Genomic testing for stage IV

Moth, Thanks for starting this thread!

These tests are here to stay and probably will be routinely used at progression to check for a newly-acquired ESR1 mutation, for example, or for other mutants associated with progression. It's helpful to know what the tests do and do not look for, Foundation One is looking at mutants, not at loss or gain of protein expression. I spoke with my MO today, who said the Foundation One test does not routinely detect PI3KCA mutations (why not?) and those usually need tissue biopsy.

I'm not sure if any particular result is "good" or "bad" so much as having the information helps us better understand know what we are dealing with. The issue of TMB and MSI, for example. TMB greater than ten is a ticket to immunotherapy, so that's great, but if you don't have that then you can try to work around it by adding in a DNA damage drug. Another issue is the tumor microenvironment (immunological phenotype) and there again, either you have high infiltrating T cells or you don't. If you do, that's great, but if you don't you can try to fix that- for example, this paper shows that Aurora Kinase A inhibitors can increase the infiltrating T cell numbers, and so one might need to take that drug if the tumor is "cold"

https://advances.sciencemag.org/content/7/4/eabd78...

In pre-clinical work, inhibitors of CDK12 were also really good at increasing tumor-infiltrating T cells. Apparently the requirement for IO response is that the tumor has to have high mutations and the environment needs to allow access to T cells.

Hi. Interesting topic. I had just asked for a copy of my foundation one results. I took it back in 8/2020. It says specimen type FFPE-block-bone. But I do remember them also taking blood. Here is what it said. It's 26 pages long but I think this is the sum of it all.

I don’t know what any of this means. I need to ask onc next time I see him.

Hi I has DMTN1 mutation in liquid biopsy, I have read Cure-ious that you had it as well. Do you think it is something affected the blood cells by CDK4-6? I mean may be this mutation is in neutrophils not in cfDNA from tumor?. It is written there that it has something with blood cancers or aging. I am 46, so not that old

Phet,

I think these genetics tests are so new, we will be a kind of trial group that finds out if they are consistent from time to time. I do wonder if I had another tesr right now, would these same mutations show up, or another four "maybe something" mutations would be there. I think the CHEK2 mutation might recurr because it is a moderate-risk factor for getting breast cancer, and mine showed up at 48 and had clearly been growing there for quite awhile. Your question about mRNA amplification, by that you mean protein expression levels as opposed to DNA amplifications?

Figtree, Well, that's weird and wonderful to lose two more aggressive cancer mutations in the more recent blood test, but then also calls to question how reliable are these tests anyway?! But still new, so definitely the newer test is better.

And like you say, most important that both of them picked up loss of CDK12- at least it is consistent! I will be back shortly with a link to the trial, anyone with a CDK12 mutation is eligible for immunotherapy, it causes a huge increase in T cells infiltrating the tumor. The studies started out with pre-clinical trial data on prostate cancer, and then they looked and saw the small number of prostate cancer patients who did respond to immunotherapy were ones that had CDK12 mutation. That started a clinical trial for anyone with any solid tumor having a CDK12 mutation, and I wonder if there are now updates. Whether the mutation is by itself sufficient to confer response or you still want a combo trial is also a relevant question- back shortly..

I had a STRATA test on a bone biopsy. It showed an amplification of CCND1- UCSF says no known treatment for this. I am MS Stable, TB low and PD-L1 low with a score of 18. The Strata immune signature is low. I do not have ESR1 or PIK3CA. there were some additional mutations - the only only being studied per UCSF right now is my ARID1A and it is not being studied in breast cancer. I have 2 MAPs and NF1 (which I think is in all lobular cancers). There were a few that couldn't be assessed due to "quality control parameters"

The CCND1 is present in 13% of cancers- along with breast it is Esophageal and prostate.

I am also Her 2 low from my original breast biopsy 2+ with negative FISH which makes Enhertu a possibility at some point.

does anyone one knowwhy i can’t post links ??

I found this is a very helpful site to search clinical trials based on any bio markers.

Mycancergenome.org

Wondering if anyone out there has the combination of ESR1 amplification, NSD3 amplification and FGFR1 amplification? I've been doing some reading around and apparently ESR1 and NSD3 are almost always amplified together (as they are in me), meanwhile NSD3 and FGFR1 come from the same part of the chromosome and are thus also related. Also this amplification signature is seen mostly (almost always?) in highly ER+ cancers that are nonetheless endocrine resistant. These three all came up in my liquid biopsy and I'm curious as, at least according to biopsy of my mediastinal nodes, my mets are TNBC (but I was originally highly ER+). As it was a liquid biopsy this might suggest there's an ER+ tumour in there shedding dead cancer cells? Those cells couldn't from my primary could they (removed in August 2019)?

I know there's a far bit of research on ESR1 mutations but much less on ESR1 amplification, which despite seeming like it would make cancer extra responsive to estrogen suppression apparently does the opposite and helps make the tumours grow independently of estrogen itself.

Also wondering - how might I find out how many copy numbers are involved in my amplifications? Would I contact Foundation One? I have a lot of amplifications and wondering if some are more amplified than others (to help work out what might be driving things)

Here is a Nature paper from 2019: https://www.nature.com/articles/s41586-019-1007-8showing that just four of the 11 IntClust breast cancer subtypes are most likely to lead to a late (greater than five years) recurrences for ER-positive tumors. So perhaps most of us will sort in one of these four categories:

"Among ER-positive patients, those with IntClust3, IntClust7, IntClust8 and IntClust4ER⁺ subtypes exhibited a better prognosis, whereas patients with IntClust1, IntClust2, IntClust6 and IntClust9 subtypes exhibited late-recurring cancer with distant relapse up to 20 years after diagnosis. The IntClus1,2,6, and 9 subtypes together account for around one quarter of all ER-positive tumours and the vast majority of late recurrences. Importantly, the four 'high risk of relapse' subgroups were enriched in characteristic genomic-copy-number alterations, which represent the likely drivers of each subgroup."

IntClust2 tumours (4.5% of ER-positive cases) are defined by amplification and concomitant overexpression of multiple oncogenes on chromosome 11q13, including CCND1, FGF3, EMSY, PAK1 and RSF1. Approximately 96% of IntClust2 have the RSF1 amplification, compared with 0–22% in other subgroups.

IntClust6 (5.5% of ER-positive tumours) is characterized by focal amplification of ZNF703 and FGFR1 on chromosome 8p12 (100% of IntClust6 cases, versus 2–21% of others).

IntClust1 (8% of ER-positive tumours) exhibited amplification of chromosome 17q23 in a region spanning the mTOR effector RPS6KB1 (also known as S6K1), which was gained or amplified in 96% and 70% of cases, respectively (versus amplification in 0–25% of other subtypes).

IntClust9 (8% of ER-positive cases) was characterized by amplification of the MYC oncogene at chromosome 8q24, with amplification in 89% of these tumours (versus 3–42% of other groups).

"Thus the late-recurring ER-positive subgroups are defined by genomic drivers, several of which are viable therapeutic targets."

Thank you Cure-ious! That's really useful. Yes I also wonder whether, with FGFR1 in the mix, it would be dependent on ER at all (I've also switched in at least some of my tumor to TNBC, despite this continuance of ER+ gene mutations).

I've tried before to work out what IntClust I am, but as I only had genomic testing on the metastasis and not the primary, and was ER+ at primary and TNBC at spread, I can't get my head around it. If you switch ER+ to TNBC do you also switch clusters? I have a hunch my primary might have been IntClust 6, assuming the NSD3 and FGFR1 were there in the primary (the 8p11.23 amplicon). That would explain relapse, though mine was rapid not late stage I had no lymph spread and no LVI at primary, so I clearly have a very biologically aggressive tumor to have spread anyway. I've also read that IntClust 6 is highly genomically unstable which would make sense given I switched types and also have quite a lot of mutations/amplifications.

Buttonsmachine - very interesting you were able to find out your IntClust. Did they give you any more info about 6? I think you have FGFR1 too, is that right? Are there other mutations you have that characterise this cluster?

Oh, you guys. I'm sitting ere crying because I don't understand any of this. I doubt my ONC goes either. He's just a cancer doctor not a breast cancer doctor.

Is this how the normal visits occur for you? (He's always an hour late even though I've called him on it) When he enters the room, he as no idea what current bloodwork is, what latest scans reports or anything. He spends half my visit reading to catch up.

Last time I was in there h e was telling my son my history and said cancer had mildly proceeded on my breast. I said, mildly? I told my son to leave the room so I could undress and show him the cancer was all over the top of my breast, underneath to my ribs and there were two holes boring thru my breast, not to mention my right side.

He seemed mortified. "why did I not know about this? He started rustling papers. BUT, hr did know, last visit I had showed him and said this was moving fast. He left me with no hope that day. He said the only chemo I can offer you is Haveline, then there's nothing. Th other chemos are too harsh for you.

So, I feel abandoned

Snooky, is your cancer breaking through your skin? That often does not show up on imaging like PET/CTs, which is probably why your MO was surprised by it - not that I am defending him - he should have seen it before now. Doesn't he examine you regularly? Did he forget what he saw?

I have some lesions under my skin that I think will break through one of these days. They seem to grow despite chemo. I think the chemo just doesn't reach them. :-(

I haven't been on Haveline so I cannot say how that is, but maybe it is worth a try for you? I'm so sorry you are going through this. This disease can be so discouraging to say the least.