Abstract

We are addressing the general problem of how patterns form within fields of cells by studying antero-posterior pattern formation in C. elegans. Our entry point has been the gene mab-5, which we showed to be a homeotic gene required for ectodermal and mesodermal cells located in a posterior body region to undergo position-specific migrations, divisions and differentiations. We are now trying to learn how mab-5 activity is targeted to posterior cells, and to understand how mab-5 controls cell differentiation. During the current funding period, we have found that mab-5 RNA is localized in the posterior body region, which implies that at least one mechanism that positions mab-5 activity acts at the level of mab-5 RNA. We have identified a number of genes that may influence this localization. In particular, we have found that a regulated system of local cell-cell interactions positions mab-5 function in laterally located cells. In addition, we have found that mab-5 contains a homeobox closely related to those of Drosophila homeotic genes within the bithorax and Antennapedia complexes. This finding suggests that mab-5 regulates transcription and that there may be an underlying similarity between this pattern forming system and that of Drosophila. We now plan to utilize the information and molecular probes obtained in the current funding period to study mechanisms of mab-5 localization and function with much greater depth and resolution than was possible previously. We plan to determine exactly which cells express mab-5 during development, to learn what types of position-specific, cell-specific and sex-specific regulation ?nab-5 is subject to. We will localize cis-acting regulatory regions required for specific modes of regulation, and identify and analyze genes that may encode transacting regulatory factors. We will initiate a detailed genetic and molecular study of the local cell interactions that regulate mab-5 expression. We will analyze genes in C. elegans we, have identified that are homologous to Drosophila patterning genes, to determine whether additional similarities exist between these two regulatory systems. Finally, we will determine whether mab-5 activity is sufficient to cause anterior cells to adopt posteror-specific fates, and we will begin to identify genes that may be regulated by mab-5 to initiate specific pathways of cell differentiation.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM037053-05
Application #
3291977
Study Section
Genetics Study Section (GEN)
Project Start
1986-09-01
Project End
1994-08-31
Budget Start
1990-09-01
Budget End
1991-08-31
Support Year
5
Fiscal Year
1990
Total Cost
Indirect Cost

  Institution

Name
University of California San Francisco
Department
Type
Schools of Medicine
DUNS #
073133571
City
San Francisco
State
CA
Country
United States
Zip Code
94143

  Publications

Yang, Lucie; Sym, Mary; Kenyon, Cynthia (2005) The roles of two C. elegans HOX co-factor orthologs in cell migration and vulva development. Development 132:1413-28
Ch'ng, QueeLim; Williams, Lisa; Lie, Yung S et al. (2003) Identification of genes that regulate a left-right asymmetric neuronal migration in Caenorhabditis elegans. Genetics 164:1355-67
Alper, Scott; Kenyon, Cynthia (2002) The zinc finger protein REF-2 functions with the Hox genes to inhibit cell fusion in the ventral epidermis of C. elegans. Development 129:3335-48
Alper, S; Kenyon, C (2001) REF-1, a protein with two bHLH domains, alters the pattern of cell fusion in C. elegans by regulating Hox protein activity. Development 128:1793-804
Whangbo, J; Harris, J; Kenyon, C (2000) Multiple levels of regulation specify the polarity of an asymmetric cell division in C. elegans. Development 127:4587-98
Whangbo, J; Kenyon, C (1999) A Wnt signaling system that specifies two patterns of cell migration in C. elegans. Mol Cell 4:851-8
Ch'ng, Q; Kenyon, C (1999) egl-27 generates anteroposterior patterns of cell fusion in C. elegans by regulating Hox gene expression and Hox protein function. Development 126:3303-12
Hunter, C P; Harris, J M; Maloof, J N et al. (1999) Hox gene expression in a single Caenorhabditis elegans cell is regulated by a caudal homolog and intercellular signals that inhibit wnt signaling. Development 126:805-14
Maloof, J N; Whangbo, J; Harris, J M et al. (1999) A Wnt signaling pathway controls hox gene expression and neuroblast migration in C. elegans. Development 126:37-49
Herman, M A; Ch'ng, Q; Hettenbach, S M et al. (1999) EGL-27 is similar to a metastasis-associated factor and controls cell polarity and cell migration in C. elegans. Development 126:1055-64

Showing the most recent 10 out of 19 publications