Induction of angiogenesis by normal and malignant plasma cells.

نویسندگان

  • Dirk Hose
  • Jérôme Moreaux
  • Tobias Meissner
  • Anja Seckinger
  • Hartmut Goldschmidt
  • Axel Benner
  • Karène Mahtouk
  • Jens Hillengass
  • Thierry Rème
  • John De Vos
  • Michael Hundemer
  • Maud Condomines
  • Uta Bertsch
  • Jean-François Rossi
  • Anna Jauch
  • Bernard Klein
  • Thomas Möhler
چکیده

Abundant bone marrow angiogenesis is present in almost all myeloma patients requiring therapy and correlated to treatment response and survival. We assessed the expression of 402 angiogenesis-associated genes by Affymetrix DNA microarrays in 466 samples, including CD138-purified myeloma cells (MMCs) from 300 previously untreated patients, in vivo microcirculation by dynamic contrast-enhanced magnetic resonance imaging, and in vitro angiogenesis (AngioKit-assay). Normal bone marrow plasma cells (BMPCs) express a median of 39 proangiogenic (eg, VEGFA, ADM, IGF-1) and 28 antiangiogenic genes (eg, TIMP1, TIMP2). Supernatants of BMPCs unlike those of memory B cells induce angiogenesis in vitro. MMCs do not show a significantly higher median number of expressed proangiogenic (45) or antiangiogenic (31) genes, but 97% of MMC samples aberrantly express at least one of the angiogenic factors HGF, IL-15, ANG, APRIL, CTGF, or TGFA. Supernatants of MMCs and human myeloma cell lines induce significantly higher in vitro angiogenesis compared with BMPCs. In conclusion, BMPCs express a surplus of proangiogenic over antiangiogenic genes transmitting to the ability to induce in vitro angiogenesis. Aberrant expression of proangiogenic and down-regulation of antiangiogenic genes by MMCs further increases the angiogenic stimulus, together leading to bone marrow angiogenesis at various degrees in all myeloma patients.

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عنوان ژورنال:
  • Blood

دوره 114 1  شماره 

صفحات  -

تاریخ انتشار 2009