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Ovulation induction

December 27, 2022

"Induced ovulation" redirects here. For ovulation that is induced by copulation, see Induced ovulation (animals).

Ovulation induction is the stimulation of ovulation by medication. It is usually used in the sense of stimulation of the development of ovarian follicles[1][2][3] to reverse anovulation or oligoovulation.

Ovulation induction
Specialtyreproductive endocrinology and infertility, obstetrics
MeSHD010062
[edit on Wikidata]

Scope

The term ovulation induction can potentially also be used for:

  • Final maturation induction, in the sense of triggering oocyte release from relatively mature ovarian follicles during late follicular phase. In any case, ovarian stimulation (in the sense of stimulating the development of oocytes) is often used in conjunction with triggering oocyte release, such as for proper timing of artificial insemination.[4]
  • Controlled ovarian hyperstimulation (stimulating the development of multiple follicles of the ovaries in one single cycle), has also appeared in the scope of ovulation induction.[4] Controlled ovarian hyperstimulation is generally part of in vitro fertilization, and the aim is generally to develop multiple follicles (optimally between 11 and 14 antral follicles measuring 2–8 mm in diameter),[5] followed by transvaginal oocyte retrieval, co-incubation, followed by embryo transfer of a maximum of two embryos at a time.[6]
  • Also, where anovulation or oligovulation is secondary to another disease, the treatment for the underlying disease can be regarded as ovulation induction, by indirectly resulting in ovulation.

However, this article focuses on medical ovarian stimulation, during early to mid-follicular phase, without subsequent in vitro fertilization, with the aim of developing one or two ovulatory follicles (the maximum number before recommending sexual abstinence).[7]

Indications

Ovulation induction helps reversing anovulation or oligoovulation, that is, helping women who do not ovulate on their own regularly,[2] such as those with polycystic ovary syndrome (PCOS).[8]

Regimen alternatives

 
Hypothalamic–pituitary–gonadal axis in females, with estrogen exerting mainly negative feedback on follicle-stimulating hormone secretion from the pituitary gland.

The main alternatives for ovulation induction medications are:

Antiestrogens

Clomifene citrate

Clomifene citrate (or clomid) is the medication which is most commonly used to treat anovulation. It is a selective estrogen-receptor modulator, affecting the hypothalamic–pituitary–gonadal axis to respond as if there was an estrogen deficit in the body, in effect increasing the production of follicle-stimulating hormone. It is relatively easy and convenient to use.[10] Clomifene appears to inhibit estrogen receptors in hypothalamus, thereby inhibiting negative feedback of estrogen on production of follicle-stimulating hormone.[11] It may also result in direct stimulation of the hypothalamic-pituitary axis.[11] It also has an effect on cervical mucus quality and uterine mucosa, which might affect sperm penetration and survival, hence its early administration during the menstrual cycle. Clomifene citrate is a very efficient ovulation inductor, and has a success rate of 67%. Nevertheless, it only has a 37% success rate in inducing pregnancy. This difference may be due to the anti-estrogenic effect which clomifene citrate has on the endometrium, cervical mucus, uterine blood flow, as well as the resulting decrease in the motility of the fallopian tubes and the maturation of the oocytes.[12]

Letrozole

Letrozole has been used for ovarian stimulation by fertility doctors since 2001 because it has fewer side-effects than clomiphene and less chance of multiple gestation.[citation needed] A study of 150 babies following treatment with letrozole or letrozole and follicle-stimulating hormone presented at the American Society of Reproductive Medicine 2005 Conference found no difference in overall abnormalities but did find a significantly higher rate of locomotor and cardiac abnormalities among the group having taken letrozole compared to natural conception.[13] A larger, follow-up study with 911 babies compared those born following treatment with letrozole to those born following treatment with clomiphene.[14] That study also found no significant difference in the rate of overall abnormalities, but found that congenital cardiac anomalies was significantly higher in the clomiphene group compared to the letrozole group.

Dosage is generally 2.5 to 7.5 mg daily over 5 days. A higher dose of up to 12.5 mg per day results in increased follicular growth and a higher number of predicted ovulations, without a detrimental effect on endometrial thickness, and is considered in those who do not respond adequately to a lower dose.[15]

Tamoxifen

Tamoxifen affects estrogen receptors in a similar fashion as clomifene citrate. It is often used in the prevention and treatment of breast cancer. It can therefore also be used to treat patients that have a reaction to clomifene citrate.[16]

Follicle-stimulating hormone

Further information: Gonadotropin preparations

Preparations of follicle-stimulating hormone mainly include those derived from the urine of menopausal women, as well as recombinant preparations. The recombinant preparations are more pure and more easily administered, but they are more expensive. The urinary preparations are equally effective and less expensive, but are not as convenient to administer as they are available in vials versus injection pens.

Gonadotropin-releasing hormone pump

The gonadotropin-releasing hormone pump is used to release doses in a pulsatile fashion. This hormone is synthesised by the hypothalamus and induces the secretion of follicle-stimulating hormone by the pituitary gland. Gonadotropin-releasing hormone must be delivered in a pulsatile fashion to imitate the random secretion of the hypothalamus in order to stimulate the pituitary into secreting luteinizing hormone and follicle-stimulating hormone. The gonadotropin-releasing hormone pump is the size of a cigarette box and has a small catheter. Unlike other treatments, using the gonadotropin-releasing hormone pump usually does not result in multiple pregnancies. Filicori from the University of Bologna suggests that this might be because gonadotrophins are absent when the treatment is initiated, and therefore the hormones released by the pituitary (luteinizing hormone and follicle-stimulating hormone) can still take part in the retro-control of gonadotrophin secretion, mimicking the natural cycle.[17] This treatment can also be used for underweight and/or anorexic patients;[18] it has also been used in certain cases of hyperprolactimenia.

National and regional usage

In the Nordic countries, letrozole is practically the standard initial regimen used for ovulation induction, since no formulation of clomifene is registered for use there.[19][20]

India banned the usage of letrozole in 2011, citing potential risks to infants.[21] In 2012, an Indian parliamentary committee said that the drug controller office colluded with letrozole's makers to approve the drug for infertility in India.[22]

Technique

Although there are many possible additional diagnostic and interventional techniques, protocols for ovulation induction generally consist of:

Ultrasonography

 
Pregnancy rates in ovulation induction when using antiestrogens, as functions of the size of the leading follicle as measured by transvaginal ultrasonography at days 11 - 13 (bottom scale), as well as the thickness of the endometrial lining (4 different curves).[25]

During ovulation induction, it is recommended to start at a low dose and monitor the ovarian response with transvaginal ultrasound, including discernment of the number of developing follicles. Initial exam is most commonly started 4–6 days after last pill. Serial transvaginal ultrasound can reveal the size and number of developing follicles. It can also provide presumptive evidence of ovulation such as sudden collapse of the preovulatory follicle, and an increase in fluid volume in the rectouterine pouch. After ovulation, it may reveal signs of luteinization such as loss of clearly defined follicular margins and appearance of internal echoes.

Supernumerary follicles

A cycle with supernumerary follicles is usually defined as one where there are more than two follicles >16 mm in diameter.[26] It is generally recommended to have such cycles cancelled because of the risk of multiple pregnancy (see also the "Risks and side effects" section below).[26][7] In cancelled cycles, the woman or couple should be warned of the risks in case of supernumerary follicles, and should avoid sexual intercourse or use contraception until the next menstruation.[26] Induction of final maturation (such as done with hCG) may need to be withheld because of increased risk of ovarian hyperstimulation syndrome.[26] The starting dose of the inducing drug should be reduced in the next cycle.[26]

Alternatives to cancelling a cycle are mainly:

  • Aspiration of supernumerary follicles until one or two remain.[26][27]
  • Converting the protocol to IVF treatment with embryo transfer of up to two embryos only.[26]
  • Selective fetal reduction. This alternative confers a high risk of complications.[26]
  • Proceeding with any multiple pregnancy without fetal reduction, with the ensuing risk of complications. This alternative is not recommended.[26]

Lab tests

The following laboratory tests may be used to monitor induced cycles:[28]

  • Serum estradiol levels, starting 4–6 days after last pill
  • Adequacy of luteinizing hormone surge LH surge by urine tests 3 to 4 days after last clomifene pill
  • Post-coital test 1–3 days before ovulation to check whether there are at least 5 progressive sperm per HPF
  • Mid-luteal progesterone, with at least 10 ng/ml 7–9 days after ovulation being regarded as adequate.

Final maturation induction

Further information: Final maturation induction

Final maturation induction and release, such as by human chorionic gonadotropin (HCG or hCG) or recombinant luteinizing hormone, results in a predictable time of ovulation, with the interval from drug administration to ovulation depending on the type of drug. This avails for sexual intercourse or intrauterine insemination to conveniently be scheduled at ovulation, the most likely time to achieve pregnancy.[4]

As evidenced by clomifene-induced cycles, however, triggering oocyte release has been shown to decrease pregnancy chances compared to frequent monitoring with LH surge tests.[28] Therefore, in such cases, triggering oocyte release is best reserved for women who require intrauterine insemination and in whom luteinizing hormone monitoring proves difficult or unreliable.[28] It may also be used when luteinizing hormone monitoring has no shown an luteinizing hormone surge by cycle day 18 (where cycle day 1 is the first day of the preceding menstruation) and there is an ovarian follicle of over 20 mm in size.[29]

Repeat cycles

Ovulation induction can be repeated every menstrual cycle. For clomifene, the dosage may be increased by 50-mg increments in subsequent cycles until ovulation is achieved.[28][30] However, at a dosage of 200 mg, further increments are unlikely to increase pregnancy chances.[28]

It is not recommended by the manufacturer of clomifene to use it for more than 6 consecutive cycles.[31][32] In women with anovulation, 7 - 12 attempted cycles of pituitary feedback regimens (as evidenced by clomifene citrate) are recommended before switching to gonadotrophins, since the latter ones are more expensive and less easy to control.[9]

It is no longer recommended to perform an ultrasound examination to exclude any significant residual ovarian enlargement before each new treatment cycle.[28]

Risks and side effects

Ultrasound and regular hormone checks mitigate risks throughout the process. However, there are still some risks with the procedure.

Ovarian hyperstimulation syndrome occurs in 5-10% of cases.[33] Symptoms depend on whether the case is mild, moderate, or severe, and can range from bloating and nausea, through to shortness of breathe, pleural effusion, and excessive weight gain (more than 2 pounds per day).

Multiple pregnancy

There is also the risk that more than one egg is produced, leading to twins or triplets. Women with polycystic ovary syndrome may be particularly at risk. Multiple pregnancy occurs in approximately 15-20% of cases following cycles induced with gonadotrophins such as human menopausal gonadotropin and follicle-stimulating hormone.[26] The risks associated with multiple pregnancy are much higher than singleton pregnancy; incidence of perinatal death is seven times higher in triplet births and five times higher in twin births than the risks associated with a singleton pregnancy.[34][35] It is therefore important to adapt the treatment to each individual patient.[36] If more than one or two ovulatory follicles are detected on ultrasonography, sexual abstinence is recommended.[7]

Alternatives

References

  1. ^ Ovulation Problems and Infertility: Treatment of ovulation problems with Clomid and other fertility drugs. Advanced Fertility Center of Chicago. Gurnee & Crystal Lake, Illinois. Retrieved on Mars 7, 2010
  2. ^ a b Flinders reproductive medicine > Ovulation Induction 2009-10-03 at the Wayback Machine Retrieved on Mars 7, 2010
  3. ^ fertilityLifeLines > Ovulation Induction 2013-03-10 at the Wayback Machine Retrieved on Mars 7, 2010
  4. ^ a b c IVF.com > Ovulation Induction 2012-02-26 at the Wayback Machine Retrieved on Mars 7, 2010
  5. ^ Antral Follicle Counts, Resting Follicles, Ovarian Volume and Ovarian Reserve. Testing of egg supply and predicting response to ovarian stimulation drugs Advanced Fertility Center of Chicago. Retrieved on October 2, 2009
  6. ^ Fertility: assessment and treatment for people with fertility problems. NICE clinical guideline CG156 - Issued: February 2013
  7. ^ a b c "Ovulation Induction". Manchester University. Retrieved 2019-04-04.
  8. ^ Ovulation Problems and Infertility: Treatment of ovulation problems with Clomid and other fertility drugs Advanced Fertility Center of Chicago. Gurnee & Crystal Lake, Illinois
  9. ^ a b c Weiss, N. S.; Braam, S.; Konig, T. E.; Hendriks, M. L.; Hamilton, C. J.; Smeenk, J. M. J.; Koks, C. A. M.; Kaaijk, E. M.; Hompes, P. G. A.; Lambalk, C. B.; van der Veen, F.; Mol, B. W. J.; van Wely, M. (2014). "How long should we continue clomiphene citrate in anovulatory women?". Human Reproduction. 29 (11): 2482–2486. doi:10.1093/humrep/deu215. ISSN 0268-1161. PMID 25164024.
  10. ^ Lord JM, Flight IH, Norman RJ (October 2003). "Metformin in polycystic ovary syndrome: systematic review and meta-analysis". BMJ. 327 (7421): 951–0. doi:10.1136/bmj.327.7421.951. PMC 259161. PMID 14576245.
  11. ^ a b DrugBank > Clomifene. Updated on April 19, 2011
  12. ^ Kousta E, White DM, Franks S (1997). "Modern use of clomiphene citrate in induction of ovulation". Hum. Reprod. Update. 3 (4): 359–365. doi:10.1093/humupd/3.4.359. PMID 9459281.
  13. ^ Biljan MM, Hemmings R, Brassard N (2005). "The Outcome of 150 Babies Following the Treatment With Letrozole or Letrozole and Gonadotropins". Fertility and Sterility. 84: S95. doi:10.1016/j.fertnstert.2005.07.230.
  14. ^ Tulandi T, Martin J, Al-Fadhli R, et al. (June 2006). "Congenital malformations among 911 newborns conceived after infertility treatment with letrozole or clomiphene citrate". Fertility and Sterility. 85 (6): 1761–5. doi:10.1016/j.fertnstert.2006.03.014. PMID 16650422.
  15. ^ Pritts, Elizabeth A.; Yuen, Alexander K.; Sharma, Shefaali; Genisot, Robert; Olive, David L. (2011). "The Use of High Dose Letrozole in Ovulation Induction and Controlled Ovarian Hyperstimulation". ISRN Obstetrics and Gynecology. 2011: 1–4. doi:10.5402/2011/242864. ISSN 2090-4436. PMC 3236406. PMID 22191042.
  16. ^ Boostanfar R, Jain JK, Mishell DR, Paulson RJ (May 2001). "A prospective randomized trial comparing clomiphene citrate with tamoxifen citrate for ovulation induction". Fertil. Steril. 75 (5): 1024–1026. doi:10.1016/S0015-0282(01)01749-6. PMID 11334921.
  17. ^ Filicori M, Flamigni C, Dellai P, et al. (October 1994). "Treatment of anovulation with pulsatile gonadotropin-releasing hormone: prognostic factors and clinical results in 600 cycles". J. Clin. Endocrinol. Metab. 79 (4): 1215–1220. doi:10.1210/jcem.79.4.7962297. PMID 7962297.
  18. ^ Braat DD, Schoemaker R, Schoemaker J (February 1991). "Life table analysis of fecundity in intravenously gonadotropin-releasing hormone-treated patients with normogonadotropic and hypogonadotropic amenorrhea". Fertil. Steril. 55 (2): 266–71. doi:10.1016/S0015-0282(16)54113-2. PMID 1991525.
  19. ^ "Pergotime avregistreres 31.12.2016". Statens legemiddelverk. 2016-09-09.
  20. ^ "Pergotime". FASS.
  21. ^ Sinha, Kounteya (18 October 2011). . The Times of India. Archived from the original on 14 August 2013. Retrieved 14 November 2011.
  22. ^ . The Times of India. 10 April 2007. Archived from the original on 12 November 2013. Retrieved 9 May 2012.
  23. ^ Emre Seli, Aydin Arici. "Patient education: Ovulation induction with clomiphene (Beyond the Basics)". UpToDate. Topic last updated: Aug 01, 2017
  24. ^ Robert F Casper. "Ovulation induction with letrozole". UpToDate. Topic last updated: Sep 17, 2018.
  25. ^ Palatnik, Anna; Strawn, Estil; Szabo, Aniko; Robb, Paul (2012). "What is the optimal follicular size before triggering ovulation in intrauterine insemination cycles with clomiphene citrate or letrozole? An analysis of 988 cycles". Fertility and Sterility. 97 (5): 1089–1094.e3. doi:10.1016/j.fertnstert.2012.02.018. ISSN 0015-0282. PMID 22459633.
  26. ^ a b c d e f g h i j Hong Kong College of Obstetricians and Gynaecologists > Guidelines for use of gonadotrophins- revised September 9, 2012, at the Wayback Machine. Number 1. April 2003.
  27. ^ Albano, C.; Platteau, P.; Nogueira, D.; Cortvrindt, R.; Smitz, J.; Devroey, P. (2001). "Avoidance of multiple pregnancies after ovulation induction by supernumerary preovulatory follicular reduction". Fertility and Sterility. 76 (4): 820–822. doi:10.1016/S0015-0282(01)02379-2. PMID 11591420.
  28. ^ a b c d e f Practice Committee of the American Society for Reproductive Medicine (August 2013). "Use of clomiphene citrate in infertile women: a committee opinion". Fertil. Steril. 100 (2): 341–8. doi:10.1016/j.fertnstert.2013.05.033. PMID 23809505.
  29. ^ Clomiphene Citrate, Clomid Archived 2014-05-10 at archive.today. By Robert B. McWilliams. The Center for Reproduction and Women's Health Care, Houston, Texas. Retrieved May 2014
  30. ^ Medications for Inducing Ovulation from American Society for Reproductive Medicine. Revised 2012.
  31. ^ "Clomiphene citrate tablets label" (PDF). Revised October 2012: FDA. (PDF) from the original on September 27, 2016. Retrieved September 11, 2016.{{cite web}}: CS1 maint: location (link)
  32. ^ Trabert, B.; Lamb, E. J.; Scoccia, B.; Moghissi, K. S.; Westhoff, C. L.; Niwa, S.; Brinton, L. A. (2013). "Ovulation-inducing drugs and ovarian cancer risk: Results from an extended follow-up of a large US infertility cohort". Fertility and Sterility. 100 (6): 1660–6. doi:10.1016/j.fertnstert.2013.08.008. PMC 3873340. PMID 24011610.
  33. ^ Ovulation Induction Risks and Overview
  34. ^ Bergh T, Ericson A, Hillensjö T, Nygren KG, Wennerholm UB (November 1999). "Deliveries and children born after in-vitro fertilisation in Sweden 1982-95: a retrospective cohort study". Lancet. 354 (9190): 1579–1585. doi:10.1016/S0140-6736(99)04345-7. PMID 10560671. S2CID 11057942.
  35. ^ Fisk NM, Trew G (November 1999). "Two's company, three's a crowd for embryo transfer". Lancet. 354 (9190): 1572–1573. doi:10.1016/S0140-6736(99)00290-1. PMID 10560665. S2CID 37575727.
  36. ^ Eshre Capri Workshop Group (2003). "Mono-ovulatory cycles: a key goal in profertility programmes". Hum. Reprod. Update. 9 (3): 263–274. doi:10.1093/humupd/dmg020. PMID 12859047.
  37. ^ a b (PDF). Archived from the original (PDF) on 2012-03-09. Retrieved 2011-09-25.

December 27, 2022
ovulation, induction, induced, ovulation, redirects, here, ovulation, that, induced, copulation, induced, ovulation, animals, stimulation, ovulation, medication, usually, used, sense, stimulation, development, ovarian, follicles, reverse, anovulation, oligoovu. Induced ovulation redirects here For ovulation that is induced by copulation see Induced ovulation animals Ovulation induction is the stimulation of ovulation by medication It is usually used in the sense of stimulation of the development of ovarian follicles 1 2 3 to reverse anovulation or oligoovulation Ovulation inductionSpecialtyreproductive endocrinology and infertility obstetricsMeSHD010062 edit on Wikidata Contents 1 Scope 2 Indications 3 Regimen alternatives 3 1 Antiestrogens 3 1 1 Clomifene citrate 3 1 2 Letrozole 3 1 3 Tamoxifen 3 2 Follicle stimulating hormone 3 3 Gonadotropin releasing hormone pump 3 4 National and regional usage 4 Technique 4 1 Ultrasonography 4 1 1 Supernumerary follicles 4 2 Lab tests 4 3 Final maturation induction 4 4 Repeat cycles 5 Risks and side effects 5 1 Multiple pregnancy 6 Alternatives 7 ReferencesScope EditThe term ovulation induction can potentially also be used for Final maturation induction in the sense of triggering oocyte release from relatively mature ovarian follicles during late follicular phase In any case ovarian stimulation in the sense of stimulating the development of oocytes is often used in conjunction with triggering oocyte release such as for proper timing of artificial insemination 4 Controlled ovarian hyperstimulation stimulating the development of multiple follicles of the ovaries in one single cycle has also appeared in the scope of ovulation induction 4 Controlled ovarian hyperstimulation is generally part of in vitro fertilization and the aim is generally to develop multiple follicles optimally between 11 and 14 antral follicles measuring 2 8 mm in diameter 5 followed by transvaginal oocyte retrieval co incubation followed by embryo transfer of a maximum of two embryos at a time 6 Also where anovulation or oligovulation is secondary to another disease the treatment for the underlying disease can be regarded as ovulation induction by indirectly resulting in ovulation However this article focuses on medical ovarian stimulation during early to mid follicular phase without subsequent in vitro fertilization with the aim of developing one or two ovulatory follicles the maximum number before recommending sexual abstinence 7 Indications EditOvulation induction helps reversing anovulation or oligoovulation that is helping women who do not ovulate on their own regularly 2 such as those with polycystic ovary syndrome PCOS 8 Regimen alternatives Edit Hypothalamic pituitary gonadal axis in females with estrogen exerting mainly negative feedback on follicle stimulating hormone secretion from the pituitary gland The main alternatives for ovulation induction medications are Antiestrogen causing an inhibition of the negative feedback of estrogen on the pituitary gland resulting in an increase in secretion of follicle stimulating hormone Medications in use for this effect are mainly clomifene citrate and tamoxifen both being selective estrogen receptor modulators as well as letrozole an aromatase inhibitor citation needed Follicle stimulating hormone directly stimulating the ovaries In women with anovulation it may be an alternative after 7 to 12 attempted cycles of antiestrogens as evidenced by clomifene citrate since the latter ones are less expensive and more easy to control 9 Antiestrogens Edit Clomifene citrate Edit Clomifene citrate or clomid is the medication which is most commonly used to treat anovulation It is a selective estrogen receptor modulator affecting the hypothalamic pituitary gonadal axis to respond as if there was an estrogen deficit in the body in effect increasing the production of follicle stimulating hormone It is relatively easy and convenient to use 10 Clomifene appears to inhibit estrogen receptors in hypothalamus thereby inhibiting negative feedback of estrogen on production of follicle stimulating hormone 11 It may also result in direct stimulation of the hypothalamic pituitary axis 11 It also has an effect on cervical mucus quality and uterine mucosa which might affect sperm penetration and survival hence its early administration during the menstrual cycle Clomifene citrate is a very efficient ovulation inductor and has a success rate of 67 Nevertheless it only has a 37 success rate in inducing pregnancy This difference may be due to the anti estrogenic effect which clomifene citrate has on the endometrium cervical mucus uterine blood flow as well as the resulting decrease in the motility of the fallopian tubes and the maturation of the oocytes 12 Letrozole Edit Letrozole has been used for ovarian stimulation by fertility doctors since 2001 because it has fewer side effects than clomiphene and less chance of multiple gestation citation needed A study of 150 babies following treatment with letrozole or letrozole and follicle stimulating hormone presented at the American Society of Reproductive Medicine 2005 Conference found no difference in overall abnormalities but did find a significantly higher rate of locomotor and cardiac abnormalities among the group having taken letrozole compared to natural conception 13 A larger follow up study with 911 babies compared those born following treatment with letrozole to those born following treatment with clomiphene 14 That study also found no significant difference in the rate of overall abnormalities but found that congenital cardiac anomalies was significantly higher in the clomiphene group compared to the letrozole group Dosage is generally 2 5 to 7 5 mg daily over 5 days A higher dose of up to 12 5 mg per day results in increased follicular growth and a higher number of predicted ovulations without a detrimental effect on endometrial thickness and is considered in those who do not respond adequately to a lower dose 15 Tamoxifen Edit Tamoxifen affects estrogen receptors in a similar fashion as clomifene citrate It is often used in the prevention and treatment of breast cancer It can therefore also be used to treat patients that have a reaction to clomifene citrate 16 Follicle stimulating hormone Edit Further information Gonadotropin preparations Preparations of follicle stimulating hormone mainly include those derived from the urine of menopausal women as well as recombinant preparations The recombinant preparations are more pure and more easily administered but they are more expensive The urinary preparations are equally effective and less expensive but are not as convenient to administer as they are available in vials versus injection pens Gonadotropin releasing hormone pump Edit The gonadotropin releasing hormone pump is used to release doses in a pulsatile fashion This hormone is synthesised by the hypothalamus and induces the secretion of follicle stimulating hormone by the pituitary gland Gonadotropin releasing hormone must be delivered in a pulsatile fashion to imitate the random secretion of the hypothalamus in order to stimulate the pituitary into secreting luteinizing hormone and follicle stimulating hormone The gonadotropin releasing hormone pump is the size of a cigarette box and has a small catheter Unlike other treatments using the gonadotropin releasing hormone pump usually does not result in multiple pregnancies Filicori from the University of Bologna suggests that this might be because gonadotrophins are absent when the treatment is initiated and therefore the hormones released by the pituitary luteinizing hormone and follicle stimulating hormone can still take part in the retro control of gonadotrophin secretion mimicking the natural cycle 17 This treatment can also be used for underweight and or anorexic patients 18 it has also been used in certain cases of hyperprolactimenia National and regional usage Edit In the Nordic countries letrozole is practically the standard initial regimen used for ovulation induction since no formulation of clomifene is registered for use there 19 20 India banned the usage of letrozole in 2011 citing potential risks to infants 21 In 2012 an Indian parliamentary committee said that the drug controller office colluded with letrozole s makers to approve the drug for infertility in India 22 Technique EditAlthough there are many possible additional diagnostic and interventional techniques protocols for ovulation induction generally consist of Determining the first day of the last menstruation which is termed day 1 In case of amenorrhea a period can be induced by intake of an oral progestin for 10 days Daily administration of the ovulation induction regimen starting on day 3 4 or 5 23 and it is usually taken for 5 days 9 24 Sexual intercourse or artificial insemination by the time of ovulation Ultrasonography Edit Pregnancy rates in ovulation induction when using antiestrogens as functions of the size of the leading follicle as measured by transvaginal ultrasonography at days 11 13 bottom scale as well as the thickness of the endometrial lining 4 different curves 25 During ovulation induction it is recommended to start at a low dose and monitor the ovarian response with transvaginal ultrasound including discernment of the number of developing follicles Initial exam is most commonly started 4 6 days after last pill Serial transvaginal ultrasound can reveal the size and number of developing follicles It can also provide presumptive evidence of ovulation such as sudden collapse of the preovulatory follicle and an increase in fluid volume in the rectouterine pouch After ovulation it may reveal signs of luteinization such as loss of clearly defined follicular margins and appearance of internal echoes Supernumerary follicles Edit A cycle with supernumerary follicles is usually defined as one where there are more than two follicles gt 16 mm in diameter 26 It is generally recommended to have such cycles cancelled because of the risk of multiple pregnancy see also the Risks and side effects section below 26 7 In cancelled cycles the woman or couple should be warned of the risks in case of supernumerary follicles and should avoid sexual intercourse or use contraception until the next menstruation 26 Induction of final maturation such as done with hCG may need to be withheld because of increased risk of ovarian hyperstimulation syndrome 26 The starting dose of the inducing drug should be reduced in the next cycle 26 Alternatives to cancelling a cycle are mainly Aspiration of supernumerary follicles until one or two remain 26 27 Converting the protocol to IVF treatment with embryo transfer of up to two embryos only 26 Selective fetal reduction This alternative confers a high risk of complications 26 Proceeding with any multiple pregnancy without fetal reduction with the ensuing risk of complications This alternative is not recommended 26 Lab tests Edit The following laboratory tests may be used to monitor induced cycles 28 Serum estradiol levels starting 4 6 days after last pill Adequacy of luteinizing hormone surge LH surge by urine tests 3 to 4 days after last clomifene pill Post coital test 1 3 days before ovulation to check whether there are at least 5 progressive sperm per HPF Mid luteal progesterone with at least 10 ng ml 7 9 days after ovulation being regarded as adequate Final maturation induction Edit Further information Final maturation induction Final maturation induction and release such as by human chorionic gonadotropin HCG or hCG or recombinant luteinizing hormone results in a predictable time of ovulation with the interval from drug administration to ovulation depending on the type of drug This avails for sexual intercourse or intrauterine insemination to conveniently be scheduled at ovulation the most likely time to achieve pregnancy 4 As evidenced by clomifene induced cycles however triggering oocyte release has been shown to decrease pregnancy chances compared to frequent monitoring with LH surge tests 28 Therefore in such cases triggering oocyte release is best reserved for women who require intrauterine insemination and in whom luteinizing hormone monitoring proves difficult or unreliable 28 It may also be used when luteinizing hormone monitoring has no shown an luteinizing hormone surge by cycle day 18 where cycle day 1 is the first day of the preceding menstruation and there is an ovarian follicle of over 20 mm in size 29 Repeat cycles Edit Ovulation induction can be repeated every menstrual cycle For clomifene the dosage may be increased by 50 mg increments in subsequent cycles until ovulation is achieved 28 30 However at a dosage of 200 mg further increments are unlikely to increase pregnancy chances 28 It is not recommended by the manufacturer of clomifene to use it for more than 6 consecutive cycles 31 32 In women with anovulation 7 12 attempted cycles of pituitary feedback regimens as evidenced by clomifene citrate are recommended before switching to gonadotrophins since the latter ones are more expensive and less easy to control 9 It is no longer recommended to perform an ultrasound examination to exclude any significant residual ovarian enlargement before each new treatment cycle 28 Risks and side effects EditUltrasound and regular hormone checks mitigate risks throughout the process However there are still some risks with the procedure Ovarian hyperstimulation syndrome occurs in 5 10 of cases 33 Symptoms depend on whether the case is mild moderate or severe and can range from bloating and nausea through to shortness of breathe pleural effusion and excessive weight gain more than 2 pounds per day Multiple pregnancy Edit There is also the risk that more than one egg is produced leading to twins or triplets Women with polycystic ovary syndrome may be particularly at risk Multiple pregnancy occurs in approximately 15 20 of cases following cycles induced with gonadotrophins such as human menopausal gonadotropin and follicle stimulating hormone 26 The risks associated with multiple pregnancy are much higher than singleton pregnancy incidence of perinatal death is seven times higher in triplet births and five times higher in twin births than the risks associated with a singleton pregnancy 34 35 It is therefore important to adapt the treatment to each individual patient 36 If more than one or two ovulatory follicles are detected on ultrasonography sexual abstinence is recommended 7 Alternatives EditIn vitro fertilization including controlled ovarian hyperstimulation In vitro maturation is letting ovarian follicles mature in vitro and this technique can potentially be an alternative both to anovulation reversal and oocyte release triggering Rather oocytes can mature outside the body such as prior to IVF Hence no or at least a lower dose of gonadotropins have to be injected in the body 37 However there still isn t enough evidence to prove the effectiveness and security of the technique 37 References Edit Ovulation Problems and Infertility Treatment of ovulation problems with Clomid and other fertility drugs Advanced Fertility Center of Chicago Gurnee amp Crystal Lake Illinois Retrieved on Mars 7 2010 a b Flinders reproductive medicine gt Ovulation Induction Archived 2009 10 03 at the Wayback Machine Retrieved on Mars 7 2010 fertilityLifeLines gt Ovulation Induction Archived 2013 03 10 at the Wayback Machine Retrieved on Mars 7 2010 a b c IVF com gt Ovulation Induction Archived 2012 02 26 at the Wayback Machine Retrieved on Mars 7 2010 Antral Follicle Counts Resting Follicles Ovarian Volume and Ovarian Reserve Testing of egg supply and predicting response to ovarian stimulation drugs Advanced Fertility Center of Chicago Retrieved on October 2 2009 Fertility assessment and treatment for people with fertility problems NICE clinical guideline CG156 Issued February 2013 a b c Ovulation Induction Manchester University Retrieved 2019 04 04 Ovulation Problems and Infertility Treatment of ovulation problems with Clomid and other fertility drugs Advanced Fertility Center of Chicago Gurnee amp Crystal Lake Illinois a b c Weiss N S Braam S Konig T E Hendriks M L Hamilton C J Smeenk J M J Koks C A M Kaaijk E M Hompes P G A Lambalk C B van der Veen F Mol B W J van Wely M 2014 How long should we continue clomiphene citrate in anovulatory women Human Reproduction 29 11 2482 2486 doi 10 1093 humrep deu215 ISSN 0268 1161 PMID 25164024 Lord JM Flight IH Norman RJ October 2003 Metformin in polycystic ovary syndrome systematic review and meta analysis BMJ 327 7421 951 0 doi 10 1136 bmj 327 7421 951 PMC 259161 PMID 14576245 a b DrugBank gt Clomifene Updated on April 19 2011 Kousta E White DM Franks S 1997 Modern use of clomiphene citrate in induction of ovulation Hum Reprod Update 3 4 359 365 doi 10 1093 humupd 3 4 359 PMID 9459281 Biljan MM Hemmings R Brassard N 2005 The Outcome of 150 Babies Following the Treatment With Letrozole or Letrozole and Gonadotropins Fertility and Sterility 84 S95 doi 10 1016 j fertnstert 2005 07 230 Tulandi T Martin J Al Fadhli R et al June 2006 Congenital malformations among 911 newborns conceived after infertility treatment with letrozole or clomiphene citrate Fertility and Sterility 85 6 1761 5 doi 10 1016 j fertnstert 2006 03 014 PMID 16650422 Pritts Elizabeth A Yuen Alexander K Sharma Shefaali Genisot Robert Olive David L 2011 The Use of High Dose Letrozole in Ovulation Induction and Controlled Ovarian Hyperstimulation ISRN Obstetrics and Gynecology 2011 1 4 doi 10 5402 2011 242864 ISSN 2090 4436 PMC 3236406 PMID 22191042 Boostanfar R Jain JK Mishell DR Paulson RJ May 2001 A prospective randomized trial comparing clomiphene citrate with tamoxifen citrate for ovulation induction Fertil Steril 75 5 1024 1026 doi 10 1016 S0015 0282 01 01749 6 PMID 11334921 Filicori M Flamigni C Dellai P et al October 1994 Treatment of anovulation with pulsatile gonadotropin releasing hormone prognostic factors and clinical results in 600 cycles J Clin Endocrinol Metab 79 4 1215 1220 doi 10 1210 jcem 79 4 7962297 PMID 7962297 Braat DD Schoemaker R Schoemaker J February 1991 Life table analysis of fecundity in intravenously gonadotropin releasing hormone treated patients with normogonadotropic and hypogonadotropic amenorrhea Fertil Steril 55 2 266 71 doi 10 1016 S0015 0282 16 54113 2 PMID 1991525 Pergotime avregistreres 31 12 2016 Statens legemiddelverk 2016 09 09 Pergotime FASS Sinha Kounteya 18 October 2011 Finally expert panel bans fertility drug Letrozole The Times of India Archived from the original on 14 August 2013 Retrieved 14 November 2011 House panel to govt Punish those guilty of approving Letrozole The Times of India 10 April 2007 Archived from the original on 12 November 2013 Retrieved 9 May 2012 Emre Seli Aydin Arici Patient education Ovulation induction with clomiphene Beyond the Basics UpToDate Topic last updated Aug 01 2017 Robert F Casper Ovulation induction with letrozole UpToDate Topic last updated Sep 17 2018 Palatnik Anna Strawn Estil Szabo Aniko Robb Paul 2012 What is the optimal follicular size before triggering ovulation in intrauterine insemination cycles with clomiphene citrate or letrozole An analysis of 988 cycles Fertility and Sterility 97 5 1089 1094 e3 doi 10 1016 j fertnstert 2012 02 018 ISSN 0015 0282 PMID 22459633 a b c d e f g h i j Hong Kong College of Obstetricians and Gynaecologists gt Guidelines for use of gonadotrophins revised Archived September 9 2012 at the Wayback Machine Number 1 April 2003 Albano C Platteau P Nogueira D Cortvrindt R Smitz J Devroey P 2001 Avoidance of multiple pregnancies after ovulation induction by supernumerary preovulatory follicular reduction Fertility and Sterility 76 4 820 822 doi 10 1016 S0015 0282 01 02379 2 PMID 11591420 a b c d e f Practice Committee of the American Society for Reproductive Medicine August 2013 Use of clomiphene citrate in infertile women a committee opinion Fertil Steril 100 2 341 8 doi 10 1016 j fertnstert 2013 05 033 PMID 23809505 Clomiphene Citrate Clomid Archived 2014 05 10 at archive today By Robert B McWilliams The Center for Reproduction and Women s Health Care Houston Texas Retrieved May 2014 Medications for Inducing Ovulation from American Society for Reproductive Medicine Revised 2012 Clomiphene citrate tablets label PDF Revised October 2012 FDA Archived PDF from the original on September 27 2016 Retrieved September 11 2016 a href Template Cite web html title Template Cite web cite web a CS1 maint location link Trabert B Lamb E J Scoccia B Moghissi K S Westhoff C L Niwa S Brinton L A 2013 Ovulation inducing drugs and ovarian cancer risk Results from an extended follow up of a large US infertility cohort Fertility and Sterility 100 6 1660 6 doi 10 1016 j fertnstert 2013 08 008 PMC 3873340 PMID 24011610 Ovulation Induction Risks and Overview Bergh T Ericson A Hillensjo T Nygren KG Wennerholm UB November 1999 Deliveries and children born after in vitro fertilisation in Sweden 1982 95 a retrospective cohort study Lancet 354 9190 1579 1585 doi 10 1016 S0140 6736 99 04345 7 PMID 10560671 S2CID 11057942 Fisk NM Trew G November 1999 Two s company three s a crowd for embryo transfer Lancet 354 9190 1572 1573 doi 10 1016 S0140 6736 99 00290 1 PMID 10560665 S2CID 37575727 Eshre Capri Workshop Group 2003 Mono ovulatory cycles a key goal in profertility programmes Hum Reprod Update 9 3 263 274 doi 10 1093 humupd dmg020 PMID 12859047 a b Vejledning om kunstig befrugtning 2006 Danish PDF Archived from the original PDF on 2012 03 09 Retrieved 2011 09 25 Retrieved from https en wikipedia org w index php title Ovulation induction amp oldid 1112978821, wikipedia, wiki, book, books, library,

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