Your search keyword '"Shirin Tavakoli"' showing total 28 results

1. Ubiquitin-specific peptidases in lymphoma: a path to novel therapeutics

Author

Maryam Samareh Salavatipour, Shirin Tavakoli, Aram Halimi, Shima Tavoosi, Amir-Hossein Baghsheikhi, Abdolkarim Talebi-Taheri, Mehdi Niloufari, Zahra Salehi, Javad Verdi, Soheila Rahgozar, Alireza Mosavi-Jarrahi, and Mohammad Ahmadvand

Subjects

ubiquitin-specific peptidases, USPs, cancer, lymphoma, non-Hodgkin, Hodgkin, Therapeutics. Pharmacology, RM1-950

Abstract

BackgroundUbiquitin-specific peptidases (USPs), also known as deubiquitinating enzymes (DUBs), play a crucial role in maintaining cellular homeostasis by selectively removing ubiquitin molecules from targeted proteins. This process affects protein stability, subcellular localization, and activity, thereby influencing processes such as DNA repair, cell cycle regulation, and apoptosis. Abnormal USP activities have been linked to various diseases, including cancer. Emerging evidence in lymphoma studies highlights the significance of USPs in controlling signaling pathways related to cancer initiation and progression and presents them as potential therapeutic targets.AimThis study aimed to elucidate the multifaceted roles of USPs in lymphoma.MethodsThis systematic review was conducted according to the Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA) guidelines. Articles published in English up to May 2023 were retrieved from PubMed, Web of Science, and Scopus. The inclusion criteria focused on studies investigating the role of USPs in lymphoma cancer, involving human subjects or relevant lymphoma cell lines, exploring molecular mechanisms and signaling pathways, and assessing diagnostic or prognostic value.ResultsAfter the selection process, 23 studies were selected for analysis. USPs were found to affect various aspects of lymphoma development and progression. Specific USPs were identified with roles in cell-cycle regulation, apoptosis modulation, drug resistance, DNA repair, and influence of key oncogenic pathways, such as B cell receptor (BCR) signaling.ConclusionThis systematic review underscores the emerging role of USPs in lymphoma and their potential as therapeutic targets. Inhibitors of USPs, such as USP14 inhibitors, show promise in overcoming drug resistance. The dynamic interplay between USPs and lymphoma biology presents an exciting opportunity for future research and the development of more effective treatments for patients with lymphoma. Understanding the intricate functions of USPs in lymphoma offers new insights into potential therapeutic strategies, emphasizing the significance of these enzymes in the context of cancer biology.

Published

2024

2. Excess iron ion reduction in a thalassemia model using silver nanoparticles modified by the tannin fraction of Myrtus communis extact

Author

Shirin Tavakoli, Mohammad Ali Ebrahimzadeh, Fatemeh Sameni, Pourya Biparva, Hamidreza Mohammadi, Ali Ziar, Afshin Zahedi Mazandarani, Soheil Vafaeinejad, and Shahram Eslami

Subjects

green synthesis, silver nanoparticle, myrtus communis, hydrolyzable tannins, chelation, iron overloaded, thalassemia, Medicine

Abstract

Objective(s): Nowadays, iron ions intoxication is the center of attention of interest in the management and treatment of thalassemia and different sorts of anemia associated with regular blood transfusions. Due to the major side effects of current drugs, they should be replaced with safer alternatives. Thus, in this study, functionalized hybrid silver nanoparticles, as an emerging perspective, were investigated for absorbing excess iron ions and their removal in an animal thalassemia model. Methods: The silver nanoparticles were green-synthesized using the Myrtus communis leaf methanolic extact (MC-AgNPs). The produced hybrid nano-Sorbents based on hydrolyzable tannin matrix loaded with silver nanoparticles were delivered for trying out in vivo iron chelation in thalassemia model mice in which iron-overload was imposed. MC-AgNPs and desferral were injected intraperitoneally four times a week for one month in mice with excess iron load. The total iron and Fe3+ content of serum was evaluated with the aid of plasma-atomic spectrometry microscopy and a Fe3+ ion measurement kit, respectively. Also, liver enzyme levels were evaluated by an auto-analyzer. Also, hepatic enzyme levels were appraised by using an auto-analyzer based the corresponding kits. Morphological transformations of the liver tissue were investigated by way of Prussian blue staining. Results: The mice treated with the MC-AgNPs demonstrated a significant reduction in serum iron content when compared with the iron-overload mice. MC-AgNPs revealed satisfying effectiveness to chelate excess iron in mice. Conclusions: This method could be considered as a competitive option for lowering the level of excess iron in vivo.

Published

2020

3. Sub-chronic intraperitonealy toxicity assessments of modified silver nanoparticles capped coated Myrtus communis-derived the hydrolyzable tannins in a mice model

Author

Shirin Tavakoli, Mohammad Ali Ebrahimzadeh, Emran Habibi, Pourya Biparva, Hamidreza Mohammadi, Afshin Zahedi Mazandarani, Soheil Vafaeinejad, Ali Ziar, and Shahram Eslami

Subjects

green synthesis, silver nanoparticle, myrtus communis, hydrolyzable tannins, sub-chronic, toxicity, Medicine

Abstract

Objective(s): The use of silver nanoparticles in the field of biomedicine is increasing day by day, but less attention has been paid to its toxicity. In this paper, the ability of the silver nanoparticles produced by a green synthesis procedure to protect the liver and its effects on liver function in male mice was investigated in a sub-chronic toxicity study. Methods: The silver nanoparticles functionalized the hydrolyzable tannin fraction of Myrtus communis (MC-AgNPs) were used for testing in vivo sub-chronic toxicity in mice model. The MC-AgNPs and Ag+ were intraperitoneally injected with different doses 5 times a week over 90 days. The biochemical, hematological factors were determined using an autoanalyzer following the routine procedures. In addition, histopathological test of liver tissue in laboratory mice were examined through haematoxylin & eosin staining. Results: The obtained results showed that liver enzymes (AST, ALT, and ALP) were decreased. The mean value ± standard deviation of white blood cells, lymphocytes, red blood cells and Hb were increased, while red blood cells and hemoglobin decreased. Histopathological investigations indicated no obvious effect on hepatic cyto-architecture in the group receiving silver nanoparticles (50 mg/kg), and mild inflammation in the port space. In the groups receiving silver nanoparticles (100 and 200 mg/kg), mild inflammation, and moderate inflammation were observed in the port space and pre portal, respectively. Conclusions: The findings indicated that AgNPs could be safe even for long-term use in a therapeutic period if hybridized with active biomolecules.

Published

2020

4. Safety Evaluation of Nano Iron Zero Valente Green Synthesized: A Comparative Study

Author

Shirin Tavakoli, Fatemeh Sameni, Mohammad Ali Ebrahimzadeh, Pourya Biparva, Hamidreza Mohammadi, Afshin Zahedi, Alireza Rafiei, Mostafa Kardan, and Shahram Eslami

Subjects

iron nanoparticles, myrtus communis, green synthesis, cytotoxicity, Medicine

Abstract

Objective(s): Nowadays, examining the toxicity of nanoparticles including the synthesized and functionalized iron nanoparticles using methods like green synthesis is highly considered, due to their increasing usage in various fields of medicine, biology, industrial, and pollution removal. Hence, in this study, the toxicity of the zero valent iron nanoparticles synthesized by plant-Myrtus communis (MC-ZVINP) was investigated. Methods: Human normal Foreskin Fibroblast (HFF) cells were used for cytotoxicity examination using MTT method. Also, biochemical factors such as liver enzymes level, and factors such as the number of white and red globules, lymphocytes, platelets, amount of blood hemoglobin, and histopathological test of liver tissue in laboratory small rats were examined after intraperitoneal injections of the MC-ZVINP with different concentrations daily and a duration of 3-month, with the groups receiving trivalent iron, the extract of plant-case, and normal saline. Results: Cytotoxicity concentration of iron-case nanoparticles was obtained for 50% of HFF cells (CC50=149.23±4.45μg/mL). The results obtained from the blood factors examination showed a decreased the serum level of liver enzymes as well as an increase in the number of red and white globules and hemoglobin rate in mice receiving iron nanoparticles compared to the trivalent iron receiving group. Receiving the concentrations of 100 and 200 mg/kg/bw of iron nanoparticles have caused the incidence of mild and moderate inflammation in the liver of mice. Conclusions: Generally, it can be concluded that, the MC-ZVINP have shown no significant toxicity on the levels of blood cells, enzymes, and liver tissue.

Published

2020

5. Green synthesis of multifunctional silver nanoparticles using quercetin and their therapeutic potential

Author

Saeedeh Maghsoodloo, Mohammad Ali Ebrahimzadeh, Shirin Tavakoli, Hamidreza Mohammadi, Pourya Biparva, Alireza Rafiei, Mostafa Kardan, Mahsa Mohammadyan, and Shahram Eslami

Subjects

quercetin, green synthesis, silver nanoparticle, antioxidant, anticancer, antifungal, Medicine

Abstract

Objective(s): Active species used in bio-chemical for synthesizing nanoparticles is poly phenolic compounds. The ability of flavonoids (e.g. quercetin) to dissolve in water is low and the production of metallic nanoparticles from them in the aqueous medium is hard. Previous studies recommend that quercetin was not capable of reducing Ag+ to Ag0. The current research aimed at synthesizing quercetin-mediated silver nanoparticles (Q-AgNPs) and evaluate the antioxidant and anticancer activities of Q-AgNPs in vitro. Methods: The green synthesis of Q-AgNPs in an aqueous medium has been demonstrated. The resultant nanoparticles were characterized by several analytical techniques of imaging and spectroscopic. The improved antioxidant activity of Q-AgNPs (DPPH and nitric oxide scavenging and iron chelating assay) was determined by the colorimetric method. Possible biomedical applications such as antioxidant and anticancer activities of Q-AgNPs have been assessed. Results: The DPPH and nitric oxide radical scavenging activity of Q-AgNPs was found to be (IC50=46.47±1.79 and 30.64±3.18μg/mL, respectively). Q-AgNPs exhibited better iron chelating activity than standard EDTA (IC50=3.12 ±0.44μg/mL). Significant anticancer activity of Q-AgNPs (IC50=57.42μg/mL) was found against HepG2 cell lines after 24-hour exposure. Furthermore, the antifungal activity (MIC = 4, 8 and > 64 μg/mL) was found against Candida krusei, Candida parapsilosis and Aspergillus fumigatus, respectively. Conclusions: The present method is a competitive option to produce multifunctional nanoscale hybrid materials with higher efficiency and using natural sources for diverse biomedical applications such as antioxidant and anticancer activities.

Published

2020

6. Effect of PEGylation on assembly morphology and cellular uptake of poly ethyleneimine-cholesterol conjugates for delivery of sorafenib tosylate in hepatocellular carcinoma

Author

Maryam Monajati, Shirin Tavakoli, Samira Sadat Abolmaali, Gholamhossein Yousefi, and AliMohammad Tamaddon

Subjects

poly ethyleneimine, cholesterol, lipopolymer, pegylation, polymeric micelles, sorafenib tosylate, hepatocellular carcinoma, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

Introduction: Sorafenib (SFB) is an FDA-approved chemotherapeutic agent with a high partition coefficient (log P = 4.34) for monotherapy of hepatocellular carcinoma (HCC). The oral bioavailability is low and variable, so it was aimed to study the application of the polymeric nanoassembly of cholesterol conjugates of branched polyethyleneimine (PEI) for micellar solubilization of SFB and to investigate the impact of the polymer PEGylation on the physicochemical and cellular characteristics of the lipopolymeric dispersions. Methods: Successful synthesis of cholesterol-PEI lipopolymers, either native or PEGylated, was confirmed by FTIR, 1H-NMR, pyrene assay methods. The nanoassemblies were also characterized in terms of morphology, particle size distribution and zeta-potential by TEM and dynamic light scattering (DLS). The SFB loading was optimized using general factorial design. Finally, the effect of particle characteristics on cellular uptake and specific cytotoxicity was investigated by flow cytometry and MTT assay in HepG2 cells. Results: Transmission electron microscopy (TEM) showed that PEGylation of the lipopolymers reduces the size and changes the morphology of the nanoassembly from rod-like to spherical shape. However, PEGylation of the lipopolymer increased critical micelle concentration (CMC) and reduced the drug loading. Moreover, the particle shape changes from large rods to small spheres promoted the cellular uptake and SFB-related cytotoxicity. Conclusion: The combinatory effects of enhanced cellular uptake and reduced general cytotoxicity can present PEGylated PEI-cholesterol conjugates as a potential carrier for delivery of poorly soluble chemotherapeutic agents such as SFB in HCC that certainly requires further investigations in vitro and in vivo.

Published

2018

7. Pharmacokinetics of Pullulan–Dexamethasone Conjugates in Retinal Drug Delivery

Author

Eva Kicková, Amir Sadeghi, Jooseppi Puranen, Shirin Tavakoli, Merve Sen, Veli-Pekka Ranta, Blanca Arango-Gonzalez, Sylvia Bolz, Marius Ueffing, Stefano Salmaso, Paolo Caliceti, Elisa Toropainen, Marika Ruponen, and Arto Urtti

Subjects

pullulan, dexamethasone, conjugate, retinal drug delivery, ocular fluorophotometry, optical coherence tomography, Pharmacy and materia medica, RS1-441

Abstract

The treatment of retinal diseases by intravitreal injections requires frequent administration unless drug delivery systems with long retention and controlled release are used. In this work, we focused on pullulan (≈67 kDa) conjugates of dexamethasone as therapeutic systems for intravitreal administration. The pullulan–dexamethasone conjugates self-assemble into negatively charged nanoparticles (average size 326 ± 29 nm). Intravitreal injections of pullulan and pullulan–dexamethasone were safe in mouse, rat and rabbit eyes. Fluorescently labeled pullulan particles showed prolonged retention in the vitreous and they were almost completely eliminated via aqueous humor outflow. Pullulan conjugates also distributed to the retina via Müller glial cells when tested in ex vivo retina explants and in vivo. Pharmacokinetic simulations showed that pullulan–dexamethasone conjugates may release free and active dexamethasone in the vitreous humor for over 16 days, even though a large fraction of dexamethasone may be eliminated from the eye as bound pullulan–dexamethasone. We conclude that pullulan based drug conjugates are promising intravitreal drug delivery systems as they may reduce injection frequency and deliver drugs into the retinal cells.

Published

2021

8. Intravitreal Polymeric Nanocarriers with Long Ocular Retention and Targeted Delivery to the Retina and Optic Nerve Head Region

Author

Vijayabhaskarreddy Junnuthula, Amir Sadeghi Boroujeni, Shoupeng Cao, Shirin Tavakoli, Roxane Ridolfo, Elisa Toropainen, Marika Ruponen, Jan C. M. van Hest, and Arto Urtti

Subjects

intravitreal, polymersome, polymeric micelle, drug delivery, retina, optic nerve, Pharmacy and materia medica, RS1-441

Abstract

Posterior eye tissues, such as retina, are affected in many serious eye diseases, but drug delivery to these targets is challenging due to various anatomical eye barriers. Intravitreal injections are widely used, but the intervals between invasive injections should be prolonged. We synthesized and characterized (1H NMR, gel permeation chromatography) block copolymers of poly(ethylene glycol), poly(caprolactone), and trimethylene carbonate. These polymers self-assembled to polymersomes and polymeric micelles. The mean diameters of polymersomes and polymeric micelles, about 100 nm and 30–50 nm, respectively, were obtained with dynamic light scattering. Based on single particle tracking and asymmetric flow field-flow fractionation, the polymeric micelles and polymersomes were stable and diffusible in the vitreous. The materials did not show cellular toxicity in cultured human umbilical vein endothelial cells in the Alamar Blue Assay. Pharmacokinetics of the intravitreal nanocarriers in the rabbits were evaluated using in vivo fluorophotometry. The half-lives of the polymersomes (100 nm) and the micelles (30 nm) were 11.4–32.7 days and 4.3–9.5 days. The intravitreal clearance values were 1.7–8.7 µL/h and 3.6–5.4 µL/h for polymersomes and polymeric micelles, respectively. Apparent volumes of distribution of the particles in the rabbit vitreous were 0.6–1.3 mL for polymeric micelles and 1.9–3.4 mL for polymersomes. Polymersomes were found in the vitreous for at least 92 days post-dosing. Furthermore, fundus imaging revealed that the polymersomes accumulated near the optic nerve and retained there even at 111 days post-injection. Polymersomes represent a promising technology for controlled and site-specific drug delivery in the posterior eye segment.

Published

2021

9. Light-Activated Liposomes Coated with Hyaluronic Acid as a Potential Drug Delivery System

Author

Otto K. Kari, Shirin Tavakoli, Petteri Parkkila, Simone Baan, Roosa Savolainen, Teemu Ruoslahti, Niklas G. Johansson, Joseph Ndika, Harri Alenius, Tapani Viitala, Arto Urtti, and Tatu Lajunen

Subjects

hyaluronic acid, liposome, drug release, light activation, stability, mobility, Pharmacy and materia medica, RS1-441

Abstract

Light-activated liposomes permit site and time-specific drug delivery to ocular and systemic targets. We combined a light activation technology based on indocyanine green with a hyaluronic acid (HA) coating by synthesizing HA–lipid conjugates. HA is an endogenous vitreal polysaccharide and a potential targeting moiety to cluster of differentiation 44 (CD44)-expressing cells. Light-activated drug release from 100 nm HA-coated liposomes was functional in buffer, plasma, and vitreous samples. The HA-coating improved stability in plasma compared to polyethylene glycol (PEG)-coated liposomes. Liposomal protein coronas on HA- and PEG-coated liposomes after dynamic exposure to undiluted human plasma and porcine vitreous samples were hydrophilic and negatively charged, thicker in plasma (~5 nm hard, ~10 nm soft coronas) than in vitreous (~2 nm hard, ~3 nm soft coronas) samples. Their compositions were dependent on liposome formulation and surface charge in plasma but not in vitreous samples. Compared to the PEG coating, the HA-coated liposomes bound more proteins in vitreous samples and enriched proteins related to collagen interactions, possibly explaining their slightly reduced vitreal mobility. The properties of the most abundant proteins did not correlate with liposome size or charge, but included proteins with surfactant and immune system functions in plasma and vitreous samples. The HA-coated light-activated liposomes are a functional and promising alternative for intravenous and ocular drug delivery.

Published

2020

10. Characterization, Stability, and In Vivo Efficacy Studies of Recombinant Human CNTF and Its Permeation into the Neural Retina in Ex Vivo Organotypic Retinal Explant Culture Models

Author

Jaakko Itkonen, Ada Annala, Shirin Tavakoli, Blanca Arango-Gonzalez, Marius Ueffing, Elisa Toropainen, Marika Ruponen, Marco G. Casteleijn, and Arto Urtti

Subjects

retinal penetration, neuroprotection, protein aggregation, stability, intravitreal delivery, CNTF, Pharmacy and materia medica, RS1-441

Abstract

Ciliary neurotrophic factor (CNTF) is one of the most studied neuroprotective agents with acknowledged potential in treating diseases of the posterior eye segment. Although its efficacy and mechanisms of action in the retina have been studied extensively, it is still not comprehensively understood which retinal cells mediate the therapeutic effects of CNTF. As with therapeutic proteins in general, it is poorly elucidated whether exogenous CNTF administered into the vitreous can enter and distribute into the retina and hence reach potentially responsive target cells. Here, we have characterized our purified recombinant human CNTF (rhCNTF), studied the protein’s in vitro bioactivity in a cell-based assay, and evaluated the thermodynamic and oligomeric status of the protein during storage. Biological activity of rhCNTF was further evaluated in vivo in an animal model of retinal degeneration. The retinal penetration and distribution of rhCNTF after 24 h was studied utilizing two ex vivo retina models. Based on our characterization findings, our rhCNTF is correctly folded and biologically active. Moreover, based on initial screening and subsequent follow-up, we identified two buffers in which rhCNTF retains its stability during storage. Whereas rhCNTF did not show photoreceptor preservative effect or improve the function of photoreceptors in vivo, this could possibly be due to the used disease model or the short duration of action with a single intravitreal injection of rhCNTF. On the other hand, the lack of in vivo efficacy was shown to not be due to distribution limitations; permeation into the retina was observed in both retinal explant models as in 24 h rhCNTF penetrated the inner limiting membrane, and being mostly observed in the ganglion cell layer, distributed to different layers of the neural retina. As rhCNTF can reach deeper retinal layers, in general, having direct effects on resident CNTF-responsive target cells is plausible.

Published

2020

11. Ocular barriers to retinal delivery of intravitreal liposomes: Impact of vitreoretinal interface

Author

Tatu Lajunen, Joke Devoldere, Shirin Tavakoli, Marika Ruponen, Eva M. del Amo, Karen Peynshaert, Stefaan C. De Smedt, Katrien Remaut, Arto Urtti, Division of Pharmaceutical Biosciences, Drug Delivery Unit, Pharmaceutical Nanotechnology, Drug Research Program, and Drug Delivery

Subjects

medicine.medical_specialty, Inner limiting membrane, genetic structures, education, Pharmaceutical Science, 02 engineering and technology, Retina, VITREOUS-HUMOR, MOVEMENT, 03 medical and health sciences, chemistry.chemical_compound, Drug Delivery Systems, Vitreoretinal interface, Ophthalmology, Medicine and Health Sciences, NANOPARTICLES, medicine, Animals, Cellular localization, 030304 developmental biology, 0303 health sciences, Liposome, Biology and Life Sciences, Retinal, CATIONIC LIPIDS, 021001 nanoscience & nanotechnology, DIFFUSION, eye diseases, Animal models, Posterior segment of eyeball, Chemistry, medicine.anatomical_structure, chemistry, Targeted drug delivery, 317 Pharmacy, Intravitreal Injections, CELLS, Liposomes, Drug delivery, Nanoparticles, Retinal permeation, Cattle, sense organs, Intravitreal, 0210 nano-technology

Abstract

Drug delivery to the posterior segment of the eye is challenging due to several anatomical and physiological barriers. Thus, there is a need for prolonged action and targeted drug delivery to treat retinal diseases. Intravitreal injections avoid anterior eye barriers, but the vitreoretinal interface and inner limiting membrane (ILM) may prevent access of drug delivery systems to the retina. Existing data on retinal permeation of intravitreal nanoparticles are sparse and probably misleading due to the inter-species differences of retinal structures in rodents and humans. To bridge this gap, retinal permeation of light-activated liposomes was studied in an ex vivo bovine explant system that simulates the structure of vitreoretinal interface and intact ILM. Our findings indicate that the particle size plays a significant role in determining the retinal penetration as the liposomes of >100 nm sized failed to overcome the ILM and could not permeate into the retina. In addition, our results demonstrate the impact of surface charge and PEG-coating on retinal penetration. Small (≈ 50 nm) anionic liposomes with PEG coating showed the most extensive distribution and cellular localization in the retina. In summary, this study extends understanding of ocular barriers, and provides valuable information to augment design of retinal drug delivery systems.

Published

2020

12. Exploring the Impact of Morphology on the Properties of Biodegradable Nanoparticles and Their Diffusion in Complex Biological Medium

Author

Roxane Ridolfo, Jan C. M. van Hest, Shirin Tavakoli, Vijayabhaskarreddy Junnuthula, David S. Williams, Arto Urtti, Bio-Organic Chemistry, Institute for Complex Molecular Systems, ICMS Business Operations, ICMS Core, Drug Delivery Unit, Division of Pharmaceutical Biosciences, Drug Research Program, Pharmaceutical Nanotechnology, Doctoral Programme in Drug Research, Divisions of Faculty of Pharmacy, University of Helsinki, and Drug Delivery

Subjects

Polymers and Plastics, Polymers, 116 Chemical sciences, LIPOSOMES, Nanoparticle, Bioengineering, Nanotechnology, 02 engineering and technology, 010402 general chemistry, 01 natural sciences, Micelle, Article, DISEASE, Biomaterials, Drug Delivery Systems, Amphiphile, Materials Chemistry, Copolymer, PARTICLES, Solubility, Micelles, Drug Carriers, Liposome, Chemistry, MACULAR DEGENERATION, 021001 nanoscience & nanotechnology, 0104 chemical sciences, SIZE, TARGET, ANIMAL-MODELS, 317 Pharmacy, Drug delivery, Polymersome, Nanoparticles, SHAPE, 0210 nano-technology, RELEASE KINETICS

Abstract

Nanoparticle morphology (size, shape, and composition) and surface chemistry are the determining factors underpinning the efficacy of such materials in therapeutic applications. The size, shape, and surface chemistry of a nanoparticle can strongly influence key properties such as interactions with diverse biological fluids and interfaces and, in turn, impact the delivery of bioactive cargo, modulating therapeutic performance. This is exemplified in ocular drug delivery, where potential therapeutics must navigate complex biological media such as the gel-like vitreal fluid and the retina. Biodegradable block copolymer amphiphiles are a robust tool for the engineering of various types of self-assembled nanoparticles with diverse morphologies ranging from spherical and tubular polymersomes to spherical and worm-like micelles. Here, we explore the effect of morphological features such as shape and surface chemistry upon the interactions of a series of copolymer nanoparticles with retinal (ARPE-19) cells and the release of a low solubility drug (dexamethasone) that is currently used in ocular therapy and study their diffusion in vitreous using ex vivo eyes. We demonstrate that both aspect ratio and surface chemistry of nanoparticles will influence their performance in terms of cell uptake, drug release, and diffusion with high aspect ratio shapes demonstrating enhanced properties in relation to their spherical counterparts.

Published

2020

13. Highly Concentrated Multifunctional Silver Nanoparticle Fabrication through Green Reduction of Silver Ions in Terms of Mechanics and Therapeutic Potentials

Author

Shahram Eslami, Hamid Badali, Mostafa Kardan, Hamidreza Mohammadi, Mohammad Ali Ebrahimzadeh, Pourya Biparva, Shirin Tavakoli, and Alireza Rafiei

Subjects

Cancer Research, Thermogravimetric analysis, Antifungal Agents, Silver, Antioxidant, Cell Survival, medicine.medical_treatment, Nanoparticle, Microbial Sensitivity Tests, 02 engineering and technology, 010402 general chemistry, 01 natural sciences, Antioxidants, Silver nanoparticle, Candida krusei, medicine, Humans, Chelation, Cells, Cultured, Candida, Cell Proliferation, Ions, Pharmacology, Myrtus communis, biology, Chemistry, 021001 nanoscience & nanotechnology, biology.organism_classification, 0104 chemical sciences, Nanoparticles, Molecular Medicine, 0210 nano-technology, Hybrid material, Oxidation-Reduction, Nuclear chemistry

Abstract

Background:Green synthesis of silver nanoparticles (AgNPs) is limited to produce AgNPs with only relatively low concentrations, and is unsuitable for large-scale productions. The use of Myrtus communis (MC) leaf methanolic extract (rich in hydrolyzable tannins) has been recommended to resolve the issues related to the aggregation of nanoparticles at high concentrations of silver ions with added facet of antioxidant properties.Methods:The produced highly concentrated MC-AgNPs were characterized by using imaging and spectroscopic methods. Subsequently, antioxidant, anticancer and antifungal activities of the nanoparticles were evaluated.Results:The thermogravimetric analysis and energy dispersive spectroscopy quantitative results suggested that the nanoparticles are biphasic in nature (bio-molecule + Ag0) and layered in structure, suggesting the formation of nanoparticles through a different mechanism than those described in the literature. MC-AgNPs showed greater scavenging activity of nitric oxide and iron (II) chelating ability than the extract. It also showed good reducing power compared to the standard antioxidant. Remarkable anticancer activity of MC-AgNPs (IC50 = 5.99µg/mL) was found against HCT-116 (human colon carcinoma) cell lines after 24h exposure with a therapeutic index value 2-fold higher than the therapeutic index of standard doxorubicin. Furthermore, distinct antifungal activity (MIC = 4µg/mL) was found against Candida krusei.Conclusion:The current method outperforms the existing methods because it produces a large amount of multifunctional nanoscale hybrid materials more efficiently using natural sources; thus, it may be used for diverse biomedical applications.

Published

2020

14. Pharmacokinetics of Pullulan–Dexamethasone Conjugates in Retinal Drug Delivery

Author

Eva Kicková, Amir Sadeghi, Jooseppi Puranen, Shirin Tavakoli, Merve Sen, Veli-Pekka Ranta, Blanca Arango-Gonzalez, Silvia Bolz, Marius Ueffing, Stefano Salmaso, Paolo Caliceti, Elisa Toropainen, Marika Ruponen, Arto Urtti

Published

2022

15. Pharmacokinetics of pullulan–dexamethasone conjugates in retinal drug delivery

Author

Eva Kicková, Amir Sadeghi, Jooseppi Puranen, Shirin Tavakoli, Merve Sen, Veli-Pekka Ranta, Blanca Arango-Gonzalez, Sylvia Bolz, Marius Ueffing, Stefano Salmaso, Paolo Caliceti, Elisa Toropainen, Marika Ruponen, and Arto Urtti

Subjects

RS1-441, Conjugate, Ocular fluorophotometry, Pharmacy and materia medica, Optical coherence tomography, Pharmacokinetics, sense organs, eye diseases, Article, Dexamethasone, Pullulan, Retinal drug delivery

Abstract

The treatment of retinal diseases by intravitreal injections requires frequent administration unless drug delivery systems with long retention and controlled release are used. In this work, we focused on pullulan (≈67 kDa) conjugates of dexamethasone as therapeutic systems for intravitreal administration. The pullulan–dexamethasone conjugates self-assemble into negatively charged nanoparticles (average size 326 ± 29 nm). Intravitreal injections of pullulan and pullulan–dexamethasone were safe in mouse, rat and rabbit eyes. Fluorescently labeled pullulan particles showed prolonged retention in the vitreous and they were almost completely eliminated via aqueous humor outflow. Pullulan conjugates also distributed to the retina via Müller glial cells when tested in ex vivo retina explants and in vivo. Pharmacokinetic simulations showed that pullulan–dexamethasone conjugates may release free and active dexamethasone in the vitreous humor for over 16 days, even though a large fraction of dexamethasone may be eliminated from the eye as bound pullulan–dexamethasone. We conclude that pullulan based drug conjugates are promising intravitreal drug delivery systems as they may reduce injection frequency and deliver drugs into the retinal cells.

Published

2022

16. Pharmacokinetics of Pullulan–Dexamethasone Conjugates in Retinal Drug Delivery

Author

Urtti, Eva Kicková, Amir Sadeghi, Jooseppi Puranen, Shirin Tavakoli, Merve Sen, Veli-Pekka Ranta, Blanca Arango-Gonzalez, Sylvia Bolz, Marius Ueffing, Stefano Salmaso, Paolo Caliceti, Elisa Toropainen, Marika Ruponen, and Arto

Subjects

pullulan, dexamethasone, conjugate, retinal drug delivery, ocular fluorophotometry, optical coherence tomography, pharmacokinetics, sense organs, eye diseases

Abstract

The treatment of retinal diseases by intravitreal injections requires frequent administration unless drug delivery systems with long retention and controlled release are used. In this work, we focused on pullulan (≈67 kDa) conjugates of dexamethasone as therapeutic systems for intravitreal administration. The pullulan–dexamethasone conjugates self-assemble into negatively charged nanoparticles (average size 326 ± 29 nm). Intravitreal injections of pullulan and pullulan–dexamethasone were safe in mouse, rat and rabbit eyes. Fluorescently labeled pullulan particles showed prolonged retention in the vitreous and they were almost completely eliminated via aqueous humor outflow. Pullulan conjugates also distributed to the retina via Müller glial cells when tested in ex vivo retina explants and in vivo. Pharmacokinetic simulations showed that pullulan–dexamethasone conjugates may release free and active dexamethasone in the vitreous humor for over 16 days, even though a large fraction of dexamethasone may be eliminated from the eye as bound pullulan–dexamethasone. We conclude that pullulan based drug conjugates are promising intravitreal drug delivery systems as they may reduce injection frequency and deliver drugs into the retinal cells.

Published

2021

17. Intravitreal liposomes as ocular drug delivery systems : vitreal interactions, retinal permeation and drug release characteristics

Author

Shirin Tavakoli, University of Helsinki, Faculty of Pharmacy, Division of Pharmaceutical Biosciences, Doctoral Programme in Drug Research, Helsingin yliopisto, farmasian tiedekunta, Lääketutkimuksen tohtoriohjelma, Helsingfors universitet, farmaceutiska fakulteten, Doktorandprogrammet i läkemedelsforskning, Rupenthal, Ilva, Urtti, Arto, Ruponen, Marika, and del Amo Páez, Eva M.

Subjects

biopharmacy

Abstract

The prevalence of vision-threatening diseases of the posterior eye segment, such as age-related macular degeneration (AMD), diabetic retinopathy, diabetic macular edema and glaucoma, is increasing worldwide. This is a major burden to patients and health care systems. Current therapy includes intravitreal injections of anti-angiogenic agents against vascular endothelial growth factor (VEGF), because drug delivery to the back of the eye is hampered by anatomical and physiological barriers. Intravitreal injections are uncomfortable, may cause adverse reactions and reduced compliance leading to suboptimal treatment outcomes. Furthermore, current anti-VEGF drugs are not effective in all patients. Therefore, new drugs and delivery systems for targeted and prolonged action are needed for posterior segment eye treatment. Nanoparticles have been investigated as a long-acting and targeted ocular drug delivery systems that may prolong actions of small molecule drugs (e.g. corticosteroids and tyrosine kinase inhibitors) with short vitreal half-lives. Nanoparticles are also important for delivery of labile therapeutics with intracellular targets, including some proteins, neuroprotective peptides and nucleic acids (RNA, DNA). However, several barriers hamper retinal delivery of intravitreal nanoparticles and interspecies differences may lead to poor clinical translation. Hence, the overall objective of this study was to generate improved understanding of ocular barriers to retinal delivery of nanoparticles by using translationally valid preclinical models. We systematically studied vitreal diffusion of various liposomes and other lipid-based nanoparticles by analyzing the mobility of the nanoparticles with single particle tracking in intact porcine central vitreous with similar structure to human vitreous. We evaluated the physicochemical features of nanoparticles affecting their vitreal mobility (e.g. particle size, surface change, surface coating with polyethylene glycol or hyaluronic acid). Neutral and anionic liposomes showed faster diffusion than cationic liposomes. Small size and polymer coating modestly facilitated vitreal mobility of liposomes. Kinetic analysis demonstrated that nanoparticles’ distribution in the human vitreous is controlled by convection rather than diffusion, while vitreous liquefaction may increase the role of nanoparticle diffusion. We also studied protein corona formation on liposomes’ surface, since it may affect the hydrodynamic diameter and cellular interactions. In this regard, surface plasmon resonance analysis was performed to monitor the protein corona formation in the presence of porcine vitreous. Insignificant size change was seen indicating that vitreal diffusion is not influenced by protein corona. In addition, high-resolution proteomics confirmed identity of the proteins on liposomal surface that may change the biological interactions of the liposomes. Next, retinal permeation of liposomes was studied systematically using ex vivo analyses and bovine retinal explants. Neutral and anionic liposomes with high vitreal mobility were studied for their potential in overcoming the ILM barrier. Liposomes with diameters over 100 nm fail in retinal entry irrespective of their surface charge, while small anionic PEG-coated liposomes (

Published

2021

18. Imaging, quantitation and kinetic modelling of intravitreal nanomaterials

Author

Amir Sadeghi, Marika Ruponen, Jooseppi Puranen, Shoupeng Cao, Roxane Ridolfo, Shirin Tavakoli, Elisa Toropainen, Tatu Lajunen, Veli-Pekka Ranta, Jan van Hest, Arto Urtti, Bio-Organic Chemistry, Institute for Complex Molecular Systems, ICMS Core, Divisions of Faculty of Pharmacy, Pharmaceutical Nanotechnology, Drug Delivery Unit, Drug Research Program, Division of Pharmaceutical Biosciences, and Drug Delivery

Subjects

genetic structures, Pharmaceutical Science, MACULAR EDEMA, Modelling, Retina, Drug Delivery Systems, DEXAMETHASONE INCORPORATING LIPOSOMES, RABBIT, Polymeric micelle, IMPLANT, Animals, Pharmacokinetics, RELEASE, ENCAPSULATED GANCICLOVIR, DRUG-DELIVERY SYSTEMS, IN-VITRO, eye diseases, Nanostructures, Rats, Liposome, Kinetics, 317 Pharmacy, Intravitreal Injections, Drug delivery, Rabbits, sense organs, Intravitreal, LIPID-COMPOSITION

Abstract

In this study, the intravitreal pharmacokinetics of nanomaterials were investigated in vivo in rats and rabbits. Impact of particle size and shape (spherical, longitudinal) on ocular particle distribution and elimination was investigated with fundus camera, optical coherence tomography and ocular fluorophotometry. Differently sized particles showed prolonged ocular retention and remarkable differences in vitreal elimination, but size dependence was consistent, suggesting that other features have influence on their vitreal kinetics. We also demonstrate that liposomes are eliminated from the rabbit vitreous mainly via the anterior route. Simulation of drug concentrations after injection of intravitreal particles shows the importance of synchronized particle retention and drug release rate for efficient drug delivery. In conclusion, we provide kinetic insights in intravitreally administered nanoparticles to improve retinal drug delivery.

Published

2022

19. Liposomal sunitinib for ocular drug delivery: A potential treatment for choroidal neovascularization

Author

Shirin Tavakoli, Jooseppi Puranen, Sina Bahrpeyma, Veera E. Lautala, Suvi Karumo, Tatu Lajunen, Eva M. del Amo, Marika Ruponen, Arto Urtti, Divisions of Faculty of Pharmacy, Pharmaceutical Nanotechnology, Drug Delivery Unit, Division of Pharmaceutical Biosciences, Drug Research Program, and Drug Delivery

Subjects

Vascular Endothelial Growth Factor A, BARRIERS, Age-related macular degeneration, Pharmaceutical Science, IN-VITRO, VEGF, Choroidal Neovascularization, Liposome, Disease Models, Animal, Macular Degeneration, Mice, Drug Delivery Systems, Intravitreal injection, 317 Pharmacy, Intravitreal Injections, Liposomes, KINASE, Sunitinib, Cyclodextrin, Animals

Abstract

Choroidal neovascularization (CNV) is a prevalent vision-threatening vascular disorder in aging population. CNV is associated with several diseases in the posterior segment of the eye such as age-related macular degeneration (AMD). In this study we developed sunitinib-loaded liposomes to block the neovascularization signalling pathway through inhibition of tyrosine kinase of vascular endothelial growth factor receptors (VEGFRs). Liposomal sunitinib formulations were prepared by thin film hydration method and studied for their encapsulation efficiency (EE), loading capacity (LC) and drug release profile in buffer andvitreous. Our finding showed that the liposomes (mean size 104 nm) could effectively entrap sunitinib (EE approximate to 95%) at relatively high loading capacity (LC approximate to 5%) and release sunitinib over at least 3 days. Intravitreal sunitinib-loaded liposomes revealed inhibitory effect on established neovascularization in laser-induced CNV mouse model while the intravitreal injection of sunitinib solubilized with cyclodextrin was inefficient in management of neovascularization. Accordingly, liposomal sunitinib is a promising drug delivery system that should be further studied to inhibit the CNV related to AMD.

Published

2022

20. Light-Activated Liposomes Coated with Hyaluronic Acid as a Potential Drug Delivery System

Author

Tapani Viitala, Teemu Ruoslahti, Harri Alenius, Tatu Lajunen, Petteri Parkkila, Otto K. Kari, Arto Urtti, Niklas G. Johansson, Roosa Savolainen, Joseph Ndika, Simone Baan, and Shirin Tavakoli

Subjects

Pharmaceutical Science, lcsh:RS1-441, Protein Corona, 02 engineering and technology, Polyethylene glycol, Article, lcsh:Pharmacy and materia medica, 03 medical and health sciences, chemistry.chemical_compound, Pulmonary surfactant, Hyaluronic acid, PEG ratio, hyaluronic acid, drug release, 030304 developmental biology, 0303 health sciences, Liposome, stability, 021001 nanoscience & nanotechnology, biocorona, eye diseases, mobility, chemistry, Self-healing hydrogels, Drug delivery, liposome, Biophysics, sense organs, 0210 nano-technology, light activation

Abstract

Light-activated liposomes permit site and time-specific drug delivery to ocular and systemic targets. We combined a light activation technology based on indocyanine green with a hyaluronic acid (HA) coating by synthesizing HA&ndash, lipid conjugates. HA is an endogenous vitreal polysaccharide and a potential targeting moiety to cluster of differentiation 44 (CD44)-expressing cells. Light-activated drug release from 100 nm HA-coated liposomes was functional in buffer, plasma, and vitreous samples. The HA-coating improved stability in plasma compared to polyethylene glycol (PEG)-coated liposomes. Liposomal protein coronas on HA- and PEG-coated liposomes after dynamic exposure to undiluted human plasma and porcine vitreous samples were hydrophilic and negatively charged, thicker in plasma (~5 nm hard, ~10 nm soft coronas) than in vitreous (~2 nm hard, ~3 nm soft coronas) samples. Their compositions were dependent on liposome formulation and surface charge in plasma but not in vitreous samples. Compared to the PEG coating, the HA-coated liposomes bound more proteins in vitreous samples and enriched proteins related to collagen interactions, possibly explaining their slightly reduced vitreal mobility. The properties of the most abundant proteins did not correlate with liposome size or charge, but included proteins with surfactant and immune system functions in plasma and vitreous samples. The HA-coated light-activated liposomes are a functional and promising alternative for intravenous and ocular drug delivery.

Published

2020

21. Mesenchymal stromal cells; a new horizon in regenerative medicine

Author

Ali Hassanzadeh, Ali Shariati, Hamid Reza Ghaderi Jafarbeigloo, Shirin Tavakoli, Mohammd Amin Jadidi Kouhbanani, Adel Naimi, Kamran Javidi, Afsaneh Jahangiryan, Majid Zamani, and Faezeh Jadidi

Subjects

0301 basic medicine, Physiology, Clinical Biochemistry, Adipose tissue, Context (language use), Bone Marrow Cells, Mesenchymal Stem Cell Transplantation, Regenerative Medicine, Regenerative medicine, Chondrocyte, Cell therapy, 03 medical and health sciences, 0302 clinical medicine, Medicine, Animals, Humans, Cell Proliferation, business.industry, Mesenchymal stem cell, Osteoblast, Cell Differentiation, Mesenchymal Stem Cells, Cell Biology, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Cancer research, Bone marrow, business

Abstract

In recent decades, mesenchymal stromal cells (MSCs) biomedical utilizing has attracted worldwide growing attention. After the first report of the human MSCs obtaining from the bone marrow (BM) tissue, these cells were isolated from wide types of the other tissues, ranging from adipose tissue to dental pulp. Their specific characteristics, comprising self-renewality, multipotency, and availability accompanied by their immunomodulatory properties and little ethical concern denote their importance in the context of regenerative medicine. Considering preclinical studies, MSCs can modify immune reactions during tissue repair and restoration, providing suitable milieu for tissue recovery; on the other hand, they can be differentiated into comprehensive types of the body cells, such as osteoblast, chondrocyte, hepatocyte, cardiomyocyte, fibroblast, and neural cells. Though a large number of studies have investigated MSCs capacities in regenerative medicine in varied animal models, the oncogenic capability of unregulated MSCs differentiation must be more assessed to enable their application in the clinic. In the current review, we provide a brief overview of MSCs sources, isolation, and expansion as well as immunomodulatory activities. More important, we try to collect and discuss recent preclinical and clinical research and evaluate current challenges in the context of the MSC-based cell therapy for regenerative medicine.

Published

2020

22. Design and synthesis of lipid-mimetic cationic iridium complexes and their liposomal formulation for

Author

Julia R, Shakirova, Amir, Sadeghi, Alla A, Koblova, Pavel S, Chelushkin, Elisa, Toropainen, Shirin, Tavakoli, Leena-Stiina, Kontturi, Tatu, Lajunen, Sergey P, Tunik, and Arto, Urtti

Abstract

Two iridium [Ir(N^C)

Published

2020

23. Effect of PEGylation on assembly morphology and cellular uptake of poly ethyleneimine-cholesterol conjugates for delivery of sorafenib tosylate in hepatocellular carcinoma

Author

Gholamhossein Yousefi, Maryam Monajati, Samira Sadat Abolmaali, Shirin Tavakoli, and Ali Mohammad Tamaddon

Subjects

Medicine (General), QH301-705.5, sorafenib tosylate, Pharmaceutical Science, 02 engineering and technology, 010402 general chemistry, 01 natural sciences, General Biochemistry, Genetics and Molecular Biology, R5-920, Dynamic light scattering, In vivo, MTT assay, pegylation, lipopolymer, Biology (General), Cytotoxicity, Original Research, polymeric micelles, Chemistry, cholesterol, General Medicine, hepatocellular carcinoma, 021001 nanoscience & nanotechnology, 0104 chemical sciences, Bioavailability, poly ethyleneimine, Critical micelle concentration, PEGylation, Biophysics, 0210 nano-technology, Conjugate

Abstract

Introduction: Sorafenib (SFB) is an FDA-approved chemotherapeutic agent with a high partition coefficient (log P = 4.34) for monotherapy of hepatocellular carcinoma (HCC). The oral bioavailability is low and variable, so it was aimed to study the application of the polymeric nanoassembly of cholesterol conjugates of branched polyethyleneimine (PEI) for micellar solubilization of SFB and to investigate the impact of the polymer PEGylation on the physicochemical and cellular characteristics of the lipopolymeric dispersions. Methods: Successful synthesis of cholesterol-PEI lipopolymers, either native or PEGylated, was confirmed by FTIR, 1H-NMR, pyrene assay methods. The nanoassemblies were also characterized in terms of morphology, particle size distribution and zeta-potential by TEM and dynamic light scattering (DLS). The SFB loading was optimized using general factorial design. Finally, the effect of particle characteristics on cellular uptake and specific cytotoxicity was investigated by flow cytometry and MTT assay in HepG2 cells. Results: Transmission electron microscopy (TEM) showed that PEGylation of the lipopolymers reduces the size and changes the morphology of the nanoassembly from rod-like to spherical shape. However, PEGylation of the lipopolymer increased critical micelle concentration (CMC) and reduced the drug loading. Moreover, the particle shape changes from large rods to small spheres promoted the cellular uptake and SFB-related cytotoxicity. Conclusion: The combinatory effects of enhanced cellular uptake and reduced general cytotoxicity can present PEGylated PEI-cholesterol conjugates as a potential carrier for delivery of poorly soluble chemotherapeutic agents such as SFB in HCC that certainly requires further investigations in vitro and in vivo.

Published

2018

24. Microencapsulation of (deoxythymidine)20–DOTAP complexes in stealth liposomes optimized by Taguchi design

Author

Soliman Mohammadi Samani, Shirin Tavakoli, Ali Mohammad Tamaddon, and Nasim Golkar

Subjects

Liposome, Chromatography, Materials science, Oligonucleotide, Chemistry, Pharmaceutical, Gene Transfer Techniques, Oligonucleotides, Pharmaceutical Science, Gene delivery, Taguchi design, chemistry.chemical_compound, Drug Stability, Dynamic light scattering, chemistry, Liposomes, Nucleic acid, Particle size, Particle Size, Ethidium bromide, Thymidine

Abstract

Stealth liposomes encapsulating oligonucleotides are considered as promising non-viral gene delivery carriers; however, general preparation procedures are not capable to encapsulate nucleic acids (NAs) efficiently. In this study, the lyophobic complexes of deoxythymidine20 oligonucleotide (dT20) and DOTAP were used instead of free dT20 for nano-encapsulation process by reverse phase evaporation method. Regarding the various factors that can potentially affect the liposome characteristics, Taguchi design was applied to analyze the simultaneous effects of factors comprising PEG-lipid (%), dT20/total lipid molar ratio, cholesterol (Chol%) and organic-to-aqueous phase ratio (o/w) at three levels. The response variables, hydrodynamic diameter, loading efficiency (LE%) and capacity (LC%), were studied by dynamic light scattering and ethidium bromide exclusion assay, respectively. The optimum condition described by minimum particle size as well as high LE% and LC% was obtained at 5% PEG-lipid, dT20/total lipid of 7, 20% Chol and o/w of 3 with an average size of 84 nm, LE% = 83.4% and LC% = 11.6%. Moreover, stability assessments in presence of heparin sulfate revealed the noticeable resistance, unlike DOTAP/dT20 lipoplexes, to premature release of NA. Transmission electron microscopy confirmed formation of discrete and circular vesicles encapsulating dT20.

Published

2014

25. Clomiphene citrate versus letrozole with gonadotropins in intrauterine insemination cycles: A randomized trial

Author

Leila Pourali, Sedigheh Ayati, Shirin Tavakolizadeh, Hourieh Soleimani, and Fatemeh Teimouri Sani

Subjects

Gynecology and obstetrics, RG1-991, Reproduction, QH471-489

Abstract

Background: Clomiphene citrate is one of the effective drugs for infertility treatment due to oligo-ovulation or anovulation. Intrauterine insemination (IUI) is one of more adherent methods for treatment of infertile cases which is followed by controlled ovarian hyperstimulation (COH). Objective: the aim of this study was to evaluate Clomiphene citrate versus letrozole with gonadotropins in IUI cycles. Materials and Methods: In this prospective randomized trial, 180 infertile women who were referred to Milad Hospital were selected. The first group received 5 mg/day letrozole on day 3-7 of menstrual cycle. The second group received 100 mg/day Clomiphene in the same way as letrozole. In both groups, human menopausal gonadotropin was administered every day starting on day between 6-8 of cycle. Ovulation was triggered with urinary Human Chorionic Gonadotropin (5000 IU) when have two follicles of ≥16 mm. IUI was performed 36 hr later. Results: The number of matured follicles, cycle cancellation, and abortion were the same in both groups. Endometrial thickness was higher at the time of human menopausal gonadotropin administration in letrozole group. Chemical and clinical pregnancy rates were much higher in letrozole group. Ovarian hyperstimulation was significantly higher in clomiphene group. Conclusion: Letrozole appears to be a good alternative to clomiphene citrate with fewer side effects.

Published

2017

26. Clomiphene citrate versus letrozole with gonadotropins in intrauterine insemination cycles: A prospective randomized trial

Author

Leila Pourali, Sedigheh Ayati, Shirin Tavakolizadeh, Hourieh Soleimani, and Fatemeh Teimouri Sani

Subjects

ovarian stimulation, gonadotropin, letrozole, clomiphene citrate., Gynecology and obstetrics, RG1-991, Reproduction, QH471-489

Abstract

Background: Clomiphene citrate is one of the effective drugs for infertilitytreatment due to oligo-ovulation or anovulation. Intrauterine insemination (IUI) isone of more adherent methods for treatment of infertile cases which is followed bycontrolled ovarian hyperstimulation (COH). Objective: the aim of this study was to evaluate Clomiphene citrate versus letrozolewith gonadotropins in IUI cycles. Materials and Methods: In this prospective randomized trial, 180 infertile patientswho were referred to Milad Hospital were selected. The first group received 5mg/day letrozole on day 3-7 of menstrual cycle. The second group received 100mg/day Clomiphene in the same way as letrozole. In both groups, humanmenopausal gonadotropin was administered every day starting on day between 6-8of cycle. Ovulation was triggered with urinary Human Chorionic Gonadotropin(5000 IU) when have two follicles of ≥16 mm. IUI was performed 36 hr later. Results: The number of matured follicles, cycle cancellation, and abortion were thesame in both groups. Endometrial thickness was higher at the time of humanmenopausal gonadotropin administration in letrozole group. Chemical and clinicalpregnancy rates were much higher in letrozole group. Ovarian hyperstimulation wassignificantly higher in clomiphene group. Conclusion: Letrozole appears to be a good alternative to clomiphene citrate withfewer side effects.

Published

2017

27. Nucleic acid delivery to differentiated retinal pigment epithelial cells using cell-penetrating peptide as a carrier

Author

Munia Ganguli, Shirin Tavakoli, Mika Reinisalo, Astrid Subrizi, Bano Subia, Namit Dey, and Marika Ruponen

Subjects

Swine, Retinal cell line, Transgene, Cellular differentiation, Pharmaceutical Science, Peptide, 02 engineering and technology, Cell-Penetrating Peptides, Gene delivery, Transfection, 030226 pharmacology & pharmacy, Retina, Cell Line, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Cations, Nucleic Acids, Animals, Humans, chemistry.chemical_classification, Gene knockdown, Peptide carrier, Gene Transfer Techniques, Retinal, Cell Differentiation, Epithelial Cells, General Medicine, Genetic Therapy, 021001 nanoscience & nanotechnology, Cell biology, Polyplexe, chemistry, Cell-penetrating peptide, Chondroitin sulphate, 0210 nano-technology, Retinal Pigments, Biotechnology

Abstract

Nucleic acid delivery to the eye is a promising treatment strategy for many retinal disorders. In this manuscript, retinal gene delivery with non-coated and chondroitin sulphate (CS) coated amphipathic and cationic peptides was tested. The transfection and gene knockdown efficiencies were evaluated in different retinal pigment epithelial (RPE) cell models including both dividing and differentiated cells. In addition, the mobility of peptide-based gene delivery systems was examined in porcine vitreous by particle tracking analysis. The results indicate that amphipathic and cationic peptides are safe in vitro and are capable of high transgene expression and gene knockdown in dividing cells. We further demonstrate that incorporation of CS improves the efficiency of gene delivery of peptide-based systems. Most importantly, the transgene expression mediated by both non-coated and CS coated peptides was high in differentiated as well as in human primary RPE cells which are typically difficult to transfect. Coating of peptide-based gene delivery systems with CS improved diffusion in the vitreous and enhanced the stability of the polyplexes. The results indicate that a peptide-based system can be fine-tuned as a promising approach for retinal gene delivery.

28. Design and synthesis of lipid-mimetic cationic iridium complexes and their liposomal formulation for in vitro and in vivo application in luminescent bioimaging

Author

Sergey P. Tunik, Tatu Lajunen, Julia R. Shakirova, Elisa Toropainen, Alla A. Koblova, Leena-Stiina Kontturi, Arto Urtti, Shirin Tavakoli, Amir Sadeghi, Pavel S. Chelushkin, Drug Delivery Unit, Division of Pharmaceutical Biosciences, Drug Research Program, Helsinki Institute of Life Science HiLIFE, Pharmaceutical Nanotechnology, and Drug Delivery

Subjects

OPTICAL COHERENCE TOMOGRAPHY, General Chemical Engineering, 116 Chemical sciences, chemistry.chemical_element, 010402 general chemistry, Photochemistry, 01 natural sciences, LOADED LIPOSOMES, Iridium, DRUG-DELIVERY, Lipid bilayer, Liposome, 010405 organic chemistry, Chemistry, Ligand, Bilayer, Cationic polymerization, General Chemistry, Fluorescence, PEG, 0104 chemical sciences, 3. Good health, FLUORESCENT, 317 Pharmacy, PHOTOPHYSICAL PROPERTIES, Drug delivery, LIGANDS

Abstract

Two iridium [Ir(NC)(2)(NN)](+) complexes with the diimine NN ligand containing a long polymethylene hydrophobic chain were synthesized and characterized by using NMR and ESI mass-spectrometry: NN - 2-(1-hexadecyl-1H-imidazol-2-yl)pyridine, NC - methyl-2-phenylquinoline-4-carboxylate (Ir1) and 2-phenylquinoline-4-carboxylic acid (Ir2). These complexes were used to prepare the luminescent PEGylated DPPC liposomes (DPPC/DSPE-PEG2000/Ir-complex = 95/4.5/1 mol%) using a thin film hydration method. The narrowly dispersed liposomes had diameters of about 110 nm. The photophysics of the complexes and labeled liposomes were carefully studied. Ir1 and Ir2 give red emission (lambda(em) = 667 and 605 nm) with a lifetime in the microsecond domain and quantum yields of 4.8% and 10.0% in degassed solution. Incorporation of the complexes into the liposome lipid bilayer results in shielding of the emitters from interaction with molecular oxygen and partial suppression of excited state nonradiative relaxation due to the effect of the relatively rigid bilayer matrix. Delivery of labeled liposomes to the cultured ARPE-19 cells demonstrated the usefulness of Ir1 and Ir2 in cellular imaging. Labeled liposomes were then injected intravitreally into rat eyes and imaged successfully with optical coherence tomography and funduscopy. In conclusion, iridium complexes enabled the successful labeling and imaging of liposomes in cells and animals.