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35 results on '"Shoari, Alireza"'

14. Tumor Suppression by PD-1/PD-L1 Interaction Blockage in Mice Model

Author

Salehi, Shima, primary, Ghaderi, Hajarossadat, additional, Habibi-Anbouhi, Mahdi, additional, Shoari, Alireza, additional, Hassanzadeh Eskafi, Ayda, additional, Sabouri, Alireza, additional, Hosseininejad-Chafi, Mohammad, additional, Ashja Ardalan, Arghavan, additional, Ramezani, Behzad, additional, Kazemi-Lomedasht, Fatemeh, additional, and Behdani, Mahdi, additional

Published
2023
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18. Development of polyclonal heavy chain antibodies targeting programmed death ligand-1.

Author

Oghalaie, Akbar, Shoari, Alireza, Kazemi-Lomedasht, Fatemeh, Rahimi-Jamnani, Fatemeh, Mahboudi, Fereidoun, Ghaderi, Hajarossadat, Hosseininejad-Chafi, Mohammad, Moazzami, Reza, Ardalan, Arghavan Ashja, Piri-Gavgani, Somayeh, Shahbazzadeh, Delavar, and Behdani, Mahdi

Subjects
IMMUNOGLOBULIN heavy chains, THERAPEUTIC use of antineoplastic agents, IMMUNE checkpoint inhibitors, APOPTOSIS, IMMUNIZATION
Abstract

Programmed death ligand-1 (PD-L1, CD274 and B7-H1) has been described as a ligand for immune inhibitory receptor programmed death protein 1 (PD-1). With binding to PD-1 on activated T cells, PD-L1 can prevent T cell responses via motivating apoptosis. Consequently, it causes cancers immune evasion and helps the tumor growth; hence, PD-L1 is regarded as a therapeutic target for malignant cancers. The anti-PD-L1 monoclonal antibody targeting PD-1/PD-L1 immune checkpoint has attained remarkable outcomes in clinical application and has turned to one of the most prevalent anti-cancer drugs. The present study aimed to develop polyclonal heavy chain antibodies targeting PD-L1via Camelus dromedarius immunization. The extra-cellular domain of human PD-L1 (hPD-L1) protein was cloned, expressed, and purified. Afterwards, this recombinant protein was utilized as an antigen for camel immunization to acquire polyclonal camelid sera versus this protein. Our outcomes showed that hPD-L1 protein was effectively expressed in the prokaryotic system. The antibody-based techniques, such as enzyme-linked immunosorbent assay, western blotting, and flow cytometry displayed that the hPD-L1 protein was detected by generated polyclonal antibody. Due to the advantages of multiepitope-binding ability, our study exhibited that camelid antibody is effective to be applied significantly for detection of PD-L1 protein in essential antibody-based studies. [ABSTRACT FROM AUTHOR]

Published
2023
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19. Investigation of the therapeutic potential of recombinant bispecific bivalent anti-PD-L1/VEGF nanobody in inhibition of angiogenesis.

Author

Hassanzadeh Eskafi, Ayda, Oghalaei, Akbar, Mahboudi, Fereidoun, Ghaderi, Hajarsadat, Behdani, Mahdi, Shoari, Alireza, and Kazemi-Lomedasht, Fatemeh

Subjects
BISPECIFIC antibodies, PROGRAMMED cell death 1 receptors, VASCULAR endothelial growth factors, NEOVASCULARIZATION, IMMUNE checkpoint proteins, CHORIOALLANTOIS, STARTLE reaction
Abstract

Immunotherapy using monoclonal antibodies targeting programmed death ligand-1 (PD-L1) on cancer cells as a biomarker of escape from response to immune checkpoint has demonstrated efficacy in treating many solid tumors. In addition, some of the signals, such as vascular endothelial growth factor (VEGF), bind to receptors on the surface of normal endothelial cells and encourage angiogenesis, or the formation and survival of new blood vessels. Due to the special features of nanobodies with high specificity and affinity as a powerful new tool in cancer therapy, here, a recombinant bispecific bivalent anti-PD-L1/VEGF nanobody was constructed and its functionality in inhibition of angiogenesis in vitro was investigated. Results demonstrated that bivalent anti-PD-L1/VEGF nanobody efficiently inhibited HUVEC and A431 cells proliferation and tube formation. In addition, bivalent anti-PD-L1/VEGF nanobody efficiently inhibited angiogenesis in an ex ovo Chick Chorioallantoic Membrane assay. The results indicate for the potential of bivalent anti-PD-L1/VEGF nanobody as a novel promising tool for cancer therapy. [ABSTRACT FROM AUTHOR]

Published
2023
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25. Anti-angiogenic peptides application in cancer therapy; a review.

Author

Shoari, Alireza, Khodabakhsh, Farnaz, Ahangari Cohan, Reza, Salimian, Morteza, and Karami, Elmira

Subjects
*PROTEIN-tyrosine kinase inhibitors, *PEPTIDES, *SCAFFOLD proteins, *CANCER treatment, *MONOCLONAL antibodies, *NEOVASCULARIZATION inhibitors
Abstract

Cancer is a disease advanced via surplus angiogenesis. The development of new anti-angiogenic therapeutic agents with more efficacy and fewer side effects is still quite necessary. Conventional therapies saving the life of many cancer patients but due to drug resistance and lack of specificity utilizing these methods is faced with limits. Recently, new therapeutic agents have been developed and used to treat cancers such as scaffold proteins, monoclonal antibodies, tyrosine kinase inhibitors, and peptides. In antiangiogenic drug development, anti-angiogenic peptides design is a significant aim. Peptides have developed as substantial therapeutics that are being carefully investigated in angiogenesis-dependent diseases because of their high penetrating rate into the cancer cells, high specificity, and low toxicity. In this review, we focus on anti-angiogenic peptides in the field of cancer therapy that are designed, screened, or derived from nanobodies, mimotopes, phage displays, and natural resources. [ABSTRACT FROM AUTHOR]

Published
2021
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27. In Vivo Effect of RSH-12, a Novel Selective MMP-9 Inhibitor Peptide, in the Treatment of Experimentally Induced Dry Eye Model.

Author

Shoari, Alireza, Rasaee, Mohammad Javad, Rezaei Kanavi, Mozhgan, Afsar Aski, Sasha, and Tooyserkani, Raheleh

Subjects
*DRY eye syndromes, *MATRIX metalloproteinase inhibitors, *OCULAR toxicology
Abstract

To investigate the efficacy of RSH-12, a novel selective matrix metalloproteinase 9 (MMP-9) inhibitor peptide in rabbit models of dry eye syndrome (DES). In vitro toxicity of RSH-12 on cultured human corneal fibroblasts was investigated with MTT. Ocular toxicity of RSH-12 was investigated by clinical examinations, histology, and TUNEL assay. Experimental model of dry eye was induced by 1.0% atropine sulfate administration followed after 15 min by treatment with PBS, RSH-12, and Restasis in individual groups, three times a day for 7 days. In addition to performing Schirmer's test for evaluating basic tear secretion and tear break-up time test for investigating tear stability, the occurrence of superficial punctate keratopathy was also investigated in the study groups. MTT assay demonstrated that RSH-12 was not toxic to human corneal fibroblasts in different concentrations. During the administration of atropine, TBUT values and tear volume were decreased in vehicle group while these indices improved significantly in groups treated with RSH-12 in a promising manner. RSH-12 increased the mean value of tear volume from 4.85 to 10.75 mm (P =.0001) and mean of TBUT values from 20.3 s to 34.5 s (P =.0001) compared with the vehicle. In contrast to the presence of severe superficial punctate keratopathy in the controls, no significant dotted staining was observed in the RSH-12 and Restasis groups. These outcomes propose that RSH-12 has a therapeutic effect in the rabbit model of dry eye and might be a potential treatment for severe DES. [ABSTRACT FROM AUTHOR]

Published
2021
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28. Evaluation of G2 Citric Acid-Based Dendrimer as an Adjuvant in Veterinary Rabies Vaccine

Author

Asgary, Vahid, primary, Shoari, Alireza, additional, Afshar Moayad, Majid, additional, Shafiee Ardestani, Mehdi, additional, Bigdeli, Razieh, additional, Ghazizadeh, Leila, additional, Khosravy, Mohammad Sadeq, additional, Panahnejad, Erfan, additional, Janani, Alireza, additional, Bashar, Rouzbeh, additional, Abedi, Maliheh, additional, and Ahangari Cohan, Reza, additional

Published
2018
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29. Green synthesis and evaluation of silver nanoparticles as adjuvant in rabies veterinary vaccine

Author

Asgary,Vahid, Shoari,Alireza, Baghbani-Arani,Fahimeh, Shandiz,Seyed Attaollah Sadat, Khosravy,Mohammad Sadeq, Janani,Alireza, Bigdeli,Razieh, Bashar,Rouzbeh, Cohan,Reza, Asgary,Vahid, Shoari,Alireza, Baghbani-Arani,Fahimeh, Shandiz,Seyed Attaollah Sadat, Khosravy,Mohammad Sadeq, Janani,Alireza, Bigdeli,Razieh, Bashar,Rouzbeh, and Cohan,Reza

Abstract

Vahid Asgary,1,2 Alireza Shoari,1 Fahimeh Baghbani-Arani,3 Seyed Ataollah Sadat Shandiz,4 Mohammad Sadeq Khosravy,5 Alireza Janani,1 Razieh Bigdeli,6 Rouzbeh Bashar,1 Reza Ahangari Cohan1,7 1Virology Research Group, Department of Rabies, Pasteur Institute of Iran, 2Department of Immunology, School of Medicine, Tehran University of Medical Sciences, Tehran, 3Department of Genetics and Biotechnology, School of Biological Science, Varamin-Pishva Branch, Islamic Azad University, Varamin, 4Young Researchers and Elite Club, East Tehran Branch, Islamic Azad University, 5Department of Laboratory of Animal Sciences, Pasteur Institute of Iran, 6Department of Genetic, Science and Research Branch, Islamic Azad University, 7New Technologies Research Group, Department of Pilot Nanobiotechnology, Pasteur Institute of Iran, Tehran, Iran Background: Green synthesis of nanoparticles by plant extracts plays a significant role in different applications. Recently, several studies were conducted on the use of nanoparticles as adjuvant. The main aim of this study was to evaluate green synthesized silver nanoparticles (AgNPs) as adjuvant in rabies veterinary vaccine and compare the results with the existing commercially available alum adjuvant.Materials and methods: In the current study, AgNPs were prepared by the reduction of aqueous silver nitrate by leaf extract of Eucalyptus procera. The formation of AgNPs was confirmed by ultraviolet (UV)–visible spectrophotometer, scanning electron microscopy, dynamic light scattering, and X-ray diffraction analysis. Then, different amounts of AgNPs (200 µg, 400 µg, 600 µg, and 800 µg) were added to 1 mL of inactivated rabies virus. The loaded vaccines (0.5 mL) were injected intraperitoneally into six Naval Medical Research Institute mice in each group on days 1 and 7. On the 15th day, the mice were intracerebrally challenged with 0.03 mL

Published
2016

30. Computational and nonglycosylated systems: a simpler approach for development of nanosized PEGylated proteins

Author

Mirzaei,Hadi, Kazemi,Bahram, Bandehpour,Mojgan, Shoari,Alireza, Asgary,Vahid, Shafiee Ardestani,Mehdi, Madadkar-Sobhani,Armin, Cohan,Reza, Mirzaei,Hadi, Kazemi,Bahram, Bandehpour,Mojgan, Shoari,Alireza, Asgary,Vahid, Shafiee Ardestani,Mehdi, Madadkar-Sobhani,Armin, and Cohan,Reza

Abstract

Hadi Mirzaei,1 Bahram Kazemi,1 Mojgan Bandehpour,1 Alireza Shoari,2 Vahid Asgary,2 Mehdi Shafiee Ardestani,3 Armin Madadkar-Sobhani,4 Reza Ahangari Cohan2 1Department of Biotechnology, School of Medicine, Shahid Beheshti University of Medical Sciences, Tehran, Iran; 2Department of Pilot Nanobiotechnology, Pasteur Institute of Iran, Tehran, Iran; 3Department of Radiopharmacy, Pharmacy Faculty, Tehran University of Medical Sciences, Tehran, Iran; 4Faculty of Science, University of Ontario Institute of Technology, Oshawa, Canada Abstract: Cysteine PEGylation includes several steps, and is difficult to manage in practice. In the current investigation, the cysteine PEGylation of erythropoietin analogs was examined using computational and nonglycosylated systems to define a simpler approach for specific PEGylation. Two model analogs (E31C and E89C) were selected for PEGylation based on lowest structural deviation from the native form, accessibility, and nucleophilicity of the free thiol group. The selected analogs were cloned and the expression was assessed by sodium dodecyl sulfate–polyacrylamide gel electrophoresis and Western blot using Coomassie blue staining and anti-His monoclonal antibody, respectively. PEGylation with 20 kDa mPEG-maleimide resulted in 79% and 82% conjugation yield for E31C and E89C nonglycosylated erythropoietin (ngEPO) analogs, respectively. The size distribution and charge analysis showed an increase in size and negative charge of the PEGylated forms compared with nonconjugated ones. Biological assay revealed that E31C and E89C mutations and subsequent PEGylation of ngEPO analogs have no deleterious effects on in vitro biological activity when compared to CHO-derived recombinant human erythropoietin. In addition, PEG-conjugated ngEPOs showed a significant increase in plasma half-lives after injection into rats when compared to nonconjugated ones. The development of the cysteine-PEGylated proteins using nonglycosylated expression system

Published
2016

35. Emerging innovations in vincristine-encapsulated nanoparticles: Pioneering a new era in oncological therapeutics

Author

Bakhshi, Shohreh, Shoari, Alireza, Alibolandi, Parisa, Ganji, Mahmoud, Ghazy, Esraa, Rahdar, Abbas, Fathi-karkan, Sonia, and Pandey, Sadanand

Abstract

This encompassing review article synthesizes multiple studies and methods all revolving around the innovative use of nanoparticles (NPs) for Vincristine (VCR) delivery as a cancer treatment. The study presents a broad range of applications derived from several studies, such as NP delivery systems that trigger apoptosis, targeted drug delivery strategies for Ewing's sarcoma, therapy for brain gliomas, and potential uses for non-small cell lung carcinoma (NSCLC). Several studies highlight promising results, such as the reduction of tumors, enhanced survival rates, and lower cell survival rate in cancer cells. Moreover, diverse NPs' formulations each presenting varied encapsulation efficiencies and zeta potentials, yet maintaining a consistently small size are illustrated, reinforcing the versatility of NP utilization in this field. This paper overall provides a compelling overview of state-of-art NP usage in cancer therapeutics, serving as a foundation for further exploration and improved treatment strategies to combat diverse cancer types effectively.

Published
2023
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