DNA damage induce γ-tubulin–RAD51 nuclear complexes in mammalian cells

Lesca, Claire; Germanier, Maryse; Raynaud-Messina, Brigitte; Pichereaux, Carole; Etiévant, Chantal; Emond, Stéphane; Burlet‐Schiltz, Odile; Monsarrat, Bernard; Wright, Michel; Defais, Martine

doi:10.1038/sj.onc.1208723

Cited by 52 publications

(67 citation statements)

References 59 publications

(59 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…47 A direct involvement of RAD51 and paralogues with the centrosome is not yet established but is suggested by the finding that RAD51 can physically interact with γ-tubulin, a centrosome-associated factor. 49 As a second example, while the recombination mediator BRCA2 is predominantly a nuclear factor, a fraction of the BRCA2 pool localizes to centrosomes in the S and early M phases. A reduction in the level of cytoplasmic and hence centrosomal BRCA2 causes centrosome amplification and binucleation of cells.…”

Section: Discussionmentioning

confidence: 99%

Mitotic crisis: The unmasking of a novel role for RPA

Anantha

Borowiec

2009

Cell Cycle

View full text Add to dashboard Cite

Section: Discussionmentioning

confidence: 99%

Mitotic crisis: The unmasking of a novel role for RPA

Anantha

Borowiec

2009

Cell Cycle

View full text Add to dashboard Cite

“…This cell cycle arresting effect clearly suggests that nuclear accumulation of β-tubulin, which does not occur under normal circumstances, is a process of pathophysiological significance and may represent a defense mechanism against stress or malignant transformation. In that respect, it is interesting to note that GFPtagged α-tubulin accumulates reversibly in nuclei of cultured tobacco cells, in response to low temperature (Schwarzerova et al, 2006), whereas nuclear β-and γ-tubulin have been so far detected primarily in cancer or transformed cells (Lesca et al, 2005;WalssBass et al, 2002;Xu and Luduena, 2002;Yeh and Luduena, 2004;.…”

Section: Discussionmentioning

confidence: 99%

Nucleocytoplasmic shuttling of soluble tubulin in mammalian cells

Akoumianaki

Kardassis

Polioudaki

et al. 2009

Journal of Cell Science

View full text Add to dashboard Cite

We have investigated the subcellular distribution and dynamics of soluble tubulin in unperturbed and transfected HeLa cells. Under normal culture conditions, endogenous α/β tubulin is confined to the cytoplasm. However, when the soluble pool of subunits is elevated by combined cold-nocodazole treatment and when constitutive nuclear export is inhibited by leptomycin B, tubulin accumulates in the cell nucleus. Transfection assays and FRAP experiments reveal that GFP-tagged β-tubulin shuttles between the cytoplasm and the cell nucleus. Nuclear import seems to occur by passive diffusion, whereas exit from the nucleus appears to rely on nuclear export signals (NESs). Several such motifs can be identified by sequence criteria along the β-tubulin molecule and mutations in one of these (NES-1) cause a significant accumulation in the nuclear compartment. Under these conditions, the cells are arrested in the G0-G1 phase and eventually die, suggesting that soluble tubulin interferes with important nuclear functions. Consistent with this interpretation, soluble tubulin exhibits stoichiometric binding to recombinant, normally modified and hyper-phosphorylated/acetylated histone H3. Tubulin-bound H3 no longer interacts with heterochromatin protein 1 and lamin B receptor, which are known to form a ternary complex under in vitro conditions. Based on these observations, we suggest that nuclear accumulation of soluble tubulin is part of an intrinsic defense mechanism, which tends to limit cell proliferation under pathological conditions. This readily explains why nuclear tubulin has been detected so far only in cancer or in transformed cells, and why accumulation of this protein in the nucleus increases after treatment with chemotherapeutic agents.

show abstract

“…We found that 4.1R depletion delays transitioning into S phase in untransformed RPE-1 cells, supporting the important role of 4.1R in centrosome structure. Although 4.1R depletion does (1,9,34,45,55). In addition to its functions at interphase centrosomes and in cell cycle regulation, 4.1R is required for formation of mitotic bipolar spindles and for proper cytokinesis.…”

Section: Discussionmentioning

confidence: 99%

Downregulation of Protein 4.1R, a Mature Centriole Protein, Disrupts Centrosomes, Alters Cell Cycle Progression, and Perturbs Mitotic Spindles and Anaphase

Krauss

Spence

Bahmanyar

et al. 2008

Molecular and Cellular Biology

View full text Add to dashboard Cite

Centrosomes nucleate and organize interphase microtubules and are instrumental in mitotic bipolar spindle assembly, ensuring orderly cell cycle progression with accurate chromosome segregation. We report that the multifunctional structural protein 4.1R localizes at centrosomes to distal/subdistal regions of mature centrioles in a cell cycle-dependent pattern. Significantly, 4.1R-specific depletion mediated by RNA interference perturbs subdistal appendage proteins ninein and outer dense fiber 2/cenexin at mature centrosomes and concomitantly reduces interphase microtubule anchoring and organization. 4.1R depletion causes G 1 accumulation in p53-proficient cells, similar to depletion of many other proteins that compromise centrosome integrity. In p53-deficient cells, 4.1R depletion delays S phase, but aberrant ninein distribution is not dependent on the S-phase delay. In 4.1R-depleted mitotic cells, efficient centrosome separation is reduced, resulting in monopolar spindle formation. Multipolar spindles and bipolar spindles with misaligned chromatin are also induced by 4.1R depletion. Notably, all types of defective spindles have mislocalized NuMA (nuclear mitotic apparatus protein), a 4.1R binding partner essential for spindle pole focusing. These disruptions contribute to lagging chromosomes and aberrant microtubule bridges during anaphase/telophase. Our data provide functional evidence that 4.1R makes crucial contributions to the structural integrity of centrosomes and mitotic spindles which normally enable mitosis and anaphase to proceed with the coordinated precision required to avoid pathological events.

show abstract

DNA damage induce γ-tubulin–RAD51 nuclear complexes in mammalian cells

Cited by 52 publications

References 59 publications

Mitotic crisis: The unmasking of a novel role for RPA

Mitotic crisis: The unmasking of a novel role for RPA

Nucleocytoplasmic shuttling of soluble tubulin in mammalian cells

Downregulation of Protein 4.1R, a Mature Centriole Protein, Disrupts Centrosomes, Alters Cell Cycle Progression, and Perturbs Mitotic Spindles and Anaphase

Contact Info

Product

Resources

About