C.129P2-Cx3cr1^tm1Litt/Ieg

Status	Available to order
EMMA ID	EM:00591
Citation information	RRID:IMSR_EM:00591 Research Resource Identifiers (RRID) are persistent unique ID numbers assigned to help researchers cite key resources (e.g. antibodies, model organisms and software projects) in the biomedical literature to improve transparency and reproducibility in research. See https://www.rrids.org/ for more information.
International strain name	C.129P2-Cx3cr1^tm1Litt/Ieg
Alternative name	CX3CR1/GFP
Strain type	Targeted Mutant Strains : Knock-out
Allele/Transgene symbol	Cx3cr1^tm1Litt
Gene/Transgene symbol	Cx3cr1

Information from provider

Provider	Steffen Jung
Provider affiliation	The Weizmann Institute of Science
Genetic information	The mutant mice carry a targeted replacement of the Cx3cr1 chemokine receptor gene with an EGFP reporter gene (see Jung et al. MCB 2000).
Phenotypic information	The mutant mice have no obvious defects.
References	Analysis of fractalkine receptor CX(3)CR1 function by targeted deletion and green fluorescent protein reporter gene insertion.;Jung S, Aliberti J, Graemmel P, Sunshine M J, Kreutzberg G W, Sher A, Littman D R, ;2000;Molecular and cellular biology;20;4106-14; 10805752

Information from EMMA

Archiving centre	Helmholtz Zentrum Muenchen - German Research Center for Environmental Health (GmbH), Oberschleißheim, Germany

Disease and phenotype information

IMPC phenotypes (gene matching)

abnormal kidney morphology / IMPC
small kidney / IMPC
abnormal caudal vertebrae morphology / IMPC
enlarged kidney / IMPC

MGI phenotypes (allele matching)

paresis / MGI
increased susceptibility to experimental autoimmune encephalomyelitis / MGI
microgliosis / MGI
homeostasis/metabolism phenotype / MGI
paralysis / MGI
demyelination / MGI
brain inflammation / MGI
abnormal leukocyte physiology / MGI
increased neuron apoptosis / MGI
abnormal microglial cell physiology / MGI
abnormal vascular wound healing / MGI
immune system phenotype / MGI
abnormal vascular smooth muscle physiology / MGI
brainstem hemorrhage / MGI
decreased NK cell number / MGI
increased sensitivity to induced morbidity/mortality / MGI
abnormal NK cell physiology / MGI
increased susceptibility to dopaminergic neuron neurotoxicity / MGI
abnormal dendritic cell physiology / MGI
abnormal small intestinal villus morphology / MGI
increased dendritic cell number / MGI
increased susceptibility to bacterial infection induced morbidity/mortality / MGI
decreased monocyte cell number / MGI
abnormal retina morphology / MGI
nervous system phenotype / MGI
impaired macrophage chemotaxis / MGI
decreased susceptibility to kidney reperfusion injury / MGI
choroidal neovascularization / MGI

MGI phenotypes (gene matching)

decreased monocyte cell number / MGI
paralysis / MGI
paresis / MGI
demyelination / MGI
abnormal retina morphology / MGI
retinal degeneration / MGI
brain inflammation / MGI
no abnormal phenotype detected / MGI
abnormal dendritic cell physiology / MGI
abnormal leukocyte physiology / MGI
no phenotypic analysis / MGI
increased neuron apoptosis / MGI
nervous system phenotype / MGI
abnormal microglial cell physiology / MGI
abnormal retinal photoreceptor layer morphology / MGI
impaired macrophage chemotaxis / MGI
decreased susceptibility to kidney reperfusion injury / MGI
increased susceptibility to experimental autoimmune encephalomyelitis / MGI
abnormal vascular wound healing / MGI
homeostasis/metabolism phenotype / MGI
immune system phenotype / MGI
choroidal neovascularization / MGI
abnormal vascular smooth muscle physiology / MGI
abnormal response to transplant / MGI
brainstem hemorrhage / MGI
retinal deposits / MGI
decreased NK cell number / MGI
abnormal small intestinal villus morphology / MGI
increased dendritic cell number / MGI
thin retinal outer nuclear layer / MGI
microgliosis / MGI
abnormal splenocyte physiology / MGI
increased sensitivity to induced morbidity/mortality / MGI
increased susceptibility to bacterial infection induced morbidity/mortality / MGI
abnormal NK cell physiology / MGI
increased susceptibility to dopaminergic neuron neurotoxicity / MGI

Literature references

Analysis of fractalkine receptor CX(3)CR1 function by targeted deletion and green fluorescent protein reporter gene insertion.;Jung S, Aliberti J, Graemmel P, Sunshine M J, Kreutzberg G W, Sher A, Littman D R, ;2000;Molecular and cellular biology;20;4106-14; 10805752
Microglial Cx3cr1 knockout reduces prion disease incubation time in mice.;Grizenkova Julia, Akhtar Shaheen, Brandner Sebastian, Collinge John, Lloyd Sarah E, ;2014;BMC neuroscience;15;44; 24655482
Vagus nerve stimulation dampens intestinal inflammation in a murine model of experimental food allergy.;Bosmans Goele, Appeltans Iris, Stakenborg Nathalie, Gomez-Pinilla Pedro J, Florens Morgane V, Aguilera-Lizarraga Javier, Matteoli Gianluca, Boeckxstaens Guy E, ;2019;Allergy;74;1748-1759; 30897213

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Order

Availabilities

Requesting frozen sperm or embryos is generally advisable wherever possible, in order to minimise the shipment of live mice.

Frozen embryos. Delivered in 4 weeks (after paperwork in place). €1740^*
Rederivation of mice from frozen stock, delivery time available upon request . €3880^*

Due to the dynamic nature of our processes strain availability may change at short notice. The local repository manager will advise you in these circumstances.

^* In addition users have to cover all the shipping costs (including the cost for returning dry-shippers, where applicable).

More details on pricing and delivery times

Practical information

Genotyping protocol

Example health report
(Current health report will be provided later)

Material Transfer Agreement (MTA)
Distribution of this strain is subject to a provider MTA. Both signing of the MTA and submission of the online EMMA Mutant Request Form are required before material can be shipped.

EMMA conditions
Legally binding conditions for the transfer

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C.129P2-Cx3cr1tm1Litt/Ieg