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1 ivation, birthweight, maternal age, sex, and multiple birth.
2 dicator of higher embryo quality) on risk of multiple birth.
3 , maternal education, sex of the infant, and multiple births.
4  an intention-to-treat basis, accounting for multiple births.
5 erved elevated NTD risk was mediated through multiple births.
6 comes that are known to be more prevalent in multiple births.
7 with an aim toward reducing the incidence of multiple births.
8 iated with a substantial rise in the rate of multiple births.
9 s of twin births and triplet or higher-order multiple births.
10 ears), non-European American, or products of multiple births.
11  increase in the risk of low birth weight in multiple births.
12 other's age, method of delivery, parity, and multiple births.
13                                              Multiple births account for an increasing percentage of
14 rexia nervosa was independently predicted by multiple birth (adjusted hazard ratio = 1.33, 95% confid
15                      We derived the rates of multiple births after natural conception from data on di
16 proposed as a strategy to reduce the risk of multiple birth and adverse pregnancy outcomes after in-v
17 tion, are associated with increased risks of multiple birth and concomitant sequelae and adverse outc
18 ficantly longer with birthweight 2.0-2.5 kg, multiple birth and increasing maternal age.
19            With the exception of monozygotic multiple birth and maternal hypertensive disorder, early
20 ogistic, or quantile regression adjusted for multiple birth and socioeconomic risk.
21         We identified an association between multiple births and early menopause, which connects even
22                        Subgroup analyses for multiple births and preterm infants showed some differen
23 bryo transfer in the United States to reduce multiple births and related birth complications may be a
24                                Women who had multiple births and their babies were excluded.
25 antenatal corticosteroids, whether single or multiple birth, and birth weight.
26 uded cesarean-section delivery, birthweight, multiple birth, and infant survival status.
27       Gestational age at birth, birth order, multiple birth, and parental age were not associated wit
28   Prenatal smoking exposure, being part of a multiple birth, and prematurity were not associated with
29 ncy diabetes mellitus, preterm preeclampsia, multiple birth, and termination of pregnancy.
30                         Cesarean deliveries, multiple births, and births at less than 36 weeks' gesta
31  the youngest and oldest maternal age bands, multiple births, and deprivation (Index of Multiple Depr
32 t delivery, small for gestational age [SGA], multiple births, and male sex).
33 factors, in addition to GA at delivery, SGA, multiple births, and male sex.
34 s died, those with congenital abnormalities, multiple births, and mother and infant pairs who migrate
35 ity, household income, sex, gestational age, multiple births, and small for gestational age.
36 -binomial regression adjusted for race, sex, multiple birth, any maternal pregnancy risk factors (as
37  1.93), were primiparous (aOR = 2.03), had a multiple birth (aOR = 3.5), diabetes (aOR = 1.47), or ch
38 d their own estimate of the proportion of US multiple births attributable to non-ART ovulation stimul
39 ds that controlled for observed factors (eg, multiple birth, birth order, and parental sociodemograph
40 clinical and economic burden associated with multiple births can be prevented through single-embryo t
41 cle draws on official criminal histories for multiple birth cohorts spanning a 17-y difference in bir
42 lculations in consortia studies that include multiple birth cohorts.
43 crease in the age of asthma diagnosis across multiple birth cohorts.
44 lance data, they estimated proportions of US multiple births conceived naturally and by ART and assum
45 tion, history of CS, higher maternal age and multiple birth, consideration may be given to more conse
46            Almost 15% of inpatient costs for multiple births could have been avoided if ART twins and
47 as oral clefts, and individual patients with multiple birth defects (including clefts) have been show
48 rs in about 1 in 6000 live births and causes multiple birth defects in affected infants.
49 s are autosomal dominant disorders featuring multiple birth defects including ear, renal and branchia
50 ominant congenital disorder characterized by multiple birth defects including heart defects and myelo
51  Zika virus (ZIKV) is a flavivirus linked to multiple birth defects including microcephaly, known as
52 s an autosomal dominant disorder that causes multiple birth defects including renal, ear, anal and li
53                          Hug mutants exhibit multiple birth defects typical of ciliopathies, includin
54 ion or activation of Shh signalling leads to multiple birth defects, including holoprosencephaly, neu
55 e it is associated with an increased risk of multiple birth defects, the effect of paternal MTX expos
56 ated SMO and increased Hh signaling, causing multiple birth defects.
57  The risk of perinatal death associated with multiple births did not explain this finding.
58                The unprecedented increase in multiple births during the past 3 decades is a major pub
59  account for statistical dependence owing to multiple births during the study period.
60 d by (in order of statistical significance): multiple birth; eclampsia/pre-eclampsia; maternal age 40
61 h (2.7 [1.5-4.7]); the risks associated with multiple births explained some, but not all, of this exc
62 fter adjusting for parental age at delivery, multiple births, fetal sex, obstetric comorbidities, and
63 al number of 9873 live births were reported (multiple births from 1 pregnancy were counted as 1 live
64             Based on these data, the risk of multiple births from IVF varies by maternal age and numb
65 at birth, postmenstrual age at scan, sex, or multiple birth in these populations.
66 tments has led to an increase in the rate of multiple births in the United States.
67 t adjusted for GA, small-for-GA status, sex, multiple birth, inborn status, antenatal steroid use, an
68                    Compared with singletons, multiple-birth infants consume significantly more hospit
69 odevelopmental impairment or mortality among multiple-birth infants of mothers with diabetes (aRR = 1
70                              A total of 6925 multiple-birth infants were studied; 5775 of 6925 (83.4%
71 ave low or very low birthweight or be from a multiple birth; infants with repeat specimens were less
72  maternal factors (age, parity, singleton vs multiple birth, insurance, and race) and neighborhood fa
73 with the polycystic ovary syndrome, although multiple birth is a complication.
74        While the above-mentioned increase in multiple births is well documented, the impact on the tw
75              Cesarean delivery, primiparity, multiple births, low birth weight, and prematurity were
76              We compared rates of livebirth, multiple births, low birthweight (<2.5 kg), preterm birt
77 g children with none/low maternal education, multiple births, low birthweight, short birth interval,
78                               In Bangladesh, multiple birth measurements alone or in combination, par
79 eable to one or two ancestral proteins: "the multiple birth model" for the evolution of protein seque
80 nd higher S seroprevalences were observed in multiple births (odds ratio [OR], 0.84; 95% CI, 0.75-0.9
81 depression within 24 months before delivery, multiple births or stillbirth, or a diagnosis of breast
82 te 30.0/1,000) compared to 9,640 children of multiple births out of a total of 386,637 births in West
83 at diagnosis, birth weight, singleton versus multiple birth, parity, parental age, type of assisted c
84 the ART-NTD association was explained by the multiple-births pathway.
85 -reassuring fetal status, obstructed labour, multiple birth, placental weight >= 600 g, eclampsia/pre
86 a/abruptio placenta/ante-partum haemorrhage; multiple birth; pre-delivery LoS >= 3 days; placental we
87  conception and autism diagnosis mediated by multiple birth pregnancy and related birth complications
88                                              Multiple birth, preterm birth, and cesarean delivery joi
89 dds ratios and absolute risk differences for multiple birth, preterm birth, and low birthweight were
90 intensive use in 1981 and 1995 were having a multiple birth, primiparity, being married, and maternal
91 small for gestational age, mode of delivery, multiple birth, prolonged rupture of membranes, and cent
92 tion, small for GA status, mode of delivery, multiple birth, prolonged rupture of membranes, year of
93 6 eyes developing SROP, BW, gestational age, multiple births, race, per capita income in the mother's
94 cycles, ICSI use was associated with a lower multiple birth rate compared with conventional IVF (30.9
95         Among women aged 35 to 39 years, the multiple-birth rate was 29.4% if 3 embryos were transfer
96       Among women 40 to 44 years of age, the multiple-birth rate was less than 25% even if 5 embryos
97 through 2011 were used to determine national multiple birth rates, and data on in vitro fertilization
98                               Live-birth and multiple-birth rates (percentage of live births that wer
99  ART use worldwide and persistently high ART multiple-birth rates in several countries highlight the
100                                              Multiple-birth rates increased as high as 45.7% for wome
101                               Live-birth and multiple-birth rates may vary by patient age and embryo
102                                              Multiple-birth rates varied by age and the number of emb
103                  With 2 embryos transferred, multiple-birth rates were 22.7%, 19.7%, 11.6%, and 10.8%
104            Embryo quality was not related to multiple birth risk but was associated with increased li
105 plied a fetal survival factor, and used this multiple-birth risk estimate and their own estimate of t
106 transferring more than two embryos increased multiple-birth risk, with no corresponding increase in t
107        Greater maternal age did not decrease multiple-birth risk.
108 fer multiple embryos, but this increases the multiple-birth risk.
109 = 1.54; 95% CI: 0.95, 2.49), and monozygotic multiple birth (RR = 1.94; 95% CI: 1.26, 2.99).
110 , comorbidities, parity, whether there was a multiple birth, socioeconomic deprivation, and the prese
111 h weight, gestational age, maternal age, and multiple birth status.
112 luding by gestational age, type of delivery, multiple birth, study year, and perinatal mortality.
113 re used to estimate the annual proportion of multiple births that were attributable to IVF and to non
114                                        Among multiple births, the prevalence of rectal and large inte
115 ertility by 1) increasing the probability of multiple births through the transfer of multiple embryos
116 nal age is associated with decreased risk of multiple birth; using donor eggs from younger women may
117                              Being part of a multiple birth was strongly associated with early menopa
118                               Women having a multiple birth were much more likely to have had intensi
119                                     Rates of multiple birth were related to number of embryos transfe
120 ment, preterm birth, perinatal asphyxia, and multiple births were associated with an increased risk o
121                                    Trends in multiple births were examined starting from 1998, the ye
122 eonate deaths, stillbirths, and higher order multiple births were excluded from analysis.
123                                              Multiple birth, which is associated with adverse fetal,
124 ncreased occurrence of both miscarriages and multiple births, which has resulted in a great deal of c
125 sociation is mediated through the pathway of multiple births, while the ART-NTD association was expla
126     Since 1981, the percentage of women with multiple births who received intensive prenatal care (de

 
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