Your search keyword '"Pierpaolo Ceci"' showing total 66 results

1. Nose-to-brain selective drug delivery to glioma via ferritin-based nanovectors reduces tumor growth and improves survival rate

Author

Francesco Marrocco, Elisabetta Falvo, Luciana Mosca, Giada Tisci, Alessandro Arcovito, Alice Reccagni, Cristina Limatola, Roberta Bernardini, Pierpaolo Ceci, Giuseppina D’Alessandro, and Gianni Colotti

Subjects

Cytology, QH573-671

Abstract

Abstract Gliomas are among the most fatal tumors, and the available therapeutic options are very limited. Additionally, the blood-brain barrier (BBB) prevents most drugs from entering the brain. We designed and produced a ferritin-based stimuli-sensitive nanocarrier with high biocompatibility and water solubility. It can incorporate high amounts of the potent topoisomerase 1 inhibitor Genz-644282. Here, we show that this nanocarrier, named The-0504, can cross the BBB and specifically deliver the payload to gliomas that express high amounts of the ferritin/transferrin receptor TfR1 (CD71). Intranasal or intravenous administration of The-0504 both reduce tumor growth and improve the survival rate of glioma-bearing mice. However, nose-to-brain administration is a simpler and less invasive route that may spare most of the healthy tissues compared to intravenous injections. For this reason, the data reported here could pave the way towards a new, safe, and direct ferritin-based drug delivery method for brain diseases, especially brain tumors.

Published

2024

2. Widespread in vivo efficacy of The-0504: A conditionally-activatable nanoferritin for tumor-agnostic targeting of CD71-expressing cancers

Author

Giulio Fracasso, Elisabetta Falvo, Giada Tisci, Gianluca Sala, Gianni Colotti, Sara Cingarlini, Claudia Tito, Sandra Bibbo, Cristina Frusteri, Elisa Tremante, Elena Giordani, Patrizio Giacomini, and Pierpaolo Ceci

Subjects

Targeted therapy, Solid cancer, Human ferritin, Transferrin receptor (CD71), Genz-644282, Science (General), Q1-390, Social sciences (General), H1-99

Abstract

Background: Cancer is still among the leading causes of death all over the world. Improving chemotherapy and minimizing associated toxicities are major unmet medical needs. Recently, we provided a preliminary preclinical evaluation of a human ferritin (HFt)-based drug carrier (The-0504) that selectively delivers the wide-spectrum topoisomerase I inhibitor Genz-644282 to CD71-expressing tumors. The-0504 has so far been evaluated on four different human tumor xenotransplant models (breast, colorectal, pancreatic and liver cancers). Methods: Herein, we extend our studies, by: (a) testing DNA damage in vitro, (b) treating eight additional tumor xenograft models in vivo with The-0504; (c) performing pharmacokinetic (PK) studies in rats; and (d) evaluating The-0504 anti-tumor xenotransplant efficacy by optimizing its administration schedule based on PK considerations. Results: Immunofluorescence demonstrated that The-0504 induces foci expressing the DNA double-strand break marker γH2AX. Expression increases up to 4-fold and is more persistent as compared to free Genz-644282. In vivo studies confirmed a remarkable anti-tumor activity of The-0504, resulting in tumor eradication in most murine xenograft models, regardless of embryological origin (e.g. epithelial, mesenchymal or neuroendocrine), and molecular subtypes. PK studies demonstrated a long persistence of The-0504 in rat serum (half-life of about 40 h as compared to 15 h of the free drug), with a 400-fold increase in peak concentrations as compared to the free drug. On this basis, we reduced The-0504 administration frequency from twice to once per week, with no appreciable loss in therapeutic efficacy in mice. Conclusion: The results presented here confirm that The-0504 is highly active against several human tumor xenotransplants, even when administered less frequently than previously reported. The-0504 may be a good candidate for further clinical development in a tumor histotype-agnostic setting.

Published

2023

3. High activity and low toxicity of a novel CD71-targeting nanotherapeutic named The-0504 on preclinical models of several human aggressive tumors

Author

Elisabetta Falvo, Verena Damiani, Giamaica Conti, Federico Boschi, Katia Messana, Patrizio Giacomini, Michele Milella, Vincenzo De Laurenzi, Veronica Morea, Gianluca Sala, Giulio Fracasso, and Pierpaolo Ceci

Subjects

Tumor targeted therapy, Preclinical studies, Human ferritin, Transferrin receptor 1 (CD71), Breast cancer, Gastrointestinal cancer, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Ferritin receptor (CD71) is an example of a very attractive cancer target, since it is highly expressed in virtually all tumor types, including metastatic loci. However, this target can be considered to be inaccessible to conventional target therapies, due to its presence in many healthy tissues. Here, we describe the preclinical evaluation of a tumor proteases-activatable human ferritin (HFt)-based drug carrier (The-0504) that is able to selectively deliver the wide-spectrum topoisomerase I inhibitor Genz-644282 to CD71-expressing tumors, preventing the limiting toxic effects associated with CD71-targeting therapies. Methods CD71 expression was evaluated using flow cytometry and immunohistochemistry techniques. The-0504 antiproliferative activity towards several cancer cell lines was assessed in vitro. The-0504 antitumor efficacy and survival benefit were evaluated in different human tumors, which had been grown either as xenografts or patient-derived xenografts in mice. The-0504 toxicology profile was investigated in multiple-cycle repeat-dose study in rodents. Results In vitro studies indicate that The-0504 is highly specific for CD71 expressing cells, and that there is a relationship between CD71 levels and The-0504 anticancer activity. In vivo treatments with The-0504 showed a remarkable efficacy, eradicating several human tumors of very diverse and aggressive histotypes, such as pancreas, liver and colorectal carcinomas, and triple-negative breast cancer. Conclusions Durable disease-free survival, persistent antitumor responses after discontinuation of treatment and favorable toxicology profile make The-0504 an ideal candidate for clinical development as a novel, CD71-targeted, low-toxicity alternative to chemotherapy.

Published

2021

4. Cryo-EM structure of the human ferritin–transferrin receptor 1 complex

Author

Linda Celeste Montemiglio, Claudia Testi, Pierpaolo Ceci, Elisabetta Falvo, Martina Pitea, Carmelinda Savino, Alessandro Arcovito, Giovanna Peruzzi, Paola Baiocco, Filippo Mancia, Alberto Boffi, Amédée des Georges, and Beatrice Vallone

Subjects

Science

Abstract

The human transferrin receptor 1 (CD71) is a transmembrane protein responsible for iron uptake. Here the authors present the 3.9 Å resolution cryo-EM structure of the CD71 ectodomain-human ferritin (H-Ft) complex and find that H-Ft binds a CD71 region different from the transferrin one that overlaps with the surface recognized by select pathogens.

Published

2019

5. Very low intensity ultrasounds as a new strategy to improve selective delivery of nanoparticles-complexes in cancer cells

Author

Rossella Loria, Claudia Giliberti, Angelico Bedini, Raffaele Palomba, Giulio Caracciolo, Pierpaolo Ceci, Elisabetta Falvo, Raffaella Marconi, Rita Falcioni, Gianluca Bossi, and Lidia Strigari

Subjects

Ultrasound, Nanoparticles, Chemotherapeutic drugs, Sarcoma, Colon cancer, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background The possibility to combine Low Intensity UltraSound (LIUS) and Nanoparticles (NP) could represent a promising strategy for drugs delivery in tumors difficult to treat overcoming resistance to therapies. On one side the NP can carry drugs that specifically target the tumors on the other the LIUS can facilitate and direct the delivery to the tumor cells. In this study, we investigated whether Very Low Intensity UltraSound (VLIUS), at intensities lower than 120 mW/cm2, might constitute a novel strategy to improve delivery to tumor cells. Thus, in order to verify the efficacy of this novel modality in terms of increase selective uptake in tumoral cells and translate speedily in clinical practice, we investigated VLIUS in three different in vitro experimental tumor models and normal cells adopting three different therapeutic strategies. Methods VLIUS at different intensities and exposure time were applied to tumor and normal cells to evaluate the efficiency in uptake of labeled human ferritin (HFt)-based NP, the delivery of NP complexed Firefly luciferase reported gene (lipoplex-LUC), and the tumor-killing of chemotherapeutic agent. Results Specifically, we found that specific VLIUS intensity (120 mW/cm2) increases tumor cell uptake of HFt-based NPs at specific concentration (0.5 mg/ml). Similarly, VLIUS treatments increase significantly tumor cells delivery of lipoplex-LUC cargos. Furthermore, of interest, VLIUS increases tumor killing of chemotherapy drug trabectedin in a time dependent fashion. Noteworthy, VLIUS treatments are well tolerated in normal cells with not significant effects on cell survival, NPs delivery and drug-induced toxicity, suggesting a tumor specific fashion. Conclusions Our data shed novel lights on the potential application of VLIUS for the design and development of novel therapeutic strategies aiming to efficiently deliver NP loaded cargos or anticancer drugs into more aggressive and unresponsive tumors niche.

Published

2019

6. Mitoxantrone-Loaded Nanoferritin Slows Tumor Growth and Improves the Overall Survival Rate in a Subcutaneous Pancreatic Cancer Mouse Model

Author

Giamaica Conti, Martina Pitea, Riccardo Ossanna, Roberta Opri, Giada Tisci, Elisabetta Falvo, Giulio Innamorati, Esther Ghanem, Andrea Sbarbati, Pierpaolo Ceci, and Giulio Fracasso

Subjects

targeted therapy, pancreatic cancer, human ferritin, transferrin receptor (CD71), mitoxantrone, Biology (General), QH301-705.5

Abstract

Pancreatic cancer (PC) represents an intriguing topic for researchers. To date, the prognosis of metastasized PC is poor with just 7% of patients exceeding a five-year survival period. Thus, molecular modifications of existing drugs should be developed to change the course of the disease. Our previously generated nanocages of Mitoxantrone (MIT) encapsulated in human H-chain Ferritin (HFt), designated as HFt-MP-PASE-MIT, has shown excellent tumor distribution and extended serum half-life meriting further investigation for PC treatment. Thus, in this study, we used the same nano-formulation to test its cytotoxicity using both in vitro and in vivo assays. Interestingly, both encapsulated and free-MIT drugs demonstrated similar killing capabilities on PaCa44 cell line. Conversely, in vivo assessment in a subcutaneous PaCa44 tumor model of PC demonstrated a remarkable capability for encapsulated MIT to control tumor growth and improve mouse survival with a median survival rate of 65 vs. 33 days for loaded and free-MIT, respectively. Interestingly, throughout the course of mice treatment, MIT encapsulation did not present any adverse side effects as confirmed by histological analysis of various murine tissue organs and body mass weights. Our results are promising and pave the way to effective PC targeted chemotherapy using our HFt nanodelivery platforms.

Published

2021

7. Engineered Human Nanoferritin Bearing the Drug Genz-644282 for Cancer Therapy

Author

Elisabetta Falvo, Alessandro Arcovito, Giamaica Conti, Giuseppe Cipolla, Martina Pitea, Veronica Morea, Verena Damiani, Gianluca Sala, Giulio Fracasso, and Pierpaolo Ceci

Subjects

nanomedicine, human ferritin, gastrointestinal tumors, non-camptothecin topoisomerase I inhibitors, drug-delivery, CD71, Pharmacy and materia medica, RS1-441

Abstract

Gastrointestinal tumors, including pancreatic and colorectal cancers, represent one of the greatest public health issues worldwide, leading to a million global deaths. Recent research demonstrated that the human heavy chain ferritin (HFt) can encapsulate different types of drugs in its cavity and can bind to its receptor, CD71, in several solid and hematological tumors, thus highlighting the potential use of ferritin for tumor-targeting therapies. Here, we describe the development and characterization of a novel nanomedicine based on the HFt that is named The-0504. In particular, this novel system is a nano-assembly comprising an engineered version of HFt that entraps about 80 molecules of a potent, wide-spectrum, non-camptothecin topoisomerase I inhibitor (Genz-644282). The-0504 can be produced by a standardized pre-industrial process as a pure and homogeneously formulated product with favourable lyophilization properties. The preliminary anticancer activity was evaluated in cultured cancer cells and in a mouse model of pancreatic cancer. Overall results reported here make The-0504 a candidate for further preclinical development against CD-71 expressing deadly tumors.

Published

2020

8. Therapeutic Efficacy of the Novel Stimuli-Sensitive Nano-Ferritins Containing Doxorubicin in a Head and Neck Cancer Model

Author

Verena Damiani, Elisabetta Falvo, Giulio Fracasso, Luca Federici, Martina Pitea, Vincenzo De Laurenzi, Gianluca Sala, and Pierpaolo Ceci

Subjects

pasylated ferritin, stimuli-sensitive peptides, doxorubicin, drug-delivery, head and neck cancer, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Doxorubicin is employed alone or in combination for the treatment of several hematological and solid malignancies; despite its efficacy, there are associated cardiotoxicity limits both in its application in patients with heart disease risk factors and also in its long-term use. HFt-MP-PAS40 is a genetically engineered human ferritin heavy chain (HFt)-based construct able to efficiently entrap and deliver doxorubicin to cancer cells. HF-MP-PAS contains a short motif sequence (defined as MP) responsive to proteolytic cleavage by tumor matrix metalloproteases (MMPs), located between each HFt subunit and a masking polypeptide sequence rich in proline (P), alanine (A), and serine (S) residues (PAS). This carrier displayed excellent therapeutic efficacy in a xenogenic pancreatic cancer model in vivo, leading to a significant increase in overall animal survival in treated mice. Herein, we describe the HFt-MP-PAS40-Dox efficacy against squamous cell carcinomas of the head and neck (HNSCC) with the goal of validating the application of our nano-drug for the treatment of different solid tumors. In addition, a tolerability study in healthy mice was also performed. The results indicate that HFt-MP-PAS40-Dox produced increased anti-tumor effects both in vitro and in vivo in comparison to the free drug in several HNSCC cell lines. In the acute toxicity studies, the maximum tolerated dose (MTD) of HFt-MP-PAS40-Dox was about 3.5 higher than the free drug: 25 mg/kg versus 7 mg/kg doxorubicin equivalents. Importantly, evaluation of heart tissues provided evidence that doxorubicin is less cardio-toxic when encapsulated inside the ferritin carrier. In conclusion, HFt-MP-PAS40-Dox may be administered safely at higher doses compared with the free drug, resulting in superior efficacy to control HNSCC malignancies.

Published

2017

9. Use of Ferritin-Based Metal-Encapsulated Nanocarriers as Anticancer Agents

Author

Luciana Mosca, Elisabetta Falvo, Pierpaolo Ceci, Elena Poser, Ilaria Genovese, Giulia Guarguaglini, and Gianni Colotti

Subjects

ferritin, cisplatin, neuroblastoma, drug delivery, targeting, metal ions, nanocarriers, Technology, Engineering (General). Civil engineering (General), TA1-2040, Biology (General), QH301-705.5, Physics, QC1-999, Chemistry, QD1-999

Abstract

The ability of ferritin to bind and deliver metals and metal-based drugs to human neuroblastoma SH-SY5Y cells was studied. We used heavy chain (H) ferritin-based metal-containing nanocarriers to test whether these constructs, which are able to cross the blood-brain barrier, may be used for the delivery of toxic molecules to brain cells, and to study their effect on the viability and cellular redox homeostasis of human neuroblastoma cells. We show that metal-containing nanocarriers are efficiently captured by SH-SY5Y cells. Iron-containing nanocarriers have a proliferative effect, while silver and cisplatin-encapsulated nanocarriers determine concentration-dependent neuroblastoma cell death. This work is a proof of concept for the use of ferritins for the delivery of toxic molecules to brain tumors.

Published

2017

10. Increasing the Magnetic Anisotropy of a Natural System: Co-Doped Magnetite Mineralized in Ferritin Shells

Author

Pierpaolo Ceci, Francesco Pineider, Elvira Fantechi, Claudia Innocenti, Claudio Sangregorio, Elisabetta Falvo, and Anna M. Ferretti

Subjects

Biomineralization, Ferritin, Materials science, biology, Biomedical Engineering, Iron oxide, Nucleation, Nanoparticle, Magnetic Nanoparticles, Bioengineering, General Chemistry, Condensed Matter Physics, chemistry.chemical_compound, Crystallinity, Magnetic anisotropy, chemistry, Chemical engineering, Cobalt Ferrite, biology.protein, General Materials Science, human activities, Iron oxide nanoparticles, Magnetic Fluid Hyperthermia, Magnetite

Abstract

Iron oxide nanoparticles mineralized within the internal cavity of Ferritin protein cage are extremely appealing for the realization of multifunctional therapeutic and diagnostic agents for cancer treatment by drug delivery, magnetic fluid hyperthermia (MFH) and magnetic resonance imaging. Being the maximum mean size imposed by the internal diameter of the protein shell (ca. 8 nm) too small for the use of these systems in MFH, a valuable strategy for the improvement of the hyperthermic efficiency is increasing the magnetic anisotropy by doping the iron oxide with divalent Co ions. This strategy has been demonstrated to be highly efficient in the case of iron oxide nanoparticles mineralized in Human Ferritin (HFt). However, a deterioration of nanoparticles crystallinity and consequently a reduction of the hyperthermic efficiency were observed with increasing Co-doping. In this contribution, we compare two series of Co-doped iron oxide nanoparticles (Co-doping level up to 15%) mineralized into HFt and into Ferritin from the archaea Pirococcus Furiosus (PfFt), the protein structure of which differs for the nucleation sites, with the aim of increasing the crystalline quality of the inorganic cores for larger Co doping. Highly monodisperse nanoparticles of 6-7 nm were obtained in both series. The structural and magnetic characterization indicate that the PfFt series is less subjected to crystallinity deterioration with increasing Co content with respect to the HFt one. Such difference is reflected in the hyperthermic efficiency. which reaches the maximum value for different intermediate Co-doping (10% and 5% for PfFt and HFt, respectively), and goes to zero for further Co-doping increments.

Published

2019

11. Very low intensity ultrasounds as a new strategy to improve selective delivery of nanoparticles-complexes in cancer cells

Author

Elisabetta Falvo, Giulio Caracciolo, Pierpaolo Ceci, Raffaella Marconi, Lidia Strigari, Rita Falcioni, Rossella Loria, Raffaele Palomba, Angelico Bedini, Claudia Giliberti, and Gianluca Bossi

Subjects

0301 basic medicine, Colorectal cancer, Antineoplastic Agents, lcsh:RC254-282, 03 medical and health sciences, chemotherapeutic drugs, colon cancer, nanoparticles, sarcoma, ultrasound, oncology, cancer research, 0302 clinical medicine, Drug Delivery Systems, Cell Line, Tumor, Ultrasound, medicine, Humans, Lius, Luciferase, Trabectedin, Ultrasonography, biology, Chemistry, Research, Sarcoma, medicine.disease, biology.organism_classification, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, In vitro, Colon cancer, 030104 developmental biology, Apoptosis, 030220 oncology & carcinogenesis, Cancer cell, Colonic Neoplasms, Cancer research, Nanoparticles, Chemotherapeutic drugs, medicine.drug

Abstract

Background The possibility to combine Low Intensity UltraSound (LIUS) and Nanoparticles (NP) could represent a promising strategy for drugs delivery in tumors difficult to treat overcoming resistance to therapies. On one side the NP can carry drugs that specifically target the tumors on the other the LIUS can facilitate and direct the delivery to the tumor cells. In this study, we investigated whether Very Low Intensity UltraSound (VLIUS), at intensities lower than 120 mW/cm2, might constitute a novel strategy to improve delivery to tumor cells. Thus, in order to verify the efficacy of this novel modality in terms of increase selective uptake in tumoral cells and translate speedily in clinical practice, we investigated VLIUS in three different in vitro experimental tumor models and normal cells adopting three different therapeutic strategies. Methods VLIUS at different intensities and exposure time were applied to tumor and normal cells to evaluate the efficiency in uptake of labeled human ferritin (HFt)-based NP, the delivery of NP complexed Firefly luciferase reported gene (lipoplex-LUC), and the tumor-killing of chemotherapeutic agent. Results Specifically, we found that specific VLIUS intensity (120 mW/cm2) increases tumor cell uptake of HFt-based NPs at specific concentration (0.5 mg/ml). Similarly, VLIUS treatments increase significantly tumor cells delivery of lipoplex-LUC cargos. Furthermore, of interest, VLIUS increases tumor killing of chemotherapy drug trabectedin in a time dependent fashion. Noteworthy, VLIUS treatments are well tolerated in normal cells with not significant effects on cell survival, NPs delivery and drug-induced toxicity, suggesting a tumor specific fashion. Conclusions Our data shed novel lights on the potential application of VLIUS for the design and development of novel therapeutic strategies aiming to efficiently deliver NP loaded cargos or anticancer drugs into more aggressive and unresponsive tumors niche. Electronic supplementary material The online version of this article (10.1186/s13046-018-1018-6) contains supplementary material, which is available to authorized users.

Published

2019

12. Engineered Human Nanoferritin Bearing the Drug Genz-644282 for Cancer Therapy

Author

Gianluca Sala, Giamaica Conti, Alessandro Arcovito, Elisabetta Falvo, Giulio Fracasso, Martina Pitea, Giuseppe Cipolla, Pierpaolo Ceci, Veronica Morea, and Verena Damiani

Subjects

Drug, media_common.quotation_subject, gastrointestinal tumors, lcsh:RS1-441, Pharmaceutical Science, Transferrin receptor, 02 engineering and technology, 010402 general chemistry, 01 natural sciences, Article, lcsh:Pharmacy and materia medica, CD71, drug-delivery, human ferritin, nanomedicine, non-camptothecin topoisomerase I inhibitors, Pancreatic cancer, Medicine, Receptor, Settore BIO/10 - BIOCHIMICA, media_common, biology, business.industry, 021001 nanoscience & nanotechnology, medicine.disease, 0104 chemical sciences, Ferritin, Drug delivery, Cancer cell, Cancer research, biology.protein, Nanomedicine, 0210 nano-technology, business, biomaterials

Abstract

Gastrointestinal tumors, including pancreatic and colorectal cancers, represent one of the greatest public health issues worldwide, leading to a million global deaths. Recent research demonstrated that the human heavy chain ferritin (HFt) can encapsulate different types of drugs in its cavity and can bind to its receptor, CD71, in several solid and hematological tumors, thus highlighting the potential use of ferritin for tumor-targeting therapies. Here, we describe the development and characterization of a novel nanomedicine based on the HFt that is named The-0504. In particular, this novel system is a nano-assembly comprising an engineered version of HFt that entraps about 80 molecules of a potent, wide-spectrum, non-camptothecin topoisomerase I inhibitor (Genz-644282). The-0504 can be produced by a standardized pre-industrial process as a pure and homogeneously formulated product with favourable lyophilization properties. The preliminary anticancer activity was evaluated in cultured cancer cells and in a mouse model of pancreatic cancer. Overall results reported here make The-0504 a candidate for further preclinical development against CD-71 expressing deadly tumors.

Published

2020

13. Cryo-EM structure of the human ferritin–transferrin receptor 1 complex

Author

C. Savino, Martina Pitea, Claudia Testi, Alberto Boffi, Alessandro Arcovito, Linda Celeste Montemiglio, F. Mancia, Pierpaolo Ceci, Paola Baiocco, Giovanna Peruzzi, Beatrice Vallone, A. Des Georges, and Elisabetta Falvo

Subjects

0301 basic medicine, Protein Conformation, alpha-Helical, physics and astronomy (all), Protozoan Proteins, General Physics and Astronomy, Gene Expression, 02 engineering and technology, Plasma protein binding, Epitope, Substrate Specificity, Viral Envelope Proteins, Cloning, Molecular, lcsh:Science, Arenaviruses, New World, Transferrin receptor 1, chemistry.chemical_classification, Multidisciplinary, biology, genetics and molecular biology (all), Transferrin, 021001 nanoscience & nanotechnology, Recombinant Proteins, chemistry (all), biochemistry, genetics and molecular biology (all), 3. Good health, Cell biology, Ectodomain, Receptors, Virus, 0210 nano-technology, Protein Binding, Virus genetics, Science, Genetic Vectors, Context (language use), Transferrin receptor, Cryo-EM structure, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, Antigens, CD, Receptors, Transferrin, Escherichia coli, Humans, biochemistry, Protein Interaction Domains and Motifs, Hemochromatosis Protein, Settore BIO/10 - BIOCHIMICA, Ferritin, Binding Sites, Cryoelectron Microscopy, General Chemistry, 030104 developmental biology, chemistry, Apoferritins, biology.protein, lcsh:Q, Protein Conformation, beta-Strand, Plasmodium vivax, HeLa Cells

Abstract

Human transferrin receptor 1 (CD71) guarantees iron supply by endocytosis upon binding of iron-loaded transferrin and ferritin. Arenaviruses and the malaria parasite exploit CD71 for cell invasion and epitopes on CD71 for interaction with transferrin and pathogenic hosts were identified. Here, we provide the molecular basis of the CD71 ectodomain-human ferritin interaction by determining the 3.9 Å resolution single-particle cryo-electron microscopy structure of their complex and by validating our structural findings in a cellular context. The contact surfaces between the heavy-chain ferritin and CD71 largely overlap with arenaviruses and Plasmodium vivax binding regions in the apical part of the receptor ectodomain. Our data account for transferrin-independent binding of ferritin to CD71 and suggest that select pathogens may have adapted to enter cells by mimicking the ferritin access gate., The human transferrin receptor 1 (CD71) is a transmembrane protein responsible for iron uptake. Here the authors present the 3.9 Å resolution cryo-EM structure of the CD71 ectodomain-human ferritin (H-Ft) complex and find that H-Ft binds a CD71 region different from the transferrin one that overlaps with the surface recognized by select pathogens.

Published

2019

14. The presence of glutamate residues on the PAS sequence of the stimuli-sensitive nano-ferritin improves in vivo biodistribution and mitoxantrone encapsulation homogeneity

Author

Roberta Opri, Francesco Fazi, Gianni Colotti, Elisa Tremante, Aldo Braca, Francesca Malagrinò, Elisabetta Falvo, Patrizio Di Micco, Giulio Fracasso, Alessandro Arcovito, Pierpaolo Ceci, Alessandro Giuffrè, Falvo, E., Malagrino, Francesca., Arcovito, A., Fazi, F., Colotti, G., Tremante, E., Di Micco, P., Braca, A., Opri, R., Giuffre, A., Fracasso, G., and Ceci, P.

Subjects

0301 basic medicine, Biodistribution, Proteases, Glutamic Acid, Pharmaceutical Science, Antineoplastic Agents, 02 engineering and technology, Serine, 03 medical and health sciences, Doxorubicin (PubChem CID:31703), In vivo, Cell Line, Tumor, Protein-cage nanocarrier, Pasylated ferritin, Humans, Tissue Distribution, cancer, drug-delivery, drug-encapsulation, mitoxantrone, pasylated ferritin, protein-cage nanocarrier, 3003, Settore BIO/10 - BIOCHIMICA, Peptide sequence, Cancer, Drug Carriers, Chemistry, Mitoxantrone (PubChem CID:4212), Drug-delivery, Drug-encapsulation, Mitoxantrone, 021001 nanoscience & nanotechnology, In vitro, 030104 developmental biology, Biochemistry, Doxorubicin, Apoferritins, Cancer cell, Drug delivery, Nanoparticles, 0210 nano-technology

Abstract

A genetically engineered human ferritin heavy chain (HFt)-based construct has been recently shown by our group to efficiently entrap and deliver doxorubicin to cancer cells. This construct, named HFt-MP-PAS, contained a tumor-selective sequence (MP) responsive to proteolytic cleavage by tumor proteases (MMPs), located between each HFt subunit and an outer shielding polypeptide sequence rich in proline (P), serine (S) and alanine (A) residues (PAS). HFt-MP-PAS displayed excellent therapeutic efficacy in xenogenic pancreatic and head and neck cancer models in vivo, leading to a significant increase in overall animal survivals. Here we report a new construct obtained by the genetic insertion of two glutamate residues in the PAS sequence of HFt-MP-PAS. Such new construct, named HFt-MP-PASE, is characterized by improved performances as drug biodistribution in a xenogenic pancreatic cancer model in vivo. Moreover, HFt-MP-PASE efficiently encapsulates the anti-cancer drug mitoxantrone (MIT), and the resulting MIT-loaded nanoparticles proved to be more soluble and monodispersed than the HFt-MP-PAS counterparts. Importantly, in vitro MIT-loaded HFt-MP-PASE kills several cancer cell lines of different origin (colon, breast, sarcoma and pancreas) at least as efficiently as the free drug. Finally, our MIT loaded protein nanocages allowed in vivo an impressive incrementing of the drug accumulation in the tumor with respect to the free drug.

Published

2018

15. Use of ferritin-based metal-encapsulated nanocarriers as anticancer agents

Author

Ilaria Genovese, Luciana Mosca, Gianni Colotti, Elisabetta Falvo, Giulia Guarguaglini, Elena Poser, and Pierpaolo Ceci

Subjects

0301 basic medicine, cisplatin, 02 engineering and technology, Pharmacology, lcsh:Technology, lcsh:Chemistry, Neuroblastoma cell, 03 medical and health sciences, neuroblastoma, Neuroblastoma, medicine, General Materials Science, lcsh:QH301-705.5, Instrumentation, targeting, Fluid Flow and Transfer Processes, Cisplatin, Heavy chain, biology, nanocarriers, lcsh:T, Chemistry, Process Chemistry and Technology, ferritin, General Engineering, metal ions, 021001 nanoscience & nanotechnology, medicine.disease, drug delivery, lcsh:QC1-999, Computer Science Applications, Ferritin, 030104 developmental biology, lcsh:Biology (General), lcsh:QD1-999, lcsh:TA1-2040, Drug delivery, Cancer research, biology.protein, Nanocarriers, lcsh:Engineering (General). Civil engineering (General), 0210 nano-technology, lcsh:Physics, Homeostasis, medicine.drug

Abstract

The ability of ferritin to bind and deliver metals and metal-based drugs to human neuroblastoma SH-SY5Y cells was studied. We used heavy chain (H) ferritin-based metal-containing nanocarriers to test whether these constructs, which are able to cross the blood-brain barrier, may be used for the delivery of toxic molecules to brain cells, and to study their effect on the viability and cellular redox homeostasis of human neuroblastoma cells. We show that metal-containing nanocarriers are efficiently captured by SH-SY5Y cells. Iron-containing nanocarriers have a proliferative effect, while silver and cisplatin-encapsulated nanocarriers determine concentration-dependent neuroblastoma cell death. This work is a proof of concept for the use of ferritins for the delivery of toxic molecules to brain tumors.

Published

2017

16. An EPR Study of Small Magnetic Nanoparticles

Author

Pierpaolo Ceci, Elisabetta Falvo, Alberto Cini, Dante Gatteschi, and Maria Fittipaldi

Subjects

Electron nuclear double resonance, magnetic nanoparticles, electron paramagnetic resonance, quantum behavior, Physical and Theoretical Chemistry, Materials science, 02 engineering and technology, 010402 general chemistry, 021001 nanoscience & nanotechnology, 01 natural sciences, 0104 chemical sciences, law.invention, Nuclear magnetic resonance, law, Magnetic nanoparticles, 0210 nano-technology, Electron paramagnetic resonance

Abstract

Magnetic nanoparticles (MNPs) of spinel type iron oxide (of approximately 4 nm) mineralized inside the internal cavity of a mini ferritin-type protein have been investigated by means of electron magnetic resonance (EMR) spectroscopy. EMR measurements have been recorded at different temperatures in perpendicular and parallel configurations. The spectra have been interpreted using an approach based on the giant spin model. We confirm the quantum behavior of the MNPs, moreover, the thermal evolution of the spin system in terms of population of excited spin states is showed.

Published

2017

17. A Smart Platform for Hyperthermia Application in Cancer Treatment: Cobalt-Doped Ferrite Nanoparticles Mineralized in Human Ferritin Cages

Author

Elvira Fantechi, Anna M. Ferretti, Claudio Sangregorio, Miriam Carbo, Pierpaolo Ceci, Lorenzo Di Cesare Mannelli, Alessandro Ponti, Valbona Shullani, Elisabetta Falvo, Carla Ghelardini, Matteo Zanardelli, Maria Fittipaldi, and Claudia Innocenti

Subjects

magnetic nanoparticles, Materials science, Cell Survival, Dispersity, Melanoma, Experimental, Iron oxide, Metal Nanoparticles, General Physics and Astronomy, chemistry.chemical_element, Nanotechnology, Ferric Compounds, Magnetics, Mice, chemistry.chemical_compound, cobalt ferrite, Cell Line, Tumor, Neoplasms, Animals, Humans, General Materials Science, Melanoma, Drug Carriers, biology, ferritin, technology, industry, and agriculture, General Engineering, Cobalt, Hyperthermia, Induced, magnetic fluid hyperthermia, Ferritin, chemistry, Chemical engineering, alpha-MSH, Ferritins, Drug delivery, biology.protein, cancer therapy, Anisotropy, Magnetic nanoparticles, Peptides, Drug carrier, Ethylene glycol

Abstract

Magnetic nanoparticles, MNPs, mineralized within a human ferritin protein cage, HFt, can represent an appealing platform to realize smart therapeutic agents for cancer treatment by drug delivery and magnetic fluid hyperthermia, MFH. However, the constraint imposed by the inner diameter of the protein shell (ca. 8 nm) prevents its use as heat mediator In MFH when the MNPs comprise pure iron oxide. In this contribution, we demonstrate how this limitation can be overcome through the controlled doping of the core with small amount of Co(II). Highly monodisperse doped iron oxide NPs with average size of 7 nm are mineralized inside a genetically modified variant of HFt, carrying several copies of a-melanocyte-stimulating hormone peptide, which has already been demonstrated to have excellent targeting properties toward melanoma cells. HFt is also conjugated to poly(ethylene glycol) molecules to increase its in vivo stability. The investigation of hyperthermic properties of HFt-NPs shows that a Co doping of 5% Is enough to strongly enhance the magnetic anisotropy and thus the hyperthermic efficiency with respect to the undoped sample. In vitro tests performed on B16 melanoma cell line demonstrate a strong reduction of the cell viability after treatment with Co doped HFt-NPs and exposure to the alternating magnetic field. Clear indications of an advanced stage of apoptotic process is also observed from immunocytochemistry analysis. The obtained data suggest this system represents a promising candidate for the development of a protein-based theranostic nanoplatform.

Published

2014

18. PO-207 Ferritin-engineered nanoparticles as targeted drug delivery system for cancer treatment

Author

Gianluca Sala, Verena Damiani, Giulio Fracasso, V De Laurenzi, Cosmo Rossi, Pierpaolo Ceci, Martina Pitea, and Elisabetta Falvo

Subjects

Cancer Research, biology, Chemistry, medicine.disease, In vitro, Ferritin, Oncology, Targeted drug delivery, In vivo, Pancreatic cancer, Drug delivery, medicine, Cancer research, biology.protein, Viability assay, Nanocarriers

Abstract

Introduction Cancer remains still one of the major causes of death worldwide, therefore continuous improvements in tumor-fighting strategies are necessary. Targeting drugs directly to the tumour site, to overcome the systemic side effects, represents a great challenge. Nanoparticles have increasingly been used as drug delivery system showing intriguing therapeutic efficacies. Material and methods A genetically engineered nanocarrier based on human ferritin heavy chain (HFt) able to incorporate and deliver drugs was developed. These nanoparticles contain a short motif sequence (MP) cleavable by matrix metalloproteases between the HFt subunit and a masking sequence rich in proline (P), alanine (A) and serine (S): HFt-MP-PASE40. A topoisomerase I inhibitor was loaded into these nanocarriers (HFt-MP-PASE-Topo). Cell viability of different pancreatic cancer cell lines was evaluated in vitro. In vivo the therapeutic efficacy of HFt-MP-PASE-Topo was investigated on both a pancreatic cancer cell-line-derived xenograft and a patient-derived pancreatic cancer xenograft (PDX). Results and discussions In vitro studies showed a potent cytotoxic activity of HFt-MP-PASE-Topo with an IC50 that ranges between 0,005 µM to 0,05 µM. In vivo studies further demonstrated the therapeutic efficacy of HFt-MP-PASE-Topo in pancreatic cancer-bearing mice and in PDX model. In vivo treatments exhibited a robust decrease in tumour growth furthermore the animal overall survival significantly increased in HFt-MP-PASE-Topo treated mice. Conclusion Altogether, our results indicate that HFt-MP-PASE-Topo may constitute a promising tool in anticancer therapeutics.

Published

2018

19. Electrostatic assembly of binary nanoparticle superlattices using protein cages

Author

Jani Seitsonen, Ari Laiho, Panu Hiekkataipale, Mauri A. Kostiainen, Pierpaolo Ceci, Vincent Lemieux, and Janne Ruokolainen

Subjects

Models, Molecular, Materials science, Archaeal Proteins, Static Electricity, ta221, Biomedical Engineering, Metal Nanoparticles, Physics::Optics, Nanoparticle, Bioengineering, Nanotechnology, virus, Crystal structure, Cubic crystal system, Condensed Matter::Materials Science, Nanocages, Lattice constant, Microscopy, Electron, Transmission, General Materials Science, Particle Size, Electrical and Electronic Engineering, Isostructural, ta218, ta214, ta114, nanoparticle, protein cage, self-assembly, Condensed Matter Physics, Bromovirus, Atomic and Molecular Physics, and Optics, Nanostructures, Chemical physics, Colloidal gold, Ferritins, RNA, Viral, Gold, Self-assembly

Abstract

Binary nanoparticle superlattices are periodic nanostructures with lattice constants much shorter than the wavelength of light and could be used to prepare multifunctional metamaterials. Such superlattices are typically made from synthetic nanoparticles, and although biohybrid structures have been developed, incorporating biological building blocks into binary nanoparticle superlattices remains challenging. Protein-based nanocages provide a complex yet monodisperse and geometrically well-defined hollow cage that can be used to encapsulate different materials. Such protein cages have been used to program the self-assembly of encapsulated materials to form free-standing crystals and superlattices at interfaces or in solution. Here, we show that electrostatically patchy protein cages--cowpea chlorotic mottle virus and ferritin cages--can be used to direct the self-assembly of three-dimensional binary superlattices. The negatively charged cages can encapsulate RNA or superparamagnetic iron oxide nanoparticles, and the superlattices are formed through tunable electrostatic interactions with positively charged gold nanoparticles. Gold nanoparticles and viruses form an AB(8)(fcc) crystal structure that is not isostructural with any known atomic or molecular crystal structure and has previously been observed only with large colloidal polymer particles. Gold nanoparticles and empty or nanoparticle-loaded ferritin cages form an interpenetrating simple cubic AB structure (isostructural with CsCl). We also show that these magnetic assemblies provide contrast enhancement in magnetic resonance imaging.

Published

2012

20. A fusion protein, a nanoparticle composed by a plurality of monomers of said fusion protein, and uses thereof

Author

Pierpaolo Ceci and Elisabetta Falvo

Subjects

nanoparticelle, ferritina, cancro, drug-delivery

Published

2016

21. Selective targeting of melanoma by PEG-masked protein-based multifunctional nanoparticles

Author

Jiri Krizan, Oldrich Benada, Veronica Morea, Elisabetta Falvo, Patrizio Di Micco, Pierpaolo Ceci, Alberto Boffi, Manuela Fornara, Katarina Hulikova-Capkova, Jan Svoboda, and Luca Vannucci

Subjects

Male, Medicine (General), Multifunctional nanoparticles, Melanoma, Experimental, Pharmaceutical Science, Nanoparticle, Polyethylene Glycols, Mice, Drug Delivery Systems, International Journal of Nanomedicine, Drug Discovery, Nanotechnology, Magnetite Nanoparticles, cancer-targeting, ferritin, melanoma, multifunctional nanoparticles, nanoplatform, Original Research, Microscopy, Confocal, Protein Stability, Melanoma, General Medicine, Magnetic Resonance Imaging, Recombinant Proteins, multifunctional nanoparticles, Nanomedicine, HT29 Cells, Materials science, ComputingMethodologies_IMAGEPROCESSINGANDCOMPUTERVISION, Biophysics, Bioengineering, Cancer targeting, Biomaterials, R5-920, Microscopy, Electron, Transmission, PEG ratio, melanoma, medicine, Animals, Humans, Fluorescent Dyes, Genetically engineered, ferritin, Organic Chemistry, medicine.disease, Mice, Inbred C57BL, alpha-MSH, Apoferritins, nanoplatform, cancer-targeting

Abstract

Video abstract Video, Background Nanoparticle-based systems are promising for the development of imaging and therapeutic agents. The main advantage of nanoparticles over traditional systems lies in the possibility of loading multiple functionalities onto a single molecule, which are useful for therapeutic and/or diagnostic purposes. These functionalities include targeting moieties which are able to recognize receptors overexpressed by specific cells and tissues. However, targeted delivery of nanoparticles requires an accurate system design. We present here a rationally designed, genetically engineered, and chemically modified protein-based nanoplatform for cell/tissue-specific targeting. Methods Our nanoparticle constructs were based on the heavy chain of the human protein ferritin (HFt), a highly symmetrical assembly of 24 subunits enclosing a hollow cavity. HFt-based nanoparticles were produced using both genetic engineering and chemical functionalization methods to impart several functionalities, ie, the α-melanocyte-stimulating hormone peptide as a melanoma-targeting moiety, stabilizing and HFt-masking polyethylene glycol molecules, rhodamine fluorophores, and magnetic resonance imaging agents. The constructs produced were extensively characterized by a number of physicochemical techniques, and assayed for selective melanoma-targeting in vitro and in vivo. Results Our HFt-based nanoparticle constructs functionalized with the α-melanocyte-stimulating hormone peptide moiety and polyethylene glycol molecules were specifically taken up by melanoma cells but not by other cancer cell types in vitro. Moreover, experiments in melanoma-bearing mice indicate that these constructs have an excellent tumor-targeting profile and a long circulation time in vivo. Conclusion By masking human HFt with polyethylene glycol and targeting it with an α-melanocyte-stimulating hormone peptide, we developed an HFt-based melanoma-targeting nanoplatform for application in melanoma diagnosis and treatment. These results could be of general interest, because the same strategy can be exploited to develop ad hoc nanoplatforms for specific delivery towards any cell/tissue type for which a suitable targeting moiety is available.

Published

2012

22. Effect of the charge distribution along the 'ferritin-like' pores of the proteins from the Dps family on the iron incorporation process

Author

Francesco Oteri, Gisa Di Cecca, Mattia Falconi, Pierpaolo Ceci, Emilia Chiancone, and Carlotta Zamparelli

Subjects

Models, Molecular, Protein Conformation, Iron, Molecular Sequence Data, Static Electricity, Kinetics, Cooperativity, medicine.disease_cause, Biochemistry, Micelle, Nanomaterials, Inorganic Chemistry, chemistry.chemical_compound, Bacterial Proteins, medicine, Hydrogen peroxide, Escherichia coli, biology, Mycobacterium smegmatis, Hydrogen Peroxide, Oxidants, biology.organism_classification, DNA-Binding Proteins, Oxygen, Ferritin, Crystallography, chemistry, Ferritins, Biophysics, biology.protein, Oxidation-Reduction

Abstract

DNA-binding proteins from starved cells (Dps) differ in the number and position of charged residues along the "ferritin-like" pores that are used by iron to reach the ferroxidase center and the protein cavity. These differences are shown to affect significantly the electrostatic potential at the pores, which determines the extent of cooperativity in the iron uptake kinetics and thereby the mass distribution of the ferric hydroxide micelles inside the protein cavity. These conclusions are of biotechnological value in the preparation of protein-enclosed nanomaterials and are expected to apply also to ferritins. They were reached after characterization of the Dps from Listeria innocua, Helicobacter pylori, Thermosynechococcus elongatus, Escherichia coli, and Mycobacterium smegmatis. The characterization comprised the calculation of the electrostatic potential at the pores, determination of the iron uptake kinetics in the presence of molecular oxygen or hydrogen peroxide, and analysis of the proteins by means of the sedimentation velocity after iron incorporation.

Published

2011

23. The characterization of Thermotoga maritima ferritin reveals an unusual subunit dissociation behavior and efficient DNA protection from iron-mediated oxidative stress

Author

Manuela Fornara, Gisa Di Cecca, Emilia Chiancone, Elena Forte, and Pierpaolo Ceci

Subjects

DNA, Bacterial, Models, Molecular, Hot Temperature, iron incorporation, Iron, Protein subunit, Molecular Sequence Data, Crystallography, X-Ray, Microbiology, law.invention, chemistry.chemical_compound, Bacterial Proteins, law, subunit association-dissociation properties, medicine, Thermotoga maritima, Amino Acid Sequence, Cloning, Molecular, Protein Structure, Quaternary, ros detoxification, dna protection, thermotoga maritima ferritin, biology, Protein Stability, Osmolar Concentration, General Medicine, biology.organism_classification, Recombinant Proteins, Ferritin, Oxidative Stress, Protein Subunits, Biochemistry, chemistry, Catalase, Ferritins, biology.protein, Recombinant DNA, Molecular Medicine, Ferric, Reactive Oxygen Species, Oxidation-Reduction, Bacteria, DNA, DNA Damage, medicine.drug

Abstract

Ferritin from the hyperthermophilic anaerobe Thermotoga maritima, a bacterium of ancient phylogenetic origin, is structurally similar to known bacterial and eukaryotic ferritins: 24 identical subunits assemble into a shell having octahedral symmetry and a Mr of about 460 kDa. T. maritima ferritin (TmFtn), purified to homogeneity as a recombinant protein, contains approximately 2-3 iron atoms and can incorporate efficiently up to 3,500 atoms in the form of a ferric oxy-hydroxide mineral at 80°C, the optimal growth temperature of the bacterium. The 24-mer unexpectedly dissociates reversibly into dimers at low ionic strengths. In turn, dimers re-associate into the native 24-mer assembly at high protein concentrations and upon incorporation of iron micelles containing at least 500 Fe(III). TmFtn uses O(2) as efficient iron oxidant. The reaction stoichiometry is 3-4 O(2):Fe(II) as in all bacterial ferritins. Accordingly no H(2)O(2) is released into solution, a feature reflected in the in vitro ability of TmFtn to reduce significantly iron-mediated oxidative damage to DNA at 80°C. A similar TmFtn-mediated ROS detoxifying role likely occurs in the bacterium which lacks the SOD/catalase defense systems of the aerobic world.

Published

2011

24. Hierarchical Self-Assembly and Optical Disassembly for Controlled Switching of Magnetoferritin Nanoparticle Magnetism

Author

OI Kasyutich, Jeroen J. L. M. Cornelissen, Manuela Fornara, Panu Hiekkataipale, Pierpaolo Ceci, Johan van Lierop, Mauri A. Kostiainen, Ryan D. Desautels, Roeland J. M. Nolte, and Biomolecular Nanotechnology

Subjects

Models, Molecular, Dendrimers, Materials science, Optical Phenomena, Protein Conformation, Ultraviolet Rays, Magnetism, Archaeal Proteins, Iron, Dispersity, ta221, General Physics and Astronomy, Nanoparticle, Nanotechnology, METIS-283461, 02 engineering and technology, 010402 general chemistry, 01 natural sciences, Magnetization, General Materials Science, Single domain, Nitrobenzenes, ta218, ta214, ta114, Magnetic Phenomena, dendrons, ferritin, General Engineering, Oxides, 021001 nanoscience & nanotechnology, 0104 chemical sciences, Pyrococcus furiosus, Hysteresis, magnetism, Apoferritins, Nanoparticles, Self-assembly, 0210 nano-technology, Superstructure (condensed matter), Physical Organic Chemistry

Abstract

Protein cages such as ferritin and viral capsids are interesting building blocks for nanotechnology due to their monodisperse structure and ability to encapsulate various functional moieties. Here we show that recombinant ferritin protein cages encapsulating Fe(3)O(4)-γ-Fe(2)O(3) iron oxide (magnetoferritin) nanoparticles and photodegradable Newkome-type dendrons self-assemble into micrometer-sized complexes with a face-centered-cubic (fcc) superstructure and a lattice constant of 13.1 nm. The magnetic properties of the magnetoferritin particles are affected directly by the hierarchical organization. Magnetoferritin nanoparticles dispersed in water exhibit typical magnetism of single domain noninteracting nanoparticles; however, the same nanoparticles organized into fcc superstructures show clearly the effects of the altered magnetostatic (e.g., dipole-dipole) interactions by exhibiting, for example, different hysteresis of the field-dependent magnetization. The magnetoferritin-dendron assemblies can be efficiently disassembled by a short optical stimulus resulting in release of free magnetoferritin particles. After the triggered release the nanomagnetic properties of the pristine magnetoferritin nanoparticles are regained.

Published

2011

25. The Heck Reaction of Allylic Alcohols Catalyzed by Palladium Nanoparticles in Water: Chemoenzymatic Synthesis of (R)-(−)-Rhododendrol

Author

Alexandr Shafir, Roberto Cirilli, Adelina Vallribera, Sandro Cacchi, Giancarlo Fabrizi, Alberto Boffi, Sandra Niembro, Alessandro Prastaro, and Pierpaolo Ceci

Subjects

Allylic rearrangement, Chemistry, Silica gel, Aryl, Organic Chemistry, Enantioselective synthesis, chemistry.chemical_element, Catalysis, Enzyme catalysis, Inorganic Chemistry, chemistry.chemical_compound, Heck reaction, Organic chemistry, Physical and Theoretical Chemistry, Palladium

Abstract

The use of phosphine-free perfluoro-tagged palladium nanoparticles immobilized on fluorous silica gel (FSG), either through fluorous–fluorous interactions or covalent bonding, in the Heck reaction of aryl iodides with allylic alcohols under aerobic conditions in water is described. 4-(4-Methoxyphenyl)-butan-2-one, an important fine chemical, is readily accessed by this procedure. A two-step one-pot process, involving a Heck reaction followed by an enantioselective enzyme-catalyzed reduction, to form chiral alcohols is applied to the synthesis of (R)-(−)-rhododendrol. The palladium catalysts can be recycled several times, both in the Heck reaction and in the one-pot chemoenzymatic process.

Published

2010

26. Silver Ion Incorporation and Nanoparticle Formation inside the Cavity of Pyrococcus furiosus Ferritin: Structural and Size-Distribution Analyses

Author

OI Kasyutich, Dragomir Tatchev, Andrea Ilari, Armin Hoell, Annarita Fiorillo, and Pierpaolo Ceci

Subjects

Models, Molecular, Silver, Nucleation, Metal Nanoparticles, Nanoparticle, 02 engineering and technology, Crystallography, X-Ray, 010402 general chemistry, Ferric Compounds, 01 natural sciences, Biochemistry, Catalysis, Silver nanoparticle, Metal, Colloid and Surface Chemistry, Microscopy, Electron, Transmission, Scattering, Small Angle, Organometallic Compounds, Surface plasmon resonance, biology, Chemistry, General Chemistry, Cations, Monovalent, Surface Plasmon Resonance, 021001 nanoscience & nanotechnology, biology.organism_classification, 0104 chemical sciences, Pyrococcus furiosus, Ferritin, Kinetics, Crystallography, Chemical engineering, visual_art, Ferritins, visual_art.visual_art_medium, biology.protein, 0210 nano-technology, Oxidation-Reduction, Ultracentrifugation, Biomineralization

Abstract

Highly symmetrical protein cage architectures from three different iron storage proteins, heavy and light human ferritin chains (HuHFt and HuLFt) and ferritin from the hyperthemophilic bacterium Pyrococcus furiosus (PfFt), have been used as models for understanding the molecular basis of silver ion deposition and metal core formation inside the protein cavity. Biomineralization using protein cavities is an important issue for the fabrication of biometamaterials under mild synthetic conditions. Silver nanoparticles (AgNPs) were produced with high yields within PfFt but not within HuHFt and HuLFt. To explain the molecular basis of silver incorporation, the X-ray crystal structure of Ag-containing PfFt has been solved. This is the first structure of a silver containing ferritin reported to date, and it revealed the presence of specific binding and nucleation sites of Ag(I) that are not conserved in other ferritin templates. The AgNP encapsulated by PfFt were further characterized by the combined use of different physical chemical techniques. These showed that the AgNPs are endowed with a narrow size distribution (2.1 +/- 0.4 nm), high stability in water solution at millimolar concentration, and high thermal stability. These properties make the AgNP obtained within PftFt exploitable for a range of applications, in fields as diverse as catalysis in water, preparation of metamaterials, and in vivo diagnosis and antibacterial or tumor therapy.

Published

2010

27. Thermosynechoccus elongatus DpsA binds Zn(II) at a unique three histidine-containing ferroxidase center and utilizes O2 as iron oxidant with very high efficiency, unlike the typical Dps proteins

Author

Pierpaolo Ceci, F. Alaleona, Andrea Ilari, Emilia Chiancone, and Stefano Franceschini

Subjects

Absorbance, Reaction mechanism, Crystallography, Protein structure, Ligand, Chemistry, Thylakoid, Cell Biology, Photosynthesis, Molecular Biology, Biochemistry, Peptide sequence, Histidine

Abstract

The cyanobacterium Thermosynechococcus elongatus is one the few bacteria to possess two Dps proteins, DpsA-Te and Dps-Te. The present characterization of DpsA-Te reveals unusual structural and functional features that differentiate it from Dps-Te and the other known Dps proteins. Notably, two Zn(II) are bound at the ferroxidase center, owing to the unique substitution of a metal ligand at the A-site (His78 in place of the canonical aspartate) and to the presence of a histidine (His164) in place of a hydrophobic residue at a metal-coordinating distance in the B-site. Only the latter Zn(II) is displaced by incoming iron, such that Zn(II)-Fe(III) complexes are formed upon oxidation, as indicated by absorbance and atomic emission spectroscopy data. In contrast to the typical behavior of Dps proteins, where Fe(II) oxidation by H(2)O(2) is about 100-fold faster than by O(2), in DpsA-Te the ferroxidation efficiency of O(2) is very high and resembles that of H(2)O(2). Oxygraphic experiments show that two Fe(II) are required to reduce O(2), and that H(2)O(2) is not released into solution at the end of the reaction. On this basis, a reaction mechanism is proposed that also takes into account the formation of Zn(II)-Fe(III) complexes. The physiological significance of the DpsA-Te behavior is discussed in the framework of a possible localization of the protein at the thylakoid membranes, where photosynthesis takes place, with the consequent increased formation of reactive oxygen species.

Published

2010

28. The neutrophil-activating Dps protein of Helicobacter pylori, HP-NAP, adopts a mechanism different from Escherichia coli Dps to bind and condense DNA

Author

Emilia Chiancone, Pierpaolo Ceci, Laura Mangiarotti, and Claudio Rivetti

Subjects

Models, Molecular, DNA protection, Radical, Microscopy, Atomic Force, Ferroxidase activity, medicine.disease_cause, DNA condensation, Virulence factor, chemistry.chemical_compound, Bacterial Proteins, Genetics, medicine, Deoxyribonuclease I, Molecular Biology, Escherichia coli, biology, Hydroxyl Radical, Escherichia coli Proteins, DNA, Hydrogen-Ion Concentration, Helicobacter pylori, biology.organism_classification, chemistry, Biochemistry, Bacterial Outer Membrane Proteins, Protein Binding

Abstract

The Helicobacter pylori neutrophil-activating protein (HP-NAP), a member of the Dps family, is a fundamental virulence factor involved in H.pylori-associated disease. Dps proteins protect bacterial DNA from oxidizing radicals generated by the Fenton reaction and also from various other damaging agents. DNA protection has a chemical component based on the highly conserved ferroxidase activity of Dps proteins, and a physical one based on the capacity of those Dps proteins that contain a positively charged N-terminus to bind and condense DNA. HP-NAP does not possess a positively charged N-terminus but, unlike the other members of the family, is characterized by a positively charged protein surface. To establish whether this distinctive property could be exploited to bind DNA, gel shift, fluorescence quenching and atomic force microscopy (AFM) experiments were performed over the pH range 6.5-8.5. HP-NAP does not self-aggregate in contrast to Escherichia coli Dps, but is able to bind and even condense DNA at slightly acid pH values. The DNA condensation capacity acts in concert with the ferritin-like activity and could be used to advantage by H.pylori to survive during host-infection and other stress challenges. A model for DNA binding/condensation is proposed that accounts for all the experimental observations.

Published

2007

29. In vivo targeting of cutaneous melanoma using an melanoma stimulating hormone-engineered human protein cage with fluorophore and magnetic resonance imaging tracers

Author

Manuela Fornara, Cristina Maria Failla, Jiri Krizan, Giulia Carpinelli, Dmitry Stakheev, Veronica Morea, Elisabetta Falvo, Lenka Rajsiglova, Miriam Carbo, Rossella Canese, Serena Cecchetti, Pierpaolo Ceci, Luca Vannucci, and Alberto Boffi

Subjects

Pathology, medicine.medical_specialty, Skin Neoplasms, Materials science, Fluorophore, Biomedical Engineering, Contrast Media, Pharmaceutical Science, Medicine (miscellaneous), In vivo melanoma-targeting, Bioengineering, Nanocapsules, law.invention, Metastasis, Mice, chemistry.chemical_compound, Confocal microscopy, law, In vivo, Cell Line, Tumor, medicine, Protein-based nanoparticles, Animals, General Materials Science, Magnetic resonance imaging (MRI), Particle Size, Receptor, Melanoma, Fluorescent Dyes, Ferritin, technology, industry, and agriculture, Spectroscopy (MRS), medicine.disease, Magnetic Resonance Imaging, Mice, Inbred C57BL, Microscopy, Fluorescence, chemistry, alpha-MSH, Cutaneous melanoma, Cancer research, hormones, hormone substitutes, and hormone antagonists

Abstract

Nanoparticle (NP)-based materials are promising agents for enhancing cancer diagnosis and treatment. Once functionalized for selective targeting of tumor-expressed molecules, they can specifically deliver drugs and diagnostic molecules inside tumor cells. In the present work, we evaluated the in vivo melanoma-targeting ability of a nanovector (HFt-MSH-PEG) based on human protein ferritin (HFt), functionalized with both melanoma-targeting melanoma stimulating hormone (α-MSH) and stabilizing poly(ethylene glycol) (PEG) molecules. Independent and complementary techniques, such as whole-specimen confocal microscopy and magnetic resonance imaging, were used to detect in vivo localization of NP constructs with suitable tracers (i.e., fluorophores or magnetic metals). Targeted HFt-MSH-PEG NPs accumulated persistently at the level of primary melanoma and with high selectivity with respect to other organs. Melanoma localization of untargeted HFt-PEG NPs, which lack the α-MSH moiety, was less pronounced. Furthermore, HFt-MSH-PEG NPs accumulated to a significantly lower extent and with a different distribution in a diverse type of tumor (TS/A adenocarcinoma), which does not express α-MSH receptors. Finally, in a spontaneous lung metastasis model, HFt-MSH-PEG NPs localized at the metastasis level as well. These results suggest that HFt-MSH-PEG NPs are suitable carriers for selective in vivo delivery of diagnostic or therapeutic agents to cutaneous melanoma.

Published

2015

30. Antioxidant Dps protein from the thermophilic cyanobacterium Thermosynechococcus elongatus

Author

F. Alaleona, Stefano Franceschini, Andrea Ilari, Pierpaolo Ceci, and Emilia Chiancone

Subjects

Protein family, Stereochemistry, Hydrogen bond, Thermophile, Cell Biology, Biochemistry, Catalysis, Hydrophobic effect, chemistry.chemical_compound, Crystallography, chemistry, Hydrogen peroxide, Molecular Biology, DNA, Thermostability

Abstract

DNA-binding proteins from starved cells (Dps proteins) protect bacteria primarily from oxidative damage. They are composed of 12 identical subunits assembled with 23-symmetry to form a compact cage-like structure known to be stable at temperatures > 70 °C and over a wide pH range. Thermosynechococcus elongatus Dps thermostability is increased dramatically relative to mesophilic Dps proteins. Hydrophobic interactions at the dimeric and trimeric interfaces called Dps-like are replaced by salt bridges and hydrogen bonds, a common strategy in thermophiles. Moreover, the buried surface area at the least-extended Dps-like interface is significantly increased. A peculiarity of T. elongatus Dps is the presence of a chloride ion coordinated with threefold symmetry-related arginine residues lining the opening of the Dps-like pore toward the internal cavity. T. elongatus Dps conserves the unusual intersubunit ferroxidase centre that allows the Dps protein family to oxidize Fe(II) with hydrogen peroxide, thereby inhibiting free radical production via Fenton chemistry. This catalytic property is of special importance in T. elongatus (which lacks the catalase gene) in the protection of DNA and photosystems I and II from hydrogen peroxide-mediated oxidative damage.

Published

2006

31. The Dps Protein of Agrobacterium tumefaciens Does Not Bind to DNA but Protects It toward Oxidative Cleavage

Author

Elisabetta Falvo, Pierpaolo Ceci, Andrea Ilari, and Emilia Chiancone

Subjects

chemistry.chemical_classification, Radical, Iron-binding proteins, Cell Biology, Agrobacterium tumefaciens, Biology, medicine.disease_cause, biology.organism_classification, Biochemistry, Amino acid, chemistry.chemical_compound, chemistry, medicine, biology.protein, Hydroxyl radical, Protein A, Molecular Biology, Escherichia coli, DNA

Abstract

Agrobacterium tumefaciens Dps (DNA-binding proteins from starved cells), encoded by the dps gene located on the circular chromosome of this plant pathogen, was cloned, and its structural and functional properties were determined in vitro. In Escherichia coli Dps, the family prototype, the DNA binding properties are thought to be associated with the presence of the lysine-containing N-terminal tail that extends from the protein surface into the solvent. The x-ray crystal structure of A. tumefaciens Dps shows that the positively charged N-terminal tail, which is 11 amino acids shorter than in the E. coli protein, is blocked onto the protein surface. This feature accounts for the lack of interaction with DNA. The intersubunit ferroxidase center characteristic of Dps proteins is conserved and confers to the A. tumefaciens protein a ferritin-like activity that manifests itself in the capacity to oxidize and incorporate iron in the internal cavity and to release it after reduction. In turn, sequestration of Fe(II) correlates with the capacity of A. tumefaciens Dps to reduce the production of hydroxyl radicals from H2O2 through Fenton chemistry. These data demonstrate conclusively that DNA protection from oxidative damage in vitro does not require formation of a Dps-DNA complex. In vivo, the hydroxyl radical scavenging activity of A. tumefaciens Dps may be envisaged to act in concert with catalase A to counteract the toxic effect of H2O2, the major component of the plant defense system when challenged by the bacterium.

Published

2003

32. Iron and Hydrogen Peroxide Detoxification Properties of DNA-binding Protein from Starved Cells

Author

N. Dennis Chasteen, Laura Giangiacomo, Emilia Chiancone, Thomas M. Laue, Guanghua Zhao, Andrea Ilari, and Pierpaolo Ceci

Subjects

biology, Spin trapping, DNA-binding protein from starved cells, Inorganic chemistry, Cell Biology, engineering.material, Biochemistry, Medicinal chemistry, Ferrous, Hydrous ferric oxides, Ferritin, chemistry.chemical_compound, chemistry, medicine, engineering, biology.protein, Ferric, Hydroxyl radical, Hydrogen peroxide, Molecular Biology, medicine.drug

Abstract

The DNA-binding proteins from starved cells (Dps) are a family of proteins induced in microorganisms by oxidative or nutritional stress. Escherichia coli Dps, a structural analog of the 12-subunit Listeria innocua ferritin, binds and protects DNA against oxidative damage mediated by H(2)O(2). Dps is shown to be a Fe-binding and storage protein where Fe(II) oxidation is most effectively accomplished by H(2)O(2) rather than by O(2) as in ferritins. Two Fe(2+) ions bind at each of the 12 putative dinuclear ferroxidase sites (P(Z)) in the protein according to the equation, 2Fe(2+) + P(Z) --> [(Fe(II)(2)-P](FS)(Z+2) + 2H(+). The ferroxidase site (FS) bound iron is then oxidized according to the equation, [(Fe(II)(2)-P](FS)(Z+2) + H(2)O(2) + H(2)O --> [Fe(III)(2)O(2)(OH)-P](FS)(Z-1) + 3H(+), where two Fe(II) are oxidized per H(2)O(2) reduced, thus avoiding hydroxyl radical production through Fenton chemistry. Dps acquires a ferric core of approximately 500 Fe(III) according to the mineralization equation, 2Fe(2+) + H(2)O(2) + 2H(2)O --> 2Fe(III)OOH((core)) + 4H(+), again with a 2 Fe(II)/H(2)O(2) stoichiometry. The protein forms a similar ferric core with O(2) as the oxidant, albeit at a slower rate. In the absence of H(2)O(2) and O(2), Dps forms a ferrous core of approximately 400 Fe(II) by the reaction Fe(2+) + H(2)O + Cl(-) --> Fe(II)OHCl((core)) + H(+). The ferrous core also undergoes oxidation with a stoichiometry of 2 Fe(II)/H(2)O(2). Spin trapping experiments demonstrate that Dps greatly attenuates hydroxyl radical production during Fe(II) oxidation by H(2)O(2). These results and in vitro DNA damage assays indicate that the protective effect of Dps on DNA most likely is exerted through a dual action, the physical association with DNA and the ability to nullify the toxic combination of Fe(II) and H(2)O(2). In the latter process a hydrous ferric oxide mineral core is produced within the protein, thus avoiding oxidative damage mediated by Fenton chemistry.

Published

2002

33. The Mutation K30D Disrupts the Only Salt Bridge at the Subunit Interface of the Homodimeric Hemoglobin from Scapharca inaequivalvis and Changes the Mechanism of Cooperativity

Author

Pierpaolo Ceci, Emilia Chiancone, Laura Giangiacomo, and Alberto Boffi

Subjects

Low protein, Stereochemistry, Protein subunit, Mutant, Cooperativity, Heme, Ligands, Biochemistry, Hemoglobins, chemistry.chemical_compound, Escherichia coli, Animals, Molecular Biology, Dose-Response Relationship, Drug, Lysine, Cell Biology, Hydrogen-Ion Concentration, Oxygen, Kinetics, Crystallography, chemistry, Mollusca, Sedimentation equilibrium, Mutation, Mutagenesis, Site-Directed, Salts, Salt bridge, Hemoglobin, Dimerization, Ultracentrifugation, Hydrogen, Protein Binding

Abstract

The subunit interface of the homodimeric hemoglobin from Scapharca inaequivalvis, HbI, is stabilized by a network of interactions that involve several hydrogen-bonded structural water molecules, a hydrophobic patch, and a single, symmetrical salt bridge between residues Lys-30 and Asp-89. Upon mutation of Lys-30 to Asp, the interface is destabilized markedly. Sedimentation equilibrium and velocity experiments allowed the estimate of the dimerization constants for the unliganded (K(1,2D) = 8 x 10(4) M(-1)) and for the CO-bound (K(1,2L) = 1 x 10(3) m(-1)) and oxygenated (K(1,2L) = 70 m(-1)) derivatives. For the oxygenated derivative, the destabilization of the subunit interface with respect to native HbI corresponds to about 8 kcal/mol, an unexpectedly high figure. In the K30D mutant, at variance with the native protein, oxygen affinity and cooperativity are strongly dependent on protein concentration. At low protein concentrations (e.g. 1.2 x 10(-5) m heme), at which the monomeric species becomes significant also in the unliganded derivative, oxygen affinity increases and cooperativity decreases. At protein concentrations where both derivatives are dimeric (e.g. 3.3 x 10(-3) m heme), both cooperativity and oxygen affinity decrease. Taken together, the experimental data indicate that in the K30D mutant, the mechanism of cooperativity is drastically altered and is driven by a ligand-linked monomer-dimer equilibrium rather than being based on a direct heme-heme communication as in native HbI.

Published

2002

34. Intra- and interparticle magnetism of cobalt-doped iron-oxide nanoparticles encapsulated in a synthetic ferritin cage

Author

OI Kasyutich, J. van Lierop, Elisabetta Falvo, John W. Freeland, Elizabeth Skoropata, Pierpaolo Ceci, and Ryan D. Desautels

Subjects

inorganic chemicals, Materials science, Mössbauer effect, Dopant, Magnetism, chemistry.chemical_element, Nanotechnology, Condensed Matter Physics, Electronic, Optical and Magnetic Materials, Crystallography, chemistry, Octahedron, Content (measure theory), Absorption (logic), Cobalt, Superparamagnetism

Abstract

We present an in-depth examination of the composition and magnetism of cobalt $({\mathrm{Co}}^{2+})$-doped iron-oxide nanoparticles encapsulated in Pyrococcus furiosus ferritin shells. We show that the ${\mathrm{Co}}^{2+}$ dopant ions were incorporated into the $\ensuremath{\gamma}\text{\ensuremath{-}}{\mathrm{Fe}}_{2}{\mathrm{O}}_{3}/{\mathrm{Fe}}_{3}{\mathrm{O}}_{4}$ core, with small paramagnetic-like clusters likely residing on the surface of the nanoparticle that were observed for all cobalt-doped samples. In addition, element-specific characterization using M\"ossbauer spectroscopy and polarized x-ray absorption indicated that ${\mathrm{Co}}^{2+}$ was incorporated exclusively into the octahedral B sites of the spinel-oxide nanoparticle. Comparable superparamagnetic blocking temperatures, coercivities, and effective anisotropies were obtained for 7%, 10%, and 12% cobalt-doped nanoparticles, and were only slightly reduced for 3% cobalt, indicating a strong effect of cobalt incorporation, with a lesser effect of cobalt content. Due to the regular particle size and separation that result from the use of the ferritin cage, a comparison of the effects of interparticle interactions on the disordered assembly of nanoparticles was also obtained that indicated significantly different behaviors between undoped and cobalt-doped nanoparticles.

Published

2014

35. Multifunctional Protein-Based Nanoparticles for Cancer Theranosis

Author

Elisabetta Falvo, Pierpaolo Ceci, and Luca Vannucci

Subjects

Drug, Chemistry, media_common.quotation_subject, medicine.medical_treatment, Cancer, Nanoparticle, Nanotechnology, medicine.disease, Targeted therapy, Drug delivery, Cancer cell, medicine, Nanocarriers, media_common

Abstract

Selective delivery of therapeutic and/or diagnostic (theranostic) agents to diseased sites represents a major challenge to improve the outcome of current therapy and our ability to detect cancer cells at early stages or in the spread sites. A promising route to reach this goal is the design and engineering of functionalized nanoparticle (NP)-based carriers for targeted delivery of drug or diagnostic agents. Protein-based nanocarriers are attracting growing interest due to their exceptional characteristics, namely biodegradability, solubility, functionalization versatility and extraordinary binding capacity of various drugs. We highlight the use of these cage-shaped protein-based materials, with special emphasis on ferritin, as smart building blocks for the development of multifunctional NPs for cancer theranosis.

Published

2014

36. Antibody-drug conjugates: targeting melanoma with cisplatin encapsulated in protein-cage nanoparticles based on human ferritin

Author

Elisabetta Falvo, Alberto Boffi, Rocco Fraioli, Carlotta Zamparelli, Veronica Morea, Patrizio Giacomini, Elisa Tremante, Carlo Leonetti, and Pierpaolo Ceci

Subjects

Materials science, Immunoconjugates, medicine.drug_class, Drug Compounding, Mice, Nude, Antineoplastic Agents, Monoclonal antibody, Flow cytometry, Mice, Antigen, medicine, Tumor Cells, Cultured, Animals, Humans, General Materials Science, Melanoma, Cisplatin, Drug Carriers, biology, medicine.diagnostic_test, medicine.disease, Xenograft Model Antitumor Assays, Ferritin, Immunology, Ferritins, Cancer research, biology.protein, Nanoparticles, Antibody, Breast carcinoma, medicine.drug

Abstract

A novel antibody-drug conjugate (ADC) was synthesized incorporating ferritin-based nanoparticles. An average of three molecules of monoclonal antibody (mAb) Ep1 to the human melanoma-specific antigen CSPG4 were conjugated to a single ferritin cage encapsulating about 50 cisplatin molecules (HFt-Pt-Ep1). The HFt-Pt-Ep1 nanoparticle had an estimated molecular size of about 900 kD and 33 nm, and flow cytometry demonstrated specific binding to a CSPG4(+) melanoma cell line, but not to a CSPG4(-) breast carcinoma cell line. As compared to the cisplatin-containing ferritin nanoparticle alone (HFt-Pt), which inhibited thymidine incorporation more efficiently in breast carcinoma than melanoma cells, the mAb-derivatized HFt-Pt-Ep1 nanoparticle had a 25-fold preference for the latter. A similar preference for melanoma was observed upon systemic intravenous administration of HFt-Pt-Ep1 to nude mice xenotransplanted with pre-established, palpable melanoma and breast carcinoma tumors. Thus, we have been able to determine precise combinations and stoichiometric relationships between mAbs and nanoparticle protein cages, whereby the latter lose their tropism for ubiquitously distributed cellular receptors, and acquire instead remarkably lineage-selective binding. HFt-Pt-Ep1 is therefore an interesting model to improve the therapeutic index of antiblastic therapy in a tumor such as melanoma, which at its advanced stages is totally refractory to mono- and combination-chemotherapy.

Published

2013

37. ChemInform Abstract: The Heck Reaction of Allylic Alcohols Catalyzed by Palladium Nanoparticles in Water: Chemoenzymatic Synthesis of (R)-(-)-Rhododendrol

Author

Sandra Niembro, Alberto Boffi, Roberto Cirilli, Sandro Cacchi, Giancarlo Fabrizi, Alexandr Shafir, Adelina Vallribera, Alessandro Prastaro, and Pierpaolo Ceci

Subjects

inorganic chemicals, Allylic rearrangement, Chemistry, Silica gel, organic chemicals, Aryl, food and beverages, Palladium nanoparticles, General Medicine, Catalysis, chemistry.chemical_compound, Heck reaction, Rhododendrol, Organic chemistry

Abstract

The use of phosphine-free palladium nanoparticles immobilized on fluorous silica gel in the Heck reaction of aryl iodides with allylic alcohols in water is described.

Published

2011

38. Looking for quantum effects in magnetic nanoparticles using the molecular nanomagnet approach

Author

Maria Fittipaldi, Dante Gatteschi, Lorenzo Sorace, Claudia Innocenti, Pierpaolo Ceci, Claudio Sangregorio, and Lisa Castelli

Subjects

Paramagnetism, Fermi contact interaction, Materials science, Condensed matter physics, Spin echo, Magnetic nanoparticles, Magnetic resonance force microscopy, Magnetic force microscope, Condensed Matter Physics, Ferromagnetic resonance, Nanomagnet, Electronic, Optical and Magnetic Materials

Published

2011

39. DNA-Binding Proteins From Starved Cells (Dps Proteins)

Author

Simonetta Stefanini, Matteo Ardini, Pierpaolo Ceci, and Andrea Ilari

Subjects

DNA protection, ferritin superfamily, DNA-binding proteins from starved cells, Oxidative phosphorylation, medicine.disease_cause, Ferroxidase activity, DNA-binding protein, chemistry.chemical_compound, iron detoxification/incorporation, medicine, oxidative stress, DNA binding, DNA-binding proteins from starved cells, ferritin superfamily, ferroxidase activity, oxidative stress, DNA binding, DNA protection, iron detoxification/incorporation, ferroxidase activity, biology, DNA‐binding proteins from starved cells, Cell biology, Ferritin, Biochemistry, chemistry, biology.protein, Ceruloplasmin, DNA, Oxidative stress, DNA‐binding proteins from starved cells, ferritin superfamily, ferroxidase activity, oxidative stress, DNA binding, DNA protection, iron detoxification/incorporation

Abstract

In the recent past over 200 Dps (DNA-binding proteins from starved cells) proteins have been identified in bacterial genomes. Dps proteins belong to the ferritin superfamily. They are expressed under conditions of oxidative and/or nutritional stress and are characterized by a highly conserved shell-like structure of 12 identical subunits assembled with 23 symmetry. The internal cavity is designed to accommodate up to 500 iron/atoms per molecule in a soluble and bioavailable form. Dps proteins play an important role in the complex protection mechanism against oxidative damage. The presence of a highly conserved ferroxidase center, which uses hydrogen peroxide as physiological iron oxidant, confers to all Dps proteins the capacity to decrease the production of the hydroxyl-radicals and, hence, to prevent the damage to DNA and other cellular components. Ferroxidase activity is of special importance in pathogenic bacteria since production of hydrogen peroxide in macrophages and neutrophiles represents one of the first host defense mechanisms. The capacity to bind DNA in a nonspecific manner and pack it into condensed structures, an attribute limited to some members of the family, represents the second distinctive mechanism used to advantage by Dps proteins for the survival of the organism. 3D Structure Keywords: DNA-binding proteins from starved cells; ferritin superfamily; ferroxidase activity; oxidative stress; DNA binding; DNA protection; iron detoxification/incorporation

Published

2011

40. ChemInform Abstract: Homocoupling of Arylboronic Acids and Potassium Aryltrifluoroborates Catalyzed by Protein-Stabilized Palladium Nanoparticles under Air in Water

Author

Alessandro Prastaro, Pierpaolo Ceci, Emilia Chiancone, Sandro Cacchi, Giancarlo Fabrizi, and Alberto Boffi

Subjects

inorganic chemicals, chemistry, Thermophile, Potassium, chemistry.chemical_element, Organic chemistry, Palladium nanoparticles, macromolecular substances, General Medicine, Catalysis

Abstract

The palladium nanoparticles are stabilized primarily within the protein cavity of a highly thermostable Dps protein from the thermophilic bacterium Thermosynechoccus elongatus.

Published

2010

41. ChemInform Abstract: Suzuki-Miyaura Cross-Coupling Catalyzed by Protein-Stabilized Palladium Nanoparticles under Aerobic Conditions in Water: Application to a One-Pot Chemoenzymatic Enantioselective Synthesis of Chiral Biaryl Alcohols

Author

Alberto Boffi, Roberto Cirilli, Alessandro Prastaro, Pierpaolo Ceci, Emilia Chiancone, Annarita Stringaro, Marisa Colone, Giancarlo Fabrizi, and Sandro Cacchi

Subjects

inorganic chemicals, Chemistry, DNA-binding protein from starved cells, Enantioselective synthesis, Palladium nanoparticles, General Medicine, Combinatorial chemistry, Catalysis

Abstract

The preparation of palladium nanoparticles stabilized primarily within the protein cavity of a highly thermostable Dps protein (DNA binding protein from starved cells) and the use of this precatalyst system in Suzuki-Miyaura cross-coupling reactions under aerobic conditions in water is described, as well as a two-step one-pot Suzuki-Miyaura cross-coupling followed by an enantioselective enzyme-catalyzed reduction to form chiral biaryl alcohols.

Published

2010

42. Thermosynechococcus elongatus DpsA binds Zn(II) at a unique three histidine-containing ferroxidase center and utilizes O2 as iron oxidant with very high efficiency, unlike the typical Dps proteins

Author

Flaminia, Alaleona, Stefano, Franceschini, Pierpaolo, Ceci, Andrea, Ilari, and Emilia, Chiancone

Subjects

Models, Molecular, Iron, Molecular Sequence Data, Ceruloplasmin, Crystallography, X-Ray, Cyanobacteria, Protein Structure, Tertiary, DNA-Binding Proteins, Oxygen, Zinc, Amino Acid Substitution, Bacterial Proteins, Histidine, Amino Acid Sequence, Oxidation-Reduction, Sequence Alignment

Abstract

The cyanobacterium Thermosynechococcus elongatus is one the few bacteria to possess two Dps proteins, DpsA-Te and Dps-Te. The present characterization of DpsA-Te reveals unusual structural and functional features that differentiate it from Dps-Te and the other known Dps proteins. Notably, two Zn(II) are bound at the ferroxidase center, owing to the unique substitution of a metal ligand at the A-site (His78 in place of the canonical aspartate) and to the presence of a histidine (His164) in place of a hydrophobic residue at a metal-coordinating distance in the B-site. Only the latter Zn(II) is displaced by incoming iron, such that Zn(II)-Fe(III) complexes are formed upon oxidation, as indicated by absorbance and atomic emission spectroscopy data. In contrast to the typical behavior of Dps proteins, where Fe(II) oxidation by H(2)O(2) is about 100-fold faster than by O(2), in DpsA-Te the ferroxidation efficiency of O(2) is very high and resembles that of H(2)O(2). Oxygraphic experiments show that two Fe(II) are required to reduce O(2), and that H(2)O(2) is not released into solution at the end of the reaction. On this basis, a reaction mechanism is proposed that also takes into account the formation of Zn(II)-Fe(III) complexes. The physiological significance of the DpsA-Te behavior is discussed in the framework of a possible localization of the protein at the thylakoid membranes, where photosynthesis takes place, with the consequent increased formation of reactive oxygen species.

Published

2010

43. Homocoupling of arylboronic acids and potassium aryltrifluoroborates catalyzed by protein-stabilized palladium nanoparticles under air in water

Author

Emilia Chiancone, Alberto Boffi, Giancarlo Fabrizi, Alessandro Prastaro, Pierpaolo Ceci, and Sandro Cacchi

Subjects

inorganic chemicals, biology, Chemistry, Potassium, Thermophile, DNA-binding protein from starved cells, Organic Chemistry, water, Palladium nanoparticles, chemistry.chemical_element, biology.organism_classification, Biochemistry, Combinatorial chemistry, proteins, Catalysis, potassium aryltrifluoroborates, arylboronic acids, Drug Discovery, palladium nanoparticles, Efficient catalyst, Bacteria

Abstract

Palladium nanoparticles stabilized primarily within the protein cavity of a highly thermostable Dps protein (DNA binding protein from starved cells) from the thermophilic bacterium Thermosynechoccus elongatus provide an efficient catalyst for the homocoupling of boronic acids and potassium aryltrifluoroborates in water under aerobic phosphine-free conditions. Symmetrical biaryls have been isolated in good to excellent yields. Potassium aryltrifluoroborates give similar or better results than the corresponding arylboronic acids.

Published

2010

44. The multifaceted capacity of Dps proteins to combat bacterial stress conditions: Detoxification of iron and hydrogen peroxide and DNA binding

Author

Emilia Chiancone and Pierpaolo Ceci

Subjects

DNA, Bacterial, Models, Molecular, dps-dna interaction, Iron, Molecular Sequence Data, Adaptation, Biological, Biophysics, Microbial metabolism, review, Plasma protein binding, Oxidative phosphorylation, Biology, medicine.disease_cause, Ferroxidase activity, Biochemistry, chemistry.chemical_compound, Bacterial Proteins, Stress, Physiological, medicine, Animals, Humans, Nucleoid, Amino Acid Sequence, dps (dna-binding proteins from starved cells) protein, Hydrogen peroxide, Molecular Biology, Escherichia coli, ferroxidase activity, Sequence Homology, Amino Acid, Hydrogen Peroxide, microbial survival, protection under oxidative damage condition, DNA-Binding Proteins, chemistry, Inactivation, Metabolic, DNA, Protein Binding

Abstract

Background The widely expressed Dps proteins, so named after the DNA-binding properties of the first characterized member of the family in Escherichia coli, are considered major players in the bacterial response to stress. Scope of review The review describes the distinctive features of the “ferritin-like” ferroxidation reaction, which uses hydrogen peroxide as physiological iron oxidant and therefore permits the concomitant removal of the two reactants that give rise to hydroxyl radicals via Fenton chemistry. It also illustrates the structural elements identified to date that render the interaction of some Dps proteins with DNA possible and outlines briefly the significance of Dps–DNA complex formation and of the Dps interaction with other DNA-binding proteins in relation to the organization of the nucleoid and microbial survival. General significance Understanding in molecular terms the distinctive role of Dps proteins in bacterial resistance to general and specific stress conditions. Major conclusions The state of the art is that the response to oxidative and peroxide-mediated stress is mediated directly by Dps proteins via their ferritin-like activity. In contrast, the response to other stress conditions derives from the concerted interplay of diverse interactions that Dps proteins may establish with DNA and with other DNA-binding proteins.

Published

2010

45. Dps (DNA binding proteins from starved cell)proteins

Author

Stefanini, Simonetta, Pierpaolo, Ceci, and Ardini, Matteo

Published

2010

46. Inhibitory effect of silver nanoparticles on trypanothione reductase activity and leishmania infantum proliferation

Author

Stefania Orsini, Marina Gramiccia, Pierpaolo Ceci, Andrea Ilari, Gianni Colotti, Paola Baiocco, and Trentina Di Muccio

Subjects

Glutathione reductase, Trypanothione, 02 engineering and technology, Biochemistry, Silver nanoparticle, 03 medical and health sciences, chemistry.chemical_compound, leishmania, Drug Discovery, silver, Amastigote, 030304 developmental biology, 0303 health sciences, drug delivery, nanoparticles, trypanothione reductase, biology, Organic Chemistry, Glutathione, 021001 nanoscience & nanotechnology, biology.organism_classification, Leishmania, In vitro, 3. Good health, chemistry, Leishmania infantum, 0210 nano-technology

Abstract

In Leishmania the glutathione/glutathione reductase eukaryotic redox sys-tem is replaced by the unique trypanothione/trypanothione reductase (TR) system. In vitro, silver is a more effective TR inhibitor than antimony, the first line drug against leishmaniasis in most endemic countries, and its mechanism of inhibition is similar to that of Sb(III). In particular, silver binds with high affinity to the catalytic triad Cys52, Cys57, and His461', thereby inhibiting TR. Here, Ag(0) activity was tested on the promastigote and amastigote stages of Leishmania infantum using a drug-delivery system consisting in Ag(0) nanoparticles encapsulated by ferritin molecules (PfFt-AgNPs). These were able to induce an antiproliferative effect on the parasites at metal concentrations lower than those used with antimony.

Published

2010

47. Synthesis of Iron Oxide Nanoparticles in Listeria innocua Dps (DNA-Binding Protein from Starved Cells): A Study with the Wild-Type Protein and a Catalytic Centre Mutant

Author

Giuliano Bellapadrona, OI Kasyutich, Dante Gatteschi, Emilia Chiancone, Claudio Sangregorio, Maria Fittipaldi, Claudia Innocenti, Lisa Castelli, and Pierpaolo Ceci

Subjects

Listeria, DNA-binding protein from starved cells, Organic Chemistry, Inorganic chemistry, Iron oxide, Nanoparticle, Maghemite, Ceruloplasmin, General Chemistry, engineering.material, Ferric Compounds, Catalysis, DNA-Binding Proteins, chemistry.chemical_compound, Magnetic anisotropy, chemistry, Chemical engineering, Bacterial Proteins, engineering, Magnetic nanoparticles, Nanoparticles, HYDROGEN-PEROXIDE DETOXIFICATION, HIGH-SPIN MOLECULES, GROUND-STATE SPINS, HIGH-FREQUENCY EPR, MAGNETIC-PROPERTIES, FERROMAGNETIC-RESONANCE, ESCHERICHIA-COLI, GAMMA-FE2O3 NANOPARTICLES, CONSTRAINED SYNTHESIS, FERROXIDASE CENTER, Iron oxide nanoparticles, Superparamagnetism

Abstract

A comparative analysis of the magnetic properties of iron oxide nanoparticles grown in the cavity of the DNA-binding protein from starved cells of the bacterium Listeria innocua, LiDps, and of its triple-mutant lacking the catalytic ferroxidase centre, LiDps-tm, is presented. TEM images and static and dynamic magnetic and electron magnetic resonance (EMR) measurements reveal that, under the applied preparation conditions, namely alkaline pH, high temperature (65 degrees C), exclusion of oxygen, and the presence of hydrogen peroxide, maghemite and/or magnetite nanoparticles with an average diameter of about 3 nm are mineralised inside the cavities of both LiDps and LiDps-tm. The magnetic nanoparticles (MNPs) thus formed show similar magnetic properties, with superparamagnetic behaviour above 4.5 K and a large magnetic anisotropy. Interestingly, in the EMR spectra ail absorption at half-field is observed, which call be considered as a manifestation of the quantum behaviour of the MNPs. These results indicate that Dps proteins call be advantageously used for the production of nanomagnets at the interface between molecular Clusters and traditional MNPs and that the presence of the ferroxidase centre, though increasing the efficiency of nanoparticle formation, does not affect the nature and fine structure of the MNPs. Importantly, the self-organisation of MNP-containing Dps on HRTEM grids suggests that Dps-enclosed MNPs can be deposited oil surfaces in ail ordered fashion.

Published

2010

48. Role of Dps (DNA-binding proteins from starved cells) aggregation on DNA

Author

Pierpaolo Ceci and Emilia Chiancone

Subjects

DNA, Bacterial, Models, Molecular, HMG-box, biology, Sequence Homology, Amino Acid, DNA damage, Molecular Sequence Data, Ferroxidase activity, DNA-binding protein, Models, Biological, Cell biology, Single-stranded binding protein, DNA-Binding Proteins, chemistry.chemical_compound, chemistry, Bacterial Proteins, biology.protein, Nucleoid organization, Hydroxyl radical, Amino Acid Sequence, Protein Multimerization, Protein Structure, Quaternary, DNA, Protein Binding

Abstract

The review outlines the experimental studies that have led to the current understanding at a molecular level of the protective role exerted by Dps proteins under stress conditions. After a brief description of the structural signatures and of the ferroxidase activity, which confers to all Dps proteins the capacity to decrease the hydroxyl radical induced DNA damage, the interaction of some family members with DNA is analysed. Special emphasis is given to the Dps structural elements that render the interaction with DNA possible and to the consequences that complex formation has on nucleoid organization and microbial survival.

Published

2009

49. Dps proteins prevent Fenton-mediated oxidative damage by trapping hydroxyl radicals within the protein shell

Author

Emilia Chiancone, Pierpaolo Ceci, Giuliano Bellapadrona, Simonetta Stefanini, and Matteo Ardini

Subjects

Hydroxyl radicals, DNA protection, Listeria, Radical, Iron, Free radicals, Apoptosis, Oxidative phosphorylation, medicine.disease_cause, Biochemistry, chemistry.chemical_compound, Bacterial Proteins, Physiology (medical), Catalytic Domain, medicine, Escherichia coli, Site-Directed, Hydrogen peroxide, Fenton chemistry, Chemistry, Hydroxyl Radical, Mutagenesis, Intraprotein radicals, Ceruloplasmin, Free Radical Scavengers, Hydrogen Peroxide, Dps proteins, DNA-Binding Proteins, Oxidative Stress, Mutagenesis, Site-Directed, Hydroxyl radical, Mutant Proteins, Oxidation-Reduction, Protein Binding, Oxidative stress, DNA

Abstract

Dps (DNA-binding proteins from starved cells) proteins belong to a widespread bacterial family of proteins expressed under nutritional and oxidative stress conditions. In particular, Dps proteins protect DNA against Fenton-mediated oxidative stress, as they catalyze iron oxidation by hydrogen peroxide at highly conserved ferroxidase centers and thus reduce significantly hydroxyl radical production. This work investigates the possible generation of intraprotein radicals during the ferroxidation reaction by Escherichia coli and Listeria innocua Dps, two representative members of the family. Stopped-flow analyses show that the conserved tryptophan and tyrosine residues located near the metal binding/oxidation center are in a radical form after iron oxidation by hydrogen peroxide. DNA protection assays indicate that the presence of both residues is necessary to limit release of hydroxyl radicals in solution and the consequent oxidative damage to DNA. In general terms, the demonstration that conserved protein residues act as a trap that dissipates free electrons generated during the oxidative process brings out a novel role for the Dps protein cage.

Published

2009

50. Periplasmic Cu,Zn superoxide dismutase and cytoplasmic Dps concur in protecting Salmonella enterica serovar Typhimurium from extracellular reactive oxygen species

Author

Emilia Chiancone, Paolo Pasquali, Serena Ammendola, Francesca Pacello, Andrea Battistoni, and Pierpaolo Ceci

Subjects

Salmonella typhimurium, Cytoplasm, sodC, Mutant, Biophysics, Biochemistry, Microbiology, Superoxide dismutase, chemistry.chemical_compound, Mice, Bacterial Proteins, Phagocytosis, Superoxides, Oxidative damage, Extracellular, Animals, Settore BIO/10, Molecular Biology, Cu, Respiratory Burst, chemistry.chemical_classification, Reactive oxygen species, NADPH oxidase, biology, Superoxide, Superoxide Dismutase, Salmonella enterica, Zn superoxide dismutase, Periplasmic space, Hydrogen Peroxide, Cu,Zn superoxide dismutase, Dps, sodC, Salmonella enterica, Respiratory burst, DNA-Binding Proteins, chemistry, Mutation, biology.protein, Dps, Reactive Oxygen Species

Abstract

Several bacteria possess periplasmic Cu,Zn superoxide dismutases which can confer protection from extracellular reactive oxygen species. Thus, deletion of the sodC1 gene reduces Salmonella enterica serovar Typhimurium ability to colonize the spleens of wild type mice, but enhances virulence in p47phox mutant mice. To look into the role of periplamic Cu,Zn superoxide dismutase and into possible additive effects of the ferritin-like Dps protein involved in hydrogen peroxide detoxification, we have analyzed bacterial survival in response to extracellular sources of superoxide and/or hydrogen peroxide. Exposure to extracellular superoxide of Salmonella Typhimurium mutant strains lacking the sodC1 and sodC2 genes and/or the dps gene does not cause direct killing of bacteria, indicating that extracellular superoxide is poorly bactericidal. In contrast, all mutant strains display a sharp hydrogen peroxide-dependent loss of viability, the dps,sodC1,sodC2 mutant being less resistant than the dps or the sodC1,sodC2 mutants. These findings suggest that the role of Cu,Zn superoxide dismutase in bacteria is to remove rapidly superoxide from the periplasm to prevent its reaction with other reactive molecules. Moreover, the nearly additive effect of the sodC and dps mutations suggests that localization of antioxidant enzymes in different cellular compartments is required for bacterial resistance to extracytoplasmic oxidative attack.

Published

2008