Your search keyword '"Fowler PA"' showing total 192 results

1. Strategies for Preventing COPD Exacerbations in Primary Care Settings

Author

Fowler, Pa-C Caroline and Breedena, Pa-C Amanda

Subjects

Prevention, Development and progression, Health aspects, Mortality, Roflumilast -- Health aspects, Bronchitis -- Development and progression -- Prevention

Abstract

Chronic obstructive pulmonary disease (COPD) is a prevalent disease associated with high rates of morbidity and mortality. Although the underlying etiology of COPD can vary, the disease is marked by [...]

Published

2023

2. Science and policy on endocrine disrupters must not be mixed: A reply to a "common sense" intervention by toxicology journal editors

Author

Bergman, A, Andersson, AM, Becher, G, Van Den Berg, M, Blumberg, B, Bjerregaard, P, Bornehag, CG, Bornman, R, Brandt, I, Brian, JV, Casey, SC, Fowler, PA, Frouin, H, Giudice, LC, Iguchi, T, Hass, U, Jobling, S, Juul, A, Kidd, KA, Kortenkamp, A, Lind, M, Martin, OV, Muir, D, Ochieng, R, Olea, N, Norrgren, L, Ropstad, E, Ross, PS, Rudén, C, Scheringer, M, Skakkebaek, NE, Söder, O, Sonnenschein, C, Soto, A, Swan, S, Toppari, J, Tyler, CR, Vandenberg, LN, Vinggaard, AM, Wiberg, K, and Zoeller, RT

Abstract

The "common sense" intervention by toxicology journal editors regarding proposed European Union endocrine disrupter regulations ignores scientific evidence and well-established principles of chemical risk assessment. In this commentary, endocrine disrupter experts express their concerns about a recently published, and is in our considered opinion inaccurate and factually incorrect, editorial that has appeared in several journals in toxicology. Some of the shortcomings of the editorial are discussed in detail. We call for a better founded scientific debate which may help to overcome a polarisation of views detrimental to reaching a consensus about scientific foundations for endocrine disrupter regulation in the EU. © 2013 Bergman et al.; licensee BioMed Central Ltd.

Published

2013

3. Dynamics of the transcriptional landscape during human fetal testis and ovary development

Author

Lecluze E, Rolland AD, Filis P, Evrard B, Leverrier-Penna S, Maamar MB, Coiffec I, Lavoue V, Fowler PA, Mazaud-Guittot S, Jegou B, and Chalmel F

Published

2020

4. On Singular Signed Graphs with Nullspace Spanned by a Full Vector: Signed Nut Graphs

Author

Bašić Nino, Fowler Patrick W., Pisanski Tomaž, and Sciriha Irene

Subjects

signed graph, nut graph, singular graph, graph spectrum, fowler construction, sign-balanced graph, sign-unbalanced graph, cocktail-party graph, 05c50, 15a18, 05c22, 05c92, Mathematics, QA1-939

Abstract

A signed graph has edge weights drawn from the set {+1, −1}, and is sign-balanced if it is equivalent to an unsigned graph under the operation of sign switching; otherwise it is sign-unbalanced. A nut graph has a one dimensional kernel of the 0-1 adjacency matrix with a corresponding eigenvector that is full. In this paper we generalise the notion of nut graphs to signed graphs. Orders for which regular nut graphs with all edge weights +1 exist have been determined recently for the degrees up to 12. By extending the definition to signed graphs, we here find all pairs (ρ, n) for which a ρ-regular nut graph (sign-balanced or sign-unbalanced) of order n exists with ρ ≤ 11. We devise a construction for signed nut graphs based on a smaller ‘seed’ graph, giving infinite series of both sign-balanced and sign-unbalanced ρ -regular nut graphs. Orders for which a regular nut graph with ρ = n − 1 exists are characterised; they are sign-unbalanced with an underlying graph Kn for which n ≡ 1 (mod 4). Orders for which a regular sign-unbalanced nut graph with ρ = n − 2 exists are also characterised; they have an underlying cocktail-party graph CP(n) with even order n ≥ 8.

Published

2022

5. Exposure of fetal germ cells (F2) to a complex mixture of environmentally-relevant chemicals via grand-maternal (F0) ingestion subtly affects the fetal ovarian proteome

Author

Amezaga, Maria R, Skiba, JA, Fraser, M, Loup, Benoît, Mandon-Pepin, Beatrice, Poumerol, Elodie, Kyle, CE, Lea, RG, Sinclair, KD, Rhind, SM, Cotinot, Corinne, Fowler, PA, Biologie du Développement et Reproduction (BDR), Institut National de la Recherche Agronomique (INRA), ANR REEF, Biologie du développement et reproduction (BDR), and Centre National de la Recherche Scientifique (CNRS)-École nationale vétérinaire d'Alfort (ENVA)-Institut National de la Recherche Agronomique (INRA)

Subjects

[SDV.BDLR]Life Sciences [q-bio]/Reproductive Biology, [SDV.BDD]Life Sciences [q-bio]/Development Biology

Abstract

This work was supported by the European Community 'S Seveneth Framework Programme (FP/2007-2013) agreement n° 212885; absent

Published

2011

6. Existence of Regular Nut Graphs for Degree at Most 11

Author

Fowler Patrick W., Gauci John Baptist, Goedgebeur Jan, Pisanski Tomaž, and Sciriha Irene

Subjects

nut graph, core graph, regular graph, nullity, 05c30, 05c50, 05c75, 05c90, 68r10, Mathematics, QA1-939

Abstract

A nut graph is a singular graph with one-dimensional kernel and corresponding eigenvector with no zero elements. The problem of determining the orders n for which d-regular nut graphs exist was recently posed by Gauci, Pisanski and Sciriha. These orders are known for d ≤ 4. Here we solve the problem for all remaining cases d ≤ 11 and determine the complete lists of all d-regular nut graphs of order n for small values of d and n. The existence or non-existence of small regular nut graphs is determined by a computer search. The main tool is a construction that produces, for any d-regular nut graph of order n, another d-regular nut graph of order n+2d. If we are given a sufficient number of d-regular nut graphs of consecutive orders, called seed graphs, this construction may be applied in such a way that the existence of all d-regular nut graphs of higher orders is established. For even d the orders n are indeed consecutive, while for odd d the orders n are consecutive even numbers. Furthermore, necessary conditions for combinations of order and degree for vertex-transitive nut graphs are derived.

Published

2020

7. Effects of Exposure to Environmental Chemicals During Pregnancy on the Development of the Male and Female Reproductive Axes

Author

Bellingham, M, primary, Fiandanese, N, additional, Byers, A, additional, Cotinot, C, additional, Evans, NP, additional, Pocar, P, additional, Amezaga, MR, additional, Lea, RG, additional, Sinclair, KD, additional, Rhind, SM, additional, and Fowler, PA, additional

Published

2012

8. Ovarian gonadotrophin surge-attenuating factor (GnSAF): where are we after 20 years of research?

Author

Fowler, PA, primary, Sorsa-Leslie, T, additional, Harris, W, additional, and Mason, HD, additional

Published

2003

9. Demonstration of a non-steroidal, non-inhibin factor in the ovine corpus luteum of pregnancy that reduces pituitary responsiveness to GnRH-induced LH secretion in vitro

Author

Fowler, PA, primary, Groome, NP, additional, and Al-Gubory, KH, additional

Published

2003

10. Effects of pregnancy on pulsatile secretion of LH and gonadotrophin-releasing hormone-induced LH release in sheep: a longitudinal study

Author

Al-Gubory, KH, primary, Hervieu, J, additional, and Fowler, PA, additional

Published

2003

11. Environmental chemical effects on testicular function

Author

Fowler, PA, primary, Murray, T, additional, Abramovich, DR, additional, Haites, N, additional, and Lea, RG, additional

Published

2002

12. Effect of maternal undernutrition on fetal testicular steroidogenesis during the CNS androgen-responsive period in male sheep fetuses

Author

Rae, MT, primary, Rhind, SM, additional, Fowler, PA, additional, Miller, DW, additional, Kyle, CE, additional, and Brooks, AN, additional

Published

2002

13. Safety, Tolerability, and Pharmacokinetics of Sumatriptan Suppositories Following Single and Multiple doses in Healthy Volunteers

Author

Kunka, RL, primary, Hussey, EK, additional, Shaw, S, additional, Warner, P, additional, Aubert, B, additional, Richard, I, additional, Fowler, PA, additional, and Pakes, GE, additional

Published

1997

14. The effects of oral sumatriptan, a 5-HT1 receptor agonist, on circulating ACTH and cortisol concentrations in man.

Author

Entwisle, SJ, primary, Fowler, PA, additional, Thomas, M, additional, Eckland, DJ, additional, Lettis, S, additional, York, M, additional, and Freedman, PS, additional

Published

1995

15. Lack of effect of flunarizine on the pharmacokinetics and pharmacodynamics of sumatriptan in healthy volunteers.

Author

Hecken, AM, primary, Depre, M, additional, Schepper, PJ, additional, Fowler, PA, additional, Lacey, LF, additional, and Durham, JM, additional

Published

1992

16. Validation of the in vivo measurement of adipose tissue by magnetic resonance imaging of lean and obese pigs

Author

Fowler, PA, primary, Fuller, MF, additional, Glasbey, CA, additional, Cameron, GG, additional, and Foster, MA, additional

Published

1992

17. Lack of an interaction between propranolol and sumatriptan.

Author

Scott, AK, primary, Walley, T, additional, Breckenridge, AM, additional, Lacey, LF, additional, and Fowler, PA, additional

Published

1991

18. Total and subcutaneous adipose tissue in women: the measurement of distribution and accurate prediction of quantity by using magnetic resonance imaging

Author

Fowler, PA, primary, Fuller, MF, additional, Glasbey, CA, additional, Foster, MA, additional, Cameron, GG, additional, McNeill, G, additional, and Maughan, RJ, additional

Published

1991

19. A longitudinal study of maternal serum inhibin-A, inhibin-B, activin-A, activin-AB, pro-alphaC and follistatin during pregnancy.

Author

Fowler, PA, Evans, LE, Groome, NP, Templeton, A, Knight, PG, Fowler, P A, Evans, L W, Groome, N P, and Knight, P G

Subjects

CARRIER proteins, COMPARATIVE studies, GLYCOPROTEINS, GONADOTROPIN, LONGITUDINAL method, RESEARCH methodology, MEDICAL cooperation, PEPTIDE hormones, RESEARCH, STEROIDS, TIME, EVALUATION research

Abstract

Maternal serum concentrations of inhibin-A, inhibin-B, activin-A, activin-AB, pro-alphaC-related inhibin forms, total follistatin, steroids and gonadotrophins were measured longitudinally in six normal singleton pregnancies. Maternal venous blood was collected randomly during a spontaneous follicular phase prior to donor insemination, at 5, 7, 9, 11, 16, 20, 24, 28, 32 and 36 weeks after the first missed menses and in the early puerperium. Steroid and gonadotrophin profiles conformed to previous reports. While at week 5 of gestation inhibin-A, activin-A and follistatin concentrations were similar to those at the follicular phase, all three increased progressively (P < 0.001) to maximal concentrations in week 36: approximately 48-fold (3740 +/- 1349 ng inhibin-A/ml), approximately 22-fold (6109 +/- 1443 ng activin-A/ml) and approximately 10-fold (3563 +/- 418 ng follistatin/ml) higher. Pro-alphaC concentrations reached a maximum in weeks 5 (approximately 5-fold, P < 0.001) and 36 (1027 +/- 174 pg/ml, P < 0.01). Inhibin-B (71 +/- 23 pg/ml prior to pregnancy) was undetectable (<12 pg/ml) between week 5-16 of gestation but increased slightly in the third trimester (26 +/- 7 pg/ml in week 36). Activin-AB was undetectable throughout pregnancy. Post-partum concentrations of inhibin-A (41 +/- 12 ng/ml), inhibin-B (<12 pg/ml), activin-A (950 +/- 149 pg/ml), pro-alphaC (128 +/- 22 pg/ml) and follistatin (990 +/- 79 ng/ml) were substantially lower than at week 36 of gestation. The activin-A:follistatin ratio increased from 0.5 in week 5 to 1.8 in week 36, suggesting that more free activin-A is available in the maternal circulation during late pregnancy. [ABSTRACT FROM AUTHOR]

Published

1998

20. Selection of gonadotrophin surge attenuating factor phage antibodies by bioassay

Author

Mason Helen D, Sorsa-Leslie Tarja, Harris William J, and Fowler Paul A

Subjects

Gynecology and obstetrics, RG1-991, Reproduction, QH471-489

Abstract

Abstract Background We aimed to combine the generation of "artificial" antibodies with a rat pituitary bioassay as a new strategy to overcome 20 years of difficulties in the purification of gonadotrophin surge-attenuating factor (GnSAF). Methods A synthetic single-chain antibody (Tomlinson J) phage display library was bio-panned with partially purified GnSAF produced by cultured human granulosa/luteal cells. The initial screening with a simple binding immunoassay resulted in 8 clones that were further screened using our in-vitro rat monolayer bioassay for GnSAF. Initially the antibodies were screened as pooled phage forms and subsequently as individual, soluble, single-chain antibody (scAbs) forms. Then, in order to improve the stability of the scAbs for immunopurification purposes, and to widen the range of labelled secondary antibodies available, these were engineered into full-length human immunoglobulins. The immunoglobulin with the highest affinity for GnSAF and a previously described rat anti-GnSAF polyclonal antiserum was then used to immunopurify bioactive GnSAF protein. The two purified preparations were electrophoresed on 1-D gels and on 7 cm 2-D gels (pH 4–7). The candidate GnSAF protein bands and spots were then excised for peptide mass mapping. Results Three of the scAbs recognised GnSAF bioactivity and subsequently one clone of the purified scAb-derived immunoglobulin demonstrated high affinity for GnSAF bioactivity, also binding the molecule in such as way as to block its bioactivity. When used for repeated immunopurification cycles and then Western blot, this antibody enabled the isolation of a GnSAF-bioactive protein band at around 66 kDa. Similar results were achieved using the rat anti-GnSAF polyclonal antiserum. The main candidate molecules identified from the immunopurified material by excision of 2-D gel protein spots was human serum albumin precursor and variants. Conclusion This study demonstrates that the combination of bioassay and phage display technologies is a powerful tool in the study of uncharacterised proteins that defy conventional approaches. In addition, we conclude that these data support suggestions that GnSAF may be structurally related to serum albumin or very tightly bound to serum albumin.

Published

2005

21. PAH exposure.

Author

Fowler PA, O'Shaughnessy PJ, Rhind SM, Ayres J, Choi H, Spengler J, and Perera FP

Published

2009

22. The profile of steroid hormones in human fetal and adult ovaries.

Author

Vazakidou P, Evangelista S, Li T, Lecante LL, Rosenberg K, Koekkoek J, Salumets A, Velthut-Meikas A, Damdimopoulou P, Mazaud-Guittot S, Fowler PA, Leonards PEG, and van Duursen MBM

Subjects

Humans, Female, Adult, Pregnancy, Gonadal Steroid Hormones biosynthesis, Gonadal Steroid Hormones metabolism, Gonadal Steroid Hormones analysis, Tandem Mass Spectrometry, Follicular Fluid metabolism, Follicular Fluid chemistry, Estradiol metabolism, Chromatography, Liquid, Ovary metabolism, Fetus metabolism

Abstract

Background: Reproduction in women is at risk due to exposure to chemicals that can disrupt the endocrine system during different windows of sensitivity throughout life. Steroid hormone levels are fundamental for the normal development and function of the human reproductive system, including the ovary. This study aims to elucidate steroidogenesis at different life-stages in human ovaries., Methods: We have developed a sensitive and specific LC-MS/MS method for 21 important steroid hormones and measured them at different life stages: in media from cultures of human fetal ovaries collected from elective terminations of normally progressing pregnancy and in media from adult ovaries from Caesarean section patients, and follicular fluid from women undergoing infertility treatment. Statistically significant differences in steroid hormone levels and their ratios were calculated with parametric tests. Principal component analysis (PCA) was applied to explore clustering of the ovarian-derived steroidogenic profiles., Results: Comparison of the 21 steroid hormones revealed clear differences between the various ovarian-derived steroid profiles. Interestingly, we found biosynthesis of both canonical and "backdoor" pathway steroid hormones and corticosteroids in first and second trimester fetal and adult ovarian tissue cultures. 17α-estradiol, a less potent naturally occurring isomer of 17β-estradiol, was detected only in follicular fluid. PCA of the ovarian-derived profiles revealed clusters from: adult ovarian tissue cultures with relatively high levels of androgens; first trimester and second trimester fetal ovarian tissue cultures with relatively low estrogen levels; follicular fluid with the lowest androgens, but highest corticosteroid, progestogen and estradiol levels. Furthermore, ratios of specific steroid hormones showed higher estradiol/ testosterone and estrone/androstenedione (indicating higher CYP19A1 activity, p < 0.01) and higher 17-hydroxyprogesterone/progesterone and dehydroepiandrosterone /androstenedione (indicating higher CYP17A1 activity, p < 0.01) in fetal compared to adult ovarian tissue cultures., Conclusions: Human ovaries demonstrate de novo synthesis of non-canonical and "backdoor" pathway steroid hormones and corticosteroids. Elucidating the steroid profiles in human ovaries improves our understanding of physiological, life-stage dependent, steroidogenic capacity of ovaries and will inform mechanistic studies to identify endocrine disrupting chemicals that affect female reproduction., (© 2024. The Author(s).)

Published

2024

23. In utero exposures to perfluoroalkyl substances and the human fetal liver metabolome in Scotland: a cross-sectional study.

Author

Hyötyläinen T, McGlinchey A, Salihovic S, Schubert A, Douglas A, Hay DC, O'Shaughnessy PJ, Iredale JP, Shaw S, Fowler PA, and Orešič M

Subjects

Adult, Pregnancy, Humans, Female, Male, Cross-Sectional Studies, Metabolome, Scotland, Bile Acids and Salts, Metabolic Diseases, Fluorocarbons adverse effects

Abstract

Background: Perfluoroalkyl and polyfluoroalkyl substances are classed as endocrine disrupting compounds but continue to be used in many products such as firefighting foams, flame retardants, utensil coatings, and waterproofing of food packaging. Perfluoroalkyl exposure aberrantly modulates lipid, metabolite, and bile acid levels, increasing susceptibility to onset and severity of metabolic diseases, such as diabetes and metabolic dysfunction-associated steatotic liver disease. To date, most studies in humans have focused on perfluoroalkyl-exposure effects in adults. In this study we aimed to show if perfluoroalkyls are present in the human fetal liver and if they have metabolic consequences for the human fetus., Methods: In this cross-sectional study, human fetal livers from elective termination of pregnancies at the Aberdeen Pregnancy Counselling Service, Aberdeen, UK, were analysed by both targeted (bile acids and perfluoroalkyl substances) and combined targeted and untargeted (lipids and polar metabolites) mass spectrometry based metabolomic analyses, as well as with RNA-Seq. Only fetuses from normally progressing pregnancies (determined at ultrasound scan before termination), terminated for non-medical reasons, from women older than 16 years, fluent in English, and between 11 and 21 weeks of gestation were collected. Women exhibiting considerable emotional distress or whose fetuses had anomalies identified at ultrasound scan were excluded. Stringent bioinformatic and statistical methods such as partial correlation network analysis, linear regression, and pathway analysis were applied to this data to investigate the association of perfluoroalkyl exposure with hepatic metabolic pathways., Findings: Fetuses included in this study were collected between Dec 2, 2004, and Oct 27, 2014. 78 fetuses were included in the study: all 78 fetuses were included in the metabolomics analysis (40 female and 38 male) and 57 fetuses were included in the RNA-Seq analysis (28 female and 29 male). Metabolites associated with perfluoroalkyl were identified in the fetal liver and these varied with gestational age. Conjugated bile acids were markedly positively associated with fetal age. 23 amino acids, fatty acids, and sugar derivatives in fetal livers were inversely associated with perfluoroalkyl exposure, and the bile acid glycolithocholic acid was markedly positively associated with all quantified perfluoroalkyl. Furthermore, 7α-hydroxy-4-cholesten-3-one, a marker of bile acid synthesis rate, was strongly positively associated with perfluoroalkyl levels and was detectable as early as gestational week 12., Interpretation: Our study shows direct evidence for the in utero effects of perfluoroalkyl exposure on specific key hepatic products. Our results provide evidence that perfluoroalkyl exposure, with potential future consequences, manifests in the human fetus as early as the first trimester of gestation. Furthermore, the profiles of metabolic changes resemble those observed in perinatal perfluoroalkyl exposures. Such exposures are already linked with susceptibility, initiation, progression, and exacerbation of a wide range of metabolic diseases., Funding: UK Medical Research Council, Horizon Europe Program of the European Union, Seventh Framework Programme of the European Union, NHS Grampian Endowments grants, European Partnership for the Assessment of Risks from Chemicals, Swedish Research Council, Formas, Novo Nordisk Foundation, and the Academy of Finland., Competing Interests: Declaration of interests DCH is a founder, director, and shareholder in Stemnovate and Stimuliver. All other authors declare no competing interests., (Copyright © 2024 The Author(s). Published by Elsevier Ltd. This is an Open Access article under the CC BY 4.0 license. Published by Elsevier Ltd.. All rights reserved.)

Published

2024

24. Maternal exposure to ambient black carbon particles and their presence in maternal and fetal circulation and organs: an analysis of two independent population-based observational studies.

Author

Bongaerts E, Lecante LL, Bové H, Roeffaers MBJ, Ameloot M, Fowler PA, and Nawrot TS

Subjects

Carbon analysis, Child, Cotinine analysis, Female, Humans, Infant, Newborn, Pregnancy, Soot adverse effects, Air Pollution adverse effects, Air Pollution analysis, Maternal Exposure adverse effects

Abstract

Background: Maternal exposure to particulate air pollution during pregnancy has been linked to multiple adverse birth outcomes causing burden of disease later in the child's life. To date, there is a paucity of data on whether or not ambient particles can both reach and cross the human placenta to exert direct effects on fetal organ systems during gestation., Methods: In this analysis, we used maternal-perinatal and fetal samples collected within the framework of two independent studies: the ENVIRONAGE (Environmental Influences on Ageing in Early Life) birth cohort of mothers giving birth at the East-Limburg Hospital in Genk, Belgium, and the SAFeR (Scottish Advanced Fetal Research) cohort of terminated, normally progressing pregnancies among women aged 16 years and older in Aberdeen and the Grampian region, UK. From the ENVIRONAGE study, we included 60 randomly selected mother-neonate pairs, excluding all mothers who reported that they ever smoked. From the SAFeR study, we included 36 fetuses of gestational age 7-20 weeks with cotinine concentrations indicative of non-smoking status. We used white light generation under femtosecond pulsed illumination to detect black carbon particles in samples collected at the maternal-fetal interface. We did appropriate validation experiments of all samples to confirm the carbonaceous nature of the identified particles., Findings: We found evidence of the presence of black carbon particles in cord blood, confirming the ability of these particles to cross the placenta and enter the fetal circulation system. We also found a strong correlation (r ≥0·50; p&lt;0·0001) between the maternal-perinatal particle load (in maternal blood [n=60], term placenta [n=60], and cord blood [n=60]) and residential ambient black carbon exposure during pregnancy. Additionally, we found the presence of black carbon particles in first and second trimester tissues (fetal liver [n=36], lung [n=36], and brain [n=14]) of electively terminated and normally progressing pregnancies from an independent study., Interpretation: We found that maternally inhaled carbonaceous air pollution particles can cross the placenta and then translocate into human fetal organs during gestation. These findings are especially concerning because this window of exposure is key to organ development. Further studies are needed to elucidate the mechanisms of particle translocation., Funding: European Research Council, Flemish Scientific Research Foundation, Kom op Tegen Kanker, UK Medical Research Council, and EU Horizon 2020., Competing Interests: Declaration of interests HB, MBJR, MA, and TSN declare that aspects of the work mentioned in the paper are the subject of an awarded patent (Method for detecting or quantifying carbon black and/or black carbon particles, reference codes: EP3403068B1 and US11002679B2) filed by Hasselt University (Hasselt, Belgium) and KU Leuven (Leuven, Belgium). All other authors declare no competing interests., (Copyright © 2022 The Author(s). Published by Elsevier Ltd. This is an Open Access article under the CC BY-NC-ND 4.0 license. Published by Elsevier Ltd.. All rights reserved.)

Published

2022

25. BPA disrupts meiosis I in oogonia by acting on pathways including cell cycle regulation, meiosis initiation and spindle assembly.

Author

Loup B, Poumerol E, Jouneau L, Fowler PA, Cotinot C, and Mandon-Pépin B

Subjects

Animals, Female, Humans, Meiosis, Oocytes, Phenols toxicity, Sheep, Benzhydryl Compounds toxicity, Oogonia

Abstract

The negative in utero effects of bisphenol A (BPA) on female reproduction are of concern since the ovarian reserve of primordial follicles is constituted during the fetal period. This time-window is difficult to access, particularly in humans. Animal models and explant culture systems are, therefore, vital tools for investigating EDC impacts on primordial germ cells (PGCs). Here, we investigated the effects of BPA on prophase I meiosis in the fetal sheep ovary. We established an in vitro model of early gametogenesis through retinoic acid (RA)-induced differentiation of sheep PGCs that progressed through meiosis. Using this system, we demonstrated that BPA (3 ×10 -7 M & 3 ×10 -5 M) exposure for 20 days disrupted meiotic initiation and completion in sheep oogonia and induced transcriptomic modifications of exposed explants. After exposure to the lowest concentrations of BPA (3 ×10 -7 M), only 2 probes were significantly up-regulated corresponding to NR2F1 and TMEM167A transcripts. In contrast, after exposure to 3 × 10 -5 M BPA, 446 probes were deregulated, 225 were down- and 221 were up-regulated following microarray analysis. Gene Ontology (GO) annotations of differentially expressed genes revealed that pathways mainly affected were involved in cell-cycle phase transition, meiosis and spindle assembly. Differences in key gene expression within each pathway were validated by qRT-PCR. This study provides a novel model for direct examination of the molecular pathways of environmental toxicants on early female gametogenesis and novel insights into the mechanisms by which BPA affects meiosis I. BPA exposure could thereby disrupt ovarian reserve formation by inhibiting meiotic progression of oocytes I and consequently by increasing atresia of primordial follicles containing defective oocytes., (Copyright © 2022. Published by Elsevier Inc.)

Published

2022

26. Exposure to a human relevant mixture of persistent organic pollutants or to perfluorooctane sulfonic acid alone dysregulates the developing cerebellum of chicken embryo.

Author

Yadav A, Verhaegen S, Filis P, Domanska D, Lyle R, Sundaram AYM, Leithaug M, Østby GC, Aleksandersen M, Berntsen HF, Zimmer KE, Fowler PA, Paulsen RE, and Ropstad E

Abstract

Prenatal exposure to persistent organic pollutants (POPs) is associated with neurodevelopmental disorders. In the present study, we explored whether a human-relevant POP mixture affects the development of chicken embryo cerebellum. We used a defined mixture of 29 POPs, with chemical composition and concentrations based on blood levels in the Scandinavian population. We also evaluated exposure to a prominent compound in the mixture, perfluorooctane sulfonic acid (PFOS), alone. Embryos (n = 7-9 per exposure group) were exposed by injection directly into the allantois at embryonic day 13 (E13). Cerebella were isolated at E17 and subjected to morphological, RNA-seq and shot-gun proteomics analyses. There was a reduction in thickness of the molecular layer of cerebellar cortex in both exposure scenarios. Exposure to the POP mixture significantly affected expression of 65 of 13,800 transcripts, and 43 of 2,568 proteins, when compared to solvent control. PFOS alone affected expression of 80 of 13,859 transcripts, and 69 of 2,555 proteins. Twenty-five genes and 15 proteins were common for both exposure groups. These findings point to alterations in molecular events linked to retinoid X receptor (RXR) signalling, neuronal cell proliferation and migration, cellular stress responses including unfolded protein response, lipid metabolism, and myelination. Exposure to the POP mixture increased methionine oxidation, whereas PFOS decreased oxidation. Several of the altered genes and proteins are involved in a wide variety of neurological disorders. We conclude that POP exposure can interfere with fundamental aspects of neurodevelopment, altering molecular pathways that are associated with adverse neurocognitive and behavioural outcomes., (Copyright © 2022. Published by Elsevier Ltd.)

Published

2022

27. Hepatic Mitochondrial Dysfunction and Risk of Liver Disease in an Ovine Model of "PCOS Males".

Author

Siemienowicz KJ, Filis P, Thomas J, Fowler PA, Duncan WC, and Rae MT

Abstract

First-degree male relatives of polycystic ovary syndrome (PCOS) sufferers can develop metabolic abnormalities evidenced by elevated circulating cholesterol and triglycerides, suggestive of a male PCOS equivalent. Similarly, male sheep overexposed to excess androgens in fetal life develop dyslipidaemia in adolescence. Dyslipidaemia, altered lipid metabolism, and dysfunctional hepatic mitochondria are associated with the development of non-alcoholic liver disease (NAFLD). We therefore dissected hepatic mitochondrial function and lipid metabolism in adolescent prenatally androgenized (PA) males from an ovine model of PCOS. Testosterone was directly administered to male ovine fetuses to create prenatal androgenic overexposure. Liver RNA sequencing and proteomics occurred at 6 months of age. Hepatic lipids, glycogen, ATP, reactive oxygen species (ROS), DNA damage, and collagen were assessed. Adolescent PA males had an increased accumulation of hepatic cholesterol and glycogen, together with perturbed glucose and fatty acid metabolism, mitochondrial dysfunction, with altered mitochondrial transport, decreased oxidative phosphorylation and ATP synthesis, and impaired mitophagy. Mitochondrial dysfunction in PA males was associated with increased hepatic ROS level and signs of early liver fibrosis, with clinical relevance to NAFLD progression. We conclude that excess in utero androgen exposure in male fetuses leads to a PCOS-like metabolic phenotype with dysregulated mitochondrial function and likely lifelong health sequelae.

Published

2022

28. Maternal over-the-counter analgesics use during pregnancy and adverse perinatal outcomes: cohort study of 151 141 singleton pregnancies.

Author

Zafeiri A, Raja EA, Mitchell RT, Hay DC, Bhattacharya S, and Fowler PA

Subjects

Acetaminophen, Analgesics adverse effects, Birth Weight, Cohort Studies, Female, Humans, Infant, Newborn, Male, Pregnancy, Pregnancy Outcome epidemiology, Retrospective Studies, Stillbirth epidemiology, Hypospadias, Perinatal Death, Premature Birth epidemiology

Abstract

Objectives: To identify any associations between in utero exposure to five over-the-counter (non-prescription) analgesics (paracetamol, ibuprofen, aspirin, diclofenac, naproxen) and adverse neonatal outcomes., Design: Retrospective cohort study using the Aberdeen Maternity and Neonatal Databank., Participants: 151 141 singleton pregnancies between 1985 and 2015., Main Outcome Measures: Premature delivery (<37 weeks), stillbirth, neonatal death, birth weight, standardised birthweight score, neonatal unit admission, APGAR score at 1 and 5 min, neural tube and amniotic band defects, gastroschisis and, in males, cryptorchidism and hypospadias., Results: 83.7% of women taking over-the-counter analgesics reported first trimester use when specifically asked about use at their first antenatal clinic visit. Pregnancies exposed to at least one of the five analgesics were significantly independently associated with increased risks for premature delivery <37 weeks (adjusted OR (aOR)=1.50, 95% CI 1.43 to 1.58), stillbirth (aOR=1.33, 95% CI 1.15 to 1.54), neonatal death (aOR=1.56, 95% CI 1.27 to 1.93), birth weight <2500 g (aOR=1.28, 95% CI 1.20 to 1.37), birth weight >4000 g (aOR=1.09, 95% CI 1.05 to 1.13), admission to neonatal unit (aOR=1.57, 95% CI 1.51 to 1.64), APGAR score <7 at 1 min (aOR=1.18, 95% CI 1.13 to 1.23) and 5 min (aOR=1.48, 95% CI 1.35 to 1.62), neural tube defects (aOR=1.64, 95% CI 1.08 to 2.47) and hypospadias (aOR=1.27, 95% CI 1.05 to 1.54 males only). The overall prevalence of over-the-counter analgesics use during pregnancy was 29.1%, however it rapidly increased over the 30-year study period, to include over 60% of women in the last 7 years of the study. This makes our findings highly relevant to the wider pregnant population., Conclusions: Over-the-counter (non-prescription) analgesics consumption during pregnancy was associated with a substantially higher risk for adverse perinatal health outcomes in the offspring. The use of paracetamol in combination with other non-steroidal anti-inflammatory drugs conferred the highest risk. The increased risks of adverse neonatal outcomes associated with non-prescribed, over-the-counter, analgesics use during pregnancy indicate that healthcare guidance for pregnant women regarding analgesic use need urgent updating., Competing Interests: Competing interests: DCH is a founder, director and shareholder in Stemnovate Limited. The remaining authors have no interests to disclose., (© Author(s) (or their employer(s)) 2022. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.)

Published

2022

29. Ovine fetal testis stage-specific sensitivity to environmental chemical mixtures.

Author

Lea RG, Mandon-Pépin B, Loup B, Poumerol E, Jouneau L, Egbowon BF, Bowden A, Cotinot C, Purdie L, Zhang Z, Fowler PA, and Sinclair KD

Subjects

Animals, Female, Fetus, Humans, Male, Pregnancy, Sewage adverse effects, Sheep, Testosterone metabolism, Sheep, Domestic, Testis metabolism

Abstract

Exposure of the fetal testis to numerous individual environmental chemicals (ECs) is frequently associated with dysregulated development, leading to impaired adult reproductive competence. However, 'real-life' exposure involves complex mixtures of ECs. Here we test the consequences, for the male fetus, of exposing pregnant ewes to EC mixtures derived from pastures treated with biosolids fertiliser (processed human sewage). Fetal testes from continuously exposed ewes were either unaffected at day 80 or exhibited a reduced area of testis immunostained for CYP17A1 protein at day 140. Fetal testes from day 140 pregnant ewes that were exposed transiently for 80-day periods during early (0-80 days), mid (30-110 days), or late (60-140 days) pregnancy had fewer Sertoli cells and reduced testicular area stained for CYP17A1. Male fetuses from ewes exposed during late pregnancy also exhibited reduced fetal body, adrenal and testis mass, anogenital distance, and lowered testosterone; collectively indicative of an anti-androgenic effect. Exposure limited to early gestation induced more testis transcriptome changes than observed for continuously exposed day 140 fetuses. These data suggest that a short period of EC exposure does not allow sufficient time for the testis to adapt. Consequently, testicular transcriptomic changes induced during the first 80 days of gestation may equate with phenotypic effects observed at day 140. In contrast, relatively fewer changes in the testis transcriptome in fetuses exposed continuously to ECs throughout gestation are associated with less severe consequences. Unless corrected by or during puberty, these differential effects would predictably have adverse outcomes for adult testicular function and fertility.

Published

2022

30. Six Decades of Research on Human Fetal Gonadal Steroids.

Author

Connan-Perrot S, Léger T, Lelandais P, Desdoits-Lethimonier C, David A, Fowler PA, and Mazaud-Guittot S

Subjects

Female, Humans, Immunoassay, Male, Mass Spectrometry, Ovary metabolism, Ovary ultrastructure, Sexual Development genetics, Testis metabolism, Testis ultrastructure, Fetus metabolism, Gonadal Steroid Hormones metabolism, Gonads metabolism, Research trends

Abstract

Human fetal gonads acquire endocrine steroidogenic capabilities early during their differentiation. Genetic studies show that this endocrine function plays a central role in the sexually dimorphic development of the external genitalia during fetal development. When this endocrine function is dysregulated, congenital malformations and pathologies are the result. In this review, we explain how the current knowledge of steroidogenesis in human fetal gonads has benefited from both the technological advances in steroid measurements and the assembly of detailed knowledge of steroidogenesis machinery and its expression in human fetal gonads. We summarise how the conversion of radiolabelled steroid precursors, antibody-based assays, mass spectrometry, ultrastructural studies, and the in situ labelling of proteins and mRNA have all provided complementary information. In this review, our discussion goes beyond the debate on recommendations concerning the best choice between the different available technologies, and their degrees of reproducibility and sensitivity. The available technologies and techniques can be used for different purposes and, as long as all quality controls are rigorously employed, the question is how to maximise the generation of robust, reproducible data on steroid hormones and their crucial roles in human fetal development and subsequent functions.

Published

2021

31. Pubertal FGF21 deficit is central in the metabolic pathophysiology of an ovine model of polycystic ovary syndrome.

Author

Siemienowicz KJ, Furmanska K, Filis P, Talia C, Thomas J, Fowler PA, Rae MT, and Duncan WC

Subjects

Androgens metabolism, Animals, Biomarkers metabolism, Chemokines metabolism, Disease Models, Animal, Female, Fibroblast Growth Factors metabolism, Gene Expression Regulation, Inflammation pathology, Lipids chemistry, Liver metabolism, Liver pathology, Oxidation-Reduction, Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-alpha metabolism, Polycystic Ovary Syndrome genetics, Sex Characteristics, Sheep, Signal Transduction, Subcutaneous Fat metabolism, Triglycerides metabolism, Fibroblast Growth Factors deficiency, Polycystic Ovary Syndrome metabolism, Polycystic Ovary Syndrome physiopathology, Sexual Maturation

Abstract

Polycystic ovary syndrome (PCOS), affecting over 10% of women, is associated with insulin resistance, obesity, dyslipidaemia, fatty liver and adipose tissue dysfunction. Its pathogenesis is poorly understood and consequently treatment remains suboptimal. Prenatally androgenized (PA) sheep, a clinically realistic model of PCOS, recapitulate the metabolic problems associated with PCOS. Fibroblast Growth Factor 21 (FGF21) is a metabolic hormone regulating lipid homeostasis, insulin sensitivity, energy balance and adipose tissue function. We therefore investigated the role of FGF21 in the metabolic phenotype of PA sheep. In adolescence PA sheep had decreased hepatic expression and circulating concentrations of FGF21. Adolescent PA sheep show decreased FGF21 signalling in subcutaneous adipose tissue, increased hepatic triglyceride content, trend towards reduced fatty acid oxidation capacity and increased hepatic expression of inflammatory markers. These data parallel studies on FGF21 deficiency, suggesting that FGF21 therapy during adolescence may represent a treatment strategy to mitigate metabolic problems associated with PCOS., (Copyright © 2021 Elsevier B.V. All rights reserved.)

Published

2021

32. The insulin-like growth factor system: A target for endocrine disruptors?

Author

Talia C, Connolly L, and Fowler PA

Subjects

Animals, Halogenated Diphenyl Ethers toxicity, Humans, Reproducibility of Results, Dioxins, Endocrine Disruptors toxicity, Somatomedins

Abstract

The insulin-like growth factor (IGF) system is a critical regulator of growth, especially during fetal development, while also playing a central role in metabolic homeostasis. Endocrine disruptors (EDs) are ubiquitous compounds able to interfere with hormone action and impact human health. For example, exposure to EDs is associated with decreased birthweight and increased incidence of metabolic disorders. Therefore, the IGF system is a potential target for endocrine disruption. This review summarises the state of the science regarding effects of exposure to major classes of endocrine disruptors (dioxins and dioxin-like compounds, polycyclic aromatic hydrocarbons, polybrominated diphenyl ethers, phthalates, perfluoroalkyl substances and bisphenol A) on the IGF system. Evidence from both experimental models (in vitro and in vivo) and epidemiological studies is presented. In addition, possible molecular mechanisms of action and effects on methylation are discussed. There is a large body of evidence supporting the link between dioxins and dioxin-like compounds and IGF disruption, but mixed findings have been reported in human studies. On the other hand, although only a few animal studies have investigated the effects of phthalates on the IGF system, their negative association with IGF levels and methylation status has been more consistently reported in humans. For polybrominated diphenyl ethers, perfluoroalkyl substances and bisphenol A the evidence is still limited. Despite a lack of studies for some ED classes linking ED exposure to changes in IGF levels, and the need for further research to improve reproducibility and determine the degree of risk posed by EDs to the IGF system, this is clearly an area of concern., (Copyright © 2020 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2021

33. Over-the-counter analgesics during pregnancy: a comprehensive review of global prevalence and offspring safety.

Author

Zafeiri A, Mitchell RT, Hay DC, and Fowler PA

Subjects

Acetaminophen, Female, Humans, Nonprescription Drugs adverse effects, Pregnancy, Prevalence, Analgesics adverse effects, Placenta

Abstract

Background: Analgesia during pregnancy is often necessary. Due to their widespread availability, many mothers opt to use over-the-counter (OTC) analgesics. Those analgesic compounds and their metabolites can readily cross the placenta and reach the developing foetus. Evidence for safety or associations with adverse health outcomes is conflicting, limiting definitive decision-making for healthcare professionals., Objective and Rationale: This review provides a detailed and objective overview of research in this field. We consider the global prevalence of OTC analgesia during pregnancy, explain the current mechanistic understanding of how analgesic compounds cross the placenta and reach the foetus, and review current research on exposure associations with offspring health outcomes., Search Methods: A comprehensive English language literature search was conducted using PubMed and Scopus databases. Different combinations of key search terms were used including 'over-the-counter/non-prescription analgesics', 'pregnancy', 'self-medication', 'paracetamol', 'acetaminophen', 'diclofenac', 'aspirin', 'ibuprofen', 'in utero exposure', 'placenta drug transport', 'placental transporters', 'placenta drug metabolism' and 'offspring outcomes'., Outcomes: This article examines the evidence of foetal exposure to OTC analgesia, starting from different routes of exposure to evidence, or the lack thereof, linking maternal consumption to offspring ill health. There is a very high prevalence of maternal consumption of OTC analgesics globally, which is increasing sharply. The choice of analgesia selected by pregnant women differs across populations. Location was also observed to have an effect on prevalence of use, with more developed countries reporting the highest consumption rates. Some of the literature focuses on the association of in utero exposure at different pregnancy trimesters and the development of neurodevelopmental, cardiovascular, respiratory and reproductive defects. This is in contrast to other studies which report no associations., Wider Implications: The high prevalence and the challenges of reporting exact consumption rates make OTC analgesia during pregnancy a pressing reproductive health issue globally. Even though some healthcare policy-making authorities have declared the consumption of some OTC analgesics for most stages of pregnancy to be safe, such decisions are often based on partial review of literature. Our comprehensive review of current evidence highlights that important knowledge gaps still exist. Those areas require further research in order to provide pregnant mothers with clear guidance with regard to OTC analgesic use during pregnancy., (© The Author(s) 2020. Published by Oxford University Press on behalf of European Society of Human Reproduction and Embryology. All rights reserved. For permissions, please email: journals.permissions@oup.com.)

Published

2021

34. Early pregnancy maternal progesterone administration alters pituitary and testis function and steroid profile in male fetuses.

Author

Siemienowicz KJ, Wang Y, Marečková M, Nio-Kobayashi J, Fowler PA, Rae MT, and Duncan WC

Subjects

Animals, Female, Male, Pregnancy, Progesterone adverse effects, Fetal Development drug effects, Fetus embryology, Pituitary Gland embryology, Progesterone pharmacology, Sheep metabolism, Testis embryology

Abstract

Maternal exposure to increased steroid hormones, including estrogens, androgens or glucocorticoids during pregnancy results in chronic conditions in offspring that manifest in adulthood. Little is known about effects of progesterone administration in early pregnancy on fetal development. We hypothesised that maternal early pregnancy progesterone supplementation would increase fetal progesterone, affect progesterone target tissues in the developing fetal reproductive system and be metabolised to other bioactive steroids in the fetus. We investigated the effects of progesterone treatment during early pregnancy on maternal and fetal plasma progesterone concentrations, transcript abundance in the fetal pituitary and testes and circulating steroids, at day 75 gestation, using a clinically realistic ovine model. Endogenous progesterone concentrations were lower in male than female fetuses. Maternal progesterone administration increased male, but not female, fetal progesterone concentrations, also increasing circulating 11-dehydrocorticosterone in male fetuses. Maternal progesterone administration altered fetal pituitary and testicular function in ovine male fetuses. This suggests that there may be fetal sex specific effects of the use of progesterone in early pregnancy, and highlights that progesterone supplementation should be used only when there is clear evidence of efficacy and for as limited time as necessary.

Published

2020

35. Genome-wide expression changes induced by bisphenol A, F and S in human stem cell derived hepatocyte-like cells.

Author

Lucendo-Villarin B, Nell P, Hellwig B, Filis P, Feuerborn D, O'Shaughnessy PJ, Godoy P, Rahnenführer J, Hengstler JG, Cherianidou A, Sachinidis A, Fowler PA, and Hay DC

Abstract

The debate about possible adverse effects of bisphenol A (BPA) has been ongoing for decades. Bisphenol F (BPF) and S (BPS) have been suggested as "safer" alternatives. In the present study we used hepatocyte-like cells (HLCs) derived from the human embryonic stem cell lines Man12 and H9 to compare the three bisphenol derivatives. Stem cell-derived progenitors were produced using an established system and were exposed to BPA, BPF and BPS for 8 days during their transition to HLCs. Subsequently, we examined cell viability, inhibition of cytochrome P450 (CYP) activity, and genome-wide RNA profiles. Sub-cytotoxic, inhibitory concentrations (IC 50 ) of CYP3A were 20, 9.5 and 25 µM for BPA, BPF and BPS in Man12 derived HLCs, respectively. The corresponding concentrations for H9-derived HLCs were 19, 29 and 31 µM. These IC 50 concentrations were used to study global expression changes in this in vitro study and are higher than unconjugated BPA in serum of the general population. A large overlap of up- as well as downregulated genes induced by the three bisphenol derivatives was seen. This is at least 28-fold higher compared to randomly expected gene expression changes. Moreover, highly significant correlations of expression changes induced by the three bisphenol derivatives were obtained in pairwise comparisons. Dysregulated genes were associated with reduced metabolic function, cellular differentiation, embryonic development, cell survival and apoptosis. In conclusion, no major differences in cytochrome inhibitory activities of BPA, BPF and BPS were observed and gene expression changes showed a high degree of similarity., (Copyright © 2020 Lucendo-Villarin et al.)

Published

2020

36. Putative adverse outcome pathways for female reproductive disorders to improve testing and regulation of chemicals.

Author

Johansson HKL, Damdimopoulou P, van Duursen MBM, Boberg J, Franssen D, de Cock M, Jääger K, Wagner M, Velthut-Meikas A, Xie Y, Connolly L, Lelandais P, Mazaud-Guittot S, Salumets A, Draskau MK, Filis P, Fowler PA, Christiansen S, Parent AS, and Svingen T

Subjects

Animals, Endocrine System Diseases chemically induced, Female, Humans, Mice, Ovarian Diseases chemically induced, Ovary physiopathology, Pregnancy, Risk Assessment, Toxicity Tests, Adverse Outcome Pathways, Chemical Safety, Maternal Exposure, Ovary drug effects, Reproductive Health

Abstract

Modern living challenges female reproductive health. We are witnessing a rise in reproductive disorders and drop in birth rates across the world. The reasons for these manifestations are multifaceted and most likely include continuous exposure to an ever-increasing number of chemicals. The cause-effect relationships between chemical exposure and female reproductive disorders, however, have proven problematic to determine. This has made it difficult to assess the risks chemical exposures pose to a woman's reproductive development and function. To address this challenge, this review uses the adverse outcome pathway (AOP) concept to summarize current knowledge about how chemical exposure can affect female reproductive health. We have a special focus on effects on the ovaries, since they are essential for lifelong reproductive health in women, being the source of both oocytes and several reproductive hormones, including sex steroids. The AOP framework is widely accepted as a new tool for toxicological safety assessment that enables better use of mechanistic knowledge for regulatory purposes. AOPs equip assessors and regulators with a pragmatic network of linear cause-effect relationships, enabling the use of a wider range of test method data in chemical risk assessment and regulation. Based on current knowledge, we propose ten putative AOPs relevant for female reproductive disorders that can be further elaborated and potentially be included in the AOPwiki. This effort is an important step towards better safeguarding the reproductive health of all girls and women.

Published

2020

37. Corrigendum. Testing the twin testosterone transfer hypothesis-intergenerational analysis of 317 dizygotic twins born in Aberdeen, Scotland.

Author

Talia C, Raja EA, Bhattacharya S, and Fowler PA

Published

2020

38. Expression of the Insulin-like Growth Factor System in First- and Second-Trimester Human Embryonic and Fetal Gonads.

Author

Mamsen LS, Zafeiri A, Bøtkjær JA, Hardlei JR, Ernst E, Oxvig C, Fowler PA, and Andersen CY

Subjects

Adolescent, Adult, Embryo, Mammalian, Female, Fetus metabolism, Fetus pathology, Gene Expression Profiling, Gene Expression Regulation, Developmental, Gestational Age, Humans, Insulin-Like Growth Factor Binding Proteins metabolism, Male, Microarray Analysis, Middle Aged, Pregnancy, Pregnancy Trimester, First metabolism, Pregnancy Trimester, Second metabolism, Receptors, Somatomedin metabolism, Signal Transduction genetics, Somatomedins metabolism, Young Adult, Gonads embryology, Gonads metabolism, Gonads pathology, Insulin-Like Growth Factor Binding Proteins genetics, Pregnancy Trimester, First genetics, Pregnancy Trimester, Second genetics, Receptors, Somatomedin genetics, Somatomedins genetics

Abstract

Context: Insulin-like growth factor (IGF) signaling is crucial for sex differentiation and development of Leydig and Sertoli cells in fetal mice testes. No such information is available for human embryonic and fetal testes and ovaries., Objective: To investigate presence and activity of the IGF signaling system during human embryonic and fetal ovarian and testicular development., Design: Human embryonic and fetal gonads were obtained following legal terminations of pregnancies. Gene expression was assessed by microarray and qPCR transcript analyses. Proteins of the IGF system components were detected with immunohistochemistry and immunofluorescence analyses. Specimens were included from 2010 to 2017., Setting: University Hospital., Patients/participants: Ovaries and testes from a total of 124 human embryos and fetuses aged 5 to 17 postconception weeks were obtained from healthy women aged 16 to 47 years resident in Denmark or Scotland., Main Outcome Measures: Gene expression analysis using microarray was performed in 46 specimens and qPCR analysis in 56 specimens, both sexes included. Protein analysis included 22 specimens (11 ovaries, 11 testes)., Results: IGF system members were detected in embryonic and fetal testes and ovaries, both at gene transcript and protein level. A higher expression of IGF regulators was detected in testes than ovaries, with a preferred localization to Leydig cells., Conclusions: These data indicate that the IGF system is active during very early gestation, when it may have a regulatory role in Leydig cells., (© Endocrine Society 2020. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published

2020

39. Testing the twin testosterone transfer hypothesis-intergenerational analysis of 317 dizygotic twins born in Aberdeen, Scotland.

Author

Talia C, Raja EA, Bhattacharya S, and Fowler PA

Subjects

Child, Cohort Studies, Female, Humans, Male, Pregnancy, Pregnancy, Twin, Scotland, Testosterone, Twins, Dizygotic genetics

Abstract

Study Question: Does having a male co-twin influence the female twin's reproductive outcomes?, Summary Answer: Women with a male co-twin had the same chances of being pregnant and having children compared to same-sex twin pairs., What Is Known Already: According to the twin testosterone transfer (TTT) hypothesis, in an opposite-sex twin pregnancy, testosterone transfer from the male to the female co-twin occurs. A large body of literature supports the negative impact of prenatal testosterone exposure on female's reproductive health in animal models; however, evidence from human studies remains controversial., Study Design, Size, Duration: This cohort study included all dizygotic female twins in the Aberdeen Maternity and Neonatal Databank (Scotland) born before 1 January 1979. The 317 eligible women were followed up for 40 years for any pregnancies and the outcome of those pregnancies recorded in the same database., Participants/materials, Setting, Methods: Fertility outcomes (number of pregnancies, number of livebirths and age at first pregnancy) were compared between women with a male co-twin (exposed group, n = 151) and those with a female co-twin (unexposed group, n = 166). Population averaged models were used to estimate odds ratios (OR) and 95% CI for all outcomes with adjusting for potential confounders., Main Results and the Role of Chance: There were no differences in chances of having pregnancies (adj. OR 1.33; 95% CI 0.72, 2.45) and livebirths (adj. OR 1.22; 95% CI 0.68, 2.18) between women from same-sex and opposite-sex twin pairs. Women with a male co-twin were more likely to smoke during pregnancy and, in the unadjusted model, were younger at their first pregnancy (OR 2.13; 95% CI 1.21, 3.75). After adjusting for confounding variables (year of birth and smoking status) the latter finding was no longer significant (OR 1.67; 95% CI 0.90, 3.20)., Limitations, Reasons for Caution: The dataset was relatively small. For women without a pregnancy recorded in the databank, we assumed that they had not been pregnant., Wider Implications of the Findings: Despite the evidence from animal studies concerning the adverse effects of prenatal testosterone exposure on female health, our results do not support the TTT hypothesis. The finding that women with a male co-twin are more likely to smoke during pregnancy highlights the importance of considering post-socialisation and social effects in twin studies., Study Funding/competing Interest(s): European Union's Horizon 2020 research and innovation programme under the Marie Skłodowska-Curie project PROTECTED (grant agreement No. 722634) and FREIA project (grant agreement No. 825100). No competing interests., Trial Registration Number: N/A., (© The Author(s) 2020. Published by Oxford University Press on behalf of European Society of Human Reproduction and Embryology.)

Published

2020

40. Safeguarding Female Reproductive Health against Endocrine Disrupting Chemicals-The FREIA Project.

Author

Duursen MBMV, Boberg J, Christiansen S, Connolly L, Damdimopoulou P, Filis P, Fowler PA, Gadella BM, Holte J, Jääger K, Johansson HKL, Li T, Mazaud-Guittot S, Parent AS, Salumets A, Soto AM, Svingen T, Velthut-Meikas A, Wedebye EB, Xie Y, and Berg MVD

Subjects

Animals, Endocrine System drug effects, Environmental Exposure, Environmental Pollutants adverse effects, Female, Humans, Puberty drug effects, Risk Assessment, Risk Factors, Endocrine Disruptors pharmacology, Reproduction drug effects, Reproductive Health

Abstract

Currently available test methods are not well-suited for the identification of chemicals that disturb hormonal processes involved in female reproductive development and function. This renders women's reproductive health at increasing risk globally, which, coupled with increasing incidence rates of reproductive disorders, is of great concern. A woman's reproductive health is largely established during embryonic and fetal development and subsequently matures during puberty. The endocrine system influences development, maturation, and function of the female reproductive system, thereby making appropriate hormone levels imperative for correct functioning of reproductive processes. It is concerning that the effects of human-made chemicals on the endocrine system and female reproductive health are poorly addressed in regulatory chemical safety assessment, partly because adequate test methods are lacking. Our EU-funded project FREIA aims to address this need by increasing understanding of how endocrine disrupting chemicals (EDCs) can impact female reproductive health. We will use this information to provide better test methods that enable fit-for-purpose chemical regulation and then share our knowledge, promote a sustainable society, and improve the reproductive health of women globally.

Published

2020

41. Toward a better understanding of the effects of endocrine disrupting compounds on health: Human-relevant case studies from sheep models.

Author

Viguié C, Chaillou E, Gayrard V, Picard-Hagen N, and Fowler PA

Subjects

Animals, Disease Models, Animal, Endocrine Disruptors pharmacokinetics, Endocrine System drug effects, Endocrine System pathology, Environmental Pollutants toxicity, Humans, Sheep, Endocrine Disruptors toxicity, Health

Abstract

There are many challenges to overcome in order to properly understand both the exposure to, and effects of, endocrine disruptors (EDs). This is particularly true with respect to fetal life where ED exposures are a major issue requiring toxicokinetic studies of materno-fetal exchange and identification of pathophysiological consequences. The sheep, a large, monotocous, species, is very suitable for in utero fetal catheterization allowing a modelling approach predictive of human fetal exposure. Predicting adverse effects of EDs on human health is frequently impeded by the wide interspecies differences in the regulation of endocrine functions and their effects on biological processes. Because of its similarity to humans as regards gestational and thyroid physiologies and brain ontogeny, the sheep constitutes a highly appropriate model to move one step further on thyroid disruptor hazard assessment. As a grazing animal, the sheep has also proven to be useful in the evaluation of the consequences of chronic environmental exposure to "real-life" complex mixtures at different stages of the reproductive life cycle., Competing Interests: Declaration of competing interest None of the authors has competing interests., (Copyright © 2020 Elsevier B.V. All rights reserved.)

Published

2020

42. Calretinin is a novel candidate marker for adverse ovarian effects of early life exposure to mixtures of endocrine disruptors in the rat.

Author

Johansson HKL, Svingen T, Boberg J, Fowler PA, Stead D, Vinggaard AM, and Filis P

Subjects

Androgen Antagonists toxicity, Animals, Benzhydryl Compounds toxicity, Biomarkers metabolism, Calbindin 2 metabolism, Female, Humans, Lactation, Parabens, Phenols toxicity, Pregnancy, Prenatal Exposure Delayed Effects, Rats, Rats, Wistar, Reproduction, Endocrine Disruptors toxicity, Environmental Pollutants toxicity

Abstract

Disruption of sensitive stages of ovary development during fetal and perinatal life can have severe and life-long consequences for a woman's reproductive life. Exposure to endocrine disrupting chemicals may affect ovarian development, leading to subsequent reproductive disorders. Here, we investigated the effect of early life exposure to defined mixtures of human-relevant endocrine disrupting chemicals on the rat ovary. We aimed to identify molecular events involved in pathogenesis of ovarian dysgenesis syndrome that have potential for future adverse outcome pathway development. We therefore focused on the ovarian proteome. Rats were exposed to a mixture of phthalates, pesticides, UV-filters, bisphenol A, butyl-paraben, and paracetamol during gestation and lactation. The chemicals were tested together or in subgroups of chemicals with anti-androgenic or estrogenic potentials at doses 450-times human exposure. Paracetamol was tested separately, at a dose of 360 mg/kg. Using shotgun proteomics on ovaries from pup day 17 offspring, we observed exposure effects on the proteomes. Nine proteins were affected in more than one exposure group and of these, we conclude that calretinin is a potential key event biomarker of early endocrine disruption in the ovary.

Published

2020

43. Fetal androgen exposure is a determinant of adult male metabolic health.

Author

Siemienowicz KJ, Filis P, Shaw S, Douglas A, Thomas J, Mulroy S, Howie F, Fowler PA, Duncan WC, and Rae MT

Subjects

Animals, Female, Inactivation, Metabolic, Liver blood supply, Liver metabolism, Liver pathology, Male, Pregnancy, Sheep metabolism, Testosterone metabolism, Maternal Exposure, Prenatal Exposure Delayed Effects, Sheep embryology, Testosterone administration & dosage

Abstract

Androgen signalling is a critical driver of male development. Fetal steroid signalling can be dysregulated by a range of environmental insults and clinical conditions. We hypothesised that poor adult male health was partially attributable to aberrant androgen exposure during development. Testosterone was directly administered to developing male ovine fetuses to model excess prenatal androgenic overexposure associated with conditions such as polycystic ovary syndrome (PCOS). Such in utero androgen excess recreated the dyslipidaemia and hormonal profile observed in sons of PCOS patients. 1,084 of 15,134 and 408 of 2,766 quantifiable genes and proteins respectively, were altered in the liver during adolescence, attributable to fetal androgen excess. Furthermore, prenatal androgen excess predisposed to adolescent development of an intrahepatic cholestasis-like condition with attendant hypercholesterolaemia and an emergent pro-fibrotic, pro-oxidative stress gene and protein expression profile evident in both liver and circulation. We conclude that prenatal androgen excess is a previously unrecognised determinant of lifelong male metabolic health.

Published

2019

44. Long-term exposure to chemicals in sewage sludge fertilizer alters liver lipid content in females and cancer marker expression in males.

Author

Filis P, Walker N, Robertson L, Eaton-Turner E, Ramona L, Bellingham M, Amezaga MR, Zhang Z, Mandon-Pepin B, Evans NP, Sharpe RM, Cotinot C, Rees WD, O'Shaughnessy P, and Fowler PA

Subjects

Animals, Female, Lipid Metabolism, Liver chemistry, Male, Polychlorinated Biphenyls toxicity, Polycyclic Aromatic Hydrocarbons analysis, Risk Assessment, Sex Factors, Sheep, Biomarkers, Tumor biosynthesis, Environmental Exposure, Environmental Pollutants toxicity, Fertilizers, Liver drug effects, Polycyclic Aromatic Hydrocarbons toxicity, Sewage chemistry

Abstract

Background: The increased incidence of diseases, including metabolic syndrome and infertility, may be related to exposure to the mixture of chemicals, which are ubiquitous in the modern environment (environmental chemicals, ECs). Xeno-detoxification occurs within the liver which is also the source of many plasma proteins and growth factors and plays an important role in the regulation of homeostasis., Objectives: The objective of this study was to investigate the effects of ECs on aspects of liver function, in a well characterized ovine model of exposure to a real-life EC mixture., Methods: Four groups of sheep (n = 10-12/sex/treatment) were maintained long-term on control or sewage sludge-fertilized pastures: from conception to culling at 19 months of age in females and from conception to 7 months of age and thereafter in control plots until culling at 19 months of age in males. Environmental chemicals were measured in sheep livers and RNA and protein extracts were assessed for exposure markers. Liver proteins were resolved using 2D differential in-gel electrophoresis and differentially expressed protein spots were identified by liquid chromatography/tandem mass spectroscopy., Results: Higher levels of polycyclic aromatic hydrocarbons (PAHs) and lower levels of polychlorinated biphenyls (PCBs) in the livers of control males compared to control females indicated sexually dimorphic EC body burdens. Increased levels of the PAHs Benzo[a]anthracene and chrysene and reduced levels of PCB 153 and PCB 180 were observed in the livers of continuously exposed females. EC exposure affected xenobiotic and detoxification responses and the liver proteome in both sexes and included major plasma-secreted and blood proteins, and metabolic enzymes whose pathway analysis predicted dysregulation of cancer-related pathways and altered lipid dynamics. The latter were confirmed by a reduction in total lipids in female livers and up-regulation of cancer-related transcript markers in male livers respectively by sewage sludge exposure., Conclusions: Our results demonstrate that chronic exposure to ECs causes major physiological changes in the liver, likely to affect multiple systems in the body and which may predispose individuals to increased disease risks., (Copyright © 2019 Elsevier Ltd. All rights reserved.)

Published

2019

45. Nutrient transporter expression in both the placenta and fetal liver are affected by maternal smoking.

Author

Walker N, Filis P, O'Shaughnessy PJ, Bellingham M, and Fowler PA

Subjects

Adult, Case-Control Studies, Female, Gene Expression, Gestational Age, Humans, Membrane Transport Proteins metabolism, Pregnancy, Young Adult, Fetus metabolism, Liver metabolism, Membrane Transport Proteins genetics, Nutrients metabolism, Placenta metabolism, Pregnancy Complications genetics, Pregnancy Complications metabolism, Smoking adverse effects, Smoking genetics, Smoking metabolism

Abstract

Introduction: The placenta controls nutrient transfer between mother and fetus via membrane transporters. Appropriate transplacental passage of nutrients is essential for fetal growth and development. We investigated whether transporter transcript levels in human placenta-liver pairs from first and early second trimester pregnancies exhibit gestational age- or fetal sex-specific profiles and whether these are dysregulated by maternal smoking., Methods: In a step-change for the field, paired placenta and fetal livers from 54 electively terminated, normally-progressing pregnancies (7-20 weeks of gestation, Scottish Advanced Fetal Research Study, REC 15/NS/0123) were sexed and cigarette smoking-exposure confirmed. Thirty-six nutrient transporter transcripts were quantified using RT-qPCR., Results: While fetal, liver and placenta weights were not altered by maternal smoking, levels of transporter transcripts changed with fetal age and sex in the placenta and fetal liver and their trajectories were altered if the mother smoked. Placental levels of glucose uptake transporters SLC2A1 and SLC2A3 increased in smoking-exposed fetuses while smoking was associated with altered levels of amino acid and fatty acid transporter genes in both tissues. SLC7A8, which exchanges non-essential amino acids in the fetus for essential amino acids from the placenta, was reduced in smoking-exposed placentas while transcript levels of four hepatic fatty acid uptake transporters were also reduced by smoking., Discussion: This data shows that fetal sex and age and maternal smoking are associated with altered transporter transcript levels. This could influence nutrient transport across the placenta and subsequent uptake by the fetal liver, altering trophic delivery to the growing fetus., (Copyright © 2019 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2019

46. Alternative (backdoor) androgen production and masculinization in the human fetus.

Author

O'Shaughnessy PJ, Antignac JP, Le Bizec B, Morvan ML, Svechnikov K, Söder O, Savchuk I, Monteiro A, Soffientini U, Johnston ZC, Bellingham M, Hough D, Walker N, Filis P, and Fowler PA

Subjects

Dihydrotestosterone blood, Dihydrotestosterone metabolism, Female, Humans, Male, Metabolic Networks and Pathways, Ovary metabolism, Pregnancy, Pregnancy Trimester, Second blood, RNA, Messenger genetics, RNA, Messenger metabolism, Testis metabolism, Androgens biosynthesis, Fetus physiology, Masculinity

Abstract

Masculinization of the external genitalia in humans is dependent on formation of 5α-dihydrotestosterone (DHT) through both the canonical androgenic pathway and an alternative (backdoor) pathway. The fetal testes are essential for canonical androgen production, but little is known about the synthesis of backdoor androgens, despite their known critical role in masculinization. In this study, we have measured plasma and tissue levels of endogenous steroids in second trimester human fetuses using multidimensional and high-resolution mass spectrometry. Results show that androsterone is the principal backdoor androgen in the male fetal circulation and that DHT is undetectable (<1 ng/mL), while in female fetuses, there are significantly lower levels of androsterone and testosterone. In the male, intermediates in the backdoor pathway are found primarily in the placenta and fetal liver, with significant androsterone levels also in the fetal adrenal. Backdoor intermediates, including androsterone, are only present at very low levels in the fetal testes. This is consistent with transcript levels of enzymes involved in the alternate pathway (steroid 5α-reductase type 1 [SRD5A1], aldo-keto reductase type 1C2 [AKR1C2], aldo-keto reductase type 1C4 [AKR1C4], cytochrome P450 17A1 [CYP17A1]), as measured by quantitative PCR (qPCR). These data identify androsterone as the predominant backdoor androgen in the human fetus and show that circulating levels are sex dependent, but also that there is little de novo synthesis in the testis. Instead, the data indicate that placental progesterone acts as substrate for synthesis of backdoor androgens, which occurs across several tissues. Masculinization of the human fetus depends, therefore, on testosterone and androsterone synthesis by both the fetal testes and nongonadal tissues, leading to DHT formation at the genital tubercle. Our findings also provide a solid basis to explain why placental insufficiency is associated with disorders of sex development in humans., Competing Interests: The authors have declared that no competing interests exist.

Published

2019

47. Maternal smoking and high BMI disrupt thyroid gland development.

Author

Filis P, Hombach-Klonisch S, Ayotte P, Nagrath N, Soffientini U, Klonisch T, O'Shaughnessy P, and Fowler PA

Subjects

Adult, Female, Humans, Pregnancy, Body Mass Index, Obesity complications, Smoking adverse effects, Thyroid Gland growth & development

Abstract

Background: Maternal lifestyle factors, including smoking and increased body weight, increase risks of adult diseases such as metabolic syndrome and infertility. The fetal thyroid gland is essential for the control of fetal metabolic rate, cardiac output, and brain development. Altered fetal thyroid function may contribute to increased disease onset later in life. Here, we investigated the impact of maternal smoking and high maternal weight on human fetal thyroid function during the second trimester., Methods: Thyroid glands and plasma were collected from fetuses electively terminated in the second trimester (normally progressing pregnancies). Plasma total triiodothyronine (T3) and total thyroxine (T4) were measured by solid-phase extraction-liquid chromatography-tandem mass spectrometry. Fetal plasma thyroid-stimulating hormone (TSH) levels were measured using a multiplex assay for human pituitary hormones. Histology and immunolocalization of thyroid developmental markers were examined in thyroid sections. Transcript levels of developmental, functional, apoptotic, and detoxification markers were measured by real-time PCR. Statistical analyses were performed using multivariate linear regression models with fetal age, sex, and maternal smoking or maternal body mass index (BMI) as covariates., Results: Maternal smoking was associated with significant changes in fetal plasma T4 and TSH levels during the second trimester. Smoke-exposed thyroids had reduced thyroid GATA6 and NKX2-1 transcript levels and altered developmental trajectories for ESR2 and AHR transcript levels. Maternal BMI > 25 was associated with increased fetal thyroid weight, increased plasma TSH levels, and abnormal thyroid histology in female fetuses. Normal developmental changes in AHR and ESR1 transcript expression were also abolished in fetal thyroids from mothers with BMI > 25., Conclusions: For the first time, we show that maternal smoking and high maternal BMI are associated with disturbed fetal thyroid gland development and endocrine function in a sex-specific manner during the second trimester. These findings suggest that predisposition to post-natal disease is mediated, in part, by altered fetal thyroid gland development.

Published

2018

48. The human fetal adrenal produces cortisol but no detectable aldosterone throughout the second trimester.

Author

Johnston ZC, Bellingham M, Filis P, Soffientini U, Hough D, Bhattacharya S, Simard M, Hammond GL, King P, O'Shaughnessy PJ, and Fowler PA

Subjects

Adult, Aldosterone analysis, Female, Humans, Pregnancy, Pregnancy Trimester, Second, Young Adult, Adrenal Glands metabolism, Aldosterone metabolism, Fetus drug effects

Abstract

Background: Human fetal adrenal glands are highly active and, with the placenta, regulate circulating progesterone, estrogen and corticosteroids in the fetus. At birth the adrenals are essential for neonate salt retention through secretion of aldosterone, while adequate glucocorticoids are required to prevent adrenal insufficiency. The objective of this study was to carry out the first comprehensive analysis of adrenal steroid levels and steroidogenic enzyme expression in normal second trimester human fetuses., Methods: This was an observational study of steroids, messenger RNA transcripts and proteins in adrenals from up to 109 second trimester fetuses (11 weeks to 21 weeks) at the Universities of Aberdeen and Glasgow. The study design was balanced to show effects of maternal smoking., Results: Concentrations of 19 intra-adrenal steroids were quantified using liquid chromatography and mass spectrometry. Pregnenolone was the most abundant steroid while levels of 17α-hydroxyprogesterone, dehydroepiandrosterone sulphate (DHEAS) and progesterone were also high. Cortisol was present in all adrenals, but aldosterone was undetected and Δ 4 androgens were low/undetected. CYP17A1, CYP21A2 and CYP11A1 were all highly expressed and the proteins localized to the adrenal fetal zone. There was low-level expression of HSD3B and CYP11B2, with HSD3B located mainly in the definitive zone. Maternal smoking altered fetal plasma adrenocorticotropic hormone (ACTH) (P = 0.052) and intra-adrenal progesterone, 17α-hydroxyprogesterone and 16α-hydroxyprogesterone, but not plasma or intra-adrenal cortisol, or intra-adrenal DHEAS. Fetal adrenal GATA6 and NR5A1 were increased by maternal smoking., Conclusions: The human fetal adrenal gland produces cortisol but very low levels of Δ 4 androgens and no detectable aldosterone throughout the second trimester. The presence of cortisol in fetal adrenals suggests that adrenal regulation of circulating fetal ACTH remains a factor in development of congenital adrenal hyperplasia during the second trimester, while a relative lack of aldosterone explains the salt-wasting disorders frequently seen in extreme pre-term neonates. Finally, maternal smoking may alter fetal adrenal sensitivity to ACTH, which could have knock-on effects on post-natal health.

Published

2018

49. Identification of Sertoli cell-specific transcripts in the mouse testis and the role of FSH and androgen in the control of Sertoli cell activity.

Author

Soffientini U, Rebourcet D, Abel MH, Lee S, Hamilton G, Fowler PA, Smith LB, and O'Shaughnessy PJ

Subjects

Androgens physiology, Animals, Busulfan pharmacology, Diphtheria Toxin pharmacology, Follicle Stimulating Hormone physiology, Male, Mice, Mice, Knockout, Spermatozoa metabolism, Testis drug effects, Transcriptome drug effects, Receptors, Androgen genetics, Receptors, FSH genetics, Sertoli Cells metabolism, Testis metabolism

Abstract

Background: The Sertoli cells act to induce testis differentiation and subsequent development in fetal and post-natal life which makes them key to an understanding of testis biology. As a major step towards characterisation of factors involved in Sertoli cell function we have identified Sertoli cell-specific transcripts in the mouse testis and have used the data to identify Sertoli cell-specific transcripts altered in mice lacking follicle-stimulating hormone receptors (FSHRKO) and/or androgen receptors (AR) in the Sertoli cells (SCARKO)., Results: Adult iDTR mice were injected with busulfan to ablate the germ cells and 50 days later they were treated with diphtheria toxin (DTX) to ablate the Sertoli cells. RNAseq carried out on testes from control, busulfan-treated and busulfan + DTX-treated mice identified 701 Sertoli-specific transcripts and 4302 germ cell-specific transcripts. This data was mapped against results from microarrays using testicular mRNA from 20 day-old FSHRKO, SCARKO and FSHRKO.SCARKO mice. Results show that of the 534 Sertoli cell-specific transcripts present on the gene chips, 85% were altered in the FSHRKO mice and 94% in the SCARKO mice (mostly reduced in both cases). In the FSHRKO.SCARKO mice additive or synergistic effects were seen for most transcripts. Age-dependent studies on a selected number of Sertoli cell-specific transcripts, showed that the marked effects in the FSHRKO at 20 days had largely disappeared by adulthood although synergistic effects of FSHR and AR knockout were seen., Conclusions: These studies have identified the Sertoli cell-specific transcriptome in the mouse testis and have shown that most genes in the transcriptome are FSH- and androgen-dependent at puberty although the importance of FSH diminishes towards adulthood.

Published

2017

50. Erratum to: Modelling foetal exposure to maternal smoking using hepatoblasts from pluripotent stem cells.

Author

Lucendo-Villarin B, Filis P, Swortwood MJ, Huestis MA, Meseguer-Ripolles J, Cameron K, Iredale JP, O'Shaughnessy PJ, Fowler PA, and Hay DC

Abstract

During manuscript proofing, the following sentence was not deleted in the section "Results" at the end of the paragraph: "Both male and female hepatocytes responded in a similar fashion to cotinine, whereas male hepatocyte function was more sensitive to chrysene, fluorene and naphthalene than female hepatocytes".

Published

2017