The major polypeptide of scrapie-associated fibrils (SAF) has the same size, charge distribution and N-terminal protein sequence as predicted for the normal brain protein (PrP).

Hope, James; Morton, Lorena; Farquhar, Christine; Multhaup, Gerd; Beyreuther, Konrad; Kimberlin, R.H.

doi:10.1002/j.1460-2075.1986.tb04539.x

Cited by 309 publications

(186 citation statements)

References 39 publications

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“…Mammalian amyloid disaggregase and proteolysis activities are sensitive to low and high pH pretreatment. Dialysis of HEK 293 PNS (1 mg/mL total protein) for 16 h at 4 C into buffers at low pH (and to a lesser extent high pH) decreases its ability (at a final total PNS concentration of 10 lg/mL) to disaggregate Ab fibrils (65 lg/mL) and to degrade Ab 1-40 . resistance of amyloid to proteolysis, it seems likely that the mammalian disaggregase activity precedes the proteolysis activity, [39][40][41] and the proteolysis activity is crucial for preventing reaggregation. 35 The discovery and partial characterization of the mammalian amyloid disaggregase activity(ies) are a step towards identification of its molecular underpinnings.…”

Section: Discussionmentioning

confidence: 99%

“…The tight linkage of disaggregation and proteolysis may be due to a physical linkage of proteins or protein complexes that carry out these activities. Additionally, because amyloid is known to be protease resistant, [39][40][41] it is likely that disaggregation is required for proteolysis, and this relationship would necessitate a linear correlation between disaggregation and proteolysis (Fig. 7).…”

Section: Mammalian Amyloid Disaggregase and Proteolysis Activities Armentioning

confidence: 99%

“…39 The kinetic disaggregation assay was conducted in aggregation buffer (50 mM sodium phosphate, pH 7.4, 150 mM NaCl, 0.02% NaN 3 ) containing ThT (40 lM). Mammalian tissue PNS (3-45 lg/mL total protein, as specified) or human cell PNS (3-45 lg/mL total protein, as specified) was added to the specified concentration of sonicated Ab 1-40 fibrils or sonicated 8 kDa gelsolin fibrils in Corning 96-well clear bottom plates (final volume 100 lL/well).…”

Section: Kinetic Disaggregation Assaymentioning

confidence: 99%

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Discovery and characterization of a mammalian amyloid disaggregation activity

Murray¹,

Solomon²,

Wang³

et al. 2010

Protein Science

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The formation of amyloid, a cross-b-sheet fibrillar aggregate, is associated with a variety of aging-associated degenerative diseases. Herein, we report the existence of a mammalian amyloid disaggregase activity that is present in all tissues and cell types tested. Homogenates from mammalian tissues and cell lines are able to disaggregate amyloid fibrils composed of amyloid b (Ab) 1-40 or the 8 kDa plasma gelsolin fragment. The mammalian disaggregase activity is sensitive to proteinase K digestion and can be uncoupled from proteolysis activity using a protease inhibitor cocktail. Amyloid disaggregation and proteolysis activities are remarkably resistant to changes in temperature and pH. Identification and manipulation of the proteins responsible for the amyloid disaggregation/degradation activities offers the possibility of ameliorating aggregation-associated diseases.

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Section: Discussionmentioning

confidence: 99%

Section: Mammalian Amyloid Disaggregase and Proteolysis Activities Armentioning

confidence: 99%

Section: Kinetic Disaggregation Assaymentioning

confidence: 99%

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Discovery and characterization of a mammalian amyloid disaggregation activity

Murray¹,

Solomon²,

Wang³

et al. 2010

Protein Science

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“…Seed formation is kinetically controlled and extremely slow; once a seed is present, monomer addition can ensue at a rapid rate [58,59]. [16,21,29]. Pulse-chase experiments in scrapie-infected neuroblastoma cells suggest that PrP c is converted to PrP sc either at the cell surface or following endocytosis [30].…”

Section: Biosynthesis Of Prp C and Prp Scmentioning

confidence: 99%

Molecular biology of transmissible spongiform encephalopathies

1996

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The prion, the transmissible agent that causes spongiform encephalopathies such as serapie, bovine spongiform encephalopathy (BSE) and Creutzfeldt-Jakob disease, is believed to be devoid of nucleic acid and identical with PrP so, a modified form of the normal host protein PrP ¢ which is encoded by the single cop~v gene Prnp. The 'protein only" hypothesis proposes that PrP ~c, when introduced into a normal host, causes the conversion of PrP c into prpS~; it therefore predicts that an animal devoid of PrP c should be resistant to prion diseases. We generated homozygous Prnp °1° ('PrP knockout') mice and showed that, after inoculation with prions, they remained free of scrapie for at least 2 years while wild-type controls all died within 6 months. There was no propagation of prions in the Prnp °t° animals. Surprisingly, heterozygous Prnp °t+ mice, which express PrP c at about half the normal level, also showed enhanced resistance to scrapie disease despite high levels of infectious agent and PrP ~c in the brain early on. After introduction of murine PrP transgenes Prnp °t° mice became highly susceptible to mouse but not to hamster prions, while the insertion of Syrian hamster PrP transgenes rendered them susceptible to hamster but to a much lesser extent to mouse prions. These complementation experiments paved the way to the application of reverse genetics. We have prepared animals transgenic for genes encoding PrP with amino terminal deletions of various lengths and have found that PrP lacking 48 amino proximal amino acids, which comprise four of the five octa repeats of PrP, is still biologically active.

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“…30 It is characterized by progressive neurodegeneration, including neuronal death, gliosis, spongiform changes, and deposition of partially proteinase K-resistant prion protein (PrP sc ), an abnormal isoform of the physiological host-encoded prion protein (PrP c ), in the central nervous system (CNS). 21 In contrast to bovine spongiform encephalopathy (BSE), 35 there is no evidence that scrapie is harmful to humans. However, it has been shown repeatedly that BSE is transmissible to both sheep and goats 15,16 under experimental conditions.…”

Section: Introductionmentioning

confidence: 99%

Atypical Scrapie in a Swiss Goat and Implications for Transmissible Spongiform Encephalopathy Surveillance

et al. 2007

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Abstract. Different types of transmissible spongiform encephalopathies (TSEs) affect sheep and goats. In addition to the classical form of scrapie, both species are susceptible to experimental infections with the bovine spongiform encephalopathy (BSE) agent, and in recent years atypical scrapie cases have been reported in sheep from different European countries. Atypical scrapie in sheep is characterized by distinct histopathologic lesions and molecular characteristics of the abnormal scrapie prion protein (PrP sc ). Characteristics of atypical scrapie have not yet been described in detail in goats. A goat presenting features of atypical scrapie was identified in Switzerland. Although there was no difference between the molecular characteristics of PrP sc in this animal and those of atypical scrapie in sheep, differences in the distribution of histopathologic lesions and PrP sc deposition were observed. In particular the cerebellar cortex, a major site of PrP sc deposition in atypical scrapie in sheep, was found to be virtually unaffected in this goat. In contrast, severe lesions and PrP sc deposition were detected in more rostral brain structures, such as thalamus and midbrain. Two TSE screening tests and PrP sc immunohistochemistry were either negative or barely positive when applied to cerebellum and obex tissues, the target samples for TSE surveillance in sheep and goats. These findings suggest that such cases may have been missed in the past and could be overlooked in the future if sampling and testing procedures are not adapted. The epidemiological and veterinary public health implications of these atypical cases, however, are not yet known.

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The major polypeptide of scrapie-associated fibrils (SAF) has the same size, charge distribution and N-terminal protein sequence as predicted for the normal brain protein (PrP).

Cited by 309 publications

References 39 publications

Discovery and characterization of a mammalian amyloid disaggregation activity

Discovery and characterization of a mammalian amyloid disaggregation activity

Molecular biology of transmissible spongiform encephalopathies

Atypical Scrapie in a Swiss Goat and Implications for Transmissible Spongiform Encephalopathy Surveillance

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