Schering-Plough Announces Phase II and III Data for Corifollitropin Alfa
2009年7月1日 - 10:00PM
PRニュース・ワイアー (英語)
Single-dose of investigational sustained follicle stimulant
achieves similar efficacy to daily injections of follitropin beta
given over a one week period in Phase III Study AMSTERDAM, July 1
/PRNewswire-FirstCall/ -- Schering-Plough Corp., (NYSE: SGP) today
announced results from the Phase III ENGAGE clinical trial
demonstrating that a single injection of corifollitropin alfa,
first in the class of sustained follicle stimulants, achieved
similar efficacy to recombinant follicle stimulating hormone (rFSH)
given once daily for seven days. The ENGAGE data was presented
along with data from the Phase III ENSURE trial and the Phase II
REALIZE trial at the 25th annual meeting of the European Society of
Human Reproduction and Embryology (ESHRE) in Amsterdam, The
Netherlands. "The burden of fertility treatment is a major
challenge for women experiencing difficulty conceiving," said
Thomas Koestler, executive vice president and president,
Schering-Plough Research Institute. "Schering-Plough is committed
to making fertility treatments easier, and these results
demonstrate that corifollitropin alfa in combination with a GnRH
antagonist may be an effective treatment that can reduce the number
of injections and the length of treatment protocols." ENGAGE is the
largest double-blind fertility agent trial ever performed. The
ongoing pregnancy rate, the primary endpoint of the ENGAGE
non-inferiority trial, obtained in the 150 mcg corifollitropin alfa
treatment arm (38.9 percent per started cycle) was similar to that
achieved in patients receiving a daily dose of 200 IU rFSH
(follitropin beta) for seven days (38.1 percent per started
cycle).(1) ENGAGE also demonstrated that a single injection of 150
mcg corifollitropin alfa achieved similar oocyte and embryo quality
compared to a daily dose of 200 IU rFSH given for one week.(2)
Further sub-analyses of the ENGAGE trial showed a single injection
of 150 mcg corifollitropin alfa, compared to the daily rFSH
treatment arm, achieved consistently high pregnancy outcomes
regardless of fertilization procedure (in-vitro fertilization (IVF)
or intracytoplasmic sperm injection (ICSI), number of embryos
transferred (single or double), or day of embryo transfer (day
three or five), confirming the robustness of the main efficacy
outcome.(1) An additional sub-analysis of the ENGAGE data
demonstrated that endogenous luteinizing hormone (LH) levels do not
affect ongoing pregnancy rates in women undergoing controlled
ovarian stimulation (COS) with a standardized rFSH /
gonadotropin-releasing hormone (GnRH) antagonist protocol.(3) An
analysis compared data from the ENGAGE trial to data from the
ENSURE trial. The ENSURE trial used a similar protocol to ENGAGE
with identical patient inclusion criteria but different body weight
categories. It showed that exposure and ovarian response were
similar after a single-dose of 100 mcg corifollitropin alfa in
patients weighing 60 kg or less, as compared to 150 mcg
corifollitropin alfa in patients weighing more than 60 kg.(4)
Additional data from the ENSURE trial show that in patients
weighing 60 kg or less, a single dose of 100 mcg corifollitropin
alfa resulted in significantly more oocytes and an equally short
duration of treatment as those receiving 150 IU rFSH daily during
the first week of stimulation.(5) Data was also presented from the
Phase II REALIZE study, a 50 patient, open-label uncontrolled pilot
study. In this study, a single dose of 100 mcg or 150 mcg
corifollitropin alfa in a long GnRH agonist protocol was able to
support multifollicular development during the first week of
ovarian stimulation.(6) About ENGAGE ENGAGE was a non-inferiority
trial designed to compare corifollitropin alfa 150 mcg to 200 IU
rFSH (follitropin beta). A total of 1,506 patients (greater than 60
kg) at 34 IVF clinics in North America and Europe were randomized
to receive either corifollitropin alfa 150 mcg or a daily dose of
200 IU rFSH, followed by rFSH (maximum 200 IU/day) from stimulation
day eight onward, when required. Starting on stimulation day five,
all patients received 0.25 mg gonadotropin-releasing hormone (GnRH)
antagonist until triggering of final oocyte maturation by human
chorionic gonadotropin (hCG). The primary endpoint was the ongoing
pregnancy rate assessed at ten weeks or more after embryo transfer.
The number of oocytes retrieved was the co-primary endpoint. The
incidence of ovarian hyperstimulation syndrome (OHSS) was similar
between both groups, 7.0 percent in the corifollitropin alfa group
(1.9 percent severe) and 6.3 percent in the follitropin beta group
(1.3 percent severe).(1) Key Findings -- The ongoing pregnancy rate
in the 150 mcg corifollitropin alfa treatment arm (38.9 percent per
started cycle) was similar to that achieved in patients receiving
daily 200 IU rFSH (follitropin beta) (38.1 percent per started
cycle).(1) -- Corifollitropin alfa achieved similar efficacy
regardless of fertilization procedure; number of embryos
transferred; or day of embryo transfer;(1) as detailed in the table
below: Overall IVF ICSI Single Double Day 3 Day 5 N=1506 N=481
N=830 N=363 N=1013 N=850 N=506 Corifollitropin alfa 38.9% 36.5%
39.7% 34.7% 46.9% 41.7% 47.1% rFSH 38.1% 35.4% 40.3% 28.9% 44.9%
35.1% 50.6% -- The mean number of oocytes retrieved per attempt was
13.7 (+/-8.2) for the corifollitropin alfa group and 12.5 (+/-6.7)
for the rFSH group.(2) -- The mean number of good quality embryos
obtained at day 3 and day 5 was 4.6 (+/-4.3) and 2.6 (+/-3.3) in
the corifollitropin alfa group, respectively and 4.4 (+/-3.9) and
2.6 (+/-3.1) in the rFSH group, respectively.(2) About ENSURE The
ENSURE trial is a multinational (Europe/Asia), double-blind,
randomized trial; 396 patients weighing 60 kg or less were
randomized in a 2:1 ratio to treatment with either a single dose of
100 mcg corifollitropin alfa or daily 150 IU rFSH (follitropin
beta) followed by daily follitropin beta (maximum 200 IU/day) from
stimulation day eight onwards when required, to reach the criterion
for human chorionic gonadotropin (hCG) administration (at least
three follicles 17 mm or greater). Starting on stimulation day five
all patients received 0.25 mg gonadotropin-releasing hormone (GnRH)
antagonist until induction of final oocyte maturation by hCG. About
34-36 hours after induction of final oocyte maturation, oocyte pick
up followed by IVF or ICSI was performed. At embryo transfer, three
or five days after oocyte pick up, a maximum of two embryos were
transferred. The primary endpoint of the ENSURE trial was the
number of oocytes retrieved and the predefined equivalence margin
was -3 and +5 oocytes for the 95 percent confidence interval (CI)
of the difference. The incidence of moderate and severe OHSS was
3.4 percent in the corifollitropin alfa treatment arm versus 1.6
percent in the rFSH treatment group.(5) Key Findings -- The mean
(SD) number of oocytes retrieved per started cycle in the
corifollitropin alfa group was 13.3 (+/-7.3) versus 10.6 (+/-5.9)
in the reference group.(5) -- Following a single injection of
corifollitropin alfa, patients required on average another two days
of further stimulation with rFSH to reach the criterion to
administer hCG. This was equal to the average duration of
stimulation of nine days of the reference group treated with daily
rFSH.(5) About REALIZE In this single-center, open-label,
uncontrolled, pilot study, 50 women undergoing ovarian stimulation
prior to IVF or ICSI were down-regulated with daily injections of
0.1 mg of GnRH agonist (starting on cycle day 21). Ovarian
stimulation was started with a single dose of corifollitropin alfa
(100 mcg or 150 mcg) followed by daily rFSH (follitropin beta) from
stimulation day eight until the day of triggering oocyte
maturation. Final oocyte maturation was induced by administration
of hCG as soon as three follicles 17 mm or greater were present.
Vaginal progesterone was administered for luteal phase support.
Patients with proven poor response were excluded from
participation. The main endpoint of this trial was ovarian
response. The observed number of follicles, serum estradiol levels
and number of oocytes indicated a relatively high ovarian response.
Corifollitropin alfa was well tolerated and there were no serious
adverse events or cases of OHSS.(6) Key Findings -- Both the 100
mcg and 150 mcg dose groups recruited a large number of follicles
11 mm or greater with mean (SD) values of 17.5 (+/-5.5) and 18.3
(+/-6.4), respectively on the day of hCG and median serum estradiol
levels of 10,019 and 10,221 pmol/L, respectively.(6) -- The mean
(SD) number of oocytes retrieved per started cycle was 15.4
(+/-6.7) in the 100 mcg dose group and 17.8 (+/-5.1) in the 150 mcg
dose group.(6) About corifollitropin alfa Corifollitropin alfa is
an investigational product being developed as a potential treatment
in Controlled Ovarian Stimulation (COS) for the development of
multiple follicles in women participating in an Assisted
Reproductive Technology (ART) program. Corifollitropin alfa is
designed as a sustained follicle stimulant (SFS) with the same
pharmacodynamic profile as rFSH, but with a markedly prolonged
duration of FSH activity. Due to its ability to initiate and
sustain multiple follicular growth for an entire week, a single
subcutaneous injection of the recommended dose of corifollitropin
alfa may replace the first seven injections of rFSH preparation in
a COS treatment cycle. The corifollitropin alfa regimen is being
developed in a GnRH antagonist protocol. Corifollitropin alfa was
filed in the European Union in late 2008. Corifollitropin alfa
Important Safety Information The most frequently reported adverse
drug reactions during treatment with corifollitropin alfa in
clinical trials are Ovarian Hyperstimulation Syndrome (OHSS),
pelvic pain and discomfort, headache, nausea, fatigue and breast
complaints (including tenderness). They are reported with an
incidence between 1% and 6%. About Infertility Infertility is a
disease or condition that impairs the body's ability to perform the
basic function of reproduction.(7) It is often diagnosed after a
couple has not conceived after one year of unprotected, well-timed
intercourse.(8) Women over the age of 35 are encouraged to seek
diagnosis and treatment for infertility following six months of
unprotected intercourse.(9) Around 15 percent of couples of
reproductive age have a fertility problem.(8) There are many causes
of infertility including problems with the production of sperm or
eggs, with the fallopian tubes or the uterus, endometriosis,
frequent miscarriage, as well as hormonal and autoimmune (antibody)
disorders in both men and women.(8) With infertile couples, the
source of infertility lies with the male in 40 percent of cases and
40 percent with the female. The remaining 20 percent is either a
joint problem or unknown, because the cause has not been
identified. There are a variety of treatments available for
infertility; these include surgery, hormone treatments,
insemination, IVF and natural treatments, among others.(8) About
Schering-Plough Schering-Plough is an innovation-driven,
science-centered global health care company. Through its own
biopharmaceutical research and collaborations with partners,
Schering-Plough creates therapies that help save and improve lives
around the world. The company applies its research-and-development
platform to human prescription, animal health and consumer health
care products. Schering-Plough's vision is to "Earn Trust, Every
Day" with the doctors, patients, customers and other stakeholders
served by its colleagues around the world. The company is based in
Kenilworth, N.J., and its Web site is
http://www.schering-plough.com/ SCHERING-PLOUGH DISCLOSURE NOTICE:
The information in this press release includes certain
"forward-looking statements" within the meaning of the Private
Securities Litigation Reform Act of 1995, including statements
relating to the plans for, the potential of and the potential
market for corifollitropin alfa . Forward-looking statements relate
to expectations or forecasts of future events. Schering-Plough does
not assume the obligation to update any forward-looking statement.
Many factors could cause actual results to differ materially from
Schering-Plough's forward-looking statements, including the
regulatory process for approval of corifollitropin alfa among other
uncertainties. For further details about these and other factors
that may impact the forward-looking statements, see
Schering-Plough's Securities and Exchange Commission filings,
including Part II, Item IA. "Risk Factors" in Schering-Plough's
first quarter 2009 10-Q, filed May 1, 2009. Endnotes 1.
Fernandez-Sanchez M et al, Equally high ongoing pregnancy rates
with corifollitropin alfa and recombinant FSH irrespective of
variations in ART procedures. Oral presentation at 25th European
Society of Human Reproduction and Embryology (ESHRE) on June 29,
2009. Abstract no. O-005 2. Behr B, et al Corifollitropin alfa
versus recombinant FSH treatment in controlled ovarian stimulation:
equal efficacy in terms of oocyte and embryo quality. Oral
presentation at 25th European Society of Human Reproduction and
Embryology (ESHRE) on June 29, 2009. Abstract no O-003 3. Doody K
et al, Puregon reference-'Success rates of a fixed rFSH/GnRH
antagonist protocol are not affected by enodgenous LH levels. Oral
presentation at 25th European Society of Human Reproduction and
Embryology (ESHRE) on July 1, 2009. Abstract no. O-255 4. Ledger W
et al, Two doses of corifollitropin alfa allow for similar exposure
and ovarian response in patients weighing less than or equal to 60
kg and > 60 kg. Oral presentation at 25th European Society of
Human Reproduction and Embryology (ESHRE) on July 1, 2009. Abstract
no. O-282 5. Hillensjo T et al, Corifollitropin alfa versus
recombinant FSH in a GnRH antagonist protocol for controlled
ovarian stimulation in women weighing 60 kg or less. Oral
presentation at 25th European Society of Human Reproduction and
Embryology (ESHRE) on June 29, 2009. Abstract no. O-004 6. Fatemi
HM et al, The first pilot study with corifollitropin alfa in a long
GnRH agonist protocol indicates the development of a large cohort
of follicles during the first week of ovarian stimulation. Oral
presentation at 25th European Society of Human Reproduction and
Embryology (ESHRE) on July 1, 2009. Abstract no. O-283 7.
Frequently Asked Questions About Infertility. American Society for
Reproductive Medicine Web site.
http://www.asrm.org/Patients/faqs.html. Accessed May 14, 2009 8.
http://www.icsi.ws/about_infertility. Accessed May 14, 2009 9.
Frequently Asked Questions; Questions about Infertility. Centre for
Fertility and Reproductive Medicine. http://www.csmc.edu/3830.html.
Accessed May 14, 2009 DATASOURCE: Schering-Plough CONTACT: Media,
Lisa Ellen, +1-908-298-7128, or Investors, Janet Barth or Joe
Romanelli, +1-908-298-7436, all of Schering-Plough Corp. Web Site:
http://www.schering-plough.com/
Copyright