Abstract
In some species such as flies, worms, frogs, and fish the key to forming and maintaining early germ cell populations is the assembly of germ plasm, croscopically-distinct egg cytoplasm that is rich in RNAs, RNA-binding proteins and ribosomes. Cells which inherit germ plasm are destined for the germ cell lineage. In contrast, in mammals, germ cells are formed and maintained later in development as a result of inductive signaling from one embryonic cell type to another. Research advances, using complementary approaches, including identification of key signaling factors that act during the initial stages of germ cell development, differentiation of germ cells in vitro from mouse and human embryonic stem cells and the demonstration, that homologs of germ plasm components are conserved in mammals, have shed light on key elements in the early development of mammalian germ cells. Here, we use FRET (Fluorescence Resonance Energy Transfer) to demonstrate that living mammalian germ cells possess specific RNA/protein complexes that contain germ plasm homologs, beginning in the earliest stages of development examined. Moreover, we demonstrate that although both human and mouse germ cells and embryonic stem cells express the same proteins, germ cell specific protein/protein interactions distinguish germ cells from precursor embryonic stem cells in vitro; interactions also determine sub-cellular localization of complex components. Finally, we suggest that assembly of similar protein complexes may be central to differentiation of diverse cell lineages and provide useful diagnostic tools for isolation of specific cell types from the assorted types differentiated from embryonic stem cells.
| Original language | American English |
|---|---|
| Pages (from-to) | 417-431 |
| Number of pages | 15 |
| Journal | Developmental Biology |
| Volume | 301 |
| Issue number | 2 |
| DOIs | |
| State | Published - Jan 15 2007 |
| Externally published | Yes |
Funding
We thank Andrew Feinberg and Patricial Labosky for the mouse EG lines from E8.5 E12.5 embryos, respectively. We thank Roger Tsien for the monomeric red fluorescent protein, Marvin Wickens for yeast three-hybrid components, Martin Dym for the spermatogonial stem cell resources, Pauline Yen for DAZ-2 cDNA and DAZAP-1 antibody, Nigel Killen for the mouse E14 embryonic stem cell line, Sindy Mellon for the mouse Leydig cell line and Anna Bogdanova for assistance with mice. We also thank Haifan Lin and Neils Geijsens for helpful comments on the manuscript, as well as members of the Reijo Pera laboratory. This work was supported by the Lalor Foundation (M.F.), a National Institute of Health National Research Award fellowship (to J.U.) and by grants from the National Institutes of Health (RO1 HD037095, RO1 HD047221 and R24 RR017498-03), the Sandler Family Foundation, the American Stem Cell Research Foundation and the California TRDRP (to R.A.R.P.).
| Funders | Funder number |
|---|---|
| American Stem Cell Research Foundation | |
| National Institute of Health National Research | |
| National Institutes of Health | RO1 HD047221, R24 RR017498-03 |
| Sandler Foundation | |
| Eunice Kennedy Shriver National Institute of Child Health and Human Development | R01HD037095 |
| Lalor Foundation |
ASJC Scopus Subject Areas
- Molecular Biology
- Developmental Biology
- Cell Biology
Keywords
- Germ Cells
- Germ Cell Development
- DAZ
- DAZL
- PUM2
- PUM1
- NANOS
- Germ Plasm
- RNA-binding Proteins
- Germ cells
- RNA-binding proteins
- Germ cell development
- Germ plasm
Disciplines
- Cell and Developmental Biology
- Neuroscience and Neurobiology