Recombinant Mouse Homeobox protein SIX2 (Six2)

1. Reveal a unique dose response of nephron progenitors to the level of SIX2 protein in which the role of SIX2 in progenitor proliferation versus self-renewal is separable. PMID: 29217079
2. Embryonic day 18.5 Six2Frs2alphaKO kidneys were hypoplastic and not cystic, postnatal day (P) 7 mutants had proximal tubular-derived cysts that nearly replaced the renal parenchyma by P21. Mutants had high proximal tubular proliferation rates and interstitial fibrosis, similar to known polycystic kidney disease models. PMID: 27853247
3. GATA1 may be a potential regulator of Six2-maintained population of nephron progenitor cells. PMID: 28842839
4. Six2 mediates the protective effects of GDNF on damaged DA neurons by regulating Smurf1 expression. PMID: 27148690
5. Differentiation of nephron progenitors requires downregulation of Six2, a transcription factor required for progenitor maintenance, and that Notch signaling is necessary and sufficient for Six2 downregulation. PMID: 27633993
6. Zeb1 promotes proliferation and apoptosis and inhibits the migration of metanephric mesenchyme cells, in association with Six2. PMID: 27509493
7. In Six2-positive nephrogenic progenitors, GLI3 repressor decreased progenitor cell proliferation reducing the number of nephrogenic precursor structures in the Pallister-Hall syndrome mouse model. PMID: 26604140
8. Mechanistically, LIF activates STAT, which binds to a Stat consensus sequence in the Six2 proximal promoter and sustains SIX2 levels. PMID: 26321142
9. Dicer ablation in the early metanephric mesenchyme results in severe renal dysgenesis despite normal initial specification of nephron progenitors and ureteric bud outgrowth. PMID: 24500693
10. miR181c downregulates the expression of Six2, restrain the proliferation and promote the apoptosis that even makes the nephron progenitor phenotype lose MM cells, suggesting a potential role of miR181c during the kidney development. PMID: 25187057
11. results reveal a functional link between Eya1, Six2, and Myc in driving the expansion and maintenance of the multipotent progenitors during nephrogenesis PMID: 25458011
12. Our findings establish Six2 as a regulator of metastasis in human breast cancers and demonstrate an epigenetic function for SIX family transcription factors in metastatic progression through the regulation of E-cadherin. PMID: 25348955
13. These results implied that inhibition of Nf1 may delay metanephros development via down-regulation of Six2. PMID: 24573885
14. Osr1 plays crucial roles in Six2-dependent maintenance of nephron progenitors during mammalian nephrogenesis. PMID: 24598167
15. this study concluded that by targeting the transcription factor gene Six2, miR-181b inhibits the proliferation of metanephric mesenchymal cells in vitro and might play an important role in the formation of nephrons. PMID: 24055707
16. Wnt and BMP signaling cooperate with Hox in the control of Six2 expression in limb tendon precursor. PMID: 23499659
17. The Six2 and Lef/Tcf factors form a regulatory complex that promotes progenitor maintenance while entry of beta-catenin into this complex promotes nephrogenesis. PMID: 22902740
18. Results demonstrate impaired osmoregulatory mechanisms consistent with chronic renal failure in the Br/+ mouse and indicate that six2 haploinsufficiency has a direct effect on postnatal fluid and electrolyte handling associated with fluid imbalance. PMID: 21653879
19. wnt9b signaling regulates stem cell proliferation and differention in the developing kidney depending on the activity of the transcription factor Six2 in the responding cell. PMID: 21350016
20. Six4 and Six5 repressed, while Six1 activated myogenin expression, suggesting that the differential regulation of myogenin expression is responsible for the differential effects of Six genes PMID: 20696153
21. Inactivation of Six2 in mouse identifies a novel genetic mechanism controlling development and growth of the cranial base. PMID: 20515681
22. Notch2 activation did not skew the cell fate toward the proximal nephron but resulted in severe kidney dysgenesis and depletion of Six2-positive progenitors. PMID: 20299358
23. Six2 activates Gdnf expression PMID: 15327782
24. Hoxa2 regulation of Six2 is confined to a 0.9 kb fragment of the Six2 promoter and that Hoxa2 binds to this promoter region PMID: 15634706
25. our results suggest a cell-intrinsic role of Six2 in the survival of early-generated trigeminal sensory neurons PMID: 16938278
26. in the developing kidney, Six2 activity is required for maintaining the mesenchymal progenitor population in an undifferentiated state PMID: 17036046
27. Six2 and Six6 differ in their DNA-binding mechanisms and in the consequences of their interaction with protein tyrosine phosphatase Eyes Absent in Six2/6-DNA-binding ability. PMID: 18293925
28. propose that Six2 acts to mediate Hoxa2 control over the insulin-like growth factor pathway during branchial arch development PMID: 18321982
29. Data suggest a mutation in a novel cis-acting regulatory region inhibits Six2 expression and is associated with frontonasal dysplasia and renal hypoplasia. PMID: 18570229
30. Defects are associated with embryological deficiencies of Six2, suggesting that proper levels of this protein during nephrogenesis are critical for normal glomerular development and adult renal function PMID: 19193724
31. Six2 activity regulates a gene network which includes Bmp4, Bmpr1b, Nkx2.5, Sox9, & Gremlin during the genesis of the pyloric sphincter in the mouse. It maintains a Bmp4-free PS territory for proper morphogenesis of the PS in the mouse stomach. PMID: 19660448
32. Data demonstrate that a single enhancer site upstream of the Six2 coding sequence is responsible for both activation by Hox11 proteins in the kidney and repression by Hoxa2 in the branchial arch and facial mesenchyme in vivo. PMID: 19716816

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KEGG: mmu:20472

STRING: 10090.ENSMUSP00000024947

UniGene: Mm.5039