Yelena Y. Janjigian, MD
There is a great need for novel treatments for patients with HER2-positive gastric/gastroesophageal junction (GEJ) adenocarcinomas, a patient population that makes up approximately 30% of those with the disease, says Yelena Y. Janjigian, MD, a medical oncologist at Memorial Sloan Kettering Cancer Center. OncLive
: What did we learn from the phase III LOGiC trial? Is there an understanding as to why lapatinib failed to show a survival benefit?
: Based on the trial results, as they stand right now without any additional sequencing data or biomarker results, we clearly do not have a reason why lapatinib failed both in the first- and second-line setting. Based on my experience, I think we need to look at lapatinib as a drug, the trial design, and HER2 as a target in gastric cancer, in order to understand why it failed.
Finally, what it comes down to is that lapatinib may not be sufficient for HER2 inhibition in gastric cancer. We may just need a stronger HER2 inhibitor or HER2 inhibition with other targeted agents or chemotherapy. Gastric cancer is not only HER2 driven, even in HER2 disease.
HER2 amplification by FISH was selected as a biomarker for the LOGiC trial, regardless of HER2 IHC analysis. What questions remain regarding the use of HER2 as a driver for HER2-targeted therapies?
The question everyone asks is, “Would a second study in a population that had high level of HER2 amplification be worthwhile with lapatinib?” I think the answer is, “No.”
We know enough from looking at this disease that lapatinib is probably not going to be sufficient by itself. I wouldn’t subject another 300 patients to chemotherapy plus lapatinib, even in a highly HER2-amplified population. This is because, in my experience and now emerging data suggest, combination therapies are needed. We need to look at combinations of HER2-directed agents, HER2 agents with VEGF inhibitors, and HER2 agents with PD-1 inhibitors.
That is the wave of the future. We’ve got to go forward instead of trying to correct the mistakes we’ve made in trial design and not subject another patient population to a potentially small benefit or a negative trial.
Are any ongoing trials looking at VEGF inhibition in this patient population?
There was a small phase II trial looking at FOLFOX plus bevacizumab (Avastin) and trastuzumab in first-line. That trial, even though there were only data on 35 patients reported, was unprecedented compared to historic control in response rate, OS, and PFS in that patient population.
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