Your search keyword '"Cell-penetrating Peptide (CPP)"' showing total 128 results

101. A WXW Motif Is Required for the Anticancer Activity of the TAT-RasGAP317-326 Peptide

Author

Monilola A. Olayioye, David Barras, Rosemary Dempsey, Karine Lapouge, Olivier Michielin, Nadja Chevalier, Christian Widmann, and Vincent Zoete

Subjects

Models, Molecular, Cell, Amino Acid Motifs, Molecular Sequence Data, Cell Migration, Cell-penetrating peptide (CPP), Deleted in Liver Cancer 1 (DLC1), Docking, GTPase-activating Protein (GAP), Peptides, RasGAP, TAT-RasGAP(317-326), Anticancer Peptide, Sensitizer, Peptide, Antineoplastic Agents, Apoptosis, Biology, Calorimetry, Biochemistry, Polymerase Chain Reaction, Structure-Activity Relationship, Cell Line, Tumor, medicine, Humans, Amino Acid Sequence, Molecular Biology, Peptide sequence, DNA Primers, chemistry.chemical_classification, Base Sequence, HEK 293 cells, GTPase-Activating Proteins, Cell migration, Cell Biology, Peptide Fragments, Amino acid, Cell biology, medicine.anatomical_structure, HEK293 Cells, chemistry, Cancer cell, DLC1, Signal Transduction

Abstract

TAT-RasGAP317–326, a cell-permeable 10-amino acid-long peptide derived from the N2 fragment of p120 Ras GTPase-activating protein (RasGAP), sensitizes tumor cells to apoptosis induced by various anticancer therapies. This RasGAP-derived peptide, by targeting the deleted in liver cancer-1 (DLC1) tumor suppressor, also hampers cell migration and invasion by promoting cell adherence and by inhibiting cell movement. Here, we systematically investigated the role of each amino acid within the RasGAP317–326 sequence for the anticancer activities of TAT-RasGAP317–326. We report here that the first three amino acids of this sequence, tryptophan, methionine, and tryptophan (WMW), are necessary and sufficient to sensitize cancer cells to cisplatin-induced apoptosis and to reduce cell migration. The WMW motif was found to be critical for the binding of fragment N2 to DLC1. These results define the interaction mode between the active anticancer sequence of RasGAP and DLC1. This knowledge will facilitate the design of small molecules bearing the tumor-sensitizing and antimetastatic activities of TAT-RasGAP317–326.

Published

2014

102. Design and development of stapled transmembrane peptides that disrupt the activity of G-protein-coupled receptor oligomers.

Author

Botta J, Bibic L, Killoran P, McCormick PJ, and Howell LA

Subjects

Amino Acid Sequence, Calcium metabolism, Cyclic AMP metabolism, Dimerization, HEK293 Cells, Humans, Nanotechnology, Peptides chemical synthesis, Peptides chemistry, Protein Interaction Domains and Motifs, Receptor, Cannabinoid, CB1 chemistry, Receptor, Cannabinoid, CB1 metabolism, Receptor, Serotonin, 5-HT2A chemistry, Receptor, Serotonin, 5-HT2A metabolism, Receptors, G-Protein-Coupled chemistry, Peptides metabolism, Receptors, G-Protein-Coupled metabolism

Abstract

Membrane proteins can associate into larger complexes. Examples include receptor tyrosine complexes, ion channels, transporters, and G protein-coupled receptors (GPCRs). For the latter, there is abundant evidence indicating that GPCRs assemble into complexes, through both homo- and heterodimerization. However, the tools for studying and disrupting these complexes, GPCR or otherwise, are limited. Here, we have developed stabilized interference peptides for this purpose. We have previously reported that tetrahydrocannabinol-mediated cognitive impairment arises from homo- or heterooligomerization between the GPCRs cannabinoid receptor type 1 (CB 1 R) and 5-hydroxytryptamine 2A (5-HT 2A R) receptors. Here, to disrupt this interaction through targeting CB 1 -5-HT 2A receptor heteromers in HEK293 cells and using an array of biochemical techniques, including calcium and cAMP measurements, bimolecular fluorescence complementation assays, and CD-based helicity assessments, we developed a NanoLuc binary technology (NanoBiT)-based reporter assay to screen a small library of aryl-carbon-stapled transmembrane-mimicking peptides produced by solid-phase peptide synthesis. We found that these stapling peptides have increased α-helicity and improved proteolytic resistance without any loss of disrupting activity in vitro , suggesting that this approach may also have utility in vivo In summary, our results provide proof of concept for using NanoBiT to study membrane protein complexes and for stabilizing disrupting peptides to target such membrane complexes through hydrocarbon-mediated stapling. We propose that these peptides could be developed to target previously undruggable GPCR heteromers., (© 2019 Botta et al.)

Published

2019

103. Plant-derived mitochondria-targeting cysteine-rich peptide modulates cellular bioenergetics.

Author

Kam A, Loo S, Dutta B, Sze SK, and Tam JP

Subjects

Cells, Cultured, Flow Cytometry, Hibiscus cytology, Humans, Energy Metabolism, Hibiscus chemistry, Hibiscus metabolism, Mitochondria metabolism, Plant Proteins metabolism

Abstract

Mitochondria are attractive therapeutic targets for developing agents to delay age-related frailty and diseases. However, few promising leads have been identified from natural products. Previously, we identified roseltide rT1, a hyperstable 27-residue cysteine-rich peptide from Hibiscus sabdariffa , as a knottin-type neutrophil elastase inhibitor. Here, we show that roseltide rT1 is also a cell-penetrating, mitochondria-targeting peptide that increases ATP production. Results from flow cytometry, live-cell imaging, pulldown assays, and genetically-modified cell lines supported that roseltide rT1 enters cells via glycosaminoglycan-dependent endocytosis, and enters the mitochondria through TOM20, a mitochondrial protein import receptor. We further showed that roseltide rT1 increases cellular ATP production via mitochondrial membrane hyperpolarization. Using biotinylated roseltide rT1 for target identification and proteomic analysis, we showed that human mitochondrial membrane ATP synthase subunit O is an intramitochondrial target. Collectively, these data support our discovery that roseltide rT1 is a first-in-class mitochondria-targeting, cysteine-rich peptide with potentials to be developed into tools to further our understanding of mitochrondria-related diseases., (© 2019 Kam et al.)

Published

2019

104. Discovery of peptide ligands targeting a specific ubiquitin-like domain-binding site in the deubiquitinase USP11.

Author

Spiliotopoulos A, Blokpoel Ferreras L, Densham RM, Caulton SG, Maddison BC, Morris JR, Dixon JE, Gough KC, and Dreveny I

Subjects

Amino Acid Sequence, Animals, Binding Sites, Cell Line, Crystallography, X-Ray, DNA Repair, Homologous Recombination, Humans, Kinetics, Ligands, Mice, Molecular Sequence Data, Peptides genetics, Protein Domains, Thiolester Hydrolases genetics, Ubiquitin chemistry, Ubiquitin metabolism, Ubiquitination, Peptides chemistry, Peptides metabolism, Thiolester Hydrolases chemistry, Thiolester Hydrolases metabolism

Abstract

Ubiquitin-specific proteases (USPs) reverse ubiquitination and regulate virtually all cellular processes. Defined noncatalytic domains in USP4 and USP15 are known to interact with E3 ligases and substrate recruitment factors. No such interactions have been reported for these domains in the paralog USP11, a key regulator of DNA double-strand break repair by homologous recombination. We hypothesized that USP11 domains adjacent to its protease domain harbor unique peptide-binding sites. Here, using a next-generation phage display (NGPD) strategy, combining phage display library screening with next-generation sequencing, we discovered unique USP11-interacting peptide motifs. Isothermal titration calorimetry disclosed that the highest affinity peptides ( K D of ∼10 μm) exhibit exclusive selectivity for USP11 over USP4 and USP15 in vitro Furthermore, a crystal structure of a USP11-peptide complex revealed a previously unknown binding site in USP11's noncatalytic ubiquitin-like (UBL) region. This site interacted with a helical motif and is absent in USP4 and USP15. Reporter assays using USP11-WT versus a binding pocket-deficient double mutant disclosed that this binding site modulates USP11's function in homologous recombination-mediated DNA repair. The highest affinity USP11 peptide binder fused to a cellular delivery sequence induced significant nuclear localization and cell cycle arrest in S phase, affecting the viability of different mammalian cell lines. The USP11 peptide ligands and the paralog-specific functional site in USP11 identified here provide a framework for the development of new biochemical tools and therapeutic agents. We propose that an NGPD-based strategy for identifying interacting peptides may be applied also to other cellular targets., (© 2019 Spiliotopoulos et al.)

Published

2019

105. Mechanistic studies of intracellular delivery of proteins by cell-penetrating peptides in cyanobacteria

Author

Yue-Wern Huang, Betty Revon Liu, and Han-Jung Lee

Subjects

Microbiology (medical), media_common.quotation_subject, Green Fluorescent Proteins, Endocytic cycle, Cell-Penetrating Peptides, 02 engineering and technology, Endocytosis, Microbiology, Cell-penetrating peptide (CPP), Green fluorescent protein, Cell membrane, 03 medical and health sciences, medicine, Internalization, 030304 developmental biology, media_common, Synechococcus, Macropinocytosis, 0303 health sciences, biology, Pinocytosis, Synechocystis, 021001 nanoscience & nanotechnology, biology.organism_classification, Green fluorescent protein (GFP), Transport protein, Cell biology, medicine.anatomical_structure, Microscopy, Fluorescence, 0210 nano-technology, Protein transduction, Red fluorescent protein (RFP), Research Article

Abstract

Background The plasma membrane plays an essential role in selective permeability, compartmentalization, osmotic balance, and cellular uptake. The characteristics and functions of cyanobacterial membranes have been extensively investigated in recent years. Cell-penetrating peptides (CPPs) are special nanocarriers that can overcome the plasma membrane barrier and enter cells directly, either alone or with associated cargoes. However, the cellular entry mechanisms of CPPs in cyanobacteria have not been studied. Results In the present study, we determine CPP-mediated transduction efficiency and internalization mechanisms in cyanobacteria using a combination of biological and biophysical methods. We demonstrate that both Synechocystis sp. PCC 6803 and Synechococcus elongatus PCC 7942 strains of cyanobacteria possess red autofluorescence. Green fluorescent protein (GFP), either alone or noncovalently associated with a CPP comprised of nine arginine residues (R9/GFP complexes), entered cyanobacteria. The ATP-depleting inhibitor of classical endocytosis, N-ethylmaleimide (NEM), could block the spontaneous internalization of GFP, but not the transduction of R9/GFP complexes. Three specific inhibitors of macropinocytosis, cytochalasin D (CytD), 5-(N-ethyl-N-isopropyl)-amiloride (EIPA), and wortmannin, reduced the efficiency of R9/GFP complex transduction, indicating that entry of R9/GFP complexes involves macropinocytosis. Both the 1-(4,5-dimethylthiazol-2-yl)-3,5-diphenylformazan (MTT) and membrane leakage analyses confirmed that R9/GFP complexes were not toxic to the cyanobacteria, nor were the endocytic and macropinocytic inhibitors used in these studies. Conclusions In summary, we have demonstrated that cyanobacteria use classical endocytosis and macropinocytosis to internalize exogenous GFP and CPP/GFP proteins, respectively. Moreover, the CPP-mediated delivery system is not toxic to cyanobacteria, and can be used to investigate biological processes at the cellular level in this species. These results suggest that both endocytic and macropinocytic pathways can be used for efficient internalization of regular protein and CPP-mediated protein delivery in cyanobacteria, respectively.

Published

2013

106. Intracellular Delivery of Short Interfering RNA in Rat Organ of Corti Using a Cell-penetrating Peptide PepFect6

Author

Stefan Jacob, Suvarna Dash-Wagh, Ülo Langel, Mats Ulfendahl, Anders Fridberger, and Staffan Lindberg

Subjects

inner ear, Small interfering RNA, cell-penetrating peptide (CPP), connexin, Genetic enhancement, cochlea, Connexin, Biology, Bioinformatics, FRAP, gap junctions, gene therapy, nanoparticles, siRNA, Viral vector, RNA interference, Drug Discovery, Gene expression, otorhinolaryngologic diseases, Gene knockdown, lcsh:RM1-950, Neurosciences, Cell biology, lcsh:Therapeutics. Pharmacology, Cell-penetrating peptide, Molecular Medicine, Original Article, sense organs, Neurovetenskaper

Abstract

RNA interference (RNAi) using short interfering RNA (siRNA) is an attractive therapeutic approach for treatment of dominant-negative mutations. Some rare missense dominant-negative mutations lead to congenital-hearing impairments. A variety of viral vectors have been tested with variable efficacy for modulating gene expression in inner ear. However, there is concern regarding their safety for clinical use. Here, we report a novel cell-penetrating peptide (CPP)-based nonviral approach for delivering siRNA into inner ear tissue using organotypic cultures as model system. PepFect6 (PF6), a variant of stearyl-TP10, was specially designed for improved delivery of siRNA by facilitating endosomal release. We show that PF6 was internalized by all cells without inducing cytotoxicity in cochlear cultures. PF6/siRNA nanoparticles lead to knockdown of target genes, a housekeeping gene and supporting cell-specific connexin 26. Interestingly, application of PF6/connexin 26 siRNA exhibited knockdown of both connexin 26 and 30 mRNA and their absence led to impaired intercellular communication as demonstrated by reduced transfer of calcein among the PF6/connexin 26-siRNA-treated cells. Thus, we conclude that PF6 is an efficient nonviral vector for delivery of siRNA, which can be applied as a tool for the development of siRNA-based therapeutic applications for hearing impairments.Molecular Therapy - Nucleic Acids (2012) 1, e61; doi:10.1038/mtna.2012.50; published online 11 December 2012.

Published

2012

107. Cell-Penetrating Penta-Peptides (CPP5s): Measurement of Cell Entry and Protein-Transduction Activity

Author

Masaru Miyagi, Vivian Gama, Dagmar Hajkova, Shigemi Matsuyama, Justine Ngo, Joseph Chen, Jose A. Gomez, and I-Ju Yeh

Subjects

lcsh:Medicine, lcsh:RS1-441, Pharmaceutical Science, Apoptosis, 02 engineering and technology, Biology, Endocytosis, Article, Green fluorescent protein, lcsh:Pharmacy and materia medica, 03 medical and health sciences, chemistry.chemical_compound, Cell-Penetrating Peptide (CPP), Cell-Penetrating Penta-peptide (CPP5), Bax Inhibiting Peptide (BIP), Protein Transduction, Ku70, Bax, Apoptosis, Drug Delivery, Drug Discovery, Ku70, 030304 developmental biology, Cytochalasin D, Protein Transduction, Cell-Penetrating Peptide (CPP), 0303 health sciences, Pinocytosis, Chinese hamster ovary cell, lcsh:R, 021001 nanoscience & nanotechnology, Nocodazole, Bax Inhibiting Peptide (BIP), chemistry, Cell-Penetrating Penta-peptide (CPP5), Bax, Cell culture, Immunology, Biophysics, Molecular Medicine, Drug Delivery, 0210 nano-technology, Intracellular

Abstract

Previously, we developed cell-penetrating penta-peptides (CPP5s). In the present study, VPTLK and KLPVM, two representative CPP5s, were used to characterize the cell-penetration and protein-transduction activities of these small molecules. Various inhibitors of endocytosis and pinocytosis (chlorpromazine, cytochalasin D, Filipin III, amiloride, methyl-β-cyclodextrin, and nocodazole) were tested. Only cytochalasin D showed suppression of CPP5 entry, though the effect was partial. In addition, CPP5s were able to enter a proteoglycan-deficient CHO cell line. These results suggest that pinocytosis and endocytosis may play only a minor role in the cell entry of CPP5s. By mass spectrometry, we determined that the intracellular concentration of VPTLK ranged from 20 nM to 6.0 μM when the cells were cultured in medium containing 1 μM – 1.6 mM VPTLK. To determine the protein-transduction activity of CPP5s, the Tex-LoxP EG cell line, which has a Cre-inducible green fluorescent protein (GFP) gene, was used. VPTLK and KLPVM were added to the N-terminus of Cre, and these fusion proteins were added to the culture medium of Tex-LoxP EG cells. Both VPTLK-Cre and KLPVM-Cre were able to turn on GFP expression in these cells, suggesting that CPP5s have protein-transduction activity. Since CPP5s have very low cytotoxic activity, even at a concentration of 1.6 mM in the medium, CPP5s could be utilized as a new tool for drug delivery into cells.

Published

2010

108. Intracellular Delivery of Short Interfering RNA in Rat Organ of Corti Using a Cell-penetrating Peptide PepFect6

Author

Dash-Wagh, Suvarna, Jacob, Stefan, Lindberg, Staffan, Fridberger, Anders, Langel, Ülo, Ulfendahl, Mats, Dash-Wagh, Suvarna, Jacob, Stefan, Lindberg, Staffan, Fridberger, Anders, Langel, Ülo, and Ulfendahl, Mats

Abstract

RNA interference (RNAi) using short interfering RNA (siRNA) is an attractive therapeutic approach for treatment of dominant-negative mutations. Some rare missense dominant-negative mutations lead to congenital-hearing impairments. A variety of viral vectors have been tested with variable efficacy for modulating gene expression in inner ear. However, there is concern regarding their safety for clinical use. Here, we report a novel cell-penetrating peptide (CPP)-based nonviral approach for delivering siRNA into inner ear tissue using organotypic cultures as model system. PepFect6 (PF6), a variant of stearyl-TP10, was specially designed for improved delivery of siRNA by facilitating endosomal release. We show that PF6 was internalized by all cells without inducing cytotoxicity in cochlear cultures. PF6/siRNA nanoparticles lead to knockdown of target genes, a housekeeping gene and supporting cell-specific connexin 26. Interestingly, application of PF6/connexin 26 siRNA exhibited knockdown of both connexin 26 and 30 mRNA and their absence led to impaired intercellular communication as demonstrated by reduced transfer of calcein among the PF6/connexin 26-siRNA-treated cells. Thus, we conclude that PF6 is an efficient nonviral vector for delivery of siRNA, which can be applied as a tool for the development of siRNA-based therapeutic applications for hearing impairments.

Published

2012

109. The non-enzymatic RAS effector RASSF7 inhibits oncogenic c-Myc function.

Author

Kumaraswamy A, Mamidi A, Desai P, Sivagnanam A, Perumalsamy LR, Ramakrishnan C, Gromiha M, Rajalingam K, and Mahalingam S

Subjects

Basic Helix-Loop-Helix Leucine Zipper Transcription Factors chemistry, Basic Helix-Loop-Helix Leucine Zipper Transcription Factors metabolism, Binding Sites, Binding, Competitive, Cell Line, Cell Transformation, Neoplastic metabolism, Cell Transformation, Neoplastic pathology, Cullin Proteins genetics, Cullin Proteins metabolism, HCT116 Cells, HEK293 Cells, Humans, Models, Molecular, Polyubiquitin genetics, Polyubiquitin metabolism, Promoter Regions, Genetic, Protein Binding, Protein Conformation, alpha-Helical, Protein Conformation, beta-Strand, Protein Interaction Domains and Motifs, Protein Multimerization, Proteolysis, Proto-Oncogene Mas, Proto-Oncogene Proteins c-myc chemistry, Proto-Oncogene Proteins c-myc metabolism, Signal Transduction, Transcription Factors chemistry, Transcription Factors metabolism, Transcription, Genetic, Basic Helix-Loop-Helix Leucine Zipper Transcription Factors genetics, Cell Transformation, Neoplastic genetics, Gene Expression Regulation, Neoplastic, Proto-Oncogene Proteins c-myc genetics, Transcription Factors genetics

Abstract

c-Myc is a proto-oncogene controlling expression of multiple genes involved in cell growth and differentiation. Although the functional role of c-Myc as a transcriptional regulator has been intensively studied, targeting this protein in cancer remains a challenge. Here, we report a trimodal regulation of c-Myc function by the Ras effector, Ras-association domain family member 7 (RASSF7), a nonenzymatic protein modulating protein-protein interactions to regulate cell proliferation. Using HEK293T and HeLa cell lines, we provide evidence that RASSF7 destabilizes the c-Myc protein by promoting Cullin4B-mediated polyubiquitination and degradation. Furthermore, RASSF7 competed with MYC-associated factor X (MAX) in the formation of a heterodimeric complex with c-Myc and attenuated its occupancy on target gene promoters to regulate transcription. Consequently, RASSF7 inhibited c-Myc-mediated oncogenic transformation, and an inverse correlation between the expression levels of the RASSF7 and c-Myc genes was evident in human cancers. Furthermore, we found that RASSF7 interacts with c-Myc via its RA and leucine zipper (LZ) domains and LZ domain peptide is sufficient to inhibit c-Myc function, suggesting that this peptide might be used to target oncogenic c-Myc. These results unveil that RASSF7 and c-Myc are functionally linked in the control of tumorigenesis and open up potential therapeutic avenues for targeting the "undruggable" c-Myc protein in a subset of human cancers., (© 2018 Kumaraswamy et al.)

Published

2018

110. Highly efficient cellular uptake of a cell-penetrating peptide (CPP) derived from the capsid protein of porcine circovirus type 2.

Author

Yu W, Zhan Y, Xue B, Dong Y, Wang Y, Jiang P, Wang A, Sun Y, and Yang Y

Subjects

Animals, Antibodies, Viral chemistry, Antibodies, Viral immunology, Capsid Proteins chemistry, Capsid Proteins pharmacology, Cell-Penetrating Peptides chemistry, Cell-Penetrating Peptides pharmacology, Circovirus chemistry, Circovirus genetics, DNA, Single-Stranded chemistry, DNA, Single-Stranded genetics, DNA, Viral chemistry, DNA, Viral genetics, DNA, Viral pharmacology, Epitopes chemistry, Epitopes genetics, Epitopes immunology, Humans, Nuclear Localization Signals chemistry, Swine, rev Gene Products, Human Immunodeficiency Virus chemistry, Capsid Proteins genetics, Cell-Penetrating Peptides genetics, Nuclear Localization Signals genetics, rev Gene Products, Human Immunodeficiency Virus genetics

Abstract

Porcine circovirus type 2 (PCV2) is one of the smallest, nonenveloped, single-stranded DNA viruses. The PCV2 capsid protein (Cap) is the sole viral structural protein and main antigenic determinant. Previous sequence analysis has revealed that the N terminus of the PCV2 Cap contains a nuclear localization signal (NLS) enriched in positively charged residues. Here, we report that PCV2's NLS can function as a cell-penetrating peptide (CPP). We observed that this NLS can carry macromolecules, e.g. enhanced GFP (EGFP), into cells when they are fused to the NLS, indicating that it can function as a CPP, similar to the classical CPP derived from HIV type 1 transactivator of transcription protein (HIV TAT). We also found that the first 17 residues of the NLS (NLS-A) have a key role in cellular uptake. In addition to entering cells via multiple endocytic processes, NLS-A was also rapidly internalized via direct translocation enabled by increased membrane permeability and was evenly distributed throughout cells when its concentration in cell cultures was ≥10 μm Of note, cellular NLS-A uptake was ∼10 times more efficient than that of HIV TAT. We inferred that the externalized NLS of the PCV2 Cap may accumulate to a high concentration (≥10 μm) at a local membrane area, increasing membrane permeability to facilitate viral entry into the cell to release its genome into a viral DNA reproduction center. We conclude that NLS-A has potential as a versatile vehicle for shuttling foreign molecules into cells, including pharmaceuticals for therapeutic interventions., (© 2018 Yu et al.)

Published

2018

111. Improved Protein Toxin Delivery Based on ATTEMPTS Systems.

Author

Chen Y, Zhang M, Min KA, Wang H, Shin MC, Li F, Yang VC, and Huang Y

Subjects

Animals, Cell-Penetrating Peptides chemistry, Humans, Ligands, Neoplasms drug therapy, Ribosome Inactivating Proteins chemistry, Antineoplastic Agents, Immunological chemistry, Cell-Penetrating Peptides administration & dosage, Drug Delivery Systems methods, Ribosome Inactivating Proteins administration & dosage

Abstract

Background: Ribosome-inactivating proteins (RIPs) are wildly found in multiple species of plants, bacteria and fungi. As a special family of protein toxins, RIPs can inhibit protein synthesis and induce cell death via inactivating ribosome in eukaryotic cells. Thus, RIPs have been applied for anti-tumor therapy in the past two decades. However, because of poor cell permeability, nonselective mode of action for tumor cells, poor pharmacokinetic profiles and immunogenicity, their clinical application has been severely constrained. As an effort to overcome these obstacles, tumor-specific monoclonal antibodies (mAb) have been conjugated to RIPs (forming so called "immunotoxins") specifically to increase their cytotoxicity and provide tumor targeting. Nevertheless, immunotoxins yet have not fully resolved all the issues and critical challenges still remain, such as immunogenicity and inability to penetrate into the deep site of tumor., Objective: To overcome the constrain of immunotoxins, the novel cell-penetrating peptide (CPP)- modified ATTEMPTS systems based on combination of CPP-mediated penetration and antibodymediated tumor targeting, with triggerable drug release function, were developed to achieve effective and safe delivery of protein toxin., Results: The CPP-modified ATTEMPTS systems showed effective protamine-triggered CPP-toxin release and thus enhanced CPP-mediated cellular uptake and cytotoxicity. It also showed antibodymediated in vivo tumor targeting and significantly increased in vivo tumor growth suppression with limited systematic toxicity., Conclusion: The CPP-modified ATTEMPTS systems were developed and demonstrated as a proof-ofconcept for CPP-based protein toxin delivery with triggerable antibody targeting to improve the druggability of protein toxin drugs. The systems showed the potential application of protein toxin clinical translation in anticancer treatment., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.org.)

Published

2018

112. Cell-penetrating peptides derived from Clostridium difficile TcdB2 and a related large clostridial toxin.

Author

Larabee JL, Hauck GD, and Ballard JD

Subjects

Amiloride pharmacology, Animals, CHO Cells, Cricetulus, Pinocytosis drug effects, Bacterial Proteins chemistry, Bacterial Proteins pharmacokinetics, Bacterial Proteins pharmacology, Bacterial Toxins chemistry, Bacterial Toxins pharmacokinetics, Bacterial Toxins pharmacology, Cell-Penetrating Peptides chemistry, Cell-Penetrating Peptides pharmacokinetics, Cell-Penetrating Peptides pharmacology, Clostridioides difficile chemistry, Enterotoxins chemistry, Enterotoxins pharmacokinetics, Enterotoxins pharmacology

Abstract

Clostridium difficile TcdB (2366 amino acid residues) is an intracellular bacterial toxin that binds to cells and enters the cytosol where it glucosylates small GTPases. In the current study, we examined a putative cell entry region of TcdB (amino acid residues 1753-1851) for short sequences that function as cell-penetrating peptides (CPPs). To screen for TcdB-derived CPPs, a panel of synthetic peptides was tested for the ability to enhance transferrin (Tf) association with cells. Four candidate CPPs were discovered, and further study on one peptide (PepB2) pinpointed an asparagine residue necessary for CPP activity. PepB2 mediated the cell entry of a wide variety of molecules including dextran, streptavidin, microspheres, and lentivirus particles. Of note, this uptake was dramatically reduced in the presence of the Na + /H + exchange blocker and micropinocytosis inhibitor amiloride, suggesting that PepB2 invokes macropinocytosis. Moreover, we found that PepB2 had more efficient cell-penetrating activity than several other well-known CPPs (TAT, penetratin, Pep-1, and TP10). Finally, Tf assay-based screening of peptides derived from two other large clostridial toxins, TcdA and TcsL, uncovered two new TcdA-derived CPPs. In conclusion, we have identified six CPPs from large clostridial toxins and have demonstrated the ability of PepB2 to promote cell association and entry of several molecules through a putative fluid-phase macropinocytotic mechanism., (© 2018 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2018

113. Delineating distinct heme-scavenging and -binding functions of domains in MF6p/helminth defense molecule (HDM) proteins from parasitic flatworms.

Author

Martínez-Sernández V, Mezo M, González-Warleta M, Perteguer MJ, Gárate T, Romarís F, and Ubeira FM

Subjects

Animals, Carrier Proteins genetics, Carrier Proteins metabolism, Cattle, Fasciola hepatica genetics, Fasciola hepatica metabolism, Helminth Proteins genetics, Helminth Proteins metabolism, Heme metabolism, Opisthorchis genetics, Opisthorchis metabolism, Paragonimus westermani genetics, Paragonimus westermani metabolism, Protein Domains, Carrier Proteins chemistry, Fasciola hepatica chemistry, Helminth Proteins chemistry, Heme chemistry, Opisthorchis chemistry, Paragonimus westermani chemistry

Abstract

MF6p/FhHDM-1 is a small protein secreted by the parasitic flatworm (trematode) Fasciola hepatica that belongs to a broad family of heme-binding proteins (MF6p/helminth defense molecules (HDMs)). MF6p/HDMs are of interest for understanding heme homeostasis in trematodes and as potential targets for the development of new flukicides. Moreover, interest in these molecules has also increased because of their immunomodulatory properties. Here we have extended our previous findings on the mechanism of MF6p/HDM-heme interactions and mapped the protein regions required for heme binding and for other biological functions. Our data revealed that MF6p/FhHDM-1 forms high-molecular-weight complexes when associated with heme and that these complexes are reorganized by a stacking procedure to form fibril-like and granular nanostructures. Furthermore, we showed that MF6p/FhHDM-1 is a transitory heme-binding protein as protein·heme complexes can be disrupted by contact with an apoprotein ( e.g. apomyoglobin) with higher affinity for heme. We also demonstrated that (i) the heme-binding region is located in the MF6p/FhHDM-1 C-terminal moiety, which also inhibits the peroxidase-like activity of heme, and (ii) MF6p/HDMs from other trematodes, such as Opisthorchis viverrini and Paragonimus westermani , also bind heme. Finally, we observed that the N-terminal, but not the C-terminal, moiety of MF6p/HDMs has a predicted structural analogy with cell-penetrating peptides and that both the entire protein and the peptide corresponding to the N-terminal moiety of MF6p/FhHDM-1 interact in vitro with cell membranes in hemin-preconditioned erythrocytes. Our findings suggest that MF6p/HDMs can transport heme in trematodes and thereby shield the parasite from the harmful effects of heme., (© 2017 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2017

114. An l- to d-Amino Acid Conversion in an Endosomolytic Analog of the Cell-penetrating Peptide TAT Influences Proteolytic Stability, Endocytic Uptake, and Endosomal Escape.

Author

Najjar K, Erazo-Oliveras A, Brock DJ, Wang TY, and Pellois JP

Subjects

Amino Acids pharmacokinetics, Amino Acids pharmacology, Cell-Penetrating Peptides pharmacokinetics, Cell-Penetrating Peptides pharmacology, Endosomes chemistry, Endosomes metabolism, HeLa Cells, Humans, Amino Acids chemistry, Cell-Penetrating Peptides chemistry, Models, Molecular

Abstract

Cell-penetrating peptides (CPPs) are well established as delivery agents for otherwise cell-impermeable cargos. CPPs can also theoretically be used to modulate intracellular processes. However, their susceptibility to proteolytic degradation often limits their utility in these applications. Previous studies have explored the consequences for cellular uptake of converting the residues in CPPs from l- to d-stereochemistry, but conflicting results have been reported and specific steps en route to intracellular activity have not been explored. Here we use dimeric fluorescence TAT as a model CPP to explore the broader consequences of l- to d-stereochemical conversion. We show that inversion of chirality provides protease resistance without altering the overall mode of cellular entry, a process involving endocytic uptake followed by endosomal escape and cytosolic access. However, whereas inversion of chirality reduces endocytic uptake, the d-peptide, once in the endosome, is significantly more prone to escape than its l-counterpart. Moreover, the d-peptide is retained in the cytosol of cells for several days, whereas the l-peptide is degraded within hours. Notably, while the l-peptide is relatively innocuous to cells, the d-peptide exerts a prolonged anti-proliferative activity. Together, our results establish connections between chirality, protease resistance, cellular penetration, and intracellular activity that may be useful for the development of future delivery agents with improved properties., (© 2017 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2017

115. Cell Adhesion Induced Using Surface Modification with Cell-Penetrating Peptide-Conjugated Poly(ethylene glycol)-Lipid: A New Cell Glue for 3D Cell-Based Structures.

Author

Teramura Y, Asif S, Ekdahl KN, Gustafson E, and Nilsson B

Abstract

We synthesized a novel material, cell-penetrating peptide-conjugated poly(ethylene glycol)-lipid (CPP-PEG-lipid), that can induce the adhesion of floating cells. Firm cell adhesion with spreading could be induced by cell surface modification with the CPP-PEG-lipids. Cell adhesion was induced by CPPs but not by any other cationic short peptides we tested. Here, we demonstrated adherence using the floating cell line CCRF-CEM as well as primary human T cells, B cells, erythrocytes, and hepatocytes. As compared to cells grown in suspension, adherent cells were more rapidly induced to attach to substrates with the cell-surface modification. The critical factor for attachment was localization of CPPs at the cell membrane by PEG-lipids with PEG > 20 kDa. These cationic CPPs on PEG chains were able to interact with substrate surfaces such as polystyrene (PS) surfaces, glass surfaces, and PS microfibers that are negatively charged, inducing firm cell adhesion and cell spreading. Also, as opposed to normal cationic peptides that interact strongly with cell membranes, CPPs were less interactive with the cell surfaces because of their cell-penetrating property, making them more available for adhering cells to the substrate surface. No effects on cell viability or cell proliferation were observed after the induction of cell adhesion. With this technique, cells could be easily immobilized onto PS microfibers, an important step in fabricating 3D cell-based structures. Cells immobilized onto 3D PS microfibers were alive, and human hepatocytes showed normal production of urea and albumin on the microfibers. This method is novel in inducing firm cell adhesion via a one-step treatment.

Published

2017

116. Evaluating the Delivery of Proteins to the Cytosol of Mammalian Cells.

Author

Marschall AL, Zhang C, and Dübel S

Subjects

Animals, Cell Line, Cell-Penetrating Peptides chemistry, Fibroblasts cytology, Fibroblasts metabolism, Flow Cytometry, HeLa Cells, Humans, Integrases genetics, Integrases metabolism, Myosins immunology, Myosins metabolism, Plasmids chemistry, Plasmids metabolism, Tissue Fixation methods, Tubulin immunology, Tubulin metabolism, Cell-Penetrating Peptides metabolism, Cytosol metabolism, Drug Carriers, Electroporation methods, Single-Chain Antibodies metabolism

Abstract

Delivery of proteins to the cytosol of living cells is a promising research tool. Delivery of antibodies in particular bears exciting applications such as in vivo tracking of proteins at endogenous expression levels or interference with cellular processes. In spite of the large number of methods published for protein delivery, successful applications so far are rare. A possible explanation for this is a vast overestimation of the delivery efficiency due to the use of inappropriate detection methods and/or unsuitable positive controls for cytosolic delivery. Therefore, we provide strategies for unequivocally detecting cytoplasmic protein delivery and quantifying protein transformation efficiency. Finally, we present a protocol for efficient protein delivery to the cytosol validated using these methods.

Published

2017

117. Mechanism of Four de Novo Designed Antimicrobial Peptides.

Author

Murray B, Pearson CS, Aranjo A, Cherupalla D, and Belfort G

Subjects

Antimicrobial Cationic Peptides chemical synthesis, Quartz Crystal Microbalance Techniques, Antimicrobial Cationic Peptides chemistry, Lipid Bilayers chemistry, Models, Chemical

Abstract

As pathogenic bacteria become resistant to traditional antibiotics, alternate approaches such as designing and testing new potent selective antimicrobial peptides (AMP) are increasingly attractive. However, whereas much is known regarding the relationship between the AMP sequence and potency, less research has focused on developing links between AMP properties, such as design and structure, with mechanisms. Here we use four natural AMPs of varying known secondary structures and mechanisms of lipid bilayer disruption as controls to determine the mechanisms of four rationally designed AMPs with similar secondary structures and rearranged amino acid sequences. Using a Quartz Crystal Microbalance with Dissipation, we were able to differentiate between molecular models of AMP actions such as barrel-stave pore formation, toroidal pore formation, and peptide insertion mechanisms by quantifying differential frequencies throughout an oscillating supported lipid bilayer. Barrel-stave pores were identified by uniform frequency modulation, whereas toroidal pores possessed characteristic changes in oscillation frequency throughout the bilayer. The resulting modes of action demonstrate that rearrangement of an amino acid sequence of the AMP resulted in identical overall mechanisms, and that a given secondary structure did not necessarily predict mechanism. Also, increased mass addition to Gram-positive mimetic membranes from AMP disruption corresponded with lower minimum inhibitory concentrations against the Gram-positive Staphylococcus aureus., (© 2016 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2016

118. Targeting Liver Fibrosis with a Cell-penetrating Protease-activated Receptor-2 (PAR2) Pepducin.

Author

Shearer AM, Rana R, Austin K, Baleja JD, Nguyen N, Bohm A, Covic L, and Kuliopulos A

Subjects

Animals, Hepatocytes, Humans, Liver drug effects, Liver metabolism, Liver Cirrhosis genetics, Liver Cirrhosis metabolism, Male, Mice, Mice, Inbred C57BL, Reactive Oxygen Species metabolism, Receptor, PAR-2 antagonists & inhibitors, Receptor, PAR-2 genetics, Lipopeptides administration & dosage, Liver Cirrhosis prevention & control, Receptor, PAR-2 metabolism

Abstract

Chronic liver inflammation and fibrosis in nonalcoholic steatohepatitis can lead to cirrhosis and liver failure for which there are currently no approved treatments. Protease-activated receptor-2 (PAR2) is an emerging new target expressed on liver stellate cells and hepatocytes that regulates the response to liver injury and inflammation. Here, we identified a pepducin to block the deleterious actions of PAR2 in promoting liver fibrosis. Non-alcoholic fatty liver disease and early fibrosis were induced by the methionine-choline-deficient diet in mice. Fibrotic liver disease was induced by administering carbon tetrachloride for 8 weeks. Mice were treated with the pepducin PZ-235 either from onset of the experiment or after fibrosis was established. Hepatic fibrosis, collagen content, inflammatory cytokines, steatosis, triglycerides, and NAFLD activity score were assessed as primary outcome parameters depending on the model. The activity of the PAR2 pepducin on cultured stellate cell activation and hepatocyte reactive oxygen species production was evaluated. PZ-235 significantly suppressed liver fibrosis, collagen deposition, inflammatory cytokines, NAFLD activity score, steatosis, triglycerides, aspartate transaminase, alanine transaminase, and stellate cell proliferation by up to 50-100%. The PAR2 inhibitor afforded significant protective effects against hepatocellular necrosis and attenuated PAR2-mediated reactive oxygen species production in hepatocytes. PZ-235 was distributed to liver and other mouse tissues and was found to form a well structured α-helix that closely resembles the juxtamembrane helical region of the analogous TM6 and third intracellular region of the intact receptor that is critical for coupling to internal G proteins. The ability of PZ-235 to effectively suppress fibrosis, hepatocellular necrosis, reactive oxygen species production, steatosis, and inflammation indicates the potential for PAR2 pepducin inhibitors to be broadly efficacious in the treatment of liver fibrosis., (© 2016 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2016

119. TIPE2 (Tumor Necrosis Factor α-induced Protein 8-like 2) Is a Novel Negative Regulator of TAK1 Signal.

Author

Oho M, Nakano R, Nakayama R, Sakurai W, Miyamoto A, Masuhiro Y, and Hanazawa S

Subjects

Adaptor Proteins, Signal Transducing genetics, Adaptor Proteins, Signal Transducing metabolism, Animals, Humans, Intracellular Signaling Peptides and Proteins genetics, Lipopolysaccharides pharmacology, MAP Kinase Kinase Kinases genetics, Male, Mice, RAW 264.7 Cells, Toll-Like Receptor 4 agonists, Toll-Like Receptor 4 genetics, Toll-Like Receptor 4 metabolism, Tumor Necrosis Factor-alpha pharmacology, Intracellular Signaling Peptides and Proteins metabolism, MAP Kinase Kinase Kinases metabolism, Signal Transduction, Spleen metabolism, Thymus Gland metabolism

Abstract

TIPE2 (TNF-α-induced protein 8-like 2) is a novel death effector domain protein and is a negative regulator of the innate and adaptive immune response. Although it has been demonstrated that caspase-8 contributes to the negative regulation of TIPE2, the negative regulatory mechanism is not entirely understood. Here, we demonstrate that TIPE2 interacts with TGF-β-activated kinase 1 (TAK1), a crucial regulatory molecule of inflammatory and immune signals, and consequently acts as a powerful negative regulator of TAK1. The interaction between endogenous TIPE2 and TAK1 was observed in RAW264.7 macrophage-like cells and mouse primary cells derived from spleen and thymus. The TIPE2 amino acid 101-140 region interacted with TAK1 by binding to the amino acid 200-291 region of the internal kinase domain of TAK1. TIPE2 interfered with the formation of the TAK1-TAB1-TAB2 complex and subsequently inhibited activation of TAK1 and its downstream molecules. Importantly, silencing TIPE2 through RNA interference attenuated the inhibitory action of TIPE2 on LPS- and TNF-α-stimulated TAK1 activity. Exogenous TIPE2 101-140, the region that interacts with TAK1, also inhibited LPS- and TNF-α-stimulated NF-κB reporter activity. Interestingly, cell-permeable TIPE2 protein maintained its binding ability with TAK1 and exhibited the same inhibitory action of native TIPE2 on TLR4 signaling in vitro Thus, cell-permeable TIPE2 protein is a potential candidate for intracellular protein therapy for TAK1-related diseases. The present study demonstrates that TIPE2 acts as a novel negative regulator of inflammatory and immune responses through TAK1 signaling., (© 2016 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2016

120. Membrane Oxidation Enables the Cytosolic Entry of Polyarginine Cell-penetrating Peptides.

Author

Wang TY, Sun Y, Muthukrishnan N, Erazo-Oliveras A, Najjar K, and Pellois JP

Subjects

Biological Transport, Cell Culture Techniques, Cell Line, Humans, Membrane Lipids metabolism, Oxidation-Reduction, Oxidative Stress, Reactive Oxygen Species metabolism, Cell Membrane metabolism, Cell-Penetrating Peptides metabolism, Cytosol metabolism, Fibroblasts metabolism, Peptides metabolism

Abstract

Arginine-rich peptides can penetrate cells and consequently be used as delivery agents in various cellular applications. The activity of these reagents is often context-dependent, and the parameters that impact cell entry are not fully understood, giving rise to variability and limiting progress toward their usage. Herein, we report that the cytosolic penetration of linear polyarginine peptides is dependent on the oxidation state of the cell. In particular, we find that hypoxia and cellular antioxidants inhibit cell penetration. In contrast, oxidants promote cytosolic cell entry with an efficiency proportional to the level of reactive oxygen species generated within membranes. Moreover, an antibody that binds to oxidized lipids inhibits cell penetration, whereas extracellularly administered pure oxidized lipids enhance peptide transport into cells. Overall, these data indicate that oxidized lipids are capable of mediating the transport of polyarginine peptides across membranes. These data may also explain variability in cell-penetrating peptide performance in different experimental conditions. These new findings therefore provide new opportunities for the rational design of future cell-permeable compounds and for the optimization of delivery protocols., (© 2016 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2016

121. Structure-Function Analysis of the Mcl-1 Protein Identifies a Novel Senescence-regulating Domain.

Author

Demelash A, Pfannenstiel LW, Tannenbaum CS, Li X, Kalady MF, DeVecchio J, and Gastman BR

Subjects

Animals, Antibiotics, Antineoplastic pharmacology, Caco-2 Cells, Cell Line, Tumor, Colorectal Neoplasms drug therapy, Colorectal Neoplasms genetics, Colorectal Neoplasms metabolism, Doxorubicin pharmacology, Female, HCT116 Cells, HT29 Cells, HeLa Cells, Humans, Immunoblotting, Immunohistochemistry, Mice, Nude, Microscopy, Confocal, Models, Molecular, Mutagenesis, Site-Directed, Myeloid Cell Leukemia Sequence 1 Protein chemistry, Protein Structure, Secondary, Protein Structure, Tertiary, RNA Interference, Structure-Activity Relationship, Xenograft Model Antitumor Assays, Aging genetics, Cellular Senescence genetics, Myeloid Cell Leukemia Sequence 1 Protein genetics, Myeloid Cell Leukemia Sequence 1 Protein metabolism

Abstract

Unlike other antiapoptotic Bcl-2 family members, Mcl-1 also mediates resistance to cancer therapy by uniquely inhibiting chemotherapy-induced senescence (CIS). In general, Bcl-2 family members regulate apoptosis at the level of the mitochondria through a common prosurvival binding groove. Through mutagenesis, we determined that Mcl-1 can inhibit CIS even in the absence of its apoptotically important mitochondrion-localizing domains. This finding prompted us to generate a series of Mcl-1 deletion mutants from both the N and C termini of the protein, including one that contained a deletion of all of the Bcl-2 homology domains, none of which impacted anti-CIS capabilities. Through subsequent structure-function analyses of Mcl-1, we identified a previously uncharacterized loop domain responsible for the anti-CIS activity of Mcl-1. The importance of the loop domain was confirmed in multiple tumor types, two in vivo models of senescence, and by demonstrating that a peptide mimetic of the loop domain can effectively inhibit the anti-CIS function of Mcl-1. The results from our studies appear to be highly translatable because we discerned an inverse relationship between the expression of Mcl-1 and of various senescence markers in cancerous human tissues. In summary, our findings regarding the unique structural properties of Mcl-1 provide new approaches for targeted cancer therapy., (© 2015 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2015

122. Allosteric Activation of a G Protein-coupled Receptor with Cell-penetrating Receptor Mimetics.

Author

Zhang P, Leger AJ, Baleja JD, Rana R, Corlin T, Nguyen N, Koukos G, Bohm A, Covic L, and Kuliopulos A

Subjects

Allosteric Regulation genetics, Amino Acid Motifs, Animals, COS Cells, Chlorocebus aethiops, GTP-Binding Protein alpha Subunits genetics, GTP-Binding Protein alpha Subunits metabolism, HEK293 Cells, Humans, Nuclear Magnetic Resonance, Biomolecular, Receptor, PAR-1 genetics, Receptor, PAR-1 metabolism, Biomimetic Materials chemistry, Cell-Penetrating Peptides chemistry, GTP-Binding Protein alpha Subunits chemistry, Receptor, PAR-1 chemistry

Abstract

G protein-coupled receptors (GPCRs) are remarkably versatile signaling systems that are activated by a large number of different agonists on the outside of the cell. However, the inside surface of the receptors that couple to G proteins has not yet been effectively modulated for activity or treatment of diseases. Pepducins are cell-penetrating lipopeptides that have enabled chemical and physical access to the intracellular face of GPCRs. The structure of a third intracellular (i3) loop agonist, pepducin, based on protease-activated receptor-1 (PAR1) was solved by NMR and found to closely resemble the i3 loop structure predicted for the intact receptor in the on-state. Mechanistic studies revealed that the pepducin directly interacts with the intracellular H8 helix region of PAR1 and allosterically activates the receptor through the adjacent (D/N)PXXYYY motif through a dimer-like mechanism. The i3 pepducin enhances PAR1/Gα subunit interactions and induces a conformational change in fluorescently labeled PAR1 in a very similar manner to that induced by thrombin. As pepducins can potentially be made to target any GPCR, these data provide insight into the identification of allosteric modulators to this major drug target class., (© 2015 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2015

123. A+-helix of protein C inhibitor (PCI) is a cell-penetrating peptide that mediates cell membrane permeation of PCI.

Author

Yang H, Wahlmüller FC, Sarg B, Furtmüller M, and Geiger M

Subjects

Animals, Cell Line, Tumor, Cell Membrane Permeability physiology, GPI-Linked Proteins metabolism, Humans, Mice, Serine Endopeptidases metabolism, U937 Cells, Cell-Penetrating Peptides chemistry, Cell-Penetrating Peptides metabolism, Protein C Inhibitor chemistry, Protein C Inhibitor metabolism

Abstract

Protein C inhibitor (PCI) is a serpin with broad protease reactivity. It binds glycosaminoglycans and certain phospholipids that can modulate its inhibitory activity. PCI can penetrate through cellular membranes via binding to phosphatidylethanolamine. The exact mechanism of PCI internalization and the intracellular role of the serpin are not well understood. Here we showed that testisin, a glycosylphosphatidylinositol-anchored serine protease, cleaved human PCI and mouse PCI (mPCI) at their reactive sites as well as at sites close to their N terminus. This cleavage was observed not only with testisin in solution but also with cell membrane-anchored testisin on U937 cells. The cleavage close to the N terminus released peptides rich in basic amino acids. Synthetic peptides corresponding to the released peptides of human PCI (His(1)-Arg(11)) and mPCI (Arg(1)-Ala(18)) functioned as cell-penetrating peptides. Because intact mPCI but not testisin-cleaved mPCI was internalized by Jurkat T cells, a truncated mPCI mimicking testisin-cleaved mPCI was created. The truncated mPCI lacking 18 amino acids at the N terminus was not taken up by Jurkat T cells. Therefore our model suggests that testisin or other proteases could regulate the internalization of PCI by removing its N terminus. This may represent one of the mechanisms regulating the intracellular functions of PCI., (© 2015 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2015

124. Efflux by small multidrug resistance proteins is inhibited by membrane-interactive helix-stapled peptides.

Author

Bellmann-Sickert K, Stone TA, Poulsen BE, and Deber CM

Subjects

Circular Dichroism, Erythrocytes drug effects, Ethidium chemistry, Halobacterium metabolism, Hemolysis, Humans, Lipid Bilayers chemistry, Liver drug effects, Microbial Sensitivity Tests, Protein Interaction Mapping, Protein Multimerization, Protein Structure, Secondary, ATP Binding Cassette Transporter, Subfamily B metabolism, Cell Membrane metabolism, Peptides chemistry

Abstract

Bacterial cell membranes contain several protein pumps that resist the toxic effects of drugs by efficiently extruding them. One family of these pumps, the small multidrug resistance proteins (SMRs), consists of proteins of about 110 residues that need to oligomerize to form a structural pathway for substrate extrusion. As such, SMR oligomerization sites should constitute viable targets for efflux inhibition, by disrupting protein-protein interactions between helical segments. To explore this proposition, we are using Hsmr, an SMR from Halobacter salinarum that dimerizes to extrude toxicants. Our previous work established that (i) Hsmr dimerization is mediated by a helix-helix interface in Hsmr transmembrane (TM) helix 4 (residues (90)GLALIVAGV(98)); and (ii) a peptide comprised of the full TM4(85-105) sequence inhibits Hsmr-mediated ethidium bromide efflux from bacterial cells. Here we define the minimal linear sequence for inhibitor activity (determined as TM4(88-100), and then "staple" this sequence via Grubbs metathesis to produce peptides typified by acetyl-A-(Sar)3-(88)VVGLXLIZXGVVV(100)-KKK-NH2 (X = 2-(4'-pentenyl)alanine at positions 92 and 96; Z = Val, Gly, or Asn at position 95)). The Asn(95) peptide displayed specific efflux inhibition and resensitization of Hsmr-expressing cells to ethidium bromide; and was non-hemolytic to human red blood cells. Stapling essentially prevented peptide degradation in blood plasma and liver homogenates versus an unstapled counterpart. The overall results confirm that the stapled analog of TM4(88-100) retains the structural complementarity required to disrupt the Hsmr TM4-TM4 locus in Hsmr, and portend the general validity of stapled peptides as therapeutics for the disruption of functional protein-protein interactions in membranes., (© 2015 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2015

125. A WXW motif is required for the anticancer activity of the TAT-RasGAP317-326 peptide.

Author

Barras D, Chevalier N, Zoete V, Dempsey R, Lapouge K, Olayioye MA, Michielin O, and Widmann C

Subjects

Amino Acid Sequence, Antineoplastic Agents chemistry, Apoptosis drug effects, Base Sequence, Calorimetry, Cell Line, Tumor, DNA Primers, GTPase-Activating Proteins chemistry, HEK293 Cells, Humans, Models, Molecular, Molecular Sequence Data, Peptide Fragments chemistry, Polymerase Chain Reaction, Structure-Activity Relationship, Amino Acid Motifs, Antineoplastic Agents pharmacology, GTPase-Activating Proteins pharmacology, Peptide Fragments pharmacology

Abstract

TAT-RasGAP317-326, a cell-permeable 10-amino acid-long peptide derived from the N2 fragment of p120 Ras GTPase-activating protein (RasGAP), sensitizes tumor cells to apoptosis induced by various anticancer therapies. This RasGAP-derived peptide, by targeting the deleted in liver cancer-1 (DLC1) tumor suppressor, also hampers cell migration and invasion by promoting cell adherence and by inhibiting cell movement. Here, we systematically investigated the role of each amino acid within the RasGAP317-326 sequence for the anticancer activities of TAT-RasGAP317-326. We report here that the first three amino acids of this sequence, tryptophan, methionine, and tryptophan (WMW), are necessary and sufficient to sensitize cancer cells to cisplatin-induced apoptosis and to reduce cell migration. The WMW motif was found to be critical for the binding of fragment N2 to DLC1. These results define the interaction mode between the active anticancer sequence of RasGAP and DLC1. This knowledge will facilitate the design of small molecules bearing the tumor-sensitizing and antimetastatic activities of TAT-RasGAP317-326., (© 2014 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2014

126. A cell-penetrating antibody fragment against HIV-1 Rev has high antiviral activity: characterization of the paratope.

Author

Zhuang X, Stahl SJ, Watts NR, DiMattia MA, Steven AC, and Wingfield PT

Subjects

Amino Acid Sequence, Anti-HIV Agents chemistry, Anti-HIV Agents immunology, Binding Sites, Antibody genetics, Binding Sites, Antibody immunology, Cell-Penetrating Peptides genetics, Cell-Penetrating Peptides immunology, Complementarity Determining Regions, HEK293 Cells, HIV-1 physiology, Humans, Immunoglobulin Fab Fragments genetics, Immunoglobulin Fab Fragments immunology, Kinetics, Microscopy, Electron, Transmission, Models, Molecular, Molecular Sequence Data, Mutagenesis, Site-Directed, Protein Binding, Protein Engineering, Protein Multimerization drug effects, Virus Replication drug effects, Virus Replication immunology, rev Gene Products, Human Immunodeficiency Virus genetics, rev Gene Products, Human Immunodeficiency Virus metabolism, Anti-HIV Agents pharmacology, Cell-Penetrating Peptides pharmacology, HIV-1 drug effects, HIV-1 immunology, Immunoglobulin Fab Fragments pharmacology, rev Gene Products, Human Immunodeficiency Virus antagonists & inhibitors

Abstract

The HIV-1 protein Rev oligomerizes on viral transcripts and directs their nuclear export. Previously, a Fab against Rev generated by phage display was used to crystallize and solve the structure of the Rev oligomerization domain. Here we have investigated the capability of this Fab to block Rev oligomerization and inhibit HIV-1 replication. The Fab itself did not have antiviral activity, but when a Tat-derived cell-penetrating peptide was appended, the resulting molecule (FabRev1-Tat) was strongly inhibitory of three different CCR5-tropic HIV-1 isolates (IC50 = 0.09-0.44 μg/ml), as assessed by suppression of reverse transcriptase activity in infected peripheral blood mononuclear cells, and had low cell toxicity (TC50 > 100 μg/ml). FabRev1-Tat was taken up by both peripheral blood mononuclear and HEK293T cells, appearing in both the cytoplasm and nucleus, as shown by immunofluorescence confocal laser scanning microscopy. Computational alanine scanning was used to identify key residues in the complementarity-determining regions to guide mutagenesis experiments. Residues in the light chain CDR3 (LCDR3) were assessed to be important. Residues in LCDR3 were mutated, and LCDR3-Tyr(92) was found to be critical for binding to Rev, as judged by surface plasmon resonance and electron microscopy. Peptides corresponding to all six CDR regions were synthesized and tested for Rev binding. None of the linear peptides had significant affinity for Rev, but four of the amide-cyclic forms did. Especially cyclic-LCDR3 (LGGYPAASYRTA) had high affinity for Rev and was able to effectively depolymerize Rev filaments, as shown by both surface plasmon resonance and electron microscopy., (© 2014 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2014

127. Increased membrane surface positive charge and altered membrane fluidity leads to cationic antimicrobial peptide resistance in Enterococcus faecalis

Author

Yudhishthir S. Rajput, S. K. Sood, Neha Saini, Rashmi Kumariya, and Anita Kumari Garsa

Subjects

Antimicrobial peptide (AMP), Cations, Divalent, Membrane Fluidity, Polymers, Mutant, Biophysics, Phospholipid, Peptide, Microbial Sensitivity Tests, Biochemistry, Enterococcus faecalis, Cell-penetrating peptide (CPP), Cell membrane, chemistry.chemical_compound, medicine, Membrane fluidity, Magnesium, Phospholipids, Unilamellar Liposomes, Electrophoresis, Agar Gel, chemistry.chemical_classification, biology, Cell Membrane, Fatty Acids, Polyynes, Cell Biology, Membrane lipid, Fluoresceins, biology.organism_classification, Polyacetylene Polymer, In vitro, Membrane, medicine.anatomical_structure, chemistry, Drug resistance, Mutation, Phospholipid vesicle, Colorimetry, Chromatography, Thin Layer, Antimicrobial Cationic Peptides

Abstract

To understand the role of cell membrane phospholipids during resistance development to cationic antimicrobial peptides (CAMPs) in Enterococcus faecalis, gradual dose-dependent single exposure pediocin-resistant (Pedr) mutants of E. faecalis (Efv2.1, Efv3.1, Efv3.2, Efv4.1, Efv4.2, Efv5.1, Efv5.2 and Efv5.3), conferring simultaneous resistance to other CAMPs, selected in previous study were characterized for cell membrane phospholipid head-groups and fatty acid composition. The involvement of phospholipids in resistance acquisition was confirmed by in vitro colorimetric assay using PDA (polydiacetylene)-biomimetic membranes. Estimation of ratio of amino-containing phospholipids to amino-lacking phospholipids suggests that phospholipids in cell membrane of Pedr mutants loose anionic character. At moderate level of resistance, the cell-membrane becomes neutralized while at further higher level of resistance, the cell-surface acquired positive charge. Increased expression of mprF gene (responsible for lysinylation of phospholipids) was also observed on acquiring resistance to pediocin in Pedr E. faecalis. Decreased level of branched chain fatty acids in Pedr mutants might have contributed in enhancing rigidification of cell membrane and contributing towards resistance. The interaction of pediocin with PDA-biomimetic membranes prepared from wild-type and Pedr mutants was monitored by measuring percent colorimetric response (%CR). Increased %CR of pediocin against PDA-biomimetic membranes prepared from Pedr mutants confirmed that cell membrane phospholipids are involved in the interactions of pore formation by CAMPs. There was a direct linear relationship between percent colorimetric response and IC50 of CAMPs for wild-type and Pedr mutants. This relationship further reveals that in vitro colorimetric assay can be used effectively for quantification of resistance to CAMPs.

128. PEGylated enhanced cell penetrating peptide nanoparticles for lung gene therapy

Author

Justin Hanes, Gizem Osman, Jane Chisholm, Sze Yan Chan, Namho Kim, Kevin M. Shakesheff, Jung Soo Suk, Amanda L. Tatler, James E. Dixon, Jason Rodriguez, and Gregg A. Duncan

Subjects

0301 basic medicine, Biodistribution, Cystic Fibrosis, Genetic enhancement, Plasmid DNA (pDNA), Pharmaceutical Science, Cell-Penetrating Peptides, 02 engineering and technology, Vectors in gene therapy, Transfection, Article, Cell Line, Polyethylene Glycols, Cell-penetrating peptide (CPP), Mice, 03 medical and health sciences, Gene therapy, In vivo, Animals, Humans, Lung, Glycosaminoglycans, Chemistry, Gene Transfer Techniques, DNA, Genetic Therapy, 021001 nanoscience & nanotechnology, Glycosaminoglycan-binding enhanced transduction (GET), 3. Good health, Cell biology, 030104 developmental biology, transduction (GET), Glycosaminoglycan-binding enhanced, PEGylation, Cell-penetrating peptide, Nanoparticles, 0210 nano-technology, Ex vivo

Abstract

The lung remains an attractive target for the gene therapy of monogenetic diseases such as cystic fibrosis (CF). Despite over 27 clinical trials, there are still very few gene therapy vectors that have shown any improvement in lung function; highlighting the need to develop formulations with improved gene transfer potency and the desirable physiochemical characteristics for efficacious therapy. Herein, we introduce a novel cell penetrating peptide (CPP)-based non-viral vector that utilises glycosaminoglycan (GAG)-binding enhanced transduction (GET) for highly efficient gene transfer. GET peptides couple directly with DNA through electrostatic interactions to form nanoparticles (NPs). In order to adapt the GET peptide for efficient in vivo delivery, we engineered PEGylated versions of the peptide and employed a strategy to form DNA NPs with different densities of PEG coatings. We were able to identify candidate formulations (PEGylation rates ≥ 40%) that shielded the positively charged surface of particles, maintained colloidal stability in bronchoalveolar lavage fluid (BALF) and retained gene transfer activity in human bronchial epithelial cell lines and precision cut lung slices (PCLS) in vitro. Using multiple particle tracking (MPT) technology, we demonstrated that PEG-GET complexes were able to navigate the mucus mesh and diffuse rapidly through patient CF sputum samples ex vivo. When tested in mouse lung models in vivo, PEGylated particles demonstrated superior biodistribution, improved safety profiles and efficient gene transfer of a reporter luciferase plasmid compared to non-PEGylated complexes. Furthermore, gene expression was significantly enhanced in comparison to polyethylenimine (PEI), a non-viral gene carrier that has been widely tested in pre-clinical settings. This work describes an innovative approach that combines novel GET peptides for enhanced transfection with a tuneable PEG coating for efficacious lung gene therapy.