High resolution live cell imaging reveals novel cyclin A2 degradation foci involving autophagy

Loukil, Abdelhalim; Zonca, Manuela; Rebouissou, Cosette; Baldin, Véronique; Coux, Olivier; Biard-Piechaczyk, Martine; Blanchard, Jean‐Marie; Peter, Matthias

doi:10.1242/jcs.139188

Cited by 32 publications

(40 citation statements)

References 39 publications

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“…In accordance with the reported ongoing mitophagy in arrested mitotic cells (38), LC3 puncta have been observed in mitotic cells, although at a significantly decreased level compared to interphase cells (28, 29, 39, 40). While these may also represent inefficient autophagy inhibition, Loukil et al observed LC3, p62, and lysosomal markers colocalizing with Cyclin A2 foci during mitosis and found that autophagy partially contributes to mediating mitotic Cyclin A2 degradation (40).…”

Section: Autophagy Status During Cell-cycle Progressionsupporting

confidence: 90%

“…While these may also represent inefficient autophagy inhibition, Loukil et al observed LC3, p62, and lysosomal markers colocalizing with Cyclin A2 foci during mitosis and found that autophagy partially contributes to mediating mitotic Cyclin A2 degradation (40). Thus, an intriguing although highly controversial theory is the existence of distinct sites of active autophagy during cell division.…”

Section: Autophagy Status During Cell-cycle Progressionmentioning

confidence: 99%

“…Furthermore, an alternative function for cyclin A2 in potentiating RhoA GTP loading by its GEFs has also been described (130). While the majority of cyclin A2 is degraded by the proteasome in prometaphase (131–133), a small fraction of cyclin A2 was shown to persist in foci later in mitosis and appeared to be subjected to autophagic degradation (40). It is therefore possible that autophagy may have a composite function in controlling appropriate RhoA protein levels and activity at the cytokinesis midzone, by mediating RhoA and Cyclin A2 degradation in late mitosis.…”

Section: Cell Division and Autophagymentioning

confidence: 99%

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Autophagy and the Cell Cycle: A Complex Landscape

2017

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Autophagy is a self-degradation pathway, in which cytoplasmic material is sequestered in double-membrane vesicles and delivered to the lysosome for degradation. Under basal conditions, autophagy plays a homeostatic function. However, in response to various stresses, the pathway can be further induced to mediate cytoprotection. Defective autophagy has been linked to a number of human pathologies, including neoplastic transformation, even though autophagy can also sustain the growth of tumor cells in certain contexts. In recent years, a considerable correlation has emerged between autophagy induction and stress-related cell-cycle responses, as well as unexpected roles for autophagy factors and selective autophagic degradation in the process of cell division. These advances have obvious implications for our understanding of the intricate relationship between autophagy and cancer. In this review, we will discuss our current knowledge of the reciprocal regulation connecting the autophagy pathway and cell-cycle progression. Furthermore, key findings involving nonautophagic functions for autophagy-related factors in cell-cycle regulation will be addressed.

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Section: Autophagy Status During Cell-cycle Progressionsupporting

confidence: 90%

Section: Autophagy Status During Cell-cycle Progressionmentioning

confidence: 99%

Section: Cell Division and Autophagymentioning

confidence: 99%

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Autophagy and the Cell Cycle: A Complex Landscape

2017

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“…Cyclins and CDKs are ubiquitinated and degraded through the proteasomal pathway to maintain cell‐cycle progression . Loukil et al reported that autophagy is a regulator of cyclin A2 degradation beyond the metaphase of the cell cycle in proliferating cells . We show that both of the autophagic and proteasomal degradation systems degrade cyclin D1, as demonstrated by MG132 and CQ treatment.…”

Section: Discussionsupporting

confidence: 54%

“…(22) Loukil et al reported that autophagy is a regulator of cyclin A2 degradation beyond the metaphase of the cell cycle in proliferating cells. (23) We show that both of the autophagic and proteasomal degradation systems degrade cyclin D1, as demonstrated by MG132 and CQ treatment. However, the subsequent suppression of the cell-cycle progression was only rescued by CQ treatment, but not by MG132 (Fig.…”

Section: Discussionmentioning

confidence: 66%

Hepatocellular carcinoma–related cyclin D1 is selectively regulated by autophagy degradation system

Lan

et al. 2018

Hepatology

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Dysfunction of degradation machineries causes cancers, including hepatocellular carcinoma (HCC). Overexpression of cyclin D1 in HCC has been reported. We previously reported that autophagy preferentially recruits and degrades the oncogenic microRNA (miR)‐224 to prevent HCC. Therefore, in the present study, we attempted to clarify whether cyclin D1 is another oncogenic factor selectively regulated by autophagy in HCC tumorigenesis. Initially, we found an inverse correlation between low autophagic activity and high cyclin D1 expression in tumors of 147 HCC patients and three murine models, and these results taken together revealed a correlation with poor overall survival of HCC patients, indicating the importance of these two events in HCC development. We found that increased autophagic activity leads to cyclin D1 ubiquitination and selective recruitment to the autophagosome (AP) mediated by a specific receptor, sequestosome 1 (SQSTM1), followed by fusion with lysosome and degradation. Autophagy‐selective degradation of ubiquitinated cyclin D1 through SQSTM1 was confirmed using cyclin D1/ubiquitin binding site (K33‐238R) and phosphorylation site (T286A) mutants, lentivirus‐mediated silencing autophagy‐related 5 (ATG5), autophagy‐related 7 (ATG7), and Sqstm1 knockout cells. Functional studies revealed that autophagy‐selective degradation of cyclin D1 plays suppressive roles in cell proliferation, colony, and liver tumor formation. Notably, an increase of autophagic activity by pharmacological inducers (amiodarone and rapamycin) significantly suppressed tumor growth in both the orthotopic liver tumor and subcutaneous tumor xenograft models. Our findings provide evidence of the underlying mechanism involved in the regulation of cyclin D1 by selective autophagy to prevent tumor formation. Conclusion: Taken together, our data demonstrate that autophagic degradation machinery and the cell‐cycle regulator, cyclin D1, are linked to HCC tumorigenesis. We believe these findings may be of value in the development of alternative therapeutics for HCC patients. (Hepatology 2018;68:141‐154).

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