Utvidet returrett til 31. januar 2025

Sirt1 Deficiency Compromises Embryonic and Adult Hematopoiesis in Mice

av Xuan Ou
Om Sirt1 Deficiency Compromises Embryonic and Adult Hematopoiesis in Mice

SIRT1 is a founding member of a sirtuin family of seven proteins and histone deacetylases. It is involved in cellular resistance to stress, metabolism, differentiation, aging, and tumor suppression. SIRT1-/- mice demonstrate embryonic and postnatal development defects. We examined hematopoietic and endothelial cell differentiation of SIRT1-/- mouse embryonic stem cells (ESCs) in vitro, and hematopoietic progenitors in SIRT1+/+, +/-, and -/- mice. SIRT1-/- ESCs formed fewer mature blast cell colonies. Replated SIRT1-/- BL-CFCs demonstrated defective hematopoietic potential. Endothelial cell production was unaltered, but there were defects in formation of a primitive vascular network from SIRT1-/- derived embryoid bodies. Development of primitive and definitive progenitors derived from SIRT1-/- ESCs were also delayed and/or defective. Differentiation delay/defects were associated with delayed capacity to switch off Oct4, Nanog and Fgf5 expression, decreased ¿-H1 globin, ¿-major globin, and Scl gene expression, and reduced activation of Erk1/2. Ectopic expression of SIRT1 rescued SIRT1-/- ESC differentiation deficiencies.

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  • Språk:
  • Engelsk
  • ISBN:
  • 9783844389654
  • Bindende:
  • Paperback
  • Sider:
  • 152
  • Utgitt:
  • 29. juni 2011
  • Dimensjoner:
  • 229x152x9 mm.
  • Vekt:
  • 231 g.
  • BLACK NOVEMBER
  Gratis frakt
Leveringstid: 2-4 uker
Forventet levering: 27. desember 2024
Utvidet returrett til 31. januar 2025

Beskrivelse av Sirt1 Deficiency Compromises Embryonic and Adult Hematopoiesis in Mice

SIRT1 is a founding member of a sirtuin family of seven proteins and histone deacetylases. It is involved in cellular resistance to stress, metabolism, differentiation, aging, and tumor suppression. SIRT1-/- mice demonstrate embryonic and postnatal development defects. We examined hematopoietic and endothelial cell differentiation of SIRT1-/- mouse embryonic stem cells (ESCs) in vitro, and hematopoietic progenitors in SIRT1+/+, +/-, and -/- mice. SIRT1-/- ESCs formed fewer mature blast cell colonies. Replated SIRT1-/- BL-CFCs demonstrated defective hematopoietic potential. Endothelial cell production was unaltered, but there were defects in formation of a primitive vascular network from SIRT1-/- derived embryoid bodies. Development of primitive and definitive progenitors derived from SIRT1-/- ESCs were also delayed and/or defective. Differentiation delay/defects were associated with delayed capacity to switch off Oct4, Nanog and Fgf5 expression, decreased ¿-H1 globin, ¿-major globin, and Scl gene expression, and reduced activation of Erk1/2. Ectopic expression of SIRT1 rescued SIRT1-/- ESC differentiation deficiencies.

Brukervurderinger av Sirt1 Deficiency Compromises Embryonic and Adult Hematopoiesis in Mice



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