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1 ored regularly in such trials throughout the prenatal period.
2 ildren exposed to antidepressants during the prenatal period.
3 vide information on exposure timing over the prenatal period.
4 ngements in the brain takes place during the prenatal period.
5 ks would be highest for exposures during the prenatal period.
6 s of this malformation at any age, including prenatal period.
7 gluconeogenic enzymes are not induced in the prenatal period.
8 operating prior to conception and during the prenatal period.
9 ton species) after E16 through the remaining prenatal period.
10 children younger than 5 years and during the prenatal period.
11 perinatal period, driven by increases in the prenatal period.
12 ion of alcohol and tobacco cigarettes in the prenatal period.
13 ns for limiting fluoride exposure during the prenatal period.
14 ce for antibiotic stewardship throughout the prenatal period.
15 riptional atlas of SGN maturation across the prenatal period.
16 ears and fathers' asthma symptoms during the prenatal period.
17 egions of mantle dentine formed at different prenatal periods.
18 diagnostic work-ups during the neonatal and prenatal periods.
19 with autism during neonatal and potentially prenatal periods.
22 had claims documentation of a Z code in the prenatal period; 1.14%, within 60 days post partum; and
23 n of any Z code, measured separately for the prenatal period, 60 days post partum, 12 months post par
25 rtment [ED] visits) were measured during the prenatal period and at 60 days and 6 months post partum.
26 ests that environmental exposures during the prenatal period and early childhood years increase the r
29 re effective interventions are needed in the prenatal period and first 3 years after birth for the mo
30 xt] exposures by land use regression for the prenatal period and first seven postnatal years of 2,221
31 higher [Formula: see text] levels during the prenatal period and from the fourth postnatal year were
32 e farm animals, feed, and bedding during the prenatal period and in early infancy reduce the risk of
33 ) to RR = 0.76 (95%CI 0.72, 0.80) during the prenatal period and infancy; beta = 0.07 (95%CI 0.04, 0.
34 nterfere with perceptual learning during the prenatal period and provide additional evidence for an o
35 ect in allergy may be established during the prenatal period and that the protective effect may origi
36 influences neurodevelopment during critical prenatal periods and in the absence of environmental cha
37 n in the preconception period, 23 859 in the prenatal period, and 26 610 in the postpartum period.
38 ssed in neural tissue, especially during the prenatal period, and enriched for biological pathways in
39 ns of mouse fetuses following MIA during the prenatal period, and evaluated the behavioral and bioche
40 would occur more in the postpartum than the prenatal period, and would be more prevalent with bipola
42 s and lack of detailed information about the prenatal period are major problems with current approach
43 prenatal programming places interest in the prenatal period as a critical moment during which interv
44 al brain development to date, confirming the prenatal period as a time of considerable epigenomic pla
45 ng critical examination of preconception and prenatal periods as vulnerable to environmental insults
47 The authors explored this issue during the prenatal period by pharmacologically elevating physiolog
48 ism through which maternal stress during the prenatal period could impact offspring mental health, wi
49 sing OXTR expression along the course of the prenatal period culminating in a peak during early child
50 re than 40% of women hospitalized during the prenatal period for a bipolar or a psychotic condition w
51 e importance of maternal behavior during the prenatal period for the upbringing of healthy adults.
52 ys were more vulnerable to stress during the prenatal period, girls were more affected by postnatal s
53 ts from exposure to air pollution during the prenatal period have not been not fully elucidated, espe
54 ide neurotoxicity may be greatest during the prenatal period; however, previous studies have produced
55 that the availability of choline during the prenatal period influences neural and cognitive developm
59 c acid (DHA, 22:6n-3) supplementation in the prenatal period is associated with a reduction in the in
60 exposure to stressful life events during the prenatal period is associated with an increased risk of
62 enia and with accumulating evidence that the prenatal period is involved in the origins of this disea
64 However, treatment to the mother, in the prenatal period, may provide the possibility of preventi
68 y provides a basis for understanding how the prenatal period shapes future brain function and disease
71 rformance and exposure to mercury during the prenatal period, the neonatal period (birth to 28 days),
73 genetics and parental investments, from the prenatal period through to adulthood, using data from si
74 ntestinal microbiome affects health from the prenatal period throughout childhood, and many diseases
76 child, mother, and partner from the child's prenatal period to age 10 years using data from 8467 par
78 in human post-mortem brain samples, from the prenatal period to late adulthood, we demonstrate distin
79 ion strategies for chronic diseases from the prenatal period to old age, contributing to evidence-bas
81 environmental exposures beginning during the prenatal period) to identify modifiable factors that aff
82 toneal (IP) injection or in utero during the prenatal period via dam subcutaneous (SC) injection resp
85 ignaling required for lung maturation in the prenatal period were epigenetically deregulated and coul
88 ensitive to thyroid hormone during the early prenatal period, when the fetus is entirely dependent on
90 climate factors, and green space during the prenatal period with respiratory diseases in infants.
91 ents presented with BRA, detected during the prenatal period, without additional recognizable malform