Haaotm1b(KOMP)Wtsi
Targeted Allele Detail
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| Symbol: |
Haaotm1b(KOMP)Wtsi |
| Name: |
3-hydroxyanthranilate 3,4-dioxygenase; targeted mutation 1b, Wellcome Trust Sanger Institute |
| MGI ID: |
MGI:7705379 |
| Gene: |
Haao Location: Chr17:84138585-84155392 bp, - strand Genetic Position: Chr17, 54.85 cM, cytoband E4
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| Alliance: |
Haaotm1b(KOMP)Wtsi page
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| IMPC: |
Haao gene page |
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| Germline Transmission: |
Earliest citation of germline transmission:
J:352181
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| Parent Cell Line: |
JM8A3.N1 (ES Cell)
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| Strain of Origin: |
C57BL/6N-Atm1Brd
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| Project Collection: |
KOMP-CSD
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| Allele Type: |
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Targeted (Null/knockout, Reporter) |
| Mutations: |
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Insertion, Intragenic deletion
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Mutation details: The L1L2_Bact_P cassette was inserted at position 84141911 of Chromosome 17 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 84143483. The critical exon(s) is/are thus flanked by loxP sites. A null/knockout allele was created by cre recombinase expression in mice carrying the tm1a allele to remove the neo selection cassette and loxP-flanked 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:352181)
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| Original: |
J:352181 Dang H, et al., On the benefits of the tryptophan metabolite 3-hydroxyanthranilic acid in Caenorhabditis elegans and mouse aging. Nat Commun. 2023 Dec 14;14(1):8338 |
| All: |
1 reference(s) |
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