In the article I read last night and posted, Tamoxifen did not have the same effect in creating the mutation. That makes obvious sense in that Tam doesn't eliminate estrogen. Of course, Tam has its own evil side that rears its head in the form of other cancers. Grrrr

Weareconnected

Association does not imply causation and is one of the greatest issues in interpreting trials.

I believe your confusion is over the temporal relationship of the events you are describing.

Simply put

- over the years the 'dormant' (concept still tricky to describe in full for scientists) acquire hormonal resistance - they escape

- they have now acquired higher metastatic potential

- you are quite correct if you have the mutation - you have greater metastatic potential - and you will probably do worse

In my knowledge of this what has not been elucidated is:

- is the mutation a direct result of prolonged AI use?

- what would be the prognosis in the same pool of cancer patients ( ie the one who do worse and develop endocrine resistance) if they did not use AIs

Thanks for posting above - good topic.

If you have data on those questions - would be very interested.

Hello ChiSandy,

Thank you.

You probable know this work

https://www.researchgate.net/post/How_can_I_choose_between_Aromatase_inhibitors_in_postmenopausal_hormone_positive_breast_cancer

http://www.thelancet.com/journals/lanonc/article/P...(17)30081-5/abstract

Price and country preference aside - my question is if one uses Letrozole as the first choice ( let's not call it a line:)) in early disease at high risk does that have implications for its further use should one have to deal with Stage 4.

Wildplaces, that's a good question. I'm not sure about how use early in treatment would affect later use of letrozole but I suspect that it might be possible to use it in tandem with another drug such as Ibrance if one experienced a distant recurrence. Or one might be switched to faslodex, then later back to letrozole. I'm sure some of the Stage IV women have a much, much better understanding of the strategies. I may raise the question with my MO the next time I see her.

Lilac Blue, are you saying that most of the newer drugs for secondary cancer are off the NICE list until they come down in price (if ever)? (I've always thought the 'NICE' acronym had a touch of New Speak about it.)

Well, although most patients are started out according to the “party line” on either anastrazole or letrozole (and though letrozole is given to those with diverse BMIs, I’ve not yet encountered—either in real life or on these boards—obese women started out on anastrazole or exemestane. And there is some individualization, in that patients’ tolerance or intolerance to a particular AI’s SEs often leads to switching, at least temporarily. I’ve also not seen anastrazole as the AI of choice for ER+ Stage IV, though some ER+ Stage IV patients get a combo of exemestane & everolimus (Aromasin & Afinitor). I guess the difference may be in the organ in which mets are first detected. AFAIK, using letrozole in early-stage disease doesn’t preclude its use in Stage IV patients—in the latter it’s usually given in combination with newer drugs like Ibrance (and if the mets are to bone, monthly Xgeva shots are given instead of biennial Prolia or a bisphosphonate). Letrozole may have the advantage of being both initial therapy and one of the “big guns” trotted out when the cancer spreads. (AI resistance—more correctly, tumor cell mutation to become estrogen-independent or able to synthesize its own estrogen—does not seem to be caused by the early-stage use of any one particular AI, at least from what I’ve been able to read).

I have not looked on BCO for discussion on Aromatase inhibitors for awhile. I checked out of one of the main threads a couple of years ago after reading lots, mainly because I knew I needed to be in Anastrozole at least for 5 years. This morning I decided to have another look and saw this thread. I have one more year to get to the 5 year mark and have been hearing from my MO for awhile that 10 years may be recommended. There is one woman who was on our Canadian thread until it disappeared by mistake and who I am on FB with, who is at 5 years and will discontinue as a matter of choice this week. This is what I hope I am brave enough to do in a year when my 5 years is up. The S/E are not unbearable but they are enough to make me want to see what life is like without the A/I. I am now on Prolia twice a year for osteopenia that had a rapid progression. Dry everything from lack of estrogen is annoying. Hot sweats were a big problem until I started on Venlifaxine 1.5 years ago for depression. My MO considers 150 mg to be a low dose but recently when I we lowered the does dose to 112.5 mg, within a a week, hot flashes returned. BTW, when I started on the antidepressant my MO said that 50% of women had fewer hot flashes. Bottom line, in a year I want to "walk away." Quality of life is probably what I am after.

Hi Barbe "the nice thing about Melatonin is that if you wake up in the middle of the night you can take another one without adverse effects" unless you happen to be one of those that is very sensitive to the amount you take. Actually recommended dose in the peer reviewed articles is about 10% of what's in most tabs. But most people can use much more with no problem. If you go too high it messes up your sleep cycle. It keeps me awake even at the low dose from the drug store (3 mg)!! I tried it (3 nights in a row to make sure I wasn't just having a lousy night) instead of valerian to see if it would help me get a half decent night's sleep while I go through the scans & biopsies & wait for all of my results (MRI is next week) and get ready for the surgery. Didn't help Went back to Valerian and doing better.

If you're uncomfortable with data, many medical study authors will respond to emails. But unfortunately, the hormonal stats referenced are substandard at best and very limited online. If you have access to more current & prudent "clinical endpoint & absolute data" to share, please post here.

Links to statistical data were originally provided so people can read for themselves to avoid misleading comments, misinterpretation and misrepresentation. Please kindly do not shoot the messengers. We are all united here as one sisterhood for help and support.

https://community.breastcancer.org/forum/78/topics...

Respectfully, I beg to differ, as I never stated that ESR1 mutations were the "cause" of mets; however, ESR1 is indeed only one contributing factor of many. "Cause" and "contribution" hold two distinct definitions which are not inter-changeable.

................................

TOPIC - Risk Reduction Stats. https://community.breastcancer.org/forum/78/topics...

.................................

IBIS-II http://www.thelancet.com/pdfs/journals/lancet/PIIS...(13)62292-8.pdf

Research has shown that anastrozole is more effective than tamoxifen in preventing the return of cancer in post-menopausal women who have an early breast cancer removed. In these women it reduces their risk of developing a new cancer in the opposite (contralateral) breast by 53% compared to tamoxifen¹

http://www.ibis-trials.org/thetrials/ibistrials/ib...

..................................................

Aromatase Inhibitors May Prevent Cancer

http://www.naturalmedicinejournal.com/journal/2014...

We must find and consider the bottom line. Eighteen deaths were reported in the anastrozole group and 17 in the placebo group. At this point 5 years into the experiment there is no difference in overall survival (OS), and the data do not yet support the assumption that there will be a fewer deaths from breast cancer in the anastrozole group with longer follow-up.

[Edited to add]

I would have like to have seen weareconnected posts. Not sure why they were deleted.

WildPlaces, once again, your screen name appears to be a strong representation of your actions.

The March 17th re-posts are merely mirror images of my earlier ESR1 reposts because the mods were apparently censoring my posts for video content. Video reposts by YouTube user name also got censored by the mods & deleted.

There's no secret agenda on my part, as I fully respect the 1st Amendment of the US Constitution.

Our disease must be treated with sensitivity

Do not personalise comments

please respect everybody

Dear VioletKali, Thank you for sharing! I too am bipolar. Just had a mastectomy and now my surgeon and medical oncologist want me to take Arimidex for 5 to 10 years. Your post made alot of sense to me. I also am doing great on my bipolar meds and am leading a mentally very healthy life. I am scared to take Arimidex, because it will upset my body chemistry. I have copied your post and am going to show it to the surgeon this coming Wednesday and to the medical oncologist a few days after that. Am also looking into a homeopathic clinic in Mexico. Hoping to make the right decision. All the best. Thanks so much again for your post!!

I'm not sure if this is quite the right place to post this question or not but I am interested in your opinions. I'm wondering why a MO prescribes one AI over another for those of us who are postmenopausal with no signs of osteoporosis? My MO put me on Arimidex right away, even before I started radiation, and I am curious why this particular drug as opposed to Femara?

Look up the price for your AI on goodrx.com. Much much cheaper there than using your insurance.

Dear Hopeful, thank you so much for responding to my post! I wasn't sure if this was the correct place for posting my inquiry. It's funny, I never even thought to ask my MO about the different types of AIs because, quite frankly, I was still in the "deer in the headlights" mode and had no clue about these things. My sister was also automatically placed on Arimidex. On another tangent, I have noticed on this website that many people don't start on an AI until they are completely finished with radiation; I began it before and continued with it concurrently. It's interesting how treatment strategies can differ from one doctor to the next. I'm so glad to hear that Femara worked well for you!!