Rapid in vivo evaluation system for cholestasis-related genes in mice with humanized bile acid profiles
Kihiro Wakasa,
Ryutaro Tamura,
Shuhei Osaka
et al.
Abstract:Background:
Pediatric cholestatic liver diseases (Ped-CLD) comprise many ultrarare disorders with a genetic basis. Pharmacologic therapy for severe cases of Ped-CLD has not been established. Species differences in bile acid (BA) metabolism between humans and rodents contribute to the lack of phenocopy of patients with Ped-CLD in rodents and hinder the development of therapeutic strategies. We aimed to establish an efficient in vivo system to understand BA-related pathogenesis, such as Ped-CLD.
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