• Title of article

    Phenotypic and Genotypic Diversity of Human Neuroblastoma Studied in Three IGR Cell Line Models Derived from Bone Marrow Metastases

  • Author/Authors

    Valent، نويسنده , , Alexander and Bénard، نويسنده , , Jean and Vénuat، نويسنده , , Anne-Marie and Da Silva، نويسنده , , Jacqueline and Duverger، نويسنده , , Annette and Duarte، نويسنده , , Nathalie and Hartmann، نويسنده , , Olivier and Spengler، نويسنده , , Barbara A and Bernheim، نويسنده , , Alain، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 1999
  • Pages
    6
  • From page
    124
  • To page
    129
  • Abstract
    Metastatic stage IV neuroblastoma tumors, as well as cell lines derived from them, are highly malignant and rapidly fatal. To determine whether malignant potential of these cells might be influenced by stromal tissue at sites frequently involved in metastasis, we initiated primary cultures from bone marrow of three patients (331, 337, and 91) with stage IV neuroblastoma. All three explants contained two distinct cell populations, malignant neuroblasts (Nb-type) and substrate adherent stromal-like (Str-type) cells. The cell types were separated at the first passage and studied by cytogenetic, molecular, and immunocytochemical methods. Karyotypic analyses after 3–6 passages in vitro revealed the presence of unique chromosomal abnormalities in Nb-type cells of all three lines: (1) der(1)t(1;7)(p32;q11) and der(5)t(5;17)(q35;q21) in pseudodiploid IGR-N-331 neuroblasts; (2) der(1)t(1;17)(p35;q21–22)×2 and der(7)t(7;7)(p21;q21) in IGR-N-337 hyperdiploid neuroblasts; and (3) more than six rearranged chromosomes in two related subpopulations of hypodiploid IGR-N-91 neuroblasts. Neuroblastic cells from all three tumors amplified MYCN 25- to 50-fold (with amplified genes visible as dmin or, in one IGR-N-91 subline, as an hsr(14)[q32]) and expressed N-CAM. Str-type cells from tumors 331 and 337 had a normal diploid karyotype, did not express either N-CAM or S-100, and are probably normal bone marrow fibroblasts. By contrast, S-100 negative Str-type IGR-N-91 cells were hypodiploid and shared at least two unbalanced translocations, der(4)t(1;4)(q12;p15) and der(2)t(2;10;17)(p14;q11;q22), with neuroblastic counterparts, indicating that “stromal” cells and malignant neuroblasts had a common tumor cell origin. Thus, the Str-type cells of IGR-N-91 are examples of S-type phenotypic variants frequently described for long-term human neuroblastoma cell lines in vitro, but not previously observed in vivo.
  • Journal title
    Cancer Genetics and Cytogenetics
  • Serial Year
    1999
  • Journal title
    Cancer Genetics and Cytogenetics
  • Record number

    1822099