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1. Characterization of a novel fibroblast growth factor 10 (Fgf10) knock-in mouse line to target mesenchymal progenitors during embryonic development.

2. Characterization of a Novel Fibroblast Growth Factor 10 (Fgf10) Knock-In Mouse Line to Target Mesenchymal Progenitors during Embryonic Development

4. The role of the mucin-glycan foraging Ruminococcus gnavus in the communication between the gut and the brain

5. A mesenchymal to epithelial switch in Fgf10 expression specifies an evolutionary-conserved population of ionocytes in salivary glands

7. Frizzled-10 promotes sensory neuron development in Xenopus embryos

9. Levels of mesenchymal FGFR2 signaling modulate smooth muscle progenitor cell commitment in the lung

17. Interplay between metalloproteinases and cell signalling in blood brain barrier integrity

22. FGF10 (Fibroblast Growth Factor 10) plays a causative role in the tracheal cartilage defects in a mouse model of Apert Syndrome

24. Transient Inhibition of FGFR2b-Ligands Signaling Leads to Irreversible Loss of Cellular β-Catenin Organization and Signaling in AER during Mouse Limb Development

26. Corrigendum to “Localization and fate of Fgf10-expressing cells in the adult mouse brain implicate Fgf10 in control of neurogenesis” [Mol. Cell. Neurosci. 37 (2008) 857–868]

38. The role of the mucin-glycan foraging Ruminococcus gnavusin the communication between the gut and the brain

40. Embryonic Submandibular Gland Morphogenesis: Stage-Specific Protein Localization of FGFs, BMPs, Pax6 and Pax9 in Normal Mice and Abnormal SMG Phenotypes in FgfR2-IIIc+/Δ, BMP7–/– and Pax6–/–Mice

41. A Novel Mouse Fgfr2 Mutant, Hobbyhorse (hob), Exhibits Complete XY Gonadal Sex Reversal.

43. Fgf10-Expressing Tanycytes Add New Neurons to the Appetite/Energy-Balance Regulating Centers of the Postnatal and Adult Hypothalamus.

44. Interplay between metalloproteinases and cell signalling in blood brain barrier integrity.

45. Formation and differentiation of multiple mesenchymal lineages during lung development is regulated by beta-catenin signaling.

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