Your search keyword '"Perez, Victor"' showing total 10 results

1. The Immunological Basis of Dry Eye Disease and Current Topical Treatment Options

Author

Periman, Laura M, Perez, Victor L, Saban, Daniel R, Lin, Meng C, and Neri, Piergiorgio

Subjects

Biomedical and Clinical Sciences, Ophthalmology and Optometry, Pain Research, Eye Disease and Disorders of Vision, Aetiology, 2.1 Biological and endogenous factors, Eye, Inflammatory and immune system, Administration, Topical, Clinical Decision-Making, Cyclosporine, Dry Eye Syndromes, Goblet Cells, Homeostasis, Humans, Immunologic Factors, Immunosuppressive Agents, Inflammation, Integrins, Intercellular Adhesion Molecule-1, Lacrimal Apparatus, Lymphocyte Function-Associated Antigen-1, Phenylalanine, Steroids, Sulfones, T-Lymphocytes, Tears, dry eye disease, ocular surface, inflammation, immunology, immune dysregulation, T cells, goblet cells, integrin protein, lymphocyte function-associated antigen 1, intercellular adhesion molecule 1, Opthalmology and Optometry, Pharmacology and Pharmaceutical Sciences, Ophthalmology & Optometry, Ophthalmology and optometry, Pharmacology and pharmaceutical sciences

Abstract

Homeostasis of the lacrimal functional unit is needed to ensure a well-regulated ocular immune response comprising innate and adaptive phases. When the ocular immune system is excessively stimulated and/or immunoregulatory mechanisms are disrupted, the balance between innate and adaptive phases is dysregulated and chronic ocular surface inflammation can result, leading to chronic dry eye disease (DED). According to the Tear Film and Ocular Surface Society Dry Eye Workshop II definition, DED is a multifactorial disorder of the ocular surface characterized by impairment and loss of tear homeostasis (hyperosmolarity), ocular discomfort or pain, and neurosensory abnormalities. Dysregulated ocular immune responses result in ocular surface damage, which is a further contributing factor to DED pathology. Several therapeutics are available to break the vicious circle of DED and prevent chronic disease and progression, including immunosuppressive agents (steroids) and immunomodulators (cyclosporine and lifitegrast). Given the chronic inflammatory nature of DED, each of these agents is commonly used in clinical practice. In this study, we review the immunopathology of DED and the molecular and cellular actions of current topical DED therapeutics to inform clinical decision making.

Published

2020

2. Anti-Inflammatories in the Treatment of Dry Eye Disease: A Review.

Author

Perez, Victor L., Mah, Francis S., Willcox, Mark, and Pflugfelder, Stephen

Subjects

*DRY eye syndromes, *TEARS (Body fluid), *OMEGA-3 fatty acids, *EYE inflammation, *T cells

Abstract

Inflammation is an important driver of dry eye disease (DED) pathogenesis. An initial insult that results in the loss of tear film homeostasis can initiate a nonspecific innate immune response that leads to a chronic and self-sustaining inflammation of the ocular surface, which results in classic symptoms of dry eye. This initial response is followed by a more prolonged adaptive immune response, which can perpetuate and aggravate inflammation and result in a vicious cycle of chronic inflammatory DED. Effective anti-inflammatory therapies can help patients exit this cycle, and effective diagnosis of inflammatory DED and selection of the most appropriate treatment are therefore key to successful DED management and treatment. This review explores the cellular and molecular mechanisms of the immune and inflammatory components of DED, and examines the evidence base for the use of currently available topical treatment options. These agents include topical steroid therapy, calcineurin inhibitors, T cell integrin antagonists, antibiotics, autologous serum/plasma therapy, and omega-3 fatty acid dietary supplements. [ABSTRACT FROM AUTHOR]

Published

2023

3. Use of Post-transplant Cyclophosphamide Treatment to Build a Tolerance Platform to Prevent Liquid and Solid Organ Allograft Rejection.

Author

Lightbourn, Casey O., Wolf, Dietlinde, Copsel, Sabrina N., Wang, Ying, Pfeiffer, Brent J., Barreras, Henry, Bader, Cameron S., Komanduri, Krishna V., Perez, Victor L., and Levy, Robert B.

Subjects

CORNEAL transplantation, HEMATOPOIETIC stem cell transplantation, TRANSPLANTATION of organs, tissues, etc., T cells, CYCLOPHOSPHAMIDE

Abstract

Corneal transplantation (CT) is the most frequent type of solid organ transplant (SOT) performed worldwide. Unfortunately, immunological rejection is the primary cause of graft failure for CT and therefore advances in immune regulation to induce tolerance remains an unmet medical need. Recently, our work and others in pre-clinical studies found that cyclophosphamide (Cy) administered after ("post-transplant," PTCy) hematopoietic stem cell transplantation (HSCT), i.e., liquid transplants is effective for graft vs. host disease prophylaxis and enhances overall survival. Importantly, within the past 10 years, PTCy has been widely adopted for clinical HSCT and the results at many centers have been extremely encouraging. The present studies found that Cy can be effectively employed to prolong the survival of SOT, specifically mouse corneal allografts. The results demonstrated that the timing of PTCy administration is critical for these CT and distinct from the kinetics employed following allogeneic HSCT. PTCy was observed to interfere with neovascularization, a process critically associated with immune rejection of corneal tissue that ensues following the loss of ocular "immune privilege." PTCy has the potential to delete or directly suppress allo-reactive T cells and treatment here was shown to diminish T cell rejection responses. These PTCy doses were observed to spare significant levels of CD4+ FoxP3+ (Tregs) which were found to be functional and could readily receive stimulating signals leading to their in vivo expansion via TNFRSF25 and CD25 agonists. In total, we posit future studies can take advantage of Cy based platforms to generate combinatorial strategies for long-term tolerance induction. [ABSTRACT FROM AUTHOR]

Published

2021

4. T Cells and Macrophages Responding to Oxidative Damage Cooperate in Pathogenesis of a Mouse Model of Age-Related Macular Degeneration.

Author

Cruz-Guilloty, Fernando, Saeed, Ali M., Duffort, Stephanie, Cano, Marisol, Ebrahimi, Katayoon B., Ballmick, Asha, Tan, Yaohong, Wang, Hua, Laird, James M., Salomon, Robert G., Handa, James T., and Perez, Victor L.

Subjects

T cells, MACROPHAGES, OXIDATIVE stress, LABORATORY mice, AGE factors in retinal degeneration, PYRROLES, INTERFERON gamma release tests

Abstract

Age-related macular degeneration (AMD) is a major disease affecting central vision, but the pathogenic mechanisms are not fully understood. Using a mouse model, we examined the relationship of two factors implicated in AMD development: oxidative stress and the immune system. Carboxyethylpyrrole (CEP) is a lipid peroxidation product associated with AMD in humans and AMD-like pathology in mice. Previously, we demonstrated that CEP immunization leads to retinal infiltration of pro-inflammatory M1 macrophages before overt retinal degeneration. Here, we provide direct and indirect mechanisms for the effect of CEP on macrophages, and show for the first time that antigen-specific T cells play a leading role in AMD pathogenesis. In vitro, CEP directly induced M1 macrophage polarization and production of M1-related factors by retinal pigment epithelial (RPE) cells. In vivo, CEP eye injections in mice induced acute pro-inflammatory gene expression in the retina and human AMD eyes showed distinctively diffuse CEP immunolabeling within RPE cells. Importantly, interferon-gamma (IFN-γ) and interleukin-17 (IL-17)-producing CEP-specific T cells were identified ex vivo after CEP immunization and promoted M1 polarization in co-culture experiments. Finally, T cell immunosuppressive therapy inhibited CEP-mediated pathology. These data indicate that T cells and M1 macrophages activated by oxidative damage cooperate in AMD pathogenesis. [ABSTRACT FROM AUTHOR]

Published

2014

5. High-resolution, noninvasive longitudinal live imaging of immune responses.

Author

Abdulreda, Midhat H., Faleo, Gaetano, Molano, Ruth Damaris, Lopez-Cabezas, Maite, Molina, Judith, Yaohong Tan, Ron Echeverria, Oscar A., Zahr-Akrawi, Elsie, Rodriguez-Diaz, Rayner, Edlund, Patrick K., Leibiger, Ingo, Bayer, Allison L., Perez, Victor, Ricordi, Camillo, Caicedo, Alejandro, Pileggi, Antonello, and Berggren, Per-Olof

Subjects

DIAGNOSTIC imaging, IMMUNE response, T cells, ISLANDS of Langerhans, MICROSCOPY

Abstract

Intravital imaging emerged as an indispensible tool in biological research, and a variety of imaging techniques have been developed to noninvasively monitor tissues in vivo. However, most of the current techniques lack the resolution to study events at the single-cell level. Although intravital multiphoton microscopy has addressed this limitation, the need for repeated noninvasive access to the same tissue in longitudinal in vivo studies remains largely unmet. We now report on a previously unexplored approach to study immune responses after transplantation of pancreatic islets into the anterior chamber of the mouse eye. This approach enabled (i) longitudinal, noninvasive imaging of transplanted tissues in vivo; (ii) in vivo cytolabeling to assess cellular phenotype and viability in situ; (iii) local intervention by topical application or intraocular injection; and (iv) real-time tracking of infiltrating immune cells in the target tissue. [ABSTRACT FROM AUTHOR]

Published

2011

6. Analyses and Correlation of Pathologic and Ocular Cutaneous Changes in Murine Graft versus Host Disease.

Author

Levy, Robert B., Mousa, Hazem M., Lightbourn, Casey O., Shiuey, Eric J., Latoni, David, Duffort, Stephanie, Flynn, Ryan, Du, Jing, Barreras, Henry, Zaiken, Michael, Paz, Katelyn, Blazar, Bruce R., and Perez, Victor L.

Subjects

GRAFT versus host disease, SJOGREN'S syndrome, T cells, STEM cell transplantation, STATISTICAL correlation, DRY eye syndromes

Abstract

Graft versus host disease (GVHD) is initiated by donor allo-reactive T cells activated against recipient antigens. Chronic GVHD (cGVHD) is characterized by immune responses that may resemble autoimmune features present in the scleroderma and Sjogren's syndrome. Unfortunately, ocular involvement occurs in approximately 60–90% of patients with cGVHD following allo-hematopoietic stem cell transplants (aHSCT). Ocular GVHD (oGVHD) may affect vision due to ocular adnexa damage leading to dry eye and keratopathy. Several other compartments including the skin are major targets of GVHD effector pathways. Using mouse aHSCT models, the objective was to characterize cGVHD associated alterations in the eye and skin to assess for correlations between these two organs. The examination of multiple models of MHC-matched and MHC-mismatched aHSCT identified a correlation between ocular and cutaneous involvement accompanying cGVHD. Studies detected a "positive" correlation, i.e., when cGVHD-induced ocular alterations were observed, cutaneous compartment alterations were also observed. When no or minimal ocular signs were detected, no or minimal skin changes were observed. In total, these findings suggest underlying cGVHD-inducing pathological immune mechanisms may be shared between the eye and skin. Based on the present observations, we posit that when skin involvement is present in aHSCT patients with cGVHD, the evaluation of the ocular surface by an ophthalmologist could potentially be of value. [ABSTRACT FROM AUTHOR]

Published

2022

7. In-vivo impaired T helper 1 cell development in submandibular lymph nodes due to IL-12 deficiency following antigen injection into the anterior chamber of the eye.

Author

Perez, Victor L., Biuckians, Andre, and Streilein, Wayne J.

Subjects

*T cells, *LYMPH nodes, *ANTIGENS, *CYTOLOGY

Abstract

PURPOSE: To determine the functional properties of antigen-specific T cells that accumulate in lymph nodes following injection of antigen into the anterior chamber (AC). METHODS: Ovalbumin (OVA)-specific, CD4+ transgenic T cell receptor (Tcr) T cells (KJ-126+) from DO11.10 mice were adoptively transferred into unirradiated syngeneic BALB/c mice who then received an injection of OVA in the AC or subcutaneously (SC). Three days later, KJ126+ T cells in draining and non-draining lymph nodes were analyzed for clonal expansion, activation, and cell-cycle status by flow cytometry. In addition, the cells' functional phenotype was assessed in vitro by proliferation assays and cytokine production by ELISA. RESULTS: Tcr T cells localized exclusively to draining lymph nodes after injection of OVA into the AC (neck) and SC (neck, axilla, brachial). In both cases, the KJ126+ T cells displayed evidence of in-vivo activation and proliferation. T cells from AC-injected donors when stimulated in vitro with OVA produced small amounts of IL-2, but no IFN-γ, IL-4, IL-5, IL-10, or TGFβ. By contrast, T cells from SC-injected animals displayed a Th1-like phenotype (IL-2, IFN-γ). The draining lymph nodes of mice that received systemic or intraocular administration of exogenous IL-12 at the time of the AC injection of OVA also contained KJ126+ T cells that secreted IFN-γ and IL-2. CONCLUSION: Antigen attracts antigen-specific T cells to lymph nodes that drain the injection site. Whereas responding T cells in nodes draining SC-injection sites differentiated into Th1-like cells, T cells in nodes draining AC injection failed to differentiated beyond the capacity to secrete IL-2 in response to antigen. Since the failure was reversed by exogenous IL-12, we propose that orderly differentiation of antigen-specific T cells down the Th1 pathway is aborted by the eye, because of a deficit in IL-12 production. [ABSTRACT FROM AUTHOR]

Published

2000

8. Modeling Chronic Graft-versus-Host Disease in MHC-Matched Mouse Strains: Genetics, Graft Composition, and Tissue Targets.

Author

Müller, Antonia M.S., Min, Dullei, Wernig, Gerlinde, Levy, Robert B., Perez, Victor L., Herretes, Samantha, Florek, Mareike, Burnett, Casey, Weinberg, Kenneth, and Shizuru, Judith A.

Subjects

*T cells, *GRAFT versus host disease, *MICE genetics, *T helper cells, *MOUSE diseases, *HEMATOPOIETIC stem cells, *MIRROR neurons

Abstract

• This is a first report of C57BL/6 into BALB.B mice as a representative model of chronic GVHD that mirrors the clinical syndrome observed in humans. • Thymic damage during acute GVHD is followed by impaired recovery of medullary thymic epithelial cells and dysfunctional T cell education. Graft-versus-host disease (GVHD) remains a major complication of allogeneic hematopoietic cell transplantation. Acute GVHD (aGVHD) results from direct damage by donor T cells, whereas the biology of chronic GVHD (cGVHD) with its autoimmune-like manifestations remains poorly understood, mainly because of the paucity of representative preclinical models. We examined over an extended time period 7 MHC-matched, minor antigen–mismatched mouse models for development of cGVHD. Development and manifestations of cGVHD were determined by a combination of MHC allele type and recipient strain, with BALB recipients being the most susceptible. The C57BL/6 into BALB.B combination most closely modeled the human syndrome. In this strain combination moderate aGVHD was observed and BALB.B survivors developed overt cGVHD at 6 to 12 months affecting eyes, skin, and liver. Naïve CD4+ cells caused this syndrome as no significant pathology was induced by grafts composed of purified hematopoietic stem cells (HSCs) or HSC plus effector memory CD4+ or CD8+ cells. Furthermore, co-transferred naïve and effector memory CD4+ T cells demonstrated differential homing patterns and locations of persistence. No clear association with donor Th17 cells and the phenotype of aGVHD or cGVHD was observed in this model. Donor CD4+ cells caused injury to medullary thymic epithelial cells, a key population responsible for negative T cell selection, suggesting that impaired thymic selection was an underlying cause of the cGVHD syndrome. In conclusion, we report for the first time that the C57BL/6 into BALB.B combination is a representative model of cGVHD that evolves from immunologic events during the early post-transplant period. [ABSTRACT FROM AUTHOR]

Published

2019

9. Immunological Disruption of Antiangiogenic Signals by Recruited Allospecific T Cells Leads to Corneal Allograft Rejection.

Author

Yaohong Tan, Cruz-Guilloty, Fernando, Medina-Mendez, Carlos A., Cutrufello, Nicholas J., Martinez, Rosa E., Urbieta, Maitee, Wilson, David, Yiwen Li, and Perez, Victor L.

Subjects

*T cells, *HOMOGRAFTS, *GRAFT rejection, *IMMUNOLOGY, *CORNEAL transplantation, *NEOVASCULARIZATION, *IMMUNOSUPPRESSION, *ENDOSTATIN

Abstract

Corneal transplantation is the most common solid organ transplantation. The immunologically privileged nature of the cornea results in high success rates. However, T cell-mediated rejection is the most common cause of corneal graft failure. Using antiangio-genesis treatment to prevent corneal neovascularization, which revokes immune privilege, prevents corneal allograft rejection. Endostatin is an antiangiogenic factor that maintains corneal avascularity. In this study, we directly test the role of antiangiogenic and immunological signals in corneal allograft survival, specifically the potential correlation of endostatin production and T cell recruitment. We report that 75% of the corneal allografts of BALB/c mice rejected after postoperative day (POD) 20, whereas all syngeneic grafts survived through POD60. This correlates with endogenous endostatin, which increased and remained high in syngeneic grafts but decreased after POD10 in allografts. Immunostaining demonstrated that early recruitment of allospecinc T cells into allografts around POD10 correlated with decreased endostatin production. In Rag-/- mice, both allogeneic and syngeneic corneal grafts survived; endostatin remained high throughout. However, after T cell transfer, the allografts eventually rejected, and endostatin decreased. Furthermore, exogenous endostatin treatment delayed allograft rejection and promoted survival secondary to angiogenesis inhibition. Our results suggest that endostatin plays an important role in corneal allograft survival by inhibiting neovascularization and that early recruitment of allospecinc T cells into the grafts promotes destruction of endostatin-producing cells, resulting in corneal neovascularization, massive infiltration of effector T cells, and ultimately graft rejection. Therefore, combined antiangiogenesis and immune suppression will be more effective in maintaining corneal allograft survival. [ABSTRACT FROM AUTHOR]

Published

2012

10. Peptide-Conjugated PAMAM Dendrimer as a Universal DNA Vaccine Platform to Target Antigen-Presenting Cells.

Author

Daftarian, Pirouz, Kaifer, Angel E., Wei Li, Blomberg, Bonnie B., Frasca, Daniela, Roth, Felix, Chowdhury, Raquibul, Berg, Eric A., Fishman, Jordan B., Al Sayegh, Husain A., Blackwelder, Pat, Inverardi, Luca, Perez, Victor L., Lemmon, Vance, and Serafini, Paolo

Subjects

*PEPTIDES, *DENDRIMERS, *DNA vaccines, *POLYAMIDOAMINE dendrimers, *DENDRITIC cells, *T cells

Abstract

DNA-based vaccines hold promise to outperform conventional antigen-based vaccines by virtue of many unique features. However, DNA vaccines have thus far fallen short of expectations, due in part to poor targeting of professional antigen-presenting cells (APC) and low immunogenicity. In this study, we describe a new platform for effective and selective delivery of DNA to APCs in vivo that offers intrinsic immune-enhancing characteristics. This platform is based on conjugation of fifth generation polyamidoamine (G5-PAMAM) dendrimers, a DNA-loading surface, with MHC class II--targeting peptides that can selectively deliver these dendrimers to APCs under conditions that enhance their immune stimulatory potency. DNA conjugated with this platform efficiently transfected murine and human APCs in vitro. Subcutaneous administration of DNA-peptide-dendrimer complexes in vivo preferentially transfected dendritic cells (DC) in the draining lymph nodes, promoted generation of high affinity T cells, and elicited rejection of established tumors. Taken together, our findings show how PAMAM dendrimer complexes can be used for high transfection efficiency and effective targeting of APCs in vivo, conferring properties essential to generate effective DNA vaccines. [ABSTRACT FROM AUTHOR]

Published

2011