Your search keyword '"Miranda, Les P."' showing total 40 results

1. Accelerating attribute-focused process and product development through the development and deployment of autonomous process analytical technology platform system.

Author

Wu CR, Chan B, Sarich Z, Duan Y, Chen J, Song JL, Berke M, Miranda LP, and Goudar CT

Subjects

Quality Control, Technology, Pharmaceutical

Abstract

Enabling real-time monitoring and control of the biomanufacturing processes through product quality insights continues to be an area of focus in the biopharmaceutical industry. The goal is to manufacture products with the desired quality attributes. To realize this rigorous attribute-focused Quality by Design approach, it is critical to support the development of processes that consistently deliver high-quality products and facilitate product commercialization. Time delays associated with offline analytical testing can limit the speed of process development. Thus, developing and deploying analytical technology is necessary to accelerate process development. In this study, we have developed the micro sequential injection process analyzer and the automatic assay preparation platform system. These innovations address the unmet need for an automatic, online, real-time sample acquisition and preparation platform system for in-process monitoring, control, and release of biopharmaceuticals. These systems can also be deployed in laboratory areas as an offline analytical system and on the manufacturing floor to enable rapid testing and release of products manufactured in a good manufacturing practice environment., (© 2024 Wiley Periodicals LLC.)

Published

2024

2. Process development of a SARS-CoV-2 nanoparticle vaccine.

Author

Martinez-Cano D, Ravichandran R, Le H, Wong HE, Jagannathan B, Liu EJ, Bailey W, Yang J, Matthies K, Barkhordarian H, Shah B, Srinivasan N, Zhang J, Hsu A, Wypych J, Stevens J, Piedmonte DM, Miranda LP, Carter L, Murphy M, King NP, and Soice N

Abstract

One of the outcomes from the global COVID-19 pandemic caused by SARS-CoV-2 has been an acceleration of development timelines to provide treatments in a timely manner. For example, it has recently been demonstrated that the development of monoclonal antibody therapeutics from vector construction to IND submission can be achieved in five to six months rather than the traditional ten-to-twelve-month timeline using CHO cells [1], [2]. This timeline is predicated on leveraging existing, robust platforms for upstream and downstream processes, analytical methods, and formulation. These platforms also reduce; the requirement for ancillary studies such as cell line stability, or long-term product stability studies. Timeline duration was further reduced by employing a transient cell line for early material supply and using a stable cell pool to manufacture toxicology study materials. The development of non-antibody biologics utilizing traditional biomanufacturing processes in CHO cells within a similar timeline presents additional challenges, such as the lack of platform processes and additional analytical assay development. In this manuscript, we describe the rapid development of a robust and reproducible process for a two-component self-assembling protein nanoparticle vaccine for SARS-CoV-2. Our work has demonstrated a successful academia-industry partnership model that responded to the COVID-19 global pandemic quickly and efficiently and could improve our preparedness for future pandemic threats., (© 2023 Published by Elsevier Ltd.)

Published

2023

3. Metal-Free Polymer-Based Affinity Medium for Selective Purification of His6-Tagged Proteins.

Author

Yoshimatsu K, Fruehauf KR, Zhu Q, Weisman A, Fan J, Xue M, Beierle JM, Rose PE, Aral J, Epstein LF, Tagari P, Miranda LP, and Shea KJ

Subjects

Chromatography, Affinity, Metals, Proteins, Recombinant Proteins, Escherichia coli genetics, Polymers

Abstract

We report a metal free synthetic hydrogel copolymer with affinity and selectivity for His6-tagged peptides and proteins. Small libraries of copolymers incorporating charged and hydrophobic functional groups were screened by an iterative process for His6 peptide affinity. The monomer selection was guided by interactions found in the crystal structure of an anti-His tag antibody-His6 peptide antigen complex. Synthetic copolymers incorporating a phenylalanine-derived monomer were found to exhibit strong affinity for both His6-containing peptides and proteins. The proximity of both aromatic and negatively charged functional groups were important factors for the His6 affinity of hydrogel copolymers. His6 affinity was not compromised by the presence of enzyme cleavage sequences. The His6-copolymer interactions are pH sensitive: the copolymer selectively captured His6 peptides at pH 7.8 while the interactions were substantially weakened at pH 8.6. This provided mild conditions for releasing His6-tagged proteins from the copolymer. Finally, a synthetic copolymer coated chromatographic medium was prepared and applied to the purification of a His6-tagged protein from an E. coli expression system. The results establish that a synthetic copolymer-based affinity medium can function as an effective alternative to immobilized metal ion columns for the purification of His6-tagged proteins.

Published

2021

4. Discovery of Selective Pituitary Adenylate Cyclase 1 Receptor (PAC1R) Antagonist Peptides Potent in a Maxadilan/PACAP38-Induced Increase in Blood Flow Pharmacodynamic Model.

Author

Hu E, Hong FT, Aral J, Long J, Piper DE, Poppe L, Andrews KL, Hager T, Davis C, Li H, Wong P, Gavva N, Shi L, Zhu DXD, Lehto SG, Xu C, and Miranda LP

Subjects

Animals, Humans, Insect Proteins pharmacology, Male, Mice, Migraine Disorders drug therapy, Migraine Disorders metabolism, Migraine Disorders physiopathology, Molecular Docking Simulation, Peptides pharmacokinetics, Pituitary Adenylate Cyclase-Activating Polypeptide metabolism, Rats, Rats, Sprague-Dawley, Receptors, Pituitary Adenylate Cyclase-Activating Polypeptide, Type I chemistry, Receptors, Pituitary Adenylate Cyclase-Activating Polypeptide, Type I metabolism, Vasodilator Agents pharmacology, Blood Circulation drug effects, Peptides chemistry, Peptides pharmacology, Receptors, Pituitary Adenylate Cyclase-Activating Polypeptide, Type I antagonists & inhibitors

Abstract

Inhibition of the pituitary adenylate cyclase 1 receptor (PAC1R) is a novel mechanism that could be used for abortive treatment of acute migraine. Our research began with comparative analysis of known PAC1R ligand scaffolds, PACAP38 and Maxadilan, which resulted in the selection of des(24-42) Maxadilan, 6 , as a starting point. C-terminal modifications of 6 improved the peptide metabolic stability in vitro and in vivo . SAR investigations identified synergistic combinations of amino acid replacements that significantly increased the in vitro PAC1R inhibitory activity of the analogs to the pM IC 90 range. Our modifications further enabled deletion of up to six residues without impacting potency, thus improving peptide ligand binding efficiency. Analogs 17 and 18 exhibited robust in vivo efficacy in the rat Maxadilan-induced increase in blood flow (MIIBF) pharmacodynamic model at 0.3 mg/kg subcutaneous dosing. The first cocrystal structure of a PAC1R antagonist peptide ( 18 ) with PAC1R extracellular domain is reported.

Published

2021

5. Half-life extension of peptidic APJ agonists by N-terminal lipid conjugation.

Author

Reed AB, Lanman BA, Holder JR, Yang BH, Ma J, Humphreys SC, Wang Z, Chan JCY, Miranda LP, Swaminath G, and Allen JG

Subjects

Animals, Apelin Receptors metabolism, Dose-Response Relationship, Drug, Injections, Intravenous, Lipids administration & dosage, Lipids chemistry, Molecular Structure, Myocardial Infarction metabolism, Peptides administration & dosage, Peptides chemistry, Rats, Structure-Activity Relationship, Apelin Receptors agonists, Lipids pharmacology, Myocardial Infarction drug therapy, Peptides pharmacology

Abstract

Agonism of the endothelial receptor APJ (putative receptor protein related to AT 1 ; AT 1 : angiotensin II receptor type 1) has the potential to ameliorate congestive heart failure by increasing cardiac output without inducing hypertrophy. Although the endogenous agonist, pyr-apelin-13 (1), has shown beneficial APJ-mediated inotropic effects in rats and humans, such effects are short-lived given its extremely short half-life. Here, we report the conjugation of 1 to a fatty acid, providing a lipidated peptide (2) with increased stability that retains inotropic activity in an anesthetized rat myocardial infarction (MI) model. We also report the preparation of a library of 15-mer APJ agonist peptide-lipid conjugates, including adipoyl-γGlu-OEG-OEG-hArg-r-Q-hArg-P-r-NMeLeuSHK-G-Oic-pIPhe-P-DBip-OH (17), a potent APJ agonist with high plasma protein binding and a half-life suitable for once-daily subcutaneous dosing in rats. A correlation between subcutaneous absorption rate and lipid length/type of these conjugates is also reported., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2020 Elsevier Ltd. All rights reserved.)

Published

2020

6. Use of Cryopreserved Hepatocytes as Part of an Integrated Strategy to Characterize In Vivo Clearance for Peptide-Antibody Conjugate Inhibitors of Nav1.7 in Preclinical Species.

Author

Foti RS, Biswas K, Aral J, Be X, Berry L, Cheng Y, Conner K, Falsey JR, Glaus C, Herberich B, Hickman D, Ikotun T, Li H, Long J, Huang L, Miranda LP, Murray J, Moyer B, Netirojjanakul C, Nixey TE, Sham K, Soto M, Tegley CM, Tran L, Wu B, Yin L, and Rock DA

Subjects

Administration, Intravenous, Animals, Antibodies, Monoclonal administration & dosage, Antibodies, Monoclonal pharmacokinetics, Cryopreservation, Drug Evaluation, Preclinical methods, Hepatocytes, Histocompatibility Antigens Class I genetics, Immunoconjugates administration & dosage, Macaca fascicularis, Male, Metabolic Clearance Rate, Mice, Mice, Knockout, Peptides administration & dosage, Peptides pharmacokinetics, Receptors, Fc genetics, Tissue Distribution, Voltage-Gated Sodium Channel Blockers administration & dosage, Chronic Pain drug therapy, Histocompatibility Antigens Class I metabolism, Immunoconjugates pharmacokinetics, NAV1.7 Voltage-Gated Sodium Channel metabolism, Receptors, Fc metabolism, Voltage-Gated Sodium Channel Blockers pharmacokinetics

Abstract

The identification of nonopioid alternatives to treat chronic pain has received a great deal of interest in recent years. Recently, the engineering of a series of Nav1.7 inhibitory peptide-antibody conjugates has been reported, and herein, the preclinical efforts to identify novel approaches to characterize the pharmacokinetic properties of the peptide conjugates are described. A cryopreserved plated mouse hepatocyte assay was designed to measure the depletion of the peptide-antibody conjugates from the media, with a correlation being observed between percentage remaining in the media and in vivo clearance (Pearson r = -0.5525). Physicochemical (charge and hydrophobicity), receptor-binding [neonatal Fc receptor (FcRn)], and in vivo pharmacokinetic data were generated and compared with the results from our in vitro hepatocyte assay, which was hypothesized to encompass all of the aforementioned properties. Correlations were observed among hydrophobicity; FcRn binding; depletion rates from the hepatocyte assay; and ultimately, in vivo clearance. Subsequent studies identified potential roles for the low-density lipoprotein and mannose/galactose receptors in the association of the Nav1.7 peptide conjugates with mouse hepatocytes, although in vivo studies suggested that FcRn was still the primary receptor involved in determining the pharmacokinetics of the peptide conjugates. Ultimately, the use of the cryopreserved hepatocyte assay along with FcRn binding and hydrophobic interaction chromatography provided an efficient and integrated approach to rapidly triage molecules for advancement while reducing the number of in vivo pharmacokinetic studies. SIGNIFICANCE STATEMENT: Although multiple in vitro and in silico tools are available in small-molecule drug discovery, pharmacokinetic characterization of protein therapeutics is still highly dependent upon the use of in vivo studies in preclinical species. The current work demonstrates the combined use of cryopreserved hepatocytes, hydrophobic interaction chromatography, and neonatal Fc receptor binding to characterize a series of Nav1.7 peptide-antibody conjugates prior to conducting in vivo studies, thus providing a means to rapidly evaluate novel protein therapeutic platforms while concomitantly reducing the number of in vivo studies conducted in preclinical species., (Copyright © 2019 by The American Society for Pharmacology and Experimental Therapeutics.)

Published

2019

7. Nanoscale integration of single cell biologics discovery processes using optofluidic manipulation and monitoring.

Author

Jorgolli M, Nevill T, Winters A, Chen I, Chong S, Lin FF, Mock M, Chen C, Le K, Tan C, Jess P, Xu H, Hamburger A, Stevens J, Munro T, Wu M, Tagari P, and Miranda LP

Subjects

Humans, Automation, Biological Products, Drug Discovery, Lab-On-A-Chip Devices

Abstract

The new and rapid advancement in the complexity of biologics drug discovery has been driven by a deeper understanding of biological systems combined with innovative new therapeutic modalities, paving the way to breakthrough therapies for previously intractable diseases. These exciting times in biomedical innovation require the development of novel technologies to facilitate the sophisticated, multifaceted, high-paced workflows necessary to support modern large molecule drug discovery. A high-level aspiration is a true integration of "lab-on-a-chip" methods that vastly miniaturize cellulmical experiments could transform the speed, cost, and success of multiple workstreams in biologics development. Several microscale bioprocess technologies have been established that incrementally address these needs, yet each is inflexibly designed for a very specific process thus limiting an integrated holistic application. A more fully integrated nanoscale approach that incorporates manipulation, culture, analytics, and traceable digital record keeping of thousands of single cells in a relevant nanoenvironment would be a transformative technology capable of keeping pace with today's rapid and complex drug discovery demands. The recent advent of optical manipulation of cells using light-induced electrokinetics with micro- and nanoscale cell culture is poised to revolutionize both fundamental and applied biological research. In this review, we summarize the current state of the art for optical manipulation techniques and discuss emerging biological applications of this technology. In particular, we focus on promising prospects for drug discovery workflows, including antibody discovery, bioassay development, antibody engineering, and cell line development, which are enabled by the automation and industrialization of an integrated optoelectronic single-cell manipulation and culture platform. Continued development of such platforms will be well positioned to overcome many of the challenges currently associated with fragmented, low-throughput bioprocess workflows in biopharma and life science research., (© 2019 The Authors. Biotechnology and Bioengineering Published by Wiley Periodicals, Inc.)

Published

2019

8. Engineering Na V 1.7 Inhibitory JzTx-V Peptides with a Potency and Basicity Profile Suitable for Antibody Conjugation To Enhance Pharmacokinetics.

Author

Murray JK, Wu B, Tegley CM, Nixey TE, Falsey JR, Herberich B, Yin L, Sham K, Long J, Aral J, Cheng Y, Netirojjanakul C, Doherty L, Glaus C, Ikotun T, Li H, Tran L, Soto M, Salimi-Moosavi H, Ligutti J, Amagasu S, Andrews KL, Be X, Lin MJ, Foti RS, Ilch CP, Youngblood B, Kornecook TJ, Karow M, Walker KW, Moyer BD, Biswas K, and Miranda LP

Subjects

Animals, Antibodies chemistry, Drug Discovery, Humans, Male, Mice, Molecular Targeted Therapy, NAV1.7 Voltage-Gated Sodium Channel immunology, Peptides pharmacokinetics, Spider Venoms pharmacokinetics, Immunoconjugates chemistry, Immunoconjugates pharmacokinetics, NAV1.7 Voltage-Gated Sodium Channel metabolism, Peptides chemistry, Spider Venoms chemistry, Voltage-Gated Sodium Channel Blockers chemistry, Voltage-Gated Sodium Channel Blockers pharmacokinetics

Abstract

Drug discovery research on new pain targets with human genetic validation, including the voltage-gated sodium channel Na V 1.7, is being pursued to address the unmet medical need with respect to chronic pain and the rising opioid epidemic. As part of early research efforts on this front, we have previously developed Na V 1.7 inhibitory peptide-antibody conjugates with tarantula venom-derived GpTx-1 toxin peptides with an extended half-life (80 h) in rodents but only moderate in vitro activity (hNa V 1.7 IC 50 = 250 nM) and without in vivo activity. We identified the more potent peptide JzTx-V from our natural peptide collection and improved its selectivity against other sodium channel isoforms through positional analogueing. Here we report utilization of the JzTx-V scaffold in a peptide-antibody conjugate and architectural variations in the linker, peptide loading, and antibody attachment site. We found conjugates with 100-fold improved in vitro potency relative to those of complementary GpTx-1 analogues, but pharmacokinetic and bioimaging analyses of these JzTx-V conjugates revealed a shorter than expected plasma half-life in vivo with accumulation in the liver. In an attempt to increase circulatory serum levels, we sought the reduction of the net +6 charge of the JzTx-V scaffold while retaining a desirable Na V in vitro activity profile. The conjugate of a JzTx-V peptide analogue with a +2 formal charge maintained Na V 1.7 potency with 18-fold improved plasma exposure in rodents. Balancing the loss of peptide and conjugate potency associated with the reduction of net charge necessary for improved target exposure resulted in a compound with moderate activity in a Na V 1.7-dependent pharmacodynamic model but requires further optimization to identify a conjugate that can fully engage Na V 1.7 in vivo.

Published

2019

9. Peptide-Membrane Interactions Affect the Inhibitory Potency and Selectivity of Spider Toxins ProTx-II and GpTx-1.

Author

Lawrence N, Wu B, Ligutti J, Cheneval O, Agwa AJ, Benfield AH, Biswas K, Craik DJ, Miranda LP, Henriques ST, and Schroeder CI

Subjects

Animals, Humans, Peptides chemistry, Peptides drug effects, Spider Venoms pharmacology

Abstract

Gating modifier toxins (GMTs) from spider venom can inhibit voltage gated sodium channels (Na V s) involved in pain signal transmission, including the Na V 1.7 subtype. GMTs have a conserved amphipathic structure that allow them to interact with membranes and also with charged residues in regions of Na V that are exposed at the cell surface. ProTx-II and GpTx-1 are GMTs able to inhibit Na V 1.7 with high potency, but they differ in their ability to bind to membranes and in their selectivity over other Na V subtypes. To explore these differences and gain detailed information on their membrane-binding ability and how this relates to potency and selectivity, we examined previously described Na V 1.7 potent/selective GpTx-1 analogues and new ProTx-II analogues designed to reduce membrane binding and improve selectivity for Na V 1.7. Our studies reveal that the number and type of hydrophobic residues as well as how they are presented at the surface determine the affinity of ProTx-II and GpTx-1 for membranes and that altering these residues can have dramatic effects on Na V inhibitory activity. We demonstrate that strong peptide-membrane interactions are not essential for inhibiting Na V 1.7 and propose that hydrophobic interactions instead play an important role in positioning the GMT at the membrane surface proximal to exposed Na V residues, thereby affecting peptide-channel interactions. Our detailed structure-activity relationship study highlights the challenges of designing GMT-based molecules that simultaneously achieve high potency and selectivity for Na V 1.7, as single mutations can induce local changes in GMT structure that can have a major impact on Na V -inhibitory activity.

Published

2019

10. Discovery of Tarantula Venom-Derived Na V 1.7-Inhibitory JzTx-V Peptide 5-Br-Trp24 Analogue AM-6120 with Systemic Block of Histamine-Induced Pruritis.

Author

Wu B, Murray JK, Andrews KL, Sham K, Long J, Aral J, Ligutti J, Amagasu S, Liu D, Zou A, Min X, Wang Z, Ilch CP, Kornecook TJ, Lin MJ, Be X, Miranda LP, Moyer BD, and Biswas K

Subjects

Animals, HEK293 Cells, Humans, Mice, Molecular Docking Simulation, NAV1.7 Voltage-Gated Sodium Channel chemistry, Peptides pharmacokinetics, Peptides therapeutic use, Protein Conformation, Protein Folding, Pruritus chemically induced, Structure-Activity Relationship, Tissue Distribution, Voltage-Gated Sodium Channel Blockers chemistry, Voltage-Gated Sodium Channel Blockers pharmacokinetics, Voltage-Gated Sodium Channel Blockers pharmacology, Voltage-Gated Sodium Channel Blockers therapeutic use, Drug Discovery, Histamine adverse effects, NAV1.7 Voltage-Gated Sodium Channel metabolism, Peptides chemistry, Peptides pharmacology, Pruritus drug therapy, Spider Venoms chemistry

Abstract

Inhibitors of the voltage-gated sodium channel Na V 1.7 are being investigated as pain therapeutics due to compelling human genetics. We previously identified Na V 1.7-inhibitory peptides GpTx-1 and JzTx-V from tarantula venom screens. Potency and selectivity were modulated through attribute-based positional scans of native residues via chemical synthesis. Herein, we report JzTx-V lead optimization to identify a pharmacodynamically active peptide variant. Molecular docking of peptide ensembles from NMR into a homology model-derived Na V 1.7 structure supported prioritization of key residues clustered on a hydrophobic face of the disulfide-rich folded peptide for derivatization. Replacing Trp24 with 5-Br-Trp24 identified lead peptides with activity in electrophysiology assays in engineered and neuronal cells. 5-Br-Trp24 containing peptide AM-6120 was characterized in X-ray crystallography and pharmacokinetic studies and blocked histamine-induced pruritis in mice after subcutaneous administration, demonstrating systemic Na V 1.7-dependent pharmacodynamics. Our data suggests a need for high target coverage based on plasma exposure for impacting in vivo end points with selectivity-optimized peptidic Na V 1.7 inhibitors.

Published

2018

11. Structure-guided Discovery of Dual-recognition Chemibodies.

Author

Cheng AC, Doherty EM, Johnstone S, DiMauro EF, Dao J, Luthra A, Ye J, Tang J, Nixey T, Min X, Tagari P, Miranda LP, and Wang Z

Subjects

Animals, Antibodies, Monoclonal chemistry, Catalytic Domain, Crystallography, X-Ray, Drug Design, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Immunoconjugates chemistry, Models, Molecular, Rats, Small Molecule Libraries chemistry, Structure-Activity Relationship, Dipeptidyl Peptidase 4 chemistry, Enzyme Inhibitors chemical synthesis, Immunoconjugates pharmacology

Abstract

Small molecules and antibodies each have advantages and limitations as therapeutics. Here, we present for the first time to our knowledge, the structure-guided design of "chemibodies" as small molecule-antibody hybrids that offer dual recognition of a single target by both a small molecule and an antibody, using DPP-IV enzyme as a proof of concept study. Biochemical characterization demonstrates that the chemibodies present superior DPP-IV inhibition compared to either small molecule or antibody component alone. We validated our design by successfully solving a co-crystal structure of a chemibody in complex with DPP-IV, confirming specific binding of the small molecule portion at the interior catalytic site and the Fab portion at the protein surface. The discovery of chemibodies presents considerable potential for novel therapeutics that harness the power of both small molecule and antibody modalities to achieve superior specificity, potency, and pharmacokinetic properties.

Published

2018

12. Pharmacological characterization of potent and selective NaV1.7 inhibitors engineered from Chilobrachys jingzhao tarantula venom peptide JzTx-V.

Author

Moyer BD, Murray JK, Ligutti J, Andrews K, Favreau P, Jordan JB, Lee JH, Liu D, Long J, Sham K, Shi L, Stöcklin R, Wu B, Yin R, Yu V, Zou A, Biswas K, and Miranda LP

Subjects

Action Potentials drug effects, Amino Acid Substitution, Analgesics pharmacology, Animals, Capsaicin pharmacology, Cell Line, Drug Evaluation, Preclinical, Ganglia, Spinal drug effects, Humans, Male, Mice, Inbred C57BL, Mutagenesis, Site-Directed, Nerve Fibers, Unmyelinated drug effects, Nuclear Magnetic Resonance, Biomolecular, Patch-Clamp Techniques, Physical Stimulation, Protein Engineering, Recombinant Proteins drug effects, Sodium Channel Blockers pharmacology, Structure-Activity Relationship, Tetrodotoxin pharmacology, Analgesics isolation & purification, NAV1.7 Voltage-Gated Sodium Channel drug effects, Peptides chemistry, Sodium Channel Blockers isolation & purification, Spider Venoms chemistry

Abstract

Identification of voltage-gated sodium channel NaV1.7 inhibitors for chronic pain therapeutic development is an area of vigorous pursuit. In an effort to identify more potent leads compared to our previously reported GpTx-1 peptide series, electrophysiology screening of fractionated tarantula venom discovered the NaV1.7 inhibitory peptide JzTx-V from the Chinese earth tiger tarantula Chilobrachys jingzhao. The parent peptide displayed nominal selectivity over the skeletal muscle NaV1.4 channel. Attribute-based positional scan analoging identified a key Ile28Glu mutation that improved NaV1.4 selectivity over 100-fold, and further optimization yielded the potent and selective peptide leads AM-8145 and AM-0422. NMR analyses revealed that the Ile28Glu substitution changed peptide conformation, pointing to a structural rationale for the selectivity gains. AM-8145 and AM-0422 as well as GpTx-1 and HwTx-IV competed for ProTx-II binding in HEK293 cells expressing human NaV1.7, suggesting that these NaV1.7 inhibitory peptides interact with a similar binding site. AM-8145 potently blocked native tetrodotoxin-sensitive (TTX-S) channels in mouse dorsal root ganglia (DRG) neurons, exhibited 30- to 120-fold selectivity over other human TTX-S channels and exhibited over 1,000-fold selectivity over other human tetrodotoxin-resistant (TTX-R) channels. Leveraging NaV1.7-NaV1.5 chimeras containing various voltage-sensor and pore regions, AM-8145 mapped to the second voltage-sensor domain of NaV1.7. AM-0422, but not the inactive peptide analog AM-8374, dose-dependently blocked capsaicin-induced DRG neuron action potential firing using a multi-electrode array readout and mechanically-induced C-fiber spiking in a saphenous skin-nerve preparation. Collectively, AM-8145 and AM-0422 represent potent, new engineered NaV1.7 inhibitory peptides derived from the JzTx-V scaffold with improved NaV selectivity and biological activity in blocking action potential firing in both DRG neurons and C-fibers.

Published

2018

13. Identification of Antibody and Small Molecule Antagonists of Ferroportin-Hepcidin Interaction.

Author

Ross SL, Biswas K, Rottman J, Allen JR, Long J, Miranda LP, Winters A, and Arvedson TL

Abstract

The iron exporter ferroportin and its ligand, the hormone hepcidin, control fluxes of stored and recycled iron for use in a variety of essential biochemical processes. Inflammatory disorders and malignancies are often associated with high hepcidin levels, leading to ferroportin down-regulation, iron sequestration in tissue macrophages and subsequent anemia. The objective of this research was to develop reagents to characterize the expression of ferroportin, the interaction between ferroportin and hepcidin, as well as to identify novel ferroportin antagonists capable of maintaining iron export in the presence of hepcidin. Development of investigative tools that enabled cell-based screening assays is described in detail, including specific and sensitive monoclonal antibodies that detect endogenously-expressed human and mouse ferroportin and fluorescently-labeled chemically-synthesized human hepcidin. Large and small molecule antagonists inhibiting hepcidin-mediated ferroportin internalization were identified, and unique insights into the requirements for interaction between these two key iron homeostasis molecules are provided.

Published

2017

14. Engineering Antibody Reactivity for Efficient Derivatization to Generate Na V 1.7 Inhibitory GpTx-1 Peptide-Antibody Conjugates.

Author

Biswas K, Nixey TE, Murray JK, Falsey JR, Yin L, Liu H, Gingras J, Hall BE, Herberich B, Holder JR, Li H, Ligutti J, Lin MJ, Liu D, Soriano BD, Soto M, Tran L, Tegley CM, Zou A, Gunasekaran K, Moyer BD, Doherty L, and Miranda LP

Subjects

Animals, HEK293 Cells, Humans, Immunoconjugates chemistry, Immunoconjugates pharmacokinetics, Male, Mice, Models, Molecular, Peptides chemistry, Peptides pharmacokinetics, Tissue Distribution, Voltage-Gated Sodium Channel Blockers chemistry, Voltage-Gated Sodium Channel Blockers pharmacokinetics, Immunoconjugates pharmacology, NAV1.7 Voltage-Gated Sodium Channel metabolism, Peptides pharmacology, Voltage-Gated Sodium Channel Blockers pharmacology

Abstract

The voltage-gated sodium channel Na V 1.7 is a genetically validated pain target under investigation for the development of analgesics. A therapeutic with a less frequent dosing regimen would be of value for treating chronic pain; however functional Na V 1.7 targeting antibodies are not known. In this report, we describe Na V 1.7 inhibitory peptide-antibody conjugates as an alternate construct for potential prolonged channel blockade through chemical derivatization of engineered antibodies. We previously identified Na V 1.7 inhibitory peptide GpTx-1 from tarantula venom and optimized its potency and selectivity. Tethering GpTx-1 peptides to antibodies bifunctionally couples FcRn-based antibody recycling attributes to the Na V 1.7 targeting function of the peptide warhead. Herein, we conjugated a GpTx-1 peptide to specific engineered cysteines in a carrier anti-2,4-dinitrophenol monoclonal antibody using polyethylene glycol linkers. The reactivity of 13 potential cysteine conjugation sites in the antibody scaffold was tuned using a model alkylating agent. Subsequent reactions with the peptide identified cysteine locations with the highest conversion to desired conjugates, which blocked Na V 1.7 currents in whole cell electrophysiology. Variations in attachment site, linker, and peptide loading established design parameters for potency optimization. Antibody conjugation led to in vivo half-life extension by 130-fold relative to a nonconjugated GpTx-1 peptide and differential biodistribution to nerve fibers in wild-type but not Na V 1.7 knockout mice. This study describes the optimization and application of antibody derivatization technology to functionally inhibit Na V 1.7 in engineered and neuronal cells.

Published

2017

15. Progress and challenges in the optimization of toxin peptides for development as pain therapeutics.

Author

Netirojjanakul C and Miranda LP

Subjects

Animals, Humans, Peptides therapeutic use, Toxins, Biological therapeutic use, Drug Discovery methods, Pain drug therapy, Peptides pharmacology, Toxins, Biological pharmacology

Abstract

The number of new toxin peptide discoveries has been rapidly growing in the past few decades. Because of progress in proteomics, sequencing technologies, and high throughput bioassays, the search for new toxin peptides from venom collections and potency optimization has become manageable. However, to date, only six toxin peptide-derived therapeutics have been approved by the USFDA, with only one, ziconotide, for a pain indication. The challenge of venom-derived peptide therapeutic development remains in improving selectivity to the target and more importantly, in delivery of these peptides to the sites of action in the central and peripheral nervous system. In this review, we highlight peptide toxins that target major therapeutic targets for pain and discuss the challenges of developing toxin peptides as potential therapeutics., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

16. A Potent d-Protein Antagonist of VEGF-A is Nonimmunogenic, Metabolically Stable, and Longer-Circulating in Vivo.

Author

Uppalapati M, Lee DJ, Mandal K, Li H, Miranda LP, Lowitz J, Kenney J, Adams JJ, Ault-Riché D, Kent SB, and Sidhu SS

Subjects

Calibration, Circular Dichroism, Humans, Mass Spectrometry, Reference Standards, Surface Plasmon Resonance, Vascular Endothelial Growth Factor A antagonists & inhibitors

Abstract

Polypeptides composed entirely of d-amino acids and the achiral amino acid glycine (d-proteins) inherently have in vivo properties that are proposed to be near-optimal for a large molecule therapeutic agent. Specifically, d-proteins are resistant to degradation by proteases and are anticipated to be nonimmunogenic. Furthermore, d-proteins are manufactured chemically and can be engineered to have other desirable properties, such as improved stability, affinity, and pharmacokinetics. Thus, a well-designed d-protein therapeutic would likely have significant advantages over l-protein drugs. Toward the goal of developing d-protein therapeutics, we previously generated RFX001.D, a d-protein antagonist of natural vascular endothelial growth factor A (VEGF-A) that inhibited binding to its receptor. However, RFX001.D is unstable at physiological temperatures (Tm = 33 °C). Here, we describe RFX037.D, a variant of RFX001.D with extreme thermal stability (Tm > 95 °C), high affinity for VEGF-A (Kd = 6 nM), and improved receptor blocking. Comparison of the two enantiomeric forms of RFX037 revealed that the d-protein is more stable in mouse, monkey, and human plasma and has a longer half-life in vivo in mice. Significantly, RFX037.D was nonimmunogenic in mice, whereas the l-enantiomer generated a strong immune response. These results confirm the potential utility of synthetic d-proteins as alternatives to therapeutic antibodies.

Published

2016

17. Single Residue Substitutions That Confer Voltage-Gated Sodium Ion Channel Subtype Selectivity in the NaV1.7 Inhibitory Peptide GpTx-1.

Author

Murray JK, Long J, Zou A, Ligutti J, Andrews KL, Poppe L, Biswas K, Moyer BD, McDonough SI, and Miranda LP

Subjects

Amino Acid Sequence, HEK293 Cells, High-Throughput Screening Assays, Humans, Magnetic Resonance Spectroscopy, Models, Molecular, Molecular Docking Simulation, Molecular Sequence Data, Substrate Specificity, NAV1.7 Voltage-Gated Sodium Channel drug effects, Peptides pharmacology, Sodium Channel Blockers chemistry, Sodium Channel Blockers pharmacology, Spider Venoms pharmacology

Abstract

There is interest in the identification and optimization of new molecular entities selectively targeting ion channels of therapeutic relevance. Peptide toxins represent a rich source of pharmacology for ion channels, and we recently reported GpTx-1 analogs that inhibit NaV1.7, a voltage-gated sodium ion channel that is a compelling target for improved treatment of pain. Here we utilize multi-attribute positional scan (MAPS) analoging, combining high-throughput synthesis and electrophysiology, to interrogate the interaction of GpTx-1 with NaV1.7 and related NaV subtypes. After one round of MAPS analoging, we found novel substitutions at multiple residue positions not previously identified, specifically glutamic acid at positions 10 or 11 or lysine at position 18, that produce peptides with single digit nanomolar potency on NaV1.7 and 500-fold selectivity against off-target sodium channels. Docking studies with a NaV1.7 homology model and peptide NMR structure generated a model consistent with the key potency and selectivity modifications mapped in this work.

Published

2016

18. Sustained inhibition of the NaV1.7 sodium channel by engineered dimers of the domain II binding peptide GpTx-1.

Author

Murray JK, Biswas K, Holder JR, Zou A, Ligutti J, Liu D, Poppe L, Andrews KL, Lin FF, Meng SY, Moyer BD, McDonough SI, and Miranda LP

Subjects

Dimerization, Dose-Response Relationship, Drug, Humans, Molecular Conformation, Protein Binding, Protein Structure, Tertiary, Structure-Activity Relationship, Voltage-Gated Sodium Channel Blockers chemistry, NAV1.7 Voltage-Gated Sodium Channel metabolism, Peptides chemistry, Peptides pharmacology, Protein Engineering, Voltage-Gated Sodium Channel Blockers pharmacology

Abstract

Many efforts are underway to develop selective inhibitors of the voltage-gated sodium channel NaV1.7 as new analgesics. Thus far, however, in vitro selectivity has proved difficult for small molecules, and peptides generally lack appropriate pharmacokinetic properties. We previously identified the NaV1.7 inhibitory peptide GpTx-1 from tarantula venom and optimized its potency and selectivity via structure-guided analoging. To further understand GpTx-1 binding to NaV1.7, we have mapped the binding site to transmembrane segments 1-4 of the second pseudosubunit internal repeat (commonly referred to as Site 4) using NaV1.5/NaV1.7 chimeric protein constructs. We also report that select GpTx-1 amino acid residues apparently not contacting NaV1.7 can be derivatized with a hydrophilic polymer without adversely affecting peptide potency. Homodimerization of GpTx-1 with a bifunctional polyethylene glycol (PEG) linker resulted in a compound with increased potency and a significantly reduced off-rate, demonstrating the ability to modulate the function and properties of GpTx-1 by linking to additional molecules., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2015

19. Pharmaceutical Optimization of Peptide Toxins for Ion Channel Targets: Potent, Selective, and Long-Lived Antagonists of Kv1.3.

Author

Murray JK, Qian YX, Liu B, Elliott R, Aral J, Park C, Zhang X, Stenkilsson M, Salyers K, Rose M, Li H, Yu S, Andrews KL, Colombero A, Werner J, Gaida K, Sickmier EA, Miu P, Itano A, McGivern J, Gegg CV, Sullivan JK, and Miranda LP

Subjects

Animals, CHO Cells, Cnidarian Venoms pharmacokinetics, Cnidarian Venoms pharmacology, Cricetulus, Crystallography, X-Ray, Dogs, HEK293 Cells, Humans, Interferon-gamma blood, Interferon-gamma metabolism, Interleukin-17 blood, Interleukin-17 metabolism, Interleukin-2 blood, Interleukin-2 metabolism, Kv1.1 Potassium Channel antagonists & inhibitors, Macaca fascicularis, Male, Mice, Molecular Docking Simulation, Patch-Clamp Techniques, Peptides pharmacokinetics, Peptides pharmacology, Rats, Sprague-Dawley, Species Specificity, Stereoisomerism, Structure-Activity Relationship, T-Lymphocytes drug effects, T-Lymphocytes metabolism, Cnidarian Venoms chemistry, Kv1.3 Potassium Channel antagonists & inhibitors, Peptides chemistry, Polyethylene Glycols chemistry

Abstract

To realize the medicinal potential of peptide toxins, naturally occurring disulfide-rich peptides, as ion channel antagonists, more efficient pharmaceutical optimization technologies must be developed. Here, we show that the therapeutic properties of multiple cysteine toxin peptides can be rapidly and substantially improved by combining direct chemical strategies with high-throughput electrophysiology. We applied whole-molecule, brute-force, structure-activity analoging to ShK, a peptide toxin from the sea anemone Stichodactyla helianthus that inhibits the voltage-gated potassium ion channel Kv1.3, to effectively discover critical structural changes for 15× selectivity against the closely related neuronal ion channel Kv1.1. Subsequent site-specific polymer conjugation resulted in an exquisitely selective Kv1.3 antagonist (>1000× over Kv1.1) with picomolar functional activity in whole blood and a pharmacokinetic profile suitable for weekly administration in primates. The pharmacological potential of the optimized toxin peptide was demonstrated by potent and sustained inhibition of cytokine secretion from T cells, a therapeutic target for autoimmune diseases, in cynomolgus monkeys.

Published

2015

20. Engineering potent and selective analogues of GpTx-1, a tarantula venom peptide antagonist of the Na(V)1.7 sodium channel.

Author

Murray JK, Ligutti J, Liu D, Zou A, Poppe L, Li H, Andrews KL, Moyer BD, McDonough SI, Favreau P, Stöcklin R, and Miranda LP

Subjects

Animals, Electrophysiology, Female, High-Throughput Screening Assays, Humans, Magnetic Resonance Spectroscopy, Male, Mice, Mice, Inbred C57BL, NAV1.7 Voltage-Gated Sodium Channel blood, Peptide Fragments chemistry, Protein Conformation, Rats, Spectrometry, Mass, Electrospray Ionization, Spider Venoms chemistry, Spiders, Structure-Activity Relationship, Voltage-Gated Sodium Channel Blockers chemistry, NAV1.7 Voltage-Gated Sodium Channel chemistry, Peptide Fragments pharmacology, Spider Venoms pharmacology, Voltage-Gated Sodium Channel Blockers pharmacology

Abstract

NaV1.7 is a voltage-gated sodium ion channel implicated by human genetic evidence as a therapeutic target for the treatment of pain. Screening fractionated venom from the tarantula Grammostola porteri led to the identification of a 34-residue peptide, termed GpTx-1, with potent activity on NaV1.7 (IC50 = 10 nM) and promising selectivity against key NaV subtypes (20× and 1000× over NaV1.4 and NaV1.5, respectively). NMR structural analysis of the chemically synthesized three disulfide peptide was consistent with an inhibitory cystine knot motif. Alanine scanning of GpTx-1 revealed that residues Trp(29), Lys(31), and Phe(34) near the C-terminus are critical for potent NaV1.7 antagonist activity. Substitution of Ala for Phe at position 5 conferred 300-fold selectivity against NaV1.4. A structure-guided campaign afforded additive improvements in potency and NaV subtype selectivity, culminating in the design of [Ala5,Phe6,Leu26,Arg28]GpTx-1 with a NaV1.7 IC50 value of 1.6 nM and >1000× selectivity against NaV1.4 and NaV1.5.

Published

2015

21. Epitope discovery for a synthetic polymer nanoparticle: a new strategy for developing a peptide tag.

Author

Yoshimatsu K, Yamazaki T, Hoshino Y, Rose PE, Epstein LF, Miranda LP, Tagari P, Beierle JM, Yonamine Y, and Shea KJ

Subjects

Avidin chemistry, Molecular Structure, Particle Size, Polymers chemistry, Recombinant Proteins chemistry, Recombinant Proteins isolation & purification, Surface Properties, Epitopes chemistry, Nanoparticles chemistry, Peptides chemistry, Polymers chemical synthesis

Abstract

We describe a novel epitope discovery strategy for creating an affinity agent/peptide tag pair. A synthetic polymer nanoparticle (NP) was used as the "bait" to catch an affinity peptide tag. Biotinylated peptide tag candidates of varied sequence and length were attached to an avidin platform and screened for affinity against the polymer NP. NP affinity for the avidin/peptide tag complexes was used to provide insight into factors that contribute NP/tag binding. The identified epitope sequence with an optimized length (tMel-tag) was fused to two recombinant proteins. The tagged proteins exhibited higher NP affinity than proteins without tags. The results establish that a fusion peptide tag consisting of optimized 15 amino acid residues can provide strong affinity to an abiotic polymer NP. The affinity and selectivity of NP/tMel-tag interactions were exploited for protein purification in conjunction with immobilized metal ion/His6-tag interactions to prepare highly purified recombinant proteins. This strategy makes available inexpensive, abiotic synthetic polymers as affinity agents for peptide tags and provides alternatives for important applications where more costly affinity agents are used.

Published

2014

22. Peptide antagonists of the calcitonin gene-related peptide (CGRP) receptor with improved pharmacokinetics and pharmacodynamics.

Author

Miranda LP, Shi L, Holder JR, Wright M, Gegg CV, Johnson E, Wild K, Stenkilsson M, Doellgast G, Manning BH, and Salyers K

Subjects

Calcitonin Gene-Related Peptide, Receptors, Calcitonin Gene-Related Peptide

Abstract

Antagonism of the calcitonin gene-related peptide (CGRP) receptor may be a useful approach for migraine treatment. Selective PEGylated peptide antagonists to the CGRP receptor are described, derived from CGRP(8-37) with polymer derivatization at an engineered lysine-25 residue. Potent PEGylated peptides with improved pharmacokinetics were identified through peptide side-chain modification to mitigate metabolic liabilities. PEGylated Ac-Trp-[Cit(11,18),hArg(24),Lys(25),Asp(31),Pro(34),1-Nal(35)]CGRP(8-37)-NH2, 9, elicits a dose-dependent reduction of intradermal CGRP-induced local blood flow in rodents with an ED50 of 0.52 mg kg(-1) without any overt adverse effects., (Copyright © 2013 Wiley Periodicals, Inc.)

Published

2013

23. Utilization of tyrosine- and histidine-containing dipeptides to enhance productivity and culture viability.

Author

Kang S, Mullen J, Miranda LP, and Deshpande R

Subjects

Animals, Bioreactors, Biotechnology, CHO Cells, Cell Survival physiology, Cricetinae, Cricetulus, Culture Media chemistry, Histidine chemistry, Hydrogen-Ion Concentration, Lactic Acid metabolism, Lysine chemistry, Lysine metabolism, Tyrosine chemistry, Cell Culture Techniques methods, Culture Media metabolism, Dipeptides chemistry, Dipeptides metabolism, Histidine metabolism, Tyrosine metabolism

Abstract

Adequate supply of nutrients, especially providing a sufficient level of specific amino acids, is essential for cell survival and production. Complex raw materials such as soy hydrolysates or yeast extracts are the source for both free amino acids and peptides. However, typical chemically defined (CD) media provide amino acids only in free form. While most amino acids are highly soluble in media and can be provided at fairly high concentrations, certain amino acids such as tyrosine have poor solubility and thus, only a limited amount can be added as a media component. The limited solubility of amino acids in media can raise the risk of media precipitation and instability, and could contribute to suboptimal culture performance due to insufficient nutrient levels to meet cellular demands. In this study, we examine the use of chemically synthesized dipeptides as an alternative method for delivering amino acids to various monoclonal antibody producing cell lines. In particular, we focus on tyrosine-containing dipeptides. Due to their substantially higher solubility (up to 250-fold as compared with free tyrosine), tyrosine-containing dipeptides can efficiently provide large amounts of tyrosine to cultured cells. When tested in fed-batch processes, these supplemental dipeptides exerted positive effects, including enhanced culture viability and titer. Moreover, dipeptide-supplemented cultures displayed improved metabolic profiles including lower lactate and NH 4(+) production, and better pH maintenance. In bioreactor studies using two-sided pH control, a lactate spike occurring on Day 10 and the concomitant high levels of base addition could be prevented with dipeptide supplementation. These beneficial effects could be obtained by one-time addition of dipeptides during inoculation, and did not require further feeds during the entire 11-15-day process. Non-tyrosine-containing dipeptides, such as His-Gly, also showed improved productivity and viability over control cultures., (Copyright © 2012 Wiley Periodicals, Inc.)

Published

2012

24. Molecular mechanism of hepcidin-mediated ferroportin internalization requires ferroportin lysines, not tyrosines or JAK-STAT.

Author

Ross SL, Tran L, Winters A, Lee KJ, Plewa C, Foltz I, King C, Miranda LP, Allen J, Beckman H, Cooke KS, Moody G, Sasu BJ, Nemeth E, Ganz T, Molineux G, and Arvedson TL

Subjects

Amino Acid Motifs, Amino Acid Substitution, Antimicrobial Cationic Peptides, Cation Transport Proteins genetics, HEK293 Cells, Hepcidins, Humans, Janus Kinase 2 antagonists & inhibitors, Membrane Proteins metabolism, Mutagenesis, Site-Directed, Phosphorylation, Protein Transport, Signal Transduction, Ubiquitination, Cation Transport Proteins metabolism, Janus Kinase 2 metabolism, Lysine metabolism, Protein Processing, Post-Translational, STAT Transcription Factors metabolism, Tyrosine metabolism

Abstract

Ferroportin is the primary means of cellular iron efflux and a key component of iron metabolism. Hepcidin regulates Fpn activity by inducing its internalization and degradation. The mechanism of internalization is reported to require JAK2 activation, phosphorylation of Fpn tyrosine residues 302 and 303, and initiation of transcription through STAT3 phosphorylation. These findings suggest Fpn may be a target for therapeutic intervention through JAK2 modulation. To evaluate the proposed mechanism, Fpn internalization was assessed using several techniques combined with reagents that specifically recognized cell-surface Fpn. In vitro results demonstrated that Hepc-induced Fpn internalization did not require JAK2 or phosphorylation of Fpn residues 302 and 303, nor did it induce JAK-STAT signaling. In vivo, inhibition of JAK2 had no effect on Hepc-induced hypoferremia. However, internalization was delayed by mutation of two Fpn lysine residues that may be targets of ubiquitination., (Copyright © 2012 Elsevier Inc. All rights reserved.)

Published

2012

25. Direct quantitative analysis of a 20 kDa PEGylated human calcitonin gene peptide antagonist in cynomolgus monkey serum using in-source CID and UPLC-MS/MS.

Author

Li H, Rose MJ, Holder JR, Wright M, Miranda LP, and James CA

Subjects

Amino Acid Sequence, Animals, Calcitonin Gene-Related Peptide antagonists & inhibitors, Calcitonin Gene-Related Peptide chemistry, Calcitonin Gene-Related Peptide pharmacokinetics, Humans, Least-Squares Analysis, Macaca fascicularis, Molecular Sequence Data, Polyethylene Glycols chemistry, Polyethylene Glycols pharmacokinetics, Reproducibility of Results, Calcitonin Gene-Related Peptide blood, Calcitonin Gene-Related Peptide Receptor Antagonists, Chromatography, High Pressure Liquid methods, Polyethylene Glycols analysis, Tandem Mass Spectrometry methods

Abstract

PEGylation is a successful strategy to improve the pharmacokinetic and pharmaceutical properties of therapeutic peptides. However, quantitative analysis of PEGylated peptides in biomatrix by LC-MS/MS poses significant analytical challenge due to the polydispersity of the polyethylene glycol (PEG), and the multiple charge states observed for both the peptide and PEG moieties. In this report, a novel LC-MS/MS method for direct quantitative analysis of 20 kDa PEGylated CGRP[Cit, Cit] in cynomolgus monkey serum is presented. CGRP[Cit, Cit] is an investigational human calcitonin gene peptide receptor antagonist with amino acid sequence Ac -WVTH[Cit]LAGLLS[Cit]SGGVVRKNFVPT DVGPFAF-NH(2). In-source collision-induced dissociation (in-source CID) of 20 kDa PEGylated peptide was used to generate CGRP[Cit, Cit] fragment ions, among which the most abundant b(8)(+) ion was selected and measured as a surrogate for the 20 kDa PEGylated peptide. A solid phase extraction (SPE) method was used to extract the PEGylated peptides from the biomatrix prior to the UPLC-MS/MS analysis. This method achieved a lower limit of quantitation (LLOQ) of 5.00 ng/mL with a serum sample volume of 100 μL, and was linear over the calibration range of 5.00 to 500 ng/mL in cynomolgus monkey serum. Intraday and interday accuracy and precision from QC samples were within ±15%. This method was successfully applied to a pharmacokinetic study of the 20 kDa PEGylated CGRP[Cit, Cit] in cynomolgus monkeys.

Published

2011

26. Solid-phase peptide synthesis using microwave irradiation.

Author

Murray JK, Aral J, and Miranda LP

Subjects

Acyl Carrier Protein chemical synthesis, Acyl Carrier Protein chemistry, Amino Acid Sequence, Antimicrobial Cationic Peptides chemical synthesis, Antimicrobial Cationic Peptides chemistry, Combinatorial Chemistry Techniques economics, Combinatorial Chemistry Techniques instrumentation, Fluorenes, Hepcidins, Humans, Molecular Sequence Data, Peptides chemistry, Combinatorial Chemistry Techniques methods, Microwaves, Peptides chemical synthesis

Abstract

Since the advent of solid-phase peptide synthesis (SPPS) in the late 1950s, numerous advancements in the underlying chemistry (i.e., orthogonal protection strategy, coupling reagents, and solid support matrices) have greatly improved the efficiency of the technique. More recently, application of microwave radiation to SPPS has been found to reduce reaction time and/or increase the initial purity of synthetic peptide products. In this protocol, conditions are described to accomplish rapid peptide coupling and 9-fluorenylmethoxycarbonyl (Fmoc) removal reactions under temperature-controlled conditions in either a manual or automated synthesis format using a microwave reactor. These microwave-assisted peptide synthesis procedures have been used to rapidly prepare a "difficult" peptide sequence from the acyl carrier protein, ACP(65-74), in less than 3 h and the reduced, linear precursor to human hepcidin, in high initial purity.

Published

2011

27. Dipeptidyl-quinolone derivatives inhibit hypoxia inducible factor-1α prolyl hydroxylases-1, -2, and -3 with altered selectivity.

Author

Murray JK, Balan C, Allgeier AM, Kasparian A, Viswanadhan V, Wilde C, Allen JR, Yoder SC, Biddlecome G, Hungate RW, and Miranda LP

Subjects

Combinatorial Chemistry Techniques, Dipeptides chemical synthesis, Dipeptides chemistry, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors chemistry, Hypoxia-Inducible Factor 1, alpha Subunit metabolism, Isoenzymes chemistry, Isoenzymes metabolism, Molecular Structure, Procollagen-Proline Dioxygenase chemistry, Procollagen-Proline Dioxygenase metabolism, Quinolones chemical synthesis, Quinolones chemistry, Stereoisomerism, Structure-Activity Relationship, Dipeptides pharmacology, Enzyme Inhibitors pharmacology, Isoenzymes antagonists & inhibitors, Procollagen-Proline Dioxygenase antagonists & inhibitors, Quinolones pharmacology

Abstract

Intracellular levels of the hypoxia-inducible transcription factor (HIF) are regulated under normoxic conditions by prolyl hydroxylases (PHD1, 2, and 3). Treatment of cells with PHD inhibitors stabilizes HIF-1α, eliciting an artificial hypoxic response that includes the transcription of genes involved in erythropoiesis, angiogenesis, and glycolysis. The different in vivo roles of the three PHD isoforms are not yet known, making a PHD-selective inhibitor useful as a biological tool. Although several chemical series of PHD inhibitors have been described, significant isoform selectivity has not been reported. Here we report the synthesis and activity of dipeptidyl analogues derived from a potent but non-selective quinolone scaffold. The compounds were prepared by Pd-catalyzed reductive carbonylation of the 6-iodoquinolone derivative to form the aldehyde directly, which was then attached to a solid support via reductive amination. Amino acids were coupled, and the resulting dipeptidyl-quinolone derivatives were screened, revealing retention of PHD inhibitory activity but an altered PHD1, 2, and 3 selectivity profile. The compounds were found to be ∼10-fold more potent against PHD1 and PHD3 than against PHD2, whereas the specific parent compound had shown no appreciable selectivity among the different PHD isoforms.

Published

2010

28. Oxidative folding of hepcidin at acidic pH.

Author

Zhang J, Diamond S, Arvedson T, Sasu BJ, and Miranda LP

Subjects

Chromatography, High Pressure Liquid, Combinatorial Chemistry Techniques, Dimethyl Sulfoxide chemistry, Hepcidins, Humans, Hydrogen-Ion Concentration, Oxidation-Reduction, Protein Folding, Antimicrobial Cationic Peptides chemistry

Abstract

Hepcidin is a four disulfide 25-residue peptide hormone which has a central role in the regulation of iron homeostasis. To support studies on hepcidin we have sought to establish reliable and robust synthetic methods for the preparation of correctly folded materials. While correctly-folded hepcidin has good aqueous solubility, we have found that its direct synthetic precursor, linear (reduced) hepcidin peptide, is resistant to solubilization, prone to precipitation at pH > or = 6, and thus difficult to fold efficiently. Attempts to directly fold either the crude or purified linear hepcidin peptide by air or DMSO oxidation methods under basic conditions were ineffective. However, addition of a glutathione redox pair system improved folding of purified linear hepcidin at mild basic pH (pH 7.5). Under acidic conditions, it was possible to oxidatively fold both crude and purified hepcidin using a polymer-supported oxidizing strategy. Peptide precipitation was also avoided under acidic conditions. Isolated folding yields of human hepcidin under acidic polymer-assisted conditions were superior to yields under basic folding conditions. These studies enabled identification of a reliable synthetic route for correctly-folded hepcidin.

Published

2010

29. Hepcidin revisited, disulfide connectivity, dynamics, and structure.

Author

Jordan JB, Poppe L, Haniu M, Arvedson T, Syed R, Li V, Kohno H, Kim H, Schnier PD, Harvey TS, Miranda LP, Cheetham J, and Sasu BJ

Subjects

Animals, Antimicrobial Cationic Peptides genetics, Antimicrobial Cationic Peptides metabolism, CHO Cells, Cricetinae, Cricetulus, Crystallography, X-Ray, Disulfides metabolism, Hepcidins, Humans, Nuclear Magnetic Resonance, Biomolecular, Protein Structure, Tertiary physiology, Antimicrobial Cationic Peptides chemistry, Disulfides chemistry, Protein Folding

Abstract

Hepcidin is a tightly folded 25-residue peptide hormone containing four disulfide bonds, which has been shown to act as the principal regulator of iron homeostasis in vertebrates. We used multiple techniques to demonstrate a disulfide bonding pattern for hepcidin different from that previously published. All techniques confirmed the following disulfide bond connectivity: Cys(1)-Cys(8), Cys(3)-Cys(6), Cys(2)-Cys(4), and Cys(5)-Cys(7). NMR studies reveal a new model for hepcidin that, at ambient temperatures, interconverts between two different conformations, which could be individually resolved by temperature variation. Using these methods, the solution structure of hepcidin was determined at 325 and 253 K in supercooled water. X-ray analysis of a co-crystal with Fab appeared to stabilize a hepcidin conformation similar to the high temperature NMR structure.

Published

2009

30. Development of a method for the sensitive and quantitative determination of hepcidin in human serum using LC-MS/MS.

Author

Li H, Rose MJ, Tran L, Zhang J, Miranda LP, James CA, and Sasu BJ

Subjects

Animals, Biomarkers blood, Calibration, Chromatography, High Pressure Liquid, Hepcidins, Humans, Mass Spectrometry, Rabbits, Sensitivity and Specificity, Antimicrobial Cationic Peptides blood

Abstract

Introduction: Hepcidin, a 25-amino acid peptide hormone, plays a crucial regulatory role in iron metabolism. Elevated hepcidin has been observed in response to inflammation and is speculated to be a causative factor in inflammatory anemia due to induction of functional iron deficiency. Hepcidin has been suggested as a biomarker of anemia of inflammation. An accurate assessment of human serum hepcidin is critical to understand its role in anemia., Methods: An LC-MS/MS method was developed to quantify hepcidin in human serum using chemically synthesized hepcidin as a standard and stable isotope labeled hepcidin as internal standard. Rabbit serum was used as a surrogate matrix for standards due to the presence of endogenous hepcidin in human serum. The method was validated to FDA criteria for bioanalytical assays., Results: The calibration curve was validated over the range of 2.5 to 500 ng/mL. Hepcidin was stable in serum for at least 16 h at room temperature, 90 days at -60 to -80 degrees C, and after three F/T cycles. Interday accuracy (% RE) and precision (%CV) were -11.2% and 5.6%, respectively at the LLOQ, and less than +/-7.0% and 9.2%, respectively for higher concentrations. The mean accuracy of quality control samples (5.00, 15.0, 100 and 400 ng/mL) in 21 analytical batches was between -0.7 and +2.1%, with mean precision between 5.1% and 13.4%. Hepcidin was below 2.5 ng/mL in 31 of 60 healthy subjects, while the mean concentration was less than 10 ng/mL. Sepsis and chronic kidney disease patients had mean serum concentrations of 252 ng/mL (n=16, median 121 ng/mL) and 99 ng/mL (n=50, median 68 ng/mL), respectively., Conclusions: A fully validated LC-MS/MS method has been described for the determination of hepcidin in human serum. This method was applied to the determination of hepcidin in over 1200 human samples.

Published

2009

31. Identification of potent, selective, and metabolically stable peptide antagonists to the calcitonin gene-related peptide (CGRP) receptor.

Author

Miranda LP, Holder JR, Shi L, Bennett B, Aral J, Gegg CV, Wright M, Walker K, Doellgast G, Rogers R, Li H, Valladares V, Salyers K, Johnson E, and Wild K

Subjects

Amino Acid Sequence, Animals, CHO Cells, Cricetinae, Cricetulus, Drug Design, Humans, Inhibitory Concentration 50, Kinetics, Macaca fascicularis, Male, Molecular Conformation, Molecular Sequence Data, Protein Binding, Calcitonin Gene-Related Peptide Receptor Antagonists, Chemistry, Pharmaceutical methods, Receptors, Calcitonin Gene-Related Peptide chemistry

Abstract

Calcitonin gene-related peptide (CGRP) is a 37-residue neuropeptide that can be converted to a CGRP(1) receptor antagonist by the truncation of its first seven residues. CGRP(8-37), 1, has a CGRP(1) receptor K(i) = 3.2 nM but is rapidly degraded in human plasma (t(1/2) = 20 min). As part of an effort to identify a prolonged in vivo circulating CGRP peptide antagonist, we found that the substitution of multiple residues in the CGRP peptide increased CGRP(1) receptor affinity >50-fold. Ac-Trp-[Arg(24),Lys(25),Asp(31),Pro(34),Phe(35)]CGRP(8-37)-NH(2), 5 (K(i) = 0.06 nM) had the highest CGRP(1) receptor affinity. Using complimentary in vitro and in vivo metabolic studies, we iteratively identified degradation sites and prepared high affinity analogues with significantly improved plasma stability. Ac-Trp-[Cit(11,18),hArg(24),Lys(25),2-Nal(27,37),Asp(31),Oic(29,34),Phe(35)]CGRP(8-37)-NH(2), 32 (K(i) = 3.3 nM), had significantly increased (>100-fold) stability over 1 or 5, with a cynomolgus monkey and human in vitro plasma half-life of 38 and 68 h, respectively.

Published

2008

32. Design and synthesis of conformationally constrained glucagon-like peptide-1 derivatives with increased plasma stability and prolonged in vivo activity.

Author

Miranda LP, Winters KA, Gegg CV, Patel A, Aral J, Long J, Zhang J, Diamond S, Guido M, Stanislaus S, Ma M, Li H, Rose MJ, Poppe L, and Véniant MM

Subjects

Amino Acid Sequence, Animals, Blood Glucose analysis, Body Weight drug effects, CHO Cells, Cricetinae, Cricetulus, Drug Design, Glucagon-Like Peptide 1 pharmacology, Glucagon-Like Peptide-1 Receptor, Humans, Hypoglycemic Agents pharmacology, Macaca fascicularis, Mice, Mice, Mutant Strains, Models, Molecular, Molecular Sequence Data, Plasma, Polyethylene Glycols chemistry, Protein Conformation, Radioligand Assay, Receptors, Glucagon genetics, Structure-Activity Relationship, Glucagon-Like Peptide 1 analogs & derivatives, Glucagon-Like Peptide 1 chemical synthesis, Hypoglycemic Agents chemical synthesis, Receptors, Glucagon agonists

Abstract

A series of conformationally constrained derivatives of glucagon-like peptide-1 (GLP-1) were designed and evaluated. By use of [Gly (8)]GLP-1(7-37)-NH2 (2) peptide as a starting point, 17 cyclic derivatives possessing i to i + 4, i to i + 5, or i to i + 7 side chain to side chain lactam bridges from positions 18 to 30 were prepared. The effect of a helix-promoting alpha-amino-isobutyric acid (Aib) substitution at position 22 was also evaluated. The introduction of i to i + 4 glutamic acid-lysine lactam constraints in c[Glu (18)-Lys (22)][Gly (8)]GLP-1(7-37)-NH2 (6), c[Glu (22)-Lys (26)][Gly (8)]GLP-1(7-37)-NH2 (10), and c[Glu (23)-Lys (27)][Gly (8)]GLP-1(7-37)-NH2 (11) resulted in potent functional activity and receptor affinities comparable to native GLP-1. Selected GLP-1 peptides were chemoselectively PEGylated in order to prolong their in vivo activity. PEGylated peptides [Gly (8),Aib (22)]GLP-1(7-37)-Cys ((PEG))-Ala-NH2 (23) and c[Glu (22)-Lys (26)][Gly (8)]GLP-1(7-37)-Cys ((PEG))-Ser-Gly-NH2 (24) retained picomolar functional potency and avid receptor binding properties. Importantly, PEGylated GLP-1 peptide 23 exhibited sustained in vivo efficacy with respect to blood glucose reduction and decreased body weight for several days in nonhuman primates.

Published

2008

33. A chemical approach to the pharmaceutical optimization of an anti-HIV protein.

Author

Miranda LP, Shao H, Williams J, Chen SY, Kong T, Garcia R, Chinn Y, Fraud N, O'Dwyer B, Ye J, Wilken J, Low DE, Cagle EN, Carnevali M, Lee A, Song D, Kung A, Bradburne JA, Paliard X, and Kochendoerfer GG

Subjects

Amino Acids chemistry, Animals, Anti-HIV Agents pharmacokinetics, Chromatography, Gel, Male, Models, Molecular, Molecular Structure, Polymers chemistry, Rats, Receptors, G-Protein-Coupled metabolism, Anti-HIV Agents chemistry, HIV Antibodies immunology, Human Immunodeficiency Virus Proteins immunology

Abstract

Chemical protein synthesis is important for dissecting the molecular basis of protein function. Here we advance its scope by demonstrating the significant improvement of the multifaceted pharmaceutical profile of small proteins exclusively via a chemical-based approach. The focus of this work centered on CCL-5 (RANTES) derivatives with potent anti-HIV activity. The overall chemical strategy involved a combination of coded and noncoded amino acid mutagenesis, peptide backbone engineering, and site-specific polymer attachment. The ability to alter specific protein residues, as well as precise control of the position and type of polymer attachment, allows for the exploration of specific molecular designs and resulted in novel CCL-5 analogues with significant differences in their respective biochemical and pharmaceutical properties. Using this approach, the complex-interplay of variables contributing to the noncovalent self-association (aggregation) state, CCR-5 specificity, in vivo elimination half-life, and anti-HIV activity of CCL-5-based protein analogues could be empirically evaluated via total chemical synthesis. This work has led to the identification of potent (sub-nanomolar) anti-HIV proteins with significantly improved pharmaceutical profiles, and illustrates the increasing value of protein chemical synthesis in contemporary therapeutic discovery. These antiviral molecules provide a novel mechanism of action for the development of a new generation of anti-HIV therapeutics which are still desperately needed.

Published

2007

34. Site-specific polymer attachment to a CCL-5 (RANTES) analogue by oxime exchange.

Author

Shao H, Crnogorac MM, Kong T, Chen SY, Williams JM, Tack JM, Gueriguian V, Cagle EN, Carnevali M, Tumelty D, Paliard X, Miranda LP, Bradburne JA, and Kochendoerfer GG

Subjects

Anti-HIV Agents chemistry, Anti-HIV Agents pharmacology, Binding Sites, Chemokine CCL5 chemistry, Chemokine CCL5 pharmacology, Chemokines, CC pharmacology, Glycine chemistry, HIV-1 drug effects, Humans, Models, Molecular, Polyethylene Glycols chemistry, Protein Folding, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Chemokine CCL5 analogs & derivatives, Chemokines, CC chemistry, Oximes chemistry

Abstract

A synthetic strategy that allows for the site-specific attachment of polymers such as poly(ethylene glycol) (PEG) to protein pharmaceuticals is described. PEG was attached to a 67-amino acid fully synthetic CCL-5 (RANTES) analogue at its GAG binding site both to reduce aggregation and to increase the circulating lifetime. Effective protection of an Aoaa chemoselective linker during peptide assembly, total chemical protein synthesis, and protein folding was achieved with an isopropylidene group. Mild deprotection of the resulting folded synthetic protein and subsequent polymer attachment occur without interference with the native folded structure and activity.

Published

2005

35. Probing the S100 protein family through genomic and functional analysis.

Author

Ravasi T, Hsu K, Goyette J, Schroder K, Yang Z, Rahimi F, Miranda LP, Alewood PF, Hume DA, and Geczy C

Subjects

Animals, Boron Compounds metabolism, Chemotaxis genetics, Chemotaxis physiology, Gene Expression Regulation drug effects, Gene Expression Regulation genetics, Humans, Lipopolysaccharides pharmacology, Macrophage Activation drug effects, Macrophages metabolism, Methacrylates metabolism, Methylmethacrylates metabolism, Neutrophil Activation drug effects, Neutrophils metabolism, Organ Specificity genetics, Rats, Zinc Fingers genetics, Calcium-Binding Proteins genetics, Calcium-Binding Proteins metabolism, EF Hand Motifs genetics, Evolution, Molecular, Genome, Phylogeny

Abstract

The EF-hand superfamily of calcium binding proteins includes the S100, calcium binding protein, and troponin subfamilies. This study represents a genome, structure, and expression analysis of the S100 protein family, in mouse, human, and rat. We confirm the high level of conservation between mammalian sequences but show that four members, including S100A12, are present only in the human genome. We describe three new members of the S100 family in the three species and their locations within the S100 genomic clusters and propose a revised nomenclature and phylogenetic relationship between members of the EF-hand superfamily. Two of the three new genes were induced in bone-marrow-derived macrophages activated with bacterial lipopolysaccharide, suggesting a role in inflammation. Normal human and murine tissue distribution profiles indicate that some members of the family are expressed in a specific manner, whereas others are more ubiquitous. Structure-function analysis of the chemotactic properties of murine S100A8 and human S100A12, particularly within the active hinge domain, suggests that the human protein is the functional homolog of the murine protein. Strong similarities between the promoter regions of human S100A12 and murine S100A8 support this possibility. This study provides insights into the possible processes of evolution of the EF-hand protein superfamily. Evolution of the S100 proteins appears to have occurred in a modular fashion, also seen in other protein families such as the C2H2-type zinc-finger family., (Copyright 2004 Elsevier Inc.)

Published

2004

36. A new approach to the chemical synthesis of keto-proteins.

Author

Tumelty D, Carnevali M, and Miranda LP

Subjects

Amino Acid Sequence, Chemokine CCL5 chemical synthesis, Chromatography, High Pressure Liquid, Molecular Sequence Data, Peptide Fragments chemical synthesis, Ketones chemical synthesis, Proteins chemical synthesis

Abstract

To increase the versatility of protein-conjugation, an orthogonal protection strategy is described, which enables the efficient synthesis of keto-proteins bearing a reactive ketone functionality using Boc, Fmoc, and chemical ligation methodologies. A 1,3-dithiolane group was used to protect the ketone function of levulinate- and pyruvate-derivatized peptides during solid-phase synthesis, acidolytic cleavage, and purification. When required, the 1,3-dithiolane group could be cleanly removed using aqueous silver or mercuric solutions to regenerate the reactive keto-protein at ambient temperature. The liberated keto-protein was chemoselectively conjugated in situ to an aminooxy-derivatized monodisperse polymer.

Published

2003

37. Design and chemical synthesis of a homogeneous polymer-modified erythropoiesis protein.

Author

Kochendoerfer GG, Chen SY, Mao F, Cressman S, Traviglia S, Shao H, Hunter CL, Low DW, Cagle EN, Carnevali M, Gueriguian V, Keogh PJ, Porter H, Stratton SM, Wiedeke MC, Wilken J, Tang J, Levy JJ, Miranda LP, Crnogorac MM, Kalbag S, Botti P, Schindler-Horvat J, Savatski L, Adamson JW, Kung A, Kent SB, and Bradburne JA

Subjects

Amino Acid Sequence, Animals, Cell Line, Circular Dichroism, Drug Stability, Electrophoresis, Polyacrylamide Gel, Erythropoietin chemistry, Erythropoietin pharmacology, Hematocrit, Humans, Isoelectric Point, Mice, Molecular Sequence Data, Molecular Structure, Molecular Weight, Protein Folding, Proteins pharmacokinetics, Proteins pharmacology, Rats, Receptors, Erythropoietin drug effects, Receptors, Erythropoietin metabolism, Recombinant Proteins, Spectrometry, Mass, Electrospray Ionization, Drug Design, Erythropoiesis, Polymers chemical synthesis, Polymers chemistry, Polymers pharmacokinetics, Polymers pharmacology, Proteins chemical synthesis, Proteins chemistry

Abstract

We report the design and total chemical synthesis of "synthetic erythropoiesis protein" (SEP), a 51-kilodalton protein-polymer construct consisting of a 166-amino-acid polypeptide chain and two covalently attached, branched, and monodisperse polymer moieties that are negatively charged. The ability to control the chemistry allowed us to synthesize a macromolecule of precisely defined covalent structure. SEP was homogeneous as shown by high-resolution analytical techniques, with a mass of 50,825 +/-10 daltons by electrospray mass spectrometry, and with a pI of 5.0. In cell and animal assays for erythropoiesis, SEP displayed potent biological activity and had significantly prolonged duration of action in vivo. These chemical methods are a powerful tool in the rational design of protein constructs with potential therapeutic applications.

Published

2003

38. SPOCC-194, a new high functional group density PEG-based resin for solid-phase organic synthesis.

Author

Miranda LP, Lubell WD, Halkes KM, Groth T, Grøtli M, Rademann J, Gotfredsen CH, and Meldal M

Abstract

A novel polymer matrix for solid-phase synthesis, SPOCC(194) resin (1), was designed featuring a backbone of homogeneous tetraethylene glycol (TEG(194)) macromonomer linked by quaternary carbon junctions and terminating in primary alcohol functionality. Beaded SPOCC(194) resin was effectively prepared by suspension polymerization of oxetanylated TEG macromonomer 5 in stirred silicon oil. Mechanically stable and inert to a diverse range of reaction conditions, SPOCC(194) possessed a high hydroxyl group loading (0.9-1.2 mmol/g) for substrate attachment and swelled effectively ( approximately 2-4 mL/g) in a variety of organic and aqueous solvents. Developed for solid-phase synthesis at high reactant concentrations for driving organic and aqueous reactions to completion, SPOCC(194) exhibited high functional group density (mmol/mL) similar to that of low-loaded aminomethylated polystyrene-divinylbenzene copolymer (PS-1%DVB) yet significantly higher than that of PEGA(1900), SPOCC(1500), and TentaGel S. High-resolution MAS NMR spectra of Fmoc-derivatized SPOCC(194) indicate that monitoring of functional group transformation is possible. Moreover, by employment of a nonaromatic resin-linker combination, electrophilic chemistry, such as Lewis acid catalyzed glycosylation and Friedel-Crafts acylation, was selectively performed on substrate bound to SPOCC(194) resin. Such properties make SPOCC(194) resin a promising new polymer matrix for the support-bound construction of small organic molecules by parallel and combinatorial synthesis and the scavenging of solution-phase reactants or byproducts.

Published

2002

39. Graphical Abstract.

Author

Miranda LP and Meldal M

Published

2001

40. Unichemo Protection: A Concept for Chemical Synthesis This work was supported by the Danish National Research Foundation.

Author

Miranda LP and Meldal M

Published

2001