Details

Autor(en) / Beteiligte

• DUVAL, M
• FENNETEAU, O
• VILMER, E
• CAVE, H
• GOBILLOT, C
• ROHRLICH, P
• GUIDAL, C
• LESCOEUR, B
• LEGAC, S
• SCHLEGEL, N
• STERKERS, G

Titel

Expansion of polyclonal B-cell precursors in bone marrow from children treated for acute lymphoblastic leukemia

Ist Teil von

• Hematology and cell therapy, 1997-06, Vol.39 (3), p.139-147

Ort / Verlag

Paris: Springer

Erscheinungsjahr

1997

Quelle

SpringerLINK Contemporary (Konsortium Baden-Württemberg)

Beschreibungen/Notizen

• In a series of 12 patients (mean age: 3 years at diagnosis) receiving chemotherapy for acute lymphoblastic leukemia, bone marrow examinations performed during hematopoietic recovery following treatment-induced agranulocytosis or completion of maintenance treatment showed at least 15% of non malignant immature cells which were sometimes hardly distinguishable from leukemic cells. No comparable data was observed in patients treated with G-CSF. The cytological features of these cells as well as their immunophenotyping were defined. Results showed that the majority of cells expressed HLA-DR, CD19, CD10 and cytoplasmic IgM but not the CD34 markers. This predominant and homogeneous pre-B cell population which likely represents the expansion of a minor population detectable in normal bone marrow is phenotypically indistinguishable from leukemic cells. The pattern of IgH gene rearrangements studied by PCR amplification of the CDRIII region showed that these cells were polyclonal. Except in one patient, minimal residual disease was not detected using probes specific for IgH or TCR gene rearrangement of the malignant clone. In children during the hematopoietic recovery after chemotherapy, immature marrow cells in great numbers, even with an highly homogeneous immunophenotype identical to the malignant clone's, are not sufficient for the diagnosis of relapse.