Your search keyword '"Mo Baikoghli"' showing total 9 results

1. Development of 68Ga-Labeled Hepatitis E Virus Nanoparticles for Targeted Drug Delivery and Diagnostics with PET

Author

Elisavet Lambidis, Chun-Chieh Chen, Mo Baikoghli, Surachet Imlimthan, You Cheng Khng, Mirkka Sarparanta, R. Holland Cheng, Anu J. Airaksinen, University of Helsinki, Department of Chemistry, Tracers in Molecular Imaging (TRIM), and Doctoral Programme in Chemistry and Molecular Sciences

Subjects

positron emission tomography tracers, 116 Chemical sciences, Pharmaceutical Science, Gallium Radioisotopes, Bioengineering, virus-like particle, Hepatitis, Macromolecular and Materials Chemistry, hepatotropism, Mice, Dota, Hepatotropism, gallium-68, Drug Discovery, Hepatitis E virus, Animals, Nanotechnology, Tissue Distribution, Pharmacology & Pharmacy, Liver Disease, Gallium-68, Pharmacology and Pharmaceutical Sciences, Emerging Infectious Diseases, Infectious Diseases, Good Health and Well Being, DOTA, Positron-Emission Tomography, Positron emission tomography tracers, Molecular Medicine, Nanoparticles, Biomedical Imaging, hepatitis E viral nanoparticles, Virus-like particle, Digestive Diseases, Biotechnology

Abstract

Targeted delivery of diagnostics and therapeutics offers essential advantages over nontargeted systemic delivery. These include the reduction of toxicity, the ability to reach sites beyond biological barriers, and the delivery of higher cargo concentrations to diseased sites. Virus-like particles (VLPs) can efficiently be used for targeted delivery purposes. VLPs are derived from the coat proteins of viral capsids. They are self-assembled, biodegradable, and homogeneously distributed. In this study, hepatitis E virus (HEV) VLP derivatives, hepatitis E virus nanoparticles (HEVNPs), were radiolabeled with gallium-68, and consequently, the biodistribution of the labeled [Ga-68]Ga-DOTA-HEVNPs was studied in mice. The results indicated that [Ga-68]Ga-DOTA-HEVNPs can be considered as promising theranostic nanocarriers, especially for hepatocyte-targeting therapies.

Published

2022

2. Development of thermosensitive resiquimod-loaded liposomes for enhanced cancer immunotherapy

Author

Spencer K. Tumbale, R. Holland Cheng, Elizabeth S. Ingham, Wei-Lun Tang, Sarah M. Tam, Bo Wu, Alexander D. Borowsky, Katherine W. Ferrara, Mo Baikoghli, Marina Nura Raie, Brett Z. Fite, Josquin Foiret, Azadeh Kheirolomoom, Lisa M. Mahakian, Hua Zhang, and Kenneth Lau

Subjects

Hyperthermia, Agonist, Resiquimod, medicine.drug_class, medicine.medical_treatment, Biomedical Engineering, Pharmaceutical Science, 02 engineering and technology, alpha PD-1, Article, Mice, 03 medical and health sciences, chemistry.chemical_compound, Breast cancer, Cancer immunotherapy, Neoplasms, medicine, Animals, Pharmacology & Pharmacy, Receptor, Cancer, 030304 developmental biology, 0303 health sciences, Liposome, Chemistry, Induced, Imidazoles, Pharmacology and Pharmaceutical Sciences, Hyperthermia, Induced, Immunotherapy, Chemical Engineering, 021001 nanoscience & nanotechnology, medicine.disease, Liposomes, Cancer research, αPD-1, Thermosensitive liposomes, 0210 nano-technology, CD8

Abstract

Resiquimod (R848) is a toll-like receptor 7 and 8 (TLR7/8) agonist with potent antitumor and immunostimulatory activity. However, systemic delivery of R848 is poorly tolerated because of its poor solubility in water and systemic immune activation. In order to address these limitations, we developed an intravenously-injectable formulation with R848 using thermosensitive liposomes (TSLs) as a delivery vehicle. R848 was remotely loaded into TSLs composed of DPPC: DSPC: DSPE-PEG2K (85:10:5, mol%) with 100mM FeSO4 as the trapping agent inside. The final R848 to lipid ratio of the optimized R848-loaded TSLs (R848-TSLs) was 0.09 (w/w), 10-fold higher than the previously-reported values. R848-TSLs released 80% of R848 within 5min at 42°C. These TSLs were then combined with αPD-1, an immune checkpoint inhibitor, and ultrasound-mediated hyperthermia in a neu deletion (NDL) mouse mammary carcinoma model (Her2+, ER/PR negative). Combined with αPD-1, local injection of R848-TSLs showed superior efficacy with complete NDL tumor regression in both treated and abscopal sites achieved in 8 of 11 tumor bearing mice over 100days. Immunohistochemistry confirmed enhanced CD8+ T cell infiltration and accumulation by R848-TSLs. Systemic delivery of R848-TSLs, combined with local hyperthermia and αPD-1, inhibited tumor growth and extended median survival from 28days (non-treatment control) to 94days. Upon re-challenge with reinjection of tumor cells, none of the previously cured mice developed tumors, as compared with 100% of age-matched control mice. The dose of R848 (10μg for intra-tumoral injection or 6mg/kg for intravenous injection delivered up to 4 times) was well-tolerated without weight loss or organ hypertrophy. In summary, we developed R848-TSLs that can be administered locally or systematically, resulting in tumor regression and enhanced survival when combined with αPD-1 in mouse models of breast cancer.

Published

2021

3. Development of

Author

Elisavet, Lambidis, Chun-Chieh, Chen, Mo, Baikoghli, Surachet, Imlimthan, You Cheng, Khng, Mirkka, Sarparanta, R Holland, Cheng, and Anu J, Airaksinen

Subjects

Mice, Positron-Emission Tomography, Hepatitis E virus, Animals, Nanoparticles, Gallium Radioisotopes, Tissue Distribution

Abstract

Targeted delivery of diagnostics and therapeutics offers essential advantages over nontargeted systemic delivery. These include the reduction of toxicity, the ability to reach sites beyond biological barriers, and the delivery of higher cargo concentrations to diseased sites. Virus-like particles (VLPs) can efficiently be used for targeted delivery purposes. VLPs are derived from the coat proteins of viral capsids. They are self-assembled, biodegradable, and homogeneously distributed. In this study, hepatitis E virus (HEV) VLP derivatives, hepatitis E virus nanoparticles (HEVNPs), were radiolabeled with gallium-68, and consequently, the biodistribution of the labeled [

Published

2022

4. Positron emission tomography imaging of novel AAV capsids maps rapid brain accumulation

Author

Poorva Jain, Eduardo A. Silva, Spencer K. Tumbale, Michelle L. James, Ryan D. Leib, Katherine W. Ferrara, Mo Baikoghli, Jai Woong Seo, Tatyana Dobreva, Michael Chavez, Bo Wu, David J. Segal, Nick Goeden, R. Holland Cheng, Lisa M. Mahakian, Kratika Singhal, Nicholas C. Flytzanis, Shahin Shams, Xiaozhe Ding, Elizabeth S. Ingham, Sadaf Aghevlian, and Viviana Gradinaru

Subjects

0301 basic medicine, viruses, General Physics and Astronomy, Inbred C57BL, Transduction (genetics), chemistry.chemical_compound, Mice, 0302 clinical medicine, Viral tracing, Transduction, Genetic, lcsh:Science, Receptor, Inbred BALB C, Chelating Agents, Mice, Inbred BALB C, Multidisciplinary, medicine.diagnostic_test, Chemistry, Brain, Gene Therapy, Dependovirus, Capsid, Positron emission tomography, Neurological, Biomedical Imaging, Female, Science, Genetic Vectors, Molecular imaging, Bioengineering, Article, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Transduction, Genetic, Genetics, medicine, Animals, Humans, Reporter gene, HEK 293 cells, Neurosciences, General Chemistry, Pet imaging, Mice, Inbred C57BL, 030104 developmental biology, HEK293 Cells, Copper Radioisotopes, Positron-Emission Tomography, Biophysics, lcsh:Q, 030217 neurology & neurosurgery, DNA

Abstract

Adeno-associated viruses (AAVs) are typically single-stranded deoxyribonucleic acid (ssDNA) encapsulated within 25-nm protein capsids. Recently, tissue-specific AAV capsids (e.g. PHP.eB) have been shown to enhance brain delivery in rodents via the LY6A receptor on brain endothelial cells. Here, we create a non-invasive positron emission tomography (PET) methodology to track viruses. To provide the sensitivity required to track AAVs injected at picomolar levels, a unique multichelator construct labeled with a positron emitter (Cu-64, t1/2 = 12.7 h) is coupled to the viral capsid. We find that brain accumulation of the PHP.eB capsid 1) exceeds that reported in any previous PET study of brain uptake of targeted therapies and 2) is correlated with optical reporter gene transduction of the brain. The PHP.eB capsid brain endothelial receptor affinity is nearly 20-fold greater than that of AAV9. The results suggest that novel PET imaging techniques can be applied to inform and optimize capsid design., Adeno-associated viruses (AAVs) can be targeted in a tissue-specific manner, but their tissue accumulation cannot be assessed in a non-invasive manner. Here the authors conjugate a multivalent chelator labelled with Cu-64 to the surface of AAVs and image the brain accumulation of the PHB.eB capsid by PET.

Published

2020

5. Crystal structure of the FERM-folded talin head reveals the determinants for integrin binding

Author

Pingfeng, Zhang, Latifeh, Azizi, Sampo, Kukkurainen, Tong, Gao, Mo, Baikoghli, Marie-Claude, Jacquier, Yijuan, Sun, Juha A E, Määttä, R Holland, Cheng, Bernhard, Wehrle-Haller, Vesa P, Hytönen, Jinhua, Wu, Tampere University, BioMediTech, Department of Clinical Chemistry, and Clinical Medicine

Subjects

Models, Molecular, Talin, Protein Folding, animal structures, integrin, Amino Acid Motifs, Talin/chemistry/genetics/metabolism, macromolecular substances, environment and public health, Electron, Mice, Microscopy, Electron, Transmission, Protein Domains, Leucine, Models, Leucine/metabolism, Animals, Humans, Integrin beta3/chemistry/metabolism, Transmission, Polylysine, ddc:612, NPxY motif, Microscopy, Binding Sites, 318 Medical biotechnology, fungi, Integrin beta3, Molecular, cell adhesion, FERM domain, Biological Sciences, Biophysics and Computational Biology, Mutagenesis, embryonic structures, Polylysine/chemistry, biological phenomena, cell phenomena, and immunity

Abstract

Significance Although efforts have been made to determine the structure of talin and the way it interacts with integrins through the “head” domain, our work shows now that many of the previous mechanistic models based on the talin adapter are likely to be misleading as they are constructed on a crystal structure representing an improperly folded talin head domain. In this work, we identified the problem with the current talin head model and proposed a FERM-folded talin head. By analyzing these structural features of the FERM-folded talin head in a cellular context, involving also the kindlin adapter, we are making a critical and unprecedented contribution to the understanding and regulation of cell-matrix adhesions., Binding of the intracellular adapter proteins talin and its cofactor, kindlin, to the integrin receptors induces integrin activation and clustering. These processes are essential for cell adhesion, migration, and organ development. Although the talin head, the integrin-binding segment in talin, possesses a typical FERM-domain sequence, a truncated form has been crystallized in an unexpected, elongated form. This form, however, lacks a C-terminal fragment and possesses reduced β3-integrin binding. Here, we present a crystal structure of a full-length talin head in complex with the β3-integrin tail. The structure reveals a compact FERM-like conformation and a tightly associated N-P-L-Y motif of β3-integrin. A critical C-terminal poly-lysine motif mediates FERM interdomain contacts and assures the tight association with the β3-integrin cytoplasmic segment. Removal of the poly-lysine motif or disrupting the FERM-folded configuration of the talin head significantly impairs integrin activation and clustering. Therefore, structural characterization of the FERM-folded active talin head provides fundamental understanding of the regulatory mechanism of integrin function.

Published

2020

6. In situ T-cell transfection by anti-CD3-conjugated lipid nanoparticles leads to T-cell activation, migration, and phenotypic shift

Author

Azadeh Kheirolomoom, Aris J. Kare, Elizabeth S. Ingham, Ramasamy Paulmurugan, Elise R. Robinson, Mo Baikoghli, Mohammed Inayathullah, Jai W. Seo, James Wang, Brett Z. Fite, Bo Wu, Spencer K. Tumbale, Marina N. Raie, R. Holland Cheng, Lisa Nichols, Alexander D. Borowsky, and Katherine W. Ferrara

Subjects

mRNA, Messenger, Biomedical Engineering, Biophysics, Lipid nanoparticle, T-cell transfection, Bioengineering, Transfection, Lipids, Article, Reporter gene, Biomaterials, Mice, Phenotype, Mechanics of Materials, Liposomes, T-cell activation, Ceramics and Composites, Animals, RNA, Nanoparticles, Nanotechnology, RNA, Messenger, Cancer

Abstract

Ex vivo programming of T cells can be efficacious but is complex and expensive; therefore, the development of methods to transfect T cells in situ is important. We developed and optimized anti-CD3-targeted lipid nanoparticles (aCD3-LNPs) to deliver tightly packed, reporter gene mRNA specifically to T cells. In vitro, targeted LNPs efficiently delivered mCherry mRNA to Jurkat T cells, and T-cell activation and depletion were associated with aCD3 antibody coating on the surface of LNPs. aCD3-LNPs, but not non-targeted LNPs, accumulated within the spleen following systemic injection, with mCherry and Fluc signals visible within 30 minutes after injection. At 24 h after aCD3-LNP injection, 2-4% of all splenic T cells and 2-7% of all circulating T cells expressed mCherry, and this was dependent on aCD3 coating density. Targeting and transfection were accompanied by systemic CD25(+), OX40(+), and CD69(+) T-cell activation with temporary CD3e ligand loss and depletion of splenic and circulating subsets. Migration of splenic CD8a(+) T cells from the white-pulp to red-pulp, and differentiation from naïve to memory and effector phenotypes, followed upon aCD3-LNP delivery. Additionally, aCD3-LNP injection stimulated the secretion of myeloid-derived chemokines and T-helper cytokines into plasma. Lastly, we administered aCD3-LNPs to tumor bearing mice and found that transfected T cells localized within tumors and tumor-draining lymph nodes following immunotherapy treatment. In summary, we show that CD3-targeted transfection is feasible, yet associated with complex immunological consequences that must be further studied for potential therapeutic applications.

Published

2022

7. Tumor-specific delivery of gemcitabine with activatable liposomes

Author

Azadeh Kheirolomoom, Lisa M. Mahakian, Alexander D. Borowsky, Mo Baikoghli, Samantha Tucci, Josquin Foiret, Sarah M. Tam, Neil E. Hubbard, R. Holland Cheng, Katherine W. Ferrara, and Elizabeth S. Ingham

Subjects

Antimetabolites, Pharmaceutical Science, 02 engineering and technology, Inbred C57BL, Deoxycytidine, Pancreatic ductal adenocarcinoma, Mice, Drug Delivery Systems, Breast cancer, Pharmacology & Pharmacy, Cancer, 0303 health sciences, Liposome, Tumor, Chemistry, Temperature, Pharmacology and Pharmaceutical Sciences, Chemical Engineering, 021001 nanoscience & nanotechnology, Antineoplastic, Temperature-sensitive liposome, Toxicity, Female, 0210 nano-technology, medicine.drug, Hyperthermia, Antimetabolites, Antineoplastic, Biomedical Engineering, Breast Neoplasms, Bioengineering, Article, Cell Line, 03 medical and health sciences, Pancreatic Cancer, Rare Diseases, Pharmacokinetics, In vivo, Cell Line, Tumor, Pancreatic cancer, Ultrasound, medicine, Animals, Humans, 030304 developmental biology, Induced, Hyperthermia, Induced, medicine.disease, Gemcitabine, Mice, Inbred C57BL, Pancreatic Neoplasms, Drug Liberation, Apoptosis, Delayed-Action Preparations, Liposomes, Cancer research, Digestive Diseases

Abstract

Gemcitabine delivery to pancreatic ductal adenocarcinoma is limited by poor pharmacokinetics, dense fibrosis and hypo-vascularization. Activatable liposomes, with drug release resulting from local heating, enhance serum stability and circulation, and the released drug retains the ability to diffuse within the tumor. A limitation of liposomal gemcitabine has been the low loading efficiency. To address this limitation, we used the superior solubilizing potential of copper(II) gluconate to form a complex with gemcitabine at copper:gemcitabine (1:4). Thermosensitive liposomes composed of DPPC:DSPC:DSPE-PEG2k (80:15:5, mole%) then reached 12 weight % loading, 4-fold greater than previously reported values. Cryo transmission electron microscopy confirmed the presence of a liquid crystalline gemcitabine-copper mixture. The optimized gemcitabine liposomes released 60% and 80% of the gemcitabine within 1 and 5 min, respectively, at 42°C. Liposomal encapsulation resulted in a circulation half-life of ~2 h in vivo (compared to reported circulation of 16 min for free gemcitabine in mice), and free drug was not detected within the plasma. The resulting gemcitabine liposomes were efficacious against both murine breast cancer and pancreatic cancer in vitro. Three repeated treatments of activatable gemcitabine liposomes plus ultrasound hyperthermia regressed or eliminated tumors in the neu deletion model of murine breast cancer with limited toxicity, enhancing survival when compared to treatment with gemcitabine alone. With 5% of the free gemcitabine dose (5 rather than 100 mg/kg), tumor growth was suppressed to the same degree as gemcitabine. Additionally, in a more aggressive tumor model of murine pancreatic cancer, liposomal gemcitabine combined with local hyperthermia induced cell death and regions of apoptosis and necrosis.

Published

2019

8. Surface Functionalization of Hepatitis E Virus Nanoparticles Using Chemical Conjugation Methods

Author

Marie Stark, Mo Baikoghli, Chun Chieh Chen, and R. Holland Cheng

Subjects

0301 basic medicine, Insecta, chemical conjugation, General Chemical Engineering, Nanoparticle, Bioengineering, targeting ligand, Conjugated system, virus-like particles, General Biochemistry, Genetics and Molecular Biology, Hepatitis, law.invention, 03 medical and health sciences, Issue 135, law, Hepatitis E virus, Animals, Humans, Nanotechnology, Psychology, Cancer, Cysteine replacement, General Immunology and Microbiology, Chemistry, Liver Disease, General Neuroscience, Ligand (biochemistry), Small molecule, Combinatorial chemistry, multivalent ligand display, Good Health and Well Being, 030104 developmental biology, Recombinant DNA, Nanoparticles, Surface modification, hepatitis E, Cognitive Sciences, Biochemistry and Cell Biology, Nanocarriers, Digestive Diseases, Biotechnology, Cysteine

Abstract

Virus-like particles (VLPs) have been used as nanocarriers to display foreign epitopes and/or deliver small molecules in the detection and treatment of various diseases. This application relies on genetic modification, self-assembly, and cysteine conjugation to fulfill the tumor-targeting application of recombinant VLPs. Compared with genetic modification alone, chemical conjugation of foreign peptides to VLPs offers a significant advantage because it allows a variety of entities, such as synthetic peptides or oligosaccharides, to be conjugated to the surface of VLPs in a modulated and flexible manner without alteration of the VLP assembly. Here, we demonstrate how to use the hepatitis E virus nanoparticle (HEVNP), a modularized theranostic capsule, as a multifunctional delivery carrier. Functions of HEVNPs include tissue-targeting, imaging, and therapeutic delivery. Based on the well-established structural research of HEVNP, the structurally independent and surface-exposed residues were selected for cysteine replacement as conjugation sites for maleimide-linked chemical groups via thiol-selective linkages. One particular cysteine-modified HEVNP (a Cys replacement of the asparagine at 573 aa (HEVNP-573C)) was conjugated to a breast cancer cell-specific ligand, LXY30 and labeled with near-infrared (NIR) fluorescence dye (Cy5.5), rendering the tumor-targeted HEVNPs as effective diagnostic capsules (LXY30-HEVNP-Cy5.5). Similar engineering strategies can be employed with other macromolecular complexes with well-known atomic structures to explore potential applications in theranostic delivery.

Published

2018

9. Tissue targeted nanocapsids for oral insulin delivery via drink

Author

R. Holland Cheng, Mo Baikoghli, and Chun C Chen

Subjects

medicine.medical_treatment, Insulin delivery, Drinking, Administration, Oral, 030209 endocrinology & metabolism, 02 engineering and technology, Pharmacology, medicine.disease_cause, Patents as Topic, 03 medical and health sciences, Subcutaneous injection, 0302 clinical medicine, Drug Delivery Systems, Hepatitis E virus, Nanocapsules, Diabetes mellitus, medicine, Diabetes Mellitus, Ingestion, Animals, Humans, Hypoglycemic Agents, Insulin, business.industry, General Medicine, 021001 nanoscience & nanotechnology, medicine.disease, Hepatitis E, Drug delivery, Capsid Proteins, 0210 nano-technology, business

Abstract

For the past eight decades, subcutaneous injection has been the main route used for supplementing the suboptimal insulin secretion for administering insulin as a treatment for diabetes mellitus. Although this method is effective, subcutaneous injections are painful, inconvenient and carry a high risk of infections leading to poor patient compliance. The insulin-encapsulated hepatitis E virus nanoparticle, composed of the noninfectious hepatitis E viral capsid, is expected to deliver insulin from the GI tract to the liver after ingestion. Hepatitis E virus nanoparticle could be the answer to the long search of effective and efficient means to administer insulin orally and the most preferred route of drug delivery with highest patient compliance.

Published

2018