Comprehensive molecular characterization of salivary duct carcinoma reveals actionable targets and similarity to apocrine breast cancer Journal Article

   


Authors: Dalin, M. G.; Desrichard, A.; Katabi, N.; Makarov, V.; Walsh, L. A.; Lee, K. W.; Wang, Q.; Armenia, J.; West, L.; Dogan, S.; Wang, L.; Ramaswami, D.; Ho, A. L.; Ganly, I.; Solit, D. B.; Berger, M. F.; Schultz, N. D.; Reis-Filho, J. S.; Chan, T. A.; Morris, L. G. T.
Article Title: Comprehensive molecular characterization of salivary duct carcinoma reveals actionable targets and similarity to apocrine breast cancer
Abstract: Purpose: Salivary duct carcinoma (SDC) is an aggressive salivary malignancy, which is resistant to chemotherapy and has high mortality rates. We investigated the molecular landscape of SDC, focusing on genetic alterations and gene expression profiles. Experimental Design: We performed whole-exome sequencing, RNA sequencing, and immunohistochemical analyses in 16 SDC tumors and examined selected alterations via targeted sequencing of 410 genes in a second cohort of 15 SDCs. Results: SDCs harbored a higher mutational burden than many other salivary carcinomas (1.7 mutations/Mb). The most frequent genetic alterations were mutations in TP53 (55%), HRAS (23%), PIK3CA (23%), and amplification of ERBB2 (35%). Most (74%) tumors had alterations in either MAPK (BRAF/HRAS/NF1) genes or ERBB2. Potentially targetable alterations based on supportive clinical evidence were present in 61% of tumors. Androgen receptor (AR) was overexpressed in 75%; several potential resistance mechanisms to androgen deprivation therapy (ADT) were identified, including the AR-V7 splice variant (present in 50%, often at low ratios compared with full-length AR) and FOXA1 mutations (10%). Consensus clustering and pathway analyses in transcriptome data revealed striking similarities betweenSDCand molecular apocrine breast cancer. Conclusions: This study illuminates the landscape of genetic alterations and gene expression programs in SDC, identifying numerous molecular targets and potential determinants of response to AR antagonism. This has relevance for emerging clinical studies of ADT and other targeted therapies in SDC. The similarities between SDC and apocrine breast cancer indicate that clinical data in breast cancer may generate useful hypotheses for SDC. Clin Cancer Res; 22(18); 4623-33. ©2016 American Association for Cancer Research.
Journal Title: Clinical Cancer Research
Volume: 22
Issue: 18
ISSN: 1078-0432
Publisher: American Association for Cancer Research  
Date Published: 2016-09-15
Start Page: 4623
End Page: 4633
Language: English
DOI: 10.1158/1078-0432.ccr-16-0637
PROVIDER: scopus
PMCID: PMC5026550
PUBMED: 27103403
DOI/URL:

https://www.scopus.com/inward/record.uri?eid=2-s2.0-84990889264&partnerID=40&md5=a006c85e3ec7410d921ace3be55a3e20
Notes: Article -- Export Date: 2 November 2016 -- Source: Scopus
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MSK Authors
  1. Timothy Chan
    317 Chan
  2. David Solit
    732 Solit
  3. Nora Katabi
    284 Katabi
  4. Luc Morris
    250 Morris
  5. Snjezana Dogan
    174 Dogan
  6. Lu Wang
    147 Wang
  7. Alan Loh Ho
    211 Ho
  8. Ian Ganly
    398 Ganly
  9. Michael Forman Berger
    705 Berger
  10. Logan Alexander Walsh
    19 Walsh
  11. Nikolaus D Schultz
    433 Schultz
  12. Deepa Ramaswami
    5 Ramaswami
  13. Jorge Sergio Reis-Filho
    609 Reis-Filho
  14. Vladimir Makarov
    57 Makarov
  15. Alexis Desrichard
    19 Desrichard
  16. Lyndsay Shea West
    5 West
  17. Ken-Wing Lee
    8 Lee
  18. Qingguo Wang
    5 Wang
  19. Joshua Armenia
    55 Armenia
  20. Martin Gustav Dalin
    6 Dalin
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