Positive Phase III Results for Genentech’s Emicizumab in Hemophilia A Published in The New England Journal
of Medicine
– HAVEN 1 showed emicizumab reduced bleed rate by 87 percent compared with on-demand bypassing agents
–
– All 12 secondary endpoints in HAVEN 1 were positive, including an intra-patient comparison that showed
emicizumab reduced bleed rate by 79 percent compared to prior prophylactic bypassing agents –
– Data from HAVEN 1 in adults and adolescents and interim data from HAVEN 2 in children with hemophilia A
with inhibitors are being presented today at the 26th International Society on Thrombosis and Haemostasis (ISTH) Congress –
– Data from both studies have been submitted to FDA and EMA for approval consideration –
Genentech, a member of the Roche Group (SIX: RO, ROG; OTCQX: RHHBY), announced today that data from HAVEN 1, a Phase III study
evaluating once-weekly subcutaneous emicizumab prophylaxis (preventative) in adults and adolescents with hemophilia A with
inhibitors, were published in The New England Journal of Medicine (NEJM). The primary endpoint showed a
clinically meaningful and statistically significant reduction in treated bleeds of 87 percent (risk rate [RR]=0.13, p<0.0001)
with emicizumab prophylaxis compared with on-demand (no prophylaxis; episodic use only) bypassing agents (BPAs). All 12 secondary
endpoints were positive, including a statistically significant reduction of 79 percent (RR=0.21, p=0.0003) in treated bleeds in a
first-of-its-kind intra-patient analysis in a subset of patients comparing two prophylaxis regimens (emicizumab and BPAs). Data
from HAVEN 1 and the interim analysis of the Phase III HAVEN 2 study of emicizumab in children are being presented at the 26th
International Society on Thrombosis and Haemostasis (ISTH) Congress today.
“Nearly one in three people with hemophilia A develop inhibitors to standard factor VIII therapy, leaving them at greater risk
of life-threatening bleeds and long-term joint damage,” said Sandra Horning, M.D., chief medical officer and head of Global Product
Development. “Based on the bleed reduction shown in the HAVEN 1 and HAVEN 2 studies, we believe emicizumab has the potential to
make a meaningful difference for people with hemophilia A with inhibitors, while also reducing the burden of managing the condition
with a subcutaneous, once-weekly administration.”
Further data from HAVEN 1 showed that, after a median observation time of 31 weeks, substantially more patients experienced zero
bleeds with emicizumab prophylaxis than with on-demand BPAs across all bleed measurements, including zero treated bleeds (62.9
percent vs. 5.6 percent), zero treated spontaneous bleeds (68.6 percent vs. 11.1 percent), zero treated joint bleeds (85.7 percent
vs. 50.0 percent), zero treated target joint bleeds (94.3 percent vs. 50.0 percent) and zero bleeds overall, which includes all
treated and non-treated bleeds (37.1 percent vs. 5.6 percent). A clinically meaningful and statistically significant improvement in
health-related quality of life (HRQoL) measured at 25 weeks, using two validated instruments (Haem-A-QoL and EQ-5D-5L), was also
observed.
In an additional study arm (Arm C, n=49), patients who had previously received BPA prophylaxis were treated with emicizumab
prophylaxis. A subset of patients in this arm (n=24) had previously participated in a non-interventional study (NIS), allowing for
a first-of-its-kind intra-patient analysis comparing two prophylaxis regimens. This analysis showed a 79 percent (RR=0.21,
p=0.0003) reduction in treated bleeds in patients receiving emicizumab compared with their prior BPA prophylaxis during the NIS.
Data also showed that 70.8 percent of patients in this subset experienced zero treated bleeds with emicizumab prophylaxis, whereas
only 12.5 percent of these patients had experienced zero bleeds with their prior BPA prophylaxis during the NIS.
“The HAVEN 1 study is one of the most robust clinical studies conducted to date in people with hemophilia A with inhibitors to
factor VIII, including a first ever intra-patient comparison to prior prophylaxis with bypassing agents,” said Professor Johannes
Oldenburg, Institute of Experimental Haematology and Transfusion Medicine, University of Bonn, Germany. “The reduction in bleeding
events across all measures seen with emicizumab compared to either on-demand or prophylactic bypassing agents supports that it may
be one of the most significant scientific innovations in the treatment of hemophilia A in over 30 years.”
Adverse events (AEs) occurring in five percent or more of patients treated with emicizumab were local injection site reactions,
headache, fatigue, upper respiratory tract infection and joint pain (arthralgia). As previously reported, serious adverse events of
thromboembolic events (TE) and thrombotic microangiopathy (TMA) occurred in two patients and three patients, respectively, while
receiving emicizumab prophylaxis. One event occurred after the clinical cut-off date for the primary analysis. The common aspect of
these TMA and TE events is the patients were on emicizumab prophylaxis and received more than 100 u/kg/day of the BPA activated
prothrombin complex on average for 24 hours or more before the onset of the event. Two of these patients had also received
recombinant factor Vlla (rFVlla). Neither TE event required anti-coagulation therapy and one patient restarted emicizumab. The
cases of TMA observed were transient, and one patient restarted emicizumab.
Interim results from the single arm HAVEN 2 study in children younger than 12 years of age with hemophilia A with inhibitors who
received emicizumab prophylaxis are consistent with the positive results from the HAVEN 1 study. After a median observation time of
12 weeks, the study showed that only one of 19 children receiving emicizumab reported a treated bleed. There were no reported joint
or muscle bleeds.
An intra-patient comparison (n=8) in a subset of these children who were previously enrolled in the NIS showed that all
experienced a 100 percent reduction in treated bleeds following treatment with emicizumab (previous annualized bleeding rate [ABR]
ranged from 0 to 34.24); this group included seven children who had received prior BPA prophylaxis, and one who had received prior
on-demand BPA. The data also indicate that the same dose of emicizumab is appropriate for children as for adults and adolescents,
based on the levels of emicizumab in the blood (pharmacokinetics) of the children compared with the levels of emicizumab in the
blood of adults and adolescents. The most common AEs with emicizumab in the HAVEN 2 study were mild injection site reactions and
common cold symptoms (nasopharyngitis). No TE or TMA events were observed.
“Managing hemophilia A with inhibitors to factor VIII can be especially challenging for children and their caregivers. Not only
can bleeding be difficult to control, but current treatments can require frequent intravenous infusions, which can often involve
the long-term use of a central venous access device or port,” said Guy Young, M.D., director of Hemostasis and Thrombosis Program,
Children’s Hospital Los Angeles, and professor of Pediatrics, University of Southern California Keck School of Medicine, Los
Angeles, California. “The HAVEN 2 interim results indicate that emicizumab may help prevent bleeding in children with inhibitors.
Given the once-weekly subcutaneous dosing, it may also help alleviate some of the burden of hemophilia treatment for these children
and their parents.”
Data from both HAVEN 1 and HAVEN 2 have been submitted for approval consideration to the U.S. Food and Drug Administration (FDA)
and the European Medicines Agency (EMA). The FDA granted Breakthrough Therapy Designation for emicizumab in adults and adolescents
with hemophilia A with inhibitors in September 2015. Additional studies evaluating emicizumab in people with hemophilia A both with
and without inhibitors and exploring less frequent dosing regimens are ongoing.
About HAVEN 1 (NCT02622321)
HAVEN 1 is a randomized, multicenter, open-label, Phase III study evaluating the efficacy, safety, and pharmacokinetics of
emicizumab prophylaxis compared to on-demand BPA (no prophylaxis; episodic use only) in adults and adolescents with hemophilia A
with inhibitors to factor VIII. The study included 109 patients (12 years of age or older) with hemophilia A with inhibitors to
factor VIII, who were previously treated with BPAs on-demand or as prophylaxis. Patients previously treated with on-demand BPAs
were randomized in a 2:1 fashion to receive emicizumab prophylaxis (Arm A) or no prophylaxis (Arm B). Patients previously treated
with prophylactic BPAs received emicizumab prophylaxis (Arm C). Additional patients previously on BPA (on-demand or prophylaxis)
were also enrolled in a separate arm (Arm D). On-demand treatment of breakthrough bleeds with BPAs was allowed per protocol in all
arms.
The primary endpoint of the study is the number of treated bleeds over time with emicizumab prophylaxis (Arm A) compared with no
prophylaxis (Arm B). Secondary endpoints include all bleed rate, joint bleed rate, spontaneous bleed rate, target joint bleed rate,
HRQoL/health status, intra-patient comparison to bleed rate on their prior prophylaxis regimen with BPAs (Arm C) or no prophylaxis
(Arm B). The study also evaluated safety and pharmacokinetics.
A summary of the HAVEN 1 study results to be presented at ISTH is included below.
|
|
|
|
Study name |
|
|
HAVEN 1 (NCT02622321) |
Study description |
|
|
Phase III randomized, multicenter, open-label study evaluating the efficacy, safety, and
pharmacokinetics of emicizumab prophylaxis versus no prophylaxis in patients with hemophilia A with inhibitors to factor
VIII
|
Patients |
|
|
Patients with hemophilia A with inhibitors aged ≥12 years on episodic or prophylactic treatment with
bypassing agent(s) (N=109)
|
|
Study group |
|
|
No prophylaxis
(prior episodic BPAs)
(Arm B; n=18)
|
Emicizumab prophylaxis
(prior episodic BPAs)
(Arm A; n=35)
|
Treated bleeds ABR (primary endpoint) |
Annualized bleeding rate [ABR]*
(95% CI)
|
|
|
23.3
(12.33; 43.89)
|
2.9
(1.69; 5.02)
|
% reduction
(RR, p-value)
|
|
|
87% reduction
(RR=0.13, p<0.0001)
|
Median ABR
(Interquartile range; IQR)
|
|
|
18.8
(12.97; 35.08)
|
0.0
(0.00; 3.73)
|
% patients with zero bleeds (95% CI) |
|
|
5.6
(0.1; 27.3)
|
62.9
(44.9; 78.5)
|
All bleeds ABR (secondary endpoint) |
ABR*
(95% CI)
|
|
|
28.3
(16.79; 47.76)
|
5.5
(3.58; 8.60)
|
% reduction
(RR, p-value)
|
|
|
80% reduction
(RR=0.20, p<0.0001)
|
% patients with zero bleeds (95% CI) |
|
|
5.6
(0.1; 27.3)
|
37.1
(21.5; 55.1)
|
Treated spontaneous bleeds ABR (secondary
endpoint) |
ABR*
(95% CI)
|
|
|
16.8
(9.94; 28.30)
|
1.3
(0.73; 2.19)
|
% reduction
(RR, p-value)
|
|
|
92% reduction
(RR=0.08, p<0.0001)
|
% patients with zero bleeds (95% CI) |
|
|
11.1
(1.4; 34.7)
|
68.6
(50.7; 83.1)
|
Treated joint bleeds ABR (secondary endpoint) |
ABR*
(95% CI)
|
|
|
6.7
(1.99; 22.42)
|
0.8
(0.26; 2.20)
|
% reduction
(RR, p-value)
|
|
|
89% reduction
(RR=0.11, p=0.0050)
|
% patients with zero bleeds (95% CI) |
|
|
50.0
(26.0; 74.0)
|
85.7
(69.7; 95.2)
|
Treated target joint bleeds ABR (secondary
endpoint) |
ABR*
(95% CI)
|
|
|
3.0
(0.96; 9.13)
|
0.1
(0.03; 0.58)
|
% reduction
(RR, p-value)
|
|
|
95% reduction
(RR=0.05, p=0.0002)
|
% patients with zero bleeds (95% CI) |
|
|
50.0
(26.0; 74.0)
|
94.3
(80.8; 99.3)
|
Treated bleeds ABR intra-patient comparison
(Arm C patients who participated in NIS n=24; secondary endpoint)
|
Study group |
|
|
Prior prophylaxis with a BPA |
Emicizumab prophylaxis
|
ABR*
(95% CI)
|
|
|
15.7
(11.08; 22.29)
|
3.3
(1.33; 8.08)
|
% reduction
(RR, p-value)
|
|
|
79% reduction
(RR=0.21, p=0.0003)
|
Median ABR
(IQR)
|
|
|
12.0
(5.73; 24.22)
|
0.0
(0.00; 2.23)
|
% patients with zero bleeds
(95% CI)
|
|
|
12.5
(2.7; 32.4)
|
70.8
(48.9; 87.4)
|
*Negative binomial regression model |
|
Safety summary: all emicizumab participants |
Emicizumab prophylaxis |
(N=103)
|
Total number of AEs
|
|
|
|
|
198 |
Total number of participants experiencing ≥1 AE, n (%)
|
|
|
|
|
73 (70.9) |
Related AE
|
|
|
|
|
23 (22.3) |
Serious AE
|
|
|
|
|
9 (8.7) |
Grade ≥3 AE
|
|
|
|
|
8 (7.8) |
Local injection site reaction
|
|
|
|
|
15 (14.6) |
Headache
|
|
|
|
|
12 (11.7)
|
Upper respiratory tract infection
|
|
|
|
|
9 (8.7) |
Fatigue
|
|
|
|
|
6 (5.8) |
Joint pain (arthralgia)
|
|
|
|
|
6 (5.8) |
Thrombotic microangiopathy*
|
|
|
|
|
3 (2.9)
|
Serious thromboembolic event**
|
|
|
|
|
2 (1.9)
|
Death*
|
|
|
|
|
1 (<1) |
*Third TMA event occurred after primary data cut-off; patient also experienced fatal
rectal hemorrhage |
**Serious thromboembolic events comprised skin necrosis/superficial thrombophlebitis
in one participant, and cavernous sinus thrombosis in a second participant |
No participants tested positive for anti-drug antibodies (ADAs) |
|
About HAVEN 2 (NCT02795767)
HAVEN 2 is a single-arm, multicenter, open-label, Phase III study evaluating the efficacy, safety, and pharmacokinetics of
once-weekly subcutaneous administration of emicizumab. The interim analysis after a median of 12 weeks of treatment included 19
children younger than 12 years of age with hemophilia A with inhibitors to factor VIII, who require treatment with BPAs. The
objectives of the study are to evaluate the number of treated bleeds over time with emicizumab prophylaxis, safety,
pharmacokinetics, HRQoL and proxy HRQoL with aspects of caregiver burden.
A summary of the HAVEN 2 study interim results presented at ISTH is included below.
|
Study name |
|
|
HAVEN 2 (NCT02795767) |
Study description |
|
|
Phase III single-arm, multicenter, open-label study evaluating the
efficacy, safety, and pharmacokinetics of once weekly subcutaneous administration of emicizumab |
Patients |
|
|
Patients with hemophilia A with inhibitors aged <12 years old (or 12-17 if <40 kg) previously
treated with BPAs (N=20)
|
Study group |
|
|
Emicizumab prophylaxis (n=20 total; n=19 included in efficacy analyses)
|
Treated bleeds ABR |
% patients with zero bleeds
(95% CI)
|
|
|
94.7
(74.0; 99.9)
|
All bleeds ABR |
% patients with zero bleeds
(95% CI)
|
|
|
63.2
(38.4; 83.7)
|
Treated spontaneous bleeds ABR |
% patients with zero bleeds
(95% CI)
|
|
|
94.7
(74.0; 99.9)
|
Safety |
Grade ≥3 AE, n (%)
|
|
|
3 (15.0%) |
Serious AE*
|
|
|
3 (15.0%) |
Related AE**
|
|
|
3 (15.0%) |
Local injection site reaction
|
|
|
3 (15.0%) |
*Serious AEs: bleeding of the mouth and gums (mouth hemorrhage), appendicitis,
catheter site infection |
**All related AEs were mild injection site reactions |
No TE or TMA events were observed |
No participants tested positive for ADAs |
|
About emicizumab (ACE910)
Emicizumab is an investigational bispecific monoclonal antibody designed to bring together factors IXa and X, proteins required
to activate the natural coagulation cascade and restore the blood clotting process. Emicizumab can be administered by an injection
of a ready-to-use solution under the skin (subcutaneously) once weekly. Emicizumab is being evaluated in pivotal Phase III studies
in people 12 years of age and older, both with and without inhibitors to factor VIII, and in children under 12 years of age with
factor VIII inhibitors. Additional trials are exploring less frequent dosing schedules. The clinical development program is
assessing the safety and efficacy of emicizumab and its potential to help overcome current clinical challenges: the short-lasting
effects of existing treatments, the development of factor VIII inhibitors and the need for frequent venous access. Emicizumab was
created by Chugai Pharmaceutical Co., Ltd. and is being co-developed by Chugai, Roche and Genentech.
About hemophilia A
Hemophilia A is an inherited, serious disorder in which a person’s blood does not clot properly, leading to uncontrolled and
often spontaneous bleeding. Hemophilia affects around 20,000 people in the United States, with hemophilia A being the most common
form and approximately 50-60 percent of people living with a severe form of the disorder. People with hemophilia A either lack or
do not have enough of a clotting protein called factor VIII. In a healthy person, when a bleed occurs, factor VIII brings together
the clotting factors IXa and X, which is a critical step in the formation of a blood clot to help stop bleeding. Depending on the
severity of their disorder, people with hemophilia A can bleed frequently, especially into their joints or muscles. These bleeds
can present a significant health concern as they often cause pain and can lead to chronic swelling, deformity, reduced mobility,
and long-term joint damage. In addition to impacting a person’s quality of life, these bleeds can be life threatening if they
go into vital organs, such as the brain. A serious complication of treatment is the development of inhibitors to factor VIII
replacement therapies. Inhibitors are antibodies developed by the body’s immune system that bind to and block the efficacy of
replacement factor VIII, making it difficult, if not impossible to obtain a level of factor VIII sufficient to control bleeding.
Most people with hemophilia A who develop inhibitors will infuse BPA therapies, either on-demand (episodic) or as prophylaxis, to
control bleeding. This approach is known to be less effective and less predictable than factor VIII replacement therapy in people
with hemophilia A without inhibitors.
About Genentech in hemophilia
In 1984, Genentech scientists were the first to clone recombinant factor VIII in response to the contaminated hemophilia blood
supply crisis of the early 1980s. For more than 20 years, Genentech has been developing medicines to bring innovative treatment
options to people with diseases of the blood within oncology, and is investigating emicizumab as a potential treatment option for
hemophilia A. Genentech is committed to improving treatment and care in the hemophilia community by delivering meaningful science
and clinical expertise. For more information visit http://www.gene.com/hemophilia.
About Genentech
Founded more than 40 years ago, Genentech is a leading biotechnology company that discovers, develops, manufactures and
commercializes medicines to treat patients with serious or life-threatening medical conditions. The company, a member of the Roche
Group, has headquarters in South San Francisco, California. For additional information about the company, please visit http://www.gene.com.
Genentech
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Kimberly Muscara, 650-467-6800
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or
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