I propose a T-cell receptor (TcR)-based mechanism by which immunity mediates both genetic self and microbial self thereby, connecting microbiome disease with autoimmunity. The hypothesis is based on simple principles. First, TcR are selected to avoid strong cross-reactivity with self, resulting in selection for a TcR repertoire mimicking genetic self. Second, evolution has selected for a microbial self that mimics genetic self so as to share tolerance. In consequence, our TcR repertoire also mimics microbiome antigenicity, providing a novel mechanism for modulating tolerance to it. Also, the microbiome mimics the TcR repertoire, acting as a secondary immune system. I call this TcR-microbiome mimicry holoimmunity to denote immune tolerance to the holobiont self. Logically, microbiome-host mimicry means that autoimmunity directed at host antigens will also attack components of the microbiome, and conversely, an immunological attack on the microbiome may cross-react with host antigens producing holoautoimmunity.

• 出版日期2016-11