High frequency of antitumor T cells in the blood of melanoma patients before and after vaccination with tumor antigens

doi:10.1084/jem.20041379

Published 18 January 2005. doi:10.1084/jem.20041379
Rockefeller University Press, 0022-1007 $8.00
JEM, Volume 201, Number 2, 241-248

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ARTICLE

High frequency of antitumor T cells in the blood of melanoma patients before and after vaccination with tumor antigens

Catherine Germeau¹, Wenbin Ma¹^,2, Francesca Schiavetti¹, Christophe Lurquin¹^,2, Emmanuelle Henry¹, Nathalie Vigneron¹^,2, Francis Brasseur¹^,2, Bernard Lethé¹^,2, Etienne De Plaen¹^,2, Thierry Velu³, Thierry Boon¹^,2, and Pierre G. Coulie¹

¹ Cellular Genetics Unit, Université de Louvain, B-1200 Brussels, Belgium
² Ludwig Institute for Cancer Research, Brussels Branch, B-1200 Brussels, Belgium
³ Medical Oncology, Erasme Hospital, B-1070 Brussels, Belgium

CORRESPONDENCE Pierre G. Coulie: coulie{at}gece.ucl.ac.be

After vaccination of melanoma patients with MAGE antigens, weobserved that even in the few patients showing tumor regression,the frequency of anti-vaccine T cells in the blood was ofteneither undetectable or <10^–5 of CD8 T cells. This frequencybeing arguably too low for these cells to be sole effectorsof rejection, we reexamined the contribution of T cells recognizingother tumor antigens. The presence of such antitumor T cellsin melanoma patients has been widely reported. To begin assessingtheir contribution to vaccine-induced rejection, we evaluatedtheir blood frequency in five vaccinated patients. The antitumorcytotoxic T lymphocyte (CTL) precursors ranged from 10^–4to 3 x 10^–3, which is 10–10,000 times higher thanthe anti-vaccine CTL in the same patient. High frequencies werealso observed before vaccination. In a patient showing nearlycomplete regression after vaccination with a MAGE-3 antigen,we observed a remarkably focused antitumoral response. A majorityof CTL precursors (CTLp's) recognized antigens encoded by MAGE-C2,another cancer-germline gene. Others recognized gp100 antigens.CTLp's recognizing MAGE-C2 and gp100 antigens were already presentbefore vaccination, but new clonotypes appeared afterwards.These results suggest that a spontaneous antitumor T cell response,which has become ineffective, can be reawakened by vaccinationand contribute to tumor rejection. This notion is reinforcedby the frequencies of anti-vaccine and antitumor CTLs observedinside metastases, as presented by Lurquin et al. (Lurquin,C., B. Lethé, V. Corbière, I. Théate, N.van Baren, P.G. Coulie, and T. Boon. 2004. J. Exp. Med. 201:249–257).

Abbreviations used: CTLp, CTL precursor; MLPC, mixed lymphocyte–peptideculture; MLTC, mixed lymphocyte– tumor cell culture.

C. Germeau and W. Ma contributed equally to this work.

F. Schiavetti's present address is Glaxo-SmithKline Bio, 1330Rixensart, Belgium.

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