作者
M Bocchia, S Gentili, E Abruzzese, A Fanelli, F Iuliano, A Tabilio, M Amabile, F Forconi, A Gozzetti, D Raspadori, S Amadori, F Lauria
发表日期
2005/2/19
期刊
The Lancet
卷号
365
期号
9460
页码范围
657-662
出版商
Elsevier
简介
Background
Although imatinib is the standard treatment for chronic myeloid leukaemia, not all patients reach complete cytogenetic remission (CCR) and most maintain detectable disease at the molecular level. We investigated whether a vaccine targeting the BCR-ABL-derived p210 fusion protein was an active and specific immunotherapy.
Methods
We recruited 16 patients who had chronic myeloid leukaemia (with the b3a2 fusion point of p210), stable residual disease, a minimum treatment of 12 months of imatinib or 24 months of interferon alfa, and no further reduction of residual disease for at least 6 months preceding enrolment. They were given six vaccinations with a peptide vaccine derived from the sequence p210-b3a2 plus molgramostim and QS-21 as adjuvants (CMLVAX100) before assessment of immunological and disease response, which included detecting amounts of b3a2 transcripts by standardised …
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