Spaghetti, a homolog of human RPAP3 (RNA polymerase II‐associated protein 3), determines the fate of germline stem cells in Drosophila ovary

The Drosophila ovary provides an attractive model for studying the extrinsic or intrinsic factors that regulate the fate of germline stem cells (GSCs). Using this model, we identified a new role for Drosophila spaghetti (spag), encoding a homolog of human RNA polymerase II‐associated protein 3 (RPAP...

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Bibliographic Details
Published in:Cell biology international 2018-07, Vol.42 (7), p.769-780
Main Authors: Chen, Dongsheng, Tao, Xiaoqian, Zhou, Lijuan, Sun, Fuling, Sun, Mingzhong, Fang, Xin
Format: Article
Language:English
Subjects:
Apoptosis
DNA-directed RNA polymerase
Drosophila
germline stem cell
Hsp90 protein
Insects
maintenance
Mutation
Ovaries
RNA polymerase
RNA-mediated interference
RNAi
Spag
Stem cells
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Summary:The Drosophila ovary provides an attractive model for studying the extrinsic or intrinsic factors that regulate the fate of germline stem cells (GSCs). Using this model, we identified a new role for Drosophila spaghetti (spag), encoding a homolog of human RNA polymerase II‐associated protein 3 (RPAP3), in regulating the fate of ovarian GSCs. Results from spag knockdown and genetic mosaic studies suggest that spag functions as an intrinsic factor for GSCs maintenance. Loss of Spag by, either spag RNAi or null mutation failed to trigger apoptosis in ovarian GSCs. Overexpression of spag led to negligible increases in the number of GSC/Cystoblast (CB) cells, suggesting that an excess of Spag is not sufficient to accelerate the proliferation of GSCs or delay CBs’ differentiation. Our study provides evidence supporting that spag is involved in adult stem cells maintenance. In addition, the RNAi screen results showed that knockdown of Hsp90, one of known Spag interacting partners, led to loss of ovarian GSCs in Drosophila. Heterozygous mutations in hsp90 (hsp90/+) dramatically accelerated the GSC loss in spag RNAi ovaries, suggesting that the Spag‐contained complex possibly plays an essential role in controlling the GSCs fate.
ISSN:1065-6995
1095-8355
DOI:10.1002/cbin.10900