Your search keyword '"Anna Morisco"' showing total 16 results

1. On site production of [18F]PSMA-1007 using different [18F]fluoride activities: practical, technical and economical impact

Author

Costantina Maisto, Anna Morisco, Roberta de Marino, Elisabetta Squame, Valentina Porfidia, Laura D’Ambrosio, Daria Di Martino, Paolo Gaballo, Michela Aurilio, Monica Buonanno, Aureliana Esposito, Marco Raddi, and Secondo Lastoria

Subjects

[18F]fluoride, Time of beam, [18F]PSMA-1007, Radiochemical yield (RCY), Radiochemical purity (RCP), Stability, Medical physics. Medical radiology. Nuclear medicine, R895-920, Therapeutics. Pharmacology, RM1-950

Abstract

Abstract Background Prostate-specific membrane antigen is overexpressed in prostate cancer and it is considered a good target for positron emission tomography/computed tomography imaging of primary cancer and recurrent/metastatic disease, as well as for radioligand therapy. Different PSMA-analogues labeled with [68Ga]gallium have been investigated, showing excellent imaging properties; however, only small amounts can be produced for each radiolabeling. Recently, a [18F]fluoride labeled PSMA-inhibitor, [18F]PSMA-1007, has been introduced, and it has ensured large-scale productions, overcoming this limitation of [68Ga]PSMAs. In this study, PSMA-1007 has been labeled with low (A), medium (B) and high (C) starting activities of [18F]fluoride, in order to verify if radiochemical yield, radiochemical purity and stability of [18F]PSMA-1007 were affected. These parameters have been measured in sixty-five consecutive batches. In addition, the estimation of [18F]PSMA-1007 production costs is provided. Results The radiochemical yield for low and medium activities of [18F]fluoride was 52%, while for the high one it decreased to 40%. The radiochemical purity was 99% for all three activities. [18F]PSMA-1007 did not show radiolysis up to 8 h after the end of synthesis, confirming that the radiopharmaceutical is stable and suitable to perform diagnostic studies in humans for a long period of time after the end of radiolabeling. Furthermore, radiochemical stability was demonstrated in fetal bovine serum at 4 °C and 37 °C for 120′. Conclusions A starting activity of [18F]fluoride of 90 GBq (B) seems to be the best option enabling a final amount of about of 50 GBq of [18F]PSMA-1007, which is promising as it allows to: (a) perform a large number of scans, and/or (b) supply the radiopharmaceutical to any peripheral diagnostic centers in need.

Published

2021

2. Analysis of Pros and Cons in Using [68Ga]Ga-PSMA-11 and [18F]PSMA-1007: Production, Costs, and PET/CT Applications in Patients with Prostate Cancer

Author

Costantina Maisto, Michela Aurilio, Anna Morisco, Roberta de Marino, Monica Josefa Buonanno Recchimuzzo, Luciano Carideo, Laura D’Ambrosio, Francesca Di Gennaro, Aureliana Esposito, Paolo Gaballo, Valentina Pirozzi Palmese, Valentina Porfidia, Marco Raddi, Alfredo Rossi, Elisabetta Squame, and Secondo Lastoria

Subjects

PCa, [68Ga]Ga-PSMA-11, [18F]PSMA-1007, PSMA, [68Ge]/[68Ga] generator, cyclotron RCY, Organic chemistry, QD241-441

Abstract

The aim of this work is to compare [68Ga]Ga-PSMA-11 and [18F]PSMA-1007 PET/CT as imaging agents in patients with prostate cancer (PCa). Comparisons were made by evaluating times and costs of the radiolabeling process, imaging features including pharmacokinetics, and impact on patient management. The analysis of advantages and drawbacks of both radioligands might help to make a better choice based on firm data. For [68Ga]Ga-PSMA-11, the radiochemical yield (RCY) using a low starting activity (L, average activity of 596.55 ± 37.97 MBq) was of 80.98 ± 0.05%, while using a high one (H, average activity of 1436.27 ± 68.68 MBq), the RCY was 71.48 ± 0.04%. Thus, increased starting activities of [68Ga]-chloride negatively influenced the RCY. A similar scenario occurred for [18F]PSMA-1007. The rate of detection of PCa lesions by Positron Emission Tomography/Computed Tomography (PET/CT) was similar for both radioligands, while their distribution in normal organs significantly differed. Furthermore, similar patterns of biodistribution were found among [18F]PSMA-1007, [68Ga]Ga-PSMA-11, and [177Lu]Lu-PSMA-617, the most used agent for RLT. Moreover, the analysis of economical aspects for each single batch of production corrected for the number of allowed PET/CT examinations suggested major advantages of [18F]PSMA-1007 compared with [68Ga]Ga-PSMA-11. Data from this study should support the proper choice in the selection of the PSMA PET radioligand to use on the basis of the cases to study.

Published

2022

3. A comparison of simplified protocols of personalized dosimetry in NEN patients treated by radioligand therapy (RLT) with [177Lu]Lu-DOTATATE to favor its use in clinical practice

Author

Valentina Pirozzi Palmese, Laura D’Ambrosio, Francesca Di Gennaro, Costantina Maisto, Roberta de Marino, Anna Morisco, Sergio Coluccia, Piergiacomo Di Gennaro, Francesco De Lauro, Marco Raddi, Paolo Gaballo, Salvatore Tafuto, Egidio Celentano, and Secondo Lastoria

Subjects

Radiology, Nuclear Medicine and imaging, General Medicine

Abstract

Abstract The role of internal dosimetry is usually proposed for investigational purposes in patients treated by RLT, even if its application is not yet the standard method in clinical practice. This limited use is partially justified by several concomitant factors that make calculations a complex process. Therefore, simplified dosimetry protocols are required. Methods In our study, dosimetric evaluations were performed in thirty patients with NENs who underwent RLT with [177Lu]Lu-DOTATATE. The reference method (M0) calculated the cumulative absorbed dose performing dosimetry after each of the four cycles. Obtained data were employed to assess the feasibility of simplified protocols: defining the dosimetry only after the first cycle (M1) and after the first and last one (M2). Results The mean differences of the cumulative absorbed doses between M1 and M0 were – 10% for kidney, – 5% for spleen, + 34% for liver, + 13% for red marrow, and + 37% for tumor lesions. Conversely, differences lower than ± 10% were measured between M2 and M0. Conclusion Cumulative absorbed doses obtained with the M2 protocol resembled the doses calculated by M0, while the M1 protocol overestimated the absorbed doses in all organs at risk, except for the spleen.

Published

2023

4. On site production of [18F]PSMA-1007 using different [18F]fluoride activities: practical, technical and economical impact

Author

Secondo Lastoria, Daria Di Martino, Roberta de Marino, Elisabetta Squame, Aureliana Esposito, Paolo Gaballo, Anna Morisco, Valentina Porfidia, Marco Raddi, Monica Buonanno, Michela Aurilio, L. D'Ambrosio, and Costantina Maisto

Subjects

Radiochemical yield (RCY), R895-920, Time of beam, RM1-950, urologic and male genital diseases, Analytical Chemistry, chemistry.chemical_compound, Medical physics. Medical radiology. Nuclear medicine, [18F]fluoride, Long period, Radioligand, medicine, Pharmacology (medical), Radiology, Nuclear Medicine and imaging, [18F]PSMA-1007, Membrane antigen, Pharmacology, medicine.diagnostic_test, Chemistry, Radiochemistry, Primary cancer, Positron emission tomography, Yield (chemistry), Radiochemical purity (RCP), Therapeutics. Pharmacology, 18f fluoride, Fluoride, Stability, Research Article

Abstract

Background Prostate-specific membrane antigen is overexpressed in prostate cancer and it is considered a good target for positron emission tomography/computed tomography imaging of primary cancer and recurrent/metastatic disease, as well as for radioligand therapy. Different PSMA-analogues labeled with [68Ga]gallium have been investigated, showing excellent imaging properties; however, only small amounts can be produced for each radiolabeling. Recently, a [18F]fluoride labeled PSMA-inhibitor, [18F]PSMA-1007, has been introduced, and it has ensured large-scale productions, overcoming this limitation of [68Ga]PSMAs. In this study, PSMA-1007 has been labeled with low (A), medium (B) and high (C) starting activities of [18F]fluoride, in order to verify if radiochemical yield, radiochemical purity and stability of [18F]PSMA-1007 were affected. These parameters have been measured in sixty-five consecutive batches. In addition, the estimation of [18F]PSMA-1007 production costs is provided. Results The radiochemical yield for low and medium activities of [18F]fluoride was 52%, while for the high one it decreased to 40%. The radiochemical purity was 99% for all three activities. [18F]PSMA-1007 did not show radiolysis up to 8 h after the end of synthesis, confirming that the radiopharmaceutical is stable and suitable to perform diagnostic studies in humans for a long period of time after the end of radiolabeling. Furthermore, radiochemical stability was demonstrated in fetal bovine serum at 4 °C and 37 °C for 120′. Conclusions A starting activity of [18F]fluoride of 90 GBq (B) seems to be the best option enabling a final amount of about of 50 GBq of [18F]PSMA-1007, which is promising as it allows to: (a) perform a large number of scans, and/or (b) supply the radiopharmaceutical to any peripheral diagnostic centers in need.

Published

2021

5. Radioimmunotherapy with Tenarad, a 131I-labelled antibody fragment targeting the extra-domain A1 of tenascin-C, in patients with refractory Hodgkin's lymphoma

Author

Michela Aurilio, Francesca Di Gennaro, Corradina Caracò, Secondo Lastoria, Dario Neri, Gaetana Capobianco, Antonio Pinto, Leonardo Giovannoni, Luigi Aloj, Hans D. Menssen, L. D'Ambrosio, Anna Morisco, and Ferdinando Frigeri

Subjects

Adult, Male, medicine.medical_specialty, Immunoproteins, medicine.medical_treatment, Multimodal Imaging, Gastroenterology, Iodine Radioisotopes, Autologous stem-cell transplantation, Internal medicine, Humans, Medicine, Radiology, Nuclear Medicine and imaging, Tomography, Emission-Computed, Single-Photon, Chemotherapy, business.industry, Antibodies, Monoclonal, Cancer, Tenascin, General Medicine, Radioimmunotherapy, medicine.disease, Hodgkin's lymphoma, Hodgkin Disease, Protein Structure, Tertiary, Lymphoma, B symptoms, Positron-Emission Tomography, Radionuclide therapy, Female, Radiopharmaceuticals, medicine.symptom, Tomography, X-Ray Computed, business, Nuclear medicine

Abstract

The extra-domain A1 of tenascin-C (TC-A1) is highly expressed in the extracellular matrix of tumours and on newly formed blood vessels and is thus a valuable target for radionuclide therapy. Tenarad is a fully human miniantibody or small immunoprotein (SIP, molecular weight 80 kDa) labelled with (131)I that is derived from a TC-A1-binding antibody. Previous phase I/II studies with a similar compound ((131)I-L19SIP) used for radioimmunotherapy (RIT) have shown preliminary efficacy in a variety of cancer types. In this ongoing phase I/II trial, Tenarad was administered to patients with recurrent Hodgkin's lymphoma (HL) refractory to conventional treatments.Eight patients (four men, four women; age range 19 - 41) were enrolled between April 2010 and March 2011. All patients had received a median of three previous lines of chemotherapy (range three to six) and seven had also undergone autologous stem cell transplantation (ASCT) or bone marrow transplantation. In addition, seven patients received external beam radiation. All patients had nodal disease, constitutional B symptoms and some showed extranodal disease in skeletal bone (four patients), lung (three), liver (two) and spleen (one). Baseline assessments included whole-body FDG PET with contrast-enhanced CT and diagnostic Tenarad planar and SPECT studies. Patients were considered eligible to receive a therapeutic dose of Tenarad (2.05 GBq/m(2)) if tumour uptake was more than four times higher than that of muscle.All patients were eligible and received the therapeutic dose of Tenarad. Only one patient developed grade 4 thrombocytopenia and leucocytopenia, requiring hospitalization and therapeutic intervention. All other patients had haematological toxicity of grade 3 or lower, which resolved spontaneously. At the first response assessment (4 - 6 weeks after therapy), one patient showed a complete response, one showed a partial response (PR) and five had disease stabilization (SD). Five patients were given up to three repeated Tenarad treatments. One patient showed SD which then improved to a PR, three showed clinical benefit while maintaining SD and one patient showed disease progression.Tenarad RIT is effective in chemorefractory HL and resulted in objective responses or clinical benefit in the majority of patients. Toxicity was acceptable despite the high load of prior treatments, previous ASCT and multiple Tenarad administrations. Further studies are planned to define the most effective schedule for this type of RIT in HL patients.

Published

2014

6. Pre-clinical evaluation of eight DOTA coupled gastrin-releasing peptide receptor (GRP-R) ligands for in vivo targeting of receptor-expressing tumors

Author

Rosalba Mansi, Luigi Del Pozzo, Luigi Aloj, Giancarlo Morelli, Paola Ringhieri, Antonella Accardo, Michela Aurilio, Alberto Signore, Filippo Galli, Anna Morisco, Aloj, Luigi [0000-0002-7452-4961], Apollo - University of Cambridge Repository, Accardo, Antonella, Galli, Filippo, Mansi, Rosalba, Del Pozzo, Luigi, Aurilio, Michela, Morisco, Anna, Ringhieri, Paola, Signore, Alberto, Morelli, Giancarlo, and Aloj, Luigi

Subjects

biodistribution, gastrin-releasing peptide receptor, prostate cancer, radiolabeled peptides, 0301 basic medicine, Biodistribution, Peptide, Bioinformatics, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, In vivo, Gastrin-releasing peptide receptor, Medicine, DOTA, Radiology, Nuclear Medicine and imaging, Radiolabeled peptides, Receptor, Peptide sequence, Radiolabeled peptide, Original Research, chemistry.chemical_classification, Prostate cancer, business.industry, 030104 developmental biology, chemistry, 030220 oncology & carcinogenesis, Radionuclide therapy, Cancer research, business, hormones, hormone substitutes, and hormone antagonists

Abstract

BACKGROUND: Overexpression of the gastrin-releasing peptide receptor (GRP-R) has been documented in several human neoplasms such as breast, prostate, and ovarian cancer. There is growing interest in developing radiolabeled peptide-based ligands toward these receptors for the purpose of in vivo imaging and radionuclide therapy of GRP-R-overexpressing tumors. A number of different peptide sequences, isotopes, and labeling methods have been proposed for this purpose. The aim of this work is to perform a direct side-by-side comparison of different GRP-R binding peptides utilizing a single labeling strategy to identify the most suitable peptide sequence. METHODS: Solid-phase synthesis of eight derivatives (BN1-8) designed based on literature analysis was carried out. Peptides were coupled to the DOTA chelator through a PEG4 spacer at the N-terminus. Derivatives were characterized for serum stability, binding affinity on PC-3 human prostate cancer cells, biodistribution in tumor-bearing mice, and gamma camera imaging at 1, 6, and 24 h after injection. RESULTS: Serum stability was quite variable among the different compounds with half-lives ranging from 16 to 400 min at 37 °C. All compounds tested showed K d values in the nanomolar range with the exception of BN3 that showed no binding. Biodistribution and imaging studies carried out for compounds BN1, BN4, BN7, and BN8 showed targeting of the GRP-R-positive tumors and the pancreas. The BN8 compound (DOTA-PEG-DPhe-Gln-Trp-Ala-Val-NMeGly-His-Sta-Leu-NH2) showed high affinity, the longest serum stability, and the highest target-to-background ratios in biodistribution and imaging experiments among the compounds tested. CONCLUSIONS: Our results indicate that the NMeGly for Gly substitution and the Sta-Leu substitution at the C-terminus confer high serum stability while maintaining high receptor affinity, resulting in biodistribution properties that outperform those of the other peptides.

Published

2016

7. Role of Positron Emission Tomography/Computed Tomography

Author

Corradina Caracò, Secondo Lastoria, Anna Morisco, Raffaele Farese, and Luigi Aloj

Subjects

medicine.medical_specialty, biology, medicine.diagnostic_test, Colorectal cancer, business.industry, Mortality rate, Incidence (epidemiology), Cancer, Colonoscopy, Disease, medicine.disease, digestive system diseases, Carcinoembryonic antigen, medicine, biology.protein, Radiology, Stage (cooking), business

Abstract

Colorectal cancer (CRC) incidence and mortality rates are extremely variable around the world. CRC is the second most commonly diagnosed cancer in both genders [1]. Many patients are cured with initial surgery for primary disease and postoperative chemotherapy. Nevertheless, recurrent locoregional or distant metastases occur in approximately 40% of patients with stage II and stage III CRC [2]. A significant proportion of CRC recurrences occur in a single location, such as pelvis, liver, or lung [3, 4]. Surgery may be curative in some patients with localized recurrent disease and has an impact on 5-year overall survival (OS), which is 27% among patients who undergo surgery vs. 6% in patients who do not [3, 4]. Therefore, accurate and early identification of recurrent and/or metastatic disease is a critical and challenging issue in terms of improving OS of CRC patients. The measurement of circulating carcinoembryonic antigen (CEA) is the most widely accepted test in clinical practice for screening for recurrent CRC. Additionally, periodic colonoscopy, ultrasound (US), and multi-detector computed tomography (MDCT) for localization of recurrent CRC in the early stages are often performed during follow-up. None of these imaging modalities is extremely accurate [5].

Published

2016

8. Peptide-labeled supramolecular aggregates as selective doxorubicin carriers for delivery to tumor cells

Author

Antonella Accardo, Giancarlo Morelli, Rosanna Palumbo, Diego Tesauro, Anna Morisco, Ettore Benedetti, A., Morisco, Accardo, Antonella, Tesauro, Diego, R., Palumbo, E., Benedetti, and Morelli, Giancarlo

Subjects

Cell Survival, Biophysics, Peptide, Pharmacology, Biochemistry, Sincalide, Biomaterials, Heterocyclic Compounds, 1-Ring, chemistry.chemical_compound, Drug Delivery Systems, Cell Line, Tumor, Neoplasms, medicine, supramolecular aggregates, Humans, DOTA, Doxorubicin, Amino Acid Sequence, Cytotoxicity, Cells, Cultured, chemistry.chemical_classification, Drug Carriers, Liposome, Antibiotics, Antineoplastic, Dose-Response Relationship, Drug, CCK8 peptide, Organic Chemistry, General Medicine, Flow Cytometry, chemistry, drug delivery, Liposomes, Drug delivery, cytotoxicity, Receptors, Cholecystokinin, Peptides, Drug carrier, A431 cells, medicine.drug

Abstract

New liposomal aggregates, prepared by combining together, in a 90:10 molar ratio, two amphiphilic monomers, one containing two hydrocarbon chains in the hydrophobic region and the anionic DOTA chelating agent as hydrophilic moiety, and the other containing the same hydrophobic moiety and the CCK8 peptide, are described. The liposomal aggregates because of the presence of the specific moiety, constituted by the CCK8 peptide, which selectively recognizes CCK receptors on tumor cells are used as drug carriers with the aim to deliver into tumor cells the appropriate antitumor drug. The drug loading content and the releasing properties of the liposomal aggregates are studied by the use of the cytotoxic doxorubicin as drug model. The doxorubicin loading content determination reveals that above 95% of the total drug was uptaken with a corresponding drug/lipid w/w ratio of 0.134. The cellular uptake of the targeted liposomal doxorubicin with respect to the self-assembled, nonspecific, liposomal doxorubicin is evaluated using flow cytometry assays. The doxorubicin cell content for two types of cell systems, namely, A431 and HuVEC cells, for peptide derivatized liposomes was 70- and 8-fold higher, respectively, than for nontargeted liposomes, indicating that the bioactive CCK8 peptide is able to enhance the doxorubicin uptake into the carcinoma cells in vitro. The cytotoxicity effect of liposomal doxorubicin on A431 cells has been assessed by MTT assays: in presence of drug amounts ranged between 250 and 1000 ng/ml, incubation with peptide derivatized liposomes showed significantly lower cell survival compared with nontargeted liposomes.

Published

2011

9. Micelles derivatized with octreotide as potential target-selective contrast agents in MRI

Author

Antonella Accardo, Diego Tesauro, Ettore Benedetti, Anna Morisco, Eliana Gianolio, and Giancarlo Morelli

Subjects

Pharmacology, Circular dichroism, Gadolinium, MRI contrast agent, Organic Chemistry, Analytical chemistry, chemistry.chemical_element, General Medicine, Biochemistry, Micelle, eye diseases, Fluorescence spectroscopy, Peptide Conformation, Crystallography, chemistry.chemical_compound, chemistry, Structural Biology, Drug Discovery, Molecular Medicine, DOTA, Chelation, Molecular Biology

Abstract

New amphiphilic monomers (OCA-DTPAGlu and OCA-DOTA) containing, in the same molecule, three different functions: (i) the chelating agent (DTPAGlu or DOTA) able to coordinate gadolinium ion, (ii) the octreotide bioactive peptide able to target somatostatin receptors, and (iii) a hydrophobic moiety with two 18-carbon atoms alkyl chains have been designed and synthesized by solid-phase methods. The novel amphiphilic monomers aggregate, in water solution, giving stable micelles at very low concentration (cmc values of 2.3 x 10(-6) mol kg(-1) and 2.5 x 10(-6) mol kg(-1) for OCA-DTPAGlu and OCA-DOTA, respectively) as confirmed by fluorescence spectroscopy. Fluorescence studies and circular dichroism experiments indicate, for the two compounds as well as for their gadolinium complexes (OCA-DOTA(Gd) and OCA-DTPAGlu(Gd)), the complete exposure of octreotide on the micelle surface, and the predominant presence of an antiparallel beta-sheet peptide conformation characterized by a beta-like turn. The high relaxivity value (r(1p) = 13.9 mM(-1) s(-1) at 20 MHz and 25 degrees C), measured for micelles obtained by the gadolinium complex OCA-DTPAGlu(Gd), indicates these aggregates as promising target-selective magnetic resonance imaging (MRI) contrast agents.

Published

2008

10. Bombesin labelled Liposomes as target selective delivery system for Doxorubicin: in vitro and in vivo studies

Author

MORELLI, GIANCARLO, ACCARDO, ANTONELLA, CICALA, CARLA, TESAURO, DIEGO, Antonio Parisi, Anna, Morisco, Michela Aurilio, Luigi Aloj, Giuseppe De Rosa, Autori Vari, Morelli, Giancarlo, Accardo, Antonella, Cicala, Carla, Antonio, Parisi, Anna, Morisco, Michela, Aurilio, Tesauro, Diego, Luigi, Aloj, and Giuseppe De, Rosa

Subjects

Bombesin analogs conjugate, Liposomes

Published

2012

11. Bombesin peptide antagonist for target-selective delivery of liposomal doxorubicin on cancer cells

Author

Rosalba Mansi, Giuseppina Salzano, Antonella Accardo, Barbara Ziaco, Luigi Aloj, Michela Aurilio, Anna Morisco, Francesco Maione, Diego Tesauro, Carla Cicala, Giuseppe De Rosa, Giancarlo Morelli, Antonio Parisi, Accardo, Antonella, R., Mansi, Salzano, Giuseppina, A., Morisco, M., Aurilio, A., Parisi, Maione, Francesco, Cicala, Carla, B., Ziaco, Tesauro, Diego, L., Aloj, DE ROSA, Giuseppe, and Morelli, Giancarlo

Subjects

chemistry.chemical_classification, Liposome, technology, industry, and agriculture, Antagonist, Pharmaceutical Science, Bombesin, Peptide, Pharmacology, anticancer efficacy, animal studies, chemistry.chemical_compound, doxorubicin delivery, chemistry, In vivo, Liposomes for drug delivery, bombesin peptide, Amphiphile, PEG ratio, Cancer cell

Abstract

Purpose: This study addresses novel peptide modified liposomal doxorubicin to specifically target tissues overexpressing bombesin (BN) receptors. Methods: DOTA-(AEEA)2-peptides containing the [7–14]bombesin and the new BN-AA1 sequence have been synthesized to compare their binding properties and in serum stabilities. The amphiphilic peptide derivative (MonYBN- AA1) containing BN-AA1, a hydrophobic moiety, polyethylenglycole (PEG), and diethylenetriaminepentaacetate (DTPA), has been synthesized. Liposomes have been obtained by mixing of MonY-BN-AA1 with 1,2-distearoylsn-glycero-3-phosphocholine (DSPC). Results: Both 111In labeled peptide derivatives present nanomolar Kd to PC-3 cells. 177Lu labeled peptide DOTA- (AEEA)2-BN-AA1 is very stable (half-life 414.1 h), while DOTA-(AEEA)2-BN, shows a half-life of 15.5 h. In vivo studies on the therapeutic efficacy of DSPC/MonY-BN-AA1/Dox in comparison to DSPC/MonY-BN/Dox, were performed in PC-3 xenograft bearing mice. Both formulations showed similar tumor growth inhibition (TGI) compared to control animals treated with non-targeted DSPC/Dox liposomes or saline solution. For DSPC/MonY-BN-AA1/Dox the maximum effect was observed 19 days after treatment. Conclusions: DSPC/MonY-BN-AA1/Dox nanovectors confirm the ability to selectively target and provide therapeutic efficacy in mice. The lack of receptor activation and possible acute biological side effects provided by using the AA1 antagonist bombesin sequence should provide safe working conditions for further development of this class of drug delivery vehicles.

Published

2012

12. Peptide-modified liposomes for selective targeting of bombesin receptors overexpressed by cancer cells: a potential theranostic agent

Author

Antonella Accardo, Giuseppina Salsano, Carla Cicala, Giancarlo Morelli, Antonio Parisi, Anna Morisco, Francesco Maione, Michela Aurilio, Giuseppe De Rosa, Luigi Aloj, Diego Tesauro, Aloj, Luigi [0000-0002-7452-4961], Apollo - University of Cambridge Repository, Accardo, Antonella, Salsano, G, Morisco, A, Aurilio, M, Parisi, Antonio, Maione, Francesco, Cicala, Carla, Tesauro, Diego, Aloj, L, DE ROSA, Giuseppe, Morelli, Giancarlo, Salsano, Giuseppina, Morisco, Anna, Aurilio, Michela, Aloj, Luigi, and De Rosa, Giuseppe

Subjects

Male, Pharmaceutical Science, Peptide, Pharmacology, Antineoplastic Agent, Surface-Active Agent, chemistry.chemical_compound, Mice, theranostic application, Drug Delivery Systems, Peptide Fragment, International Journal of Nanomedicine, PC-3 cell, Drug Discovery, gastrin-releasing peptide receptors, Receptor, Drug Carrier, Original Research, chemistry.chemical_classification, Liposome, Drug Carriers, Mice, Inbred BALB C, Bombesin, General Medicine, Pentetic Acid, Nanomedicine, bombesin peptide, Drug delivery, Phosphatidylcholines, lipids (amino acids, peptides, and proteins), Female, Drug carrier, medicine.drug, Human, theranostic applications, Biophysics, Mice, Nude, Bioengineering, Antineoplastic Agents, Biology, Biomaterials, Surface-Active Agents, Cell Line, Tumor, medicine, Animals, Humans, Doxorubicin, PC-3 cells, Animal, Organic Chemistry, technology, industry, and agriculture, Prostatic Neoplasms, Gastrin-releasing peptide receptor, Xenograft Model Antitumor Assays, Peptide Fragments, Receptors, Bombesin, Phosphatidylcholine, doxorubicin delivery, chemistry, Cancer cell, Prostatic Neoplasm, Liposomes, Cancer research, Drug Delivery System

Abstract

Antonella Accardo1,2*, Giuseppina Salsano3*, Anna Morisco4, Michela Aurilio4, Antonio Parisi5, Francesco Maione5, Carla Cicala5, Diego Tesauro1,2, Luigi Aloj4, Giuseppe De Rosa3, Giancarlo Morelli1,21CIRPeB, Department of Biological Sciences and IBB CNR, University of Naples “Federico II”, 2Invectors srl, 3Department of Pharmaceutical Chemistry, University of Naples “Federico II”, 4Department of Nuclear Medicine, Istituto Nazionale per lo Studio e la Cura dei Tumori, Fondazione “G. Pascale”, 5Department of Experimental Pharmacology, University of Naples “Federico II”, Napoli, Italy*These authors contributed equally to this workObjectives: Drug delivery systems consisting of liposomes displaying a cell surface receptor-targeting peptide are being developed to specifically deliver chemotherapeutic drugs to tumors overexpressing a target receptor. This study addresses novel liposome composition approaches to specifically target tissues overexpressing bombesin (BN) receptors.Methods: A new amphiphilic peptide derivative (MonY-BN) containing the BN(7–14) peptide, the DTPA (diethylenetriaminepentaacetate) chelating agent, a hydrophobic moiety with two C18 alkyl chains, and polyethylene glycol spacers, has been synthesized by solid-phase methods. Liposomes have been generated by co-aggregation of MonY-BN with 1,2-distearoyl-sn-glycero-3-phosphocholine (DSPC). The structural and biological properties of these new target-selective drug-delivery systems have been characterized.Results: Liposomes with a DSPC/MonY-BN (97/3 molar ratio) composition showed a diameter of 145.5 ± 31.5 nm and a polydispersity index of 0.20 ± 0.05. High doxorubicin (Dox) loading was obtained with the remote pH gradient method using citrate as the inner buffer. Specific binding to PC-3 cells of DSPC/MonY-BN liposomes was obtained (2.7% ± 0.3%, at 37°C), compared with peptide-free DSPC liposomes (1.4% ± 0.2% at 37°C). Incubation of cells with DSPC/MonY-BN/Dox showed significantly lower cell survival compared with DSPC/Dox-treated cells, in the presence of 100 ng/mL and 300 ng/mL drug amounts, in cytotoxicity experiments. Intravenous treatment of PC-3 xenograft-bearing mice with DSPC/MonY-BN/Dox at 10 mg/kg Dox dose produced higher tumour growth inhibition (60%) compared with nonspecific DSPC/Dox liposomes (36%) relative to control animals.Conclusion: The structural and loading properties of DSPC/MonY-BN liposomes along with the observed in-vitro and in-vivo activity are encouraging for further development of this approach for target-specific cancer chemotherapy.Keywords: bombesin peptide, doxorubicin delivery, gastrin-releasing peptide receptors, PC-3 cells, theranostic applications

Published

2012

13. Nanoparticles containing octreotide peptides and gadoliniumcomplexes for MRI applications

Author

Gaetano Mangiapia, Diego Tesauro, Antonella Accardo, Eliana Gianolio, Anna Morisco, Astrid Brandt, Aurel Radulescu, Giancarlo Morelli, Accardo, Antonella, A., Morisco, E., Gianolio, Tesauro, Diego, G., Mangiapia, A., Radulescu, A., Brandte, and Morelli, Giancarlo

Subjects

Stereochemistry, Gadolinium, Contrast Media, chemistry.chemical_element, Peptide, Octreotide, Biochemistry, chemistry.chemical_compound, Pulmonary surfactant, Structural Biology, Drug Discovery, Amphiphile, DOTA, Molecule, MRI contrast agent, Molecular Biology, Pharmacology, chemistry.chemical_classification, Organic Chemistry, Octreotide peptide, food and beverages, General Medicine, equipment and supplies, Magnetic Resonance Imaging, Cyclic peptide, Crystallography, Monomer, chemistry, Supramolecular aggregate, Small-angle neutron scattering, Nanoparticles, Molecular Medicine, lipids (amino acids, peptides, and proteins), Amphiphilic gadolinium complexe

Abstract

New mixed nanoparticles were obtained by self-aggregation of two amphiplic monomers. The first monomer (C18)(2) L5-Oct contains two C18 hydrophobic moieties bound to the N-terminus of the cyclic peptide octreotide, and spaced from the bioactive peptide by five units of dioxoethylene linkers. The second monomer, (C18)(2) DTPAGlu, (C18)(2) DTPA or (C18)(2) DOTA, and the corresponding Gd(III) complexes, contains two C18 hydrophobic moieties bound through a lysine residue to different polyamino-polycarboxy ligands: DTPAGlu, DTPA or DOTA. Mixed aggregates have been obtained and structurally characterized by small angle neutron scattering (SANS) techniques and for their relaxometric behavior. According to a decrease of negative charges in the surfactant head-group, a total or a partial micelle-to-vesicle transition is observed by passing from (C18)(2) DTPAGlu to (C18)(2) DOTA. The thicknesses of the bilayers are substantially constant, around 50 Å, in the analyzed systems. Moreover, the mixed aggregates, in which a small amount of amphiphilic octreotide monomer (C18)(2) L5-Oct (10% mol/mol) was inserted, do not differ significantly from the respective self-assembled systems. Fluorescence emission of tryptophan residue at 340 nm indicates low mobility of water molecules at the peptide surface. The proton relaxivity of mixed aggregates based on (C18)(2) DTPAGlu(Gd), (C18)(2) DTPA(Gd) and (C18)(2) DOTA(Gd) resulted to be 17.6, 15.2 and 10.0 mM(-1) s(-1) (at 20 MHz and 298K), respectively. The decrease in the relaxivity values can be ascribed to the increase in τ(M) (81, 205 and 750 ns). The presence of amphiphilic octreotide monomer exposed on mixed aggregate surface gives the entire nanoparticles a potential binding selectivity toward somatostatin sstr2 receptor subtype, and these systems could act as MRI target-specific contrast agent.

Published

2011

14. Amphiphilic CCK peptides assembled in supramolecular aggregates: structural investigations and in vitro studies

Author

Diego Tesauro, Pasquale Palladino, Rosanna Palumbo, Antonella Accardo, Giancarlo Morelli, Anna Morisco, Accardo, Antonella, A., Morisco, Palladino, Pasquale, R., Palumbo, Tesauro, Diego, and Morelli, Giancarlo

Subjects

Circular dichroism, Stereochemistry, Macromolecular Substances, Surface Properties, Supramolecular chemistry, Peptide, Micelle, Binding uptake, Amphiphile, Tumor Cells, Cultured, Humans, Tissue Distribution, Amino Acid Sequence, Molecular Biology, Peptide sequence, Micelles, chemistry.chemical_classification, Molecular Structure, Chemistry, Circular Dichroism, CCK8 peptide, amphiphilic peptide, Flow Cytometry, Peptide Fragments, Peptide Conformation, Supramolecular aggregate, drug delivery, Biophysics, biological assay, Drug carrier, Cholecystokinin, Biotechnology

Abstract

Supramolecular aggregates obtained by self-aggregation of five new cationic amphiphilic CCK8 peptides have been obtained in water solution and characterized for: (i) aggregate structure and stability; (ii) CCK8 peptide conformation and bioavailability on the external aggregate surface; and (iii) for their cell binding properties. The cationic amphiphilic CCK8 peptides self-aggregate giving a combination of liposomal and micelle structures, with radii ranging between ∼60 nm and ∼90 nm, and between ∼5 and ∼10 nm, respectively. The presence of CCK8 peptide well-exposed on the aggregate surface is demonstrated by fluorescence measurements. Peptide conformation changes in the five supramolecular aggregates: the CCK8 conformational behaviour is probably induced by the presence of three charged lysine residues close to the bioactive peptide sequence. Only aggregates in which the CCK8 peptide presents a structural arrangement similar to that found for the same peptide in DPC micelles give promising binding properties to CCK2-R receptors overexpressed by transfected A431 cells. Chemical modifications on the CCK8 N-terminus seem to play an important role in stabilizing the peptide active conformation, either when the peptide derivative is in monomeric or in aggregate form. For their easy preparation procedures and their binding properties, supramolecular aggregates based on cationic peptide amphiphiles can be considered as promising candidates for target selective drug carriers on cancer cells.

Published

2011

15. Peptide modified nanocarriers for selective targeting of bombesin receptors

Author

Aurel Radulescu, Rosalba Mansi, Luigi Aloj, Diego Tesauro, Luigi Paduano, Claudio Arra, Antonella Accardo, Anna Morisco, Gaetano Mangiapia, Giancarlo Morelli, Michela Aurilio, Accardo, A., Mansi, R., Morisco, A., Mangiapia, G., Paduano, Luigi, Tesauro, D., Radulescu, A., Aurilio, M., Aloj, L., Arra, C., and Morelli, Giancarlo

Subjects

chemistry.chemical_classification, Liposome, Hydrodynamic radius, Molecular Structure, Stereochemistry, Bombesin, Peptide, Models, Theoretical, Receptors, Bombesin, chemistry.chemical_compound, Heterocyclic Compounds, 1-Ring, Monomer, chemistry, Cell Line, Tumor, Amphiphile, Liposomes, Moiety, DOTA, Humans, Peptides, Molecular Biology, Peptide nanocarriers, Bombesin receptors, SANS and DLS techniques, Biotechnology, Chelating Agents

Abstract

The present work describes new supramolecular aggregates obtained by co-assembling two different amphiphilic molecules, one containing the bioactive bombesin peptide (BN), or a scramble sequence, and the other, the DOTA chelating agent, (C18)(2)DOTA, capable of forming stable complexes with the radioactive (111)In(III) isotope. The peptide in the amphiphilic monomer is spaced by the lipophilic moiety through ethoxylic spacers of different length: a shorter spacer with five units of dioxoethylene moieties in (C18)(2)L5-peptide, or a longer spacer consisting of a Peg3000 residue in (C18)(2)Peg3000-peptide. Structural characterization by SANS and DLS techniques indicates that, independently from the presence of the peptide containing monomer in the final composition, the predominant aggregates are liposomes of similar shape and size with a hydrodynamic radius R(h) around 200 nm and bilayer thickness, d, of 4 nm. In vitro data show specific binding of the (111)In-(C18)(2)DOTA/(C18)(2)L5-[7-14]BN 90:10 liposomes in receptor expressing cells. However, the presence of the Peg3000 unit on the external liposomal surface, could hide the peptide and prevent the receptor binding. In vivo experiments using (111)In-(C18)(2)DOTA/(C18)(2)L5-[7-14]BN show the expected biological behavior of aggregates of such size and molecular composition, moreover there is an increase in concentration of the GRPR targeting aggregate in the tumors compared to control at the 48 h time point evaluated (2.4% ID/g versus 1.6% ID/g).

Published

2010

16. Micelles Obtained by Aggregation of Gemini Surfactants Containing the CCK8 Peptide and a Gadolinium Complex

Author

Diego Tesauro, Gaetano Mangiapia, Eliana Gianolio, Richard K. Heenan, Anna Morisco, Giancarlo Morelli, Antonella Accardo, Mauro Vaccaro, Luigi Paduano, Accardo, A., Tesauro, D., Morisco, A., Mangiapia, G., Vaccaro, M., Gianolio, E., Heenan, R. K., Paduano, Luigi, and Morelli, Giancarlo

Subjects

Circular dichroism, Molecular Structure, Chemistry, Protein Conformation, Gadolinium, Supramolecular chemistry, Analytical chemistry, chemistry.chemical_element, Biochemistry, Micelle, Fluorescence spectroscopy, Peptide Fragments, Inorganic Chemistry, Crystallography, Surface-Active Agents, Peptide gemini surfactant Amphiphilic gadolinium complexes CCK8 peptide Micelles Small-angle neutron scattering (SANS), Critical micelle concentration, Amphiphile, Microemulsion, Cholecystokinin, Nuclear Magnetic Resonance, Biomolecular, Micelles

Abstract

Two gemini surfactants, [C18CysL5CCK8](2) and [C18CysDTPAGlu](2), containing, respectively, the CCK8 peptide and the DTPAGlu chelating agent or its gadolinium complex have been prepared by linking lipophilic chains through a disulfide bond between two cysteine residues. The two surfactants aggregate in water solution forming pure or mixed micelles, with a critical micellar concentration in the 5 x 10(-6)-5 x 10(-5) mol kg(-1) range, as measured by fluorescence spectroscopy. As indicated by small-angle neutron scattering, the shape and size of the micelles are influenced by the temperature: increasing temperature leads to progressive reduction of the size of the supramolecular aggregates. Cylindrical structures found at lower temperatures (10-40 degrees C) evolve into ellipsoidal micelles at 50-80 degrees C. Furthermore, the surface-exposed CCK8 peptide changes its conformation above a transition temperature of approximately 45 degrees C, going from a beta-sheet to a random-coil structure, as indicated by circular dichroism measurements. The mixed aggregate obtained by coaggregation of the two gemini-based amphiphilic compounds, [C18CysDTPAGlu(Gd)](2) and [C18CysL5CCK8](2) in 70:30 molar ratio, represents the first example of a peptide-containing gemini surfactant as a potential target-selective contrast agent in MRI. In fact, it presents a high relaxivity value of the gadolinium complex, 21.5 mM(-1) s(-1), and the CCK8 bioactive peptide exposed on the external surface is therefore capable of selective targeting of the cholecystokinin receptors.

Published

2009