Genome Medicine (Oct 2016)

Molecular profiling of advanced solid tumors and patient outcomes with genotype-matched clinical trials: the Princess Margaret IMPACT/COMPACT trial

  • Tracy L. Stockley,
  • Amit M. Oza,
  • Hal K. Berman,
  • Natasha B. Leighl,
  • Jennifer J. Knox,
  • Frances A. Shepherd,
  • Eric X. Chen,
  • Monika K. Krzyzanowska,
  • Neesha Dhani,
  • Anthony M. Joshua,
  • Ming-Sound Tsao,
  • Stefano Serra,
  • Blaise Clarke,
  • Michael H. Roehrl,
  • Tong Zhang,
  • Mahadeo A. Sukhai,
  • Nadia Califaretti,
  • Mateya Trinkaus,
  • Patricia Shaw,
  • Theodorus van der Kwast,
  • Lisa Wang,
  • Carl Virtanen,
  • Raymond H. Kim,
  • Albiruni R. A. Razak,
  • Aaron R. Hansen,
  • Celeste Yu,
  • Trevor J. Pugh,
  • Suzanne Kamel-Reid,
  • Lillian L. Siu,
  • Philippe L. Bedard

DOI
https://doi.org/10.1186/s13073-016-0364-2
Journal volume & issue
Vol. 8, no. 1
pp. 1 – 12

Abstract

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Abstract Background The clinical utility of molecular profiling of tumor tissue to guide treatment of patients with advanced solid tumors is unknown. Our objectives were to evaluate the frequency of genomic alterations, clinical “actionability” of somatic variants, enrollment in mutation-targeted or other clinical trials, and outcome of molecular profiling for advanced solid tumor patients at the Princess Margaret Cancer Centre (PM). Methods Patients with advanced solid tumors aged ≥18 years, good performance status, and archival tumor tissue available were prospectively consented. DNA from archival formalin-fixed paraffin-embedded tumor tissue was tested using a MALDI-TOF MS hotspot panel or a targeted next generation sequencing (NGS) panel. Somatic variants were classified according to clinical actionability and an annotated report included in the electronic medical record. Oncologists were provided with summary tables of their patients’ molecular profiling results and available mutation-specific clinical trials. Enrolment in genotype-matched versus genotype-unmatched clinical trials following release of profiling results and response by RECIST v1.1 criteria were evaluated. Results From March 2012 to July 2014, 1893 patients were enrolled and 1640 tested. After a median follow-up of 18 months, 245 patients (15 %) who were tested were subsequently treated on 277 therapeutic clinical trials, including 84 patients (5 %) on 89 genotype-matched trials. The overall response rate was higher in patients treated on genotype-matched trials (19 %) compared with genotype-unmatched trials (9 %; p < 0.026). In a multi-variable model, trial matching by genotype (p = 0.021) and female gender (p = 0.034) were the only factors associated with increased likelihood of treatment response. Conclusions Few advanced solid tumor patients enrolled in a prospective institutional molecular profiling trial were treated subsequently on genotype-matched therapeutic trials. In this non-randomized comparison, genotype-enrichment of early phase clinical trials was associated with an increased objective tumor response rate. Trial registration NCT01505400 (date of registration 4 January 2012).

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