γ-Secretase activity is dispensable for mesenchyme-to-epithelium transition but required for podocyte and proximal tubule formation in developing mouse kidney

Cheng, Hui-Teng; Miner, Jeffrey H.; Lin, Meei-Hua; Tansey, Malú G.; Roth, Kevin A.; Kopan, Raphael

doi:10.1242/dev.00697

Cited by 197 publications

(192 citation statements)

References 68 publications

Supporting

Mentioning

174

Contrasting

Order By: Relevance

“…The absolute cell numbers with control Fc are ϳ5-fold higher than that with Delta4-Fc, and the fold increases in the cell number after the 3-wk culture were 45.7 Ϯ 31.6-fold (n ϭ 11). To confirm that the NK cell differentiation was Notch dependent, we added a ␥-secretase inhibitor, DAPT, which strongly inhibits ligand-dependent Notch activation (24,25). The cells cultured on Delta4-Fc-coated plates in the presence of DAPT had the same immunophenotype as those cultured on the control Fc-coated plates and did not give rise to NK cells (Fig.…”

Section: Human Cb Cd34 ϩ and Cd133 ϩ Cells Gave Rise To Functional Nkmentioning

confidence: 99%

Notch Activation Induces the Generation of Functional NK Cells from Human Cord Blood CD34-Positive Cells Devoid of IL-15

Haraguchi

Suzuki²,

Koyama³

et al. 2009

The Journal of Immunology

View full text Add to dashboard Cite

The development of NK cells from hematopoietic stem cells is thought to be dependent on IL-15. In this study, we demonstrate that stimulation of human cord blood CD34 ؉ cells by a Notch ligand, Delta4, along with IL-7, stem cell factor, and Fms-like tyrosine kinase 3 ligand, but no IL-15, in a stroma-free culture induced the generation of cells with characteristics of functional NK cells, including CD56 and CD161 Ag expression, IFN-␥ secretion, and cytotoxic activity against K562 and Jurkat cells. Addition of ␥-secretase inhibitor and anti-human Notch1 Ab to the culture medium almost completely blocked NK cell emergence. Addition of anti-human IL-15-neutralizing Ab did not affect NK cell development in these culture conditions. The presence of IL-15, however, augmented cytotoxicity and was required for a more mature NK cell phenotype. CD56 ؉ cells generated by culture with IL-15, but without Notch stimulation, were negative for CD7 and cytoplasmic CD3, whereas CD56 ؉ cells generated by culture with both Delta4 and IL-15 were CD7 ؉ and cytoplasmic CD3 ؉ from the beginning and therefore more similar to in vivo human NK cell progenitors. Together, these results suggest that Notch signaling is important for the physiologic development of NK cells at differentiation stages beyond those previously postulated.

show abstract

Section: Human Cb Cd34 ϩ and Cd133 ϩ Cells Gave Rise To Functional Nkmentioning

confidence: 99%

Notch Activation Induces the Generation of Functional NK Cells from Human Cord Blood CD34-Positive Cells Devoid of IL-15

Haraguchi

Suzuki²,

Koyama³

et al. 2009

The Journal of Immunology

View full text Add to dashboard Cite

show abstract

“…Studies of several signaling pathways, as well as transcription factors, have revealed genes involved in the patterning the nephron including Fgf8 (Grieshammer et al, 2005), Pou3f3 (Nakai et al, 2003),Sprouty (Basson et al, 2005;Basson et al, 2006), Notch/presenillins (Cheng et al, 2007;Cheng et al, 2003;McCright et al, 2002), and Lhx1 (Kobayashi et al, 2005). In particular, genetic studies have shown several members of the Wnt family of lipidmodified secreted glycoproteins have important roles in the initiation and maintenance of nephron formation and branching morphogenesis Kispert et al, 1998;Majumdar et al, 2003;Stark et al, 1994).…”

Section: Screen For Genes In Nephron Formationmentioning

confidence: 99%

Transcriptional profiling of Wnt4 mutant mouse kidneys identifies genes expressed during nephron formation

Valerius

McMahon

2008

Gene Expression Patterns

View full text Add to dashboard Cite

The mature nephron forms from a simple epithelial vesicle into an elaborate structure with distinct regions of specialized physiological function. The molecular components driving the process of nephron development are not well understood. To identify genes that may be informative in this process we conducted a transcriptional profiling screen using Wnt4 mutant kidneys. In Wnt4 −/− homozygous mice, condensates and pretubular aggregates are induced, however, epithelial renal vesicles fail to form and subsequent tubulogenesis is blocked. A transcriptional profile comparison between wildtype and Wnt4−/− mutant kidneys at E14.5 was performed using Affymetrix oligonucleotide microarrays to identify nephron-expressed genes. This approach identified 236 genes with expression levels >1.8 fold higher in wildtype versus mutant kidneys, amongst these were a number of known nephron component markers confirming the validity of the screen. These results were further detailed by wholemount in situ hybridization (WISH) of E15.5 urogenital systems (UGS). We annotated the spatial expression pattern of these genes into eight categories of expression. Genes expressed in renal vesicle and their derivatives, structures absent in the mutant, accounted for the largest number of the observed expression patterns. A number of additional genes in areas not directly overlapping the Wnt4 expression domain were also identified including the cap mesenchyme, the collecting duct, and the cortical interstitium. This study provides a useful compendium of molecular markers for the study of nephrogenesis.

show abstract

“…Because both cell types share common melanin synthesis pathway, we decided to investigate whether PS is also required for the pigmentation of mouse cutaneous melanocytes by using specific PS inhibitors (34,35). We cultured primary melanocytes from newborn WT C57BL͞6J mouse skin and allowed the culture to mature and become pigmented (Fig.…”

Section: Ps Are Required For Pigmentation Of Retinal Pigment Epithelimentioning

confidence: 99%

Regulation of tyrosinase trafficking and processing by presenilins: Partial loss of function by familial Alzheimer's disease mutation

Wang

Tang

Wang

et al. 2005

Proc. Natl. Acad. Sci. U.S.A.

View full text Add to dashboard Cite

show abstract

γ-Secretase activity is dispensable for mesenchyme-to-epithelium transition but required for podocyte and proximal tubule formation in developing mouse kidney

Cited by 197 publications

References 68 publications

Notch Activation Induces the Generation of Functional NK Cells from Human Cord Blood CD34-Positive Cells Devoid of IL-15

Notch Activation Induces the Generation of Functional NK Cells from Human Cord Blood CD34-Positive Cells Devoid of IL-15

Transcriptional profiling of Wnt4 mutant mouse kidneys identifies genes expressed during nephron formation

Regulation of tyrosinase trafficking and processing by presenilins: Partial loss of function by familial Alzheimer's disease mutation

Contact Info

Product

Resources

About