Peng Peng1, Lihua Yu1, Xiaoju Yang1, Haiyan Zhou1, Yan Hu2, Taiping Chen2, Chengkon Shih1, Frank Wu1
1Biology, XuanZhu
Pharma, 2In Vivo Pharmacology,
Viva Biotech
Objective:Despite the improved patient care and the
declined mortality rate, gastric cancer is still a leading cause of cancer
deaths worldwide, particularly in Asia. Recent comprehensive molecular
characterization of gastric adenocarcinoma has not only revealed the molecular
mechanisms underlining the progression of gastric cancer, but also provided
aroadmap for personalized therapies. ErbB family is among the mostly-mutated
oncogenes in gastric adenocarcinoma. Pirotinib, a novel irreversible tyrosine
kinase inhibitor, has demonstrated highly effective anti-tumor activities
against mutations in EGFR, ErbB2, and ErbB3, suggesting its clinical value in
treatment of gastric cancer, potentially guided by genetic screening. Method:11 naïve Asian patient-derived xenograft (PDX) gastric adenocarcinoma
models were investigated using pirotinib. The tumor burden was established
subcutaneously in Balb/c nude mice. Once the mean tumor size reached
approximately 150mm3, pirotinib was orally administrated at 20mg/kg
once daily for 3 weeks. Routine monitoring to record the mobility, abnormal
activity, body weight, and tumor size was performed during the study. At the
end of the treatment, individual mouse was sacrificed and the tumor size was
measured, and the tumor growth inhibition (TGI) was calculated. Result: Among
the 11 PDXs tested, strong efficacy has been observed in 3 models with 76.3% to
80.3% TGI; approximately 50% TGI was seen in another 5 models. Conclusion: Pirotinib
demonstrated strong anti-tumor efficacy in the 11 PDX gastric
adenocarcinoma models. The next generation sequencing of the tumor tissues
was performed. Additional analysis might help reveal useful biomarkers that may
predict treatment sensitivity in patients in the ongoing clinical trial of
pirotinib.
Key
Words: Gastric cancer ErbB
Tyrosine kinase inhibitor
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