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6. Treating Transgender People

Author

Tilleman, Kelly, De Roo, Chloë, Lierman, Sylvie, De Sutter, Petra, Allahbadia, Gautam Nand, editor, Ata, Baris, editor, Lindheim, Steven R., editor, Woodward, Bryan J., editor, and Bhagavath, Bala, editor

Published
2020
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7. Low feasibility of in vitro matured oocytes originating from cumulus complexes found during ovarian tissue preparation at the moment of gender confirmation surgery and during testosterone treatment for fertility preservation in transgender men

Author

Lierman, Sylvie, Tolpe, Annelies, De Croo, Ilse, De Gheselle, Stefanie, Defreyne, Justine, Baetens, Machteld, Dheedene, Annelies, Colman, Roos, Menten, Björn, T’Sjoen, Guy, De Sutter, Petra, and Tilleman, Kelly

Published
2021
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9. MicroRNA-146b negatively affects bovine embryo development and quality

Author

Pavani, Krishna Chaitanya, primary, XueFeng, Guan, additional, Chunduru, Jayendra, additional, Meese, Tim, additional, Peelman, Luc J., additional, Van Nieuwerburgh, Filip, additional, Deforce, Dieter, additional, Hendrix, An, additional, Tilleman, Kelly, additional, Van Soom, Ann, additional, and Smits, Katrien, additional

Published
2023
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11. ESHRE guideline: number of embryos to transfer during IVF/ICSI.

Author

Transfer, ESHRE Guideline Group on the Number of Embryos to, Alteri, Alessandra, Arroyo, Gemma, Baccino, Giuliana, Craciunas, Laurentiu, Geyter, Christian De, Ebner, Thomas, Koleva, Martina, Kordic, Klaudija, Mcheik, Saria, Mertes, Heidi, Baldani, Dinka Pavicic, Rodriguez-Wallberg, Kenny A, Rugescu, Ioana, Santos-Ribeiro, Samuel, Tilleman, Kelly, Woodward, Bryan, Vermeulen, Nathalie, and Veleva, Zdravka

Subjects
EMBRYO transfer, INTRACYTOPLASMIC sperm injection, HUMAN in vitro fertilization, FERTILIZATION in vitro, MEDICAL personnel
Abstract

STUDY QUESTION Which clinical and embryological factors should be considered to apply double embryo transfer (DET) instead of elective single embryo transfer (eSET)? SUMMARY ANSWER No clinical or embryological factor per se justifies a recommendation of DET instead of eSET in IVF/ICSI. WHAT IS KNOWN ALREADY DET is correlated with a higher rate of multiple pregnancy, leading to a subsequent increase in complications for both mother and babies. These complications include preterm birth, low birthweight, and other perinatal adverse outcomes. To mitigate the risks associated with multiple pregnancy, eSET is recommended by international and national professional organizations as the preferred approach in ART. STUDY DESIGN, SIZE, DURATION The guideline was developed according to the structured methodology for development and update of ESHRE guidelines. Literature searches were performed in PUBMED/MEDLINE and Cochrane databases, and relevant papers published up to May 2023, written in English, were included. Live birth rate, cumulative live birth rate, and multiple pregnancy rate were considered as critical outcomes. PARTICIPANTS/MATERIALS, SETTING, METHODS Based on the collected evidence, recommendations were discussed until a consensus was reached within the Guideline Development Group (GDG). A stakeholder review was organized after the guideline draft was finalized. The final version was approved by the GDG and the ESHRE Executive Committee. MAIN RESULTS AND THE ROLE OF CHANCE The guideline provides 35 recommendations on the medical and non-medical risks associated with multiple pregnancies and on the clinical and embryological factors to be considered when deciding on the number of embryos to transfer. These recommendations include 25 evidence-based recommendations, of which 24 were formulated as strong recommendations and one as conditional, and 10 good practice points. Of the evidence-based recommendations, seven (28%) were supported by moderate-quality evidence. The remaining recommendations were supported by low (three recommendations; 12%), or very low-quality evidence (15 recommendations; 60%). Owing to the lack of evidence-based research, the guideline also clearly mentions recommendations for future studies. LIMITATIONS, REASONS FOR CAUTION The guideline assessed different factors one by one based on existing evidence. However, in real life, clinicians' decisions are based on several prognostic factors related to each patient's case. Furthermore, the evidence from randomized controlled trials is too scarce to formulate high-quality evidence-based recommendations. WIDER IMPLICATIONS OF THE FINDINGS The guideline provides health professionals with clear advice on best practice in the decision-making process during IVF/ICSI, based on the best evidence currently available, and recommendations on relevant information that should be communicated to patients. In addition, a list of research recommendations is provided to stimulate further studies in the field. STUDY FUNDING/COMPETING INTEREST(S) The guideline was developed and funded by ESHRE, covering expenses associated with the guideline meetings, the literature searches, and the dissemination of the guideline. The guideline group members did not receive payment. DPB declared receiving honoraria for lectures from Merck, Ferring, and Gedeon Richter. She is a member of ESHRE EXCO, and the Mediterranean Society for reproductive medicine and the president of the Croatian Society for Gynaecological Endocrinology and Reproductive Medicine. CDG is the past Chair of the ESHRE EIM Consortium and a paid deputy member of the Editorial board of Human Reproduction. IR declared receiving reimbursement from ESHRE and EDCD for attending meetings. She holds an unpaid leadership role in OBBCSSR, ECDC Sohonet, and AER. KAR-W declared receiving grants for clinical researchers and funding provision to the institution from the Swedish Cancer Society (200170F), the Senior Clinical Investigator Award, Radiumhemmets Forskningsfonder (Dnr: 201313), Stockholm County Council FoU (FoUI-953912) and Karolinska Institutet (Dnr 2020-01963), NovoNordisk, Merck and Ferring Pharmaceuticals. She received consulting fees from the Swedish Ministry of Health and Welfare. She received honoraria from Roche, Pfizer, and Organon for chairmanship and lectures. She received support from Organon for attending meetings. She participated in advisory boards for Merck, Nordic countries, and Ferring. She declared receiving time-lapse equipment and grants with payment to institution for pre-clinical research from Merck pharmaceuticals and from Ferring. SS-R received research funding from Roche Diagnostics, Organon/MSD, Theramex, and Gedeo-Richter. He received consulting fees from Organon/MSD, Ferring Pharmaceuticals, and Merck Serono. He declared receiving honoraria for lectures from Ferring Pharmaceuticals, Besins, Organon/MSD, Theramex, and Gedeon Richter. He received support for attending Gedeon Richter meetings and participated in the Data Safety Monitoring Board of the T-TRANSPORT trial. He is the Deputy of ESHRE SQART special interest group. He holds stock options in IVI Lisboa and received equipment and other services from Roche Diagnostics and Ferring Pharmaceuticals. KT declared receiving payment for honoraria for giving lectures from Merck Serono and Organon. She is member of the safety advisory board of EDQM. She holds a leadership role in the ICCBBA board of directors. ZV received reimbursement from ESHRE for attending meetings. She also received research grants from ESHRE and Juhani Aaltonen Foundation. She is the coordinator of EHSRE SQART special interest group. The other authors have no conflicts of interest to declare. DISCLAIMER This guideline represents the views of ESHRE, which were achieved after careful consideration of the scientific evidence available at the time of preparation. In the absence of scientific evidence on certain aspects, a consensus between the relevant ESHRE stakeholders has been obtained. Adherence to these clinical practice guidelines does not guarantee a successful or specific outcome, nor does it establish a standard of care. Clinical practice guidelines do not replace the need for application of clinical judgement to each individual presentation, nor variations based on locality and facility type. ESHRE makes no warranty, express or implied, regarding the clinical practice guidelines and specifically excludes any warranties of merchantability and fitness for a particular use or purpose (full disclaimer available at https://www.eshre.eu/Guidelines-and-Legal). [ABSTRACT FROM AUTHOR]

Published
2024
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17. MicroRNA-146b negatively affects bovine embryo development and quality.

Author

Pavani, Krishna Chaitanya, Guan XueFeng, Chunduru, Jayendra, Meese, Tim, Peelman, Luc J., Van Nieuwerburgh, Filip, Deforce, Dieter, Hendrix, An, Tilleman, Kelly, Van Soom, Ann, and Smits, Katrien

Subjects
EMBRYOS, CULTURE media (Biology), GENE expression, EXTRACELLULAR vesicles, BOS, CELL differentiation
Abstract

MicroRNAs (miRNAs), which can be carried inside extracellular vesicles (EVs), play a crucial role in regulating embryo development up to the blastocyst stage. Yet, the molecular mechanisms underlying blastocyst development and quality are largely unknown. Recently, our group identified 69 differentially expressed miRNAs in extracellular vesicles (EVs) isolated from culture medium conditioned by bovine embryos that either developed to the blastocyst stage or did not (non-blastocysts). We found miR-146b to be more abundant in the EVs derived from media conditioned by non-blastocyst embryos. Using RT-qPCR, we here confirmed the upregulation of miR-146b in non-blastocyst (arrested at two- to four-cell and morula stage) embryos compared to blastocysts (P < 0.005), which coincides with the upregulation of miR-146b in EVs derived from the medium of these non-blastocysts. To evaluate a functional effect, bovine embryo culture media were supplemented with miR-146b mimics, resulting in significantly decreased embryo quality, with lower blastocyst rates at day 7 and lower total cell numbers, while the opposite was found after supplementation with miR-146b inhibitors, which resulted in reduced apoptosis rates (P < 0.01). Transcriptomic analysis of embryos treated with miR-146b mimics or inhibitors showed differential expression (P < 0.01) of genes associated with apoptosis, cell differentiation, and the RNA Pol II transcription complex, including WDR36, MBNL2, ERCC6l2, PYGO1, and SNIP1. Overall, miR-146b is overexpressed in non-blastocyst embryos and in EVs secreted by these embryos, and it regulates genes involved in embryo development and apoptosis, resulting in decreased embryo quality. [ABSTRACT FROM AUTHOR]

Published
2024
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19. Reproductive health in transgender and gender diverse individuals: A narrative review to guide clinical care and international guidelines

Author

Rodriguez-Wallberg, Kenny, Obedin-Maliver, Juno, Taylor, Bernard, van Mello, Norah, Tilleman, Kelly, and Nahata, Leena

Subjects
CENTRAL PRECOCIOUS PUBERTY, ARTIFICIAL CRYPTORCHIDISM, Health (social science), fertility preservation, Health Policy, Abortion, Medicine (miscellaneous), ADOLESCENT MALES, cryopreservation, sperm, transgender, OVARIAN TISSUE CRYOPRESERVATION, Gender Studies, PREGNANCY, FINAL HEIGHT, oocytes, gender-affirming hormone therapy, BONE-MINERAL DENSITY, infertility, TERM-FOLLOW-UP, GONADAL-FUNCTION
Abstract

Background: Hormonal treatments and surgical interventions practiced with the aim to affirm gender identity in transgender and gender diverse patients may impact their future reproductive ability, family building, and family planning options. Whereas it is recommended by international guidelines to discuss the potential risks of infertility and to present fertility preservation (FP) options to transgender individuals and their families prior to initiating any of these treatments, many barriers still remain. Further, transgender and gender diverse individuals often experience barriers to accessing contraception, abortion, pre-conception care, and comprehensive perinatal care. Aims: In this review we summarize the current literature on reproductive healthcare issues reported in transgender people including fertility issues, fertility preservation (FP), contraception, pregnancy and lactation and perinatal health. Methods: A narrative literature search of major databases (Pubmed, Medline, PsycInfo, Google Scholar, Web of Science) was conducted. Given the paucity and heterogeneity of studies, summative review tactics were not available. The literature was critically reviewed by international experts in the field with focus on the impact of gender-affirming medical interventions on future fertility, current FP options and reproductive health issues in transgender people. Results: The current literature supports that transgender and gender diverse individuals may wish to have genetically related children in the future, rendering the issue of FP relevant to this patient group. The cryopreservation of mature gametes is an efficacious option for FP for post-pubertal adolescents and adults. It is recommended to discuss these options at time of planning for gender-affirming hormonal therapy (GAHT) or engaging with other gender-affirming procedures that can limit future fertility. Discontinuation of GAHT may allow individuals to undergo FP later, but data are limited and there is the concern of symptoms and consequences of stopping GAHT. For pre-pubertal and early pubertal children, FP options are limited to the cryopreservation of gonadal tissue. At present the tissue can become functional only after re-transplantation, which might be undesirable by transgender individuals in the future. Preconception counseling, prenatal surveillance, perinatal support, contraceptive, and pregnancy termination related healthcare need to be meaningfully adapted for this patient population, and many knowledge gaps remain. Discussion: Specialized FP reproductive healthcare for transgender and gender diverse individuals is in early evolution. Research should be conducted to examine effects of medical interventions on fertility, timing of FP, gamete preservation and outcome of the fertility treatments. Strategies to inform and educate transgender and gender diverse patients can lead to optimization of reproductive care and counseling and decision making of FP for this population.

Published
2022

21. Endocrine outcome and seminal parameters in young adult men born with hypospadias: A cross-sectional cohort study

Author

Tack, Lloyd J.W., primary, Spinoit, Anne-Françoise, additional, Hoebeke, Piet, additional, Riedl, Stefan, additional, Springer, Alexander, additional, Tonnhofer, Ursula, additional, Hiess, Manuela, additional, Weninger, Julia, additional, Mahmoud, Ahmed, additional, Tilleman, Kelly, additional, Van Laecke, Erik, additional, Juul, Anders, additional, Albrethsen, Jakob, additional, De Baere, Elfride, additional, Van De Velde, Julie, additional, Verdin, Hannah, additional, and Cools, Martine, additional

Published
2022
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23. Hatching is modulated by microRNA-378a-3p derived from extracellular vesicles secreted by blastocysts

Author

Pavani, Krishna Chaitanya, Meese, Tim, Pascottini, Osvaldo Bogado, Guan, XueFeng, Lin, Xiaoyuan, Peelman, Luc, Hamacher, Joachim, Van Nieuwerburgh, Filip, Deforce, Dieter, Boel, Annekatrien, Heindryckx, Björn, Tilleman, Kelly, Van Soom, Ann, Gadella, Bart M, Hendrix, An, Smits, Katrien, FAH klinische reproductie, Veterinaire biochemie, dB&C FR-RMSC FR, dES/dFAH FR, FAH klinische reproductie, Veterinaire biochemie, dB&C FR-RMSC FR, and dES/dFAH FR

Subjects
animal structures, MICRORNAS, Veterinary medicine, Mirnas, DISEASE, ACTIVATION, Embryo Culture Techniques, Hatching, Animals, General, reproductive and urinary physiology, GENE-EXPRESSION, Multidisciplinary, PROLIFERATION, Biology and Life Sciences, Extracellular vesicles, Embryo, Mammalian, CANCER, EMBRYO QUALITY, Culture Media, MicroRNAs, Blastocyst, embryonic structures, SURVIVAL, COMPLEXES, Cattle, IMPLANTATION, Engineering sciences. Technology
Abstract

Extracellular vesicles (EVs) and their cargo microRNAs (miRNAs) are important regulators of embryo development to the blastocyst stage and beyond. Before implantation can take place, hatching of blastocysts from their zona pellucida is required. However, underlying mechanisms by which blastocyst formation and hatching are initiated remain largely unknown. Here, we provide evidence that embryonic EVs containing bta-miR-378a-3p play a crucial role in blastocyst hatching, using a bovine model. A customized procedure was used to isolate EV-miRNAs from culture droplets conditioned by individual bovine embryos that either developed to the blastocyst stage or did not (nonblastocyst). RNA sequencing identified 69 differentially expressed miRNAs between EVs derived from blastocyst conditioned medium (CM) and nonblastocyst CM. Among the miRNAs up-regulated in blastocyst CM, we selected bta-miR-378a-3p for further validation by functionality testing on developing in vitro embryos by means of mimics and inhibitors. Supplementing the embryo culture medium with miR-378a-3p mimic significandy improved blastocyst quality, with higher cell numbers and reduced apoptosis, and improved hatching, while the opposite was found after supplementation with miR-378a-3p inhibitor (P < 0.01). Transcriptomic analysis of embryos treated with miR-378 mimic/inhibitor showed differential expression (P < 0.01) of genes associated with embryo development and implantation, including RAPT GAP, ARFGEF2, SLC7A6, CENPA, SP1, LDLR, PYCRJ, MYD88, TPPJ, and NCOA3. In conclusion, miR-378a-3p is up-regulated in EVs secreted by embryos that develop to the blastocyst stage, and this EV-derived miR-378a-3p increases blastocyst quality and regulates embryo hatching, which is essential for embryo implantation.

Published
2022

24. Hatching is modulated by microRNA-378a-3p derived from extracellular vesicles secreted by blastocysts

Author

FAH klinische reproductie, Veterinaire biochemie, dB&C FR-RMSC FR, dES/dFAH FR, Pavani, Krishna Chaitanya, Meese, Tim, Pascottini, Osvaldo Bogado, Guan, XueFeng, Lin, Xiaoyuan, Peelman, Luc, Hamacher, Joachim, Van Nieuwerburgh, Filip, Deforce, Dieter, Boel, Annekatrien, Heindryckx, Björn, Tilleman, Kelly, Van Soom, Ann, Gadella, Bart M, Hendrix, An, Smits, Katrien, FAH klinische reproductie, Veterinaire biochemie, dB&C FR-RMSC FR, dES/dFAH FR, Pavani, Krishna Chaitanya, Meese, Tim, Pascottini, Osvaldo Bogado, Guan, XueFeng, Lin, Xiaoyuan, Peelman, Luc, Hamacher, Joachim, Van Nieuwerburgh, Filip, Deforce, Dieter, Boel, Annekatrien, Heindryckx, Björn, Tilleman, Kelly, Van Soom, Ann, Gadella, Bart M, Hendrix, An, and Smits, Katrien

Published
2022

25. Endocrine outcome and seminal parameters in young adult men born with hypospadias:A cross-sectional cohort study

Author

Tack, Lloyd J. W., Spinoit, Anne Françoise, Hoebeke, Piet, Riedl, Stefan, Springer, Alexander, Tonnhofer, Ursula, Hiess, Manuela, Weninger, Julia, Mahmoud, Ahmed, Tilleman, Kelly, Van Laecke, Erik, Juul, Anders, Albrethsen, Jakob, De Baere, Elfride, Van De Velde, Julie, Verdin, Hannah, Cools, Martine, Tack, Lloyd J. W., Spinoit, Anne Françoise, Hoebeke, Piet, Riedl, Stefan, Springer, Alexander, Tonnhofer, Ursula, Hiess, Manuela, Weninger, Julia, Mahmoud, Ahmed, Tilleman, Kelly, Van Laecke, Erik, Juul, Anders, Albrethsen, Jakob, De Baere, Elfride, Van De Velde, Julie, Verdin, Hannah, and Cools, Martine

Abstract

Background: Hypospadias affects around 1/200 newborn males. Intrauterine testicular dysfunction may underlie a subset of cases. The long-term endocrine and reproductive outcomes in these men remain largely unknown. Methods: Cross-sectional study in Ghent and Vienna University Hospitals to assess the endocrine and seminal parameters of young adult men (16–21 years) born with non-syndromic hypospadias (NSH) (n = 193) compared to healthy typical males (n = 50). Assessments included physical exam, semen analysis, hormone assays and exome-based gene panel analysis (474 genes). Findings: All participants had experienced a spontaneous puberty, in spite of higher LH and INSL3 levels than typical males. Oligo- or azoospermia was observed in 32/172 (18·6%; 99%-CI: 12·2–27·4%) of NSH men; but in 5/16 (31·3%; 99%-CI: 11·1;62·4%) of complex NSH men and in 13/22 (59·1%; 99%-CI: 33·2–80·7%) of those born small for gestational age (SGA). No (likely) pathogenic coding variants were found in the investigated genes. Suboptimal statural growth affected 8/23 (34·8%; 99%-CI: 15·4–61·0%) of men born SGA with NSH. Interpretation: Spermatogenesis is significantly compromised in NSH men, especially in those born SGA or those with complex NSH. Long-term andrological follow-up is recommended, including end-pubertal semen analysis. No clear monogenic causes could be demonstrated in our cohort even in proximal or complex NSH. Being born SGA with NSH is frequently associated with poor catch-up growth, requiring growth hormone therapy in some. Funding: Research grants from the European Society of Paediatric Endocrinology, the Belgian Society of Pediatrics, the Belgian Society of Pediatric Endocrinology and Diabetology and the Research Foundation Flanders (FWO).

Published
2022

26. Good practice recommendations for information provision for those involved in reproductive donation

Author

Kirkman-Brown, Jackson, Calhaz-Jorge, Carlos, Dancet, Eline AF, Lundin, Kersti, Martins, Mariana, Tilleman, Kelly, Thorn, Petra, Vermeulen, Nathalie, Frith, Lucy, Donation, ESHRE Working Grp Reprod, and Faculdade de Psicologia e de Ciências da Educação

Subjects
Reproductive Biology, Science & Technology, egg donation, donor-conception, direct-to-consumer genetic testing, gamete sharing, Social Sciences, Obstetrics & Gynecology, sperm donation, ESHRE TASK-FORCE, information, SPERM DONORS, counselling, IDENTITY-RELEASE, GAMETE DONOR ANONYMITY, EGG DONORS, Medicine and Health Sciences, HETEROSEXUAL COUPLES, OOCYTE DONATION, PARENTAL DISCLOSURE, PSYCHOLOGICAL ADJUSTMENT, FOLLOW-UP, disclosure, oocyte, Life Sciences & Biomedicine
Abstract

STUDY QUESTION What information and support should be offered to donors, intended parents and donor-conceived people, in general and in consideration of the availability of direct-to-consumer genetic testing and matching services? SUMMARY ANSWER For donors, intended parents and donor-conceived offspring, recommendations are made that cover information needs and informed consent, psychosocial implications and disclosure. WHAT IS KNOWN ALREADY Trends indicate that the use of donor-assisted conception is growing and guidance is needed to help these recipients/intended parents, the donors and offspring, navigate the rapidly changing environment in which donor-assisted conception takes place. STUDY DESIGN, SIZE, DURATION A working group (WG) collaborated on writing recommendations based, where available, on evidence collected from a literature search and expert opinion. Draft recommendations were published for stakeholder review and adapted where relevant based on the comments received. PARTICIPANTS/MATERIALS, SETTING, METHODS Papers retrieved from PUBMED were included from 1 January 2014 up to 31 August 2020, focusing on studies published since direct-to-consumer genetic testing has become more widespread and accessible. The current paper is limited to reproductive donation performed in medically assisted reproduction (MAR) centres (and gamete banks): donation outside the medical context was not considered. MAIN RESULTS AND THE ROLE OF CHANCE In total, 32 recommendations were made for information provision and support to donors, 32 for intended parents and 27 for donor-conceived offspring requesting information/support. LIMITATIONS, REASONS FOR CAUTION The available evidence in the area of reproductive donation is limited and diverse with regards to the context and types of donation. General conclusions and recommendations are largely based on expert opinion and may need to be adapted in light of future research. WIDER IMPLICATIONS OF THE FINDINGS These recommendations provide guidance to MAR centres and gamete banks on good practice in information provision and support but should also be considered by regulatory bodies and policymakers at a national and international level to guide regulatory and legislative efforts towards the protection of donors and donor-conceived offspring. STUDY FUNDING/COMPETING INTEREST(S) The development of this good practice paper was funded by European Society of Human Reproduction and Embryology (ESHRE), covering expenses associated with the WG meetings, the literature searches and dissemination. The WG members did not receive any payment. The authors have no conflicts of interest to declare. DISCLAIMER This document represents the views of ESHRE, which are the result of consensus between the relevant ESHRE stakeholders and where relevant based on the scientific evidence available at the time of preparation. The recommendations should be used for informational and educational purposes. They should not be interpreted as setting a standard of care, or be deemed inclusive of all proper methods of care nor exclusive of other methods of care reasonably directed to obtaining the same results. They do not replace the need for application of clinical judgement to each individual presentation, nor variations based on locality and facility type. †ESHRE pages content is not externally peer reviewed. The manuscript has been approved by the Executive Committee of ESHRE.

Published
2022

27. Additional file 1 of The fatty acid composition in follicles is related to the developmental potential of oocytes up to the blastocyst stage: a single-centre cohort study

Author

Liu, Yujie, Tilleman, Kelly, Vlaeminck, Bruno, Gervais, Rachel, Chouinard, P Yvan, De Sutter, Petra, and Fievez, Veerle

Abstract

Additional file 1. Correlation analysis for proportions (% by weight) of specific FF FA and FA groups with embryo outcome among normal weight women (n = 83) in 3 age groups.

Published
2022
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28. Additional file 2 of The fatty acid composition in follicles is related to the developmental potential of oocytes up to the blastocyst stage: a single-centre cohort study

Author

Liu, Yujie, Tilleman, Kelly, Vlaeminck, Bruno, Gervais, Rachel, Chouinard, P Yvan, De Sutter, Petra, and Fievez, Veerle

Abstract

Additional file 2. Correlation analysis for proportions (% by weight) of specific FF FA and FA groups with embryo outcome among overweight/obese women (n = 54) in 3 age groups.

Published
2022
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30. Reproductive health in transgender and gender diverse individuals: A narrative review to guide clinical care and international guidelines.

Author

Rodriguez-Wallberg, Kenny, Obedin-Maliver, Juno, Taylor, Bernard, Van Mello, Norah, Tilleman, Kelly, and Nahata, Leena

Subjects
CONTRACEPTION, LACTATION, MATERNAL health services, GENDER affirming care, HORMONE therapy, GENDER affirmation surgery, COUNSELING, GENDER-nonconforming people, INFERTILITY, FERTILITY preservation, FERTILITY, REPRODUCTIVE health, CRYOPRESERVATION of organs, tissues, etc., PRECONCEPTION care
Abstract

Hormonal treatments and surgical interventions practiced with the aim to affirm gender identity in transgender and gender diverse patients may impact their future reproductive ability, family building, and family planning options. Whereas it is recommended by international guidelines to discuss the potential risks of infertility and to present fertility preservation (FP) options to transgender individuals and their families prior to initiating any of these treatments, many barriers still remain. Further, transgender and gender diverse individuals often experience barriers to accessing contraception, abortion, pre-conception care, and comprehensive perinatal care. In this review we summarize the current literature on reproductive healthcare issues reported in transgender people including fertility issues, fertility preservation (FP), contraception, pregnancy and lactation and perinatal health. A narrative literature search of major databases (Pubmed, Medline, PsycInfo, Google Scholar, Web of Science) was conducted. Given the paucity and heterogeneity of studies, summative review tactics were not available. The literature was critically reviewed by international experts in the field with focus on the impact of gender-affirming medical interventions on future fertility, current FP options and reproductive health issues in transgender people. The current literature supports that transgender and gender diverse individuals may wish to have genetically related children in the future, rendering the issue of FP relevant to this patient group. The cryopreservation of mature gametes is an efficacious option for FP for post-pubertal adolescents and adults. It is recommended to discuss these options at time of planning for gender-affirming hormonal therapy (GAHT) or engaging with other gender-affirming procedures that can limit future fertility. Discontinuation of GAHT may allow individuals to undergo FP later, but data are limited and there is the concern of symptoms and consequences of stopping GAHT. For pre-pubertal and early pubertal children, FP options are limited to the cryopreservation of gonadal tissue. At present the tissue can become functional only after re-transplantation, which might be undesirable by transgender individuals in the future. Preconception counseling, prenatal surveillance, perinatal support, contraceptive, and pregnancy termination related healthcare need to be meaningfully adapted for this patient population, and many knowledge gaps remain. Specialized FP reproductive healthcare for transgender and gender diverse individuals is in early evolution. Research should be conducted to examine effects of medical interventions on fertility, timing of FP, gamete preservation and outcome of the fertility treatments. Strategies to inform and educate transgender and gender diverse patients can lead to optimization of reproductive care and counseling and decision making of FP for this population. [ABSTRACT FROM AUTHOR]

Published
2023
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36. Charting Extracellular Transcriptomes in The Human Biofluid RNA Atlas

Author

Hulstaert, Eva, primary, Morlion, Annelien, additional, Avila Cobos, Francisco, additional, Verniers, Kimberly, additional, Nuytens, Justine, additional, Vanden Eynde, Eveline, additional, Yigit, Nurten, additional, Anckaert, Jasper, additional, Geerts, Anja, additional, Hindryckx, Pieter, additional, Jacques, Peggy, additional, Brusselle, Guy, additional, Bracke, Ken R., additional, Maes, Tania, additional, Malfait, Thomas, additional, Derveaux, Thierry, additional, Ninclaus, Virginie, additional, Van Cauwenbergh, Caroline, additional, Roelens, Kristien, additional, Roets, Ellen, additional, Hemelsoet, Dimitri, additional, Tilleman, Kelly, additional, Brochez, Lieve, additional, Kuersten, Scott, additional, Simon, Lukas M., additional, Karg, Sebastian, additional, Kautzky-Willers, Alexandra, additional, Leutner, Michael, additional, Nöhammer, Christa, additional, Slaby, Ondrej, additional, Prins, Roméo Willinge, additional, Koster, Jan, additional, Lefever, Steve, additional, Schroth, Gary P., additional, Vandesompele, Jo, additional, and Mestdagh, Pieter, additional

Published
2020
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41. Abstract PR15: Charting extracellular transcriptomes in The Human Biofluid RNA Atlas

Author

Hulstaert, Eva, primary, Morlion, Annelien, additional, Cobos, Francisco Avila, additional, Verniers, Kimberly, additional, Nuytens, Justine, additional, Eynde, Eveline Vanden, additional, Yigit, Nurten, additional, Anckaert, Jasper, additional, Geerts, Anja, additional, Hindryckx, Pieter, additional, Jacques, Peggy, additional, Brusselle, Guy, additional, Bracke, Ken, additional, Maes, Tania, additional, Malfait, Thomas, additional, Derveaux, Thierry, additional, Ninclaus, Virginie, additional, Van Cauwenbergh, Caroline, additional, Roelens, Kristien, additional, Roets, Ellen, additional, Hemelsoet, Dimitri, additional, Tilleman, Kelly, additional, Brochez, Lieve, additional, Kuersten, Scott, additional, Simon, Lukas, additional, Karg, Sebastian, additional, Nöhammer, Christa, additional, Kautzky-Willers, Alexandra, additional, Leutner, Michael, additional, Slaby, Ondrej, additional, Schroth, Gary, additional, Vandesompele, Jo, additional, and Mestdagh, Pieter, additional

Published
2020
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44. Good practice recommendations for information provision for those involved in reproductive donation†.

Author

Donation, ESHRE Working Group on Reproductive, Kirkman-Brown, Jackson, Calhaz-Jorge, Carlos, Dancet, Eline A F, Lundin, Kersti, Martins, Mariana, Tilleman, Kelly, Thorn, Petra, Vermeulen, Nathalie, and Frith, Lucy

Subjects
GENETIC testing, STAKEHOLDERS, REPRODUCTIVE technology
Abstract

STUDY QUESTION What information and support should be offered to donors, intended parents and donor-conceived people, in general and in consideration of the availability of direct-to-consumer genetic testing and matching services? SUMMARY ANSWER For donors, intended parents and donor-conceived offspring, recommendations are made that cover information needs and informed consent, psychosocial implications and disclosure. WHAT IS KNOWN ALREADY Trends indicate that the use of donor-assisted conception is growing and guidance is needed to help these recipients/intended parents, the donors and offspring, navigate the rapidly changing environment in which donor-assisted conception takes place. STUDY DESIGN, SIZE, DURATION A working group (WG) collaborated on writing recommendations based, where available, on evidence collected from a literature search and expert opinion. Draft recommendations were published for stakeholder review and adapted where relevant based on the comments received. PARTICIPANTS/MATERIALS, SETTING, METHODS Papers retrieved from PUBMED were included from 1 January 2014 up to 31 August 2020, focusing on studies published since direct-to-consumer genetic testing has become more widespread and accessible. The current paper is limited to reproductive donation performed in medically assisted reproduction (MAR) centres (and gamete banks): donation outside the medical context was not considered. MAIN RESULTS AND THE ROLE OF CHANCE In total, 32 recommendations were made for information provision and support to donors, 32 for intended parents and 27 for donor-conceived offspring requesting information/support. LIMITATIONS, REASONS FOR CAUTION The available evidence in the area of reproductive donation is limited and diverse with regards to the context and types of donation. General conclusions and recommendations are largely based on expert opinion and may need to be adapted in light of future research. WIDER IMPLICATIONS OF THE FINDINGS These recommendations provide guidance to MAR centres and gamete banks on good practice in information provision and support but should also be considered by regulatory bodies and policymakers at a national and international level to guide regulatory and legislative efforts towards the protection of donors and donor-conceived offspring. STUDY FUNDING/COMPETING INTEREST(S) The development of this good practice paper was funded by European Society of Human Reproduction and Embryology (ESHRE), covering expenses associated with the WG meetings, the literature searches and dissemination. The WG members did not receive any payment. The authors have no conflicts of interest to declare. DISCLAIMER This document represents the views of ESHRE, which are the result of consensus between the relevant ESHRE stakeholders and where relevant based on the scientific evidence available at the time of preparation. The recommendations should be used for informational and educational purposes. They should not be interpreted as setting a standard of care, or be deemed inclusive of all proper methods of care nor exclusive of other methods of care reasonably directed to obtaining the same results. They do not replace the need for application of clinical judgement to each individual presentation, nor variations based on locality and facility type. ESHRE pages content is not externally peer reviewed. The manuscript has been approved by the Executive Committee of ESHRE. [ABSTRACT FROM AUTHOR]

Published
2022
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46. Blastocyst transfer for all? Higher cumulative live birth chance in a blastocyst-stage transfer policy compared to a cleavage-stage transfer policy

Author

Croo, Ilse, Roos Colman, Petra De Sutter, and Tilleman, Kelly

Subjects
Cleavage-stage transfer, blastocyst-stage transfer, Medicine and Health Sciences, cumulative live birth rate
Abstract

Background: In an unselected patient population, what is the cumulative live birth rate per oocyte collection cycle in a blastocyst-stage transfer policy compared to a cleavage-stage transfer policy? Methods: A retrospective cohort analysis of 1656 IVF and ICSI cycles was performed in two timeframes between January 2010 and December 2016. Transfer was scheduled, either on day 3 (n=729) or on day 5 (n=927). In this study, the main outcome measure was cumulative live birth rate per oocyte collection cycle including fresh and frozen embryo transfers in both groups. Results: The cumulative live birth rates per oocyte collection cycle were comparable between patients with cleavage-stage transfers (day 3 group) and those with blastocyst-stage transfers (day 5 group) (23.7% versus 25.5%, respectively; p = 0.42). After controlling for confounders, there was a 34% increased chance of live birth with blastocyst-stage transfer policy compared with cleavage-stage transfer policy (odds ratio (OR) =1.34; 95% confidence interval (CI), 1.051 to 1.704; p = 0.018). Conclusion: In an unselected patient cohort, the cumulative live birth chance per oocyte collection cycle is higher in a blastocyst-stage transfer policy compared to a cleavage-stage transfer policy.

Published
2019

47. ESHRE guideline: medically assisted reproduction in patients with a viral infection/disease†.

Author

infection/disease, ESHRE Guideline Group on Viral, Mocanu, Edgar, Drakeley, Andrew, Kupka, Markus S, Lara-Molina, Evelin E, Clef, Nathalie Le, Ombelet, Willem, Patrat, Catherine, Pennings, Guido, Semprini, Augusto Enrico, Tilleman, Kelly, Tognon, Mauro, Tonch, Nino, and Woodward, Bryan

Subjects
REPRODUCTIVE technology, VIRUS diseases, HEPATITIS B virus, PAPILLOMAVIRUSES, GUIDELINES, VERTICAL transmission (Communicable diseases)
Abstract

STUDY QUESTION What is the recommended management for medically assisted reproduction (MAR) in patients with a viral infection or disease, based on the best available evidence in the literature? SUMMARY ANSWER The ESHRE guideline on MAR in patients with a viral infection/disease makes 78 recommendations on prevention of horizontal and vertical transmission before, during and after MAR, and the impact on its outcomes, and these also include recommendations regarding laboratory safety on the processing and storage of gametes and embryos testing positive for viral infections. WHAT IS KNOWN ALREADY The development of new and improved anti-viral medications has resulted in improved life expectancy and quality of life for patients with viral infections/diseases. Patients of reproductive age are increasingly exploring their options for family creation. STUDY DESIGN, SIZE, DURATION The guideline was developed according to the structured methodology for the development of ESHRE guidelines. After the formulation of nine key questions for six viruses (hepatitis B virus, hepatitis C virus, human immunodeficiency virus, human papilloma virus, human T-lymphotropic virus I/II and Zika virus) by a group of experts, literature searches and assessments were performed. Papers published up to 2 November 2020 and written in English were included in the review. Evidence was analyzed by female, male or couple testing positive for the virus. PARTICIPANTS/MATERIALS, SETTING, METHODS Based on the collected evidence, recommendations were formulated and discussed until consensus was reached within the guideline group. There were 61 key questions to be answered by the guideline development group (GDG), of which 12 were answered as narrative questions and 49 as PICO (Patient, Intervention, Comparison, Outcome) questions. A stakeholder review was organized after the finalization of the draft. The final version was approved by the GDG and the ESHRE Executive Committee. MAIN RESULTS AND THE ROLE OF CHANCE This guideline aims to help providers meet a growing demand for guidance on the management of patients with a viral infection/disease presenting in the fertility clinic. The guideline makes 78 recommendations on prevention of viral transmission before and during MAR, and interventions to reduce/avoid vertical transmission to the newborn. Preferred MAR treatments and interventions are described together with the effect of viral infections on outcomes. The GDG formulated 44 evidence-based recommendations—of which 37 were formulated as strong recommendations and 7 as weak—33 good practice points (GPP) and one research only recommendation. Of the evidence-based recommendations, none were supported by high-quality evidence, two by moderate-quality evidence, 15 by low-quality evidence and 27 by very low-quality evidence. To support future research in the field of MAR in patients with a viral infection/disease, a list of research recommendations is provided. LIMITATIONS, REASONS FOR CAUTION Most interventions included are not well-studied in patients with a viral infection/disease. For a large proportion of interventions, evidence was very limited and of very low quality. More evidence is required for these interventions, especially in the field of human papilloma virus (HPV). Such future studies may require the current recommendations to be revised. WIDER IMPLICATIONS OF THE FINDINGS The guideline provides clinicians with clear advice on best practice in MAR for patients with a viral infection/disease, based on the best evidence currently available. In addition, a list of research recommendations is provided to stimulate further studies in the field. STUDY FUNDING/COMPETING INTEREST(S) The guideline was developed and funded by ESHRE, covering expenses associated with the guideline meetings, with the literature searches and with the dissemination of the guideline. The guideline group members did not receive any financial incentives, all work was provided voluntarily. A.D. reports research fees from Ferring and Merck, consulting fees from Ferring, outside the submitted work. C.P. reports speakers fees from Merck and MSD outside the submitted work. K.T. reports speakers fees from Cooper Surgical and Ferring and consultancy fees as member of the advisory board BioTeam of Ferring, outside the submitted work. The other authors have no conflicts of interest to declare. DISCLAIMER This guideline represents the views of ESHRE, which were achieved after careful consideration of the scientific evidence available at the time of preparation. In the absence of scientific evidence on certain aspects, a consensus between the relevant ESHRE stakeholders has been obtained. Adherence to these clinical practice guidelines does not guarantee a successful or specific outcome, nor does it establish a standard of care. Clinical practice guidelines do not replace the need for application of clinical judgment to each individual presentation, nor variations based on locality and facility type. ESHRE makes no warranty, express or implied, regarding the clinical practice guidelines and specifically excludes any warranties of merchantability and fitness for a particular use or purpose. (Full disclaimer available at www.eshre.eu/guidelines.) [ABSTRACT FROM AUTHOR]

Published
2021
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48. The Maribor consensus: report of an expert meeting on the development of performance indicators for clinical practice in ART.

Author

Group, ESHRE Clinic PI Working, Vlaisavljevic, Veljko, Apter, Susanna, Capalbo, Antonio, D'Angelo, Arianna, Gianaroli, Luca, Griesinger, Georg, Kolibianakis, Efstratios M, Lainas, George, Mardesic, Tonko, Motrenko, Tatjana, Pelkonen, Sari, Romualdi, Daniela, Vermeulen, Nathalie, and Tilleman, Kelly

Subjects
OVARIAN hyperstimulation syndrome, MULTIPLE pregnancy, ACQUISITION of data
Abstract

STUDY QUESTION Is it possible to define a set of performance indicators (PIs) for clinical work in ART, which can create competency profiles for clinicians and for specific clinical process steps? SUMMARY ANSWER The current paper recommends six PIs to be used for monitoring clinical work in ovarian stimulation for ART, embryo transfer, and pregnancy achievement: cycle cancellation rate (before oocyte pick-up (OPU)) (%CCR), rate of cycles with moderate/severe ovarian hyperstimulation syndrome (OHSS) (%mosOHSS), the proportion of mature (MII) oocytes at ICSI (%MII), complication rate after OPU (%CoOPU), clinical pregnancy rate (%CPR), and multiple pregnancy rate (%MPR). WHAT IS KNOWN ALREADY PIs are objective measures for evaluating critical healthcare domains. In 2017, ART laboratory key PIs (KPIs) were defined. STUDY DESIGN, SIZE, DURATION A list of possible indicators was defined by a working group. The value and limitations of each indicator were confirmed through assessing published data and acceptability was evaluated through an online survey among members of ESHRE, mostly clinicians, of the special interest group Reproductive Endocrinology. PARTICIPANTS/MATERIALS, SETTING, METHODS The online survey was open for 5 weeks and 222 replies were received. Statements (indicators, indicator definitions, or general statements) were considered accepted when ≥70% of the responders agreed (agreed or strongly agreed). There was only one round to seek levels of agreement between the stakeholders. Indicators that were accepted by the survey responders were included in the final list of indicators. Statements reaching less than 70% were not included in the final list but were discussed in the paper. MAIN RESULTS AND THE ROLE OF CHANCE Cycle cancellation rate (before OPU) and the rate of cycles with moderate/severe OHSS, calculated on the number of started cycles, were defined as relevant PIs for monitoring ovarian stimulation. For monitoring ovarian response, trigger and OPU, the proportion of MII oocytes at ICSI and complication rate after OPU were listed as PIs: the latter PI was defined as the number of complications (any) that require an (additional) medical intervention or hospital admission (apart from OHSS) over the number of OPUs performed. Finally, clinical pregnancy rate and multiple pregnancy rate were considered relevant PIs for embryo transfer and pregnancy. The defined PIs should be calculated every 6 months or per 100 cycles, whichever comes first. Clinical pregnancy rate and multiple pregnancy rate should be monitored more frequently (every 3 months or per 50 cycles). Live birth rate (LBR) is a generally accepted and an important parameter for measuring ART success. However, LBR is affected by many factors, even apart from ART, and it cannot be adequately used to monitor clinical practice. In addition to monitoring performance in general, PIs are essential for managing the performance of staff over time, and more specifically the gap between expected performance and actual performance measured. Individual clinics should determine which indicators are key to the success in their organisation based on their patient population, protocols, and procedures, and as such, which are their KPIs. LIMITATIONS, REASONS FOR CAUTION The consensus values are based on data found in the literature and suggestions of experts. When calculated and compared to the competence/benchmark limits, prudent interpretation is necessary taking into account the specific clinical practice of each individual centre. WIDER IMPLICATIONS OF THE FINDINGS The defined PIs complement the earlier defined indicators for the ART laboratory. Together, both sets of indicators aim to enhance the overall quality of the ART practice and are an essential part of the total quality management. PIs are important for education and can be applied during clinical subspecialty. STUDY FUNDING/COMPETING INTEREST(S) This paper was developed and funded by ESHRE, covering expenses associated with meetings, literature searches, and dissemination. The writing group members did not receive payment. Dr G.G. reports personal fees from Merck, MSD, Ferring, Theramex, Finox, Gedeon-Richter, Abbott, Biosilu, ReprodWissen, Obseva, PregLem, and Guerbet, outside the submitted work. Dr A.D. reports personal fees from Cook, outside the submitted work; Dr S.A. reports starting a new employment in May 2020 at Vitrolife. Previously, she has been part of the Nordic Embryology Academic Team, with meetings were sponsored by Gedeon Richter. The other authors have no conflicts of interest to declare. DISCLAIMER This document represents the views of ESHRE, which are the result of consensus between the relevant ESHRE stakeholders and where relevant based on the scientific evidence available at the time of preparation. The recommendations should be used for informational and educational purposes. They should not be interpreted as setting a standard of care, or be deemed inclusive of all proper methods of care nor exclusive of other methods of care reasonably directed to obtaining the same results. They do not replace the need for application of clinical judgment to each individual presentation, nor variations based on locality and facility type. Furthermore, ESHREs recommendations do not constitute or imply the endorsement, recommendation, or favouring of any of the included technologies by ESHRE. [ABSTRACT FROM AUTHOR]

Published
2021
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49. Charting extracellular transcriptomes in The Human Biofluid RNA Atlas

Author

Hulstaert, Eva, primary, Morlion, Annelien, additional, Cobos, Francisco Avila, additional, Verniers, Kimberly, additional, Nuytens, Justine, additional, Eynde, Eveline Vanden, additional, Yigit, Nurten, additional, Anckaert, Jasper, additional, Geerts, Anja, additional, Hindryckx, Pieter, additional, Jacques, Peggy, additional, Brusselle, Guy, additional, Bracke, Ken R., additional, Maes, Tania, additional, Malfait, Thomas, additional, Derveaux, Thierry, additional, Ninclaus, Virginie, additional, Van Cauwenbergh, Caroline, additional, Roelens, Kristien, additional, Roets, Ellen, additional, Hemelsoet, Dimitri, additional, Tilleman, Kelly, additional, Brochez, Lieve, additional, Kuersten, Scott, additional, Simon, Lukas, additional, Karg, Sebastian, additional, Kautzky-Willers, Alexandra, additional, Leutner, Michael, additional, Nöhammer, Christa, additional, Slaby, Ondrej, additional, Prins, Roméo Willinge, additional, Koster, Jan, additional, Lefever, Steve, additional, Schroth, Gary P., additional, Vandesompele, Jo, additional, and Mestdagh, Pieter, additional

Published
2019
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