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Elonva: A new
patient friendly
approach in ART
Daniel S. Seidman, MD
Department of Ob/Gyn,
Sheba Medical Center,
Sackler School of Medicine,
Tel-Aviv University
2
3
4
5
6
6%
6%
8%
8%
9%
11%
25%
28%
0 5 10 15 20 25 30
Physical or Psychological Treatment Burden
is a Primary Reason for Dropout
Physical or psychological burden of treatment
Unknown
Relational problems/divorce
Ethical objections to ICSI treatment after failed
IVF treatment
Adoption
Poor embryo quality
Poor response/signs of ovarian aging
Other
Among 384 couples undergoing IVF treatment, 65 (17%) dropped out
Reason for Dropout
Percentage
Adapted from Verberg et al. Hum Reprod. 2008;23:2050.
7
Reasons couples discontinued
treatments before achieving two live
children at each stage:
Ceased ART for 1st
child (25)
Did not return for
2nd child (13)
Ceased ART for 2nd
child (13)
Stage treatment
discontinued (n)
9 (36%)5 (38.5%)4 (30.8%)Psychological
burden
9 (36%)04 (30.8%)Lost hope of success
4 (16%)01 (7.7%)Medical staff advice
1 (4%)02 (15.4%)Bureaucratic
difficulties
2 (8%)3 (23.1%)1 (7.7%)Divorce
01 (7.7%)1 (7.7%)Major illness
04 (30.8%)0Not ready yet for 2nd
child
12 (48%)8 (61.5%)4 (30.8%)Eventually returned
/ plan to return for
treatments
Lande et al., 2014
8
Reasons couples chose to cease ART
treatments before completing all
subsidized cycles
Brandes et al.Olivius et al.Smeenk et al.Lande et al.
15.3%21%20.5%34.3%*Drop-out rate
1-21-21.55.2**Number of
cycles
49%32.3%38.5%39.1%Psychological
burden
33%31%30.8%10.9%Physician
recommendation
9%18.1%08.7%Divorce /
relational
problem
18%1.9%04.3%Health problem
0021.8%8.7%Postpone
treatment
7%0028.3%Lost hope
9
1 2 3 4 5 6
ECPR = expected cumulative pregnancy rate; RCPR = real cumulative pregnancy rate.
Schroder et al. RBM Online. 2004;8:600.
Difference between
expected and real
pregnancy rates is caused
by the diminishing size of
the cohort due to dropout
frequency
Dropouts Negatively Impact Real
Cumulative Pregnancy Rates
Data from 4102 IVF cycles in 2130 women
Cycles
0
10
20
30
40
50
60
70
Percent
Dropout rate ECPR RCPR
(n=2130) (n=1087) (n=518) (n=222) (n=74) (n=36)
10
Patient-Centered Approach in
IVF
 Increase cumulative live birth rates
 Optimize risk/benefit ratio
–Individualization of management
strategies
– Reduce OHSS and cycle
cancellation
 Reduce complexity and patient
burden
–Shorter treatment cycles
–Fewer overall injections
11
12
The objective of the individualization
of the treatment strategy
To increase the
percentage of patients
with an appropriate
number of retrieved
oocytes, while reducing
the number of women at
high risk of cycle
cancellation due to poor
response or ovarian
hyperstimulation
syndrome (OHSS).
13
Elonva:
Individualization
of treatment
10Elonva 100 mg
+ rFSH
± Agonist trigger
Elonva 150
mg
+ pure hMG
Elonva 100 or 150 mg
+rFSH
14
33 Injections
Normal
respon
se
patient
s
Hp hMG
15
Only 6 Injection
‱ 24
oocytes
‱ 10
fertilized
‱ 2
embryos
Normal
respon
se
patient
s
rFSH/LH
16
36 Injections 11 Injections
hMG hMG
17
Low response Good
response
18
‱ 9 Oocytes
Fertilized
‱5 embryos
transferred
Good response
patients
hMG
19
29 oocytes
14 fertilized
3 embryos
transferred
Pregnant
Good response
patients
hMG
20
21
Study Question:
 Is the ovarian response to
controlled ovarian stimulation
(COS) related to the ongoing
pregnancy rate when taking into
account the main covariates
affecting the probabilities of
pregnancy following fresh embryo
transfer?
22
23
24
25
26
27
Summary answer:
 In patients treated with
corifollitropin alfa or daily
recombinant FSH (rFSH) in a
GnRH-antagonist protocol:
– A high ovarian response did NOT
compromise ongoing pregnancy
rates
– Increased cumulative pregnancy
rates following fresh and frozen-
thawed embryo transfer.
28
Corifollitropin alfa (ElonvaÂź)
 Is it safe?
29
30
Comparative incidence of OHSS
following ovarian stimulation with
corifollitropin alfa or recombinant
FSH
 Overall, 1705 patients received
corifollitropin alfa and 5.6%
experienced mild, moderate or severe
OHSS.
 In the randomized controlled trials,
Engage and Ensure, the pooled
incidence of OHSS with corifollitropin
alfa was 6.9% (71/1023 patients)
compared with 6.0% (53/880 patients) in
31
Comparative incidence of OHSS
following ovarian stimulation with
corifollitropin alfa or recombinant
FSH
 Adjusted for trial, the odds ratio for
OHSS was 1.18 (95% CI 0.81–1.71)
indicating that the risk of OHSS for
corifollitropin alfa was similar to that
for rFSH.
 Despite a higher ovarian response with
corifollitropin alfa compared with rFSH
for the first 7 days of ovarian
stimulation, the incidence of OHSS was
32
33
Good Response Patient
Small follicles
hMG
34
Good Response Patient
35
Agonist trigger !
0.2 mg Decapeptyl
Good Response
Patient
Large follicles
hMG
36
Poor responders
 Most difficult patients and fastest
growing group
 Difficult to define
 Bologna criteria
–AMA (≄ 40 y)
–previous poor response (≀ 3
oocytes)
–AFC<7 or AMH < 1.1ng/mL
37
10 Injections
Poor
response
patients
hMG
38
3 oocytes
3 embryos
transferred
Pregnant
Poor
response
patients
hMG
39
Poor Response Patient  18 Days
 1 oocyte
hMG
40
Poor Response
 12 Days
 3
oocytes
hMG
41
Poor
response
patients
HP hMG
42
43
Objective:
 To identify whether women with
poor ovarian response may benefit
from treatment with corifollitropin
alfa in a GnRH antagonist protocol.
 Design: Retrospective pilot study.
 Intervention: Corifollitropin alfa
(150 mg) followed by 300 IU rFSH
in a GnRH antagonist protocol.
Polyzos et al. Fertil Steril 2013
44
45
Conclusions:
 Treatment of poor ovarian
responders, as described by the
Bologna criteria, with
corifollitropin alfa in a GnRH
antagonist protocol results in low
pregnancy rates, similarly to
conventional stimulation with a
short agonist protocol.
Polyzos et al. Fertil Steril 2013
46
47
Study Question:
 Will sequential administration of
highly purified (hp)-HMG after
corifollitropin alfa in a GnRH
antagonist protocol benefit women
with poor ovarian response
according to the Bologna criteria?
48
49
50
Endocrine profiles during the follicular phase
in women who are poor ovarian responders,
according to age
E2, estradiol. *P . 0.05 for all comparisons between age groups
at Days 2, 7, 9 and day of hCG triggering.
51
Summary Answer:
 Corifollitropin alfa followed by hp-
HMG in a GnRH antagonist
protocol results in very promising
pregnancy rates, albeit only in
young (<40 years old) poor ovarian
responders fulfilling the Bologna
criteria.
52
53
54
55
56
Objective:
 To identify predictors of ovarian
response in women undergoing
ovarian stimulation with
corifollitropin alfa in a GnRH
antagonist protocol and determine
specific thresholds for the
prediction of low and excessive
responders.
57
58
59
Conclusions:
 AMH and AFC are the best
predictors for low and excessive
response in women treated with
corifollitropin alfa in an antagonist
protocol.
 Using AMH and AFC to select
suitable candidates for treatment
with corifollitropin alfa may result
in a safe and convenient
60
Corifollitropin alfa (ElonvaÂź)
61
62
Elonva:
Individualization
of treatment
10Elonva 100 mg
+ rFSH
± Agonist trigger
Elonva 150
mg
+ pure hMG
Elonva 100 or 150 mg
+rFSH
63
64
Day When hCG Criterion Was Met
0
5
10
15
20
25
30
35
40
5 6 7 8 9 10 11 12 13 14 15 16 17 18
Stimulation day
%ofpatients
Corifollitropin alfa 150 ”g
rFSH 200 IU/d
One-third of the patients did not require any rFSH
Engage
Adapted with permission from Fauser BC et al. Reprod Biomed Online. 2010;21:593‒601.
65
Corifollitropin alfa daily
rFSH
66
Conclusions
 Early responders receiving HCG prior
to or on stimulation day 8 have
advanced follicular development but
the final number and size of
preovulatory follicles is comparable to
those of normal responders.
 A short follicular phase of stimulation
did not affect the number of oocytes
retrieved, the number of good-quality
embryos obtained or the ongoing
pregnancy rates.
67
68
69
Corifollitropin alpha: donors
Requena et al. RBMOnline 2013
Efficacy
Corifollitropin
(n=60)
recFSH
(n=60)
Age (y) 23.2 24.4
Weight (kg) 65.6 64.9
Days of stim 10 10
ready at D8 26% 27%
COC 15.1 16.5
MII 85% 77%
OHSS - -
70
Corifollitropin alpha: donors
Requena et al. RBMOnilne 2013
Patient satisfaction
Corifollitropin
(n=60)
recFSH
(n=60)
satisfaction
(10=completely satisfied)
9.1 9.3
pain
(VAS 0-100)
13.5 12.9
preference
(if previous cycle)
75% 25%
71
Study Conclusions
 No significant differences were found
in any analysed parameters between
treatments.
 However, when donors who had
undergone both treatments chose
which treatment they preferred, the
results clearly showed a positive trend
towards choosing corifollitropin a,
confirming that this protocol may
reduce treatment burden and increase
donor compliance.
72
Overall Conclusions
 Corifollitropin alfa offers an attractive
new option for ovarian stimulation.
 Proper patient selection avoids over
response.
 OHSS totally preventable by triggering
with GnRH agonist.
 Corifollitropin alfa may offer an
advantage to young poor response
patients
 Corifollitropin alfa use is associated
73
Thanks for listening
74
75
Conclusions
 Treatment flexibility of ovarian stimulation does not
substantially affect the clinical outcome in patients’
treatment following initiation of ovarian stimulation
with either corifollitropin alfa or with daily rFSH in a
gonadotropin-releasing hormone antagonist
76
Day 4
77
78
79
80
81
82
83
84
85
86
37 years old
Severe OTA
87
88
89

 1.Usage of estradiol pretreatment for planning cycles
2. Elevated levels of progesterone at the start of
stimulation, approaches to manage it
3. When (which day) to start gonadotropins (particularly
ELONVA)?
4. Does hCG delay for 1-2 day influence on the chance
of pregnancy?
5. How “quickly” the ovaries will respond to Elonva
stimulation?
6. Trigger agonist
7. Which extra dose of rFSH required on the 8th day, if
not met the criteria for the hCG?
90
91
92
93
Results
 The total dose of rFSH at the end of the follicular
phase was significantly reduced in the CD4 group
compared with the CD2.
 A significant reduction of total duration of rFSH
stimulation in the CD4 group was also observed.
 The number of cumulus-oocyte-complexes was
comparable in both treatment groups
 Ongoing pregnancy rates of 48% in the CD2 group
and 41% in the CD4 group were achieved.
 Final oocyte maturation was triggered with GnRH
agonist instead of hCG in two patients in the CD2
group and in eight patients in the CD4 group,
because of an increased risk of ovarian
94
Conclusion
 If the approach of starting ovarian
stimulation on Day4 of the cycle
could be implemented in a large
population of infertile patients, it
would result in a significant
reduction of gonadotrophin
consumption.

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Đ˜ĐœĐŽĐžĐČĐžĐŽŃƒĐ°Đ»ĐžĐ·Đ°Ń†ĐžĐž КСЯ. ĐŸŃ€ĐŸĐłĐœĐŸĐ·ĐžŃ€ĐŸĐČĐ°ĐœĐžĐ” ĐŸŃ‚ĐșлОĐșĐ° - путь Đș Đ±Đ”Đ·ĐŸĐżĐ°ŃĐœĐŸŃŃ‚Đž ВРб
 
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Đ Đ”Đ·ĐžŃŃ‚Đ”ĐœŃ‚ĐœĐžĐč Ń‚ĐŸĐœĐșĐžĐč Đ”ĐœĐŽĐŸĐŒĐ”Ń‚Ń€Ń–Đč. Đ©ĐŸ Ń€ĐŸĐ±ĐžŃ‚Đž?
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Đ Đ”Đ·ĐžŃŃ‚Đ”ĐœŃ‚ĐœĐžĐč Ń‚ĐŸĐœĐșĐžĐč Đ”ĐœĐŽĐŸĐŒĐ”Ń‚Ń€Ń–Đč. Đ©ĐŸ Ń€ĐŸĐ±ĐžŃ‚Đž?
 
The modern approach in ART today and tomorrow
The modern approach in ART today and tomorrowThe modern approach in ART today and tomorrow
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ĐšĐ»Ń–ĐœŃ–ĐșĐ° бДз ĐłŃ–ĐżĐ”Ń€ŃŃ‚ĐžĐŒŃƒĐ»ŃŃ†Ń–Ń—. ПраĐșŃ‚ĐžŃ‡ĐœŃ– ĐșŃ€ĐŸĐșĐž.
ĐšĐ»Ń–ĐœŃ–ĐșĐ° бДз ĐłŃ–ĐżĐ”Ń€ŃŃ‚ĐžĐŒŃƒĐ»ŃŃ†Ń–Ń—. ПраĐșŃ‚ĐžŃ‡ĐœŃ– ĐșŃ€ĐŸĐșĐž.ĐšĐ»Ń–ĐœŃ–ĐșĐ° бДз ĐłŃ–ĐżĐ”Ń€ŃŃ‚ĐžĐŒŃƒĐ»ŃŃ†Ń–Ń—. ПраĐșŃ‚ĐžŃ‡ĐœŃ– ĐșŃ€ĐŸĐșĐž.
ĐšĐ»Ń–ĐœŃ–ĐșĐ° бДз ĐłŃ–ĐżĐ”Ń€ŃŃ‚ĐžĐŒŃƒĐ»ŃŃ†Ń–Ń—. ПраĐșŃ‚ĐžŃ‡ĐœŃ– ĐșŃ€ĐŸĐșĐž.
 
Đ’ŃĐżĐŸĐŒĐŸĐłĐ°Ń‚Đ”Đ»ŃŒĐœŃ‹Đ” Ń€Đ”ĐżŃ€ĐŸĐŽŃƒĐșтоĐČĐœŃ‹Đ” Ń‚Đ”Ń…ĐœĐŸĐ»ĐŸĐłĐžĐž ĐČ Đ‘Đ”Đ»Đ°Ń€ŃƒŃĐž. На путо Đ°ĐșтоĐČĐœĐŸĐłĐŸ разĐČ...
Đ’ŃĐżĐŸĐŒĐŸĐłĐ°Ń‚Đ”Đ»ŃŒĐœŃ‹Đ” Ń€Đ”ĐżŃ€ĐŸĐŽŃƒĐșтоĐČĐœŃ‹Đ” Ń‚Đ”Ń…ĐœĐŸĐ»ĐŸĐłĐžĐž ĐČ Đ‘Đ”Đ»Đ°Ń€ŃƒŃĐž. На путо Đ°ĐșтоĐČĐœĐŸĐłĐŸ разĐČ...Đ’ŃĐżĐŸĐŒĐŸĐłĐ°Ń‚Đ”Đ»ŃŒĐœŃ‹Đ” Ń€Đ”ĐżŃ€ĐŸĐŽŃƒĐșтоĐČĐœŃ‹Đ” Ń‚Đ”Ń…ĐœĐŸĐ»ĐŸĐłĐžĐž ĐČ Đ‘Đ”Đ»Đ°Ń€ŃƒŃĐž. На путо Đ°ĐșтоĐČĐœĐŸĐłĐŸ разĐČ...
Đ’ŃĐżĐŸĐŒĐŸĐłĐ°Ń‚Đ”Đ»ŃŒĐœŃ‹Đ” Ń€Đ”ĐżŃ€ĐŸĐŽŃƒĐșтоĐČĐœŃ‹Đ” Ń‚Đ”Ń…ĐœĐŸĐ»ĐŸĐłĐžĐž ĐČ Đ‘Đ”Đ»Đ°Ń€ŃƒŃĐž. На путо Đ°ĐșтоĐČĐœĐŸĐłĐŸ разĐČ...
 
ĐŸĐ”Ń€ŃˆŃ– Ń€Đ”Đ·ŃƒĐ»ŃŒŃ‚Đ°Ń‚Đž Đ·Đ°ŃŃ‚ĐŸŃŃƒĐČĐ°ĐœĐœŃ ĐșĐŸŃ€Ń–Ń„ĐŸĐ»Đ»Ń–Ń‚Ń€ĐŸĐżŃ–ĐœŃƒ ĐČ ĐżŃ€ĐŸŃ‚ĐŸĐșĐŸĐ»Đ°Ń… КОС (Đ”ĐŸŃĐČіЮ ІРМ)
ĐŸĐ”Ń€ŃˆŃ– Ń€Đ”Đ·ŃƒĐ»ŃŒŃ‚Đ°Ń‚Đž Đ·Đ°ŃŃ‚ĐŸŃŃƒĐČĐ°ĐœĐœŃ ĐșĐŸŃ€Ń–Ń„ĐŸĐ»Đ»Ń–Ń‚Ń€ĐŸĐżŃ–ĐœŃƒ ĐČ ĐżŃ€ĐŸŃ‚ĐŸĐșĐŸĐ»Đ°Ń… КОС (Đ”ĐŸŃĐČіЮ ІРМ)ĐŸĐ”Ń€ŃˆŃ– Ń€Đ”Đ·ŃƒĐ»ŃŒŃ‚Đ°Ń‚Đž Đ·Đ°ŃŃ‚ĐŸŃŃƒĐČĐ°ĐœĐœŃ ĐșĐŸŃ€Ń–Ń„ĐŸĐ»Đ»Ń–Ń‚Ń€ĐŸĐżŃ–ĐœŃƒ ĐČ ĐżŃ€ĐŸŃ‚ĐŸĐșĐŸĐ»Đ°Ń… КОС (Đ”ĐŸŃĐČіЮ ІРМ)
ĐŸĐ”Ń€ŃˆŃ– Ń€Đ”Đ·ŃƒĐ»ŃŒŃ‚Đ°Ń‚Đž Đ·Đ°ŃŃ‚ĐŸŃŃƒĐČĐ°ĐœĐœŃ ĐșĐŸŃ€Ń–Ń„ĐŸĐ»Đ»Ń–Ń‚Ń€ĐŸĐżŃ–ĐœŃƒ ĐČ ĐżŃ€ĐŸŃ‚ĐŸĐșĐŸĐ»Đ°Ń… КОС (Đ”ĐŸŃĐČіЮ ІРМ)
 
ĐŸĐŸĐłĐ°ĐœĐ° (Đ±Ń–ĐŽĐœĐ°) ĐČŃ–ĐŽĐżĐŸĐČіЮь ĐœĐ° ĐșĐŸĐœŃ‚Ń€ĐŸĐ»ŃŒĐŸĐČĐ°ĐœŃƒ ŃŃ‚ĐžĐŒŃƒĐ»ŃŃ†Ń–ŃŽ ŃŃ”Ń‡ĐœĐžĐșіĐČ
ĐŸĐŸĐłĐ°ĐœĐ° (Đ±Ń–ĐŽĐœĐ°) ĐČŃ–ĐŽĐżĐŸĐČіЮь ĐœĐ° ĐșĐŸĐœŃ‚Ń€ĐŸĐ»ŃŒĐŸĐČĐ°ĐœŃƒ ŃŃ‚ĐžĐŒŃƒĐ»ŃŃ†Ń–ŃŽ ŃŃ”Ń‡ĐœĐžĐșіĐČĐŸĐŸĐłĐ°ĐœĐ° (Đ±Ń–ĐŽĐœĐ°) ĐČŃ–ĐŽĐżĐŸĐČіЮь ĐœĐ° ĐșĐŸĐœŃ‚Ń€ĐŸĐ»ŃŒĐŸĐČĐ°ĐœŃƒ ŃŃ‚ĐžĐŒŃƒĐ»ŃŃ†Ń–ŃŽ ŃŃ”Ń‡ĐœĐžĐșіĐČ
ĐŸĐŸĐłĐ°ĐœĐ° (Đ±Ń–ĐŽĐœĐ°) ĐČŃ–ĐŽĐżĐŸĐČіЮь ĐœĐ° ĐșĐŸĐœŃ‚Ń€ĐŸĐ»ŃŒĐŸĐČĐ°ĐœŃƒ ŃŃ‚ĐžĐŒŃƒĐ»ŃŃ†Ń–ŃŽ ŃŃ”Ń‡ĐœĐžĐșіĐČ
 
ĐžĐżŃ‚ĐžĐŒŃ–Đ·Đ°Ń†Ń–Ń КОС ĐČ Ń†ĐžĐșлах Đ·Đ°ĐżĐ»Ń–ĐŽĐœĐ”ĐœĐœŃ in vitro Đ· ĐŽĐŸĐœĐ°Ń†Ń–Ń”ŃŽ ĐŸĐŸŃ†ĐžŃ‚Ń–ĐČ
ĐžĐżŃ‚ĐžĐŒŃ–Đ·Đ°Ń†Ń–Ń КОС ĐČ Ń†ĐžĐșлах Đ·Đ°ĐżĐ»Ń–ĐŽĐœĐ”ĐœĐœŃ in vitro Đ· ĐŽĐŸĐœĐ°Ń†Ń–Ń”ŃŽ ĐŸĐŸŃ†ĐžŃ‚Ń–ĐČĐžĐżŃ‚ĐžĐŒŃ–Đ·Đ°Ń†Ń–Ń КОС ĐČ Ń†ĐžĐșлах Đ·Đ°ĐżĐ»Ń–ĐŽĐœĐ”ĐœĐœŃ in vitro Đ· ĐŽĐŸĐœĐ°Ń†Ń–Ń”ŃŽ ĐŸĐŸŃ†ĐžŃ‚Ń–ĐČ
ĐžĐżŃ‚ĐžĐŒŃ–Đ·Đ°Ń†Ń–Ń КОС ĐČ Ń†ĐžĐșлах Đ·Đ°ĐżĐ»Ń–ĐŽĐœĐ”ĐœĐœŃ in vitro Đ· ĐŽĐŸĐœĐ°Ń†Ń–Ń”ŃŽ ĐŸĐŸŃ†ĐžŃ‚Ń–ĐČ
 
ĐžŃĐœĐŸĐČĐœŃ– сĐșĐ»Đ°ĐŽĐŸĐČі ĐżĐ°Ń‚ĐŸĐłĐ”ĐœĐ”Đ·Ńƒ Ń€ĐŸĐ·ĐČотĐșу СГЯ
ĐžŃĐœĐŸĐČĐœŃ– сĐșĐ»Đ°ĐŽĐŸĐČі ĐżĐ°Ń‚ĐŸĐłĐ”ĐœĐ”Đ·Ńƒ Ń€ĐŸĐ·ĐČотĐșу ĐĄĐ“ĐŻĐžŃĐœĐŸĐČĐœŃ– сĐșĐ»Đ°ĐŽĐŸĐČі ĐżĐ°Ń‚ĐŸĐłĐ”ĐœĐ”Đ·Ńƒ Ń€ĐŸĐ·ĐČотĐșу СГЯ
ĐžŃĐœĐŸĐČĐœŃ– сĐșĐ»Đ°ĐŽĐŸĐČі ĐżĐ°Ń‚ĐŸĐłĐ”ĐœĐ”Đ·Ńƒ Ń€ĐŸĐ·ĐČотĐșу СГЯ
 
ĐžŃĐŸĐ±Đ»ĐžĐČĐŸŃŃ‚Ń– ĐżŃ€Đ”ĐœĐ°Ń‚Đ°Đ»ŃŒĐœĐŸĐłĐŸ сĐșŃ€ĐžĐœŃ–ĐœĐłŃƒ ĐżŃ–ŃĐ»Ń ДРб
ĐžŃĐŸĐ±Đ»ĐžĐČĐŸŃŃ‚Ń– ĐżŃ€Đ”ĐœĐ°Ń‚Đ°Đ»ŃŒĐœĐŸĐłĐŸ сĐșŃ€ĐžĐœŃ–ĐœĐłŃƒ ĐżŃ–ŃĐ»Ń ДРб ĐžŃĐŸĐ±Đ»ĐžĐČĐŸŃŃ‚Ń– ĐżŃ€Đ”ĐœĐ°Ń‚Đ°Đ»ŃŒĐœĐŸĐłĐŸ сĐșŃ€ĐžĐœŃ–ĐœĐłŃƒ ĐżŃ–ŃĐ»Ń ДРб
ĐžŃĐŸĐ±Đ»ĐžĐČĐŸŃŃ‚Ń– ĐżŃ€Đ”ĐœĐ°Ń‚Đ°Đ»ŃŒĐœĐŸĐłĐŸ сĐșŃ€ĐžĐœŃ–ĐœĐłŃƒ ĐżŃ–ŃĐ»Ń ДРб
 
ĐšŃ€ĐžĐŸĐżŃ€ĐŸŃ‚ĐŸĐșĐŸĐ». ПраĐșтОчДсĐșОД аспДĐșты
ĐšŃ€ĐžĐŸĐżŃ€ĐŸŃ‚ĐŸĐșĐŸĐ». ПраĐșтОчДсĐșОД аспДĐșŃ‚Ń‹ĐšŃ€ĐžĐŸĐżŃ€ĐŸŃ‚ĐŸĐșĐŸĐ». ПраĐșтОчДсĐșОД аспДĐșты
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ĐĐ°Ń€ŃƒŃˆĐ”ĐœĐžĐ” праĐČ Đ’Đ˜Đ§-ĐžĐœŃ„ĐžŃ†ĐžŃ€ĐŸĐČĐ°ĐœĐœŃ‹Ń… ЎДтДĐč ĐČ ĐŁĐșŃ€Đ°ĐžĐœĐ”
ĐĐ°Ń€ŃƒŃˆĐ”ĐœĐžĐ” праĐČ Đ’Đ˜Đ§-ĐžĐœŃ„ĐžŃ†ĐžŃ€ĐŸĐČĐ°ĐœĐœŃ‹Ń… ЎДтДĐč ĐČ ĐŁĐșŃ€Đ°ĐžĐœĐ”ĐĐ°Ń€ŃƒŃˆĐ”ĐœĐžĐ” праĐČ Đ’Đ˜Đ§-ĐžĐœŃ„ĐžŃ†ĐžŃ€ĐŸĐČĐ°ĐœĐœŃ‹Ń… ЎДтДĐč ĐČ ĐŁĐșŃ€Đ°ĐžĐœĐ”
ĐĐ°Ń€ŃƒŃˆĐ”ĐœĐžĐ” праĐČ Đ’Đ˜Đ§-ĐžĐœŃ„ĐžŃ†ĐžŃ€ĐŸĐČĐ°ĐœĐœŃ‹Ń… ЎДтДĐč ĐČ ĐŁĐșŃ€Đ°ĐžĐœĐ”
 
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Elonva: A new patient friendly approach in ART

  • 1. 1 Elonva: A new patient friendly approach in ART Daniel S. Seidman, MD Department of Ob/Gyn, Sheba Medical Center, Sackler School of Medicine, Tel-Aviv University
  • 2. 2
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  • 6. 6 6% 6% 8% 8% 9% 11% 25% 28% 0 5 10 15 20 25 30 Physical or Psychological Treatment Burden is a Primary Reason for Dropout Physical or psychological burden of treatment Unknown Relational problems/divorce Ethical objections to ICSI treatment after failed IVF treatment Adoption Poor embryo quality Poor response/signs of ovarian aging Other Among 384 couples undergoing IVF treatment, 65 (17%) dropped out Reason for Dropout Percentage Adapted from Verberg et al. Hum Reprod. 2008;23:2050.
  • 7. 7 Reasons couples discontinued treatments before achieving two live children at each stage: Ceased ART for 1st child (25) Did not return for 2nd child (13) Ceased ART for 2nd child (13) Stage treatment discontinued (n) 9 (36%)5 (38.5%)4 (30.8%)Psychological burden 9 (36%)04 (30.8%)Lost hope of success 4 (16%)01 (7.7%)Medical staff advice 1 (4%)02 (15.4%)Bureaucratic difficulties 2 (8%)3 (23.1%)1 (7.7%)Divorce 01 (7.7%)1 (7.7%)Major illness 04 (30.8%)0Not ready yet for 2nd child 12 (48%)8 (61.5%)4 (30.8%)Eventually returned / plan to return for treatments Lande et al., 2014
  • 8. 8 Reasons couples chose to cease ART treatments before completing all subsidized cycles Brandes et al.Olivius et al.Smeenk et al.Lande et al. 15.3%21%20.5%34.3%*Drop-out rate 1-21-21.55.2**Number of cycles 49%32.3%38.5%39.1%Psychological burden 33%31%30.8%10.9%Physician recommendation 9%18.1%08.7%Divorce / relational problem 18%1.9%04.3%Health problem 0021.8%8.7%Postpone treatment 7%0028.3%Lost hope
  • 9. 9 1 2 3 4 5 6 ECPR = expected cumulative pregnancy rate; RCPR = real cumulative pregnancy rate. Schroder et al. RBM Online. 2004;8:600. Difference between expected and real pregnancy rates is caused by the diminishing size of the cohort due to dropout frequency Dropouts Negatively Impact Real Cumulative Pregnancy Rates Data from 4102 IVF cycles in 2130 women Cycles 0 10 20 30 40 50 60 70 Percent Dropout rate ECPR RCPR (n=2130) (n=1087) (n=518) (n=222) (n=74) (n=36)
  • 10. 10 Patient-Centered Approach in IVF  Increase cumulative live birth rates  Optimize risk/benefit ratio –Individualization of management strategies – Reduce OHSS and cycle cancellation  Reduce complexity and patient burden –Shorter treatment cycles –Fewer overall injections
  • 11. 11
  • 12. 12 The objective of the individualization of the treatment strategy To increase the percentage of patients with an appropriate number of retrieved oocytes, while reducing the number of women at high risk of cycle cancellation due to poor response or ovarian hyperstimulation syndrome (OHSS).
  • 13. 13 Elonva: Individualization of treatment 10Elonva 100 mg + rFSH ± Agonist trigger Elonva 150 mg + pure hMG Elonva 100 or 150 mg +rFSH
  • 15. 15 Only 6 Injection ‱ 24 oocytes ‱ 10 fertilized ‱ 2 embryos Normal respon se patient s rFSH/LH
  • 16. 16 36 Injections 11 Injections hMG hMG
  • 18. 18 ‱ 9 Oocytes Fertilized ‱5 embryos transferred Good response patients hMG
  • 19. 19 29 oocytes 14 fertilized 3 embryos transferred Pregnant Good response patients hMG
  • 20. 20
  • 21. 21 Study Question:  Is the ovarian response to controlled ovarian stimulation (COS) related to the ongoing pregnancy rate when taking into account the main covariates affecting the probabilities of pregnancy following fresh embryo transfer?
  • 22. 22
  • 23. 23
  • 24. 24
  • 25. 25
  • 26. 26
  • 27. 27 Summary answer:  In patients treated with corifollitropin alfa or daily recombinant FSH (rFSH) in a GnRH-antagonist protocol: – A high ovarian response did NOT compromise ongoing pregnancy rates – Increased cumulative pregnancy rates following fresh and frozen- thawed embryo transfer.
  • 29. 29
  • 30. 30 Comparative incidence of OHSS following ovarian stimulation with corifollitropin alfa or recombinant FSH  Overall, 1705 patients received corifollitropin alfa and 5.6% experienced mild, moderate or severe OHSS.  In the randomized controlled trials, Engage and Ensure, the pooled incidence of OHSS with corifollitropin alfa was 6.9% (71/1023 patients) compared with 6.0% (53/880 patients) in
  • 31. 31 Comparative incidence of OHSS following ovarian stimulation with corifollitropin alfa or recombinant FSH  Adjusted for trial, the odds ratio for OHSS was 1.18 (95% CI 0.81–1.71) indicating that the risk of OHSS for corifollitropin alfa was similar to that for rFSH.  Despite a higher ovarian response with corifollitropin alfa compared with rFSH for the first 7 days of ovarian stimulation, the incidence of OHSS was
  • 32. 32
  • 35. 35 Agonist trigger ! 0.2 mg Decapeptyl Good Response Patient Large follicles hMG
  • 36. 36 Poor responders  Most difficult patients and fastest growing group  Difficult to define  Bologna criteria –AMA (≄ 40 y) –previous poor response (≀ 3 oocytes) –AFC<7 or AMH < 1.1ng/mL
  • 39. 39 Poor Response Patient  18 Days  1 oocyte hMG
  • 40. 40 Poor Response  12 Days  3 oocytes hMG
  • 42. 42
  • 43. 43 Objective:  To identify whether women with poor ovarian response may benefit from treatment with corifollitropin alfa in a GnRH antagonist protocol.  Design: Retrospective pilot study.  Intervention: Corifollitropin alfa (150 mg) followed by 300 IU rFSH in a GnRH antagonist protocol. Polyzos et al. Fertil Steril 2013
  • 44. 44
  • 45. 45 Conclusions:  Treatment of poor ovarian responders, as described by the Bologna criteria, with corifollitropin alfa in a GnRH antagonist protocol results in low pregnancy rates, similarly to conventional stimulation with a short agonist protocol. Polyzos et al. Fertil Steril 2013
  • 46. 46
  • 47. 47 Study Question:  Will sequential administration of highly purified (hp)-HMG after corifollitropin alfa in a GnRH antagonist protocol benefit women with poor ovarian response according to the Bologna criteria?
  • 48. 48
  • 49. 49
  • 50. 50 Endocrine profiles during the follicular phase in women who are poor ovarian responders, according to age E2, estradiol. *P . 0.05 for all comparisons between age groups at Days 2, 7, 9 and day of hCG triggering.
  • 51. 51 Summary Answer:  Corifollitropin alfa followed by hp- HMG in a GnRH antagonist protocol results in very promising pregnancy rates, albeit only in young (<40 years old) poor ovarian responders fulfilling the Bologna criteria.
  • 52. 52
  • 53. 53
  • 54. 54
  • 55. 55
  • 56. 56 Objective:  To identify predictors of ovarian response in women undergoing ovarian stimulation with corifollitropin alfa in a GnRH antagonist protocol and determine specific thresholds for the prediction of low and excessive responders.
  • 57. 57
  • 58. 58
  • 59. 59 Conclusions:  AMH and AFC are the best predictors for low and excessive response in women treated with corifollitropin alfa in an antagonist protocol.  Using AMH and AFC to select suitable candidates for treatment with corifollitropin alfa may result in a safe and convenient
  • 61. 61
  • 62. 62 Elonva: Individualization of treatment 10Elonva 100 mg + rFSH ± Agonist trigger Elonva 150 mg + pure hMG Elonva 100 or 150 mg +rFSH
  • 63. 63
  • 64. 64 Day When hCG Criterion Was Met 0 5 10 15 20 25 30 35 40 5 6 7 8 9 10 11 12 13 14 15 16 17 18 Stimulation day %ofpatients Corifollitropin alfa 150 ”g rFSH 200 IU/d One-third of the patients did not require any rFSH Engage Adapted with permission from Fauser BC et al. Reprod Biomed Online. 2010;21:593‒601.
  • 66. 66 Conclusions  Early responders receiving HCG prior to or on stimulation day 8 have advanced follicular development but the final number and size of preovulatory follicles is comparable to those of normal responders.  A short follicular phase of stimulation did not affect the number of oocytes retrieved, the number of good-quality embryos obtained or the ongoing pregnancy rates.
  • 67. 67
  • 68. 68
  • 69. 69 Corifollitropin alpha: donors Requena et al. RBMOnline 2013 Efficacy Corifollitropin (n=60) recFSH (n=60) Age (y) 23.2 24.4 Weight (kg) 65.6 64.9 Days of stim 10 10 ready at D8 26% 27% COC 15.1 16.5 MII 85% 77% OHSS - -
  • 70. 70 Corifollitropin alpha: donors Requena et al. RBMOnilne 2013 Patient satisfaction Corifollitropin (n=60) recFSH (n=60) satisfaction (10=completely satisfied) 9.1 9.3 pain (VAS 0-100) 13.5 12.9 preference (if previous cycle) 75% 25%
  • 71. 71 Study Conclusions  No significant differences were found in any analysed parameters between treatments.  However, when donors who had undergone both treatments chose which treatment they preferred, the results clearly showed a positive trend towards choosing corifollitropin a, confirming that this protocol may reduce treatment burden and increase donor compliance.
  • 72. 72 Overall Conclusions  Corifollitropin alfa offers an attractive new option for ovarian stimulation.  Proper patient selection avoids over response.  OHSS totally preventable by triggering with GnRH agonist.  Corifollitropin alfa may offer an advantage to young poor response patients  Corifollitropin alfa use is associated
  • 74. 74
  • 75. 75 Conclusions  Treatment flexibility of ovarian stimulation does not substantially affect the clinical outcome in patients’ treatment following initiation of ovarian stimulation with either corifollitropin alfa or with daily rFSH in a gonadotropin-releasing hormone antagonist
  • 77. 77
  • 78. 78
  • 79. 79
  • 80. 80
  • 81. 81
  • 82. 82
  • 83. 83
  • 84. 84
  • 85. 85
  • 87. 87
  • 88. 88
  • 89. 89   1.Usage of estradiol pretreatment for planning cycles 2. Elevated levels of progesterone at the start of stimulation, approaches to manage it 3. When (which day) to start gonadotropins (particularly ELONVA)? 4. Does hCG delay for 1-2 day influence on the chance of pregnancy? 5. How “quickly” the ovaries will respond to Elonva stimulation? 6. Trigger agonist 7. Which extra dose of rFSH required on the 8th day, if not met the criteria for the hCG?
  • 90. 90
  • 91. 91
  • 92. 92
  • 93. 93 Results  The total dose of rFSH at the end of the follicular phase was significantly reduced in the CD4 group compared with the CD2.  A significant reduction of total duration of rFSH stimulation in the CD4 group was also observed.  The number of cumulus-oocyte-complexes was comparable in both treatment groups  Ongoing pregnancy rates of 48% in the CD2 group and 41% in the CD4 group were achieved.  Final oocyte maturation was triggered with GnRH agonist instead of hCG in two patients in the CD2 group and in eight patients in the CD4 group, because of an increased risk of ovarian
  • 94. 94 Conclusion  If the approach of starting ovarian stimulation on Day4 of the cycle could be implemented in a large population of infertile patients, it would result in a significant reduction of gonadotrophin consumption.