Showing total 435 results

151. Viruses and immunity in transplant patients.

Author

Cavallo, Rossana, Antonelli, Guido, and Hirsch, Hans H

Published

2013

152. Evaluation of Clinical Interest of Anti-Aquaporin-4 Autoantibody Followup in Neuromyelitis Optica.

Author

Chanson, Jean-Baptiste, Alame, Melissa, Collongues, Nicolas, Blanc, Frédéric, Fleury, Marie, Rudolf, Gabrielle, Seze, JérÔme de, and Vincent, Thierry

Subjects

MYELITIS, AQUAPORINS, AUTOANTIBODIES, CELL-mediated cytotoxicity, DISEASE relapse

Abstract

Neuromyelitis optica (NMO) is an autoimmune disease in which a specific biomarker named NMO-IgG and directed against aquaporin-4 (AQP4) has been found. A correlation between disease activity and anti-AQP4 antibody (Ab) serum concentration or complement-mediated cytotoxicity has been reported, but the usefulness of longitudinal evaluation of these parameters remains to be evaluated in actual clinical practice. Thirty serum samples from 10 NMO patients positive for NMO-IgG were collected from 2006 to 2011. Anti-AQP4 Ab serum concentration and complement-mediated cytotoxicity were measured by flow cytometry using two quantitative cell-based assays (CBA) and compared with clinical parameters. We found a strong correlation between serum anti-AQP4 Ab concentration and complement-mediated cytotoxicity (P < 0.0001). Nevertheless, neither relapse nor worsening of impairment level was closely associated with a significant increase in serum Ab concentration or cytotoxicity. These results suggest that complement-mediated serumcytotoxicity assessment does not provide extra insight compared to anti-AQP4 Ab serum concentration. Furthermore, none of these parameters appears closely related to disease activity and/or severity. Therefore, in clinical practice, serum anti-AQP4 reactivity seems not helpful as a predictive biomarker in the followup of NMO patients as a means of predicting the onset of a relapse and adapting the treatment accordingly. [ABSTRACT FROM AUTHOR]

Published

2013

153. Glucocorticoid-Induced TNFR-Related Protein Stimulation Reverses Cardiac Allograft Acceptance Induced by CD40-CD40L Blockade.

Author

Krill, Kenneth T., Csencsits-Smith, Keri, Wood, Sherri C., Faust, Susan, Lu, Guanyi, and Keith Bishop, D.

Subjects

IMMUNOSUPPRESSION, GLUCOCORTICOIDS, PROTEINS, HOMOGRAFTS, EOSINOPHILIA, T cells, LABORATORY mice

Abstract

CD40-CD40L blockade has potent immunosuppressive effects in cardiac allograft rejection but is less effective in the presence of inflammatory signals. To better understand the factors that mediate CD40-CD40L blockade-resistant rejection, we studied the effects of stimulation through glucocorticoid-induced TNFR-related protein (GITR), a costimulatory protein expressed by regulatory and effector T cells. Stimulation of CD40-/- or wild-type recipient mice treated with anti-CD40L mAb (WT+anti- CD40L) and with agonistic anti-GITR mAb resulted in cardiac allograft rejection. GITR stimulation did not induce rejection once long-term graft acceptance was established. In vitro, GITR stimulation increased proliferation of effector T cells and decreased regulatory T cell (Treg) differentiation in both treatment groups. GITR-stimulated CD40-/- recipients rejected their allografts more rapidly compared to GITR-stimulated WT+anti-CD40L recipients, and this rejection, characterized by a robust Th2 response and significant eosinophilic infiltrate, could be mediated by CD4+ T cells alone. In contrast, both CD4+ and CD8+ T cells were required to induce rejection in GITR-stimulated WT+anti-CD40L-treated recipients, and the pathology of rejection was less severe. Hence, early GITR stimulation could initiate graft rejection despite CD40 deficiency or anti-CD40L mAb treatment, though the recipient response was dependent on the mechanism of CD40-CD40L disruption. [ABSTRACT FROM AUTHOR]

Published

2013

154. CUZD1 and Anti-CUZD1 Antibodies as Markers of Cancer and Inflammatory Bowel Diseases.

Author

Liaskos, Christos, Rigopoulou, Eirini I., Orfanidou, Timoklia, Bogdanos, Dimitrios P., and Papandreou, Christos N.

Subjects

INFLAMMATORY bowel diseases, IMMUNOGLOBULINS, ANTIGENS, AUTOANTIBODIES, CHROMOSOMES, OVARIAN diseases, TUMORS, CARCINOGENESIS

Abstract

CUZD1, the CUB, and zona pellucida-like domains-containing protein 1, is a newly identified antigen of pancreatic autoantibodies (PAB) giving a reticulogranular pattern in patients with inflammatory bowel diseases, and in particular Crohn's disease. The exact mechanisms by which this pancreatic antigen becomes the target of IBD-specific pancreatic autoantibodies are unclear. At the same time, evolving data strongly support a role for CUZD1 in carcinogenesis. Human CUZD1 is mapped at chromosome 10q26.13 and the loss of this region is a frequent event in various malignant tumours. mRNA overexpression of CUZD1 has been noted in ovarian cancer and serum levels of CUZD1 are elevated in women with ovarian cancer and patients suffering from pancreatic cancer. CUZD1 appears to be one of the relatively few biomarkers that serve as both cancer biomarker and autoantigen of autoantibodies in an autoimmune disease unrelated to cancerous organs. This review discusses the role of CUZD1 in cancer and autoimmunity. We anticipate that a better understanding of the function of CUZD1 will help us to understand how it becomes the focus of an autoimmune attack specifically targeting the intestine and its enigmatic role in carcinogenesis. [ABSTRACT FROM AUTHOR]

Published

2013

155. Viral Aetiology in Adults with Acute Upper Respiratory Tract Infection in Jinan, Northern China.

Author

Yanqin Lu, Jiabei Tong, Fengyan Pei, Yanping Yang, Dong Xu, Mingyu Ji, Chunyan Xing, Pingdong Jia, Chao Xu, Yunshan Wang, Gongchao Li, Zhenbin Chai, Yan Liu, and Jinxiang Han

Subjects

RESPIRATORY infections, ETIOLOGY of diseases, POLYMERASE chain reaction, DISEASES in adults

Abstract

Our study investigated the epidemiology of respiratory viruses in adult patients with upper respiratory tract infection (URTI) between August 2009 and September 2010 in Jinan, northern China. Nasal and throat swabs (n = 596) were collected from adult patients with URTIs. Nine respiratory-related viruses, including IFV, PIV, HRV, HMPV, HBoV, HCoV, ADV, RSV, and EV, were detected in all samples by conventional and reverse transcription polymerase chain reactions. Positive detection rate for respiratory virus was 38.76% and codetection rate was 4.70% in adults with acute respiratory tract infections. IFV (20.81%) was the dominant agent detected and IFVB had a higher incidence (12.58%) than IFVA (7.72%). Detection rates of 8.22%, 5.03%, 3.69%, and 2.52% were observed for HBoV, HRV, EV, and RSV, respectively. HCoV had the lowest detection rate of 0.50%. HBoV, HRV, EV, and ADV infection rates were higher in the 14-25-year-old group than in the 26-65-year-old group. Codetection rates were higher (7.52%) in the 14-25-year-old group than in the older age group (2.64%).The spectrum of respiratory virus infection in adult patients with URTIs was different in Jinan compared with other cities in China. [ABSTRACT FROM AUTHOR]

Published

2013

156. Autoimmune Cytopenias in Chronic Lymphocytic Leukemia.

Author

D'Arena, Giovanni, Guariglia, Roberto, La Rocca, Francesco, Trino, Stefania, Condelli, Valentina, De Martino, Laura, De Feo, Vincenzo, and Musto, Pellegrino

Subjects

CHRONIC lymphocytic leukemia, AUTOIMMUNE diseases, PURE red cell aplasia, AGRANULOCYTOSIS, AUTOANTIBODIES, RITUXIMAB, B cells, HEMATOLOGY

Abstract

The clinical course of chronic lymphocytic leukemia (CLL) may be complicated at any time by autoimmune phenomena. The most common ones are hematologic disorders, such as autoimmune hemolytic anemia (AIHA) and immune thrombocytopenia (ITP). Pure red cell aplasia (PRCA) and autoimmune agranulocytosis (AG) are, indeed, more rarely seen. However, they are probably underestimated due to the possible misleading presence of cytopenias secondary to leukemic bone marrow involvement or to chemotherapy cytotoxicity. The source of autoantibodies is still uncertain, despite the most convincing data are in favor of the involvement of resting normal B-cells. In general, excluding the specific treatment of underlying CLL, the management of these complications is not different from that of idiopathic autoimmune cytopenias or of those associated to other causes. Among different therapeutic approaches, monoclonal antibody rituximab, given alone or in combination, has shown to be very effective. [ABSTRACT FROM AUTHOR]

Published

2013

157. Enteropathic Spondyloarthritis: From Diagnosis to Treatment.

Author

Peluso, Rosario, Dario DiMinno, Matteo Nicola, Iervolino, Salvatore, Mangus, Francesco, Tramontano, Giuseppina, Ambrosino, Pasquale, Esposito, Carmela, Scalera, Antonella, Castiglione, Fabiana, and Scarpa, Raffaele

Subjects

ARTHRITIS, INFLAMMATORY bowel diseases, GASTROINTESTINAL diseases, SPONDYLOARTHROPATHIES, RHEUMATISM, FIBROMYALGIA, DIAGNOSIS, THERAPEUTICS

Abstract

Enteropathic arthritis (EA) is a spondyloarthritis (SpA) which occurs in patients with inflammatory bowel diseases (IBDs) and other gastrointestinal diseases. Diagnosis is generally established on the medical history and physical examination. It was, generally, made according to the European Spondyloarthropathy Study Group (ESSG) criteria. Rheumatic manifestations are the most frequent extra intestinal findings of IBD with a prevalence between 17% and 39%, and IBD is associated, less frequently, with other rheumatic disease such as rheumatoid arthritis, Sjogren syndrome, Takayasu arteritis, and fibromyalgia. Although the pathogenesis of EA has not been plainly clarified, the most popular theory supposes that joint inflammation occurs in genetically predisposed subjects with bacterial gut infections, provided an important evidence for a possible relationship between inflammation of the gut mucosa and arthritis. The management of patients with EA requires an active cooperation between the gastroenterologist and rheumatologist. [ABSTRACT FROM AUTHOR]

Published

2013

158. Understanding Dendritic Cells and Their Role in Cutaneous Carcinoma and Cancer Immunotherapy.

Author

Yanofsky, Valerie R., Mitsui, Hiroshi, Felsen, Diane, and Carucci, John A.

Subjects

DENDRITIC cells, ANTIGENS, IMMUNE system, CANCER immunotherapy, LANGERHANS cells, SQUAMOUS cell carcinoma, CANCER treatment, SKIN cancer

Abstract

Dendritic cells (DC) represent a diverse group of professional antigen-presenting cells that serve to link the innate and adaptive immune systems. Their capacity to initiate a robust and antigen-specific immune response has made them the ideal candidates for cancer immunotherapies. To date, the clinical impact of DC immunotherapy has been limited, which may, in part, be explained by the complex nature of DC biology. Multiple distinct subsets of DCs have been identified in the skin, where they can be broadly subcategorized into epidermal Langerhans cells (LC), myeloid-derived dermal dendritic cells (mDC) and plasmacytoid dendritic cells (pDC). Each subset is functionally unique and may activate alternate branches of the immune system. This may be relevant for the treatment of squamous cell carcinoma, where we have shown that the tumor microenvironment may preferentially suppress the activity of mDCs, while LCs remain potent stimulators of immunity. Here, we provide an in depth analysis of DC biology, with a particular focus on skin DCs and their role in cutaneous carcinoma. We further explore the current approaches to DC immunotherapy and provide evidence for the targeting of LCs as a promising new strategy in the treatment of skin cancer. [ABSTRACT FROM AUTHOR]

Published

2013

159. Polyomavirus JC in the Context of Immunosuppression: A Series of Adaptive, DNA Replication-Driven Recombination Events in the Development of Progressive Multifocal Leukoencephalopathy.

Author

Johnson, Edward M., Wortman, Margaret J., Dagdanova, Ayuna V., Lundberg, Patric S., and Daniel, Dianne C.

Subjects

POLYOMAVIRUSES, ETIOLOGY of diseases, PROGRESSIVE multifocal leukoencephalopathy, IMMUNOSUPPRESSION, DNA replication, NEUROGLIA

Abstract

Polyomavirus JC (JCV) is the etiological agent of progressive multifocal leukoencephalopathy (PML), a demyelinating infection of oligodendrocytes in the brain. PML, a frequently fatal opportunistic infection in AIDS, has also emerged as a consequence of treatment with several new immunosuppressive therapeutic agents. Although nearly 80% of adults are seropositive, JCV attains an ability to infect glial cells in only a minority of people. Data suggest that JCV undergoes sequence alterations that accompany this ability, and these changes can be derived from an archetype strain by mutation, deletion, and duplication. While the introductory source and primary tissue reservoir of JCV remain unknown, lymphoid cells have been identified as potential intermediaries in progression of JCV to the brain. This review is focused on sequence changes in the noncoding control region (NCCR) of the virus. We propose an adaptive mechanism that involves a sequential series of DNA replication-driven NCCR recombination events involving stalled DNA replication forks at NCCR palindromic secondary structures. We shall describe how the NCCR sequence changes point to a model in which viral DNA replication drives NCCR recombination, allowing JCV adaptation to different cell types in its progression to neurovirulence. [ABSTRACT FROM AUTHOR]

Published

2013

160. NFAT Signaling in Osteoblasts Regulates the Hematopoietic Niche in the Bone Microenvironment.

Author

Sesler, Cheryl L. and Zayzafoon, Majd

Subjects

OSTEOBLASTS, HEMATOPOIETIC growth factors, T cells, BONE growth, GENE expression, PROTEINS, B cells, LABORATORY mice

Abstract

Osteoblasts support hematopoietic cell development, including B lymphopoiesis. We have previously shown that the nuclear factor of activated T cells (NFAT) negatively regulates osteoblast differentiation and bone formation. Interestingly, in smooth muscle, NFAT has been shown to regulate the expression of vascular cellular adhesion molecule-1 (VCAM-1), a mediator of cell adhesion and signaling during leukocyte development. To examine whether NFAT signaling in osteoblasts regulates hematopoietic development in vivo, we generated a mouse model expressing dominant-negative NFAT driven by the 2.3 kb fragment of the collagen-αI promoter to disrupt NFAT activity in osteoblasts (dnNFATOB). Bone histomorphometry showed that dnNFATOB mice have significant increases in bone volume (44%) and mineral apposition rate (131%) and decreased trabecular thickness (18%). In the bone microenvironment, dnNFATOB mice displayed a significant increase (87%) in Lineage-cKit+Sca-1+ (LSK) cells and significant decreases in B220+CD19-IgM- pre-pro-B cells (41%) and B220+CD19+IgM+ immature B cells (40%). Concurrent with these findings, LSK cell differentiation into B220+ cells was inhibited when cocultured on differentiated primary osteoblasts harvested from dnNFATOB mice. Gene expression and protein levels of VCAM-1 in osteoblasts decreased in dnNFATOB mice compared to controls. These data suggest that osteoblast-specific NFAT activity mediates early B lymphopoiesis, possibly by regulating VCAM-1 expression on osteoblasts. [ABSTRACT FROM AUTHOR]

Published

2013

161. A Review on JC Virus Infection in Kidney Transplant Recipients.

Author

Delbue, Serena, Ferraresso, Mariano, Ghio, Luciana, Carloni, Camilla, Carluccio, Silvia, Belingheri, Mirco, Edefonti, Alberto, and Ferrante, Pasquale

Subjects

PROGRESSIVE multifocal leukoencephalopathy, VIRUS diseases, KIDNEY diseases, DNA viruses, DNA virus diseases

Abstract

The polyomavirus (PyV), JC virus (JCV), is a small nonenveloped DNA virus that asymptomatically infects about 80%of healthy adults and establishes latency in the kidney tissue. In case of immunodeficient hosts, JCV can lytically infect the oligodendrocytes, causing a fatal demyelinating disease, known as progressive multifocal leukoencephalopathy (PML). Although the reactivation of another human PyV, BK virus (BKV), is relatively common and its association with the polyomavirus associated nephropathy (PyVAN) following renal transplantation is proven, JCV replication and its impact on graft function and survival are less well studied. Here we describe the biology of JCV and its pathological features and we review the literature regarding the JCV infection analyzed in the setting of transplantations. [ABSTRACT FROM AUTHOR]

Published

2013

162. Modulation of Tumor Immunity by Soluble and Membrane-Bound Molecules at the Immunological Synapse.

Author

González, Pablo A., Carreño, Leandro J., Céspedes, Pablo F., Bueno, Susan M., Riedel, Claudia A., and Kalergis, Alexis M.

Subjects

T cells, LYMPHOCYTES, MEMBRANE proteins, TUMOR growth, IMMUNE system

Abstract

To circumvent pathology caused by infectious microbes and tumor growth, the host immune system must constantly clear harmful microorganisms and potentially malignant transformed cells. This task is accomplished in part by T-cells, which can directly kill infected or tumorigenic cells. Acrucial event determining the recognition and elimination of detrimental cells is antigen recognition by the T cell receptor (TCR) expressed on the surface of T cells. Upon binding of the TCR to cognate peptide-MHC complexes presented on the surface of antigen presenting cells (APCs), a specialized supramolecular structure known as the immunological synapse (IS) assembles at the T cell-APC interface. Such a structure involves massive redistribution of membrane proteins, including TCR/pMHC complexes, modulatory receptor pairs, and adhesion molecules. Furthermore, assembly of the immunological synapse leads to intracellular events that modulate and define the magnitude and characteristics of the T cell response. Here, we discuss recent literature on the regulation and assembly of IS and the mechanisms evolved by tumors to modulate its function to escape T cell cytotoxicity, as well as novel strategies targeting the IS for therapy. [ABSTRACT FROM AUTHOR]

Published

2013

163. Erratum to "Sensitization to Cockroach Allergen: Immune Regulation and Genetic Determinants".

Author

Gao, Peisong

Subjects

IMMUNE system, GENETIC regulation

Abstract

A correction to the article "Sensitization to Cockroach Allergen: Immune Regulation and Genetic Determinants" that was published in the previous issue is presented.

Published

2012

164. Hyper-IgE Syndrome with STAT3 Mutation: A Case Report in Mainland China.

Author

Xie L, Hu X, Li Y, Zhang W, and Chen L

Abstract

Hyper-immunoglobulin E syndromes (HIES) including compound primary immunodeficiency and nonimmunological abnormalities are characterized by extremely high serum IgE levels, eosinophilia, eczema, susceptibility to infections, distinctive facial appearance, retention of deciduous teeth, cyst-forming pneumonias, and skeletal abnormalities. Itis reported that some cases of familial HIES are relative to autosomal dominant or recessive inheritance, but most cases are sporadic, and result from mutations in the human signal transducer and activator of transcription 3 (STAT3) gene. In this paper, we firstly report a young man diagnosed of Hyper-IgE syndrome with STAT3 mutation in Mainland China, and investigate the autosomal dominant trait of his family members. [ABSTRACT FROM AUTHOR]

Published

2010

165. Renal failure associated with APECED and terminal 4q deletion: evidence of autoimmune nephropathy.

Author

Al-Owain, Mohammed, Kaya, Namik, Al-Zaidan, Hamad, Bin Hussain, Ibrahim, Al-Manea, Hadeel, Al-Hindi, Hindi, Kennedy, Shelley, Iqbal, M Anwar, Al-Mojalli, Hamad, Al-Bakheet, Albandary, Puel, Anne, Casanova, Jean-Laurent, and Al-Muhsen, Saleh

Abstract

Autoimmune polyendocrinopathy-candidiasis-ectodermal dystrophy (APECED) is a rare autosomal recessive disorder caused by mutations in the autoimmune regulator gene (AIRE). Terminal 4q deletion is also a rare cytogenetic abnormality that causes a variable syndrome of dysmorphic features, mental retardation, growth retardation, and heart and limb defects. We report a 12-year-old Saudi boy with mucocutaneous candidiasis, hypoparathyroidism, and adrenocortical failure consistent with APECED. In addition, he has dysmorphic facial features, growth retardation, and severe global developmental delay. Patient had late development of chronic renal failure. The blastogenesis revealed depressed lymphocytes' response to Candida albicans at 38% when compared to control. Chromosome analysis of the patient revealed 46,XY,del(4)(q33). FISH using a 4p/4q subtelomere DNA probe assay confirmed the deletion of qter subtelomere on chromosome 4. Parental chromosomes were normal. The deleted array was further defined using array CGH. AIRE full gene sequencing revealed a homozygous mutation namely 845_846insC. Renal biopsy revealed chronic interstitial nephritis with advanced fibrosis. In addition, there was mesangial deposition of C3, C1q, and IgM. This is, to the best of our knowledge, the first paper showing evidence of autoimmune nephropathy by renal immunofluorescence in a patient with APECED and terminal 4q deletion. [ABSTRACT FROM AUTHOR]

Published

2010

166. Mycoketide: A CD1c-Presented Antigen with Important Implications in Mycobacterial Infection.

Author

Matsunaga, Isamu and Sugita, Masahiko

Subjects

ANTIGENS, MYCOBACTERIAL diseases, TUBERCULOSIS, MICROBIAL virulence, BACTERIAL cell walls

Abstract

Mycobacterium tuberculosis and related mycobacteria species are unique in that the acid-fast bacilli possess a highly lipid-rich cell wall that not simply confers resistance to treatment with acid alcohol, but also controls their survival and virulence. It has recently been established that a fraction of the cell wall lipid components of mycobacteria can function as antigens targeted by the acquired immunity of the host. Human group 1 CD1 molecules (CD1a, CD1b, and CD1c) bind a pool of lipid antigens expressed by mycobacteria and present them to specific T cells, thereby mediating an effective pathway for host defense against tuberculosis. The contrasting and mutually complementary functions of CD1a and CD1b molecules in terms of the repertoire of antigens they bind have been well appreciated, but it remains to be established how CD1c may play a unique role. Nevertheless, recent advances in our understanding of the CD1c structure as well as the biosynthetic pathway of a CD1c-presented antigen, mannose-1, β-phosphomycoketide, expressed by pathogenic mycobacteria now unravel a new aspect of the group 1 CD1 biology that has not been appreciated in previous studies of CD1a and CD1b molecules. [ABSTRACT FROM AUTHOR]

Published

2012

167. Inflammation as an Animal Development Phenomenon.

Author

Ramos, Gustavo Campos

Subjects

INFLAMMATION, BACTERIOLOGY, MICROORGANISMS, PHARMACOLOGY

Abstract

Inflammation is a term that has been used throughout history in different contexts; it may represent a simple collection of clinical symptoms for which drugs are developed, a diseasemechanism, or even a defense mechanism againstmicrobes validating Pasteur's studies on bacteriology and Darwin's proposed struggle for survival. Thus, an explanation of this term must also consider the scientific questions addressed. In this study, I propose that several of the inflammatory events typically described in immunological, pathological, and pharmacological contexts can also be perceived asmechanisms of animal development. Thus, by recognizing that the generation of an animal form, its conservation, and its regeneration after tissue damage are phenomena of the same nature, inflammation can be addressed through the approach of developmental biology, thereby acquiring a much neglected physiological counterpart. [ABSTRACT FROM AUTHOR]

Published

2012

168. Seizures in Primary Antiphospholipid Syndrome:The Relevance of Smoking to Stroke.

Author

De Carvalho, Jozélio Freire, Pasoto, Sandra Gofinet, and Appenzeller, Simone

Subjects

ANTIPHOSPHOLIPID syndrome, SPASMS, SMOKING, STROKE, SEIZURES (Medicine)

Abstract

Objectives. To evaluate the frequency of seizures in primary antiphospholipid syndrome (PAPS) and their possible clinical and laboratory associations. Methods. Eighty-eight PAPS patients (Sydney's criteria) were analyzed by a standard interview, physical examination and review of medical charts. Risk factors for seizures, clinical manifestations, associated comorbidities, and antiphospholipid antibodies were evaluated. Results. Nine (10.2%) patients with seizures were identified, 77.8% had convulsions onset after PAPS diagnosis.Mean age, gender, and race were comparable in groups with or without seizures. Interestingly, a higher frequency of current smoking (44.4 versus 10.1%, P = 0.019) was observed in the first group. Stroke, Sneddon's syndrome, and livedo reticularis were more frequent in PAPS patients with seizures than those without seizures, although not statistically significant (P > 0.05). Comparison between patients with seizures onset after PAPS diagnosis (n = 7) and those without convulsions (n = 79) demonstrated a higher frequency of current smoking (42.9 versus 10%, P = 0.042) and stroke in the first group (71.4 versus 30.4%, P = 0.041). Regression analysis confirmed that smoking (P = 0.030) and stroke (P = 0.042) were independently associated to seizures. Conclusion. About 10.2% of PAPS patients had convulsions, predominantly after PAPS diagnosis, and seizures were associated to current smoking and stroke. [ABSTRACT FROM AUTHOR]

Published

2012

169. Genetic Risk Factors of Systemic Lupus Erythematosus in the Malaysian Population: A Minireview.

Author

Hwa Chia Chai, Phipps, Maude Elvira, and Kek Heng Chua

Subjects

SYSTEMIC lupus erythematosus, AUTOANTIBODIES, INTERLEUKINS, T-cell receptor genes, DISEASE risk factors

Abstract

SLE is an autoimmune disease that is not uncommon in Malaysia. In contrast toMalays and Indians, the Chinese seem to be most affected. SLE is characterized by deficiency of body's immune response that leads to production of autoantibodies and failure of immune complex clearance. This minireview attempts to summarize the association of several candidate genes with risk for SLE in the Malaysian population and discuss the genetic heterogeneity that exists locally in Asians and in comparison with SLE in Caucasians. Several groups of researchers have been actively investigating genes that are associated with SLE susceptibility in the Malaysian population by screening possible reported candidate genes across the SLE patients and healthy controls. These candidate genes include MHC genes and genes encoding complement components, TNF, FcγR, T-cell receptors, and interleukins. However, most of the polymorphisms investigated in these genes did not show significant associations with susceptibility to SLE in the Malaysian scenario, except for those occurring in MHC genes and genes coding for TNF-α, IL-1β, IL-1RN, and IL-6. [ABSTRACT FROM AUTHOR]

Published

2012

170. Cardiovascular Risk in Systemic Autoimmune Diseases:Epigenetic Mechanisms of Immune Regulatory Functions.

Author

López-Pedrera, Chary, Pérez-Sánchez, Carlos, Ramos-Casals, Manuel, Santos-Gonzalez, Monica, Rodriguez-Ariza, Antonio, and Cuadrado, Ma José

Subjects

CARDIOVASCULAR diseases risk factors, AUTOIMMUNE diseases, EPIGENESIS, ATHEROSCLEROSIS, INFLAMMATION

Abstract

Autoimmune diseases (AIDs) have been associated with accelerated atherosclerosis (AT) leading to increased cardio- and cerebrovascular disease risk. Traditional risk factors, as well as systemic inflammation mediators, including cytokines, chemokines, proteases, autoantibodies, adhesion receptors, and others, have been implicated in the development of these vascular pathologies. Yet, the characteristics of vasculopathies may significantly differ depending on the underlying disease. In recent years, many new genes and signalling pathways involved in autoimmunity with often overlapping patterns between different disease entities have been further detected. Epigenetics, the control of gene packaging and expression independent of alterations in the DNA sequence, is providing new directions linking genetics and environmental factors. Epigenetic regulatory mechanisms comprise DNA methylation, histone modifications, and microRNA activity, all of which act upon gene and protein expression levels. Recent findings have contributed to our understanding of how epigenetic modifications could influence AID development, not only showing differences between AID patients and healthy controls, but also showing how one disease differs from another and even how the expression of key proteins involved in the development of each disease is regulated. [ABSTRACT FROM AUTHOR]

Published

2012

171. Immune Modulation in Primary Vaccinia virus Zoonotic Human Infections.

Author

Silva Gomes, Juliana Assis, De Araújo, Fernanda Fortes, Trindade, Giliane de Souza, Quinan, Bárbara Resende, Drumond, Betâ nia Paiva, Siqueira Ferreira, Jaqueline Maria, Fernandes Mota, Bruno Eduardo, Nogueira, Maurício Lacerda, Kroon, Erna Geessien, Abrahã o, Jô natas Santos, Côrrea-Oliveira, Rodrigo, and Da Fonseca, Flávio Guimarães

Subjects

ZOONOSES, VACCINIA, IMMUNOREGULATION, ORTHOPOXVIRUSES

Abstract

In 2010, the WHO celebrated the 30th anniversary of the smallpox eradication. Ironically, infections caused by viruses related to smallpox are being increasingly reported worldwide, including Monkeypox, Cowpox, and Vaccinia virus (VACV). Little is known about the human immunological responses elicited during acute infections caused by orthopoxviruses. We have followed VACV zoonotic outbreaks taking place in Brazil and analyzed cellular immune responses in patients acutely infected by VACV. Results indicated that these patients show a biased immune modulation when compared to noninfected controls. Amounts of B cells are low and less activated in infected patients. Although present, T CD4+ cells are also less activated when compared to noninfected individuals, and so are monocytes/macrophages. Similar results were obtained when Balb/C mice were experimentally infected with a VACV sample isolated during the zoonotic outbreaks. Taking together, the data suggest that zoonotic VACVs modulate specific immune cell compartments during an acute infection in humans. [ABSTRACT FROM AUTHOR]

Published

2012

172. Current Concepts of Immunology and Diagnosis in Amniotic Fluid Embolism.

Author

Benson, Michael D.

Subjects

AMNIOTIC fluid embolism, MATERNAL mortality, IMMUNE response, PREGNANCY complications, CELLULAR immunity

Abstract

Amniotic fluid embolism (AFE) is one of the leading causes of maternal mortality and morbidity in developed countries. Current thinking about pathophysiology has shifted away from embolism toward a maternal immune response to the fetus. Two immunologic mechanisms have been studied to date. Anaphylaxis appears to be doubtful while the available evidence supports a role for complement activation. With the mechanism remaining to be elucidated, AFE remains a clinical diagnosis. It is diagnosed based on one or more of four key signs/symptoms: cardiovascular collapse, respiratory distress, coagulopathy, and/or coma/seizures. The only laboratory test that reliably supports the diagnosis is the finding of fetal material in the maternal pulmonary circulation at autopsy. Perhaps the most compelling mystery surrounding AFE is not why one in 20,000 parturients are afflicted, but rather how the vast majority of women can tolerate the foreign antigenic presence of their fetus both within their uterus and circulation? [ABSTRACT FROM AUTHOR]

Published

2012

173. Association of Intrarenal B-Cell Infiltrates with Clinical Outcome in Lupus Nephritis: A Study of 192 Cases.

Author

Yan Shen, Chuan-Yin Sun, Feng-XiaWu, Yi Chen, Min Dai, Yu-Cheng Yan, and Cheng-De Yang

Subjects

B cells, LUPUS nephritis, CREATININE, IMMUNOHISTOCHEMISTRY, BLOOD urea nitrogen

Abstract

Background. Lupus nephritis (LN) remains a major cause of morbidity and end-stage renal disease. Dysfunction of B lymphocytes is thought to be important in the pathogenesis of SLE/LN. Intrarenal B cells have been found in several forms of inflammatory kidney diseases although their role in LN renal is not well defined. Methods. Intrarenal B cells were analyzed in 192 renal biopsies from patients diagnosed with lupus nephritis. Immunohistochemical staining of serial sections was performed for each LN patient using CD20, CD3, and CD21 antibodies. Results. Intrarenal B cells were more likely to be associated with class IV LN and were mainly distributed in the renal interstitium, with very few in the glomerulus. The systemic lupus erythematosus disease activity index (SLEDAI), blood urea nitrogen, and serum creatinine levels were all significantly greater in the LN-B cell groups (all P < 0.05). LN renal activity and chronicity indices correlated with B-cells infiltrates (all P < 0.0001). Renal biopsies were classified into four distinct categories according to the organizational grade of inflammatory cell infiltrates. Germinal center- (GC-) like structures were not identified in any LN biopsies. Conclusion. It is hypothesized that intrarenal B cells enhance immunological responses and exaggerate the local immune response to persisting autoimmune damage in the tubulointerstitium. [ABSTRACT FROM AUTHOR]

Published

2012

174. Immune-Regulatory Mechanisms in Systemic Autoimmune and Rheumatic Diseases.

Author

Konttinen, Yrjö T. and Takakubo, Yuya

Subjects

AUTOIMMUNE diseases, RHEUMATISM, IMMUNOREGULATION, IMMUNOLOGICAL tolerance, DENDRITIC cells, T cells, B cells

Abstract

Systemic autoimmune and rheumatic diseases (SAIRDs) are thought to develop due to the failure of autoimmune regulation and tolerance. Current therapies, such as biologics, have improved the clinical results of SAIRDs; however, they are not curative treatments. Recently, new discoveries have been made in immune tolerance and inflammation, such as tolerogenic dendritic cells, regulatory T and B cells, Th 17 cells, inflammatory and tolerogenic cytokines, and intracellular signaling pathways. They lay the foundation for the next generation of the therapies beyond the currently used biologic therapies. New drugs should target the core processes involved in disease mechanisms with the aim to attain complete cure combined with safety and low costs compared to the biologic agents. Re-establishment of autoimmune regulation and tolerance in SAIRDs by the end of the current decade should be the final and realistic target. [ABSTRACT FROM AUTHOR]

Published

2012

175. Vaccination with Enzymatically Cleaved GPI-Anchored Proteins from Schistosoma mansoni Induces Protection against Challenge Infection.

Author

Martins, Vicente P., Pinheiro, Carina S., Figueiredo, Barbara C. P., Assis, Natan R. G., Morais, Suellen B., Caliari, Marcelo V., Azevedo, Vasco, Castro-Borges, William, Wilson, R. Alan, and Oliveira, Sergio C.

Subjects

SCHISTOSOMA mansoni, DRUG therapy, ANTIGENS, IMMUNIZATION, DIURETICS

Abstract

The flatworm Schistosoma mansoni is a blood fluke parasite that causes schistosomiasis, a debilitating disease that occurs throughout the developing world. Current schistosomiasis control strategies are mainly based on chemotherapy, but many researchers believe that the best long-termstrategy to control schistosomiasis is through immunization with an antischistosomiasis vaccine combined with drug treatment. In the search for potential vaccine candidates, numerous tegument antigens have been assessed. As the major interface between parasite and mammalian host, the tegument plays crucial roles in the establishment and further course of schistosomiasis. Herein, we evaluated the potential of a GPI fraction, containing representative molecules located on the outer surface of adult worms, as vaccine candidate. Immunization of mice with GPI-anchored proteins induced a mixed Th1/Th2 type of immune response with production of IFN-γ and TNF-α, and low levels of IL-5 into the supernatant of splenocyte cultures. The protection engendered by this vaccination protocol was confirmed by 42% reduction in worm burden, 45% reduction in eggs per gram of hepatic tissue, 29% reduction in the number of granulomas per area, and 53% reduction in the granuloma fibrosis. Taken together, the data herein support the potential of surface-exposed GPI-anchored antigens from the S. mansoni tegument as vaccine candidate. [ABSTRACT FROM AUTHOR]

Published

2012

176. Macrophages in Tumor Microenvironments and the Progression of Tumors.

Author

Ning-Bo Hao, Mu-Han Lü, Ya-Han Fan, Ya-Ling Cao, Zhi-Ren Zhang, and Shi-Ming Yang

Subjects

MACROPHAGES, CANCER invasiveness, IMMUNE response, CELLULAR immunity, IMMUNOSUPPRESSION

Abstract

Macrophages are widely distributed innate immune cells that play indispensable roles in the innate and adaptive immune response to pathogens and in-tissue homeostasis.Macrophages can be activated by a variety of stimuli and polarized to functionally different phenotypes. Two distinct subsets of macrophages have been proposed, including classically activated (M1) and alternatively activated (M2)macrophages.M1macrophages express a series of proinflammatory cytokines, chemokines, and effectormolecules, such as IL-12, IL-23, TNF-α, iNOS and MHCI/II. In contrast, M2 macrophages express a wide array of anti-inflammatory molecules, such as IL-10, TGF-β, and arginase1. In most tumors, the infiltrated macrophages are considered to be of the M2 phenotype, which provides an immunosuppressive microenvironment for tumor growth. Furthermore, tumor-associated macrophages secrete many cytokines, chemokines, and proteases, which promote tumor angiogenesis, growth, metastasis, and immunosuppression. Recently, it was also found that tumor-associated macrophages interact with cancer stem cells. This interaction leads to tumorigenesis, metastasis, and drug resistance. So mediating macrophage to resist tumors is considered to be potential therapy. [ABSTRACT FROM AUTHOR]

Published

2012

177. Tolerogenic versus Inflammatory Activity of Peripheral Blood Monocytes and Dendritic Cells Subpopulations in Systemic Lupus Erythematosus.

Author

Carvalheiro, Tiago, Rodrigues, Ana, Lopes, Ana, Inês, Luís, Velada, Isabel, Ribeiro, Andreia, Martinho, António, Silva, José A. P., Pais, Maria L., and Paiva, Artur

Subjects

SYSTEMIC lupus erythematosus, DENDRITIC cells, GENE expression, MONOCYTES, CHEMOKINES

Abstract

Abnormalities in monocytes and in peripheral blood dendritic cells (DC) subsets have been reported in systemic lupus erythematosus (SLE).We aim to clarify the tolerogenic or inflammatory role of these cells based on ICOSL or IFN-α and chemokine mRNA expression, respectively, after cell purification. The study included 18 SLE patients with active disease (ASLE), 25 with inactive disease (ISLE), and 30 healthy controls (HG). In purified plasmacytoid DC (pDC) was observed a lower ICOSL mRNA expression in ASLE and an increase in ISLE; similarly, a lower ICOSL mRNA expression in monocytes of ALSE patients was found. However, a higher ICOSL mRNA expression was observed in ASLE compared to HG in myeloid DCs. Interestingly, clinical parameters seem to be related with ICOSL mRNA expression. Regarding the inflammatory activity it was observed in purified monocytes and CD14-/low CD16+ DCs an increase of CCL2, CXCL9, and CXCL10 mRNA expression in ASLE compared to HG. In myeloid DC no differences were observed regarding chemokines, and IFN-α mRNA expression. In pDC, a higher IFN-α mRNA expression was observed in ASLE. Deviations in ICOSL, chemokine, and IFN-α mRNA expression in peripheral blood monocytes and dendritic cells subpopulations in SLE appear to be related to disease activity. [ABSTRACT FROM AUTHOR]

Published

2012

178. Inaccuracy of Death Certificate Diagnosis of Tuberculosis and Potential Underdiagnosis of TB in a Region of High HIV Prevalence.

Author

Liu, Theresa T., Wilson, Douglas, Dawood, Halima, Cameron, D.William, and Alvarez, Gonzalo G.

Subjects

TUBERCULOSIS mortality, DEATH certificates, HIV infection complications, PROOF & certification of death, HIGHLY active antiretroviral therapy

Abstract

Despite the South African antiretroviral therapy rollout, which should reduce the incidence of HIV-associated tuberculosis (TB), the number of TB-attributable deaths in KwaZuluNatal (KZN) remains high. TB is often diagnosed clinically, without microbiologic confirmation, leading to inaccurate estimates of TB-attributed deaths. This may contribute to avoidable deaths, and impact population-based TB mortality estimates. Objectives. (1) To measure the number of cases with microbiologically confirmed TB in a retrospective cohort of deceased inpatients with TB-attributed hospital deaths. (2) To estimate the rates of multi-drug resistant (MDR) and extensively drug resistant (XDR) TB in this cohort. Results. Of 2752 deaths at EDH between September 2006 andMarch 2007, 403 (15%) were attributed to TB on the death certificate. 176 of the TB-attributed deaths (44%) had a specimen sent for smear or culture; only 64 (36%) had a TB diagnosis confirmed by either test. Of the 39 culture-confirmed cases, 27/39 (69%) had fully susceptible TB and 27/39 (69%) had smear-negative culture-positive TB (SNTB). Two patients had drug monoresistance, three patients had MDR-TB, and one had XDR-TB. Conclusions. Most TB-attributed deaths in this cohort were not microbiologically confirmed. Of confirmed cases, most were smear-negative, culture positive and were susceptible to all first line drugs. [ABSTRACT FROM AUTHOR]

Published

2012

179. Rituximab-Based Treatment, HCV Replication, and Hepatic Flares.

Author

Sagnelli, Evangelista, Pisaturo, Mariantonietta, Sagnelli, Caterina, and Coppola, Nicola

Subjects

RITUXIMAB, HEPATITIS C virus, CD20 antigen, HEPATITIS C treatment, VIRAL replication

Abstract

Rituximab, a chimeric mouse-human monoclonal antibody directed to the CD20 antigen expressed on pre-B lymphocytes and mature lymphocytes, causes a profound B-cell depletion. Due to its peculiar characteristics, this drug has been used to treat oncohaematological diseases, B cell-related autoimmune diseases, rheumatoid arthritis, and, more recently,HCV-associated mixed cryoglobulinaemic vasculitis. Rituximab-based treatment, however, may induce an increased replication of several viruses such as hepatitis B virus, cytomegalovirus, varicella-zoster virus, echovirus, and parvovirus B19. Recent data suggest that rituximab-based chemotherapy induces an increase in HCV expression in hepatic cells, which may become a target for a cell-mediated immune reaction after the withdrawal of treatment and the restoration of the immune control. Only a few small studies have investigated the occurrence of HCV reactivation and an associated hepatic flare in patients with oncohaematological diseases receiving RCHOP (rituximab, cyclophosphamide, doxorubicin, vincristine, and prednisone). These studies suggest that the hepatic flares are frequently asymptomatic, but life-threatening liver failure occurs in nearly 10% of cases. [ABSTRACT FROM AUTHOR]

Published

2012

180. Transfer of Maternal Immunity to Newborns of Diabetic Mothers.

Author

França, Eduardo Luzía, Paranhos Calderon, Iracema de Mattos, Vieira, Elisa Lima, Morceli, Glilciane, and Honorio-França, Adenilda Cristina

Subjects

MATERNALLY acquired immunity, GESTATIONAL diabetes, HYPERGLYCEMIA, PEOPLE with diabetes, IMMUNOGLOBULIN G, CORD blood, COLOSTRUM

Abstract

This study was carried out with hyperglycemic pregnant women to investigate the transfer of antibody classes to newborns across the placenta or by colostrum and the functional activity of phagocytes in maternal blood, cord blood, and colostrum from diabetes mothers. Samples from maternal blood, cord blood, and colostrum were collected from 20 normoglycemic and 20 hyperglycemic pregnant women. We determined antibodies levels, superoxide release, phagocytosis and bactericidal activity of phagocytes. We demonstrated that IgG levels in cord blood were higher in the hyperglycemic group. IgA and IgM levels were higher in maternal than in cord blood samples. Plasma antibody levels were lower in hyper- than in normoglycemic women. The colostrum of diabetic mothers had lower IgA and IgG levels. Colostrum andmaternal blood phagocytes when exposed to EPEC increased the superoxide release. Cord blood phagocytes of hyperglycemic group, independently of bacteria, had higher superoxide release. Colostrum and blood phagocytes from diabetic group exhibited some phagocytic and microbicidal activity in response to EPEC. Mononuclear phagocytes from cord blood had the lowest phagocytosis, and bactericidal activity for EPEC, regardless of glycemic status. These data showed that hyperglycemia altered IgG transfer across the placenta and decreases immunoglobulin levels in maternal blood and colostrum. [ABSTRACT FROM AUTHOR]

Published

2012

181. Impact of Previous ART and of ART Initiation on Outcome of HIV-Associated Tuberculosis.

Author

Girardi, Enrico, Palmieri, Fabrizio, Angeletti, Claudio, Vanacore, Paola, Matteelli, Alberto, Gori, Andrea, Carbonara, Sergio, and Ippolito, Giuseppe

Subjects

TUBERCULOSIS treatment, HIV infection complications, HIGHLY active antiretroviral therapy, HIV-positive persons, TREATMENT effectiveness, THERAPEUTICS

Abstract

Background. Combination antiretroviral therapy (cART) has progressively decreased mortality of HIV-associated tuberculosis .To date, however, limited data on tuberculosis treatment outcomes among coinfected patients who are not ART-naive at the time of tuberculosis diagnosis are available. Methods. A multicenter, observational study enrolled 246 HIV-infected patients diagnosed with tuberculosis, in 96 Italian infectious diseases hospital units, who started tuberculosis treatment. A polytomous logistic regression model was used to identify baseline factors associated with the outcome. A Poisson regression model was used to explain the effect of ART during tuberculosis treatment on mortality, as a time-varying covariate, adjusting for baseline characteristics. Results. Outcomes of tuberculosis treatment were as follows: 130 (52.8%) were successfully treated, 36 (14.6%) patients died in a median time of 2 months (range: 0-16), and 80 (32.6%) had an unsuccessful outcome. Being foreign born or injecting drug users was associated with unsuccessful outcomes. In multivariable Poisson regression, cART during tuberculosis treatment decreased the risk of death, while this risk increased for those who were not ART-naive at tuberculosis diagnosis. Conclusions. ART during tuberculosis treatment is associated with a substantial reduction of death rate among HIV-infected patients. However, patients who are not ART-naive when they develop tuberculosis remain at elevated risk of death. [ABSTRACT FROM AUTHOR]

Published

2012

182. Gestational Medication Use, Birth Conditions, and Early Postnatal Exposures for Childhood Asthma.

Author

Yang-Ching Chen, Ching-Hui Tsai, and Yungling Lee

Subjects

ASTHMA in children, PREGNANCY, DELIVERY (Obstetrics), BREASTFEEDING

Abstract

Our aim is to explore (1) whether gestational medication use, mode of delivery, and early postnatal exposure correlate with childhood asthma, (2) the dose responsiveness of such exposure, and (3) their links to early- and late-onset asthma.We conducted a matched case-control study based on the Taiwan Children Health Study, which was a nationwide survey that recruited 12-to-14- year-old school children in 14 communities. 579 mothers of the participants were interviewed by telephone. Exclusive breastfeeding protected children from asthma. Notably, childhood asthma was significantly associated with maternal medication use during pregnancy, vacuum use during vaginal delivery, recurrent respiratory tract infections, hospitalization, main caregiver cared for other children, and early daycare attendance. Exposure to these factors led to dose responsiveness in relationships to asthma.Most of the exposures revealed a greater impact on early-onset asthma, except for vacuum use and daycare attendance. [ABSTRACT FROM AUTHOR]

Published

2012

183. Association between Functional Polymorphisms of Foxp3 Gene and the Occurrence of Unexplained Recurrent Spontaneous Abortion in a Chinese Han Population.

Author

Zaigui Wu, Zeshan You, Cai Zhang, Zhuyu Li, Xiumei Su, Xiuming Zhang, and Yinguang Li

Subjects

FORKHEAD transcription factors, ABORTION, GENETIC polymorphisms, T cells

Abstract

Unexplained recurrent spontaneous abortion (URSA) is an alloimmune disease associated with the failure of fetal-maternal immunologic tolerance in which the regulatory T lymphocytes (Treg) play a pivotal role. It is well known that Forkhead box P3 (Foxp3) is a crucial regulatory factor for the development and function of Treg cells. It has also been established that deficiency of the Foxp3 gene suppresses the regulatory function of Treg cells. To determine if functional polymorphisms at the Foxp3 loci are associated with URSA in humans, we genotyped four common polymorphisms of Foxp3 gene in 146 unrelated URSA patients and 112 healthy women. The results showed that rs3761548A/C and rs2232365A/G polymorphisms were significantly associated with URSA. Additionally, we found that the allelic distribution of rs5902434 del/ATT in URSA group was slightly different from that in the control group. We conclude that functional polymorphisms of the Foxp3 gene may confer an important susceptibility to URSA in the Chinese Han population, probably by altering Foxp3 function and/or its expression. [ABSTRACT FROM AUTHOR]

Published

2012

184. Inhibition of Arterial Allograft Intimal Hyperplasia Using Recipient Dendritic Cells Pretreated with B7 Antisense Peptide.

Author

Yu-Feng Yao, Yi-Ming Zhou, Jian-Bin Xiang, Xiao-Dong Gu, and Duan Cai

Subjects

HOMOGRAFTS, HYPERPLASIA, DENDRITIC cells, ANTISENSE peptides, LABORATORY mice, BONE marrow cells

Abstract

Background. Low expression or absence of dendritic cell (DC) surface B7molecules can induce immune tolerance or hyporesponse. Whether DCs could induce indirect allogeneic-specific cross-tolerance or hyporesponse to recipient T cells remains unclear. Methods. Generated from C3H/He mice bone marrow cells pulsed with donor antigen from C57BL/6 mice, recipient DCs were incubated with B7 antisense peptide (B7AP). Immune regulatory activities were examined in vitro by a series of mixed lymphocyte reactions. Murine allogeneic carotid artery orthotopic transplantation was performed from C57BL/6 to C3H/He. Recipients were given B7AP-treated DCs 7 days before transplantation. Allograft pathological analysis was done 2 months after transplantation. Results. B7AP-pretreated DCs markedly inhibited T-cell proliferation compared with untreated group. Pretreated T cells exhibited markedly reduced response to alloantigen versus third-party antigen. Pathological analysis of arterial allografts demonstrated significant reduction of intimal hyperplasia in B7-AP pretreated group versus control. Conclusion. Blockade of B7 molecules by B7AP could induce indirect allogeneic-specific hyporesponse and inhibit arterial allograft intimal hyperplasia, which may be involved in future strategies for human allograft chronic rejection. [ABSTRACT FROM AUTHOR]

Published

2012

185. Emergence of Exhausted B Cells in Asymptomatic HIV-1-Infected Patients Naïve for HAART is Related to Reduced Immune Surveillance.

Author

Fogli, Manuela, Torti, Carlo, Malacarne, Fabio, Fiorentini, Simona, Albani, Melania, Izzo, Ilaria, Giagulli, Cinzia, Maggi, Fabrizio, Carosi, Giampiero, and Caruso, Arnaldo

Subjects

HIV-positive persons, HIGHLY active antiretroviral therapy, B cells, CD4 antigen, T cells

Abstract

Alterations of B cell subpopulations have been described up to date as characterizing advanced stage of HIV-1 infection. However, whether such defects are relevant in subjects with a preserved number of CD4+ T cells (>350 cells/μL) is unclear. In a crosssectional study, we investigated if signs of B cells exhaustion and impaired viral immune surveillance are present in a cohort of 43 asymptomatic HIV-1-infected patients with preserved CD4+ T cell counts (>350 cells/μL) and highly active antiretroviral therapy (HAART) untreated. A dramatic expansion of exhausted tissue-like memory B cells (CD10-CD21lowCD27-) was observed. B cells alteration was related to an increase in Torque teno virus (TTV) load, used as surrogate marker of immune function. Successfully HAART-treated patients showed normalization of B cell subpopulations frequency and TTV load. These results provide new insights on B cell in HIV-1 infection and show that development of B cell abnormalities precedes CD4+ T cell decline. [ABSTRACT FROM AUTHOR]

Published

2012

186. Characterization of Chronic Cutaneous Lesions from TNF-Receptor-1-Deficient Mice Infected by Leishmania major.

Author

Oliveira, Carolina Ferreira, Manzoni-de-Almeida, Daniel, Seixas Mello, Paula, Cotta Natale, Caio, Costa Santiago, Helton da, Da SilvaMiranda, Luíza, Oliveira Ferraz, Fernanda, Martins dos Santos, Liliane, Martins Teixeira, Mauro, Esteves Arantes, Rosa Maria, and Quercia Vieira, Leda

Subjects

TUMOR necrosis factors, LABORATORY mice, LEISHMANIA, PARASITISM, CD8 antigen, INTERLEUKINS

Abstract

Leishmania major-infected TNF receptor 1 deficient (TNFR1 KO) mice resolve parasitism but fail to resolve lesions, while wildtype mice completely heal. We investigated the cell composition, cytokine production, and apoptosis in lesions from L. majorinfected TNFR1 KO and wild-type (WT) mice. Chronic lesions from L. major-infected TNFR1 KO mice presented larger number of CD8+ T and Ly6G+ cells. In addition, higher concentrations of mRNA for IFN-γ CCL2 and CCL5, as well as protein, but lower numbers of apoptotic cells, were found in lesions from TNFR1 KO mice than in WT, at late time points of infection. Our studies showed that persistent lesions in L. major-infected TNFR1 KO mice may be mediated by continuous migration of cells to the site of inflammation due to the presence of chemokines and also by lower levels of apoptosis. We suggest that this model has some striking similarities to the mucocutaneous clinical form of leishmaniasis. [ABSTRACT FROM AUTHOR]

Published

2012

187. Development of Murine Hepatic NK Cells during Ontogeny: Comparison with Spleen NK Cells.

Author

XianWu, Yongyan Chen, HaimingWei, Rui Sun, and Zhigang Tian

Subjects

KILLER cells, ONTOGENY, SPLEEN, HEMATOPOIETIC system, LYMPHOID tissue, LABORATORY mice, PERFORINS

Abstract

The phenotype of developing liver NK cells (CD3-NK1.1+) was investigated during mouse ontogeny comparing with spleen NK cells. The highest percentage of hepatic CD27-CD11b- NK cells occurred at the fetal stage. After birth, the percentage of CD27- CD11b-NK cells in both the liver and spleen gradually decreased to their lowest level at 6 weeks.More CD27+CD11b-NK cells were detected in the liver than that in spleen from week 1 to 6. Expression of NKG2A on liver NK cells was decreased but still much higher than that of spleenNK cells after 1 week. The NKG2D expression on liverNK cells increased to its highest level and was significantly higher than on spleenNK cells till 4 weeks.During mouse ontogeny, weaker expression of NKp46 and CD2 and stronger expression of CD69, CD11c, 2B4, and CD73 were observed on liver NK cells. Furthermore, neonatal liver NK cells express higher IFN-γ and perforin than adult .These results suggest that thematuration process of NK cells is unique in the livers, and liver microenvironments might play critical roles to keep NK cells in an immature status. [ABSTRACT FROM AUTHOR]

Published

2012

188. Pulmonary Arterial Hypertension in Systemic Lupus Erythematosus: Current Status and Future Direction.

Author

Dhala, Atiya

Subjects

SYSTEMIC lupus erythematosus, CONNECTIVE tissue cells, SYSTEMIC scleroderma, HYPERTENSION, THROMBOSIS, PULMONARY fibrosis

Abstract

Pulmonary arterial hypertension (PAH) is commonly associated with connective tissue diseases (CTDs) including systemic sclerosis and systemic lupus erythematosus (SLE). The prevalence of PAH in SLE is estimated to be 0.5% to 17.5%. The pathophysiology of PAH involves multiple mechanisms from vasculitis and in-situ thrombosis to interstitial pulmonary fibrosis which increases pulmonary vascular resistance, potentially leading to right heart failure. Immune and inflammatory mechanisms may play a significant role in the pathogenesis or progression of PAH in patients with CTDs, establishing a role for anti-inflammatory and immunosuppressive therapies. The leading predictors of PAH in SLE are Raynaud phenomenon, anti-U1RNP antibody, and anticardiolipin antibody positivity. The first-line of diagnostic testing for patients with suspected SLE-associated PAH (SLE-aPAH) involves obtaining a Doppler echocardiogram. Once the diagnosis is confirmed by right heart catheterization, SLE-aPAH patients are generally treated with oxygen, anticoagulants, and vasodilators. Although the prognosis and therapeutic responsiveness of these patients have improved with the addition of intensive immunosuppressive therapies, these treatments are still largely unproven. Recent data put the one-year survival rate for SLE-aPAH patients at 94%. Pregnant women are most at risk of dying due to undiagnosed SLE-aPAH, and screening should be considered essential in this population. [ABSTRACT FROM AUTHOR]

Published

2012

189. A Systematic Review of the Epidemiology, Immunopathogenesis, Diagnosis, and Treatment of Pleural TB in HIV- Infected Patients.

Author

Aljohaney, A., Amjadi, K., and Alvarez, G. G.

Subjects

HIV-positive persons, TUBERCULOSIS patients, MEDLINE, CYTOKINES, IMMUNOPATHOLOGY

Abstract

Background. High HIV burden countries have experienced a high burden of pleural TB in HIV-infected patients. Objective. To review the epidemiology, immunopathogenesis, diagnosis, and treatment of pleural TB in HIV-infected patients. Methods. A literature search from 1950 to June 2011 in MEDLINE was conducted. Results. Two-hundred and ninety-nine studies were identified, of which 30 met the inclusion criteria. The immunopathogenesis as denoted by cells and cytokine profiles is distinctly different between HIV and HIV-uninfected pleural TB disease. Adenosine deaminase and interferon gamma are good markers of pleural TB disease even in HIV-infected patients. HIV-uninfected TB suspects with pleural effusions commonly have a low yield of TB organisms however the evidence suggests that in dually infected patients smear and cultures have a higher yield. The Gene Xpert MTB/RIF assay has significant potential to improve the diagnosis of pleural TB in HIV-positive patients. Conclusions. Pleural TB in HIV-infected patients has a different immunopathogenesis than HIV-uninfected pleural TB and these findings in part support the differences noted in this systematic review. Research should focus on developing an interferon gamma-based point of care diagnostic test and expansion of the role of Gene Xpert in the diagnosis of pleural TB. [ABSTRACT FROM AUTHOR]

Published

2012

190. Immunological Evaluation and Comparison of Different EV71 Vaccine Candidates.

Author

Ai-Hsiang Chou, Chia-Chyi Liu, Jui-Yuan Chang, Shu-Pei Lien, Meng-Shin Guo, Hau-Pong Tasi, Kuang-Nan Hsiao, Shih-Jen Liu, Charles Sia, Suh-Chin Wu, Min-Shi Lee, Chia-Hsin Hsiao, Jen-Ren Wang, Yen-Hung Chow, and Pele Chong

Subjects

ENTEROVIRUSES, TESCHEN disease virus, COXSACKIEVIRUSES, HAND, foot & mouth disease, IMMUNOGLOBULINS

Abstract

Enterovirus 71 (EV71) and coxsackievirus A16 (CVA16) are major causative agents of hand, foot, and mouth diseases (HFMDs), and EV71 is now recognized as an emerging neurotropic virus in Asia. Effective medications and/or prophylactic vaccines against HFMD are not available. The current results from mouse immunogenicity studies using in-house standardized RD cell virus neutralization assays indicate that (1) VP1 peptide (residues 211-225) formulated with Freund's adjuvant (CFA/IFA) elicited low virus neutralizing antibody response (1/32 titer); (2) recombinant virus-like particles produced from baculovirus formulated with CFA/IFA could elicit good virus neutralization titer (1/160); (3) individual recombinant EV71 antigens (VP1, VP2, and VP3) formulated with CFA/IFA, only VP1 elicited antibody response with 1/128 virus neutralization titer; and (4) the formalininactivated EV71 formulated in alum elicited antibodies that cross-neutralized different EV71 genotypes (1/640), but failed to neutralize CVA16. In contrast, rabbits antisera could cross-neutralize strongly against different genotypes of EV71 but weakly against CVA16, with average titers 1/6400 and 1/32, respectively. The VP1 amino acid sequence dissimilarity between CVA16 and EV71 could partially explain why mouse antibodies failed to cross-neutralize CVA16. Therefore, the best formulation for producing cost-effective HFMD vaccine is a combination of formalin-inactivated EV71 and CAV16 virions. [ABSTRACT FROM AUTHOR]

Published

2012

191. Impact of Temozolomide on Immune Response during Malignant Glioma Chemotherapy.

Author

Sengupta, Sadhak, Marrinan, Jaclyn, Frishman, Caroline, and Sampath, Prakash

Subjects

GLIOBLASTOMA multiforme, BRAIN tumors, IMMUNE response, DRUG therapy, TUMOR surgery, KILLER cells

Abstract

Malignant glioma, or glioblastoma, is the most common and lethal formof brain tumor with amedian survival time of 15months. The established therapeutic regimen includes a tripartite therapy of surgical resection followed by radiation and temozolomide (TMZ) chemotherapy, concurrently with radiation and then as an adjuvant. TMZ, a DNA alkylating agent, is the most successful antiglioma drug and has added several months to the life expectancy of malignant glioma patients. However, TMZ is also responsible for inducing lymphopenia and myelosuppression in malignant glioma patients undergoing chemotherapy. Although TMZ-induced lymphopenia has been attributed to facilitate antitumor vaccination studies by inducing passive immune response, in general lymphopenic conditions have been associated with poor immune surveillance leading to opportunistic infections in glioma patients, as well as disrupting active antiglioma immune response by depleting both T and NK cells. Deletion of O6- methylguanine-DNA-methyltransferase (MGMT) activity, a DNA repair enzyme, by temozolomide has been determined to be the cause of lymphopenia. Drug-resistant mutation of the MGMT protein has been shown to render chemoprotection against TMZ. The immune modulating role of TMZ during glioma chemotherapy and possible mechanisms to establish a strong TMZ-resistant immune response have been discussed. [ABSTRACT FROM AUTHOR]

Published

2012

192. Evaluation of Clinical and Ultrasonographic Parameters in Psoriatic Arthritis Patients Treated with Adalimumab: A Retrospective Study.

Author

Teoli, M., Zangrilli, A., Chimenti, M. S., Talamonti, M., Bavetta, M., Graceffa, D., Perricone, R., and Chimenti, S.

Subjects

PSORIATIC arthritis, ULTRASONIC imaging, ADALIMUMAB, C-reactive protein, BLOOD sedimentation, SYNOVIAL fluid, PATIENTS

Abstract

Objectives. The aim of this study was to evaluate clinical and US-PD parameters in PsA during adalimumab treatment. Methods. A retrospective study has been conducted in forty patients affected by moderate-to-severe peripheral PsA. Clinical, laboratory, and US-PD evaluations were performed at baseline, after 4, 12, and 24 weeks of treatment. They included erythrocyte sedimentation rate (ESR), C-reactive protein (CRP), visual analogue scale (VAS), Health Assessment Questionnaire (HAQ) modified for Spondyloarthritis, Psoriasis Area Severity Index (PASI) score, the 28-joint Disease Activity Score (DAS 28), and US-PD assessment. US-PD findings were scored according to a semiquantitative scale (ranging 0-3) for synovial proliferation (SP), joint effusion (SE), bone erosions (BE), and PD. Results. Data obtained for clinical, laboratory findings and US-PD evaluation showed statistical significant improvement in all the measures performed except for BE. A significant parallel decrease in SE, SP, and PD values were demonstrated. Conclusion. This study demonstrated that US-PD is a valid technique in monitoring the response to adalimumab in moderate-to-severe PsA [ABSTRACT FROM AUTHOR]

Published

2012

193. Adaptive Immunity in Ankylosing Spondylitis: Phenotype and Functional Alterations of T-Cells before and during Infliximab Therapy.

Author

Szalay, Balázs, Mészáros, Gergő, Cseh, Áron, Ács, Lilla, Deák, Magdolna, Kovács, László, Vásárhelyi, Barna, and Balog, Attila

Subjects

ANKYLOSING spondylitis, RHEUMATISM, FLOW cytometry, T cells, INFLIXIMAB, PHENOTYPES, PATIENTS

Abstract

Our aim was to assess the phenotype of T-cell subsets in patients with ankylosing spondylitis (AS), a chronic inflammatory rheumatic disease. In addition, we also tested short-term T-cell activation characteristics. Measurements were done in 13 AS patients before and during the intravenous therapy with anti-TNF agent infliximab (IFX). Flow cytometry was used to determine T-cell subsets in peripheral blood and their intracellular signaling during activation. The prevalence of Th2 and Th17 cells responsible for the regulation of adaptive immunity was higher in AS than in 9 healthy controls. Although IFX therapy improved patients' condition, immune phenotype did not normalize. Cytoplasmic andmitochondrial calcium responses of CD4+ and CD8+ cells to a specific activation were delayed, while NO generation was increased in AS. NO generation normalized sooner upon IFX than calcium response. These results suggest an abnormal immune phenotype with functional disturbances of CD4+ and CD8+ cells in AS. [ABSTRACT FROM AUTHOR]

Published

2012

194. Shining a Light on Intestinal Traffic.

Author

Murphy, Carola T., Nally, Kenneth, Shanahan, Fergus, and Melgar, Silvia

Subjects

INFLAMMATORY bowel diseases, CROHN'S disease, ULCERATIVE colitis, LEUCOCYTES, CHEMOKINES, INTEGRINS

Abstract

Inflammatory bowel disease (IBD), encompassing Crohn's disease and ulcerative colitis, is associated with enhanced leukocyte infiltration to the gut, which is directly linked to the clinical aspects of these disorders. Thus, leukocyte trafficking is a major target for IBD therapy. Past and emerging techniques to study leukocyte trafficking both in vitro and in vivo have expanded our knowledge of the leukocyte migration process and the role of inhibitors. Various strategies have been employed to target chemokine- and integrin-ligand interactions within the multistep adhesion cascade and the S1P/S1PR1 axis in leukocyte migration. Though there is an abundance of preclinical data demonstrating efficacy of leukocyte trafficking inhibitors, many have yet to be confirmed in clinical studies. Vigilance for toxicity and further research is required into this complex and emerging area of IBD therapy. [ABSTRACT FROM AUTHOR]

Published

2012

195. The Role of Airway Epithelial Cells in Response to Mycobacteria Infection.

Author

Yong Li, Yujiong Wang, and Xiaoming Liu

Subjects

EPITHELIAL cells, MYCOBACTERIA, TUBERCULOSIS, PATHOGENIC microorganisms, IMMUNE response, IMMUNOCYTOCHEMISTRY

Abstract

Airway epithelial cells (AECs) are part of the frontline defense against infection of pathogens by providing both a physical barrier and immunological function. The role of AECs in the innate and adaptive immune responses, through the production of antimicrobial molecules and proinflammatory factors against a variety of pathogens, has been well established. Tuberculosis (TB), a contagious disease primarily affecting the lungs, is caused by the infection of various strains of mycobacteria. In response to mycobacteria infection, epithelial expression of Toll-like receptors and surfactant proteins plays the most prominent roles in the recognition and binding of the pathogen, as well as the initiation of the immune response.Moreover, the antimicrobial substances, proinflammatory factors secreted by AECs, composed a major part of the innate immune response and mediation of adaptive immunity against the pathogen. Thus, a better understanding of the role and mechanism of AECs in response to mycobacteria will provide insight into the relationship of epithelial cells and lung immunocytes against TB, which may facilitate our understanding of the pathogenesis and immunological mechanism of pulmonary tuberculosis disease. [ABSTRACT FROM AUTHOR]

Published

2012

196. Host-Parasite Relationship in Cystic Echinococcosis: An Evolving Story.

Author

Siracusano, Alessandra, Delunardo, Federica, Teggi, Antonella, and Ortona, Elena

Subjects

ECHINOCOCCUS granulosus, ECHINOCOCCOSIS, PUBLIC health, IMMUNE system, IMMUNE response

Abstract

The larval stage of Echinococcus granulosus causes cystic echinococcosis, a neglected infectious disease that constitutes a major public health problem in developing countries. Despite being under constant barrage by the immune system, E. granulosus modulates antiparasite immune responses and persists in the human hosts with detectable humoral and cellular responses against the parasite. In vitro and in vivo immunological approaches, together withmolecular biology and immunoproteomic technologies, provided us exciting insights into the mechanisms involved in the initiation of E. granulosus infection and the consequent induction and regulation of the immune response. Although the last decade has clarifiedmany aspects of host-parasite relationship in human cystic echinococcosis, establishing the full mechanisms that cause the disease requires more studies. Here, we review some of the recent developments and discuss new avenues in this evolving story of E. granulosus infection in man. [ABSTRACT FROM AUTHOR]

Published

2012

197. Mechanisms and Mediators of Inflammation: Potential Models for Skin Rejection and Targeted Therapy in Vascularized Composite Allotransplantation.

Author

Hautz, Theresa, Wolfram, Dolores, Grahammer, Johanna, Starzl, Ravi, Krapf, Christoph, Pratschke, Johann, Andrew Lee, W. P., Brandacher, Gerald, and Schneeberger, Stefan

Subjects

TRANSPLANTATION of organs, tissues, etc., SKIN diseases, IMMUNOSUPPRESSION, QUALITY of life, ORGAN donor registries, CYTOKINES, THERAPEUTICS

Abstract

Vascularized composite allotransplantation (VCA) is an effective treatment option for patients suffering from limb loss or severe disfigurement. However, postoperative courses of VCA recipients have been complicated by skin rejection, and long-term immunosuppression remains a necessity for allograft survival. To widen the scope of this quality-of-life improving procedure minimization of immunosuppression in order to limit risks and side effects is needed. In some aspects, the molecular mechanisms and dynamics of skin allograft rejection seem similar to inflammatory skin conditions. T cells are key players in skin rejection and are recruited to the skin via activation of adhesion molecules, cytokines, and chemokines. Blocking these molecules has not only shown success in the treatment of inflammatory dermatoses, but also prolonged graft survival in various models of solid organ transplantation. In addition to T cell recruitment, ectopic lymphoid structures within the allograft associated with chronic rejection in solid organ transplantationmight contribute to the strong alloimmune response towards the skin. Selectively targeting the molecules involved offers exciting novel therapeutic options in the prevention and treatment of skin rejection after VCA. [ABSTRACT FROM AUTHOR]

Published

2012

198. Macrophage Migration Inhibitory Factor in Fetoplacental Tissues from Preeclamptic Pregnancies with or without Fetal Growth Restriction.

Author

Cardaropoli, Simona, Paulesu, Luana, Romagnoli, Roberta, Ietta, Francesca, Marzioni, Daniela, Castellucci, Mario, Rolfo, Alessandro, Vasario, Elena, Piccoli, Ettore, and Todros, Tullia

Subjects

CYTOKINES, MACROPHAGE migration inhibitory factor, PREGNANCY, PREECLAMPSIA, FETAL development

Abstract

The proinflammatory cytokine MIF (macrophage migration inhibitory factor) is involved in physiological and pathological processes in pregnancy. MIF maternal serum levels are increased in preeclampsia (PE). We hypothesize that pregnancy tissues are the source of MIF overexpression in PE.MIF protein was studied inmaternal sera, placental tissues, fetal membranes, and umbilical cord of 8 control and 20 PE pregnancies: 10 with normal fetal growth (PE-AGA) and 10 with fetal growth restriction (PE-FGR). MIF levels were significantly higher in PE-AGA membranes than in controls and PE-FGR. In PE-FGR, MIF cord concentrations were higher than in PE-AGA while MIF placental levels were lower than in controls. MIF maternal serum levels were higher in PE, compared to controls, and the difference wasmainly due to PE-FGR samples. These data support MIF involvement in PE pathogenesis and suggest that different pregnancy tissues contribute to MIF production in PE with and without fetoplacental compromise. [ABSTRACT FROM AUTHOR]

Published

2012

199. Role of Immune Escape Mechanisms in Hodgkin's Lymphoma Development and Progression: A Whole New World with Therapeutic Implications.

Author

Cruz-Merino, Luis de la, Lejeune, Marylène, Fernández, Esteban Nogales, Carrasco, Fernando Henao, López, Ana Grueso, Vacas, Ana Illescas, Pulla, Mariano Provencio, Callau, Cristina, and Álvaro, Tomás

Subjects

HODGKIN'S disease, LYMPHOPROLIFERATIVE disorders, CELL proliferation, IMMUNOLOGICAL deficiency syndromes, LYMPHATIC diseases, DISEASES in youths, CYTOKINES

Abstract

Hodgkin's lymphoma represents one of the most frequent lymphoproliferative syndromes, especially in young population. Although HL is considered one of the most curable tumors, a sizeable fraction of patients recur after successful upfront treatment or, less commonly, are primarily resistant. This work tries to summarize the data on clinical, histological, pathological, and biological factors in HL, with special emphasis on the improvement of prognosis and their impact on therapeutical strategies. The recent advances in our understanding of HL biology and immunology show that infiltrated immune cells and cytokines in the tumoral microenvironment may play different functions that seem tightly related with clinical outcomes. Strategies aimed at interfering with the crosstalk between tumoral Reed-Sternberg cells and their cellular partners have been taken into account in the development of new immunotherapies that target different cell components of HL microenvironment. This new knowledge will probably translate into a change in the antineoplastic treatments in HL in the next future and hopefully will increase the curability rates of this disease. [ABSTRACT FROM AUTHOR]

Published

2012

200. Glutamine Randomized Studies in Early Life: The Unsolved Riddle of Experimental and Clinical Studies.

Author

Briassouli, Efrossini and Briassoulis, George

Subjects

GLUTAMINE, CLINICAL trials, HEALTH outcome assessment, HEAT shock proteins regulation, PREMATURE infant diseases, ANIMAL models in research

Abstract

Glutamine may have benefits during immaturity or critical illness in early life but its effects on outcome end hardpoints are controversial. Our aim was to review randomized studies on glutamine supplementation in pups, infants, and children examining whether glutamine affects outcome. Experimental work has proposed various mechanisms of glutamine action but none of the randomized studies in early life showed any effect onmortality and only a few showed some effect on inflammatory response, organ function, and a trend for infection control. Although apparently safe in animal models (pups), premature infants, and critically ill children, glutamine supplementation does not reduce mortality or late onset sepsis, and its routine use cannot be recommended in these sensitive populations. Large prospectively stratified trials are needed to better define the crucial interrelations of "glutamineheat shock proteins-stress response" in critical illness and to identify the specific subgroups of premature neonates and critically ill infants or children who may have a greater need for glutamine and who may eventually benefit from its supplementation. The methodological problems noted in the reviewed randomized experimental and clinical trials should be seriously considered in any future well-designed large blinded randomized controlled trial involving glutamine supplementation in critical illness. [ABSTRACT FROM AUTHOR]

Published

2012