Negative selection of murine medullary-type single positive thymocytes

Negative selection depletes self-reactive T cells, thus ensuring self-tolerance. It is usually considered that negative selection imposed on double-positive (DP) thymocytes that reside at the cortico-medullary junction. Negative selection model was set up by injecting mice with anti-T cell receptor (TCR) monoclonal antibody (mAb) intraperitoneally in this work. As shown in phenotypic analysis of thymocytes, negative selection destroys not only cortical-type DP thymocytes, but also medullary-type CD3+TCRαβ+CD4SP and CD3+TCRαβ+CD8SP thymocytes. Negative selection of medullary-type single positive (SP) are more susceptible to apoptosis, while with development of the cells, their resistance to apoptosis increases. Therefore, negative selection does not operate on functionally mature thymocytes at the late stage. This result is a supplement to the traditional theory of negative selection. Negative selection of medullary-type thymocytes is probably to further deplete self-reactive T cells, thus producing precise TCR repertoire and inducing self-tolerance.     

Molecular and cellular mechanisms of T Cell development

The thymus is central to the establishment of a functioning immune system. Here is the place where T cells mature from hematopoietic progenitors, driven by mutual interactions of stromal cells and the developing thymocytes. As a result, different types of T cells are generated, all of which have been carefully selected for the ability to act in host defense towards non-self and against the potential to mount pathogenic self-reactive autoimmune responses. In this review we summarize our present knowlege on the lineage decisions taking place during this development, the selection processes responsible for shaping the T cell antigen-receptor repertoire, the interactions with the stromal components and the signal transduction pathways which transform the interactions with the thymic microenvironment into cellular responses of survival, proliferation, differentiation and, importantly, also of cell death. Received 12 June 2003; received after revision 22 July 2003; accepted 28 July 2003     

A dioestrous increase in thymocyte proliferation during the oestrous cycle

Summary Coitus, which precedes internal fertilisation, is a unique physiological event which allows motile allogeneic spermatozoa to enter the female host and invade her tissues. The cyclic cellular proliferation observed in the thymus of the female rat may be an important preparation of her immune system for this event.     

Effect of MTECl on the functional expression of TCRαβ~ + 3G11~- 6C10~-CD4~+CD8~- thymocyte subset

A murine CD4+ thymocyte subset with phenotype of TCRαβ + 3G11- 6C10- CD4 + CD8- CD69 +/- HSAmed/locontains the cells in relatively functional matured status. The functional property of the cells in this subset is characterized by the unique pattern of cytokine production at transitional stage from Th0 to Th2 type with the latter being the dominant type. After being co-cultured with murine thymic medullary epithelial cell line (MTEC1) cells, a murine thymic medullary type epithelial cell line, the TCRαβ(T 3G11 6C10-CD4 + CD8- CD69+/- HSAmed/l? thy-mocytes, has exhibited significantly higher levels of proliferation capability and IL-6 production, whereas the production of IL-4 and IL-10 is suppressed after co-culturing with MTECl. By contrast, MTECl could not induce thymocytes to secrete Th1 type of cytokines. The results suggest that MTECl can regulate functional status of this thymocyte subset and induce them to develop into a specialized Th2 subset.     

Inhibitory Effect of Lithium Chloride on Mouse Thymocyte Apoptosis

This study investigates the effect of lithium chloride (LiCI) on mouse thymocyte apoptosis. A primary culture of mouse thymocytes was preincubated with LiCI (from 5 to 500μmol/L) before exposure to dexamethasone (DEX), the apoptosis inducer. With 100μmol/L of LiCI, apoptotic cell death induced by DEX was almost completely prevented as determined by flow cytometric analysis, terminal deoxynudeotidyltransferase (TdT)-mediated dUTP nick end labeling (TUNEL) assay and DNA laddering assay. The results show that the DEX-induced increment of caspase-3 activity in thymocytes is completelye liminated by LiCI preincubation. The results suggest that LiCI may protect Balb/c mouse thymocytes from apoptosis induced by glucocorticoid in a dose-dependent matter.     

Functional maturation of two murine medullary-type CD8SP thymocytes

TCRαβCD4-CD8+ thymocytes are heterogeneity. They may undergo phenotypic and functional maturation within thymic medulla. Medullary-type CD8SP thymocytes were divided into seven subsets based on phenotypic analysis, and their precursor-progeny relationship along with the differential pathway was also delineated. To further testify the validity of the maturation pathway, we purified 6C10-CD69+ cells representing the early stage and 6C10-Qa-2+ cells representing the later stage among medullary-type CD8SP thymocytes and compared their functional maturation levels. CD8+ T cells of spleen were used as the control. It is shown that there is no obvious difference of proliferation ability among these three subsets; however, intracytoplasmic cytokine assay shows that there is a hier archy of IFN-γ and TNFα secretion among these subsets, strikingly comparable to their phenotypic status among medullary type CD8SP thymocytes. The bioassays of IL-2 and IFN-γ in culture supernatant give the similar results.     

胸腺内双阴胸腺细胞重建动态的数学模型

根据小鼠的胸腺细胞实验数据,建立了描述胸腺细胞（ｔｈｙｍｏｃｙｔｅ）发育过程的数学模型,该模型考虑了胸腺细胞与胸腺基质细胞（ｔｈｙｍｉｃ ｓｔｒｏｍａｌ ｃｅｌｌ,ＴＳＣ）之间的相互作用,能够模拟ＣＤ４－ＣＤ８－ＤＮ细胞重建动态及正常小鼠胸腺细胞的发育过程,研究表明,模型中的一些参数应该是含有时间延迟的,通过模型研究了胸腺细胞与ＴＳＣ之间亲和力在胸腺选择过程中的阳性与阴性选择中的差异,理论预言与实     

Effect of MTEC1 on the functional expression of TCRaβ+ 3G11− 6C10− CD4+ CD8− thymocyte subset

A murine CD4⁺ thymocyte subset with phenotype of TCRαβ⁺ 3G11⁻ 6C10⁻ CD4⁺ CD8⁻ CD69^+/- HSA^med/lo contains the cells in relatively functional matured status. The functional property of the cells in this subset is characterized by the unique pattern of cytokine production at transitional stage from Th0 to Th2 type with the latter being the dominant type. After being co-cultured with murine thymic medullary epithelial cell line (MTEC1) cells, a murine thymic medullary type epithelial cell line, the TCRαβ⁺ 3G11⁻ 6C10⁻ CD4⁺ CD8⁻ CD69^+/- HSA^med/lo thymocytes, has exhibited significantly higher levels of proliferation capability and IL-6 production, whereas the production of IL-4 and IL-10 is suppressed after co-culturing with MTECl. By contrast, MTECl could not induce thymocytes to secrete Thl type of cytokines. The results suggest that MTECl can regulate functional status of this thymocyte subset and induce them to develop into a specialized Th2 subset.     

胸腺素对增强Sarcoma180小鼠免疫力的研究

本文报道小鼠荷瘤后,随肿瘤细胞的增长,瘤鼠体重、瘤重、脾重及脾细胞数/克,胸腺重及胸腺细胞数/克,有丝分裂指数的变化,并用~3H-TdR掺入法测定胸腺淋巴细胞在ConA作用下的淋转反应,从酵母多糖混合玫瑰花形成试验观察胸腺淋巴细胞亚群的动态变化;同时,观察外源性胸腺素在胸腺淋巴细胞增殖速度和抑癌观察中的作用,结果表明:外源性胸腺素对S_(180)小鼠胸腺淋巴细胞具有增殖作用,并提高瘤鼠免疫力,从而抑制瘤细胞的增殖。