T-lymphocytes, or T cells, are a principal component of the body’s adaptive immune system. Together, these cells express a large repertoire of antigen specific receptors that recognise foreign material derived, for example, from pathogens and tumour cells. The generation of these antigen receptors occurs during T cell development in the thymus. This constitutes, however, a random process that also includes the formation of antigen receptors which respond well to the body’s own proteins, so-called self-antigens. To prevent T cells bearing a self-reactive antigen receptor to exit from the thymus to the rest of the body where they may cause autoimmunity, a mechanism is in place that involves mTECs. These specialised thymic epithelial cells express most of the body’s self-antigens. T cells that recognise their specific antigen presented by mTECs will undergo a process of programmed cell death and are consequently deleted in the thymus.
Very little is presently known about how cTECs and mTECs develop, or how they relate to each other. A Swiss-Japanese research team now reports that mTECs derive from cells that already express β5t, a proteasome subunit that is densely concentrated in cTECs and no other cell types, including mTECs themselves. This finding, which is published in the May 27-30, 2013 edition of PNAS, suggests that mTECs may evolve from cTECs. This finding has not only implications for how mTECs develop, but also how they may have evolved.
The research project was led in Switzerland by Prof. Georg Holländer, Professor of Paediatric Immunology at the University of Basel and Action Research Professor of Paediatrics at the University of Oxford. In Japan, the project was led by Prof. Yousuke Takahama of the Institute for Genome Research at the University of Tokushima, which initially discovered the β5t proteasome subunit. Dr. Izumi Ohigashi of the Institute for Genome Research at the University of Tokushima and Dr. Saulius Zuklys at the University Children’s Hospital of Basel serve as first authors.
Professor Holländer believes that the benefits of a better understanding of the origins and functions of mTECs and cTECs extend well beyond basic research. The team’s findings suggest that evolutionary pressures have caused the body to check the quality of T cells that it produces. The T cell antigen receptor repertoire in evolutionary older species have a receptor, and did not require the body to implement quality control – but as the capacity developed to produce a seemingly infinite number of T cell antigen receptors the vital need to control their specificities has arisen. For this purpose the body may have “hijacked” existing cells, namely cTECs. Holländer also believes that the findings could inform attempts to reconstruct or develop in-vitro thymuses, which could in turn be used to help people who lack a normal thymus function because of inborn or acquired defects. “You can fix things if you know how they are formed in the first place,” he claims.
The research was supported by Grants-In-Aid for Scientific Research from the Ministry of Education, Culture, Sports, Science, and Technology and the Japan Society for the Promotion of Science, and by a Strategic Japanese-Swiss Cooperative Program on Molecular Medical Research from the Japan Science and Technology Agency and the Federal Institute of Technology (ETH)-Zürich.
Izumi Ohigashi, Saulius Zuklys, Mie Sakata, Carlos E. Mayer, Saule Zhanybekova, Shigeo Murata, Keiji Tanaka, Georg Holländer, and Yousuke Takahama.
Aire-expressing thymic medullary epithelial cells originate from β5t-expressing progenitor cells.
Proceedings of the National Academy of Sciences of the United States of America, May 27-May 31, 2013. doi:10.1073/pnas.1301799110
Professor Georg Holländer, Department of Biomedicine, University of Basel, Mattenstrasse 28 4058 Basel, Tel. +41 61 695 30 69, e-mail: email@example.com
Professor Yousuke Takahama, Division of Experimental Immunology, Institute for Genome Research, University of Tokushima, 3-18-15 Kuramoto, Tokushima, Japan 770-8503 Tel. +81 88 633 9452, e-mail: firstname.lastname@example.org