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New Modality for suppression of
LH surge
Why & How?
Hesham Al-Inany, PhD (Amsterdam)
Why LH suppression?
• The original concept of the existence of a
therapeutic window for LH during ovarian
stimulation was first put forward by Hillier.
• According to this, there is not only a threshold
requirement for LH to guarantee an optimal
cycle but also a ceiling level beyond which LH
might be deleterious to ovarian stimulation.
The criteria for premature luteinization
• Decreased cycle outcome has been reported
when LH is >10 IU/L and P>1.0 ng/L
• others elected to choose a cut-off value of
>1.2 ng/mL for progesterone to define
premature luteinization
The ideal IVF protocol
• a high chance of embryo transfer
• a low cancellation rate,
• a reasonable pregnancy rate
• few side-effects,
• low costs
• practical convenience both for the patient and
the clinician
History
• 1970 Clomifen
hMG
• 1980 GnRH-agonist / hMG
• 1990 recFSH / hMG
GnRH-antagonist / hMG or recFSH
Protocols for IVF
GnRH Antagonist
Protocols
GnRH Agonist
Protocols
225 IU per day
(150 IU Europe)
Individualized Dosing of FSH/HMG
250 mg per day antagonist
Individualized Dosing of FSH/HMG
GnRHa 1.0 mg per day
up to 21 days
0.5 mg per day of GnRHa
225 IU per day
(150 IU Europe)
Day 6
of FSH/HMG
Day
of hCG
Day 1
of FSH/HMG
Day 6
of FSH/HMG
Day
of hCG
7 – 8 days
after estimated ovulation
Down regulation
Day 2 or 3
of menses
Day 1
FSH/HMG
How Science is advancing!!
Observation
Further Observation
Then search the medical literature
How Science is advancing!!
Idea
• CC antiestrogenic effect may suppress
premature LH rise while maintaining a positive
influence on ovarian follicle development if
continued till the day of hCG
How Science is advancing!!
Then performing a Trial
Current practice of O.i in IUI
Clomiphene Citrate
hMG or FSH
______________________________________________
Emerging protocol: Reversed hMG/CC
Clomiphene Citrate
hMG or FSH
______________________________________________
• Some cases are CC resistant
• about 25% of IUI cycles suffer from
premature LH surge cancellation.
WHY
If true : Double Benefits
• The use of hMG at start of cycle for few
days will avoid CC resistant cases
• use of CC till the day of hCG will prevent
LH surge
Outcome Parameters
Primary outcome parameters
Clinical pregnancy rate per women randomised (i.e.
fetal heart pulsations demonstrated by TVS at 6 –7
weeks’ gestation)
Premature LH
Secondary outcome parameters
E2 levels,
Number of mature follicles
Endometrial thickness
On day of HCG
Sample size calculation
• if premature LH surge rate among the hMG only
group is 20%.
• Assuming CC is effective by reducing it by 15%
• Then hMG + CC group will be 5%,
• So we will need to study 75 couples in each arm in
order to reach a power of 80%.
Drop out cases
• In order to compensate for discontinuations, we
recruited 115 women in each arm
• If more than 10% drop out cases, this would
affect the validity of the trial
25
New concept has to be tested
Participants
RandomlyAssigned
Intervention Group
Control Group
Follow-up
Follow-up
Intervention Group
Control Group
Novel protocol
75 IU/HMG
CD3 CD?7
150 mg CC
hCG IUI
DF ≥ 18 mm
34-36h
DF ≥ 12 mm
Control group
75 IU/HMG
CD3 hCG IUI
DF ≥ 18 mm
CD7
34-36h
DF ≥ 12 mm
CD?7
Results
Variable Group I
(n=115)
Group II
(n=115)
P value
Age (years) 27.3 ± 4.7 28.4 ± 2.7 NS
Duration of infertility (years) 3.1 ± 1.9 2.4 ± 1.6 NS
Cause of infertility
Mild male factor
Unexplained infertility
61 (53%)
54 (47%)
58 (50.4%)
57 (49.6%)
NS
NS
BMI 28.5 ± 1.6 28.1 ± 3.1 NS
Results (cont.)
Variable Group I
(n=110)
Group II
(n=107)
P value
Number of cancelled cycles
Inadequate response
Hyper response
5/110
4/5
1/5
8/107
6/8
2/8
NS
NS
NS
Basal LH (mIU/mL) 6.4 ± 2.2 5.8 ± 2.4 NS
Basal FSH (mIU/mL) 6.7 ± 2.5 7.2 ± 4.8 NS
Days of stimulation 7.2 ± 1.8 8.1 ± 1.3 NS
E2 at time of HCG (pg/mL) 360.3 ± 162.9 280 ± 110.0 P <.05*
Results (cont.)
Variable HMG/CC
(n=110)
HMG
(n=107)
P value
LH on day of hCG (miu/ml) for cases with
no premature LH surge
7.3 ± 1.8 7.8 ± 2.2 NS
Number of Follicles ≥ 16 mm 2.4 ± 0.97 1.3 ± 1.1 P < 0.05*
Number of patients with premature LH
surge
6 (5.45%) 17 (15.89%) P<0.001*
End. Thickness (mm) 5.9 ± 0.7 4.9 ± 1.9 NS
Clinical Pregnancy 11 (10%) 9 (8.41%) NS
How Science is advancing!!
 No OCP pretreatment
 Check patient cycle day 2
 FSH 100-225 IU
 Antagonist earlier than later
 LH not necessary
Suggested GnRH Antagonist Protocol
Cycle day 2
Transvaginal US +
(if desired) hormonal profile
This suggested protocol represents a “best estimate” given current
data and clinical experience. Further data are required before more
concrete recommendations can be made.
For regular IVF patients:
 5-9 antral follicles per
ovary
 Age <35 years
 No PCOS
 No history of poor
responses
 No endometriosis
Duration of treatment
based on clinical judgment
in consultation with patient
(usually 2 USs)
Cycle day 2/3
Start FSH 150-200 IU. Continue
Stimulation days 5-6
Start GnRH antagonist
administered daily. Continue
Monitoring according to clinic practice
 US (+ blood test if required)
 FSH dose adjustments may be considered
3 follicles 17 mm
Day of triggering
 Ensure interval between antagonist and hCG does not exceed 30 h
 hCG 5000-10,000 IU
Oocyte retrieval
36 h
YES
NO
US = ultrasonogram; OCP = oral contraceptive pill. Devroey et al. Hum Reprod. 2009;24:764.
How Science is advancing!!
Antagonist shortage
How Science is advancing!!
Proof of concept study
• Not a RCT • Small number
• To proof the theory
Proof of concept study
• Seven cases undergoing ICSI
• Strict criteria: young age
• Unexplained infertility
• Mild male factor
• Failed 2-3 IUI cycles • No PCOS
• No endometriomas
• 2-3 ampoules daily
• CC staring from follicle diameter 11mm
• Usually for 3-4 d
• hCG if follicle 17mm
Results
• No premature lutenisation was reported
till now
• Number of retrieved oocytes ranged
between 7-16
• MII oocytes more than 50%
Waiting for pregnancy rate
Should we rush?
• To apply it
• Too early
• Needs more cases
• Not magic
There was enthusiasm for PGS
• Advanced maternal age
• Gianaroli 1999, Munne 1999, Kahraman 2000, Obasaji 2001, Munne 2003;
Montag 2004; Platteau 2005
• Repeated IVF failure
• Gianaroli 1999, Kahraman 2000, Pehlivan 2003,Munne 2003,
Wilding 2004
• Recurrent miscarriage
• Pellicer 1999, Rubio 2003, Rubio 2005, Munne 2005
• Severe male factor
• Silber 2003, Platteau 2004
Preimplantation genetic screening
for advanced maternal age –
reduced live birth rates
OR 0.59
(0.44, 0.81)
Triggering – GnRH agonist or hCG?
Youssef et al, updated CR 2013
• 17 RCTs
– 9 report OHSS
– 5 report live birth rate
• Risk of bias
– Only 2/17 used blinding
– 4/17 studies stopped prematurely for differing
reasons
– All studies were either funded by pharmaceutical
companies or did not report their funding
Ovarian hyperstimulation rate is
reduced with agonist trigger in high
risk women only
OR 0.06
(0.01, 0.34)
Youssef et al, updated 2013
*4 studies no events in either arm
Live birth rate reduced with GnRHa
triggering
Conclusion
• It is a valid idea with scientific background
evidence
• Needs more cases to ensure its validity
For whom
• for young women,
• for those with unexplained infertility
• mild male factor
•i.e good responders

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Cc for suppression of lh surge

  • 1. New Modality for suppression of LH surge Why & How? Hesham Al-Inany, PhD (Amsterdam)
  • 2. Why LH suppression? • The original concept of the existence of a therapeutic window for LH during ovarian stimulation was first put forward by Hillier. • According to this, there is not only a threshold requirement for LH to guarantee an optimal cycle but also a ceiling level beyond which LH might be deleterious to ovarian stimulation.
  • 3. The criteria for premature luteinization • Decreased cycle outcome has been reported when LH is >10 IU/L and P>1.0 ng/L • others elected to choose a cut-off value of >1.2 ng/mL for progesterone to define premature luteinization
  • 4. The ideal IVF protocol • a high chance of embryo transfer • a low cancellation rate, • a reasonable pregnancy rate • few side-effects, • low costs • practical convenience both for the patient and the clinician
  • 5. History • 1970 Clomifen hMG • 1980 GnRH-agonist / hMG • 1990 recFSH / hMG GnRH-antagonist / hMG or recFSH
  • 6. Protocols for IVF GnRH Antagonist Protocols GnRH Agonist Protocols 225 IU per day (150 IU Europe) Individualized Dosing of FSH/HMG 250 mg per day antagonist Individualized Dosing of FSH/HMG GnRHa 1.0 mg per day up to 21 days 0.5 mg per day of GnRHa 225 IU per day (150 IU Europe) Day 6 of FSH/HMG Day of hCG Day 1 of FSH/HMG Day 6 of FSH/HMG Day of hCG 7 – 8 days after estimated ovulation Down regulation Day 2 or 3 of menses Day 1 FSH/HMG
  • 7. How Science is advancing!!
  • 10. Then search the medical literature
  • 11.
  • 12.
  • 13.
  • 14. How Science is advancing!!
  • 15. Idea • CC antiestrogenic effect may suppress premature LH rise while maintaining a positive influence on ovarian follicle development if continued till the day of hCG
  • 16. How Science is advancing!!
  • 18. Current practice of O.i in IUI Clomiphene Citrate hMG or FSH ______________________________________________
  • 19. Emerging protocol: Reversed hMG/CC Clomiphene Citrate hMG or FSH ______________________________________________
  • 20. • Some cases are CC resistant • about 25% of IUI cycles suffer from premature LH surge cancellation. WHY
  • 21. If true : Double Benefits • The use of hMG at start of cycle for few days will avoid CC resistant cases • use of CC till the day of hCG will prevent LH surge
  • 22. Outcome Parameters Primary outcome parameters Clinical pregnancy rate per women randomised (i.e. fetal heart pulsations demonstrated by TVS at 6 –7 weeks’ gestation) Premature LH Secondary outcome parameters E2 levels, Number of mature follicles Endometrial thickness On day of HCG
  • 23. Sample size calculation • if premature LH surge rate among the hMG only group is 20%. • Assuming CC is effective by reducing it by 15% • Then hMG + CC group will be 5%, • So we will need to study 75 couples in each arm in order to reach a power of 80%.
  • 24. Drop out cases • In order to compensate for discontinuations, we recruited 115 women in each arm • If more than 10% drop out cases, this would affect the validity of the trial
  • 25. 25 New concept has to be tested Participants RandomlyAssigned Intervention Group Control Group Follow-up Follow-up Intervention Group Control Group
  • 26. Novel protocol 75 IU/HMG CD3 CD?7 150 mg CC hCG IUI DF ≥ 18 mm 34-36h DF ≥ 12 mm
  • 27. Control group 75 IU/HMG CD3 hCG IUI DF ≥ 18 mm CD7 34-36h DF ≥ 12 mm CD?7
  • 28. Results Variable Group I (n=115) Group II (n=115) P value Age (years) 27.3 ± 4.7 28.4 ± 2.7 NS Duration of infertility (years) 3.1 ± 1.9 2.4 ± 1.6 NS Cause of infertility Mild male factor Unexplained infertility 61 (53%) 54 (47%) 58 (50.4%) 57 (49.6%) NS NS BMI 28.5 ± 1.6 28.1 ± 3.1 NS
  • 29. Results (cont.) Variable Group I (n=110) Group II (n=107) P value Number of cancelled cycles Inadequate response Hyper response 5/110 4/5 1/5 8/107 6/8 2/8 NS NS NS Basal LH (mIU/mL) 6.4 ± 2.2 5.8 ± 2.4 NS Basal FSH (mIU/mL) 6.7 ± 2.5 7.2 ± 4.8 NS Days of stimulation 7.2 ± 1.8 8.1 ± 1.3 NS E2 at time of HCG (pg/mL) 360.3 ± 162.9 280 ± 110.0 P <.05*
  • 30. Results (cont.) Variable HMG/CC (n=110) HMG (n=107) P value LH on day of hCG (miu/ml) for cases with no premature LH surge 7.3 ± 1.8 7.8 ± 2.2 NS Number of Follicles ≥ 16 mm 2.4 ± 0.97 1.3 ± 1.1 P < 0.05* Number of patients with premature LH surge 6 (5.45%) 17 (15.89%) P<0.001* End. Thickness (mm) 5.9 ± 0.7 4.9 ± 1.9 NS Clinical Pregnancy 11 (10%) 9 (8.41%) NS
  • 31. How Science is advancing!!
  • 32.  No OCP pretreatment  Check patient cycle day 2  FSH 100-225 IU  Antagonist earlier than later  LH not necessary Suggested GnRH Antagonist Protocol Cycle day 2 Transvaginal US + (if desired) hormonal profile This suggested protocol represents a “best estimate” given current data and clinical experience. Further data are required before more concrete recommendations can be made. For regular IVF patients:  5-9 antral follicles per ovary  Age <35 years  No PCOS  No history of poor responses  No endometriosis Duration of treatment based on clinical judgment in consultation with patient (usually 2 USs) Cycle day 2/3 Start FSH 150-200 IU. Continue Stimulation days 5-6 Start GnRH antagonist administered daily. Continue Monitoring according to clinic practice  US (+ blood test if required)  FSH dose adjustments may be considered 3 follicles 17 mm Day of triggering  Ensure interval between antagonist and hCG does not exceed 30 h  hCG 5000-10,000 IU Oocyte retrieval 36 h YES NO US = ultrasonogram; OCP = oral contraceptive pill. Devroey et al. Hum Reprod. 2009;24:764.
  • 33. How Science is advancing!!
  • 35. How Science is advancing!!
  • 36. Proof of concept study • Not a RCT • Small number • To proof the theory
  • 37. Proof of concept study • Seven cases undergoing ICSI • Strict criteria: young age • Unexplained infertility • Mild male factor • Failed 2-3 IUI cycles • No PCOS • No endometriomas
  • 38. • 2-3 ampoules daily • CC staring from follicle diameter 11mm • Usually for 3-4 d • hCG if follicle 17mm
  • 39. Results • No premature lutenisation was reported till now • Number of retrieved oocytes ranged between 7-16 • MII oocytes more than 50% Waiting for pregnancy rate
  • 40. Should we rush? • To apply it • Too early • Needs more cases • Not magic
  • 41. There was enthusiasm for PGS • Advanced maternal age • Gianaroli 1999, Munne 1999, Kahraman 2000, Obasaji 2001, Munne 2003; Montag 2004; Platteau 2005 • Repeated IVF failure • Gianaroli 1999, Kahraman 2000, Pehlivan 2003,Munne 2003, Wilding 2004 • Recurrent miscarriage • Pellicer 1999, Rubio 2003, Rubio 2005, Munne 2005 • Severe male factor • Silber 2003, Platteau 2004
  • 42. Preimplantation genetic screening for advanced maternal age – reduced live birth rates OR 0.59 (0.44, 0.81)
  • 43. Triggering – GnRH agonist or hCG? Youssef et al, updated CR 2013 • 17 RCTs – 9 report OHSS – 5 report live birth rate • Risk of bias – Only 2/17 used blinding – 4/17 studies stopped prematurely for differing reasons – All studies were either funded by pharmaceutical companies or did not report their funding
  • 44. Ovarian hyperstimulation rate is reduced with agonist trigger in high risk women only OR 0.06 (0.01, 0.34) Youssef et al, updated 2013 *4 studies no events in either arm
  • 45. Live birth rate reduced with GnRHa triggering
  • 46. Conclusion • It is a valid idea with scientific background evidence • Needs more cases to ensure its validity
  • 47. For whom • for young women, • for those with unexplained infertility • mild male factor •i.e good responders