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VOMIT: Validating the Effect og Ondansetron and Mirtazapine in Treating Hyperemesis Gravidarum

Sponsor
Nordsjaellands Hospital (Other)
Overall Status
Recruiting
CT.gov ID
NCT03785691
Collaborator
Bispebjerg Hospital (Other), Aarhus University Hospital (Other), Herlev and Gentofte Hospital (Other), Hvidovre University Hospital (Other), Odense University Hospital (Other), Rigshospitalet, Denmark (Other), Regionernes Medicinpulje (Other), Kolding Sygehus (Other)
180
Enrollment
8
Locations
3
Arms
49
Anticipated Duration (Months)
22.5
Patients Per Site
0.5
Patients Per Site Per Month

Study Details

Study Description

Brief Summary

The aim is to investigate the efficacy of mirtazapine and ondansetron as treatment for hyperemesis gravidarum(HG).

The setup is a double-blind multicenter trial where patients suffering from HG will be randomized to treatment with either mirtazapine, ondansetron or placebo (1:1:1).

Condition or Disease Intervention/Treatment Phase
Phase 2

Study Design

Study Type:
Interventional
Anticipated Enrollment :
180 participants
Allocation:
Randomized
Intervention Model:
Parallel Assignment
Intervention Model Description:
Randomized placebo controlled multicenter trial testing already marketed drugs on a new indication.Randomized placebo controlled multicenter trial testing already marketed drugs on a new indication.
Masking:
Quadruple (Participant, Care Provider, Investigator, Outcomes Assessor)
Masking Description:
All oral tablets will be encapsulated in gelatine to ensure identical look, smell and taste.
Primary Purpose:
Treatment
Official Title:
Validating the Effect of Ondansetron and Mirtazapine in Treating Hyperemesis Gravidarum: A Double-Blind Randomised Placebo-Controlled Multicentre Trial
Actual Study Start Date :
Mar 1, 2019
Anticipated Primary Completion Date :
Jul 31, 2022
Anticipated Study Completion Date :
Mar 31, 2023

Arms and Interventions

Arm Intervention/Treatment
Experimental: Mirtazapine

Mirtazapine 15 mg oral tablet (incapsulated in gelatine to provide blinding) will be administered once daily (bedtime) for 7 days. Placebo (empty gelatine capsule) will be administered once daily (morning). On Day 7 dosage increase is optional. If desired, mirtazapine 30 mg oral tablet (incapsulated in gelatine) will be administered once daily (bedtime) for 7 days. Placebo (empty gelatine capsule) will be administered three times daily (morning, noon and late afternoon). In case dosage increase is not desired, the subject will continue the initial treatment for an additional 7 days.

Drug: Mirtazapine
Mirtazapine 15 mg oral tablet (incapsulated in gelatine to provide blinding) will be administered once daily (bedtime) for 7 days. Placebo (empty gelatine capsule) will be administered once daily (morning). On Day 7 dosage increase is optional. If desired, mirtazapine 30 mg oral tablet (incapsulated in gelatine) will be administered once daily (bedtime) for 7 days. Placebo (empty gelatine capsule) will be administered three times daily (morning, noon and late afternoon). In case dosage increase is not desired, the subject will continue the initial treatment for an additional 7 days.
Other Names:
  • KRKA Mirtazapine Oral Tablet

    		•
    Experimental: Ondansetron

    Ondansetron 8 mg oral tablet (incapsulated in gelatine) will be administered twice daily (morning and bedtime) for 7 days. On Day 7 dosage increase is optional. If desired, ondansetron 8 mg oral tablet (incapsulated in gelatine) will be administered four times daily (morning, noon, late afternoon and bedtime) for 7 days. In case dosage increase is not desired, the subject will continue the initial treatment for an additional 7 days.

    Drug: Ondansetron
    Ondansetron 8 mg oral tablet (incapsulated in gelatine) will be administered twice daily (morning and bedtime) for 7 days. On Day 7 dosage increase is optional. If desired, ondansetron 8 mg oral tablet (incapsulated in gelatine) will be administered four times daily (morning, noon, late afternoon and bedtime) for 7 days. In case dosage increase is not desired, the subject will continue the initial treatment for an additional 7 days.
    Other Names:
  • Bluefish Ondansetron Oral Tablet

    		•
    Placebo Comparator: Placebo

    Placebo oral tablet (empty gelatine capsule) will be administered twice daily (morning and bedtime) for 7 days. On Day 7 dosage increase is optional. If desired, placebo oral tablet (empty gelatine capsule) will be administered four times daily (morning, noon, late afternoon and bedtime) for 7 days. In case dosage increase is not desired, the subject will continue the initial treatment for an additional 7 days.

    Drug: Placebo
    Placebo oral tablet (empty gelatine capsule) will be administered twice daily (morning and bedtime) for 7 days. On Day 7 dosage increase is optional. If desired, placebo oral tablet (empty gelatine capsule) will be administered four times daily (morning, noon, late afternoon and bedtime) for 7 days. In case dosage increase is not desired, the subject will continue the initial treatment for an additional 7 days.
    Other Names:
  • Placebo Oral Tablet

    		•

    Outcome Measures

    Primary Outcome Measures

    1. Change in nausea and vomiting from baseline to Day 2 (short term) in the mirtazapine group versus the placebo group. [2 days]

      Change in Pregnancy Unique Quantification of Emesis 24 score (PUQE-24 score) (patient reported) from baseline to Day 2 (short term) in the mirtazapine group versus the placebo group. PUQE-24 score ranges 3-15 with 3 being better and 15 being worse.

    2. Change in nausea and vomiting from baseline to Day 2 (short term) in the ondansetron group versus the placebo group. [2 days]

      Change in PUQE-24 score (patient reported) from baseline to Day 2 (short term) in the ondansetron group versus the placebo group.

    3. Change in nausea and vomiting from baseline to Day 14(+/-1) (long term) in the mirtazapine group versus the placebo group. [14 days]

      Change in PUQE-24 score (patient reported) from baseline to Day 14(+/-) (long term) in the mirtazapine group versus the placebo group. Only tested if outcome 1 is significant.

    4. Change in nausea and vomiting from baseline to Day 14(+/-1) (long term) in the ondansetron group versus the placebo group. [14 days]

      Change in PUQE-24 score (patient reported) from baseline to Day 14(+/-) (long term) in the ondansetron group versus the placebo group. Only tested if outcome 2 is significant.

    5. Change in nausea and vomiting from baseline to Day 2 (short term) in the mirtazapine group versus the ondansetron group. [2 days]

      Change in PUQE-24 score (patient reported) from baseline to Day 2 (short term) in the mirtazapine group versus the ondansetron group. Only tested if outcome 1 is significant.

    Secondary Outcome Measures

    1. Change in nausea and vomiting from baseline to Day 14(+/-1) in the mirtazapine group versus the ondansetron group. [14 days]

      Change in PUQE-24 score (patient reported) from baseline to Day 14(+/-1) in the mirtazapine group versus the ondansetron group.

    2. Overall nausea and vomiting during the intervention in the three different groups. [14 days]

      Area under the curve for PUQE-24 score (patient reported) during the intervention in the three different groups.

    3. Change in well-being during the intervention in the three different groups. [14 days]

      Change in PUQE well-being score (patient reported) during the intervention in the three different groups.

    4. Change in nausea during the intervention in the three different groups. [14 days]

      Change in daily nausea visual analog scale (VAS) (patient reported) during the intervention in the three different groups. VAS score ranges 0-100 with 0 being better and 100 being worse. Numbers are not visible to subjects.

    5. Change in vomiting during the intervention in the three different groups. [14 days]

      Change in number of daily vomiting episodes (patient reported) during the intervention in the three different groups.

    6. Occurrence of side effects in the three different groups. [19 days]

      Occurrence of side effects (patient reported and registered by trial personnel) during and until 5 days after the intervention in the three different groups.

    7. Change in quality of life for nausea and vomiting during pregnancy from baseline to Day 7(+/-1) and baseline to Day 14(+/-1) in the three different groups. [14 days]

      Change in Health-Related Quality of Life for Nausea and Vomiting during Pregnancy (NVPQOL) score (patient reported) from baseline to Day 7(+/-1) and baseline to Day 14(+/-1) in the three different groups. NVPQOL score ranges 30-210 with 30 being better and 210 being worse.

    8. Change in severity of hyperemesis gravidarum from baseline to Day 7(+/-1) and baseline to Day 14(+/-1) in the three different groups. [14 days]

      Change in HyperEmesis Level Prediction (HELP) score (patient reported) from baseline to Day 7(+/-1) and baseline to Day 14(+/-1) in the three different groups. HELP score ranges 0-50 with 0 being better and 50 being worse.

    9. Change in health-related quality of life from baseline to Day 7(+/-1) and baseline to Day 14(+/-1) in the three different groups. [14 days]

      Change in health status (EQ-5D-5L) (patient reported) from baseline to Day 7(+/-1) and baseline to Day 14(+/-1) in the three different groups.

    10. Change in sleep quality from baseline to Day 7(+/-1) and baseline to Day 14(+/-1) in the three different groups. [14 days]

      Change in modified Pittsburg Sleep Quality Index (PSQI) (patient reported) from baseline to Day 7(+/-1) and baseline to Day 14(+/-1) in the three different groups.Modified PSQI score ranges 0-12 with 0 being better and 12 being worse.

    11. Patient satisfaction with treatment Day 7(+/-1) and Day 14(+/-1) in the three different groups. [14 days]

      Patient satisfaction with treatment VAS (patient reported) on Day 7(+/-1) and Day 14(+/-1) in the three different groups. VAS score ranges 0-100 with 0 being better and 100 being worse. Numbers are not visible to subjects.

    12. Change in patient consideration of termination of pregnancy from baseline to Day 7(+/-1) and baseline to Day 14(+/-1) in the three different groups. [14 days]

      Change in patient consideration of termination of pregnancy (patient reported) from baseline to Day 7(+/-1) and baseline to Day 14(+/-1) in the three different groups.

    13. Request for dosage increase in the three different groups. [14 days]

      Frequency of request for dosage increase in the three different groups.

    14. Request for continuation of trial medication after end of intervention in the three different groups. [14 days]

      Frequency of request for continuation of trial medication after end of intervention in the three different groups.

    15. Use of rescue medication during the intervention in the three different groups. [14 days]

      Use of rescue medication during (patient reported) the intervention in the three different groups.

    16. Number of days on sick leave during the intervention in the three different groups [14 days]

      Number of days on sick leave (patient reported) during the intervention in the three different groups

    17. Necessity of i.v.-fluids during the intervention in the three different groups. [14 days]

      Amount of treatments with i.v.-fluids during the intervention in the three different groups.

    18. Need of hospitalisation during the intervention in the three different groups. [14 days]

      Number of days of hospitalisations during the intervention in the three different groups.

    19. Weight change from baseline to Day 7(+/-1) and baseline to Day 14(+/-1) in the three different groups. [14 days]

      Weight change in kg from baseline to Day 7(+/-1) and baseline to Day 14(+/-1) in the three different groups.

    20. Pregnancy outcome: Live birth, loss or termination of pregnancy [8 months]

      Live birth, loss or termination of pregnancy.

    21. Delivery outcome: Mode of delivery [8 months]

      Mode of delivery: Vaginal, cesarian, vacuum extraction.

    22. Delivery outcome: Delivery complications [8 months]

      Eg. postpartum hemorrhage, shoulder dystocia, sphincter rupture

    23. Live birth outcome: birth weight. [8 months]

      Birth weight in g.

    24. Live birth outcome: gestational age at birth. [8 months]

      Gestational age at birth in weeks plus days.

    25. Live birth outcome: APGAR score. [8 months]

      APGAR score at 1, 5 and 10 minutes after birth. APGAR score ranges 0-10 with 0 being worse and 10 being better.

    26. Live birth outcome: umbilical cord pH. [8 months]

      Umbilical cord pH at birth.

    27. Live birth outcome: placenta weight. [8 months]

      placenta weight in g.

    28. Live birth outcome: sex. [8 months]

      offsprings sex.

    29. Live birth outcome: hospitalizations on neonatal ward during the first month post-partum. [9 months]

      Hospitalizations of the offspring in neonatal ward during the first month post-partum.

    30. Live birth outcome: congenital malformations (depending on gestational age also registered on early ended pregnancies). [8 months]

      Congenital malformations.

    31. Occurrence of treatment failure in the three different groups. [14 days]

      Frequency of and time to treatment failure in the three different groups.

    Eligibility Criteria

    Criteria

    Ages Eligible for Study:
    18 Years and Older
    Sexes Eligible for Study:
    Female
    Accepts Healthy Volunteers:
    Yes
    Inclusion Criteria:

    • Written informed consent obtained before any trial related procedures are performed

    • Female age >18 years

    • Pregnant woman with gestational age between 5+0 and 19+6

    • Nausea and vomiting without other obvious reason

    • PUQE-24 score ≥13 OR PUQE-24 score ≥7 AND

    1. weight loss >5% of pre-pregnancy weight and/or

    2. hospitalisation due to nausea and vomiting of pregnancy

    • Singleton pregnancy

    • The subject must be willing and able to comply with trial protocol

    Exclusion Criteria:

    • Mola pregnancy, multiple gestation or non-vital pregnancy

    • Nausea and vomiting of other aetiology than NVP

    • Allergic to selective 5-HT3-receptor antagonists

    • Ongoing treatment with antidepressant medication

    • Pre-existing diagnosis of chronic kidney disease, diabetes type 1 or 2, significant cardiac disease (incl. long QT syndrome), epilepsy, HIV. In case of other pre-existing conditions subjects might be excluded based on individual assessment by an MD

    • Elevated liver enzymes (ALAT>150 U/l)

    • Elevated creatinine (>100 µmol/l)

    • ECG showing long QT-syndrome (QTc >460msek)

    • Weekly alcohol intake >2 units of alcohol

    • Not able to take medicine orally

    • Not able to understand spoken and/or written Danish

    • Participation in another investigational drug trial within current pregnancy

    Contacts and Locations

    Locations

    Site City State Country Postal Code
    1 Department of Gynaecology and Obstetrics, Aalborg University Hospital Aalborg Denmark 9000
    2 Department of Gynaecology and Obstetrics, Aarhus University Hospital Aarhus Denmark 8200
    3 Department of Gynaecology and Obstetrics, Rigshospitalet Copenhagen Denmark 2100
    4 Department of Gynaecology and Obstetrics, Herlev Hospital Herlev Denmark 2730
    5 Department of Gynaecology and Obstetrics, Nordsjællands Hospital Hillerød Denmark 3400
    6 Department of Gynaecology and Obstetrics, Hvidovre Hospital Hvidovre Denmark 2650
    7 Department of Gynaecology and Obstetrics, Kolding Sygehus Kolding Denmark 6000
    8 Department of Gynaecology and Obstetrics, Odense University Hospital Odense Denmark 5000

    Sponsors and Collaborators

    • Nordsjaellands Hospital
    • Bispebjerg Hospital
    • Aarhus University Hospital
    • Herlev and Gentofte Hospital
    • Hvidovre University Hospital
    • Odense University Hospital
    • Rigshospitalet, Denmark
    • Regionernes Medicinpulje
    • Kolding Sygehus

    Investigators

    • Principal Investigator: Anne Ostenfeld, MD, Department of Obstetrics and gynecology, Nordsjællands Hospital Hillerød

    Study Documents (Full-Text)

    More Information

    Publications

    None provided.
    Responsible Party:
    Anne Ostenfeld, MD, PhD student, Nordsjaellands Hospital
    ClinicalTrials.gov Identifier:
    NCT03785691
    Other Study ID Numbers:
    • VOMIT
    First Posted:
    Dec 24, 2018
    Last Update Posted:
    Jun 8, 2022
    Last Verified:
    Jun 1, 2022
    Individual Participant Data (IPD) Sharing Statement:
    Yes
    Plan to Share IPD:
    Yes
    Studies a U.S. FDA-regulated Drug Product:
    No
    Studies a U.S. FDA-regulated Device Product:
    No
    Product Manufactured in and Exported from the U.S.:
    No
    Keywords provided by Anne Ostenfeld, MD, PhD student, Nordsjaellands Hospital
    Hyperemesis Gravidarum (HG)
    Mirtazapine
    Ondansetron
    Pregnancy
    Nausea and Vomiting of Pregnancy (NVP)
    Randomized Controlled Trial (RCT)
    Additional relevant MeSH terms:
    Hyperemesis Gravidarum
    Nausea
    Vomiting
    Ondansetron
    Mirtazapine

    Study Results

    No Results Posted as of Jun 8, 2022