Tompkins S M, Kraft J R, Dao C T, Soloski M J, Jensen P E
Department of Pathology and Laboratory Medicine, Emory University School of Medicine, Atlanta, Georgia 30322, USA.
J Exp Med. 1998 Sep 7;188(5):961-71. doi: 10.1084/jem.188.5.961.
T cell hybridomas isolated from nonresponder H-2(b) mice immunized with pork insulin were stimulated by insulin in the presence of major histocompatibility complex (MHC)-unmatched antigen presenting cells. The restriction element used by these CD4(-) T cells was mapped to an oligomorphic MHC class Ib protein encoded in the T region and identified as Qa-1(b) using transfectants. The antigenic determinant was localized to the insulin B chain, and experiments with truncated peptides suggested that it is unexpectedly long, comprising most or all of the 30 amino acid B chain. The antigen processing pathway used to present insulin to the Qa-1(b)- restricted T cells does not require transporters associated with antigen processing (TAP), and it is inhibited by chloroquine. A wide variety of cell lines from different tissues efficiently present soluble insulin to Qa-1(b)-restricted T cells, and insulin presentation is not enhanced by phagocytic stimuli. Our results demonstrate that Qa-1(b) can function to present exogenous protein to T cells in a manner similar to MHC class II molecules. Therefore, this class Ib protein may have access to a novel antigen processing pathway that is not available to class Ia molecules.
从用猪胰岛素免疫的无反应H-2(b)小鼠中分离出的T细胞杂交瘤,在主要组织相容性复合体(MHC)不匹配的抗原呈递细胞存在的情况下受到胰岛素刺激。这些CD4(-) T细胞使用的限制元件被定位到T区域编码的一种寡态MHC Ib类蛋白,并通过转染体鉴定为Qa-1(b)。抗原决定簇定位于胰岛素B链,对截短肽的实验表明它出乎意料地长,包含30个氨基酸B链的大部分或全部。用于将胰岛素呈递给Qa-1(b)限制的T细胞的抗原加工途径不需要与抗原加工相关的转运体(TAP),并且它被氯喹抑制。来自不同组织的多种细胞系有效地将可溶性胰岛素呈递给Qa-1(b)限制的T细胞,吞噬刺激不会增强胰岛素呈递。我们的结果表明,Qa-1(b)可以以类似于MHC II类分子的方式将外源性蛋白质呈递给T细胞。因此,这种Ib类蛋白可能能够进入Ia类分子无法利用的新抗原加工途径。
