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Literature DB >> 33423298

Fanconi anemia and mTOR pathways functionally interact during stalled replication fork recovery.

Matthew Nolan¹, Kenneth Knudson¹, Marina K Holz², Indrajit Chaudhury^1,3.

Abstract

We have previously demonstrated that Fanconi anemia (FA) proteins work in concert with other FA and non-FA proteins to mediate stalled replication fork restart. Previous studies suggest a connection between the FA protein FANCD2 and the non-FA protein mechanistic target of rapamycin (mTOR). A recent study showed that mTOR is involved in actin-dependent DNA replication fork restart, suggesting possible roles in the FA DNA repair pathway. In this study, we demonstrate that during replication stress mTOR interacts and cooperates with FANCD2 to provide cellular stability, mediate stalled replication fork restart, and prevent nucleolytic degradation of the nascent DNA strands. Taken together, this study unravels a novel functional cross-talk between two important mechanisms: mTOR and FA DNA repair pathways that ensure genomic stability.

Entities: Chemical

Keywords: DNA repair; Fanconi anemia; mTOR; replication restart

Mesh：

Substances：

Year: 2021 PMID： 33423298 PMCID： PMC7993987 DOI： 10.1002/1873-3468.14035

Source DB: PubMed Journal: FEBS Lett ISSN： 0014-5793 Impact factor: 4.124

34 in total

1. Effects of combining rapamycin and resveratrol on apoptosis and growth of TSC2-deficient xenograft tumors.

Authors: Anya Alayev; Rachel S Salamon; Yang Sun; Naomi S Schwartz; Chenggang Li; Jane J Yu; Marina K Holz
Journal: Am J Respir Cell Mol Biol Date: 2015-11 Impact factor: 6.914

2. The Fanconi Anemia Pathway in Cancer.

Authors: Joshi Niraj; Anniina Färkkilä; Alan D D'Andrea
Journal: Annu Rev Cancer Biol Date: 2018-12-03

3. The role of S6K1 in ER-positive breast cancer.

Authors: Marina K Holz
Journal: Cell Cycle Date: 2012-08-16 Impact factor: 4.534

4. FANCD2, FANCJ and BRCA2 cooperate to promote replication fork recovery independently of the Fanconi Anemia core complex.

Authors: Maya Raghunandan; Indrajit Chaudhury; Stephanie L Kelich; Helmut Hanenberg; Alexandra Sobeck
Journal: Cell Cycle Date: 2015 Impact factor: 4.534

2. A Multidrug Approach to Modulate the Mitochondrial Metabolism Impairment and Relative Oxidative Stress in Fanconi Anemia Complementation Group A.

Authors: Enrico Cappelli; Nadia Bertola; Silvia Bruno; Paolo Degan; Stefano Regis; Fabio Corsolini; Barbara Banelli; Carlo Dufour; Silvia Ravera
Journal: Metabolites Date: 2021-12-21

2 in total

Fanconi anemia and mTOR pathways functionally interact during stalled replication fork recovery.

1. Effects of combining rapamycin and resveratrol on apoptosis and growth of TSC2-deficient xenograft tumors.

2. The Fanconi Anemia Pathway in Cancer.

3. The role of S6K1 in ER-positive breast cancer.

4. FANCD2, FANCJ and BRCA2 cooperate to promote replication fork recovery independently of the Fanconi Anemia core complex.

5. Estrogen induces RAD51C expression and localization to sites of DNA damage.

6. CtIP mediates replication fork recovery in a FANCD2-regulated manner.

7. mTOR regulates DNA damage response through NF-κB-mediated FANCD2 pathway in hematopoietic cells.

Review 8. C. elegans: a model of Fanconi anemia and ICL repair.

9. S6 kinase 1 regulates estrogen receptor alpha in control of breast cancer cell proliferation.

10. mTORC1 directly phosphorylates and activates ERα upon estrogen stimulation.

Review 1. Autophagy-related Proteins in Genome Stability: Autophagy-Dependent and Independent Actions.

2. A Multidrug Approach to Modulate the Mitochondrial Metabolism Impairment and Relative Oxidative Stress in Fanconi Anemia Complementation Group A.