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فهرست مطالب tahereh shahrestani

  • مهرناز مصداقی، محمد وجگانی، عیسی صالحی، جمشید حاجتی، عبدالفتاح صراف نژاد، مسعود موحدی، فریده برجیسیان، طاهره شهرستانی
    رینیت آلرژیکAllergic Rhinitis یک اختلال علامت دار در بینی است که پس از تماس با آلرژن القاء شده و در اثر التهاب وابسته به IgE غشاهای پوشاننده بینی ایجاد می شود. این بیماری در سال 1929 توسط Hansel شرح داده شد. رینیت آلرژیک یک مشکل بهداشتی جهانی است که در کل دنیا باعث بیماری و ناتوانی زیادی می شود. در طی چهل سال آخر قرن گذشته شیوع AR افزایش پیدا کرده و در طی دهه گذشته دو برابر شده است. به همین دلیل در طی دهه اخیر توجه زیادی به مکانیسم های ایجاد کننده این بیماری ها شده است. یکی از پیشرفت های مهم در این زمینه شناسایی نقش سایتوکاین ها در پاتوژنز این بیماری ها بوده است. سایتوکاین های نوع 2 در بروز بیماری های آلرژیک نقش مهمی دارند. امروزه مشخص شده است که سایتوکاین های نوع 2 فقط توسط سلول های CD4+ ترشح نمی شود. دسته هایی از سلول های TCD8+، سلول های دندریتیک و سلول های NK نیز می توانند این سایتوکاین ها را ترشح کنند.
    Mehrnaz Mesdaghi, Mohammad Vodjgani, Eisa Salehi, Jamshid Hadjati, Abdolfattah Sarrafnejad, Masoud Movahedi, Farideh Berjisian, Tahereh Shahrestani
    Allergic rhinitis is a common disorder with great morbidity. Its prevalence has increased during recent years, therefore attracting attentions to its mechanisms. Type 2 cytokines play a major role in allergies. It has been proposed that Natural killer (NK) cells may be able to produce type 2 cytokines. This study was done to evaluate NK cells number and subtypes in patients with allergic rhinitis, comparing healthy subjects. >>>
  • Alireza Rezaei, Asghar Aghamohammadi, Mohammad, Hassan Moradinejad, Nima Parvaneh, Nima Rezaei, Roheila Seyedtabaei, Hossein Asgarian, Omran, Tahereh Shahrestani, Ali, Akbar Amirzargar
    Objective
    Juvenile idiopathic arthritis (JIA) is the most common rheumatic disease in children. The exact causes of disease are still poorly understood. It seems that B cells have several functions in JIA, including production of autoantibodies, antigen presentation, production of cytokines, and activation of T cells. Here, we aimed to evaluate B-cell lineage and its precursors in the bone marrow of patients with JIA.
    Methods
    Twenty consecutive patients with JIA were enrolled in this study. JIA is subdivided into three groups of Pauciarticular, Polyarticular, and Systemic JIA. Bone marrow mononuclear cells were separated. Then we analyzed the immunophenotype of the JIA patients by flow cytometry. After separation, the mononuclear cells were stained specific for B cell lineage [CD10, CD19 and CD20], T cell lineage [CD3] and non specific lineage [CD34, HLA-DR and TdT].
    Findings
    Flow cytometric study of bone marrow showed that JIA patients had low level of CD10, CD19, and CD20. Polyarticular patients had lower level of D10, CD19, and CD20 than pauciarticular JIA patients and systemic onset JIA patients had lower levels than both of them.
    Conclusion
    Decreasing of B cell precursor in bone marrow is one of mechanisms for pathogenesis of JIA and the more decreased B cell precursors in bone marrow are, the worst severity of the disease is. Significant differences in CD10 content of bone marrow were detected between the polyarticular and pauciarticular groups. So, it seems that polyarticular JIA patients had lower percentage of pre B cell stage.
  • Masoud Ravanbakhsh, Abdolfatah Sarafnejad, Asghar Aghamohammadi, Gholam Ali Kardar, Hossein Asgarian Omran, Lida Atarod, Nima Rezaei, Tahereh Shahrestani, Mostafa Hosseini, Mostafa Moin
    Common variable immunodeficiency (CVID) is the most common symptomatic primary antibody deficiency, characterized by reduced serum immunoglobulins levels and increased susceptibility to recurrent pyogenic infections. In this study, we evaluated CD40 ligand expression on stimulated versus unstimulated T-helper lymphocytes of nine Common variable immunodeficient patients in comparison with fifteen normal controls. Phorbol myristate acetate (PMA) and Ionomycin were used to stimulate cells in vitro. After six hours stimulation, the cells were subjected to surface staining with three-color staining procedure. Events were analyzed by flow cytometer, using FloMax software. Results were reported as the percentage of lymphocytes expressing CD markers. We did not find any significant statistical difference in CD40 ligand expression between patients and controls (p>0.05), despite having stimulation documented by CD69 expression as activation marker in each run. The results of this study are in agreement with some other studies, indicating that CD40 ligand expression on stimulated T-helper lymphocytes of Common variable immunodeficiency patients is similar to normal controls.
  • Hossein Asgarian Omran, Mahdi Shabani, Tahereh Shahrestani, Abdolfattah Sarafnejad, Jalal Khoshnoodi, Parvaneh Vosoogh, Mohammad Faranoush, Ramzan A. Sharifian, Mahmood Jeddi, Tehrani, Hodjatallah Rabbani, Fazel Shokri
    Background
    Immunophenotypic characterization of the leukemic cells has been widely used as a tool for diagnosis, classification, stratification and prognosis of leukaemia.
    Objective
    To investigate the immunophenotypic subtype profiles of Iranian patients with acute lymphoblastic leukemia (ALL) and its association to disease outcome.
    Methods
    In this study, a total of 60 Iranian patients with ALL were immunophenotyped by flow cytometry using a panel of monoclonal antibodies specific for CD2, CD3, CD5, CD10, CD13, CD14, CD19, CD20, CD33, CD34, CD45, HLA-DR and TdT molecules.
    Results
    The samples were initially categorized into T-ALL (n=9), B-ALL (n=50) and mixed lineage (n=1) based on the expression patterns of CD3 and CD19 molecules. B-ALL patients could further be classified into four subtypes, including Pro-B (n=7, 11.7%), Pre-B I (n=28, 46.7%), Pre-B II (n=13, 21.7%) and immature/mature B cells (n=2, 3.3%) on the basis of expression of CD10, CD19, CD20, HLA-DR and TdT. Clinical manifestations and laboratory findings of the patients did not reveal association with immunophenotypic sub-types of ALL, with the exception of mediastinal mass and WBC count at the time of diag-nosis which were found to be significantly higher in patients with T-ALL compared with B-ALL (p=0.001 and 0.014), respectively.
    Conclusion
    Our results indicate that overall the immunophenotypic profile of Iranian ALL patients is similar to previous reports and it might be used for monitoring of minimal residual disease and prognosis.
  • Hossein Asgarian, Mahdi Shabani, Parvaneh Vosoogh, Ramazan Ali Sharifian, Soheila Gharagozlou, Jalal Khoshnoodi, Tahereh Shahrestani, Mahin Kordmahin, Abdolfattah Sarrafnejad, Mahmood Jeddi Tehrani, Hodjatallah Rabbani, Fazel Shokri
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