Nam Soo Lee scite author profile

The swface-enhanced Raman spectra (SERS) of dopamine, norepinephrlne, epinephrine, eplnlne, isoproterenol, 3meth-oxytyramlne, and oatechd In pH 7.2 buffers on a silver ektrod@ are reported. Catechol and the c a t -are shown to be COordlMted to diver through both oxygens. The methoxylated derlvatlve Is a monodentate complex. Intenskies maximize near -0.9 V vs saturated calomel electrode. The strongest bands In the spwtra are phendic carbon-oxygen stretches and the vlOb modes around 1270 and 1480 cm-l, respectively. Ascorbate, acetylchdlne, glutathione, L-Dopa, and the catecholamine acetlc acid metabolites are SERShracHveunderthemeasuementcondltknr. Dopamkre detectlon lM for the vl Ob band Is 3 X lo-' Y wlth a 10-s measurement tlme.

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TRAIP/RNF206 is required for recruitment of RAP80 to sites of DNA damage

Lee

Chung

Kim

et al. 2016

Nat Commun

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RAP80 localizes to sites of DNA insults to enhance the DNA-damage responses. Here we identify TRAIP/RNF206 as a novel RAP80-interacting protein and find that TRAIP is necessary for translocation of RAP80 to DNA lesions. Depletion of TRAIP results in impaired accumulation of RAP80 and functional downstream partners, including BRCA1, at DNA lesions. Conversely, accumulation of TRAIP is normal in RAP80-depleted cells, implying that TRAIP acts upstream of RAP80 recruitment to DNA lesions. TRAIP localizes to sites of DNA damage and cells lacking TRAIP exhibit classical DNA-damage response-defect phenotypes. Biochemical analysis reveals that the N terminus of TRAIP is crucial for RAP80 interaction, while the C terminus of TRAIP is required for TRAIP localization to sites of DNA damage through a direct interaction with RNF20–RNF40. Taken together, our findings demonstrate that the novel RAP80-binding partner TRAIP regulates recruitment of the damage signalling machinery and promotes homologous recombination.

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Factors forming the BRCA1-A complex orchestrate BRCA1 recruitment to the sites of DNA damage

Her

Lee

Kim

et al. 2016

ABBS

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Sustaining genomic integrity is essential for preventing onset of cancers. Therefore, human cells evolve to have refined biological pathways to defend genetic materials from various genomic insults. DNA damage response and DNA repair pathways essential for genome maintenance are accomplished by cooperative executions of multiple factors including breast cancer type 1 susceptibility protein (BRCA1). BRCA1 is initially identified as an altered gene in the hereditary breast cancer patients. Since then, tremendous efforts to understand the functions of BRAC1 reveal that BRCA1 is found in distinct complexes, including BRCA1-A, BRCA1-B, BRCA1-C, and the BRCA1/ PALB2/BRCA2 complex, and plays diverse roles in a context-dependent manner. Among the complexes, BRCA1-A is critical for BRCA1 recruitment to the sites of DNA damage. Factors comprising the BRCA1-A include RAP80, CCDC98/Abraxas, BRCC36, BRCC45, BARD1, BRCA1, and MERIT40, a RAP80-associated factor. In this review, we summarize recent findings of the factors that form the BRCA1-A complex.

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The active species in surface-enhanced Raman scattering of flavins on silver colloids

Lee¹,

Sheng²,

Morris³

et al. 1986

J. Am. Chem. Soc.

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Cdk1 Protein-mediated Phosphorylation of Receptor-associated Protein 80 (RAP80) Serine 677 Modulates DNA Damage-induced G2/M Checkpoint and Cell Survival

Cho

Han

et al. 2013

Journal of Biological Chemistry

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Background: RAP80, a component of the BRCA1-A complex, is crucial in the cell cycle checkpoint and DNA damage repair. Results: RAP80 phosphorylation by Cdk1 is important for sensitivity to ionizing radiation and G 2 /M checkpoint control. Conclusion: Cdk1-mediated RAP80 phosphorylation is important for the DNA damage response. Significance: The findings provide new implications for the interplay of the DNA damage signaling pathway and RAP80 phosphorylation.

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Nam Soo Lee

Surface-enhanced Raman spectroscopy of the catecholamine neurotransmitters and related compounds

TRAIP/RNF206 is required for recruitment of RAP80 to sites of DNA damage

Factors forming the BRCA1-A complex orchestrate BRCA1 recruitment to the sites of DNA damage

The active species in surface-enhanced Raman scattering of flavins on silver colloids

Cdk1 Protein-mediated Phosphorylation of Receptor-associated Protein 80 (RAP80) Serine 677 Modulates DNA Damage-induced G2/M Checkpoint and Cell Survival

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