Frontiers in Oncology (Mar 2023)

Case report: A de novo ERBB3 mutation develops in a gallbladder cancer patient carrying BRCA1 mutation after effective treatment with olaparib

  • Jing-Xiao Yang,
  • Zi-Yao Jia,
  • Fa-Tao Liu,
  • Wen-Guang Wu,
  • Xue-Chuan Li,
  • Xue-Chuan Li,
  • Xue-Chuan Li,
  • Lu Zou,
  • Lu Zou,
  • Lu Zou,
  • Huai-Feng Li,
  • Huai-Feng Li,
  • Huai-Feng Li,
  • Fei Zhang,
  • Fei Zhang,
  • Fei Zhang,
  • Run-Fa Bao,
  • Run-Fa Bao,
  • Run-Fa Bao,
  • Shu-You Peng,
  • Wan Yee Lau,
  • Yun Liu,
  • Mao-Lan Li,
  • Ying-Bin Liu,
  • Ying-Bin Liu,
  • Ying-Bin Liu

DOI
https://doi.org/10.3389/fonc.2023.1078388
Journal volume & issue
Vol. 13

Abstract

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BackgroundGallbladder cancer (GBC) is highly lethal and resistant to most chemotherapeutic drugs. GBC was reported to carry multiple genetic mutations such as TP53, K-RAS, and ERBB2/3. Here, we unexpectedly identified a patient with GBC harboring germline BRCA1 p.Arg1325Lys heterozygous mutation. We sought to determine if olaparib, the poly ADP-ribose polymerase inhibitor (PARPi) commonly treated for BRCA mutation, can inhibit cancer development via a therapeutic trial on this patient.Case presentationThe patient received GBC R0 resection after an 8-week olaparib treatment. After surgery and 6-month follow-up treatment with olaparib, the patient’s blood carbohydrate antigen 19-9 (CA19-9) level declined from 328 to 23.6 U/ml. No recurrence in CT scanning was observed, indicating a disease-free survival of 6 months with conventional therapy. Two months later, CT examination and CA19-9 level showed cancer relapse. A blood biopsy revealed a new ERBB3 p.Gly337Arg mutation. GBC cell lines ectopically expressing BRCA1 p.Arg1325Lys together with ERBB3 p.Gly337Arg mutations were challenged with olaparib and/or afatinib, an ERBB2/3 inhibitor. The dual mutation cells were more responsive to the combined olaparib with afatinib than a single drug in the cell proliferation assay.ConclusionOlaparib is effective in a GBC patient with a BRAC1 mutation. The efficacy of olaparib and afatinib in both cultured BRAC1 and ERBB3 mutation cell lines suggests that a combined regimen targeting BRCA1/2 and ERBB2/3 mutations may be an optimal strategy to treat GBC patients who carry both gene mutations.

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