World Endometriosis Research Foundation Endometriosis Phenome and Biobanking Harmonization Project: III. Fluid biospecimen collection, processing, and storage in endometriosis research

Nilüfer Rahmioğlu(University of Oxford), Amelie Fassbender(Organ Recovery Systems (Belgium)), Allison F. Vitonis(Brigham and Women's Hospital), Shelley S. Tworoger(Harvard University), Lone Hummelshøj(Endometriosis), Thomas D’Hooghe(KU Leuven), G. David Adamson(Endometriosis), Linda C. Giudice(World Endometriosis Research Foundation), Christian M. Becker(University of Oxford), Krina T. Zondervan(Centre for Human Genetics), Stacey A. Missmer(Brigham and Women's Hospital), G. David Adamson(Endometriosis), Catherine Allaire(Bayer (United States)), Raymond M. Anchan(University of Oxford), Christian M. Becker(University of Oxford), Mohamed A. Bedaiwy(Organ Recovery Systems (Belgium)), Germaine M. Buck Louis(Bayer (United States)), Carlos Calhaz–Jorge(University of Oxford), Kristof Chwalisż(Leuven Institute for Fertility and Embryology), Thomas D’Hooghe(Leuven Institute for Fertility and Embryology), Amelie Fassbender(Organ Recovery Systems (Belgium)), Thomas Faustmann(University of Oxford), Asgerally T. Fazleabas(University of Oxford), Idhaliz Flores(University of Oxford), Axel Forman(John Radcliffe Hospital), I.S. Fraser(Roche (Switzerland)), Linda C. Giudice(Endometriosis), Martin Götte(Boston Children's Hospital), Peter K. Gregersen(Bayer (United States)), Sun‐Wei Guo(University of Oxford), Tasuku Harada(John Radcliffe Hospital), D. Hartwell(Boston Children's Hospital), Andrew W. Horne(John Radcliffe Hospital), M. Louise Hull(John Radcliffe Hospital), Lone Hummelshøj(Endometriosis), Mohamed Gamal Ibrahim(John Radcliffe Hospital), Ludwig Kiesel(Centre for Human Genetics), Marc R. Laufer(Roche (Switzerland)), K. Machens(Leuven Institute for Fertility and Embryology), Sylvia Mechsner(Brigham and Women's Hospital), Stacey A. Missmer(Brigham and Women's Hospital), Grant W. Montgomery(Bayer (United States)), A. Nap(University of Oxford), Mette Nyegaard(Harvard University), Kevin G. Osteen(University of Oxford), Carlos Alberto Petta(University of Oxford), Nilüfer Rahmioğlu(University of Oxford), Stefan P. Renner(Bayer (United States)), J. Riedlinger(Endometriosis), S. Roehrich(Boston Children's Hospital), Peter A. W. Rogers(Roche (Switzerland)), Luk Rombauts(Centre for Human Genetics), Andres Salumets(John Radcliffe Hospital), Ertan Sarıdoğan(Bayer (United States)), Tamer Seckin(University of Oxford), Pamela Stratton(Leuven Institute for Fertility and Embryology), Kathy L. Sharpe-Timms(John Radcliffe Hospital), Shelley S. Tworoger(Brigham and Women's Hospital), Paola Viganò(Leuven Institute for Fertility and Embryology), Katy Vincent(Bayer (United States)), Allison F. Vitonis(Boston Children's Hospital), Ursula‐Henrike Wienhues‐Thelen(Roche (Switzerland)), P.P. Yeung(John Radcliffe Hospital), Paul J. Yong(John Radcliffe Hospital), Krina T. Zondervan(University of Oxford)
Fertility and Sterility
September 22, 2014
10.1016/j.fertnstert.2014.07.1208
Cited by 226Open Access
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Abstract

OBJECTIVE: To harmonize standard operating procedures (SOPs) and standardize the recording of associated data for collection, processing, and storage of fluid biospecimens relevant to endometriosis. DESIGN: An international collaboration involving 34 clinical/academic centers and 3 industry collaborators from 16 countries on 5 continents. SETTING: In 2013, 2 workshops were conducted, followed by global consultation, bringing together 54 leaders in endometriosis research and sample processing worldwide. PATIENT(S): None. INTERVENTION(S): Consensus SOPs were based on: [1] systematic comparison of SOPs from 18 global centers collecting fluid samples from women with and without endometriosis on a medium/large scale (publication on >100 cases), [2] literature evidence where available, or consultation with laboratory experts otherwise, and [3] several global consultation rounds. MAIN OUTCOME MEASURE(S): Standard recommended and minimum required SOPs for biofluid collection, processing, and storage in endometriosis research. RESULT(S): We developed recommended standard and minimum required SOPs for the collection, processing, and storage of plasma, serum, saliva, urine, endometrial/peritoneal fluid, and menstrual effluent, and a biospecimen data-collection form necessary for interpretation of sample-derived results. CONCLUSION(S): The Endometriosis Phenome and Biobanking Harmonisation Project SOPs allow endometriosis research centers to decrease variability in biofluid sample results, facilitating between-center comparisons and collaborations. The procedures are also relevant to research into other female conditions involving biofluid samples subject to cyclic reproductive influences. The consensus SOPs are based on the best available evidence; areas with limited evidence are identified as requiring further pilot studies. The SOPs will be reviewed based on investigator feedback, and through systematic tri-annual follow-up. Updated versions will be made available at: endometriosisfoundation.org/ephect.

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