Dead-End 1 (DND1) encodes an RNA binding protein critical for viable primordial germ cells in vertebrates. When introduced into cancer cell lines, DND1 suppresses cell proliferation and enhances apoptosis. However, the molecular function of mammalian wild-type DND1 has mostly been studied in cell lines and not verified in the organism. To facilitate study of wild-type DND1 function in mammalian systems, we generated a novel transgenic mouse line, LSL-FM-DND1 , which conditionally expresses genetically engineered, FLAG-tagged and myc-tagged DND1 in a cell type-specific manner. We report that FLAG-myc-DND1 is indeed expressed in specific tissues of the mouse when LSL-FM-DND1 is combined with mouse strains expressing Cre-recombinase. LSL-FM-DND1 mice are fertile with no overt health effects. We expressed FLAG-myc-DND1 in the pancreas and found that chronic, ectopic expression of FLAG-myc-DND1 led to increase in fasting glucose levels in older mice. Thus, this novel LSL-FM-DND1 mouse strain will facilitate studies on the biological and molecular function of wild-type DND1.

Download full-text PDF

Source
http://dx.doi.org/10.1002/dvg.23335DOI Listing

Publication Analysis

Top Keywords

wild-type dnd1
12
mouse strain
8
cell lines
8
molecular function
8
function mammalian
8
mouse lsl-fm-dnd1
8
dnd1
7
mouse
5
generation novel
4
novel mouse
4

Similar Publications

Want AI Summaries of new PubMed Abstracts delivered to your In-box?

Enter search terms and have AI summaries delivered each week - change queries or unsubscribe any time!