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1. Editor's Note

Author

Scialli Ar

Subjects
medicine.medical_specialty, business.industry, Family medicine, Alternative medicine, Medicine, Toxicology, business, Medical literature
Published
1999

4. Effectiveness of a low-fat vegetarian diet in altering serum lipids in healthy premenopausal women.

Author

Barnard ND, Scialli AR, Bertron P, Hurlock D, Edmonds K, Talev L, Barnard, N D, Scialli, A R, Bertron, P, Hurlock, D, Edmonds, K, and Talev, L

Abstract

Few controlled trials have studied cholesterol-lowering diets in premenopausal women. None has examined the cholesterol-lowering effect of a low-fat vegetarian diet, which, in other population groups, leads to marked reductions in serum cholesterol concentrations and, in combination with other life-style changes, a regression of atherosclerosis. We tested the hypothesis that a low-fat, vegetarian diet significantly reduces serum total and low-density lipoprotein (LDL) cholesterol concentrations in premenopausal women. In a crossover design, 35 women, aged 22 to 48, followed a low-fat vegetarian diet deriving approximately 10% of energy from fat for 2 menstrual cycles. For 2 additional cycles, they followed their customary diet while also taking a "supplement" (placebo) pill. Serum lipid concentrations were assessed at baseline and during each intervention phase. Mean serum LDL, high-density lipoprotein (HDL), and total cholesterol concentrations decreased 16. 9%, 16.5%, and 13.2%, respectively, from baseline to the intervention diet phase (p<0.001), whereas mean serum triacylglycerol concentration increased 18.7% (p<0.01). LDL/HDL ratio remained unchanged. Thus, in healthy premenopausal women, a low-fat vegetarian diet led to rapid and sizable reductions in serum total, LDL, and HDL cholesterol concentrations. [ABSTRACT FROM AUTHOR]

Published
2000
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7. Pregnancy Outcomes in Patients Treated with Upadacitinib: Analysis of Data from Clinical Trials and Postmarketing Reports.

Author

Mahadevan U, Levy G, Gensler L, Ali M, Lacerda AP, Wegrzyn L, Palac H, Bhutani-Jacques T, Long M, Clowse MEB, Kimball AB, Chambers C, and Scialli AR

Subjects
Humans, Pregnancy, Female, Adult, Clinical Trials as Topic, Retrospective Studies, Pregnancy Complications drug therapy, Young Adult, Abnormalities, Drug-Induced epidemiology, Pregnancy Outcome epidemiology, Product Surveillance, Postmarketing, Heterocyclic Compounds, 3-Ring adverse effects, Heterocyclic Compounds, 3-Ring therapeutic use
Abstract

Background and Objective: Upadacitinib is indicated for diseases affecting persons of childbearing potential including rheumatoid arthritis, psoriatic arthritis, axial spondyloarthritis, atopic dermatitis, Crohn's disease, and ulcerative colitis; however, teratogenicity was observed in animal studies. Given the potential for human fetal risk, pregnancy avoidance measures were required during clinical trials. This analysis describes pregnancy outcomes in patients exposed to upadacitinib during pregnancy., Methods: Clinical trial and postmarketing cases of in utero exposure to upadacitinib were identified in AbbVie's safety database through 25 April, 2023. Analysis of clinical trial cases and postmarketing reports are presented separately; prospective and retrospectively reported pregnancy outcomes are integrated for each. Descriptive rates are presented to summarize outcomes., Results: There were 128 maternal upadacitinib-exposed pregnancies with known outcomes identified; 80 and 48 pregnancies were reported in clinical trials and the postmarketing setting, respectively. In clinical trials (mean in utero exposure of 5 weeks, 3 days), live births (54%), spontaneous abortions (24%), elective terminations (21%), and ectopic pregnancy (1%) were reported. There was one report of a congenital malformation: a 35-week infant with an atrial septal defect. In postmarketing cases, live births (46%), spontaneous abortions (38%), elective terminations (15%), and ectopic pregnancy (2%) were reported., Conclusions: As the data are limited for in utero exposure to upadacitinib, definitive conclusions cannot be drawn regarding the effect of upadacitinib on pregnancy outcomes. Rates of adverse pregnancy outcomes with upadacitinib exposure were comparable to rates observed in the general population or patients with autoimmune inflammatory diseases. To date, no apparent evidence of teratogenicity exists in the analyses of human pregnancies exposed to upadacitinib during the first trimester., (© 2024. The Author(s).)

Published
2024
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8. Paternal Valproate Treatment and Risk of Childhood Neurodevelopmental Disorders: Precautionary Regulatory Measures Are Insufficiently Substantiated.

Author

Garey JD, Damkier P, Scialli AR, Lusskin S, Braddock SR, Chouchana L, Cleary B, Conover EA, Diav-Citrin O, Dragovich RS, Garcia-Bournissen F, Hodson K, Kennedy D, Lamm SH, Lavigne SA, Običan SG, Panchaud A, Perrotta K, Romeo AN, Shechtman S, and Weber-Schoendorfer C

Subjects
Humans, Male, Child, Epilepsy drug therapy, United Kingdom, Anticonvulsants adverse effects, Anticonvulsants therapeutic use, Female, Valproic Acid adverse effects, Neurodevelopmental Disorders prevention & control, Neurodevelopmental Disorders chemically induced
Abstract

On January 12, 2024 the safety committee of the European Medicines Agency (EMA) recommended precautionary measures over a potential risk of neurodevelopmental disorders in children born to men treated with valproate. These new measures recommend patient supervision by a specialist in the management of epilepsy, bipolar disorder, or migraine. In the United Kingdom, the Medicines and Healthcare products Regulatory Agency (MHRA) issued a far more stringent precaution, warning against prescribing valproate to anyone under 55 years of age. We, members of the European Network of Teratology Information Services (ENTIS) and the Organization of Teratology Information Specialists (OTIS), believe that the EMA and MHRA warnings were premature. We are of the opinion that the underlying scientific data do not convincingly substantiate the inference of a paternally mediated risk from valproate to children, much less to an extent that justifies these far-reaching recommendations., (© 2024 Wiley Periodicals LLC.)

Published
2024
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9. Decamethylcyclopentasiloxane developmental neurotoxicity testing.

Author

Scialli AR

Subjects
Humans, Toxicity Tests, Neurotoxicity Syndromes etiology, Teratology, Toxicology, Siloxanes
Abstract

Competing Interests: Declaration of Competing Interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: Anthony Scialli reports financial support was provided by American Chemistry Council Silicones Environmental Health and Safety Center. Anthony Scialli reports a relationship with American Chemistry Council Silicones Environmental Health and Safety Center that includes: consulting or advisory.

Published
2024
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10. The COVID-19 Vaccines International Pregnancy Exposure Registry (C-VIPER): Protocol and Methodological Considerations.

Author

Wyszynski DF, Bhattacharya M, Martínez-Pérez O, Scialli AR, Tassinari M, Bar-Zeev N, Renz C, and Hernández-Díaz S

Subjects
Pregnancy, Female, Infant, Newborn, Humans, COVID-19 Vaccines adverse effects, Prospective Studies, Treatment Outcome, COVID-19 epidemiology, COVID-19 prevention & control, Vaccines
Abstract

Introduction: The advent of the coronavirus disease 2019 (COVID-19) pandemic has led to the development of vaccines against severe acute respiratory syndrome coronavirus 2. Prospective evidence regarding safety for pregnant people and their developing fetuses is lacking. The aim of the COVID-19 Vaccines International Pregnancy Exposure Registry (C-VIPER) is to estimate the relative risk of obstetric, neonatal, and infant outcomes by comparing participants vaccinated against COVID-19 during pregnancy to a reference group of people enrolled in the Pregistry International Pregnancy Exposure Registry (PIPER) who remained unvaccinated during pregnancy., Methods: The C-VIPER and the PIPER are international, non-interventional, real-world cohort studies. Participants receiving a COVID-19 vaccine during pregnancy will be matched in the analyses by country and gestational age at enrollment to unvaccinated individuals. Self-enrolled and self-consented participants complete online questionnaires at enrollment, during pregnancy, and for 12 months after the delivery of a live infant. Where possible, outcomes are verified by medical records. The study aims to recruit at least 500 pregnancies for each approved or authorized vaccine and will last for 5 years for each product., Conclusions: By collecting data for each vaccine brand, the C-VIPER will be able to determine individual safety profiles. The study design allows for analysis of the effects of exposure to COVID-19 vaccines during specific etiologically relevant periods of gestation. Although the sample size may be too small to detect associations with rare outcomes, the study will be used to generate hypotheses for future research. Ultimately, the C-VIPER should provide data that will allow pregnant people and their healthcare providers to make informed decisions about COVID-19 vaccination., Clinical Trial Registration: ClinicalTrials.gov NCT04705116. Registered on 12 January, 2021. EU PAS EUPAS39096. Registered on 20 January, 2021., (© 2023. The Author(s), under exclusive licence to Springer Nature Switzerland AG.)

Published
2023
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13. Systematic assessment of quaternary ammonium compounds for the potential to elicit developmental and reproductive effects.

Author

DeSesso JM, Harris SB, Scialli AR, and Williams AL

Subjects
Animals, Benzalkonium Compounds, Fertility, Mice, Rabbits, Rats, Reproduction, Disinfectants toxicity, Quaternary Ammonium Compounds toxicity
Abstract

Introduction: Quaternary ammonium compounds (QUATs) are commonly found in cleaning products, disinfectants, hand sanitizers, and personal care products. They have been used for >50 years and are considered safe when used according to directions. Recent papers report reduced fertility and neural tube defects in rodents after low-level exposures. To determine if QUATs interfere with mammalian reproduction and development, we conducted a methodical assessment of all available data., Methods: A systematic literature search identified 789 potential articles. Review of titles and abstracts found eight relevant studies, including two dissertation chapters; to these, 10 unpublished, guideline-compliant developmental and reproductive toxicity (DART) studies of QUATs (alkyldimethylbenzylammonium chloride [ADBAC] and dialkyldimethylammonium chloride [DDAC]) were added. ToxRTool was utilized to evaluate all 18 studies for data quality., Results: Six studies were scored as "reliable without restriction"; four studies were considered "reliable with restriction" (mainly due to small rabbit group sizes). No test article-related, adverse DART endpoints were reported in these studies. ToxRTool scored the remaining eight studies as "not reliable." The unreliable studies failed to fully describe methods and/or endpoints, did not quantify (and in some cases, did not verify) exposures, utilized non-standard test methods, reported endpoints incorrectly, and assessed endpoints at inappropriate times. Some (not all) unreliable studies reported adverse effects after 7.5 mg QUATs/kg/day (mice), but these results were inconsistent. The reliable studies tested exposures ≥100 mg/kg/day (rats) with no effects., Conclusions: The available weight of evidence indicates no adverse DART effects after QUATs exposures at anticipated concentrations and normal use., (© 2021 The Authors. Birth Defects Research published by Wiley Periodicals LLC.)

Published
2021
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14. Teratogen update: Amphetamines.

Author

Garey JD, Lusskin SI, and Scialli AR

Subjects
Amphetamines toxicity, Animals, Female, Pregnancy, Teratogens toxicity, Attention Deficit Disorder with Hyperactivity chemically induced, Attention Deficit Disorder with Hyperactivity drug therapy, Central Nervous System Stimulants toxicity, Drug-Related Side Effects and Adverse Reactions
Abstract

Amphetamines are synthetic noncatecholamine sympathomimetic amines that act as psychostimulants. They have been prescribed for the treatment of attention-deficit/hyperactivity disorder (ADHD), narcolepsy, and additional health conditions. Amphetamines are also drugs of abuse. Some experimental animal studies suggested adverse developmental effects of amphetamines, including structural malformations. These effects were most often observed in experimental animals at higher dose levels than those used for treatment or abuse and at dose levels that produce maternal toxicity. Controlled studies of amphetamine use for the treatment of ADHD and other indications did not suggest that amphetamines are likely to cause structural malformations, although there are three studies associating medication for ADHD or methamphetamine abuse with gastroschisis. We did not locate studies on the neurobehavioral effects of prenatal exposures to therapeutic amphetamine use. Amphetamine abuse was associated with offspring neurobehavioral abnormalities, but lack of adequate adjustment for confounding interferes with interpretation of the associations. Adverse effects of methamphetamine abuse during pregnancy may be due to factors associated with drug abuse rather than methamphetamine itself. The adverse effects observed in methamphetamine abuse studies may not be extrapolatable to amphetamine medication use., (© 2020 Wiley Periodicals LLC.)

Published
2020
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15. Teratogen?

Author

Scialli AR

Subjects
Caspases, Humans, Abnormalities, Drug-Induced, Teratogens toxicity
Published
2020
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18. Bone development in laboratory mammals used in developmental toxicity studies.

Author

DeSesso JM and Scialli AR

Subjects
Animals, Bone Development drug effects, Disease Models, Animal, Drug-Related Side Effects and Adverse Reactions, Embryonic Development drug effects, Fetus, Humans, Mammals, Organogenesis, Primates anatomy & histology, Rabbits anatomy & histology, Rodentia anatomy & histology, Skeleton diagnostic imaging, Skeleton drug effects, Bone Development physiology, Bone and Bones drug effects, Embryology methods
Abstract

Evaluation of the skeleton in laboratory animals is a standard component of developmental toxicology testing. Standard methods of performing the evaluation have been established, and modification of the evaluation using imaging technologies is under development. The embryology of the rodent, rabbit, and primate skeleton has been characterized in detail and summarized herein. The rich literature on variations and malformations in skeletal development that can occur in the offspring of normal animals and animals exposed to test articles in toxicology studies is reviewed. These perturbations of skeletal development include ossification delays, alterations in number, shape, and size of ossification centers, and alterations in numbers of ribs and vertebrae. Because the skeleton is undergoing developmental changes at the time fetuses are evaluated in most study designs, transient delays in development can produce apparent findings of abnormal skeletal structure. The determination of whether a finding represents a permanent change in embryo development with adverse consequences for the organism is important in study interpretation. Knowledge of embryological processes and schedules can assist in interpretation of skeletal findings., (© 2018 The Authors. Birth Defects Research Published by Wiley Periodicals, Inc.)

Published
2018
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19. Rethinking developmental toxicity testing: Evolution or revolution?

Author

Scialli AR, Daston G, Chen C, Coder PS, Euling SY, Foreman J, Hoberman AM, Hui J, Knudsen T, Makris SL, Morford L, Piersma AH, Stanislaus D, and Thompson KE

Subjects
Animals, Female, Humans, Pregnancy, Risk Assessment, Embryonic Development physiology, Fetal Development physiology, Toxicity Tests methods
Abstract

Background: Current developmental toxicity testing adheres largely to protocols suggested in 1966 involving the administration of test compound to pregnant laboratory animals. After more than 50 years of embryo-fetal development testing, are we ready to consider a different approach to human developmental toxicity testing?, Methods: A workshop was held under the auspices of the Developmental and Reproductive Toxicology Technical Committee of the ILSI Health and Environmental Sciences Institute to consider how we might design developmental toxicity testing if we started over with 21st century knowledge and techniques (revolution). We first consider what changes to the current protocols might be recommended to make them more predictive for human risk (evolution)., Results: The evolutionary approach includes modifications of existing protocols and can include humanized models, disease models, more accurate assessment and testing of metabolites, and informed approaches to dose selection. The revolution could start with hypothesis-driven testing where we take what we know about a compound or close analog and answer specific questions using targeted experimental techniques rather than a one-protocol-fits-all approach. Central to the idea of hypothesis-driven testing is the concept that testing can be done at the level of mode of action. It might be feasible to identify a small number of key events at a molecular or cellular level that predict an adverse outcome and for which testing could be performed in vitro or in silico or, rarely, using limited in vivo models. Techniques for evaluating these key events exist today or are in development., Discussion: Opportunities exist for refining and then replacing current developmental toxicity testing protocols using techniques that have already been developed or are within reach., (© 2018 The Authors. Birth Defects Research Published by Wiley Periodicals, Inc.)

Published
2018
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20. Predictivity of Nonclinical Male Reproductive Findings for Human Effects.

Author

Scialli AR, Clark RV, and Chapin RE

Subjects
Animals, Drug-Related Side Effects and Adverse Reactions etiology, Humans, Male, Models, Animal, Reproducibility of Results, Genitalia, Male drug effects, Predictive Value of Tests, Reproduction drug effects
Abstract

Background: Testing of pharmaceutical products for reproductive toxicity in male laboratory animals is required for registration., Methods: We evaluated whether the results of studies showing male reproductive toxicity in experimental animals was predictive of reproductive effects in men participating in clinical trials. We surveyed companies for information on pharmaceutical candidates that had shown male reproductive toxicity in nonclinical studies for which there was information on male reproductive effects in clinical trials., Results: Among 12 pharmaceutical candidates submitted by five companies, only one compound that had shown male reproductive toxicity in experimental animals also demonstrated reproductive toxicity in men., Conclusion: In this sample of compounds, nonclinical studies appeared to over-predict reproductive toxicity in men. We identified possible reasons for the apparent lack of predictivity of the experimental animal studies. Birth Defects Research 110:17-26, 2018. © 2017 Wiley Periodicals, Inc., (© 2017 Wiley Periodicals, Inc.)

Published
2018
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21. Testosterone and sexual function.

Author

Fugh-Berman A and Scialli AR

Subjects
Aged, Cardiovascular Diseases, Humans, Hypogonadism, Male, Treatment Outcome, Aging physiology, Erectile Dysfunction drug therapy, Randomized Controlled Trials as Topic, Sexual Dysfunction, Physiological drug therapy, Testosterone therapeutic use
Abstract

Purpose of Review: Testosterone therapy has been advocated in the treatment of symptoms that may represent normal aging. We briefly review randomized clinical trials on the effects of testosterone therapy on sexual function., Recent Findings: About half of clinical trials showed no benefit of testosterone therapy on any aspect of sexual function. In those studies showing a benefit on some aspect of sexual function, most sexual function domains were not improved. Testosterone therapy has been disappointing in the treatment of erectile dysfunction. Potential risks of therapy include an increase in thromboembolic and other cardiovascular diseases., Summary: The limited and inconsistent benefits of testosterone therapy for sexual function argue against use of this therapy in aging men, including those with 'low testosterone'.

Published
2017
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22. A quantitative weight of evidence assessment of confidence in modes-of-action and their human relevance.

Author

Dekant W, Bridges J, and Scialli AR

Subjects
Animals, Area Under Curve, Humans, Species Specificity, Drug-Related Side Effects and Adverse Reactions, Models, Animal, Pharmacological Phenomena, Toxicity Tests methods
Abstract

A quantitative weight of evidence (QWoE) methodology was developed to assess confidence in postulated mode(s) of action for adverse effects in animal toxicity studies. The QWoE is appropriate for assessing adverse effects as relevant endpoints for classification and labeling purposes. The methodology involves definition of mode of actions and scoring supporting data for all key steps using predefined criteria for quality and relevance/strength of effects. Scores for all key steps are summarized, and the summary score is compared to the maximal achievable score for the mode of action. The ratio of the summary score to the maximal achievable scores gives an indication of confidence in a specific mode of action in animals. The mode of action in animals with highest confidence is then taken forward to assess appropriateness to humans. If one of the key steps cannot occur in humans, the mode of action is not relevant to humans. The methodology developed is applied to four case studies., (Copyright © 2017. Published by Elsevier Inc.)

Published
2017
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23. Biological relevance of effects following chronic administration of octamethylcyclotetrasiloxane (D4) in Fischer 344 rats.

Author

Dekant W, Scialli AR, Plotzke K, and Klaunig JE

Subjects
Administration, Inhalation, Animals, Drug Administration Schedule, Estrous Cycle drug effects, Female, Liver anatomy & histology, Organ Size, Rats, Rats, Inbred F344, Siloxanes administration & dosage, Siloxanes chemistry, Siloxanes pharmacokinetics, Endometrial Neoplasms chemically induced, Liver drug effects, Siloxanes toxicity
Abstract

Octamethylcyclotetrasiloxane (D4) is a cyclic siloxane primarily used as a monomer or intermediate in the production of silicone polymers resulting in potential exposure of workers, and potential low level inhalation or dermal exposure for consumers and the general public. Following a two-year inhalation toxicity study with D4 in rats, increases in uterine endometrial cystic hyperplasia and adenomas were observed at the highest concentration of D4 administered (700ppm). No other neoplasms were increased with D4 treatment. In addition, chronic inhalation exposure of rats to D4 induced changes in relative liver and kidney weights, and produced a chronic nephropathy. This manuscript examines the biological relevance and possible modes of action for the effects observed in the F344 rat following chronic inhalation exposure to D4. D4 is not genotoxic and appears to exert its effects through a nongenotoxic mode of action. An alteration in the estrous cycle in the aging F344 rat was the most likely mode of action for the observed uterine effects following chronic inhalation exposure. Data support the conclusion that D4 acts indirectly via a dopamine-like mechanism leading to alteration of the pituitary control of the estrous cycle in aging F344 rats with a decrease in progesterone and an increase in the estrogen/progesterone ratio most likely induced by a decrease in prolactin concentration. D4 also inhibited the pre-ovulatory LH surge causing a delay in ovulation, persistent follicles and thus a prolonged exposure to elevated estrogen in the adult Sprague Dawely rat. A lengthening of the estrous cycle in the F344 rat with an increase in endogenous estrogen was also induced by D4 inhalation. Although the mode of action responsible for induction of uterine adenomas in the female F344 rat has not been clearly confirmed, the subtlety of effects on the effects of D4 on cyclicity may prevent further assessment and definition of the mode of action. The occurrence of uterine endometrial adenoma in the rat is not relevant for human risk characterization because (1) there are differences in ovulatory cycle regulation in rats compared to humans, (2) cystic hyperplasia without atypia in women is not a cancer precursor, and (3) there is no endometrial lesion in women that is directly analogous to endometrial adenoma in the rat. The effects of D4 on liver are due to a phenobarbital-like mechanism that results in induction of cytochrome P450 and other enzymes of xenobiotic biotransformation. The liver effects are adaptive and not adverse. Kidney findings included chonic progressive nephropathy, a rat lesion that has no counterpart in the human and that should not be used in human risk assessment., (Copyright © 2017 The Authors. Published by Elsevier B.V. All rights reserved.)

Published
2017
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24. Comments on the safety assessment of decamethylcyclopentasiloxane (D5) published in regulatory toxicology and pharmacology, 2017, 83:117-118.

Author

Bridges J, Dekant W, Klaunig JE, and Scialli AR

Subjects
Animals, Female, Humans, Inhalation Exposure adverse effects, Receptors, Dopamine metabolism, Siloxanes administration & dosage, Uterine Neoplasms chemically induced, Uterine Neoplasms diagnosis, Uterine Neoplasms metabolism, Consumer Product Safety standards, Cosmetics metabolism, Cosmetics toxicity, Siloxanes metabolism, Siloxanes toxicity
Published
2017
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26. Treatment of Men for "Low Testosterone": A Systematic Review.

Author

Huo S, Scialli AR, McGarvey S, Hill E, Tügertimur B, Hogenmiller A, Hirsch AI, and Fugh-Berman A

Abstract

Testosterone products are recommended by some prescribers in response to a diagnosis or presumption of "low testosterone" (low-T) for cardiovascular health, sexual function, muscle weakness or wasting, mood and behavior, and cognition. We performed a systematic review of 156 eligible randomized controlled trials in which testosterone was compared to placebo for one or more of these conditions. We included studies in bibliographic databases between January 1, 1950 and April 9, 2016, and excluded studies involving bodybuilding, contraceptive effectiveness, or treatment of any condition in women or children. Studies with multiple relevant endpoints were included in all relevant tables. Testosterone supplementation did not show consistent benefit for cardiovascular risk, sexual function, mood and behavior, or cognition. Studies that examined clinical cardiovascular endpoints have not favored testosterone therapy over placebo. Testosterone is ineffective in treating erectile dysfunction and controlled trials did not show a consistent effect on libido. Testosterone supplementation consistently increased muscle strength but did not have beneficial effects on physical function. Most studies on mood-related endpoints found no beneficial effect of testosterone treatment on personality, psychological well-being, or mood. The prescription of testosterone supplementation for low-T for cardiovascular health, sexual function, physical function, mood, or cognitive function is without support from randomized clinical trials., Competing Interests: Adriane Fugh-Berman is an expert witness at the request of plaintiffs in litigation regarding pharmaceutical marketing practices (Adriane Fugh-Berman was briefly engaged as an expert in testosterone litigation last year but has no relevant conflicts now). Adriane Fugh-Berman also directs PharmedOut, a Georgetown University Medical Center project that advances evidence-based prescribing and educates healthcare professionals about pharmaceutical marketing practices, and provides educational content for the Washington DC Department of Health-funded DC Center for Rational Prescribing through a contract with the George Washington University Milken School of Public Health. Alessandra Hirsch is a former project manager of PharmedOut and Alycia Hogenmiller is the current project manager of PharmedOut; their salaries are provided by Georgetown University Medical Center. Dr. Scialli is the sole participant in Scialli Consulting LLC. He is a reproductive toxicologist who consults for industry, government, and educational institutions. He has consulted for manufacturers of testosterone products, but never about testosterone. There are no patents, products in development or marketed products to declare. This does not alter our adherence to all the PLOS ONE policies on sharing data and materials.

Published
2016
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29. Chronic toxicity and oncogenicity of decamethylcyclopentasiloxane in the Fischer 344 Rat.

Author

Jean PA, Plotzke KP, and Scialli AR

Subjects
Adenocarcinoma pathology, Administration, Inhalation, Animals, Carcinogenicity Tests, Endometrial Neoplasms pathology, Endometrium drug effects, Endometrium pathology, Female, Male, Rats, Inbred F344, Respiratory System drug effects, Respiratory System pathology, Siloxanes pharmacokinetics, Species Specificity, Toxicity Tests, Chronic, Adenocarcinoma chemically induced, Endometrial Neoplasms chemically induced, Siloxanes toxicity
Abstract

Decamethylcyclopentasiloxane (D5) is a cyclic polydimethylsiloxane used in the synthesis of silicon-based materials and as a component in consumer products. Male and female Fischer 344 rats were exposed to D5 vapor (0, 10, 40, 160 ppm; whole-body inhalation) for 6 h/d, 5 d/wk, for up to 104 weeks. Microscopic examination of tissues revealed test article effects at 160 ppm in the upper respiratory tract (hyaline inclusions in males and females at 6, 12, and 24 months) and an increased incidence of uterine endometrial adenocarcinoma at 24-months. The hyaline inclusions were considered a non-adverse tissue response for lack of any other respiratory tract non-neoplastic or neoplastic changes. Uterine endometrial adenocarcinoma was not anticipated. Toxicity testing (mutagenicity/genotoxicity, acute, sub-acute and sub-chronic descriptive toxicity) performed prior to the conduct of the chronic bioassay provided no indication that the uterus was a potential target organ. The target organ and tumor type specificity (adenocarcinoma is a common spontaneous tumor in the aged Fischer 344 rat) suggests the effect is associated with estrous cycle alteration. A robust assessment of potential mode(s) of action responsible for the uterine tumors and relevance to humans is addressed in a companion manuscript (Klaunig et al., 2015)., (Copyright © 2015 Elsevier Inc. All rights reserved.)

Published
2016
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30. Biological relevance of decamethylcyclopentasiloxane (D5) induced rat uterine endometrial adenocarcinoma tumorigenesis: Mode of action and relevance to humans.

Author

Klaunig JE, Dekant W, Plotzke K, and Scialli AR

Subjects
Administration, Inhalation, Aging, Animals, Carcinogenicity Tests, Estrous Cycle, Female, Humans, Male, Rats, Rats, Inbred F344, Risk Assessment, Species Specificity, Toxicity Tests, Chronic, Adenocarcinoma chemically induced, Endometrial Neoplasms chemically induced, Siloxanes toxicity
Abstract

Decamethylcyclopentasiloxane (D5) is a cyclic siloxane used in the production and formulation of consumer products with potential exposure to manufacturing workers, consumer, and the general public. Following a combined 2-year inhalation chronic bioassay performed in Fischer 344 (F344) rats, an increase in uterine endometrial adenocarcinomas was noted at the highest concentration to which animals were exposed. No other neoplasms were detected. In this study, a dose of 160 ppm produced an incidence of 8% endometrial adenocarcinomas. Based on a number of experimental studies with D5, the current manuscript examines the biological relevance and possible modes of action for the uterine endometrial adenocarcinomas observed in the rat following chronic exposure to D5. Variable rates of spontaneous uterine endometrial adenocarcinomas have been reported for untreated F344 CrlBr rats. As such, we concluded that the slight increase in uterine endometrial adenocarcinomas observed in the D5 chronic bioassay might not be the result of D5 exposure but may be related to variability of the spontaneous tumor incidence in this strain of rat. However, if the uterine endometrial adenocarcinomas are related to D5-exposure, alteration in the estrous cycle in the aging F344 rat is the most likely mode of action. D5 is not genotoxic or estrogenic. The alteration in the estrous cycle is caused by a decrease in progesterone with an increase in the estrogen:progesterone ratio most likely induced by a decrease in prolactin concentration. Available data support that exposure to D5 influences prolactin concentration. Although the effects on prolactin concentrations in a number of experiments were not always consistent, the available data support the conclusion that D5 is acting via a dopamine receptor agonist-like mechanism to alter the pituitary control of the estrous cycle. In further support of this mode of action, studies in F344 aged animals showed that the effects of D5 on estrous cyclicity produced a response consistent with a dopamine-like effect and further suggest that D5 is accelerating the aging of the reproductive endocrine system in the F344 rat utilized in this study. This mode of action for uterine endometrial adenocarcinoma tumorigenesis is not relevant for humans., (Copyright © 2015 The Authors. Published by Elsevier Inc. All rights reserved.)

Published
2016
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31. Reprint of "Potential seminal transport of pharmaceuticals to the conceptus".

Author

Scialli AR, Bailey G, Beyer BK, Bøgh IB, Breslin WJ, Chen CL, DeLise AM, Hui JY, Moffat GJ, Stewart J, and Thompson KE

Subjects
Animals, Antibodies, Monoclonal administration & dosage, Antibodies, Monoclonal chemistry, Antibodies, Monoclonal toxicity, Biological Transport, Embryo, Mammalian drug effects, Female, Fetus drug effects, Haplorhini, Humans, Male, Maternal Exposure, Mice, Models, Animal, Models, Biological, Paternal Exposure, Peptides chemistry, Peptides toxicity, Permeability, Pharmaceutical Preparations administration & dosage, Pharmaceutical Preparations chemistry, Rabbits, Risk Assessment, Vaginal Absorption, Antibodies, Monoclonal metabolism, Embryo, Mammalian metabolism, Fetus metabolism, Peptides metabolism, Pharmaceutical Preparations metabolism, Semen metabolism, Vagina metabolism
Abstract

Small molecule pharmaceutical products are assumed to reach concentrations in semen similar to those in blood plasma. Exposure modeling for these small-molecule products in humans assumes a daily dose of 5mL of semen and 100% absorption from the vagina with distribution to the conceptus through the maternal systemic circulation. Monoclonal antibody drugs are present in semen at concentrations about 2% or less of those in blood, and the modeling used for small molecules will over-estimate the possibility of conceptus exposure to immunoglobulins. It is not known whether peptide products reach semen, but in general peptide medications are destroyed by vaginal peptidases, and conceptus exposure is predicted to be minimal. Theoretical exposure routes to pharmaceuticals that might result in exposure of the conceptus greater than that of maternal systemic exposures include direct access through the cervical canal, adsorption to sperm for carriage into the oocyte, and direct delivery from the vaginal veins or lymphatics to the uterine artery. There is some evidence for direct access to the uterus for progesterone, terbutaline, and danazol, but the evidence does not involve exposures during pregnancy in most instances. Studies in mice, rats, rabbits, and monkeys do not suggest that exposure to small molecule pharmaceuticals in semen imposes risks to the conceptus beyond those that can be predicted using modeling of systemic maternal exposure. Monoclonal antibody and peptide exposure in semen does not pose a significant risk to the conceptus., (Copyright © 2015 The Authors. Published by Elsevier Inc. All rights reserved.)

Published
2016
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32. Potential seminal transport of pharmaceuticals to the conceptus.

Author

Scialli AR, Bailey G, Beyer BK, Bøgh IB, Breslin WJ, Chen CL, DeLise AM, Hui JY, Moffat GJ, Stewart J, and Thompson KE

Subjects
Animals, Antibodies, Monoclonal adverse effects, Biological Transport, Cervix Uteri drug effects, Embryo, Mammalian drug effects, Female, Humans, Male, Models, Biological, Pregnancy, Proteins adverse effects, Risk Assessment, Risk Factors, Species Specificity, Vagina drug effects, Antibodies, Monoclonal metabolism, Cervix Uteri metabolism, Embryo, Mammalian metabolism, Pharmaceutical Preparations metabolism, Proteins metabolism, Semen metabolism, Vagina metabolism
Abstract

Small molecule pharmaceutical products are assumed to reach concentrations in semen similar to those in blood plasma. Exposure modeling for these small-molecule products in humans assumes a daily dose of 5mL of semen and 100% absorption from the vagina with distribution to the conceptus through the maternal systemic circulation. Monoclonal antibody drugs are present in semen at concentrations about 2% or less of those in blood, and the modeling used for small molecules will over-estimate the possibility of conceptus exposure to immunoglobulins. It is not known whether peptide products reach semen, but in general peptide medications are destroyed by vaginal peptidases, and conceptus exposure is predicted to be minimal. Theoretical exposure routes to pharmaceuticals that might result in exposure of the conceptus greater than that of maternal systemic exposures include direct access through the cervical canal, adsorption to sperm for carriage into the oocyte, and direct delivery from the vaginal veins or lymphatics to the uterine artery. There is some evidence for direct access to the uterus for progesterone, terbutaline, and danazol, but the evidence does not involve exposures during pregnancy in most instances. Studies in mice, rats, rabbits, and monkeys do not suggest that exposure to small molecule pharmaceuticals in semen imposes risks to the conceptus beyond those that can be predicted using modeling of systemic maternal exposure. Monoclonal antibody and peptide exposure in semen does not pose a significant risk to the conceptus., (Copyright © 2015 The Authors. Published by Elsevier Inc. All rights reserved.)

Published
2015
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33. Agent Orange Exposure and 2,3,7,8-Tetrachlorodibenzo-p-Dioxin (TCDD) in Human Milk.

Author

Scialli AR, Watkins DK, and Ginevan ME

Subjects
2,4,5-Trichlorophenoxyacetic Acid chemistry, 2,4,5-Trichlorophenoxyacetic Acid pharmacokinetics, 2,4-Dichlorophenoxyacetic Acid chemistry, 2,4-Dichlorophenoxyacetic Acid pharmacokinetics, Adult, Agent Orange, Environmental Pollutants chemistry, Female, Humans, Infant, Polychlorinated Dibenzodioxins chemistry, Polychlorinated Dibenzodioxins pharmacokinetics, Vietnam, 2,4,5-Trichlorophenoxyacetic Acid analysis, 2,4-Dichlorophenoxyacetic Acid analysis, Environmental Exposure analysis, Environmental Pollutants analysis, Milk, Human chemistry, Polychlorinated Dibenzodioxins analysis
Abstract

Agent Orange was sprayed in parts of southern Vietnam during the U.S.-Vietnam war and was a mixture of two chlorophenoxy herbicides. The mixture was contaminated with 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD). TCDD and other dioxins and furans are measurable in the milk of Vietnamese women. We explored whether the TCDD in milk from these women was from Agent Orange and whether lactational exposure can be a mode of transgenerational effects of TCDD from Agent Orange. A review of the world's literature on milk concentrations of polychlorinated compounds showed the presence of TCDD and other dioxins and furans in all countries that have been assessed. The congener profile of these chemicals, that is, the proportion of different congeners in the sample, can be used to assess the source of milk contamination. Measurements in most countries, including contemporary measurements in Vietnam, are consistent with non-Agent Orange exposure sources, including industrial activities and incineration of waste. Models and supporting human data suggest that TCDD from breastfeeding does not persist in a child past adolescence and that the adult body burden of TCDD is independent of whether the individual was breast- or bottle-fed as a child. These findings suggest that exposure to Agent Orange in Vietnam did not result in persistent transgenerational exposure through human milk., (© 2015 Wiley Periodicals, Inc.)

Published
2015
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34. Exposure-based validation list for developmental toxicity screening assays.

Author

Daston GP, Beyer BK, Carney EW, Chapin RE, Friedman JM, Piersma AH, Rogers JM, and Scialli AR

Subjects
Biological Assay, High-Throughput Screening Assays, In Vitro Techniques, Risk Assessment, Fetal Development drug effects, Teratogenesis drug effects, Teratogens toxicity, Toxicity Tests
Abstract

Validation of alternative assays requires comparison of the responses to toxicants in the alternative assay with in vivo responses. Chemicals have been classified as "positive" or "negative" in vivo, despite the fact that developmental toxicity is conditional on magnitude of exposure. We developed a list of positive and negative developmental exposures, with exposure defined by toxicokinetic data, specifically maternal plasma Cmax . We selected a series of 20 chemicals that caused developmental toxicity and for which there were appropriate toxicokinetic data. Where possible, we used the same chemical for both positive and negative exposures, the positive being the Cmax at a dose level that produced significant teratogenicity or embryolethality, the negative being the Cmax at a dose level not causing developmental toxicity. It was not possible to find toxicokinetic data at the no-effect level for all positive compounds, and the negative exposure list contains Cmax values for some compounds that do not have developmental toxicity up to the highest dose level tested. This exposure-based reference list represents a fundamentally different approach to the evaluation of alternative tests and is proposed as a step toward application of alternative tests in quantitative risk assessment., (© 2014 Wiley Periodicals, Inc.)

Published
2014
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35. The National Birth Defects Prevention Study: how to communicate data.

Author

Scialli AR

Subjects
Case-Control Studies, Female, Humans, Male, Pregnancy, Risk Factors, United States, Congenital Abnormalities prevention & control, Information Dissemination
Abstract

The National Birth Defects Prevention Study is a population-based case-control study. The study has actively sought to identify children with any of 34 specified types of malformation. The mothers of affected and unaffected children have been interviewed with regard to demographic information, lifestyle factors, and exposures. A large number of published studies have appeared and continue to appear on diverse exposures and outcomes. An example of such a study identified an increased odds ratio for ondansetron use among the mothers of children with cleft palate. Possible explanations for associations between exposures and outcomes are chance, error, and causation. The ondansetron-cleft palate association may have arisen by chance given the large number of comparisons made in the study. Error appears unlikely as an explanation of the association. The assessment of causation in teratology uses a systematic evaluation based on the Hill criteria or similar criteria of Shepard or Brent., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published
2014
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36. Atrazine and pregnancy outcomes: a systematic review of epidemiologic evidence.

Author

Goodman M, Mandel JS, DeSesso JM, and Scialli AR

Subjects
Abortion, Spontaneous chemically induced, Abortion, Spontaneous pathology, Animals, Birth Weight drug effects, Disease Models, Animal, Female, Fetal Development drug effects, Gestational Age, Herbicides toxicity, Humans, Maternal Exposure adverse effects, Pregnancy, Atrazine toxicity, Pregnancy Outcome
Abstract

Atrazine (ATR) is a commonly used agricultural herbicide that has been the subject of epidemiologic studies assessing its relation to reproductive health problems. This review evaluates both the consistency and the quality of epidemiologic evidence testing the hypothesis that ATR exposure, at usually encountered levels, is a risk factor for birth defects, small for gestational age birth weight, prematurity, miscarriages, and problems of fetal growth and development. We followed the current methodological guidelines for systematic reviews by using two independent researchers to identify, retrieve, and evaluate the relevant epidemiologic literature on the relation of ATR to various adverse outcomes of birth and pregnancy. Each eligible paper was summarized with respect to its methods and results with particular attention to study design and exposure assessment, which have been cited as the main areas of weakness in ATR research. As a quantitative meta-analysis was not feasible, the study results were categorized qualitatively as positive, null, or mixed. The literature on ATR and pregnancy-related health outcomes is growing rapidly, but the quality of the data is poor with most papers using aggregate rather than individual-level information. Without good quality data, the results are difficult to assess; however, it is worth noting that none of the outcome categories demonstrated consistent positive associations across studies. Considering the poor quality of the data and the lack of robust findings across studies, conclusions about a causal link between ATR and adverse pregnancy outcomes are not warranted., (© 2014 Wiley Periodicals, Inc.)

Published
2014
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37. Developmental toxicity studies with atrazine and its major metabolites in rats and rabbits.

Author

Scialli AR, DeSesso JM, and Breckenridge CB

Subjects
Animals, Atrazine administration & dosage, Dose-Response Relationship, Drug, Female, Fetal Weight drug effects, Fetus drug effects, Herbicides administration & dosage, Herbicides toxicity, Maternal Exposure adverse effects, Pregnancy, Rabbits, Rats, Toxicity Tests, Atrazine analogs & derivatives, Atrazine toxicity
Abstract

Atrazine (ATR), hydroxyatrazine (OH-ATR), and the three chloro metabolites of ATR (deethylatrazine [DEA], deisopropylatrazine [DIA], diaminochlorotriazine [DACT]) were evaluated for developmental effects in rats and rabbits. Three developmental toxicity studies were conducted on ATR in rats (two studies) and rabbits and a developmental toxicity study was conducted in rats for each of the four ATR metabolites DEA, DIA, DACT, and OH-ATZ. ATR administration by gavage to pregnant rats and rabbits from implantation (gestation day [GD] 6 in rat, GD 7 in rabbit) through closure of the palate (GD 15 in rat and GD 19 in rabbit) did not statistically significantly alter the incidence of developmental abnormalities or malformations at dose levels up to 100 (rat) or 75 (rabbit) mg/kg bw/day. There were no effects on developmental toxicity parameters for DEA, DIA, DACT, or OH-ATR at oral dose levels up to 100, 100, 150, or 125 mg/kg bw/day, respectively, with the exception of reductions in fetal body weight by DACT and OH-ATR in the presence of decreased maternal body weight gain. ATR did not adversely affect developmental end points in a two-generation study conducted in rats exposed to dose levels up to 500 ppm (38.7 mg/kg/day) in the diet. The 500-ppm dose level resulted in significantly reduced maternal body weight gain. Overall, data show that neither ATR nor its metabolites statistically significantly affected rat or rabbit embryo-fetal development even at dose levels producing maternal toxicity., (© 2014 Wiley Periodicals, Inc.)

Published
2014
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38. Multigeneration reproduction and male developmental toxicity studies on atrazine in rats.

Author

DeSesso JM, Scialli AR, White TE, and Breckenridge CB

Subjects
Administration, Oral, Animals, Atrazine administration & dosage, Body Weight, Dose-Response Relationship, Drug, Endpoint Determination, Epididymis drug effects, Epididymis metabolism, Female, Lactation, Male, Maternal Exposure, No-Observed-Adverse-Effect Level, Organ Size drug effects, Pregnancy, Rats, Spermatozoa drug effects, Testosterone blood, Atrazine toxicity, Reproduction drug effects
Abstract

Background: Reproductive toxicity of Atrazine (ATR) was evaluated in two rat multigenerational studies. Development of male reproductive parameters was evaluated in separate studies after prenatal or postnatal exposure., Methods: In multigenerational studies, rats received dietary concentrations of 0, 10, 50, 100 or 500 ppm ATR. In separate studies in female rats, ATR was administered by gavage at 0, 1, 5, 25 or 125 mg/kg/day during pregnancy (GD6-21) or lactation (LD2-21). Plasma testosterone concentration, testicular and epididymal weights, and sperm counts were measured in male offspring on PND70 and 170., Results: In the multigenerational studies, parental systemic toxicity occurred at 500 ppm (38.7 mg/kg/day), but reproductive endpoints were unaffected. In the prenatal study, maternal toxicity and embryo-fetal mortality occurred at 125 mg/kg/day. In male offspring, testosterone levels and sperm counts were unaffected, although the percentage of abnormal sperm increased at 125 mg/kg/day (PND 70) and 25 mg/kg/day (PND170). In the postnatal study, maternal toxicity and reduced body weights of male offspring occurred at 125 mg/kg/day. Additionally, reduced testicular (PND70, PND170) and epididymal (PND70) weights and increased numbers of abnormal sperm (PND70, PND170) were seen, but no changes in plasma testosterone or sperm counts., Conclusions: Dietary administration of ATR did not affect rat reproduction up to a parentally toxic dose of 38.7 mg/kg/day. Some effects on male reproductive system development occurred after high dose, bolus administration to dams, but doses were much higher than expected under normal use conditions. Thus, oral RfDs for ATR would be protective for reproductive effects., (© 2014 Wiley Periodicals, Inc.)

Published
2014
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39. Teratology public affairs committee position paper: iodine deficiency in pregnancy.

Author

Obican SG, Jahnke GD, Soldin OP, and Scialli AR

Subjects
Animals, Congenital Hypothyroidism metabolism, Dietary Supplements standards, Female, Fishes, Humans, Iodine administration & dosage, Iodine metabolism, Malnutrition, Nutritional Requirements physiology, Pregnancy, Seaweed, Sodium Chloride, Dietary administration & dosage, Teratology, Thyroid Gland drug effects, Thyroid Gland metabolism, Thyroid Hormones biosynthesis, Vitamins, Congenital Hypothyroidism prevention & control, Dietary Supplements supply & distribution, Iodine deficiency
Abstract

Iodine deficiency is an important nutritional deficiency, with more than 2 billion people worldwide estimated to be at risk. The developing fetus and young children are particularly at risk. During pregnancy and lactation, iodine requirements increase, whether in iodine-poor or iodine-sufficient countries, making the mother and the developing fetus vulnerable. The American Thyroid Association (ATA) recommends 250 micrograms per day of iodine intake for pregnant and lactating women. The thyroid gland is able to adapt to the changes associated with pregnancy as long as sufficient iodine is present. Dietary intake is the sole source of iodine, which is essential to the synthesis of thyroid hormones. Iodine is found in multiple dietary sources including iodized salt, dairy products, seaweed, and fish. Prenatal vitamins containing iodine are a good source of iodine, but iodine content in multivitamin supplements is highly variable. Congenital hypothyroidism is associated with cretinism. Clinical hypothyroidism has been associated with increased risk of poor perinatal outcome including prematurity, low birth weight, miscarriage, preeclampsia, fetal death, and impaired fetal neurocognitive development. Subclinical hypothyroidism is also associated with poor pregnancy outcomes and potential fetal neurocognitive deficits, but the data are more variable than those for clinical hypothyroidism. We concur with the ATA recommendation that all pregnant and lactating women should ingest (through diet and supplements) 250 micrograms of iodine daily. To achieve this goal, we recommend that all pregnant and lactating women take daily iodine supplementation of 150 micrograms., (Copyright © 2012 Wiley Periodicals, Inc.)

Published
2012
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40. Teratogen update: methotrexate.

Author

Hyoun SC, Običan SG, and Scialli AR

Subjects
Abnormalities, Drug-Induced pathology, Abnormalities, Multiple pathology, Aminopterin toxicity, Animals, Female, Fetal Diseases etiology, Folic Acid Antagonists toxicity, Humans, Mice, Mice, Inbred C57BL, Pregnancy, Pregnancy Complications drug therapy, Pregnancy, Ectopic drug therapy, Rabbits, Rats, Rats, Sprague-Dawley, Tetrahydrofolate Dehydrogenase drug effects, Abnormalities, Drug-Induced etiology, Abnormalities, Multiple chemically induced, Methotrexate toxicity, Teratogens toxicity
Abstract

Methotrexate and aminopterin are folic acid antagonists that inhibit dihydrofolate reductase, resulting in a block in the synthesis of thymidine and inhibition of DNA synthesis. Methotrexate has been used for the treatment of malignancy, rheumatic disorders, and psoriasis and termination of intrauterine pregnancy. Recently, methotrexate has become a standard treatment for ectopic pregnancy. The misdiagnosis of an intrauterine pregnancy as an ectopic pregnancy can result in exposure of a continuing pregnancy to dose levels of methotrexate of 50 mg/m(2) (maternal body surface area). Experimental animal studies have associated methotrexate therapy with embryo death in mice, rats, rabbits, and monkeys. Structural malformations have been most consistently produced in rabbits at a maternal dose level of 19.2 mg/kg. Abnormalities in rabbits include hydrocephalus, microphthalmia, cleft lip and palate, micrognathia, dysplastic sacral and caudal vertebrate, phocomelia, hemimelia, syndactyly, and ectrodactyly. Based on human case reports of methotrexate exposure during pregnancy, a methotrexate embryopathy has been described that includes growth deficiency, microcephaly, hypoplasia of skull bones, wide fontanels, coronal or lambdoidal craniosynostosis, upswept frontal scalp hair, broad nasal bridge, shallow supraorbital ridges, prominent eyes, low-set ears, maxillary hypoplasia, epicanthal folds, short limbs, talipes, hypodactyly, and syndactyly. This syndrome may be associated with exposures between 6 and 8 weeks after conception and dose levels of 10 mg/week or greater. More recent case reports of methotrexate exposure for the misdiagnosis of ectopic pregnancy involve treatment before 6 weeks after conception and have raised the suggestion of a distinct syndrome due to such early exposures. Tetralogy of Fallot and perhaps other neural crest cell-related abnormalities may be features of this early syndrome. A disproportionality analysis of methotrexate and aminopterin case reports and series provides support for pulmonary atresia, craniosynostosis, and limb deficiencies as reported more often than expected in methotrexate-exposed children. Denominator-based data will be welcome to better define elements of a methotrexate embryopathy and possibly to distinguish an early exposure syndrome from anomalies traditionally associated with methotrexate exposure., (Copyright © 2012 Wiley Periodicals, Inc.)

Published
2012
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41. Correlation of chemical structure with reproductive and developmental toxicity as it relates to the use of the threshold of toxicological concern.

Author

Laufersweiler MC, Gadagbui B, Baskerville-Abraham IM, Maier A, Willis A, Scialli AR, Carr GJ, Felter SP, Blackburn K, and Daston G

Subjects
Animals, Dose-Response Relationship, Drug, Humans, No-Observed-Adverse-Effect Level, Risk Assessment, Toxicity Tests, Drug-Related Side Effects and Adverse Reactions, Embryonic Development drug effects, Fetal Development drug effects, Hazardous Substances toxicity, Reproduction drug effects
Abstract

In the absence of toxicological data on a chemical, the threshold of toxicological concern (TTC) approach provides a system to estimate a conservative exposure below which there is a low probability of risk for adverse health effects. The original toxicology dataset underlying the TTC was based on NOELs from repeat dose studies. Subsequently there have been several efforts to assess whether or not these limits are also protective for reproductive/developmental effects. This work expands the database of chemicals with reproductive and developmental data, presents these data in a comprehensive and transparent format and groups the chemicals according to the TTC "Cramer Class" rules. Distributions of NOAELs from each of these classes were used to assess whether the previously proposed TTC values based on repeat dose data are protective for reproductive/developmental toxicity endpoints as well. The present analysis indicates that, for each Cramer Class, the reproductive and developmental endpoints would be protected at the corresponding general TTC tiers derived by Munro et al. (1996)., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published
2012
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42. REACH and reproductive and developmental toxicology: still questions.

Author

Scialli AR and Guikema AJ

Subjects
Animal Testing Alternatives, Animals, Developmental Biology standards, European Union, Guidelines as Topic, Humans, Models, Animal, Models, Chemical, Risk Assessment, Structure-Activity Relationship, Developmental Biology legislation & jurisprudence, Government Regulation, Hazardous Substances toxicity, Reproduction drug effects, Toxicity Tests methods, Toxicity Tests standards
Abstract

Registration, Evaluation, Authorization, and Restriction of Chemicals (REACH) is a new chemicals regulation law in the European Union (EU). The law is supplemented by tens of thousands of pages of guidance documents, and the implementation of REACH is still a work in progress. Requirements for chemical testing are based on the annual volume of a chemical or 'substance' that is produced or imported into the EU. These requirements include reproductive and developmental toxicity testing in experimental animals for an annual volume of 10 metric tonnes or more. However, under REACH, the testing in vertebrate animals may not be performed without permission, and the law encourages the use of alternative methods of filling data gaps on the toxicological properties of chemicals. These alternatives might include in vitro and structure-activity relationship studies, but the REACH technical guidance indicates that these kinds of studies are not adequate to replace reproductive and developmental toxicity testing in whole animals. The most practical opportunity for the avoidance of whole animal testing may be 'read-across,' a process in which gaps are filled using data from related compounds. A method called 'weight of evidence' under REACH may also be used to avoid whole animal reproductive and developmental toxicity testing based on existing data in regulation and non-regulation studies and based on factors such as chemical structure and anticipated exposure. It is also possible that thresholds of toxicological concerns will be accepted under REACH as a method to avoid vertebrate animal testing.

Published
2012
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43. Critical evaluation of current developmental toxicity testing strategies: a case of babies and their bathwater.

Author

Carney EW, Ellis AL, Tyl RW, Foster PM, Scialli AR, Thompson K, and Kim J

Subjects
Animals, Female, Humans, Mice, Pregnancy, Rabbits, Rats, Risk Assessment, Safety, Fetal Development drug effects, Models, Animal, Toxicity Tests methods
Abstract

This review is the second in a series of four papers emanating from a workshop entitled "Developmental Toxicology-New Directions," which was sponsored by the ILSI Health and Environmental Sciences Institute's (HESI) Developmental and Reproductive Toxicology Technical Committee. The present review analyzes the strengths and weaknesses of current developmental safety testing approaches in an effort to identify those strengths that should be retained in the future versus the weaknesses that should be eliminated. Workshop participants considered the following to be key strengths of current testing approaches: the integrated biology of pregnant animal models including pharmacokinetic and pharmacodynamic processes, the ability to detect low incidence malformations as well as maternally mediated toxicity, and the long history of use coupled with extensive historical data. A number of weaknesses were related to the resource-intensive nature of developmental toxicity testing (e.g., large number of animals, high costs, low throughput, the inability to keep pace with the demand for more toxicity data). Other weaknesses included the use of very high dose levels that often far exceed human exposure levels, the confounding influence of maternal toxicity, sparse understanding of basic developmental mechanisms and genetics of standard animal models relative to mouse or lower organisms, difficulties interpreting low incidence findings, and issues surrounding the interpretation of minor skeletal variations. An appreciation of these strengths and weaknesses is critical for the design of new approaches to developmental toxicity testing in the 21st century., (© 2011 Wiley Periodicals, Inc.)

Published
2011
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44. Teratogenic exposures.

Author

Običan S and Scialli AR

Subjects
Abnormalities, Drug-Induced etiology, Animals, Female, Humans, Maternal Exposure adverse effects, Pregnancy, Pregnancy Complications, Infectious, Substance-Related Disorders complications, Drug-Related Side Effects and Adverse Reactions, Environmental Exposure adverse effects, Teratogens toxicity
Abstract

A consideration of teratogenic exposures includes not only an agent (chemical, radiation, biologic) but an exposure level and timing of exposure. There are criteria by which exposures are evaluated for a causal connection with an abnormal outcome. We here review some teratogenic exposures and discuss how they were initially described and confirmed. We have limited our discussion to some of the exposures for which a connection to structural malformations has been accepted in some quarters, and we indicate some exposures for which a causal association awaits confirmation. We recommend that counselors find a reliable and updatable source of information on exposures during pregnancy., (Copyright © 2011 Wiley-Liss, Inc.)

Published
2011
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45. Thalidomide: the tragedy of birth defects and the effective treatment of disease.

Author

Kim JH and Scialli AR

Subjects
Animals, Dose-Response Relationship, Drug, Ectromelia chemically induced, Female, Humans, Lenalidomide, Nausea drug therapy, Oxidative Stress, Pregnancy, Teratogens pharmacology, Thalidomide analogs & derivatives, Thalidomide pharmacology, Treatment Outcome, United States, Abnormalities, Drug-Induced, Angiogenesis Inhibitors adverse effects, Leprosy drug therapy, Multiple Myeloma drug therapy, Thalidomide adverse effects
Abstract

Thalidomide was a widely used drug in the late 1950s and early 1960s for the treatment of nausea in pregnant women. It became apparent in the 1960s that thalidomide treatment resulted in severe birth defects in thousands of children. Though the use of thalidomide was banned in most countries at that time, thalidomide proved to be a useful treatment for leprosy and later, multiple myeloma. In rural areas of the world that lack extensive medical surveillance initiatives, thalidomide treatment of pregnant women with leprosy has continued to cause malformations. Research on thalidomide mechanisms of action is leading to a better understanding of molecular targets. With an improved understanding of these molecular targets, safer drugs may be designed. The thalidomide tragedy marked a turning point in toxicity testing, as it prompted United States and international regulatory agencies to develop systematic toxicity testing protocols; the use of thalidomide as a tool in developmental biology led to important discoveries in the biochemical pathways of limb development. In celebration of the Society of Toxicology's 50th Anniversary, which coincides with the 50th anniversary of the withdrawal of thalidomide from the market, it is appropriate to revisit the lessons learned from the thalidomide tragedy of the 1960s.

Published
2011
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46. Reproductive effects of the parabens.

Author

Scialli AR

Subjects
Animals, Humans, Endocrine Disruptors toxicity, Environmental Exposure adverse effects, Environmental Pollutants toxicity, Parabens toxicity, Preservatives, Pharmaceutical toxicity
Published
2011
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47. Promotional tone in reviews of menopausal hormone therapy after the Women's Health Initiative: an analysis of published articles.

Author

Fugh-Berman A, McDonald CP, Bell AM, Bethards EC, and Scialli AR

Subjects
Adult, Breast Neoplasms diagnosis, Breast Neoplasms epidemiology, Cardiovascular Diseases epidemiology, Estrogen Replacement Therapy trends, Female, Humans, Menopause, Physicians psychology, Review Literature as Topic, United States epidemiology, Women's Health, Attitude of Health Personnel, Conflict of Interest, Estrogen Replacement Therapy adverse effects, Randomized Controlled Trials as Topic
Abstract

Background: Even after the Women's Health Initiative (WHI) found that the risks of menopausal hormone therapy (hormone therapy) outweighed benefit for asymptomatic women, about half of gynecologists in the United States continued to believe that hormones benefited women's health. The pharmaceutical industry has supported publication of articles in medical journals for marketing purposes. It is unknown whether author relationships with industry affect promotional tone in articles on hormone therapy. The goal of this study was to determine whether promotional tone could be identified in narrative review articles regarding menopausal hormone therapy and whether articles identified as promotional were more likely to have been authored by those with conflicts of interest with manufacturers of menopausal hormone therapy., Methods and Findings: We analyzed tone in opinion pieces on hormone therapy published in the four years after the estrogen-progestin arm of the WHI was stopped. First, we identified the ten authors with four or more MEDLINE-indexed reviews, editorials, comments, or letters on hormone replacement therapy or menopausal hormone therapy published between July 2002 and June 2006. Next, we conducted an additional search using the names of these authors to identify other relevant articles. Finally, after author names and affiliations were removed, 50 articles were evaluated by three readers for scientific accuracy and for tone. Scientific accuracy was assessed based on whether or not the findings of the WHI were accurately reported using two criteria: (1) Acknowledgment or lack of denial of the risk of breast cancer diagnosis associated with hormone therapy, and (2) acknowledgment that hormone therapy did not benefit cardiovascular disease endpoints. Determination of promotional tone was based on the assessment by each reader of whether the article appeared to promote hormone therapy. Analysis of inter-rater consistency found moderate agreement for scientific accuracy (κ=0.57) and substantial agreement for promotional tone (κ=0.65). After discussion, readers found 86% of the articles to be scientifically accurate and 64% to be promotional in tone. Themes that were common in articles considered promotional included attacks on the methodology of the WHI, arguments that clinical trial results should not guide treatment for individuals, and arguments that observational studies are as good as or better than randomized clinical trials for guiding clinical decisions. The promotional articles we identified also implied that the risks associated with hormone therapy have been exaggerated and that the benefits of hormone therapy have been or will be proven. Of the ten authors studied, eight were found to have declared payment for speaking or consulting on behalf of menopausal hormone manufacturers or for research support (seven of these eight were speakers or consultants). Thirty of 32 articles (90%) evaluated as promoting hormone therapy were authored by those with potential financial conflicts of interest, compared to 11 of 18 articles (61%) by those without such conflicts (p=0.0025). Articles promoting the use of menopausal hormone therapy were 2.41 times (95% confidence interval 1.49-4.93) as likely to have been authored by authors with conflicts of interest as by authors without conflicts of interest. In articles from three authors with conflicts of interest some of the same text was repeated word-for-word in different articles., Conclusion: There may be a connection between receiving industry funding for speaking, consulting, or research and the publication of promotional opinion pieces on menopausal hormone therapy., (© 2011 Fugh-Berman et al.)

Published
2011
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48. ILSI/HESI maternal toxicity workshop summary: maternal toxicity and its impact on study design and data interpretation.

Author

Beyer BK, Chernoff N, Danielsson BR, Davis-Bruno K, Harrouk W, Hood RD, Janer G, Liminga UW, Kim JH, Rocca M, Rogers J, and Scialli AR

Subjects
Animals, Body Weight, Embryonic Development, Female, Fetus pathology, Humans, Mice, Pregnancy, Prenatal Exposure Delayed Effects pathology, Rabbits, Rats, Maternal Exposure, Research Design, Statistics as Topic, Toxicity Tests methods
Abstract

Workshops on maternal toxicity were held at the annual Society of Toxicology, Teratology Society, and European Teratology Society meetings in 2009. Speakers presented background information prior to a general discussion on this topic. The following recommendations/options are based on the outcome of the discussions at the workshops: 1. A comprehensive evaluation of all available data from general toxicity studies, range-finding Developmental and Reproductive Toxicology (DART) studies, class effects, structure-activity relationships, exposure studies, etc. is essential for appropriate dose selection for definitive DART studies. The intent is to avoid marked maternal toxicity leading to mortality or decreased body weight gains of greater than 20% for prolonged periods. (a) Evaluate alternative endpoints for dose selection and data interpretation (e.g., target tissue effects and pharmacology) for biotherapeutics. (B) Evaluate additional maternal parameters based on effects and/or target organs observed in short-term (e.g., 2- or 4-week) general toxicity studies. 2. Evaluate all available data to determine a cause-effect relationship for developmental toxicity. (a) Conduct a pair-feeding/pair-watering study as a follow-up. (b) Evaluate individual data demonstrating maternal toxicity in the mother with adverse embryo-fetal outcomes in the litter associated with the affected mother. (c) Conduct single-dose studies at increasing doses as a complement to conventional embryo-fetal toxicity studies for certain classes of compounds that affect the hERG channel. 3. Support statements that embryo-fetal effects are caused by maternal toxicity and/or exaggerated pharmacology, especially for malformations. (a) Provide mechanistic or other supporting data. (b) Establish the relevance of the DART findings in animals for human exposures. Birth Defects Res (Part B) 92:36-51, 2010. © 2011 Wiley-Liss, Inc., (© 2010 Wiley-Liss, Inc.)

Published
2011
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49. A review of the literature on the effects of acetaminophen on pregnancy outcome.

Author

Scialli AR, Ang R, Breitmeyer J, and Royal MA

Subjects
Abnormalities, Drug-Induced, Animals, Female, Fetal Growth Retardation chemically induced, Gastroschisis chemically induced, Humans, Pre-Eclampsia chemically induced, Pregnancy, Premature Birth chemically induced, Acetaminophen adverse effects, Analgesics, Non-Narcotic adverse effects, Antipyretics adverse effects, Pregnancy Outcome
Abstract

Acetaminophen is commonly used during pregnancy. Experimental animal studies do not suggest increased malformations after therapeutic use of single-ingredient acetaminophen during pregnancy. Cohort studies in humans in which exposure is prospectively ascertained show no detectable increase in congenital malformation risk associated with single-ingredient acetaminophen use during pregnancy. A case-control study identified an association between acetaminophen use during pregnancy and risk of gastroschisis in the offspring, but the study was limited by recall bias, unblinded interviewers, possible misclassification of gastroschisis, confounding by indication, difficulty in separating out the effects of combination products, and possible selection bias. Two case-control studies failed to identify a statistically significant association between acetaminophen use during pregnancy and gastroschisis. No other malformation has been shown to be causally associated with single-ingredient acetaminophen. A reported association between pre-eclampsia, preterm birth, and acetaminophen may be explained by reverse causation. Concerns expressed about childhood asthma and prenatal acetaminophen use has been addressed in a separate review. The use of single-ingredient acetaminophen during pregnancy can be justified based on outcome data. Data on the effects of acetaminophen cannot necessarily be extended to acetaminophen combination products., (Copyright © 2010 Elsevier Inc. All rights reserved.)

Published
2010
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50. A different approach to validating screening assays for developmental toxicity.

Author

Daston GP, Chapin RE, Scialli AR, Piersma AH, Carney EW, Rogers JM, and Friedman JM

Subjects
Animals, Biological Assay, Dose-Response Relationship, Drug, Drug Evaluation, Preclinical methods, Embryo Culture Techniques, Embryo, Mammalian drug effects, Time Factors, Animal Testing Alternatives, Embryonic Development drug effects, Teratogens toxicity, Toxicity Tests methods, Validation Studies as Topic
Abstract

Background: There continue to be many efforts around the world to develop assays that are shorter than the traditional embryofetal developmental toxicity assay, or use fewer or no mammals, or use less compound, or have all three attributes. Each assay developer needs to test the putative assay against a set of performance standards, which traditionally has involved testing the assays against a list of compounds that are generally recognized as "positive" or "negative" in vivo. However, developmental toxicity is highly conditional, being particularly dependent on magnitude (i.e. dose) and timing of exposure, which makes it difficult to develop lists of compounds neatly assigned as developmental toxicants or not., Approach: Here we offer an alternative approach for the evaluation of developmental toxicity assays based on exposures. Exposures are classified as "positive" or "negative" in a system, depending on the compound and the internal concentration. Although this linkage to "internal dose" departs from the recent approaches to validation, it fits well with widely accepted principles of developmental toxicology., Conclusions: This paper introduces this concept, discusses some of the benefits and drawbacks of such an approach, and lays out the steps we propose to implement it for the evaluation of developmental toxicity assays., (© 2010 Wiley-Liss, Inc.)

Published
2010
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