Your search keyword '"Santulli-Marotto S"' showing total 15 results

1. Immunologic signatures of response and resistance to nivolumab with ipilimumab in advanced metastatic cancer.

Author

Tsimberidou AM, Alayli FA, Okrah K, Drakaki A, Khalil DN, Kummar S, Khan SA, Hodi FS, Oh DY, Cabanski CR, Gautam S, Meier SL, Amouzgar M, Pfeiffer SM, Kageyama R, Yang E, Spasic M, Tetzlaff MT, Foo WC, Hollmann TJ, Li Y, Adamow M, Wong P, Moore JS, Velichko S, Chen RO, Kumar D, Bucktrout S, Ibrahim R, Dugan U, Salvador L, Hubbard-Lucey VM, O'Donnell-Tormey J, Santulli-Marotto S, Butterfield LH, Da Silva DM, Fairchild J, LaVallee TM, Padrón LJ, and Sharma P

Subjects

Adult, Aged, Female, Humans, Male, Middle Aged, Immune Checkpoint Inhibitors therapeutic use, Immune Checkpoint Inhibitors pharmacology, Neoplasm Metastasis, Neoplasms drug therapy, Neoplasms immunology, Neoplasms pathology, Tumor Microenvironment immunology, CD8-Positive T-Lymphocytes immunology, CD8-Positive T-Lymphocytes drug effects, Drug Resistance, Neoplasm, Ipilimumab therapeutic use, Nivolumab therapeutic use, Nivolumab administration & dosage

Abstract

Identifying pan-tumor biomarkers that predict responses to immune checkpoint inhibitors (ICI) is critically needed. In the AMADEUS clinical trial (NCT03651271), patients with various advanced solid tumors were assessed for changes in intratumoral CD8 percentages and their response to ICI. Patients were grouped based on tumoral CD8 levels: those with CD8 <15% (CD8-low) received nivolumab (anti-PD-1) plus ipilimumab (anti-CTLA4) and those with CD8 ≥15% (CD8-high) received nivolumab monotherapy. 79 patients (72 CD8-low and 7 CD8-high) were treated. The disease control rate was 25.0% (18/72; 95% CI: 15.8-35.2) in CD8-low and 14.3% (1/7; 95% CI: 1.1-43.8) in CD8-high. Tumors from 35.9% (14/39; 95% CI: 21.8-51.4) of patients converted from CD8 <15% pretreatment to ≥15% after treatment. Multiomic analyses showed that CD8-low responders had an inflammatory tumor microenvironment pretreatment, enhanced by an influx of CD8 T cells, CD4 T cells, B cells, and macrophages upon treatment. These findings reveal crucial pan-cancer immunological features for ICI response in patients with metastatic disease., (© 2024 Tsimberidou et al.)

Published

2024

2. Characterization of a Novel Bispecific Antibody That Activates T Cells In Vitro and Slows Tumor Growth In Vivo .

Author

Chornoguz O, Leettola CN, Leander K, Brosnan K, Emmell E, Chiu ML, and Santulli-Marotto S

Subjects

Animals, CD3 Complex genetics, CD8-Positive T-Lymphocytes immunology, Cell Proliferation genetics, Epithelial Cell Adhesion Molecule genetics, Epithelial Cell Adhesion Molecule immunology, Humans, Immunoglobulin Fc Fragments immunology, Mice, Neoplasms therapy, Signal Transduction immunology, Antibodies, Bispecific immunology, CD3 Complex immunology, Neoplasms immunology, T-Lymphocytes immunology

Abstract

Although CD3 T cell redirecting antibodies have been successfully utilized for the treatment of hematological malignancies (blinatumomab), the T cell signaling pathways induced by these molecules are incompletely understood. To gain insight into the mechanism of action for T cell redirection antibodies, we created a novel murine CD3xEpCAM bispecific antibody that incorporates a silent Fc to dissect function and signaling of murine CD8 OT1 T cells upon stimulation. T cell-mediated cytotoxicity, cytokine secretion, expression of activation markers, and proliferation were directly induced in T cells treated with the novel CD3xEpCAM bispecific molecule in vitro in the presence of epithelial cell adhesion molecule (EpCAM) expressing tumor cells. Nanostring analysis showed that CD3xEpCAM induced a gene expression profile that resembled antigen-mediated activation, although the magnitude was lower than that of the antigen-induced response. In addition, this CD3xEpCAM bispecific antibody exhibited in vivo efficacy. This is the first study that investigates both in vitro and in vivo murine CD8 T cell function and signaling induced by a CD3xEpCAM antibody having a silent Fc to delineate differences between antigen-independent and antigen-specific T cell activation. These findings expand the understanding of T cell function and signaling induced by CD3 redirection bispecific antibodies and may help to develop more efficacious CD3 redirection therapeutics for cancer treatment, particularly for solid tumors.

Published

2019

3. TIM-3 Engagement Promotes Effector Memory T Cell Differentiation of Human Antigen-Specific CD8 T Cells by Activating mTORC1.

Author

Sabins NC, Chornoguz O, Leander K, Kaplan F, Carter R, Kinder M, Bachman K, Verona R, Shen S, Bhargava V, and Santulli-Marotto S

Subjects

Antibodies, Monoclonal pharmacology, Cell Division, Cells, Cultured, Gene Expression Profiling, Gene Expression Regulation immunology, Humans, Lymphocyte Activation, Lymphokines biosynthesis, Lymphokines genetics, MART-1 Antigen immunology, Phosphorylation, Protein Processing, Post-Translational, T-Cell Antigen Receptor Specificity, ras Proteins biosynthesis, ras Proteins genetics, Antigens immunology, CD8-Positive T-Lymphocytes immunology, Hepatitis A Virus Cellular Receptor 2 immunology, Immunologic Memory immunology, Mechanistic Target of Rapamycin Complex 1 immunology

Abstract

T cell expression of TIM-3 following Ag encounter has been associated with a continuum of functional states ranging from effector memory T cells to exhaustion. We have designed an in vitro culture system to specifically address the impact of anti-TIM-3/TIM-3 engagement on human Ag-specific CD8 T cells during a normal response to Ag and found that anti-TIM-3 treatment enhances T cell function. In our in vitro T cell culture system, MART1-specific CD8 T cells were expanded from healthy donors using artificial APCs. To ensure that the T cells were the only source of TIM-3, cells were rechallenged with peptide-loaded artificial APCs in the presence of anti-TIM-3 Ab. In these conditions, anti-TIM-3 treatment promotes generation of effector T cells as shown by acquisition of an activated phenotype, increased cytokine production, enhanced proliferation, and a transcription program associated with T cell differentiation. Activation of mTORC1 has been previously demonstrated to enhance CD8 T cell effector function and differentiation. Anti-TIM-3 drives CD8 T cell differentiation through activation of the mTORC1 as evidenced by increased levels of phosphorylated S6 protein and rhebl1 transcript. Altogether these findings suggest that anti-TIM-3, together with Ag, drives differentiation in favor of effector T cells via the activation of mTOR pathway. To our knowledge, this is the first report demonstrating that TIM-3 engagement during Ag stimulation directly influences T cell differentiation through mTORC1., (Copyright © 2017 by The American Association of Immunologists, Inc.)

Published

2017

4. Differential Expression of Immune Checkpoint Modulators on In Vitro Primed CD4(+) and CD8(+) T Cells.

Author

Sabins NC, Harman BC, Barone LR, Shen S, and Santulli-Marotto S

Abstract

PD-1, TIM-3, and LAG-3 are molecules shown to have immune modulatory properties, and although initially classified as indicators of T cell hyporesponsiveness, it has become clear that they are also associated with the normal course of T cell activation. Functional studies have focused mainly on CD8(+) T cells during chronic inflammation due to interest in co-opting the cellular immune response to eliminate viral or cancerous threats; however, there remains a relative lack of data regarding the expression of these molecules on CD4(+) T cells. Here, we report that expression of the immune checkpoint (IC) molecules PD-1, LAG-3, and TIM-3 are differentially expressed on CD4(+) and CD8(+) T cells in the allogeneic response resulting from a mixed lymphocyte reaction. In these studies, PD-1 expression is higher on CD4(+) T cells compared to CD8(+) T cells. In contrast, TIM-3 is expressed at higher levels on CD8(+) T cells compared to CD4(+) T cells with an apparent reciprocity in that PD-1(+) CD4(+) T cells are frequently TIM-3(lo/-), while TIM-3-expressing CD8(+) T cells are largely PD-1(lo/-). In addition, there is a decrease in the frequency of TIM-3(+) CD4(+) cells producing IFN-γ and IL-5 compared to TIM-3(+) CD8(+) cells. Lastly, the memory T cell phenotype within each IC-expressing subset differs between CD4(+) and CD8(+) T cells. These findings highlight key differences in IC expression patterns between CD4(+) and CD8(+) T cells and may allow for more effective therapeutic targeting of these molecules in the future.

Published

2016

5. Human umbilical tissue-derived cells rescue retinal pigment epithelium dysfunction in retinal degeneration.

Author

Cao J, Murat C, An W, Yao X, Lee J, Santulli-Marotto S, Harris IR, and Inana G

Subjects

Animals, Coculture Techniques, Disease Models, Animal, Eye Proteins biosynthesis, Humans, Rats, Retinal Degeneration pathology, Retinal Pigment Epithelium pathology, Umbilical Cord pathology, Umbilical Cord transplantation, Retinal Degeneration metabolism, Retinal Degeneration therapy, Retinal Pigment Epithelium metabolism, Umbilical Cord metabolism

Abstract

Retinal pigment epithelium (RPE) cells perform many functions crucial for retinal preservation and vision. RPE cell dysfunction results in various retinal degenerative diseases, such as retinitis pigmentosa and age-related macular degeneration (AMD). Currently, there are no effective treatments for retinal degeneration except for a small percentage of individuals with exudative AMD. Cell therapies targeting RPE cells are being developed in the clinic for the treatment of retinal degeneration. Subretinal injection of human umbilical tissue-derived cells (hUTC) in the Royal College of Surgeons (RCS) rat model of retinal degeneration was shown to preserve photoreceptors and visual function. However, the precise mechanism remains unclear. Here, we demonstrate that hUTC rescue phagocytic dysfunction in RCS RPE cells in vitro. hUTC secrete receptor tyrosine kinase (RTK) ligands brain-derived neurotrophic factor (BDNF), hepatocyte growth factor (HGF), and glial cell-derived neurotrophic factor (GDNF), as well as opsonizing bridge molecules milk-fat-globule-epidermal growth factor 8 (MFG-E8), growth arrest-specific 6 (Gas6), thrombospondin (TSP)-1, and TSP-2. The effect of hUTC on phagocytosis rescue in vitro is mimicked by recombinant human proteins of these factors and is abolished by siRNA-targeted gene silencing in hUTC. The bridge molecules secreted from hUTC bind to the photoreceptor outer segments and facilitate their ingestion by the RPE. This study elucidates novel cellular mechanisms for the repair of RPE function in retinal degeneration through RTK ligands and bridge molecules, and demonstrates the potential of using hUTC for the treatment of retinal degenerative diseases., (© 2015 AlphaMed Press.)

Published

2016

6. Discovering Molecules That Regulate Efferocytosis Using Primary Human Macrophages and High Content Imaging.

Author

Santulli-Marotto S, Gervais A, Fisher J, Strake B, Ogden CA, Riveley C, and Giles-Komar J

Subjects

Animals, Antibodies classification, Cells, Cultured, Humans, Mice, Mice, Inbred BALB C, Proto-Oncogene Proteins genetics, Proto-Oncogene Proteins immunology, Receptor Protein-Tyrosine Kinases genetics, Receptor Protein-Tyrosine Kinases immunology, c-Mer Tyrosine Kinase, Antibodies immunology, Apoptosis, Macrophages immunology, Phagocytosis

Abstract

Defective clearance of apoptotic cells can result in sustained inflammation and subsequent autoimmunity. Macrophages, the "professional phagocyte" of the body, are responsible for efficient, non-phlogistic, apoptotic cell clearance. Controlling phagocytosis of apoptotic cells by macrophages is an attractive therapeutic opportunity to ameliorate inflammation. Using high content imaging, we have developed a system for evaluating the effects of antibody treatment on apoptotic cell uptake in primary human macrophages by comparing the Phagocytic Index (PI) for each antibody. Herein we demonstrate the feasibility of evaluating a panel of antibodies of unknown specificities obtained by immunization of mice with primary human macrophages and show that they can be distinguished based on individual PI measurements. In this study ~50% of antibodies obtained enhance phagocytosis of apoptotic cells while approximately 5% of the antibodies in the panel exhibit some inhibition. Though the specificities of the majority of antibodies are unknown, two of the antibodies that improved apoptotic cell uptake recognize recombinant MerTK; a receptor known to function in this capacity in vivo. The agonistic impact of these antibodies on efferocytosis could be demonstrated without addition of either of the MerTK ligands, Gas6 or ProS. These results validate applying the mechanism of this fundamental biological process as a means for identification of modulators that could potentially serve as therapeutics. This strategy for interrogating macrophages to discover molecules regulating apoptotic cell uptake is not limited by access to purified protein thereby increasing the possibility of finding novel apoptotic cell uptake pathways.

Published

2015

7. CCL22-specific Antibodies Reveal That Engagement of Two Distinct Binding Domains on CCL22 Is Required for CCR4-mediated Function.

Author

Santulli-Marotto S, Wheeler J, Lacy ER, Boakye K, Luongo J, Wu SJ, and Ryan M

Subjects

Animals, Antibodies, Monoclonal biosynthesis, Arrestins genetics, Binding Sites, Binding, Competitive, Cell Line, Chemokine CCL17 genetics, Chemokine CCL17 immunology, Chemokine CCL22 genetics, Dendritic Cells cytology, Dendritic Cells immunology, Epitopes chemistry, Epitopes genetics, Gene Expression Regulation, Humans, Immunity, Innate, Mice, Protein Binding, Protein Structure, Tertiary, Receptors, CCR4 genetics, Signal Transduction, T-Lymphocytes cytology, T-Lymphocytes immunology, beta-Arrestins, Antibodies, Monoclonal chemistry, Arrestins immunology, Chemokine CCL22 immunology, Epitopes immunology, Receptors, CCR4 immunology

Abstract

CCL22 inactivation in vivo occurs by cleavage at the N-terminus; however, it is unclear whether this encompasses the entire site of CCR4 interaction. CCL17 also binds CCR4 and its function requires binding via two discrete binding sites. Using monoclonal antibodies (MAbs), we report that there are two separate sites on CCL22 that are required for CCR4-mediated function. The CCL22-specific antibodies bind with affinities of 632 ± 297 pM (MC2B7) and 308 ± 43 pM (MAB4391) and neither exhibited detectable binding to CCL17. Both antibodies are comparable in their ability to inhibit CCL22-mediated calcium mobilization; however, competition binding studies demonstrate that MC2B7 and MAB4391 bind to distinct epitopes on CCL22. Both antibodies inhibit function through CCR4, which is demonstrated by loss of β-arrestin recruitment in a reporter cell line. In both assays, blocking either site independently abolished CCL22 function, suggesting that concurrent engagement of both sites with CCR4 is necessary for function. This is the first demonstration that CCL22 has two distinct binding sites that are required for CCR4 function. These antibodies are valuable tools for better understanding the interaction and function of CCL22 and CCR4 and will potentially help further understanding of the differential outcomes of CCL17 and CCL22 interaction with CCR4.

Published

2015

8. TIM-3 Suppresses Anti-CD3/CD28-Induced TCR Activation and IL-2 Expression through the NFAT Signaling Pathway.

Author

Tomkowicz B, Walsh E, Cotty A, Verona R, Sabins N, Kaplan F, Santulli-Marotto S, Chin CN, Mooney J, Lingham RB, Naso M, and McCabe T

Subjects

Calcium metabolism, Cell Differentiation, Cells, Cultured, Cytokines metabolism, Genes, Reporter, Hepatitis A Virus Cellular Receptor 2, Humans, Lymphocyte Activation immunology, Membrane Proteins chemistry, NF-kappa B metabolism, Promoter Regions, Genetic genetics, Protein Structure, Tertiary, T-Lymphocytes cytology, T-Lymphocytes metabolism, Antigens, CD metabolism, Interleukin-2 metabolism, Membrane Proteins metabolism, NFATC Transcription Factors metabolism, Receptors, Antigen, T-Cell metabolism, Signal Transduction

Abstract

TIM-3 (T cell immunoglobulin and mucin-domain containing protein 3) is a member of the TIM family of proteins that is preferentially expressed on Th1 polarized CD4+ and CD8+ T cells. Recent studies indicate that TIM-3 serves as a negative regulator of T cell function (i.e. T cell dependent immune responses, proliferation, tolerance, and exhaustion). Despite having no recognizable inhibitory signaling motifs, the intracellular tail of TIM-3 is apparently indispensable for function. Specifically, the conserved residues Y265/Y272 and surrounding amino acids appear to be critical for function. Mechanistically, several studies suggest that TIM-3 can associate with interleukin inducible T cell kinase (ITK), the Src kinases Fyn and Lck, and the p85 phosphatidylinositol 3-kinase (PI3K) adaptor protein to positively or negatively regulate IL-2 production via NF-κB/NFAT signaling pathways. To begin to address this discrepancy, we examined the effect of TIM-3 in two model systems. First, we generated several Jurkat T cell lines stably expressing human TIM-3 or murine CD28-ECD/human TIM-3 intracellular tail chimeras and examined the effects that TIM-3 exerts on T cell Receptor (TCR)-mediated activation, cytokine secretion, promoter activity, and protein kinase association. In this model, our results demonstrate that TIM-3 inhibits several TCR-mediated phenotypes: i) NF-kB/NFAT activation, ii) CD69 expression, and iii) suppression of IL-2 secretion. To confirm our Jurkat cell observations we developed a primary human CD8+ cell system that expresses endogenous levels of TIM-3. Upon TCR ligation, we observed the loss of NFAT reporter activity and IL-2 secretion, and identified the association of Src kinase Lck, and PLC-γ with TIM-3. Taken together, our results support the conclusion that TIM-3 is a negative regulator of TCR-function by attenuating activation signals mediated by CD3/CD28 co-stimulation.

Published

2015

9. Isolation and optimization for affinity and biophysical characteristics of anti-CCL17 antibodies from the VH1-69 germline gene.

Author

Kehoe JW, Whitaker B, Bethea D, Lacy ER, Boakye K, Santulli-Marotto S, Ryan MH, Feng Y, and Wheeler JC

Subjects

Animals, Antibody Affinity, Calcium Signaling, Cell Line, Humans, Immunoglobulin G chemistry, Immunoglobulin G genetics, Immunoglobulin G isolation & purification, Immunoglobulin Heavy Chains chemistry, Immunoglobulin Heavy Chains isolation & purification, Macaca fascicularis, Peptide Library, Protein Binding, Protein Engineering, Chemokine CCL17 immunology, Immunoglobulin Heavy Chains genetics

Abstract

CCL17 is a homeostatic chemokine associated with several human inflammatory pathologies. This makes CCL17 a potential point of intervention in inflammatory diseases. Using a Fab-pIX phage display system we were able to select antibodies that specifically bind to CCL17 and neutralize CCL17-mediated signaling. Many of the selected antibodies belong to the VH1-69 germline gene family. The VH1-69 germline gene is represented at a high frequency in the human antibody repertoire and is seen in the early immune response to a variety of pathogens. The heavy chain CDR2 of this germline gene is notably hydrophobic and can insert into hydrophobic pockets of antigens, providing much of the binding energy for these antibodies. Affinity maturation of our primary binders by light chain mutagenesis produced antibodies with sub-nanomolar affinities, with affinity improvements up to 100-fold. These were screened for non-specific protein-protein interactions as a filter for solubility. All of our high affinity antibodies were found to have high levels of non-specific protein-protein interactions. We speculated that this was due to the hydrophobicity within the germline heavy chain CDR1 and CDR2. To ameliorate this problem, we generated a phage display library for one of the clones, where the surface-exposed residues within H-CDR1 and H-CDR2 were randomized. High stringency panning of this library against human CCL17 resulted in further affinity improvement, along with reduction in protein-protein interaction in some new variants. In addition, we improved the cross-reactivity to cynomolgus CCL17. We demonstrate that affinity maturation through targeted libraries in the VH1-69 germline gene can improve both affinity and biophysical characteristics of antibodies derived from this gene scaffold., (© The Author 2014. Published by Oxford University Press. All rights reserved. For Permissions, please e-mail: journals.permissions@oup.com.)

Published

2014

10. Engagement of two distinct binding domains on CCL17 is required for signaling through CCR4 and establishment of localized inflammatory conditions in the lung.

Author

Santulli-Marotto S, Boakye K, Lacy E, Wu SJ, Luongo J, Kavalkovich K, Coelho A, Hogaboam CM, and Ryan M

Subjects

Animals, Antibodies, Neutralizing immunology, Chemokine CCL17 immunology, Chemokine CCL22 metabolism, Female, Mice, Protein Binding, Protein Structure, Tertiary, Chemokine CCL17 chemistry, Chemokine CCL17 metabolism, Lung metabolism, Lung pathology, Receptors, CCR4 metabolism, Signal Transduction

Abstract

CCL17 (TARC) function can be completely abolished by mAbs that block either one of two distinct sites required for CCR4 signaling. This chemokine is elevated in sera of asthma patients and is responsible for establishing inflammatory sites through CCR4-mediated recruitment of immune cells. CCL17 shares the GPCR CCR4, with CCL22 (MDC) but these two chemokines differentially affect the immune response. To better understand chemokine mediated effects through CCR4, we have generated chimeric anti-mouse CCL17 surrogate antibodies that inhibit function of this ligand in vitro and in vivo. The affinities of the surrogate antibodies for CCL17 range from 685 pM for B225 to 4.9 nM for B202. One antibody, B202, also exhibits weak binding to CCL22 (KD∼2 µM) and no binding to CCL22 is detectable with the second antibody, B225. In vitro, both antibodies inhibit CCL17-mediated calcium mobilization, β-arrestin recruitment and chemotaxis; B202 can also partially inhibit CCL22-mediated β-arrestin recruitment. Both B202 and B225 antibodies neutralize CCL17 in vivo as demonstrated by reduction of methacholine-induced airway hyperreactivity in the A. fumigatus model of asthma. That both antibodies block CCL17 function but only B202 shows any inhibition of CCL22 function suggests that they bind CCL17 at different sites. Competition binding studies confirm that these two antibodies recognize unique epitopes that are non-overlapping despite the small size of CCL17. Taking into consideration the data from both the functional and binding studies, we propose that effective engagement of CCR4 by CCL17 involves two distinct binding domains and interaction with both is required for signaling.

Published

2013

11. Surrogate antibodies that specifically bind and neutralize CCL17 but not CCL22.

Author

Santulli-Marotto S, Fisher J, Petley T, Boakye K, Panavas T, Luongo J, Kavalkovich K, Rycyzyn M, Wu B, Gutshall L, Coelho A, Hogaboam CM, and Ryan M

Subjects

Animals, Antibody Affinity immunology, Arrestins immunology, Cell Line, Chemotaxis immunology, Humans, Rats, beta-Arrestins, Antibodies, Neutralizing immunology, Chemokine CCL17 immunology, Chemokine CCL22 immunology, Receptors, CCR4 immunology

Abstract

The chemokines CCL17 (TARC) and CCL22 (MDC) function through the same receptor, CCR4, but have been proposed to differentially affect the immune response. To better understand the role of the individual ligands, a panel of rat anti-mouse CCL17 surrogate antibodies was generated that can be used to differentiate CCL17 and CCL22 function in vitro and in vivo. We have successfully identified a panel of neutralizing antibodies by screening hybridomas for the ability to inhibit CCL17-mediated calcium mobilization. Chemotaxis in response to CCL17 is also inhibited, providing further evidence that the antibodies in this panel are antagonistic. Using a recombinant cell line expressing human CCR4, we show that the antibodies block β-arrestin recruitment as evidence that the antibodies are specifically blocking CCL17 signaling through CCR4. The antibodies within this panel inhibit calcium mobilization with varying potency in the calcium flux assay, having apparent IC50 ranging from approximately 1 to >400 ng/mL. Although both CCL17 and CCL22 function through CCR4, only a single antibody was identified as having detectable binding to CCL22. This panel of CCL17-specific antibodies provides tools that can be used to differentiate CCL17 and CCL22 function through CCR4 interaction in vitro and in vivo.

Published

2013

12. Multivalent RNA aptamers that inhibit CTLA-4 and enhance tumor immunity.

Author

Santulli-Marotto S, Nair SK, Rusconi C, Sullenger B, and Gilboa E

Subjects

Animals, Antigens, CD, Antigens, Differentiation genetics, Antigens, Differentiation metabolism, Base Sequence, CTLA-4 Antigen, Cricetinae, Female, Melanoma, Experimental immunology, Melanoma, Experimental metabolism, Melanoma, Experimental therapy, Mice, Mice, Inbred BALB C, Mice, Inbred C3H, Mice, Inbred C57BL, Oligonucleotides genetics, Oligonucleotides immunology, Oligonucleotides metabolism, Oligonucleotides pharmacology, RNA genetics, RNA immunology, RNA metabolism, Antigens, Differentiation immunology, RNA pharmacology

Abstract

The potency of cancer immunotherapy can be enhanced by administration of high-avidity ligands specific to receptors expressed on T cells. Antibodies or cytokines are the main agents used in such capacity. Antibody-mediated inhibition of cytotoxic T cell antigen-4 (CTLA-4) function in mice augments antitumor immunity and could serve as an important adjunct in cancer immunotherapy. However, antibody-based therapy used in the setting of chronic diseases such as cancer poses significant cost, manufacturing, and regulatory challenges. Here we describe the development of RNA aptamers that bind CTLA-4 with high affinity and specificity. These aptamers inhibit CTLA-4 function in vitro and enhance tumor immunity in mice. Moreover, assembly of the aptamers into tetrameric forms significantly enhances their bioactivity in vitro and in vivo. These results demonstrate that aptamers can be used to manipulate the immune system for therapeutic applications and that multivalent versions of aptamers may be particularly potent agents in vivo.

Published

2003

13. Anti-Sm B cell differentiation in Ig transgenic MRL/Mp-lpr/lpr mice: altered differentiation and an accelerated response.

Author

Santulli-Marotto S, Qian Y, Ferguson S, and Clarke SH

Subjects

Aging genetics, Aging immunology, Animals, Antigens, Differentiation, B-Lymphocyte biosynthesis, Autoantibodies biosynthesis, Autoimmune Diseases genetics, B-Lymphocyte Subsets metabolism, Biomarkers, Cell Differentiation genetics, Cell Differentiation immunology, Dose-Response Relationship, Immunologic, Gene Expression Regulation immunology, Genes, bcl-2 immunology, Immunophenotyping, Mice, Mice, Inbred MRL lpr, Mice, Transgenic, Peritoneum cytology, Peritoneum immunology, Peritoneum metabolism, Spleen cytology, Spleen immunology, Spleen metabolism, Transgenes immunology, Up-Regulation genetics, Up-Regulation immunology, snRNP Core Proteins, Autoantigens immunology, B-Lymphocyte Subsets cytology, B-Lymphocyte Subsets immunology, Immunoglobulin Heavy Chains genetics, Lymphocyte Activation genetics, Ribonucleoproteins, Small Nuclear immunology

Abstract

To determine the regulation of B cells specific for the ribonucleoprotein Sm, a target of the immune system in human and mouse lupus, we have generated mice carrying an anti-Sm H chain transgene (2-12H). Anti-Sm B cells in nonautoimmune 2-12H-transgenic (Tg) mice are functional, but, in the absence of immunization, circulating anti-Sm Ab levels are not different from those of non-Tg mice. In this report, we compare the regulation of anti-Sm B cells in nonautoimmune and autoimmune MRL/Mp-lpr/lpr (MRL/lpr) and bcl-2-22-Tg mice. Activation markers are elevated on splenic and peritoneal anti-Sm B cells of both nonautoimmune and autoimmune genetic backgrounds indicating Ag encounter. Although tolerance to Sm is maintained in 2-12H/bcl-2-22-Tg mice, it is lost in 2-12H-Tg MRL/lpr mice, as the transgene accelerates and increases the prevalence of the anti-Sm response. The 2-12H-Tg MRL/lpr mice have transitional anti-Sm B cells in the spleen similar to nonautoimmune mice. However, in contrast to nonautoimmune mice, there are few if any peritoneal anti-Sm B-1 cells. These data suggest that a defect in B-1 differentiation may be a factor in the loss of tolerance to Sm and provide insight into the low prevalence of the anti-Sm response in lupus.

Published

2001

14. T cell autoimmunity in Ig transgenic mice.

Author

Shinde S, Gee R, Santulli-Marotto S, Bockenstedt LK, Clarke SH, and Mamula MJ

Subjects

Animals, Antigen Presentation, Autoantigens immunology, Autoantigens metabolism, B-Lymphocytes immunology, B-Lymphocytes metabolism, CD4-Positive T-Lymphocytes immunology, CD4-Positive T-Lymphocytes metabolism, Flow Cytometry, Histocompatibility Antigens Class II immunology, Histocompatibility Antigens Class II metabolism, Mice, Mice, Inbred C57BL, Mice, Inbred MRL lpr, Mice, Transgenic, Peptides immunology, Peptides metabolism, Receptors, Antigen, B-Cell metabolism, Ribonucleoproteins, Small Nuclear immunology, T-Lymphocytes metabolism, Genes, Immunoglobulin genetics, Lupus Erythematosus, Systemic genetics, Lupus Erythematosus, Systemic immunology, T-Lymphocytes immunology

Abstract

Autoantibodies directed at a diverse group of proteins of the U1/Sm ribonucleoprotein (snRNP) are characteristic of systemic lupus erythematosus and are found in the MRL murine model of this disease. This study examines the role of transgenic B lymphocytes in the regulation of autoreactive T cells to the snRNP autoantigen. Transgenic mice were developed bearing an Ig heavy chain gene specific for the D protein component of murine snRNP. B lymphocytes in these mice are neither deleted nor anergic and are of an immature (heat-stable Aghigh) phenotype. T lymphocytes from anti-snRNP transgenic mice were examined using a recombinant form of the D protein of the murine snRNP complex. Our results revealed that transgenic anti-snRNP B cell APCs stimulated CD4 T cells from wild-type C57BL/6 and MRL lpr/lpr mice, while nonspecific APCs failed to stimulate CD4 T cells. This study demonstrates that autoreactive T cells are not deleted from wild-type mice, although their activation is facilitated by autoantigen-specific APCs. The snRNP-reactive T cells in C57BL/6 transgenic mice are tolerized, in contrast to those T cells from MRL lpr/lpr transgenic mice. These studies implicate a role for autoreactive B lymphocytes in the in vivo activation and/or diversification of autoreactive T cells.

Published

1999

15. Autoreactive B cell regulation: peripheral induction of developmental arrest by lupus-associated autoantigens.

Author

Santulli-Marotto S, Retter MW, Gee R, Mamula MJ, and Clarke SH

Subjects

Animals, Autoantigens genetics, Bone Marrow immunology, Cell Differentiation, DNA, Single-Stranded immunology, Enzyme-Linked Immunosorbent Assay, Fluorescent Antibody Technique, Gene Rearrangement, B-Lymphocyte, Heavy Chain, Hematopoietic Stem Cells, Hybridomas, Immune Tolerance, Lupus Erythematosus, Systemic etiology, Lymphocyte Activation, Mice, Mice, Inbred MRL lpr, Mice, Transgenic, Ribonucleoproteins, Small Nuclear immunology, Spleen immunology, snRNP Core Proteins, Autoantigens immunology, B-Lymphocytes immunology, Lupus Erythematosus, Systemic immunology

Abstract

Anti-Sm and anti-ssDNA transgenic (Tg) mice were generated using the VH-D-JH rearrangement of an anti-Sm hybridoma of MRL/Mp-lpr/lpr origin. B cells of each specificity account for 15%-35% of the splenic repertoire, but no circulating anti-Sm or anti-ssDNA antibodies are detected. Most autoreactive cells exhibit an immature B cell phenotype and have short half-lives equivalent to those of non-Tg immature B cells. However, at least some anti-Sm B cells are functional, because immunization with murine snRNPs induces anti-Sm secretion. We propose that anti-Sm and anti-ssDNA are eliminated during the transition to mature B cells and that this late stage of tolerance induction is consequential to their spontaneous activation in murine lupus.

Published

1998