Showing total 435 results

51. Releasing the Brake: Targeting Cbl-b to Enhance Lymphocyte Effector Functions.

Author

Wallner, Stephanie, Gruber, Thomas, Baier, Gottfried, and Wolf, Dominik

Subjects

UBIQUITIN ligases, T cells, CELL-mediated lympholysis, IMMUNE response, AUTOIMMUNITY, TUMOR markers, CANCER immunotherapy

Abstract

The E3 ubiquitin ligase Cbl-b is an established nonredundant negative regulator of T-cell activation. Cbl-b fine-tunes the activation threshold of T cells and uncouples T cells from their vital need of a costimulatory signal to mount a productive immune response. Accordingly, mice deficient in cblb are prone to autoimmunity and reject tumors. The latter has been described to be mediated via CD8+ T cells, which are hyperactive and more abundant in shrinking tumors of cblb-deficient animals. This might at least also in part be mediated by resistance of cblb-deficient T cells to negative cues exerted by tumor-associated immuno-suppressive factors, such as TGF-βand regulatory T cells (Treg). Experiments using cblb-deficient T cells either alone or in combination with vaccines validate the therapeutic concept of enhancing the efficacy of adoptively transferred lymphocytes to treat malignant tumors. This paper summarizes the current knowledge about the negative regulatory role of Cbl-b in T-cell activation and its potential therapeutic implications for cancer immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2012

52. Incomplete Immune Recovery in HIV Infection: Mechanisms, Relevance for Clinical Care, and Possible Solutions.

Author

Gaardbo, Julie C., Hartling, Hans J., Gerstoft, Jan, and Nielsen, Susanne D.

Subjects

HIV infections, APOPTOSIS, IMMUNE response, ANTIRETROVIRAL agents, VIRAL replication

Abstract

Treatment of HIV-infected patients with highly active antiretroviral therapy (HAART) usually results in diminished viral replication, increasing CD4+ cell counts, a reversal of most immunological disturbances, and a reduction in risk of morbidity and mortality. However, approximately 20% of all HIV-infected patients do not achieve optimal immune reconstitution despite suppression of viral replication. These patients are referred to as immunological nonresponders (INRs). INRs present with severely altered immunological functions, including malfunction and diminished production of cells within lymphopoetic tissue, perturbed frequencies of immune regulators such as regulatory T cells and Th17 cells, and increased immune activation, immunosenescence, and apoptosis. Importantly, INRs have an increased risk of morbidity and mortality compared toHIV-infected patients with an optimal immune reconstitution. Additional treatment to HAART that may improve immune reconstitution has been investigated, but results thus far have proved disappointing. The reason for immunological nonresponse is incompletely understood. This paper summarizes the known and unknown factors regarding the incomplete immune reconstitution in HIV infection, including mechanisms, relevance for clinical care, and possible solutions. [ABSTRACT FROM AUTHOR]

Published

2012

53. Indolent B-Cell Lymphomas Associated with HCV Infection: Clinical and Virological Features and Role of Antiviral Therapy.

Author

Arcaini, Luca, Merli, Michele, Volpetti, Stefano, Rattotti, Sara, Gotti, Manuel, and Zaja, Francesco

Subjects

HEPATITIS C virus, B cells, HODGKIN'S disease, EPIDEMIOLOGY, ANTIVIRAL agents

Abstract

The association between hepatitis C virus (HCV) infection and B-cell non-Hodgkin's lymphomas (NHL) has been demonstrated by epidemiological studies, in particular in highly endemic geographical areas such as Italy, Japan, and southern parts of United States. In these countries, together with diffuse large B-cell lymphomas, marginal zone lymphomas are the histotypes most frequently associated with HCV infection; in Italy around 20-30% cases of marginal zone lymphomas are HCV positive. Recently, antiviral treatment with interferon with or without ribavirin has been proved to be effective in the treatment of HCV-positive patients affected by indolent lymphoma, prevalently of marginal zone origin. An increasing number of experiences confirmed the validity of this approach in marginal zone lymphomas and in other indolent NHL subtypes like lymphoplasmacytic lymphoma. Across different studies, overall response rate was approximately 75%. Hematological responses resulted significantly associated with the eradication of the virus. This is the strongest evidence of a causative link between HCV and lymphomas. The aim of this paper is to illustrate the relationship between HCV infection and different subtypes of indolent B-cell lymphomas and to systematically summarize the data from the therapeutic studies that reported the use of antiviral treatment as hematological therapy in patients with HCV-associated indolent lymphomas. [ABSTRACT FROM AUTHOR]

Published

2012

54. Bartonella Infection in Immunocompromised Hosts: Immunology of Vascular Infection and Vasoproliferation.

Author

Mosepele, Mosepele, Mazo, Dana, and Cohn, Jennifer

Subjects

BARTONELLA, IMMUNE system, IMMUNOSUPPRESSION, IMMUNOLOGY, IMMUNOCOMPROMISED patients

Abstract

Most infections by genus Bartonella in immunocompromised patients are caused by B. henselae and B. quintana. Unlike immunocompetent hosts who usually develop milder diseases such as cat scratch disease and trench fever, immunocompromised patients, including those living with HIV/AIDS and posttransplant patients, are more likely to develop different and severe lifethreatening disease. This paper will discuss Bartonella's manifestations in immunosuppressed patients and will examine Bartonella's interaction with the immune system including its mechanisms of establishing infection and immune escape. Gaps in current understanding of the immunology of Bartonella infection in immunocompromised hosts will be highlighted. [ABSTRACT FROM AUTHOR]

Published

2012

55. Sex Differences Associated with Primary Biliary Cirrhosis.

Author

Smyk, Daniel S., Rigopoulou, Eirini I., Pares, Albert, Billinis, Charalambos, Burroughs, Andrew K., Muratori, Luigi, Invernizzi, Pietro, and Bogdanos, Dimitrios P.

Subjects

CIRRHOSIS of the liver, LIVER diseases, AUTOIMMUNITY, FIBROSIS, DISEASE incidence

Abstract

Primary biliary cirrhosis (PBC) is a cholestatic liver disease of autoimmune origin, characterised by the destruction of small intrahepatic bile ducts. The disease has an unpredictable clinical course but may progress to fibrosis and cirrhosis. The diagnostic hallmark of PBC is the presence of disease-specific antimitochondrial antibodies (AMA), which are pathognomonic for the development of PBC. The disease overwhelmingly affects females, with some cases of male PBC being reported. The reasons underlying the low incidence of males with PBC are largely unknown. Epidemiological studies estimate that approximately 7-11% of PBC patients are males. There does not appear to be any histological, serological, or biochemical differences between male and female PBC, although the symptomatology may differ, with males being at higher risk of life-threatening complications such as gastrointestinal bleeding and hepatoma. Studies on X chromosome and sex hormones are of interest when studying the low preponderance of PBC in males; however, these studies are far from conclusive. This paper will critically analyze the literature surrounding PBC in males. [ABSTRACT FROM AUTHOR]

Published

2012

56. Sorafenib Prevents Escape from Host Immunity in Liver Cirrhosis Patients with Advanced Hepatocellular Carcinoma.

Author

Nagai, Hidenari, Mukozu, Takanori, Matsui, Daigo, Kanekawa, Takenori, Kanayama, Masahiro, Wakui, Noritaka, Momiyama, Kouichi, Shinohara, Mie, Iida, Kazunari, Ishii, Koji, Igarashi, Yoshinori, and Sumino, Yasukiyo

Subjects

CYTOKINES, ANTINEOPLASTIC agents, IMMUNITY, T cells, CIRRHOSIS of the liver, LIVER cancer

Abstract

Purpose. It has been reported that Th2 cytokines downregulate antitumor immunity, while activation of type T cells promotes antitumor immunity. The aim of this paper was to evaluate host immunity in liver cirrhosis (LC) patients with advanced hepatocellular carcinoma (aHCC) receiving sorafenib therapy. Methods. Forty-five adult Japanese LC patients received sorafenib for aHCC between 2009 and 2011 at our hospital. Sorafenib was administered at a dose of 200-800 mg/day for 4 weeks. Blood samples were collected before and after treatment. Results. Eleven patients were treated with sorafenib at 200 mg/day (200 group), 27 patients received sorafenib at 400 mg/day (400 group), and 7 patients were given sorafenib at 800 mg/day (800 group). There was no significant change in the percentage of Th1 cells after treatment in any group. However, the percentages of Th2 cells and regulatory T cells were significantly decreased after treatment in the 400 group and 800 group compared with before treatment, although there was no significant change after treatment in the 200 group. Conclusions. These results indicate that treatment with sorafenib might induce Th1 dominance and prevent the escape of tumor cells from the host immune system in LC patients with aHCC [ABSTRACT FROM AUTHOR]

Published

2012

57. Clinical and Pathological Roles of Ro/SSA Autoantibody System.

Author

Yoshimi, Ryusuke, Ueda, Atsuhisa, Ozato, Keiko, and Ishigatsubo, Yoshiaki

Subjects

IMMUNOGLOBULINS, AUTOANTIBODIES, ANTIGENS, SYSTEMIC lupus erythematosus, SJOGREN'S syndrome

Abstract

Anti-Ro/SSA antibodies are among the most frequently detected autoantibodies against extractable nuclear antigens and have been associated with systemic lupus erythematosus (SLE) and Sjögren's syndrome (SS). Although the presence of these autoantibodies is one of the criteria for the diagnosis and classification of SS, they are also sometimes seen in other systemic autoimmune diseases. In the last few decades, the knowledge of the prevalence of anti-Ro/SSA antibodies in various autoimmune diseases and symptoms has been expanded, and the clinical importance of these antibodies is increasing. Nonetheless, the pathological role of the antibodies is still poorly understood. In this paper, we summarize the milestones of the anti-Ro/SSA autoantibody system and provide new insights into the association between the autoantibodies and the pathogenesis of autoimmune diseases. [ABSTRACT FROM AUTHOR]

Published

2012

58. Role of MHC-Linked Susceptibility Genes in the Pathogenesis of Human and Murine Lupus.

Author

Relle, Manfred and Schwarting, Andreas

Subjects

SYSTEMIC lupus erythematosus, AUTOIMMUNE diseases, AUTOANTIBODIES, LUPUS erythematosus treatment, DISEASE susceptibility

Abstract

Systemic lupus erythematosus (SLE) is a chronic autoimmune disease characterized by the production of autoantibodies against nuclear antigens and a systemic inflammation that can damage a broad spectrumof organs. SLE patients suffer from a wide variety of symptoms, which can affect virtually almost any tissue. As lupus is difficult to diagnose, the worldwide prevalence of SLE can only be roughly estimated to range from 10 and 200 cases per 100,000 individuals with dramatic differences depending on gender, ethnicity, and location. Although the treatment of this disease has been significantly ameliorated by new therapies, improved conventional drug therapy options, and a trained expert eye, the underlying pathogenesis of lupus still remain widely unknown. The complex etiology reflects the complex genetic background of the disease, which is also not well understood yet. However, in the past few years advances in lupus genetics have been made, notably with the publication of genome-wide association studies (GWAS) in humans and the identification of susceptibility genes and loci in mice. This paper reviews the role of MHC-linked susceptibility genes in the pathogenesis of systemic lupus erythematosus. [ABSTRACT FROM AUTHOR]

Published

2012

59. Genetics of SLE: Functional Relevance for Monocytes/Macrophages in Disease.

Author

Byrne, Jennifer C., Ní Gabhann, Joan, Lazzari, Elisa, Mahony, Rebecca, Smith, Siobhán, Stacey, Kevin, Wynne, Claire, and Jefferies, Caroline A.

Subjects

SYSTEMIC lupus erythematosus, MONOCYTES, MACROPHAGES, IMMUNE system, PATHOLOGICAL physiology, AUTOANTIGENS, TOLL-like receptors

Abstract

Genetic studies in the last 5 years have greatly facilitated our understanding of how the dysregulation of diverse components of the innate immune system contributes to pathophysiology of SLE. A role for macrophages in the pathogenesis of SLE was first proposed as early as the 1980s following the discovery that SLE macrophages were defective in their ability to clear apoptotic cell debris, thus prolonging exposure of potential autoantigens to the adaptive immune response. More recently, there is an emerging appreciation of the contribution both monocytes and macrophages play in orchestrating immune responses with perturbations in their activation or regulation leading to immune dysregulation. This paper will focus on understanding the relevance of genes identified as being associated with innate immune function of monocytes and macrophages and development of SLE, particularly with respect to their role in (1) immune complex (IC) recognition and clearance, (2) nucleic acid recognition via toll-like receptors (TLRs) and downstream signalling, and (3) interferon signalling. Particular attention will be paid to the functional consequences these genetic associations have for disease susceptibility or pathogenesis. [ABSTRACT FROM AUTHOR]

Published

2012

60. Mesangial Cell-Specific Antibodies Are Central to the Pathogenesis of Lupus Nephritis.

Author

Seret, Guillaume, Le Meur, Yannick, Renaudineau, Yves, and Youinou, Pierre

Subjects

SYSTEMIC lupus erythematosus, NEPHRITIS, DISEASE complications, DNA antibodies, FIBRONECTINS, CHROMATIN, CELL proliferation

Abstract

Not only is nephritis a common complaint in systemic lupus erythematosus, but it is also the most life-threatening complication of the disease. Anti-double-stranded DNA antibodies (Abs), which are found in up to 80% of these patients, might be nephritogenic per se. That is, they may cross-react with mesangial cell (MC) surface proteins, such as alpha-actinin and annexin A2, they may cross-react with mesangial matrix protein such as laminine and fibronectin, or they may recognize chromatin material previously deposited in the glomeruli. The consequence of the binding of anti-MC Abs may be their internalization, which results in activation and proliferation of theseMCs. In turn, these activated MCs are suspected of promoting immune complex formation by sequestering and thereby protecting chromatin from degradation. The present paper will explain the mechanisms through which such autoAbs may initiate nephritis. [ABSTRACT FROM AUTHOR]

Published

2012

61. The Clinical Significance of the Dense Fine Speckled Immunofluorescence Pattern on HEp-2 Cells for the Diagnosis of Systemic Autoimmune Diseases.

Author

Mahler, Michael and Fritzler, Marvin J.

Subjects

IMMUNOFLUORESCENCE, ANTINUCLEAR factors, IMMUNOGLOBULINS, IMMUNOCYTOCHEMISTRY, AUTOIMMUNE diseases, AUTOIMMUNITY, IMMUNOLOGIC diseases

Abstract

Antinuclear antibodies (ANAs) are a serological hallmark in the diagnosis of systemic autoimmune rheumatic diseases (SARD). The indirect immunofluorescence (IIF) assay on HEp-2 cells is a commonly used test for the detection of ANA and has been recently recommended as the screening test of choice by a task force of the American College of Rheumatology. However, up to 20% of apparently healthy individuals (HI) have been reported to have a positive IIF ANA test, primarily related to autoantibodies that target the dense fine speckles 70 (DFS70) antigen. Even more important, the DFS IIF pattern has been reported in up to 33% of ANA positive HI, but not in ANA positive SARD sera. Since the intended use of the ANA HEp-2 test is to aid in the diagnosis and classification of SARD, the detection and reporting of anti-DFS70 antibodies and their associated pattern (DFS) as a positive test significantly reduce the specificity and the positive likelihood of the ANA test. This has significant implications for medical management and diagnostic algorithms involving the detection of ANA. Recently, a novel immunoadsorption method has been developed that specifically blocks anti-DFS70 antibodies and, therefore, significantly increases the specificity of the ANA test for SARD. This immunoadsorption method has the potential to overcome a significant limitation of the ANA HEp-2 assay. The present paper summarizes the current knowledge about anti-DFS70 antibodies and their clinical impact on ANA testing. [ABSTRACT FROM AUTHOR]

Published

2012

62. Modulation of Immunity by Antiangiogenic Molecules in Cancer.

Author

Terme, Magali, Colussi, Orianne, Marcheteau, Elie, Tanchot, Corinne, Tartour, Eric, and Taieb, Julien

Subjects

IMMUNOREGULATION, NEOVASCULARIZATION, CANCER treatment, IMMUNOLOGY, ANTIGENS, IMMUNOSUPPRESSION, T cells

Abstract

In the last decades a new class of therapeutic drugs have been developed that block tumor angiogenesis. These antiangiogenic molecules, which target VEGF or VEGFR, PDGFR, and c-kit, can act not only on endothelial cells but also on immune cells. Some antiangiogenic molecules inhibit the development of immunosuppressive mechanisms developed by the tumors to escape the immune system (such as regulatory T cells, myeloid-derived suppressor cells, and immunosuppressive cytokines). These immunomodulatory effects must be characterized in detail to enable a better prescription of these treatments. In this paper we will focus on the impact of anti-angiogenic drugs on immunosuppression and their potential combination with immunotherapeutic strategies. Interestingly, immune parameters or their modulation during treatment could serve as potential biomarkers of response or resistance to anti-angiogenic therapies. [ABSTRACT FROM AUTHOR]

Published

2012

63. CD154: An Immunoinflammatory Mediator in Systemic Lupus Erythematosus and Rheumatoid Arthritis.

Author

Alaaeddine, Nada, Hassan, Ghada S., Yacoub, Daniel, and Mourad, Walid

Subjects

SYSTEMIC lupus erythematosus, RHEUMATOID arthritis, AUTOIMMUNE diseases, VASCULAR diseases, IMMUNOLOGY, INFLAMMATORY mediators, BIOMOLECULES

Abstract

Systemic lupus erythematosus and rheumatoid arthritis are two major chronic inflammatory autoimmune diseases with significant prevalence rates among the population. Although the etiology of these diseases remains unresolved, several evidences support the key role of CD154/CD40 interactions in initiating and/or propagating these diseases. The discovery of new receptors (αIIbβ3, α5β1, and αMβ2) for CD154 has expanded our understanding about the precise role of this critical immune mediator in the physiopathology of chronic inflammatory autoimmune diseases in general, and in systemic lupus erythematosus and rheumatoid arthritis in particular. This paper presents an overview of the interaction of CD154 with its various receptors and outlines its role in the pathogenesis of systemic lupus erythematosus and rheumatoid arthritis. Moreover, the potential usefulness of various CD154-interfering agents in the treatment and prevention of these diseases is also discussed. [ABSTRACT FROM AUTHOR]

Published

2012

64. Toxin-Based Targeted Therapy for Malignant Brain Tumors.

Author

Chandramohan, Vidyalakshmi, Sampson, John H., Pastan, Ira, and Bigner, Darell D.

Subjects

BRAIN tumors, THERAPEUTICS, CYSTS (Pathology), CLINICAL medicine, MEDICAL radiology, DRUG therapy

Abstract

Despite advances in conventional treatment modalities for malignant brain tumors-surgery, radiotherapy, and chemotherapy- the prognosis for patients with high-grade astrocytic tumor remains dismal. The highly heterogeneous and diffuse nature of astrocytic tumors calls for the development of novel therapies. Advances in genomic and proteomic research indicate that treatment of brain tumor patients can be increasingly personalized according to the characteristics of the targeted tumor and its environment. Consequently, during the last two decades, a novel class of investigative drug candidates for the treatment of central nervous system neoplasia has emerged: recombinant fusion protein conjugates armed with cytotoxic agents targeting tumor-specific antigens. The clinical applicability of the tumor-antigen-directed cytotoxic proteins as a safe and viable therapy for brain tumors is being investigated. Thus far, results fromongoing clinical trials are encouraging, as disease stabilization and patient survival prolongation have been observed in at least 109 cases. This paper summarizes the major findings pertaining to treatment with the different antiglioma cytotoxins at the preclinical and clinical stages. [ABSTRACT FROM AUTHOR]

Published

2012

65. Initiation and Regulation of Complement during Hemolytic Transfusion Reactions.

Author

Stowell, Sean R., Winkler, Anne M., Maier, Cheryl L., Maridith Arthur, C., Smith, Nicole H., Girard-Pierce, Kathryn R., Cummings, Richard D., Zimring, James C., and Hendrickson, Jeanne E.

Subjects

BLOOD transfusion, BLOOD cells, RED blood cell transfusion, AUTOIMMUNE hemolytic anemia, HEMOGLOBINS, DONOR blood supply, BLOOD groups

Abstract

Hemolytic transfusion reactions represent one of the most common causes of transfusion-related mortality. Although many factors influence hemolytic transfusion reactions, complement activation represents one of the most common features associated with fatality. In this paper we will focus on the role of complement in initiating and regulating hemolytic transfusion reactions and will discuss potential strategies aimed at mitigating or favorably modulating complement during incompatible red blood cell transfusions. [ABSTRACT FROM AUTHOR]

Published

2012

66. Interplay of Polarity Proteins and GTPases in T-Lymphocyte Function.

Author

Fung, Ivan, Russell, SarahM., and Oliaro, Jane

Subjects

POLARITY (Chemistry), CYTOTOXIC T cells, CELL physiology, IMMUNE response, GENETIC mutation, CELLS, ANTIGEN presentation

Abstract

Polarity refers to the asymmetric distribution of different cellular components within a cell and is central to many cell functions. In T-cells, polarity regulates the activation, migration, and effector function of cytotoxic T-cells (CTLs) during an immune response. The regulation of asymmetric cell division by polarity proteins may also dictate CTL effector and memory differentiation following antigen presentation. Small GTPases, along with their associated polarity and adaptor proteins, are critical for mediating the polarity changes necessary for T-cell activation and function, and in turn, are regulated by guanine exchange factors (GEFS) and GTPase activating proteins (GAPS). For example, a novel GEF, dedicator of cytokinesis 8 (DOCK8) was recently identified as a regulator of immune cell function and mutations in DOCK8 have been detected in patients with severe combined immunodeficiency. Both B and T-cells from DOCK8 mutant mice form defective immunological synapses and have abnormal functions, in addition to impaired immune memory development. This paper will discuss the interplay between polarity proteins and GTPases, and their role in T-cell function [ABSTRACT FROM AUTHOR]

Published

2012

67. The Role of Complement System in Septic Shock.

Author

Charchaflieh, Jean, Jiandong Wei, Labaze, Georges, Yunfang Joan Hou, Babarsh, Benjamin, Stutz, Helen, Lee, Haekyung, Worah, Samrat, and Ming Zhang

Subjects

SEPTIC shock, BACTERIAL disease complications, AMINO acids, SEPSIS, LECTINS

Abstract

Septic shock is a critical clinical condition with a high mortality rate. A better understanding of the underlying mechanisms is important to develop effective therapies. Basic and clinical studies suggest that activation of complements in the common cascade, for example, complement component 3 (C3) and C5, is involved in the development of septic shock. The involvement of three upstream complement pathways in septic shock is more complicated. Both the classical and alternative pathways appear to be activated in septic shock, but the alternative pathway may be activated earlier than the classical pathway. Activation of these two pathways is essential to clear endotoxin. Recent investigations have shed light on the role of lectin complement pathway in septic shock. Published reports suggest a protective role of mannose-binding lectin (MBL) against sepsis. Our preliminary study of MBL-associated serine protease-2 (MASP-2) in septic shock patients indicated that acute decrease of MASP-2 in the early phase of septic shock might correlate with in-hospital mortality. It is unknown whether excessive activation of these three upstream complement pathways may contribute to the detrimental effects in septic shock. This paper also discusses additional complementrelated pathogenic mechanisms and intervention strategies for septic shock. [ABSTRACT FROM AUTHOR]

Published

2012

68. Immunological HCV-Associated Thrombocytopenia: Short Review.

Author

Dimitroulis, Dimitrios, Valsami, Serena, Stamopoulos, Paraskevas, and Kouraklis, Gregory

Subjects

HEPATITIS C virus, THROMBOCYTOPENIA, LIVER diseases, VIRAL hepatitis

Abstract

Infection with Hepatitis C virus (HCV) is affecting about 3% of the world's population, leading to liver damage, end-stage liver disease, and development of hepatocellular carcinoma, being thus the first indication for liver transplantation in the USA. Apart from the cirrhotic-liver-derived clinical signs and symptoms several conditions with immunological origin can also arise, such as, glomerulonephritis, pulmonary fibrosis, and thrombocytopenia. HCV-related autoimmune thrombocytopenia shows specific pathogenetic characteristics as well as symptoms and signs that differ in severity and frequency from symptoms in patients that are not HCV infected. Aim of this short paper is to estimate the epidemiological characteristics of the disease, to investigate the pathogenesis and clinical manifestation, and to propose treatment strategies according to the pertinent literature. [ABSTRACT FROM AUTHOR]

Published

2012

69. Making the Most of Major Histocompatibility Complex Molecule Multimers: Applications in Type 1 Diabetes.

Author

Gojanovich, Greg S. and Hess, Paul R.

Subjects

MAJOR histocompatibility complex, DIABETES, CELL proliferation, LANGERHANS cells, CELL receptors

Abstract

Classical major histocompatibility complex (MHC) class I and II molecules present peptides to cognate T-cell receptors on the surface of T lymphocytes. The specificity with which T cells recognize peptide-MHC (pMHC) complexes has allowed for the utilization of recombinant, multimeric pMHC ligands for the study of minute antigen-specific T-cell populations. In type 1 diabetes (T1D), CD8+ cytotoxic T lymphocytes, in conjunction with CD4+ T helper cells, destroy the insulin-producing β cells within the pancreatic islets of Langerhans. Due to the importance of T cells in the progression of T1D, the ability to monitor and therapeutically target diabetogenic clonotypes of T cells provides a critical tool that could result in the amelioration of the disease. By administering pMHC multimers coupled to fluorophores, nanoparticles, or toxic moieties, researchers have demonstrated the ability to enumerate, track, and delete diabetogenic T-cell clonotypes that are, at least in part, responsible for insulitis; some studies even delay or prevent diabetes onset in the murine model of T1D. This paper will provide a brief overview of pMHC multimer usage in defining the role T-cell subsets play in T1D etiology and the therapeutic potential of pMHC for antigen-specific identification and modulation of diabetogenic T cells. [ABSTRACT FROM AUTHOR]

Published

2012

70. Epstein-Barr Virus and Systemic Lupus Erythematosus.

Author

Draborg, Anette Holck, Duus, Karen, and Houen, Gunnar

Subjects

EPSTEIN-Barr virus, VASCULAR diseases, CUTANEOUS tuberculosis, ANTIGENS, T cells

Abstract

The etiology of SLE is not fully established. SLE is a disease with periods of waning disease activity and intermittent flares. This fits well in theory to a latent virus infection, which occasionally switches to lytic cycle, and EBV infection has for long been suspected to be involved. This paper reviews EBV immunobiology and how this is related to SLE pathogenesis by illustrating uncontrolled reactivation of EBV as a diseasemechanism for SLE. Studies on EBV in SLE patients show enlarged viral load, abnormal expression of viral lytic genes, impaired EBV-specific T-cell response, and increased levels of EBV-directed antibodies. These results suggest a role for reactivation of EBV infection in SLE. The increased level of EBV antibodies especially comprises an elevated titre of IgA antibodies, and the total number of EBV-reacting antibody isotypes is also enlarged. As EBV is known to be controlled by cell-mediated immunity, the reduced EBV-specific T-cell response in SLE patients may result in defective control of EBV causing frequent reactivation and expression of lytic cycle antigens. This gives rise to enhanced apoptosis and amplified cellular waste load resulting in activation of an immune response and development of EBV-directed antibodies and autoantibodies to cellular antigens. [ABSTRACT FROM AUTHOR]

Published

2012

71. The Tumor Necrosis Factor Superfamily of Cytokines in the Inflammatory Myopathies: Potential Targets for Therapy.

Author

Paepe, Boel De, Creus, KimK., and De Bleecker, Jan L.

Subjects

TUMOR necrosis factors, MYOSITIS, CYTOKINES, AUTOIMMUNE diseases, DERMATOMYOSITIS, THERAPEUTICS

Abstract

The idiopathic inflammatorymyopathies (IM) represent a heterogeneous group of autoimmune diseases, of which dermatomyositis (DM), polymyositis (PM), and sporadic inclusion bodymyositis (IBM) are the most common. The crucial role played by tumor necrosis factor alpha (TNFα) in the IM has long been recognized. However, so far, 18 other members of the TNF superfamily have been characterized, and many of these have not yet received the attention they deserve. In this paper, we summarize current findings for all TNF cytokines in IM, pinpointing what we know already and where current knowledge fails. For each TNF family member, possibilities for treating inflammatory diseases in general and the IM in particular are explored. [ABSTRACT FROM AUTHOR]

Published

2012

72. Notch Signaling Mediates TNF-α-Induced IL-6 Production in Cultured Fibroblast-Like Synoviocytes from Rheumatoid Arthritis.

Author

Zhijun Jiao, Wenhong Wang, Jie Ma, Shengjun Wang, Zhaoliang Su, and Huaxi Xu

Subjects

RHEUMATOID arthritis, FIBROBLASTS, MESSENGER RNA, AUTOIMMUNE diseases, SYNOVIAL membranes

Abstract

It has been reported that Notch family proteins are expressed in synovium tissue and involved in the proliferation of synoviocyte from rheumatoid arthritis (RA). The aim of this paper was to investigate whether Notch signaling mediated TNF-α-induced cytokine production of cultured fibroblast-like synoviocytes (FLSs) from RA. Exposure of RA FLSs to TNF-α (10 ng/ml) led to increase of Hes-1, a target gene of Notch signaling, and a marked upregulation of Notch 2, Delta-like 1, and Delta-like 3 mRNA levels. Blockage of Notch signaling by a γ-secretase inhibitor (DAPT) inhibited IL-6 secretion of RA FLSs in response to TNF-α while treatment with recombinant fusion protein of Notch ligand Delta-like 1 promoted such response. TNF-α stimulation also induced IL-6 secretion in OA FLSs; however, the Hes-1 level remained unaffected. Our data confirm the functional involvement of Notch pathway in the pathophysiology of RA FLSs which may provide a new target for RA therapy. [ABSTRACT FROM AUTHOR]

Published

2012

73. The Place of Immunotherapy in the Management of HCV-Induced Vasculitis: An Update.

Author

Chiche, Laurent, Bataille, Stanislas, Kaplanski, Gilles, and Jourde, Noemie

Subjects

CHRONIC hepatitis C, IMMUNOTHERAPY, RITUXIMAB, ANTIVIRAL agents, ANTI-inflammatory agents, ANTIPYRETICS, T cells, INTERLEUKIN-2

Abstract

Patients with chronic hepatitis C virus (HCV) can develop systemic cryoglobulinemic vasculitis. Combination of pegylatedinterferon α and ribavirin is the first-line treatment of this condition. However, in case of severe or life-threatening manifestations, absence of a virological response, or autonomized vasculitis, immunotherapy (alone or in addition to the antiviral regimen) is necessary. Rituximab is to date the only biologic with a sufficient level of evidence to support its use in this indication. Several studies have demonstrated that rituximab is highly effective when cryoglobulinaemic vasculitis is refractory to antiviral regimen, that association of rituximab with antiviral regimen may induce a better and faster clinical remission, and, recently, that rituximab is more efficient than traditional immunosuppressive treatments. Some issues with regard to the optimal dose of rituximab or its use as maintenance treatment remain unsolved. Interestingly, in balance with this anti-inflammatory strategy, a recent pilot study reported the significant expansion of circulating regulatory T lymphocytes with concomitant clinical improvement in patients with refractory HCV-induced cryoglobulinaemic vasculitis using low dose of subcutaneous interleukin-2. This paper provides an updated overview on the place of immunotherapy, especially biologics, in the management of HCV-induced cryoglobulinaemic vasculitis. [ABSTRACT FROM AUTHOR]

Published

2012

74. New Platform Technology for Comprehensive Serological Diagnostics of Autoimmune Diseases.

Author

Willitzki, Annika, Hiemann, Rico, Peters, Vanessa, Sack, Ulrich, Schierack, Peter, Rödiger, Stefan, Anderer, Ursula, Conrad, Karsten, Bogdanos, Dimitrios P., Reinhold, Dirk, and Roggenbuck, Dirk

Subjects

AUTOIMMUNE diseases, RHEUMATISM, IMMUNOFLUORESCENCE, ANTINUCLEAR factors, IMMUNOASSAY, ARTHRITIS, MUSCULOSKELETAL system diseases

Abstract

Antibody assessment is an essential part in the serological diagnosis of autoimmune diseases. However, different diagnostic strategies have been proposed for the work up of sera in particular from patients with systemic autoimmune rheumatic disease (SARD). In general, screening for SARD-associated antibodies by indirect immunofluorescence (IIF) is followed by confirmatory testing covering different assay techniques. Due to lacking automation, standardization, modern data management, and human bias in IIF screening, this two-stage approach has recently been challenged by multiplex techniques particularly in laboratories with high workload. However, detection of antinuclear antibodies by IIF is still recommended to be the gold standard method for antibody screening in sera from patients with suspected SARD. To address the limitations of IIF and to meet the demand for costefficient autoantibody screening, automated IIF methods employing novel pattern recognition algorithms for image analysis have been introduced recently. In this respect, the AKLIDES technology has been the first commercially available platformfor automated interpretation of cell-based IIF testing and provides multiplexing by addressable microbead immunoassays for confirmatory testing. This paper gives an overview of recently published studies demonstrating the advantages of this new technology for SARD serology. [ABSTRACT FROM AUTHOR]

Published

2012

75. Non-MHC Risk Alleles in Rheumatoid Arthritis and in the Syntenic Chromosome Regions of Corresponding Animal Models.

Author

Besenyei, Timea, Kadar, Andras, Tryniszewska, Beata, Kurko, Julia, Rauch, Tibor A., Glant, Tibor T., Mikecz, Katalin, and Szekanecz, Zoltan

Subjects

RHEUMATOID arthritis, AUTOIMMUNE diseases, ARTHRITIS, RHEUMATISM, JOINT diseases, LABORATORY rats

Abstract

Rheumatoid arthritis (RA) is a polygenic autoimmune disease primarily affecting the synovial joints. Numerous animal models show similarities to RA in humans; some of them not only mimic the clinical phenotypes but also demonstrate the involvement of homologous genomic regions in RA. This paper compares corresponding non-MHC genomic regions identified in rodent and human genome-wide association studies (GWAS). To date, over 30 non-MHC RA-associated loci have been identified in humans, and over 100 arthritis-associated loci have been identified in rodentmodels of RA. The genomic regions associated with the disease are designated by the name(s) of the gene having the most frequent and consistent RA-associated SNPs or a function suggesting their involvement in inflammatory or autoimmune processes. Animal studies on rats and mice preferentially have used single sequence length polymorphism (SSLP) markers to identify disease-associated qualitative and quantitative trait loci (QTLs) in the genome of F2 hybrids of arthritis-susceptible and arthritis-resistant rodent strains. Mouse GWAS appear to be far ahead of rat studies, and significantly more mouse QTLs correspond to human RA risk alleles. [ABSTRACT FROM AUTHOR]

Published

2012

76. Perinatal Gene-Gene and Gene-Environment Interactions on IgE Production and Asthma Development.

Author

Chang, Jen-Chieh, Wang, Lin, Chang, Rong-Fu, and Liu, Chieh-An

Subjects

ASTHMA in children, NUCLEOTIDE sequence, GENOTYPE-environment interaction, ASTHMA prevention, CHROMOSOMES, GENE regulatory networks, SEQUENCE alignment

Abstract

Atopic asthma is a complex disease associated with IgE-mediated immune reactions. Numerous genome-wide studies identified more than 100 genes in 22 chromosomes associated with atopic asthma, and different genetic backgrounds in different environments could modulate susceptibility to atopic asthma. Current knowledge emphasizes the effect of tobacco smoke on the development of childhood asthma. This suggests that asthma, although heritable, is significantly affected by gene-gene and gene-environment interactions. Evidence has recently shown that molecular mechanism of a complex disease may be limited to not only DNA sequence differences, but also gene-environmental interactions for epigenetic difference. This paper reviews and summarizes how gene-gene and gene-environment interactions affect IgE production and the development of atopic asthma in prenatal and childhood stages. Based on the mechanisms responsible for perinatal gene-environment interactions on IgE production and development of asthma, we formulate several potential strategies to prevent the development of asthma in the perinatal stage. [ABSTRACT FROM AUTHOR]

Published

2012

77. Correlation of Circulating Glucocorticoid-Induced TNFR-Related Protein Ligand Levels with Disease Activity in Patients with Systemic Lupus Erythematosus.

Author

Lei Gu, Lingxiao Xu, Xiaojun Zhang, Wenfeng Tan, HongWang, and Miaojia Zhang

Subjects

TUMOR necrosis factor receptors, SYSTEMIC lupus erythematosus, BLOOD sedimentation, VASCULITIS, AUTOIMMUNE diseases, GLUCOCORTICOIDS, VASCULAR diseases

Abstract

The aim of this paper is to investigate the correlation of glucocorticoid-induced tumor necrosis factor receptor- (TNFR-) related protein ligand (GITRL) with disease activity and organ involvement in patients with systemic lupus erythematosus (SLE). Serum GITRL levels were measured in 58 patients with SLE and 30 healthy controls matched for age and sex. Patients were assessed for clinical and laboratory variables. Correlations of serum GITRL levels with SLEDAI, laboratory values, and clinical manifestations were assessed. Serum GITRL levels were determined by ELISA. Serum GITRL levels were markedly increased in patients with SLE compared with healthy controls (mean 401.3 ng/mL and 36.59 ng/mL, resp.; P < 0.0001). SLE patients with active disease showed higher serum GITRL levels compared to those with inactive disease (mean 403.3 ng/mL and 136.3 ng/mL, resp; P = 0.0043) as well as normal controls (36.59 ng/mL; P < 0.0001). Serum GITRL levels were positively correlated with SLEDAI, titers of antidsDNA antibody, erythrocyte sedimentation rate (ESR), and IgM and negatively correlated with complement3 (C3). SerumGITRL levels were higher in SLE patients with renal involvement and vasculitis compared with patients without the above-mentioned manifestations. [ABSTRACT FROM AUTHOR]

Published

2012

78. RP105-Negative B Cells in Systemic Lupus Erythematosus.

Author

Koarada, Syuichi and Tada, Yoshifumi

Subjects

B cells, SYSTEMIC lupus erythematosus, AUTOANTIBODIES, NUCLEAR proteins, TOLL-like receptors, IMMUNOLOGY

Abstract

Systemic lupus erythematosus (SLE) is a multisystem disease characterized by B cells producing autoantibodies against nuclear proteins and DNA, especially anti-double-strand DNA (dsDNA) antibodies. RP105 (CD180), the toll-like receptor- (TLR-) associated molecule, is expressed on normal B cells. However, RP105-negative B cells increase in peripheral blood from patients with active SLE. RP105 may regulate B-cell activation, and RP105-negative B cells produce autoantibodies and take part in pathophysiology of SLE. It is possible that targeting RP105-negative B cells is one of the treatments of SLE. In this paper, we discuss the RP105 biology and clinical significance in SLE. [ABSTRACT FROM AUTHOR]

Published

2012

79. Immunologic Regulation in Pregnancy: From Mechanism to Therapeutic Strategy for Immunomodulation.

Author

Chen, Shyi-Jou, Liu, Yung-Liang, and Sytwu, Huey-Kang

Subjects

IMMUNOREGULATION, HLA histocompatibility antigens, INFLAMMATORY mediators, IMMUNOLOGICAL aspects of pregnancy, IMMUNOLOGY

Abstract

The immunologic interaction between the fetus and the mother is a paradoxical communication that is regulated by fetal antigen presentation and/or by recognition of and reaction to these antigens by the maternal immune system. There have been significant advances in understanding of abnormalities in the maternal-fetal immunologic relationship in the placental bed that can lead to pregnancy disorders. Moreover, immunologic recognition of pregnancy is vital for the maintenance of gestation, and inadequate recognition of fetal antigens may cause abortion. In this paper, we illustrate the complex immunologic aspects of human reproduction in terms of the role of human leukocyte antigen (HLA), immune cells, cytokines and chemokines, and the balance of immunity in pregnancy. In addition, we review the immunologic processes of human reproduction and the current immunologic therapeutic strategies for pathological disorders of pregnancy. [ABSTRACT FROM AUTHOR]

Published

2012

80. Dermatitis Herpetiformis: From the Genetics to the Development of Skin Lesions.

Author

Bonciani, Diletta, Verdelli, Alice, Bonciolini, Veronica, D'Errico, Antonietta, Antiga, Emiliano, Fabbri, Paolo, and Caproni, Marzia

Subjects

DERMATITIS herpetiformis, AUTOIMMUNE diseases, CELIAC disease, GLUTEN allergenicity, IMMUNOGLOBULIN A, IMMUNOLOGY

Abstract

Dermatitis herpetiformis (DH) is a rare autoimmune disease linked to gluten sensitivity with a chronic-relapsing course. It is currently considered to be the specific cutaneous manifestation of celiac disease (CD). Both conditions are mediated by the IgA class of autoantibodies, and the diagnosis of DH is dependent on the detection of granular deposits of IgA in the skin. There is an underlying genetic predisposition to the development of DH, but environmental factors are also important. This paper describes these different factors and discusses the known mechanism that lead to the development of skin lesions. [ABSTRACT FROM AUTHOR]

Published

2012

81. The Impact of Osteopontin Gene Variations on Multiple Sclerosis Development and Progression.

Author

Comi, Cristoforo, Cappellano, Giuseppe, Chiocchetti, Annalisa, Orilieri, Elisabetta, Buttini, Sara, Ghezzi, Laura, Galimberti, Daniela, Guerini, Franca, Barizzone, Nadia, Perla, Franco, Leone, Maurizio, D'Alfonso, Sandra, Caputo, Domenico, Scarpini, Elio, Cantello, Roberto, and Dianzani, Umberto

Subjects

OSTEOPONTIN, MULTIPLE sclerosis, SINGLE nucleotide polymorphisms, DISEASE relapse, DISEASE progression, IMMUNOLOGY

Abstract

Osteopontin is a proinflammatory molecule, modulating TH1 and TH17 responses. Several reports suggest its involvement in multiple sclerosis (MS) pathogenesis. We previously reported that OPN gene variations at the 3' end are a predisposing factor for MS development and evolution. In this paper, we extended our analysis to a gene variation at the 5' end on the -156G > GG single nucleotide polymorphism (SNP) and replicated our previous findings at the 3' end on the +1239A > C SNP. We found that only +1239A > C SNP displayed a statistically significant association with MS development, but both +1239A > C and -156G > GG had an influence onMS progression, since patients homozygous for both +1239A and -156GG alleles displayed slower progression of disability and slower switch to secondary progression than those carrying +1239C and/or -156G and those homozygous for +1239A only. Moreover, patients homozygous for +1239A also displayed a significantly lower relapse rate than those carrying +1239C, which is in line with the established role of OPN in MS relapses. [ABSTRACT FROM AUTHOR]

Published

2012

82. Cellular and Humoral Mechanisms Involved in the Control of Tuberculosis.

Author

Zuñiga, Joaquin, Torres-García, Diana, Santos-Mendoza, Teresa, Rodriguez-Reyna, Tatiana S., Granados, Julio, and Yunis, Edmond J.

Subjects

MYCOBACTERIUM tuberculosis, PUBLIC health, CYTOKINES, CHEMOKINES, DENDRITIC cells, MACROPHAGES, AUTOIMMUNE diseases

Abstract

Mycobacterium tuberculosis (Mtb) infection is a major international public health problem. One-third of the world's population is thought to have latent tuberculosis, a condition where individuals are infected by the intracellular bacteria without active disease but are at risk for reactivation, if their immune system fails. Here, we discuss the role of nonspecific inflammatory responses mediated by cytokines and chemokines induced by interaction of innate receptors expressed in macrophages and dendritic cells (DCs). We also review current information regarding the importance of several cytokines including IL-17/IL-23 in the development of protective cellular and antibody-mediated protective responses against Mtb and their influence in containment of the infection. Finally, in this paper, emphasis is placed on the mechanisms of failure of Mtb control, including the immune dysregulation induced by the treatment with biological drugs in different autoimmune diseases. Further functional studies, focused on the mechanisms involved in the early host-Mtb interactions and the interplay between host innate and acquired immunity against Mtb, may be helpful to improve the understanding of protective responses in the lung and in the development of novel therapeutic and prophylactic tools in TB. [ABSTRACT FROM AUTHOR]

Published

2012

83. The Role of the Intestinal Context in the Generation of Tolerance and Inflammation.

Author

Sgarbi Reis, Bernardo and Mucida, Daniel

Subjects

ANTIGENS, LYMPHOID tissue, IMMUNE response, IMMUNE system, ANTIBODY formation

Abstract

The mucosal surface of the intestine alone forms the largest area exposed to exogenous antigens as well as the largest collection of lymphoid tissue in the body. The enormous amount of nonpathogenic and pathogenic bacteria and food-derived antigens that we are daily exposed sets an interesting challenge to the immune system: a protective immune activity must coexist with efficient regulatory mechanisms in order to maintain a health status of these organisms. This paper discusses how the immune system assimilates the perturbations from the environment without generating tissue damage. [ABSTRACT FROM AUTHOR]

Published

2012

84. Different Implications of Paternal and Maternal Atopy for Perinatal IgE Production and Asthma Development.

Author

Chih-Chiang Wu, Rong-Fu Chen, and Ho-Chang Kuo

Subjects

IMMUNOGLOBULIN E, ATOPY, POSTNATAL care, ASTHMA prevention, EPIGENETICS

Abstract

Asthma is a hereditary disease associated with IgE-mediated reaction. Whether maternal atopy and paternal atopy have different impacts on perinatal IgE production and asthma development remains unclear. This paper reviews and summarizes the effects of maternal and paternal atopy on the developmental aspects of IgE production and asthma. Maternal atopy affects both pre- and postnatal IgE production, whereas paternal atopy mainly affects the latter. Maternally transmitted genes GSTP1 and FceRI-beta are associated with lung function and allergic sensitization, respectively. In IgE production and asthma development, the maternal influence on gene-environment interaction is greater than paternal influence. Maternal, paternal, and/or postnatal environmental modulation of allergic responses have been linked to epigenetic mechanisms, which may be good targets for early prevention of asthma. [ABSTRACT FROM AUTHOR]

Published

2012

85. Mechanisms behind Functional Avidity Maturation in T Cells.

Author

Von Essen, Marina Rode, Kongsbak, Martin, and Geisler, Carsten

Subjects

T cells, IMMUNE response, ANTIBODY formation, ANTIGENS, B cells

Abstract

During an immune response antigen-primed B-cells increase their antigen responsiveness by affinity maturation mediated by somatic hypermutation of the genes encoding the antigen-specific B-cell receptor (BCR) and by selection of higher-affinity B cell clones. Unlike the BCR, the T-cell receptor (TCR) cannot undergo affinity maturation. Nevertheless, antigen-primed T cells significantly increase their antigen responsiveness compared to antigen-inexperienced (naïve) T cells in a process called functional aviditymaturation. This paper covers studies that describe differences in T-cell antigen responsiveness during T-cell differentiation along with examples of the mechanisms behind functional avidity maturation in T cells. [ABSTRACT FROM AUTHOR]

Published

2012

86. Lung Cancer: A Classic Example of Tumor Escape and Progression While Providing Opportunities for Immunological Intervention.

Author

Jadus, Martin R., Natividad, Josephine, Mai, Anthony, YiOuyang, Lambrecht, Nils, Szabo, Sandor, Ge, Lisheng, Hoa, Neil, and Dacosta-Iyer, Maria G.

Subjects

LUNG cancer treatment, IMMUNOLOGY, RADIOTHERAPY, TREATMENT effectiveness, IMMUNOTHERAPY

Abstract

Lung cancers remain one of the most common and deadly cancers in the world today (12.5% of newly diagnosed cancers) despite current advances in chemo- and radiation therapies. Often, by the time these tumors are diagnosed, they have already metastasized. These tumors demonstrate the classic hallmarks of cancer in that they have advanced defensive strategies allowing them to escape various standard oncological treatments. Immunotherapy is making inroads towards effectively treating other fatal cancers, such as melanoma, glioblastoma multiforme, and castrate-resistant prostate cancers. This paper will cover the escape mechanisms of bronchogenic lung cancer thatmust be overcome before they can be successfully treated.We also review the history of immunotherapy directed towards lung cancers. [ABSTRACT FROM AUTHOR]

Published

2012

87. Mucosal Herpes Immunity and Immunopathology to Ocular and Genital Herpes Simplex Virus Infections.

Author

Chentoufi, Aziz Alami and Ben Mohamed, Lbachir

Subjects

HERPES simplex virus, IMMUNE response, IMMUNOPATHOLOGY, PATHOGENIC microorganisms, HERPES genitalis

Abstract

Herpes simplex viruses type 1 and type 2 (HSV-1 and HSV-2) are amongst the most common human infectious viral pathogens capable of causing serious clinical diseases at every stage of life, from fatal disseminated disease in newborns to cold sores genital ulcerations and blinding eye disease. Primary mucocutaneous infection with HSV-1 & HSV-2 is followed by a lifelong viral latency in the sensory ganglia. In themajority of cases, herpes infections are clinically asymptomatic.However, in symptomatic individuals, the latentHSV can spontaneously and frequently reactivate, reinfecting themuco-cutaneous surfaces and causing painful recurrent diseases. The innate and adaptive mucosal immunities to herpes infections and disease remain to be fully characterized. The understanding of innate and adaptive immune mechanisms operating at muco-cutaneous surfaces is fundamental to the design of next-generation herpes vaccines. In this paper, the phenotypic and functional properties of innate and adaptive mucosal immune cells, their role in antiherpes immunity, and immunopathology are reviewed. The progress and limitations in developing a safe and efficient mucosal herpes vaccine are discussed [ABSTRACT FROM AUTHOR]

Published

2012

88. Autoantibodies and Resident Renal Cells in the Pathogenesis of Lupus Nephritis: Getting to Know the Unknown.

Author

Susan Yung and TakMao Chan

Subjects

AUTOANTIBODIES, LUPUS nephritis, SYSTEMIC lupus erythematosus, CHRONIC kidney failure, PROTEIN binding

Abstract

Systemic lupus erythematosus is characterized by a breakdown of self-tolerance and production of autoantibodies. Kidney involvement (i.e., lupus nephritis) is both common and severe and can result in permanent damage within the glomerular, vascular, and tubulo-interstitial compartments of the kidney, leading to acute or chronic renal failure. Accumulating evidence shows that anti-dsDNA antibodies play a critical role in the pathogenesis of lupus nephritis through their binding to cell surface proteins of resident kidney cells, thereby triggering the downstream activation of signaling pathways and the release of mediators of inflammation and fibrosis. This paper describes themechanisms through which autoantibodies interact with resident renal cells and how this interaction plays a part in disease pathogenesis that ultimately leads to structural and functional alterations in lupus nephritis. [ABSTRACT FROM AUTHOR]

Published

2012

89. Are Toll-Like Receptors and Decoy Receptors Involved in the Immunopathogenesis of Systemic Lupus Erythematosus and Lupus-Like Syndromes?

Author

Guggino, Giuliana, Rita Giardina, Anna, Ciccia, Francesco, Triolo, Giovanni, Dieli, Francesco, and Sireci, Guido

Subjects

TOLL-like receptors, SYSTEMIC lupus erythematosus, LABORATORY mice, AUTOIMMUNE diseases, CLINICAL trials, GENETICS

Abstract

In this paper we focus our attention on the role of two families of receptors, Toll-like receptors (TLR) and decoy receptors (DcR) involved in the generation of systemic lupus erythematosus (SLE) and lupus-like syndromes in human and mouse models. To date, these molecules were described in several autoimmune disorders such as rheumatoid arthritis, antiphospholipids syndrome, bowel inflammation, and SLE. Here, we summarize the findings of recent investigations on TLR and DcR and their role in the immunopathogenesis of the SLE. [ABSTRACT FROM AUTHOR]

Published

2012

90. Immunology and Immunodiagnosis of Cystic Echinococcosis: An Update.

Author

Wenbao Zhang, Hao Wen, Jun Li, Renyong Lin, and McManus, Donald P.

Subjects

DIAGNOSIS of Echinococcosis, IMMUNODIAGNOSIS, IMMUNOLOGY, ECHINOCOCCUS granulosus, IMMUNE response

Abstract

Cystic echinococcosis (CE) is a cosmopolitan zoonosis caused by the larval cystic stage of the dog tapeworm Echinococcus granulosus. This complex multicellular pathogen produces various antigens which modulate the host immune response and promote parasite survival and development. The recent application of modern molecular and immunological approaches has revealed novel insights on the nature of the immune responses generated during the course of a hydatid infection, although many aspects of the Echinococcus-host interplay remain unexplored. This paper summarizes recent developments in our understanding of the immunology and diagnosis of echinococcosis, indicates areas where information is lacking, and suggests possible new strategies to improve serodiagnosis for practical application. [ABSTRACT FROM AUTHOR]

Published

2012

91. The Inhibitory Role of B7-H4 in Antitumor Immunity: Association with Cancer Progression and Survival.

Author

Changjun He, Haiquan Qiao, Hongchi Jiang, and Xueying Sun

Subjects

*CANCER invasiveness, *SURVIVAL, *MOLECULES, *CANCER patients, *THERAPEUTICS

Abstract

B7-H4 is one of the most recently identified members of B7 superfamily of costimulatory molecules serving as an inhibitory modulator of T-cell response. B7-H4 is broadly expressed in human peripheral tissues and inducibly expressed in immune cells. The expression of B7-H4 has been observed in various types of human cancer tissues, and its soluble form has been detected in blood samples fromcancer patients. However, its precise physiological role is still elusive, as its receptor has not been identified and the expression levels are not consistent. This paper summarizes the pertinent data on the inhibitory role of B7-H4 in antitumor immunity and its association with cancer progression and survival in human patients. The paper also discusses the clinical significance of investigating B7-H4 as potential markers for cancer diagnosis and prognosis, and as therapeutic targets. [ABSTRACT FROM AUTHOR]

Published

2011

92. Flavonoid-membrane interactions: A protective role of flavonoids at the membrane surface?

Author

Oteiza, Patricia I., Erlejman, Alejandra G., Verstraeten, Sandra V., Keen, Carl L., and Fraga, César G.

Subjects

FLAVONOIDS, CELL membranes, POLYPHENOLS, HYDROPHOBIC surfaces, MEMBRANE lipids, OXIDATION

Abstract

Flavonoids can exert beneficial health effects through multiple mechanisms. In this paper, we address the important, although not fully understood, capacity of flavonoids to interact with cell membranes. The interactions of polyphenols with bilayers include: (a) the partition of the more non-polar compounds in the hydrophobic interior of the membrane, and (b) the formation of hydrogen bonds between the polar head groups of lipids and the more hydrophilic flavonoids at the membrane interface. The consequences of these interactions are discussed. The induction of changes in membrane physical properties can affect the rates of membrane lipid and protein oxidation. The partition of certain flavonoids in the hydrophobic core can result in a chain breaking antioxidant activity. We suggest that interactions of polyphenols at the surface of bilayers through hydrogen bonding, can act to reduce the access of deleterious molecules (i.e. oxidants), thus protecting the structure and function of membranes. [ABSTRACT FROM AUTHOR]

Published

2005

93. The Possible Role of Natural Idiotopes in Immune Memory.

Author

Ljiljana Dimitrijević, Snezana Živančević-Simonović, Marijana Stojanović, Aleksandra Inić-Kanada, and Irena Žvković

Subjects

IMMUNOLOGIC memory, BACTERIAL antigens, MONOCLONAL antibodies, IDIOTYPIC networks, LACTIC acid, IMMUNOGLOBULINS

Abstract

In this paper we report on the generation of Abs possessing specificities similar to those of Abs used in immunization, and on the generation of Id and anti-Id specificities in the sera of mice immunized with commensal bacterial antigens. The human monoclonal antibody IgM DJ (VH3/VL2) expresses natural antibody properties, natural idiotope (Y7). and specificity towards Lactic acid bacteria (LAB). When used in immunization it generates LAB-specific antibodies. Immunization with LAB, as detected in the presence of biotin-labelled mouse monoclonal anti-idiotopic antibodies Y7 and IgM DJ generates Abs I and Abs2. respectively. These findings may imply that the recognition of bacterial motifs accords with the rules of idiotypic network theory. This theory. First proposed by Jerne in 1974 and often overlooked since, has been subject to change during the course of immunological research. Recent experiments concerning the recognition of bacterial motifs and natural memory in the immune system have inspired us in our attempt at explaining the possible role of natural Id in immune memory. [ABSTRACT FROM AUTHOR]

Published

2004

94. Determinants of Vessel Targeting in Vasculitis.

Author

Hoffman, Gary S.

Subjects

VASCULITIS, AORTA, GIANT cell arteritis, ATHEROSCLEROSIS, VASCULAR diseases, INFLAMMATION

Abstract

Studies of autoimmune diseases have not yet elucidated why certain organs or vessels become the objects of injury while others are spared- This paper will explore the hypothesis that important differences exist in regions of the aorta that determine vulnerability to diseases, such as atherosclerosis, aortitis, giant cell arteritis and Takayasu's disease. The reader is invited to reassess; (1) whether the aorta is indeed a single homogeneous structure, and (2) whether the initial stage of aortitis (and indeed other diseases considered"autoimmune) may be primarily due to acquired alterations of substrate, that influence unique immune profiles, which by themselves may not be pathogenic. Disease susceptibility and patterns are influenced by many factors that are inborn and acquired. Examples include genetic background, gender, ethnicity, aging, prior and concomitant illnesses, habits, diet, toxin and environmental exposures. Studies of vascular diseases must assess how such variables may affect regional differences in endothelial cells, subendothelial matrix, vascular smooth muscle and the response of each to a variety of stimuli. [ABSTRACT FROM AUTHOR]

Published

2004

95. Tolerance and Inflammation at the Gut Mucosa.

Author

Faria, AnaMaria C., Mucida, Daniel, McCafferty, Donna-Marie, Tsuji, Noriko M., and Verhasselt, Valerie

Subjects

INFLAMMATORY bowel diseases, IMMUNE response, FOOD allergy

Abstract

An introduction is presented in which the editor discusses various reports within the issue on topics including the pathogenesis of inflammatory bowel diseases (IBDs), gut immune responses, and food allergy development.

Published

2012

96. Immunity to Ocular and Genital Herpes Simplex Viruses Infections.

Author

Chentoufi, Aziz Alami, BenMohamed, Lbachir, De Perre, Philippe Van, and Ashkar, Ali A.

Subjects

HERPESVIRUS diseases, VACCINATION, CELLULAR immunity

Abstract

An introduction is presented in which the editor discusses various reports within the issue on topics including human herpesviruses, herpes vaccine development, and mucosal immunity.

Published

2012

97. Immunity to Human Immunodeficiency Virus (HIV) Infection.

Author

Torti, Carlo, Paiardini, Mirko, and Gori, Andrea

Subjects

HIV, HIGHLY active antiretroviral therapy, IMMUNITY

Abstract

An introduction is presented in which the editors discuss various reports within the issue on topics including HIV, highly active antiretroviral therapy (HAART) and immunity.

Published

2012

98. Immunonutrition in Early Life: Diet and Immune Development.

Author

Pérez-Cano, Francisco J., Yaqoob, Parveen, Martín,, Rocío, Castell Escuer, Margarida, and Juárez-Rubio, Cándido

Subjects

UNSATURATED fatty acids, CELIAC disease, NUTRITION

Abstract

An introduction is presented in which the editor discusses various reports within the issue on topics including the influence of polyunsaturated fatty acids (PUFAs) on atopic and respiratory diseases, the maintenance of a gluten-free diet in patients with coeliac disease (CD) and the environmental factors contributing to the development of CD.

Published

2012

99. Perinatal Programming of Childhood Asthma: Early Fetal Size, Growth Trajectory during Infancy, and Childhood Asthma Outcomes.

Author

Turner, Steve

Subjects

*PERINATOLOGY, *ASTHMA in children, *ETIOLOGY of diseases, *BIRTH weight, *DEVELOPMENTAL programs

Abstract

The "fetal origins hypothesis" or concept of "developmental programming" suggests that faltering fetal growth and subsequent catch-up growth are implicated in the aetiology of cardiovascular disease. Associations between reduced birth weight, rapid postnatal weight gain, and asthma suggest that there are fetal origins to respiratory disease. The present paper first summarises the literature relating birth weight and post natal growth trajectories to asthma outcomes. Second, issues regarding the interpretation of antenatal fetal ultrasound measurements are discussed. Finally, recent reports linking antenatal measurement and growth trajectory to early childhood asthma outcomes are discussed. Understanding the nature and timing of factors which influence antenatal growth may give important insight into the antecedents of early-onset asthma with implications for interventions. [ABSTRACT FROM AUTHOR]

Published

2012

100. A Spotlight on Liquefaction: Evidence from Clinical Settings and Experimental Models in Tuberculosis.

Author

Cardona, Pere-Joan

Subjects

*TUBERCULOSIS, *MACROPHAGES, *FIBROSIS, *IMMUNE response, *APOPTOSIS

Abstract

Liquefaction is one of the most intriguing aspects of human tuberculosis. It is a major cause of the transition from the infection to active disease (tuberculosis, TB) as well as the transmission of M. tuberculosis to other persons. This paper reviews the natural history of liquefaction in humans from a pathological and radiological point of view and discusses how the experimental models available can be used to address the topic of liquefaction and cavity formation. Different concepts that have been related to liquefaction, from the influence of immune response to mechanical factors, are reviewed. Synchronic necrosis or apoptosis of infected macrophages in a close area, together with an ineffective fibrosis, appears to be clue in this process, in which macrophages, the immune response, and bacillary load interact usually in a particular scenario: the upper lobes of the lung. The summary would be that even if being a stochastic effect, liquefaction would result if the organization of the intragranulomatous necrosis (by means of fibrosis) would be disturbed. [ABSTRACT FROM AUTHOR]

Published

2011