Springer Protocols: Abstract: Estimating Thymic Function Through Quantification of T-Cell Receptor Excision Circles

Estimating Thymic Function Through Quantification of T-Cell Receptor Excision Circles

By: Marie-Lise Dion^{2 3}, Rafick-Pierre Sékaly^{2 3 4}, Rémi Cheynier⁵

Abstract

Full Text

Download PDF (299K)

Analysis of immune reconstitution is of major importance in clinical settings such as following bone marrow transplantation or during anti-retroviral treatment of HIV-infected patients. In these patients, thymic function is essential for the reconstitution of a diversified T-cell receptor (TCR) repertoire. During thymopoiesis, several genetic rearrangements lead to the generation of fully functional TCR. By-products of these processes, the T-cell receptor excision circles (TRECs), are present in cells exported from the thymus but do not replicate during mitosis; they can thus be used as molecular markers for recent thymic emigrants. We demonstrate how thymic function can be assessed in a quantitative and noninvasive fashion in humans by estimating intrathymic precursor T-cell proliferation through the quantification of distinct TREC molecules in peripheral blood cells.

Affiliation(s): (2) Laboratoire d’Immunologie, Centre de Recherches du CHUM, Montréal, Canada
(3) Department of Microbiology and Immunology, McGill University, Montréal, Canada
(4) Département de Microbiologie et Immunologie, Université de Montréal, Montréal, Canada
(5) Unité des Virus Lents, Institut Pasteur, Paris, France

Book Title: Immunological Tolerance: Methods and Protocols

Series: Methods in Molecular Biology | Volume: 380 | Pub. Date: Jun-08-2007 | Page Range: 197-213 | DOI: 10.1007/978-1-59745-395-0_12

Subject: Immunology

Key Words: T-cell receptor excision circle - thymic production - real-time quantitative PCR - sj/βTREC ratio - thymus

References

Download References

1.	Staton, T. L., Johnston, B., Butcher, E. C., and Campbell, D. J. (2004) Murine CD8⁺ recent thymic emigrants are alphaE integrin-positive and CC chemokine ligand 25 responsive. J. Immunol. 172, 7282–7288.

2.	Tough, D. F. and Sprent, J. (1994) Turnover of naïve-and memory-phenotype T cells. J. Exp. Med. 179, 1127–1135.

3.	Taub, D. D. and Longo, D. L. (2005) Insights into thymic aging and regeneration. Immunol. Rev. 205, 72–93.

4.	Douek, D. C., McFarland, R. D., Keiser, P. H., et al. (1998) Changes in thymic function with age and during the treatment of HIV infection. Nature 396, 690–695.

5.	Dion, M. L., Poulin, J. F., Bordi, R., et al. (2004) HIV infection rapidly induces and maintains a substantial suppression of thymocyte proliferation. Immunity 21, 757–768.

6.	Anderson, G., Moore, N. C., Owen, J. J., and Jenkinson, E. J. (1996) Cellular interactions in thymocyte development. Annu. Rev. Immunol. 14, 73–99.

7.	Boyd, R. L., Tucek, L., Godfrey, D. L, et al. (1993) The thymic microenvironment. Immunol. Today 14, 445–459.

8.	van Ewijk, W. (1991) T-cell differentiation is influenced by thymic microenvironments. Annu. Rev. Immunol. 9, 591–615.

9.	Jameson, S. C., Hogquist, K. A., and Bevan, M. J. (1995) Positive selection of thymocytes. Annu. Rev. Immunol. 13, 93–126.

10.	Starr, T. K., Jameson, S. C., and Hogquist, K. A. (2003) Positive and negative selection of T cells. Annu. Rev. Immunol. 21, 139–176.

11.	Haynes, B. E, Markert, M. L., Sempowski, G. D., Patel, D. D., and Hale, L. P. (2000) The role of the thymus in immune reconstitution in aging, bone marrow transplantation and HIV-1 infection. Annu. Rev. Immunol. 18, 529–560.

12.	De Rossi, A., Walker, A. S., Klein, N., De Forni, D., King, D., and Gibb, D. M. (2002) Increased thymic output after initiation of antiretroviral therapy in human immunodeficiency virus type I-infected children in the Paediatric European Network for Treatment of AIDS (PENTA) 5 Trial. J. Infect. Dis. 186, 312–320.

13.	Delgado, J., Leal, M., Ruiz-Mateos, E., et al. (2002) Evidence of thymic function in heavily antiretroviral-treated humanimmunodeficiency virus type 1-infected adults with long term virologic treatment failure. J. Infect. Dis. 186, 410–414.

14.	Douek, D. C., Betts, M. R., Hill, B. J., et al. (2001) Evidence for increased T cell turnover and decreased thymic output in HIV infection. J. Immunol. 167, 6663–6668.

15.	Hatzakis, A., Touloumi, G., Karanicolas, R., et al. (2000) Effect of recent thymic emigrants on progression of HIV-1 disease. Lancet 355, 599–604.

16.	Kolte, L., Dreves, A. M., Ersboll, A. K., et al. (2002) Association between larger thymic size and higher thymic oputput in human immunodeficiency virus-infected patients receiving highly active antiretrovial therapy. J. Infect. Dis. 185, 1578–1585.

17.	Ometto, L., De Forni, D., Patiri, F., et al. (2002) Immune reconstitution in HIV-1 infected children nonantiretroviral therapy: role of thymic output and viral fitness. AIDS 16, 839–849.

18.	Harris, J. M., Hazenberg, M. D., Poulin, J. E, et al. (2005) Multiparameter evaluation of human thymic function: interpretations and caveats. Clin. Immunol. 115, 138–146.

Comments (Loading...)

Post comment/View all comments