion infection in vivo and in vitro.

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Knockdown of prion protein (PrP) by RNA interference weakens the protective activity of wild-type PrP against copper ion and antagonizes the cytotoxicity of fCJD-associated PrP mutants in cultured cells

Cited by 2 publications

References 17 publications

El silenciamiento de la proteína priónica celular (PrPC) mediante RNA de interferencia (siRNA) reduce la infección por HSV-1 y HSV-2 en células SK-SY5Y

El silenciamiento de la proteína priónica celular (PrPC) mediante RNA de interferencia (siRNA) reduce la infección por HSV-1 y HSV-2 en células SK-SY5Y

Different Aberrant Changes of mGluR5 and Its Downstream Signaling Pathways in the Scrapie-Infected Cell Line and the Brains of Scrapie-Infected Experimental Rodents

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