Figure 4. The ectodomain of Tmem2 is critical for promoting cardiac fusion.

In situ hybridization indicates expression of myl7 in Mtmem2 (A,D,G,I) and MZtmem2 (B,C,E,F,H,J) mutant embryos at 24 hpf; dorsal views, anterior up. The heart tube assembles normally in Mtmem2 embryos (A), with no evident defects or delay in cardiac fusion, just as is observed in wild-type and Ztmem2 mutant embryos (Totong et al., 2011). MZtmem2 mutant siblings, however, display either cardia bifida (B) or, less frequently, partial cardiac fusion (C). Expression of full-length tmem2 in MZtmem2 mutants can facilitate cardiomyocyte movement to the midline (E) and frequently restores heart tube formation (F) (Table 2). Expression of htrc-tmem2 in MZtmem2 mutants can also rescue the MZtmem2 cardiac fusion defects (H; Table 2). As with ΔC-term and all other extracellular domain deletion variants, expression of the ΔG8 variant does not rescue cardiac fusion in MZtmem2 mutants (J; Table 2). Mtmem2 sibling embryos appear unaffected by expression of tmem2 (D) or tmem2 variants (G,I; Table 2).