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Identification of survivin as a promising target for the immunotherapy of adult B-cell acute lymphoblastic leukemia

  • Laura Freire Boullosa
    ,
  • Payalben Savaliya
    ,
  • Stephanie A. Bonney
    ,
  • Laurence Orchard
    ,
  • Hannah Wickenden
    ,
  • Cindy Lee
  • University of Antwerp
    ,
  • University of Hull
    ,
  • University of Bedfordshire
    ,
  • University of Southampton
    ,
  • University Hospital Southampton NHS Foundation Trust
    ,
  • University of Oxford
Research Output: Contribution to journal Article Peer-review

Open access

Abstract

B-cell acute lymphoblastic leukemia (B-ALL) is a rare heterogeneous disease characterized by a block in lymphoid differentiation and a rapid clonal expansion of immature, non-functioning B cells. Adult B-ALL patients have a poor prognosis with less than 50% chance of survival after five years and a high relapse rate after allogeneic haematopoietic stem cell transplantation. Novel treatment approaches are required to improve the outcome for patients and the identification of B-ALL specific antigens are essential for the development of targeted immunotherapeutic treatments. We examined twelve potential target antigens for the immunotherapy of adult B-ALL. RT-PCR indicated that only survivin and WT1 were expressed in B-ALL patient samples (7/11 and 6/11, respectively) but not normal donor control samples (0/8). Real-time quantitative (RQ)-PCR showed that survivin was the only antigen whose transcript exhibited significantly higher expression in the B-ALL samples (n = 10) compared with healthy controls (n = 4)(p = 0.015). Immunolabelling detected SSX2, SSX2IP, survivin and WT1 protein expression in all ten B-ALL samples examined, but survivin was not detectable in healthy volunteer samples. To determine whether these findings were supported by the analyses of a larger cohort of patient samples, we performed metadata analysis on an already published microarray dataset. We found that only survivin was significantly over-expressed in B-ALL patients (n = 215) compared to healthy B-cell controls (n = 12)(p = 0.013). We have shown that survivin is frequently transcribed and translated in adult B-ALL, but not healthy donor samples, suggesting this may be a promising target patient group for survivin-mediated immunotherapy.

Publication Information

Output type

Research Output: Contribution to journal Article Peer-review

Original language

English

Pages from-to (Number of pages)

Pages 3853-3866

Journal (Volume, Issue Number)

Oncotarget (Volume 9, Issue 3)

Publication milestones

  • Published - 17/12/2017

Publication status

Published - 17/12/2017

External Publication IDs

  • handle.net: 10547/623086
  • Scopus: 85040197983