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1. Targeting Intracranial Tumours with a Combination of RNA and Chemotherapy

Author

Abdulhamid S. Fatani, Andreas G. Schätzlein, and Ijeoma F. Uchegbu

Subjects
siRNA anti-ITCH, 6-O-glycolchitosan, brain, intracranial tumours, intranasal, brain delivery, Pharmacy and materia medica, RS1-441
Abstract

Glioblastoma multiforme (GBM) is a fast-growing and aggressive brain tumour, which remains largely resistant to treatment; the prognosis for patients is poor, with a median survival time of about 12–18 months, post diagnosis. In an effort to bring more efficacious treatments to patients, we targeted the down regulation of ITCH, an E3 ligase that is overexpressed in a variety of cancers, and which inhibits P73, a tumour suppressor gene. 6-O-glycolchitosan (GC) was used to deliver siRNA ITCH (GC60-siRNA-ITCH) and gemcitabine via the nose to brain route in CD-1 nude mice which had previously been implanted intracranially with U87-MG-luc2 cells. Prior to this in vivo study, an in vitro study established the synergistic effect of siRNA-ITCH in combination with a chemotherapy drug—gemcitabine. A downregulation of ITCH, an upregulation of p73 and enhanced apoptosis were observed in vitro in U87-MG cells, using qPCR, Western blot analysis, confocal laser scanning microscopy, flow cytometry and cytotoxicity assays. When GC60-siRNA-ITCH was combined with gemcitabine, there was a resultant decrease in cell proliferation in vitro. In CD1 mice, the administration of siRNA-ITCH (7 doses of 0.081 mg/kg) alone did not significantly affect animal survival (increasing mean survival from 29 to 33 days when compared to untreated animals), whereas intranasal gemcitabine had a significant effect on survival (increasing survival from 29 to 45 days when compared to untreated animals, p < 0.01). The most significant effect was seen with combination therapy (GC60-siRNA-ITCH plus gemcitabine), where survival increased by 89%, increasing from 29 to 54 days (p < 0.01). Our data demonstrate that siRNA chemosensitises brain tumours to gemcitabine and that the nose-to-brain delivery route may be a viable route for the treatment of intracranial tumours.

Published
2024
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2. SARS-CoV-2 inhibition using a mucoadhesive, amphiphilic chitosan that may serve as an anti-viral nasal spray

Author

Krzysztof Pyrć, Aleksandra Milewska, Emilia Barreto Duran, Paweł Botwina, Agnieszka Dabrowska, Malwina Jedrysik, Malgorzata Benedyk, Rui Lopes, Alejandro Arenas-Pinto, Moutaz Badr, Ryan Mellor, Tammy L. Kalber, Delmiro Fernandez-Reyes, Andreas G. Schätzlein, and Ijeoma F. Uchegbu

Subjects
Medicine, Science
Abstract

Abstract There are currently no cures for coronavirus infections, making the prevention of infections the only course open at the present time. The COVID-19 pandemic has been difficult to prevent, as the infection is spread by respiratory droplets and thus effective, scalable and safe preventive interventions are urgently needed. We hypothesise that preventing viral entry into mammalian nasal epithelial cells may be one way to limit the spread of COVID-19. Here we show that N-palmitoyl-N-monomethyl-N,N-dimethyl-N,N,N-trimethyl-6-O-glycolchitosan (GCPQ), a positively charged polymer that has been through an extensive Good Laboratory Practice toxicology screen, is able to reduce the infectivity of SARS-COV-2 in A549ACE2+ and Vero E6 cells with a log removal value of − 3 to − 4 at a concentration of 10–100 μg/ mL (p

Published
2021
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3. Quaternary Ammonium Palmitoyl Glycol Chitosan (GCPQ) Loaded with Platinum-Based Anticancer Agents—A Novel Polymer Formulation for Anticancer Therapy

Author

Yvonne Lerchbammer-Kreith, Michaela Hejl, Nadine S. Sommerfeld, Xian Weng-Jiang, Uchechukwu Odunze, Ryan D. Mellor, David G. Workman, Michael A. Jakupec, Andreas G. Schätzlein, Ijeoma F. Uchegbu, Mathea S. Galanski, and Bernhard K. Keppler

Subjects
platinum(IV) complexes, quaternary ammonium glycol chitosan (GCPQ), anticancer, drug delivery, Medicine, Pharmacy and materia medica, RS1-441
Abstract

Quaternary ammonium palmitoyl glycol chitosan (GCPQ) has already shown beneficial drug delivery properties and has been studied as a carrier for anticancer agents. Consequently, we synthesised cytotoxic platinum(IV) conjugates of cisplatin, carboplatin and oxaliplatin by coupling via amide bonds to five GCPQ polymers differing in their degree of palmitoylation and quaternisation. The conjugates were characterised by 1H and 195Pt NMR spectroscopy as well as inductively coupled plasma mass spectrometry (ICP-MS), the latter to determine the amount of platinum(IV) units per GCPQ polymer. Cytotoxicity was evaluated by the MTT assay in three human cancer cell lines (A549, non-small-cell lung carcinoma; CH1/PA-1, ovarian teratocarcinoma; SW480, colon adenocarcinoma). All conjugates displayed a high increase in their cytotoxic activity by factors of up to 286 times compared to their corresponding platinum(IV) complexes and mostly outperformed the respective platinum(II) counterparts by factors of up to 20 times, also taking into account the respective loading of platinum(IV) units per GCPQ polymer. Finally, a biodistribution experiment was performed with an oxaliplatin-based GCPQ conjugate in non-tumour-bearing BALB/c mice revealing an increased accumulation in lung tissue. These findings open promising opportunities for further tumouricidal activity studies especially focusing on lung tissue.

Published
2023
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4. Platinum(IV)-Loaded Degraded Glycol Chitosan as Efficient Platinum(IV) Drug Delivery Platform

Author

Yvonne Lerchbammer-Kreith, Nadine S. Sommerfeld, Klaudia Cseh, Xian Weng-Jiang, Uchechukwu Odunze, Andreas G. Schätzlein, Ijeoma F. Uchegbu, Mathea S. Galanski, Michael A. Jakupec, and Bernhard K. Keppler

Subjects
platinum(IV) complexes, glycol chitosan, anticancer, drug delivery, Pharmacy and materia medica, RS1-441
Abstract

A new class of anticancer prodrugs was designed by combining the cytotoxicity of platinum(IV) complexes and the drug carrier properties of glycol chitosan polymers: Unsymmetrically carboxylated platinum(IV) analogues of cisplatin, carboplatin and oxaliplatin, namely (OC-6-44)-acetatodiammine(3-carboxypropanoato)dichloridoplatinum(IV), (OC-6-44)-acetaodiammine(3-carboxypropanoato)(cyclobutane-1,1-dicarboxylato)platinum(IV) and (OC-6-44)-acetato(3-carboxypropanoato)(1R,2R-cyclohexane-1,2-diamine)oxalatoplatinum(IV) were synthesised and conjugated via amide bonding to degraded glycol chitosan (dGC) polymers with different chain lengths (5, 10, 18 kDa). The 15 conjugates were investigated with 1H and 195Pt NMR spectroscopy, and average amounts of platinum(IV) units per dGC polymer molecule with ICP-MS, revealing a range of 1.3–22.8 platinum(IV) units per dGC molecule. Cytotoxicity was tested with MTT assays in the cancer cell lines A549, CH1/PA-1, SW480 (human) and 4T1 (murine). IC50 values in the low micromolar to nanomolar range were obtained, and higher antiproliferative activity (up to 72 times) was detected with dGC-platinum(IV) conjugates in comparison to platinum(IV) counterparts. The highest cytotoxicity (IC50 of 0.036 ± 0.005 µM) was determined in CH1/PA-1 ovarian teratocarcinoma cells with a cisplatin(IV)–dGC conjugate, which is hence 33 times more potent than the corresponding platinum(IV) complex and twice more potent than cisplatin. Biodistribution studies of an oxaliplatin(IV)–dGC conjugate in non-tumour-bearing Balb/C mice showed an increased accumulation in the lung compared to the unloaded oxaliplatin(IV) analogue, arguing for further activity studies.

Published
2023
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5. Brain Gene Silencing with Cationic Amino-Capped Poly(ethylene glycol) Polyplexes

Author

Abdullah A. Alamoudi, Paula A. Méndez, David Workman, Andreas G. Schätzlein, and Ijeoma F. Uchegbu

Subjects
siRNA delivery, brain, gene silencing, polyethylene glycol (PEG), nanoparticles, intranasal, Biology (General), QH301-705.5
Abstract

Therapeutic gene silencing in the brain is usually achieved using highly invasive intracranial administration methods and/or comparatively toxic vectors. In this work, we use a relatively biocompatible vector: poly(ethylene glycol) star-shaped polymer capped with amine groups (4APPA) via the nose to brain route. 4APPA complexes anti- itchy E3 ubiquitin protein ligase (anti-ITCH) siRNA to form positively charged (zeta potential +15 ± 5 mV) 150 nm nanoparticles. The siRNA-4APPA polyplexes demonstrated low cellular toxicity (IC50 = 13.92 ± 6 mg mL−1) in the A431 cell line and were three orders of magnitude less toxic than Lipofectamine 2000 (IC50 = 0.033 ± 0.04 mg mL−1) in this cell line. Cell association and uptake of fluorescently labelled siRNA bound to siRNA-4APPA nanoparticles was demonstrated using fluorescent activated cell sorting (FACS) and confocal laser scanning microscopy (CLSM), respectively. Gene silencing of the ITCH gene was observed in vitro in the A431 cell line (65% down regulation when compared to the use of anti-ITCH siRNA alone). On intranasal dosing with fluorescently labelled siRNA-4APPA polyplexes, fluorescence was seen in the cells of the olfactory bulb, cerebral cortex and mid-brain regions. Finally, down regulation of ITCH was seen in the brain cells (54 ± 13% ITCH remaining compared to untreated controls) in a healthy rat model, following intranasal dosing of siRNA-4APPA nanoparticles (0.15 mg kg−1 siRNA twice daily for 3 days). Gene silencing in the brain may be achieved by intranasal administration of siRNA- poly(ethylene glycol) based polyplexes.

Published
2022
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6. Gene Targeting to the Cerebral Cortex Following Intranasal Administration of Polyplexes

Author

Asya I. Petkova, Ilona Kubajewska, Alexandra Vaideanu, Andreas G. Schätzlein, and Ijeoma F. Uchegbu

Subjects
nose to brain delivery, gene therapy, polyplexes, hyaluronidase, glycol chitosan, Pharmacy and materia medica, RS1-441
Abstract

Gene delivery to the cerebral cortex is challenging due to the blood brain barrier and the labile and macromolecular nature of DNA. Here we report gene delivery to the cortex using a glycol chitosan—DNA polyplex (GCP). In vitro, GCPs carrying a reporter plasmid DNA showed approximately 60% of the transfection efficiency shown by Lipofectamine lipoplexes (LX) in the U87 glioma cell line. Aiming to maximise penetration through the brain extracellular space, GCPs were coated with hyaluronidase (HYD) to form hyaluronidase-coated polyplexes (GCPH). The GCPH formulation retained approximately 50% of the in vitro hyaluronic acid (HA) digestion potential but lost its transfection potential in two-dimensional U87 cell lines. However, intranasally administered GCPH (0.067 mg kg−1 DNA) showed high levels of gene expression (IVIS imaging of protein expression) in the brain regions. In a separate experiment, involving GCP, LX and naked DNA, the intranasal administration of the GCP formulation (0.2 mg kg−1 DNA) resulted in protein expression predominantly in the cerebral cortex, while a similar dose of intranasal naked DNA led to protein expression in the cerebellum. Intranasal LX formulations did not show any evidence of protein expression. GCPs may provide a means to target protein expression to the cerebral cortex via the intranasal route.

Published
2022
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7. Development of Bio-Functionalized, Raman Responsive, and Potentially Excretable Gold Nanoclusters

Author

Ryan D. Mellor, Andreas G. Schätzlein, and Ijeoma F. Uchegbu

Subjects
ultrasmall-in-nano, excretable, gold, Raman, theranostic, Chemistry, QD1-999
Abstract

Gold nanoparticles (AuNPs) are used experimentally for non-invasive in vivo Raman monitoring because they show a strong absorbance in the phototherapeutic window (650–850 nm), a feature that is accompanied by a particle size in excess of 100 nm. However, these AuNPs cannot be used clinically because they are likely to persist in mammalian systems and resist excretion. In this work, clustered ultrasmall (sub-5 nm) AuNP constructs for in vivo Raman diagnostic monitoring, which are also suitable for mammalian excretion, were synthesized and characterized. Sub-5 nm octadecyl amine (ODA)-coated AuNPs were clustered using a labile dithiol linker: ethylene glycol bis-mercaptoacetate (EGBMA). Upon clustering via a controlled reaction and finally coating with a polymeric amphiphile, a strong absorbance in the phototherapeutic window was demonstrated, thus showing the potential suitability of the construct for non-invasive in vivo detection and monitoring. The clusters, when labelled with a biphenyl-4-thiol (BPT) Raman tag, were shown to elicit a specific Raman response in plasma and to disaggregate back to sub-5 nm particles under physiological conditions (37 °C, 0.8 mM glutathione, pH 7.4). These data demonstrate the potential of these new AuNP clusters (Raman NanoTheranostics—RaNT) for in vivo applications while being in the excretable size window.

Published
2021
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8. Polymeric Micelles for the Enhanced Deposition of Hydrophobic Drugs into Ocular Tissues, without Plasma Exposure

Author

Ijeoma F. Uchegbu, Jan Breznikar, Alessandra Zaffalon, Uche Odunze, and Andreas G. Schätzlein

Subjects
cyclosporine A, Molecular Envelope Technology (MET), N-palmitoyl-N-monomethyl-N,N-dimethyl-N,N,N-trimethyl-6-O-glycolchitosan (GCPQ), eye, penetration enhancer, Pharmacy and materia medica, RS1-441
Abstract

Commercial topical ocular formulations for hydrophobic actives rely on the use of suspensions or oil in water emulsions and neither of these formulation modalities adequately promote drug penetration into ocular tissues. Using the ocular relevant hydrophobic drug, cyclosporine A (CsA), a non-irritant ocular penetration enhancer is showcased, which may be used for the formulation of hydrophobic actives. The activity of this penetration enhancer is demonstrated in a healthy rabbit model. The Molecular Envelope Technology (MET) polymer (N-palmitoyl-N-monomethyl-N,N-dimethyl-N,N,N-trimethyl-6-O-glycolchitosan), a self-assembling, micelle-forming polymer, was used to formulate CsA into sterile filtered nanoparticulate eye drop formulations and the stability of the formulation tested. Healthy rabbits were dosed with a single dose of a MET–CsA (NM133) 0.05% formulation and ocular tissues analyzed. Optically clear NM133 formulations were prepared containing between 0.01–0.1% w/v CsA and 0.375–0.75% w/v MET polymer. NM133 0.01%, NM133 0.02% and NM133 0.05% were stable for 28 days when stored at refrigeration temperature (5–6 °C) and room temperature (16–23 °C), but there was evidence of evaporation of the formulation at 40 °C. There was no change in drug content when NM133 0.05% was stored for 387 days at 4 °C. On topical dosing to rabbits, corneal, conjunctival and scleral AUC0–24 levels were 25,780 ng.h g−1, 12,046 ng.h g−1 and 5879 ng.h g−1, respectively, with NM133 0.05%. Meanwhile, a similar dose of Restasis 0.05% yielded lower values of 4726 ng.h/g, 4813 ng.h/g and 1729 ng.h/g for the drug corneal, conjunctival and scleral levels, respectively. NM133 thus delivered up to five times more CsA to the ocular surface tissues when compared to Restasis. The MET polymer was non-irritant up to a concentration of 4% w/v. The MET polymer is a non-irritant ocular penetration enhancer that may be used to deliver hydrophobic drugs in optically clear topical ocular formulations.

Published
2021
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9. Increased Efficacy of Oral Fixed-Dose Combination of Amphotericin B and AHCC® Natural Adjuvant against Aspergillosis

Author

Alba Pérez-Cantero, Dolores R. Serrano, Patricia Navarro-Rodríguez, Andreas G. Schätzlein, Ijeoma F. Uchegbu, Juan J. Torrado, and Javier Capilla

Subjects
aspergillosis, amphotericin B, oral delivery, chitosan, shiitake, Lentinula edodes, AHCC®, Molecular Envelope Technology, Pharmacy and materia medica, RS1-441
Abstract

Invasive pulmonary aspergillosis represents one of the most serious fungal infections among immunocompromised patients. In this study, we aimed to analyze the in vivo efficacy of prophylactic oral amphotericin B (AMB) encapsulated in modified chitosan-nanoparticles (Nanomerics’ Molecular Envelope Technology (MET)) supplemented with a standardized extract of cultured Lentinula edodes mycelia (AHCC®) in a murine model of pulmonary aspergillosis. We determined fungal burden and survival of mice and additionally, we carried out a cytokine analysis in an attempt to understand the immunomodulation of the extract. Our results evidenced equivalent efficacy between orally administered AMB-MET and the intravenous liposomal AMB marketed formulation. Addition of the AHCC® supplement significantly improved efficacy in terms of burden reduction and survival increase of both oral and intravenous AMB therapies compared to the untreated control group. Moreover, a protective effect of the extract was observed in terms of weight loss. Regarding the cytokine profiles, the Th1 immune response was stimulated in treated animals when compared to the control group. This response was marked by an enhancement in the MCP-1, GM-CSF, VEGF, RANTES and IL-17 levels and a decrease in the IL-6, a biomarker related to the severity of the infection.

Published
2019
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11. Achieving highly efficient gene transfer to the bladder by increasing the molecular weight of polymer-based nanoparticles

Author

Gang Li, Shanshan He, Darryl T. Martin, Robert M. Weiss, Ijeoma F. Uchegbu, and Andreas G. Schätzlein

Subjects
Polymers, Genetic enhancement, Urinary Bladder, Pharmaceutical Science, 02 engineering and technology, Mice, 03 medical and health sciences, medicine, Animals, Luciferase, Urothelium, Gene, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, Lamina propria, Chemistry, Polymer, Penetration (firestop), 021001 nanoscience & nanotechnology, Molecular Weight, Administration, Intravesical, medicine.anatomical_structure, Permeability (electromagnetism), Biophysics, Nanoparticles, 0210 nano-technology
Abstract

Short dwell-time and poor penetration of the bladder permeability barrier (BPB) are the main obstacles to intravesical treatments for bladder diseases, and is evidenced by the lack of such therapeutic options on the market. Herein, we demonstrate that by finely tuning the molecular weight of our cationic polymer mucoadhesive nanoparticles, we enhanced our gene transfer, leading to improved adherence and penetrance through the BPB in a safe and efficient manner. Specifically, increasing the polymer molecular weight from 45 kDa to 83 kDa enhanced luciferase plasmid transfer to the healthy murine bladder, leading to 1.35 ng/g luciferase protein expression in the urothelium and lamina propria regions. The relatively higher molecular weight polymer (83 kDa) did not induce morphologic changes or inflammatory responses in the bladder. This approach of altering polymer molecular weight for prolonging gene transfer residence time and deeper penetration through the BPB could be the basis for the design of future gene therapies for bladder diseases.

Published
2021

13. Particulate levodopa nose-to-brain delivery targets dopamine to the brain with no plasma exposure

Author

Savvas Dimiou, Rui M. Lopes, Ilona Kubajewska, Ryan D. Mellor, Corinna S. Schlosser, Manjunath S. Shet, Hugh Huang, Ozgur Akcan, Garth T. Whiteside, Andreas G. Schätzlein, and Ijeoma F. Uchegbu

Subjects
Levodopa, Dopamine, Pharmaceutical Science, Animals, Biological Availability, Brain, Parkinson Disease, Rats
Abstract

Levodopa (L-DOPA) is an oral Parkinson's Disease drug that generates the active metabolite - dopamine (DA) in vivo. However, oral L-DOPA exhibits low oral bioavailability, limited brain uptake, peripheral DA-mediated side effects and its poor brain bioavailability can lead to long-term complications. Here we show that L-DOPA forms stable (for at least 5 months) 300 nm nanoparticles when encapsulated within N-palmitoyl-N-monomethyl-N,N-dimethyl-N,N,N-trimethyl-6-O-glycolchitosan (GCPQ). A nano-in-microparticle GCPQ-L-DOPA formulation (D

Published
2021

14. Development of Bio-Functionalized, Raman Responsive, and Potentially Excretable Gold Nanoclusters

Author

Andreas G. Schätzlein, Ijeoma F. Uchegbu, and Ryan Mellor

Subjects
General Chemical Engineering, theranostic, Dithiol, gold, Photochemistry, Article, Nanoclusters, Absorbance, symbols.namesake, chemistry.chemical_compound, Chemistry, chemistry, In vivo, Colloidal gold, Amphiphile, symbols, General Materials Science, excretable, Raman spectroscopy, ultrasmall-in-nano, Ethylene glycol, QD1-999, Raman
Abstract

Gold nanoparticles (AuNPs) are used experimentally for non-invasive in vivo Raman monitoring because they show a strong absorbance in the phototherapeutic window (650–850 nm), a feature that is accompanied by a particle size in excess of 100 nm. However, these AuNPs cannot be used clinically because they are likely to persist in mammalian systems and resist excretion. In this work, clustered ultrasmall (sub-5 nm) AuNP constructs for in vivo Raman diagnostic monitoring, which are also suitable for mammalian excretion, were synthesized and characterized. Sub-5 nm octadecyl amine (ODA)-coated AuNPs were clustered using a labile dithiol linker: ethylene glycol bis-mercaptoacetate (EGBMA). Upon clustering via a controlled reaction and finally coating with a polymeric amphiphile, a strong absorbance in the phototherapeutic window was demonstrated, thus showing the potential suitability of the construct for non-invasive in vivo detection and monitoring. The clusters, when labelled with a biphenyl-4-thiol (BPT) Raman tag, were shown to elicit a specific Raman response in plasma and to disaggregate back to sub-5 nm particles under physiological conditions (37 °C, 0.8 mM glutathione, pH 7.4). These data demonstrate the potential of these new AuNP clusters (Raman NanoTheranostics—RaNT) for in vivo applications while being in the excretable size window.

Published
2021

15. Facile aqueous, room temperature preparation of high transverse relaxivity clustered iron oxide nanoparticles

Author

Nguyen T. K. Thanh, Nicholas J Hobson, Andreas G. Schätzlein, Marianne Ashford, Ijeoma F. Uchegbu, and Xian Weng

Subjects
Relaxometry, Materials science, Aqueous solution, Sonication, Iron oxide, 02 engineering and technology, 010402 general chemistry, 021001 nanoscience & nanotechnology, 01 natural sciences, 0104 chemical sciences, chemistry.chemical_compound, Colloid and Surface Chemistry, chemistry, Chemical engineering, Zeta potential, Particle size, 0210 nano-technology, Iron oxide nanoparticles, Superparamagnetism
Abstract

Clustering superparamagnetic iron oxide nanoparticles (SPIONs) is one method of providing the biomedical benefits of larger SPIONs [e.g. superior T2 weighted magnetic resonance imaging (MRI) contrast] without increasing particle size. The work presented herein, describes the facile synthesis of clustered SPIONs that are suitable for MRI applications, by using a chitosan based polymer: N-palmitoyl-N-monomethyl-N-N-dimethyl-N-N-N-trimethyl-6-O-glycolchitosan (GCPQ) and aqueous nanoprecipitation followed by probe sonication, in the absence of organic solvents or elevated temperatures. The resulting clustered SPIONs consist of individual 8 nm iron oxide nanoparticles clustered into a 150 nm particle with a positive zeta potential (+23 mV) at neutral pH. X-ray diffraction confirms the presence of crystalline magnetic iron oxide, while magnetometer experiments show the clustered SPIONs are superparamagnetic giving an overall Ms of 63.5 ± 1.3 emu g−1. Relaxometry analyses revealed that the clustered SPIONs (inclusive of coatings) had a high r2 value of 294.8 mM−1 s−1 and an r2/r1 of 21.1 making the clustered SPIONs suitable for T2 weighted (negative) MRI contrast imaging applications. The resulting clustered SPIONs demonstrate that highly sensitive T2 contrast agents may be produced in mild room temperature conditions, without the need for organic solvents or low molecular weight surfactants.

Published
2019

16. Unusual Enthalpy Driven Self Assembly at Room Temperature with Chitosan Amphiphiles

Author

Lisa Godfrey, Andreas G. Schätzlein, Uchechukwu Odunze, Fionn O'Brien, and Ijeoma F. Uchegbu

Subjects
endothermic, polymer, Enthalpy, Biomedical Engineering, exothermic, Pharmaceutical Science, 02 engineering and technology, 010402 general chemistry, 01 natural sciences, Micelle, Article, Chitosan, thermodynamics, chemistry.chemical_compound, Colloid, enthalpy, GCPQ, micelle, Amphiphile, Colloids, Micelles, chemistry.chemical_classification, Temperature, critical micelle concentration (CMC), Hydrogen Bonding, Isothermal titration calorimetry, Polymer, 021001 nanoscience & nanotechnology, nanomedicine, 0104 chemical sciences, Molecular Weight, chemistry, Chemical engineering, Nanoparticles, Self-assembly, entropy, 0210 nano-technology, Dimerization, Hydrophobic and Hydrophilic Interactions
Abstract

Background: GCPQ (N-palmitoyl-N-monomethyl-N,N-dimethyl-N,N,N-trimethyl- 6-O-glycolchitosan) is a self-assembling polymer being investigated as a pharmaceutical nano-carrier. GCPQ nanoparticles shuttle drugs across biological barriers, improving drug performance. The exact chemistry of GCPQ is varied by the relative proportion of hydrophobic (N-palmitoyl) and hydrophilic (quaternary ammonium) groups and molecular weight. Objective: We hypothesised that the thermodynamics of self-assembly is controlled by the polymer molecular weight and hydrophobicity. Method: The thermodynamics of self-assembly was investigated using isothermal calorimetry. Results: GCPQs (Mw = 8-15 kDa) formed micellar aggregates at critical micellar concentrations of 1-2.4 µM at 25°C and micellisation was unusually enthalpy driven. There was a positive correlation between ΔHmic and mole% quaternary groups (Q): ΔHmic = 3.8 Q- 159 (r2 = 0.93) and a negative correlation between ΔHmic and molecular weight (Mw): ΔHmic = -13.5 Mw-26.3 (r2 = 0.99). Conclusion: These findings provide insights into the positive drivers of stable selfassemblies, namely hydrophobicity and molecular weight, as both hydrophobicity and molecular weight are associated with an increased enthalpy contribution to micellisation.

Published
2019

17. The topical ocular delivery of rapamycin to posterior eye tissues and the suppression of retinal inflammatory disease

Author

Moutaz Y. Badr, Abdulrahman A. Halwani, Uchechukwu Odunze, Malihe Eskandarpour, Virginia L. Calder, Andreas G. Schätzlein, and Ijeoma F. Uchegbu

Subjects
Sirolimus, Uveitis, Mice, Animals, Pharmaceutical Science, Posterior Eye Segment, Rabbits, Ophthalmic Solutions, Retina
Abstract

Treatment of posterior eye diseases with intravitreal injections of drugs, while effective, is invasive and associated with side effects such as retinal detachment and endophthalmitis. In this work, we have formulated a model compound, rapamycin (RAP), in nanoparticle-based eye drops and evaluated the delivery of RAP to the posterior eye tissues in a healthy rabbit. We have also studied the formulation in experimental autoimmune uveitis (EAU) mouse model with retinal inflammation. Aqueous RAP eye drops were prepared using N-palmitoyl-N-monomethyl-N,N-dimethyl-N,N,N-trimethyl-6-O-glycolchitosan (Molecular Envelope Technology - MET) containing 0.23 ± 0.001% w/v RAP with viscosity, osmolarity, and pH within the ocular comfort range, and the formulation (MET-RAP) was stable in terms of drug content at both refrigeration and room temperature for one month. The MET-RAP eye drops delivered RAP to the choroid-retina with a Cmax of 145 ± 49 ng/g (tmax = 1 h). The topical application of the MET-RAP eye drops to the EAU mouse model resulted in significant disease suppression compared to controls, with activity similar to dexamethasone eye drops. The MET-RAP eye drops also resulted in a reduction of RORγt and an increase in both Foxp3 expression and IL-10 secretion, indicating a mechanism involving the inhibition of Th17 cells and the up-regulation of T-reg cells. The MET-RAP formulation delivers RAP to the posterior eye segments, and the formulation is active in EAU.

Published
2022

18. Tissue-Engineering the Fibrous Pancreatic Tumour Stroma Capsule in 3D Tumouroids to Demonstrate Paclitaxel Response

Author

Mark Emberton, Umber Cheema, Katerina Stamati, Marilena Loizidou, Rawiya Al Hosni, Judith Pape, Andreas G. Schätzlein, and Ijeoma F. Uchegbu

Subjects
Stromal cell, Paclitaxel, endocrine system diseases, QH301-705.5, pancreatic cancer, Fluorescent Antibody Technique, Catalysis, Article, Inorganic Chemistry, chemistry.chemical_compound, Tissue engineering, Stroma, Cell Line, Tumor, Spheroids, Cellular, Pancreatic cancer, Hyaluronic acid, hyaluronic acid, Tumor Cells, Cultured, Tumor Microenvironment, medicine, Humans, Physical and Theoretical Chemistry, Biology (General), Molecular Biology, QD1-999, Spectroscopy, Cell Proliferation, Dose-Response Relationship, Drug, Tissue Engineering, Chemistry, desmoplasia, Organic Chemistry, Cancer, chemoresistance, General Medicine, 3D tumour models, medicine.disease, Immunohistochemistry, Computer Science Applications, Desmoplasia, Pancreatic Neoplasms, Drug Resistance, Neoplasm, Cancer research, Stromal Cells, medicine.symptom
Abstract

Pancreatic cancer is a unique cancer in that up to 90% of its tumour mass is composed of a hypovascular and fibrotic stroma. This makes it extremely difficult for chemotherapies to be delivered into the core of the cancer mass. We tissue-engineered a biomimetic 3D pancreatic cancer (“tumouroid”) model comprised of a central artificial cancer mass (ACM), containing MIA Paca-2 cells, surrounded by a fibrotic stromal compartment. This stromal compartment had a higher concentration of collagen type I, fibronectin, laminin, and hyaluronic acid (HA) than the ACM. The incorporation of HA was validated with alcian blue staining. Response to paclitaxel was determined in 2D MIA Paca-2 cell cultures, the ACMs alone, and in simple and complex tumouroids, in order to demonstrate drug sensitivity within pancreatic tumouroids of increasing complexity. The results showed that MIA Paca-2 cells grew into the complex stroma and invaded as cell clusters with a maximum distance of 363.7 µm by day 21. In terms of drug response, the IC50 for paclitaxel for MIA Paca-2 cells increased from 0.819 nM in 2D to 3.02 nM in ACMs and to 5.87 nM and 3.803 nM in simple and complex tumouroids respectively, indicating that drug penetration may be significantly reduced in the latter. The results demonstrate the need for biomimetic models during initial drug testing and evaluation.

Published
2021

19. Fundamentals of Pharmaceutical Nanoscience

Author

Ijeoma F. Uchegbu, Andreas G. Schätzlein, Aikaterini Lalatsa, Dolores Remedios Serrano Lopez, Ijeoma F. Uchegbu, Andreas G. Schätzlein, Aikaterini Lalatsa, and Dolores Remedios Serrano Lopez

Subjects
Pharmacology, Pharmacy, Nanotechnology, Physical chemistry, Polymers, Biotechnology
Abstract

Nanoscience or the science of the very small offers the pharmaceutical scientist a wealth of opportunities. By fabricating at the nanoscale, it is possible to exert unprecedented control on drug activity. This textbook will showcase a variety of nanosystems working from their design and construction to their application in the field of drug delivery. The book is intended for graduate students in drug delivery, physical and polymer chemistry, and applied pharmaceutical sciences courses that involve fundamental nanoscience. The purpose of the text is to present physicochemical and biomedical properties of synthetic polymers with an emphasis on their application in polymer therapeutics i.e., pharmaceutical nanosystems, drug delivery and biological performance. There are two main objectives of this text. The first is to provide advanced graduate students with knowledge of the principles of nanosystems and polymer science including synthesis, structure, and characterization of solution and solid state properties. The second is to describe the fundamentals of therapeutic applications of polymers in drug delivery, targeting, response modifiers as well as regulatory issues. The courses, often listed as Advanced Drug Delivery and Applied Pharmaceutics; Polymer Therapeutics; or Nanomedicine, are designed as an overview of the field specifically for graduate students in the Department of Pharmaceutical Sciences Graduate Programs. However, the course content may also be of interest for graduate students in related biomedical research programs. These courses generally include a discussion of the major principles of polymer science and fundamental concepts of application of polymers as modern therapeutics. All courses are moving away from the above mentioned course names and going by ‘pharmaceutical nanoscience or nanosystems'. This area of research and technology development has attracted tremendous attention during the last twodecades and it is expected that it will continue to grow in importance. However, the area is just emerging and courses are limited but they are offered.

Published
2024

20. SARS-CoV-2 inhibition using a mucoadhesive, amphiphilic chitosan that may serve as an anti-viral nasal spray

Author

Malwina Jedrysik, Andreas G. Schätzlein, Rui Lopes, Pawel Botwina, Moutaz Badr, Krzysztof Pyrc, Malgorzata Benedyk, Agnieszka Dabrowska, Alejandro Arenas-Pinto, Ijeoma F. Uchegbu, Delmiro Fernandez-Reyes, Emilia Barreto Duran, Aleksandra Milewska, Ryan Mellor, and Tammy L. Kalber

Subjects
Male, medicine.medical_treatment, Science, Mice, Transgenic, Pharmacology, Antiviral Agents, Methylation, Article, Surface-Active Agents, Viral entry, In vivo, Chlorocebus aethiops, medicine, Animals, Humans, Respiratory system, Vero Cells, Infectivity, Mice, Inbred BALB C, Multidisciplinary, business.industry, SARS-CoV-2, Nasal Sprays, Viral Load, COVID-19 Drug Treatment, medicine.anatomical_structure, Nasal spray, A549 Cells, Viral infection, Vero cell, Medicine, business, Viral load, Biomedical materials, Respiratory tract
Abstract

There are currently no cures for coronavirus infections, making the prevention of infections the only course open at the present time. The COVID-19 pandemic has been difficult to prevent, as the infection is spread by respiratory droplets and thus effective, scalable and safe preventive interventions are urgently needed. We hypothesise that preventing viral entry into mammalian nasal epithelial cells may be one way to limit the spread of COVID-19. Here we show that N-palmitoyl-N-monomethyl-N,N-dimethyl-N,N,N-trimethyl-6-O-glycolchitosan (GCPQ), a positively charged polymer that has been through an extensive Good Laboratory Practice toxicology screen, is able to reduce the infectivity of SARS-COV-2 in A549ACE2+ and Vero E6 cells with a log removal value of − 3 to − 4 at a concentration of 10–100 μg/ mL (p p 50/mL) showed a trend for nasal GCPQ (20 mg/kg) to inhibit viral load in the respiratory tract and brain, although the study was not powered to detect statistical significance. GCPQ’s electrostatic binding to the virus, preventing viral entry into the host cells, is the most likely mechanism of viral inhibition. Radiolabelled GCPQ studies in mice show that at a dose of 10 mg/kg, GCPQ has a long residence time in mouse nares, with 13.1% of the injected dose identified from SPECT/CT in the nares, 24 h after nasal dosing. With a no observed adverse effect level of 18 mg/kg in rats, following a 28-day repeat dose study, clinical testing of this polymer, as a COVID-19 prophylactic is warranted.

Published
2020

21. SARS-CoV-2 inhibition in human airway epithelial cells using a mucoadhesive, amphiphilic chitosan that may serve as an anti-viral nasal spray

Author

Krzysztof Pyrć, Aleksandra Milewska, Emilia Barreto Duran, Paweł Botwina, Rui Lopes, Alejandro Arenas-Pinto, Moutaz Badr, Ryan Mellor, Tammy L. Kalber, Delmiro Fernandes-Reyes, Andreas G. Schätzlein, and Ijeoma F. Uchegbu

Abstract

There are currently no cures for coronavirus infections, making the prevention of infections the only course open at the present time. The COVID-19 pandemic has been difficult to prevent, as the infection is spread by respiratory droplets and thus effective, scalable and safe preventive interventions are urgently needed. We hypothesise that preventing viral entry into mammalian nasal epithelial cells may be one way to limit the spread of COVID-19. Here we show that N-palmitoyl-N-monomethyl-N,N-dimethyl-N,N,N-trimethyl-6-O-glycolchitosan (GCPQ), a positively charged polymer that has been through an extensive Good Laboratory Practice toxicology screen, is able to reduce the infectivity of SARS-COV-2 in A549ACE2+ and Vero E6 cells with a log removal value of −3 to −4 at a concentration of 10 – 100 μg/ mL (p < 0.05 compared to untreated controls) and to limit infectivity in human airway epithelial cells at a concentration of 500 μg/ mL (p < 0.05 compared to untreated controls). GCPQ is currently being developed as a pharmaceutical excipient in nasal and ocular formulations. GCPQ’s electrostatic binding to the virus, preventing viral entry into the host cells, is the most likely mechanism of viral inhibition. Radiolabelled GCPQ studies in mice show that at a dose of 10 mg/ kg, GCPQ has a long residence time in mouse nares, with 13.1% of the injected dose identified from SPECT/CT in the nares, 24 hours after nasal dosing. With a no observed adverse effect level of 18 mg/ kg in rats, following a 28-day repeat dose study, clinical testing of this polymer, as a COVID-19 prophylactic is warranted.

Published
2020

22. Down-regulation of GP130 signaling sensitizes bladder cancer to cisplatin by impairing Ku70 DNA repair signaling and promoting apoptosis

Author

Ijeoma F. Uchegbu, Andreas G. Schätzlein, Darryl T. Martin, Peter A. Humphrey, Gang Li, Shanshan He, and Robert M. Weiss

Subjects
0301 basic medicine, Male, DNA Repair, DNA repair, Down-Regulation, Apoptosis, 03 medical and health sciences, 0302 clinical medicine, medicine, Cytokine Receptor gp130, Humans, Viability assay, Ku Autoantigen, Cisplatin, Ku70, Bladder cancer, Chemistry, digestive, oral, and skin physiology, Cancer, Cell Biology, medicine.disease, Neoplasm Proteins, Gene Expression Regulation, Neoplastic, 030104 developmental biology, HEK293 Cells, Urinary Bladder Neoplasms, Lipofectamine, 030220 oncology & carcinogenesis, Cancer research, MCF-7 Cells, Female, medicine.drug, Signal Transduction
Abstract

Chemoresistance is one of the barriers for the development of bladder cancer treatments. Previously, we showed that glycoprotein-130 (GP130) is overexpressed in chemoresistant bladder cancer cells and that knocking down GP130 expression reduced cell viability. In our current work, we showed that down-regulation of GP130 sensitized bladder cancer cells to cisplatin-based chemotherapy by activating DNA repair signaling. We performed immunohistochemistry and demonstrated a positive correlation between the levels of Ku70, an initiator of canonical non-homologous end joining repair (c-NHEJ) and suppressor of apoptosis, and GP130 in human bladder cancer specimens. GP130 knockdown by SC144, a small molecule inhibitor, in combination with cisplatin, increased the number of DNA lesions, specifically DNA double-stranded breaks, with a subsequent increase in apoptosis and reduced cell viability. Furthermore, GP130 inhibition attenuated Ku70 expression in bladder and breast cancer cells as well as in transformed kidney cells. In addition, we fabricated a novel polymer-lipid hybrid delivery system to facilitate GP130 siRNA delivery that had a similar efficiency when compared with Lipofectamine, but induced less toxicity.

Published
2020

23. Hyaluronidase Coated Molecular Envelope Technology Nanoparticles Enhance Drug Absorption via the Subcutaneous Route

Author

Asya Petkova, George Wang, Ijeoma F. Uchegbu, Andreas G. Schätzlein, and Ramesh Soundararajan

Subjects
Polymers, Pharmaceutical Science, Nanoparticle, Hyaluronoglucosaminidase, Mice, Nude, Antineoplastic Agents, 02 engineering and technology, Pharmacology, Hydroxamic Acids, 030226 pharmacology & pharmacy, Histone Deacetylases, Histones, 03 medical and health sciences, Mice, 0302 clinical medicine, Drug Delivery Systems, Microscopy, Electron, Transmission, Hyaluronidase, Cell Line, Tumor, Drug Discovery, medicine, Animals, Particle Size, Envelope (waves), Chitosan, Drug Carriers, Polymeric micelles, Chemistry, 021001 nanoscience & nanotechnology, Patient preference, Xenograft Model Antitumor Assays, Subcutaneous route, Rats, Histone Deacetylase Inhibitors, Solubility, Carcinoma, Squamous Cell, Quinazolines, Molecular Medicine, Nanoparticles, Female, 0210 nano-technology, Hydrophobic and Hydrophilic Interactions, medicine.drug
Abstract

Parenteral chemotherapy is usually administered intravenously, although patient preference and health economics suggest the subcutaneous (sc) route could be an attractive alternative. However, due to the low aqueous solubility of hydrophobic drugs and injection volume limitations, the total amount of drug that can be administered in a single sc injection is frequently insufficient. We have developed hyaluronidase coated nanoparticles (NPs) that efficiently encapsulate such drugs, thus addressing both issues and allowing sufficient amounts of hydrophobic drug to be administered and absorbed effectively. CUDC-101, a poorly water-soluble multitargeted anticancer drug that simultaneously inhibits the receptor tyrosine kinases (RTKs) EGFR and HER2, as well as histone deacetylase (HDAC), was encapsulated in polymeric Molecular Envelope Technology (MET) NPs. The role of polymer chemistry, formulation parameters, and coating with hyaluronidase (HYD) on MET-CUDC-101 NP formulations was examined and optimized to yield high drug loading and colloidal stability, and, after freeze-drying, stable storage at room temperature for up to 90 days. The pharmacokinetic studies in healthy rats showed that plasma AUC

Published
2020

24. Nanomedicines in the treatment of brain tumors

Author

Andreas G. Schätzlein, Funmilola A. Fisusi, and Ijeoma F. Uchegbu

Subjects
0301 basic medicine, Paclitaxel, Biomedical Engineering, Brain tumor, Medicine (miscellaneous), Bioengineering, Development, Theranostic Nanomedicine, 03 medical and health sciences, chemistry.chemical_compound, Drug Delivery Systems, 0302 clinical medicine, medicine, Humans, General Materials Science, Doxorubicin, Brain Neoplasms, business.industry, medicine.disease, Nanomedicine, 030104 developmental biology, chemistry, 030220 oncology & carcinogenesis, Cancer research, Nanoparticles, Glioblastoma, business, medicine.drug
Published
2018

25. Limiting the level of tertiary amines on polyamines leads to biocompatible nucleic acid vectors

Author

Qi Zhang, Kai Zheng, Margarida Isabel Simão Carlos, David G. Workman, Natalie L. Garrett, Julian Moger, Andreas G. Schätzlein, Abdulrahman A. Halwani, Ilona Kubajewska, Natrah Arifin, and Ijeoma F. Uchegbu

Subjects
0301 basic medicine, Tertiary amine, Biocompatibility, Cell Survival, Genetic Vectors, Pharmaceutical Science, Biocompatible Materials, 02 engineering and technology, Transfection, Cell Line, Rats, Sprague-Dawley, 03 medical and health sciences, chemistry.chemical_compound, Nucleic Acids, Polyamines, Animals, Humans, RNA, Messenger, RNA, Small Interfering, Nuclease, biology, DNA, 021001 nanoscience & nanotechnology, Lipids, 030104 developmental biology, chemistry, Biochemistry, Cell culture, Lipofectamine, Nucleic acid, biology.protein, 0210 nano-technology
Abstract

We have designed an efficient, synthetic nucleic acid vector, which is relatively non-toxic. [N-(2-ethylamino)-6-O-glycolchitosan – EAGC] polymers were 10–50 fold less toxic than Lipofectamine 2000, able to complex DNA, mRNA and siRNA into positively charged (zeta potential = + 40 − 50 mV), 50–450 nm nanoparticles. The level of tertiary amine N-2-ethylamino substitution (DStert) was inversely proportional to the IC50 of the EAGC polymers in the A431 cell line: IC50 = 6.18 DStert−0.9, r2 = 0.9991. EAGC polyplexes were stable against a heparin challenge, able to protect the nucleic acids from nuclease degradation and achieve levels of transfection comparable to Lipofectamine 2000 formulations. The relative biocompatibility of the vector allowed 10 fold higher doses of DNA (1 μg compared to 0.1 μg per well with Lipofectamine 2000) and siRNA (10.7 μg per well vs 1.3 μg with Lipofectamine 2000) to be applied to cells, when compared to Lipofectamine 2000. Finally intranasal application of EAGC – siRNA complexes resulted in siRNA transfer to the neurons of the olfactory bulb.

Published
2017

26. A Self-Assembling Lipidic Peptide and Selective Partial V2 Receptor Agonist Inhibits Urine Production

Author

Sahar Awwad, Andreas G. Schätzlein, Sunish Patel, Boqian Liu, Antonella Bavuso Volpe, Ijeoma F. Uchegbu, and Shozeb Haider

Subjects
0301 basic medicine, Agonist, Male, Vasopressin, Receptors, Vasopressin, Cell biology, medicine.drug_class, lcsh:Medicine, Peptide, 02 engineering and technology, Pharmacology, Urine, Article, Madin Darby Canine Kidney Cells, Rats, Sprague-Dawley, 03 medical and health sciences, Lipopeptides, Dogs, In vivo, Arginine vasopressin receptor 2, medicine, Animals, Rats, Wistar, Receptor, lcsh:Science, chemistry.chemical_classification, Multidisciplinary, Drug discovery, lcsh:R, Antidiuretic Agents, Prodrug, 021001 nanoscience & nanotechnology, Receptor antagonist, Rats, Arginine Vasopressin, 030104 developmental biology, chemistry, Drug delivery, lcsh:Q, Female, 0210 nano-technology
Abstract

Lipidised analgesic peptide prodrugs self-assemble into peptide nanofibers; with the nanofiber morphology protecting the peptide from plasma degradation and improving therapeutic efficacy. Extending this learning, we hypothesised that a self-assembling lipidized peptide arginine vasopressin (AVP) receptor agonist, that had not been designed as a prodrug, could prove pharmacologically active and control urine production. The only approved AVP receptor agonist, desmopressin is indicated for the treatment of central diabetes insipidus (DI), bedwetting, haemophilia A and von Willebrand disease. Desmopressin is well tolerated by most patients, however adverse effects, such as hyponatraemia and water intoxication necessitate a strict fluid intake, thus motivating the search for alternative DI treatments. Selective V2 receptor agonism is required for anti-DI activity and we hypothesised that our new lipidized peptide (METx) would lead to selective AVP receptor agonism. METx was synthesised and characterised and then tested for activity against the V2, V1a and OT uterine receptors and not tested against the V1b receptor as METx was not expected to cross the blood brain barrier. METx was also tested in vivo in a healthy rat model. METx forms nanofibers and is a partial V2 receptor agonist (determined by measuring MDCK cell line cAMP accumulation), producing 57% of AVP’s maximal activity (EC50 = 2.7 nM) and is not a V1a agonist up to a concentration of 1 μM (determined by measuring A7r5 cell line D-myo-inositol-1-phosphate accumulation). METx is a weak OT receptor antagonist, reducing the frequency of OT induced contractions (EC50 = 350 nM) and increasing the OT EC50 from 0.081 nM to 21 nM at a concentration of 600 nM. METx (41 nM) had no effect on spontaneous uterine contractions and METx (100 nM) had no effect on OT induced uterine contractions. Simulated binding studies show that binding avidity to the receptors follows the trend: V2 > OT > V1a. On intravenous injection, a nanoparticle formulation of METx reduced urine production in a healthy rat model in a dose responsive manner, with 40 mg kg−1 METx resulting in no urine production over 4 hours. The lipidized self-assembling peptide – METx - is a selective competitive V2 receptor agonist and an anti-diuretic.

Published
2019

27. Increased Efficacy of Oral Fixed-Dose Combination of Amphotericin B and AHCC® Natural Adjuvant against Aspergillosis

Author

Juan J. Torrado, Ijeoma F. Uchegbu, Patricia Navarro-Rodríguez, Alba Pérez-Cantero, Dolores R. Serrano, Andreas G. Schätzlein, and Javier Capilla

Subjects
Lentinula edodes, medicine.medical_treatment, Fixed-dose combination, lcsh:RS1-441, Pharmaceutical Science, Pharmacology, Aspergillosis, shiitake, lcsh:Pharmacy and materia medica, 03 medical and health sciences, Tecnología farmaceútica, In vivo, Weight loss, Amphotericin B, medicine, aspergillosis, 030304 developmental biology, Molecular Envelope Technology, 0303 health sciences, 030306 microbiology, business.industry, technology, industry, and agriculture, medicine.disease, oral delivery, amphotericin B, Cytokine, AHCC®, Biomarker (medicine), medicine.symptom, chitosan, business, Adjuvant, medicine.drug
Abstract

Invasive pulmonary aspergillosis represents one of the most serious fungal infections among immunocompromised patients. In this study, we aimed to analyze the in vivo efficacy of prophylactic oral amphotericin B (AMB) encapsulated in modified chitosan-nanoparticles (Nanomerics&rsquo, Molecular Envelope Technology (MET)) supplemented with a standardized extract of cultured Lentinula edodes mycelia (AHCC&reg, ) in a murine model of pulmonary aspergillosis. We determined fungal burden and survival of mice and additionally, we carried out a cytokine analysis in an attempt to understand the immunomodulation of the extract. Our results evidenced equivalent efficacy between orally administered AMB-MET and the intravenous liposomal AMB marketed formulation. Addition of the AHCC&reg, supplement significantly improved efficacy in terms of burden reduction and survival increase of both oral and intravenous AMB therapies compared to the untreated control group. Moreover, a protective effect of the extract was observed in terms of weight loss. Regarding the cytokine profiles, the Th1 immune response was stimulated in treated animals when compared to the control group. This response was marked by an enhancement in the MCP-1, GM-CSF, VEGF, RANTES and IL-17 levels and a decrease in the IL-6, a biomarker related to the severity of the infection.

Published
2019
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29. Nose-to-Brain Delivery

Author

Guojun Xiong, Ijeoma F. Uchegbu, Wai Chun Tsang, Andreas G. Schätzlein, and Zian Wang

Subjects
0301 basic medicine, Nasal cavity, Drug, media_common.quotation_subject, Nose, Blood–brain barrier, 03 medical and health sciences, 0302 clinical medicine, Drug Delivery Systems, medicine, Animals, Humans, Respiratory system, Olfactory Region, Administration, Intranasal, media_common, Pharmacology, business.industry, Neurodegeneration, Brain, medicine.disease, Nasal Mucosa, 030104 developmental biology, medicine.anatomical_structure, Molecular Medicine, Nasal Cavity, business, Neuroscience, 030217 neurology & neurosurgery, Astrocyte
Abstract

The global prevalence of neurologic disorders is rising, and yet we are still unable to deliver most drug molecules, in therapeutic quantities, to the brain. The blood brain barrier consists of a tight layer of endothelial cells surrounded by astrocyte foot processes, and these anatomic features constitute a significant barrier to drug transport from the blood to the brain. One way to bypass the blood brain barrier and thus treat diseases of the brain is to use the nasal route of administration and deposit drugs at the olfactory region of the nares, from where they travel to the brain via mechanisms that are still not clearly understood, with travel across nerve fibers and travel via a perivascular pathway both being hypothesized. The nose-to-brain route has been demonstrated repeatedly in preclinical models, with both solution and particulate formulations. The nose-to-brain route has also been demonstrated in human studies with solution and particle formulations. The entry of device manufacturers into the arena will enable the benefits of this delivery route to become translated into approved products. The key factors that determine the efficacy of delivery via this route include the following: delivery to the olfactory area of the nares as opposed to the respiratory region, a longer retention time at the nasal mucosal surface, penetration enhancement of the active through the nasal epithelia, and a reduction in drug metabolism in the nasal cavity. Indications where nose-to-brain products are likely to emerge first include the following: neurodegeneration, post-traumatic stress disorder, pain, and glioblastoma.

Published
2019

30. A polymeric aqueous tacrolimus formulation for topical ocular delivery

Author

Nurul S. Abdulrahman, Moutaz Y. Badr, Ijeoma F. Uchegbu, and Andreas G. Schätzlein

Subjects
medicine.medical_specialty, Biodistribution, Conjunctiva, genetic structures, Administration, Topical, medicine.medical_treatment, Pharmaceutical Science, 02 engineering and technology, 030226 pharmacology & pharmacy, Tacrolimus, Chitosan, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Tandem Mass Spectrometry, Ophthalmology, Cornea, medicine, Animals, Distribution (pharmacology), Tissue Distribution, Whole blood, Eye drop, 021001 nanoscience & nanotechnology, medicine.disease, eye diseases, medicine.anatomical_structure, chemistry, Rabbits, sense organs, Ophthalmic Solutions, 0210 nano-technology, Vernal keratoconjunctivitis, Chromatography, Liquid
Abstract

Tacrolimus (TAC) suspension is used to treat moderate to severe atopic keratoconjunctivitis (AKC) and vernal keratoconjunctivitis (VKC). The objectives of this study were to formulate the hydrophobic compound TAC (TAC) in an aqueous eye drop formulation and study its ocular biodistribution on topical ocular application to a healthy rabbit model, with the overall aim of using the formulation to treat AKC and VKC. A thin-film hydration method was used to encapsulate TAC within the chitosan-based amphiphile: N-palmitoyl-N-monomethyl-N,N-dimethyl-N,N,N-trimethyl-6-O-glycolchitosan (Molecular Envelope Technology – MET) in an aqueous formulation. The formulation was characterized, and its stability studied under three storage conditions for one month. The ocular distribution of the formulation was studied in healthy rabbits and the ocular tissues and the whole blood analyzed by LC-MS/MS. A 200 nm nanoparticle formulation (MET-TAC) containing 0.1 ± 0.002% w/v TAC was produced with viscosity, osmolarity and pH within the ocular comfort range, and the formulation was stable on refrigeration for one month. On topical application, the TAC concentrations in rabbit cornea and conjunctiva one hour after dosing were 4452 ± 2289 and 516 ± 180 ng/g of tissue, respectively. A topical ocular aqueous TAC eye drop formulation has been prepared with the ability to deliver sufficient drug to the relevant ocular surface tissues.

Published
2021

31. Direct in vivo evidence on the mechanism by which nanoparticles facilitate the absorption of a water insoluble, P-gp substrate

Author

Kenji Sasaki, Andreas G. Schätzlein, Lisa Godfrey, Uchechukwu Odunze, Ramesh Soundararajan, Nancy Fereira, and Ijeoma F. Uchegbu

Subjects
Male, Paclitaxel, Administration, Oral, Pharmaceutical Science, 02 engineering and technology, Absorption (skin), Pharmacology, 030226 pharmacology & pharmacy, Intestinal absorption, Tight Junctions, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Ileum, In vivo, Cell Line, Tumor, Animals, Humans, Dissolution testing, ATP Binding Cassette Transporter, Subfamily B, Member 1, Rats, Wistar, Chitosan, Drug Carriers, Tight junction, Water, Biological Transport, Epithelial Cells, 021001 nanoscience & nanotechnology, Rats, Intestinal Absorption, Solubility, Verapamil, chemistry, Caco-2, Biophysics, Nanoparticles, Caco-2 Cells, 0210 nano-technology, Drug carrier
Abstract

Here we examine the mechanisms by which nanoparticles enable the oral absorption of water-insoluble, P-glycoprotein efflux pump (P-gp) substrates, without recourse to P-gp inhibitors. Both 200nm paclitaxel N-(2-phenoxyacetyl)-6-O-glycolchitosan (GCPh) nanoparticles (GCPh-PTX) and a simulated Taxol formulation, facilitate drug dissolution in biorelevant media, unlike paclitaxel nanocrystals. Verapamil (40mgkg-1) increased the oral absorption from low dose Taxol (6 or 10mgkg-1) by 100%, whereas the oral absorption from high dose Taxol (20mgkg-1) or low dose GCPh-PTX (6 or 10mgkg-1) was largely unchanged by verapamil. There was virtually no absorption from control paclitaxel nanocrystals (20mgkg-1). Imaging of ex-vivo rat ileum samples showed that fluorescently labelled GCPh nanoparticles are mucoadhesive and are taken up by ileum epithelial cells. GCPh nanoparticles were also found to open Caco-2 cell tight junctions. In conclusion, mucoadhesive, drug solubilising GCPh nanoparticles enable the oral absorption of paclitaxel via the saturation of the P-gp pump (by high local drug concentrations) and by particle uptake and tight junction opening mechanisms.

Published
2016

32. Nanoparticulate peptide delivery exclusively to the brain produces tolerance free analgesia

Author

Lisa, Godfrey, Antonio, Iannitelli, Natalie L, Garrett, Julian, Moger, Ian, Imbert, Tamara, King, Frank, Porreca, Ramesh, Soundararajan, Aikaterini, Lalatsa, Andreas G, Schätzlein, and Ijeoma F, Uchegbu

Subjects
Male, Rats, Sprague-Dawley, Analgesics, Morphine, Hyperalgesia, Conditioning, Psychological, Animals, Brain, Nanoparticles, Pain, Drug Tolerance, Analgesia, Enkephalin, Leucine
Abstract

The delivery of peptide drugs to the brain is challenging, principally due to the blood brain barrier and the low metabolic stability of peptides. Exclusive delivery to the brain with no peripheral exposure has hitherto not been demonstrated with brain quantification data. Here we show that polymer nanoparticles encapsulating leucine

Published
2017

33. The Oral and Intranasal Delivery of Propofol Using Chitosan Amphiphile Nanoparticles

Author

Andreas G. Schätzlein, Ijeoma F. Uchegbu, Per Holm, Marie-Christine Jones, Davide Laghezza, Lisa Godfrey, Federica Corrente, and Maria Carafa

Subjects
Drug, medicine.drug_class, media_common.quotation_subject, medicine.medical_treatment, Biomedical Engineering, Pharmaceutical Science, N-palmitoylation-N-monomethyl-N, Pharmacology, Animal data, Ntrimethyl- 6-O-glycolchitosan, Anaesthetic, GCPQ, medicine, Saline, media_common, propofol, business.industry, GABAA receptor, nasal delivery, oral propofol, N-dumethyl-N, Sedative, Pharmacodynamics, Anesthesia, nanoparticles, Nasal administration, Propofol, business, N, medicine.drug
Abstract

The intravenous anaesthetic propofol acts on gamma amino butyric acid A (GABAA) receptors in the brain. Propofol is often used as a procedural sedative and is also effective (at sub-anaesthetic doses) against intractable migraine and non-migraine headaches. However intravenous propofol is associated with pain on injection and with peripherally mediated hypotension. Here we introduce N-palmitoyl-N-monomethyl-N,N-dimethyl-N,N,N-trimethyl-6-O-glycolchitosan (GCPQ) - propofol nanoparticles and demonstrate, for the first time, that propofol nanoparticles are centrally active via the oral and the intranasal routes. Utilising these routes would abolish the pain on injection and, with respect to the nasal route, reduce peripheral exposure. The nanoparticles are 40-500 nm in size and stable for 21 days at room temperature. Brain drug exposure with orally administered GCPQ-propofol nanoparticles (350 mg kg-1 propofol) was not significantly different from a comparable oral dose of Diprivan. However there was less inter-individual variability with the GCPQ formulation (brain concentration coefficient of variation at the 5 minute peak time point = 1.24 and 0.72 for the Diprivan and GCPQ nanoparticle formulations respectively). Furthermore there was increased inter-individual variability in the pharmacodynamic response to oral Diprivan when compared to oral GCPQ-propofol, as measured by the loss of righting reflex (LORR) time. The LORR time after oral doses of 250 mg kg-1 and 350 mg kg-1 propofol as Diprivan was 15.7±24.6 minutes and 47.2±35.70 minutes respectively while the LORR time after oral 250 mg kg-1 and 350 mg kg-1 GCPQpropofol was 0 minutes and 52.7±22.9 minutes respectively. These data have implications for the safety of oral Diprivan. Via the intranasal route, the LORR time with Diprivan (4mg kg-1 propofol) was not significantly different from that of intranasal saline, while the intranasal administration of GCPQ-propofol formulations (4 mg kg-1 and 8 mg kg-1 propofol) produced significantly higher LORR times than when saline was administered. In summary, these animal data demonstrate that GCPQ-propofol nanoparticles may provide an effective method of administering non-parenteral propofol for potential use in non-anaesthetic settings.

Published
2014

34. Physical Characterisation and Long-Term Stability Studies on Quaternary Ammonium Palmitoyl Glycol Chitosan (GCPQ)—A New Drug Delivery Polymer

Author

Andreas G. Schätzlein, Ramesh Soundararajan, Kar Wai Chooi, Ijeoma F. Uchegbu, Simon Gaisford, Margarida Isabel Simão Carlos, and Natrah Arifin

Subjects
chemistry.chemical_classification, Chitosan, Drug Carriers, Aqueous solution, Chromatography, Polymers, Viscosity, Pharmaceutical Science, Polymer, Dynamic mechanical analysis, Micelle, Palmitic acid, chemistry.chemical_compound, Drug Delivery Systems, Monomer, chemistry, Ammonium Compounds, Rheology, Weak base, Micelles, Methyl iodide
Abstract

N-palmitoyl-N-monomethyl-N,N-dimethyl-N,N,N-trimethyl-6-O-glycolchitosan (GCPQ) is a self-assembling polymer, which enables the oral bioavailability of peptide and hydrophobic drugs. In preparation for clinical testing, here we examine GCPQ's synthesis reproducibility, pKa, thermal, and rheological properties. GCPQ was synthesised by acid degradation of glycol chitosan (GC), reaction with palmitic acid N-hydroxysuccinimide (PNS) and methylation. A GC monomer, PNS molar feed ratio of 0.92 together with a gravimetric feed ratio for N-palmitoyl-6-O-glycolchitosan, methyl iodide of 3.3, reproducibly produces GCPQ48 (Mw = 19.9 ± 9.9 kDa, Mn = 13.1 ± 2.4 kDa, mol % palmitoylation = 23 ± 2.7, mol % quaternisation = 10 ± 0.23, n = 56). GCPQ48 decomposes at 218 ± 4.3°C, is glassy at room temperature (Tg = 164.4 ± 8.5°C), is a weak base (pKa = 5.99 ± 0.15), and produces micellar dispersions at neutral pH. Below a concentration of 0.07 g mL−1, GCPQ48 dispersions showed Newtonian rheological behaviour but at higher concentrations, the polymer undergoes shear thinning because of the chain disentanglement at high shear rates. GCPQ48 forms a network of micelles and concentrated (0.09 g mL−1) dispersions are viscoelastic, with the storage modulus exceeding the loss modulus at high frequencies. Solid GCPQ48 was stable when stored at room temperature for 18 months. © 2014 Wiley Periodicals, Inc. and the American Pharmacists Association J Pharm Sci 103:2296–2306, 2014

Published
2014

35. Strategies To Deliver Peptide Drugs to the Brain

Author

Andreas G. Schätzlein, Aikaterini Lalatsa, and Ijeoma F. Uchegbu

Subjects
Molecular Sequence Data, Pharmaceutical Science, Peptide, Transferrin receptor, Pharmacy, Pharmacology, Blood–brain barrier, Gastrointestinal epithelium, RS, Drug Delivery Systems, Drug Discovery, medicine, Animals, Humans, Amino Acid Sequence, Opioid peptide, Peptide sequence, chemistry.chemical_classification, business.industry, Brain, medicine.anatomical_structure, chemistry, Blood-Brain Barrier, Nanoparticles for drug delivery to the brain, Nanoparticles, Molecular Medicine, Nasal administration, Peptides, business
Abstract

Neurological diseases such as neurodegeneration, pain, psychiatric disorders, stroke, and brain cancers would greatly benefit from the use of highly potent and specific peptide pharmaceuticals. Peptides are especially desirable because of their low inherent toxicity. The presence of the blood brain barrier (BBB), their short duration of action, and their need for parenteral administration limits their clinical use. However, over the past decade there have been significant advances in delivering peptides to the central nervous system. Angiopep peptides developed by Angiochem (Montreal, Canada), transferrin antibodies developed by ArmaGen (Santa Monica, USA), and cell penetrating peptides have all shown promise in delivering therapeutic peptides across the BBB after intravenous administration. Noninvasive methods of delivering peptides to the brain include the use of chitosan amphiphile nanoparticles for oral delivery and nose to brain strategies. The uptake of the chitosan amphiphile nanoparticles by the gastrointestinal epithelium is important for oral peptide delivery. Finally protecting peptides from plasma degradation is integral to the success of most of these peptide delivery strategies.

Published
2014

36. Amphotericin B Formulations – The Possibility of Generic Competition

Author

Juan J. Torrado, Maria Paloma Ballesteros, Ijeoma F. Uchegbu, Dolores R. Serrano, and Andreas G. Schätzlein

Subjects
Drug, Antifungal, Second line treatment, business.industry, medicine.drug_class, media_common.quotation_subject, Biomedical Engineering, Pharmaceutical Science, Pharmacology, Bioequivalence, Clinical trial, Innovator, Amphotericin B, Medicine, business, medicine.drug, media_common
Abstract

From the 1950s, Amphotericin B (AmB) in the form of Fungizone® was considered the “gold standard” in anti- fungal therapy. This was due to its broad-spectrum of activity. In the 1990s, Fungizone® was relegated to a second line treatment option after the commercialization of lipid-based formulations (AmBisome®, Abelcet® and Amphocil®). These new medicines have similar efficacies but more favourable safety profiles. These formulations will be coming off patent over the coming months and so there is an opportunity for generics manufacturers to enter the arena. However, the lack of clear regulatory guidance on how to perform bioequivalence studies with liposomal drugs makes it difficult to ensure that generic parenteral formulations present quality, efficacy and safety profiles similar to the innovator product. To date, AmB therapy relies mostly on parenteral administration although infusion-related side effects and nephrotoxicity can lead to treatment being halted. Non-parenteral AmB administration would potentially lead to safer treatments and expand the benefits of antifungal and antileishmanial therapy with this drug worldwide. Despite real scientific advances in the area over the last ten years, very few delivery systems have progressed from proof-of-concept to clinical trials as oral, topical or pulmonary AmB medicines. Cyclodextrins and nanoparticle based formulations (self-emulsifying systems, cochleates and liposomes) are the most promising delivery systems to date.

Published
2013

37. Dextran-pegylated microparticles for enhanced cellular uptake of hydrophobic drugs

Author

Sonia Trombino, Andreas G. Schätzlein, Ijeoma F. Uchegbu, Roberta Cassano, and Teresa Ferrarelli

Subjects
Time Factors, Polymers, Radical polymerization, Pharmaceutical Science, Polyethylene glycol, Cell Line, Polyethylene Glycols, Inhibitory Concentration 50, chemistry.chemical_compound, Spectroscopy, Fourier Transform Infrared, PEG ratio, Polymer chemistry, Mucoadhesion, Humans, Drug Carriers, Microscopy, Confocal, Comonomer, Water, Dextrans, General Medicine, Hydrogen-Ion Concentration, Controlled release, Microspheres, Mucus, Ketoconazole, Dextran, chemistry, Drug Design, Microscopy, Electron, Scanning, Biophysics, Caco-2 Cells, Drug carrier, HT29 Cells, Hydrophobic and Hydrophilic Interactions, Biotechnology
Abstract

Polyethylene glycol monosubstituted with a polymerizable acrylic moiety was linked to 6-carboxy free position on dextran side chains and then subjected to radical polymerization with a comonomer in order to obtain microspheres for the oral controlled release of ketoconazole, a hydrophobic model drug. Microparticles were submitted to studies on their ability to absorb and retain water. Cell uptake studies, in the presence and absence of mucus, across two different monolayers, respectively, HT29-MTX-E12 and Caco-2, were done. Cytotoxicity studies were carried out to calculate the IC₅₀ value. The ability of microspheres to open monolayers tight junctions was tested by measuring their TEER values. Images of cell uptake were visualized by CLSM. In HT29-MTX-E12 cells, more mucoadhesion and drug internalization is seen thanks to the presence of PEG and dextran chains.

Published
2013

38. Phase II studies of polymer-doxorubicin (PK1, FCE28068) in the treatment of breast, lung and colorectal cancer

Author

David J. Kerr, Jim Cassidy, Richard Poyner, Leonard W. Seymour, D. R. Ferry, Hilary Calvert, Ruth Duncan, Andreas G. Schätzlein, Stuart Hesslewood, Duncan I. Jodrell, Daniel Rea, Robert Blackie, Adele Robbins, Michael J. Lind, Maggie Whitlock, Donald Bissett, Sally Burtles, Christopher M Boivin, and Chris Twelves

Subjects
Oncology, Adult, Male, Cancer Research, medicine.medical_specialty, Pathology, Lung Neoplasms, Anthracycline, Colorectal cancer, Breast Neoplasms, Iodine Radioisotopes, Breast cancer, Breast cancer 3, Internal medicine, Carcinoma, Non-Small-Cell Lung, medicine, Humans, Tissue Distribution, Lung cancer, Survival rate, Aged, Acrylamides, Antibiotics, Antineoplastic, business.industry, Cancer, Middle Aged, medicine.disease, Prognosis, Survival Rate, Treatment Outcome, Doxorubicin, Female, Breast disease, business, Colorectal Neoplasms
Abstract

Phase I studies of [N-(2-hydroxypropyl)methacrylamide] (HPMA) copolymer-doxorubicin previously showed signs of activity coupled with 5-fold decreased anthracycline toxicity in chemotherapy-refractory patients. Here we report phase H studies using a similar material (FCE28068) in patients with breast (n=17), non-small cell lung (NSCLC, n=29) and colorectal (n=16) cancer. Up to 8 courses of PK1 (280 mg/m(2) doxorubicin-equivalent) were given i.v., together with I-123-labelled imaging analogue. Toxicities were tolerable, with grade 3 neutropenia more prominent in patients with breast cancer (4/17, 23.5% compared with 5/62, 8.1% overall). Of 14 evaluable patients with breast cancer 3 had partial responses (PR), all anthracycline-naive patients. In 26 evaluable patients with NSCLC, 3 chemotherapy-naive patients had PR. In contrast, none of the 16 evaluable patients with colorectal cancer responded. Imaging of 16 patients (5 with breast cancer, 6 NSCLC, 5 colorectal cancer) showed obvious tumour accumulation in 2 metastatic breast cancers, although unfortunately no images were obtained from patients who responded. These results show 6/62 PR with limited side effects, Supporting the concept that polymer-bound therapeutics can have modified and improved anticancer activities and suggesting the approach should be explored further for breast cancer and NSCLC.

Published
2016

39. Polymer Based Gene Silencing: In Vitro Delivery of SiRNA

Author

Ijeoma F. Uchegbu, Andreas G. Schätzlein, and Margarida Isabel Simão Carlos

Subjects
0301 basic medicine, Transfection, Gene delivery, Biology, Molecular biology, In vitro, Cell biology, Blot, 03 medical and health sciences, 030104 developmental biology, Downregulation and upregulation, RNA interference, Gene silencing, Intracellular
Abstract

Gene silencing may be achieved by harnessing the RNA interference mechanism to effect down-regulation of protein expression. The therapeutic use of siRNA is dependent on its delivery to the intracellular space. This chapter describes the delivery of siRNA by N-(2-ethylamino)-6-O-glycolchitosan (EAGC). EAGC is a chitosan-based polymer, which binds to siRNA to form nanoparticles (NPs). The steps necessary to determine the delivery capacity of a polymer are presented in this chapter using EAGC as an example. The steps include: the transfection of cells with EAGC-siRNA polyplexes and protein detection by a Western Blotting assay.

Published
2016

40. Dendrimers for gene therapy

Author

Manuel J. Santander-Ortega, Andreas G. Schätzlein, Ijeoma F. Uchegbu, and M. V. Lozano

Subjects
Low toxicity, Chemistry, In vivo, Dendrimer, Genetic enhancement, Nanotechnology
Abstract

Dendrimers have a number of favorable properties, such as good transfection efficiency and relatively low toxicity, which have promoted their wider investigation as synthetic vectors for gene therapy. Their well-defined branched molecular architecture is highly adaptable thanks to the facile attachment of tunable functional groups that allow a range of chemical modifications. These are, for example, targeted at improving the gene condensation capacity, reducing toxicity, as well as aiming to give stealth or targeting properties after administration. These modification strategies have now been widely tested in tightly controlled in vitro environments. However, in more complex and changeable in vivo milieu, individual chemical modifications, aimed at selectively modulating a specific aspect in vitro, can end up causing in parallel undesirable side effects in vivo. The development of evaluation strategies for these systems will therefore need continue so that in-depth in vitro characterization of these colloidal systems become predictive of their actual properties after in vivo administration. This will allow the accelerated development of strategies aimed at tailoring of plain or chemically modified dendriplexes in order to overcome the different physiological and biological barriers in vivo and will allow these vectors to reach their full therapeutic potential.

Published
2016

41. Delivery of Peptides to the Blood and Brain after Oral Uptake of Quaternary Ammonium Palmitoyl Glycol Chitosan Nanoparticles

Author

Julian Moger, Ijeoma F. Uchegbu, Aikaterini Lalatsa, Andreas G. Schätzlein, Natalie L. Garrett, and T Ferrarelli

Subjects
Male, Biodistribution, Administration, Oral, Pharmaceutical Science, Peptide, Absorption (skin), Pharmacology, Dosage form, Mice, Oral administration, Drug Discovery, Animals, chemistry.chemical_classification, Chitosan, Mice, Inbred BALB C, Gastrointestinal tract, Chemistry, Brain, Mucus, Bioavailability, Molecular Weight, Quaternary Ammonium Compounds, Biochemistry, Nanoparticles, Molecular Medicine, Peptides
Abstract

The clinical development of therapeutic peptides has been restricted to peptides for non-CNS diseases and parenteral dosage forms due to the poor permeation of peptides across the gastrointestinal mucosa and the blood-brain barrier. Quaternary ammonium palmitoyl glycol chitosan (GCPQ) nanoparticles facilitate the brain delivery of orally administered peptides such as leucine(5)-enkephalin, and here we examine the mechanism of GCPQ facilitated oral peptide absorption and brain delivery. By analyzing the oral biodistribution of radiolabeled GCPQ nanoparticles, the oral biodistribution of the model peptide leucine(5)-enkephalin and coherent anti-Stokes Raman scattering microscopy tissue images after an oral dose of deuterated GCPQ nanoparticles, we have established a number of facts. Although 85-90% of orally administered GCPQ nanoparticles are not absorbed from the gastrointestinal tract, a peak level of 2-3% of the oral GCPQ dose is detected in the blood 30 min after dosing, and these GCPQ particles appear to transport the peptides to the blood. Additionally, although peptide loaded nanoparticles from low (6 kDa) and high (50 kDa) molecular weight GCPQ are taken up by enterocytes, polymer particles with a polymer molecular weight greater than 6 kDa are required to facilitate peptide delivery to the brain after oral administration. By examining our current and previous data, we conclude that GCPQ particles facilitate oral peptide absorption by protecting the peptide from gastrointestinal degradation, adhering to the mucus to increase the drug gut residence time and transporting GCPQ associated peptide across the enterocytes and to the systemic circulation, enabling the GCPQ stabilized peptide to be transported to the brain. Orally administered GCPQ particles are also circulated from the gastrointestinal tract to the liver and onward to the gall bladder, presumably for final transport back to the gastrointestinal tract.

Published
2012

42. Exploring uptake mechanisms of oral nanomedicines using multimodal nonlinear optical microscopy

Author

Andreas G. Schätzlein, Julian Moger, Ijeoma F. Uchegbu, Aikaterini Lalatsa, and Natalie L. Garrett

Subjects
Male, Drug, Optical Phenomena, Polymers, media_common.quotation_subject, Administration, Oral, General Physics and Astronomy, Nanotechnology, Spectrum Analysis, Raman, General Biochemistry, Genetics and Molecular Biology, Imaging modalities, Mice, Animals, General Materials Science, media_common, Mice, Inbred BALB C, Chemistry, General Engineering, Biological Transport, General Chemistry, Chitosan nanoparticles, Polymeric nanoparticles, Two photon fluorescence, Nonlinear optical microscopy, Microscopy, Fluorescence, Multiphoton, Nanomedicine, Organ Specificity, Drug delivery, Biophysics, Nanoparticles
Abstract

Advances in pharmaceutical nanotechnology have yielded ever increasingly sophisticated nanoparticles for medicine delivery. When administered via oral, intravenous, ocular and transcutaneous delivery routes, these nanoparticles can elicit enhanced drug performance. In spite of this, little is known about the mechanistic processes underlying interactions between nanoparticles and tissues, or how these correlate with improved pharmaceutical effects. These mechanisms must be fully understood before nanomedicines can be rationally engineered to optimise their performance. Methods to directly visualise these particulates within tissue samples have traditionally involved imaging modalities requiring covalent labelling of fluorescent or radioisotope contrast agents. We present CARS, second harmonic generation and two photon fluorescence microscopy combined as a multi-modal label-free method for pinpointing polymeric nanoparticles within the stomach, intestine, gall bladder and liver. We demonstrate for the first time that orally administered chitosan nanoparticles follow a recirculation pathway from the GI tract via enterocytes, to the liver hepatocytes and intercellular spaces and then to the gall bladder, before being re-released into the gut together with bile.

Published
2012

43. Cancer-Specific Transgene Expression Mediated by Systemic Injection of Nanoparticles

Author

Andreas G. Schätzlein, Ming-Shen Dai, Patrick Baril, Inge Peerlinck, Bruno Pitard, Jerome Burnet, Andrew Merron, Pilar Martin-Duque, Raphaël Chèvre, Olivier Lambert, Mark E. Weeks, Georges Vassaux, Katherine Bolton, Ghassan Alusi, Stephen J. Mather, Ijeoma F. Uchegbu, Edward J. Chisholm, Chimie et Biologie des Membranes et des Nanoobjets (CBMN), Université de Bordeaux (UB)-École Nationale d'Ingénieurs des Travaux Agricoles - Bordeaux (ENITAB)-Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS), Centre for Molecular Oncology and Imaging, Centre for Molecular Oncology and Imaging, Barts Cancer Institute, Centre de biophysique moléculaire (CBM), and Université d'Orléans (UO)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Institut de Chimie du CNRS (INC)

Subjects
Dendrimers, Cancer Research, Biodistribution, Light, [SDV]Life Sciences [q-bio], Transgene, Transplantation, Heterologous, Mice, Nude, Enhanced permeability and retention effect, Gene delivery, Biology, Polypropylenes, Mice, 03 medical and health sciences, 0302 clinical medicine, Drug Stability, Microscopy, Electron, Transmission, Gene expression, Animals, Humans, Scattering, Radiation, Colloids, 030304 developmental biology, Mice, Inbred BALB C, Mice, Inbred C3H, 0303 health sciences, Reporter gene, Fourier Analysis, Macrophages, Gene Transfer Techniques, DNA, Transfection, Molecular biology, 3. Good health, Cell biology, Transplantation, Oncology, 030220 oncology & carcinogenesis, Nanoparticles, Female, HeLa Cells, Plasmids
Abstract

The lack of safe and efficient systemic gene delivery vectors has largely reduced the potential of gene therapy in the clinic. Previously, we have reported that polypropylenimine dendrimer PPIG3/DNA nanoparticles are capable of tumor transfection upon systemic administration in tumor-bearing mice. To be safely applicable in the clinic, it is crucial to investigate the colloidal stability of nanoparticles and to monitor the exact biodistribution of gene transfer in the whole body of the live subject. Our biophysical characterization shows that dendrimers, when complexed with DNA, are capable of forming spontaneously in solution a supramolecular assembly that possesses all the features required to diffuse in experimental tumors through the enhanced permeability and retention effect. We show that these nanoparticles are of sizes ranging from 33 to 286 nm depending on the DNA concentration, with a colloidal stable and well-organized fingerprint-like structure in which DNA molecules are condensed with an even periodicity of 2.8 nm. Whole-body nuclear imaging using small-animal nano-single-photon emission computed tomography/computer tomography scanner and the human Na/I symporter (NIS) as reporter gene shows unique and highly specific tumor targeting with no detection of gene transfer in any of the other tissues of tumor-bearing mice. Tumor-selective transgene expression was confirmed by quantitative reverse transcription-PCR at autopsy of scanned animals, whereas genomic PCR showed that the tumor sites are the predominant sites of nanoparticle accumulation. Considering that NIS imaging of transgene expression has been recently validated in humans, our data highlight the potential of these nanoparticles as a new formulation for cancer gene therapy. [Cancer Res 2009;69(6):2655–62]

Published
2009

44. Oral particle uptake and organ targeting drives the activity of amphotericin B nanoparticles

Author

Ijeoma F. Uchegbu, Javier Capilla, Andreas G. Schätzlein, Pablo Bilbao-Ramos, Juan J. Torrado, M. Paloma Ballesteros, Julian Moger, Aikaterini Lalatsa, Dolores R. Serrano, M. Auxiliadora Dea-Ayuela, Josep Guarro, Natalie L. Garrett, and F Bolás

Subjects
Drug, Male, Antifungal Agents, media_common.quotation_subject, Antiprotozoal Agents, Pharmaceutical Science, Administration, Oral, Pharmacy, Pharmacology, RS, Mice, WNU, Therapeutic index, Drug Delivery Systems, Drug Stability, Amphotericin B, Drug Discovery, medicine, Animals, Dissolution testing, media_common, Liposome, Mice, Inbred BALB C, business.industry, Bioavailability, Nanomedicine, Drug delivery, Molecular Medicine, Nanoparticles, business, medicine.drug
Abstract

There are very few drug delivery systems that target key organs via the oral route, as oral delivery advances normally address gastrointestinal drug dissolution, permeation, and stability. Here we introduce a nanomedicine in which nanoparticles, while also protecting the drug from gastric degradation, are taken up by the gastrointestinal epithelia and transported to the lung, liver, and spleen, thus selectively enhancing drug bioavailability in these target organs and diminishing kidney exposure (relevant to nephrotoxic drugs). Our work demonstrates, for the first time, that oral particle uptake and translocation to specific organs may be used to achieve a beneficial therapeutic response. We have illustrated this using amphotericin B, a nephrotoxic drug encapsulated within N-palmitoyl-N-methyl-N,N-dimethyl-N,N,N-trimethyl-6-O-glycol chitosan (GCPQ) nanoparticles, and have evidenced our approach in three separate disease states (visceral leishmaniasis, candidiasis, and aspergillosis) using industry standard models of the disease in small animals. The oral bioavailability of AmB-GCPQ nanoparticles is 24%. In all disease models, AmB-GCPQ nanoparticles show comparable efficacy to parenteral liposomal AmB (AmBisome). Our work thus paves the way for others to use nanoparticles to achieve a specific targeted delivery of drug to key organs via the oral route. This is especially important for drugs with a narrow therapeutic index.

Published
2015

45. Dendrimers in gene delivery

Author

Ijeoma F. Uchegbu, Andreas G. Schätzlein, and Christine Dufès

Subjects
Dendrimers, Chemical Phenomena, Chemistry, Physical, Genetic Vectors, Genetic transfer, Gene Transfer Techniques, Gene Expression, Pharmaceutical Science, Nanotechnology, Genetic Therapy, Biology, Gene delivery, RS, Pharmaceutical technology, Dendrimer, Nucleic acid, Animals, Humans, Dna complex
Abstract

Dendrimers have unique molecular architectures and properties that make them attractive materials for the development of nanomedicines. Key properties such as defined architecture and a high ratio of multivalent surface moieties to molecular volume also make these nanoscaled materials highly interesting for the development of synthetic (non-viral) vectors for therapeutic nucleic acids. Rational development of such vectors requires the link to be made between dendrimer structure and the morphology and physicochemistry of the respective nucleic acid complexes and, furthermore, to the biological performance of these systems at the cellular and systemic level. The review focuses on the current understanding of the role of dendrimers in those aspects of synthetic vector development. Dendrimer-based transfection agents have become routine tools for many molecular and cell biologists but therapeutic delivery of nucleic acids remains a challenge.

Published
2005

46. Synthetic Anticancer Gene Medicine Exploits Intrinsic Antitumor Activity of Cationic Vector to Cure Established Tumors

Author

Irina Proutski, Christine Dufès, W. Nicol Keith, Ijeoma F. Uchegbu, Alan Bilsland, and Andreas G. Schätzlein

Subjects
Cancer Research, Telomerase, Genetic enhancement, Transgene, Genetic Vectors, Uterine Cervical Neoplasms, Adenocarcinoma, Biology, Polypropylenes, Transfection, Cell Line, Tumor, Neoplasms, Animals, Humans, Telomerase reverse transcriptase, Promoter Regions, Genetic, Expression vector, Tumor Necrosis Factor-alpha, Genetic transfer, Genetic Therapy, Xenograft Model Antitumor Assays, Nanostructures, Lac Operon, Oncology, Epidermoid carcinoma, Immunology, Carcinoma, Squamous Cell, Cancer research, Female, Colorectal Neoplasms, Plasmids
Abstract

The systemic delivery of genetic therapies required for the treatment of inaccessible tumors and metastases remains a challenge despite the development of various viral and synthetic vector systems. Here we show that a synthetic vector system based on polypropylenimine dendrimers has the desired properties of a systemic delivery vehicle and mediates efficient transgene expression in tumors after i.v. administration. The systemic tumor necrosis factor α (TNFα) gene therapy was efficacious in the experimental treatment of established A431 epidermoid carcinoma, C33a cervix carcinoma, and LS174T colorectal adenocarcinoma. Specifically, the systemic injection of dendrimer nanoparticles containing a TNFα expression plasmid regulated by telomerase gene promoters (hTR and hTERT) leads to transgene expression, regression of remote xenograft murine tumors, and long-term survival of up to 100% of the animals. Interestingly, these dendrimers and, to a lesser extent, other common polymeric transfection agents also exhibit plasmid-independent antitumor activity, ranging from pronounced growth retardation to complete tumor regression. The genetic therapy as well as treatment with dendrimer alone was well tolerated with no apparent signs of toxicity in the animals. The combination of intrinsic dendrimer activity and transcriptionally targeted TNFα when complexed was significantly more potent than either treatment alone or when both were administered in sequence. The combination of pharmacologically active synthetic transfection agent and transcriptionally targeted antitumor gene creates an efficacious gene medicine for the systemic treatment of experimental solid tumors.

Published
2005

47. Tumour gene expression from C12 spermine amphiphile gene delivery systems

Author

Andreas G. Schätzlein, Carolyn A. Converse, Ijeoma F. Uchegbu, Pei Lee Kan, Alexander I. Gray, and Laurence Tetley

Subjects
Stereochemistry, Genetic transfer, Bolaamphiphile, Pharmaceutical Science, Spermine, Genetic Therapy, Gene delivery, Biology, Rats, Gene Expression Regulation, Neoplastic, Structure-Activity Relationship, Surface-Active Agents, chemistry.chemical_compound, Drug Delivery Systems, chemistry, Neoplasms, Amphiphile, PEG ratio, Animals, Ammonium, Ethylene glycol
Abstract

Gene therapy requires safe and efficient gene delivery systems. Towards this aim both the gene formulation and tumour transfection ability of C12 spermine amphiphiles were tested. Five amphiphiles were synthesised and characterised: 1-[N,N-bis(3-aminopropyl)-1,4-butane diamine] dodecane (12G0--a C12 spermine amphiphile), a poly(ethylene glycol) (PEG, MW = 2 kDa) derivative of 12G0, 1,12-[N,N-bis(3-aminopropyl)-1,4-butane diamine] dodecane (12G1--a C12 spermine bolaamphiphile) and N-methyl quaternary ammonium derivatives of both 12G0 (12QG0) and 12G1 (12QG1). All amphiphiles except 12G0, which precipitates, yield nanoparticles in aqueous media with and without DNA. Thus when 12G0 is substituted with either quaternary ammonium or PEG groups it forms nanoparticles both with and without DNA. The minimum nitrogen, phosphate ratio required to completely condense DNA (NP) was inversely proportional to the particles' zeta potential (zeta), NP = 1626/zeta(0.98). Biological testing showed that both PEG and quaternary ammonium groups diminished the membrane lytic ability of these C12 amphiphiles. On intratumoural injection, while PEG groups hamper gene transfer, the quaternary ammonium amphiphile (12QG0) produces tumour confined gene expression that is 80% of that produced by linear poly(ethylenimine) (LPEI, MW = 22 kDa); while the intratumoural injection of LPEI produced significant gene expression in the liver and lung, making 12QG0 suitable for the administration of cytotoxic tumouricidal genes.

Published
2005

48. Preferential liver gene expression with polypropylenimine dendrimers

Author

Martyn C. Davies, Ya Tsz A. Chim, Andreas G. Schätzlein, Christine Dufès, Adurrahim Elouzi, Ijeoma F. Uchegbu, Alexander I. Gray, Bernd H. Zinselmeyer, Avril Anstruther Munro, and Clive J. Roberts

Subjects
Genetic enhancement, Pharmaceutical Science, Gene delivery, Biology, Polypropylenes, Transfection, Mice, chemistry.chemical_compound, Drug Delivery Systems, In vivo, Cell Line, Tumor, Dendrimer, Gene expression, Animals, Humans, Mice, Inbred BALB C, Gene Transfer Techniques, DNA, Molecular biology, In vitro, Liver, chemistry, Biochemistry, Female, Ethidium bromide
Abstract

Previously, the lower generation (DAB 8-generation 2 and DAB 16-generation 3) polypropylenimine dendrimers have been shown to be effective gene delivery systems in vitro. In the current work, we sought to: (a) test the effect of the strength of the carrier, DNA electrostatic interaction on gene transfer and (b) to study the in vivo gene transfer activity of these low molecular weight (

Published
2005

49. Functional characterization of heat shock protein 90 targeted compounds

Author

Yixi Zhang, Andreas G. Schätzlein, Min Yang, Maria de la Fuente, and Isa N. Cruz

Subjects
Adenosine Triphosphatases, ATPase, Biophysics, food and beverages, Antineoplastic Agents, Cell Biology, Plasma protein binding, Biology, Biochemistry, Hsp90, Inhibitory Concentration 50, In vivo, Heat shock protein, biology.protein, medicine, Chaperone complex, Bioassay, Biological Assay, HSP90 Heat-Shock Proteins, Molecular Biology, Novobiocin, Protein Binding, medicine.drug
Abstract

Heat shock protein 90 (Hsp90) is an attractive cancer target that possesses two potential binding domains at the C and N termini. Nevertheless, assays that can reliably distinguish between the C- and N-terminal Hsp90 inhibitors and quantitatively characterize candidate drugs are limited. Here we report an Hsp90 binding assay and ATPase inhibition assay that can not only separate the C- and N-terminal inhibitors but also quantitatively determine their respective IC50 values.

Published
2013

50. Glucose-targeted niosomes deliver vasoactive intestinal peptide (VIP) to the brain

Author

Andreas G. Schätzlein, Jean-Marc Muller, Frederic Gaillard, Ijeoma F. Uchegbu, Christine Dufès, and Jean-Christophe Olivier

Subjects
Male, medicine.medical_specialty, Central nervous system, Vasoactive intestinal peptide, Drug Evaluation, Preclinical, Pharmaceutical Science, Pharmacology, Blood–brain barrier, RS, Iodine Radioisotopes, Mice, Drug Delivery Systems, In vivo, Internal medicine, Animals, Technology, Pharmaceutical, Medicine, Tissue Distribution, Niosome, Chromatography, High Pressure Liquid, Drug Carriers, business.industry, Vesicle, Brain, Transporter, Glucose, medicine.anatomical_structure, Endocrinology, Blood-Brain Barrier, Injections, Intravenous, business, Drug carrier, hormones, hormone substitutes, and hormone antagonists, Vasoactive Intestinal Peptide
Abstract

The aim of this study was to evaluate glucose-bearing niosomes as a brain targeted delivery system for the vasoactive intestinal peptide (VIP). To this end, VIP/125I-VIP-loaded glucose-bearing niosomes were intravenously injected to mice. Brain uptake was determined by measuring the radioactivity of 125I-labeled VIP using gamma-counting, after intravenous administration of VIP in solution or encapsulated in glucose-bearing niosomes or in control niosomes. VIP integrity was assessed by reversed-phase HPLC analysis of brain extracts. Distribution of 125I-VIP derived radioactivity was examined from serial brain slices. HPLC analysis confirmed the presence of intact VIP in brain after administration of VIP-loaded niosomes, but not after administration of VIP solution. Encapsulation within glucose-bearing niosomes mainly allowed a significantly higher VIP brain uptake compared to control niosomes (up to 86%, 5min after treatment). Brain distribution of intact VIP after injection of glucose-bearing niosomes, indicated that radioactivity was preferentially located in the posterior and the anterior parts of the brain, whereas it was homogeneously distributed in the whole brain after the administration of control vesicles. In conclusion, this novel vesicular formulation of VIP delivers intact VIP to particular brain regions in mice. Glucose-bearing vesicles might be therefore a novel tool to deliver drugs across the blood-brain barrier (BBB).

Published
2004

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