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B-Sp7-iCre mice
Strain Name

C57BL/6-Sp7tm1(icre)Bcgen/Bcgen

Stock No.  110131
Common name

B-Sp7-F2A-iCre mice

Gene symbol and name  Sp7(transcription factor 7), Osx
Strain of origin

C57BL/6

Chromosome  15
Coat color Black Dietary information Growth and reproduction diet for experimental mice
NCBI Gene ID
170574

Application

  • Function research of genes
  • This Sp7iCre model is an efficient tool to study various gene functions when crossed with mice with different loxP site-flanked genes of interest, especially in studies of bone development, osteoblast lineage, and Hedgehog/Wnt signaling.

Expression


Expressed gene

iCre, improved cre recombinase, bacteriophage P1


Site of expression

osteoblast lineage, embryos perichondrium, bone trabeculae, bone collars


Gene editing strategy


from clipboard


An F2A-iCre sequence cassette was placed between the coding sequence of exon 2 and 3’UTR of the Sp7 gene in C57BL/6 ES cells. This strain was maintained on a C57BL/6 genetic background.


Phenotype Analysis


from clipboard


Fig 4. qPCR, Western blot, and Immunofluorescence analyses showed that Fam20c knockout resulted in a decreased expression of Calpastatin in OB Fam20cKO cells (Fig. 4A, B, E), whereas accompanied by a decreased phosphorylated expression level of Calpastatin (Fig. 4C). These were consistent with the results of proteomics and phosphoproteomics. Furthermore, Fam20cdeficient osteoblasts displayed a diminished expression of Calpain 1 and Calpain 2 (Fig. 4A, B, E) and attenuation of Calpain activity (Fig. 4D).



(source: Liu et al. Journal of Translational Medicine (2023) 21:417)


Reference


1. Rodda SJ; McMahon AP. 2006. Distinct roles for Hedgehog and canonical Wnt signaling in specification, differentiation and maintenance of osteoblast progenitors. Development 133(16):3231-44. [PubMed: 16854976]

2. Canalis E; Parker K; Feng JQ; Zanotti S. 2013. Osteoblast lineage-specific effects of notch activation in the skeleton. Endocrinology 154(2):623-34. [PubMed: 23275471]  [MGI Ref ID J:194661] Canalis E; Parker K; Feng JQ; Zanotti S. 2013. Osteoblast lineage-specific effects of notch activation in the skeleton. Endocrinology 154(2):623-34. [PubMed: 23275471]

3. Chen J; Shi Y; Regan J; Karuppaiah K; Ornitz DM; Long F. 2014. Osx-Cre targets multiple cell types besides osteoblast lineage in postnatal mice. PLoS One 9(1):e85161. [PubMed: 24454809]

4. Liu Y; Strecker S; Wang L; Kronenberg MS; Wang W; Rowe DW; Maye P. 2013. Osterix-cre labeled progenitor cells contribute to the formation and maintenance of the bone marrow stroma. PLoS One 8(8):e71318. [PubMed: 23951132]

5. Shekaran A; Shoemaker JT; Kavanaugh TE; Lin AS; LaPlaca MC; Fan Y; Guldberg RE; Garcia AJ. 2014. The effect of conditional inactivation of beta 1 integrins using twist 2 Cre, Osterix Cre and osteocalcin Cre lines on skeletal phenotype. Bone 68:131-41. [PubMed: 25183373]

6. Liu J, Liang C, Guo B, Wu X, Li D, Zhang Z, Zheng K, Dang L, He X, Lu C, Peng S, Pan X, Zhang BT, Lu A, Zhang G. Increased PLEKHO1 within osteoblasts suppresses Smad-dependent BMP signaling to inhibit bone formation during aging. Aging Cell. 2017 Apr;16(2):360-376. [PubMed: 28083909]