Gene Summary
IMPC Data Collections
- No Body Weight Data
- No Embryo Imaging Data
- Viability Data
The IMPC applies a panel of phenotyping screens to characterise single-gene knockout mice by comparison to wild types. Click on the different tabs to visualise significant phenotypes identified by the IMPC, as well as all data that was measured.
The analysis uses data from IMPC, along with published data on other mouse mutants, in comparison to human disease reports in OMIM, Orphanet, and DECIPHER.
Phenotype comparisons summarize the similarity of mouse phenotypes with human disease phenotypes.
The table below shows human diseases associated to Dnah9 by orthology or direct annotation.
Disease | Similarity of phenotypes |
Matching phenotypes | Source |
---|---|---|---|
Ciliary Dyskinesia, Primary, 40 | Absent outer dynein arms, Azoospermia | OMIM:618300 | |
Primary Ciliary Dyskinesia | Nasal polyposis | ORPHA:244 |
The table below shows human diseases predicted to be associated to Dnah9 by phenotypic similarity.
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MGI Allele | Allele Type | Produced |
---|---|---|
Dnah9tm44288(L1L2_gt2) | KO first allele (reporter-tagged insertion with conditional potential) | Targeting vectors |
Dnah9tm44288(L1L2_gt1) | KO first allele (reporter-tagged insertion with conditional potential) | Targeting vectors |
Dnah9em1(IMPC)Tcp | Exon Deletion | Mice, Tissue |
Dnah9tm44288(L1L2_Bact_P) | KO first allele (reporter-tagged insertion with conditional potential) | Targeting vectors |
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