CEE alone showed no overall increase in the incidence of coronary heart disease (CHD; HR, 0.91; 95% CI, 0.75–1.12) in the WHI trial, although a trend toward increased risk of peripheral arterial events (categorized as carotid artery disease, abdominal aortic aneurysm, or lower extremity arterial disease) was observed (HR, 1.32; 95% CI, 0.99–1.77) [40,41]. Risk of CHD associated with CEE therapy was somewhat increased in women aged 70 to 79 years (HR, 1.13; 95% CI, 0.82–1.54) but there was reduced risk of CHD in women aged 50 to 59 years (HR, 0.63; 95% CI, 0.36–1.09) (Table 1) [42]. In an ancillary substudy of women aged 50 to 59 years participating in the WHI trial, calcified-plaque burden in the coronary arteries, as measured by change in coronary artery calcium scores, was significantly lower with CEE vs. PBO (p = 0.02) [43].

An increased risk of stroke and venous thromboembolic events (VTEs) was observed with CEE during the WHI trial [41], and these risks were generally greater in older women compared with younger women [44,45]. The overall HR for stroke was 1.37 (95% CI, 1.09–1.73; p = 0.008) [44]; however, CEE alone was associated with a decreased risk of stroke in a subgroup of younger women aged 50 to 59 years [42]. For VTEs, there was a 32% increased risk with CEE overall (HR, 1.32; 95% CI, 0.99–1.75); risk was lower in women aged 50 to 59 years at baseline (HR, 1.37; 95% CI, 0.70–2.68) than in women aged 70 to 79 years at baseline (HR, 3.77; 95% CI, 2.07–6.89) (Table 1) [45].

HT, particularly EPT, has also been associated with some breast-related safety concerns, which are discussed below. No increase in the risk of invasive breast cancer was initially observed for CEE compared with PBO in the WHI trial (HR, 0.80; 95% CI, 0.62–1.04) [46]. At a mean follow-up of 10.7 years, CEE showed a significantly decreased risk of breast cancer compared with PBO (HR, 0.77; 95% CI, 0.62–0.95; p = 0.02) and no increased or decreased risk of total mortality (HR, 1.02; 95% CI, 0.91–1.15) [47].

In contrast to CEE alone, CEE/MPA was associated with a 29% increase in the incidence of CHD (HR, 1.29; 95% CI, 1.02–1.63; p < 0.05) in the WHI trial [39]. Further analyses have shown that the risk of CHD correlates with the timing of CEE/MPA initiation, with increased risk of CHD observed for women who were ≥20 years past menopause (HR, 1.66; 95% CI, 1.14–2.41) while younger women <10 years past the onset of menopause at HT initiation showed a risk of CHD comparable to PBO (HR, 0.88; 95% CI, 0.54–1.43); this trend toward decreased risk with decreasing time since menopause was statistically significant (p = 0.05) [42]. When analyzed by age at initiation of CEE/MPA, CHD risk remained consistent across age groups (Table 1) [42].

Similar to CEE alone, CEE/MPA was also associated with an increased risk of stroke and VTEs during the WHI trial [39], with risks generally greater in older vs. younger women [48,49]. The overall HR for stroke was 1.31 (95% CI, 1.02–1.68) for CEE/MPA [49], with an increased risk in the subgroup of younger women aged 50 to 59 years (Table 1) [42]. When stroke risk data from the CEE and CEE/MPA studies were combined, there was no significant increase in the risk of stroke in this subgroup (HR, 1.13; 95% CI, 0.73–1.76). For VTEs, greater risk was observed with CEE/MPA, which showed a 2-fold increase (HR, 2.06; 95% CI, 1.57–2.70), compared with the 32% increase with CEE described above [45,48]. The HR for VTEs in women aged 50 to 59 years at baseline was lower (2.27 [95% CI, 1.19–4.33]) compared with that for women aged 70 to 79 years at baseline (7.46 [95% CI, 4.32–14.38] for EPT) (Table 1) [48]. For women aged 50 to 59 years at randomization, the absolute excess risk of VTEs with either CEE or CEE/MPA is considered rare [9].

As mentioned above, EPT has been associated with some breast-related safety concerns. HT has been shown to increase mammographic breast density in postmenopausal women, with EPT having a greater effect on breast density compared with ET [50,51,52,53]. High mammographic breast density has been shown to be a risk factor for breast cancer [54], as confirmed in a recent systemic meta-analysis [55]; however, this relationship is not well understood. High breast density may also decrease the sensitivity of mammograms for detecting breast abnormalities [56]. In the WHI trial, CEE/MPA was associated with a 26% increase in the incidence of invasive breast cancer (HR, 1.26; 95% CI, 1.00–1.59) [39,57] and with increased breast cancer mortality (HR, 1.96; 95% CI, 1.00–4.04) [58] compared with PBO. The increase in absolute risk of invasive breast cancer for CEE/MPA compared with PBO was 8 cases per 10,000 women-years, which is considered rare [9].

EPT has also been associated with some tolerability issues including increased incidences of breast pain and irregular vaginal bleeding [35,59,60]. In the WHI trial, women receiving CEE/MPA who were asymptomatic at baseline were significantly more likely to develop breast tenderness than women receiving PBO (p < 0.001) [60]; additional analyses have also linked new-onset breast tenderness after initiating CEE/MPA (but not CEE) to an increased risk of breast cancer (HR, 1.33; 95% CI, 1.02–1.72; p = 0.03) [61]. Vaginal bleeding was reported by 51% of women on CEE/MPA and only 5% of women on PBO at 6 months during the WHI trial [60]. Likewise, in the Heart and Estrogen/Progestin Replacement Study, women receiving CEE/MPA were more likely to experience bleeding and breast symptoms than those receiving PBO [35]. In the Postmenopausal Estrogen/Progestin Interventions Trial, breast tenderness was associated with EPT but not ET [18]. In a retrospective study to determine compliance with HT among 821 women attending a menopause clinic, the most common reason women discontinued therapy was irregular vaginal bleeding (23%) [59].

The North American Menopause Society currently recommends that HT be used at the lowest effective dose to treat postmenopausal women for whom the benefits of treatment outweigh the risks [9]. Overall, the benefit-to-risk ratio for HT, particularly ET, is favorable for younger women initiating therapy close to the onset of menopause than for older women who are many years postmenopause [9]. In general, when a specific population is carefully chosen, ET is not associated with an increased risk of many of these safety concerns. Assessment of the benefits and risks of HT for each individual woman is therefore important for determining whether HT may be appropriate.

Review of the clinical data above suggests that many of the concerns associated with HT appear to be related to the progestin component, as CHD risk, increased breast density, breast cancer risk, breast pain, and irregular vaginal bleeding are more often associated with EPT (particularly CEE/MPA) than with ET (i.e., CEE alone). These effects are broadly consistent with the known pharmacologic and physiologic effects of progestins. For example, in normal menstrual cycles in pre-menopausal women, progesterone acts to protect the endometrium from the proliferative effect of estrogens, but also promotes menstrual bleeding [62]. Moreover, there are differential effects with different types of progestins. In a French study that compared the association between different HTs and breast cancer risk, there was no association between route of estrogen administration and risk; however, risk of breast cancer with estrogen-progesterone compared with women who had never used HT (RR, 1.00; 95% CI, 0.83–1.22) was similar to the risk with estrogen alone (RR, 1.29; 95% CI, 1.02–1.65) and significantly lower than the risk with estrogen-other progestogens, including MPA (RR, 1.69; 95% CI, 1.50–1.91; p for homogeneity <0.001) [63]. Therefore, alternatives to progestin are needed that will protect the endometrium while avoiding other progestin-associated effects and preserving the desired effects of estrogens in postmenopausal women.

The key issues a potential TSEC should address include endometrial and breast protection without counteracting the positive effects of estrogens on the central nervous system, skeleton, and vagina. Because each SERM and CE pairing will exhibit a different tissue selectivity profile, some pairings may not adequately achieve these goals. Results from preclinical studies evaluating various SERM/CE combinations further support this concept.

Preclinical studies assessing different SERM/CE combinations have shown promising results for the pairing of bazedoxifene (BZA) with CE, while data do not support the combination of CE with other SERMs. In mature/reproductively competent, ovariectomized (OVX) rats, coadministration of BZA with CE prevented CE-induced increases in uterine wet weight and preserved BMD [70,71]. Studies in OVX, sexually immature mice showed that BZA was more effective than raloxifene (RLX) and lasofoxifene (LAS) in inhibiting CE-induced increases in uterine wet weight [72]. In this model, BZA also demonstrated less agonist activity in the mammary gland and was a more effective antagonist of CE-induced breast stimulation than RLX and LAS [72]. Moreover, the addition of BZA did not inhibit the efficacy of CE in reducing tail skin temperature in a model of VMS [70].

Taken together, these preclinical data suggest that BZA/CE is a promising TSEC pairing, while the combination of RLX or LAS with CE may not be suitable, as these pairings cause unacceptable uterine stimulation. Published clinical studies of RLX combined with oral or transdermal estrogens further reinforce these preclinical findings and show endometrial stimulation with this SERM/estrogen combination [73,74,75]. In 2 clinical trials evaluating the combination of RLX and an oral estrogen (the first with 17β-estradiol [73] and the second with esterified CE) [75], both showed an increase in endometrial thickness from baseline after 52 weeks and 3 months of therapy, respectively. Another study reported a reduction in endometrial thickness with RLX plus PBO (−0.9 mm) compared with an increase in endometrial thickness with RLX plus low-dose transdermal estradiol after 8 weeks of therapy (0.8 mm; p = 0.021) [74]. In contrast, studies of other estrogen formulations (e.g., 17β-estradiol percutaneous or vaginal ring) administered in combination with RLX did not show signs of endometrial stimulation [76,77]. Based on these findings, BZA/CE was selected for further development and is the first TSEC in clinical development.

The effect of BZA/CE on VMS was evaluated in the SMART-1 trial in a subset of women with ≥7 moderate-to-severe hot flushes daily at baseline (n = 216) and in the SMART-2 trial (n = 310) [80,82]. In both studies, BZA 20 mg/CE 0.45 and 0.625 mg showed significantly greater decreases from baseline in the mean daily number and severity of hot flushes compared with PBO at 12 weeks (p < 0.05 for all; Figure 1 and Table 3). The efficacy of BZA/CE on VMS was sustained over 2 years of treatment in the SMART-1 trial [87]. In the SMART-2 trial, the efficacy of BZA/CE in reducing the frequency and severity of hot flushes compared with PBO was observed as early as Week 3; both BZA/CE doses also showed significantly higher percentages of subjects with at least a 50% or 75% decrease in the number of moderate-to-severe hot flushes at Weeks 4 and 12 compared with PBO (p < 0.001). Moreover, in a subanalysis of the SMART-2 study, the number of hot flush symptom-free days was significantly increased with both BZA/CE doses vs. PBO (p < 0.0001) over 12 weeks of therapy [89].

Quality of life and patient satisfaction tools were also used to assess the efficacy of BZA/CE on VMS in the SMART-2 study. Significant improvements were reported with BZA 20 mg/CE 0.45 and 0.625 mg at 12 weeks compared with PBO in the vasomotor function domain of the MENQOL questionnaire and significantly greater satisfaction in the ability to control hot flushes during the day and night according to the Menopause Symptoms Treatment Satisfaction Questionnaire (MS-TSQ) [83]. A range of components of the Medical Outcomes Study (MOS) sleep scale also showed significant improvements with BZA/CE vs. PBO, including significant decreases in sleep disturbance (effect size [95% CI] vs. PBO: −0.65 [−0.98 to −0.31] for BZA 20 mg/CE 0.45 mg, −0.75 [−1.08 to −0.41] for BZA 20 mg/CE 0.625 mg) and significant increases in sleep adequacy (effect size [95% CI] vs. PBO: 0.55 [0.22 to 0.88] for BZA 20 mg/CE 0.45 mg, 0.59 [0.25 to 0.92] for BZA 20 mg/CE 0.625 mg) [83]. In summary, BZA/CE was associated with a clinically meaningful reduction in VMS, comparable to that observed with HT. Moreover, this efficacy was also correlated with improvements in sleep and menopause-related quality of life.

The efficacy of BZA/CE on measures of VVA was assessed in the SMART-1 trial in a subset of women with ≤5% superficial cells at screening who had a baseline and ≥1 on-therapy measurement (n = 1,867) [80]. In the SMART-3 trial, VVA parameters were evaluated in subjects who had a baseline and ≥1 on-therapy value for the parameter being assessed (n = 617, n = 637, and n = 634, respectively, for assessments of vaginal epithelial maturation, vaginal pH, and the most bothersome VVA symptom) [85]. Significantly greater increases from baseline in the mean proportion of superficial cells compared with PBO were observed for BZA 20 mg/CE 0.625 mg at 24 months in the SMART-1 trial and for BZA 20 mg/CE 0.45 and 0.625 mg at 12 weeks in the SMART-3 trial (p < 0.01 vs. PBO for all; Table 3). Both BZA/CE doses also showed significantly greater improvements from baseline in the mean proportions of intermediate and parabasal cells compared with PBO at 24 months and 12 weeks, respectively, in the SMART-1 and SMART-3 studies (p < 0.01 vs. PBO for all; Table 3). In the SMART-1 trial, the incidence of dyspareunia was significantly lower for subjects who received BZA 20 mg/CE 0.45 and 0.625 mg during Weeks 9 to 12 compared with those who received PBO (p < 0.05). In the SMART-2 trial, both BZA/CE doses showed a significantly greater improvement from baseline in vaginal dryness at Week 12 vs. PBO (p < 0.05). BZA 20 mg/CE 0.625 mg also showed a significantly greater decrease from baseline vs. PBO in vaginal pH (p < 0.001) and in the subjects’ most bothersome VVA symptom (p < 0.05) at Week 12. Taken together, these data support the ability of BZA/CE to improve vaginal health for non-hysterectomized postmenopausal women.

The SMART-1 trial included 2 osteoporosis substudies [79]. Substudy I (n = 1,454) enrolled women who had a BMD T-score between −1 and −2.5 at screening and ≥1 additional risk factor for osteoporosis, and whose last menstrual period (LMP) was >5 years prior to screening. Substudy II (n = 861) enrolled women with ≥1 risk factor for osteoporosis whose LMP was between 1 and 5 years prior to screening. In both substudies, all BZA/CE doses showed significantly greater increases from baseline in lumbar spine (p < 0.001) and total hip (p < 0.01) BMD at 12 and 24 months compared with PBO, which showed decreases from baseline (Table 3). The BZA/CE groups had significantly higher percentages of responders for lumbar spine BMD (defined as subjects who had no change or an increase from baseline in lumbar spine BMD at Months 12 and 24) compared with PBO in both substudies (p < 0.001). Substudy II also evaluated BTM, with all BZA/CE doses showing a significantly greater reduction from baseline in serum levels of osteocalcin and C-telopeptide (p < 0.001) compared with PBO at all time points assessed. These data for BZA/CE are supported by the established efficacy of each agent alone in osteoporosis. Single-agent BZA 20 and 40 mg/day significantly reduced the risk of new vertebral fractures compared with PBO in a large 3-year, phase 3 study; in a post hoc subgroup analysis of women at higher risk for fracture, BZA 20 mg was associated with a 50% reduction in nonvertebral fracture risk compared with PBO (p = 0.02) and of 44% compared with RLX 60 mg (p = 0.05) [90]. Likewise, as mentioned previously, ET showed significant reductions in total fracture risk during the WHI trial compared with PBO [27]. Taken together, these results suggest that BZA/CE may provide benefits in terms of fracture risk reduction in the postmenopausal osteoporosis population.

BZA/CE was associated with improvement in quality of life and sleep. The effects of BZA/CE on sleep parameters were evaluated in the SMART-2 trial using the MOS sleep scale in randomized subjects who received ≥1 dose of study medication and had a baseline and ≥1 on-therapy measurement [83]. At Week 12, BZA 20 mg/CE 0.45 and 0.625 mg showed significant improvements in various sleep parameters including time to fall asleep, sleep disturbance, sleep adequacy, and sleep problems indexes I and II compared with PBO (p < 0.001; Table 3). BZA 20 mg/CE 0.625 mg also showed a significant improvement in sleep quantity vs. PBO (p = 0.01). Based on regression analysis, improvements in sleep parameters were significantly associated with reductions in the frequency of moderate-to-severe hot flushes.

Quality of life was assessed using the MENQOL questionnaire in the SMART-2 and SMART-3 trials in randomized subjects who received ≥1 dose of study medication and had a baseline and ≥1 on-therapy measurement [83,84]. In both trials, BZA 20 mg/CE 0.45 and 0.625 mg showed clinically significant improvements in vasomotor function and total MENQOL scores at 12 weeks compared with PBO (p ≤ 0.001; Table 3). Significant improvement in sexual function score was observed for BZA 20 mg/CE 0.625 mg in the SMART-2 trial and for both BZA/CE doses in the SMART-3 trial compared with PBO (p < 0.01 for all). BZA 20 mg/CE 0.625 mg also showed significant improvements vs. PBO in physical function score in both trials, and in psychosocial score in the SMART-2 trial (p < 0.0 for all). In the SMART-3 trial, sexual function was also evaluated using the Arizona Sexual Experiences (ASEX) scale. At Week 12, both BZA/CE doses showed significant improvement in ease of lubrication compared with PBO (p < 0.05).

In the SMART-2 and SMART-3 trials, satisfaction with treatment was evaluated using the MS-TSQ in subjects who received ≥1 dose of study medication and had ≥1 on-therapy measurement [83,84]. In both trials, significantly higher proportions of subjects who received BZA/CE reported overall satisfaction with treatment at Week 12 compared with those who received PBO (SMART-2 trial, 73.5% to 78.2% for BZA/CE vs. 44.4% for PBO; SMART-3 trial, 62.6% to 69.4% for BZA/CE vs. 47.4% for PBO; p < 0.05 for all; Table 3). BZA/CE-treated subjects reported significantly greater satisfaction than those who received PBO with the ability to control hot flushes during the day and night, the effect on quality of sleep, and the effect on mood or emotions (p < 0.05 for all).

BZA/CE treatment has been shown in the SMART trials to be generally safe and well tolerated in postmenopausal women with a uterus. Across the SMART-1, SMART-2, and SMART-3 trials, no significant differences were observed between the BZA/CE and PBO groups in the overall incidences of adverse events (AEs) or study discontinuations due to AEs (Table 4) [80,82,85,91].