%0 Journal Article
%T Altered expression of the TCR signaling related genes CD3 and Fc¦ĹRI¦Ă in patients with aplastic anemia
%A Bo Li
%A Sichu Liu
%A Yuzhe Niu
%A Su Fang
%A Xiuli Wu
%A Zhi Yu
%A Shaohua Chen
%A Lijian Yang
%A Yangqiu Li
%J Journal of Hematology & Oncology
%D 2012
%I BioMed Central
%R 10.1186/1756-8722-5-6
%X To elucidate the T cell receptor (TCR) signal transduction features in AA, the expression levels of CD3¦Ă, ¦Ä, ¦Ĺ and ¦Ć chain and Fc¦ĹRI¦Ă genes, which are involved in TCR signal transduction, and the negative correlation of the expression levels between the CD3¦Ć and Fc¦ĹRI¦Ă genes in T cells from peripheral blood mononuclear cells (PBMCs) were analyzed. Real-time RT-PCR using the SYBR Green method was used to detect the expression level of these genes in PBMCs from 18 patients with AA and 14 healthy individuals. The ¦Â2microglobulin gene (¦Â2M) was used as an endogenous reference. The expression levels of the CD3¦Ă, CD3¦Ä, CD3¦Ĺ and CD3¦Ć genes in patients with AA were significantly increased compared to a healthy control group, whereas the Fc¦ĹRI¦Ă gene expression level was significantly decreased in patients with AA in comparison with the healthy control group. Moreover, the negative correlation of the expression levels between the CD3¦Ć and Fc¦ĹRI¦Ă genes was lost.To our knowledge, this is the first report of the CD3¦Ă, CD3¦Ä, CD3¦Ĺ, CD3¦Ć and Fc¦ĹRI¦Ă gene expression in patients with AA. The abnormally expressed TCR signaling related genes may relate to T cells dysfunction in AA.Aplastic anemia (AA) is a potentially fatal bone marrow failure disorder that is characterized by pancytopenia and bone marrow hypoplasia. In most cases, AA behaves as an immune-mediated disease [1]. Immunosuppression is a key treatment strategy for patients who are not suitable bone marrow transplant (BMT) candidates due to age or the lack of a suitable donor. Immunosuppression with antithymocyte globulins and cyclosporine is effective for restoring blood cell production in the majority of patients [2,3]. The thought that T cells play a major role in the pathophysiology of AA became evident in the late 1970s with the finding that marrow and peripheral blood lymphocytes from patients with AA were able to suppress hematopoiesis in vitro. Subsequently, activated CD8+ T cells were identified as the lymphocyte sub
%K Aplastic anemia
%K CD3¦Ă
%K CD3¦Ä
%K CD3¦Ĺ
%K CD3¦Ć
%K Fc¦ĹRI¦Ă
%K Gene expression
%U http://www.jhoonline.org/content/5/1/6