Zometa - Latest News out of San Antonio Meeting

I am meeting with someone today about this so I will share what I learn!

everyminute,

I was wondering the exact same thing.  I'm supposing that with regular menopause, it takes that long for your body to slowly lose its estrogen and that's why they say 5 yrs out.  But with hyster/ooph, it is immediate, so I'm thinking we are in the same boat estrogen-wise as a 5yr. out post-menopausal woman. 

I guess that would also explain why it didn't seem to help estrogen negative gals--they wouldn't have been on an estrogen depriver.

Please, anyone, let us know what you find out!

Since estrogen levels can be tested, I'd like to know what level of estrogen would put a women into the same level as a woman 5 years into menopause.  My wife is currently in chemopause, and wondering if it is permanent, and whether it is sufficient to get benefit from bisphosphonates in terms of cancer recurrance prevention.  I've read that 10-20 pg/ml is a typical menopausal level of estradiol.  Also that less than 25 is typical of a woman 5 years into menopause.  So if a woman tests in that range, is she as likely to get benefit from zometa as the women who did in AZURE?

Here is evidence support zometa for early-stage breast cancer in the Nov. 2010 issue of Annals of Oncology:

Efficacy of Zoledronic Acid in Postmenopausal Women With Early Breast Cancer Receiving Adjuvant Letrozole: 36-Month Results of the ZO-FAST Study
Ann Oncol. 2010 Nov 1;21(11):2188-2194, H Eidtmann, R de Boer, N Bundred, A Llombart-Cussac, N Davidson, P Neven, G von Minckwitz, J Miller, N Schenk, R Coleman
After a 36-month follow-up period, early initiation of ZOL provided significant benefits in bone health and improved DFS in postmenopausal women receiving adjuvant AI therapy for early hormone-receptor...

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After a 36-month follow-up period, early initiation of ZOL provided significant benefits in bone health and improved DFS in postmenopausal women receiving adjuvant AI therapy for early hormone-receptor positive breast cancer.

Abstract
SUMMARY
OncologySTAT Editorial Team
Aromatase inhibitors (AIs) have greater efficacy than tamoxifen as adjuvant endocrine therapy for postmenopausal women with hormone receptor-positive early breast cancer. Bisphosphonates such as zoledronic acid (ZOL) have been demonstrated to prevent bone loss and reduce the risk of fracture associated with AIs, and have also been demonstrated to improve cancer outcomes. Eidtmann et al reported the results of a 36-month follow-up of the Zometa-Femara Adjuvant Synergy Trial (ZO-Fast). Patients for whom ZOL treatment was initiated immediately after randomization (immediate ZOL group) experienced improved bone health and disease-free survival (DFS) compared with those for whom ZOL treatment was delayed (delayed ZOL group).

In this open-label multicenter randomized trial, patients were postmenopausal women or women who were recently menopausal because of chemotherapy or ovarian suppression for hormone-receptor positive early breast cancer. Baseline lumbar spine (LS) and total hip bone mineral density (BMD) T-scores were required to be > -2.0. Patients were randomly assigned to receive immediate or delayed ZOL treatment. All patients received oral daily letrozole for 5 years and daily calcium and vitamin D supplements. In the immediate ZOL group, ZOL was provided beginning immediately after randomization. In the delayed ZOL group, ZOL was provided if the patient's T-score became < -2.0 after a nontraumatic bone fracture or if an asymptomatic fracture was detected by spinal x-ray.

A total of 1065 patients were randomly assigned in the original ZO-Fast trial. Baseline and 36-month BMD data were available for 314 patients in the immediate ZOL group and 319 in the delayed ZOL group. From baseline to 36 months, LS BMD increased by 4.39% (95% confidence interval [CI], 3.69%-5.11%) in the immediate ZOL group, and decreased by 4.9% (95% CI, -5.54% to -4.25%) in the delayed ZOL group (least squares mean difference between groups, 92.9%; 95% CI, 8.37%-10.20%; P < .0001). Slightly smaller but still significant changes were observed for total hip BMD (P < .0001). More patients in the immediate ZOL group than in the delayed ZOL group with baseline lumbar T-scores between -2.0 and -1.0 transitioned to normal BMD (P < .001), and more patients in the delayed ZOL group than in the immediate ZOL group developed severe osteopenia/osteoporosis (P < .001). However, similar proportions of patients in the immediate and delayed ZOL groups experienced fractures (5.0% vs 6.0%; P = .502).

A total of 506 of 532 immediate ZOL patients and 489 of532 delayed ZOL patients were disease free and alive, corresponding to an absolute difference of 3.2% between the two groups and a relative reduction of 41% in the risk of having a DFS event (hazard ratio [HR] = 0.588; 95% CI, 0.361-0.959; P = .0314). Compared with the delayed ZOL group, the immediate ZOL group had fewer local (0.4% vs 1.9%) and distant (3.8% vs 5.6%) recurrences, and fewer immediate than delayed ZOL patients developed bone metastases (1.7% vs 3.2%). Adverse events were similar between groups. Influenza-like symptoms were more common in the immediate than in the delayed ZOL group. Renal failure or impairment was less common in the immediate than in the delayed ZOL group (0.2% vs 0.6%). Osteonecrosis of the jaw occurred in 2 patients in the immediate ZOL group.

The results of this analysis showed that early initiation of ZOL provided significant benefits in bone health and improved DFS in postmenopausal women receiving adjuvant AI therapy for early hormone-receptor positive breast cancer.

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Kward but didn't your doctor atleast feel it was benificial for bone loss?

My second Zometa is supposed to be next Monday in conjunction with my onc visit.  I'm also curious about his take on this.  He's a colleague of Dr. Gralow who's been involved in the SWOG study and they are still aways out from publishing results.  So I'm curious what he'll say.

I saw my oncologist today for a 3-month follow-up.  I was scheduled to have my 4th Zometa treatment in March 2011.  He said he was stopping it for me.  We discussed it and I'm comfortable with the decision.  I was 38 and pre-menopausal at the time of my diagnosis.  It doesn't seem, even with being on Tamoxifen, that my "flavor" of menopause (whether it's still chemo-pause, or my body slowly getting itself into a true menopause), that I would fall into any of the groups that show clear benefit from the Zometa.  He said that some of his patients he currently has on Zometa, he will keep on it; mainly older women who are truly post-menopausal (not borderline like me), and who are on AI's, so at a minimum they will benefit from the bone strengthening that Zometa gives you.  I currently get that benefit from Tamoxifen.

O.k., here is what I was told: it is very curious that Zometa did not show any effect in this study, but this surely is not representing Zometa not having an effect. Rather, it seems to be a question of dosage. The positive results for Zometa exist and that plentiful. They should not be discarded simply on this one study.

I know these types of study results can cause a lot of questions, second quessing and anxiety regarding the most effective treatment plan for each of us.  I too am very interested in hearing about any additional studies or research data that can better clarify the role Zometa may play in reducing the chance of metastatic spread.  I have learned some time ago however, not to believe that any study can be completely accurate or even applicable under all the varied circumstances cancer can present.

I have a heavy investment both emotionally and physically in Zometa since I have been receiving IV infusions for almost 5 years now.  Obviously, there is no way I can know beyond certainty why I still remain NED 5 years after having 23 positive nodes but my gut tells me the Zometa has had a role to play in that.  I will be seeing my onc in mid January and will discuss the topic with her but I am more than willing to continue to get what will be my last Zometa dose in July of 2011.

Based on the Azure results it appears I may meet the criteria for the subgroup of women who did show benefit from Zometa.  I went into chemo induced menopause in 2000 after my first BC dx at the age of 47 so was definitely post-menopausal in 2005 when I had my second primary BC dx at the age of 52.  My estrogen levels a few years ago were at a low of 8 plus I have been on Aromasin for 4.5 years.  I started on Zometa infusions in 2006 immediately following chemo and radiation txs and have now had a total of 10 infusions with my 11th and final dose scheduled for July.

I know that my oncologist will have an opinion on the recent study data and I will be very interested to hear her perspective as it relates to me and my cancer presentation specifically.  Obviously, each of us has to be treated uniquely and with therapy that is designed to target our BC pathology and presentation.  I still hold out strong hope that Zometa will be found to be a powerful cancer treatment weapon for many of us.  I am not inclined to disregard its usefulness based solely on the Azure trial but hope to see a trend revealed by future studies that can refine under what circumstances Zometa is best used.

Its not time to give up on Zometa yet. I believe the jury is still out and there is just too much positive data to disregard at this point. I do believe, however that it is wise to have ongoing discussions with your oncologists to help understand why it may be more appropriate for some and not others.  

Here is some positive data just released

2010: ABSTRACT #P5-11-02: The Carry-Over Effect of Adjuvant Zoledronic Acid: Comparison of 48- and 62-Month Analyses of ABCSG-12 Suggests That the Benefits of Combining Zoledronic Acid with Adjuvant Endocrine Therapy Persist Long after Completion of Therapy[San Antonio Breast Cancer Symposium]

Background: ABCSG-12 examined the efficacy of ovarian suppression using goserelin combined with tamoxifen (TAM) or anastrozole (ANA) ± zoledronic acid (ZOL) in premenopausal patients with endocrine-responsive early breast cancer. Results: at 48 months and at 62 months show that adding ZOL significantly improved disease-free survival (DFS) and reduced disease recurrence.
Methods: Premenopausal patients with endocrine-responsive early breast cancer (N = 1,803) were randomized to goserelin (3.6 mg q28d) and TAM (20 mg/d) or ANA (1 mg/d) ± ZOL (4 mg q6mo) for 3 years. Endpoints included DFS and overall survival, both analyzed using log-rank test and Cox models.
Results: At 48 months' median follow-up, ZOL significantly reduced the risk of DFS events by 36% versus no-ZOL (hazard ratio [HR] = 0.64; P = .01); this was maintained at 62 months' follow-up (HR = 0.68; P = .009). In addition, the trend toward reduced risk of death with ZOL was maintained at both 48 months (HR = 0.60; P = .11) and 62 months (HR = 0.66; P = .10) compared with no-ZOL. Patients receiving ZOL also had fewer distant recurrences compared with no-ZOL: 29 versus 41 events at 48 months, and 44 versus 56 events at 62 months. No significant renal adverse events or confirmed cases of osteonecrosis of the jaw (ONJ) have been reported.
Conclusions: Comparisons of 48- and 62-month data suggest a possible carry-over of the ZOL anticancer benefit 2 years after treatment completion. Additional analyses will be presented, including disease outcomes during therapy and after treatment, as well as overall survival

I'm still wondering if I'll be able to get the zometa, too.  Not because of the cost--my onc was going to prescribe it and she said if she prescribes it, it will be covered, but now. . . who knows if she will even still prescribe it.  I got my dental clearance last week and emailed to let her know I was finally ready to start.  I still haven't heard back from her--I'm assuming it's because of the new controversy (but I could just be being a big pessimist and it might actually be because of the holidays.)  I'm going to give her tomorrow, but I think on Tuesday, I'll either email her again or even call her office.  I hate being a pest, but I really want that zometa!

Peace of mind is priceless, and that's what second opinions give us, right?

The ABCSG study looked at women who were pre-menopausal, never had chemo, but on ovarian suppression (zolodex / goserilin), and they benefitted from zometa and continue to benefit after continued follow up.  This is not contradicted by the other study in which premenopausal women were not on ovarian suppression (and did not receive benefit from zometa).

Why would the chemo vs. no chemo affect much?  Does anyone know?  I understand why the ovarian suppression would because of the estrogen involvement, but why the chemo?  Would it be because chemo pushes many premenoupausal women into chemo-pause?