PLoS ONE (Jan 2011)

MicroRNA expression characterizes oligometastasis(es).

  • Yves A Lussier,
  • H Rosie Xing,
  • Joseph K Salama,
  • Nikolai N Khodarev,
  • Yong Huang,
  • Qingbei Zhang,
  • Sajid A Khan,
  • Xinan Yang,
  • Michael D Hasselle,
  • Thomas E Darga,
  • Renuka Malik,
  • Hanli Fan,
  • Samantha Perakis,
  • Matthew Filippo,
  • Kimberly Corbin,
  • Younghee Lee,
  • Mitchell C Posner,
  • Steven J Chmura,
  • Samuel Hellman,
  • Ralph R Weichselbaum

DOI
https://doi.org/10.1371/journal.pone.0028650
Journal volume & issue
Vol. 6, no. 12
p. e28650

Abstract

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Cancer staging and treatment presumes a division into localized or metastatic disease. We proposed an intermediate state defined by ≤ 5 cumulative metastasis(es), termed oligometastases. In contrast to widespread polymetastases, oligometastatic patients may benefit from metastasis-directed local treatments. However, many patients who initially present with oligometastases progress to polymetastases. Predictors of progression could improve patient selection for metastasis-directed therapy.Here, we identified patterns of microRNA expression of tumor samples from oligometastatic patients treated with high-dose radiotherapy.Patients who failed to develop polymetastases are characterized by unique prioritized features of a microRNA classifier that includes the microRNA-200 family. We created an oligometastatic-polymetastatic xenograft model in which the patient-derived microRNAs discriminated between the two metastatic outcomes. MicroRNA-200c enhancement in an oligometastatic cell line resulted in polymetastatic progression.These results demonstrate a biological basis for oligometastases and a potential for using microRNA expression to identify patients most likely to remain oligometastatic after metastasis-directed treatment.