New Roles For TRF2 In Chromatin Architecture

Baker, Asmaa M.

04 November 2008

Telomeres are specialized nucleoprotein structures found at the end of eukaryotic chromosomes. The telomere DNA in humans is composed of the sequence "5'-TTAGGG-3'" tandemly repeated in a stretch of 5-30kb of double stranded DNA. TTAGGG Repeat Factor 2 (TRF2) is a telomere DNA binding protein that has a critical role in telomere end protection. The current model for telomere protection by TRF2 is through its ability to remodel telomeres into looped higher-order structures, called the t-loop, which sequesters the end from DNA damage sensors. Since telomeres are known to be comprised of nucleosomal chromatin, it is important to determine how TRF2 binds to and affects the structure of nucleosomal arrays. The ability of TRF2 to bind to unusual DNA structures such as the t-loop and the single stranded/double (ss/ds) stranded telomere DNA junction may facilitate its binding to DNA in the form of nucleosomal arrays and promote higher-order chromatin structures. In this study, we have reconstituted a 2kb DNA fragment containing 550bp of telomere DNA into nucleosomal arrays and tested the binding of full-lengthTRF2 and four truncation mutants to telomeric nucleosomal arrays. Our data indicates that TRF2 and its truncation mutants bind to telomere nucleosomal arrays as well as it binds to telomere DNA. We used a novel electrophoretic technique, Analytical Agarose Gel Electrophoresis (AAGE), to measure changes in surface charge density, hydrodynamic radius, and conformational flexibility of DNA and nucleosomal arrays upon protein binding. Our results indicate that the C-terminal DNA binding Myb/SANT domain of TRF2 might be rearranging nucleosomal structure through either nucleosome sliding, unwrapping, or changing the arrangement of the linker DNA, while the N-terminal basic DNA binding region is causing nucleosomal arrays compaction. Instead of significant compaction, histone-free DNA undergoes DNA condensation and self-association. This activity is observed with the full-length protein and all regions of the protein, with the exception of TRF2-DBD, participate in the process. We speculate that the ability of TRF2-DBD to rearrange nucleosomal structure and N-terminal basic region to cause nucleosomal fiber compaction may allow TRF2 to promote t-loop formation in the context of chromatin. We propose that TRF2, possessing all the features, has a new role at telomeres as a chromatin architectural protein.

Telomere Higher Order Structure

Telomere Nucleosomal Arrays

Studies on Formation Mechanism of Higher-Order Structures in Aqueous Solutions of Associating Polymers / 会合性高分子水溶液における高次構造の形成機構に関する研究

Shibata, Motoki

23 March 2022

京都大学 / 新制・課程博士 / 博士(工学) / 甲第23921号 / 工博第5008号 / 新制||工||1782(附属図書館) / 京都大学大学院工学研究科高分子化学専攻 / (主査)教授 古賀 毅, 教授 中村 洋, 教授 竹中 幹人 / 学位規則第4条第1項該当 / Doctor of Philosophy (Engineering) / Kyoto University / DGAM

associating polymer

higher-order structure

micelle

hydrogel

phase separation

random copolymer

methylcellulose

500

RIPPLiT and ChimeraTie: High throughput tools for understanding higher order RNP structures

Metkar, Mihir

30 July 2018

Even after their discovery more than 60 years ago, little is known about how messenger RNAs (mRNAs) are packaged inside the cells. To ensure efficient and accurate delivery of the intended message to its proper destination, it is important to package the informational molecule in a way that protects it from premature degradation but also proper decoding at the destination. However, very little is known about the this fundamentally important step of mRNA packaging inside eukaryotic cells. To this end, we developed a novel approach, RIPPLiT (RNA ImmunoPrecipitation and Proximity Ligation in Tandem), to capture the 3D architecture of the ribonucleoprotein particles (RNPs) of interest transcriptome-wide. To begin with, we applied RIPPLiT to the exon-junction complex (EJC), a set of proteins stably bound to a spliced RNA. EJCs have been shown to interact with other proteins like SR- and SR-like to form megadalton sized complexes and help protect large regions of mRNAs. Thus, we hypothesized that these RNPs would provide an ideal system to elucidate the higher order organization of mRNPs. Preliminary analysis of data obtained from RIPPLiT consisted of “chimeric reads”, reads with multiple RNA fragments ligated together, which could not be analyzed with any of the existing bioinformatics tools. Thus, we developed a new bioinformatics suite, ChimeraTie, to map, analyze and visualize chimeric reads. Performing polymer analysis on chimeric reads obtained for hundreds of mRNAs, we were able to predict that mRNPs are linearly and densely packed into flexible rod-like structures before they undergo translation. In this thesis, along with the detailed biological conclusion, I have also provided a step-wise manual to perform RIPPLiT experiment and analyze the ensuing data using ChimeraTie.

mRNA

RNA-RNA interactions

RNA higher order structure

proximity ligations

RIPPLiT

ChimeraTie

chimeric reads

Biochemistry

Bioinformatics

Molecular Biology

Structural Biology

Fundamental and Applied Studies on Self-assembling of Polymer-brush-modified Nanoparticles in Ionic Liquid / イオン液体中におけるポリマーブラシ付与微粒子の自己組識化に関する基礎と応用研究

Nakanishi, Yohei

26 March 2018

京都大学 / 0048 / 新制・課程博士 / 博士(工学) / 甲第21124号 / 工博第4488号 / 新制||工||1697(附属図書館) / 京都大学大学院工学研究科高分子化学専攻 / (主査)教授 辻井 敬亘, 教授 山子 茂, 教授 竹中 幹人 / 学位規則第4条第1項該当 / Doctor of Philosophy (Engineering) / Kyoto University / DFAM

Polymer brush

Nanoparticle

Ionic liquid

Small-angle X-ray scattering

Higher-order structure

Ionic conductivity

Dye-sensitized solar cell

500

Investigation on the Secondary Structures Formed in Full-length Telomere Overhang and Rational Design of Ligands for Targeting Telomere G-quadruplexes

Abraham Punnoose, Jibin

22 February 2018

No description available.

Molecular Biology

Biochemistry

Chemistry

Study on the higher-order structure of DNA and gene expression / DNA高次構造の多様性と遺伝子発現活性 / DNA コウジ コウゾウ ノ タヨウセイ ト イデンシ ハツゲン カッセイ

西尾 天志, Takashi Nishio

22 March 2022

博士(工学) / Doctor of Philosophy in Engineering / 同志社大学 / Doshisha University

DNA高次構造

遺伝子発現活性

ポリアミン

DNA

Higher-order structure of DNA

Gene expression

Gene regulation

Polyamine