Warning: Undefined array key "mm" in /www/wwwroot/www.ai-bt.com/si.php on line 10 Deprecated: trim(): Passing null to parameter #1 ($string) of type string is deprecated in /www/wwwroot/www.ai-bt.com/si.php on line 10 Mitotic phosphorylation of Bloom helicase at Thr182 is required for its proteasomal degradation and maintenance of chromosomal stability.

Literature DB >> 26028025

Mitotic phosphorylation of Bloom helicase at Thr182 is required for its proteasomal degradation and maintenance of chromosomal stability.

S S Kharat¹, V Tripathi¹, A P Damodaran¹, R Priyadarshini¹, S Chandra¹, S Tikoo¹, R Nandhakumar¹, V Srivastava¹, S Priya¹, M Hussain¹, S Kaur¹, J B Fishman², S Sengupta¹.

Abstract

Mutations in Bloom helicase (BLM) lead to Bloom Syndrome (BS). BS is characterized by multiple clinical manifestations including predisposition to a wide spectrum of cancers. Studies have revealed the mechanism of BLM recruitment after stalled replication and its role during the repair of DNA damage. We now provide evidence that BLM undergoes K48-linked ubiquitylation and subsequent degradation during mitosis due to the E3 ligase, Fbw7α. Fbw7α carries out its function after GSK3β- and CDK2/cyclin A2-dependent phosphorylation events on Thr171 and Ser175 of BLM which lies within a well-defined phosphodegron, a sequence which is conserved in all primates. Phosphorylation on BLM Thr171 and Ser175 depends on prior phosphorylation at Thr182 by Chk1/Chk2. Thr182 phosphorylation not only controls BLM ubiquitylation and degradation during mitosis but is also a determinant for its localization on the ultrafine bridges. Consequently lack of Thr182 phosphorylation leads to multiple manifestations of chromosomal instability including increased levels of DNA damage, lagging chromatin, micronuclei formation, breaks and quadriradials. Hence Thr182 phosphorylation on BLM has two functions-it regulates BLM turnover during mitosis and also helps to maintain the chromosomal stability.

Entities: Chemical Disease Gene

Mesh：

Substances：

Year: 2015 PMID： 26028025 DOI： 10.1038/onc.2015.157

Source DB: PubMed Journal: Oncogene ISSN： 0950-9232 Impact factor: 9.867

57 in total

Review 1. The renaissance of GSK3.

Authors: P Cohen; S Frame
Journal: Nat Rev Mol Cell Biol Date: 2001-10 Impact factor: 94.444

2. Role for BLM in replication-fork restart and suppression of origin firing after replicative stress.

Authors: Sally L Davies; Phillip S North; Ian D Hickson
Journal: Nat Struct Mol Biol Date: 2007-06-24 Impact factor: 15.369

3. SAG/RBX2/ROC2 E3 ubiquitin ligase is essential for vascular and neural development by targeting NF1 for degradation.

Authors: Mingjia Tan; Yongchao Zhao; Sun-Jung Kim; Margaret Liu; Lijun Jia; Thomas L Saunders; Yuan Zhu; Yi Sun
Journal: Dev Cell Date: 2011-11-23 Impact factor: 12.270

4. SKP1 connects cell cycle regulators to the ubiquitin proteolysis machinery through a novel motif, the F-box.

Authors: C Bai; P Sen; K Hofmann; L Ma; M Goebl; J W Harper; S J Elledge
Journal: Cell Date: 1996-07-26 Impact factor: 41.582

5. BLM is required for faithful chromosome segregation and its localization defines a class of ultrafine anaphase bridges.

Authors: Kok-Lung Chan; Phillip S North; Ian D Hickson
Journal: EMBO J Date: 2007-06-28 Impact factor: 11.598

6. Human exonuclease 1 and BLM helicase interact to resect DNA and initiate DNA repair.

Authors: Amitabh V Nimonkar; A Zeynep Ozsoy; Jochen Genschel; Paul Modrich; Stephen C Kowalczykowski
Journal: Proc Natl Acad Sci U S A Date: 2008-10-29 Impact factor: 11.205

Review 7. Cdc25A phosphatase: combinatorial phosphorylation, ubiquitylation and proteolysis.

Authors: Luca Busino; Massimo Chiesa; Giulio F Draetta; Maddalena Donzelli
Journal: Oncogene Date: 2004-03-15 Impact factor: 9.867

8. Cyclin A2 mutagenesis analysis: a new insight into CDK activation and cellular localization requirements.

Authors: Nawal Bendris; Bénédicte Lemmers; Jean-Marie Blanchard; Nikola Arsic
Journal: PLoS One Date: 2011-07-28 Impact factor: 3.240

9. Regulation of c-Myc ubiquitination controls chronic myelogenous leukemia initiation and progression.

Authors: Linsey Reavie; Shannon M Buckley; Evangelia Loizou; Shoichiro Takeishi; Beatriz Aranda-Orgilles; Delphine Ndiaye-Lobry; Omar Abdel-Wahab; Sherif Ibrahim; Keiichi I Nakayama; Iannis Aifantis
Journal: Cancer Cell Date: 2013-03-18 Impact factor: 31.743

Mitotic phosphorylation of Bloom helicase at Thr182 is required for its proteasomal degradation and maintenance of chromosomal stability.

Review 1. The renaissance of GSK3.

2. Role for BLM in replication-fork restart and suppression of origin firing after replicative stress.

3. SAG/RBX2/ROC2 E3 ubiquitin ligase is essential for vascular and neural development by targeting NF1 for degradation.

4. SKP1 connects cell cycle regulators to the ubiquitin proteolysis machinery through a novel motif, the F-box.

5. BLM is required for faithful chromosome segregation and its localization defines a class of ultrafine anaphase bridges.

6. Human exonuclease 1 and BLM helicase interact to resect DNA and initiate DNA repair.

Review 7. Cdc25A phosphatase: combinatorial phosphorylation, ubiquitylation and proteolysis.

8. Cyclin A2 mutagenesis analysis: a new insight into CDK activation and cellular localization requirements.

9. Regulation of c-Myc ubiquitination controls chronic myelogenous leukemia initiation and progression.

10. Chk1 protects against chromatin bridges by constitutively phosphorylating BLM serine 502 to inhibit BLM degradation.

1. Replication checkpoint-mediated symmetric DNA synthesis: beginning to understand mechanism.

2. Abrogation of FBW7α-dependent p53 degradation enhances p53's function as a tumor suppressor.

3. FBW7 regulates DNA interstrand cross-link repair by modulating FAAP20 degradation.

4. MRN complex-dependent recruitment of ubiquitylated BLM helicase to DSBs negatively regulates DNA repair pathways.