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Old 03-17-2008, 04:41 PM   #1
CLTann
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Anyone trying lower dosage for AI due to side effects?

Under the separate thread of Arimidex or Femara side effects, it has been well concluded that about 40% of patients complained about bone and joint aches. Do those of you with side effects ever consulted with you oncs to see whether a half dosage of AI is the answer. I would be very much interested in going this route if there are indeed precedents to this approach. Please report.
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Ann

Stage 1 dx Sept 05
ER/PR positive HER2 +++ Grade 3
Invasive carcinoma 1 cm, no node involvement
Mastec Sept 05
Annual scans all negative, Oct 06
Postmenopause. Arimidex only since Sept 06, bone or muscle ache after 3 month
Off Arimidex, change to Femara 1/12-07, ache stopped
Sept 07 all tests negative, pass 2 year mark
Feb 08 continue doing well.
Sep 09 four year NED still on Femara.
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Old 03-17-2008, 09:13 PM   #2
Debra
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Ann -

I just wanted to provide some input. I am 42 had been on arimidex for less then a year and really struggled with the joint pain. I was switched to aromasin and it made a HUGE difference. Other then my feet causing me some problems, although they always have, I am about 95% better. I also started exercising so I am not sure if it is 100% the aromasin or the exercise but I will say, I am a new person and life is so much better! I don't see aromasin mentioned a whole lot here on the sight but my oncologist felt there was absolutely no reason to suffer if there was other options that alleviated the pain and even indicated studies have shown it to be superior over some of the other AI's. Just my two cents!
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Diag. 11/05 at age 40 triple positive
3.8 cm tumor and 9 mm tumor
Stage IIb/SN positive(no other nodes)Grade 3
Bilat. mastect. 12/05 (Rt.prophylactic) followed with AC/taxol/Herceptin/tamoxifen then switched to arimidex after hysterectomy in 12/06. August 07 switched to Aromasin due to severe jt. pain from Arimidex. Nov. 2011 No more meds and NED!
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Old 03-17-2008, 10:23 PM   #3
sadie
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I am glad to hear that it's not just me that is experiencing the joint pain (legs & feet).
I attribute it to weight gain and the arimidex (1mg daily).
I am continuing the arimidex because I am afraid to change from something that seems to be working for me.
I'm hoping that exercise will help the situation. I feel like my body is that of an 80 year old.
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Old 03-18-2008, 06:56 AM   #4
Hopeful
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I reviewed the dosing and metabolism information from the websites of both Arimidex and Fermara prior to my fall onc visit, to see if I could go on a reduced dosage. According to the information I read, the standard dose is higher than the average patient requires to attain the degree of aromatase suppression the drug is designed to deliver. Arimidex does not provide for reduced dosing, even in patients with poor liver function, but Femara does. The reduced dosage is administered by taking a pill every other day, rather than every day. My onc said he has only done the lower dose regimen with very elderly patients whom he believed would have less aggressive disease. His opinion was that the half dosage did not work as well. This is another area I believe requires more immediate attention and study.

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Old 03-18-2008, 07:43 AM   #5
TSund
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Hopeful,

I am very interested in this QOL issue. Does your onc base this opinion on any clinical evidence?

TRS
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Terri, spouse of Ruth, Dallas/Ft. Worth area
Ruth dx 05/01/07 (age 50) Filipino
multifocal, several tumors .5 -2.5 cm, large area
Breast MRI showed 2 enlarged nodes, not palpable
100%ER+, 95%PR+, HER2+++
6x pre-surgery TCH chemo finished 9/15/7 Dramatic tumor shrinkage
1 year Herceptin till 6/08
MRM 10/11/07, SNB: 0/4 nodes + Path: tumors reduced to only a few "scattered cells"
now 50% ER+, PR- ???
Rads finished 1/16/08
Added Tamoxifen,
Finished Herceptin 05/08
NOW is the time to appreciate life to the fullest.
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Old 03-18-2008, 08:56 AM   #6
Hopeful
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Terri,

None that I am aware of, though, truthfully, I don't think there is any. I think the Phase I trials of the drugs were done to test toxicity (i.e., what is the maximum dose you can take without it killing you) vs. what is the minimum amount you need to take for it to be effective. In private correspondence with a friend who works in the medical field, I was advised that the doses of the meds are likely set at levels that enable the fastest metabolizers to maintain the steady-state level of the drug in the blood that is the recommended dosage. What this means is that normal or slow metabolizers are having more of the drug floating around in their body than is probably required to do the job. I brought this up with my onc, and he said 1) he wished I had asked him the question a month earlier, as the "inventor of Femara" was a guest speaker at his practice's lunchtime CME and he could have gotten a good answer for me, and 2) it is his belief that circulating hormone levels do not remain level, even on these drugs, and go up and down somewhat. The latter is something I had never heard, and I am not sure why he thinks this; however, it was part of his rationale for not halving the dose. Perhaps the "Femara expert" discussed it in the CME.

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Old 03-18-2008, 07:15 PM   #7
TSund
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This is good info Hopeful.

Re: circulating hormone levels; it actually makes some sense as women naturally have fluctuating levels. I read something recently that indicated estrogen is not completely controlled by ER moderating drugs including AI's and thus stressed the importance of exercize and weight control, both of which help control estrogen levels in the body. Brings in an irony; as if the AI's side affects are too extreme it could prevent the woman from getting regular exercize. (and that in turn could contribute to weight imbalance). Several here have said that exercize helped their symptoms, so I guess that's a win/win for them.
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Terri, spouse of Ruth, Dallas/Ft. Worth area
Ruth dx 05/01/07 (age 50) Filipino
multifocal, several tumors .5 -2.5 cm, large area
Breast MRI showed 2 enlarged nodes, not palpable
100%ER+, 95%PR+, HER2+++
6x pre-surgery TCH chemo finished 9/15/7 Dramatic tumor shrinkage
1 year Herceptin till 6/08
MRM 10/11/07, SNB: 0/4 nodes + Path: tumors reduced to only a few "scattered cells"
now 50% ER+, PR- ???
Rads finished 1/16/08
Added Tamoxifen,
Finished Herceptin 05/08
NOW is the time to appreciate life to the fullest.
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Old 03-20-2008, 10:17 AM   #8
Hopeful
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I just wanted to post this link from a 2003 interview with Dr. Paul Goss from Breast Cancer Update: http://www.breastcancerupdate.com/bcu2003/5/goss1.htm

as I think it has some information that comes to bear on some of the questions raised in this thread. I found his closing comments particularly interesting:

"I am very interested in how closely a woman’s health is related to a small range of estrogen. The slope of the postmenopausal estrogen range is a very small curve and is tightly related to breast cancer risk, osteoporosis and probably cardiovascular risk.

My personal feeling is that healthy postmenopausal women without breast cancer need their estrogen level “customized.” We can tone it up with HRT, but now we have a subtle way of toning it down. We have tried the two extremes — blockbuster ablation or massive replacement — but we haven’t tried zoning in on a middle range. I’m 100 percent convinced that in the next 10 to 15 years we will develop an understanding of women’s estrogen levels and their impact on health."

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Old 03-21-2008, 08:20 AM   #9
miss di
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I have been asking about this since first go round. Always wondering why I have to take as much as someone with ovaries? (I had mine removed in 2000) obviously I would have less estrogen. When I asked, reply is always, but you still have "some". It also is stored in body fat, at this point I have no body fat and still have to take same amount, 1mg Arimidex daily.
Also, my second cancer is "mildly" estrogen positive, first time was "highly".
Would love an answer.
My best to all,
Di
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Old 03-21-2008, 10:30 AM   #10
Donna
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Another Question

Hi Amazing Group,

What I am wondering is this: I was already post menopausal and had none of these side effects. Is there something else in these medications doing the damage to the joints? I don't hear menopausal women complaining of trigger finger. This seems to uniformly hit our tendons, thumb first - should we as a group go to the manufacturers and demand answers?

I am thinking of visiting a remarkable hand specialist I know to see if he can shed some light on this.

Hoping we figure this out! Happy Easter to all!

Donna
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Donna in the Sierra Foothills of California

Diagnosed 6/7/06 invasive ductal carcinoma/ductal carcinoma in situ
Lumpectomy 6/21/06
Pathology: Er 99% Pr 10% Her2/neu 3+
DNA Index 1.0
S-Phase 3/High
Primary Tumor 2.4 cm Sentinel Node Tumor 2.1cm
A/C/T+ Herceptin + rads + Arimidex
stopped Herceptin after 7 mos. due to low MUGA
Surgery for thickened uterine tissue May 2008 - conclusion: side effect of Arimidex
Switched from Arimidex to Femara - joint/tendon problems significantly better!
2 year mark Pet scan and Echo shows all clear!
5 year mammogram with ultrasound shows no sign of cancer - yay!
11 years, 11 months new breast cancer - found lump
Mastectomy 4/30/2018
Pathology: Er99%, PR 28%, Her2 negative! (new type)
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Old 03-21-2008, 11:33 AM   #11
Becky
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Menopausal women still have some estrogen. The adrenal glands make it and fat cells make it. It is made using androgens that get converted via a (bio)chemical reaction to estrogen. The reaction needs an enzyme to make it go and that enzyme is aromotase. An aromatase inhibitor binds to aromatase and makes it unable to function as an enzyme in this reaction. Therefore you make less or in many cases no estrogen. Women with functioning ovaries (premenopausal) cannot take an AI because the ovaries produce estrogen in a different way so an AI would still block the way it is made from the adrenal and fat but that is such a small amount versus the ovarian mechanism - and a premenopausal woman would have no benefit as there would be tons of estrogen around.

Therefore, there can be a big difference in a menopausal woman versus a menopausal woman on an AI especially a menopausal woman who is also overweight (as they would be producing more estrogen).

No or very little estrogen is what is causing the symptoms - not necessarily the AI itself.
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Becky

Found lump via BSE
Diagnosed 8/04 at age 45
1.9cm tumor, ER+PR-, Her2 3+(rt side)
2 micromets to sentinel node
Stage 2A
left 3mm DCIS - low grade ER+PR+Her2 neg
lumpectomies 9/7/04
4DD AC followed by 4 DD taxol
Used Leukine instead of Neulasta
35 rads on right side only
4/05 started Tamoxifen
Started Herceptin 4 months after last Taxol due to
trial results and 2005 ASCO meeting & recommendations
Oophorectomy 8/05
Started Arimidex 9/05
Finished Herceptin (16 months) 9/06
Arimidex Only
Prolia every 6 months for osteopenia

NED 18 years!

Said Christopher Robin to Pooh: "You must remember this: You're braver than you believe and stronger than you seem and smarter than you think"
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Old 03-21-2008, 01:55 PM   #12
Hopeful
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Becky,

Question for you. I have read a few places that the "next generation" of AI's will be ones that target only aromatase in breast tissue. My question is, when bc develops, even if some of the cells move out of the breast and into the body, they are still breast cells, right? So that an AI that targeted breast tissue would be able to exert its effect on all ER+ bc cells, wherever they may roam?

Hopeful
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Old 03-21-2008, 02:02 PM   #13
TSund
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Re: Becky's post

Apparantly it is even more serious than that, I think there is speculation that the AI's can "turn on" the ovaries to produce extra estrogen when pre-menopausal. Like adding fuel to the fire.

TRS
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Terri, spouse of Ruth, Dallas/Ft. Worth area
Ruth dx 05/01/07 (age 50) Filipino
multifocal, several tumors .5 -2.5 cm, large area
Breast MRI showed 2 enlarged nodes, not palpable
100%ER+, 95%PR+, HER2+++
6x pre-surgery TCH chemo finished 9/15/7 Dramatic tumor shrinkage
1 year Herceptin till 6/08
MRM 10/11/07, SNB: 0/4 nodes + Path: tumors reduced to only a few "scattered cells"
now 50% ER+, PR- ???
Rads finished 1/16/08
Added Tamoxifen,
Finished Herceptin 05/08
NOW is the time to appreciate life to the fullest.
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Old 03-21-2008, 05:36 PM   #14
Becky
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Hopeful

I wonder how that would work. For example, you might stop the estrogen reaction in the breast but what about the rest of the body where estrogen would enter the blood stream and make it to the breast cells anyway - and the rest of the body, who knows? I really can't comment now but didn't want you to think I didn't read your question.

Terri - it is true that Femara is used to help induce multiple ovulations during invitro fertization procedures (at least in the UK it is).
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Kind regards

Becky

Found lump via BSE
Diagnosed 8/04 at age 45
1.9cm tumor, ER+PR-, Her2 3+(rt side)
2 micromets to sentinel node
Stage 2A
left 3mm DCIS - low grade ER+PR+Her2 neg
lumpectomies 9/7/04
4DD AC followed by 4 DD taxol
Used Leukine instead of Neulasta
35 rads on right side only
4/05 started Tamoxifen
Started Herceptin 4 months after last Taxol due to
trial results and 2005 ASCO meeting & recommendations
Oophorectomy 8/05
Started Arimidex 9/05
Finished Herceptin (16 months) 9/06
Arimidex Only
Prolia every 6 months for osteopenia

NED 18 years!

Said Christopher Robin to Pooh: "You must remember this: You're braver than you believe and stronger than you seem and smarter than you think"
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Old 03-21-2008, 08:08 PM   #15
Joanne S
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My oncologist just recently switched me from Tamoxifen to Arimidex. I haven't noticed any difference in bone/joint pain as I've only been on Arimidex for 7 days, but the hot flashes with sweat pouring off my head and face is just overwhelmingly horrible. I imagine being overweight makes makes these symptons worse. Will these private summers improve? I too was wondering about the possibility of a lower or half dose of Arimidex.

My doctor explained that Arimidex blocks the production of estrogen where as Tamoxifen blocks the effects of estrogen.

Jo
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Aug06...Dx Age 50, IDC Left Breast, 6+/16 lymph nodes, Stg 3, ER+/PR+/HER2+
Sep06-Jan07...Mediport. Chemo: AC x 4, T x 4
Dec06-Nov07...Herceptin
Feb12,2007...Surg MRM Left & SM Right, reconstruct w/expanders
Mar07-Jun07...Saline Exp
Jun07...Start Tamoxifen
Jun07-Aug07...Rad x 25
Jun07-Oct07...Persistent fevers-unknown origin
Jun07-Nov07...PT for Severe PMPS & Capsular Contracture
Nov07...Surg Capsulectomy, Gel Implants, PMPS pain gone instantly.
Feb08...NED 1st CANCERVERSARY!!!!!
Feb08...2 months post surgery Caps Cont again :(
Mar08...Stop Tamoxifen. Start Arimidex.
Apr08...Sudden high fever, Hosp ICU 10 days, staph infect, emerg surg, implants removed. Outpt IVantibiotics Daily x 6 weeks
Feb11...NED 5th CANCERVERSARY!!!!!
Feb12...NED 6th CANCERVERSARY!!!!!
Aug12...Spotting. Surg=D&C
Sep12...STAGE IV = RARE BC METS TO UTERUS ILC ER+/PR+/HER2-Negative) (Different BC than originally diagnosed = IDC ER+/PR+/HER2+).
Sep12...Stop Arimidex. Start Afinitor & Aromasin.
Jan13...MRI = no progression no reduction
Apr13...Progression. Stop Afinitor & Aromasin.
Apr13...Start Chemo: Taxol & Carboplatin.
Nov13...Scans & Pelvic 95+% Reduction. Nueropathy>Stop chemo start Fareston.
Jan14...PET scan = no progression stable.
May14...Pelvic > Bleeding & cramps. TMs up.
May14...PET scan = uterine progression :(
May14...Stop Fareston. Start Chemo: Xeloda.



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Old 03-23-2008, 11:40 AM   #16
TSund
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Becky, have no idea of that one, but it sure is interesting if so. I was theorizing that working ovaries "sense" the lowering of estrogen in the body from the AI's and thus work harder to make more.

TO all following this conversation; do you have any opinions on DIM supplements? I didn't realize these may work specifically on the estrogen factor until reading a bit more lately.

TRS
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Terri, spouse of Ruth, Dallas/Ft. Worth area
Ruth dx 05/01/07 (age 50) Filipino
multifocal, several tumors .5 -2.5 cm, large area
Breast MRI showed 2 enlarged nodes, not palpable
100%ER+, 95%PR+, HER2+++
6x pre-surgery TCH chemo finished 9/15/7 Dramatic tumor shrinkage
1 year Herceptin till 6/08
MRM 10/11/07, SNB: 0/4 nodes + Path: tumors reduced to only a few "scattered cells"
now 50% ER+, PR- ???
Rads finished 1/16/08
Added Tamoxifen,
Finished Herceptin 05/08
NOW is the time to appreciate life to the fullest.
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Old 03-28-2008, 12:25 AM   #17
harrie
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Beckys post

Becky,
If the lack of estrogen is what is causing the symptoms of joint pain, I wonder why it is that some some AIs such as Aromasin or Femera cause some women less joint pain then Arimadex?

maryanne
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*** MARYANNE *** aka HARRIECANARIE

1993: right side DCIS, lumpectomy, rads
1999: left side DCIS, lumpectomy, rads, tamoxifen

2006:
BRCA 2 positive
Stage I, invasive DCIS (6mm x 5mm)
Grade: intermediate
sentinal node biopsy: neg
HER2/neu amplified 4.7
ER+/PR+
TOPO II neg
Oncotype dx 20
Bilat mastectomy with DIEP flap reconstruction
oophorectomy

2007:
6 cycles TCH (taxotere, carboplatin, herceptin)
finished 1 yr herceptin 05/07
Arimidex, stopped after almost 1 yr
Femara
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Old 03-28-2008, 08:05 AM   #18
Melinda
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I just recently started taking Aromastin. For those of you that have been on ANY these AI's how long did it take before you became aware of the side effects such as trigger finger and joint pain. Any other side effects noticed?
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DX BC 12/06
tumor .9
Lumpectomy 1/8
Mammosite radiation completed 2/10
Stage1/Grade 1
clear Margins /Nodes Neg
ER+
IHC +2 Fish +
ONCO 23
Started TCH on 3/2 for 6 rounds of TC once every three weels and a year of Herceptin every 3 weeks -
Finished everything and now on Aromasin
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Old 03-28-2008, 09:41 AM   #19
Donna
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Thank you, again!

Dear Becky,

Thanks so much for once again for your time and trouble to answer my question in terms I can understand. Your responses are always clear and illuminating. Your participation on this board is invaluable and I just want to say THANK YOU! HAVE A GREAT DAY!

Donna

P.S. just a "I wonder if" thought, would overweight women have a greater propensity to this tendon anomaly? I am overweight and I wonder just how hard those poor AI's have to work.....:-)
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Donna in the Sierra Foothills of California

Diagnosed 6/7/06 invasive ductal carcinoma/ductal carcinoma in situ
Lumpectomy 6/21/06
Pathology: Er 99% Pr 10% Her2/neu 3+
DNA Index 1.0
S-Phase 3/High
Primary Tumor 2.4 cm Sentinel Node Tumor 2.1cm
A/C/T+ Herceptin + rads + Arimidex
stopped Herceptin after 7 mos. due to low MUGA
Surgery for thickened uterine tissue May 2008 - conclusion: side effect of Arimidex
Switched from Arimidex to Femara - joint/tendon problems significantly better!
2 year mark Pet scan and Echo shows all clear!
5 year mammogram with ultrasound shows no sign of cancer - yay!
11 years, 11 months new breast cancer - found lump
Mastectomy 4/30/2018
Pathology: Er99%, PR 28%, Her2 negative! (new type)
Faslodex
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Old 03-28-2008, 10:28 AM   #20
KRISS
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I was only on tamoxafine for about 3 months when they switched me to femara after my hysterectomy. I had no side affects for the first 2 months but for the last three have had horrible joint and bone pain, not to mention the swelling in my hands. Some days I have no feelinging in either hand or only partial fingers. My knees hurt the most and with my physical job I'm in trouble. My Onc wants me to stay on it for at least 9 months to see if it lessens and then he might switch me. He believes there is no validity to switch. So we will wait it out a little longer.
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DX IDC AT 42 12/7/06
2.2CM STAGE I GRADE 2
NODE NEG
PARTIAL 12/18/06
HER2+ /ER+(75%) PR+(5%)
4 DD AC CHEMO STARTING 1/10/07
4 DD Taxol Starting 3/5/07
1year weekly Herceptin starting 3/5/07
finished 2/18/08
changed to every 3 weeks 4/23/07
completed 33 radiation treatments 7/6/07
TAH and BSO 9/24/07
start Femarra 10/8/07
Started Neritinib trial 12/14/09
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