Your search keyword '"Iyer SV"' showing total 108 results

1. Immune regulatory adjuvant approach to mitigate subcutaneous immunogenicity of monoclonal antibodies.

Author

Jarvi NL, Patel M, Shetty KA, Nguyen NH, Grasperge BF, Mager DE, Straubinger RM, and Balu-Iyer SV

Subjects

Animals, Mice, Injections, Subcutaneous, Humans, Phosphatidylserines immunology, Female, Adalimumab immunology, Adalimumab administration & dosage, Rituximab immunology, Rituximab administration & dosage, Rituximab pharmacology, Trastuzumab immunology, Trastuzumab administration & dosage, T-Lymphocytes, Regulatory immunology, T-Lymphocytes, Regulatory drug effects, Dendritic Cells immunology, Adjuvants, Immunologic administration & dosage, Antibodies, Monoclonal immunology, Antibodies, Monoclonal administration & dosage

Abstract

Introduction: Immunogenicity continues to be a challenge for development and clinical utility of monoclonal antibodies, and there are gaps in our current ability to prevent anti-drug antibody development in a safe and antigen-specific manner., Methods: To mitigate immunogenicity of monoclonal antibodies administered subcutaneously, O-phospho-L-serine (OPLS)-the head group of the tolerance-inducing phospholipid, phosphatidylserine-was investigated as an immunoregulatory adjuvant., Results: Formulations of adalimumab, trastuzumab or rituximab with OPLS showed reduction in relative immunogenicity in mice compared to vehicle formulations, indicated by reduced anti-drug antibody development and significant reductions in CD138+ plasma cell differentiation in bone marrow. Titer development toward recombinant human hyaluronidase, a dispersion enhancer that was co-formulated with monoclonal antibodies, was similarly reduced. Subcutaneous administration of adalimumab with OPLS resulted in a two-fold increase in expression of type 1 regulatory (Tr1) T cell subset in the spleen. This is consistent with in vitro studies where co-culturing of dendritic cells primed with ovalbumin in the presence and absence of OPLS and antigen specific T-cells induced expression of Tr1 phenotype on live CD4+ T cells., Conclusion: This adjuvant does not impact immune competence of non-human primates and mice, and repeated administration of the adjuvant does not show renal or hepatic toxicity. Formulation of monoclonal antibodies with the immunoregulatory adjuvant, OPLS, was found to be safe and effective at mitigating immunogenicity., Competing Interests: Author NN was employed by the company Truvai Biosciences, LLC. Author DM was employed by the company Enhanced Pharmacodynamics, LLC. Authors SB, DM, and RS have financial interest in Truvai Biosciences, LLC. SB and KS are inventors on a patent for use of OPLS as an immunomodifier. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be constructed as a potential conflict of interest. The authors declare that this study received funding from Truvai Biosciences, LLC. The funder had the following involvement in the study: study design., (Copyright © 2024 Jarvi, Patel, Shetty, Nguyen, Grasperge, Mager, Straubinger and Balu-Iyer.)

Published

2024

2. Gliocidin is a nicotinamide-mimetic prodrug that targets glioblastoma.

Author

Chen YJ, Iyer SV, Hsieh DC, Li B, Elias HK, Wang T, Li J, Ganbold M, Lien MC, Peng YC, Xie XP, Jayewickreme CD, van den Brink MRM, Brady SF, Lim SK, and Parada LF

Subjects

Animals, Humans, Mice, Cell Line, Tumor, IMP Dehydrogenase metabolism, IMP Dehydrogenase antagonists & inhibitors, IMP Dehydrogenase chemistry, Nicotinamide-Nucleotide Adenylyltransferase metabolism, Nicotinamide-Nucleotide Adenylyltransferase chemistry, Nicotinamide-Nucleotide Adenylyltransferase antagonists & inhibitors, Female, NAD metabolism, Blood-Brain Barrier metabolism, Cryoelectron Microscopy, Niacinamide analogs & derivatives, Niacinamide pharmacology, Niacinamide chemistry, Male, Models, Molecular, Brain Neoplasms drug therapy, Brain Neoplasms pathology, Brain Neoplasms metabolism, Glioblastoma drug therapy, Glioblastoma pathology, Glioblastoma metabolism, Prodrugs pharmacology, Prodrugs chemistry, Prodrugs metabolism, Xenograft Model Antitumor Assays, Temozolomide pharmacology, Temozolomide chemistry

Abstract

Glioblastoma is incurable and in urgent need of improved therapeutics 1 . Here we identify a small compound, gliocidin, that kills glioblastoma cells while sparing non-tumour replicative cells. Gliocidin activity targets a de novo purine synthesis vulnerability in glioblastoma through indirect inhibition of inosine monophosphate dehydrogenase 2 (IMPDH2). IMPDH2 blockade reduces intracellular guanine nucleotide levels, causing nucleotide imbalance, replication stress and tumour cell death 2 . Gliocidin is a prodrug that is anabolized into its tumoricidal metabolite, gliocidin-adenine dinucleotide (GAD), by the enzyme nicotinamide nucleotide adenylyltransferase 1 (NMNAT1) of the NAD + salvage pathway. The cryo-electron microscopy structure of GAD together with IMPDH2 demonstrates its entry, deformation and blockade of the NAD + pocket 3 . In vivo, gliocidin penetrates the blood-brain barrier and extends the survival of mice with orthotopic glioblastoma. The DNA alkylating agent temozolomide induces Nmnat1 expression, causing synergistic tumour cell killing and additional survival benefit in orthotopic patient-derived xenograft models. This study brings gliocidin to light as a prodrug with the potential to improve the survival of patients with glioblastoma., Competing Interests: Competing interests: The authors declare no competing interests., (© 2024. The Author(s), under exclusive licence to Springer Nature Limited.)

Published

2024

3. Immunogenicity risk assessment of empty capsids present in adeno-associated viral vectors using predictive innate immune responses.

Author

Jarvi N, Hofman K, Venkatesh A, Gorecki E, and Balu-Iyer SV

Subjects

Animals, Humans, Mice, Risk Assessment methods, Mice, Inbred C57BL, Cytokines metabolism, Genetic Therapy methods, Capsid Proteins immunology, Capsid Proteins genetics, Dependovirus genetics, Dependovirus immunology, Immunity, Innate immunology, Capsid immunology, Killer Cells, Natural immunology, Genetic Vectors, Dendritic Cells immunology

Abstract

Immunogenicity of gene therapy and the impacts on safety and efficacy are of increasing interest in the pharmaceutical industry. Unique structural aspects of gene therapy delivery vectors, such as adeno-associated viral (AAV) vectors, are expected to activate the innate immune system. The risk of innate immune activation is critical to understand due to the potential impacts on safety and on subsequent adaptive immune responses. In this study, we investigated the responses of key innate immune players-dendritic cells, natural killer (NK) cells, and the complement system-to AAV8 capsids. Immunogenicity risk was also predicted in the presence empty AAV capsids for AAV gene therapy. Compared to genome-containing "full" AAV8 capsids, empty AAV8 capsids more strongly induced proinflammatory cytokine production and migration by human and mouse dendritic cells, but the "full" capsid increased expression of co-stimulatory markers. Furthermore, in an NK cell degranulation assay, we found mixtures of empty and full AAV8 capsids to activate expression of TNF-α, IFN-γ, and CD107a more strongly in multiple NK cell populations compared to either capsid type alone. Serum complement C3a was also induced more strongly in the presence of mixed empty and full AAV8 capsid formulations. Risk for innate immune activation suggests the importance to determine acceptable limits of empty capsids. Immunogenicity risk assessment of novel biological modalities will benefit from the aforementioned in vitro innate immune activation assays providing valuable mechanistic information., Competing Interests: Declaration of competing interest The author is an Editor for Journal of Phamaceutical Sciences and was not involved in the editorial review or the decision to publish this article. The authors declare the following financial interests/personal relationships which may be considered as potential competing interests., (Copyright © 2024 American Pharmacists Association. Published by Elsevier Inc. All rights reserved.)

Published

2024

4. Leveraging the power of long reads for targeted sequencing.

Author

Iyer SV, Goodwin S, and McCombie WR

Subjects

Humans, Genomics methods, Genome, Human, Animals, High-Throughput Nucleotide Sequencing methods, Sequence Analysis, DNA methods

Abstract

Long-read sequencing technologies have improved the contiguity and, as a result, the quality of genome assemblies by generating reads long enough to span and resolve complex or repetitive regions of the genome. Several groups have shown the power of long reads in detecting thousands of genomic and epigenomic features that were previously missed by short-read sequencing approaches. While these studies demonstrate how long reads can help resolve repetitive and complex regions of the genome, they also highlight the throughput and coverage requirements needed to accurately resolve variant alleles across large populations using these platforms. At the time of this review, whole-genome long-read sequencing is more expensive than short-read sequencing on the highest throughput short-read instruments; thus, achieving sufficient coverage to detect low-frequency variants (such as somatic variation) in heterogenous samples remains challenging. Targeted sequencing, on the other hand, provides the depth necessary to detect these low-frequency variants in heterogeneous populations. Here, we review currently used and recently developed targeted sequencing strategies that leverage existing long-read technologies to increase the resolution with which we can look at nucleic acids in a variety of biological contexts., (© 2024 Iyer et al.; Published by Cold Spring Harbor Laboratory Press.)

Published

2024

5. A mechanistic marker-based screening tool to predict clinical immunogenicity of biologics.

Author

Jarvi NL and Balu-Iyer SV

Abstract

Background: The efficacy and safety of therapeutic proteins are undermined by immunogenicity driven by anti-drug antibodies. Immunogenicity risk assessment is critically necessary during drug development, but current methods lack predictive power and mechanistic insight into antigen uptake and processing leading to immune response. A key mechanistic step in T-cell-dependent immune responses is the migration of mature dendritic cells to T-cell areas of lymphoid compartments, and this phenomenon is most pronounced in the immune response toward subcutaneously delivered proteins., Methods: The migratory potential of monocyte-derived dendritic cells is proposed to be a mechanistic marker for immunogenicity screening. Following exposure to therapeutic protein in vitro, dendritic cells are analyzed for changes in activation markers (CD40 and IL-12) in combination with levels of the chemokine receptor CXCR4 to represent migratory potential. Then a transwell assay captures the intensity of dendritic cell migration in the presence of a gradient of therapeutic protein and chemokine ligands., Results: Here, we show that an increased ability of the therapeutic protein to induce dendritic cell migration along a gradient of chemokine CCL21 and CXCL12 predicts higher immunogenic potential. Expression of the chemokine receptor CXCR4 on human monocyte-derived dendritic cells, in combination with activation markers CD40 and IL-12, strongly correlates with clinical anti-drug antibody incidence., Conclusions: Mechanistic understanding of processes driving immunogenicity led to the development of a predictive tool for immunogenicity risk assessment of therapeutic proteins. These predictive markers could be adapted for immunogenicity screening of other biological modalities., (© 2023. The Author(s).)

Published

2023

6. Immunogenicity of Therapeutic Biological Modalities - Lessons from Hemophilia A Therapies.

Author

Nguyen NH, Jarvi NL, and Balu-Iyer SV

Subjects

Humans, Factor VIII, Recombinant Proteins, Treatment Outcome, Hemophilia A therapy, Antibodies, Bispecific therapeutic use

Abstract

The introduction and development of biologics such as therapeutic proteins, gene-, and cell-based therapy have revolutionized the scope of treatment for many diseases. However, a significant portion of the patients develop unwanted immune reactions against these novel biological modalities, referred to as immunogenicity, and no longer benefit from the treatments. In the current review, using Hemophilia A (HA) therapy as an example, we will discuss the immunogenicity issue of multiple biological modalities. Currently, the number of therapeutic modalities that are approved or recently explored to treat HA, a hereditary bleeding disorder, is increasing rapidly. These include, but are not limited to, recombinant factor VIII proteins, PEGylated FVIII, FVIII Fc fusion protein, bispecific monoclonal antibodies, gene replacement therapy, gene editing therapy, and cell-based therapy. They offer the patients a broader range of more advanced and effective treatment options, yet immunogenicity remains the most critical complication in the management of this disorder. Recent advances in strategies to manage and mitigate immunogenicity will also be reviewed., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2023 American Pharmacists Association. Published by Elsevier Inc. All rights reserved.)

Published

2023

7. Phosphatidylserine-mediated oral tolerance.

Author

Nguyen NH, Chak V, Keller K, Wu H, and Balu-Iyer SV

Subjects

Antigen-Presenting Cells, Autoantigens, Immune Tolerance, Apoptosis, Phosphatidylserines, Immunotherapy

Abstract

Phosphatidylserine (PS) is an anionic phospholipid exposed on the surface of apoptotic cells. The exposure of PS typically recruits and signals phagocytes to engulf and silently clear these dying cells to maintain tolerance via immunological ignorance. However, recent and emerging evidence has demonstrated that PS converts an "immunogen" into a "tolerogen", and PS exposure on the surface of cells or vesicles actively promotes a tolerogenic environment. This tolerogenic property depends on the biophysical characteristics of PS-containing vesicles, including PS density on the particle surface to effectively engage tolerogenic receptors, such as TIM-4, which is exclusively expressed on the surface of antigen-presenting cells. We harnessed the cellular and molecular mechanistic insight of PS-mediated immune regulation to design an effective oral tolerance approach. This immunotherapy has been shown to prevent/reduce immune response against life-saving protein-based therapies, food allergens, autoantigens, and the antigenic viral capsid peptide commonly used in gene therapy, suggesting a broad spectrum of potential clinical applications. Given the good safety profile of PS together with the ease of administration, oral tolerance achieved with PS-based nanoparticles has a very promising therapeutic impact., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2022 Elsevier Inc. All rights reserved.)

Published

2023

8. Effectiveness of training primary care internal medicine residents in etonogestrel implants and impact on their future practice: A cross-sectional study.

Author

Holaday LW, Gover M, Iyer SV, DeLuca JP, Stella J, Gold M, and Goss E

Subjects

Clinical Competence, Cross-Sectional Studies, Curriculum, Desogestrel, Humans, Primary Health Care, Internship and Residency

Abstract

Objective: To evaluate the impact of an etonogestrel implant training program within a primary care Internal Medicine residency training program., Study Design: We surveyed graduates of our primary care Internal Medicine residency program in the Bronx, New York who performed implant procedures though the first 32 months after implementation of a monthly faculty-supervised resident implant clinic. We assessed the number of implants placed and removed per graduate, and surveyed graduates' satisfaction with the implant training program, perceived competence with implant procedures, and intent and ability to perform implant procedures and barriers to performing implant procedures postgraduation., Results: Between July 2017 and February 2020, 14 residents placed a total of 34 devices and removed four. All 14 program graduates completed the survey in August 2020. All but one respondent felt this training was valuable and 11 felt competent placing implants without supervision. Although 10 planned to provide implants following graduation, none have been able to, largely because of credentialing and clinic-practice level barriers., Conclusions: The primary care Internal Medicine program graduates we surveyed (n = 14) valued our etonogestrel implant training program and perceived competence, particularly with implant placement. However, even those who intended to provide etonogestrel implants postgraduation were unable to do so., Implications: Internal Medicine residents trained to place and remove etonogestrel implants are most comfortable with implant placement. However, these physicians may face barriers related to credentialing and ambulatory practice scope when attempting to provide this care in clinical practice., (Copyright © 2022. Published by Elsevier Inc.)

Published

2022

9. Biophysical Characterization of Tolerogenic Lipid-Based Nanoparticles Containing Phosphatidylcholine and Lysophosphatidylserine.

Author

Nguyen NH, Chen M, Chak V, and Balu-Iyer SV

Subjects

Lecithins, Lysophospholipids chemistry, Lysophospholipids pharmacology, Organic Chemicals, Phosphatidylserines, Nanoparticles, Phosphatidylcholines chemistry

Abstract

Autoimmune conditions, allergies, and immunogenicity against therapeutic proteins are initiated by the unwanted immune response against self and non-self proteins. The development of tolerance induction approaches can offer an effective treatment modality for these clinical conditions. We recently showed that oral administration of lipidic nanoparticles containing phosphatidylcholine (PC) and lysophosphatidylserine (Lyso-PS) converted an immunogen to a tolerogen and induced immunological tolerance towards several antigens. While the biophysical properties such as lamellar characteristics of this binary lipid system are critical for stability, therapeutic delivery, and mechanism of tolerance induction, such information has not been thoroughly investigated. In the current study, we evaluated the lamellar phase properties of PC/Lyso-PS system using orthogonal biophysical methods such as fluorescence (steady-state, anisotropy, PSvue, and Laurdan), dynamic light scattering, and differential scanning calorimetry. The results showed that Lyso-PS partitioned into the PC bilayers and led to changes in the particles' lamellar phase properties, lipid-packing, and lipid-water dynamics. Additionally, the biophysical characteristics of PC/Lyso-PS system are different from the well-studied PC/double-chain phosphatidylserine (PS) system. Notably, the incorporation of Lyso-PS significantly reduced the hydrodynamic diameter of PC particles. Results from the in vivo uptake study and intestinal loop assay utilizing flow cytometry analysis also indicated that the uptake of Lyso-PS-containing nanoparticles by immune cells in the gut and Peyer's patches is significantly higher than that of double-chain PS due to the differential transport through microfold cells. It was also found that the acyl chain mismatch between PC and Lyso-PS is critical for the miscibility and particle stability. Collectively, the results suggest that these biophysical characteristics likely influence the in vivo behaviors and contribute to the oral tolerance property of PC/Lyso-PS system., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper. The authors declare that they have no conflict of interest., (Copyright © 2022 American Pharmacists Association. Published by Elsevier Inc. All rights reserved.)

Published

2022

10. SLC5A3-Dependent Myo-inositol Auxotrophy in Acute Myeloid Leukemia.

Author

Wei Y, Huang YH, Skopelitis DS, Iyer SV, Costa ASH, Yang Z, Kramer M, Adelman ER, Klingbeil O, Demerdash OE, Polyanskaya SA, Chang K, Goodwin S, Hodges E, McCombie WR, Figueroa ME, and Vakoc CR

Subjects

Animals, Developmental Biology, Humans, Mice, Heat-Shock Proteins genetics, Inositol biosynthesis, Leukemia, Myeloid, Acute drug therapy, Symporters genetics

Abstract

An enhanced requirement for nutrients is a hallmark property of cancer cells. Here, we optimized an in vivo genetic screening strategy in acute myeloid leukemia (AML), which led to the identification of the myo-inositol transporter SLC5A3 as a dependency in this disease. We demonstrate that SLC5A3 is essential to support a myo-inositol auxotrophy in AML. The commonality among SLC5A3-dependent AML lines is the transcriptional silencing of ISYNA1 , which encodes the rate-limiting enzyme for myo-inositol biosynthesis, inositol-3-phosphate synthase 1. We use gain- and loss-of-function experiments to reveal a synthetic lethal genetic interaction between ISYNA1 and SLC5A3 in AML, which function redundantly to sustain intracellular myo-inositol. Transcriptional silencing and DNA hypermethylation of ISYNA1 occur in a recurrent manner in human AML patient samples, in association with IDH1/IDH2 and CEBPA mutations. Our findings reveal myo-inositol as a nutrient dependency in AML caused by the aberrant silencing of a biosynthetic enzyme. SIGNIFICANCE: We show how epigenetic silencing can provoke a nutrient dependency in AML by exploiting a synthetic lethality relationship between biosynthesis and transport of myo-inositol. Blocking the function of this solute carrier may have therapeutic potential in an epigenetically defined subset of AML. This article is highlighted in the In This Issue feature, p. 275 ., (©2021 The Authors; Published by the American Association for Cancer Research.)

Published

2022

11. PHI-base in 2022: a multi-species phenotype database for Pathogen-Host Interactions.

Author

Urban M, Cuzick A, Seager J, Wood V, Rutherford K, Venkatesh SY, Sahu J, Iyer SV, Khamari L, De Silva N, Martinez MC, Pedro H, Yates AD, and Hammond-Kosack KE

Subjects

Animals, Apicomplexa classification, Apicomplexa genetics, Apicomplexa pathogenicity, Bacteria classification, Bacteria genetics, Bacteria pathogenicity, Diplomonadida classification, Diplomonadida genetics, Diplomonadida pathogenicity, Fungi classification, Fungi genetics, Fungi pathogenicity, Insecta classification, Insecta genetics, Insecta pathogenicity, Internet, Nematoda classification, Nematoda genetics, Nematoda pathogenicity, Phylogeny, Plants microbiology, Plants parasitology, Virulence, Databases, Factual, Host-Pathogen Interactions genetics, Phenotype, User-Computer Interface

Abstract

Since 2005, the Pathogen-Host Interactions Database (PHI-base) has manually curated experimentally verified pathogenicity, virulence and effector genes from fungal, bacterial and protist pathogens, which infect animal, plant, fish, insect and/or fungal hosts. PHI-base (www.phi-base.org) is devoted to the identification and presentation of phenotype information on pathogenicity and effector genes and their host interactions. Specific gene alterations that did not alter the in host interaction phenotype are also presented. PHI-base is invaluable for comparative analyses and for the discovery of candidate targets in medically and agronomically important species for intervention. Version 4.12 (September 2021) contains 4387 references, and provides information on 8411 genes from 279 pathogens, tested on 228 hosts in 18, 190 interactions. This provides a 24% increase in gene content since Version 4.8 (September 2019). Bacterial and fungal pathogens represent the majority of the interaction data, with a 54:46 split of entries, whilst protists, protozoa, nematodes and insects represent 3.6% of entries. Host species consist of approximately 54% plants and 46% others of medical, veterinary and/or environmental importance. PHI-base data is disseminated to UniProtKB, FungiDB and Ensembl Genomes. PHI-base will migrate to a new gene-centric version (version 5.0) in early 2022. This major development is briefly described., (© The Author(s) 2021. Published by Oxford University Press on behalf of Nucleic Acids Research.)

Published

2022

12. Tolerogenic form of Factor VIII to prevent inhibitor development in the treatment of Hemophilia A.

Author

Nguyen NH, Dingman RK, and Balu-Iyer SV

Subjects

Animals, Antibodies, Factor VIII, Humans, Mice, Hemophilia A drug therapy, Hemostatics, Nanoparticles

Abstract

Background: The development of antidrug antibodies, also termed inhibitors, against administered factor VIII (FVIII) is one of the major complications in the clinical management of hemophilia A. Once formed, these inhibitory antibodies abrogate the activity of FVIII, resulting in loss of hemostatic efficacy and patients are subjected to increased risk of bleeding tendencies. Current treatment options after inhibitor development are expensive and ineffective in some cases. Therefore, treatment strategies that can prevent inhibitor formation is an effective approach in the management of hemophilia A., Objectives: We aimed to evaluate and discuss the use of a tolerogenic form of FVIII as an immunotherapy strategy to prevent inhibitor risk., Methods: FVIII was associated with nanoparticles containing lysophosphatidylserine (Lyso-PS) and administered to hemophilia A mice via intravenous route. These animals then received weekly rechallenge injections with free FVIII, and plasma was collected at the end of the study to evaluate for inhibitor development. To investigate whether Lyso-PS nanoparticles influence the plasma survival of FVIII, a pharmacokinetic study following a single intravenous administration of FVIII in the presence and absence of Lyso-PS nanoparticles was performed. For dosing convenience, the tolerogenic effect of Lyso-PS nanoparticles following oral administration was also examined., Results and Conclusions: The results demonstrated that FVIII associated with Lyso-PS nanoparticles significantly reduced inhibitor development while improving plasma survival of FVIII following intravenous administration, suggesting a multifunctional FVIII form to improve clinical utility. Additionally, reduction in inhibitor formation can also be achieved using Lyso-PS nanoparticles through the user-friendly oral route of administration., (© 2021 International Society on Thrombosis and Haemostasis.)

Published

2021

13. Pharmaceutical Aspects and Clinical Evaluation of COVID-19 Vaccines.

Author

Hofman K, Shenoy GN, Chak V, and Balu-Iyer SV

Subjects

Antibodies, Neutralizing immunology, Clinical Trials as Topic, Humans, Pandemics prevention & control, SARS-CoV-2 immunology, COVID-19 immunology, COVID-19 Vaccines immunology

Abstract

COVID-19, the disease caused by the novel severe acute respiratory syndrome-associated coronavirus 2 (SARS-CoV-2), was first detected in December 2019 and has since morphed into a global pandemic claiming over 2.4 million human lives and severely impacting global economy. The race for a safe and efficacious vaccine was thus initiated with government agencies as well as major pharmaceutical companies as frontrunners. An ideal vaccine would activate multiple arms of the adaptive immune system to generate cytotoxic T cell responses as well as neutralizing antibody responses, while avoiding pathological or deleterious immune responses that result in tissue damage or exacerbation of the disease. Developing an effective vaccine requires an inter-disciplinary effort involving virology, protein biology, biotechnology, immunology and pharmaceutical sciences. In this review, we provide a brief overview of the pathology and immune responses to SARS-CoV-2, which are fundamental to vaccine development. We then summarize the rationale for developing COVID-19 vaccines and provide novel insights into vaccine development from a pharmaceutical science perspective, such as selection of different antigens, adjuvants, delivery platforms and formulations. Finally, we review multiple clinical trial outcomes of novel vaccines in terms of safety and efficacy.

Published

2021

14. Novel phosphatidylserine-binding molecule enhances antitumor T-cell responses by targeting immunosuppressive exosomes in human tumor microenvironments.

Author

Bhatta M, Shenoy GN, Loyall JL, Gray BD, Bapardekar M, Conway A, Minderman H, Kelleher RJ Jr, Carreno BM, Linette G, Shultz LD, Odunsi K, Balu-Iyer SV, Pak KY, and Bankert RB

Subjects

Animals, Cell Line, Tumor, Female, Humans, Mice, Mice, Inbred NOD, Ovarian Neoplasms pathology, Tumor Microenvironment, Exosomes metabolism, Neoplasms immunology, Ovarian Neoplasms genetics, Phosphatidylserines metabolism, T-Lymphocytes metabolism

Abstract

Background: The human tumor microenvironment (TME) is a complex and dynamic milieu of diverse acellular and cellular components, creating an immunosuppressive environment, which contributes to tumor progression. We have previously shown that phosphatidylserine (PS) expressed on the surface of exosomes isolated from human TMEs is causally linked to T-cell immunosuppression, representing a potential immunotherapeutic target. In this study, we investigated the effect of ExoBlock, a novel PS-binding molecule, on T-cell responses in the TME., Methods: We designed and synthesized a new compound, (ZnDPA) 6 -DP-15K, a multivalent PS binder named ExoBlock. The PS-binding avidity of ExoBlock was tested using an in vitro competition assay. The ability of this molecule to reverse exosome-mediated immunosuppression in vitro was tested using human T-cell activation assays. The in vivo therapeutic efficacy of ExoBlock was then tested in two different human tumor xenograft models, the melanoma-based xenomimetic (X-)mouse model, and the ovarian tumor-based omental tumor xenograft (OTX) model., Results: ExoBlock was able to bind PS with high avidity and was found to consistently and significantly block the immunosuppressive activity of human ovarian tumor and melanoma-associated exosomes in vitro. ExoBlock was also able to significantly enhance T cell-mediated tumor suppression in vivo in both the X-mouse and the OTX model. In the X-mouse model, ExoBlock suppressed tumor recurrence in a T cell-dependent manner. In the OTX model, ExoBlock treatment resulted in an increase in the number as well as function of CD4 and CD8 T cells in the TME, which was associated with a reduction in tumor burden and metastasis, as well as in the number of circulating PS+ exosomes in tumor-bearing mice., Conclusion: Our results establish that targeting exosomal PS in TMEs with ExoBlock represents a promising strategy to enhance antitumor T-cell responses., Competing Interests: Competing interests: The corresponding author, RB, is an officer and founder of Immune Modulatory Therapies LLC. A patent is currently pending for ExoBlock., (© Author(s) (or their employer(s)) 2021. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.)

Published

2021

15. Rational design of a nanoparticle platform for oral prophylactic immunotherapy to prevent immunogenicity of therapeutic proteins.

Author

Nguyen NH, Glassman FY, Dingman RK, Shenoy GN, Wohlfert EA, Kay JG, Bankert RB, and Balu-Iyer SV

Subjects

Animals, Mice, Immunotherapy, Nanoparticles

Abstract

The safety and efficacy of several life-saving therapeutic proteins are compromised due to their immunogenicity. Once a sustained immune response against a protein-based therapy is established, clinical options that are safe and cost-effective become limited. Prevention of immunogenicity of therapeutic proteins prior to their initial use is critical as it is often difficult to reverse an established immune response. Here, we discuss a rational design and testing of a phosphatidylserine-containing nanoparticle platform for novel oral prophylactic reverse vaccination approach, i.e., pre-treatment of a therapeutic protein in the presence of nanoparticles to prevent immunogenicity of protein therapies., (© 2021. The Author(s).)

Published

2021

16. Transcriptional Silencing of ALDH2 Confers a Dependency on Fanconi Anemia Proteins in Acute Myeloid Leukemia.

Author

Yang Z, Wu XS, Wei Y, Polyanskaya SA, Iyer SV, Jung M, Lach FP, Adelman ER, Klingbeil O, Milazzo JP, Kramer M, Demerdash OE, Chang K, Goodwin S, Hodges E, McCombie WR, Figueroa ME, Smogorzewska A, and Vakoc CR

Subjects

Cell Line, Tumor, Humans, Ubiquitination, Aldehyde Dehydrogenase, Mitochondrial genetics, Fanconi Anemia Complementation Group Proteins metabolism, Leukemia, Myeloid, Acute genetics

Abstract

Hundreds of genes become aberrantly silenced in acute myeloid leukemia (AML), with most of these epigenetic changes being of unknown functional consequence. Here, we demonstrate how gene silencing can lead to an acquired dependency on the DNA repair machinery in AML. We make this observation by profiling the essentiality of the ubiquitination machinery in cancer cell lines using domain-focused CRISPR screening, which revealed Fanconi anemia (FA) proteins UBE2T and FANCL as unique dependencies in AML. We demonstrate that these dependencies are due to a synthetic lethal interaction between FA proteins and aldehyde dehydrogenase 2 (ALDH2), which function in parallel pathways to counteract the genotoxicity of endogenous aldehydes. We show DNA hypermethylation and silencing of ALDH2 occur in a recurrent manner in human AML, which is sufficient to confer FA pathway dependency. Our study suggests that targeting of the ubiquitination reaction catalyzed by FA proteins can eliminate ALDH2-deficient AML. SIGNIFICANCE: Aberrant gene silencing is an epigenetic hallmark of human cancer, but the functional consequences of this process are largely unknown. In this study, we show how an epigenetic alteration leads to an actionable dependency on a DNA repair pathway through the disabling of genetic redundancy. This article is highlighted in the In This Issue feature, p. 2113 ., (©2021 American Association for Cancer Research.)

Published

2021

17. Stem-like cells drive NF1-associated MPNST functional heterogeneity and tumor progression.

Author

Sun D, Xie XP, Zhang X, Wang Z, Sait SF, Iyer SV, Chen YJ, Brown R, Laks DR, Chipman ME, Shern JF, and Parada LF

Subjects

Animals, Disease Models, Animal, Mice, Neoplasm Recurrence, Local, Neurofibromatosis 1 genetics, Neurofibrosarcoma

Abstract

NF1-associated malignant peripheral nerve sheath tumors (MPNSTs) are the major cause of mortality in neurofibromatosis. MPNSTs arise from benign peripheral nerve plexiform neurofibromas that originate in the embryonic neural crest cell lineage. Using reporter transgenes that label early neural crest lineage cells in multiple NF1 MPNST mouse models, we discover and characterize a rare MPNST cell population with stem-cell-like properties, including quiescence, that is essential for tumor initiation and relapse. Following isolation of these cells, we derive a cancer-stem-cell-specific gene expression signature that includes consensus embryonic neural crest genes and identify Nestin as a marker for the MPNST cell of origin. Combined targeting of cancer stem cells along with antimitotic chemotherapy yields effective tumor inhibition and prolongs survival. Enrichment of the cancer stem cell signature in cognate human tumors supports the generality and relevance of cancer stem cells to MPNST therapy development., Competing Interests: Declaration of interests The authors declare no competing interests, (Copyright © 2021 Elsevier Inc. All rights reserved.)

Published

2021

18. Immunogenicity Challenges Associated with Subcutaneous Delivery of Therapeutic Proteins.

Author

Jarvi NL and Balu-Iyer SV

Subjects

Administration, Intravenous, Antigens, Humans, Injections, Subcutaneous, Antibodies, Monoclonal, Antigen-Presenting Cells

Abstract

The subcutaneous route of administration has provided convenient and non-inferior delivery of therapeutic proteins compared to intravenous infusion, but there is potential for enhanced immunogenicity toward subcutaneously administered proteins in a subset of patients. Unwanted anti-drug antibody response toward proteins or monoclonal antibodies upon repeated administration is shown to impact the pharmacokinetics and efficacy of multiple biologics. Unique immunogenicity challenges of the subcutaneous route have been realized through various preclinical and clinical examples, although subcutaneous delivery has often demonstrated comparable immunogenicity to intravenous administration. Beyond route of administration as a treatment-related factor of immunogenicity, certain product-related risk factors are particularly relevant to subcutaneously administered proteins. This review attempts to provide an overview of the mechanism of immune response toward proteins administered subcutaneously (subcutaneous proteins) and comments on product-related risk factors related to protein structure and stability, dosage form, and aggregation. A two-wave mechanism of antigen presentation in the immune response toward subcutaneous proteins is described, and interaction with dynamic antigen-presenting cells possessing high antigen processing efficiency and migratory activity may drive immunogenicity. Mitigation strategies for immunogenicity are discussed, including those in general use clinically and those currently in development. Mechanistic insights along with consideration of risk factors involved inspire theoretical strategies to provide antigen-specific, long-lasting effects for maintaining the safety and efficacy of therapeutic proteins.

Published

2021

19. Preclinical evaluation of cancer immune therapy using patient-derived tumor antigen-specific T cells in a novel xenograft platform.

Author

Shenoy GN, Greene CJ, Bhatta M, Baroja ML, Loyall JL, Balu-Iyer SV, Kelleher RJ Jr, Carreno BM, Linette GP, Shultz LD, and Bankert RB

Abstract

Objectives: With a rapidly growing list of candidate immune-based cancer therapeutics, there is a critical need to generate highly reliable animal models to preclinically evaluate the efficacy of emerging immune-based therapies, facilitating successful clinical translation. Our aim was to design and validate a novel in vivo model (called Xenomimetic or 'X' mouse) that allows monitoring of the ability of human tumor-specific T cells to suppress tumor growth following their entry into the tumor., Methods: Tumor xenografts are established rapidly in the greater omentum of globally immunodeficient NOD- scid IL2Rγ null (NSG) mice following an intraperitoneal injection of melanoma target cells expressing tumor neoantigen peptides, as well as green fluorescent protein and/or luciferase. Changes in tumor burden, as well as in the number and phenotype of adoptively transferred patient-derived tumor neoantigen-specific T cells in response to immunotherapy, are measured by imaging to detect fluorescence/luminescence and flow cytometry, respectively., Results: The tumors progress rapidly and disseminate in the mice unless patient-derived tumor-specific T cells are introduced. An initial T cell-mediated tumor arrest is later followed by a tumor escape, which correlates with the upregulation of the checkpoint molecules programmed cell death-1 (PD-1) and lymphocyte-activation gene 3 (LAG3) on T cells. Treatment with immune-based therapies that target these checkpoints, such as anti-PD-1 antibody (nivolumab) or interleukin-12 (IL-12), prevented or delayed the tumor escape. Furthermore, IL-12 treatment suppressed PD-1 and LAG3 upregulation on T cells., Conclusion: Together, these results validate the X-mouse model and establish its potential to preclinically evaluate the therapeutic efficacy of immune-based therapies., Competing Interests: Triggered loading technology used in this study has been patented (US Patent 7 662 405 entitled ‘Composition and Method of Liposomal Microparticulate IL12’), and Immune Modulatory Therapies, LLC, has exclusive rights to this patent. The authors declare no other conflicts of interest., (© 2021 The Authors. Clinical & Translational Immunology published by John Wiley & Sons Australia, Ltd on behalf of Australian and New Zealand Society for Immunology, Inc.)

Published

2021

20. Biological Function and Immunotherapy Utilizing Phosphatidylserine-based Nanoparticles.

Author

Glassman FY, Dingman R, Yau HC, and Balu-Iyer SV

Subjects

Animals, Apoptosis drug effects, Drug Design, Drug Development, Humans, Molecular Structure, Phagocytes drug effects, Phagocytes immunology, Phagocytes metabolism, Phagocytosis drug effects, Phagocytosis immunology, Immunotherapy methods, Nanoparticles chemistry, Phosphatidylserines chemistry, Theranostic Nanomedicine methods

Abstract

Phosphatidylserine (PS) is a naturally occurring anionic phospholipid that is primarily located in the inner leaflet of eukaryotic cell membranes. The role of PS during apoptosis is one of the most studied biological functions of PS. Externalization of PS during apoptosis mediates an "eat me" signal for phagocytic uptake, leading to clearance of apoptotic cells and thus maintain self-tolerance by immunological ignorance. However, an emerging view is that PS exposure-mediated cellular uptake is not an immunologically silent event, but rather promoting an active tolerance towards self and foreign proteins. This biological property of PS has been exploited by parasites and viruses in order to evade immune surveillance of the host immune system. Further, this novel immune regulatory property of PS that results in tolerance induction can be harnessed for clinical applications, such as to treat autoimmune conditions and to reduce immunogenicity of therapeutic proteins. This review attempts to provide an overview of the biological functions of PS in the immune response and its potential therapeutic applications.

Published

2020

21. Immunogenicity of Protein Pharmaceuticals.

Author

Dingman R and Balu-Iyer SV

Subjects

Animals, Antibodies immunology, Humans, Antibody Formation drug effects, Antibody Formation immunology, Proteins immunology, Proteins pharmacology

Abstract

Protein therapeutics have drastically changed the landscape of treatment for many diseases by providing a regimen that is highly specific and lacks many off-target toxicities. The clinical utility of many therapeutic proteins has been undermined by the potential development of unwanted immune responses against the protein, limiting their efficacy and negatively impacting its safety profile. This review attempts to provide an overview of immunogenicity of therapeutic proteins, including immune mechanisms and factors influencing immunogenicity, impact of immunogenicity, preclinical screening methods, and strategies to mitigate immunogenicity., (Copyright © 2019 American Pharmacists Association®. Published by Elsevier Inc. All rights reserved.)

Published

2019

22. Gboxin is an oxidative phosphorylation inhibitor that targets glioblastoma.

Author

Shi Y, Lim SK, Liang Q, Iyer SV, Wang HY, Wang Z, Xie X, Sun D, Chen YJ, Tabar V, Gutin P, Williams N, De Brabander JK, and Parada LF

Subjects

Allografts, Animals, Astrocytes cytology, Astrocytes drug effects, Cell Line, Tumor, Fibroblasts cytology, Fibroblasts drug effects, Humans, Hydrogen-Ion Concentration, Mice, Mitochondrial Membrane Transport Proteins metabolism, Mitochondrial Membranes drug effects, Mitochondrial Membranes enzymology, Mitochondrial Membranes metabolism, Mitochondrial Permeability Transition Pore, Neoplasm Transplantation, Organ Specificity, Proton-Motive Force drug effects, Proton-Translocating ATPases antagonists & inhibitors, Proton-Translocating ATPases metabolism, Xenograft Model Antitumor Assays, Glioblastoma drug therapy, Glioblastoma metabolism, Oxidative Phosphorylation drug effects

Abstract

Cancer-specific inhibitors that reflect the unique metabolic needs of cancer cells are rare. Here we describe Gboxin, a small molecule that specifically inhibits the growth of primary mouse and human glioblastoma cells but not that of mouse embryonic fibroblasts or neonatal astrocytes. Gboxin rapidly and irreversibly compromises oxygen consumption in glioblastoma cells. Gboxin relies on its positive charge to associate with mitochondrial oxidative phosphorylation complexes in a manner that is dependent on the proton gradient of the inner mitochondrial membrane, and it inhibits the activity of F 0 F 1 ATP synthase. Gboxin-resistant cells require a functional mitochondrial permeability transition pore that regulates pH and thus impedes the accumulation of Gboxin in the mitochondrial matrix. Administration of a metabolically stable Gboxin analogue inhibits glioblastoma allografts and patient-derived xenografts. Gboxin toxicity extends to established human cancer cell lines of diverse organ origin, and shows that the increased proton gradient and pH in cancer cell mitochondria is a mode of action that can be targeted in the development of antitumour reagents.

Published

2019

23. Sialic Acid-Dependent Inhibition of T Cells by Exosomal Ganglioside GD3 in Ovarian Tumor Microenvironments.

Author

Shenoy GN, Loyall J, Berenson CS, Kelleher RJ Jr, Iyer V, Balu-Iyer SV, Odunsi K, and Bankert RB

Subjects

Ascites, Cells, Cultured, Female, Humans, Immune Tolerance, NF-kappa B metabolism, Neoplasm Staging, Ovarian Neoplasms immunology, Tumor Microenvironment, Ascitic Fluid metabolism, Exosomes metabolism, Gangliosides metabolism, Immunotherapy methods, N-Acetylneuraminic Acid metabolism, Ovarian Neoplasms metabolism, T-Lymphocytes immunology

Abstract

The tumor microenvironment is rendered immunosuppressive by a variety of cellular and acellular factors that represent potential cancer therapeutic targets. Although exosomes isolated from ovarian tumor ascites fluids have been previously reported to induce a rapid and reversible T cell arrest, the factors present on or within exosomes that contribute to immunosuppression have not been fully defined. In this study, we establish that GD3, a ganglioside expressed on the surface of exosomes isolated from human ovarian tumor ascites fluids, is causally linked to the functional arrest of T cells activated through their TCR. This arrest is inhibited by Ab blockade of exosomal GD3 or by the removal of GD3 + exosomes. Empty liposomes expressing GD3 on the surface also inhibit the activation of T cells, establishing that GD3 contributes to the functional arrest of T cells independent of factors present in exosomes. Finally, we demonstrate that the GD3-mediated arrest of the TCR activation is dependent upon sialic acid groups, because their enzymatic removal from exosomes or liposomes results in a loss of inhibitory capacity. Collectively, these data define GD3 as a potential immunotherapeutic target., (Copyright © 2018 by The American Association of Immunologists, Inc.)

Published

2018

24. Subcutaneous administration of Lyso-phosphatidylserine nanoparticles induces immunological tolerance towards Factor VIII in a Hemophilia A mouse model.

Author

Glassman FY and Balu-Iyer SV

Subjects

Animals, Antibodies immunology, Disease Models, Animal, Factor VIII administration & dosage, Factor VIII genetics, Factor VIII immunology, Injections, Subcutaneous, Mice, Transgenic, Ovalbumin immunology, Phosphatidylserines immunology, T-Lymphocytes, Regulatory immunology, Hemophilia A immunology, Immune Tolerance drug effects, Membrane Proteins immunology, Nanoparticles administration & dosage, Phosphatidylserines administration & dosage

Abstract

A major complication with enzyme replacement therapy of Factor VIII (FVIII) in Hemophilia A (HA) is the development of anti-drug antibodies. Recently, we have shown that FVIII administration in the presence of heterogeneous phosphatidylserine (PS) nanoparticles derived from a natural source induces tolerance to FVIII, suggesting that PS converts an immunogen to a tolerogen. However, the specific structural features responsible for the immune-regulatory properties of PS is unclear. Identifying a specific PS species that is responsible is critical in order to further develop and optimize this nanoparticle. Further, clinical development of this lipid-based strategy requires optimization of the lipid particle that is homogeneous and synthetic. Here, we investigate the ability of mono-acylated Lyso-PS to induce hypo-responsiveness towards FVIII in HA mice. Administration of both PS and Lyso-PS FVIII significantly reduced anti-FVIII antibody responses despite rechallenge with FVIII. Additionally, the Lyso-PS-mediated effect was shown to be antigen-specific as mice responded normally against a rechallenge with an unrelated antigen, ovalbumin. Furthermore, the hypo-responsiveness observed with Lyso-PS may involve interactions with a specific PS receptor, TIM-4, along with increasing regulatory T-cells. These data indicate that using Lyso-PS allows for a more homogenous formulation in order to induce tolerance towards therapeutic proteins., (Copyright © 2018 Elsevier B.V. All rights reserved.)

Published

2018

25. Phosphatidylserine Is Not Just a Cleanup Crew but Also a Well-Meaning Teacher.

Author

Glassman FY, Schneider JL, Ramakrishnan R, Dingman RK, Ramanathan M, Bankert RB, and Balu-Iyer SV

Subjects

Animals, Antibody Formation, Apoptosis, Dexamethasone administration & dosage, Disease Models, Animal, Encephalomyelitis, Autoimmune, Experimental immunology, Factor VIII administration & dosage, Factor VIII immunology, Female, Hemophilia A immunology, Humans, Immune Tolerance, Immunosuppressive Agents administration & dosage, Liposomes administration & dosage, Liposomes immunology, Mice, Mice, Inbred C57BL, Myelin-Oligodendrocyte Glycoprotein administration & dosage, Myelin-Oligodendrocyte Glycoprotein immunology, Phosphatidylserines administration & dosage, alpha-Glucosidases administration & dosage, Dexamethasone immunology, Glycogen Storage Disease Type II immunology, Immunosuppressive Agents immunology, Phosphatidylserines immunology, alpha-Glucosidases immunology

Abstract

Phosphatidylserine (PS) exposure during apoptosis leads to silent clearance of cells without adverse immune reactions to self-proteins. Given the biological functions of PS in cellular cleanup and global immunosuppression, we hypothesized that administration of PS-protein complexes would reduce immunogenicity. Here, we report that exposing Pompe disease mice to acid alpha glucosidase (rhGAA) with PS or immunosuppressant dexamethasone resulted in lower anti-rhGAA antibodies than in animals receiving rhGAA alone. However, upon rechallenge with rhGAA, only PS-rhGAA pre-exposed mice displayed a durable hyporesponsiveness even after PS administration was ceased. Thus, pre-exposure of antigens administered together with PS were not silently cleared, but the immune system acquired memory about the antigen that averted mounting of a response during rechallenge. In hemophilia A mice, PS hyporesponsiveness toward Factor VIII was reversed by administration of function-blocking antibody against the PS receptor T-cell immunoglobulin and mucin 4, implicating this receptor in PS's effect. Moreover, pre-exposure of myelin oligodendrocyte glycoprotein peptide with PS delayed the onset and reduced the severity of experimental autoimmune encephalomyelitis. These observations suggest that PS's function in apoptosis is not limited to silent antigen clearance without immune responses toward self-proteins but shows that PS reduces immune response during rechallenge to several antigens that also involves initiation of antigen tolerance., (Copyright © 2018 American Pharmacists Association®. Published by Elsevier Inc. All rights reserved.)

Published

2018

26. Challenges and Opportunities for the Subcutaneous Delivery of Therapeutic Proteins.

Author

Turner MR and Balu-Iyer SV

Subjects

Animals, Drug-Related Side Effects and Adverse Reactions immunology, Humans, Injections, Subcutaneous adverse effects, Pharmaceutical Preparations administration & dosage, Pharmacokinetics, Proteins adverse effects, Proteins immunology, Recombinant Proteins administration & dosage, Recombinant Proteins adverse effects, Recombinant Proteins immunology, Recombinant Proteins pharmacokinetics, Skin anatomy & histology, Skin immunology, Skin metabolism, Subcutaneous Tissue anatomy & histology, Subcutaneous Tissue immunology, Proteins administration & dosage, Proteins pharmacokinetics, Subcutaneous Tissue metabolism

Abstract

Biotherapeutics is a rapidly growing drug class, and over 200 biotherapeutics have already obtained approval, with about 50 of these being approved in 2015 and 2016 alone. Several hundred protein therapeutic products are still in the pipeline, including interesting new approaches to treatment. Owing to patients' convenience of at home administration and reduced number of hospital visits as well as the reduction in treatment costs, subcutaneous (SC) administration of biologics is of increasing interest. Although several avenues for treatment using biotherapeutics are being explored, there is still a sufficient gap in knowledge regarding the interplay of formulation conditions, immunogenicity, and pharmacokinetics (PK) of the absorption of these compounds when they are given SC. This review seeks to highlight the major concerns and important factors governing this route of administration and suggest a holistic approach for effective SC delivery., (Copyright © 2018 American Pharmacists Association®. Published by Elsevier Inc. All rights reserved.)

Published

2018

27. MTBP inhibits the Erk1/2-Elk-1 signaling in hepatocellular carcinoma.

Author

Ranjan A, Iyer SV, Ward C, Link T, Diaz FJ, Dhar A, Tawfik OW, Weinman SA, Azuma Y, Izumi T, and Iwakuma T

Abstract

Hepatocellular carcinoma (HCC) is one of the most common cancers worldwide, and the prognosis of HCC patients, especially those with metastasis, remains extremely poor. This is partly due to unclear molecular mechanisms underlying HCC metastasis. Our previous study indicates that MDM2 Binding Protein (MTBP) suppresses migration and metastasis of HCC cells. However, signaling pathways regulated by MTBP remain unknown. To identify metastasis-associated signaling pathways governed by MTBP, we have performed unbiased luciferase reporter-based signal array analyses and found that MTBP suppresses the activity of the ETS-domain transcription factor Elk-1, a downstream target of Erk1/2 MAP kinases. MTBP also inhibits phosphorylation of Elk-1 and decreases mRNA expression of Elk-1 target genes. Reduced Elk-1 activity is caused by inhibited nuclear translocation of phosphorylated Erk1/2 (p-Erk) by MTBP and subsequent inhibition of Elk-1 phosphorylation. We also reveal that MTBP inhibits the interaction of p-Erk with importin-7/RanBP7 (IPO7), an importin family member which shuttles p-Erk into the nucleus, by binding to IPO7. Moreover, high levels of MTBP in human HCC tissues are correlated with cytoplasmic localization of p-Erk1/2. Our study suggests that MTBP suppresses metastasis, at least partially, by down-modulating the Erk1/2-Elk-1 signaling pathway, thus identifying a novel regulatory mechanism of HCC metastasis by regulating the subcellular localization of p-Erk., Competing Interests: CONFLICTS OF INTEREST No potential conflicts of interest were disclosed.

Published

2018

28. Lipidic Nanoparticles Comprising Phosphatidylinositol Mitigate Immunogenicity and Improve Efficacy of Recombinant Human Acid Alpha-Glucosidase in a Murine Model of Pompe Disease.

Author

Schneider JL, Dingman RK, and Balu-Iyer SV

Subjects

Animals, Antibody Formation drug effects, Disease Models, Animal, Factor VIII metabolism, Glycogen Storage Disease Type II metabolism, Humans, Liposomes administration & dosage, Mice, Mice, Knockout, Glycogen Storage Disease Type II drug therapy, Nanoparticles administration & dosage, Phosphatidylinositols administration & dosage, Recombinant Proteins metabolism, alpha-Glucosidases metabolism

Abstract

Enzyme replacement therapy with recombinant human acid α-glucosidase (rhGAA) is complicated by the formation of anti-rhGAA antibodies, a short circulating half-life, instability in the plasma, and limited uptake into target tissue. Previously, we have demonstrated that phosphatidylinositol (PI) containing liposomes can reduce the immunogenicity and extend plasma survival of factor VIII (FVIII) in a mouse model of hemophilia A. In this article, we investigate the ability of PI liposomes to be used as a delivery vehicle to overcome the issues that complicate therapy with rhGAA. In a murine model of Pompe disease, administration of PI-rhGAA mitigated the immunogenicity of rhGAA, resulting in a significantly lower formation of anti-rhGAA antibodies. PI-rhGAA also showed minimal improvements to the pharmacokinetic parameters and efficacy measures compared to free rhGAA. Overall, these data suggest that PI-rhGAA may have the potential to be a useful therapeutic option for improving the treatment of Pompe disease., (Copyright © 2018 American Pharmacists Association®. Published by Elsevier Inc. All rights reserved.)

Published

2018

29. Exosomes Associated with Human Ovarian Tumors Harbor a Reversible Checkpoint of T-cell Responses.

Author

Shenoy GN, Loyall J, Maguire O, Iyer V, Kelleher RJ Jr, Minderman H, Wallace PK, Odunsi K, Balu-Iyer SV, and Bankert RB

Subjects

Cell Proliferation, Exosomes immunology, Female, Humans, Ovarian Neoplasms immunology, Microscopy, Electron, Transmission methods, T-Lymphocytes metabolism

Abstract

Nano-sized membrane-encapsulated extracellular vesicles isolated from the ascites fluids of ovarian cancer patients are identified as exosomes based on their biophysical and compositional characteristics. We report here that T cells pulsed with these tumor-associated exosomes during TCR-dependent activation inhibit various activation endpoints including translocation of NFκB and NFAT into the nucleus, upregulation of CD69 and CD107a, production of cytokines, and cell proliferation. In addition, the activation of virus-specific CD8 + T cells that are stimulated with the cognate viral peptides presented in the context of class I MHC is also suppressed by the exosomes. The inhibition occurs without loss of cell viability and coincidentally with the binding and internalization of these exosomes. This exosome-mediated inhibition of T cells was transient and reversible: T cells exposed to exosomes can be reactivated once exosomes are removed. We conclude that tumor-associated exosomes are immunosuppressive and represent a therapeutic target, blockade of which would enhance the antitumor response of quiescent tumor-associated T cells and prevent the functional arrest of adoptively transferred tumor-specific T cells or chimeric antigen receptor T cells. Cancer Immunol Res; 6(2); 236-47. ©2018 AACR ., (©2018 American Association for Cancer Research.)

Published

2018

30. Novel siRNA formulation to effectively knockdown mutant p53 in osteosarcoma.

Author

Kundu AK, Iyer SV, Chandra S, Adhikari AS, Iwakuma T, and Mandal TK

Subjects

Bone Neoplasms genetics, Bone Neoplasms metabolism, Cell Survival, Humans, Mutation, Nanoparticles, Osteosarcoma genetics, Osteosarcoma metabolism, Tumor Cells, Cultured, Tumor Suppressor Protein p53 genetics, Tumor Suppressor Protein p53 metabolism, Bone Neoplasms pathology, Gene Silencing, Osteosarcoma pathology, RNA, Small Interfering genetics, Tumor Suppressor Protein p53 antagonists & inhibitors

Abstract

Objectives: The tumor suppressor p53 plays a crucial role in the development of osteosarcoma. The primary objective of this study is to develop and optimize lipid based nanoparticle formulations that can carry siRNA and effectively silence mutant p53 in 318-1, a murine osteosarcoma cell line., Methods: The nanoparticles were composed of a mixture of two lipids (cholesterol and DOTAP) and either PLGA or PLGA-PEG and prepared by using an EmulsiFlex-B3 high pressure homogenizer. A series of studies that include using different nanoparticles, different amount of siRNAs, cell numbers, incubation time, transfection media volume, and storage temperature was performed to optimize the gene silencing efficiency., Key Findings: Replacement of lipids by PLGA or PLGA-PEG decreased the particle size and overall cytotoxicity. Among all lipid-polymer nanoformulations, nanoparticles with 10% PLGA showed highest mutant p53 knockdown efficiency while maintaining higher cell viability when a nanoparticle to siRNA ratio equal to 6.8:0.66 and 75 nM siRNA was used. With long term storage the mutant p53 knockdown efficiency decreased to a greater extent., Conclusions: This study warrants a future evaluation of this formulation for gene silencing efficiency of mutant p53 in tissue culture and animal models for the treatment of osteosarcoma.

Published

2017

31. Suppressive roles of A3AR and TMIGD3 i1 in osteosarcoma malignancy.

Author

Ranjan A, Iyer SV, and Iwakuma T

Subjects

DNA, Complementary genetics, Humans, Protein Isoforms metabolism, Bone Neoplasms metabolism, Bone Neoplasms pathology, Membrane Proteins metabolism, Osteosarcoma metabolism, Osteosarcoma pathology, Receptor, Adenosine A3 metabolism

Published

2017

32. Genome-wide RNAi screening identifies TMIGD3 isoform1 as a suppressor of NF-κB and osteosarcoma progression.

Author

Iyer SV, Ranjan A, Elias HK, Parrales A, Sasaki H, Roy BC, Umar S, Tawfik OW, and Iwakuma T

Subjects

Animals, Bone Neoplasms genetics, Cell Line, Tumor, Cell Movement genetics, Disease Progression, Gene Expression Regulation, Neoplastic, Gene Knockdown Techniques, Humans, Lung pathology, Lung Neoplasms genetics, Lung Neoplasms secondary, Membrane Glycoproteins genetics, Membrane Proteins genetics, Mice, Mice, Nude, Osteosarcoma genetics, Osteosarcoma secondary, Protein Isoforms genetics, Protein Isoforms metabolism, RNA Interference, RNA, Small Interfering genetics, RNA, Small Interfering metabolism, Receptor, Adenosine A3 genetics, Signal Transduction genetics, Xenograft Model Antitumor Assays, Bone Neoplasms pathology, Lung Neoplasms pathology, Membrane Glycoproteins metabolism, Membrane Proteins metabolism, NF-kappa B metabolism, Osteosarcoma pathology, Receptor, Adenosine A3 metabolism

Abstract

The ability of cancer cells to survive and grow in anchorage- and serum-independent conditions is well correlated with their aggressiveness. Here, using a human whole-genome shRNA library, we identify TMIGD3 isoform1 (i1) as a factor that suppresses this ability in osteosarcoma (OS) cells, mainly by inhibiting NF-κB activity. Knockdown of TMIGD3 increases proliferation, tumour formation and metastasis of OS cells. Overexpression of TMIGD3 isoform1 (i1), but not isoform3 (i3) which shares a common C-terminal region, suppresses these malignant properties. Adenosine A3 receptor (A3AR) having an identical N-terminal region shows similar biological profiles to TMIGD3 i1. Protein expression of TMIGD3 and A3AR is lower in human OS tissues than normal tissues. Mechanistically, TMIGD3 i1 and A3AR commonly inhibit the PKA-Akt-NF-κB axis. However, TMIGD3 i1 only partially rescues phenotypes induced by A3AR knockdown, suggesting the presence of distinct pathways. Our findings reveal an unappreciated role for TMIGD3 i1 as a suppressor of NF-κB activity and OS progression.

Published

2016

33. DNAJA1 controls the fate of misfolded mutant p53 through the mevalonate pathway.

Author

Parrales A, Ranjan A, Iyer SV, Padhye S, Weir SJ, Roy A, and Iwakuma T

Subjects

Cell Line, Tumor, Cell Transformation, Neoplastic drug effects, Cell Transformation, Neoplastic genetics, DNA metabolism, Humans, Mevalonic Acid pharmacology, Protein Binding genetics, Tumor Suppressor Protein p53 genetics, Ubiquitination, Cell Movement genetics, HSP40 Heat-Shock Proteins metabolism, Mutation genetics, Tumor Suppressor Protein p53 metabolism

Abstract

Stabilization of mutant p53 (mutp53) in tumours greatly contributes to malignant progression. However, little is known about the underlying mechanisms and therapeutic approaches to destabilize mutp53. Here, through high-throughput screening we identify statins, cholesterol-lowering drugs, as degradation inducers for conformational or misfolded p53 mutants with minimal effects on wild-type p53 (wtp53) and DNA contact mutants. Statins preferentially suppress mutp53-expressing cancer cell growth. Specific reduction of mevalonate-5-phosphate by statins or mevalonate kinase knockdown induces CHIP ubiquitin ligase-mediated nuclear export, ubiquitylation, and degradation of mutp53 by impairing interaction of mutp53 with DNAJA1, a Hsp40 family member. Knockdown of DNAJA1 also induces CHIP-mediated mutp53 degradation, while its overexpression antagonizes statin-induced mutp53 degradation. Our study reveals that DNAJA1 controls the fate of misfolded mutp53, provides insights into potential strategies to deplete mutp53 through the mevalonate pathway-DNAJA1 axis, and highlights the significance of p53 status in impacting statins' efficacy on cancer therapy.

Published

2016

34. Effect of Biophysical Properties of Phosphatidylserine Particle on Immune Tolerance Induction Toward Factor VIII in a Hemophilia A Mouse Model.

Author

Ramakrishnan R and Balu-Iyer SV

Subjects

Animals, Factor VIII administration & dosage, Humans, Immune Tolerance drug effects, Injections, Subcutaneous, Mice, Mice, Knockout, Particle Size, Phosphatidylserines administration & dosage, Recombinant Proteins administration & dosage, Recombinant Proteins immunology, Treatment Outcome, Disease Models, Animal, Factor VIII immunology, Hemophilia A drug therapy, Hemophilia A immunology, Immune Tolerance immunology, Phosphatidylserines immunology

Abstract

A major complication in the replacement therapy of Factor VIII (FVIII) for Hemophilia A is the development of unwanted immune responses. Previous studies from our laboratory have shown that pretreatment of FVIII in the presence of phosphatidylserine (PS) resulted in hyporesponsiveness to subsequent administration of FVIII alone, due to the ability of PS to convert an immunogen to a tolerogen. We investigated the importance of biophysical properties of PS liposomes on its ability to convert an immunogen to a tolerogen. PS particles were prepared differing in size, protein-lipid topology, lamellarity, and % association to FVIII keeping the composition of the particle same. PS particles were prepared in 2 different sizes with differing biophysical properties: smaller particles in the nanometer range (200 nm) and larger size particles in the micron range (2 μm). Hemophilia A animals treated with both the nanometer and micron size PS particles showed a significant reduction in anti-FVIII antibody titers when compared to animals receiving free FVIII alone. Upon rechallenge with free FVIII animals that received FVIII along with the nanometer size particle continued to show reduced antibody responses. Animals receiving the micron size particle showed a slight increase in titers although they remained significantly lower than the free FVIII treated group. Upon culture with bone marrow derived dendritic cells, the nanometer size particle showed a reduction in CD40 expression and an increase in transforming growth factor-β cytokine production, which was not observed with the micron size particle. These results show that biophysical properties of PS play an important role in tolerance., (Copyright © 2016 American Pharmacists Association®. Published by Elsevier Inc. All rights reserved.)

Published

2016

35. Phosphatidylserine Converts Immunogenic Recombinant Human Acid Alpha-Glucosidase to a Tolerogenic Form in a Mouse Model of Pompe Disease.

Author

Schneider JL and Balu-Iyer SV

Subjects

Animals, Cells, Cultured, Dose-Response Relationship, Drug, HEK293 Cells, Humans, Immunization methods, Immunogenicity, Vaccine drug effects, Male, Mice, Mice, 129 Strain, Mice, Inbred C57BL, Mice, Knockout, Organic Chemicals administration & dosage, Organic Chemicals immunology, Phosphatidylserines administration & dosage, alpha-Glucosidases administration & dosage, Disease Models, Animal, Glycogen Storage Disease Type II drug therapy, Glycogen Storage Disease Type II immunology, Immunogenicity, Vaccine immunology, Phosphatidylserines immunology, alpha-Glucosidases immunology

Abstract

Development of unwanted immune responses against therapeutic proteins is a major clinical complication. Recently, we have shown that exposure of Factor VIII in the presence of phosphatidylserine (PS) induces antigen-specific hyporesponsiveness to Factor VIII rechallenge, suggesting that PS is not immune suppressive, but rather immune regulatory in that PS converts an immunogen to a tolerogen. Since PS is exposed in the outer leaflet during apoptosis, we hypothesize that PS imparts tolerogenic activity to this natural process. Thus, immunization with PS containing liposomes would mimic this natural process. Here, we investigate the immune regulatory effects of PS in inducing tolerance toward recombinant human acid alpha-glucosidase (rhGAA). rhGAA was found to complex with PS liposomes through hydrophobic interactions, and incubation PS-rhGAA with dendritic cells resulted in the increased secretion of transforming growth factor-β. Immunization with PS-rhGAA or O-phospho-L-serine-rhGAA led to a reduction in anti-rhGAA antibody response which persisted despite rechallenge with free rhGAA. Importantly, the titer levels in a majority of these animals remained unchanged after rechallenge and can be considered nonresponders. These data provide evidence that PS liposomes can be used to induce tolerance toward therapeutic proteins, in general., (Copyright © 2016 American Pharmacists Association®. Published by Elsevier Inc. All rights reserved.)

Published

2016

36. Factor VIII associated with lipidic nanoparticles retains efficacy in the presence of anti-factor VIII antibodies in hemophilia A mice.

Author

Shetty KA, Kosloski MP, Mager DE, and Balu-Iyer SV

Subjects

Animals, Factor VIII immunology, Factor VIII pharmacokinetics, Factor VIII therapeutic use, Hemophilia A blood, Hemophilia A immunology, Mice, Inbred C57BL, Models, Biological, Phosphatidylinositols chemistry, Recombinant Proteins administration & dosage, Recombinant Proteins immunology, Recombinant Proteins pharmacokinetics, Recombinant Proteins therapeutic use, Treatment Outcome, Antibodies blood, Factor VIII administration & dosage, Hemophilia A drug therapy, Nanoparticles administration & dosage

Abstract

The development of inhibitory antibodies against factor VIII (FVIII) is a major challenge in hemophilia A (HA) therapy. Such antibodies develop in nearly 30% of patients receiving replacement FVIII, abrogating therapeutic efficacy. This work evaluated whether B-domain deleted FVIII encapsulated in phosphatidylinositol containing lipid nanoparticles (PI-BDD FVIII) could serve as an efficacious FVIII replacement therapy in the presence of inhibitors. The HA mice were given clinically relevant doses of FVIII to develop inhibitors. The efficacy of free and PI-BDD FVIII was studied in inhibitor-positive HA mice using a tail clip assay. Mathematical modeling of these data was conducted to evaluate the hypothesis that lipid association sterically shields the protein from inhibitor binding. The immunization protocol resulted in a mean inhibitory titer level of 198 ± 52 BU/ml. Free BDD FVIII was ineffective at controlling blood loss in inhibitor-positive HA mice as early as 2 h post dose. In contrast, PI-BDD FVIII treated animals retained partial hemostatic efficacy as long as 18 h post dose. Mathematical modeling supports the hypotheses that a greater fraction of lipid-associated FVIII remains unbound to inhibitors and that PI-BDD FVIII has lower binding affinity to inhibitors than does the free protein. In addition, the modeling approaches extend current efforts to model the impact of immunogenicity on PK and the therapeutically meaningful endpoint of efficacy, thereby addressing an important knowledge gap, particularly in the FVIII scientific literature. Clinical translation of these findings could result in a significant improvement in the quality of care of inhibitor-positive HA patients. Copyright © 2016 John Wiley & Sons, Ltd., Competing Interests: The authors have no financial or non-financial conflicts of interest to declare., (Copyright © 2016 John Wiley & Sons, Ltd.)

Published

2016

37. Soy Phosphatidylinositol-Containing Lipid Nanoparticle Prolongs the Plasma Survival and Hemostatic Efficacy of B-domain-Deleted Recombinant Canine Factor VIII in Hemophilia A Dogs.

Author

Shetty KA, Merricks EP, Raymer R, Rigsbee N, Nichols TC, and Balu-Iyer SV

Subjects

Animals, Dogs, Drug Compounding, Drug Stability, Factor VIII administration & dosage, Factor VIII therapeutic use, Female, Hemophilia A blood, Hemostatics administration & dosage, Hemostatics therapeutic use, Injections, Intravenous, Models, Biological, Recombinant Proteins, Drug Carriers chemistry, Factor VIII pharmacokinetics, Hemophilia A drug therapy, Hemostatics blood, Nanoparticles chemistry, Phosphatidylinositols chemistry, Glycine max chemistry

Abstract

Soy phosphatidylinositol (PI)-containing lipid nanoparticles prolong plasma survival, improve hemostatic efficacy, and decrease immunogenicity of human B-domain-deleted factor VIII (BDD FVIII) in hemophilia A (HA) mice. We hypothesize that PI-associated BDD FVIII is more potent than the free protein and, using mathematical modeling, have projected that PI-associated BDD FVIII could be used for once-weekly prophylactic dosing in patients. To facilitate translation to the clinic, comparative plasma survival and ex vivo efficacy of PI-associated recombinant canine FVIII (PI-rcFVIII) were evaluated in HA dogs. Two HA dogs were administered a 50-U/kg intravenous dose of free or PI-rcFVIII. rcFVIII activity measurements and ex vivo efficacy analyses such as whole blood clotting time and thromboelastography were conducted on recovered plasma and whole blood samples. PI association decreased clearance (∼25%) and increased plasma exposure (∼1.4-fold) of rcFVIII. PI-rcFVIII-treated animals had prolonged improvements in whole blood clotting time and thromboelastography parameters compared to free rcFVIII-treated animals. Because rcFVIII is a BDD form of FVIII, these studies provide proof of principle that observations with human BDD FVIII in mice translate to higher animal species. In addition, PI-rcFVIII has potential applications in canine HA management and as a bypass therapy in inhibitor-positive HA patients., (Copyright © 2016 American Pharmacists Association®. Published by Elsevier Inc. All rights reserved.)

Published

2016

38. Genome-wide gene-based analysis suggests an association between Neuroligin 1 (NLGN1) and post-traumatic stress disorder.

Author

Kilaru V, Iyer SV, Almli LM, Stevens JS, Lori A, Jovanovic T, Ely TD, Bradley B, Binder EB, Koen N, Stein DJ, Conneely KN, Wingo AP, Smith AK, and Ressler KJ

Subjects

Adult, Black or African American genetics, Amygdala diagnostic imaging, Amygdala physiopathology, Brain diagnostic imaging, Facial Expression, Facial Recognition, Fear, Female, Functional Neuroimaging, Genetic Predisposition to Disease, Genome-Wide Association Study, Histocompatibility Antigens Class I genetics, Humans, Magnetic Resonance Imaging, Male, Middle Aged, Polymorphism, Single Nucleotide, Prefrontal Cortex diagnostic imaging, Prefrontal Cortex physiopathology, Reflex, Startle physiology, Stress Disorders, Post-Traumatic diagnostic imaging, Stress Disorders, Post-Traumatic physiopathology, Stress Disorders, Post-Traumatic psychology, Temporal Lobe diagnostic imaging, Temporal Lobe physiopathology, Thalamus diagnostic imaging, Thalamus physiopathology, White People genetics, Young Adult, Brain physiopathology, Cell Adhesion Molecules, Neuronal genetics, Stress Disorders, Post-Traumatic genetics

Abstract

Post-traumatic stress disorder (PTSD) develops in only some people following trauma exposure, but the mechanisms differentially explaining risk versus resilience remain largely unknown. PTSD is heritable but candidate gene studies and genome-wide association studies (GWAS) have identified only a modest number of genes that reliably contribute to PTSD. New gene-based methods may help identify additional genes that increase risk for PTSD development or severity. We applied gene-based testing to GWAS data from the Grady Trauma Project (GTP), a primarily African American cohort, and identified two genes (NLGN1 and ZNRD1-AS1) that associate with PTSD after multiple test correction. Although the top SNP from NLGN1 did not replicate, we observed gene-based replication of NLGN1 with PTSD in the Drakenstein Child Health Study (DCHS) cohort from Cape Town. NLGN1 has previously been associated with autism, and it encodes neuroligin 1, a protein involved in synaptogenesis, learning, and memory. Within the GTP dataset, a single nucleotide polymorphism (SNP), rs6779753, underlying the gene-based association, associated with the intermediate phenotypes of higher startle response and greater functional magnetic resonance imaging activation of the amygdala, orbitofrontal cortex, right thalamus and right fusiform gyrus in response to fearful faces. These findings support a contribution of the NLGN1 gene pathway to the neurobiological underpinnings of PTSD., Competing Interests: SB is a consultant for Myriad Genetics and a director for Psynova Neurotech. The remaining authors declare no conflict of interest.

Published

2016

39. Allele-specific silencing of mutant p53 attenuates dominant-negative and gain-of-function activities.

Author

Iyer SV, Parrales A, Begani P, Narkar A, Adhikari AS, Martinez LA, and Iwakuma T

Subjects

Alleles, Animals, Apoptosis, Blotting, Western, Carcinogenesis genetics, Cell Adhesion, Cell Movement, Cell Proliferation, Down-Regulation, Genes, Dominant, Humans, Imidazoles metabolism, Immunoenzyme Techniques, Mice, Neoplasms genetics, Neoplasms pathology, Piperazines metabolism, RNA, Messenger genetics, RNA, Small Interfering genetics, Real-Time Polymerase Chain Reaction, Reverse Transcriptase Polymerase Chain Reaction, Tumor Cells, Cultured, Carcinogenesis pathology, Mutant Proteins genetics, Mutation genetics, Neoplasms prevention & control, Tumor Suppressor Protein p53 genetics

Abstract

Many p53 hotspot mutants not only lose the transcriptional activity, but also show dominant-negative (DN) and oncogenic gain-of-function (GOF) activities. Increasing evidence indicates that knockdown of mutant p53 (mutp53) in cancer cells reduces their aggressive properties, suggesting that survival and proliferation of cancer cells are, at least partially, dependent on the presence of mutp53. However, these p53 siRNAs can downregulate both wild-type p53 (wtp53) and mutp53, which limits their therapeutic applications. In order to specifically deplete mutp53, we have developed allele-specific siRNAs against p53 hotspot mutants and validated their biological effects in the absence or presence of wtp53. First, the mutp53-specific siRNAs selectively reduced protein levels of matched p53 mutants with minimal reduction in wtp53 levels. Second, downregulation of mutp53 in cancer cells expressing a mutp53 alone (p53mut) resulted in significantly decreased cell proliferation and migration. Third, transfection of mutp53-specific siRNAs in cancer cells expressing both wtp53 and mutp53 also reduced cell proliferation and migration with increased transcripts of p53 downstream target genes, which became further profound when cells were treated with an MDM2 inhibitor Nutlin-3a or a chemotherapeutic agent doxorubicin. These results indicate that depletion of mutp53 by its specific siRNA restored endogenous wtp53 activity in cells expressing both wtp53 and mutp53. This is the first study demonstrating biological effects and therapeutic potential of allele-specific silencing of mutp53 by mutp53-specific siRNAs in cancer cells expressing both wtp53 and mutp53, thus providing a novel strategy towards targeted cancer therapies.

Published

2016

40. The Effect of Small Oligomeric Protein Aggregates on the Immunogenicity of Intravenous and Subcutaneous Administered Antibodies.

Author

Fathallah AM, Chiang M, Mishra A, Kumar S, Xue L, Russell Middaugh C, and Balu-Iyer SV

Subjects

Animals, Antibodies, Bispecific administration & dosage, Antibodies, Bispecific chemistry, Antibodies, Monoclonal administration & dosage, Antibodies, Monoclonal chemistry, Dendritic Cells immunology, Humans, Immunization, Mice, Protein Conformation, Protein Unfolding, Tumor Necrosis Factor-alpha immunology, Antibodies, Bispecific immunology, Antibodies, Monoclonal immunology, Antibody Formation, Protein Aggregates

Abstract

The role of aggregates in the immunogenicity of biologics is a major concern. A recent US FDA guidance on the issue suggests that a gap in knowledge exists regarding the type and size of aggregates involved in the immunogenicity of biologics. Furthermore, the guidance suggests that current techniques cannot capture the crucial stages of protein aggregation. Using a protein unfolding model developed earlier, we generated and classified aggregates of two therapeutic antibodies based on size and conformation. The immunogenic potential of these aggregates were then tested in a murine model. Our findings show that small native-like oligomeric aggregates (<100 nm) are more immunogenic toward the native protein than monomer and large non-native aggregates in the micron-size range, irrespective of route of administration [intravenous (i.v.) vs. subcutaneous (s.c.)]. Those smaller oligomeric aggregates represented 5%-20% of the total protein concentration in the test formulations. Furthermore, in vitro data suggest that TNF-α production by bone marrow-derived dendritic cells could serve as a predictive marker for increased immunogenic risk of aggregates after s.c. administration. The use of orthogonal techniques such as fluorescence anisotropy and quasielastic light scattering may be useful to detect these oligomeric aggregates., (© 2015 Wiley Periodicals, Inc. and the American Pharmacists Association.)

Published

2015

41. An improved intrafemoral injection with minimized leakage as an orthotopic mouse model of osteosarcoma.

Author

Sasaki H, Iyer SV, Sasaki K, Tawfik OW, and Iwakuma T

Subjects

Animals, Cell Line, Tumor, Disease Models, Animal, Humans, Mice, Bone Neoplasms pathology, Cell Transformation, Neoplastic, Femur, Injections methods, Osteosarcoma pathology

Abstract

Osteosarcoma, the most common type of primary bone cancer, is the second highest cause of cancer-related death in pediatric patients. To understand the mechanisms behind osteosarcoma progression and to discover novel therapeutic strategies for this disease, a reliable and appropriate mouse model is essential. For this purpose, osteosarcoma cells need to be injected into the bone marrow. Previously, the intratibial and intrafemoral injection methods were reported; however, the major drawback of these methods is the potential leakage of tumor cells from the injection site during or after these procedures. To overcome this, we have established an improved method to minimize leakage in an orthotopic mouse model of osteosarcoma. By taking advantage of the anatomical benefits of the femur with less bowing and larger medullary cavity than those of the tibia, osteosarcoma cells are injected directly into the femoral cavity following reaming of its intramedullary space. To prevent potential leakage of tumor cells during and after the surgery, the injection site is sealed with bone wax. This method requires a minor surgery of approximately 15min under anesthesia. Our established orthotopic osteosarcoma model could serve as a valuable and reliable tool for examining progression of various types of bone tumors., (Copyright © 2015 Elsevier Inc. All rights reserved.)

Published

2015

42. Exposure of FVIII in the Presence of Phosphatidyl Serine Reduces Generation of Memory B-Cells and Induces Regulatory T-Cell-Mediated Hyporesponsiveness in Hemophilia A Mice.

Author

Ramakrishnan R, Davidowitz A, and Balu-Iyer SV

Subjects

Animals, Antibodies, Neutralizing analysis, Antibodies, Neutralizing biosynthesis, Antibody Specificity, B-Lymphocytes drug effects, B-Lymphocytes immunology, Drug Hypersensitivity prevention & control, Factor VIII genetics, Factor VIII metabolism, Factor VIII therapeutic use, Forkhead Transcription Factors blood, Forkhead Transcription Factors metabolism, Hematinics adverse effects, Hematinics metabolism, Hematinics therapeutic use, Hemophilia A blood, Hemophilia A immunology, Hemophilia A metabolism, Humans, Liposomes, Mice, Knockout, Mice, Transgenic, Phosphatidylglycerols chemistry, Recombinant Proteins metabolism, Recombinant Proteins therapeutic use, T-Lymphocytes, Regulatory drug effects, T-Lymphocytes, Regulatory immunology, T-Lymphocytes, Regulatory metabolism, Factor VIII administration & dosage, Hematinics administration & dosage, Hemophilia A drug therapy, Immune Tolerance drug effects, Immunologic Memory drug effects, Pharmaceutical Vehicles chemistry, Phosphatidylserines chemistry

Abstract

A major complication of replacement therapy with Factor VIII (FVIII) for hemophilia A (HA) is the development of unwanted immune responses. Previous studies showed that administration of FVIII in the presence of phosphatidyl serine (PS) reduced the development of anti-FVIII antibodies in HA mice. However, the impact of PS-mediated effects on immunological memory, such as generation of memory B-cells, is not clear. The effect of PS on memory B-cells was therefore investigated using adoptive transfer approach in FVIII(-/-) HA mice. Adoptive transfer of memory B-cells from a PS-FVIII-treated group to naïve mice followed by challenge of the recipient mice with FVIII showed a significantly reduced anti-FVIII antibody response in the recipient mice, compared with animals that received memory B-cells from free FVIII and FVIII-charge matched phosphatidyl glycerol (PG) group. The decrease in memory B-cell response is accompanied by an increase in FoxP3 expressing regulatory T-cells (Tregs). Flow cytometry studies showed that the generation of Tregs is higher in PS-treated animals as compared with FVIII and FVIII-PG treated animals. The PS-mediated hyporesponsiveness was found to be antigen-specific. The PS-FVIII immunization showed hyporesponsiveness toward FVIII rechallenge but not against ovalbumin (OVA) rechallenge, an unrelated antigen. This demonstrates that PS reduces immunologic memory of FVIII and induces antigen-specific peripheral tolerance in HA mice., (© 2015 Wiley Periodicals, Inc. and the American Pharmacists Association.)

Published

2015

43. Proton Pump Inhibitor Usage and the Risk of Myocardial Infarction in the General Population.

Author

Shah NH, LePendu P, Bauer-Mehren A, Ghebremariam YT, Iyer SV, Marcus J, Nead KT, Cooke JP, and Leeper NJ

Subjects

Adult, Clopidogrel, Humans, Middle Aged, Prospective Studies, Risk Factors, Ticlopidine adverse effects, Young Adult, Myocardial Infarction chemically induced, Proton Pump Inhibitors adverse effects, Ticlopidine analogs & derivatives

Abstract

Background and Aims: Proton pump inhibitors (PPIs) have been associated with adverse clinical outcomes amongst clopidogrel users after an acute coronary syndrome. Recent pre-clinical results suggest that this risk might extend to subjects without any prior history of cardiovascular disease. We explore this potential risk in the general population via data-mining approaches., Methods: Using a novel approach for mining clinical data for pharmacovigilance, we queried over 16 million clinical documents on 2.9 million individuals to examine whether PPI usage was associated with cardiovascular risk in the general population., Results: In multiple data sources, we found gastroesophageal reflux disease (GERD) patients exposed to PPIs to have a 1.16 fold increased association (95% CI 1.09-1.24) with myocardial infarction (MI). Survival analysis in a prospective cohort found a two-fold (HR = 2.00; 95% CI 1.07-3.78; P = 0.031) increase in association with cardiovascular mortality. We found that this association exists regardless of clopidogrel use. We also found that H2 blockers, an alternate treatment for GERD, were not associated with increased cardiovascular risk; had they been in place, such pharmacovigilance algorithms could have flagged this risk as early as the year 2000., Conclusions: Consistent with our pre-clinical findings that PPIs may adversely impact vascular function, our data-mining study supports the association of PPI exposure with risk for MI in the general population. These data provide an example of how a combination of experimental studies and data-mining approaches can be applied to prioritize drug safety signals for further investigation.

Published

2015

44. Effects of hypertonic buffer composition on lymph node uptake and bioavailability of rituximab, after subcutaneous administration.

Author

Fathallah AM, Turner MR, Mager DE, and Balu-Iyer SV

Subjects

Animals, Antibodies, Monoclonal, Murine-Derived blood, Biological Availability, Buffers, Injections, Subcutaneous, Male, Mannitol pharmacology, Mice, Phosphoserine pharmacology, Rituximab, Sodium Chloride pharmacology, Tromethamine pharmacology, Antibodies, Monoclonal, Murine-Derived administration & dosage, Antibodies, Monoclonal, Murine-Derived pharmacokinetics, Hypertonic Solutions pharmacology, Lymph Nodes drug effects, Lymph Nodes metabolism

Abstract

The subcutaneous administration of biologics is highly desirable; however, incomplete bioavailability after s.c. administration remains a major challenge. In this work we investigated the effects of excipient dependent hyperosmolarity on lymphatic uptake and plasma exposure of rituximab as a model protein. Using Swiss Webster (SW) mice as the animal model, we compared the effects of NaCl, mannitol and O-phospho-L-serine (OPLS) on the plasma concentration of rituximab over 5 days after s.c. administration. An increase was observed in plasma concentrations in animals administered rituximab in hypertonic buffer solutions, compared with isotonic buffer. Bioavailability, as estimated by our pharmacokinetic model, increased from 29% in isotonic buffer to 54% in hypertonic buffer containing NaCl, to almost complete bioavailability in hypertonic buffers containing high dose OPLS or mannitol. This improvement in plasma exposure is due to the improved lymphatic trafficking as evident from the increase in the fraction of dose trafficked through the lymph nodes in the presence of hypertonic buffers. The fraction of the dose trafficked through the lymphatics, as estimated by the model, increased from 0.05% in isotonic buffer to 13% in hypertonic buffer containing NaCl to about 30% for hypertonic buffers containing high dose OPLS and mannitol. The data suggest that hypertonic solutions may be a viable option for improving s.c. bioavailability., (Copyright © 2014 John Wiley & Sons, Ltd.)

Published

2015

45. Anatomical, physiological, and experimental factors affecting the bioavailability of sc-administered large biotherapeutics.

Author

Fathallah AM and Balu-Iyer SV

Subjects

Biological Availability, Biological Products metabolism, Humans, Injections, Subcutaneous, Biological Products administration & dosage, Biological Products pharmacokinetics, Biological Therapy

Abstract

Subcutaneous route of administration is highly desirable for protein therapeutics. It improves patient compliance and quality of life (McDonald TA, Zepeda ML, Tomlinson MJ, Bee WH, Ivens IA. 2010. Curr Opin Mol Ther 12(4):461-470; Dychter SS, Gold DA, Haller MF. 2012. J Infus Nurs 35(3):154-160), while reducing healthcare cost (Dychter SS, Gold DA, Haller MF. 2012. J Infus Nurs 35(3):154-160). Recent evidence also suggests that sc administration of protein therapeutics can increase tolerability to some treatments such as intravenous immunoglobulin therapy by administering it subcutaneously (subcutaneous immunoglobulin therapy SCIG), which will reduce fluctuation in plasma drug concentration (Kobrynski L. 2012. Biologics 6:277-287). Furthermore, sc administration may reduce the risk of systemic infections associated with i.v. infusion (McDonald TA, Zepeda ML, Tomlinson MJ, Bee WH, Ivens IA. 2010. Curr Opin Mol Ther 12(4):461-470; Dychter SS, Gold DA, Haller MF. 2012. J Infus Nurs 35(3):154-160). This route, however, has its challenges, especially for large multidomain proteins. Poor bioavailability and poor scalability from preclinical models are often cited. This commentary will discuss barriers to sc absorption as well as physiological and experimental factors that could affect pharmacokinetics of subcutaneously administered large protein therapeutics in preclinical models. A mechanistic pharmacokinetic model is proposed as a potential tool to address the issue of scalability of sc pharmacokinetic from preclinical models to humans., (© 2014 Wiley Periodicals, Inc. and the American Pharmacists Association.)

Published

2015

46. Soy phosphatidylinositol containing nanoparticle prolongs hemostatic activity of B-domain deleted factor VIII in hemophilia A mice.

Author

Shetty KA, Kosloski MP, Mager DE, and Balu-Iyer SV

Subjects

Animals, Factor VIII administration & dosage, Factor VIII pharmacokinetics, Hemostatics administration & dosage, Hemostatics pharmacokinetics, Hemostatics pharmacology, Injections, Intravenous, Male, Mice, Mice, Inbred C57BL, Nanoparticles administration & dosage, Nanoparticles chemistry, Peptide Fragments administration & dosage, Peptide Fragments pharmacokinetics, Phosphatidylinositols administration & dosage, Phosphatidylinositols pharmacokinetics, Phosphatidylinositols therapeutic use, Factor VIII pharmacology, Factor VIII therapeutic use, Hemophilia A drug therapy, Hemostatics therapeutic use, Nanoparticles therapeutic use, Peptide Fragments pharmacology, Peptide Fragments therapeutic use, Phosphatidylinositols pharmacology, Glycine max chemistry

Abstract

Factor VIII (FVIII) replacement therapy in hemophilia A (HA) is complicated by a short half-life and high incidence of inhibitory antibody response against the protein. Phosphatidylinositol (PI) containing lipidic nanoparticles have previously been shown to reduce the immunogenicity and prolong the half-life of full length FVIII. It has not been established whether this prolongation in half-life improves hemostatic efficacy and whether this approach could be extended to the B-domain deleted form of FVIII (BDD FVIII). In the current study, we evaluated the pharmacokinetics (PK), hemostatic efficacy, and immunogenicity of BDD FVIII associated with PI nanoparticles (PI-BDD FVIII) in HA mice. Comparative human PK was predicted using an "informed scaling" approach. PI-BDD FVIII showed an approximate 1.5-fold increase in terminal half-life compared with free BDD FVIII following i.v. bolus doses of 40 IU/kg. PI-BDD FVIII-treated animals retained hemostatic efficacy longer than the free FVIII-treated group in a tail vein transection model of hemostasis. PI association reduced the development of inhibitory and binding antibodies against BDD FVIII after a series of i.v. injections. The combined improvements in circulating half-life and hemostatic efficacy could significantly prolong the time above clinically established therapeutic thresholds of prophylactic FVIII replacement therapy in humans., (© 2014 Wiley Periodicals, Inc. and the American Pharmacists Association.)

Published

2015

47. Intravenous administration of Factor VIII-O-Phospho-L-Serine (OPLS) complex reduces immunogenicity and preserves pharmacokinetics of the therapeutic protein.

Author

Gaitonde P, Purohit VS, and Balu-Iyer SV

Subjects

Administration, Intravenous, Animals, Area Under Curve, Factor VIII administration & dosage, Half-Life, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Phosphoserine administration & dosage, T-Lymphocyte Subsets, Factor VIII chemistry, Factor VIII immunology, Hemophilia A therapy, Phosphoserine analogs & derivatives, Phosphoserine pharmacology

Abstract

Hemophilia A is a bleeding disorder caused by the deficiency of an important coagulation factor; Factor VIII (FVIII). Replacement therapy using exogenously administered recombinant FVIII is the most commonly used method of treatment. However, approximately 30% of Hemophilia A patients develop neutralizing antibodies (Nabs) against the recombinant protein. Nabs abolish FVIII activity and drastically influence efficacy of the protein. The immunogenic epitopes of FVIII reside predominantly in the C2 domain of FVIII. However, the C2 domain also contains a lipid binding region. O-Phospho-L-Serine (OPLS) which is the head-group moiety of phosphatidylserine, interacts with the lipid binding region of FVIII. Previous studies have shown that FVIII complexed with OPLS lowered Nab development against FVIII following subcutaneous administration. In dendritic cell-T-cell co-culture studies, OPLS treatment increased the secretion of immunosuppressive cytokines (Transforming Growth Factor-β and Interleukin-10), and simultaneously decreased pro-inflammatory IL-17 cytokine. Here, we investigated FVIII immune response and pharmacokinetics upon intravenous administration of FVIII-OPLS complex. We studied the effect of FVIII-OPLS complex on the interaction between a professional antigen presenting cell; dendritic cell and T-cell, and T-cell clonal expansion. Pharmacokinetics parameters were estimated following intravenous administration of FVIII and FVIII-OPLS. The results suggest that OPLS lowers FVIII immune response following intravenous administration. OPLS also hinders FVIII-specific T-cell clonal proliferation and preserves FVIII PK profile. Thus, the ease of protein-lipid complexation, preservation of FVIII activity and in vivo behavior, and improved in vitro FVIII stability, makes OPLS an attractive excipient in the preparation of next generation or biosimilar FVIII products with improved safety profile., (Copyright © 2014 Elsevier B.V. All rights reserved.)

Published

2015

48. Clinical profile and mutation analysis of xeroderma pigmentosum in Indian patients.

Author

Tamhankar PM, Iyer SV, Ravindran S, Gupta N, Kabra M, Nayak C, Kura M, Sanghavi S, Joshi R, Chennuri VS, and Khopkar U

Subjects

Adult, Child, Child, Preschool, DNA Mutational Analysis, Female, Homozygote, Humans, India, Male, Xeroderma Pigmentosum complications, DNA Helicases genetics, DNA-Binding Proteins genetics, Intellectual Disability genetics, Xeroderma Pigmentosum genetics, Xeroderma Pigmentosum Group A Protein genetics

Abstract

Background: Xeroderma pigmentosum (XP) is an autosomal recessive genetic disorder characterized by cutaneous and ocular photosensitivity and an increased risk of developing cutaneous neoplasms. Progressive neurological abnormalities develop in a quarter of XP patients., Aim: To study the clinical profile and perform a mutation analysis in Indian patients with xeroderma pigmentosum., Methods: Ten families with 13 patients with XP were referred to our clinic over 2 years. The genes XPA, XPB and XPC were sequentially analyzed till a pathogenic mutation was identified., Results: Homozygous mutations in the XPA gene were seen in patients with moderate to severe mental retardation (6/10 families) but not in those without neurological features. Two unrelated families with a common family name and belonging to the same community from Maharashtra were found to have an identical mutation in the XPA gene, namely c.335&#95;338delTTATinsCATAAGAAA (p.F112SfsX2). Testing of the XPC gene in two families with four affected children led to the identification of the novel mutations c.1243C>T or p.R415X and c.1677C>A or p.Y559X. In two families, mutations could not be identified in XPA, XPB and XPC genes., Limitation: The sample size is small., Conclusion: Indian patients who have neurological abnormalities associated with XP should be screened for mutations in the XPA gene.

Published

2015

49. O-phospho-l-serine mediates hyporesponsiveness toward FVIII in hemophilia A-murine model by inducing tolerogenic properties in dendritic cells.

Author

Fathallah AM, Ramakrishnan R, and Balu-Iyer SV

Subjects

Animals, Antibodies blood, CD40 Antigens metabolism, Cells, Cultured, Coagulants immunology, Dendritic Cells immunology, Dendritic Cells metabolism, Disease Models, Animal, Factor VIII immunology, Hemophilia A blood, Hemophilia A genetics, Hemophilia A immunology, Interleukin-12 metabolism, Mice, Transgenic, Time Factors, Transforming Growth Factor beta metabolism, Tumor Necrosis Factor-alpha metabolism, Adjuvants, Immunologic pharmacology, Coagulants pharmacology, Dendritic Cells drug effects, Factor VIII pharmacology, Hemophilia A drug therapy, Immune Tolerance drug effects, Phosphoserine pharmacology

Abstract

The clinical use of therapeutic proteins can be complicated by the development of anti-product antibodies. We have previously observed that O-phospho-l-serine (OPLS) reduced antibody response to FVIII in Hemophilia-A (HA) mice. However, the mechanism underlying this observation is not clear. We hypothesize that OPLS reduces immunogenicity by inducing tolerogenic properties in dendritic cells (DCs). We tested this hypothesis using in vivo, in vitro, and ex vivo methods. Naive HA mice that were pre-exposed to FVIII in the presence of OPLS showed substantially lower antibody response following rechallenge with OPLS free FVIII as compared with dexamethasone-pretreated mice. Exposure of OPLS to bone-marrow-derived dendritic cells (BMDCs) in culturing conditions resulted in an increase in the regulatory cytokine TGF-β and a decrease in proinflammatory cytokines TNF-α and IL12p70. This was accompanied by a significant reduction in upregulation of costimulatory marker CD40, as measured by flow cytometry. Furthermore, ex vivo matured BMDCs in the presence of FVIII and OPLS failed to elicit a robust immune response in HA mice compared with FVIII-treated BMDCs. Our data suggest that OPLS modulates the immune response by altering the function and maturation of DCs, resulting in the induction of tolerogenic properties. © 2014 Wiley Periodicals, Inc. and the American Pharmacists Association J Pharm Sci 103:3457-3463, 2014., (© 2014 Wiley Periodicals, Inc. and the American Pharmacists Association.)

Published

2014

50. Toward personalizing treatment for depression: predicting diagnosis and severity.

Author

Huang SH, LePendu P, Iyer SV, Tai-Seale M, Carrell D, and Shah NH

Subjects

Depressive Disorder classification, Diagnosis, Differential, Female, Humans, Male, Models, Psychological, Precision Medicine, ROC Curve, Severity of Illness Index, Depressive Disorder diagnosis, Electronic Health Records

Abstract

Objective: Depression is a prevalent disorder difficult to diagnose and treat. In particular, depressed patients exhibit largely unpredictable responses to treatment. Toward the goal of personalizing treatment for depression, we develop and evaluate computational models that use electronic health record (EHR) data for predicting the diagnosis and severity of depression, and response to treatment., Materials and Methods: We develop regression-based models for predicting depression, its severity, and response to treatment from EHR data, using structured diagnosis and medication codes as well as free-text clinical reports. We used two datasets: 35,000 patients (5000 depressed) from the Palo Alto Medical Foundation and 5651 patients treated for depression from the Group Health Research Institute., Results: Our models are able to predict a future diagnosis of depression up to 12 months in advance (area under the receiver operating characteristic curve (AUC) 0.70-0.80). We can differentiate patients with severe baseline depression from those with minimal or mild baseline depression (AUC 0.72). Baseline depression severity was the strongest predictor of treatment response for medication and psychotherapy., Conclusions: It is possible to use EHR data to predict a diagnosis of depression up to 12 months in advance and to differentiate between extreme baseline levels of depression. The models use commonly available data on diagnosis, medication, and clinical progress notes, making them easily portable. The ability to automatically determine severity can facilitate assembly of large patient cohorts with similar severity from multiple sites, which may enable elucidation of the moderators of treatment response in the future., (Published by the BMJ Publishing Group Limited. For permission to use (where not already granted under a licence) please go to http://group.bmj.com/group/rights-licensing/permissions.)

Published

2014