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Published September 17, 2004 | Supplemental Material
Journal Article Open

C. elegans LIN-18 Is a Ryk Ortholog and Functions in Parallel to LIN-17/Frizzled in Wnt Signaling

Inoue, Takao
Oz, Helieh S.
Wiland, Debra
Gharib, Shahla
Deshpande, Rashmi
Hill, Russell J.
Katz, Wendy S.
Sternberg, Paul W. ORCID icon

Abstract

Wnt proteins are intercellular signals that regulate various aspects of animal development. In Caenorhabditis elegans, mutations in lin-17, a Frizzled-class Wnt receptor, and in lin-18 affect cell fate patterning in the P7.p vulval lineage. We found that lin-18 encodes a member of the Ryk/Derailed family of tyrosine kinase-related receptors, recently found to function as Wnt receptors. Members of this family have nonactive kinase domains. The LIN-18 kinase domain is dispensable for LIN-18 function, while the Wnt binding WIF domain is required. We also found that Wnt proteins LIN-44, MOM-2, and CWN-2 redundantly regulate P7.p patterning. Genetic interactions indicate that LIN-17 and LIN-18 function independently of each other in parallel pathways, and different ligands display different receptor specificities. Thus, two independent Wnt signaling pathways, one employing a Ryk receptor and the other a Frizzled receptor, function in parallel to regulate cell fate patterning in the C. elegans vulva.

Additional Information

© 2004 Cell Press. Received 16 March 2004, Revised 14 July 2004, Accepted 24 July 2004, Available online 16 September 2004. Published: September 16, 2004. We thank J. Goodwin for technical assistance, X.Z.S. Xu for DsRed2 plasmids, and B.P. Gupta for lin-17 plasmids. We thank A. Fire, S. Xu, J. Ahnn, and G. Seydoux for gfp vectors, D. Eisenmann and S. Kim for ga75, and Y. Kohara for cDNA clones and in situ data. Some strains were obtained from Caenorhabditis Genetics Center, funded by NIH, National Center for Research Resources. P.W.S. is an Investigator with and W.S.K. was an Associate with the HHMI, which supported this work. T.I. was supported by fellowship DRG-1646 from the Damon Runyon Cancer Research Foundation. W.S.K. was also supported by grants: March of Dimes 5-FY97-0674, ACS IRG-163H, and EPSCoR OSR-9452895. R.J.H. was supported by March of Dimes 5-FY00-550.

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Identifiers Funding Dates
Created:
August 19, 2023
Modified:
October 25, 2023