Fertility Disorders Clinical Trial
— RPLOfficial title:
Intravenous Immunoglobulin and Prednisolone to Women With Unexplained Recurrent Pregnancy Loss After Assisted Reproductive Technology Treatment: a Randomised, Double-blind, Placebo-controlled Trial
Recurrent pregnancy loss (RPL) affects around 5 % of women in reproductive age. The underlying cause of RPL is most often unknown, probably multifactorial, and no treatment with documented effect on chance of live birth exists. In unexplained cases of RPL, primarily the immune system is hypothesized to play a pivotal, causative role, since autoantibodies and specific human leukocyte antigen (HLA) alleles as well as unbalanced distribution of leucocyte subsets, especially natural killer (NK) cells and T-helper (Th) cells, occurs more frequently in patients with unexplained RPL. For that reason, many treatment regimens used in autoimmune diseases have been tested on RPL patients, as for example prednisolone and intravenous immunoglobulin (IVIg). IVIg (Privigen) consist of a broad spectrum of structurally and functionally intact IgG antibodies. The mechanism of action is not fully elucidated, but certainly IVIg do help opsonise and neutralize foreign cells and pathogens. Prednisolone support this anti-inflammatory action by suppressing migration of polymorphonuclear leukocytes, and reducing the volume and activity of the immune system and the capillary permeability. A retrospective, observational pilot study suggested that a combination of prednisone and IVIg in first trimester improves the chance of a live birth in women with RPL after assisted reproductive technologies (ART) (Nyborg et al., 2014). A randomized controlled study is necessary for determining if this immunomodulatory treatment definitely is effective in patients with unexplained RPL after ART (defined as IVF or ICSI ad FER). Potentially, this study will be able to establish evidence for an effective treatment to women with unexplained RPL after ART, who otherwise have a poor prognosis.
Status | Recruiting |
Enrollment | 74 |
Est. completion date | August 1, 2023 |
Est. primary completion date | June 1, 2023 |
Accepts healthy volunteers | No |
Gender | Female |
Age group | 18 Years to 41 Years |
Eligibility | Inclusion Criteria: - Women with = 2 consecutive pregnancy losses (miscarriages or biochemical pregnancies) = completed gestational week 10 after ART with the present partner or with an egg/semen donor* - The gestational week of the non-induced pregnancy losses will be based on the date of clinical signs of miscarriage or the fetus' crown-rump-length of a missed abortion measured on the ultrasonic scan detecting the pregnancy loss. If the participant plan to use egg donation in the study cycle, the previous two pregnancy losses must also have happened with the use of egg donation; however, it is not required to use the same egg donor in all three embryo transfers. Exclusion Criteria: 1. BMI =35 2. Age =41 3. Significant uterine malformation(s) 4. Known parental balanced chromosomal translocations 5. =2 previous pregnancies with fetuses with known abnormal karyotype 6. Patients with IgA deficiency, IgA-autoantibodies or hyperprolinaemia 7. Treatment with medication interacting with prednisolone - CYP3A4-inhibitors (fx erythromycin, itraconazole, ritonavir, lopinavir), CYP3A4-inductors (fx phenobarbital, phenytoin og rifampicin), loop diuretics, thiazides, amphotericin B, beta2-agonists, antidiabetics, interleukin-2, somatotropins, anticholinergics and regular treatment with NSAIDs. 8. Patients with moderate/severe hypertension, diabetes mellitus, heart insufficiency, severe mental disorders, Cushing syndrome, myasthenia gravis, ocular herpes simplex, pheochromocytoma, systemic sclerosis, and moderate/severe renal dysfunction. 9. Patients with a clinical or biochemical profile indicating need for heparin or levothyroxine treatment during pregnancy 10. Previous treatment with IVIg 11. Allergy to prednisolone and/or IVIg 12. AMH <4 pmol/L. If transfer of donor egg is planned for her IVF cycle, the AMH value will not be an exclusion criterion. |
Country | Name | City | State |
---|---|---|---|
Denmark | • The Centre for Recurrent Pregnancy Loss of Western Denmark, Department of Obstetrics and Gynaecology, Aalborg University Hospital | Aalborg |
Lead Sponsor | Collaborator |
---|---|
Aalborg University Hospital | Beckett Foundation, Clinical Immunological Department, Aalborg University Hospital, GCP department of Aalborg University Hospital, L.F. Foghts Foundation, Svend Andersen Fonden, The Pharmacy of Aalborg University Hospital |
Denmark,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | A normal live fetus at nuchal scan in ITT population | The frequency of participants with minimum one apparently normal fetus alive at the time of nuchal scan (approx. week 12) in patients receiving active and placebo treatment, respectively.
Here, the primary analyses will be undertaken as an intention-to-treat (ITT) analysis, including all participants who were allocated to either active or placebo treatment at the start of the ART cycle, even if they did not receive infusion with IVIg or albumin due to cancellation of embryo/blastocyst transfer. |
12 week after embryo transfer | |
Primary | A normal live fetus at nuchal scan in PP population | The frequency of participants with minimum one apparently normal fetus alive at the time of nuchal scan (approx. week 12) in patients receiving active and placebo treatment, respectively.
Here, the primary analyses will be undertaken as a per-protocol (PP) analysis, including patients who were randomized and received the allocated infusion of study medicine at the time of embryo/blastocyst transfer and had this transfer performed. |
12 week after embryo transfer | |
Primary | Live birth rate in ITT population | The frequency of participants with a liveborn (sign of life immediately af delivery >24 weeks) among all randomized participants | At delivery | |
Primary | Live birth rate in the PP population | The frequency of participants with a liveborn (sign of life immediately af delivery >24 weeks) among all participants who fulfill criteria for PP-analysis | At delivery | |
Primary | A normal live fetus at nuchal scan among participants who become pregnant after embryo transfer in the ITT population | The frequency of participants in the ITT population with minimum one apparently normal fetus alive at the time of nuchal scan (approx. week 12) in patients receiving active and placebo treatment, respectively, and who become pregnant after embryo transfer. | 12 week after embryo transfer | |
Primary | A normal live fetus at nuchal scan among participants who become pregnant after embryo transfer in the PP population | The frequency of participants in the PP population with minimum one apparently normal fetus alive at the time of nuchal scan (approx. week 12) in patients receiving active and placebo treatment, respectively, and who become pregnant after embryo transfer. | 12 week after embryo transfer | |
Secondary | Maternal adverse reactions | Number of participants with adverse reactions including headache, skin rash, and fever that might be associated to study medicine in the ITT population. | 9 months after embryo transfer. | |
Secondary | Negative pregnancy test | Number of participants with a negative pregnancy test after ET in the ITT population. | 9 months after embryo transfer. | |
Secondary | Miscarriage rate | Number of participants with a miscarriage (defined as any loss before 24 weeks of gestation) among the number of participants becoming pregnant (defined as a rise in serum beta hCG concentration >25 UI/L per transfer) in the ITT population. | Before 24 weeks of gestation | |
Secondary | Rate of Abnormal karyotype in Miscarried fetuses | The frequency of pregnancy losses with unknown or normal karyotype among all participants with a pregnancy loss having an evac. and chromosome typing. | Before 24 weeks of gestation | |
Secondary | Rate of Stillbirth rate | Number of participants with a still birth (defined as fetal death at 24 weeks or more or no sign of life after delivery) among the number of participants becoming pregnant (defined as a rise in serum beta hCG concentration >25 UI/L per transfer) in the ITT population. | 9 months after embryo transfer. | |
Secondary | Rate of Congenital deformities | Number of live-born babies with a of congenital deformity among all live-borns in the ITT population. | 1 week after delivery | |
Secondary | Rate of Preterm birth | Number of live-born before 37+0 weeks of gestation among all live-borns in the ITT population. | 1 week after delivery | |
Secondary | Rate of Low birth weight (BW) | Number of live-born with a BW <2500 g among all live-borns in the ITT population. | 1 week after delivery | |
Secondary | Rate of Preeclampsia | Number pregnant participants >24 weeks with hypertension (systolic blood pressure (SBP) greater than or equal to 140 mm Hg or a diastolic blood pressure (DBP) greater than or equal to 90 mm Hg) and proteinuria (>0.3 g per day or urine albumine/creatinine ratio= 300 mg/g) among all pregnant participants >24 weeks in the ITT population. | 1 week after delivery | |
Secondary | Rate of Gestational diabetes | Number pregnant participants >24 weeks with gestation diabetes (i.e.efined as an oral glucose challenge test (OGCT) with >9.0 mmol/l 2 hours after oral intake of 75g glucose solution) among all pregnant participants >24 weeks in the ITT population. | 1 week after delivery | |
Secondary | Rate of gestational hypertension | Number pregnant participants >24 weeks with hypertension (i.e. systolic blood pressure (SBP) greater than or equal to 140 mm Hg or a diastolic blood pressure (DBP)) among all pregnant participants >24 weeks in the ITT population. | 1 week after delivery | |
Secondary | Rate of abnormal embryonic/fetal karyotype | Number of miscarriages with a abnormal embryonic/fetal karyotype among all miscarriages having a karyotype test in the ITT population. | Before 24 weeks of gestation | |
Secondary | Frequency of a boy | The percentage of live births that was a boy | Right after delivery |
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