E-ISSN: 2149-9330
The effects of growth hormone supplementation in poor ovarian responders undergoing In vitro fertilization or Intracytoplasmic sperm injection: A systematic review and meta-analysis of randomized controlled trials
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VOLUME: 21 ISSUE: 3
P: 208-218
September 2024

The effects of growth hormone supplementation in poor ovarian responders undergoing In vitro fertilization or Intracytoplasmic sperm injection: A systematic review and meta-analysis of randomized controlled trials

Turk J Obstet Gynecol 2024;21(3):208-218
DOI: 10.4274/tjod.galenos.2024.59944
Faezeh Zakerinasab 1
Qumars Behfar 2
Reza Parsaee 3
Fariba Arbab Mojeni 4
Arina Ansari 5
Niloofar Deravi 6
Reza Khademi 7
1. Mashhad University of Medical Sciences Department of Obstetrics and Gynecology, Mashhad, Iran
2. University of Cologne Faculty of Medicine and University Hospital Cologne Department of Neurology, Cologne, Germany
3. Shiraz University of Medical Sciences Transplant Research Center, Shiraz, Iran
4. Mazandaran University of Medical Sciences School of Medicine, Student Research Committee, Sari, Iran
5. North Khorasan University of Medical Sciences School of Medicine, Student Research Committee, Bojnurd, Iran
6. Shahid Beheshti University of Medical Sciences School of Medicine, Tehran, Iran
7. Mashhad University of Medical Sciences Faculty of Medicine Student Research Committee, Mashhad, Iran
No information available.
No information available
Received Date: 28.06.2024
Accepted Date: 27.08.2024
Online Date: 04.09.2024
Publish Date: 04.09.2024
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Abstract

To evaluate the effect of growth hormone (GH) supplementation on outcomes of in vitro fertilization (IVF) or Intracytoplasmic sperm injection (ICSI) for women with poor ovarian response. Relevant randomized controlled trials (RCTs) were obtained through search in several databases including PubMed, Scopus, Clinicaltrials.gov, Google Scholar, and Cochrane Library. Outcome measures included live birth rate, clinical pregnancy rate, cycle cancelation rate, number of retrieved oocytes, number of transferred embryos, total dose of gonadotropin, duration of gonadotropin treatment, and peak estradiol level. Additionally, a meta-regression analysis was performed to acknowledge any potential linear relationships between these outcomes and IVF success. After analyzing 18 RCTs comprising of 1870 patients, the study found that GH supplementation improved the number of retrieved oocytes [standardized mean difference (SMD), 0.65; 95% confidence interval (CI), 0.29-1.00] and transferred embryos group (SMD, 0.80, 95% CI, 0.39, 1.21) as well as peak E2 level (SMD, 1.20; 95% CI, 0.59, 1.81). While reduced the total dose and duration of gonadotropin treatment (SMD, -0.82, 95% CI, -1.25, -0.39, and SMD, -0.63, 95% CI, -1.04, -0.22, respectively). The meta-regression analysis found no linear relationship between clinical pregnancy, live birth rate, or cycle cancelation rate and the outcomes measured (p>0.1). Based on the available evidence, GH supplementation appears to improve the outcomes of IVF or ICSI in women with poor response. However, there is a need for further RCTs with larger sample sizes to determine the cost-effectiveness of adding GH to conventional protocols of IVF/ICSI for treating infertility in women with poor ovarian response.

Introduction

Diminished ovarian reserve (DOR) affects a significant percentage of women, between 8-15%, and its incidence increases in women over 40, affecting more than half of them(1). Poor responders (POR) are women with DOR who experience difficulties producing enough mature oocytes, leading to lower embryo quality and higher cycle cancellation rates(2). The European Society for Human Reproduction and Embryology introduced a standardized set of criteria named Bologna in 2011 to diagnose women with poor ovarian response(3). To diagnose a patient with POR, at least two of the following three criteria must be met: (i) advanced maternal age (40 years or older) or another risk factor for POR; (ii) a history of poor ovarian response (three or fewer oocytes retrieved or a previous cycle that was canceled); and (iii) abnormal results from ovarian reserve tests (antral follicle count [AFC] of less than 5-7 follicles or Anti-Mullerian hormone [AMH] levels below 0.5-1.1 ng/mL). If a patient experiences two instances of POR despite receiving maximal stimulation, she can be diagnosed with the condition, even if the other criteria are not met. When considering treatment strategies for stimulating ovarian function in POR, one potential option is to administer gonadotropin-releasing hormone (GnRH) agonists(4). While this approach has shown promise, it can also have its limitations. For example, it may inhibit ovarian function and response and require an increased dose of gonadotropin, thus leading to early luteinizing hormone (LH) secretion and potentially contributing to in vitro fertilization (IVF) failure rates(5). In an effort to improve outcomes, various ovarian hyper-stimulation protocols have been explored, including  the use of growth hormone as an additional treatment in stimulation protocols. However, an ideal protocol for POR has yet to be established, and more research is needed to optimize treatment strategies.

GH is a protein originating from the ovary and pituitary gland that targets the uterine and ovarian tissues in the female reproductive system. In general, GH promotes the overall ovarian health through its antioxidant effect(6). However, the specific effects of GH are mediated by its receptors in myometrium(7), uterine decidua(8), granulosa cells and stroma of human ovary(9). Ovarian GH, by creating a GH-GH receptor complex, increases the phosphorylation of janus kinase-2 and subsequently activates STAT molecules, thereby changing gene expression and cell performance. It also intercedes the development of primordial follicles to pre-antral in a paracrine manner. With gonadotropin receptors upregulation, GH increases the sensitivity of granulosa cells to follicle-stimulating hormone (FSH) and LH. Moreover, some studies have suggested its steroidogenesis effect, too. Additionally, GH enhances the oocytes quality by increasing the nucleal and cytoplasm maturation, which is done by the inhibitory effect of GH on connexin 43 and the increase of cumulus cells. Finally, GH improves implantation through its proliferative effect on uterine decidua cells(6). Growth hormone is primarily released by the pituitary gland and plays a key role in cell growth, development, and metabolism.

GH is secreted mostly by pituitary gland, and affects cell growth, development as well as metabolism(10). The use of GH as a co-treatment for various ovarian stimulation protocols in reproductive medicine has been the subject of extensive research. GH stimulates insulin-like growth factor 1 (IGF-1) production in both the liver and ovarian follicles. IGF-1 helps regulate steroidogenesis, enhances gonadotropin effect on granulosa and theca cells, and increases ovarian sensitivity to gonadotrophins, thereby advancing early follicular development, preventing of antral follicles involution, and promoting oocyte maturation(11-13). Furthermore, recent studies indicate that GH takes part in enhancing follicular survival and cell proliferation as well as promoting high-quality embryos and increasing implantation rate(14, 15). However, the effect of GH administration on IVF/intracytoplasmic sperm injection (ICSI), outcomes is still not clearly understood, with studies showing contradictory results. While some research has shown that growth hormone (GH) positively affects oocytes, the endometrium, and improves embryo development outcomes, others have not replicated these results(16-19). In conclusion, t the majority of evidence suggests GH is crucial for follicular development, estrogen production, and the maturation of oocytes via IGF-1, while its effect on the efficacy of IVF or ICSI techniques remains a subject of ongoing research.

The addition of GH to IVF/ICSI protocols has been the subject of several recent studies, including a 2020 meta-analysis which reported improved outcomes for poor ovarian responders(20). Since then, several new randomized controlled trials (RCTs) have been published investigating the influence of GH on IVF/ICSI outcomes. To provide a thorough understanding of the subject, our aim is to conduct a rigorous meta-analysis of the available evidence from relevant RCTs to date.

Materials and Methods

In this meta-analysis, we aim to investigate the impact of GH supplementation on the outcomes of IVF or ICSI in poor ovarian responders. We have taken measures to ensure the rigor and transparency of our study, including registering our research protocol on the Open Science Framework and utilizing a checklist for search strategy, screening, and data selection. Our methodology conforms to the Preferred Reporting Items for Systematic Reviews and Meta-analyses guidelines to maintain a high standard of reporting(21). The systematic review protocol was registered in Open Science Framework (https://osf.io/bv9zm).

Literature Search

A comprehensive literature search was conducted up to May 25, 2023 to identify relevant RCTs and systematic reviews. The following databases were searched: Cochrane Library, PubMed, SCOPUS, Google Scholar, and Clinical Trials. To generate subsets of relevant citations, we used a combination of Medical Subject Headings (MESH) and text words. Two subsets were created for studies of poor ovarian response, using keywords related to “reserve” and “poor”. Additional two subsets were also created for studies on IVF/ICS and GH supplementation, using relevant keywords. the subsets were combined using the “AND” operator to generate a refined set of citations, and a publication type filter was applied to obtain only RCTs and systematic reviews. To adhere to the search engine specifications for each database, the search strategy was adjusted accordingly. There were no restrictions on language or date. Additionally, we screened the reference lists of relevant systematic reviews and included studies to identify any additional articles that met our inclusion criteria. Two independent reviewers conducted the search and screened all records for eligibility. Any differences were addressed through discussion and agreement among the reviewers.

Criteria for Selecting Studies

Prior to conducting the literature search, we established the inclusion and exclusion criteria for this meta-analysis. To be considered for inclusion, studies had to be RCTs that met the following criteria: inclusion of women characterized as POR, women subjected to IVF or ICSI with any ovarian stimulation protocol, and reporting of clinical pregnancy outcomes. Studies that used adjuvant treatments alongside GH or lacked a comparison group not using GH were excluded from the analysis.

Extraction of Relevant Data

Two reviewers (AA, FA) undertook a meticulous evaluation of each study’s title and abstract to determine its eligibility for inclusion in this meta-analysis. Studies that did not meet the inclusion criteria were excluded. The complete texts of the remaining studies were reviewed to confirm they met the eligibility criteria for the data extraction process. Next, the following information was selected for extraction in three sets: 1. patient-specific factors [i.e. what POR criteria are met, age, body mass index (BMI), and the duration of infertility], 2. study design (i.e. number of participants, details of IVF or ICSI protocol, doses and details of GH administration), 3. outcomes (i.e. pregnancy rate, live birth rate, number of retrieved oocytes, number of transferred embryos, rate of cycle cancellation, and total dose of gonadotropins administered, and peak estradiol level).

Study Quality Assessment

To ensure the reliability and accuracy of the meta-analysis, two independent authors (FZ, QB) evaluated the quality of the included literature using the Cochrane risk of bias assessment tools for RCTs. Any inconsistencies in the evaluations were resolved by a third author, (FA).

Statistical Analysis

This meta-analysis was conducted on the effects of co administration of gonadotropins and GH during the ovarian stimulation on IVF outcome for POR’s patients compared to a control group using Stata version 15 (Stata Corp, College Station, TX, USA). After the authors have extracted data, meta-analysis has been on the adequate data. We have gathered all information in Tables 1-3 to be systematically studied and explained in the result section. Standardized mean difference (SMD) between the control and the patient’s group was selected  as the main unit of analysis for each variable. The cut-off values have been set by Cohen for the interpretation of medium, small, and large effect sizes (0.5, 0.2, and 0.8, respectively). Analyses have been performed employing the random effects model. The authors have assessed heterogeneity by I2 statistics and values larger than 50% were announced as moderate to high heterogeneity. We also have done meta-regression when we found enough studies to examine the relationship between pregnancy rate, and live birth rate as potential effect modifiers. Publication bias was assessed visually using funnel plots and quantitatively through Begg’s and Egger’s regression tests.

Results

Study Selection and Included Studies

After an extensive search using MESH terms, a total of 234 studies were identified. Of these, 37 duplicates were removed. Then, the abstracts of the remaining articles went through further assessment, which resulted in exclusion of 163 studies for not meeting the inclusion criteria. The full text of the remaining 34 studies were retrieved, and 16 of them were excluded following the reasons outlined in Figure 1. At last, only 18 studies matched the selection criteria and were included for meta-analysis. Eligible studies were published from 1991-2022, and included a total of 1870 women identified as POR. Among them, 934 women received GH co-treatment during ovarian stimulation and were assigned to the intervention group, while the remaining 936 women, who received conventional COS, were assigned to the comparison group. The definition of poor ovarian response was not consistent across the studies due to some being published before the establishment of the Bologna criteria. Out of articles included, four were carried out in Egypt(16, 17, 22, 23), three were from Iran(18, 24, 25), two from China(26, 27), and one from South Korea(28), Israel(29), Taiwan(30), Turkey(5), Australia(31), UK(32), Finland(33), Sweden(34), and Spain(35). All articles aimed to determine whether GH co-treatment could enhance IVF or ICSI outcomes for patients with poor ovarian response. GnRH agonists were used in 10 studies(5, 17, 22, 23, 29, 30, 32-35), and total of five RCTs used GnRH antagonists(16, 18, 24, 25, 28). Detailed information on these studies can be found in Table 1.

Demographics

A total of 14, 12, and 8 studies reported the age(5,16-18,22-26,28,30,31,34,35), and duration of infertility(18,22-24,26,28) of the study participants, respectively. The findings of the analysis indicated that there was no significant difference with regard to these demographic factors among studies, exhibiting low to moderate heterogeneity (age: I2=41.9%, BMI: I2=15.5%, duration of infertility: I2=0.0%). Nevertheless, a random-effects model was used as illustrated in Figure 2.

Number of Retrieved Oocytes

A total of 15 studies reported number of retrieved oocytes. two of which(29, 32) did not provide standard deviation of data, finally, 13 studies(16-18,22-24,26-28,30,31,34,35) including 1554 patients (770 in the GH group and 784 in the control group) were included in the meta-analysis. A significant increase in the number of retrieved oocytes was found in the GH group compared to the control group (SMD, 0.65; 95% CI, 0.29-1.00), as shown in Figure 3A. However, significant heterogeneity was observed among these studies (I2=90.6%), as a result, the random effects model was applied.

Number of Transferred Embryo

A total of 15 studies reported the number of transferred embryo, four of which(22, 29, 32, 35) did not provide standard deviation of data or lacked specific data required for a meta-analysis. The meta-analysis finally included 11 studies(5,16-18,23,24,26-28,30,31) for 1255 patients (621 in the GH group and 634 in the control group). The result showed a significant increase in the number of transferred embryo in the group given GH o-treatment compared to the control group (SMD, 0.80, 95% CI, 0.39, 1.21). A random effects model was applied due to the significant heterogeneity among these studies. (I2=91.4%), as shown in Figure 3B.

Total Dose of Gonadotropin

A total of 15 studies reported total dose of gonadotropin, four of which(29, 32-34) did not provide standard deviation of data or lacked specific data required for a meta-analysis. The meta-analysis finally included 11 studies(5,16-18,22,24-28,31) for 1449 patients (716 in the GH group and 733 in the control group). The result indicated a significant decrease in the gonadotropin dosage with the administration of GH [SMD=-0.82, 95% CI=(-1.25, -0.39)]. A random effects model was applied due to the significant heterogeneity among these studies. (I2=92.8%), as shown in Figure 4A.

Duration of Gonadotropin Therapy

A total of 14 studies reported the duration of gonadotropin therapy, three of which(22, 32, 34) did not provide standard deviation of data or lacked specific data required for a meta-analysis. The meta-analysis finally included 11 studies(5,16-18,23-27,31,35) for 1478 patients (732 in the GH group and 746 in the control group). The findings showed a notable reduction in gonadotropin dosage with GH administration (SMD, -0.63, 95% CI, -1.04, -0.22). A random effects model was applied due to the significant heterogeneity among these studies (I2=91.7%), as shown in Figure 4B.

Peak E2 Level

A total of 14 studies reported peak E2 level. Three of which(32-34) did not provide standard deviation of data, Finally, 11 studies(5,16-18,22,23,26-28,30,35) including 1395 patients (691 in the GH group and 704 in the control group) were eligible for the meta-analysis. A significant increase in the level of peak E2 was observed in the GH group compared to the control group (SMD, 1.20; 95% CI, 0.59, 1.81), as shown in Figure 4C. However, significant heterogeneity was observed among these studies (I2=96.1%), therefore, the random effects model was applied.

Meta-regression Analysis

A meta-regression analysis was conducted to investigate whether the differences of reported outcomes in GH and control group were correlated to effectiveness of intervention in regards to cycle cancellation rate, pregnancy rate, and live birth rate. The findings of the meta-regression analysis indicated that there was no significant linear relationship between the effectiveness of intervention and any of the reported outcomes, including the number of retrieved oocytes, the total dose of gonadotropin, the duration of gonadotropin therapy, the number of transferred embryos, and the peak E2 level. Further details can be found in Table 3.

Sensitivity and Bias Analysis

The sensitivity analysis indicated that no single study or group of similar studies significantly affected the SMD and its corresponding CI, suggesting the overall findings are robust.   Also, Egger’s regression test, Begg’s test, and funnel plot analysis were performed to detect publication bias in relation to the number of retrieved oocytes. Both Egger’s regression test and Begg’s test did not reveal any evidence of publication bias (p>0.1), and funnel plot analysis yielded a symmetric plot for the number of retrieved oocytes (Figure 5). Therefore, giving no indication of publication bias.

Discussion

This systematic review and meta-analysis included 18 studies involving 1870 participants. The findings revealed a significant correlation between the usage of GH and various factors, such as the number of retrieved oocytes, embryo transfer, total dose of gonadotropin, duration of gonadotropin therapy, and peak E2 level. However, there was no significant association between the improvement in these factors and the success of IVF, including LBR, pregnancy rate, and cycle cancellation rate.

Several studies, consistent with our findings, demonstrated a concurrence regarding the number of retrieved oocytes(5,16-18,22-24). GH is believed to play a crucial role in enhancing ovarian function by stimulating follicular growth, gametogenesis, increasing estrogen production, and promoting oocyte maturation(16, 18, 23). It facilitates the growth of small follicles, increasing gonadotropin sensitivity, and reduces follicular degeneration and atresia before ovulation, thus improving ovulation(18). Additionally, GH stimulates the synthesis of IGF-1 by influencing granulosa cells, which mediates the action of GH(24). Lower doses of GH have shown more favorable responses on the ovary(30). Although some studies did not support this outcome and did not report a significant relationship in terms of oocyte retrieval(29, 31).

Another aspect investigated in this study was the number of transfer embryos, which exhibited a significant improvement, consistent with several other studies(18,22-24,30). Nonetheless, conflicting results were reported in some studies(29, 31).

Our study observed a correlation between the usage of GH and a decrease in the dose and duration of gonadotropin use, supported by several studies(5, 16, 17, 22, 31). GH concentration in follicular fluid plays a role in enhancing ovarian response to gonadotropin(22). Together with IGF-1, GH enhances the function of FSH, leading to a reduction in the required dose and duration of gonadotropins(22, 32). However, this effect was more pronounced in patients with poor ovarian response, whereas patients with normal ovarian response required higher doses of gonadotropin, resulting in a less favorable response(32). Taking a lower dose of GH has been reported to increase the need for gonadotropin and reduce ovarian response(30), while a higher dose of GH has the opposite effect(5). Another mechanism that may explain this effect is the acceleration of ovarian follicle development and earlier oocyte production during GH administration, thereby reducing the need for higher gonadotropin doses(31).

GH induces changes in the hormonal profile of patients, with one of the most notable effects being the increase in peak E2 levels, supported by several studies(5, 17, 23). Elevated E2 levels indicate an increase in the number of follicles stimulated by GH and, consequently, an increase in the number of produced oocytes(17). It is proposed that GH may enhance the chance of pregnancy by elevating the E2 level in follicular fluid(5, 23); however, this outcome was not observed in our study.

Theoretically, GH can influence the pregnancy rate through various mechanisms, such as improving oocyte quantity and quality, enhancing embryo quantity and quality, increasing the number of transferable embryos, and promoting implantation potential(5, 16, 17, 22). GH may improve the success of embryo implantation by enhancing endometrial blood supply and increasing endometrial receptivity(30). Even though a study by Safdarian et al.(24) reported a notably higher clinical pregnancy rate, although there was no significant difference in LBR. Nevertheless, our study, along with several others, supports the notion that improving these factors does not significantly impact the outcomes of IVF(16-18,22,28).GH consumption affect the quality and quantity of oocyte production but does not have significant correlation with pregnancy rate and LBR(16, 17, 22). While the administration of a high dose of GH in the late luteal phase demonstrated an increase in the pregnancy rate in Kucuk et al.’s study(5), that was not statistically significant.

Overall, the effectiveness of GH is influenced by various factors, including the hormonal background, patient characteristics, and GH dosage(24). GH deficiency may be a necessary condition for its effectiveness in IVF(24). The timing of GH administration during the cycle is another influential factor(28). It has been reported that the effect of GH administration is more pronounced in PORs compared to normal responders, particularly in terms of qualitative response rather than quantitative response(28).Furthermore, increasing age leads to a decrease in GH, making older women with GH deficiency an ideal group to receive GH supplementation(22).

Study Limitations

This study encompassed diverse ethnic groups, thereby enhancing the generalizability of the results to other populations. However, our study had some limitations, too. Included studies had used various criteria for diagnosing POR, although the dominant method was the Bologna criterion. Also, some studies had small populations, which indicates the requirement of future studies with larger populations.

Conclusion

In summary, this systematic review and meta-analysis investigated the relationship between GH usage and factors related to IVF. The findings indicate a significant association between GH and improved outcomes such as the number of retrieved oocytes, transferable embryos, total gonadotropin dosage, duration of gonadotropin therapy, and peak E2 levels. However, despite these positive effects, there was no significant impact on the success of IVF in terms of LBR, pregnancy rate, and cycle cancellation rate. The effectiveness of GH appears to depend on individual factors and the timing and dosage of administration. Further research is needed to clarify its role in IVF outcomes and identify the specific patient groups that may benefit most from GH supplementation.

References

1Mohamed KA, Davies WA, Allsopp J, Lashen H. Agonist “flare-up” versus antagonist in the management of poor responders undergoing in vitro fertilization treatment. Fertil Steril. 2005;83:331-5.
2Loutradis D, Vomvolaki E, Drakakis P. Poor responder protocols for in-vitro fertilization: options and results. Curr Opin Obstet Gynecol. 2008;20:374-8.
3Ferraretti AP, La Marca A, Fauser BC, Tarlatzis B, Nargund G, Gianaroli L; ESHRE working group on Poor Ovarian Response Definition. ESHRE consensus on the definition of ‘poor response’ to ovarian stimulation for in vitro fertilization: the Bologna criteria. Hum Reprod. 2011;26:1616-24.
4Hamdine O, Eijkemans MJ, Lentjes EW, Torrance HL, Macklon NS, Fauser BC, et al. Ovarian response prediction in GnRH antagonist treatment for IVF using anti-Müllerian hormone. Hum Reprod. 2015;30:170-8.
5Kucuk T, Kozinoglu H, Kaba A. Growth hormone co-treatment within a GnRH agonist long protocol in patients with poor ovarian response: a prospective, randomized, clinical trial. J Assist Reprod Genet. 2008;25:123-7.
6Chang CW, Sung YW, Hsueh YW, Chen YY, Ho M, Hsu HC, et al. Growth hormone in fertility and infertility: Mechanisms of action and clinical applications. Front Endocrinol (Lausanne). 2022;13:1040503.
7Harvey S. Extrapituitary growth hormone. Endocrine. 2010;38:335-59.
8Sbracia M, Scarpellini F, Poverini R, Alò PL, Rossi G, Di Tondo U. Immunohistochemical localization of the growth hormone in human endometrium and decidua. Am J Reprod Immunol. 2004;51:112-6.
9Abir R, Garor R, Felz C, Nitke S, Krissi H, Fisch B. Growth hormone and its receptor in human ovaries from fetuses and adults. Fertil Steril. 2008;90(4 Suppl):1333-9.
10Bidlingmaier M, Strasburger CJ. Growth hormone. Doping in Sports: Biochemical Principles, Effects and Analysis. 2010: p. 187-200.
11Yoshimura Y, Iwashita M, Karube M, Oda T, Akiba M, Shiokawa S, et al. Growth hormone stimulates follicular development by stimulating ovarian production of insulin-like growth factor-I. Endocrinology. 1994;135:887-94.
12Hull KL, Harvey S. Growth hormone: roles in female reproduction. J Endocrinol. 2001;168:1-23.
13Slot KA, Kastelijn J, Bachelot A, Kelly PA, Binart N, Teerds KJ. Reduced recruitment and survival of primordial and growing follicles in GH receptor-deficient mice. Reproduction. 2006;131:525-32.
14Mendoza C, Cremades N, Ruiz-Requena E, Martinez F, Ortega E, Bernabeu S, et al. Relationship between fertilization results after intracytoplasmic sperm injection, and intrafollicular steroid, pituitary hormone and cytokine concentrations. Hum Reprod. 1999;14:628-35.
15Mendoza C, Ruiz-Requena E, Ortega E, Cremades N, Martinez F, Bernabeu R, et al. Follicular fluid markers of oocyte developmental potential. Hum Reprod. 2002;17:1017-22.
16Bassiouny YA, Dakhly DMR, Bayoumi YA, Hashish NM. Does the addition of growth hormone to the in vitro fertilization/intracytoplasmic sperm injection antagonist protocol improve outcomes in poor responders? A randomized, controlled trial. Fertil Steril. 2016;105:697-702.
17Bayoumi YA, Dakhly DM, Bassiouny YA, Hashish NM. Addition of growth hormone to the microflare stimulation protocol among women with poor ovarian response. Int J Gynaecol Obstet. 2015;131:305-8.
18Eftekhar M, Aflatoonian A, Mohammadian F, Eftekhar T. Adjuvant growth hormone therapy in antagonist protocol in poor responders undergoing assisted reproductive technology. Arch Gynecol Obstet. 2013;287:1017-21.
19Lattes K, Brassesco M, Gomez M, Checa MA. Low-dose growth hormone supplementation increases clinical pregnancy rate in poor responders undergoing in vitro fertilisation. Gynecol Endocrinol. 2015;31:565-8.
20Yang P, Wu R, Zhang H. The effect of growth hormone supplementation in poor ovarian responders undergoing IVF or ICSI: a meta-analysis of randomized controlled trials. Reprod Biol Endocrinol. 2020;18:76.
21Moher D, Liberati A, Tetzlaff J, Altman DG; PRISMA Group. Preferred reporting items for systematic reviews and meta-analyses: the PRISMA statement. PLoS Med. 2009;6:e1000097.
22Dakhly DMR, Bassiouny YA, Bayoumi YA, Hassan MA, Gouda HM, Hassan AA. The addition of growth hormone adjuvant therapy to the long down regulation protocol in poor responders undergoing in vitro fertilization: Randomized control trial. Eur J Obstet Gynecol Reprod Biol. 2018;228:161-5.
23Mohammad EH, Abou El Serour AG, Mohamed EAH, Abbasy AH, Zaatar M, Rageh KA, et al. Efficacy of growth hormone supplementation with ultrashort GnRH antagonist in IVF/ICSI for poor responders; randomized controlled trial. Taiwan J Obstet Gynecol. 2021;60:51-5.
24Safdarian L, Aghahosseini M, Alyasin A, Samaei Nouroozi A, Rashidi S, Shabani Nashtaei M, et al. Growth Hormone (GH) Improvement of Ovarian Responses and Pregnancy Outcome in Poor Ovarian Responders: A Randomized Study. Asian Pac J Cancer Prev. 2019;20:2033-7.
25Zafardoust S, Ansaripor S, Karimi A, Hosseinirad H, Ataei M. Effects of Adjuvant Growth Hormone Therapy on Poor Ovarian Responders in Assisted Reproductive Technology. Maedica (Bucur). 2022;17:336-43.
26Gong Y, Zhang K, Xiong D, Wei J, Tan H, Qin S. Growth hormone alleviates oxidative stress and improves the IVF outcomes of poor ovarian responders: a randomized controlled trial. Reprod Biol Endocrinol. 2020;18:91.
27Zhuang GL, Wong SX, Zhou CQ. [The effect of co-administration of low dosage growth hormone and gonadotropin for ovarian hyperstimulation in vitro fertilization and embryo transfer]. Zhonghua Fu Chan Ke Za Zhi. 1994;29:471-4, 510.
28Choe SA, Kim MJ, Lee HJ, Kim J, Chang EM, Kim JW, et al. Increased proportion of mature oocytes with sustained-release growth hormone treatment in poor responders: a prospective randomized controlled study. Arch Gynecol Obstet. 2018;297:791-6.
29Dor J, Seidman DS, Amudai E, Bider D, Levran D, Mashiach S. Adjuvant growth hormone therapy in poor responders to in-vitro fertilization: a prospective randomized placebo-controlled double-blind study. Hum Reprod. 1995;10:40-3.
30Lee YX, Shen MS, Tzeng CR. Low Dose Growth Hormone Adjuvant Treatment With Ultra-Long Ovarian Stimulation Protocol in Poor Responders Showed Non-inferior Pregnancy Outcome Compared With Normal Responders. Front Endocrinol (Lausanne). 2019;10:892.
31Norman RJ, Alvino H, Hull LM, Mol BW, Hart RJ, Kelly TL, et al; LIGHT investigators. Human growth hormone for poor responders: a randomized placebo-controlled trial provides no evidence for improved live birth rate. Reprod Biomed Online. 2019;38:908-15.
32Owen EJ, West C, Mason BA, Jacobs HS. Co-treatment with growth hormone of sub-optimal responders in IVF-ET. Hum Reprod. 1991;6:524-8.
33Suikkari A, MacLachlan V, Koistinen R, Seppälä M, Healy D. Double-blind placebo controlled study: human biosynthetic growth hormone for assisted reproductive technology. Fertil Steril. 1996;65:800-5.
34Bergh C, Hillensjö T, Wikland M, Nilsson L, Borg G, Hamberger L. Adjuvant growth hormone treatment during in vitro fertilization: a randomized, placebo-controlled study. Fertil Steril. 1994;62:113-20.
35Tesarik J, Hazout A, Mendoza C. Improvement of delivery and live birth rates after ICSI in women aged >40 years by ovarian co-stimulation with growth hormone. Hum Reprod. 2005;20:2536-41.
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