PARP-3 localizes preferentially to the daughter centriole and interferes with the G1/S cell cycle progression

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Abstract

A novel member of the poly(ADP-ribose) polymerase (PARP) family, hPARP-3, is identified here as a core component of the centrosome. hPARP-3 is preferentially localized to the daughter centriole throughout the cell cycle. The N-terminal domain (54 amino acids) of hPARP-3 is responsible for its centrosomal localization. Full-length hPAPR-3 (540 amino acids, with an apparent mass of 67 kDa) synthesizes ADP-ribose polymers during its automodification. Overexpression of hPARP-3 or its N-terminal domain does not influence centrosomal duplication or amplification but interferes with the G1/S cell cycle progression. PARP-1 also resides for part of the cell cycle in the centrosome and interacts with hPARP-3. The presence of both PARP-1 and PARP-3 at the centrosome may link the DNA damage surveillance network to the mitotic fidelity checkpoint.

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APA

Augustin, A., Spenlehauer, C., Dumond, H., Ménisier-de Murcia, J., Piel, M., Schmit, A. C., … de Murcia, G. (2003, April 15). PARP-3 localizes preferentially to the daughter centriole and interferes with the G1/S cell cycle progression. Journal of Cell Science. https://doi.org/10.1242/jcs.00341

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