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A triple-transgenic immunotolerant mouse model.

Brenden, Nina (author)
AstraZeneca, Safety Assessment, Södertälje, Sweden
Madeyski-Bengtson, Katja (author)
AstraZeneca, Discovery Sciences, Mölndal, Sweden
Martinsson, Klara (author)
AstraZeneca, Safety Assessment, Södertälje, Sweden
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Svärd, Rebecka (author)
AstraZeneca, Innovative Medicines, Mölndal, Sweden
Albery-Larsdotter, Sara (author)
AstraZeneca, Innovative Medicines, Mölndal, Sweden
Granath, Britta (author)
AstraZeneca, Safety Assessment, Södertälje, Sweden
Lundgren, Hanna (author)
AstraZeneca, Safety Assessment, Södertälje, Sweden
Lövgren, Ann (author)
AstraZeneca, Innovative Medicines, Mölndal, Sweden
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 (creator_code:org_t)
Elsevier BV, 2013
2013
English.
In: Journal of Pharmaceutical Sciences. - : Elsevier BV. - 0022-3549 .- 1520-6017. ; 102:3, s. 1116-24
  • Journal article (peer-reviewed)
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  • Avoiding unwanted immunogenicity is of key importance in the development of therapeutic drug proteins. Animal models are of less predictive value because most of the drug proteins are recognized as foreign proteins. However, different methods have been developed to obtain immunotolerant animal models. So far, the immunotolerant animal models have been developed to assess one protein at a time and are not suitable for the assessment of combination products. Our aim was to develop an animal model for evaluating the impact of manufacturing and formulation changes on immunogenicity, suitable for both single protein and combination products. We constructed two lines of transgenic mice expressing the three human coagulation factors, II, VII, and X, by inserting a single vector containing the three coagulation factors encoding sequences separated by insulator sequences derived from the chicken beta-globin locus into the mouse genome. Immunization of transgenic mice from the two lines and their wild-type littermates showed that transgenic mice from both lines were immunotolerant to the expressed human coagulation factors. We conclude that transgenic mice immunotolerant to multiple proteins can be obtained, and that these mice are potentially useful as animal models in the assessment of immunogenicity in response to manufacturing changes.

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