don't know! would like 2 hear answers too. i got so sick,crazy onco. took me off it. said lower doses w/not work.anyone ?..3jaysmom

I have seen on this site women from other countries who say that their DR. ok'd half pill or even every other day.  I tried Femara for a few months and chose not to take it.  I feel much better without it, not to mention the long term s/e's.  I work with the public and have met several women also w/in my support group who are long term survivors and who chose to take nothing for various reasons.

Do your research.  There are so many other options out there.  I take Lugol's iodine which does much of the same thing the Femara does.  It blocks estrogen.

Good luck.

Yes,
Femara caused joint pain, and I could bearly get up from the sofa!  Now that I am off it, I feel "normal" once again.   I am taking tap dancing also!  60 years old.... not ready to deal with all the s/e's and/or the bombardment of meds to counteract each other.

Fortunately, my onc is very open minded and said the less medical intervention, the better I will be!

I have met too many women who chose to just live their life holistically that are long term survivors (some 20 years!)   so I not willing  to succomb to all these horrible drugs.

never heard of total hair loss w Femara. So experience some thinning but never heard of anything severe.

Did you have succes using 1.25 femara?

I was suppose to start taking the al's last January and did not start until 2 days ago, eight months later. Every dr. I saw kept scaring me and telling me to take it. I finally started taking it out of fear. Not sure if I will continue, so far no side effects but I am definitly fearful. I am seeing a different oncologist next week and hoping I could get some support not to take it.



My oncotyle was only 6 and they said if I did not take the drugs it would double to 12. When they tested me for estrogene mine was very low. I am 65 and do not understand why we need to take it if our estrogene is low.

I started developing hideous side effects a little over a year into my Femara chemo--which i am to take the rest of my life.  I may have a damaged left kidney as a result of Femara. I cut my dose in half last night because I had bloody urine and it was midnight and I feared to take the full nasty dose.  I'm sure my oncologist will scream.  All the other chemo therapies are worse than Femara.  I don't know what to do.  I do feel better on this half dose.  I'll talk to the doctors tomorrow.

The Medical World tends to use a big hammer when it comes to medication. When they first started out with birthcontrol, the doses were way too high.  When the medical world went to hormone replacement therapy for menopause, the doses were way too high as well and they used horse urine.  I guess I'm betting my life, but I am in terrible pain with what is probably a kidney infection.  I hadn't had a UTI in 50 years prior to going on the Femara.  

I think the Medical World may have this Femara dose too high as well.  I'll see if I have enough nerve to take another half dose tonight.

I have not had my period in over 4 years after chemo induced menopause. Have been on Tamoxafin for almost 4 years now and just started 'menstrating' 4 days ago. I'm 46, was 42 when diagnosed, I'm a bit concerned... Anyone here had similar experience???  

KR13, thanks so much for this info!  So, it appears that 0.5 mgs works as well as larger doses, in that anything at or above 0.5 mgs makes estrogen undetectable.  I started splitting my pills a few nights ago because of hot flashes and insomnia, and it has helped.  If 0.5 makes estrogen undetectable, then using over twice that amount (1.25) should be just dandy if not overkill.  I don't know if I'm going to mention that I'm doing this to my doctor, but if I do, I will probably have these results printed up when I talk to him.  

The real question here seems to be "will altering my dosing keep my estrogen levels low enough so that any estrogen receptive cancer cells lurking in my body cannot use my estrogen to stimulate growth".   We know that is why we're offered these drugs, not because our doctors want to torture us.

Estradiol in the blood and saliva can be measured.  When I was first diagnosed, before starting Femara, my oncologist ran lots of blood tests, and estradiol was one of them.  Perhaps your oncologist would agree to let you try it every other day or a half pill, then measure your blood estradiol to see how it works for you?  If he/she will not, there are online kits and labs who will measure it for you without your Dr approval (in the U.S.), but using your own doctor is always best (IMO).

I still do take it every day until I feel sick again.  Then I go to 4 days a week until I catch up on my sleep and get rid of the nausea.  I have an appt with my oncologist soon and I do plan to talk it over with him again, although with my oncotype he is sure I need the AI for at least 10 years (He hinted at forever). 

My tongue felt fat when I start anastrozole. It was a little scary but it seemed to go away.

The final straw was when I couldn't get out of bed one morning really achy. I was switched to exemestane.

I'm ok but tired oh yah the ringing in my one ear and the degenerative arthitis in my neck(That does feel a little better).

Bump, and could people please answer the originally posed question about whether they tried a half dose and what the effects might have been, rather than simply describing the negative side effects of AI's that they've taken? Not to minimize anyone's negative experience with AI's in general, but the question is about noted effects of taking only half the dose of Femara/letrozole.

I am supposed to start taking this and like so many am quite scared, so would really like to hear anyone's response to the original question here.

I have read that doses of .5 all the way to 5.0 can result in undetectable levels of estrogen. I continue to be baffled as to why everyone is supposed to take 2.5 per day in our cases. I have also read that taking 1.25 each day (half the 2.5 prescribed) is not the same as taking the 2.5 every other day, and that 2.5 every other day actually provides better coverage. It supposedly has to do with the half life of the drug which is 48 hours according to most sources, although I did see one that indicated the half life of letrozole is 72 hours.

I would really like to hear other people's thoughts and experiences about this, because it would be so much better to just take this pill every other day, if even these lower doses can result in effective estrogen suppression. Aside from the side effects, taking it every other day would cut the cost in half and only half of the dyes, fillers, etc. would wind up in our bodies - and in the water table, etc. (causing damage to fish and more).

Has anyone heard why the 2.5 per day dose is prescribed, when lower doses have been shown to produce undetectable levels of estrogen? Has anyone had their estrogen levels checked routinely during the course of their letrozole treatment? I also fail to understand why my oncologist at least, has not done any estrogen level checking. I thought the goal was to achieve an acceptably low level of estrogen. If lower doses can do that, why is everyone prescribed the 2.5 mg per day without even knowing what their estrogen levels are? When I asked the oncologist why estrogen levels aren't checked, she said, "We just don't do that", and seemed to not want to talk about it any more.

Very curious about this whole issue.

Double-blind, Randomized Trial of Alternative Letrozole Dosing Regimens in Postmenopausal Women with Increased Breast Cancer Risk

https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4740217/

.

"We conclude that low and intermittent doses of letrozole (as low as 1/24th of the total dose received in the standard dose arm) were not inferior to the standard dose in estrogen suppression at the end of agent intervention. The effective estrogen suppression with low and intermittent letrozole doses was accompanied by similar adverse effects on C-telopeptide levels when compared to standard dose. The changes in QoL and self-reported AEs were also similar among the dose groups."