Question regarding Mutually Exclusive Oncogenic Alterations - 1270638

I believe that's what it means when it happens in a lab but it hasn't been shown to work that way in real life. Let me have a faculty field this question.

Janine

Hi Tjv, I am not aware of any clinical evidence in lung cancer patients suggesting that having both EGFR mutations and Erbb2 (HER2) amplification prior to starting treatment has any effect on the eventual cause of acquired resistance after treatment. T790M is common (~50%) in patients with EGFR mutations (like L858R) who have developed resistance to drugs like Tarceva and afatinib, but T790M is very rare in treatment naive patients. Having Erbb2 amplification should not affect whether the tumor develops a secondary T790M mutation at some point after treatment, again at least as far as I am aware this hasn't been shown in patients.

If you have seen studies suggesting otherwise please feel free to post the references, I am happy to take a look!

Thanks Dr. Pennell! I'm afraid I was wrong in my statement, alluding to other research that doesn't apply here, and didn't check my understanding since we were waiting on your reply.

tjv87, very sorry for my confusion. So glad for our ability to check with our great faculty.

Janine

Thank you for posting the papers! Indeed HER2 amplification is probably one of the mechanisms for developing acquired resistance to EGFR inhibitors, and yes it would likely be mutually exclusive of T790M, but I do not think HER2 amplification in treatment naive patients would necessarily mean you would not develop T790M at some point.

HER2 amplifications in conjunction with EGFR mutations at diagnosis appear to be rare, but when the cancer becomes resistant to the EGFR inhibitor there are many ways the cancer can "get around" the EGFR inhibition. The most common way is the secondary mutation T790M, and if this is the mechanism then there probably won't be another one present as well most of the time (i.e. mutually exclusive). If there is no T790M, though, then something else is going on to cause resistance. In some cases, HER2 amplification could be the way the cancer becomes resistant to the EGFR inhibitor. In this case, the HER2 amplification was not present at diagnosis, only when resistance developed.

However, none of that suggests that if you DID happen to have HER2 amplification at diagnosis that you would necessarily be resistant to an EGFR inhibitor or that if the cancer eventually acquired resistance that it would have to be because of the HER2 amplification and not some other mechanism like T790M.

Does that make sense?

Yes I did see your tagline so your questions are very reasonable! I have had patients with both EGFR mutations and HER2 amplification at diagnosis who have responded to EGFR inhibitors, although for most of the time we have been using these drugs and testing for mutations we haven't routinely been looking for HER2 amplification so I think the outcomes for patients with this combination is not well known. I think you have a good grasp on the data for this situation, which is very little. I'm sorry there isn't more to convey!