Cancers (Jul 2021)

Clinically Advanced Pheochromocytomas and Paragangliomas: A Comprehensive Genomic Profiling Study

  • Gennady Bratslavsky,
  • Ethan S. Sokol,
  • Michael Daneshvar,
  • Andrea Necchi,
  • Oleg Shapiro,
  • Joseph Jacob,
  • Nick Liu,
  • Tom S. Sanford,
  • Ruben Pinkhasov,
  • Hanan Goldberg,
  • Jonathan K. Killian,
  • Shakti Ramkissoon,
  • Eric A. Severson,
  • Richard S. P. Huang,
  • Natalie Danziger,
  • Mehdi Mollapour,
  • Jeffrey S. Ross,
  • Karel Pacak

DOI
https://doi.org/10.3390/cancers13133312
Journal volume & issue
Vol. 13, no. 13
p. 3312

Abstract

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Patients with clinically advanced paragangliomas (CA-Para) and pheochromocytomas (CA-Pheo) have limited surgical or systemic treatments. We used comprehensive genomic profiling (CGP) to compare genomic alterations (GA) in CA-Para and CA-Pheo to identify potential therapeutic targets. Eighty-three CA-Para and 45 CA-Pheo underwent hybrid-capture-based CGP using a targeted panel of 324 genes. Tumor mutational burden (TMB) and microsatellite instability (MSI) were determined. The GA/tumor frequencies were low for both tumor types (1.9 GA/tumor for CA-Para, 2.3 GA/tumor for CA-Pheo). The most frequent potentially targetable GA in CA-Para were in FGFR1 (7%, primarily amplifications), NF1, PTEN, NF2, and CDK4 (all 2%) and for CA-Pheo in RET (9%, primarily fusions), NF1 (11%) and FGFR1 (7%). Germline mutations in known cancer predisposition genes were predicted in 13 (30%) of CA-Pheo and 38 (45%) of CA-Para cases, predominantly involving SDHA/B genes. Both CA-Para and CA-Para had low median TMB, low PD-L1 expression levels and none had MSI high status. While similar GA frequency is seen in both CA-Para and CA-Para, germline GA were seen more frequently in CA-Para. Low PD-L1 expression levels and no MSI high status argue against strong potential for novel immune checkpoint inhibitors. However, several important potential therapeutic targets in both CA-Para and CA-Para are identified using CGP.

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