Cd55<tm1c(EUCOMM)Hmgu> Targeted Allele Detail MGI Mouse (MGI:6502875)

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Cd55^{tm1c(EUCOMM)Hmgu}
Targeted Allele Detail

Summary | Mutation origin | Mutation description | Find Mice (IMSR) | References

Summary

Symbol:	Cd55^{tm1c(EUCOMM)Hmgu}
Name:	CD55 molecule, decay accelerating factor for complement; targeted mutation 1c, Helmholtz Zentrum Muenchen GmbH
MGI ID:	MGI:6502875
Synonyms:	DAF^fl
Gene:	Cd55 Location: Chr1:130366764-130390481 bp, - strand Genetic Position: Chr1, 56.89 cM
Alliance:	Cd55^{tm1c(EUCOMM)Hmgu} page
IMPC:	Cd55 gene page

Mutation
origin

Germline Transmission:	Earliest citation of germline transmission: J:294941
Parent Cell Line:	JM8A3.N1 (ES Cell)
Strain of Origin:	C57BL/6N-A^tm1Brd
Project Collection:	EUCOMM

Mutation
description

Allele Type:		Targeted (Conditional ready)
Mutation:		Insertion
		Mutation details: The L1L2_Bact_P cassette was inserted at position 130385505 of Chromosome 1 upstream of the critical exon(s) (Build GRCm39). The cassette is composed of an FRT site followed by lacZ sequence and a loxP site. This first loxP site is followed by a neomycin resistance gene under the control of the human beta-actin promoter, SV40 polyA, a second FRT site and a second loxP site. A third loxP site is inserted downstream of the targeted exon(s) at position 130388040. The critical exon(s) is/are thus flanked by loxP sites. A "conditional ready" (floxed) allele was created by flp recombinase expression in mice carrying this allele to remove the lacZ sequence and neo selection cassette, leaving loxP sites flanking the critical exon(s). Further information on targeting strategies used for this and other IKMC alleles can be found at http://www.informatics.jax.org/mgihome/nomen/IKMC_schematics.shtml (J:294941)

Find Mice (IMSR)

Mouse strains and cell lines available from the International Mouse Strain Resource (IMSR)
Carrying this Mutation:	Mouse Strains: 0 strains available Cell Lines: 0 lines available
Carrying any Cd55 Mutation:	37 strains or lines available

References

Original:	J:294941 Angeletti A, et al., Loss of decay-accelerating factor triggers podocyte injury and glomerulosclerosis. J Exp Med. 2020 Sep 7;217(9)
All:	1 reference(s)

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