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Publication : Generation and Characterization of an <i>Abcc1</i> Humanized Mouse Model (<i>hABCC1<sup>flx/flx</sup></i> ) with Knockout Capability.

First Author  Krohn M Year  2019
Journal  Mol Pharmacol Volume  96
Issue  2 Pages  138-147
PubMed ID  31189668 Mgi Jnum  J:284731
Mgi Id  MGI:6391901 Doi  10.1124/mol.119.115824
Citation  Krohn M, et al. (2019) Generation and Characterization of an Abcc1 Humanized Mouse Model (hABCC1(flx/flx) ) with Knockout Capability. Mol Pharmacol 96(2):138-147
abstractText  ATP-binding cassette (ABC) transporters such as ABCB1 (P-glycoprotein), ABCC1 (MRP1), and ABCG2 (BCRP) are well known for their role in rendering cancer cells resistant to chemotherapy. Additionally, recent research provided evidence that, along with other ABC transporters (ABCA1 and ABCA7), they might be cornerstones to tackle neurodegenerative diseases. Overcoming chemoresistance in cancer, understanding drug-drug interactions, and developing efficient and specific drugs that alter ABC transporter function are hindered by a lack of in vivo research models, which are fully predictive for humans. Hence, the humanization of ABC transporters in mice has become a major focus in pharmaceutical and neurodegenerative research. Here, we present a characterization of the first Abcc1 humanized mouse line. To preserve endogenous expression profiles, we chose to generate a knockin mouse model that leads to the expression of a chimeric protein that is fully human except for one amino acid. We found robust mRNA and protein expression within all major organs analyzed (brain, lung, spleen, and kidney). Furthermore, we demonstrate the functionality of the expressed human ABCC1 protein in brain and lungs using functional positron emission tomography imaging in vivo. Through the introduction of loxP sites, we additionally enabled this humanized mouse model for highly sophisticated studies involving cell type-specific transporter ablation. Based on our data, the presented mouse model appears to be a promising tool for the investigation of cell-specific ABCC1 function. It can provide a new basis for better translation of preclinical research.
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