Suzuki A , Thies RS , Yamaji N , Song JJ , Wozney JM , Murakami K , Ueno N .

	FIG. 1. Amino acid sequence and homology of mTFR11. (A) Translated amino acid sequence of the mTFR11 cDNA. The signal peptide and transmembrane domains are indicated by a single underline. Potential sites of N-linked glycosylation are indicated by asterisks. The ends of the kinase domain are indicated by arrows. Ten of the conserved cysteine residues in the extracellular domain are in reverse print. Type I box is indicated by a double underline. An arrowhead is under the tyrosine residue that changes to stop codon in the dominant negative BMP receptor. (B) Homology of the mTFR11/hALK-3 to other receptors for ligands of the TGF-(3 superfamily. Percent amino acid identity is indicated. Light-shaded boxes, extracellular domain; black boxes, transmembrane domain; dark-shaded boxes, type I box; hatched boxes, intracellular kinase domain. ALK-2, -3, -5, and -6, activin receptor-like kinases 2, 3, 5, and 6(26); xTFR11, Xenopus TFR11 (accession no. D32066); mTGFf3RI, mouse TGF-(3 type I receptor (27); mActRI, mouse activin type I receptor (28); mActRII, mouse activin type II receptor (13); mTGF-fBRII, mouse TGF-f type II receptor (29);daf4, C. elegans daf-4 gene product (30).
	FIG. 2. Specific binding of iodinated BMP-4 to COS cells transfected with mTFR11. (A) 'MI-BMP4 binding to COS cells transfected with mTFR11. Binding was performed on cell monolayers as described below and was competitively inhibited with unlabeled BMP-4. (Inset) Scatchard analysis. o, pMV2; *, mTfr11/pMV2. (B) Specificity of mI-BMPA binding to COS cells transfected with mTFR11. Binding of 125I-BMP4 to COS cells transfected with mTFR11 was performed with or without increasing concentrations ofunlabeled ligands. *, BMP-2; o, BMP-4;m, activin A; *, TGF-.l1. (C) Chemical cross-linking ofiodinated BMP-4 to COS cells transfected with mTFR11/pMV2 orpMV2. COS cells were transfected with either pMV2 (lane 1) or mTFR11/pMV2 (lanes 2-5) and incubated with 5 ng of 125I-BMP-4 per ml (all lanes) and 500 ng ofBMP-4 per ml (lane 3), 500 ng of BMP-2 per ml (lane 4), or 500 ng of activin per ml (lane 5). Molecular masses are indicated in kDa.
	FIG. 3. Truncated BMP receptor inhibits BMP signaling pathway in early Xenopus embryo. At the four-cell stage, embryos were injected with the indicated samples into the dorsal marginal region and allowed to develop until stage 37 or 38. (A) Distilled H20. (B) BMP-4 mRNA, 200 pg. (C) AmnTFR11 mRNA, 200 pg. (D) BMP-4 plus AmTFR11 mRNA, 200 pg of each.
	FIG. 5. Effect of inhibition of BMP signaling pathway on expression of early mesodermal markers. AmTFR11 mRNA was injected into the marginal region of ventral blastomeres at the four-cell stage. Uninjected control embryo (A, C, and E), and AmTFR11-injected embryos (B, D, and F) were developed until early gastrula stage and subjected to whole-mount in situ analysis. The probe for goosecoid was used in A and B; the probe for Xpo was used in C and D; the probe for Xenopus brachyury was used in E and F. Views of the vegetal pole are shown and dorsal is up. Note that the expression of Xpo gene disappeared in the ventral part of embryo that received truncated BMP receptor mRNA (arrowheads) but that of brachyury gene, normally expressed through mesoderm, was not affected.

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