Prenatal exposure to sodium valproate and levetiracetam : consequences for neurodevelopmental outcomes?

Bromley, Rebecca

January 2012

Research has demonstrated that prenatal exposure to antiepileptic drugs is associated with an increased risk of physical malformations. The potential risk such exposure conveys to the developing brain and therefore the later cognitive functioning of the child is now the focus of both national and international research. This thesis investigated the relationship between prenatal exposure to antiepileptic drugs and child cognitive functioning. This investigation was undertaken in three phases: a systematic review of the published literature; an original research piece investigating prenatal exposure to sodium valproate and levetiracetam and finally a critical review of the research undertaken as part of this thesis and in the wider published literature. The systematic review identified 30 studies which had investigated the cognitive abilities of children with a history of prenatal exposure to antiepileptic drugs. Methodological quality of the studies was considered against the criteria of the Newcastle Ottawa Scale. Differential findings were noted across the antiepileptic drug types, with the largest number of studies documenting increased risks associated with prenatal exposure to sodium valproate. A lack of high quality research across all antiepileptic drugs, and in particular the more recently licensed antiepileptic drugs is highlighted. In the research paper presented here children aged between five and nine years of age exposed to either levetiracetam (n=37), sodium valproate (n=40) or who were born to women with epilepsy but did not require medication (n=43) were recruited from throughout the UK. Demographic and health information was collected from prospective records and supplemented with maternal interview. Formal standardised neuropsychological assessments were undertaken to inform on the child's current level of intellectual, memory, language, attentional and executive functioning. Following adjustment for variables likely to influence child cognitive ability, prenatal exposure to sodium valproate was found to be associated with poorer intellectual and language functioning in a dose dependent manner. When stratified by dose, 57.9% of children exposed to doses of sodium valproate above 800mg daily scored below the average range for their global intellectual ability. Prenatal exposure to levetiracetam was not found to be associated with poorer cognitive functioning. The critical review highlighted a number of methodological strengths of this research, despite time and resource implications. However, consideration should be given to the retrospective nature of this cohort and the potential for recruitment bias. This thesis concludes that women who require continuation of their treatment during pregnancy to control their seizures should be counselled regarding the risks and the benefits of their treatment to allow them to make informed decisions.

Epilepsy ; Pregnancy ; in utero exposure

Desenvolvimento e validação de método para análise de nicotina e cotinina em amostras de mecônio utilizando a cromatografia em fase gasosa acoplada à espectrometria de massas / Development and validation of a methodology for analysis of nicotine and cotinine in meconium samples using gas chromatography-mass spectrometry.

Barros, Luiza Saldanha Ribeiro

18 April 2011

O mecônio é uma matéria fecal que começa a acumular no intestino do feto por volta do terceiro mês de gestação e normalmente é eliminado nos primeiros dias de vida do recém nascido. No mecônio ocorre o acúmulo de substâncias com as quais a mãe entrou em contato durante o período de gestação e, portanto, sendo possível avaliar a exposição fetal. Nos casos de mães fumantes, compostos presentes no tabaco tais como nicotina e substâncias que são formadas após a metabolização da nicotina como por exemplo a cotinina, podem ser também detectadas nas amostras de mecônio, já que ocorre o acúmulo de nicotina e seus metabólitos no mesmo. O uso do cigarro durante o período gestacional acarreta em uma série de problemas ao feto como baixo peso ao nascer, parto pré-maturo, doenças no trato respiratório, dentre outros. Nos dias atuais é possível fazer a pesquisa de drogas lícitas e ilícitas em várias amostras biológicas tais como, sangue, urina, cabelo, fluido oral, mecônio, entre outras. O mecônio é uma boa opção, por vários motivos: amostragem fácil e não invasiva (a coleta pode ser feita na fralda), indica o histórico do uso de substâncias pela mãe durante a gestação por ser cumulativo, etc. O objetivo foi desenvolver e validar um método analítico empregando cromatografia em fase gasosa acoplada a espectrometria de massas para a determinação de nicotina e, seu metabólito, cotinina em amostras de mecônio coletadas de recém nascidos. Para o desenvolvimento do método foi utilizado 0,5g de mecônio e os analitos foram extraídos com metanol e em seguida a amostra foi submetida a purificação através da extração em fase sólida utilizando cartuchos Bond Elut Certify I. O método foi validado de acordo com os parâmetros estabelecidos pela ANVISA e demonstrou linearidade de 160 1600 ng/g para nicotina e de 160 1000 ng/g para cotinina. Os limites de detecção estabelecidos foram de 10 ng/g para nicotina e 60 ng/g para cotinina, enquanto os limites de quantificação foram de 60 ng/g para nicotina e 100 ng/g para cotinina. A exatidão apresentou valores de 91,73% a 103,73%, a precisão intra-ensaio variou entre 3,21% a 10,86%, e a precisão inter-ensaio obteve valores entre 4,91% a 9,88%. O método validado foi aplicado em amostras de mecônio coletadas no Hospital das Clínicas da Faculdade de Medicina de Ribeirão Preto (HCFMRP-USP). / Meconium is a fecal matter passed by the newborn after birth. It begins to form around the 3th month of gestation and accumulates in the fetus until birth. Substances which the mothers had contact during the gestation period may accumulate in meconium and, therefore, its possible to assess fetal exposure. Substances from the tobacco smoke, like nicotine and its metabolite cotinine, also accumulates in the meconium and can be detected .Maternal smoking during pregnancy is hazardous to the fetus and it is associated with low birth weight, prematurity, respiratory tract infections and others. Nowadays it is possible to assess licit and illicit drugs in several biological samples like blood, urine, hair, oral fluid, meconium and others. Meconium is the best choice because its easy to collect and its noninvasive, indicates a history of substances use by the mother in the latter half of pregnancy, etc. The purpose of this study was to develop and validate a methodology using gas chromatography-mass spectrometry to assess nicotine and cotinine in meconium samples collected from newborns. To the development of the methodology 0,5g of meconium was used per assay and the analytes were extracted from the matrix using methanol. Then, a solid phase extraction was applied using Bond Elut Certify I cartridges. The methodology was validated in the range of 160 1600 ng/g for nicotine and 160 - 1000 ng/g for cotinine. The limit of detection established was 10 ng/g for nicotine and 60 ng/g for cotinine, while the limit of quantification was 60 ng/g for nicotine and 100 ng/g for cotinine. The accuracy showed values between 91,73% and 103,73%, the intra-assay precision between 3,21% and 10,86% and the inter-assay precision between 4,91% and 9,88%. The validated methodology was applied to analysis of meconium samples collected from newborns in the Hospital das Clínicas da Faculdade de Medicina de Ribeirão Preto (HCFMRP-USP).

CG-EM

cotinina

cotinine

exposição intra-uterina

GC-MS

in utero exposure.

mecônio

meconium

nicotina

nicotine

Desenvolvimento e validação de método para análise de nicotina e cotinina em amostras de mecônio utilizando a cromatografia em fase gasosa acoplada à espectrometria de massas / Development and validation of a methodology for analysis of nicotine and cotinine in meconium samples using gas chromatography-mass spectrometry.

Luiza Saldanha Ribeiro Barros

18 April 2011

O mecônio é uma matéria fecal que começa a acumular no intestino do feto por volta do terceiro mês de gestação e normalmente é eliminado nos primeiros dias de vida do recém nascido. No mecônio ocorre o acúmulo de substâncias com as quais a mãe entrou em contato durante o período de gestação e, portanto, sendo possível avaliar a exposição fetal. Nos casos de mães fumantes, compostos presentes no tabaco tais como nicotina e substâncias que são formadas após a metabolização da nicotina como por exemplo a cotinina, podem ser também detectadas nas amostras de mecônio, já que ocorre o acúmulo de nicotina e seus metabólitos no mesmo. O uso do cigarro durante o período gestacional acarreta em uma série de problemas ao feto como baixo peso ao nascer, parto pré-maturo, doenças no trato respiratório, dentre outros. Nos dias atuais é possível fazer a pesquisa de drogas lícitas e ilícitas em várias amostras biológicas tais como, sangue, urina, cabelo, fluido oral, mecônio, entre outras. O mecônio é uma boa opção, por vários motivos: amostragem fácil e não invasiva (a coleta pode ser feita na fralda), indica o histórico do uso de substâncias pela mãe durante a gestação por ser cumulativo, etc. O objetivo foi desenvolver e validar um método analítico empregando cromatografia em fase gasosa acoplada a espectrometria de massas para a determinação de nicotina e, seu metabólito, cotinina em amostras de mecônio coletadas de recém nascidos. Para o desenvolvimento do método foi utilizado 0,5g de mecônio e os analitos foram extraídos com metanol e em seguida a amostra foi submetida a purificação através da extração em fase sólida utilizando cartuchos Bond Elut Certify I. O método foi validado de acordo com os parâmetros estabelecidos pela ANVISA e demonstrou linearidade de 160 1600 ng/g para nicotina e de 160 1000 ng/g para cotinina. Os limites de detecção estabelecidos foram de 10 ng/g para nicotina e 60 ng/g para cotinina, enquanto os limites de quantificação foram de 60 ng/g para nicotina e 100 ng/g para cotinina. A exatidão apresentou valores de 91,73% a 103,73%, a precisão intra-ensaio variou entre 3,21% a 10,86%, e a precisão inter-ensaio obteve valores entre 4,91% a 9,88%. O método validado foi aplicado em amostras de mecônio coletadas no Hospital das Clínicas da Faculdade de Medicina de Ribeirão Preto (HCFMRP-USP). / Meconium is a fecal matter passed by the newborn after birth. It begins to form around the 3th month of gestation and accumulates in the fetus until birth. Substances which the mothers had contact during the gestation period may accumulate in meconium and, therefore, its possible to assess fetal exposure. Substances from the tobacco smoke, like nicotine and its metabolite cotinine, also accumulates in the meconium and can be detected .Maternal smoking during pregnancy is hazardous to the fetus and it is associated with low birth weight, prematurity, respiratory tract infections and others. Nowadays it is possible to assess licit and illicit drugs in several biological samples like blood, urine, hair, oral fluid, meconium and others. Meconium is the best choice because its easy to collect and its noninvasive, indicates a history of substances use by the mother in the latter half of pregnancy, etc. The purpose of this study was to develop and validate a methodology using gas chromatography-mass spectrometry to assess nicotine and cotinine in meconium samples collected from newborns. To the development of the methodology 0,5g of meconium was used per assay and the analytes were extracted from the matrix using methanol. Then, a solid phase extraction was applied using Bond Elut Certify I cartridges. The methodology was validated in the range of 160 1600 ng/g for nicotine and 160 - 1000 ng/g for cotinine. The limit of detection established was 10 ng/g for nicotine and 60 ng/g for cotinine, while the limit of quantification was 60 ng/g for nicotine and 100 ng/g for cotinine. The accuracy showed values between 91,73% and 103,73%, the intra-assay precision between 3,21% and 10,86% and the inter-assay precision between 4,91% and 9,88%. The validated methodology was applied to analysis of meconium samples collected from newborns in the Hospital das Clínicas da Faculdade de Medicina de Ribeirão Preto (HCFMRP-USP).

CG-EM

cotinina

exposição intra-uterina

mecônio

nicotina

cotinine

GC-MS

in utero exposure.

meconium

nicotine

The effect of maternal exposure to alcohol and nicotine on pancreas and kidney size, aorta and carotid intima thickness and visceral fat in their children.

De Smidt, Juléy Janice Abigail

January 2019

Doctor Scientiae / In utero exposure to teratogens, increasing urbanization, rapid nutritional transition from poverty to affluence, adoption of a Western-style diet and physical inactivity have contributed to the growing obesity epidemic in the low-income countries. To investigate the associations between in utero exposure to alcohol and nicotine on the growth and development of children aged five years from a low-income setting. These effects will be observed in children aged five years as a reduced pancreas and kidney size, higher aorta and carotid intima thickness as well as higher visceral abdominal adiposity measurements.

Alcohol and nicotine

Utero exposure

Low-income setting

Children aged five years

Visceral fat

CIMT and cardiovascular risk in five-year-old children in a low socioeconomic population exposed to alcohol and nicotine during pregnancy: a case-control study

Hartel, Tammy Charlene

January 2020

Magister Scientiae (Medical Bioscience) - MSc(MBS) / Cardiovascular diseases (CVD) are among the top 10 causes of death in all ages in South Africa. The prevalence of maternal smoking and alcohol consumption during pregnancy is alarmingly high in South Africa. In utero exposure to nicotine and alcohol may cause CVD later in life. There is a global need for early detection of CVD especially those vulnerable during early childhood, to prevent the development of CVD risk factors in adulthood. The aim of this study was to compare CVD risk in five-year-old children from a low socio-economic population with in utero dual exposure to nicotine and alcohol and in utero nicotine exposure by measuring carotid intima-media thickness (cIMT), anthropometric measurements and clinical measurements including blood pressure. A case-control study was conducted on 468 children at five years old through interviews to collect data on demographic characteristics and health statistics. The cIMT was measured using B-mode ultrasonography. Anthropometric measurements were taken such as skinfold thickness, waist circumference, height and weight to calculate Body Mass Index (BMI). Blood pressure measurements such as systolic blood pressure (SBP), diastolic blood pressure (DBP), mean arterial pressure (MAP) and heart rate (HR) were taken. The data was analysed using SPSS version 26. Descriptive and inferential statistics (Spearman’s correlations, non-parametric partial correlations), Kruskal-Wallis H, Chi-square tests and logistic regression were used for statistical analysis. Results showed a significantly higher right cIMT (RcIMT) (0.36 ± 0.05 mm; P < 0.01) in children with in utero exposure to nicotine and alcohol during pregnancy and a higher RcIMT in males (0.37 ± 0.06 mm; P < 0.01) with in utero dual exposure to nicotine and alcohol when compared to females. A significant association was found between in utero dual exposure to nicotine and alcohol and a high RcIMT, specifically in females at five years old after the adjustment for confounders (B= -1.618, P = 0.002). Consequently, females in the dual exposed group were 7.6 times more likely to exhibit higher RcIMT with a relative risk of 2.6 times greater to children with no exposure. Females also had significantly higher SBP (U= 3829.50, p <0.01), DBP (U= 3527.50, p <0.05), MAP (U= 3561.00, p <0.05) and HR (U= 3887.50, p <0.01) in the dual exposed group. Cardiovascular risk factors were modestly prevalent at five years old in children with in utero teratogen exposures. However, increased adiposity indices were not observed in this population at five years old and were not associated with teratogen exposures. This may indicate that dual exposure to nicotine and alcohol has a significant effect on the intima-media thickness of the carotid arteries in children, but not necessarily on central and peripheral adiposity at five years old. Therefore, CVD risk factors need to be identified early in children in low socioeconomic regions with in utero exposure to nicotine and alcohol to prevent CVD later in life.

Alcohol

Cardiovascular risk

Children

Carotid intima-media thickness

In utero exposure

Low-income population

Nicotine

The Role of Prostaglandin H Synthase (PHS) Bioactivation and Nuclear Factor Erythroid 2-related Factor 2 (Nrf2)-Mediated Protection in Endogenous and Methamphetamine-initiated Neurotoxicity

Ramkissoon, Annmarie

24 July 2013

Endogenous brain compounds and xenobiotics, including the neurotoxins such as the amphetamine analogs 3,4-methylenedioxymethamphetamine (MDMA,Ecstasy), methamphetamine (METH, Speed) and methylenedioxyamphetamine (MDA, active metabolite of MDMA), may be bioactivated by prostaglandin H synthase (PHS) to free radicals that generate reactive oxygen species (ROS). In the absence of adequate antioxidant or repair mechanisms, ROS oxidize macromolecules such as DNA, protein and lipids, which can lead to toxicity. In vitro, we evaluated bioactivation using both purified ovine PHS-1 and cultured cells stably overexpressing either human PHS-1 or hPHS-2 isozymes. We found the neurotransmitter dopamine, its precursors and some metabolites, as well as METH and MDA, can be bioactivated by ovine and/or human PHS in an isozyme-dependent fashion that generates ROS, which oxidize DNA and protein and increase toxicity. This process is blocked by both the PHS inhibitor acetylsalicylic acid (ASA) and the ROS detoxifying enzyme catalase. Our data are the first to reveal isozyme-dependent bioactivation by PHS as a potential mechanism for enhanced susceptibility to both exogenous and endogenous neurotoxins, the latter of which may be particularly important in aging. METH-initiated ROS can also activate redox-sensitive transcription factors such as nuclear factor erythroid 2-related factor 2 (Nrf2), which is involved in the induction of an array of protective mechanisms in both adult and fetal brain. Using Nrf2 knockout mice, we showed Nrf2 has a novel neuroprotective role in METH-initiated oxidative stress, neurotoxicity and functional deficits in both fetal development and adulthood, especially with multiple exposures allowing time for the induction of neuroprotective mechanisms. Our studies are the first to show that Nrf2 afforded protection against both motor coordination deficits and olfactory deficits caused by METH in utero and in adults, suggesting that deficiencies in Nrf2 activation constitute a risk factor for ROS-mediated neurotoxicity in the fetus and adult.

cyclooxygenase

Nrf2

prostaglandin H synthase

oxidative stress

methamphetamine

neurotoxicity

fetal toxicity

in utero exposure

0383

0419

0307

0317

The Role of Prostaglandin H Synthase (PHS) Bioactivation and Nuclear Factor Erythroid 2-related Factor 2 (Nrf2)-Mediated Protection in Endogenous and Methamphetamine-initiated Neurotoxicity

Ramkissoon, Annmarie

24 July 2013

Endogenous brain compounds and xenobiotics, including the neurotoxins such as the amphetamine analogs 3,4-methylenedioxymethamphetamine (MDMA,Ecstasy), methamphetamine (METH, Speed) and methylenedioxyamphetamine (MDA, active metabolite of MDMA), may be bioactivated by prostaglandin H synthase (PHS) to free radicals that generate reactive oxygen species (ROS). In the absence of adequate antioxidant or repair mechanisms, ROS oxidize macromolecules such as DNA, protein and lipids, which can lead to toxicity. In vitro, we evaluated bioactivation using both purified ovine PHS-1 and cultured cells stably overexpressing either human PHS-1 or hPHS-2 isozymes. We found the neurotransmitter dopamine, its precursors and some metabolites, as well as METH and MDA, can be bioactivated by ovine and/or human PHS in an isozyme-dependent fashion that generates ROS, which oxidize DNA and protein and increase toxicity. This process is blocked by both the PHS inhibitor acetylsalicylic acid (ASA) and the ROS detoxifying enzyme catalase. Our data are the first to reveal isozyme-dependent bioactivation by PHS as a potential mechanism for enhanced susceptibility to both exogenous and endogenous neurotoxins, the latter of which may be particularly important in aging. METH-initiated ROS can also activate redox-sensitive transcription factors such as nuclear factor erythroid 2-related factor 2 (Nrf2), which is involved in the induction of an array of protective mechanisms in both adult and fetal brain. Using Nrf2 knockout mice, we showed Nrf2 has a novel neuroprotective role in METH-initiated oxidative stress, neurotoxicity and functional deficits in both fetal development and adulthood, especially with multiple exposures allowing time for the induction of neuroprotective mechanisms. Our studies are the first to show that Nrf2 afforded protection against both motor coordination deficits and olfactory deficits caused by METH in utero and in adults, suggesting that deficiencies in Nrf2 activation constitute a risk factor for ROS-mediated neurotoxicity in the fetus and adult.

cyclooxygenase

Nrf2

prostaglandin H synthase

oxidative stress

methamphetamine

neurotoxicity

fetal toxicity

in utero exposure

0383

0419

0307

0317

The Use of Environmental Justice Screening Tool and Self-Reported Data to Inform Pregnancy and Birth Outcomes in a Population of Central Ohio Deliveries

Bollinger, Claire Eastment

January 2017

No description available.

Public Health

Epidemiology

Environmental Health