| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 1929578 | Biochemical and Biophysical Research Communications | 2012 | 7 Pages |
The position of the mitotic spindle plays a key role in spatial control of cell division. It is generally believed that when a spindle is positioned asymmetrically in a dividing cell, the resulting daughter cells are usually unequal in size due to eccentric cleavage of the mother cell. Molecular mechanisms underlying the generation of unequal sized daughter cells have been extensively studied in Drosophila neuroblast and Caenorhabditis elegans zygote where the Gα subunit of the heterotrimeric G proteins and its binding partner – Pins in Drosophila and GPR-1/2 in C. elegans – are shown to be critical in governing spindle positioning and asymmetric cleavage of the mother cell. In mammalian system, although Gα and LGN (mammalian Pins homolog) are also required for spindle orientation, whether they can mediate asymmetric spindle positioning or asymmetric cleavage of the mother cell is not known. Here, by artificially targeting Gαi to the apical cortex in 3-D cultured MDCK cells, we established a system where asymmetric spindle positioning can be consistently induced. Interestingly, this asymmetrically positioned spindle does not lead to asymmetric cleavage; instead it results in equal sized daughter cells. Live cell time-lapse analysis revealed that anaphase spindle elongation compensated the original asymmetric spindle positioning. Our findings demonstrate that asymmetric spindle positioning does not necessarily lead to unequal sized daughter cells in mammalian system. We discuss potential mechanisms in generating unequal sized daughter cells.
► Apical targeting of Gαi1/LGN leads to asymmetric spindle positioning in 3-D cultured MDCK cells. ► We established a system where asymmetric spindle positioning can be consistently induced. ► Live cell time-lapse analysis of cell division in 3-D cultured MDCK cells. ► Asymmetric spindle positioning does not lead to the generation of unequal sized daughter cells.
