Abstract 4339

INTRODUCTION:

Relapses occur in 25–30% of childhood ALL. We evaluated the outcome of this group of patients (pts) according to the duration of the 1st CR, immunophenotype and site of relapse in our Institution.

PATIENTS AND METHODS:

From Sept’94 to Aug’09, 245 ALL relapses were diagnosed: 73 cases were not evaluable due to: different treatments received (n: 36), palliative care (n: 26) and insufficient data (n: 11); 172 pts were evaluable (54 F/118 M), with a mean age at the moment of the relapse of 9.8 (range 1.8–20.8) years. Induction therapy combined a pre-phase with 10 days of prednisone and 1 block of high doses of chemotherapy, followed by 5 blocks of similar intensity, CNS or testicular (preventive/therapeutic) radiotherapy, and weekly rotational maintenance, until completing two years from the moment of diagnosis. High-risk relapsed pts who had an available identical donor received HSCT.

RESULTS:

Immunophenotype was B-cell precursor (Bcp) in 89% of the pts and T-cell in 11 %. The duration of the 1st CR was <18 mo in 41 (24%), 18–36 mo in 79 (46%), >36 mo in 52 (30%) pts. The sites of relapse were bone marrow (BM) in 106 pts (61%), combined bone marrow (cBM) in 27 pts (17%) and isolated extramedullar in 39 pts (22%). The response to induction was: CR 134 pts (78%), death during induction 20 pts (12%) and partial/null response 18 pts (10%). Among the 134 pts who achieved CR, 69 (52%) presented a second relapse at 18,8 (r 0.7–88.8) mo from the 2nd CR, 10 (7%) died in CR and 1 developed a 2nd neoplasm. With a mean follow-up of 49 (r 2–155) mo, 54 pts remain in CR, 37 of them out of therapy. Of the 26 pts who received HSCT, 12 relapsed and 3 died in CR. The EFSp (SE) for the total group of pts was 25 (3)% and LFS probability (SE) 33 (4)%; for Bcp relapses it was 28%, and for T relapses 6% (P=0.0025); for BM+cBM cases it was 21%, and 40% for extramedullar (P=0.0061). However, testicular relapses achieved EFSp of 80%, and 12% for the remaining extramedullar cases (P=0.0004). The EFSp for relapses at <18mo of 1st CR was 5%, between 18–36 mo 25% and >36 m 41% (P=0.0001).

CONCLUSIONS:

The immunophenotype, the duration of the 1st CR and site of relapse significantly influenced the EFSp. Isolated testicular relapses achieved the best EFSp. HSCT is an eligible option for a small group of pts. New therapeutic approaches must be developed to improve outcome of most of relapsed ALL patients.

Disclosures:

No relevant conflicts of interest to declare.

Topics:
acute lymphocytic leukemia, b-lymphocytes, bone marrow, brachial plexus neuritis, chemotherapy regimen, child, donors, follow-up, hematopoietic stem cell transplantation, immunophenotyping

Author notes

*

Asterisk with author names denotes non-ASH members.

© 2010 by The American Society of Hematology
2010
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