Your search keyword '"Teratology methods"' showing total 66 results

1. Broad Spectrum epidemiological contribution of cannabis and other substances to the teratological profile of northern New South Wales: geospatial and causal inference analysis.

Author

Reece AS and Hulse GK

Subjects

Alcohol Drinking adverse effects, Cannabis adverse effects, Congenital Abnormalities diagnosis, Female, Humans, Male, Marijuana Use adverse effects, Mediation Analysis, New South Wales epidemiology, Tobacco Use adverse effects, Alcohol Drinking epidemiology, Congenital Abnormalities epidemiology, Geographic Information Systems, Marijuana Use epidemiology, Teratology methods, Tobacco Use epidemiology

Abstract

Background: Whilst cannabis commercialization is occurring rapidly guided by highly individualistic public narratives, evidence that all congenital anomalies (CA) increase alongside cannabis use in Canada, a link with 21 CA's in Hawaii, and rising CA's in Colorado indicate that transgenerational effects can be significant and impact public health. It was therefore important to study Northern New South Wales (NNSW) where cannabis use is high., Methods: Design: Cohort. 2008-2015., Setting: NNSW and Queensland (QLD), Australia., Participants: Whole populations. Exposures. Tobacco, alcohol, cannabis., Source: National Drug Strategy Household Surveys 2010, 2013., Main Outcomes: CA Rates. NNSW-QLD comparisons. Geospatial and causal regression., Results: Cardiovascular, respiratory and gastrointestinal anomalies rose with falling tobacco and alcohol but rising cannabis use rates across Queensland. Maternal age NNSW-QLD was not different (2008-2015: 4265/22084 v. 96,473/490514 > 35 years/total, Chi.Sq. = 1.687, P = 0.194). A higher rate of NNSW cannabis-related than cannabis-unrelated defects occurred (prevalence ratio (PR) = 2.13, 95%C.I. 1.80-2.52, P = 3.24 × 10 - 19 ). CA's rose more potently with rising cannabis than with rising tobacco or alcohol use. Exomphalos and gastroschisis had the highest NNSW:QLD PR (6.29(2.94-13.48) and 5.85(3.54-9.67)) and attributable fraction in the exposed (84.11%(65.95-92.58%) and 82.91%(71.75-89.66%), P = 2.83 × 10 - 8 and P = 5.62 × 10 - 15 ). In multivariable geospatial models cannabis was significantly linked with cardiovascular (atrial septal defect, ventricular septal defect, tetralogy of Fallot, patent ductus arteriosus), genetic (chromosomal defects, Downs syndrome), gastrointestinal (small intestinal atresia), body wall (gastroschisis, diaphragmatic hernia) and other (hypospadias) (AVTPCDSGDH) CA's. In linear modelling cannabis use was significantly linked with anal stenosis, congenital hydrocephalus and Turner syndrome (ACT) and was significantly linked in borderline significant models (model P < 0.1) with microtia, microphthalmia, and transposition of the great vessels. At robust and mixed effects inverse probability weighted multivariable regression cannabis was related to 18 defects. 16/17 E-Values in spatial models were > 1.25 ranging up to 5.2 × 10 13 making uncontrolled confounding unlikely., Conclusions: These results suggest that population level CA's react more strongly to small rises in cannabis use than tobacco or alcohol; cardiovascular, chromosomal, body wall and gastrointestinal CA's rise significantly with small increases in cannabis use; that cannabis is a bivariate correlate of AVTPCDSGDH and ACT anomalies, is robust to adjustment for other substances; and is causal.

Published

2020

2. Noncoding RNAs in development and teratology, with focus on effects of cannabis, cocaine, nicotine, and ethanol.

Author

Pinson MR and Miranda RC

Subjects

Animals, Cannabis adverse effects, Cocaine adverse effects, Ethanol adverse effects, Humans, Nicotine adverse effects, Teratology methods, Abnormalities, Drug-Induced genetics, Congenital Abnormalities genetics, Gene Regulatory Networks drug effects, RNA, Untranslated genetics

Abstract

Completion of the Human Genome Project has led to the identification of a large number of transcription start sites that are not paired with protein-coding genes, supporting the growing recognition of the abundance of encoded nonprotein-coding RNAs (ncRNAs) and their importance for speciation and species-specific development. Present in both plants and animals, ncRNAs vary in size, function, primary sequence, and secondary structure. While microRNAs (miRNAs) are the best known, there are a number of other ncRNAs (long[er] nonprotein-coding RNA, pseudogenes, circular RNAs, and so on) that have been shown to play an important role in the development either directly or via networks of proteins and other ncRNAs, including modulating the impact of miRNAs. Furthermore, these ncRNAs and their developmental regulatory networks are sensitive to teratogens such as ethanol, cannabis, cocaine, and nicotine. A better understanding of the developmental role of ncRNAs and their capacity to mediate teratogenesis is a necessary step in efforts to minimize the long-term consequences of developmental exposures to drugs-of-abuse. Moreover, with increasing awareness of the prevalence of polydrug use, experimental models will need to incorporate more complex drug exposure paradigms into meaningful assessments of developmental ncRNA function., (© 2019 Wiley Periodicals, Inc.)

Published

2019

3. Reversal of neurobehavioral teratogenicity in animal models and human: Three decades of progress.

Author

Yanai J, Vigoda MJ, and Ornoy A

Subjects

Animals, Behavior, Animal drug effects, Congenital Abnormalities physiopathology, Disease Models, Animal, Female, Humans, Nervous System Diseases physiopathology, Pregnancy, Prenatal Exposure Delayed Effects, Teratogens, Nervous System Diseases therapy, Teratology methods, Teratology trends

Abstract

Early studies of behavioral teratology were mostly descriptive, fulfilling the necessary first requirement in a new field. The next obvious stage was put forward in the 80's as mechanism driven science enabled reversal of the teratogens-induced deficits. Three decades later a plethora of studies have been published demonstrating the success of the new direction. Complete and long-term (ostensibly permanent) reversal has been demonstrated in numerous animal models representing the realization of the ultimate goal of the field. Perhaps less sought after, but still significant, are the studies on recovery which needs consistent treatment for its persistence The studies reviewed here have been summarized in Tables 1 and 2. Clinically, the field is only in its incipient stage because of the paucity in translational findings for complete reversal or even complete alleviation. Human findings are emerging but in partial alleviation, noteworthy were the demonstration of FASD children who showed improvement after choline treatment while others showed no effect. Consequently, while further studies in an animal model on the mechanism by which the teratogen exerts its deleterious effects and the reversal procedure action are important, the main thrust of the research should now be translation of the animal model findings into a standard clinical routine. Indeed, first steps towards these goals are being made in children with various neurodevelopmental disorders via the application of a variety of rehabilitation programs by physiotherapists, occupational therapists and speech and language therapists, but the results are partial and may not be long-lasting., (Copyright © 2019 Elsevier Inc. All rights reserved.)

Published

2019

4. First use of anatomical networks to study modularity and integration of heads, forelimbs and hindlimbs in abnormal anencephalic and cyclopic vs normal human development.

Author

Diogo R, Ziermann JM, Smith C, Alghamdi M, Fuentes JSM, and Duerinckx A

Subjects

Adult, Arm abnormalities, Arm growth & development, Female, Fetal Development physiology, Fetus abnormalities, Head abnormalities, Head growth & development, Homeostasis physiology, Humans, Infant, Newborn, Leg abnormalities, Leg growth & development, Male, Anencephaly physiopathology, Holoprosencephaly physiopathology, Musculoskeletal Development physiology, Teratogenesis physiology, Teratology methods

Abstract

The ill-named "logic of monsters" hypothesis of Pere Alberch - one of the founders of modern evo-devo - emphasized the importance of "internal rules" due to strong developmental constraints, linked teratologies to developmental processes and patterns, and contradicted hypotheses arguing that birth defects are related to a chaotic and random disarray of developmental mechanisms. We test these hypotheses using, for the first time, anatomical network analysis (AnNA) to study and compare the musculoskeletal modularity and integration of both the heads and the fore- and hindlimbs of abnormal cyclopic trisomy 18 and anencephalic human fetuses, and of normal fetal, newborn, and adult humans. Our previous works have shown that superficial gross anatomical analyses of these specimens strongly support the "logic of monsters" hypothesis, in the sense that there is an 'order' or 'logic' within the gross anatomical patterns observed in both the normal and abnormal individuals. Interestingly, the results of the AnNA done in the present work reveal a somewhat different pattern: at least concerning the musculoskeletal modules obtained in our AnNA, we observe a hybrid between the "logic of monsters" and the "lack of homeostasis" hypotheses. For instance, as predicted by the latter hypothesis, we found a high level of left-right asymmetry in the forelimbs and/or hindlimbs of the abnormal cyclopic trisomy 18 and anencephalic human fetuses. That is, a network analysis of the organization of/connection between the musculoskeletal structures of these fetuses reveals a more "chaotic" pattern than that detected by superficial gross anatomical comparisons. We discuss the broader developmental, evolutionary, and medical implications of these results.

Published

2019

5. Ethical approval for multicenter cohort studies on drug exposure during pregnancy: A survey among members of the European Network of Teratology Information Services (ENTIS).

Author

Winterfeld U, Weber-Schöndorfer C, Schaefer C, von Elm E, and Buclin T

Subjects

Abnormalities, Drug-Induced epidemiology, Abnormalities, Drug-Induced etiology, Adverse Drug Reaction Reporting Systems ethics, Cohort Studies, Ethics Committees, Research legislation & jurisprudence, Europe, Female, Humans, Multicenter Studies as Topic legislation & jurisprudence, Pregnancy, Prenatal Exposure Delayed Effects chemically induced, Prenatal Exposure Delayed Effects epidemiology, Surveys and Questionnaires, Teratology methods, Drug Information Services, Maternal Exposure ethics, Multicenter Studies as Topic ethics, Teratology ethics

Abstract

The European Network of Teratology Information Services (ENTIS) is in a privileged position to perform independent post-marketing surveillance of drugs in pregnancy. The aim of this survey was to describe the legal requirements and procedures involved in obtaining ethical approval for collaborative cohort studies. We sent a survey questionnaire to all 28 Teratology Information Services (TIS), of which 25 (89%) in 18 countries completed our questionnaire. For 15 TIS, specific research ethical approval was mandatory. The review process was estimated to last from 2 up to 16 weeks. Procedures for patients' information and consent were oral (12), written (5) or both (3). Five TIS had no requirement to inform patients and seek consent. Since data on drug exposure during pregnancy are scarce, ENTIS research efforts should be further encouraged, and procedures optimized so that legitimate ethical and legal requirements do not translate into deterrent administrative constraints and costs., (Copyright © 2018 Elsevier Inc. All rights reserved.)

Published

2018

6. A shortened study design for embryo-fetal development studies in the minipig.

Author

Pique C, Marsden E, Quesada P, Blondel A, and Mikkelsen LF

Subjects

Animals, Bone Development drug effects, Female, Pregnancy, Swine, Teratogens toxicity, Teratology economics, Time Factors, Embryo, Mammalian drug effects, Embryonic Development drug effects, Fetal Development drug effects, Research Design trends, Swine, Miniature, Teratology methods

Abstract

The minipig is accepted from scientific and regulatory perspectives for the safety evaluation of drug candidates on embryo-fetal development. The relative size and the duration of gestation (112-115 days) in the minipig is, however, considered a drawback compared with routine smaller species. We evaluated if study duration and cost could be optimized without impacting scientific validity by performing all terminal procedures around mid-gestation (60 days). At this stage, minipig fetal size is not too dissimilar to full term rabbit and therefore better suited to fetal processing/examination compared with at the end of gestation. Despite encountering higher than anticipated embryo-fetal death, morphological defects clearly associated with a known teratogen, pyrimethamine, were detected. Although the gonads are poorly differentiated macroscopically at mid-term, a histological examination confirmed that external sexing of the fetuses was accurate. Double staining of the bone and cartilage of the mid-term fetal skeleton allowed a more refined examination., (Copyright © 2018 Elsevier Inc. All rights reserved.)

Published

2018

7. Approach to evaluating pregnancy safety of anti-rheumatic medications in the OTIS MotherToBaby pregnancy studies: what have we learned?

Author

Chambers C, Johnson DL, and Kiernan E

Subjects

Antirheumatic Agents adverse effects, Case-Control Studies, Female, Humans, Pregnancy, Prospective Studies, Antirheumatic Agents analysis, Maternal Exposure adverse effects, Pregnancy Complications drug therapy, Rheumatic Diseases drug therapy, Teratogens analysis, Teratology methods

Abstract

For the last 30 years, pregnancy exposure studies, with varying methodologies, have been the mainstay of post-marketing surveillance for new drugs likely to be used by women of reproductive age. While they provide valuable data to inform use during pregnancy, they have limitations that render them necessary but not sufficient in supplying timely information to patients and prescribers. The Organization of Teratology Information Specialists MotherToBaby Pregnancy Studies' collaborative research group operates to help fill this gap. This paper provides an overview of the research that has been and is currently being conducted, as well as best practices determined over the past two decades. The Organization of Teratology Information Specialists MotherToBaby studies can provide earlier signaling with regard to concerns following possible teratogenic exposures, which when examined in conjunction with larger database studies and case-control designs, can move us closer to developing a fuller picture of drug safety for women of reproductive age.

Published

2018

8. Categorization of fetal external findings in developmental toxicology studies by the Terminology Committee of the Japanese Teratology Society.

Author

Izumi Y, Ooshima Y, Chihara K, Fujiwara M, Katsumata Y, and Shiota K

Subjects

Abnormalities, Drug-Induced diagnosis, Abnormalities, Drug-Induced physiopathology, Animals, Congenital Abnormalities pathology, Fetus, Humans, Japan, Mice, Rabbits, Rats, Societies, Scientific, Teratology methods, Toxicology methods, Abnormalities, Drug-Induced classification, Abnormalities, Drug-Induced veterinary, Congenital Abnormalities classification, Congenital Abnormalities veterinary, Teratogens toxicity, Terminology as Topic

Abstract

Categorization of fetal external findings in common laboratory animals, intended to make the agreement at Berlin Workshop in 2014 more practical, was proposed by the Terminology Committee of the Japanese Teratology Society at the Workshop in the 55th Japanese Teratology Society Annual Meeting in 2015. In the Workshop, 73 external findings, which had been categorized as "Gray zone" anomalies but not as "Malformation" or "Variation" in the 2014 Berlin Workshop, were discussed and classified as Malformation, "Non-structural abnormality," Variation, and "Not applicable." The proposal was based on the results of a survey conducted in 2014, where 20 facilities (including pharmaceutical, chemical, and pesticide companies and contract laboratories) and 2 selected expert teratologists in Japan were asked for their opinions on the categorization of these findings. Based on the discussion, Japanese Teratology Society members have agreed that 42 out of the 73 findings can be classified as Malformations (38), Non-structural abnormalities (3), Malformations/Non-structural abnormalities (1), and Variations (0), while the remaining 31 findings were recommended to be categorized as Not applicable for fetuses. The details of the classification are shown on the website of the Japanese Teratology Society (http://www.umin.ac.jp/cadb/External.pdf)., (© 2018 Japanese Teratology Society.)

Published

2018

9. Use of Human Embryoid Bodies for Teratology.

Author

Flamier A, Singh S, and Rasmussen TP

Subjects

Embryonic Stem Cells drug effects, Humans, Pluripotent Stem Cells drug effects, Toxicity Tests methods, Embryoid Bodies drug effects, Teratology methods

Abstract

Human birth defects are relatively common and can be caused by exposure to environmental teratogens or to pharmaceuticals with teratogenic activities. Human embryonic stem cells (hESCs), by virtue of their pluripotent nature, provide an excellent cellular platform for teratogen detection and risk assessment. This unit describes detailed protocols for the preparation and validation of highly pluripotent hESCs, the production of large quantities of aggregated multicellular spheroids composed of hESCs, and these spheroids' differentiation into embryoid bodies (EBs). EBs contain a variety of cells of endodermal, ectodermal, and mesodermal origin and can be subjected to compound exposure in vitro. Hence, they are useful for the detection of chemicals with teratogenic activities. Beyond describing protocols to assemble and culture EBs, this unit details methods to exploit the EB system for teratological assessment. In addition, strategies to distinguish compounds with bona fide teratogenic activity versus simple toxicity are discussed. © 2018 by John Wiley & Sons, Inc., (Copyright © 2018 John Wiley & Sons, Inc.)

Published

2018

10. Comparison of a modified mid-coronal sectioning technique and Wilson's technique when conducting eye and brain examinations in rabbit teratology studies.

Author

Ziejewski MK, Solomon HM, Rendemonti J, and Stanislaus D

Subjects

Animals, Brain embryology, Embryo, Mammalian abnormalities, Embryonic Development, Female, Fetus abnormalities, Rabbits, Brain abnormalities, Eye Abnormalities diagnosis, Teratology methods

Abstract

Background: There are two methods used when examining fetal rabbit eyes and brain in teratology studies. One method employs prior fixation before serial sectioning (Wilson's technique) and the other uses fresh tissue (mid-coronal sectioning)., Methods: We modified the mid-coronal sectioning technique to include removal of eyes and brain for closer examination and to increase the number of structures that can be evaluated and compared it to the Wilson's technique. We found that external examination of the head, in conjunction with either sectioning method, is equally sensitive in identifying developmental defects. We evaluated 40,401 New Zealand White (NZW) and Dutch-Belted (DB) rabbit fetuses for external head alterations, of which 28,538 fetuses were further examined for eye and brain alterations using the modified mid-coronal sectioning method (16,675 fetuses) or Wilson's technique (11,863 fetuses). The fetuses were from vehicle control or drug-treated pregnant rabbits in embryo-fetal development studies conducted to meet international regulatory requirements for the development of new drugs., Results: Both methods detected the more common alterations (microphthalmia and dilated lateral cerebral ventricles) and other less common findings (changes in size and/or shape of eye and brain structures)., Conclusions: While both methods are equally sensitive at detecting common and rare developmental defects, the modified mid-coronal sectioning technique eliminates the use of chemicals and concomitant fixation artifacts that occur with the Wilson's technique and allows for examination of 100% intact fetuses thereby increasing potential for detecting eye and brain alterations as these findings occur infrequently in rabbits., (© 2015 Wiley Periodicals, Inc.)

Published

2015

11. Imaging and morphology in reproductive toxicology - progress to date and future directions.

Author

French JM

Subjects

Animals, Drug Evaluation, Preclinical, Embryonic Development, Fetal Development, Diagnostic Imaging, Teratology methods, Toxicology methods

Abstract

This review looks at the recent development and application of imaging techniques for the morphological examination of fetuses from preclinical regulatory reproductive toxicology studies. Full replacement of the examination methods currently used in routine studies (microdissection, Bouin's fluid fixation/sectioning and alizarin red S/alcian blue preparations) by imaging techniques has yet to be achieved. Progress, especially in the application of micro-CT for skeletal examination, has been made but challenges, particularly the financial investment required, remain. Despite this apparent lack of progress the application of imaging techniques to "non-routine" preclinical reproductive toxicology studies has been used to good effect. The ability to acquire multiple images over a time course i.e. longitudinally has enabled the fate, particularly of skeletal features, to be determined. The additional evidence gained from such studies can be used to better inform the prenatal developmental hazard assessment of test compounds., (Copyright © 2014 Elsevier Inc. All rights reserved.)

Published

2014

12. Zebrafish models for assessing developmental and reproductive toxicity.

Author

He JH, Gao JM, Huang CJ, and Li CQ

Subjects

Animals, Behavior, Animal drug effects, Drug Evaluation, Preclinical, Larva drug effects, Larva growth & development, Reproduction drug effects, Teratogens toxicity, Zebrafish embryology, Models, Animal, Teratology methods, Zebrafish growth & development, Zebrafish physiology

Abstract

The zebrafish is increasingly used as a vertebrate animal model for in vivo drug discovery and for assessing chemical toxicity and safety. Numerous studies have confirmed that zebrafish and mammals are similar in their physiology, development, metabolism and pathways, and that zebrafish responses to toxic substances are highly predictive of mammalian responses. Developmental and reproductive toxicity assessments are an important part of new drug safety profiling. A significant number of drug candidates have failed in preclinical tests due to their adverse effect on development and reproductivity. Compared to conventional mammal testing, zebrafish testing for assessing developmental and reproductive toxicity offers several compelling experimental advantages, including transparency of embryo and larva, higher throughput, shorter test period, lower cost, smaller amount of compound required, easier manipulation and direct compound delivery. Toxicity and safety assessments using zebrafish have also been accepted by the FDA and EMEA for investigative new drug (IND) approval., (Copyright © 2014 Elsevier Inc. All rights reserved.)

Published

2014

13. Zebrafish model systems for developmental neurobehavioral toxicology.

Author

Bailey J, Oliveri A, and Levin ED

Subjects

Animals, Behavior, Animal physiology, Humans, Zebrafish abnormalities, Zebrafish growth & development, Behavior, Animal drug effects, Cognition drug effects, Disease Models, Animal, Embryo, Nonmammalian drug effects, Teratology methods, Toxicity Tests methods, Zebrafish physiology

Abstract

Zebrafish offer many advantages that complement classic mammalian models for the study of normal development as well as for the teratogenic effects of exposure to hazardous compounds. The clear chorion and embryo of the zebrafish allow for continuous visualization of the anatomical changes associated with development, which, along with short maturation times and the capability of complex behavior, makes this model particularly useful for measuring changes to the developing nervous system. Moreover, the rich array of developmental, behavioral, and molecular benefits offered by the zebrafish have contributed to an increasing demand for the use of zebrafish in behavioral teratology. Essential for this endeavor has been the development of a battery of tests to evaluate a spectrum of behavior in zebrafish. Measures of sensorimotor plasticity, emotional function, cognition and social interaction have been used to characterize the persisting adverse effects of developmental exposure to a variety of chemicals including therapeutic drugs, drugs of abuse and environmental toxicants. In this review, we present and discuss such tests and data from a range of developmental neurobehavioral toxicology studies using zebrafish as a model. Zebrafish provide a key intermediate model between high throughput in vitro screens and the classic mammalian models as they have the accessibility of in vitro models and the complex functional capabilities of mammalian models., (Copyright © 2013 Wiley Periodicals, Inc.)

Published

2013

14. Combined fertility and embryotoxicity study.

Author

Reynaud L and Marsden E

Subjects

Animal Husbandry, Animals, Autopsy, Cesarean Section, Female, Fetus cytology, Fetus drug effects, Fetus embryology, Fetus metabolism, Guidelines as Topic, Male, Mice, Organ Size drug effects, Pharmacokinetics, Pregnancy, Rats, Spermatozoa cytology, Spermatozoa drug effects, Spermatozoa physiology, Teratology standards, Toxicity Tests standards, Fertility drug effects, Teratogens toxicity, Teratology methods, Toxicity Tests methods

Abstract

Under normal circumstances, fertility and embryotoxicity studies are run separately according to the ICH S5(R2) guideline for the detection of toxicity to reproduction of medicinal products (1). However, the flexible approach of the S5(R2) guideline also allows the reproduction stages covered in the fertility and embryo-fetal development studies (stages A to D) to be combined into a single study design. The administration period covers the pre-mating and gestation phases through to closure of the hard palate. The principal advantages of the combined study include reductions in the number of animals required and cost. Although the rat is the routine species of choice, the mouse may also be used.

Published

2013

15. The enhanced pre- and postnatal development study for monoclonal antibodies.

Author

Weinbauer GF, Luft J, and Fuchs A

Subjects

Animals, Callithrix embryology, Female, Macaca fascicularis embryology, Male, Pregnancy, Prenatal Diagnosis, Antibodies, Monoclonal toxicity, Embryonic Development drug effects, Teratology methods, Toxicity Tests methods

Abstract

The enhanced pre- and postnatal (ePPND) study design has been developed in response to new scientific knowledge and subsequent guideline changes [ICH M3(R2) and ICH S6(R1)]. The changes in study design were basically driven by the experiences obtained during preclinical development of biopharmaceuticals. The standard ePPND concept does not apply to conventional small molecule pharmaceuticals. In essence, the ePPND design is a pre- and postnatal development (PPND) study in which key elements of an embryo-fetal development study are investigated in newborns and infants rather than in the fetus. The cynomolgus monkey is the current relevant nonhuman primate model. The ICH S6(R1) guideline reached step 5 in June 2011 and provides detailed recommendations on various parameters and the conduct of an ePPND study. This chapter provides working guidance for monitoring menstrual cycles to generate pregnant animals, ultrasound monitoring of pregnancy, morphometric measurements of fetuses and newborns, in vivo skeletal examination, various protocols for evaluation of infants (e.g., neurobehavioral assessment, learning and memory test, grip strength, immune system evaluation) and a comprehensive list of additional infant evaluation parameters for the cynomolgus monkey.

Published

2013

16. Teratology studies in the rat.

Author

Leroy M and Allais L

Subjects

Animal Husbandry, Animals, Autopsy, Cesarean Section, Female, Fetus abnormalities, Fetus drug effects, Fetus embryology, Fetus pathology, Humans, Male, Pharmacokinetics, Pregnancy, Rats, Teratology legislation & jurisprudence, Toxicity Tests standards, Teratology methods, Toxicity Tests methods

Abstract

The rat is the rodent species of choice for the regulatory safety testing of xenobiotics, such as medicinal products, food additives, and other chemicals. Many decades of experience and extensive data have accumulated for both general and developmental toxicology investigations in this species. The high fertility and large litter size of the rat are advantages for teratogenicity testing. The study designs are well defined in the regulatory guidelines and are relatively standardized between testing laboratories across the world. Teratology studies address maternal- and embryo-toxicity following exposure during the period of organogenesis. This chapter describes the design and conduct of a teratology study in the rat in compliance with the regulatory guidelines. The procedures for the handling and housing of the pregnant animals, the caesarean examinations and the sampling of fetuses for morphological examinations are described. The utility and design of preliminary studies and the inclusion of satellite animals in the main study for toxicokinetic sampling are discussed.

Published

2013

17. Developmental toxicity testing of vaccines.

Author

Barrow PC and Allais L

Subjects

Adjuvants, Immunologic toxicity, Animals, Female, Fertility drug effects, Government Regulation, Humans, Male, Pregnancy, Rabbits, Rats, Teratology legislation & jurisprudence, Vaccines immunology, Teratology methods, Toxicity Tests methods, Vaccines toxicity

Abstract

Preventative and therapeutic vaccines are increasingly used during pregnancy and present special considerations for developmental toxicity testing. The various components of the vaccine formulation (i.e., protein or polysaccharide antigen, adjuvants, and excipients) need to be assessed for direct effects on the developing conceptus. In addition, possible adverse influences of the induced antibodies on fetal and/or postnatal development need to be evaluated. A guidance document on the preclinical testing of preventative and therapeutic vaccines for developmental toxicity was issued by the FDA in 2006. Preclinical studies are designed to assess possible influences of vaccines on pre- and postnatal development. The choice of model animal for these experiments is influenced by species differences in the timing and extent of the transfer of the induced maternal antibodies to the fetus. The cross-placental transport of maternal immunoglobulins generally only occurs in late gestation and tends to be greater in humans and monkeys than in non-primate species. For many vaccines, the rabbit shows a greater rate of prenatal transfer of the induced antibodies than rodents. For biotechnology-derived vaccines that are not immunogenic in lower species, nonhuman primates may be the only appropriate models. It may be advisable to test new adjuvants using the ICH study designs for conventional pharmaceuticals in addition to the developmental toxicity study with the final vaccine formulation.

Published

2013

18. Reporting of teratology studies.

Author

Barrow PC and Reynaud L

Subjects

Animals, Humans, Mice, Quality Control, Rats, Statistics as Topic, Vocabulary, Research Design standards, Teratology methods

Abstract

The regulatory toxicology report is an unusual document that requires a particular skill to write. The report must be clear, accurate, concise, and focused. A clear and direct writing style is required. The end-users of the report will hope to find the information they seek with as little effort as possible. Few, or none, will read the entire document. The author should aim to appease the user by obliging him to read as little text and turn as few pages as possible. This chapter gives tips and guidance on how to present the experimental data and write the narrative text in the final study report for a teratology study.

Published

2013

19. Reproductive toxicity risk assessment for pesticides.

Author

Ulbrich B

Subjects

Animals, Dose-Response Relationship, Drug, Female, Humans, Male, Mice, Pregnancy, Rats, Risk Assessment, Safety, Social Control, Formal, Teratology legislation & jurisprudence, Toxicity Tests standards, Pesticides toxicity, Reproduction drug effects, Teratology methods, Toxicity Tests methods

Abstract

Human health risk assessment for pesticides is based mainly on animal studies submitted by the applicant and aims to determine safe exposure levels for operators (farmers and agricultural workers) and consumers of all age groups. Critical effects, including those resulting from reproductive toxicity, are identified during hazard assessment from an evaluation of all studies in the toxicity package. Reproductive or developmental effects are considered critical if they are more severe or occur at lower doses than other toxicities. Reference values for human exposure are then derived from No Adverse Effect Levels for the relevant critical effects by applying safety factors. This paper describes methods and caveats applicable to the evaluation of prenatal toxicity and two-generation studies from the view of a regulator, stressing the importance of individual litter data and the relationship between different endpoints.

Published

2013

20. The developmental toxicity testing of biologics.

Author

Hazelden KP

Subjects

Animals, Drug Evaluation, Preclinical standards, Guidelines as Topic, Humans, Toxicity Tests standards, Biological Products toxicity, Drug Evaluation, Preclinical methods, Teratology methods, Toxicity Tests methods

Abstract

The characteristics of biologic drugs, as compared with small molecules, confer significant advantages for both the drug developer and the prospective patients. The necessity for, and the timing of, developmental toxicity testing in the preclinical program must be considered. Choice of an appropriate test system is of particular importance, one that shows pharmacodynamic activity comparable to man. Where the conventional rodent/non-rodent species show such functional cross-reactivity, those species can be used in developmental testing, but often the only relevant species will be a nonhuman primate, in which case an extended study design (the ePPND) should be the default. Such an approach provides appropriate toxicity screening while reducing animal usage.

Published

2013

21. Zebrafish teratogenicity testing.

Author

Brannen KC, Charlap JH, and Lewis EM

Subjects

Animal Husbandry, Animals, Animals, Genetically Modified, Embryo, Nonmammalian abnormalities, Embryo, Nonmammalian drug effects, Environment, Controlled, Female, Gene Expression Regulation, Developmental drug effects, Injections, Male, Morpholinos genetics, RNA, Messenger genetics, RNA, Messenger metabolism, Zebrafish genetics, Teratology methods, Toxicity Tests methods, Zebrafish abnormalities, Zebrafish embryology

Abstract

As a model for teratogenicity research, zebrafish are gaining popularity and creditability. Zebrafish embryos have been proven to be a highly valuable tool in genetics and developmental biology research and have advanced our understanding of a number of known developmental toxicants. It has yet to be determined conclusively how reliably a zebrafish embryo screening assay predicts what will happen in mammalian models, but results from initial assessments have been encouraging. Here we have presented procedures for the basic care of a zebrafish colony to support embryo production, embryo collection and culturing, and teratogenicity experiments.

Published

2013

22. Teratology studies in the mouse.

Author

Marsden E and Leroy M

Subjects

Animal Husbandry, Animals, Autopsy, Cesarean Section, Female, Fetus abnormalities, Fetus drug effects, Fetus embryology, Fetus pathology, Male, Mice, Pharmacokinetics, Pregnancy, Teratology methods, Toxicity Tests methods

Abstract

The rat is the routine species of choice as the rodent model for regulatory safety testing of xenobiotics such as medicinal products, food additives, and other chemicals. However, the rat is not always suitable for pharmacological, toxicological, immunogenic, pharmacokinetic, or even practical reasons. Under such circumstances, the mouse offers an alternative for finding a suitable rodent model acceptable to the regulatory authorities. Since all essential routes of administration are possible, the short reproductive cycle and large litter size of the mouse make it a species well adapted for use in teratology studies. Given that good quality animals, including virgin mated females, can be acquired relatively easily and inexpensively, the mouse has been used in reproductive toxicity studies for decades and study protocols are well established.

Published

2013

23. Maternal toxicity.

Author

Danielsson BR

Subjects

Animals, Body Weight drug effects, Data Interpretation, Statistical, Fetus abnormalities, Fetus drug effects, Fetus embryology, Humans, Mothers, Teratology methods, Toxicity Tests methods

Abstract

Although demonstration of some degree of maternal toxicity is required in regulatory developmental toxicology studies, marked maternal toxicity may be a confounding factor in data interpretation. Reduction in maternal body weight gain is the far most frequently used endpoint of toxicity, but alternative endpoints, like organ toxicity or exaggerated pharmacological response, can also be taken into consideration. The following conclusions are based on literature data and discussions at maternal toxicity workshops attended by representatives from regulatory agencies, academia, and industry: (1) Available results do not support that maternal toxicity (defined as clinical signs, decreased body weight gain or absolute body weight loss of up to 15% in rats or 7% in rabbits) can be used to explain the occurrence of major malformations. (2) There is clear evidence that substantial reductions in maternal weight gain (or absolute weight loss) are linked with other manifestations of developmental toxicity. Among these can be mentioned decreased fetal weight, and skeletal anomalies (e.g., wavy ribs) in rats and decreased fetal weights, post implantation loss, abortions, and some skeletal anomalies in rabbits. (3) There are several examples of misinterpretation among companies, where it was incorrectly expected that regulatory authorities would not label chemicals/drugs as "teratogens/developmental toxicants" because embryo fetal adverse effects were only observed at doses also causing signs of maternal toxicity. (4) Similarly, even if mechanistic studies indicate that a substance causes developmental toxicity via exaggerated pharmacological effects in the mother, such a mechanism does not automatically negate the observed fetal adverse effects.From a regulatory perspective, an observed developmental toxic finding is considered to be of potential human relevance (even if it is mediated via maternal pharmacological effects or occur at doses causing signs of maternal toxicity) unless the company can provide appropriate mechanistic and/or other convincing evidence to the contrary.

Published

2013

24. Teratology testing under REACH.

Author

Barton S

Subjects

Animals, Data Interpretation, Statistical, Dose-Response Relationship, Drug, Humans, Legislation as Topic, Teratology legislation & jurisprudence, Guidelines as Topic, Teratology methods, Teratology standards, Toxicity Tests methods, Toxicity Tests standards

Abstract

REACH guidelines may require teratology testing for new and existing chemicals. This chapter discusses procedures to assess the need for teratology testing and the conduct and interpretation of teratology tests where required.

Published

2013

25. Frog embryo teratogenesis assay on Xenopus and predictivity compared with in vivo mammalian studies.

Author

Leconte I and Mouche I

Subjects

Animals, Embryo, Mammalian abnormalities, Embryo, Mammalian drug effects, Embryo, Nonmammalian abnormalities, Embryo, Nonmammalian drug effects, Female, Fetus abnormalities, Fetus drug effects, Male, Rabbits, Rats, Teratogens toxicity, Teratology legislation & jurisprudence, Teratology methods, Xenopus laevis embryology

Abstract

Frog embryo teratogenesis assay on Xenopus (FETAX) has been routinely used in our laboratory for the last 12 years as a routine developmental toxicity screening test for pharmaceutical candidate compounds. To date, out of more than 400 candidates tested in FETAX, around 60 have also been evaluated in mammalian embryotoxicity studies according to standard ICH protocols.Compound teratogenic potential in both FETAX and mammalian embryotoxicity studies is determined after analysis of the developmental toxicity characterized by embryotoxicity, growth delay, and/or potential to induce malformations. Based on this experience, the predictivity of FETAX is 81% with a minimal proportion of false positive results.

Published

2013

26. The teratology testing of food additives.

Author

Barrow PC and Spézia F

Subjects

Animals, Chemistry, Pharmaceutical, Dose-Response Relationship, Drug, Drug Administration Routes, Endpoint Determination, Female, Fetal Development drug effects, Food Additives administration & dosage, Food Additives chemistry, Government Regulation, Humans, Male, Mothers, Pregnancy, Rabbits, Rats, Reproduction drug effects, Species Specificity, Teratology legislation & jurisprudence, United States, United States Food and Drug Administration legislation & jurisprudence, Food Additives toxicity, Teratology methods, Toxicity Tests methods

Abstract

The developmental and reproductive toxicity testing (including teratogenicity) of new foods and food additives is performed worldwide according to the guidelines given in the FDA Redbook. These studies are not required for substances that are generally recognized as safe, according to the FDA inventory. The anticipated cumulated human exposure level above which developmental or reproduction studies are required depends on the structure-alert category. For food additives of concern, both developmental (prenatal) and reproduction (multigeneration) studies are required. The developmental studies are performed in two species, usually the rat and the rabbit. The reproduction study is generally performed in the rat. The two rat studies are preferably combined into a single experimental design, if possible. The test methods described in the FDA Redbook are similar to those specified by the OECD for the reproductive toxicity testing of chemicals.

Published

2013

27. Teratology studies in the rabbit.

Author

Allais L and Reynaud L

Subjects

Animal Husbandry, Animals, Autopsy, Cesarean Section, Female, Fetus abnormalities, Fetus cytology, Fetus drug effects, Fetus metabolism, Guidelines as Topic, Male, Pharmacokinetics, Pregnancy, Rabbits, Teratology standards, Toxicity Tests standards, Teratogens toxicity, Teratology methods, Toxicity Tests methods

Abstract

The rabbit is generally the non-rodent species or second species after the rat recommended by the regulatory authorities and is part of the package of regulatory reproductive studies for the detection of potential embryotoxic and/or teratogenic effects of pharmaceuticals, chemicals, food additives, and other compounds, including vaccines (see Chapters 1-7).Its availability, practicality in housing and in mating as well as its large size makes the rabbit the preferred choice as a non-rodent species. The study protocols are essentially similar to those established for the rat (Chapter 9), with some particularities. The study designs are well defined in guidelines and are relatively standardized between testing laboratories across the world.As for the rat, large litter sizes and extensive background data in the rabbit are valuable criteria for an optimal assessment of in utero development of the embryo or fetus and for the detection of potential external or internal fetal malformations.

Published

2013

28. The teratology testing of cosmetics.

Author

Spézia F and Barrow PC

Subjects

Animals, Cell Line, Embryo Culture Techniques, Embryonic Stem Cells drug effects, Government Regulation, Guidelines as Topic, Mesenchymal Stem Cells drug effects, Mice, Rats, Teratogens toxicity, Teratology legislation & jurisprudence, Toxicity Tests standards, Cosmetics toxicity, Teratology methods, Toxicity Tests methods

Abstract

In Europe, the developmental toxicity testing (including teratogenicity) of new cosmetic ingredients is performed according to the Cosmetics Directive 76/768/EEC: only alternatives leading to full replacement of animal experiments should be used. This chapter presents the three scientifically validated animal alternative methods for the assessment of embryotoxicity: the embryonic stem cell test (EST), the micromass (MM) assay, and the whole embryo culture (WEC) assay.

Published

2013

29. Toxicogenomic approaches in developmental toxicology testing.

Author

Robinson JF and Piersma AH

Subjects

Animals, Genome drug effects, Humans, Genomics methods, Teratology methods, Toxicity Tests methods

Abstract

The emergence of toxicogenomic applications provides new tools to characterize, classify, and potentially predict teratogens. However, due to the vast number of experimental and statistical procedural steps, toxicogenomic studies are challenging. Here, we guide researchers through the basic framework of conducting toxicogenomic investigations in the field of developmental toxicology, providing examples of biological and technical factors that may influence response and interpretation. Furthermore, we review current, diverse applications of toxicogenomic-based approaches in teratology testing, including exposure-response characterization (dose and duration), chemical classification studies, and cross-model comparisons study designs. This review is intended to guide scientists through the challenging and complex structure of conducting toxicogenomic analyses, while considering the many applications of using toxicogenomics in study designs and the future of these types of "omics" approaches in developmental toxicology.

Published

2013

30. Teratology studies in the minipig.

Author

McAnulty PA

Subjects

Animal Husbandry, Animals, Female, Fetus abnormalities, Male, Mothers, Pregnancy, Species Specificity, Swine, Swine, Miniature embryology, Teratology methods

Abstract

The minipig is a suitable species for regulatory teratology testing and may be regarded as an alternative to the rabbit, dog, and primate. The first successful regulatory teratology studies in the minipig were performed in the 1990s. It became clear that minipigs have several benefits over the other non-rodents, as they are purpose-bred for laboratory use, they are sexually mature at approximately 5 months of age, and they produce multiple offspring. The minipig has subsequently gained regulatory acceptance in the teratology testing of new drugs.

Published

2013

31. OTIS special issue preface.

Author

Chambers C and Friedman JM

Subjects

Female, History, 20th Century, History, 21st Century, Humans, Societies, Medical history, Teratology history, Teratology methods, Maternal Exposure adverse effects, Societies, Medical organization & administration, Teratogens toxicity, Teratology organization & administration

Published

2012

32. Physico-chemical properties mediating reproductive and developmental toxicity of engineered nanomaterials.

Author

Campagnolo L, Massimiani M, Magrini A, Camaioni A, and Pietroiusti A

Subjects

Animals, Female, Humans, Pregnancy, Teratology methods, Toxicity Tests methods, Embryonic Development drug effects, Nanoparticles chemistry, Nanoparticles toxicity, Nanostructures chemistry, Nanostructures toxicity, Reproduction drug effects

Abstract

With the increasing production of engineered nanomaterials (ENMs) exploited in many consumer products, a wider number of people is expected to be exposed to such materials in the near future, both in occupational and environmental settings. This has raised concerns about the possible implications on public health. In particular, very recently the scientific community has focused on the effect that ENMs might exert on the reproductive apparatus and on embryonic development. Indications that ENMs might have adverse effects on cells of the germ line and on the developing embryos have been reported. In the present minireview we will perform a critical analysis of the published work on reproductive and developmental toxicity of the most commonly used nanoparticles with a major focus on mammalian models. We will place emphasis on the main physico-chemical characteristics that can affect NP behaviour in biological systems, i.e. presence of contaminants and nanoparticle destabilization, size, dosage, presence of functional groups, influence of the solvent used for their suspension in biological media, aggregation/agglomeration, intrinsic chemical composition and protein corona/opsonisation. The importance of this specific field of nanotoxicology is documented by the rapidly increasing number of published papers registered in the last three years, which might be a consequence of the growing concerns on the possible interference of ENMs with reproductive ability and pregnancy outcome, in a time in which reproductive age has increased and the possibility to bear children appears reduced.

Published

2012

33. Introduction to zebrafish: current discoveries and emerging technologies for neurobehavioral toxicology and teratology.

Author

Levin ED and Tanguay RL

Subjects

Animals, Embryo, Nonmammalian drug effects, Larva, Nervous System embryology, Nervous System growth & development, Behavior, Animal drug effects, Models, Animal, Nervous System drug effects, Teratology methods, Toxicology methods, Zebrafish embryology, Zebrafish growth & development

Published

2011

34. In vivo imaging and quantitative analysis of changes in axon length using transgenic zebrafish embryos.

Author

Kanungo J, Lantz S, and Paule MG

Subjects

Animals, Axons metabolism, Axons ultrastructure, Embryo, Nonmammalian metabolism, Embryo, Nonmammalian ultrastructure, Ethanol toxicity, Green Fluorescent Proteins genetics, High-Throughput Screening Assays, Motor Neurons drug effects, Motor Neurons metabolism, Motor Neurons ultrastructure, Teratogens toxicity, Teratology methods, Toxicology methods, Zebrafish genetics, Zebrafish metabolism, Axons drug effects, Embryo, Nonmammalian drug effects, Image Processing, Computer-Assisted methods, Nerve Tissue Proteins genetics, Transcription Factors genetics, Transgenes, Zebrafish embryology, Zebrafish Proteins genetics

Abstract

We describe an imaging procedure to measure axon length in zebrafish embryos in vivo. Automated fluorescent image acquisition was performed with the ImageXpress Micro high content screening reader and further analysis of axon lengths was performed on archived images using AcuityXpress software. We utilized the Neurite Outgrowth Application module with a customized protocol (journal) to measure the axons. Since higher doses of ethanol (2-2.5%, v/v) have been shown to deform motor neurons and axons during development, here we used ethanol to treat transgenic [hb9:GFP (green fluorescent protein)] zebrafish embryos at 28 hpf (hours post-fertilization). These embryos express GFP in the motor neurons and their axons. Embryos after ethanol treatment were arrayed in 384-well plates for automated fluorescent image acquisition in vivo. Average axon lengths of high dose ethanol-treated embryos were significantly lower than the control. Another experiment showed that there was no significant difference in the axon lengths between the embryos grown for 24h at 22°C and 28.5°C. These test experiments demonstrate that using axon development as an end-point, compound screening can be performed in a time-efficient manner., (Published by Elsevier Inc.)

Published

2011

35. Fetal behavioral teratology.

Author

Visser GH, Mulder EJ, and Tessa Ververs FF

Subjects

Congenital Abnormalities etiology, Congenital Abnormalities physiopathology, Drug-Related Side Effects and Adverse Reactions, Female, Fetal Movement physiology, Humans, Mothers, Pregnancy, Stress, Psychological complications, Ultrasonography, Prenatal, Behavior physiology, Fetus physiology, Teratology methods

Abstract

Ultrasound studies of fetal motor behavior provide direct – in vivo – insight in the functioning of the motor component of the fetal central nervous system. In this article, studies are reviewed showing changes in the first timetable of appearance of fetal movements, changes in quality and/or quantity of movements and disturbances in the development of fetal behavioral states in case of endogenous malfunctions, maternal diseases and exogenous behavioral teratogens.

Published

2010

36. Report of the thirty-third annual meeting of the Neurobehavioral Teratology Society, 2009.

Author

Grant KS

Subjects

Animals, Behavioral Sciences methods, Biomedical Research methods, Biomedical Research trends, Environmental Exposure adverse effects, Hazardous Substances adverse effects, Humans, Neuropharmacology methods, Neurotoxins toxicity, Puerto Rico, Teratology methods, Toxicology methods, Behavioral Sciences trends, Neuropharmacology trends, Neurotoxicity Syndromes physiopathology, Teratology trends, Toxicology trends

Published

2010

37. Teratology: from science to birth defects prevention.

Author

Rasmussen SA, Erickson JD, Reef SE, and Ross DS

Subjects

Adult, Cytomegalovirus Infections prevention & control, Cytomegalovirus Infections virology, Female, Fetal Alcohol Spectrum Disorders etiology, Fetal Alcohol Spectrum Disorders prevention & control, Humans, Infant, Newborn, Neural Tube Defects etiology, Neural Tube Defects prevention & control, Pregnancy, Pregnancy Complications, Infectious prevention & control, Pregnancy Complications, Infectious virology, Rubella Syndrome, Congenital prevention & control, Rubella Syndrome, Congenital virology, Biomedical Research, Congenital Abnormalities etiology, Congenital Abnormalities prevention & control, Teratology methods

Abstract

One of the goals of birth defects research is to better understand risk or preventive factors for birth defects so that strategies for prevention can be developed. In this article, we have selected four areas of birth defects research that have led to the development of prevention strategies. These areas include rubella virus as a cause of congenital rubella syndrome, folic acid as a preventive factor for neural tube defects, cytomegalovirus infection as a cause of birth defects and developmental disabilities, and alcohol as a cause of fetal alcohol spectrum disorders. For each of these areas, we review key clinical and research findings that led to the identification of the risk or preventive factor, milestones in the development of prevention strategies, and the progress made thus far toward prevention.

Published

2009

38. Predictive teratology: teratogenic risk-hazard identification partnered in the discovery process.

Author

Augustine-Rauch KA

Subjects

Animals, Drug Design, Endothelin Receptor Antagonists, Humans, Risk Assessment, Structure-Activity Relationship, Drug-Related Side Effects and Adverse Reactions, Teratogens toxicity, Teratology methods

Abstract

Unexpected teratogenicity is ranked as one of the most prevalent causes for toxicity-related attrition of drug candidates. Without proactive assessment, the liability tends to be identified relatively late in drug development, following significant investment in compound and engagement in pre clinical and clinical studies. When unexpected teratogenicity occurs in pre-clinical development, three principle questions arise: Can clinical trials that include women of child bearing populations be initiated? Will all compounds in this pharmacological class produce the same liability? Could this effect be related to the chemical structure resulting in undesirable off-target adverse effects? The first question is typically addressed at the time of the unexpected finding and involves considering the nature of the teratogenicity, whether or not maternal toxicity could have had a role in onset, human exposure margins and therapeutic indication. The latter two questions can be addressed proactively, earlier in the discovery process as drug target profiling and lead compound optimization is taking place. Such proactive approaches include thorough assessment of the literature for identification of potential liabilities and follow-up work that can be conducted on the level of target expression and functional characterization using molecular biology and developmental model systems. Developmental model systems can also be applied in the form of in vitro teratogenicity screens, and show potential for effective hazard identification or issue resolution on the level of characterizing teratogenic mechanism. This review discusses approaches that can be applied for proactive assessment of compounds for teratogenic liability.

Published

2008

39. A hitchhiker's guide to the older literature of descriptive teratology.

Author

Beckwith JB

Subjects

Animals, Congenital Abnormalities, Databases, Bibliographic, Genetics history, History, 19th Century, History, 20th Century, Humans, Literature, Teratology history, Teratology methods

Abstract

Though relatively neglected in the age of molecular biology, the older literature of teratology includes superb illustrations and descriptions of malformations, and other information of permanent value to science and medicine. Accessing that literature can be challenging, as most is in works that are rare, published in languages other than English, and not available in digital form. This article describes some valuable sources of information concerning the antiquarian literature of descriptive teratology., ((c) 2007 Wiley-Liss, Inc.)

Published

2007

40. Omphalocele induction in the chick embryo by administration of cadmium.

Author

Thompson JM and Bannigan JG

Subjects

Abnormalities, Drug-Induced embryology, Animals, Hernia, Umbilical embryology, Hernia, Umbilical pathology, Lordosis chemically induced, Lordosis embryology, Somites drug effects, Species Specificity, Teratology methods, Abnormalities, Drug-Induced etiology, Acetates toxicity, Cadmium toxicity, Chick Embryo drug effects, Disease Models, Animal, Hernia, Umbilical chemically induced

Abstract

Background: Ventral body wall (VBW) defects occur in 1:2000 live births. We examined the association of VBW defect with somite abnormality and lordosis in the chick using in vitro and in ovo methods., Methods: Explanted chick embryos were treated at 60 hours with 50 microL sodium acetate or 0.001% cadmium acetate solution to produce VBW defects. Mortality and abnormality rates were assessed. A further cohort of chicks was treated in ovo by dropping 50 microL 0.001% to 0.01% cadmium acetate onto the embryo and allowing development to 16.5 days for further assessment of the defect and skeletal staining with alcian blue and alizarin red., Results: Cadmium treatment at 24 hours induced VBW defects in chicks treated in both shell-less culture and in ovo. Material herniating through the VBW defects was covered by a membrane in all fresh specimens. Membrane removal revealed large defects containing liver and bowel. These criteria clearly indicate that the defect observed is an omphalocele. Affected embryos had reduced somite numbers within 24 hours. Chicks exhibiting exomphalos at 16.5 days invariably had lumbosacral lordosis., Conclusions: The cadmium-treated chick embryo is a reliable model for exomphalos. A positive association was found between exomphalos and lumbar lordosis in the chick.

Published

2007

41. Embryonic cardiac arrhythmia and generation of reactive oxygen species: common teratogenic mechanism for IKr blocking drugs.

Author

Danielsson BR, Danielsson C, and Nilsson MF

Subjects

Abnormalities, Drug-Induced embryology, Abnormalities, Drug-Induced prevention & control, Animals, Anticonvulsants toxicity, Arrhythmias, Cardiac embryology, Arrhythmias, Cardiac metabolism, Arrhythmias, Cardiac prevention & control, Astemizole toxicity, Cisapride toxicity, Dimethadione toxicity, Ether-A-Go-Go Potassium Channels metabolism, Female, Free Radical Scavengers pharmacology, Free Radical Scavengers therapeutic use, Gastrointestinal Agents toxicity, Heart drug effects, Heart embryology, Histamine Antagonists toxicity, Humans, Hypoxia embryology, Hypoxia metabolism, Hypoxia prevention & control, Phenytoin toxicity, Pregnancy, Toxicity Tests, Abnormalities, Drug-Induced metabolism, Anti-Arrhythmia Agents toxicity, Arrhythmias, Cardiac chemically induced, Ether-A-Go-Go Potassium Channels antagonists & inhibitors, Hypoxia chemically induced, Potassium Channel Blockers toxicity, Reactive Oxygen Species metabolism, Teratology methods

Abstract

In the adult organism, it is well established that hypoxia followed by reperfusion may be fatal and result in generation of reactive oxygen species (ROS) and subsequent tissue damage. There is also considerable evidence that temporary decrease or interruption in oxygen supply to the embryo and ROS generation during reperfusion result in tissue damage in embryonic tissues. A wide spectrum of different malformations by transient embryonic hypoxia could be produced, depending on the duration, extent, and timing of the hypoxic event. It is the contention of this paper that drugs that block the potassium channel IKr, either as an intended pharmacologic effect or as an unwanted side-effect, are potentially teratogenic by a common ROS related mechanism. Drugs blocking the IKr channel, such as almokalant, dofetilide, phenytoin, cisapride and astemizole, do all produce a similar pattern of hypoxia-related malformations. Mechanistic studies show that the malformations are preceded by embryonic cardiac arrhythmia and periods of hypoxia/reoxygenation in embryonic tissues. Pretreatment or simultaneous treatment with radical scavengers with capacity to capture ROS, markedly decrease the teratogenicity of different IKr blocking drugs. A second aim of this review is to demonstrate that the conventional design of teratology studies is not optimal to detect malformations caused by IKr blocking drugs. Repeated high doses result in high incidences of embryonic death due embryonic cardiac arrhythmia, thus masking their teratogenic potential. Instead, single dosing on specific days is proposed to be a better way to characterize the teratogenic potential of Ikr blocking drugs.

Published

2007

42. Teratogenic effects of static magnetic field on mouse fetuses.

Author

Saito K, Suzuki H, and Suzuki K

Subjects

Animals, Brain abnormalities, Brain radiation effects, Female, Fetus abnormalities, Forelimb abnormalities, Forelimb radiation effects, Hindlimb abnormalities, Hindlimb radiation effects, Male, Maternal Exposure, Mice, Mice, Inbred Strains, Polydactyly embryology, Polydactyly etiology, Pregnancy, Ribs abnormalities, Ribs radiation effects, Stomach abnormalities, Stomach radiation effects, Temperature, Teratology methods, Electromagnetic Fields adverse effects, Fetal Development radiation effects, Fetus radiation effects

Abstract

A short period of exposure of pregnant mice to a strong static magnetic field of 400 mT -- 8000 times that of the earth -- in a dorso-ventral direction had teratogenic effects on developing fetuses. Fetuses were exposed to the static magnetic field in utero for 6 min on 1 day from 7.5 to 14.5 days of pregnancy. Exposed and control groups consisted of 10 pregnant mice each; thus 160 animals were used in total. Various malformations were observed in 15.1%, 13.4%, 15.8%, 16.7%, 20.8%, 24.3%, 24.4%, and 14.1% of fetuses exposed on days 7.5, 8.5, 9.5, I0.5, 11.5, 12.5, 13.5, and 14.5 of pregnancy, respectively. Types of malformations were polydactylism, abdominal fissure, fused rib, vestigial 13th rib, lumbar rib, brain hernia, and curled tail, while only a low incidence (up to 2.8%) of curled tail was detected in control group. These deformations apparently caused by SMF exposure but the effect did not reflect so-called exposure period specificity.

Published

2006

43. Gastrulating chick embryo as a model for evaluating teratogenicity: a comparison of three approaches.

Author

Drake VJ, Koprowski SL, Lough JW, and Smith SM

Subjects

Animals, Drug Evaluation, Preclinical methods, Models, Biological, Chick Embryo abnormalities, Chick Embryo drug effects, Gastrula, Teratogens toxicity, Teratology methods

Abstract

Background: Teratology studies must be carefully designed to minimize potential secondary effects of vehicle and delivery routes. A systematic method to evaluate chick models of early embryogenesis is lacking., Methods: We investigated 3 experimental approaches that are popular for studies of early avian development, in terms of their utility for teratogen assessment starting at gastrulation. These included in vitro embryo culture, egg windowing followed by direct application of a carrier vehicle to the embryo, and injection of a carrier vehicle into the egg yolk. We also developed a morphologically based scoring system to assess development of the early embryo., Results: The in vitro culture and egg windowing approaches both caused an unacceptably high incidence of central nervous system and cardiac abnormalities in vehicle-treated embryos, which made it difficult to identify teratogen-specific defects. In contrast, exposing chick embryos to vehicle via direct egg yolk injection did not induce developmental anomalies., Conclusions: Optimization of the exposure route of potential toxicants to the embryo is critical because control treatments can cause developmental anomalies. In ovo yolk injection minimizes perturbation of young embryos and may be appropriate for teratogen delivery., (Copyright (c) 2005 Wiley-Liss, Inc.)

Published

2006

44. The contribution of new findings and ideas to the old principles of teratology.

Author

Jelínek R

Subjects

Adult, Animals, Congenital Abnormalities genetics, Female, History, 19th Century, History, 20th Century, History, 21st Century, Humans, Pregnancy, Risk Assessment, Congenital Abnormalities etiology, Molecular Biology, Teratology history, Teratology methods

Abstract

Although the last generally accepted concept of principles of teratology was issued more than 30 years ago, the cause of less than 50% of all congenital anomalies is known and no substantial change in their incidence has been observed worldwide. In the meantime, powerful techniques of molecular biology as well as many sophisticated preventive measures have been introduced with marginal effects on the overall birth defects numbers. In this paper, we follow the history of basic concepts of teratology starting with Isidore Geoffroy Saint-Hilaire and Dareste, followed in the 20th century by James Wilson. Since that time no bright and completely new idea, which would deserve the name principle, has emerged. The advanced molecular studies support the long-existing principles and disclose the great variability of individuals and their responses to adverse exposures. In this way, the future of teratology counseling may be seen in a deep analysis of any individual case.

Published

2005

45. Morphological studies in modern teratological investigations.

Author

Burdan F, Szumiło J, Dudka J, Klepacz R, Błaszczak M, Solecki M, Korobowicz A, Chałas A, Klepacki J, Palczak M, Zuchnik-Wrona A, Hadała-Kiś A, Urbanowicz Z, and Wójtowicz Z

Subjects

Alcian Blue chemistry, Animals, Anthraquinones chemistry, Bone and Bones anatomy & histology, Bone and Bones chemistry, Coloring Agents chemistry, Female, Fetus drug effects, Humans, Maternal Exposure, Rats, Xenobiotics pharmacology, Fetus anatomy & histology, Teratology methods

Abstract

Despite the variety of modern molecular techniques available, examination of foetal anatomy is still a fundamental part of teratological studies in evaluating the developmental toxicity of xenobiotics or other non-chemical factors. The article presents contemporary methods of embryotoxicity and foetotoxicity assessment. A single alizarin red S and double alcian blue followed by alizarin red S staining, as well as various methods of soft tissue examination are discussed.

Published

2005

46. Application of the mouse exo utero development system in the study of developmental biology and teratology.

Author

Hatta T, Matsumoto A, and Otani H

Subjects

Animals, Cerebral Cortex embryology, Cerebral Cortex physiology, Extremities embryology, Extremities physiology, Female, Fetal Development physiology, Fibroblast Growth Factor 2 metabolism, Male, Mice, Developmental Biology methods, Embryo Research, Teratology methods

Abstract

The mouse exo utero development system is useful for analyzing the roles of molecules or interactions between tissues in the histogenesis of organs after the mid-gestational period. In the article presented here, we review the mouse exo utero development system and its specific modifications depending on different purposes as well as its advantages over and limitations compared to other systems in the study of developmental biology and teratology.

Published

2004

47. Radiofrequency fields and teratogenesis.

Author

Heynick LN and Merritt JH

Subjects

Animals, Environmental Exposure statistics & numerical data, Female, Hot Temperature, Humans, Pregnancy, Pregnancy Complications etiology, Reproduction radiation effects, Abnormalities, Radiation-Induced etiology, Body Temperature radiation effects, Embryonic and Fetal Development radiation effects, Environmental Exposure adverse effects, Fetal Viability radiation effects, Microwaves, Radio Waves, Teratology methods

Abstract

Experimental studies that sought teratologic effects or developmental abnormalities from exposure to radiofrequency electromagnetic fields (RFEMF) in the range 3 kHz-300 GHz are critically reviewed for their possible consequences on human health. Those studies were conducted on beetles, birds, rodents, and nonhuman primates. Collectively, those experimental studies indicate that teratologic effects can occur only from exposure levels that cause biologically detrimental increases in body temperature. No reliable experimental evidence was found for nonthermal teratologic effects; rodents, mouse fetuses, and perinatal mice are more susceptible to such effects than rats. The primary confirmed effect in rats at high RFEMF levels was initial weight deficits in fetuses and neonates that decreased with infant growth. More generally from findings with pregnant mammals, exposures at RFEMF levels far higher than those permitted under the IEEE human exposure guidelines are necessary to reach or exceed cited experimental thresholds for maternal temperature increases. Some results indicated that the levels necessary to cause such effects in pregnant mammals could exceed those lethal to the dams. In a behavioral study of squirrel monkeys, no effects were observed on usual dam-offspring interactions or EEGs, but unexpected deaths of a number of offspring had occurred. However, this finding was not confirmed in a study solely on infant death using a larger number of subjects for greater statistical validity. Also reviewed were epidemiologic studies of various human populations considered to have been chronically exposed to environmental levels of RFEMF. Early studies on the incidence of congenital anomalies yielded no credible evidence that chronic exposure of pregnant women or of fathers exposed to RFEMF from nearby sources at levels below those guidelines would cause any anomalies in their offspring. The findings of studies on pregnancy outcomes of female physiotherapists occupationally exposed while treating patients with RFEMF were mixed, but taken collectively, the findings were negative., (Published 2003 Wiley-Liss, Inc.)

Published

2003

48. Joint models for toxicology studies with dose-dependent number of implantations.

Author

Allen AS and Barnhart HX

Subjects

Abnormalities, Drug-Induced etiology, Animals, Dose-Response Relationship, Drug, Female, Fetal Death chemically induced, Fetal Resorption chemically induced, Male, Mice, Monte Carlo Method, Pregnancy, Risk, Teratogens toxicity, Embryo Implantation drug effects, Teratology methods

Abstract

Many chemicals interfere with the natural reproductive processes in mammals. The chemicals may prevent the fertilization of an egg or keep a zygote from implanting in the uterine wall. For this reason, toxicology studies with pre-implantation exposure often exhibit a dose-related trend in the number of observed implantations per litter. Standard methods for analyzing developmental toxicology studies are conditioned on the number of implantations in the litter and therefore cannot estimate this effect of the chemical on the reproductive process. This article presents a joint modeling approach to estimating risk in toxicology studies with pre-implantation exposure. In the joint modeling approach, both the number of implanted fetuses and the outcome of each implanted fetus is modeled. Using this approach we show how to estimate the overall risk of a chemical that incorporates the risk of lost implantation due to pre-implantation exposure. Our approach has several distinct advantages over previous methods: (1) it is based on fitting a model for the observed data and, therefore, diagnostics of model fit and selection apply; (2) all assumptions are explicitly stated; and (3) it can be fit using standard software packages We illustrate our approach by analyzing a dominant lethal assay data set (Luning et al., 1966, Mutation Research, 3, 444-451) and compare ourresults with those of Rai and Van Ryzin (1985, Biometrics, 41,1-9) and Dunson (1998, Biometrics, 54, 558-569). In a simulation study, our approach has smaller bias and variance than the multiple imputation procedure of Dunson.

Published

2002

49. Optimal designs for estimating the effective dose in developmental toxicity experiments.

Author

Krewski D, Smythe R, and Fung KY

Subjects

Abnormalities, Drug-Induced etiology, Animals, Dose-Response Relationship, Drug, Female, Fetal Death chemically induced, Mice, Models, Biological, Models, Statistical, Pregnancy, Rabbits, Rats, Risk Assessment, Teratogens toxicity, Teratology methods

Abstract

Recent advances in risk assessment have led to the development of joint dose-response models to describe prenatal death and fetal malformation rates in developmental toxicity experiments. These models can be used to estimate the effective dose corresponding to a 5% excess risk for both these toxicological endpoints, as well as for overall toxicity. In this article, we develop optimal experimental designs for the estimation of the effective dose for developmental toxicity using joint Weibull dose-response models for prenatal death and fetal malformation. Based on an extended series of developmental studies, near-optimal designs for prenatal death, malformation, and overall toxicity were found to involve three dose groups: an unexposed control group, a high dose equal to the maximum tolerated dose, and a low dose above or comparable to the effective dose. The effect on the optimal designs of changing the number of implants and the degree of intra-litter correlation is also investigated. Although the optimal design has only three dose groups in most cases, practical considerations involving model lack of fit and estimation of the shape of the dose-response curve suggest that, in practice, suboptimal designs with more than three doses will often be preferred.

Published

2002

50. Conceptual issues in behavioral teratology and their application in determining long-term sequelae of prenatal marihuana exposure.

Author

Fried PA

Subjects

Adolescent, Child Behavior Disorders diagnosis, Cognition Disorders diagnosis, Female, Follow-Up Studies, Humans, Male, Neuropsychological Tests, Pregnancy, Child Behavior Disorders epidemiology, Cognition Disorders epidemiology, Marijuana Abuse epidemiology, Mothers psychology, Prenatal Exposure Delayed Effects, Teratology methods

Abstract

Background: Behavioral teratology, particularly as it is applied to the evaluation of cognition and behavior of children beyond the toddler stage, has become an area of burgeoning activity. In the area of drug abuse, children exposed in utero are often at developmental peril because of non-drug pre- and postnatal risk factors that make a causal association between the drug of interest and a behavioral teratogenic outcome increasingly problematic as the child gets older., Methods: In the first portion of this review, the strategies that behavioral teratologists have undertaken to investigate the putative consequences of in utero exposure are discussed in terms of research design, statistical methods and interpretative approaches. In the second part of the paper, the relatively limited literature dealing with the behavioral teratological consequences of prenatal marihuana exposure, particularly in school age offspring, is reviewed., Results: An emergent theme arising from primarily two longitudinal investigations is that in utero cannabis exposure does not impact upon standardized derived IQ scores but is negatively associated with attentional behavior and visual analysis/hypothesis testing. These findings are interpreted as supporting the hypothesis that, among offspring beyond the toddler stage, prenatal marihuana exposure has a negative influence on aspects of executive function. Executive function is a 'top-down', multifaceted cognitive construct involved in organizing and integrating specific cognitive and output processes over a interval of time and is largely mediated by the late developing, prefrontal region of the brain., Conclusions: The results and the interpretation of the prenatal marihuana findings are discussed in terms of the behavioral teratogenic effects (or lack of effects) during the various developmental stages of the offspring, the non-unitary nature of executive function, cannabis receptors, and the consequences of chronic marihuana use in the non-pregnant population.

Published

2002