AGBL2
AGBL carboxypeptidase 2
- Ensembl:
- ENSG00000165923, ENSG00000285501
- UniProt:
- Q5U5Z8
- OMIM:
- 617345
- Synonyms:
- CCP2, FLJ23598
Cilia effects upon perturbation of AGBL2
- Cilia number / % ciliated:
- Decreased cilia number
- Loss-of-function effect:
- Shorter cilia
Ciliogenesis screen results (2 screens)
- Wheway et al. 2015 (siRNA) [siRNA]: Ciliogenesis Defect (z=-2.95) PMID:26167766
- Breslow et al. 2018 (CRISPR) [CRISPR]: No Significant Effect PMID:29459680
Phenotypes
- Mouse phenotype:
- increased grip strength
Ciliopathy associations
- Nonsyndromic Tetralogy of Fallot
Subcellular localization
basal body, cytosol
Functional category
- Ciliary assembly/disassembly
Function
AGBL2 has localized in basal body. We first examined the subcellular localization of these ciliary genes in both mouse embryonic fibroblasts (MEFs) and E10.5 mouse OFTs. Immunofluorescence staining analysis revealed that Mlf1 and Pkhd1l1 colocalized with acetylated α-tubulin and specifically accumulated in cilia axonemes, Sptbn5 colocalized with both acetylated α-tubulin and γ-tubulin along the entire cilia, Ppef2 and Tekt3 were localized to basal bodies of cilia, and Agbl2 was located at the base of cilia and overlapped with Nek2, a marker of centriole (Fig. 5A and fig. S16). We first examined the subcellular localization of these ciliary genes in both mouse embryonic fibroblasts (MEFs) and E10.5 mouse OFTs. Immunofluorescence staining analysis revealed that Mlf1 and Pkhd1l1 colocalized with acetylated α-tubulin and specifically accumulated in cilia axonemes, Sptbn5 colocalized with both acetylated α-tubulin and γ-tubulin along the entire cilia, Ppef2 and Tekt3 were localized to basal bodies of cilia, and Agbl2 was located at the base of cilia and overlapped with Nek2, a marker of centriole (Fig. 5A and fig. S16). However, because of the polygenic genetic architecture and low penetrance of nonsyndromic TOF, it was impossible to construct mouse models for each candidate ciliary gene to verify its pathogenic role in TOF. We therefore selected six previously unidentified genes (namely AGBL2, MLF1, PKHD1L1, PPEF2, SPTBN5, and TEKT3) with recurrent mutations for mouse models construction and phenotype validation, both to illustrate the reliability of our screening strategy and to provide in vivo evidence supporting the contribution of ciliary gene variants to TOF pathogenesis. (41071877)