Evista (Raloxifene Hydrochloride) - Side Effects and Adverse Reactions

6  ADVERSE REACTIONS

6.1  Clinical Trials Experience

Because clinical studies are conducted under widely varying conditions, adverse reaction rates observed in the clinical trials of a drug cannot be directly compared to rates in the clinical trials of another drug and may not reflect the rates observed in practice.

The data described below reflect exposure to EVISTA in 8429 patients who were enrolled in placebo-controlled trials, including 6666 exposed for 1 year and 5685 for at least 3 years.

Osteoporosis Treatment Clinical Trial (MORE) — The safety of raloxifene in the treatment of osteoporosis was assessed in a large (7705 patients) multinational, placebo-controlled trial. Duration of treatment was 36 months, and 5129 postmenopausal women were exposed to raloxifene hydrochloride (2557 received 60 mg/day, and 2572 received 120 mg/day). The incidence of all-cause mortality was similar among groups: 23 (0.9%) placebo, 13 (0.5%) EVISTA-treated (raloxifene HCl 60 mg), and 28 (1.1%) raloxifene HCl 120 mg women died. Therapy was discontinued due to an adverse reaction in 10.9% of EVISTA-treated women and 8.8% of placebo-treated women.

Venous Thromboembolism: The most serious adverse reaction related to EVISTA was VTE (deep venous thrombosis, pulmonary embolism, and retinal vein thrombosis). During an average of study-drug exposure of 2.6 years, VTE occurred in about 1 out of 100 patients treated with EVISTA. Twenty-six EVISTA-treated women had a VTE compared to 11 placebo-treated women, the hazard ratio was 2.4 (95% confidence interval, 1.2, 4.5), and the highest VTE risk was during the initial months of treatment.

Common adverse reactions considered to be related to EVISTA therapy were hot flashes and leg cramps. Hot flashes occurred in about one in 10 patients on EVISTA and were most commonly reported during the first 6 months of treatment and were not different from placebo thereafter. Leg cramps occurred in about one in 14 patients on EVISTA.

Placebo-Controlled Osteoporosis Prevention Clinical Trials — The safety of raloxifene has been assessed primarily in 12 Phase 2 and Phase 3 studies with placebo, estrogen, and estrogen-progestin therapy control groups. The duration of treatment ranged from 2 to 30 months, and 2036 women were exposed to raloxifene HCl (371 patients received 10 to 50 mg/day, 828 received 60 mg/day, and 837 received from 120 to 600 mg/day).

Therapy was discontinued due to an adverse reaction in 11.4% of 581 EVISTA-treated women and 12.2% of 584 placebo-treated women. Discontinuation rates due to hot flashes did not differ significantly between EVISTA and placebo groups (1.7% and 2.2%, respectively).

Common adverse reactions considered to be drug-related were hot flashes and leg cramps. Hot flashes occurred in about one in four patients on EVISTA versus about one in six on placebo. The first occurrence of hot flashes was most commonly reported during the first 6 months of treatment.

Table 1 lists adverse reactions occurring in either the osteoporosis treatment or in five prevention placebo-controlled clinical trials at a frequency ≥2.0% in either group and in more EVISTA-treated women than in placebo-treated women. Adverse reactions are shown without attribution of causality. The majority of adverse reactions occurring during the studies were mild and generally did not require discontinuation of therapy.

Table 1: Adverse Reactions Occurring in Placebo–Controlled Osteoporosis Clinical Trials at a Frequency ≥2.0% and in More EVISTA-Treated (60 mg Once Daily) Women than Placebo–Treated Women ¹

	Treatment		Prevention
	EVISTA N=2557 %	Placebo N=2576 %	EVISTA N=581 %	Placebo N=584 %
Body as a Whole
Infection	A	A	15.1	14.6
Flu Syndrome	13.5	11.4	14.6	13.5
Headache	9.2	8.5	A	A
Leg Cramps	7.0	3.7	5.9	1.9
Chest Pain	A	A	4.0	3.6
Fever	3.9	3.8	3.1	2.6
Cardiovascular System
Hot Flashes	9.7	6.4	24.6	18.3
Migraine	A	A	2.4	2.1
Syncope	2.3	2.1	B	B
Varicose Vein	2.2	1.5	A	A
Digestive System
Nausea	8.3	7.8	8.8	8.6
Diarrhea	7.2	6.9	A	A
Dyspepsia	A	A	5.9	5.8
Vomiting	4.8	4.3	3.4	3.3
Flatulence	A	A	3.1	2.4
Gastrointestinal Disorder	A	A	3.3	2.1
Gastroenteritis	B	B	2.6	2.1
Metabolic and Nutritional
Weight Gain	A	A	8.8	6.8
Peripheral Edema	5.2	4.4	3.3	1.9
Musculoskeletal System
Arthralgia	15.5	14.0	10.7	10.1
Myalgia	A	A	7.7	6.2
Arthritis	A	A	4.0	3.6
Tendon Disorder	3.6	3.1	A	A
Nervous System
Depression	A	A	6.4	6.0
Insomnia	A	A	5.5	4.3
Vertigo	4.1	3.7	A	A
Neuralgia	2.4	1.9	B	B
Hypesthesia	2.1	2.0	B	B
Respiratory System
Sinusitis	7.9	7.5	10.3	6.5
Rhinitis	10.2	10.1	A	A
Bronchitis	9.5	8.6	A	A
Pharyngitis	5.3	5.1	7.6	7.2
Cough Increased	9.3	9.2	6.0	5.7
Pneumonia	A	A	2.6	1.5
Laryngitis	B	B	2.2	1.4
Skin and Appendages
Rash	A	A	5.5	3.8
Sweating	2.5	2.0	3.1	1.7
Special Senses
Conjunctivitis	2.2	1.7	A	A
Urogenital System
Vaginitis	A	A	4.3	3.6
Urinary Tract Infection	A	A	4.0	3.9
Cystitis	4.6	4.5	3.3	3.1
Leukorrhea	A	A	3.3	1.7
Uterine Disorder 2 , 3	3.3	2.3	A	A
Endometrial Disorder	B	B	3.1	1.9
Vaginal Hemorrhage	2.5	2.4	A	A
Urinary Tract Disorder	2.5	2.1	A	A

Comparison of EVISTA and Hormone Therapy — EVISTA was compared with estrogen-progestin therapy in three clinical trials for prevention of osteoporosis. Table 2 shows adverse reactions occurring more frequently in one treatment group and at an incidence ≥2.0% in any group. Adverse reactions are shown without attribution of causality.

Table 2: Adverse Reactions Reported in the Clinical Trials for Osteoporosis Prevention with EVISTA (60 mg Once Daily) and Continuous Combined or Cyclic Estrogen Plus Progestin (Hormone Therapy) at an Incidence ≥2.0% in any Treatment Group ¹

	EVISTA (N=317)	Hormone Therapy–Continuous Combined 2 (N=96)	Hormone Therapy–Cyclic 3 (N=219)
	%	%	%
Urogenital
Breast Pain	4.4	37.5	29.7
Vaginal Bleeding 4	6.2	64.2	88.5
Digestive
Flatulence	1.6	12.5	6.4
Cardiovascular
Hot Flashes	28.7	3.1	5.9
Body as a Whole
Infection	11.0	0	6.8
Abdominal Pain	6.6	10.4	18.7
Chest Pain	2.8	0	0.5

Breast Pain — Across all placebo-controlled trials, EVISTA was indistinguishable from placebo with regard to frequency and severity of breast pain and tenderness. EVISTA was associated with less breast pain and tenderness than reported by women receiving estrogens with or without added progestin.

Gynecologic Cancers — EVISTA-treated and placebo-treated groups had similar incidences of endometrial cancer and ovarian cancer.

Placebo-Controlled Trial of Postmenopausal Women at Increased Risk for Major Coronary Events (RUTH) — The safety of EVISTA (60 mg once daily) was assessed in a placebo-controlled multinational trial of 10,101 postmenopausal women (age range 55-92) with documented coronary heart disease (CHD) or multiple CHD risk factors. Median study drug exposure was 5.1 years for both treatment groups [see Clinical Studies] . Therapy was discontinued due to an adverse reaction in 25% of 5044 EVISTA-treated women and 24% of 5057 placebo-treated women. The incidence per year of all-cause mortality was similar between the raloxifene (2.07%) and placebo (2.25%) groups.

Adverse reactions reported more frequently in EVISTA-treated women than in placebo-treated women included peripheral edema (14.1% raloxifene versus 11.7% placebo), muscle spasms/leg cramps (12.1% raloxifene versus 8.3% placebo), hot flashes (7.8% raloxifene versus 4.7% placebo), venous thromboembolic events (2.0% raloxifene versus 1.4% placebo), and cholelithiasis (3.3% raloxifene versus 2.6% placebo) [see Clinical Studies (14.3, 14.5)] .

Tamoxifen-Controlled Trial of Postmenopausal Women at Increased Risk for Invasive Breast Cancer (STAR) — The safety of EVISTA 60 mg/day versus tamoxifen 20 mg/day over 5 years was assessed in 19,747 postmenopausal women (age range 35-83 years) in a randomized, double-blind trial. As of 31 December 2005, the median follow-up was 4.3 years. The safety profile of raloxifene was similar to that in the placebo-controlled raloxifene trials [see Clinical Studies] .

6.2  Postmarketing Experience

Because these reactions are reported voluntarily from a population of uncertain size, it is not always possible to reliably estimate their frequency or establish a causal relationship to drug exposure.

Adverse reactions reported very rarely since market introduction include retinal vein occlusion, stroke, and death associated with venous thromboembolism (VTE).

REPORTS OF SUSPECTED EVISTA SIDE EFFECTS / ADVERSE REACTIONS

Possible Evista side effects / adverse reactions in 92 year old female

Reported by a physician from United States on 2011-10-06

Patient: 92 year old female

Reactions: Vitamin D Deficiency, Vaginal Prolapse, Joint Instability, Femur Fracture, Flatulence, Chronic Obstructive Pulmonary Disease, Iron Deficiency Anaemia, Carotid Artery Occlusion, Ingrowing Nail, Sinus Congestion, LOW Turnover Osteopathy, Intervertebral Disc Protrusion, Dysphagia, Pneumonia, Drug Intolerance, Anaemia, Sinus Operation, Inguinal Hernia, Glaucoma, Pain, Myelodysplastic Syndrome, Cystocele, Fibrocystic Breast Disease, Road Traffic Accident, Overdose, Gastrooesophageal Reflux Disease, Blood Iron Increased, Tooth Fracture, Blood Urea Increased, Nephrogenic Anaemia, Blood Potassium Increased, Osteoarthritis, Carotid Artery Stenosis, Blood Pressure, Hypothyroidism

Adverse event resulted in: hospitalization

Suspect drug(s):
Alendronate Sodium
    Administration route: Oral
    Start date: 2008-08-02
    End date: 2009-03-13

Evista
    Administration route: Oral
    Indication: Osteoporosis
    Start date: 2005-10-27

Actonel
    Administration route: Oral
    Indication: Osteoporosis
    Start date: 2005-08-13
    End date: 2005-11-01

Actonel
    Administration route: Oral
    Start date: 2006-04-12
    End date: 2006-04-20

Actonel
    Administration route: Oral
    Start date: 2004-09-28
    End date: 2004-11-01

Fosamax
    Administration route: Oral
    Start date: 2001-03-08

Fosamax
    Administration route: Oral
    Indication: Osteoporosis
    Start date: 2001-03-13
    End date: 2004-09-28

Fosamax
    Administration route: Oral
    Start date: 2005-07-13
    End date: 2010-01-11

Fosamax
    Administration route: Oral
    Start date: 1999-01-01
    End date: 2001-03-13

Alendronate Sodium
    Administration route: Oral
    Indication: Osteoporosis
    Start date: 2008-06-07
    End date: 2008-08-01

Possible Evista side effects / adverse reactions in 102 year old female

Reported by a consumer/non-health professional from United States on 2011-10-14

Patient: 102 year old female

Reactions: Death

Adverse event resulted in: death

Suspect drug(s):
Evista

Possible Evista side effects / adverse reactions in 88 year old female

Reported by a physician from Japan on 2011-10-26

Patient: 88 year old female

Reactions: Bile Duct Stone, Enterocolitis, Diverticulum Intestinal, Arrhythmia, Pyelonephritis

Adverse event resulted in: hospitalization

Suspect drug(s):
Amlodipine Besylate
    Dosage: 5 mg, 1x/day
    Administration route: Oral
    Indication: Hypertension
    Start date: 2009-10-21

Aricept
    Dosage: 5 mg, daily
    Administration route: Oral
    Indication: Dementia Alzheimer's Type
    Start date: 2010-10-20
    End date: 2011-03-23

Evista
    Dosage: 60 mg, 1x/day
    Administration route: Oral
    Indication: Osteoporosis
    Start date: 2007-11-07

ONE-Alpha
    Dosage: 1 ug, 1x/day
    Administration route: Oral
    Indication: Osteoporosis
    Start date: 2007-11-07