Your search keyword '"Udengaard, Hanne"' showing total 5 results

1. Impact of letrozole co-treatment during ovarian stimulation with gonadotrophins for IVF:a multicentre, randomized, double-blinded placebo-controlled trial

Author

Bülow, Nathalie Søderhamn, Skouby, Sven Olaf, Warzecha, Agnieszka Katarzyna, Udengaard, Hanne, Andersen, Claus Yding, Holt, Marianne Dreyer, Grøndahl, Marie Louise, Nyboe Andersen, Anders, Sopa, Negjyp, Mikkelsen, Anne Lis Englund, Pinborg, Anja, Macklon, Nicholas Stephen, Bülow, Nathalie Søderhamn, Skouby, Sven Olaf, Warzecha, Agnieszka Katarzyna, Udengaard, Hanne, Andersen, Claus Yding, Holt, Marianne Dreyer, Grøndahl, Marie Louise, Nyboe Andersen, Anders, Sopa, Negjyp, Mikkelsen, Anne Lis Englund, Pinborg, Anja, and Macklon, Nicholas Stephen

Abstract

Study Question: Does letrozole co-treatment during ovarian stimulation with gonadotrophins for IVF reduce the proportion of women with premature progesterone levels above 1.5 ng/ml at the time of triggering final oocyte maturation? Summary Answer: The proportion of women with premature progesterone above 1.5 ng/ml was not significantly affected by letrozole co-treatment. WHAT IS KNOWN ALREADY: IVF creates multiple follicles with supraphysiological levels of sex steroids interrupting the endocrine milieu and affects the window of implantation. Letrozole is an effective aromatase inhibitor, normalizing serum oestradiol, thereby ameliorating some of the detrimental effects of IVF treatment. STUDY DESIGN, SIZE, DURATION: A randomized, double-blinded placebo-controlled trial investigated letrozole intervention during stimulation for IVF with FSH. The trial was conducted at four fertility clinics at University Hospitals in Denmark from August 2016 to November 2018. PARTICIPANTS/MATERIALS, SETTING, METHODS: A cohort of 129 women with expected normal ovarian reserve (anti-Müllerian hormone 8-32 nmol/l) completed an IVF cycle with fresh embryo transfer and received co-treatment with either 5 mg/day letrozole (n = 67) or placebo (n = 62), along with the FSH. Progesterone, oestradiol, FSH, LH and androgens were analysed in repeated serum samples collected from the start of the stimulation to the mid-luteal phase. In addition, the effect of letrozole on reproductive outcomes, total FSH consumption and adverse events were assessed. MAIN RESULTS AND THE ROLE OF CHANCE: The proportion of women with premature progesterone >1.5 ng/ml was similar (6% vs 0% (OR 0.0, 95% CI [0.0; 1.6], P = 0.12) in the letrozole versus placebo groups, respectively), whereas the proportion of women with mid-luteal progesterone >30 ng/ml was significantly increased in the letrozole group: (59% vs 31% (OR 3.3, 95% CI [1.4; 7.1], P = 0.005)). Letrozole versus placebo decreased oestradiol levels on

Published

2022

2. Treatment with the anti-IgE monoclonal antibody omalizumab in women with asthma undergoing fertility treatment:a proof-of-concept study - The PRO-ART study protocol

Author

Tidemandsen, Casper, Juul Gade, Elisabeth, Ulrik, Charlotte Suppli, Nielsen, Henriette Svarre, Oxlund-Mariegaard, Birgitte Sophie, Kristiansen, Karsten, Freiesleben, Nina La Cour, Nøhr, Bugge, Udengaard, Hanne, Backer, Vibeke, Tidemandsen, Casper, Juul Gade, Elisabeth, Ulrik, Charlotte Suppli, Nielsen, Henriette Svarre, Oxlund-Mariegaard, Birgitte Sophie, Kristiansen, Karsten, Freiesleben, Nina La Cour, Nøhr, Bugge, Udengaard, Hanne, and Backer, Vibeke

Abstract

Introduction Asthma is associated with prolonged time to pregnancy and a higher need for fertility treatment. However, the mechanism underlying this association remains incompletely understood. Previous research points to asthma-driven systemic inflammation also affecting the reproductive organs and thereby fertility. The aim of this study was to determine if treatment with omalizumab prior to fertility treatment will increase pregnancy rate among women with asthma by decreasing the systemic asthma-related inflammation and, by that, to provide insight into the underlying mechanisms. Methods and analysis This is an ongoing prospective multicentre randomised controlled trial planned to enrol 180 women with asthma recruited from fertility clinics in Denmark. The patients are randomised 1:1 to either omalizumab or placebo. The primary endpoint is the difference in pregnancy rate confirmed with ultrasound at gestational week 7 of pregnancy. The secondary endpoints are change in sputum and blood eosinophil cell count, change in biomarkers, change in microbiota, together with rate of pregnancy loss, frequency of malformations, pre-eclampsia, preterm birth, birth weight, small for gestational age and perinatal death between groups. Ethics and dissemination The methods used in this study are of low risk, but if successful, our findings will have a large impact on a large group of patients as infertility and asthma are the most common chronic diseases among the young population. The study has been approved by the Ethics Committee-Danish national research ethics committee (H-18016605) and the Danish Medicines Agency (EudraCT no: 2018-001137-41) and the Danish Data Protection Agency (journal number: VD-2018486 and I-Suite number 6745). The test results will be published regardless of whether they are positive, negative or inconclusive. Publication in international peer-reviewed scientific journals is planned. Trial registration number NCT03727971.

Published

2020

3. Treatment with the anti-IgE monoclonal antibody omalizumab in women with asthma undergoing fertility treatment:a proof-of-concept study - The PRO-ART study protocol

Author

Tidemandsen, Casper, Juul Gade, Elisabeth, Ulrik, Charlotte Suppli, Nielsen, Henriette Svarre, Oxlund-Mariegaard, Birgitte Sophie, Kristiansen, Karsten, Freiesleben, Nina La Cour, Nøhr, Bugge, Udengaard, Hanne, Backer, Vibeke, Tidemandsen, Casper, Juul Gade, Elisabeth, Ulrik, Charlotte Suppli, Nielsen, Henriette Svarre, Oxlund-Mariegaard, Birgitte Sophie, Kristiansen, Karsten, Freiesleben, Nina La Cour, Nøhr, Bugge, Udengaard, Hanne, and Backer, Vibeke

Abstract

Introduction Asthma is associated with prolonged time to pregnancy and a higher need for fertility treatment. However, the mechanism underlying this association remains incompletely understood. Previous research points to asthma-driven systemic inflammation also affecting the reproductive organs and thereby fertility. The aim of this study was to determine if treatment with omalizumab prior to fertility treatment will increase pregnancy rate among women with asthma by decreasing the systemic asthma-related inflammation and, by that, to provide insight into the underlying mechanisms. Methods and analysis This is an ongoing prospective multicentre randomised controlled trial planned to enrol 180 women with asthma recruited from fertility clinics in Denmark. The patients are randomised 1:1 to either omalizumab or placebo. The primary endpoint is the difference in pregnancy rate confirmed with ultrasound at gestational week 7 of pregnancy. The secondary endpoints are change in sputum and blood eosinophil cell count, change in biomarkers, change in microbiota, together with rate of pregnancy loss, frequency of malformations, pre-eclampsia, preterm birth, birth weight, small for gestational age and perinatal death between groups. Ethics and dissemination The methods used in this study are of low risk, but if successful, our findings will have a large impact on a large group of patients as infertility and asthma are the most common chronic diseases among the young population. The study has been approved by the Ethics Committee-Danish national research ethics committee (H-18016605) and the Danish Medicines Agency (EudraCT no: 2018-001137-41) and the Danish Data Protection Agency (journal number: VD-2018486 and I-Suite number 6745). The test results will be published regardless of whether they are positive, negative or inconclusive. Publication in international peer-reviewed scientific journals is planned. Trial registration number NCT03727971.

Published

2020

4. Non-invasive prenatal paternity testing using a standard forensic genetic massively parallel sequencing assay for amplification of human identification SNPs

Author

Christiansen, Sofie Lindgren, Jakobsen, Britt, Børsting, Claus, Udengaard, Hanne, Buchard, Anders, Kampmann, Marie-Louise, Grøndahl, Marie Louise, Morling, Niels, Christiansen, Sofie Lindgren, Jakobsen, Britt, Børsting, Claus, Udengaard, Hanne, Buchard, Anders, Kampmann, Marie-Louise, Grøndahl, Marie Louise, and Morling, Niels

Abstract

Prenatal paternity testing often relies on invasive procedures that cause risk to both the mother and the foetus. Non-invasive, prenatal paternity testing by investigating paternally inherited single nucleotide polymorphisms (SNPs) in cell-free foetal DNA (cffDNA) in maternal plasma was performed at consecutive time points during early gestation. Plasma from 15 pregnant women was investigated at consecutive time points from gestational weeks (GWs) 4–20. The Precision ID Identity Panel and an Ion S5 Sequencer was used to analyse the cffDNA. Paternally inherited foetal SNP alleles were detected from GW7. The median foetal fractions were 0%, 3.9%, 5.1%, 5.2%, and 4.7% at GWs 4, 7, 12, 16, and 20, respectively. The corresponding median numbers of detected paternally inherited foetal autosomal SNP alleles were 0, 3, 9, 10, and 12, respectively. The typical (i.e. geometric mean) paternity indices at GW12 and GW20 were 24 (range 0.0035–8389) and 199 (range 5.1–30,137), respectively. The method is very promising. However, the method can be improved by shortening the lengths of the PCR amplicons and increasing the number of SNPs. To our knowledge, this is the first study to successfully identify paternally inherited foetal SNP alleles at consecutive time points in early gestation independently of the foetal gender.

Published

2019

5. Non-invasive prenatal paternity testing using the Precision ID Identity Panel

Author

Christiansen, Sofie Lindgren, Jakobsen, Britt, Børsting, Claus, Udengaard, Hanne, Buchard, Anders, Kampmann, Marie-Louise, Grøndahl, Marie Louise, Morling, Niels, Christiansen, Sofie Lindgren, Jakobsen, Britt, Børsting, Claus, Udengaard, Hanne, Buchard, Anders, Kampmann, Marie-Louise, Grøndahl, Marie Louise, and Morling, Niels

Published

2018