Your search keyword '"Richard M. Sharpe"' showing total 7 results

1. Effect of fetal or neonatal exposure to monobutyl phthalate (MBP) on testicular development and function in the marmoset

Author

Richard M. Sharpe, Marion F Walker, Chris Kelnar, Chris McKinnell, Rod T. Mitchell, Keith Morris, and W. Hamish B. Wallace

Subjects

Male, germ cells, endocrine system, medicine.medical_specialty, Offspring, Phthalic Acids, Reproductive biology, testis, Testicle, neonatal, Pregnancy, Internal medicine, biology.animal, Obstetrics and Gynaecology, medicine, Animals, Testosterone, monobutyl phthalate, Fetus, Sertoli Cells, biology, Rehabilitation, Obstetrics and Gynecology, Marmoset, Callithrix, Original Articles, fetal, Sertoli cell, Endocrinology, medicine.anatomical_structure, Animals, Newborn, Reproductive Medicine, Maternal Exposure, Prenatal Exposure Delayed Effects, Gestation, Female, Germ cell

Abstract

BACKGROUND Fetal exposure of male rats to some phthalates induces reproductive abnormalities, raising concerns for similar effects in humans. In order to address this in a more appropriate animal model, the aim of the present studies was to investigate the effect of fetal/neonatal exposure to monobutyl phthalate (MBP) in a non-human primate, the marmoset. In particular, to determine if exposure resulted in effects at birth, or in adulthood, similar to those in male rats, and whether there was evidence for induction of carcinoma-in-situ (CIS) or testicular germ cell tumours (TGCT).METHODS Pregnant female marmosets were dosed from ∼7–15 weeks gestation with 500 mg/kg/day MBP and male offspring studied at birth (1–5 days; n = 6) or in adulthood (n = 5). In another study, newborn males (n = 5 co-twins) were dosed with 500 mg/kg/day MBP for 14 days, commencing at ∼4 days of age.RESULTS Fetal exposure of marmosets to MBP did not affect gross testicular morphology, reproductive tract development or testosterone levels at birth, nor were germ cell number and proliferation, Sertoli cell number or germ:Sertoli cell ratio affected. In two of six MBP-exposed animals, unusual clusters of undifferentiated germ cells were found, but their significance is unclear. Neonatal MBP treatment did not affect germ cell numbers or differentiation. Fetal exposure to MBP did not affect testis size/morphology, germ cell numbers or fertility in adulthood. There was no evidence for CIS or TGCT.CONCLUSIONS Fetal exposure of marmosets to MBP does not measurably affect testis development/function or cause testicular dysgenesis, and no effects emerge by adulthood. Some effects on germ cell development were found, but these were inconsistent and of uncertain significance.

Published

2009

2. Germ cell differentiation in the marmoset (Callithrix jacchus) during fetal and neonatal life closely parallels that in the human

Author

H.M. Fraser, Gillian Cowan, K.J. Mckenzie, Philippa T. K. Saunders, Keith Morris, Richard A. Anderson, William Wallace, Rod T. Mitchell, Richard M. Sharpe, and C.J.H. Kelnar

Subjects

Male, Homeobox protein NANOG, germ cells, endocrine system, medicine.medical_specialty, animal diseases, Cellular differentiation, testis, common marmoset, DEAD-box RNA Helicases, Andrology, Gonocyte, Germ cell proliferation, biology.animal, Internal medicine, Obstetrics and Gynaecology, medicine, Animals, Humans, Cell Proliferation, Homeodomain Proteins, Reproductive Biology, biology, Rehabilitation, RNA-Binding Proteins, carcinoma in situ, Obstetrics and Gynecology, Marmoset, Callithrix, Cell Differentiation, Nanog Homeobox Protein, Original Articles, biology.organism_classification, Spermatogonia, Rats, Endocrinology, medicine.anatomical_structure, Animals, Newborn, Transcription Factor AP-2, Reproductive Medicine, Models, Animal, Germ line development, Octamer Transcription Factor-3, Germ cell

Abstract

BACKGROUND: Testicular germ cell tumours (TGCT) are thought to originate from fetal germ cells that fail to differentiate normally, but no animal model for these events has been described. We evaluated the marmoset (Callithrix jacchus) as a model by comparing perinatal germ cell differentiation with that in humans. METHODS: Immunohistochemical profiling was used to investigate germ cell differentiation (OCT4, NANOG, AP-2g ,M AGE-A4, VASA, NANOS-1) and proliferation (Ki67) in fetal and neonatal marmoset testes in comparison with the human and, to a lesser extent, the rat. RESULTS: In marmosets and humans, differentiation of gonocytes into spermatogonia is associated with the gradual loss of pluripotency markers such as OCT4 and NANOG, and the expression of germ cell-specific proteins such as VASA. This differentiation occurs asynchronously within individual cords during fetal and early postnatal life. This contrasts with rapid and synchronous germ cell differentiation within and between cords in the rat. Similarly, germ cell proliferation in the marmoset and human occurs throughout perinatal life, in contrast to rats in which proliferation ceases during this period. CONCLUSIONS: The marmoset provides a good model for normal human germ cell differentiation and proliferation. The perinatal marmoset may be a useful model in which to establish factors that lead to failure of normal germ cell differentiation and the origins of TGCT.

Published

2008

3. Infant feeding with soy formula milk: effects on puberty progression, reproductive function and testicular cell numbers in marmoset monkeys in adulthood

Author

Keith Morris, Irene Greig, J. Ian Mason, Richard M. Sharpe, Marion F Walker, and Karen A. L. Tan

Subjects

Male, Pituitary gland, medicine.medical_specialty, medicine.drug_class, Biology, Testicle, Internal medicine, biology.animal, Testis, medicine, Animals, Testosterone, Leydig cell, Body Weight, Rehabilitation, Obstetrics and Gynecology, Marmoset, Callithrix, Organ Size, Sertoli cell, Androgen, Infant Formula, Soy Milk, Fertility, medicine.anatomical_structure, Endocrinology, Reproductive Medicine, Germ cell

Abstract

Background This marmoset study addresses concerns about feeding human male infants with soy formula milk (SFM). Methods From age 4 to 5 days, seven male co-twin sets were fed standard formula milk (SMA) or SFM for 5-6 weeks; blood samples were subsequently collected at 10-week intervals. Testes from co-twins killed at 120-138 weeks were fixed for cell counts. Results SFM- and SMA-fed twins showed normal weight gain; puberty started and progressed normally, based on blood testosterone measurements. Body weight, organ weights (prostate, seminal vesicles, pituitary, thymus and spleen) and penis length were comparable in co-twins. All SMA- and 6/7 SFM-fed males were fertile. Unexpectedly, testis weight (P = 0.041), Sertoli (P = 0.025) and Leydig cell (P = 0.026) numbers per testis were consistently increased in SFM-fed co-twins; the increase in Leydig cell numbers was most marked in males with consistently low-normal testosterone levels. Seminiferous epithelium volume per tubule showed a less consistent, non-significant increase in SFM-fed males; raised germ cell numbers per testis, probably due to increased Sertoli cells, conceivably resulted in larger testes. Average lumen size, although greater in SFM-fed group, was inconsistent between co-twins and the difference was not significant. Conclusions Infant feeding with SFM has no gross adverse reproductive effects in male marmosets, though it alters testis size and cell composition, and there is consistent, if indirect, evidence for possible 'compensated Leydig cell failure'. Similar and perhaps larger changes likely occur in adult men who were fed SFM as infants.

Published

2006

4. Role of the neonatal period of pituitary-testicular activity in germ cell proliferation and differentiation in the primate testis

Author

K D Morris, Mark F. H. Brougham, Hamish M. Fraser, C.J.H. Kelnar, Chris McKinnell, William Wallace, Marion F Walker, and Richard M. Sharpe

Subjects

Male, endocrine system, Pituitary gland, medicine.medical_specialty, medicine.drug_class, Twins, Gonadotropin-releasing hormone, Gonadotropin-releasing hormone antagonist, Gonadotropin-Releasing Hormone, Gonocyte, Germ cell proliferation, biology.animal, Internal medicine, Testis, medicine, Animals, Cellular Senescence, biology, Rehabilitation, Obstetrics and Gynecology, Marmoset, Callithrix, Cell Differentiation, Sertoli cell, Spermatozoa, Spermatogonia, medicine.anatomical_structure, Endocrinology, Animals, Newborn, Reproductive Medicine, Pituitary Gland, Cell Division, Germ cell

Abstract

BACKGROUND: The neonatal period of pituitary‐testicular activity (NPTA) in human males has been hypothesized to play a role in germ cell proliferation and differentiation and to be defective in cryptorchid testes. The present study was carried out to establish in the marmoset if suppression of the NPTA, by treatment with a GnRH antagonist, results in impaired germ cell proliferation and/or differentiation. METHODS: Comparison of germ cell (GC) numbers and differentiation from gonocytes to pre-spermatogonia and spermatogonia, at birth (in controls) and at the end of the NPTA in marmoset co-twin males treated from birth to age 14 weeks with vehicle or GnRH antagonist. RESULTS: From birth to age 18‐24 weeks, testis weight increased ~5-fold and GC number ~10-fold, including increased numbers of gonocytes and pre-spermatogonia and the first appearance of spermatogonia. Treatment with GnRH antagonist attenuated the increase in testis weight and GC numbers, but the effect was only partial (24‐30% reduction), and the relative proportions of gonocytes, pre-spermatogonia and spermatogonia in the GnRH antagonist-treated group were unchanged from control values. CONCLUSIONS: The NPTA plays only a minor, if any, role in GC proliferation and differentiation in the marmoset. The changes in GnRH antagonist-treated co-twins may reflect impaired GC survival due to withdrawal of gonadotrophin support for Sertoli cells. These findings do not support a pivotal role for the NPTA in neonatal GC development in primates.

Published

2003

5. Bisphenol A exposure and sexual dysfunction in men: Editorial commentary on the article 'Occupational exposure to bisphenol-A (BPA) and the risk of self-reported male sexual dysfunction' Li et al., 2009

Author

Richard M. Sharpe

Subjects

medicine.medical_specialty, Bisphenol A, business.industry, media_common.quotation_subject, Rehabilitation, Obstetrics and Gynecology, Toxicology, chemistry.chemical_compound, Sexual dysfunction, Reproductive Medicine, chemistry, Adverse health effect, medicine, Male sexual dysfunction, Occupational exposure, medicine.symptom, Worry, Cancer Induction, Psychiatry, business, media_common

Abstract

There is a long, ongoing controversy about the potential health effects of bisphenol A in humans (Bucher et al., 2009 ). There are two, diametrically opposed views. One side argues vociferously, based on animal experiments, that bisphenol A may exert numerous adverse effects in humans, ranging from reproductive development disorders through obesity effects to cancer induction/progression. The other side argues, also based on animal experiments, that bisphenol A poses no significant health risks to humans. This stand-off is not simply about ‘scientists squabbling about who is right or wrong’, as there are similar differences in reaction between authorities, as Canada and some US states have chosen to ban use of bisphenol A in baby feeding bottles, whereas others (e.g. EU) have said there is nothing for consumers to worry about. What is not disputed is that we are all exposed daily to bisphenol A (Calafat et al., 2008 ); our exposure is mainly via bisphenol A that has leached into food from containers (Kang et al., 2006 ), as it is used in the making of (heat-resistant) polycarbonate plastics that are used widely as containers for food and beverages as well as in tin-can linings. As with all ‘environmental’ chemicals, the question is whether our exposure is sufficient to cause adverse health effects. Based on the same evidence, different scientists and different authorities appear to have deciphered a very different answer to this question (Bucher et al., 2009 ), so the noninvolved outsider has every reason to be confused.

Published

2009

6. Session 60: Female fertility 2

Author

Helen Louise McFerran, Phillip Cash, Richard M. Sharpe, K.d. Miller, Stewart M. Rhind, Natalie Dora, Alan S. McNeilly, Richard G. Lea, and Paul Fowler

Subjects

Fetus, medicine.anatomical_structure, Reproductive Medicine, business.industry, Dietary exposure, Rehabilitation, Obstetrics and Gynecology, Medicine, Physiology, Ovary, business

Published

2007

7. Infant feeding with soy formula milk: effects on puberty progression, reproductive function and testicular cell numbers in marmoset monkeys in adulthood.

Author

Karen A.L. Tan, Marion Walker, Keith Morris, Irene Greig, J. Ian Mason, and Richard M. Sharpe

Subjects

SOYMILK, INFANT formulas, TESTIS, MALE reproductive organs

Abstract

BACKGROUND: This marmoset study addresses concerns about feeding human male infants with soy formula milk (SFM). METHODS: From age 4 to 5 days, seven male co-twin sets were fed standard formula milk (SMA) or SFM for 5–6 weeks; blood samples were subsequently collected at 10-week intervals. Testes from co-twins killed at 120–138 weeks were fixed for cell counts. RESULTS: SFM- and SMA-fed twins showed normal weight gain; puberty started and progressed normally, based on blood testosterone measurements. Body weight, organ weights (prostate, seminal vesicles, pituitary, thymus and spleen) and penis length were comparable in co-twins. All SMA- and 6/7 SFM-fed males were fertile. Unexpectedly, testis weight (P = 0.041), Sertoli (P = 0.025) and Leydig cell (P = 0.026) numbers per testis were consistently increased in SFM-fed co-twins; the increase in Leydig cell numbers was most marked in males with consistently low-normal testosterone levels. Seminiferous epithelium volume per tubule showed a less consistent, non-significant increase in SFM-fed males; raised germ cell numbers per testis, probably due to increased Sertoli cells, conceivably resulted in larger testes. Average lumen size, although greater in SFM-fed group, was inconsistent between co-twins and the difference was not significant. CONCLUSIONS: Infant feeding with SFM has no gross adverse reproductive effects in male marmosets, though it alters testis size and cell composition, and there is consistent, if indirect, evidence for possible ‘compensated Leydig cell failure’. Similar and perhaps larger changes likely occur in adult men who were fed SFM as infants. [ABSTRACT FROM AUTHOR]

Published

2006