Recombinant Mouse Exostosin-1 (Ext1), partial

1. reactivating SHH signaling in mutant lungs rescued the tip dilation phenotype and attenuated FGF signaling. Importantly, the reduced SHH signaling activity did not appear to be caused by decreased Shh expression or protein stability; instead, biologically active form of SHH proteins were reduced in both the Ext1 mutant epithelium and surrounding wild type mesenchymal cells. PMID: 28859094
2. crucial for outflow tract formation in distinct progenitor cells and modulates FGF signaling during early heart development PMID: 26295701
3. Normal heparin sulfate levels and Ext1 activity in the stromal microenvironment and hematopoietic stem cells are required for the transplant engraftment following non-myeloablative conditioning. PMID: 25976459
4. Heterozygous loss of function of EXT1 and EXT2 results in a decreased arteriolar endothelial glycocalyx but improved flow mediated vasodilation. PMID: 25468659
5. Ext genes and heparan sulfate are needed to establish and maintain perichondrium's phenotype and border function. PMID: 23458899
6. Levels of Ext1 and HPSE influence the motility of FBJ osteosarcoma cells. PMID: 23054193
7. stromal Ext1-levels modulate tumor cell proliferation and affect the interstitial fluid pressure in a 3-D spheroid model. PMID: 22848466
8. The study indicates that formation of stereotypic exostoses requires a significant, but not complete, loss of Ext expression. PMID: 21310272
9. local Ext1 expression and heparan sulfate production are needed to maintain the phenotype and function of joint-forming cells. PMID: 21185280
10. Ext1 has a role in regulation of bone morphogenic protein signaling and skeletal defects PMID: 20404326
11. inactivation of Ext1 in a small fraction of chondrocytes is sufficient for the development of osteochondromas and other skeletal defects associated with multiple hereditary exostoses PMID: 20534475
12. for a model of multiple osteochondromas, we created the chimeric tissue genotype of somatic loss of heterozygosity, by conditionally inactivating Ext1 in chondrocytes PMID: 20080592
13. loss of heterozygosity is required for osteochondroma formation and a proliferating chondrocyte is suggested as its cell of origin PMID: 20133829
14. Induction of EXT1 knockdown in vivo dramatically suppresses the growth of bone marrow localized myeloma. PMID: 19965677
15. Data suggest that the length of the heparan sulfate (HS) chains is a critical determinant of HS-protein interactions and emphasize the essential role of EXT1 in providing specific binding sites for growth factors and extracellular matrix proteins. PMID: 19850926
16. EXT1 peaks during early postnatal period in the cerebrum and around birth in the cerebellum. EXT1 was localized primarily in the neuroepithelial cells surrounding the lateral ventricles, the mesencephalic vesicle, and the fourth ventricle. PMID: 12644256
17. Ext1 may have a role in normal mouse development PMID: 15161920
18. Reduced heparan sulfate synthesis in mice carrying a hypomorphic mutation in Ext1 results in an elevated range of Indian hedgehog (Ihh) signaling during embryonic chondrocyte differentiation. PMID: 15177029
19. Defects in EXT1 and the resulting reduction in heparan sulfate lead to enhanced Indian hedgehog diffusion causing an increase in chondrocyte proliferation and delayed hypertrophic differentiation. PMID: 15777636
20. NDST1 competes with EXT1 for binding to EXT2. PMID: 18337501

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KEGG: mmu:14042

STRING: 10090.ENSMUSP00000076505

UniGene: Mm.309395