Your search keyword '"Aaron R. Hieb"' showing total 18 results

1. The Port Delivery System with ranibizumab: a new paradigm for long-acting retinal drug delivery

Author

Shrirang V. Ranade, Mark R. Wieland, Tammy Tam, Jennifer C. Rea, Judit Horvath, Aaron R. Hieb, Weitao Jia, Lori Grace, Giulio Barteselli, and Jay M. Stewart

Subjects

Ranibizumab, Port Delivery System, continuous drug delivery, nAMD, ocular implant, retina, Therapeutics. Pharmacology, RM1-950

Abstract

The Port Delivery System with ranibizumab (PDS) is an innovative intraocular drug delivery system designed for the continuous delivery of ranibizumab into the vitreous for 6 months and beyond. The PDS includes an ocular implant, a customized formulation of ranibizumab, and four dedicated ancillary devices for initial fill, surgical implantation, refill-exchange, and explantation, if clinically indicated. Ranibizumab is an ideal candidate for the PDS on account of its unique physicochemical stability and high solubility. Controlled release is achieved via passive diffusion through the porous release control element, which is tuned to specific drug characteristics to accomplish a therapeutic level of ranibizumab in the vitreous. To characterize drug release from the implant, release rate was measured in vitro with starting concentrations of ranibizumab 10, 40, and 100 mg/mL, with release of ranibizumab 40 and 100 mg/mL found to remain quantifiable after 6 months. Using a starting concentration of 100 mg/mL, active release rate at approximately 6 months was consistent after the initial fill and first, second, and third refills, demonstrating reproducibility between implants and between multiple refill-exchanges of the same implant. A refill-exchange performed with a single 100-µL stroke using the refill needle was shown to replace over 95% of the implant contents with fresh drug. In vitro data support the use of the PDS with fixed refill-exchange intervals of at least 6 months in clinical trials.

Published

2022

2. Using differential scanning calorimetry for the development of non-reduced capillary electrophoresis sodium dodecyl sulfate methods for monoclonal antibodies

Author

Galahad Deperalta, Patricia Molina, Arthur J. Schick, Gabriella del Hierro, Leslie Welch, Thomas Niedringhaus, and Aaron R. Hieb

Subjects

Protein Denaturation, Capillary action, medicine.drug_class, Biophysics, Monoclonal antibody, 01 natural sciences, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, Capillary electrophoresis, Differential scanning calorimetry, Protein structure, medicine, Humans, Thermal stability, Denaturation (biochemistry), Sodium dodecyl sulfate, Molecular Biology, Chromatography, High Pressure Liquid, 030304 developmental biology, 0303 health sciences, Chromatography, Calorimetry, Differential Scanning, Protein Stability, Chemistry, 010401 analytical chemistry, Temperature, Antibodies, Monoclonal, Electrophoresis, Capillary, Sodium Dodecyl Sulfate, Cell Biology, Hydrogen-Ion Concentration, Trastuzumab, Chromatography, Ion Exchange, 0104 chemical sciences

Abstract

Analysis of non-reduced and reduced monoclonal antibodies (mAbs) by capillary electrophoresis-sodium dodecyl sulfate (CE-SDS) is routinely used to detect product size variants and process-related impurities. Levels of high molecular weight (HMW) forms obtained from this method usually trend comparably to those obtained by orthogonal methods such as size-exclusion ultra-high performance liquid chromatography (SE-UHPLC). However, in the presented case study, comparison of CE-SDS data for three IgG1 mAbs (trastuzumab, mAb1, and mAb2) showed a discrepancy between amounts of observed HMW forms in mAb2 compared with its native forms determined by SE-UHPLC (~17% vs. ~0.5%, respectively). SDS chemical denaturation, as measured by differential scanning calorimetry, demonstrated that the high thermal stability of mAb2 caused an unidentified HMW peak observed by non-reduced (NR)-CE-SDS, which was the result of improper denaturing, resulting in a partially folded species. More so, this strategy enabled the rapid identification of optimal SDS concentration and temperature conditions needed for suitable denaturation for mAb2. This case study presents an alternative option for quick optimization of NR-CE-SDS methods when characterizing mAbs or other thermally stable proteins. Also, this strategy can be used to understand basic biophysical mechanisms of protein unfolding and investigate the higher-order structure imparted by specific sequences and understand how these sequences might affect the results of an analytical method such as CE-SDS.

Published

2020

3. Stability of Nucleosomes Containing Homogenously Ubiquitylated H2A and H2B Prepared Using Semisynthesis

Author

Sinan Kilic, Tom W. Muir, Beat Fierz, Aaron R. Hieb, and Karolin Luger

Subjects

Models, Molecular, Histone-modifying enzymes, Chemical biology, chemical biology, Biochemistry, Article, Catalysis, Histones, Colloid and Surface Chemistry, Ubiquitin, biophysics, Chromosomal Instability, Histone H2A, Nucleosome, ubiquitylation, Binding Sites, biology, Chemistry, Ubiquitination, General Chemistry, Semisynthesis, Molecular biology, Nucleosomes, Chromatin, Histone, biology.protein, Biophysics, chromatin

Abstract

Post-translational modifications (PTMs) of histones are an essential feature in the dynamic regulation of chromatin. One of these modifications, ubiquitylation, has been speculated to directly influence the stability of the nucleosome, which represents the basic building block of chromatin. Here we report a strategy for the semisynthesis of site-specifically ubiquitylated histone H2A (uH2A). This branched protein was generated through a three-piece expressed protein ligation (EPL) approach including a traceless ligation at valine. uH2A could be efficiently incorporated into nucleosomes, thereby opening the way to detailed biochemical and biophysical studies on the function of this PTM. Accordingly, we used uH2A, as well as a previously generated ubiquitylated H2B (uH2B), in chaperone-coupled nucleosome stability assays to demonstrate that the direct effect of ubiquitylated histones on nucleosomal stability is in fact modest.

Published

2012

4. Histone Chaperone FACT Coordinates Nucleosome Interaction through Multiple Synergistic Binding Events

Author

Aaron R. Hieb, Duane D. Winkler, Karolin Luger, and Uma M. Muthurajan

Subjects

FACT, Cell Cycle Proteins, Xenopus Proteins, Biochemistry, Histones, Xenopus laevis, 03 medical and health sciences, Histone H1, Histone H2A, Histone methylation, Animals, Humans, Histone code, Nucleosome, Histone octamer, Molecular Biology, Chromatin Structure, 030304 developmental biology, Genetics, 0303 health sciences, biology, Chromatin Remodeling, 030302 biochemistry & molecular biology, High Mobility Group Proteins, Histone Chaperone, Cell Biology, Chromatin Assembly and Disassembly, Linker DNA, Nucleosomes, Protein Structure, Tertiary, Cell biology, DNA-Binding Proteins, Chromosomes/Non-histone Chromosomal Proteins, Histone, Multiprotein Complexes, biology.protein, Transcriptional Elongation Factors, Molecular Biophysics, Transcription Factors

Abstract

Background: The histone chaperone FACT binds and reorganizes nucleosomes during critical cellular processes. Results: FACT binds histones, DNA, and mono- and tri-nucleosomes with high affinity. FACT reduces non-nucleosomal histone/DNA interactions. Conclusion: Multiple regions of FACT strategically bind target sites on nucleosomes to coordinate (dis)assembly. Significance: The thermodynamic parameters guiding multiple FACT/nucleosome interaction(s) coincide with reorganization events., In eukaryotic cells, DNA maintenance requires ordered disassembly and re-assembly of chromatin templates. These processes are highly regulated and require extrinsic factors such as chromatin remodelers and histone chaperones. The histone chaperone FACT (facilitates chromatin transcription) is a large heterodimeric complex with roles in transcription, replication, and repair. FACT promotes and subsequently restricts access to DNA as a result of dynamic nucleosome reorganization. However, until now, there lacked a truly quantitative assessment of the critical contacts mediating FACT function. Here, we demonstrate that FACT binds histones, DNA, and intact nucleosomes at nanomolar concentrations. We also determine roles for the histone tails in free histone and nucleosome binding by FACT. Furthermore, we propose that the conserved acidic C-terminal domain of the FACT subunit Spt16 actively displaces nucleosomal DNA to provide access to the histone octamer. Experiments with tri-nucleosome arrays indicate a possible mode for FACT binding within chromatin. Together, the data reveal that specific FACT subunits synchronize interactions with various target sites on individual nucleosomes to generate a high affinity binding event and promote reorganization.

Published

2011

5. Nucleosome accessibility governed by the dimer/tetramer interface

Author

Vera Böhm, Karolin Luger, Andrea Rocker, Alexander Gansen, Andrew J. Andrews, Jörg Langowski, Katalin Tóth, and Aaron R. Hieb

Subjects

Models, Molecular, animal structures, Nucleosome disassembly, Dimer, Gene Regulation, Chromatin and Epigenetics, Sodium Chloride, 010402 general chemistry, 01 natural sciences, Histones, 03 medical and health sciences, chemistry.chemical_compound, Tetramer, Genetics, Fluorescence Resonance Energy Transfer, Nucleosome, Polymerase, 030304 developmental biology, 0303 health sciences, biology, Single-molecule FRET, Chromatin Assembly and Disassembly, 0104 chemical sciences, Nucleosomes, Histone, Spectrometry, Fluorescence, chemistry, Biochemistry, embryonic structures, biology.protein, Biophysics, Protein Multimerization, DNA

Abstract

Nucleosomes are multi-component macromolecular assemblies which present a formidable obstacle to enzymatic activities that require access to the DNA, e.g. DNA and RNA polymerases. The mechanism and pathway(s) by which nucleosomes disassemble to allow DNA access are not well understood. Here we present evidence from single molecule FRET experiments for a previously uncharacterized intermediate structural state before H2A-H2B dimer release, which is characterized by an increased distance between H2B and the nucleosomal dyad. This suggests that the first step in nucleosome disassembly is the opening of the (H3-H4)(2) tetramer/(H2A-H2B) dimer interface, followed by H2A-H2B dimer release from the DNA and, lastly, (H3-H4)(2) tetramer removal. We estimate that the open intermediate state is populated at 0.2-3% under physiological conditions. This finding could have significant in vivo implications for factor-mediated histone removal and exchange, as well as for regulating DNA accessibility to the transcription and replication machinery.

Published

2010

6. TFIIA Changes the Conformation of the DNA in TBP/TATA Complexes and Increases their Kinetic Stability

Author

Jennifer F. Kugel, Wayne A. Halsey, Meredith D. Betterton, James A. Goodrich, Thomas T. Perkins, and Aaron R. Hieb

Subjects

Models, Molecular, TATA box, RNA polymerase II, Biology, chemistry.chemical_compound, Structural Biology, Transcription (biology), Fluorescence Resonance Energy Transfer, Humans, Molecular Biology, Transcription factor, Promoter, DNA, TATA-Box Binding Protein, TATA Box, Molecular biology, Kinetics, chemistry, Transcription Factor TFIIA, Mutation, biology.protein, Biophysics, Nucleic Acid Conformation, Thermodynamics, TATA-binding protein, Transcription factor II A

Abstract

Eukaryotic mRNA transcription by RNA polymerase II is a highly regulated complex reaction involving numerous proteins. In order to control tissue and promoter specific gene expression, transcription factors must work in concert with each other and with the promoter DNA to form the proper architecture to activate the gene of interest. The TATA binding protein (TBP) binds to TATA boxes in core promoters and bends the TATA DNA. We have used quantitative solution fluorescence resonance energy transfer (FRET) and gel-based FRET (gelFRET) to determine the effect of TFIIA on the conformation of the DNA in TBP/TATA complexes and on the kinetic stability of these complexes. Our results indicate that human TFIIA decreases the angle to which human TBP bends consensus TATA DNA from 104 degrees to 80 degrees when calculated using a two-kink model. The kinetic stability of TBP/TATA complexes was greatly reduced by increasing the KCl concentration from 50 mM to 140 mM, which is more physiologically relevant. TFIIA significantly enhanced the kinetic stability of TBP/TATA complexes, thereby attenuating the effect of higher salt concentrations. We also found that TBP bent non-consensus TATA DNA to a lesser degree than consensus TATA DNA and complexes between TBP and a non-consensus TATA box were kinetically unstable even at 50 mM KCl. Interestingly, TFIIA increased the calculated bend angle and kinetic stability of complexes on a non-consensus TATA box, making them similar to those on a consensus TATA box. Our data show that TFIIA induces a conformational change within the TBP/TATA complex that enhances its stability under both in vitro and physiological salt conditions. Furthermore, we present a refined model for the effect that TFIIA has on DNA conformation that takes into account potential changes in bend angle as well as twist angle.

Published

2007

7. A quantitative investigation of linker histone interactions with nucleosomes and chromatin

Author

Alison E. White, Aaron R. Hieb, and Karolin Luger

Subjects

0301 basic medicine, Multidisciplinary, Solenoid (DNA), DNA, Biology, Linker DNA, Molecular biology, Chromatin, Article, Nucleosomes, Histones, 03 medical and health sciences, Mice, 030104 developmental biology, Histone, Chromatosome, Histone methylation, biology.protein, Biophysics, Histone code, Nucleosome, Animals, Protein Interaction Domains and Motifs, Protein Binding

Abstract

Linker histones such as H1 are abundant basic proteins that bind tightly to nucleosomes, thereby acting as key organizers of chromatin structure. The molecular details of linker histone interactions with the nucleosome and in particular the contributions of linker DNA and of the basic C-terminal tail of H1, are controversial. Here we combine rigorous solution-state binding assays with native gel electrophoresis and Atomic Force Microscopy, to quantify the interaction of H1 with chromatin. We find that H1 binds nucleosomes and nucleosomal arrays with very tight affinity by recognizing a specific DNA geometry minimally consisting of a solitary nucleosome with a single ~18 base pair DNA linker arm. The association of H1 alters the conformation of trinucleosomes so that only one H1 can bind to the two available linker DNA regions. Neither incorporation of the histone variant H2A.Z, nor the presence of neighboring nucleosomes affects H1 affinity. Our data provide a comprehensive thermodynamic framework for this ubiquitous chromatin architectural protein.

Published

2015

8. An 8 nt RNA triggers a rate-limiting shift of RNA polymerase II complexes into elongation

Author

Aaron R. Hieb, Jennifer F. Kugel, James A. Goodrich, and Sean Baran

Subjects

Transcription, Genetic, RNA-dependent RNA polymerase, RNA polymerase II, Article, General Biochemistry, Genetics and Molecular Biology, Abortive initiation, Transcription Factors, TFII, RNA polymerase I, Humans, Promoter Regions, Genetic, Molecular Biology, RNA polymerase II holoenzyme, Polymerase, General Immunology and Microbiology, biology, General Neuroscience, Templates, Genetic, Molecular biology, Cell biology, Transcription preinitiation complex, biology.protein, Nucleic Acid Conformation, RNA, RNA Polymerase II, Transcription Factor TFIIH, Transcription factor II A

Abstract

To better understand the critical conversions that RNA polymerase II complexes undergo during promoter escape, we determined in vitro the precise positions of the rate-limiting step and the last step requiring negative superhelicity or TFIIE and TFIIH. We found that both steps occur after synthesis of an 8 nt RNA during the stage encompassing translocation of the polymerase active site to the ninth register. When added to reactions just before this step, TFIIE and TFIIH overcame the requirement for negative superhelicity. The positions at which both steps occur were strictly dependent on RNA length as opposed to the location of the polymerase relative to promoter elements, showing that the transcript itself controls transformations during promoter escape. We propose a model in which completion of promoter escape involves a rate-limiting conversion of early transcribing complexes into elongation complexes. This transformation is triggered by synthesis of an 8 nt RNA, occurs independent of the general transcription factors, and requires under-winding in the DNA template via negative superhelicity or the action of TFIIE and TFIIH.

Published

2006

9. The conformational state of the nucleosome entry-exit site modulates TATA box-specific TBP binding

Author

Alexander Gansen, Jörg Langowski, Aaron R. Hieb, and Vera Böhm

Subjects

Binding Sites, biology, Base Sequence, TATA-Box Binding Protein, TATA box, Gene regulation, Chromatin and Epigenetics, RNA polymerase II, Promoter, Acetylation, DNA, Molecular biology, TATA Box, Nucleosomes, Histones, Transcription Factor TFIIA, Genetics, Biophysics, biology.protein, Nucleosome, Nucleic Acid Conformation, TATA-binding protein, Binding site, Transcription factor II A, Protein Binding

Abstract

The TATA binding protein (TBP) is a critical transcription factor used for nucleating assembly of the RNA polymerase II machinery. TBP binds TATA box elements with high affinity and kinetic stability and in vivo is correlated with high levels of transcription activation. However, since most promoters use less stable TATA-less or TATA-like elements, while also competing with nucleosome occupancy, further mechanistic insight into TBP's DNA binding properties and ability to access chromatin is needed. Using bulk and single-molecule FRET, we find that TBP binds a minimal consensus TATA box as a two-state equilibrium process, showing no evidence for intermediate states. However, upon addition of flanking DNA sequence, we observe non-specific cooperative binding to multiple DNA sites that compete for TATA-box specificity. Thus, we conclude that TBP binding is defined by a branched pathway, wherein TBP initially binds with little sequence specificity and is thermodynamically positioned by its kinetic stability to the TATA box. Furthermore, we observed the real-time access of TBP binding to TATA box DNA located within the DNA entry–exit site of the nucleosome. From these data, we determined salt-dependent changes in the nucleosome conformation regulate TBP's access to the TATA box, where access is highly constrained under physiological conditions, but is alleviated by histone acetylation and TFIIA.

Published

2014

10. Quantifying chromatin-associated interactions: the HI-FI system

Author

Duane D, Winkler, Karolin, Luger, and Aaron R, Hieb

Subjects

Staining and Labeling, Chromosomal Proteins, Non-Histone, Buffers, Xenopus Proteins, Protein Refolding, Nucleosomes, DNA-Binding Proteins, Histones, Solutions, Spectrometry, Fluorescence, Protein Interaction Mapping, Fluorescence Resonance Energy Transfer, Animals, Humans, Thermodynamics, Electrophoresis, Polyacrylamide Gel, Fluorescent Dyes, Protein Binding

Abstract

Chromatin plays a vital role in regulating cellular processes that occur on the DNA. Modulation of chromatin structure is conducted through interactions with binding factors that direct critical actions such as posttranslational modifications, nucleosome remodeling, and incorporation of histone variants. Specific factors recognize and act upon the various physical states of chromatin to modulate DNA accessibility. The ability to quantitatively characterize these interactions in vitro can provide valuable insight into the mechanisms that dictate chromatin architecture. Here, we describe in detail fluorescence methodologies for quantifying the thermodynamic principles that guide interactions between nucleosomal arrays, mononucleosomes, or nucleosome components and chromatin-associated factors through application of the HI-FI (High-throughput Interactions by Fluorescence Intensity) system. These measurements utilize fluorescence (de)quenching and FRET assays performed in 384-well microplates, making the assays suitable for high-throughput characterization of interactions at low concentrations. Further, this system can be used to determine the stoichiometric composition of complexes and specific sites of interaction. After quantification on a plate reader or similar instrument, the solution-based assays can be directly transferred to native gels for visualization of interaction(s). We also highlight procedural details on the efficient attachment of fluorescent dyes to histones and DNA. In all, the HI-FI system of assays can be used to elucidate mechanistic details of how specific chromatin-associated factors function at the molecular level.

Published

2012

11. Closing the gap between single molecule and bulk FRET analysis of nucleosomes

Author

Vera Böhm, Aaron R. Hieb, Alexander Gansen, Jörg Langowski, and Katalin Tóth

Subjects

Fluorescence-lifetime imaging microscopy, Protein Conformation, Biophysics, lcsh:Medicine, Biochemistry, Physical Chemistry, Histones, Biophysics Theory, Histone H3, Nucleic Acids, Fluorescence Resonance Energy Transfer, Genetics, Molecule, Nucleosome, lcsh:Science, Biology, Multidisciplinary, Chemical Physics, biology, Chemistry, lcsh:R, Acetylation, Single-molecule FRET, DNA, Molecular biology, Chromatin, Nucleosomes, Histone, Förster resonance energy transfer, Energy Transfer, biology.protein, Nucleic Acid Conformation, lcsh:Q, Epigenetics, Single-Cell Analysis, Research Article

Abstract

Nucleosome structure and stability affect genetic accessibility by altering the local chromatin morphology. Recent FRET experiments on nucleosomes have given valuable insight into the structural transformations they can adopt. Yet, even if performed under seemingly identical conditions, experiments performed in bulk and at the single molecule level have given mixed answers due to the limitations of each technique. To compare such experiments, however, they must be performed under identical conditions. Here we develop an experimental framework that overcomes the conventional limitations of each method: single molecule FRET experiments are carried out at bulk concentrations by adding unlabeled nucleosomes, while bulk FRET experiments are performed in microplates at concentrations near those used for single molecule detection. Additionally, the microplate can probe many conditions simultaneously before expending valuable instrument time for single molecule experiments. We highlight this experimental strategy by exploring the role of selective acetylation of histone H3 on nucleosome structure and stability; in bulk, H3-acetylated nucleosomes were significantly less stable than non-acetylated nucleosomes. Single molecule FRET analysis further revealed that acetylation of histone H3 promoted the formation of an additional conformational state, which is suppressed at higher nucleosome concentrations and which could be an important structural intermediate in nucleosome regulation.

Published

2012

12. Quantifying Chromatin-Associated Interactions

Author

Karolin Luger, Aaron R. Hieb, and Duane D. Winkler

Subjects

Genetics, Quenching (fluorescence), biology, Chromatin, chemistry.chemical_compound, Förster resonance energy transfer, Histone, chemistry, Biophysics, biology.protein, Nucleosome, Plate reader, DNA, Function (biology)

Abstract

Chromatin plays a vital role in regulating cellular processes that occur on the DNA. Modulation of chromatin structure is conducted through interactions with binding factors that direct critical actions such as posttranslational modifications, nucleosome remodeling, and incorporation of histone variants. Specific factors recognize and act upon the various physical states of chromatin to modulate DNA accessibility. The ability to quantitatively characterize these interactions in vitro can provide valuable insight into the mechanisms that dictate chromatin architecture. Here, we describe in detail fluorescence methodologies for quantifying the thermodynamic principles that guide interactions between nucleosomal arrays, mononucleosomes, or nucleosome components and chromatin-associated factors through application of the HI-FI (High-throughput Interactions by Fluorescence Intensity) system. These measurements utilize fluorescence (de)quenching and FRET assays performed in 384-well microplates, making the assays suitable for high-throughput characterization of interactions at low concentrations. Further, this system can be used to determine the stoichiometric composition of complexes and specific sites of interaction. After quantification on a plate reader or similar instrument, the solution-based assays can be directly transferred to native gels for visualization of interaction(s). We also highlight procedural details on the efficient attachment of fluorescent dyes to histones and DNA. In all, the HI-FI system of assays can be used to elucidate mechanistic details of how specific chromatin-associated factors function at the molecular level.

Published

2012

13. Deconstructing the late phase of vimentin assembly by total internal reflection fluorescence microscopy (TIRFM)

Author

Jörg Langowski, Stefan Winheim, Eva Maria Surmann, Tatjana Wedig, Norbert Mücke, Harald Herrmann, Aaron R. Hieb, and Marleen Silbermann

Subjects

Intermediate Filaments, Biophysics, lcsh:Medicine, Vimentin, macromolecular substances, Biochemistry, Physical Chemistry, law.invention, law, Microscopy, Molecular Cell Biology, Humans, Intermediate filament, Cytoskeleton, lcsh:Science, Biology, Persistence length, Multidisciplinary, Total internal reflection fluorescence microscope, Chemical Physics, biology, Chemistry, Physics, lcsh:R, Microscopy, Fluorescence, biology.protein, lcsh:Q, Electron microscope, Elongation, Ultracentrifugation, Research Article

Abstract

Quantitative imaging of intermediate filaments (IF) during the advanced phase of the assembly process is technically difficult, since the structures are several µm long and therefore they exceed the field of view of many electron (EM) or atomic force microscopy (AFM) techniques. Thereby quantitative studies become extremely laborious and time-consuming. To overcome these difficulties, we prepared fluorescently labeled vimentin for visualization by total internal reflection fluorescence microscopy (TIRFM). In order to investigate if the labeling influences the assembly properties of the protein, we first determined the association state of unlabeled vimentin mixed with increasing amounts of labeled vimentin under low ionic conditions by analytical ultracentrifugation. We found that bona fide tetrameric complexes were formed even when half of the vimentin was labeled. Moreover, we demonstrate by quantitative atomic force microscopy and electron microscopy that the morphology and the assembly properties of filaments were not affected when the fraction of labeled vimentin was below 10%. Using fast frame rates we observed the rapid deposition of fluorescently labeled IFs on glass supports by TIRFM in real time. By tracing their contours, we have calculated the persistence length of long immobilized vimentin IFs to 1 µm, a value that is identical to those determined for shorter unlabeled vimentin. These results indicate that the structural properties of the filaments were not affected significantly by the dye. Furthermore, in order to analyze the late elongation phase, we mixed long filaments containing either Alexa 488- or Alexa 647-labeled vimentin. The ‘patchy’ structure of the filaments obtained unambiguously showed the elongation of long IFs through direct end-to-end annealing of individual filaments.

Published

2011

14. Human TBP Bending of DNA Measured at the Single Molecule Level

Author

Amanda E. Carpenter, Thomas T. Perkins, Meredith D. Betterton, James A. Goodrich, and Aaron R. Hieb

Subjects

biology, Chemistry, Eukaryotic transcription, Biophysics, Polyethylene glycol, chemistry.chemical_compound, Crystallography, Optical tweezers, Transcription (biology), Covalent bond, biology.protein, Molecule, TATA-binding protein, DNA

Abstract

TATA binding protein (TBP) binds to DNA and bends it as a critical step of eukaryotic transcription. Human TBP induces an ∼100° bend in the DNA helix. To help elucidate the role of DNA architecture in transcription, we developed a single-molecule, optical-trapping assay to study the TBP-induced bending of DNA. We hypothesized that DNA bending would lead to an apparent shortening of the DNA. The predicted signal size is small (∼5 nm at 1 pN) and expected to decrease with increasing force. Moreover, the dynamics of TBP are slow, with a measured off-rate of ∼10−2 s−1 at physiological salt conditions. To detect these small, infrequent events, we developed an actively stabilized optical trapping instrument. We achieved high spatiotemporal resolution [0.56 nm (Δf = 0.01-1 Hz) over 200 s] at low force (1 pN) by developing a vertical optical trapping assay using short DNA tethers (92 nm) along with small beads (330 nm dia.). Detection of distinct TBP and TATA-box dependent signals required DNA molecules engineered to contain only one consensus TATA-box with no TATA-box like sequences in the flanking DNA. Significant nonspecific binding to the glass surfaces was minimized by covalently attaching polyethylene glycol (PEG) to the glass. With these experimental procedures, we directly observed individual bending and unbending events. The TBP-dependent DNA conformational changes were dynamic on the timescale of tens of seconds at a [TBP] ≈ 20 nM and a force of 1 pN. The change in DNA extension (∼5 nm) agreed well with theoretical predictions at 1 pN, but, unlike the simplest theory, showed little change in magnitude as the force was decreased. We expect that this assay will be broadly useful for studying DNA-protein interactions at high spatiotemporal resolution.

Published

2009

15. B2 RNA binds directly to RNA polymerase II to repress transcript synthesis

Author

Aaron R. Hieb, Tiffany A Allen, Jennifer F. Kugel, James A. Goodrich, and Celso A. Espinoza

Subjects

Small RNA, Hot Temperature, Time Factors, Transcription, Genetic, RNA-dependent RNA polymerase, RNA polymerase II, Mice, Structural Biology, Animals, Humans, RNA, Messenger, Promoter Regions, Genetic, Molecular Biology, RNA polymerase II holoenzyme, Cell Nucleus, Binding Sites, biology, General transcription factor, Dose-Response Relationship, Drug, Models, Genetic, DNA, Molecular biology, Kinetics, biology.protein, RNA, Transcription factor II F, Transcription factor II E, RNA Polymerase II, Transcription factor II D, Plasmids

Abstract

B2 RNA is a small noncoding RNA polymerase III transcript that represses mRNA transcription in response to heat shock in mouse cells. Here we define the mechanism by which B2 RNA inhibits RNA polymerase II (Pol II) transcription. Using a purified Pol II transcription system, we found that B2 RNA potently inhibits transcription by binding to core Pol II with high affinity and specificity. Through this interaction, B2 RNA assembles into preinitiation complexes at the promoter and blocks RNA synthesis. Once B2 RNA is removed from preinitiation complexes, transcriptional activity is restored. Our studies describe a previously unobserved mechanism of transcriptional repression by a small RNA and suggest that B2 RNA associates with Pol II at promoters in heat shocked cells to actively inhibit transcription.

Published

2004

16. Fluorescence strategies for high-throughput quantification of protein interactions

Author

Sheena D'Arcy, Aaron R. Hieb, Karolin Luger, Alison E. White, and Michael A. Kramer

Subjects

Saccharomyces cerevisiae Proteins, Fluorescence spectroscopy, Protein–protein interaction, Histones, Mice, 03 medical and health sciences, Bimolecular fluorescence complementation, Histone H1, Protein Interaction Mapping, Fluorescence Resonance Energy Transfer, Genetics, Animals, Nucleosome, Fluorometry, 030304 developmental biology, 0303 health sciences, Nucleosome Assembly Protein 1, biology, 030302 biochemistry & molecular biology, DNA, High-Throughput Screening Assays, Nucleosomes, Histone, Förster resonance energy transfer, Biochemistry, Chaperone (protein), biology.protein, Biophysics, Methods Online, Poly(ADP-ribose) Polymerases, Protein Binding

Abstract

Advances in high-throughput characterization of protein networks in vivo have resulted in large databases of unexplored protein interactions that occur during normal cell function. Their further characterization requires quantitative experimental strategies that are easy to implement in laboratories without specialized equipment. We have overcome many of the previous limitations to thermodynamic quantification of protein interactions, by developing a series of in-solution fluorescence-based strategies. These methods have high sensitivity, a broad dynamic range, and can be performed in a high-throughput manner. In three case studies we demonstrate how fluorescence (de)quenching and fluorescence resonance energy transfer can be used to quantitatively probe various high-affinity protein-DNA and protein-protein interactions. We applied these methods to describe the preference of linker histone H1 for nucleosomes over DNA, the ionic dependence of the DNA repair enzyme PARP1 in DNA binding, and the interaction between the histone chaperone Nap1 and the histone H2A-H2B heterodimer.

Published

2011

17. Closing the gap between single molecule and bulk FRET analysis of nucleosomes.

Author

Alexander Gansen, Aaron R Hieb, Vera Böhm, Katalin Tóth, and Jörg Langowski

Subjects

Medicine, Science

Abstract

Nucleosome structure and stability affect genetic accessibility by altering the local chromatin morphology. Recent FRET experiments on nucleosomes have given valuable insight into the structural transformations they can adopt. Yet, even if performed under seemingly identical conditions, experiments performed in bulk and at the single molecule level have given mixed answers due to the limitations of each technique. To compare such experiments, however, they must be performed under identical conditions. Here we develop an experimental framework that overcomes the conventional limitations of each method: single molecule FRET experiments are carried out at bulk concentrations by adding unlabeled nucleosomes, while bulk FRET experiments are performed in microplates at concentrations near those used for single molecule detection. Additionally, the microplate can probe many conditions simultaneously before expending valuable instrument time for single molecule experiments. We highlight this experimental strategy by exploring the role of selective acetylation of histone H3 on nucleosome structure and stability; in bulk, H3-acetylated nucleosomes were significantly less stable than non-acetylated nucleosomes. Single molecule FRET analysis further revealed that acetylation of histone H3 promoted the formation of an additional conformational state, which is suppressed at higher nucleosome concentrations and which could be an important structural intermediate in nucleosome regulation.

Published

2013

18. Deconstructing the late phase of vimentin assembly by total internal reflection fluorescence microscopy (TIRFM).

Author

Stefan Winheim, Aaron R Hieb, Marleen Silbermann, Eva-Maria Surmann, Tatjana Wedig, Harald Herrmann, Jörg Langowski, and Norbert Mücke

Subjects

Medicine, Science

Abstract

Quantitative imaging of intermediate filaments (IF) during the advanced phase of the assembly process is technically difficult, since the structures are several µm long and therefore they exceed the field of view of many electron (EM) or atomic force microscopy (AFM) techniques. Thereby quantitative studies become extremely laborious and time-consuming. To overcome these difficulties, we prepared fluorescently labeled vimentin for visualization by total internal reflection fluorescence microscopy (TIRFM). In order to investigate if the labeling influences the assembly properties of the protein, we first determined the association state of unlabeled vimentin mixed with increasing amounts of labeled vimentin under low ionic conditions by analytical ultracentrifugation. We found that bona fide tetrameric complexes were formed even when half of the vimentin was labeled. Moreover, we demonstrate by quantitative atomic force microscopy and electron microscopy that the morphology and the assembly properties of filaments were not affected when the fraction of labeled vimentin was below 10%. Using fast frame rates we observed the rapid deposition of fluorescently labeled IFs on glass supports by TIRFM in real time. By tracing their contours, we have calculated the persistence length of long immobilized vimentin IFs to 1 µm, a value that is identical to those determined for shorter unlabeled vimentin. These results indicate that the structural properties of the filaments were not affected significantly by the dye. Furthermore, in order to analyze the late elongation phase, we mixed long filaments containing either Alexa 488- or Alexa 647-labeled vimentin. The 'patchy' structure of the filaments obtained unambiguously showed the elongation of long IFs through direct end-to-end annealing of individual filaments.

Published

2011