No chemo for low Mammaprint?

I had an oncotype of 20, and a low mammaprint score. and I'm going with the mammaprint. The new studies show Mammaprint is a good predictor of who needs chemo and chemo would have only helped 3% anyway. I'm younger, I just turned 41 when diagnosed and my doc said she would never push for chemo for a Onco 20 with stage 1A and good margins. I had a BMX and am on Tamoxifen.

EXACTLY - my doctor(s) weren't giving the mammoprint as much credibility at the time. I'm thrilled to see that things have progressed in the short time since I have been diagnosed!!!!

My oncatype score came back as 19, my first MO recommends chemo, I went for a 2nd opinion and he sent for mammaprint test. I am waiting for the results. I am 52, post menopause, would be a good idea to base chemo treatment based on the mammaprint, low - no chemo and high - get chemo? I am not sure what to do, any suggestions would help. I am ER+, PR+, Her2-, lymph nodes were negative.

I'm going to jump in here because I have questions. Thank God for BC.org or I'd be in real trouble through this exciting journey! I need advice from experienced BC team members. Thanks in advance.

Okay, I got Oncotype results yesterday. Score: 14. I realize this is in the low range, but I guess I was thinking, if I get 10 or below (like the TailorX study which placed low at 10 and below) I'll know NO chemo without question. I don't want chemo, but I want to make the best decision with what I consider the most important time to make it. I think my only true other risk factors are age (49), 1.8cm tumor and family history. Genetics clean, nodes clean (they only got 2) and clear margins. 2.3cm, which was initially a worry because it backed up to the chest wall. No radiation called for. I got BMX.

So -- just to make damn sure I'm making the right call, I've asked my MO for Mammoprint. I'm fine if I have to shell out for it. Though I have good insurance. Why not, I ask? I guess I'm one who overloads on info -- but give me the info. She was not thrilled but agreed she could maybe make it happen "but not sure how". Huh? She's at MD Anderson!!! And what also bugs me is: (1) she said the latest study with Mammoprint is "flawed" -- Mindact -- and she said if she got a result in the mid range (18-30) she would not run Mammoprint for that patient. She's very nice, but I feel I may be switching to a local MO -- one I do not have to fly to see -- because this MO is going so by the book, and I feel it's a totally standard book. She was also strictly on the tamoxifen train, too, without even considering the option of ovarian oblation and AIs. I'm actually okay trying tamox but was already assumed to be in perimen. a couple of years ago. I went to MDA and a teaching institution for more robust discussions about what is on the horizon and ways to treat. I got great surgery, btw, and LOVE my BS and PS team.

Would you guys get a Mammoprint run with a 14? Am I crazy to push? I've gotten a rec. for a local MO and look like I'm going to change but I'm happy to have the MDA MO run Mammoprint if she will. If not, I'll ask the new MO. I don't feel I am going to do chemo but want to feel sure of this decision. Is it okay if I don't start tamox. for another month or so? My surgery was 2/27.

THANKS!!!! I need advice as you can see.

also, you can start tamoxifen immediately and always stop if you need to do chemo.

Hi EastcoastTS:

In considering whether you should push for the MammaPrint test, you may wish to ask your Medical Oncologist for advice about your "Clinical risk classification" according to MINDACT trial criteria. Then ask her to explain the two possible outcomes of the MammaPrint test with your Clinical risk classification, as well as how the test results may or may not better inform your decision-making in light of available clinical trial data.

For example, a person who is deemed to be "Clinical Low Risk" under MINDACT criteria, would either be found to be in either the (a) or (c) groups per my post above:

(a) Clinical Low / Genomic (MammaPrint) Low;

or

(c) Clinical Low / Genomic (MammaPrint) High <===== "discordant"

What would be the medical advice in case of each of these outcomes? Would it impact advice regarding chemotherapy in your particular case, in light of all applicable factors? Please explain.

By the way, regarding Oncotype, with ILC, "high risk" Recurrence Scores are not very common. See e.g.,

http://www.clinical-breast-cancer.com/article/S1526-8209(15)00168-8/pdf

Also, you may be interested in the references in this postregarding Aromatase Inhibitors in ILC:

https://community.breastcancer.org/forum/96/topics/849708?page=1#post_4903818

BarredOwl

Hey, guys --

Thanks for all responses!

BarredOwl, you're so famous on BC.org, I was hoping you would respond!!!

Okay, update somewhat. When I mentioned MindAct to my MO, she was very adamant that MindAct is "flawed" -- she did not explain why. She was also opposed to running Mammaprint and said "MD Anderson does not use it", which I find hard to believe. So I'm flying by the seat of my pants a bit, but I asked for it (and said I would pay if insurance does not) and they have agreed. Basically to appease me I feel. At least I'll have the score. I'm not in panic mode at all; I simply want data to base my decision(s) upon. Truth be told, I'm not going to get any more info on MindAct or Mamma much from this MO. I'll get the score and little else I bet. Also, again, I'm disappointed that this is my MO response from a leading institution. Had hoped for a more robust discussion regarding everything in my future. I did ask her about my overall "clinical risk" (not based on any trial because I did not know how to pose that in this manner) and she said: low. Which I'd already kinda figured out myself from path, etc.

I will take all results to my local MO when I have them, whom I've yet to meet. Arranging this as 2nd opinion, not just for chemo but Tamoxifen discussion (since I'm in perimena and fairly close to mena. perhaps.) I am not opposed to Tamoxifen actually at all but just want to discuss my options. I don't know why some doctors do not seem to want to do that. I have researched a lot; some don't seem to want informed patients. I'm being very nice -- but firm -- about my treatment decisions. Like, who else is going to champion for me? Well, ME!!!

What a fun merry-go-round we find ourselves on!!! It's lucky I like parsing through data. Good grief.

Hi EastcoastTS:

If you enjoy parsing data, then you should find Cardoso, its Supplementary Appendix, and the Hunter Perspective linked above, to be of great interest.

I note that these types of biomarker tests provide prognostic information about recurrence risk based on clinical studies comparing outcomes between groups of patients. The recurrence risk information associated with a particular test result (e.g., Oncotype Recurrence Score; Clinical risk-Genomic risk classification by MammaPrint) is statistical in nature, and cannot predict outcome at the individual patient level. Because of this, while certainty is not possible, you should have enough information to help you reach an informed decision.

It is unfortunate that your MO did not explain the basis for her opinion that the MINDACT trial was "flawed" or provide you with a reasoned explanation for why she did not recommend the test in your specific case. Like all clinical trials, MINDACT was subject to certain practical constraints, and the trial design resulted in some findings at five years that are less definitive for certain clinical endpoints / subgroups than one might wish. For example, in one feature, Dr. Lee Schwartzberg, MD, FACP, commented:

"Additionally, the lack of conclusive guidance in the clinical-low/genomic-high group, in whom decision-making would be aided by a definitive result as to adding chemotherapy or not, makes the judgment to order the 70-gene assay in the clinic still a difficult one."

For those receiving the test, to understand how the MINDACT results apply in the individual case, the clinical risk categorization should be made using the same criteria used in the MINDACT trial. Your second opinion Medical Oncologist should be able to advise you in this regard.

BarredOwl