Topline
results from exploratory Phase 2b RESPOND clinical trial of Sildenafil Cream, 3.6%
On
June 5, 2023, Daré announced topline results from its exploratory Phase 2b RESPOND clinical trial of Sildenafil Cream, 3.6% (Sildenafil
Cream) in patients with female sexual arousal disorder (FSAD). The exploratory Phase 2b RESPOND study was a multi-center, double-blind,
randomized, placebo-controlled study to evaluate the efficacy and safety of Sildenafil Cream in premenopausal patients with FSAD. The
study was a first of its kind Phase 2b clinical study that includes patient reported outcome (PRO) instruments to screen eligible women
with FSAD and included two co-primary endpoints, a secondary endpoint, and a number of exploratory endpoints to measure, among other
things, improvement in localized genital sensations of arousal, reduction in the distress that women experience with FSAD and satisfactory
sexual events.
There
are no treatments approved by the U.S. Food and Drug Administration (FDA) for FSAD and thus there are no efficacy endpoints that have
been previously validated in a Phase 3 pivotal study for potential treatments for FSAD. The exploratory Phase 2b RESPOND study also served
as a validation study of exploratory endpoints that could be candidate endpoints in a Phase 3 study of Sildenafil Cream. The FDA requested
that any PROs for use in the assessment of efficacy in a Phase 3 study be adequately validated. Part of that validation of the PROs
includes exit interviews performed as part of the exploratory Phase 2b RESPOND study to better understand qualitatively what constitutes
a meaningful change to the subjects. These qualitative assessments of meaningful change were utilized to determine which endpoints achieved
meaningful improvement in the Sildenafil Cream group. Additional psychometric analyses using the exploratory Phase 2b RESPOND
study dataset is planned to further refine and validate the measures to inform the most appropriate endpoints for use in a Phase
3 pivotal study of Sildenafil Cream.
The
exploratory Phase 2b RESPOND study began with 99 subjects in the Sildenafil Cream intent to treat population and 93 subjects in the placebo
intent to treat population, with 70 subjects in the Sildenafil Cream intent to treat population and 60 subjects in the placebo intent
to treat population completing the study, and therefore was underpowered to assess statistical significance, although certain
endpoints achieved statistical significance. During the study, participants used Sildenafil Cream and a placebo cream in their home setting
and documented their experience using PRO instruments. The study evaluated Sildenafil Cream compared to placebo cream over 12 weeks of
dosing following both a non-drug and placebo run-in period.
Daré
intends to review the data with the FDA, including discussing the data from assessments as early as the 4- and 8-week mark after randomization,
and to continue the development of Sildenafil Cream, including advancing Sildenafil Cream into a Phase 3 pivotal study for the treatment
of FSAD. Following clinical development, Daré intends to leverage the existing safety and efficacy data on the active ingredient
in Sildenafil Cream to utilize the FDA’s 505(b)(2) pathway to obtain marketing approval of Sildenafil Cream in the U.S.
Summary
of Topline Data
A
co-primary endpoint of the Phase 2b RESPOND study was to evaluate the efficacy of Sildenafil Cream compared to placebo as measured by
change from baseline to the end of the study in the Arousal-Sensation Domain of the 28-item Sexual Function Questionnaire (SFQ28). The
endpoint did not achieve statistical significance. However, the change at the end of the study in the group treated with Sildenafil Cream
was consistent with how women reported meaningful improvement in an exit interview at the end of the study.
The
other co-primary endpoint was to evaluate the efficacy of Sildenafil Cream compared to placebo as measured by change from baseline to
the end of the study in the score for feeling concerned by difficulties with sexual arousal. The change was assessed using the previously
validated Female Sexual Distress Scale – Desire, Arousal and Orgasm (FSDS-DAO) Survey. This assessment did not differentiate Sildenafil
Cream from placebo.
The
secondary endpoint was to evaluate the efficacy of Sildenafil Cream compared to placebo as measured by change from baseline to the end
of the study in the number of satisfactory sexual events based on the subjects’ response to a question answered and recorded via
electronic diary within 24 hours after each sexual event. The endpoint was selected because it can serve as a primary endpoint in a Phase
3 study based on the FDA draft 2016 guidance document for female sexual dysfunction. When measured at the 4- and 8-week mark after randomization,
subjects treated with Sildenafil Cream had a higher proportion of satisfying sexual events during the prior month (68.6% and 74.1% at
the 4- and 8-week mark, respectively) compared to those treated with placebo (47.9% and 67.9% at the 4- and 8-week mark, respectively)
(week 4 P value = 0.04).
The
exploratory endpoints (selected based on the content validity study previously conducted by SST and Daré) included endpoints related
to genital arousal, genital blood flow, lubrication, orgasm, concerns about difficulties with sexual arousal, and other assessments including
questions regarding satisfying sexual events. The exploratory endpoints were assessed at multiple periods over the course of the study
via electronic diary.
| ● | An
exploratory endpoint regarding concerns about difficulties with sexual arousal differentiated
Sildenafil Cream versus placebo. Specifically, when asked about their overall impression
of change regarding their concerns about difficulties with sexual arousal, women treated
with Sildenafil Cream were more likely to report an overall improvement. Based on responses
to the question at the 4-, 8- and 12-week mark after randomization, 44% to 49% of the subjects
treated with Sildenafil Cream reported an overall improvement compared to 37% to 44% of the
subjects treated with placebo (P value < 0.01). |
| ● | Exploratory
endpoints related to arousal lubrication and achievement and pleasure of orgasm also demonstrated
important differences between the subjects treated with Sildenafil Cream compared to placebo
as measured by change from baseline to the 8-week mark after randomization, at P value =
0.059 and P value = 0.066, respectively (trending toward significance despite the small number
of subjects in each group, n=73 in the Sildenafil Cream intent to treat group and n=64 in
the placebo intent to treat group for these assessments). |
| ● | 48.7%
of the subjects treated with Sildenafil Cream reported an increase in their overall satisfaction
with sexual activity measured at the end of the study, compared to 42.6% of the subjects
treated with placebo. |
Summary
of Cited Top Line Data
The
exploratory Phase 2b RESPOND study was underpowered to assess statistical significance, although statistical significance was
achieved on certain assessments. The following table sets forth certain data regarding the co-primary endpoints, the secondary endpoint,
and certain exploratory endpoints:
| Objective/Endpoint |
|
Measured
At |
|
Sildenafil
Cream, N(1) |
|
Placebo,
N(1) |
|
P value |
| Co-Primary:
SFQ28 Arousal Sensation Domain |
|
End
of study (week 12) |
|
70 |
|
60 |
|
>0.05 |
| Co-Primary:
FSDS-DAO Survey (Q14 only (Concerned by difficulties with sexual arousal)) |
|
End
of study (week 12) |
|
70 |
|
60 |
|
>0.05 |
| Secondary:
Proportion of Satisfactory Sexual Events per Month during Double Blind Treatment Period |
|
Week
4
Week
8
Week
12 |
|
78
73
71 |
|
68
64
61 |
|
0.04
>0.05
>0.05 |
| Exploratory:
Arousal Lubrication PROs |
|
Week
8 |
|
73 |
|
64 |
|
0.059 |
| Exploratory:
Orgasm PROs |
|
Week
8 |
|
73 |
|
64 |
|
0.066 |
| Exploratory:
Regarding Concern for FSAD Symptoms(2) |
|
Weeks
4 - 12 |
|
78 |
|
68 |
|
<0.01 |
| Exploratory:
Regarding Satisfactory Sexual Activity(2) |
|
Weeks
4 - 12 |
|
78 |
|
68 |
|
<0.01 |
| (1)
The numbers in this column represent the number of subjects included in the assessment at the indicated time point. |
| |
| (2)
This exploratory endpoint was measured periodically beginning at week 4 after randomization through the end of the study. |
Safety
Sildenafil
Cream was generally safe and well-tolerated. There were no treatment related serious adverse events and the majority of treatment related
adverse events were mild in severity.
Other
Matters
Daré
currently continues to anticipate the following upcoming milestone events for its portfolio:
| ● | 2Q-2023:
First commercial sale in the United States of XACIATO™ (clindamycin phosphate) vaginal
gel, 2%, an FDA-approved product indicated for the treatment of bacterial vaginosis in females
12 years and older; |
| ● | Mid-2023:
Initiation of patient recruitment for the planned pivotal Phase 3 clinical study of Ovaprene®,
an investigational hormone-free, monthly intravaginal contraceptive; and |
| ● | 2023:
Announcement of topline results from the ongoing Phase 1 clinical study of DARE-PDM1, an
investigational proprietary hydrogel formulation of diclofenac, a nonsteroidal anti-inflammatory
drug, being developed as a vaginally-administered treatment for primary dysmenorrhea. |
Cautionary
Statement Regarding Forward-Looking Statements
Daré
cautions you that all statements, other than statements of historical facts, contained in this report, are forward-looking statements.
Forward-looking statements, in some cases, can be identified by terms such as “believe,” “may,” “will,”
“estimate,” “continue,” “anticipate,” “design,” “intend,” “expect,”
“could,” “plan,” “potential,” “predict,” “seek,” “should,” “would,”
“contemplate,” “project,” “target,” “objective,” or the negative version of these words
and similar expressions. In this report, forward-looking statements include, but are not limited to, statements relating to Sildenafil
Cream’s potential as a safe and effective therapy for FSAD, Daré’s plans for continued clinical development of Sildenafil
Cream, the anticipated regulatory pathway for Sildenafil Cream, the potential for Sildenafil Cream to be the first FDA-approved treatment
for FSAD, the potential market opportunity for Sildenafil Cream, plans and expectations with respect to Daré’s product candidates,
including anticipated timing for the first commercial sale of XACIATO, for commencement and conduct of clinical trials and for announcement
of topline results. Forward-looking statements involve known and unknown risks, uncertainties and other factors that may cause Daré’s
actual results, performance or achievements to be materially different from future results, performance or achievements expressed or
implied by the forward-looking statements in this report, including, without limitation, risk and uncertainties related to: the risk
that topline results from a clinical trial, including the Phase 2b RESPOND study, are based on Daré’s preliminary analysis
of key efficacy and safety data and, following a comprehensive review of the study data, topline results may not accurately reflect the
complete results from the study and the differences between topline results and complete results may be significant and may adversely
impact the continued clinical development of the investigational product, including anticipated time and expense of continued development;
the risk that data from the Phase 2b RESPOND study, which assessed multiple patient reported outcomes at 4, 8 and 12 weeks after randomization,
may not be predictive of results of any future clinical study that assesses safety and efficacy of Sildenafil Cream at time points beyond
12 weeks after randomization, and the double-blind dosing period the FDA may require for a pivotal Phase 3 study of Sildenafil Cream
is unknown at this time; the risk that the FDA, other regulatory authorities, members of the scientific or medical communities or investors
may not accept or agree with Daré’s interpretation of or conclusions regarding the study data; Daré’s ability
to raise additional capital when and as needed to advance its product candidates, execute its business strategy and continue as a going
concern; the risk that positive findings in early clinical and/or nonclinical studies of a product candidate may not be predictive of
success in subsequent clinical and/or nonclinical studies of that candidate; the risk that development of a product candidate requires
more clinical or nonclinical studies than Daré anticipates; Daré’s ability to develop, obtain FDA or foreign regulatory
approval for, and commercialize its product candidates and to do so on communicated timelines; failure or delay in starting, conducting
and completing clinical trials of a product candidate; Daré’s ability to design and conduct successful clinical trials,
to enroll a sufficient number of patients, to meet established clinical endpoints, to avoid undesirable side effects and other safety
concerns, and to demonstrate sufficient safety and efficacy of its product candidates; Daré’s dependence on third parties
to conduct clinical trials and manufacture and supply clinical trial material and commercial product; the loss of, or inability to attract,
key personnel; the effects of the COVID-19 pandemic, macroeconomic conditions and geopolitical events on Daré’s operations,
financial results and condition, and ability to achieve current plans and objectives, including the potential impact of the pandemic
on Daré’s ability to timely commence, enroll, conduct and report results of its clinical trials and on the ability of third
parties on which Daré relies to assist in the conduct of its business to fulfill their contractual obligations to Daré;
the impact of pharmaceutical industry regulation and health care legislation in the United States and internationally; the risk that
developments by competitors make Daré’s product or product candidates less competitive or obsolete; difficulties establishing
and sustaining relationships with development and/or commercial collaborators; failure of Daré’s product or product candidates,
if approved, to gain market acceptance or obtain adequate coverage or reimbursement from third-party payers; Daré’s ability
to retain its licensed rights to develop and commercialize a product or product candidate; Daré’s ability to satisfy the
monetary obligations and other requirements in connection with its exclusive, in-license agreements covering the critical patents and
related intellectual property related to its product and product candidates; Daré’s ability to adequately protect or enforce
its, or its licensor’s, intellectual property rights; the lack of patent protection for the active ingredients in certain of Daré’s
product candidates which could expose its products to competition from other formulations using the same active ingredients; product
liability claims; governmental investigations or actions relating to Daré’s product or product candidates or the business
activities of Daré, its commercial collaborators or other third parties on which Daré relies; the impact of pharmaceutical
industry regulation and health care legislation in the United States and internationally; global trends toward health care cost containment;
cyber attacks, security breaches or similar events that compromise Daré’s technology systems or those of third parties on
which it relies and/or significantly disrupt Daré’s business; and disputes or other developments concerning Daré’s
intellectual property rights. Daré’s forward-looking statements are based upon its current expectations and involve assumptions
that may never materialize or may prove to be incorrect. All forward-looking statements are expressly qualified in their entirety by
these cautionary statements. For a detailed description of Daré’s risks and uncertainties, you are encouraged to review
its documents filed with the SEC including Daré’s recent filings on Form 8-K, Form 10-K and Form 10-Q. You are cautioned
not to place undue reliance on forward-looking statements, which speak only as of the date on which they were made. Daré undertakes
no obligation to update such statements to reflect events that occur or circumstances that exist after the date on which they were made,
except as required by law.