Physiological Notch Signaling Maintains Bone Homeostasis via RBPjk and Hey Upstream of NFATc1
Notch signaling between neighboring cells controls many cell fate decisions in metazoans both during embryogenesis and in postnatal life. Previously, we uncovered a critical role for physiological Notch signaling in suppressing osteoblast differentiation in vivo. However, the contribution of individual Notch receptors and the downstream signaling mechanism have not been elucidated. Here we report that removal of Notch2, but not Notch1, from the embryonic limb mesenchyme markedly increased trabecular bone mass in adolescent mice. Deletion of the transcription factor RBPjk, a mediator of all canonical Notch signaling, in the mesenchymal progenitors but not the more mature osteoblast-lineage cells, caused a dramatic high-bone-mass phenotype characterized by increased osteoblast numbers, diminished bone marrow mesenchymal progenitor pool, and rapid age-dependent bone loss. Moreover, mice deficient in Hey1 and HeyL, two target genes of Notch-RBPjk signaling, exhibited high bone mass. Interestingly, Hey1 bound to and suppressed the NFATc1 promoter, and RBPjk deletion increased NFATc1 expression in bone. Finally, pharmacological inhibition of NFAT alleviated the high-bone-mass phenotype caused by RBPjk deletion. Thus, Notch-RBPjk signaling functions in part through Hey1-mediated inhibition of NFATc1 to suppress osteoblastogenesis, contributing to bone homeostasis in vivo.
Vyšlo v časopise:
Physiological Notch Signaling Maintains Bone Homeostasis via RBPjk and Hey Upstream of NFATc1. PLoS Genet 8(3): e32767. doi:10.1371/journal.pgen.1002577
Kategorie:
Research Article
prolekare.web.journal.doi_sk:
https://doi.org/10.1371/journal.pgen.1002577
Souhrn
Notch signaling between neighboring cells controls many cell fate decisions in metazoans both during embryogenesis and in postnatal life. Previously, we uncovered a critical role for physiological Notch signaling in suppressing osteoblast differentiation in vivo. However, the contribution of individual Notch receptors and the downstream signaling mechanism have not been elucidated. Here we report that removal of Notch2, but not Notch1, from the embryonic limb mesenchyme markedly increased trabecular bone mass in adolescent mice. Deletion of the transcription factor RBPjk, a mediator of all canonical Notch signaling, in the mesenchymal progenitors but not the more mature osteoblast-lineage cells, caused a dramatic high-bone-mass phenotype characterized by increased osteoblast numbers, diminished bone marrow mesenchymal progenitor pool, and rapid age-dependent bone loss. Moreover, mice deficient in Hey1 and HeyL, two target genes of Notch-RBPjk signaling, exhibited high bone mass. Interestingly, Hey1 bound to and suppressed the NFATc1 promoter, and RBPjk deletion increased NFATc1 expression in bone. Finally, pharmacological inhibition of NFAT alleviated the high-bone-mass phenotype caused by RBPjk deletion. Thus, Notch-RBPjk signaling functions in part through Hey1-mediated inhibition of NFATc1 to suppress osteoblastogenesis, contributing to bone homeostasis in vivo.
Zdroje
1. Artavanis-TsakonasSRandMDLakeRJ 1999 Notch signaling: cell fate control and signal integration in development. Science 284 770 776
2. ChibaS 2006 Notch signaling in stem cell systems. Stem Cells 24 2437 2447
3. D'SouzaBMeloty-KapellaLWeinmasterG 2010 Canonical and non-canonical Notch ligands. Curr Top Dev Biol 92 73 129
4. SchroeterEHKisslingerJAKopanR 1998 Notch-1 signalling requires ligand-induced proteolytic release of intracellular domain. Nature 393 382 386
5. KopanRGoateA 2000 A common enzyme connects notch signaling and Alzheimer's disease. Genes Dev 14 2799 2806
6. KopanRIlaganMX 2009 The canonical Notch signaling pathway: unfolding the activation mechanism. Cell 137 216 233
7. HonjoT 1996 The shortest path from the surface to the nucleus: RBP-J kappa/Su(H) transcription factor. Genes Cells 1 1 9
8. IsoTKedesLHamamoriY 2003 HES and HERP families: multiple effectors of the Notch signaling pathway. J Cell Physiol 194 237 255
9. Martinez AriasAZecchiniVBrennanK 2002 CSL-independent Notch signalling: a checkpoint in cell fate decisions during development? Curr Opin Genet Dev 12 524 533
10. McDaniellRWarthenDMSanchez-LaraPAPaiAKrantzID 2006 NOTCH2 mutations cause Alagille syndrome, a heterogeneous disorder of the notch signaling pathway. Am J Hum Genet 79 169 173
11. SandersPGMunoz-DescalzoSBalayoTWirtz-PeitzFHaywardP 2009 Ligand-independent traffic of Notch buffers activated Armadillo in Drosophila. PLoS Biol 7 e1000169 doi:10.1371/journal.pbio.1000169
12. DunwoodieSLClementsMSparrowDBSaXConlonRA 2002 Axial skeletal defects caused by mutation in the spondylocostal dysplasia/pudgy gene Dll3 are associated with disruption of the segmentation clock within the presomitic mesoderm. Development 129 1795 1806
13. ShenJBronsonRTChenDFXiaWSelkoeDJ 1997 Skeletal and CNS defects in Presenilin-1-deficient mice. Cell 89 629 639
14. WongPCZhengHChenHBecherMWSirinathsinghjiDJ 1997 Presenilin 1 is required for Notch1 and DII1 expression in the paraxial mesoderm. Nature 387 288 292
15. ZhangNGridleyT 1998 Defects in somite formation in lunatic fringe-deficient mice. Nature 394 374 377
16. PanYLiuZShenJKopanR 2005 Notch1 and 2 cooperate in limb ectoderm to receive an early Jagged2 signal regulating interdigital apoptosis. Dev Biol 286 472 482
17. JiangRLanYChapmanHDShawberCNortonCR 1998 Defects in limb, craniofacial, and thymic development in Jagged2 mutant mice. Genes Dev 12 1046 1057
18. BulmanMPKusumiKFraylingTMMcKeownCGarrettC 2000 Mutations in the human delta homologue, DLL3, cause axial skeletal defects in spondylocostal dysostosis. Nat Genet 24 438 441
19. LiLKrantzIDDengYGeninABantaAB 1997 Alagille syndrome is caused by mutations in human Jagged1, which encodes a ligand for Notch1. Nat Genet 16 243 251
20. OdaTElkahlounAGPikeBLOkajimaKKrantzID 1997 Mutations in the human Jagged1 gene are responsible for Alagille syndrome. Nat Genet 16 235 242
21. HiltonMJTuXWuXBaiSZhaoH 2008 Notch signaling maintains bone marrow mesenchymal progenitors by suppressing osteoblast differentiation. Nat Med 14 306 314
22. ZanottiSSmerdel-RamoyaAStadmeyerLDurantDRadtkeF 2008 Notch inhibits osteoblast differentiation and causes osteopenia. Endocrinology 149 3890 3899
23. EnginFYaoZYangTZhouGBertinT 2008 Dimorphic effects of Notch signaling in bone homeostasis. Nat Med 14 299 305
24. TaoJChenSYangTDawsonBMunivezE 2010 Osteosclerosis owing to Notch gain of function is solely Rbpj-dependent. J Bone Miner Res 25 2175 2183
25. GargVMuthANRansomJFSchlutermanMKBarnesR 2005 Mutations in NOTCH1 cause aortic valve disease. Nature 437 270 274
26. MohamedSAAherrahrouZLiptauHErasmiAWHagemannC 2006 Novel missense mutations (p.T596M and p.P1797H) in NOTCH1 in patients with bicuspid aortic valve. Biochem Biophys Res Commun 345 1460 1465
27. SimpsonMAIrvingMDAsilmazEGrayMJDafouD 2011 Mutations in NOTCH2 cause Hajdu-Cheney syndrome, a disorder of severe and progressive bone loss. Nature genetics 43 303 305
28. IsidorBLindenbaumPPichonOBezieauSDinaC 2011 Truncating mutations in the last exon of NOTCH2 cause a rare skeletal disorder with osteoporosis. Nature genetics 43 306 308
29. GraefIAChenFCrabtreeGR 2001 NFAT signaling in vertebrate development. Curr Opin Genet Dev 11 505 512
30. RangerAMGerstenfeldLCWangJKonTBaeH 2000 The nuclear factor of activated T cells (NFAT) transcription factor NFATp (NFATc2) is a repressor of chondrogenesis. J Exp Med 191 9 22
31. TakayanagiHKimSKogaTNishinaHIsshikiM 2002 Induction and activation of the transcription factor NFATc1 (NFAT2) integrate RANKL signaling in terminal differentiation of osteoclasts. Dev Cell 3 889 901
32. KogaTMatsuiYAsagiriMKodamaTde CrombruggheB 2005 NFAT and Osterix cooperatively regulate bone formation. Nat Med 11 880 885
33. WinslowMMPanMStarbuckMGalloEMDengL 2006 Calcineurin/NFAT signaling in osteoblasts regulates bone mass. Dev Cell 10 771 782
34. LoganMMartinJFNagyALobeCOlsonEN 2002 Expression of Cre Recombinase in the developing mouse limb bud driven by a Prxl enhancer. Genesis 33 77 80
35. RoddaSJMcMahonAP 2006 Distinct roles for Hedgehog and canonical Wnt signaling in specification, differentiation and maintenance of osteoblast progenitors. Development 133 3231 3244
36. MiaoDHeBJiangYKobayashiTSoroceanuMA 2005 Osteoblast-derived PTHrP is a potent endogenous bone anabolic agent that modifies the therapeutic efficacy of administered PTH 1-34. J Clin Invest 115 2402 2411
37. BaiSKopanRZouWHiltonMJOngCT 2008 NOTCH1 regulates osteoclastogenesis directly in osteoclast precursors and indirectly via osteoblast lineage cells. J Biol Chem 283 6509 6518
38. SalieRKneisselMVukevicMZamurovicNKramerI 2010 Ubiquitous overexpression of Hey1 transcription factor leads to osteopenia and chondrocyte hypertrophy in bone. Bone 46 680 694
39. FischerASteidlCWagnerTULangEJakobPM 2007 Combined loss of Hey1 and HeyL causes congenital heart defects because of impaired epithelial to mesenchymal transition. Circ Res 100 856 863
40. DongYJesseAMKohnAGunnellLMHonjoT 2010 RBPjkappa-dependent Notch signaling regulates mesenchymal progenitor cell proliferation and differentiation during skeletal development. Development 137 1461 1471
41. ZanottiSSmerdel-RamoyaACanalisE 2010 Reciprocal regulation of notch and nuclear factor of activated T-cells (NFAT)c1 transactivation in osteoblasts. J Biol Chem
42. MizutaniKYoonKDangLTokunagaAGaianoN 2007 Differential Notch signalling distinguishes neural stem cells from intermediate progenitors. Nature 449 351 355
43. ChengHTKimMValeriusMTSurendranKSchuster-GosslerK 2007 Notch2, but not Notch1, is required for proximal fate acquisition in the mammalian nephron. Development 134 801 811
44. SurendranKBoyleSBarakHKimMStomberskiC 2009 The contribution of Notch1 to nephron segmentation in the developing kidney is revealed in a sensitized Notch2 background and can be augmented by reducing Mint dosage. Dev Biol 337 386 395
45. RangarajanATaloraCOkuyamaRNicolasMMammucariC 2001 Notch signaling is a direct determinant of keratinocyte growth arrest and entry into differentiation. Embo J 20 3427 3436
46. DemehriSTurkozAKopanR 2009 Epidermal Notch1 loss promotes skin tumorigenesis by impacting the stromal microenvironment. Cancer Cell 16 55 66
47. PanYLinMHTianXChengHTGridleyT 2004 gamma-secretase functions through Notch signaling to maintain skin appendages but is not required for their patterning or initial morphogenesis. Dev Cell 7 731 743
48. McCrightBLozierJGridleyT 2006 Generation of new Notch2 mutant alleles. Genesis 44 29 33
49. HanHTanigakiKYamamotoNKurodaKYoshimotoM 2002 Inducible gene knockout of transcription factor recombination signal binding protein-J reveals its essential role in T versus B lineage decision. Int Immunol 14 637 645
50. FischerASchumacherNMaierMSendtnerMGesslerM 2004 The Notch target genes Hey1 and Hey2 are required for embryonic vascular development. Genes Dev 18 901 911
51. AliprantisAOUekiYSulyantoRParkASigristKS 2008 NFATc1 in mice represses osteoprotegerin during osteoclastogenesis and dissociates systemic osteopenia from inflammation in cherubism. J Clin Invest 118 3775 3789
52. ChuvpiloSJankevicsETyrsinDAkimzhanovAMorozD 2002 Autoregulation of NFATc1/A expression facilitates effector T cells to escape from rapid apoptosis. Immunity 16 881 895
53. HuppertSSLeASchroeterEHMummJSSaxenaMT 2000 Embryonic lethality in mice homozygous for a processing-deficient allele of Notch1. Nature 405 966 970
54. VihmaHPruunsildPTimmuskT 2008 Alternative splicing and expression of human and mouse NFAT genes. Genomics 92 279 291
55. WeiCLWuQVegaVBChiuKPNgP 2006 A global map of p53 transcription-factor binding sites in the human genome. Cell 124 207 219
Štítky
Genetika Reprodukčná medicínaČlánok vyšiel v časopise
PLOS Genetics
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