Your search keyword '"Molecular Probes chemistry"' showing total 2,987 results

201. Identifying Receptors for Neuropeptides and Peptide Hormones: Challenges and Recent Progress.

Author

Abid MSR, Mousavi S, and Checco JW

Subjects

Animals, Humans, Ligands, Machine Learning, Molecular Probes chemistry, Receptors, G-Protein-Coupled chemistry, Receptors, G-Protein-Coupled metabolism, Receptors, Neuropeptide chemistry, Receptors, Neuropeptide metabolism, Neuropeptides metabolism, Peptide Hormones metabolism, Receptors, G-Protein-Coupled analysis, Receptors, Neuropeptide analysis

Abstract

Intercellular signaling events mediated by neuropeptides and peptide hormones represent important targets for both basic science and drug discovery. For many bioactive peptides, the protein receptors that transmit information across the receiving cell membrane are not known, severely limiting these signaling pathways as potential therapeutic targets. Identifying the receptor(s) for a given peptide of interest is complicated by several factors. Most notably, cell-cell signaling peptides are generated through dynamic biosynthetic pathways, can act on many different families of receptor proteins, and can participate in complex ligand-receptor interactions that extend beyond a simple one-to-one archetype. Here, we discuss recent methodological advances to identify signaling partners for bioactive peptides. Recent efforts have centered on methods to identify candidate receptors via transcript expression, methods to match peptide-receptor pairs through high throughput screening, and methods to capture direct ligand-receptor interactions using chemical probes. Future applications of the receptor identification approaches discussed here, as well as technical advancements to address their limitations, promise to lead to a greater understanding of how cells communicate to deliver complex physiologies. Importantly, such advancements will likely provide novel targets for the treatment of human diseases within the central nervous and endocrine systems.

Published

2021

202. Ratiometric Fluorescence Assay for Nitroreductase Activity: Locked-Flavylium Fluorophore as a NTR-Sensitive Molecular Probe.

Author

Kim SJ, Yoon JW, Yoon SA, and Lee MH

Subjects

A549 Cells, Animals, Cell Death, Chromatography, High Pressure Liquid, Endocytosis, HeLa Cells, Humans, Hydrogen-Ion Concentration, Mice, Molecular Probes chemical synthesis, NIH 3T3 Cells, Spectrometry, Fluorescence, Enzyme Assays methods, Fluorescent Dyes chemistry, Molecular Probes chemistry, Nitroreductases metabolism

Abstract

Nitroreductases belong to a member of flavin-containing enzymes that can reduce nitroaromatic compounds to amino derivatives with NADH as an electron donor. NTR activity is known to be elevated in the cancerous environment and is considered an advantageous target in therapeutic prodrugs for the treatment of cancer. Here, we developed a ratiometric fluorescent molecule for observing NTR activity in living cells. This can provide a selective and sensitive response to NTR with a distinct increase in fluorescence ratio (FI 530 /FI 630 ) as well as color changes. We also found a significant increase in NTR activity in cervical cancer HeLa and lung cancer A549 cells compared to non-cancerous NIH3T3. We proposed that this new ratiometric fluorescent molecule could potentially be used as a NTR-sensitive molecular probe in the field of cancer diagnosis and treatment development related to NTR activity.

Published

2021

203. Surface engineered amphiphilic carbon dots: solvatochromic behavior and applicability as a molecular probe.

Author

Pandit S, Mondal S, and De M

Subjects

Molecular Probes chemical synthesis, Molecular Structure, Particle Size, Solvents chemistry, Surface Properties, Surface-Active Agents chemical synthesis, Carbon chemistry, Molecular Probes chemistry, Quantum Dots chemistry, Surface-Active Agents chemistry

Abstract

Carbon dots (C-dots) have attracted great attention in the fields of nanotechnology and bioengineering owing to their unique and tunable optical properties with excellent photoluminescence characteristics. Herein, we have engineered amphiphilic C-dots (AC-dots) using positional isomers of diamino benzene with citric acid under mild microwave irradiation to minimize any background reactions. The optical properties changed from excitation-dependent to excitation-independent depending on the isomer used. This unique optical property of the AC-dots was studied in the presence of various solvents and we extensively inspected the AC-dot-solvent interactions. The intensity of the emission wavelength varied with solvent polarity and showed a linear relationship. Furthermore, we extended this property to investigate the molecular environment in biomolecular systems such as proteins. Interestingly, we found that, in the presence of various proteins, the emission intensity was enhanced, quenched or remained unchanged depending on the nature of the protein surface. The mode of interaction between AC-dots and protein was determined using temperature-dependent fluorescence spectroscopy. This study could provide vital information about the surfaces of proteins and the potential application of C-Dots as a fluorescent probe to detect biological molecules and environments.

Published

2021

204. Engineered TALE Repeats for Enhanced Imaging-Based Analysis of Cellular 5-Methylcytosine.

Author

Muñoz-López Á, Jung A, Buchmuller B, Wolffgramm J, Maurer S, Witte A, and Summerer D

Subjects

Genetic Engineering, HEK293 Cells, Humans, Molecular Probes chemistry, Transcription Activator-Like Effectors chemistry, 5-Methylcytosine analysis, DNA Methylation, Image Processing, Computer-Assisted methods, Molecular Probes metabolism, Repetitive Sequences, Nucleic Acid, Transcription Activator-Like Effectors metabolism

Abstract

Transcription-activator-like effectors (TALEs) are repeat-based, programmable DNA-binding proteins that can be engineered to recognize sequences of canonical and epigenetically modified nucleobases. Fluorescent TALEs can be used for the imaging-based analysis of cellular 5-methylcytosine (5 mC) in repetitive DNA sequences. This is based on recording fluorescence ratios from cell co-stains with two TALEs: an analytical TALE targeting the cytosine (C) position of interest through a C-selective repeat that is blocked by 5 mC, and a control TALE targeting the position with a universal repeat that binds both C and 5 mC. To enhance this approach, we report herein the development of novel 5 mC-selective repeats and their integration into TALEs that can replace universal TALEs in imaging-based 5 mC analysis, resulting in a methylation-dependent response of both TALEs. We screened a library of size-reduced repeats and identified several 5 mC binders. Compared to the 5 mC-binding repeat of natural TALEs and to the universal repeat, two repeats containing aromatic residues showed enhancement of 5 mC binding and selectivity in cellular transcription activation and electromobility shift assays, respectively. In co-stains of cellular SATIII DNA with a corresponding C-selective TALE, this selectivity results in a positive methylation response of the new TALE, offering perspectives for studying 5 mC functions in chromatin regulation by in situ imaging with increased dynamic range., (© 2020 The Authors. ChemBioChem published by Wiley-VCH GmbH.)

Published

2021

205. Facilitation of molecular motion to develop turn-on photoacoustic bioprobe for detecting nitric oxide in encephalitis.

Author

Qi J, Feng L, Zhang X, Zhang H, Huang L, Zhou Y, Zhao Z, Duan X, Xu F, Kwok RTK, Lam JWY, Ding D, Xue X, and Tang BZ

Subjects

Animals, Biosensing Techniques instrumentation, Disease Models, Animal, Encephalitis pathology, Male, Mice, Molecular Imaging methods, Molecular Probes chemistry, Photoacoustic Techniques instrumentation, Biosensing Techniques methods, Encephalitis diagnosis, Encephalitis metabolism, Nitric Oxide isolation & purification, Photoacoustic Techniques methods

Abstract

Nitric oxide (NO) is an important signaling molecule overexpressed in many diseases, thus the development of NO-activatable probes is of vital significance for monitoring related diseases. However, sensitive photoacoustic (PA) probes for detecting NO-associated complicated diseases (e.g., encephalitis), have yet to be developed. Herein, we report a NO-activated PA probe for in vivo detection of encephalitis by tuning the molecular geometry and energy transformation processes. A strong donor-acceptor structure with increased conjugation can be obtained after NO treatment, along with the active intramolecular motion, significantly boosting "turn-on" near-infrared PA property. The molecular probe exhibits high specificity and sensitivity towards NO over interfering reactive species. The probe is capable of detecting and differentiating encephalitis in different severities with high spatiotemporal resolution. This work will inspire more insights into the development of high-performing activatable PA probes for advanced diagnosis by making full use of intramolecular motion and energy transformation processes.

Published

2021

206. A glycan FRET assay for detection and characterization of catalytic antibodies to the Cryptococcus neoformans capsule.

Author

Crawford CJ, Wear MP, Smith DFQ, d'Errico C, McConnell SA, Casadevall A, and Oscarson S

Subjects

Complement System Proteins metabolism, Epitope Mapping, Kinetics, Macrophages immunology, Models, Molecular, Molecular Probes chemistry, Oligosaccharides chemical synthesis, Oligosaccharides chemistry, Peptides chemistry, Phagocytosis, Protein Structure, Secondary, Antibodies, Catalytic immunology, Antibodies, Fungal immunology, Biological Assay, Cryptococcus neoformans immunology, Fluorescence Resonance Energy Transfer, Polysaccharides chemistry

Abstract

Classic antibody functions include opsonization, complement activation, and enhancement of cellular antimicrobial function. Antibodies can also have catalytic activity, although the contribution of catalysis to their biological functions has been more difficult to establish. With the ubiquity of catalytic antibodies against glycans virtually unknown, we sought to advance this knowledge. The use of a glycan microarray allowed epitope mapping of several monoclonal antibodies (mAbs) against the capsule of Cryptococcus neoformans From this, we designed and synthesized two glycan-based FRET probes, which we used to discover antibodies with innate glycosidase activity and analyze their enzyme kinetics, including mAb 2H1, the most efficient identified to date. The validity of the FRET assay was confirmed by demonstrating that the mAbs mediate glycosidase activity on intact cryptococcal capsules, as observed by a reduction in capsule diameter. Furthermore, the mAb 18B7, a glycosidase hydrolase, resulted in the appearance of reducing ends in the capsule as labeled by a hydroxylamine-armed fluorescent (HAAF) probe. Finally, we demonstrate that exposing C. neoformans cells to catalytic antibodies results in changes in complement deposition and increased phagocytosis by macrophages, suggesting that the antiphagocytic properties of the capsule have been impaired. Our results raise questions over the ubiquity of antibodies with catalytic activity against glycans and establish the utility of glycan-based FRET and HAAF probes as tools for investigating this activity., Competing Interests: The authors declare no competing interest.

Published

2021

207. α-Methylene-β-Lactone Scaffold for Developing Chemical Probes at the Two Ends of the Selectivity Spectrum.

Author

Wang L, Riel LP, Bajrami B, Deng B, Howell AR, and Yao X

Subjects

Humans, Lactones chemistry, Molecular Probes chemistry, Molecular Structure, Orlistat analysis, Proteomics, Sesquiterpenes analysis, Tandem Mass Spectrometry, Lactones chemical synthesis, Molecular Probes chemical synthesis

Abstract

The utilities of an α-methylene-β-lactone (MeLac) moiety as a warhead composed of multiple electrophilic sites are reported. We demonstrate that a MeLac-alkyne not only reacts with diverse proteins as a broadly reactive measurement probe, but also recruits reduced endogenous glutathione (GSH) to assemble a selective chemical probe of GSH-β-lactone (GSH-Lac)-alkyne in live cells. Tandem mass spectrometry reveals that MeLac reacts with nucleophilic cysteine, serine, lysine, threonine, and tyrosine residues, through either Michael or acyl addition. A peptide-centric proteomics platform demonstrates that the proteomic selectivity profiles of orlistat and parthenolide, which have distinct reactivities, are measurable by MeLac-alkyne as a high-coverage probe. The GSH-Lac-alkyne selectively probes the glutathione S-transferase P responsible for multidrug resistance. The assembly of the GSH-Lac probe exemplifies a modular and scalable route to develop selective probes with different recognizing moieties., (© 2020 Wiley-VCH GmbH.)

Published

2021

208. Encoding DNA Frameworks for Amplified Multiplexed Imaging of Intracellular microRNAs.

Author

Zhu D, Wei Y, Sun T, Zhang C, Ang L, Su S, Mao X, Li Q, Fan C, Zuo X, Chao J, and Wang L

Subjects

Cell Line, Tumor, Cell Survival, Humans, Intracellular Space metabolism, Microscopy, Atomic Force, Molecular Probes chemistry, Nanotechnology methods, Nucleic Acid Conformation, DNA chemistry, MicroRNAs chemistry, Molecular Imaging methods

Abstract

Real-time imaging of multiple low-abundance microRNAs (miRNAs) simultaneously in living cells with high sensitivity is of vital importance for accurate cancer clinical diagnosis and prognosis studies. Maintaining stability of nanoprobes resistant to enzyme degradation and enabling effective signal amplification is highly needed for in vivo imaging studies. Herein, a rationally designed one-pot assembled multicolor tetrahedral DNA frameworks (TDFs) by encoding multicomponent nucleic acid enzymes (MNAzymes) was developed for signal-amplified multiple miRNAs imaging in living cells with high sensitivity and selectivity. TDFs could enter cells via self-delivery with good biocompatibility and stability. Two kinds of MNAzymes specific for miRNA-21 and miRNA-155 with fluorescein labeling were encoded in the structure of TDFs respectively through one-step thermal annealing. In the intracellular environment, the TDFs could be specifically bound with its specific miRNA target and form an active DNAzyme structure. The cleavage of the active site would trigger the release of target miRNA and circular fluorescence signal amplification, which enabled accurate diagnosis on miRNA identifications of different cell lines with high sensitivity. Meanwhile, with the specific AS1411 aptamer targeting for nucleolin overexpressed on the surface of the carcinoma cells, this well-designed TDFs nanoprobe exhibited good discrimination between cancer cells and normal cells. The strategy provides an efficient tool for understanding the biological function of miRNAs in cancer pathogenesis and therapeutic applications.

Published

2021

209. Intraoperative Molecular Imaging Utilizing a Folate Receptor-Targeted Near-Infrared Probe Can Identify Macroscopic Gastric Adenocarcinomas.

Author

Newton AD, Predina JD, Frenzel-Sulyok LG, Low PS, Singhal S, and Roses RE

Subjects

Adenocarcinoma diagnosis, Drug Delivery Systems, Female, Fluorescence, Humans, Lymph Nodes diagnostic imaging, Lymph Nodes pathology, Male, Middle Aged, Adenocarcinoma diagnostic imaging, Folate Receptor 1 metabolism, Intraoperative Care, Molecular Imaging, Molecular Probes chemistry, Spectroscopy, Near-Infrared, Stomach Neoplasms diagnosis, Stomach Neoplasms diagnostic imaging

Abstract

Purpose: Current methods of assessing disease burden in gastric adenocarcinoma are imperfect. Improved visualization during surgery with intraoperative molecular imaging (IMI) could improve gastric adenocarcinoma staging and guide surgical decision-making. The goal of this study was to evaluate if IMI with a folate receptor-targeted near-infrared fluorescent agent, OTL38, could identify gastric adenocarcinomas during surgery., Procedures: Five patients were enrolled in an IMI clinical trial. Patients received a folate receptor-targeted near-infrared dye (OTL38) 1.5-6 h prior to surgery. During staging laparoscopy and gastric resection, IMI was utilized to identify the primary tumor and any fluorescent lymph nodes. Resected tumors were analyzed for folate receptor alpha (FRα) and CD68 expression using immunohistochemistry. Microscopic OTL38 accumulation was examined with immunofluorescence., Results: Four out of five patients underwent total or subtotal gastrectomy; one had a staging laparoscopy only. All four patients who underwent gastric resection had invasive gastric adenocarcinoma; three had fluorescent tumors, mean tumor to background ratio (TBR) 4.1 ± 2.9. The one patient with a non-fluorescent tumor had a T1a tumor with two 0.4 cm tumor foci within a larger polyp. In each case with a fluorescent tumor, the fluorescence was evident from the exterior of the stomach. Two of the fluorescent tumors had modest FRα expression and no CD68 expression. One fluorescent tumor had high CD68 expression and no FRα expression., Conclusions: Intraoperative molecular imaging of gastric adenocarcinoma with OTL38 is feasible. Further studies should evaluate the clinical utility of this technique.

Published

2021

210. Assessing The Key Photophysical Properties of Triangulenium Dyes for DNA Binding by Alteration of the Fluorescent Core.

Author

Lewis BW, Bisballe N, Santella M, Summers PA, Vannier JB, Kuimova MK, Laursen BW, and Vilar R

Subjects

Electron Transport, Fluorescent Dyes analysis, Molecular Probes analysis, Molecular Probes chemistry, DNA analysis, DNA chemistry, Fluorescence, Fluorescent Dyes chemistry, G-Quadruplexes

Abstract

Four-stranded G-quadruplex (G4) DNA is a non-canonical DNA topology that has been proposed to form in cells and play key roles in how the genome is read and used by the cellular machinery. Previously, a fluorescent triangulenium probe (DAOTA-M2) was used to visualise G4s in cellulo, thanks to its distinct fluorescence lifetimes when bound to different DNA topologies. Herein, the library of available triangulenium probes is expanded to explore how modifications to the fluorescent core of the molecule affect its photophysical characteristics, interaction with DNA and cellular localisation. The benzo-bridged and isopropyl-bridged diazatriangulenium dyes, BDATA-M2 and CDATA-M2 respectively, featuring ethyl-morpholino substituents, were synthesised and characterised. The interactions of these molecules with different DNA topologies were studied to determine their binding affinity, fluorescence enhancement and fluorescence lifetime response. Finally, the cellular uptake and localisation of these optical probes were investigated. Whilst structural modifications to the triangulenium core only slightly alter the binding affinity to DNA, BDATA-M2 and CDATA-M2 cannot distinguish between DNA topologies through their fluorescence lifetime. It is argued theoretically and experimentally that this is due to reduced effectiveness of photoinduced electron transfer (PET) quenching. This work presents valuable new evidence into the critical role of PET quenching when using the fluorescence lifetime of triangulenium dyes to discriminate G4 DNA from duplex DNA, highlighting the importance of fine tuning redox and spectral properties when developing new triangulenium-based G4 probes., (© 2020 Wiley-VCH GmbH.)

Published

2021

211. NeissLock provides an inducible protein anhydride for covalent targeting of endogenous proteins.

Author

Scheu AHA, Lim SYT, Metzner FJ, Mohammed S, and Howarth M

Subjects

Anhydrides metabolism, Animals, Molecular Imaging methods, Molecular Probes chemistry, Molecular Probes genetics, Proteolysis, Recombinant Fusion Proteins chemistry, Recombinant Fusion Proteins genetics, Bacterial Proteins genetics, Membrane Proteins genetics, Molecular Probes metabolism, Protein Engineering methods, Recombinant Fusion Proteins metabolism, Staining and Labeling methods

Abstract

The Neisseria meningitidis protein FrpC contains a self-processing module (SPM) undergoing autoproteolysis via an aspartic anhydride. Herein, we establish NeissLock, using a binding protein genetically fused to SPM. Upon calcium triggering of SPM, the anhydride at the C-terminus of the binding protein allows nucleophilic attack by its target protein, ligating the complex. We establish a computational tool to search the Protein Data Bank, assessing proximity of amines to C-termini. We optimize NeissLock using the Ornithine Decarboxylase/Antizyme complex. Various sites on the target (α-amine or ε-amines) react with the anhydride, but reaction is blocked if the partner does not dock. Ligation is efficient at pH 7.0, with half-time less than 2 min. We arm Transforming Growth Factor-α with SPM, enabling specific covalent coupling to Epidermal Growth Factor Receptor at the cell-surface. NeissLock harnesses distinctive protein chemistry for high-yield covalent targeting of endogenous proteins, advancing the possibilities for molecular engineering.

Published

2021

212. Harnessing reaction-based probes to preferentially target pancreatic β-cells and β-like cells.

Author

Kahraman S, Manna D, Dirice E, Maji B, Small J, Wagner BK, Choudhary A, and Kulkarni RN

Subjects

Animals, Flow Cytometry, Fluorescent Antibody Technique, Fluorescent Dyes chemistry, Humans, Islets of Langerhans cytology, Islets of Langerhans metabolism, Mice, Molecular Structure, Insulin-Secreting Cells metabolism, Molecular Imaging methods, Molecular Probes chemistry

Abstract

Highly sensitive approaches to target insulin-expressing cells would allow more effective imaging, sorting, and analysis of pancreatic β-cells. Here, we introduce the use of a reaction-based probe, diacetylated Zinpyr1 (DA-ZP1), to image pancreatic β-cells and β-like cells derived from human pluripotent stem cells. We harness the high intracellular zinc concentration of β-cells to induce a fluorescence signal in cells after administration of DA-ZP1. Given its specificity and rapid uptake by cells, we used DA-ZP1 to purify live stem cell-derived β-like cells as confirmed by immunostaining analysis. We tested the ability of DA-ZP1 to image transplanted human islet grafts and endogenous mouse pancreatic islets in vivo after its systemic administration into mice. Thus, DA-ZP1 enables purification of insulin-secreting β-like cells for downstream applications, such as functional studies, gene-expression, and cell-cell interaction analyses and can be used to label engrafted human islets and endogenous mouse islets in vivo., (© 2021 Kahraman et al.)

Published

2021

213. Steric-Free Bioorthogonal Labeling of Acetylation Substrates Based on a Fluorine-Thiol Displacement Reaction.

Author

Lyu Z, Zhao Y, Buuh ZY, Gorman N, Goldman AR, Islam MS, Tang HY, and Wang RE

Subjects

Acetyl Coenzyme A chemistry, Acetylation, Biotin analogs & derivatives, Fluorescent Dyes chemistry, HEK293 Cells, Humans, Molecular Probes chemistry, Molecular Structure, Proof of Concept Study, Rhodamines chemistry, Acetyl Coenzyme A metabolism, Acetyltransferases metabolism, Molecular Probes metabolism, Sulfhydryl Compounds chemistry

Abstract

We have developed a novel bioorthogonal reaction that can selectively displace fluorine substitutions alpha to amide bonds. This fluorine-thiol displacement reaction (FTDR) allows for fluorinated cofactors or precursors to be utilized as chemical reporters, hijacking acetyltransferase-mediated acetylation both in vitro and in live cells, which cannot be achieved with azide- or alkyne-based chemical reporters. The fluoroacetamide labels can be further converted to biotin or fluorophore tags using FTDR, enabling the general detection and imaging of acetyl substrates. This strategy may lead to a steric-free labeling platform for substrate proteins, expanding our chemical toolbox for functional annotation of post-translational modifications in a systematic manner.

Published

2021

214. One-Step Azolation Strategy for Site- and Chemo-Selective Labeling of Proteins with Mass-Sensitive Probes.

Author

Tang KC and Raj M

Subjects

Amino Acid Sequence, Chromatography, High Pressure Liquid, Tandem Mass Spectrometry, Azoles chemistry, Molecular Probes chemistry, Myoglobin chemistry

Abstract

The chemical modification of proteins in a site-selective manner leads to many advances in various scientific fields. The major challenges with conventional N-terminal bioconjugation techniques are the lack of universal sequence compatibility and poor mass-detection sensitivity of the resulting bioconjugates. This approach efficiently analyzes proteolytic fragments and native proteins in a complex mixture. Multiple chemical steps are usually required for the site-selective synthesis of bioconjugates with enhanced mass-detection sensitivity. We present a single-step, versatile strategy for the selective modification of protein N-termini with mass boosters. The chemical tag enhances the peptide detection by multiple orders thus leading to the unambiguous analysis of the resulting bioconjugates. We demonstrate that tagging proteolytic fragments with mass sensitivity probes in a complex mixture improves the detection of resulting bioconjugates., (© 2020 Wiley-VCH GmbH.)

Published

2021

215. Profiling of Haemophilus influenzae strain R2866 with carbohydrate-based covalent probes.

Author

Metier C, Dow J, Wootton H, Lynham S, Wren B, and Wagner GK

Subjects

Bacterial Proteins metabolism, Haemophilus influenzae isolation & purification, Carbohydrate Metabolism, Carbohydrates chemistry, Haemophilus influenzae metabolism, Molecular Probes chemistry, Molecular Probes metabolism

Abstract

We demonstrate the application of four covalent probes based on anomerically pure d-galactosamine and d-glucosamine scaffolds for the profiling of Haemophilus influenzae strain R2866. The probes have been used successfully for the labelling of target proteins not only in cell lysates, but also in intact cells. Differences in the labelling patterns between lysates and intact cells indicate that the probes can penetrate into the periplasm, but not the cytoplasm of H. influenzae. Analysis of selected target proteins by LC-MS/MS suggests predominant labelling of nucleotide-binding proteins, including several known antibacterial drug targets. Our protocols will aid the identification of molecular determinants of bacterial pathogenicity in Haemophilus influenzae and other bacterial pathogens.

Published

2021

216. A novel electrochemical biosensor for ultrasensitive Hg 2+ detection via a triple signal amplification strategy.

Author

He W, Qiao B, Li F, Pan L, Chen D, Cao Y, Tu J, Wang X, Lv C, and Wu Q

Subjects

DNA chemistry, DNA metabolism, Exodeoxyribonucleases metabolism, Gold chemistry, Metal Nanoparticles chemistry, Molecular Probes chemistry, Particle Size, Biosensing Techniques, DNA genetics, Electrochemical Techniques, Mercury analysis, Nucleic Acid Amplification Techniques

Abstract

We developed a novel electrochemical biosensor for ultrasensitive Hg2+ detection via a triple signal amplification strategy of a DNA dual cycle, organic-inorganic hybrid nanoflowers (Cu3(PO4)2 HNFs) and gold nanoparticle (AuNP) probe. The DNA dual cycle was triggered by exonuclease III (Exo III) in the presence of Hg2+, and Cu3(PO4)2 HNFs were synthesized as an AuNP probe carrier. The electrochemical biosensor displayed high stability, high sensitivity and excellent specificity, which was improved by up to seven orders of magnitude compared to the World Health Organization (WHO) allowed Hg2+ levels in drinking water. This signal amplification strategy could be easily modified and extended to detect other hazardous heavy metals and nucleic acids.

Published

2021

217. Trifluorinated Keto-Enol Tautomeric Switch in Probing Domain Rotation of a G Protein-Coupled Receptor.

Author

Wang X, Zhao W, Al-Abdul-Wahid S, Lu Y, Cheng T, Madsen JJ, and Ye L

Subjects

Ligands, Protein Conformation, Rotation, Stereoisomerism, Fluorine chemistry, Molecular Probes chemistry, Receptors, G-Protein-Coupled chemistry

Abstract

Conformational dynamics and transitions of biologically active molecules are pivotal for understanding the physiological responses they elicit. In the case of receptor activation, there are major implications elucidating disease mechanisms and drug discovery innovation. Yet, incorporation of these factors into drug screening systems remains challenging in part due to the lack of suitable approaches to include them. Here, we present a novel strategy to probe the GPCR domain rotation by utilizing the 19 fluorine signal variability of a trifluorinated keto-enol (TFKE) chemical equilibrium. The method takes advantage of the high sensitivity of the TFKE tautomerism toward microenvironmental changes resulting from receptor conformational transitions upon ligand binding. We validated the method using the adenosine A 2A R receptor as a model system in which the TFKE was attached to two sites exhibiting opposing motions upon ligand binding, namely, V229C 6.31 on transmembrane domain VI (TM6) and A289C 7.54 on TM7. Our results demonstrated that the TFKE switch was an excellent reporter for the domain rotation and could be used to study the conformational transition and dynamics of relative domain motions. Although further studies are needed in order to establish a quantitative relationship between the rotational angle and the population distribution of different components in a particular system, the research presented here provides a foundation for its application in studying receptor domain rotation and dynamics, which could be useful in drug screening efforts.

Published

2021

218. Probing Biomolecular Interactions by a Pattern-Forming Peptide-Conjugate Sensor.

Author

Heermann T, Franquelim HG, Glock P, Harrington L, and Schwille P

Subjects

DNA, Single-Stranded chemistry, Dimerization, Protein Binding, Cell Cycle Proteins chemistry, Escherichia coli Proteins chemistry, Molecular Probes chemistry, Peptides chemistry

Abstract

As a key mechanism underpinning many biological processes, protein self-organization has been extensively studied. However, the potential to apply the distinctive, nonlinear biochemical properties of such self-organizing systems to biotechnological problems such as the facile detection and characterization of biomolecular interactions has not yet been explored. Here, we describe an in vitro assay in a 96-well plate format that harnesses the emergent behavior of the Escherichia coli Min system to provide a readout of biomolecular interactions. Crucial for the development of our approach is a minimal MinE-derived peptide that stimulates MinD ATPase activity only when dimerized. We found that this behavior could be induced via any pair of foreign, mutually binding molecular entities fused to the minimal MinE peptide. The resulting MinD ATPase activity and the spatiotemporal nature of the produced protein patterns quantitatively correlate with the affinity of the fused binding partners, thereby enabling a highly sensitive assay for biomolecular interactions. Our assay thus provides a unique means of quantitatively visualizing biomolecular interactions and may prove useful for the assessment of domain interactions within protein libraries and for the facile investigation of potential inhibitors of protein-protein interactions.

Published

2021

219. Synthesis of functionalized copillar[4+1]arenes and rotaxane as heteromultivalent scaffolds.

Author

Chen W, Mohy Ei Dine T, and Vincent SP

Subjects

Macrocyclic Compounds chemical synthesis, Molecular Probes chemical synthesis, Molecular Structure, Rotaxanes chemical synthesis, Macrocyclic Compounds chemistry, Molecular Probes chemistry, Rotaxanes chemistry

Abstract

In this study, novel copillar[4+1]arenes were used as central heteromultivalent scaffolds via orthogonal couplings with a series of biologically relevant molecules such as carbohydrates, α-amino acids, biotin and phenylboronic acid. Further modifications by introducing maleimides or cyclooctyne groups provided molecular probes adapted to copper-free click chemistry. An octa-azidated fluorescent rotaxane bearing two distinct ligands was also generated in a fully controlled manner.

Published

2021

220. A Molecular Probe with Both Chromogenic and Fluorescent Units for Detecting Serine Proteases.

Author

Ishida K, Nakamura Y, Ohta T, and Oe Y

Subjects

Humans, Aniline Compounds chemistry, Chymotrypsin analysis, Fluorescent Dyes chemistry, Molecular Probes chemistry, Papain analysis, Trypsin analysis

Abstract

A molecular probe with l-phenylalanine p -nitroanilide and l-lysin 4-methylcoumaryl-7-amide, in which these amino acid derivatives are connected through a succinic-acid spacer, was prepared. Trypsin and papain were detected by blue-fluorescence emission of generated 7-amino-4-methylcoumarin (AMC). α-Chymotrypsin and nattokinase were detected from both the blue-fluorescence emission of AMC and the UV absorbance of p -nitroaniline. In addition, different time courses of p -nitroaniline and AMC were observed between the reaction of P1 with α-chymotrypsin and that with nattokinase. In the case of nattokinase, both the fluorescence emission and UV absorbance slowly increased. In contrast, the increasing UV absorbance was saturated at the early stage of the reaction of the present probe with chymotrypsin, whereas the fluorescence emission continuously increased in the following stages.

Published

2021

221. Use of Synthetic Glycolipids to Probe the Number and Position of Arabinan Chains on Mycobacterial Arabinogalactan.

Author

Angala SK, Joe M, McNeil MR, Liav A, Lowary TL, and Jackson M

Subjects

Carbohydrate Conformation, Carbohydrate Sequence, Chromatography, Liquid methods, Spectrometry, Mass, Electrospray Ionization methods, Tandem Mass Spectrometry methods, Galactans chemistry, Glycolipids chemistry, Molecular Probes chemistry, Mycobacterium chemistry

Abstract

The arabinogalactan of Corynebacterianeae is a critical heteropolysaccharide that tethers outer membrane mycolic acids to peptidoglycan thus forming the characteristic cell wall core of these prokaryotes. An essential α-(1→5)-arabinosyltransferase, AftA, is responsible for the transfer of the first arabinofuranosyl (Ara f ) unit of the arabinan domain to the galactan backbone of arabinogalactan, but the number and precise position at which Ara f residue(s) is/are added in mycobacteria remain ill-defined. Using membrane preparations from Mycobacterium smegmatis overexpressing aftA , farnesyl-phospho-arabinose as an Ara f donor, and a series of synthetic galactan acceptors of various lengths, we here show that a single priming arabinosyl residue substitutes the C-5 position of a precisely positioned internal 6-linked galactofuranosyl residue of the galactan acceptors, irrespective of their length. This unexpected result suggests that, like the structurally related mycobacterial lipoarabinomannans, the arabinogalactan of mycobacteria may in fact harbor a single arabinan chain.

Published

2021

222. Design Strategies of Photoacoustic Molecular Probes.

Author

Wang S and Zhang X

Subjects

Animals, Humans, Molecular Probes chemistry, Molecular Structure, Molecular Imaging, Molecular Probes chemical synthesis, Photoacoustic Techniques

Abstract

Photoacoustic (PA) probes have been developed very quickly and applied in broad areas in recent years. Most of them are constructed based on organic dyes with intrinsic near-infrared (NIR) absorption properties. To increase PA contrast and improve imaging resolution and the sensitivity of detection, various methods for the design of PA probes have been developed. This minireview mainly focuses on the development and design strategies of activatable small-molecule PA probes in four aspects: reaction-cleavage, metal ion chelation, photoswitch, and protonation-deprotonation. It highlights some key points of designing PA probes corresponding to their properties and applications. The challenges and perspectives for small-molecule PA probes are also discussed., (© 2020 Wiley-VCH GmbH.)

Published

2021

223. Harnessing Ionic Selectivity in Acetyltransferase Chemoproteomic Probes.

Author

Jing Y, Montano JL, Levy M, Lopez JE, Kung PP, Richardson P, Krajewski K, Florens L, Washburn MP, and Meier JL

Subjects

Amino Acid Sequence, Chromatography, High Pressure Liquid methods, Electrophoresis, Polyacrylamide Gel methods, Reproducibility of Results, Substrate Specificity, Tandem Mass Spectrometry methods, Acetyltransferases chemistry, Molecular Probes chemistry, Proteomics methods

Abstract

Chemical proteomics provides a powerful strategy for the high-throughput assignment of enzyme function or inhibitor selectivity. However, identifying optimized probes for an enzyme family member of interest and differentiating signal from the background remain persistent challenges in the field. To address this obstacle, here we report a physiochemical discernment strategy for optimizing chemical proteomics based on the coenzyme A (CoA) cofactor. First, we synthesize a pair of CoA-based sepharose pulldown resins differentiated by a single negatively charged residue and find this change alters their capture properties in gel-based profiling experiments. Next, we integrate these probes with quantitative proteomics and benchmark analysis of "probe selectivity" versus traditional "competitive chemical proteomics." This reveals that the former is well-suited for the identification of optimized pulldown probes for specific enzyme family members, while the latter may have advantages in discovery applications. Finally, we apply our anionic CoA pulldown probe to evaluate the selectivity of a recently reported small molecule N-terminal acetyltransferase inhibitor. These studies further validate the use of physical discriminant strategies in chemoproteomic hit identification and demonstrate how CoA-based chemoproteomic probes can be used to evaluate the selectivity of small molecule protein acetyltransferase inhibitors, an emerging class of preclinical therapeutic agents.

Published

2021

224. A "Three-in-One" Multifunctional Probe for Bcl-2/Mcl-1 Profiling and Visualizing in Situ.

Author

Zhang X, Wang Z, Guo Z, Song T, He N, Zhu J, Cao K, and Zhang Z

Subjects

Fluorescence, Humans, Molecular Probes chemical synthesis, Optical Imaging, Molecular Probes chemistry, Myeloid Cell Leukemia Sequence 1 Protein chemistry, Neoplasms diagnostic imaging, Proto-Oncogene Proteins c-bcl-2 chemistry

Abstract

Bcl-2 and Mcl-1, the two arms of the anti-apoptotic Bcl-2 family proteins, have been identified as key regulators of apoptosis and effective therapeutic targets of cancer. However, no small-molecular probe is capable of profiling and visualizing both Bcl-2 and Mcl-1 simultaneously in situ. Herein, we report a multifunctional molecular probe (BnN 3 -OPD-Alk) by a "three-in-one" molecular designing strategy, which integrated the Bcl-2/Mcl-1 binding ligand, fluorescent reporter group and photoreactive group azido into the same scaffold. BnN 3 -OPD-Alk exhibited sub-micromolar affinities to Bcl-2/Mcl-1 and bright green self-fluorescence. It was then successfully applied for Bcl-2/Mcl-1 labeling, capturing, enriching, and bioimaging both in vitro and in cells. This strategy could facilitate the precise early diagnosis and effective therapy of dual Bcl-2/Mcl-1-related diseases., (© 2020 Wiley-VCH GmbH.)

Published

2021

225. Site-specific covalent labeling of His-tag fused proteins with N-acyl-N-alkyl sulfonamide reagent.

Author

Thimaradka V, Hoon Oh J, Heroven C, Radu Aricescu A, Yuzaki M, Tamura T, and Hamachi I

Subjects

HEK293 Cells, Histidine metabolism, Humans, Indicators and Reagents metabolism, Lysine chemistry, Lysine metabolism, Models, Molecular, Molecular Probes metabolism, Molecular Structure, Nickel chemistry, Nickel metabolism, Nitrilotriacetic Acid chemistry, Nitrilotriacetic Acid metabolism, Proteins metabolism, Sulfonamides metabolism, Histidine chemistry, Indicators and Reagents chemistry, Molecular Probes chemistry, Proteins chemistry, Staining and Labeling, Sulfonamides chemistry

Abstract

The ability to incorporate a desired functionality into proteins of interest in a site-specific manner can provide powerful tools for investigating biological systems and creating therapeutic conjugates. However, there are not any universal methods that can be applied to all proteins, and it is thus important to explore the chemical strategy for protein modification. In this paper, we developed a new reactive peptide tag/probe pair system for site-specific covalent protein labeling. This method relies on the recognition-driven reaction of a peptide tag and a molecular probe, which comprises the lysine-containing short histidine tag (KH6 or H6K) and a binuclear nickel (II)- nitrilotriacetic acid (Ni 2+ -NTA) complex probe containing a lysine-reactive N-acyl-N-alkyl sulfonamide (NASA) group. The selective interaction of the His-tag and Ni 2+ -NTA propeles a rapid nucleophilic reaction between a lysine residue of the tag and the electrophilic NASA group of the probe by the proximity effect, resulting in the tag-site-specific functionalization of proteins. We characterized the reactive profile and site-specificity of this method using model peptides and proteins in vitro, and demonstrated the general utility for production of a nanobody-chemical probe conjugate without compromising its binding ability., (Copyright © 2020 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2021

226. Fluorine-18 Radiolabelling and Photophysical Characteristics of Multimodal PET-Fluorescence Molecular Probes.

Author

Klenner MA, Pascali G, Massi M, and Fraser BH

Subjects

Fluorescent Dyes chemistry, Fluorescence, Fluorine Radioisotopes chemistry, Molecular Probes chemistry, Positron-Emission Tomography

Abstract

Positron emission tomography (PET)-fluorescence imaging is an emerging field of multimodality imaging seeking to attain synergy between the two techniques. The probes employed in PET-fluorescence imaging incorporate both a fluorophore and radioisotope which enable complementary information to be obtained from both imaging techniques via the administration of a single agent. Fluorine-18 is the most commonly used radioisotope in PET imaging and consequently many novel attempts to radiofluorinate various fluorophores have transpired over the past decade. In this Minireview, the most relevant fluorine-18 labelled PET-fluorescence probes have been classified into four groups as per the implemented fluorophore: 1) boron-dipyrromethene (BODIPY) dyes, 2) cyanine dyes, 3) alternative organic fluorophores and 4) organometallics, such as quantum dots (QDs) and rhenium complexes. The biological, radiochemical and photophysical properties of each probe have been systematically compared to aid future endeavours in PET-fluorescence chemistry., (© 2020 Wiley-VCH GmbH.)

Published

2021

227. Comparison of Bioorthogonal β-Lactone Activity-Based Probes for Selective Labeling of Penicillin-Binding Proteins.

Author

Brown NW Jr, Shirley JD, Marshall AP, and Carlson EE

Subjects

Anti-Bacterial Agents chemistry, Lactones chemistry, Molecular Conformation, Molecular Probes chemistry, Penicillin-Binding Proteins metabolism, Spectrometry, Fluorescence, Staining and Labeling, Streptococcus pneumoniae metabolism, Anti-Bacterial Agents metabolism, Lactones metabolism, Molecular Probes metabolism, Penicillin-Binding Proteins analysis, Streptococcus pneumoniae chemistry

Abstract

Penicillin-binding proteins (PBPs) are a family of bacterial enzymes that are key components of cell-wall biosynthesis and the target of β-lactam antibiotics. Most microbial pathogens contain multiple structurally homologous PBP isoforms, making it difficult to target individual PBPs. To study the roles and regulation of specific PBP isoforms, a panel of bioorthogonal β-lactone probes was synthesized and compared. Fluorescent labeling confirmed selectivity, and PBPs were selectively enriched from Streptococcus pneumoniae lysates. Comparisons between fluorescent labeling of probes revealed that the accessibility of bioorthogonal reporter molecules to the bound probe in the native protein environment exerts a more significant effect on labeling intensity than the bioorthogonal reaction used, observations that are likely applicable beyond this class of probes or proteins. Selective, bioorthogonal activity-based probes for PBPs will facilitate the activity-based determination of the roles and regulation of specific PBP isoforms, a key gap in knowledge that has yet to be filled., (© 2020 Wiley-VCH GmbH.)

Published

2021

228. Simultaneous Zn 2+ tracking in multiple organelles using super-resolution morphology-correlated organelle identification in living cells.

Author

Fang H, Geng S, Hao M, Chen Q, Liu M, Liu C, Tian Z, Wang C, Takebe T, Guan JL, Chen Y, Guo Z, He W, and Diao J

Subjects

Autophagosomes metabolism, Autophagy, Carbonyl Cyanide m-Chlorophenyl Hydrazone pharmacology, Cell Survival, Endoplasmic Reticulum metabolism, Fluorescent Dyes metabolism, HeLa Cells, Humans, Induced Pluripotent Stem Cells metabolism, Intracellular Space metabolism, Lysosomes metabolism, Molecular Probes chemistry, Molecular Probes metabolism, Naphthalimides metabolism, Organoids metabolism, Spectrometry, Fluorescence, Cell Tracking, Organelles metabolism, Zinc metabolism

Abstract

Zn 2+ plays important roles in metabolism and signaling regulation. Subcellular Zn 2+ compartmentalization is essential for organelle functions and cell biology, but there is currently no method to determine Zn 2+ signaling relationships among more than two different organelles with one probe. Here, we report simultaneous Zn 2+ tracking in multiple organelles (Zn-STIMO), a method that uses structured illumination microscopy (SIM) and a single Zn 2+ fluorescent probe, allowing super-resolution morphology-correlated organelle identification in living cells. To guarantee SIM imaging quality for organelle identification, we develop a new turn-on Zn 2+ fluorescent probe, NapBu-BPEA, by regulating the lipophilicity of naphthalimide-derived Zn 2+ probes to make it accumulate in multiple organelles except the nucleus. Zn-STIMO with this probe shows that CCCP-induced mitophagy in HeLa cells is associated with labile Zn 2+ enhancement. Therefore, direct organelle identification supported by SIM imaging makes Zn-STIMO a reliable method to determine labile Zn 2+ dynamics in various organelles with one probe. Finally, SIM imaging of pluripotent stem cell-derived organoids with NapBu-BPEA demonstrates the potential of super-resolution morphology-correlated organelle identification to track biospecies and events in specific organelles within organoids.

Published

2021

229. Probing the structure and function of acyl carrier proteins to unlock the strategic redesign of type II polyketide biosynthetic pathways.

Author

Sulpizio A, Crawford CEW, Koweek RS, and Charkoudian LK

Subjects

Amino Acid Sequence, Biosynthetic Pathways, Molecular Probes chemistry, Polyketide Synthases chemistry, Polyketide Synthases metabolism, Protein Binding, Protein Conformation, Sequence Homology, Amino Acid, Structure-Activity Relationship, Acyl Carrier Protein chemistry, Acyl Carrier Protein metabolism, Polyketides metabolism

Abstract

Type II polyketide synthases (PKSs) are protein assemblies, encoded by biosynthetic gene clusters in microorganisms, that manufacture structurally complex and pharmacologically relevant molecules. Acyl carrier proteins (ACPs) play a central role in biosynthesis by shuttling malonyl-based building blocks and polyketide intermediates to catalytic partners for chemical transformations. Because ACPs serve as central hubs in type II PKSs, they can also represent roadblocks to successfully engineering synthases capable of manufacturing 'unnatural natural products.' Therefore, understanding ACP conformational dynamics and protein interactions is essential to enable the strategic redesign of type II PKSs. However, the inherent flexibility and transience of ACP interactions pose challenges to gaining insight into ACP structure and function. In this review, we summarize how the application of chemical probes and molecular dynamic simulations has increased our understanding of the structure and function of type II PKS ACPs. We also share how integrating these advances in type II PKS ACP research with newfound access to key enzyme partners, such as the ketosynthase-chain length factor, sets the stage to unlock new biosynthetic potential., Competing Interests: Conflict of interest The authors declare that they have no conflicts of interest with the contents of this article., (Copyright © 2021 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2021

230. Activatable Zymography Probes Enable In Situ Localization of Protease Dysregulation in Cancer.

Author

Soleimany AP, Kirkpatrick JD, Su S, Dudani JS, Zhong Q, Bekdemir A, and Bhatia SN

Subjects

Animals, Humans, Male, Mice, Molecular Imaging, Prostatic Neoplasms enzymology, Proteolysis, Disease Models, Animal, Molecular Probes chemistry, Peptide Hydrolases analysis, Peptide Hydrolases metabolism, Prostatic Neoplasms pathology, Proto-Oncogene Proteins c-myc genetics

Abstract

Recent years have seen the emergence of conditionally activated diagnostics and therapeutics that leverage protease-cleavable peptide linkers to enhance their specificity for cancer. However, due to a lack of methods to measure and localize protease activity directly within the tissue microenvironment, the design of protease-activated agents has been necessarily empirical, yielding suboptimal results when translated to patients. To address the need for spatially resolved protease activity profiling in cancer, we developed a new class of in situ probes that can be applied to fresh-frozen tissue sections in a manner analogous to immunofluorescence staining. These activatable zymography probes (AZP) detected dysregulated protease activity in human prostate cancer biopsy samples, enabling disease classification. AZPs were leveraged within a generalizable framework to design conditional cancer diagnostics and therapeutics and showcased in the Hi-Myc mouse model of prostate cancer, which models features of early pathogenesis. Multiplexed screening against barcoded substrates yielded a peptide, S16, that was robustly and specifically cleaved by tumor-associated metalloproteinases in the Hi-Myc model. In situ labeling with an AZP incorporating S16 revealed a potential role of metalloproteinase dysregulation in proliferative, premalignant Hi-Myc prostatic glands. Systemic administration of an in vivo imaging probe incorporating S16 perfectly classified diseased and healthy prostates, supporting the relevance of ex vivo activity assays to in vivo translation. We envision AZPs will enable new insights into the biology of protease dysregulation in cancer and accelerate the development of conditional diagnostics and therapeutics for multiple cancer types. SIGNIFICANCE: Visualization of protease activity within the native tissue context using AZPs provides new biological insights into protease dysregulation in cancer and guides the design of conditional diagnostics and therapeutics., (©2020 American Association for Cancer Research.)

Published

2021

231. Anion Receptors for the Discrimination of ATP and ADP in Biological Media.

Author

Butler SJ and Jolliffe KA

Subjects

Animals, Biosensing Techniques, Humans, Molecular Probes chemistry, Adenosine Diphosphate metabolism, Adenosine Triphosphate metabolism, Molecular Probes metabolism

Abstract

The design and synthesis of molecular receptors for the selective binding of nucleoside phosphate anions (e. g. ATP, ADP, GTP, GDP, UDP) in aqueous media at physiological pH is a valuable research endeavour, which could lead to new sensing tools for biomedical and drug discovery research. However, this target is very challenging due to similarities in anion size, structure and charge. This Minireview provides an account of the development of receptors capable of discriminating between ATP and ADP, and their utilisation in biological sensing applications. Particular focus is given to the application of receptors for the determination of ATP or ADP concentrations in biological media, tracking ATP levels (or the ATP/ADP ratio) in cells using fluorescence microscopy, or real-time monitoring of enzyme reactions involving ATP and ADP in vitro., (© 2020 The Authors. ChemPlusChem published by Wiley-VCH GmbH.)

Published

2021

232. Analyzing the Integrin Adhesome by In Situ Proximity Ligation Assay.

Author

Perrino BA, Xie Y, and Alexandru C

Subjects

Actin Cytoskeleton metabolism, Actin Cytoskeleton ultrastructure, Antibodies chemistry, Extracellular Matrix metabolism, Extracellular Matrix ultrastructure, Focal Adhesions ultrastructure, Gastric Mucosa metabolism, Gastric Mucosa ultrastructure, Humans, Image Processing, Computer-Assisted, Integrin alpha Chains chemistry, Integrin beta1 chemistry, Microscopy, Fluorescence, Molecular Probes chemistry, Molecular Probes metabolism, Multiprotein Complexes chemistry, Muscle, Smooth metabolism, Muscle, Smooth ultrastructure, Oligonucleotides chemical synthesis, Protein Binding, Focal Adhesions metabolism, Immunohistochemistry methods, Integrin alpha Chains metabolism, Integrin beta1 metabolism, Multiprotein Complexes metabolism, Oligonucleotides metabolism

Abstract

The in situ proximity ligation assay (PLA) is capable of detecting single protein events such as protein protein-interactions and posttranslational modifications (e.g., protein phosphorylation) in tissue and cell samples prepared for analysis by immunofluorescent or immunohistochemical microscopy. The targets are detected using two primary antibodies which must be from different host species. A pair of secondary antibodies (PLA probes) conjugated to complementary oligonucleotides is applied to the sample, and a signal is generated only when the two PLA probes are in close proximity by their binding to the two primary antibodies that have bound to their targets in close proximity. The signal from each pair of PLA probes is visualized as an individual fluorescent spot. These PLA signals can be quantified (counted) using image analysis software (ImageJ), and also assigned to a specific subcellular location based on microscopy image overlays. In principle, in situ PLA offers a relatively simple and sensitive technique to analyze interactions among any proteins for which suitable antibodies are available. Integrin-mediated focal adhesions (FAs) are large multiprotein complexes consisting of more than 150 proteins, also known as the integrin adhesome, which link the extracellular matrix (ECM) to the actin cytoskeleton and regulate the functioning of mechanosignaling pathways. The in situ PLA approach is well suited for examining the spatiotemporal aspects of protein posttranslational modifications and protein interactions occurring in dynamic multiprotein complexes such as integrin mediated focal adhesions.

Published

2021

233. Chemical Tools for Illumination of Tuberculosis Biology, Virulence Mechanisms, and Diagnosis.

Author

Kumar G, Narayan R, and Kapoor S

Subjects

Alcohol Oxidoreductases chemistry, Alcohol Oxidoreductases metabolism, Animals, Bacterial Proteins chemistry, Bacterial Proteins metabolism, Cell Wall metabolism, Fluorescent Dyes chemistry, Humans, Lipids chemistry, Molecular Probes chemistry, Mycobacterium tuberculosis drug effects, Mycobacterium tuberculosis pathogenicity, Peptidoglycan chemistry, Sulfatases chemistry, Sulfatases metabolism, Trehalose chemistry, Tuberculosis microbiology, Virulence genetics, Mycobacterium tuberculosis metabolism, Tuberculosis diagnosis

Abstract

Tuberculosis (TB) remains one of the deadliest infectious diseases and begs the scientific community to up the ante for research and exploration of completely novel therapeutic avenues. Chemical biology-inspired design of tunable chemical tools has aided in clinical diagnosis, facilitated discovery of therapeutics, and begun to enable investigation of virulence mechanisms at the host-pathogen interface of Mycobacterium tuberculosis . This Perspective highlights chemical tools specific to mycobacterial proteins and the cell lipid envelope that have furnished rapid and selective diagnostic strategies and provided unprecedented insights into the function of the mycobacterial proteome and lipidome. We discuss chemical tools that have enabled elucidating otherwise intractable biological processes by leveraging the unique lipid and metabolite repertoire of mycobacterial species. Some of these probes represent exciting starting points with the potential to illuminate poorly understood aspects of mycobacterial pathogenesis, particularly the host membrane-pathogen interactions.

Published

2020

234. Development of Second Generation Activity-Based Chemical Probes for Sirtuins.

Author

Curry AM, Barton E, Kang W, Mongeluzi DV, and Cen Y

Subjects

Chemistry Techniques, Synthetic, Diazomethane chemistry, Drug Design, Histone Deacetylase Inhibitors chemistry, Histone Deacetylase Inhibitors pharmacology, Humans, Isoenzymes, Ligands, Molecular Structure, NAD metabolism, Sirtuins antagonists & inhibitors, Sirtuins metabolism, Staining and Labeling, Structure-Activity Relationship, Drug Discovery methods, Molecular Probes chemistry, Sirtuins chemistry

Abstract

NAD + (nicotinamide adenine dinucleotide)-dependent protein deacylases, namely, the sirtuins, are important cell adaptor proteins that alter cell physiology in response to low calorie conditions. They are thought to mediate the beneficial effects of calorie restriction to extend longevity and improve health profiles. Novel chemical probes are highly desired for a better understanding of sirtuin's roles in various biological processes. We developed a group of remarkably simple activity-based chemical probes for the investigation of active sirtuin content in complex native proteomes. These probes harbor a thioacyllysine warhead, a diazirine photoaffinity tag, as well as a terminal alkyne bioorthogonal functional group. Compared to their benzophenone-containing counterparts, these new probes demonstrated improved labeling efficiency and sensitivity, shortened irradiation time, and reduced background signal. They were applied to the labeling of individual recombinant proteins, protein mixtures, and whole cell lysate. These cell permeable small molecule probes also enabled the cellular imaging of sirtuin activity change. Taken together, our study provides new chemical biology tools and future drug discovery strategies for perturbing the activity of different sirtuin isoforms.

Published

2020

235. Reactivity-Based Screening for Citrulline-Containing Natural Products Reveals a Family of Bacterial Peptidyl Arginine Deiminases.

Author

Harris LA, Saint-Vincent PMB, Guo X, Hudson GA, DiCaprio AJ, Zhu L, and Mitchell DA

Subjects

Molecular Probes chemistry, Phenylglyoxal chemistry, Phylogeny, Protein Processing, Post-Translational, Protein-Arginine Deiminases classification, Reproducibility of Results, Bacteria enzymology, Biological Products chemistry, Citrulline analysis, Protein-Arginine Deiminases metabolism

Abstract

Ribosomally synthesized and post-translationally modified peptides (RiPPs) are a family of natural products defined by a genetically encoded precursor peptide that is processed by associated biosynthetic enzymes to form the mature product. Lasso peptides are a class of RiPP defined by an isopeptide linkage between the N-terminal amine and an internal Asp/Glu residue with the C-terminal sequence threaded through the macrocycle. This unique lariat topology, which typically provides considerable stability toward heat and proteases, has stimulated interest in lasso peptides as potential therapeutics. Post-translational modifications beyond the class-defining, threaded macrolactam have been reported, including one example of Arg deimination to yield citrulline (Cit). Although a Cit-containing lasso peptide (i.e., citrulassin) was serendipitously discovered during a genome-guided campaign, the gene(s) responsible for Arg deimination has remained unknown. Herein, we describe the use of reactivity-based screening to discriminate bacterial strains that produce Arg- versus Cit-bearing citrulassins, yielding 13 new lasso peptide variants. Partial phylogenetic profiling identified a distally encoded peptidyl arginine deiminase (PAD) gene ubiquitous to the Cit-containing variants. Absence of this gene correlated strongly with lasso peptide variants only containing Arg (i.e., des -citrulassin). Heterologous expression of the PAD gene in a des -citrulassin producer resulted in the production of the deiminated analog, confirming PAD involvement in Arg deimination. The PADs were then bioinformatically surveyed to provide a deeper understanding of their taxonomic distribution and genomic contexts and to facilitate future studies that will evaluate any additional biochemical roles for the superfamily.

Published

2020

236. Special issue preface.

Author

Schultz PG

Subjects

Cellular Reprogramming, Combinatorial Chemistry Techniques, Drug Design, Molecular Probes chemistry, Molecular Probes metabolism, Nucleic Acids chemistry, Nucleic Acids metabolism, Proteins chemistry, Proteins metabolism, Computational Biology

Published

2020

237. Driving integrative structural modeling with serial capture affinity purification.

Author

Liu X, Zhang Y, Wen Z, Hao Y, Banks CAS, Lange JJ, Slaughter BD, Unruh JR, Florens L, Abmayr SM, Workman JL, and Washburn MP

Subjects

Cell Cycle Proteins genetics, Cell Cycle Proteins isolation & purification, Cell Cycle Proteins metabolism, Co-Repressor Proteins genetics, Co-Repressor Proteins isolation & purification, Co-Repressor Proteins metabolism, Feasibility Studies, Fluorescent Dyes chemistry, HEK293 Cells, Humans, Intravital Microscopy, Microtubule-Associated Proteins genetics, Microtubule-Associated Proteins isolation & purification, Microtubule-Associated Proteins metabolism, Molecular Imaging methods, Molecular Probes chemistry, Phosphoproteins genetics, Phosphoproteins isolation & purification, Phosphoproteins metabolism, Protein Binding, Recombinant Proteins genetics, Recombinant Proteins isolation & purification, Recombinant Proteins metabolism, Chromatography, Affinity methods, Mass Spectrometry methods, Models, Molecular

Abstract

Streamlined characterization of protein complexes remains a challenge for the study of protein interaction networks. Here we describe serial capture affinity purification (SCAP), in which two separate proteins are tagged with either the HaloTag or the SNAP-tag, permitting a multistep affinity enrichment of specific protein complexes. The multifunctional capabilities of this protein-tagging system also permit in vivo validation of interactions using acceptor photobleaching Förster resonance energy transfer and fluorescence cross-correlation spectroscopy quantitative imaging. By coupling SCAP to cross-linking mass spectrometry, an integrative structural model of the complex of interest can be generated. We demonstrate this approach using the Spindlin1 and SPINDOC protein complex, culminating in a structural model with two SPINDOC molecules docked on one SPIN1 molecule. In this model, SPINDOC interacts with the SPIN1 interface previously shown to bind a lysine and arginine methylated sequence of histone H3. Our approach combines serial affinity purification, live cell imaging, and cross-linking mass spectrometry to build integrative structural models of protein complexes., Competing Interests: The authors declare no competing interest., (Copyright © 2020 the Author(s). Published by PNAS.)

Published

2020

238. pH/Reduction Dual Stimuli-Triggered Self-Assembly of NIR Theranostic Probes for Enhanced Dual-Modal Imaging and Photothermal Therapy of Tumors.

Author

Wang A, Mao Q, Zhao M, Ye S, Fang J, Cui C, Zhao Y, Zhang Y, Zhang Y, Zhou F, and Shi H

Subjects

Animals, Cell Line, Tumor, Glutathione metabolism, Humans, Hydrogen-Ion Concentration, Mice, Molecular Probes chemistry, Photoacoustic Techniques, Tumor Microenvironment, Diagnostic Imaging methods, Infrared Rays, Molecular Probes metabolism, Photothermal Therapy methods

Abstract

Tumor microenvironment plays a pivotal role in the growth and metastasis of tumors, and has become a promising target for precise diagnosis and treatment of tumors. Herein, a novel smart NIR theranostic probe Cy-1 that can simultaneously respond to low intracellular pH and reductive glutathione (GSH) is reported. This probe has demonstrated to be able to intermolecularly undergo a biologically compatible CBT-Cys condensation reaction to selectively form large nanoaggregates in the tumor microenvironment resulting in its enhanced accumulation and retention in the tumor, which as a consequence significantly improves the sensitivity of NIR/photoacoustic imaging and photothermal therapeutic efficacy of tumors in living mice. We thus believe that this dual stimuli-mediated self-assembly strategy may offer a promising and universal platform for cancer theranostics.

Published

2020

239. Quantitative photoconversion analysis of internal molecular dynamics in stress granules and other membraneless organelles in live cells.

Author

Amen T and Kaganovich D

Subjects

Benzothiazoles chemistry, Biomolecular Condensates metabolism, Biomolecular Condensates physiology, HEK293 Cells, Humans, Molecular Dynamics Simulation, Molecular Probes chemistry, Molecular Probes genetics, Organelles metabolism, Proteins metabolism, Stress Granules physiology, Molecular Probe Techniques instrumentation, Optical Imaging methods, Stress Granules metabolism

Abstract

Photoconversion enables real-time labeling of protein sub-populations inside living cells, which can then be tracked with submicrometer resolution. Here, we detail the protocol of comparing protein dynamics inside membraneless organelles in live HEK293T cells using a CRISPR-Cas9 PABPC1-Dendra2 marker of stress granules. Measuring internal dynamics of membraneless organelles provides insight into their functional state, physical properties, and composition. Photoconversion has the advantage over other imaging techniques in that it is less phototoxic and allows for dual color tracking of proteins. For complete details on the use and execution of this protocol, please refer to Amen and Kaganovich (2020)., Competing Interests: The authors declare no competing interests., (© 2020 The Author(s).)

Published

2020

240. Multicolor Activatable Raman Probes for Simultaneous Detection of Plural Enzyme Activities.

Author

Fujioka H, Shou J, Kojima R, Urano Y, Ozeki Y, and Kamiya M

Subjects

Aminopeptidases chemistry, Cell Line, Tumor, Glycoside Hydrolases chemistry, Humans, Isotope Labeling, Microscopy, Fluorescence, Nitriles chemistry, Substrate Specificity, Aminopeptidases metabolism, Glycoside Hydrolases metabolism, Molecular Probes chemistry, Spectrum Analysis, Raman methods

Abstract

Raman probes based on alkyne or nitrile tags hold promise for highly multiplexed imaging. However, sensing of enzyme activities with Raman probes is difficult because few mechanisms are available to modulate the vibrational response. Here we present a general strategy to prepare activatable Raman probes that show enhanced Raman signals due to electronic preresonance (EPR) upon reaction with enzymes under physiological conditions. We identified a xanthene derivative bearing a nitrile group at position 9 (9CN-JCP) as a suitable scaffold dye, and synthesized four types of activatable Raman probes, which are targeted to different enzymes (three aminopeptidases and a glycosidase) and tuned to different vibrational frequencies by isotope editing of the nitrile group. We validated the activation of the Raman signals of these probes by the target enzymes and succeeded in simultaneous imaging of the four enzyme activities in live cells. Different cell lines showed different patterns of these enzyme activities.

Published

2020

241. A dual-labeling probe to track functional mitochondria-lysosome interactions in live cells.

Author

Chen Q, Fang H, Shao X, Tian Z, Geng S, Zhang Y, Fan H, Xiang P, Zhang J, Tian X, Zhang K, He W, Guo Z, and Diao J

Subjects

Fluorescence Recovery After Photobleaching methods, Fluorescent Dyes chemistry, HeLa Cells, Humans, Lysosomes chemistry, Microscopy, Fluorescence methods, Mitochondria chemistry, Molecular Probe Techniques, Photobleaching, Intravital Microscopy methods, Lysosomes metabolism, Mitochondria metabolism, Mitophagy, Molecular Probes chemistry

Abstract

Mitochondria-lysosome interactions are essential for maintaining intracellular homeostasis. Although various fluorescent probes have been developed to visualize such interactions, they remain unable to label mitochondria and lysosomes simultaneously and dynamically track their interaction. Here, we introduce a cell-permeable, biocompatible, viscosity-responsive, small organic molecular probe, Coupa, to monitor the interaction of mitochondria and lysosomes in living cells. Through a functional fluorescence conversion, Coupa can simultaneously label mitochondria with blue fluorescence and lysosomes with red fluorescence, and the correlation between the red-blue fluorescence intensity indicates the progress of mitochondria-lysosome interplay during mitophagy. Moreover, because its fluorescence is sensitive to viscosity, Coupa allowed us to precisely localize sites of mitochondria-lysosome contact and reveal increases in local viscosity on mitochondria associated with mitochondria-lysosome contact. Thus, our probe represents an attractive tool for the localization and dynamic tracking of functional mitochondria-lysosome interactions in living cells.

Published

2020

242. In vivo O 2 imaging in hepatic tissues by phosphorescence lifetime imaging microscopy using Ir(III) complexes as intracellular probes.

Author

Mizukami K, Katano A, Shiozaki S, Yoshihara T, Goda N, and Tobita S

Subjects

Animals, HT29 Cells, HeLa Cells, Humans, Male, Mice, Inbred BALB C, Spheroids, Cellular metabolism, Intracellular Space metabolism, Iridium chemistry, Liver metabolism, Luminescence, Microscopy, Confocal, Molecular Probes chemistry, Optical Imaging, Oxygen metabolism

Abstract

Phosphorescence lifetime imaging microscopy (PLIM) combined with an oxygen (O 2 )-sensitive luminescent probe allows for high-resolution O 2 imaging of living tissues. Herein, we present phosphorescent Ir(III) complexes, (btp) 2 Ir(acac-DM) (Ir-1) and (btp-OH) 3 Ir (Ir-2), as useful O 2 probes for PLIM measurement. These small-molecule probes were efficiently taken up into cultured cells and accumulated in specific organelles. Their excellent cell-permeable properties allowed for efficient staining of three-dimensional cell spheroids, and thereby phosphorescence lifetime measurements enabled the evaluation of the O 2 level and distribution in spheroids, including the detection of alterations in O 2 levels by metabolic stimulation with an effector. We took PLIM images of hepatic tissues of living mice by intravenously administrating these probes. The PLIM images clearly visualized the O 2 gradient in hepatic lobules with cellular-level resolution, and the O 2 levels were derived based on calibration using cultured cells; the phosphorescence lifetime of Ir-1 gave reasonable O 2 levels, whereas Ir-2 exhibited much lower O 2 levels. Intravenous administration of NH 4 Cl to mice caused the hepatic tissues to experience hypoxia, presumably due to O 2 consumption to produce ATP required for ammonia detoxification, suggesting that the metabolism of the probe molecule might affect liver O 2 levels.

Published

2020

243. Synthesis of [ 18 F]F-γ-T-3, a Redox-Silent γ-Tocotrienol (γ-T-3) Vitamin E Analogue for Image-Based In Vivo Studies of Vitamin E Biodistribution and Dynamics.

Author

Roselt P, Cullinane C, Noonan W, Elsaidi H, Eu P, and Wiebe LI

Subjects

Animals, Antioxidants chemistry, Antioxidants pharmacokinetics, Cell Line, Tumor, Female, Fluorides pharmacokinetics, Fluorine Radioisotopes pharmacokinetics, Humans, Isotope Labeling methods, Mice, Mice, Inbred BALB C, Mice, Nude, Molecular Probes chemistry, Molecular Probes pharmacokinetics, Oxidation-Reduction, Positron-Emission Tomography methods, Radiochemistry methods, Radiopharmaceuticals metabolism, gamma-Tocopherol chemistry, gamma-Tocopherol pharmacokinetics, Fluorides chemistry, Fluorine Radioisotopes chemistry, Tissue Distribution physiology, Tocotrienols chemistry, Tocotrienols pharmacokinetics, Vitamin E chemistry, Vitamin E pharmacokinetics

Abstract

Vitamin E, a natural antioxidant, is of interest to scientists, health care pundits and faddists; its nutritional and biomedical attributes may be validated, anecdotal or fantasy. Vitamin E is a mixture of tocopherols (TPs) and tocotrienols (T-3s), each class having four substitutional isomers (α-, β-, γ-, δ-). Vitamin E analogues attain only low concentrations in most tissues, necessitating exacting invasive techniques for analytical research. Quantitative positron emission tomography (PET) with an F-18-labeled molecular probe would expedite access to Vitamin E's biodistributions and pharmacokinetics via non-invasive temporal imaging. ( R )-6-(3-[ 18 F]Fluoropropoxy)-2,7,8-trimethyl-2-(4,8,12-trimethyltrideca-3,7,11-trien-1-yl)-chromane ([ 18 F]F-γ-T-3) was prepared for this purpose. [ 18 F]F-γ-T-3 was synthesized from γ-T-3 in two steps: (i) 1,3-di- O -tosylpropane was introduced at C6-O to form TsO-γ-T-3, and (ii) reaction of this tosylate with [ 18 F]fluoride in DMF/K 222 . Non-radioactive F-γ-T-3 was synthesized by reaction of γ-T-3 with 3-fluoropropyl methanesulfonate. [ 18 F]F-γ-T-3 biodistribution in a murine tumor model was imaged using a small-animal PET scanner. F-γ-T-3 was prepared in 61% chemical yield. [ 18 F]F-γ-T-3 was synthesized in acceptable radiochemical yield (RCY 12%) with high radiochemical purity (>99% RCP) in 45 min. Preliminary F-18 PET images in mice showed upper abdominal accumulation with evidence of renal clearance, only low concentrations in the thorax (lung/heart) and head, and rapid clearance from blood. [ 18 F]F-γ-T-3 shows promise as an F-18 PET tracer for detailed in vivo studies of Vitamin E. The labeling procedure provides acceptable RCY, high RCP and pertinence to all eight Vitamin E analogues.

Published

2020

244. A New Molecular Probe for Colorimetric and Fluorometric Detection and Removal of Hg 2+ and its Application as Agarose Film-Based Sensor for On-Site Monitoring.

Author

Bhatt S, Vyas G, and Paul P

Subjects

Colorimetry, Fluorometry, Limit of Detection, Mercury chemistry, Chemistry Techniques, Analytical instrumentation, Mercury analysis, Mercury isolation & purification, Molecular Probes chemistry, Sepharose chemistry

Abstract

A new molecule incorporating two units of 7-nitro-benzoxadiazole (NBD), bridged by m-xylylenediamine, was synthesized and characterized on the basis of analytical and spectroscopic techniques. The metal ion sensing property of this molecule was studied spectroscopically with a large number of metal ions. This study revealed that it can perform as a dual-channel probe for colorimetric as well as fluorometric detection of Hg 2+ . In presence of Hg 2+ , a substantial change in UV-Vis spectrum with the appearance of a new band at 545 nm and a distinct colour change from yellow to red was observed. In the fluorescence spectrum, the intensity of the emission band was substantially quenched only upon addition of Hg 2+ . No significant interference from any other metal ion used in this study was noted, the limit of detection (LOD) for Hg 2+ was found to be 60 and 10 nM for colorimetric and fluorometric detection method, respectively. This new chemosensor was used for removal of Hg 2+ from aqueous solution with 92% efficiency. For on-site monitoring and field application, this molecule was immobilized into the agarose based hydrogel film, which was used successfully for detection of Hg 2+ in water. The study on reversible behaviour of this chemosensor revealed that it can be recycled in solution as well as in solid phase by treatment with Na 2 S.

Published

2020

245. Peptidyl Acyloxymethyl Ketones as Activity-Based Probes for the Main Protease of SARS-CoV-2*.

Author

van de Plassche MAT, Barniol-Xicota M, and Verhelst SHL

Subjects

Binding Sites, COVID-19 diagnosis, COVID-19 virology, Catalytic Domain, Coronavirus M Proteins metabolism, Humans, Ketones metabolism, Kinetics, Molecular Docking Simulation, Molecular Probes metabolism, Peptides chemistry, SARS-CoV-2 isolation & purification, Coronavirus M Proteins chemistry, Ketones chemistry, Molecular Probes chemistry, SARS-CoV-2 enzymology

Abstract

The global pandemic caused by SARS-CoV-2 calls for the fast development of antiviral drugs against this particular coronavirus. Chemical tools to facilitate inhibitor discovery as well as detection of target engagement by hit or lead compounds from high-throughput screens are therefore in urgent need. We here report novel, selective activity-based probes that enable detection of the SARS-CoV-2 main protease. The probes are based on acyloxymethyl ketone reactive electrophiles combined with a peptide sequence including unnatural amino acids that targets the nonprimed site of the main protease substrate binding cleft. They are the first activity-based probes for the main protease of coronaviruses and display target labeling within a human proteome without background. We expect that these reagents will be useful in the drug-development pipeline, not only for the current SARS-CoV-2, but also for other coronaviruses., (© 2020 Wiley-VCH GmbH.)

Published

2020

246. Discovery of Electrophiles and Profiling of Enzyme Cofactors.

Author

Dettling SE, Ahmadi M, Lin Z, He L, and Matthews ML

Subjects

Click Chemistry, Coenzymes metabolism, Humans, Molecular Probes chemistry, Protein Processing, Post-Translational, Coenzymes analysis, Proteomics

Abstract

Reverse-polarity activity-based protein profiling (RP-ABPP) is a chemical proteomics approach that uses nucleophilic probes amenable to "click" chemistry deployed into living cells in culture to capture, immunoprecipitate, and identify protein-bound electrophiles. RP-ABPP is used to characterize the structure and function of reactive electrophilic post-translational modifications (PTMs) and the proteins harboring them, which may uncover unknown or novel functions. RP-ABPP has demonstrated utility as a versatile method to monitor the metabolic regulation of electrophilic cofactors, using a pyruvoyl cofactor in S-adenosyl-L-methionine decarboxylase (AMD1), and to discover novel types of electrophilic modifications on proteins in human cells, such as the glyoxylyl modification on secernin-3 (SCRN3). These cofactors cannot be predicted by sequence, and therefore this area is relatively undeveloped. RP-ABPP is the only global, unbiased approach to discover such electrophiles. Here, we describe the utility of these experiments and provide a detailed protocol for de novo discovery, quantitation, and global profiling of electrophilic functionality of proteins. © 2020 The Authors. Basic Protocol 1: Identification and quantification of probe-reactive proteins Basic Protocol 2: Characterization of the site of probe labeling Basic Protocol 3: Determination and quantitation of electrophile structure., (© 2020 The Authors.)

Published

2020

247. Quantifying the dynamics of IRES and cap translation with single-molecule resolution in live cells.

Author

Koch A, Aguilera L, Morisaki T, Munsky B, and Stasevich TJ

Subjects

Base Pairing, Biosensing Techniques, Cell Line, Tumor, Encephalomyocarditis virus metabolism, Epithelial Cells virology, Epitopes chemistry, Epitopes genetics, Epitopes metabolism, Host-Pathogen Interactions genetics, Humans, Inverted Repeat Sequences, Jumonji Domain-Containing Histone Demethylases genetics, Jumonji Domain-Containing Histone Demethylases metabolism, Kinesins genetics, Kinesins metabolism, Molecular Probes chemistry, Molecular Probes metabolism, Nuclear Proteins genetics, Nuclear Proteins metabolism, Nucleic Acid Conformation, Open Reading Frames, RNA Caps chemistry, RNA Caps metabolism, Repressor Proteins genetics, Repressor Proteins metabolism, Ribosomes genetics, Ribosomes metabolism, Single Molecule Imaging methods, Encephalomyocarditis virus genetics, Epithelial Cells metabolism, Internal Ribosome Entry Sites, Protein Biosynthesis, RNA Caps genetics

Abstract

Viruses use internal ribosome entry sites (IRES) to hijack host ribosomes and promote cap-independent translation. Although they are well-studied in bulk, the dynamics of IRES-mediated translation remain unexplored at the single-molecule level. Here, we developed a bicistronic biosensor encoding distinct repeat epitopes in two open reading frames (ORFs), one translated from the 5' cap, and the other from the encephalomyocarditis virus IRES. When combined with a pair of complementary probes that bind the epitopes cotranslationally, the biosensor lights up in different colors depending on which ORF is translated. Using the sensor together with single-molecule tracking and computational modeling, we measured the kinetics of cap-dependent versus IRES-mediated translation in living human cells. We show that bursts of IRES translation are shorter and rarer than bursts of cap translation, although the situation reverses upon stress. Collectively, our data support a model for translational regulation primarily driven by transitions between translationally active and inactive RNA states.

Published

2020

248. PAQMAN: Protein-nucleic acid affinity quantification by MAss spectrometry in nuclear extracts.

Author

Gräwe C, Makowski MM, and Vermeulen M

Subjects

Amino Acid Sequence, Cell Line, Tumor, Cell Nucleus metabolism, Chromatography, Affinity methods, DNA chemistry, DNA isolation & purification, DNA metabolism, Humans, Isotope Labeling, Molecular Probe Techniques, Molecular Probes chemistry, Molecular Probes metabolism, Oligonucleotide Probes chemistry, Oligonucleotide Probes metabolism, Polymorphism, Single Nucleotide, Telomerase analysis, Telomerase genetics, Telomerase isolation & purification, Telomerase metabolism, High-Throughput Screening Assays methods, Mass Spectrometry methods

Abstract

In recent years, various mass spectrometry-based approaches have been developed to determine global protein-DNA binding specificities using DNA affinity purifications from crude nuclear extracts. However, these assays are semi-quantitative and do not provide information about interaction affinities. We recently developed a technology that we call Protein-nucleic acid Affinity Quantification by MAss spectrometry in Nuclear extracts or PAQMAN, that can be used to determine apparent affinities between multiple nuclear proteins and a nucleic acid sequence of interest in one experiment. In PAQMAN, a series of affinity purifications with increasing bait concentrations and fixed amounts of crude nuclear extracts are combined with isobaric stable isotope labeling and quantitative mass spectrometry to generate Hill-like K d curves for dozens of proteins in a single experiment. Here, we apply PAQMAN to determine apparent affinities for a genetic variant, rs36115365-C, which regulates TERT expression and is associated with an increased risk to develop various malignancies. Furthermore, we describe a detailed protocol for this method including important quality checks., (Copyright © 2019 Elsevier Inc. All rights reserved.)

Published

2020

249. Evaluation of an antibody-PNA conjugate as a clearing agent for antibody-based PNA-mediated radionuclide pretargeting.

Author

Myrhammar A, Vorobyeva A, Westerlund K, Yoneoka S, Orlova A, Tsukahara T, Tolmachev V, Karlström AE, and Altai M

Subjects

Animals, Antibodies, Neoplasm metabolism, Cell Line, Tumor, Cetuximab administration & dosage, Cetuximab blood, Cetuximab chemistry, Female, Humans, Immunoconjugates pharmacokinetics, Mice, Molecular Probes administration & dosage, Molecular Probes chemistry, Molecular Probes pharmacokinetics, Molecular Targeted Therapy methods, Peptide Nucleic Acids pharmacokinetics, Receptor, ErbB-2 antagonists & inhibitors, Receptor, ErbB-2 immunology, Tissue Distribution, Trastuzumab administration & dosage, Trastuzumab blood, Trastuzumab chemistry, Antibodies, Neoplasm administration & dosage, Antibodies, Neoplasm chemistry, Immunoconjugates administration & dosage, Immunoconjugates chemistry, Peptide Nucleic Acids administration & dosage, Peptide Nucleic Acids chemistry, Radioimmunotherapy methods

Abstract

Radionuclide molecular imaging of cancer-specific targets is a promising method to identify patients for targeted antibody therapy. Radiolabeled full-length antibodies however suffer from slow clearance, resulting in high background radiation. To overcome this problem, a pretargeting system based on complementary peptide nucleic acid (PNA) probes has been investigated. The pretargeting relies on sequential injections of primary, PNA-tagged antibody and secondary, radiolabeled PNA probe, which are separated in time, to allow for clearance of non-bound primary agent. We now suggest to include a clearing agent (CA), designed for removal of primary tumor-targeting agent from the blood. The CA is based on the antibody cetuximab, which was conjugated to PNA and lactosaminated by reductive amination to improve hepatic clearance. The CA was evaluated in combination with PNA-labelled trastuzumab, T-ZHP1, for radionuclide HER2 pretargeting. Biodistribution studies in normal mice demonstrated that the CA cleared ca. 7 times more rapidly from blood than unmodified cetuximab. Injection of the CA 6 h post injection of the radiolabeled primary agent [ 131 I]I-T-ZHP1 gave a moderate reduction of the radioactivity concentration in the blood after 1 h from 8.5 ± 1.8 to 6.0 ± 0.4%ID/g. These proof-of-principle results could guide future development of a more efficient CA.

Published

2020

250. Development of a Squaraine-Based Molecular Probe for Dual-Modal in Vivo Fluorescence and Photoacoustic Imaging.

Author

Park YD, Park JE, Kim HS, Choi SH, Park JE, Jeon J, and Park SH

Subjects

Animals, Heterografts, Humans, Integrin alphaVbeta3 metabolism, Mice, Mice, Inbred BALB C, Neoplasms metabolism, Peptides, Cyclic chemistry, Solubility, Spectroscopy, Near-Infrared methods, Cyclobutanes chemistry, Molecular Probes chemistry, Optical Imaging methods, Phenols chemistry, Photoacoustic Techniques methods

Abstract

Dual-modular imaging approaches combining near-infrared (NIR) fluorescence (FLI) and photoacoustic imaging (PAI) require suitable contrast agents to produce dual-modular signals. Although nanoparticles have been used to develop PAI agents, small molecule-based imaging agents have not been extensively studied, highlighting the need to design new fluorophores with an enhanced multifunctional ability. Thus, in this study, we designed a novel squaraine (SQ)-based dye and reported its rational preparation and conjugation with a cancer targeting peptide. Specifically, benzoindole-derived SQ (BSQ) showed strong absorption and fluorescence properties at above 650 nm under aqueous conditions, with a maximum absorption and emission at 665 and 680 nm, respectively. Moreover, PA signal scanning experiments revealed a maximum signal intensity in the range 680-700 nm. BSQ was also conjugated with cyclic arginine-glycine-aspartic acid (cRGD) to improve its active targeting ability for the α v β 3 integrin, which is overexpressed in various cancer and angiogenic cells. A series of in vitro , in vivo , and ex vivo FLI studies showed that the cRGD conjugated BSQ (BSQ-RGD 2 ) successfully stained and targeted α v β 3 integrin-overexpressing tumor cells and xenografts, which were clearly visualized by FLI and PAI. Therefore, BSQ-RGD 2 can successfully be applied to dual-modular imaging of the specific biomarker in living animals.

Published

2020