Clinical Investigations of Sjogren's Syndrome

干燥综合征的临床研究

• 批准号: 7967085
• 负责人: Gabor Illei
• 金额: $ 148.01万
• 依托单位: NATIONAL INSTITUTE OF DENTAL & CRANIOFACIAL RESEARCH
• 依托单位国家: 美国
• 资助国家: 美国
• 起止时间: 至
• 项目状态: 未结题
• 来源: https://reporter.nih.gov/project-details/7967085
• 关键词: Accounting; Address; Adopted; Area; Autoantibodies; Autoimmune Diseases; Autoimmune Process; Autoimmunity; Autonomic nervous system; B-Lymphocytes; Basic Science; Biological Markers; Biopsy; Body Surface; Cardiovascular system; Categories; Classification; Clinic; Clinical; Clinical Research; Clinical Trials; Clinical Trials Design; Collaborations; Collection; DNA Library; Data; Data Analyses; Defect; Diagnosis; Diagnostic; Disease; Disease model; Dryness; Endocrinology; Enrollment; Evaluation; Exocrine Glands; Female; Functional disorder; Future; Gene Expression; Genetic; Genetic Polymorphism; Gland; Goals; Homeostasis; Image; Immune system; Immunoglobulins; Immunohistochemistry; Immunology; In Vitro; Individual; Inflammation; Inflammatory; Institution; Intervention; Investigation; Investigational Drugs; Joints; Knowledge; Laboratories; Laboratory Study; Lead; Learning; Manuscripts; Measurement; Mediating; Messenger RNA; Metabolic; Methodology; Methods; MicroRNAs; Minor salivary gland structure; Modeling; Monoclonal Antibodies; Mus; National Institute of Dental and Craniofacial Research; National Institute of Neurological Disorders and Stroke; Natural History; Nervous System Physiology; Nervous system structure; Oklahoma; Organ; Outcome Measure; Paper; Pathogenesis; Pathway interactions; Patients; Pattern; Peripheral Blood Mononuclear Cell; Phase; Phase II Clinical Trials; Physiological; Pilot Projects; Placebo Control; Placebos; Play; Process; Production; Protein Tyrosine Kinase; Protocols documentation; Psoriasis; Publishing; Raptiva; Reporting; Research; Research Personnel; Research Project Grants; Retrospective Studies; Role; STIM1 gene; Safety; Saliva; Salivary; Salivary Glands; Sampling; Scientist; Sjogren' s Syndrome; Skin; Smooth Muscle; Staging; Symptoms; Syndrome; System; Testing; Therapeutic; Therapy Clinical Trials; Time; Toxic effect; Translational Research; United States National Institutes of Health; Variant; Xerostomia; clinical practice; cohort; design; efalizumab; eye dryness; gene therapy; genome wide association study; healthy volunteer; improved; male; medical specialties; meetings; metabolomics; neurochemistry; novel; peripheral blood; preclinical study; prognostic; response; tool; volunteer

Sjogrens Syndrome (SS) is an autoimmune disease, characterized by widespread inflammation in the exocrine glands and other organs resulting in dryness of the lining surfaces of the body, most notably, dry mouth and dry eyes. In addition, it can involve numerous other organs such as the joints, skin and nervous system. The MPTB- SS Clinic conducts clinical investigations and clinical trials, and collaborates with laboratory investigators in MPTB, other NIH laboratories and Institutions outside the NIH in order to understand the mechanisms underlying this disease. The ultimate goal of our research is to find treatments for SS that are safe, effective and target specific steps in the pathogenesis of SS. We focus our research in two broad categories. Natural history studies include observational and retrospective studies with the goal to expand our knowledge about the pathogenesis of SS, to improve our diagnostic and prognostic tools and to identify targets for new therapies. The other major area involves the evaluation of novel treatments in patients with SS. Treatment study using efalizumab (Raptiva) an anti-LFA1 monoclonal antibody In this study we tested Raptiva (efalizumab, Genentech), an anti-LFA1 monoclonal antibody targeting the LFA1-ICAM pathway involved in several functions in Sjogrens Syndrome, in a pilot Phase 2 study. The protocol was prematurely terminated due to serious complications reported with Raptiva in patients with psoriasis. Up to then we had enrolled ten patients and treated nine. Six patients received Raptiva and three placebo during the first placebo controlled phase of the study. Primary response criteria were only met by one of the placebo recipients. Raptiva has increased inflammation in the salivary gland, worsened salivary gland function in most patients and led to significant increase in immunoglobulin production and the emergence of new autoantibodies in two patients. The mechanism of these unexpected effects are currently under investigation by a variety of methods including gene expression analysis in the peripheral blood and salivary gland biopsies, microRNA arrays of biopsies, immunohistochemistry and metabolomics. Autonomic nervous system (ANS) dysfunction in SS The range of symptoms in SS suggests that there may be perturbations in the nervous and immune systems and in pathways through which these systems communicate and mediate each other. Compared to normal healthy individuals, SS patients have significantly more prevalent nervous system involvement including impaired ANS function (which regulates the homeostasis via effects on the smooth muscle, glands and cardiovascular system) unique to these patients. We hypothesize that ANS dysfunction is central to the pathogenesis of SS and, in collaboration with Dr. David Goldsteins group (NINDS), we are conducting a protocol to investigate ANS function in patients with SS and the association between ANS dysfunction and autoimmunity. This protocol consists of a comprehensive evaluation of autonomic function, using physiological, neuropharmacologic, neurochemical, and imaging approaches, to identify consistent distinctive patterns of ANS involvement in SS and thereby improve the diagnosis and understanding of pathophysiologic mechanisms of SS. We completed testing in 14 patients and 5 controls We also completed non-invasive testing of the ANS in over 200 subjects in the natural history protocol. We are currently analyzing the data and plan to prepare a manuscript by the end of the year. Natural history of Sjogrens Syndrome protocol Current classification criteria of SS use whole unstimulated salivary flow as the measurement of SG function. This has been adopted by most investigators primarily because its simplicity. Some other academic SS centers, including us, have used glandular collection of saliva for classification purposes. To test if this was reasonable we compared these two measurement and their impact of EACG classification using 340 concomitant observations and have shown a reasonable good correlation between the two methods. In another study we evaluated the association between salivary gland inflammation and hypofunction. In a cohort of 339 pSS patients we found that inflammation accounted only for 10 percent of the variation if flow. These data suggest that salivary inflammation and dysfunction may be two different processes in the pathogenesis of SS. This may have significant implications on evaluating disease models, selecting appropriate outcome measures and designing clinical trials of pSS. Biomarker studies Salivary gland microRNA expression A major focus of this study was to evaluate the potential of microRNAs (miRNAs) as biomarkers. In a pilot study we used 24 Agilent microRNA microarrays to profile miRNAs isolated from healthy volunteers and Sjogrens patients minor salivary glands (MSGs) with high or low grade inflammation. In each group half of the patients had normal and half had decreased salivary flow. Using a novel method for data normalization we identified microRNA profiles that can serve as biomarkers for diagnosis (SS vs controls), function (salivary flow) or degree of inflammation in SS. We identified two miRNAs that changed in opposite direction between the low and high focus score samples. The ratio of expression levels of those 2 microRNAs correlated very well with the inflammatory status of the MSGs in an independent set of samples. We also found significant difference between patient with preserved and decreased salivary flow in the high focus score group. Salivary exosomal microRNAs We have published a paper of our methodology for the identification of microRNAs from exosomes in whole and glandular saliva. Genetic studies We have continued to expand our DNA bank for patients with SS. We have provided DNAs to Dr. John Harleys group in Oklahoma for genome wide association studies SS. The first results of these studies identified a BLK (a B lymphocyte tyrosine kinase) polymorphism for pSS and were presented at the 2008 ACR meeting. MPTB translational research project on Sjogrens Syndrome To narrow the gap between basic science and clinical practice we continued our collaboration several groups in NIDCR. Several gene therapy projects are underway in Dr. Chiorinis laboratory targeting various molecules in murine models of SS. As part of the salivary gland initiative we have successfully completed mRNA gene expression studies of 11 normal volunteer and 46 pSS samples in collaboration with the Chiorini group. We are analyzing the differences between healthy male and female salivary glands as well as differences between various patient subsets and controls. With the Ambudkar group we confirmed that miR150, one of the most differentially expressed microRNAs in SS salivary gland, decreases the expression of STIM-1 in vitro and showed patients with SS have a defect in STIM1 expression with significantly lower STIM1 levels in peripheral blood mononuclear cells compared to controls. These data suggest that STIM1 may play an important role in the pathogenesis of SS and that it may be downregulated by miR150. Future plans We plan to develop several early stage clinical studies to establish the safety and toxicity of an intervention, and at the same time, collect data about its possible efficacy. We establish collaborations to combine these clinical trials with thorough basic science evaluations. We will continue to collaborate on preclinical studies to learn about the pathogenesis of SS and to enable gene therapy and cellular therapy in the future. In addition to these treatment studies we will do non-interventional clinical studies to address clinical manifestations of Sjogrens Syndrome that are poorly understood and/or not explained by systemic autoimmunity, such as ANS dysfunction and metabolic abnormalities.

干燥综合征（Sjogrens Syndrome， SS）是一种自身免疫性疾病，其特征是外分泌腺和其他器官的广泛炎症，导致身体内膜表面干燥，最明显的是口干和眼干。此外，它还可能涉及许多其他器官，如关节、皮肤和神经系统。MPTB- SS诊所进行临床调查和临床试验，并与MPTB实验室研究人员、其他NIH实验室和NIH以外的机构合作，以了解这种疾病的潜在机制。