| Literature DB >> 26587837 |
Fiona Houston1, Wilfred Goldmann1, James Foster1, Lorenzo González2, Martin Jeffrey2, Nora Hunter1.
Abstract
Sheep are natural hosts of the prion disease, scrapie. They are also susceptible to experimental challenge with various scrapie strains and with bovine spongiform encephalopathy (BSE), which affects cattle and has been accidentally transmitted to a range of other species, including man. Incidence and incubation period of clinical disease in sheep following inoculation is controlled by the PRNP gene, which has different alleles defined on the basis of polymorphisms, particularly at codons 136, 154 and 171, although other codons are associated with survival time, and the exact responses of the sheep may be influenced by other breed-related differences. Here we report the results of a long term single study of experimental scrapie and BSE susceptibility of sheep of Cheviot, Poll Dorset and Suffolk breeds, originating from New Zealand and of a wide range of susceptible and resistant PRNP genotypes. Responses were compared with those of sheep from a closed Cheviot flock of UK origin (Roslin Cheviot flock). The unusually long observation period (6-8 years for most, but up to 12 years for others) allows us to draw robust conclusions about rates of survival of animals previously regarded as resistant to infection, particularly PRNP heterozygotes, and is the most comprehensive such study reported to date. BSE inoculation by an intracerebral route produced disease in all genotype groups with differing incubation periods, although M112T and L141F polymorphisms seemed to give some protection. Scrapie isolate SSBP/1, which has the shortest incubation period in sheep with at least one VRQ PRNP allele, also produced disease following sub-cutaneous inoculation in ARQ/ARQ animals of New Zealand origin, but ARQ/ARQ sheep from the Roslin flock survived the challenge. Our results demonstrate that the links between PRNP genotype and clinical prion disease in sheep are much less secure than previously thought, and may break down when, for example, a different breed of sheep is moved into a new flock.Entities:
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Year: 2015 PMID: 26587837 PMCID: PMC4654545 DOI: 10.1371/journal.pone.0143251
Source DB: PubMed Journal: PLoS One ISSN: 1932-6203 Impact factor: 3.240
Experimental design.
| PRNP genotype | TSE challenge and route | Dose | Number of sheep challenged | Breed | Number of NZ sheep | Number of Roslin sheep |
|---|---|---|---|---|---|---|
|
|
| 0.5ml, 10% brain homogenate | 10 | Cheviot | 5 | - |
| Poll Dorset | 5 | - | ||||
|
| ditto | ditto | 10 | Cheviot | 5 | - |
| Poll Dorset | 5 | - | ||||
|
| ditto | ditto | 11 | Cheviot | 5 | 2 |
| Poll Dorset | 4 | - | ||||
|
| ditto | ditto | 19 | Cheviot | 5 | - |
| Poll Dorset | 4 | - | ||||
| Suffolk | 10 | - | ||||
|
| ditto | ditto | 22 | Cheviot | 5 | 2 |
| Poll Dorset | 6 | - | ||||
| Suffolk | 9 | - | ||||
|
| ditto | ditto | 1 | Cheviot | - | 1 |
|
| ditto | ditto | 31 | Cheviot | 5 | 12 |
| Poll Dorset | 4 | - | ||||
| Suffolk | 10 | - | ||||
|
|
| 2ml, 10% brain pool | 18 | Cheviot | 5 | 8 |
| Poll Dorset | 5 | - | ||||
|
| ditto | ditto | 28 | Cheviot | 5 | 18 |
| Poll Dorset | 5 | - | ||||
|
| ditto | ditto | 7 | Cheviot | - | 7 |
|
| ditto | ditto | 23 | Cheviot | 5 | 14 |
| Poll Dorset | 4 | - | ||||
|
| ditto | ditto | 22 | Cheviot | 4 | 3 |
| Poll Dorset | 5 | - | ||||
| Suffolk | 10 | - | ||||
|
| ditto | ditto | 1 | Cheviot | 1 | 7 |
|
| ditto | ditto | 37 | Cheviot | 5 | 17 |
| Poll Dorset | 5 | - | ||||
| Suffolk | 10 | - | ||||
|
| ditto | ditto | 3 | Cheviot | - | 3 |
|
| ditto | ditto | 27 | Cheviot | 6 | 6 |
| Poll Dorset | 5 | - | ||||
| Suffolk | 10 | - |
Outcome of intracerebral challenges with cattle BSE in New Zealand sheep.
|
| Codon 141 subgroup | Codon 112 subgroup | Number challenged | Clinically positive and IHC positive | Clinically negative and IHC positive | Clinically negative and IHC negative | |||
|---|---|---|---|---|---|---|---|---|---|
| Number | Mean incubation period in days (±SD) | Number | Mean survival time post infection in days (±SD) | Number surviving <2000 days post infection (range of survival times) | Number surviving >2000 days post infection (range of survival times in days) | ||||
| ARQ/ARQ | LL | MM | 12 | 12 | 537 (±33) | 0 | NA | 0 | 0 |
| LL | MT | 1 | 0 | NA | 1 | 2414 | 0 | 0 | |
| LL | TT | 1 | 0 | NA | 0 | NA | 0 | 1 (2414) | |
| FF | MM | 5 | 5 | 608 (±38) | 0 | NA | 0 | 0 | |
| VRQ/VRQ | LL | MM | 10 | 10 | 1099 (±44) | 0 | NA | 0 | 0 |
| VRQ/ARQ | LL | MM | 7 | 7 | 875 (±77) | 0 | NA | 0 | 0 |
| LF | MM | 3 | 3 | 2017 (±56) | 0 | NA | 0 | 0 | |
| ARR/ARR | LL | MM | 19 | 10 | 1486 (±398) | 0 | NA | 3 (822–1930) | 6 (2224–2418) |
| VRQ/ARR | LL | MM | 9 | 4 | 1846 (±72) | 1 | 2228 | 2 (106,1906) | 2 (2228,2360) |
| ARQ/ARR | LL | MM | 15 | 4 | 2024 (±110) | 4 | 2320 (±109) | 3 (938–1744) | 4 (2151–2312) |
| LF | MM | 5 | 0 | NA | 0 | NA | 3 (661–1428) | 2 (2395,2396) | |
a Immunohistochemistry results for PrPd detection in brain sections.
b These animals were culled before the end of the experiment due to intercurrent disease or welfare concerns.
c These animals were culled at the end of the experiment.
NA not applicable
Outcome of intracerebral challenges with cattle BSE in the Roslin Flock.
| Cattle brain isolate |
| Number challenged | Clinically positive and IHC positive | Clinically negative and IHC negative | ||
|---|---|---|---|---|---|---|
| Number | Incubation period in days (mean ±SD) | Number surviving <2000 days post infection (range of survival times in days) | Number surviving >2000 days post infection (range of survival times in days) | |||
| BSE-I | VRQ/ARR | 2 | 1 | 1874 | 0 | 1 (2379) |
| ARQ/ARR | 2 | 2 | 1886, 1923 | 0 | 0 | |
| AHQ/ARR | 1 | 1 | 2353 | 0 | 0 | |
| ARR/ARR | 6 | 3 | 1582 ±110 | 1 (1523 | 2 (2204 | |
| BSE-II | ARR/ARR | 6 | 6 | 1712 ±375 | 0 | 0 |
a All animals had codon 141 LL genotype.
b Immunohistochemistry results for PrPd detection in brain sections.
c Previously published data.
d Intercurrent deaths.
e Tissues unavailable for analysis
Outcome of subcutaneous challenges with SSBP/1 in New Zealand sheep.
|
| Codon 141 subgroup | Codon 112 subgroup | Number challenged | Clinically positive and IHC positive | Clinically negative and IHC negative | ||
|---|---|---|---|---|---|---|---|
| Number | Mean incubation period in days post infection (± SD) | Number surviving <2000 days post infection (range of survival times in days) | Number surviving >2000 days post infection (range of survival times in days) | ||||
| VRQ/VRQ | LL | MM | 10 | 10 | 150 ± 15 | 0 | 0 |
| VRQ/ARQ | LL | MM | 6 | 6 | 192 ± 21 | 0 | 0 |
| LF | MM | 4 | 4 | 271 ± 37 | 0 | 0 | |
| VRQ/ARR | LL | MM | 9 | 9 | 233 ± 38 | 0 | 0 |
| ARQ/ARQ | LL | MM | 13 | 12 | 1140 ± 226 | 1 (802) | 0 |
| LL | MT | 1 | 0 | NA | 0 | 1 (2780) | |
| FF | MM | 4 | 4 | 1241 ± 53 | 0 | 0 | |
| n.d. | n.d. | 1 | 0 | NA | 1 (335) | 0 | |
| ARQ/AHQ | LF | MM | 1 | 0 | NA | 0 | 1 (2249) |
| ARQ/ARR | LL | MM | 15 | 0 | NA | 3 (811–1730) | 12 (2242–2779) |
| LF | MM | 4 | 0 | NA | 1 (518) | 3 (2776–2777) | |
| n.d. | n.d. | 1 | 0 | NA | 1 (222) | 0 | |
| ARR/ARR | LL | MM | 21 | 0 | NA | 4 (22–1729) | 17 (2248–2779) |
a These animals were culled before the end of the experiment due to intercurrent disease or welfare concerns.
b These animals were culled at the end of the experiment.
NA, not applicable
n.d., not determined
Outcome of subcutaneous challenges with SSBP/1 in the Roslin Flock.
|
| Codon 141 subgroup | Number challenged | Clinically positive and IHC positive | Clinically negative and IHC negative | ||
|---|---|---|---|---|---|---|
| Number | Mean incubation period in days post infection (± SD) | Number surviving <2000 days post infection (range of survival times in days) | Number surviving >2000 days post infection (range of survival times in days) | |||
| VRQ/VRQ | LL | 8 | 8 | 170 (± 27) | 0 | 0 |
| VRQ/ARQ | n.d. | 10 | 10 | 273 (± 37) | 0 | 0 |
| LF | 6 | 6 | 230 (± 40) | 0 | 0 | |
| LL | 2 | 2 | 291, 351 | 0 | 0 | |
| VRQ/AHQ | LL | 7 | 7 | 361 (± 65) | 0 | 0 |
| VRQ/ARR | LL | 14 | 14 | 323 (± 34) | 0 | 0 |
| ARQ/ARQ | n.d. | 3 | 0 | NA | 1 (1860) | 2 (2331, 2532) |
| ARQ/AHQ | LL/n.d. | 7 | 0 | NA | 3 (1242–1994) | 4 (2284–2813) |
| ARQ/ARR | LL/LF/n.d. | 17 | 0 | NA | 7 (567–1601) | 10 (2107–4256) |
| AHQ/ARR | LL | 3 | 0 | NA | 1 (1693) | 2 (2284,2813) |
| ARR/ARR | LL | 6 | 0 | NA | 1 (568) | 5 (2284–2937) |
a These animals were culled before the end of the experiment due to intercurrent disease or welfare concerns.
b These animals were culled at the end of the experiment.
NA, not applicable
n.d., not determined
The distribution of PrPd in lymphoid tissues of BSE- and SSBP/1-infected New Zealand sheep.
|
| No. clinical cases/no. inoculated with BSE (intracerebral) | BSE: no. positive tissues/no. tissues examined | No. clinical cases/no. inoculated with SSBP/1 (sub- cutaneous) | SSBP/1: no. positive tissues/no. tissues examined | ||||||
|---|---|---|---|---|---|---|---|---|---|---|
| Brain | Tonsil | MLN | Spleen | Brain | Tonsil | MLN | Spleen | |||
| VLRQ/VLRQ | 10/10 | 10/10 | 6/10 | 5/10 | 7/10 | 10/10 | 10/10 | 10/10 | 10/10 | 10/10 |
| VLRQ/ALRQ | 7/7 | 7/7 | 1/7 | 1/6 | 1/7 | 6/6 | 6/6 | 6/6 | 6/6 | 6/6 |
| VLRQ/AFRQ | 3/3 | 3/3 | 1/3 | 1/3 | 1/3 | 4/4 | 4/4 | 4/4 | 3/4 | 3/4 |
| ALRQ/ALRQ | 12/12 | 12/12 | 4/4 | 4/4 | 4/4 | 12/14 | 12/14 | 11/14 | 11/13 | 12/14 |
| AFRQ/AFRQ | 5/5 | 5/5 | 4/4 | 4/4 | 4/4 | 4/4 | 4/4 | 4/4 | 4/4 | 4/4 |
| VLRQ/ALRR | 4/9 | 5/9 | 0/7 | 0/7 | 0/7 | 9/9 | 9/9 | 3/9 | 1/9 | 2/9 |
| ALRQ/ALRR | 4/15 | 8/15 | 0/10 | 0/12 | 0/12 | 0/15 | 0/15 | 0/15 | 0/15 | 0/15 |
| AFRQ/ALRR | 0/5 | 0/5 | 0/1 | 0/1 | 0/1 | 0/4 | 0/4 | 0/4 | 0/4 | 0/4 |
| ALRR/ALRR | 10/19 | 10/19 | 0/14 | 0/14 | 0/14 | 0/20 | 0/20 | 0/20 | 0/20 | 0/20 |
* The results for animals that had polymorphisms at codons 112 (112MT and 112TT) or 154 (154RH) were excluded from this table as none had positive staining in lymphoid tissues.
MLN = mesenteric lymph node
Fig 1Detection of disease-related PrPSc in IHC of brain and lymphoid tissues of TSE inoculated sheep.
IHC carried out using anti-PrP antibody BG4. (A), (B) and (C) positive staining in tissues from three sheep clinically affected following intracerebral inoculation with BSE. (A) ALRQ/ALRQ thalamus (x10); (B) AFRQ/AFRQ medulla (x10); (C) ALRQ/ALRQ mesenteric lymph node (x10). (D), (E) and (F) positive staining in tissues from three sheep clinically affected following sub-cutaneous inoculation with SSBP/1 scrapie. (D) VLRQ/VLRQ frontal cortex (x4); (E) VLRQ/ALRQ basal ganglia (x20); (F) VLRQ/AFRQ prescapular lymph node. (G) negative staining in tonsil of non-clinical AFRQ/ALRR BSE inoculated sheep. (H) negative staining in basal ganglia of non-clinical SSBP/1 ALRR/ALRR inoculated sheep.