Neoadjuvant HER-2–targeted breast cancer therapies less effective in patients with PIK3CA mutations

Daniel F. Hayes, MD

When we consider how tumor markers can be used to take care of patients, there are several important points to consider. First, we need to know that the assay that is used is highly validated and analytically validated. That means it’s accurate, it’s reproducible and it has a fairly narrow coefficient of variation. Second, we need to know that it has clinical validity, meaning it takes one population and splits it into two, and those populations are different in some way. The third point is that it offers clinical utility, meaning there are high levels of evidence that demonstrate that application of the marker test either improves patient outcomes, or that the outcomes are the same with lower costs, improved quality of life or less inconvenience. In other words: Is it really better for the patient to have this test done than not?

In this very nicely done study, the researchers have shown clinical validity of PIK3CA mutations in these patients. What they didn’t show — not because they didn’t understand this, but because the data didn’t support it — is that this information would in any way be useful right now to take care of patients who receive anti–HER-2 therapies. The combination of lapatinib and trastuzumab was better than either agent alone, regardless of whether patients were mutated or wild-type. Those with mutations were less likely to respond to any of the three, but the difference in prognosis was not to the extent that I would treat these patients differently.

One of the things I have learned through the years about tumor biomarkers is that, in oncology, we really don’t use them to decide who we should treat. Rather, we typically use them to decide who we should not treat. The findings in this study don’t tell me there is one group of patients who shouldn’t have received the combination vs. single-agent treatment. Patients whose cancers had the PIK3CA mutations were less likely to respond to any of the three regimens, but nothing here tells me I should withhold lapatinib or trastuzumab just because a patient’s cancer has the mutation, because there is still a chance they will respond.

Finally, the 600-pound gorilla in the room is the ALTTO study presented at last year’s ASCO Annual Meeting (Piccart-Gebhart MJ. Abstract #LBA4. Presented at: ASCO Annual Meeting; May 30-June 3, 2014; Chicago). Everyone thought ALTTO would confirm what we “knew” — that the addition of lapatinib to trastuzumab as adjuvant treatment of early-stage, HER-2–positive breast cancer would improve outcomes. But that wasn’t the case.

Do these data from the NEO-ALTTO study justify re-evaluating the ALTTO samples to see if you can “save” the combination vs. single-agent trastuzumab by identifying a group of people who would actually benefit? Those are precious samples and you want to use them for your best bet. Is this the “best bet” or are there other markers that can be evaluated with those samples that might have a better chance of identifying patients who would benefit from the combination? I’m not sure, but I am certain the investigators who led ALTTO will think very carefully about what analyses should be done using these specimens. These deliberations will be done thoughtfully, and I believe there is a possibility we will, indeed, find a subgroup that appears to have benefited from the combination. Until we do, we all need to scratch our heads over the discordance between the neo-adjuvant studies that suggest the combination of trastuzumab and lapatinib is superior to single agent trastuzumab, and the overall results of ALTTO.