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Norwegian moose CWD induces clinical disease and neuroinvasion in gene-targeted mice expressing cervid S138N prion protein
by
Zemlyankina, Irina
, Ng, Raychal Ashlyn
, Kaczmarczyk, Lech
, Arifin, Maria Immaculata
, Jackson, Walker S.
, Hannaoui, Samia
, Schatzl, Hermann M.
, Zeng, Doris
, Benestad, Sylvie L.
, Gilch, Sabine
, Ahmed-Hassan, Hanaa
in
Alces alces
/ Amino acid sequence
/ Animal models
/ Animals
/ Brain
/ Brain - metabolism
/ Brain - pathology
/ Brain research
/ Cervus elaphus
/ Chronic wasting disease
/ Deer
/ Disease
/ Diseases
/ Elk
/ Gene Targeting
/ Genetically modified mice
/ Grants
/ Health aspects
/ Infections
/ Inoculum
/ Invasiveness
/ Mice
/ Mice, Transgenic
/ Molecular weight
/ Moose
/ Nervous system
/ Norway
/ Pathogenesis
/ Prion protein
/ Prion Proteins - genetics
/ Prion Proteins - metabolism
/ Prions
/ Prions - genetics
/ Prions - metabolism
/ Prions - pathogenicity
/ Propagation
/ Protein seeding
/ Proteins
/ Reindeer
/ Spleen
/ Transgenic animals
/ Transgenic mice
/ Transmissible spongiform encephalopathy
/ Wasting Disease, Chronic - metabolism
/ Wasting Disease, Chronic - transmission
2024
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Norwegian moose CWD induces clinical disease and neuroinvasion in gene-targeted mice expressing cervid S138N prion protein
by
Zemlyankina, Irina
, Ng, Raychal Ashlyn
, Kaczmarczyk, Lech
, Arifin, Maria Immaculata
, Jackson, Walker S.
, Hannaoui, Samia
, Schatzl, Hermann M.
, Zeng, Doris
, Benestad, Sylvie L.
, Gilch, Sabine
, Ahmed-Hassan, Hanaa
in
Alces alces
/ Amino acid sequence
/ Animal models
/ Animals
/ Brain
/ Brain - metabolism
/ Brain - pathology
/ Brain research
/ Cervus elaphus
/ Chronic wasting disease
/ Deer
/ Disease
/ Diseases
/ Elk
/ Gene Targeting
/ Genetically modified mice
/ Grants
/ Health aspects
/ Infections
/ Inoculum
/ Invasiveness
/ Mice
/ Mice, Transgenic
/ Molecular weight
/ Moose
/ Nervous system
/ Norway
/ Pathogenesis
/ Prion protein
/ Prion Proteins - genetics
/ Prion Proteins - metabolism
/ Prions
/ Prions - genetics
/ Prions - metabolism
/ Prions - pathogenicity
/ Propagation
/ Protein seeding
/ Proteins
/ Reindeer
/ Spleen
/ Transgenic animals
/ Transgenic mice
/ Transmissible spongiform encephalopathy
/ Wasting Disease, Chronic - metabolism
/ Wasting Disease, Chronic - transmission
2024
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Norwegian moose CWD induces clinical disease and neuroinvasion in gene-targeted mice expressing cervid S138N prion protein
by
Zemlyankina, Irina
, Ng, Raychal Ashlyn
, Kaczmarczyk, Lech
, Arifin, Maria Immaculata
, Jackson, Walker S.
, Hannaoui, Samia
, Schatzl, Hermann M.
, Zeng, Doris
, Benestad, Sylvie L.
, Gilch, Sabine
, Ahmed-Hassan, Hanaa
in
Alces alces
/ Amino acid sequence
/ Animal models
/ Animals
/ Brain
/ Brain - metabolism
/ Brain - pathology
/ Brain research
/ Cervus elaphus
/ Chronic wasting disease
/ Deer
/ Disease
/ Diseases
/ Elk
/ Gene Targeting
/ Genetically modified mice
/ Grants
/ Health aspects
/ Infections
/ Inoculum
/ Invasiveness
/ Mice
/ Mice, Transgenic
/ Molecular weight
/ Moose
/ Nervous system
/ Norway
/ Pathogenesis
/ Prion protein
/ Prion Proteins - genetics
/ Prion Proteins - metabolism
/ Prions
/ Prions - genetics
/ Prions - metabolism
/ Prions - pathogenicity
/ Propagation
/ Protein seeding
/ Proteins
/ Reindeer
/ Spleen
/ Transgenic animals
/ Transgenic mice
/ Transmissible spongiform encephalopathy
/ Wasting Disease, Chronic - metabolism
/ Wasting Disease, Chronic - transmission
2024
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Norwegian moose CWD induces clinical disease and neuroinvasion in gene-targeted mice expressing cervid S138N prion protein
Journal Article
Norwegian moose CWD induces clinical disease and neuroinvasion in gene-targeted mice expressing cervid S138N prion protein
2024
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Overview
Chronic wasting disease (CWD) is a prion disease affecting deer, elk and moose in North America and reindeer, moose and red deer in Northern Europe. Pathogenesis is driven by the accumulation of PrP Sc , a pathological form of the host’s cellular prion protein (PrP C ), in the brain. CWD is contagious among North American cervids and Norwegian reindeer, with prions commonly found in lymphatic tissue. In Nordic moose and red deer CWD appears exclusively in older animals, and prions are confined to the CNS and undetectable in lymphatic tissues, indicating a sporadic origin. We aimed to determine transmissibility, neuroinvasion and lymphotropism of Nordic CWD isolates using gene-targeted mice expressing either wild-type (138SS/226QQ) or S138N (138NN/226QQ) deer PrP. When challenged with North American CWD strains, mice expressing S138N PrP did not develop clinical disease but harbored prion seeding activity in brain and spleen. Here, we infected these models intracerebrally or intraperitoneally with Norwegian moose, red deer and reindeer CWD isolates. The moose isolate was the first CWD type to cause full-blown disease in the 138NN/226QQ model in the first passage, with 100% attack rate and shortened survival times upon second passage. Furthermore, we detected prion seeding activity or PrP Sc in brains and spinal cords, but not spleens, of 138NN/226QQ mice inoculated intraperitoneally with the moose isolate, providing evidence of prion neuroinvasion. We also demonstrate, for the first time, that transmissibility of the red deer CWD isolate was restricted to transgenic mice overexpressing elk PrP C (138SS/226EE), identical to the PrP primary structure of the inoculum. Our findings highlight that susceptibility to clinical disease is determined by the conformational compatibility between prion inoculum and host PrP primary structure. Our study indicates that neuroinvasion of Norwegian moose prions can occur without, or only very limited, replication in the spleen, an unprecedented finding for CWD.
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