Lawler J , Duquette M , Whittaker CA , Adams JC , McHenry K , DeSimone DW .

HD26402 NICHD NIH HHS , HL28749 NHLBI NIH HHS , HL42443 NHLBI NIH HHS , R01 HD026402 NICHD NIH HHS

	Figure 1. Alignment of Xenopus thrombospondin-4 clones. Restriction endonuclease sites are indicated for the two families (TSP-4A and TSP-4B). The clones that have been isolated in the first (XF1- XF4), second (XSS-XS10), and third (XTI1-XTI4) rounds of screening have been grouped into their appropriate family by restriction endonuclease mapping and nucleotide sequencing.
	lqgure 2. Northern blot of Xenopus stage 17 RNA. Two micrograms of total stage 17 mRNA was electrophoresed and blotted. The blot was probed with the XF3 clone. The positions and sizes of the markers are indicated on the letL
	Figure 3. The nucleotide sequence and corresponding amino acid sequence of Xenopus thrombospondin-4. The predicted site for signal sequence cleavage is indicated (open triangle). The termination codon TAA and the polyadanylation signal AATAAA are underlined. The sites for potential N-linked glyeosylation are circled and the site for potential ~-hydroxylation is boxed. Note that asparagine(314) could be either glycosylated or ~-l~xlmxylated. These sequence data are available from EMBL/GenBank/DDBJ under accession number, Z19091.
	Figure 4. The amino acid sequence of the type 2 (A) and 3 (B) repeats of thrombospondin-4. The amino acid sequences for the four type 2 repeats P(217)-K(394) and seven type 3 repeats (D[416]-I[647]) have been aligued. The positions of gaps ~ marked by dashes. The consensus sequence for the type 3 repeats of Xenop~ thmmbospondin-4 is compared to that for human and mouse thrombospondin-1 and chicken thrombospondin-2 at the bottom of the figure. The underline indicates that an N occupies one of the positions that is occupied by a D.
	Figure 5. Developmental expression of thrombospondin-4 mRNAs during Xenopus development as determined by RNase protection analyses. Ten embryo equivalents total mRNA per lane were bybridized with a 3~P-labeled thrombospondin-4 antisense transcript synthesized in vitro. EFI-,~ mRNA analysis is included as a control for RNA loading. The relative stage-specific levels of EFI-,v shown here are equivalent to those described by Krieg et al. (1989). Embryos were staged according to Nieuwkoop and Faber (1967). Stage 8 corresponds to the mid-blastula, which is marked by the onset of zygotic transcription in Xenopus (Newport and Kirschner, 1982). (P), probe alone, unhybridized transcript, no RNAse; (t) tRNA control lane, no protected fragments after RNAse digestion. Stages include: (1) fertilized egg, (8) mid-blastula, 00-12) early-late gastrula, 07) neurula, (25-35) tailbud stages, (45) feeding tadpole. Thrombospondin-4 protected fragment is ,,o300 nucleotides. EFI-a protected fragment is ,x,75 nucleotides. Full length EFI-c~ probe (90 nucleotides) is not shown.
	Figure 6. The expression of thrombospondin-4 in adult human tissue. A northern blot ofpoly A + RNA from adult human heart (a), brain (b), placenta (c), lung (d), liver (e), skeletal muscle (f), kidney (g), and pancreas (h). The blot was probed with a 2.2-kb fragment of Xenopus thrombospondin-4. The positions and sizes (kb) of the markers are indicated on the left.
	Figure 7. Schematic model of thrombospondin-4. The molecular architecture of thrombospondin-4 is shown below that of thrombospondin-1 or 2. The NH2 terminal is to the left and the COOH terminal is to the right. Whereas the NH2-terminal domains are similar in size, they share very little sequence homology. Two interchain disulfides of thrombospondin-1 and 2 are depicted as vertical lines between the NH~-terminal domain and the region of homology with procollagen. Whereas two cysteine residues are present in a similar location in thrombospondin-4, the structure of the protein that contains the thrombospondin-4 polypeptide remains to be determined.

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