2015
DOI: 10.1128/jvi.01262-15
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Genetic and Pathological Follow-Up Study of Goats Experimentally and Naturally Exposed to a Sheep Scrapie Isolate

Abstract: Thirty-seven goats carrying different prion protein genotypes (PRNP) were orally infected with a classical scrapie brain homogenate from wild-type (ARQ/ARQ) sheep and then mated to obtain 2 additional generations of offspring, which were kept in the same environment and allowed to be naturally exposed to scrapie. Occurrence of clinical or subclinical scrapie was observed in the experimentally infected goats (F 0 ) and in only one (F 1b ) of the naturally exposed offspring groups. In both groups (F 0 and F 1b )… Show more

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Cited by 17 publications
(37 citation statements)
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“…According to Hardy–Weinberg equilibrium calculations, homozygotes for one rare allele (< 5%) will have a frequency of less than 0.3%, while heterozygotes for two rare alleles will have a frequency of less than 0.5%. The published surveys with full genotype information confirm the expected low frequencies: all homozygotes (excluding wild‐type alleles) were 0.48% and all double heterozygotes (no wild‐type alleles) were 0.43% (based on a total of almost 2600 genotypes) (Billinis et al., ; Acutis et al., ; Vaccari et al., ; Papasavva‐Stylianou et al., ; Bouzalas et al., ; Fragkiadaki et al., ; Goldmann et al., , ; Papasavva‐Stylianou et al., ; Maestrale et al., ; Acín et al., Corbière et al., ; Barillet et al., ). Despite the overall problem with assigning resistance to rare homozygotes due to their observed frequencies, a protective phenotype has been described for MM142 homozygotes similar to IM142 heterozygotes (Table ) (González et al., ; Goldmann et al., ) and also for SS146 and DD146 homozygotes compared to NS146 and ND146 heterozygotes (Georgiadou et al., ).…”
Section: Assessmentmentioning
confidence: 75%
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“…According to Hardy–Weinberg equilibrium calculations, homozygotes for one rare allele (< 5%) will have a frequency of less than 0.3%, while heterozygotes for two rare alleles will have a frequency of less than 0.5%. The published surveys with full genotype information confirm the expected low frequencies: all homozygotes (excluding wild‐type alleles) were 0.48% and all double heterozygotes (no wild‐type alleles) were 0.43% (based on a total of almost 2600 genotypes) (Billinis et al., ; Acutis et al., ; Vaccari et al., ; Papasavva‐Stylianou et al., ; Bouzalas et al., ; Fragkiadaki et al., ; Goldmann et al., , ; Papasavva‐Stylianou et al., ; Maestrale et al., ; Acín et al., Corbière et al., ; Barillet et al., ). Despite the overall problem with assigning resistance to rare homozygotes due to their observed frequencies, a protective phenotype has been described for MM142 homozygotes similar to IM142 heterozygotes (Table ) (González et al., ; Goldmann et al., ) and also for SS146 and DD146 homozygotes compared to NS146 and ND146 heterozygotes (Georgiadou et al., ).…”
Section: Assessmentmentioning
confidence: 75%
“…(Cyprus, 2015), HR154 (i.c., p.o.) (Lacroux et al., ; Maestrale et al., ), QR211 (i.c., p.o.) (Lacroux et al., ; Maestrale et al., ); and QK222 (i.c., p.o.)…”
Section: Assessmentmentioning
confidence: 99%
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“…Some allelic variations in the PRNP gene could potentially protect species against the disease, or at least extend the incubation period. Those identified are: S/G127, I/M142, G/D145, H/R143, N/S146, N/D146, R/H154, R/Q211 and Q/K222 (Goldmann and others 1996, 2011, Billinis and others 2002, Acutis and others 2006, Vaccari and others 2006, 2009, Papasavva-Stylianou and others 2007, 2011, Barillet and others 2009, Gonzalez and others 2009, Serrano and others 2009, Bouzalas and others 2010, Hussain and others 2011, Acin and others 2013, Corbiere and others 2013, Maestrale and others 2015). …”
mentioning
confidence: 99%