- no phenotypic analysis / MGI
B6.129(C)-Cx3cr1tm2.1(cre/ERT2)Jung/Orl
Status | Available to order |
EMMA ID | EM:06350 |
International strain name | B6.129(C)-Cx3cr1tm2.1(cre/ERT2)Jung/Orl |
Alternative name | CX3CR1-CreER |
Strain type | Targeted Mutant Strains : Knock-in |
Allele/Transgene symbol | Cx3cr1tm2.1(cre/ERT2)Jung, |
Gene/Transgene symbol | Cx3cr1 |
Information from provider
Provider | Steffen Jung |
Provider affiliation | Immunology, Weizmann Institute of Science |
Genetic information | For the generation of the CX3CR1-CreER mice the homologous regions of the vector contained a 1.2 kb fragment upstream of the Cx3cr1 start codon (Short Homology) and an 8 kb fragment spanning the 3' end of the Cx3cr1 coding exon (Long Homology). The CreERT2 cassette gene, a kind gift of D. Metzger (Indra et al., 1999), and loxP flanked neomycin resistance gene were introduced replacing the first 390 bp of the Cx3cr1 gene, a HSV-tk gene was cloned downstream of the LH to select against random integration (Jung et al., 2000). ES cells were manipulated as described previously (Jung et al., 2000). Briefly, linearized targeting vector was electroporated into ES cells (129 R1 cells). CX3CR1CreER ES cells were negatively selected against random integration by the addition of ganciclovir. Cells were positively selected for neomycin resistance with G418 (200 µg/ml) and resistant colonies were isolated and analyzed for homologous recombination by PCR. |
Phenotypic information | CX3CR1-CreER mice harbor a gene encoding a cre recombinase-estrogen receptor fusion. This leads in Cx3cr1 expressing cells to latent cre activity that can be activated by tamoxifen administration. |
Breeding history | The strain was backcrossed more than 10 generations to C57BL/6 and the neo gene was removed by a cross to PGK-cre transgenic mice (also on C57BL/6). |
References |
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Homozygous fertile | yes |
Homozygous viable | yes |
Homozygous matings required | no |
Immunocompromised | no |
Information from EMMA
Archiving centre | Institut de Transgenose, INTRAGENE, Orléans, France |
Animals used for archiving | homozygous C57BL/6J |
Disease and phenotype information
MGI phenotypes (allele matching)
Literature references
- Fate mapping reveals origins and dynamics of monocytes and tissue macrophages under homeostasis.;Yona Simon, Kim Ki-Wook, Wolf Yochai, Mildner Alexander, Varol Diana, Breker Michal, Strauss-Ayali Dalit, Viukov Sergey, Guilliams Martin, Misharin Alexander, Hume David A, Perlman Harris, Malissen Bernard, Zelzer Elazar, Jung Steffen, ;2013;Immunity;38;79-91; 23273845
- A new type of microglia gene targeting shows TAK1 to be pivotal in CNS autoimmune inflammation.;Goldmann Tobias, Wieghofer Peter, Müller Philippe F, Wolf Yochai, Varol Diana, Yona Simon, Brendecke Stefanie M, Kierdorf Katrin, Staszewski Ori, Datta Moumita, Luedde Tom, Heikenwalder Mathias, Jung Steffen, Prinz Marco, ;2013;Nature neuroscience;16;1618-26; 24077561
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