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1. FANCI Regulates Recruitment of the FA Core Complex at Sites of DNA Damage Independently of FANCD2.

2. A disease-associated XPA allele interferes with TFIIH binding and primarily affects transcription-coupled nucleotide excision repair

3. Two interaction surfaces between XPA and RPA organize the preincision complex in nucleotide excision repair

4. Structural basis of the fanconi anemia-associated mutations within the FANCA and FANCG complex

5. Functional cross talk between the Fanconi anemia and ATRX/DAXX histone chaperone pathways promotes replication fork recovery

6. Single-molecule visualization reveals the damage search mechanism for the human NER protein XPC-RAD23B

7. Molecular basis for damage recognition and verification by XPC-RAD23B and TFIIH in nucleotide excision repair

8. ERCC1 mutations impede DNA damage repair and cause liver and kidney dysfunction in patients

9. Two interaction surfaces between XPA and RPA organize the preincision complex in nucleotide excision repair.

10. SDE2 integrates into the TIMELESS-TIPIN complex to protect stalled replication forks

11. A key interaction with RPA orients XPA in NER complexes

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

14. Ring-expansion protocol: preparation of synthetically versatile dihydrotropones

15. Convergent synthesis of new types of stabilized carotenoid compounds

16. Ring-Expansion Protocol: Preparation of Synthetically Versatile Dihydrotropones

17. Expeditious and Practical Synthesis of Lycopene

18. FANCI Regulates Recruitment of the FA Core Complex at Sites of DNA Damage Independently of FANCD2

19. Synthesis of site-specific DNA-protein conjugates and their effects on DNA replication

20. The efficiencies of damage recognition and excision correlate with duplex destabilization induced by acetylaminofluorene adducts in human nucleotide excision repair

21. Lack of recognition by global-genome nucleotide excision repair accounts for the high mutagenicity and persistence of aristolactam-DNA adducts

22. ChemInform Abstract: Ring-Expansion Protocol: Preparation of Synthetically Versatile Dihydrotropones

23. The Intramolecular Baylis—Hillman Reaction: Easy Preparation of Versatile Substrates, Facile Reactions, and Synthetic Applications

28. SDE2 integrates into the TIMELESS-TIPIN complex to protect stalled replication forks

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