FEMARA (letrozole tablets) Breast Cancer Research: The MA-17 Breast Cancer Study & BIG 1-98 Clinical Trial

· What Is FEMARA?

· Why FEMARA?

· How To Take FEMARA

· How FEMARA Works

· Research

Research

Novartis Oncology, the makers of FEMARA, never stop searching for scientific discoveries that may benefit the lives of cancer patients, including women with breast cancer and their families, friends and loved ones.

Original studies first showed FEMARA to be an effective treatment for postmenopausal women with advanced breast cancer¹. Since 1997, two large, international clinical trials —BIG 1-98 and MA-17— have taken place that evaluated the efficacy of FEMARA for women with early stage breast cancer. Both studies provided important results to the breast cancer community and the excitement of each garnered numerous mentions in The New York Times, the Wall Street Journal and more.

Adjuvant therapy/ BIG 1-98 Trial
This international study involving more than 8,000 postmenopausal women shows that FEMARA is more effective than tamoxifen at reducing the risk of recurrence in women with early stage breast cancer based on 24 months of treatment¹. Due to the results from this ongoing trial, many oncologists are prescribing FEMARA over tamoxifen—the "gold standard" for more than 30 years. Click here for more information on the BIG 1-98 Trial.

Extended Adjuvant therapy/ MA-17
This international study involving more than 5,000 women shows that, compared to placebo, FEMARA significantly reduces the risk of recurrence for postmenopausal women who have completed 5 years of tamoxifen. As a result of this study, women now have a treatment option that picks up where tamoxifen leaves off¹. FEMARA is the first and only post-tamoxifen treatment of its kind. Click here for more information on the MA-17 study.

¹ Femara Prescribing Information, December 2006. Novartis Pharmaceuticals Corporation.

Indication

Femara® (letrozole tablets) is approved for the adjuvant (following surgery) treatment of postmenopausal women with hormone receptor–positive early stage breast cancer. The benefits of Femara in clinical trials are based on 24 months of treatment. Further follow-up will be needed to determine long-term results, safety and efficacy.

Femara is also approved for the extended adjuvant treatment of early stage breast cancer in postmenopausal women who are within three months of completion of five years of tamoxifen therapy. The benefits of Femara in clinical trials are based on 24 months of treatment. Further follow-up will be needed to determine long-term results, including side effects.

In addition, Femara is approved for the treatment of postmenopausal women with estrogen receptor–positive or estrogen receptor–unknown breast cancer that has spread to another part of the body (metastatic cancer).

Ask your oncologist if Femara is right for you.

Important Safety Information

You should not take Femara if you are premenopausal. Your doctor should discuss the need for adequate birth control if you have the potential to become pregnant, if you are not sure of your postmenopausal status, or if you recently became postmenopausal. Femara is only indicated for postmenopausal women. Talk to your doctor if you're allergic to Femara or any of its ingredients. Femara should be used with caution by nursing mothers. You should not take Femara if you are pregnant as it may cause fetal harm. Some women reported fatigue and dizziness with Femara. Until you know how it affects you, use caution before driving or operating machinery. Some patients taking Femara had an increase in cholesterol. Additional follow-up is needed to determine the risk of bone fracture associated with long-term use of Femara.

In the adjuvant setting, commonly reported side effects are generally mild to moderate. Side effects that are comparable between Femara and tamoxifen include night sweats, weight gain, nausea and tiredness. Side effects seen more often with tamoxifen versus Femara were hot flashes and vaginal bleeding. Joint pain was experienced more often with Femara versus tamoxifen. The incidence of stroke was 1.1% for women on Femara and 1% for women on tamoxifen, and the incidence of other cardiovascular events was 6.6% for Femara versus 6.2% for tamoxifen. The percentage of women on Femara reporting bone fracture was 5.6% versus 4% for women on tamoxifen. The percentage of women reporting osteoporosis was 2% for Femara versus 1.1% for tamoxifen. Additional side effects for both Femara and tamoxifen are heart attack, thromboembolic events, endometrial cancer and second malignancies.

In the extended adjuvant setting, commonly reported side effects are generally mild to moderate. Those seen more often with Femara versus placebo were hot flashes (50% vs 43%), joint pain (22% vs 18%) and muscle pain (7% vs 5%). Other side effects, which were comparable to placebo, include fatigue (34% vs 32%), swelling due to fluid retention (18% vs 16%), headache (20% vs 20%), increase in sweating (24% vs 22%) and increase in cholesterol (16% vs 16%). The percentage of patients on Femara versus placebo reporting a fracture was 5.9% versus 5.5%. The percentage of patients reporting osteoporosis was 6.9% versus 5.5%. Bisphosphonates, drugs to increase bone strength, were given to 21.1% of Femara patients and 18.7% of placebo patients. Additional side effects seen in study are arthritis, dizziness, constipation, nausea and cardiovascular ischemic events.

In the metastatic cancer setting, commonly reported side effects are generally mild to moderate and may include bone pain, hot flashes, back pain, nausea, joint pain, shortness of breath, tiredness, coughing, constipation, limb pain, chest pain and headache.

Femara is a once-daily, convenient prescription tablet.

For additional safety information, please see the prescribing information.