Dynamic Changes in the Copy Number of Pluripotency and Cell Proliferation Genes in Human ES and iPS Cells during Reprogramming and Time in Culture

نویسندگان

  • Louise C. Laurent
  • Igor Ulitsky
  • Ileana Slavin
  • Ha Tran
  • Andrew Schork
  • Robert Morey
  • Candace Lynch
  • Julie V. Harness
  • Sunray Lee
  • Maria J. Barrero
  • Sherman Ku
  • Marina Martynova
  • Ruslan Semechkin
  • Vasiliy Galat
  • Joel Gottesfeld
  • Juan Carlos Izpisua Belmonte
  • Chuck Murry
  • Hans S. Keirstead
  • Hyun-Sook Park
  • Uli Schmidt
  • Andrew L. Laslett
  • Franz-Josef Muller
  • Caroline M. Nievergelt
  • Ron Shamir
  • Jeanne F. Loring
چکیده

Genomic stability is critical for the clinical use of human embryonic and induced pluripotent stem cells. We performed high resolution SNP (single nucleotide polymorphism) analysis on 186 pluripotent and 119 non-pluripotent samples. We report a higher frequency of subchromosomal copy number variations in pluripotent samples compared to non-pluripotent samples, with variations enriched in specific genomic regions. The distribution of these variations differed between hESCs and hiPSCs, characterized by large numbers of duplications found in a few hESC samples and moderate numbers of deletions distributed across many hiPSC samples. For hiPSCs, the reprogramming process was associated with deletions of tumor suppressor genes, while time in culture was associated with duplications of oncogenic genes. We also observed duplications that arose during a differentiation protocol. Our results illustrate the dynamic nature of genomic abnormalities in pluripotent stem cells and the need for frequent genomic monitoring to assure phenotypic stability and clinical safety.

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تاریخ انتشار 2011