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Download and posterior (tail)
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Cell movements during gastrulation suggest geometry for the embryo Frog A A P Chick P Gene expression, particularly in mesoderm, and local signaling distinguish A-P axis from early gastrulation onward in register with cell movements Chordin Dorsal lip of blastopore Chordin Chordin Frog …and antagonistic signaling establishes further local and axial distinctions Chick The geometry of cell movements during gastrulation in the mouse is distinct, but the results are the same… head tail Germ layers are divided into anterior (head) and posterior (tail) territories by antagonistic signaling pathways that result in local expression of transcription factor targets antagonist signal TF target Noggin TF target Essential antagonist/agonist pairs of signals, from distinct local sources establish A-P patterning in the germ layers Anteriorizing Posteriorizing noggin chordin Bmps Dkk SFRPs Wnts Lefty Cerberus Nodal The localization of antagonists in the anterior region suggests that “head” is a default, and “tail” must be actively constructed A schematic review of Bmp Signaling Loss of Bmp antagonist function disrupts head development +/+ Chord-/- Nog:Chord-/- Multiple mechanisms can inhibit Wnt Signaling Loss of Wnt antagonism via Dkk causes head to be transformed into posterior tissue Nodal signaling uses pathways similar to that for Bmp: both are members of the Tgfb superfamily of signals Loss of Nodal antagonism causes expansion of visceral endoderm, normally restricted to posterior of embryo Hex is a marker for visceral endoderm Heads or Tails: The balance of Bmp, Wnt and Nodal signaling decides! There is more to posterior development than making a tail: posterior regionalization via the Hox genes Paralogues on different chromsomes: 3’=anterior, 5’=posterior Colinear expression relies on temporally controlled chromatin remodeling in a 3’to 5’ direction Is there a terminal posterior identity: ParaHox genes and establishing the end of the “tail” most posteriorly restricted in all 3 germ layers Regulation of Hox/ParaHox expression reflects antagonist/agonist signaling Cyp26 RA degrading enzyme Hoxb1 Cyps RA Raldh2 RA synthesizing enzyme Head/Tail antagonism holds for RA signaling Posterior signals include Wnts, and Fgfs: establish graded gene expression in concert with RA Hox in the head: maintaining posterior segmentation in anteriorized territory ParaHox and Hox genes are central regulators of A-P identity 1.Conditional mutation of Cdx2 in the post-gastrula endoderm causes posterior gut dismorphogenesis goblet cells (alcian blue) 2a.Primary differentiated cellular characteristics of intestinal epithelium are absent in posterior gut of Cdx2 conditional mutant enterocytes: alkaline phosphatase 2b. Cellular architecture is disrupted, and cell proliferation is altered in posterior gut of Cdx2 conditional mutant 3. The dysmorphogenic posterior gut has been “anteriorized” to resemble esophageal epithleium by loss of Cdx2 in post-gastrula endoderm. 4. Anteriorization of gut epithelium to esophageal epithelium is accompanied by shifted expression (spatial or temporal) of anterior endoderm genes, including Hox cluster 5. Shift of expression of Wnts, transcriptional regulators, and down stream targets (all evidence of M-E signaling in which Wnt10a, 3a are available from M and act on E) in anterior gut, and in posterior mutant gut
