Hostname: page-component-586b7cd67f-t7czq Total loading time: 0 Render date: 2024-11-23T23:25:37.077Z Has data issue: false hasContentIssue false
  • English
  • Français

Neurodevelopmental Outcome Among Multiples and Singletons: A Regional Neonatal Intensive Care Unit's Experience in Turkey

Published online by Cambridge University Press:  21 January 2013

Zeynep Eras ,
Banu Mutlu Ozyurt ,
Gozde Kanmaz ,
Omer Erdeve ,
Evrim Durgut Sakrucu ,
Serife Suna Oguz ,
Fuat Emre Canpolat ,
Nurdan Uras  and
Ugur Dilmen
Zeynep Eras*
Affiliation:
Department of Developmental Behavioral Pediatrics, Zekai Tahir Burak Maternity Teaching and Research Hospital, Ankara, Turkey
Banu Mutlu Ozyurt
Affiliation:
Department of Developmental Behavioral Pediatrics, Zekai Tahir Burak Maternity Teaching and Research Hospital, Ankara, Turkey
Gozde Kanmaz
Affiliation:
Department of Developmental Behavioral Pediatrics, Zekai Tahir Burak Maternity Teaching and Research Hospital, Ankara, Turkey
Omer Erdeve
Affiliation:
Department of Developmental Behavioral Pediatrics, Zekai Tahir Burak Maternity Teaching and Research Hospital, Ankara, Turkey
Evrim Durgut Sakrucu
Affiliation:
Department of Developmental Behavioral Pediatrics, Zekai Tahir Burak Maternity Teaching and Research Hospital, Ankara, Turkey
Serife Suna Oguz
Affiliation:
Department of Developmental Behavioral Pediatrics, Zekai Tahir Burak Maternity Teaching and Research Hospital, Ankara, Turkey
Fuat Emre Canpolat
Affiliation:
Department of Developmental Behavioral Pediatrics, Zekai Tahir Burak Maternity Teaching and Research Hospital, Ankara, Turkey
Nurdan Uras
Affiliation:
Department of Developmental Behavioral Pediatrics, Zekai Tahir Burak Maternity Teaching and Research Hospital, Ankara, Turkey
Ugur Dilmen
Affiliation:
Department of Developmental Behavioral Pediatrics, Zekai Tahir Burak Maternity Teaching and Research Hospital, Ankara, Turkey
*
address for correspondence: Zeynep Eras, MD, Department of Developmental Behavioral Pediatrics, Zekai Tahir Burak Maternity Teaching Hospital, 06230 Ankara, Turkey. E-mail: [email protected]

Abstract

Objective: The aim of this study was to compare the neurodevelopmental outcome at 12–18 months’ corrected age between multiples and singleton preterm infants. Methods: We designed a prospective study of preterm infants (≤32 weeks gestation) born and hospitalized in the neonatal intensive care unit between November 2008 and November 2009, whose assessments were performed at 12–18 months’ corrected age. Neurodevelopmental impairment was defined as the presence of any one of the following: moderate or severe cerebral palsy, severe bilateral hearing loss or bilateral blindness, mental developmental index score, or psychomotor developmental index score less than 70. Results were compared for both multiples and singleton infants. Results: One hundred and fifty-nine multiples and 211 singleton infants were assessed at 12–18 months’ corrected age. The neurodevelopmental outcome including all parameters at 12–18 months’ corrected age in multiples was not significantly different from singleton preterm infants. Conclusions: Multiple gestation in preterm infants is not associated with an increased risk of neurodevelopmental impairment at 12–18 months’ corrected age compared with singleton preterm infants. For further information, long term and high participation in neurodevelopmental follow-up and evaluation at pre-school age will be needed.

Keywords

pretermmultiple birthtwinneurodevelopmental outcome
Type
Articles
Information
Twin Research and Human Genetics , Volume 16 , Issue 2 , April 2013 , pp. 614 - 618
Copyright
Copyright © The Authors 2013

Over the past two decades, there has been a regular increase in the incidence of preterm births all over the world, with a range of 7–13% (Hamilton et al., Reference Hamilton, Martin and Ventura2006). Most of this increase was due to an increase in multiple gestations because of the use of assisted reproductive medicine (Asztalos et al., Reference Asztalos, Barrett, Lacy and Luther2001; Klebanoff & Keim, Reference Klebanoff and Keim2011; Shinwell, Reference Shinwell2002). Currently, 3–4.5% of all births are multiple births (Martin et al., Reference Martin, Kung, Mathews, Hoyert, Strobino, Guyer and Sutton2008). Among very low birth weight (VLBW) infants, the percentage of multiples increased from 19% to 26% between 1997 and 2002 (Fanaroff et al., Reference Fanaroff, Stoll, Wright, Carlo, Ehrenkranz, Stark and Poole2007). Advances in neonatal intensive care have resulted in improved survival of preterm (≤32 weeks’ gestational age) and VLBW infants (≤1,500 g) born from singleton and multiple gestations (Tamaru et al., Reference Tamaru, Kikuchi, Takagi, Wakamatsu, Ono, Horikoshi, Kihara and Nakamura2011; Wilson-Castello et al., Reference Wilson-Castello, Friedman, Minich, Fanaroff and Hack2005).

Long-term morbidity of multiples may differ from singletons because of the greater incidence of prematurity and intrauterine growth retardation (IUGR) in multiples (Asztalos et al., Reference Asztalos, Barrett, Lacy and Luther2001; Ingram Cooke, Reference Ingram Cooke2010). However, studies about morbidities have shown conflicting results related to outcomes. Some of the studies have emphasized that multiples are at greater risk for long-term problems in their growth and development, including cerebral palsy (CP), cognitive impairment, language delay, and learning disabilities (Blickstein & Keith, Reference Blickstein and Keith2003; Bonellie et al., Reference Bonellie, Currie and Chalmers2005; Ingram Cooke, Reference Ingram Cooke2010; Suri et al., Reference Suri, Bhandari, Lerer, Rosenkrantz and Hussain2001; Sutcliffe & Derom, Reference Sutcliffe and Derom2006; The ESHRE Capri Workshop Group, 2000; Wadhawan et al., Reference Wadhawan, Oh, Perritt, McDonald, Das, Poole, Vohr and Higgins2009). However, other studies have found no significant differences in the incidence of major morbidity between singletons and multiples, and it has been suggested that a higher neonatal adverse outcome rate was not seen when VLBW twins and singleton infants were studied adjusting for birth weight (Asztalos et al., Reference Asztalos, Barrett, Lacy and Luther2001; Donovan et al., Reference Donovan, Ehrenkranz, Shankaran, Stevenson, Wright, Younes and Papile1998; Hajnal et al., Reference Hajnal, Braun-Fahrländer, von Siebenthal, Bucher and Largo2005).

The objective of our study was to present the neurodevelopmental outcome of a single-center cohort of multiple preterm infants born at ≤32 weeks gestational age in a one-year period in Turkey and compare the neurodevelopmental outcome among those and singleton preterm infants.

Materials and Methods

This was a prospective cohort study of preterm infants (≤32 weeks gestational age) born and hospitalized at Zekai Tahir Burak Maternity Teaching Hospital neonatal intensive care unit (NICU) between November 2008 and November 2009. Infants (n = 370) were categorized into two groups: singletons and multiple births. Data on infant perinatal characteristics were collected from the medical records. The infants were followed up to 12–18 months’ corrected age (CA) by a neonatologist and a pediatrician.

The outcome of our study was the neurodevelopmental comparison of the two groups. A comprehensive assessment at 12–18 months’ CA was performed, consisting of the following evaluation: hearing, vision, neurologic, and development.

Hearing status was obtained by audiological test results. Eye examinations were performed by an ophthalmologist who was expert in assessing VLBW preterm infants. Physical and neurological examinations were performed by a pediatrician, and the presence of CP, bilateral blindness or deafness was recorded. Diagnosis of CP, including diplegia, quadriplegia, and hemiplegia, was based on the presence of hypertonicity, hyperreflexia, and dystonic or spastic movement in the involved extremities. Developmental assessment was performed with the Bayley Scales of Infant Development II for subjects up to 42 months (Bayley, Reference Bayley1993), and the Mental Developmental Index (MDI) and Psychomotor Developmental Index (PDI) were also used. Neurodevelopmental impairment was defined as the presence of any one of the following: CP, bilateral blindness, bilateral deafness, MDI or PDI scores on the Bayley II Scales of Infant Development < 70. All evaluations were performed by certified and experienced examiners who were blinded to both groups.

The study protocol was approved by the local ethical committee and study participation by written consent was obtained from all parents.

Statistical Analysis

Statistical analysis was performed with the SPSS 16.0 statistical package. The χ2 test was used for categorical variables and a t test was used for continuous variables. A p value of <.05 was considered significant.

Results

A total of 780 preterm infants born at ≤32 weeks gestational age were admitted to our NICU during the study period. Of these, 487 were singletons and 293 were multiples. During the NICU stay, 85 singletons and 40 multiples died. The developmental test could not be performed for 191 singletons and 94 multiples, either because of incomplete follow-up (68 singletons and 31 multiples) or because the parents did not wish to participate (72 singletons and 28 multiples) or because of lost follow-up (51 singletons and 35 multiples). As a result, 211 singletons and 159 multiples were approached for this prospective follow-up study and assessed at 12–18 months’ CA (Figure 1).

FIGURE 1 Flowchart of the study population.

In the singleton group (n = 211), the mean birth weight was 1,200 ± 271 g and 53 (25.1%) infants were ≤1,000 g. Their mean gestational age was 29.0 ± 2.3 weeks and 93 (44.1%) infants were of ≤28 weeks gestation. In the multiples group (n = 159), the mean birth weight was 1,311 ± 316 g and 29 (18.2%) infants were ≤1,000 g. Their mean gestational age was 29.8 ± 2.1 weeks and 49 (30.8%) were ≤28 weeks gestation. The mean birth weight and gestational age were significantly lower in the singletons group than in the multiples (p < .01 and p < .05).

Table 1 shows perinatal characteristics of the study infants. There were no significant differences in perinatal characteristics such as respiratory distress syndrome (RDS), patent ductus arteriosus (PDA), necrotizing enterocolitis (NEC), sepsis, bronchopulmonary disease (BPD), grade 3–4 intraventricular hemorrhage (IVH), and hydrocephalus between the two groups, except that preterm infants in the singleton group were more likely to have retinopathy than in the multiples group (p < .05).

TABLE 1 Perinatal Characteristics of Infants

BPD = bronchopulmonary disease; IVH: intraventricular hemorrhage; NEC = necrotizing enterocolitis; PDA = patent ductus arteriosus; RDS = respiratory distress syndrome.

Of the surviving infants, 211 (52.5%) singleton and 159 (62.8%) multiple preterm infants were assessed at a mean age of 16.7 ± 2.1 months. The mean of the MDI scores was 96.1 ± 21.1 in the singleton group and 99.0 ± 20.4 in the multiples group. The mean of the PDI scores was 94.3 ± 21.9 in the singleton group and 89.7 ± 22.7 in the multiples group. There were no significant differences between groups for mean MDI and PDI scores (p = .58 and .079, respectively).

The neurosensory outcomes of the singletons and multiples at 12–18 months’ CA are shown in Table 2. Cerebral palsy was present in 7 (3.3%) of 211 singletons and in 7 (4.4%) of 159 multiples; no significant difference was found between the groups (p = .60) for CP rate. In our cohort, there was no infant who was diagnosed as blind or deaf. Fifteen percent of singletons and 8.2% of multiples had MDI scores <70. Twenty percent of singletons and 18.2% of multiples had PDI scores <70. Among those with MDI scores and PDI scores <70, the number of infants did not differ in singletons compared to multiples (p = .089, p = .067). The proportion of patients who had neurodevelopmental impairment at 12–18 months’ CA (CP, deafness or blindness, MDI < 70, PDI < 70) was 26.5% in singletons and 18.2% in multiples; the difference was not statistically significant (p = .06).

TABLE 2 Long-Term Outcomes of Study Infants at 12–18 Months Corrected Age

CP = cerebral palsy; MDI = Mental Developmental Index; PDI = Psychomotor Developmental Index.

Discussion

Multiple gestation is associated with a higher prematurity rate and a higher incidence of VLBW. In many of the studies, infants born from multiple gestation have been shown to have a higher incidence of adverse outcomes, including an increase in the prevalence of CP and cognitive impairment (Blickstein, Reference Blickstein2002; Blickstein & Keith, Reference Blickstein and Keith2003; Doyle, Reference Doyle1996; Ingram Cooke, Reference Ingram Cooke2010; Martin & Park, Reference Martin and Park1999; Mazhar et al., Reference Mazhar, Peerzade and Mahmud2002; The ESHRE Capri Workshop Group, 2000; Wadhawan et al., Reference Wadhawan, Oh, Perritt, McDonald, Das, Poole, Vohr and Higgins2009).

In our study of a cohort of multiples and singletons born at ≤32 weeks gestational age at a big maternity center in Turkey over a one-year period, we examined the outcomes of the group at 12–18 months’ CA. Our results showed that for CP and neurodevelopmental impairment, there were no significant differences between singletons and multiples (p = .60 and .06); that is, multiple birth did not influence neurodevelopmental outcome in the preterm infants born at ≤32 weeks gestational age.

Our findings are consistent with studies published by the following authors, who compared the outcomes of singletons and multiples preterm infants. Donovan et al. (Reference Donovan, Ehrenkranz, Shankaran, Stevenson, Wright, Younes and Papile1998) examined the outcomes of singletons and multiples born at <28 weeks gestational age and with birth weights of 401–1,500 g. The authors found no significant differences in the incidence of major morbidity and mortality. They suggested that a higher neonatal adverse outcome rate was not seen when VLBW twins and singleton infants were studied adjusting for birth weight using the National Institute of Child Health and Human Development (NICHD) database (Donovan et al., Reference Donovan, Ehrenkranz, Shankaran, Stevenson, Wright, Younes and Papile1998). Asztalos et al. (Reference Asztalos, Barrett, Lacy and Luther2001) evaluated 52 twins and 101 singleton infants born between 24 and 30 weeks gestational age. Their primary outcome was death or the presence of a severe neurodevelopmental deficit at 18–24 months’ CA. The incidence of death or severe disability was 29.7% in twins versus 22.8% in singletons (p = .337). They reported that severe neurodevelopmental morbidity was not significantly higher in twins than in singletons in their cohort (Asztalos et al., Reference Asztalos, Barrett, Lacy and Luther2001). Hajnal et al. (Reference Hajnal, Braun-Fahrländer, von Siebenthal, Bucher and Largo2005) examined the neurodevelopmental outcome of multiples and singletons born <1250 g at two years’ CA. The Bayley Scales of Infant Development and a standardized neurologic examination were administered. They found that the neurodevelopmental outcome of multiple births was similar to that of singletons (Hajnal et al., Reference Hajnal, Braun-Fahrländer, von Siebenthal, Bucher and Largo2005).

On the contrary, there are some studies indicating differences between the multiplets and singletons in long-term outcome. Wadhawan et al. (Reference Wadhawan, Oh, Perritt, McDonald, Das, Poole, Vohr and Higgins2009) conducted a retrospective study to evaluate the incidence of neurodevelopmental impairment at 18–22 months’ CA between twins and singletons of extremely low birth weight (ELBW). The cohort of infants consisted of 7,630 singleton infants and 1,376 twins. The authors indicated that twin gestation in ELBW infants was associated with an independent, increased risk of neurodevelopmental impairment at 18–22 months’ CA compared with singleton-gestation infants (Wadhawan et al., Reference Wadhawan, Oh, Perritt, McDonald, Das, Poole, Vohr and Higgins2009). In another study of Wadhawan et al., ELBW (birth weight 401–1,000 g) multiple births born were assessed for neurodevelopmental impairment at 18–22 months’ CA. Their results showed that the risk of neurodevelopmental impairment was increased in triplets or higher order multiples when compared with singletons (adjusted odds ratio: 1.7; Wadhawan et al., Reference Wadhawan, Oh, Vohr, Wrage, Das and Bell2011).

In our study, it was shown that multiple births did not influence neurodevelopmental outcome in preterm ≤32 weeks gestational age. However, we think that if the groups were equal in variables such as BW and GA, the developmental results may have been influenced in favor of singletons. It should be taken into consideration that neurological handicaps and mental retardation may become prominent several years after birth, so an assessment at the age of 5–7 years is preferable.

Although this is the first long-term comparison between singletons and multiples in Turkey, our study had few limitations. First, our study was a small cohort of VLBW patients and, second, it had low response rate of follow-up (47.4%). This may raise a concern about the possibility of a non-response bias.

In conclusion, in our population of preterm infants at ≤32 weeks gestational age, there were no significant differences between multiples and singleton infants for neurodevelopmental outcome at 12–18 months’ CA. We suggest that a longer and more participatory follow-up and assessment at pre-school age is undertaken.

References

Asztalos, E., Barrett, J. F., Lacy, M., & Luther, M. (2001). Evaluating 2 year outcome in twins ≤30 weeks gestation at birth: A regional perinatal unit's experience. Twin Research and Human Genetics, 4, 431438.Google Scholar
Bayley, N. (1993). Bayley scales of infant development II. San Antonio, TX: Psychological Corp.Google Scholar
Blickstein, I. (2002). Cerebral palsy in multifoetal pregnancies. Developmental Medicine and Child Neurology, 44, 352355.Google Scholar
Blickstein, I., & Keith, L. G. (2003). Outcome of triplets and high-order multiple pregnancies. Current Opinion in Obstetrics and Gynecology, 15, 113117.CrossRefGoogle ScholarPubMed
Bonellie, S. R., Currie, D., & Chalmers, J. (2005). Comparison of risk factors for cerebral palsy in twins and singletons. Developmental Medicine and Child Neurology, 47, 587591.Google Scholar
Donovan, E. F., Ehrenkranz, R. A., Shankaran, S., Stevenson, D. K., Wright, L. L., Younes, N., . . . Papile, L. A. (1998). Outcomes of very low birth weight twins cared for in the National Institute of Child Health and Human Development Neonatal Research Network's intensive care units. American Journal of Obstetrics and Gynecology, 179, 742749.Google Scholar
Doyle, P. (1996). The outcome of multiple pregnancy. Human Reproduction, 11 (Suppl. 4), 110117.Google Scholar
Fanaroff, A. A., Stoll, B. J., Wright, L. L., Carlo, W. A., Ehrenkranz, R. A., Stark, A. R., . . . Poole, W. K. (2007). Trends in neonatal morbidity and mortality for very low birth weight infants. American Journal of Obstetrics and Gynecology, 196, e1147.CrossRefGoogle Scholar
Hajnal, B. L., Braun-Fahrländer, C., von Siebenthal, K., Bucher, H. U., & Largo, R. H. (2005). Improved outcome for very low birth weight multiple births. Pediatric Neurology, 32, 8793.CrossRefGoogle ScholarPubMed
Hamilton, B. E., Martin, J. A., & Ventura, S. J. (2006). Births: Preliminary data for 2005. National Vital Statistics Reports, 55, 18.Google Scholar
Ingram Cooke, R. W. (2010). Does neonatal and infant neurodevelopmental morbidity of multiples and singletons differ? Seminars in Fetal and Neonatal Medicine, 15, 362366.CrossRefGoogle ScholarPubMed
Klebanoff, M. A., & Keim, S. A. (2011). Epidemiology: The changing face of preterm birth, Clinics in Perinatology, 38, 339350.Google Scholar
Martin, J. A., Kung, H. C., Mathews, T. J., Hoyert, D. L., Strobino, D. M., Guyer, B., & Sutton, S. R. (2008). Annual summary of vital statistics: 2006. Pediatrics, 121, 788801.Google Scholar
Martin, J. A., & Park, M. M. (1999). Trends in twin and triplet births: 1980–97. National Vital Statistics Reports, 47, 116.Google Scholar
Mazhar, S. B., Peerzade, A., & Mahmud, G. (2002). Maternal and perinatal complications in multiple versus singleton pregnancies: A prospective two years study. Journal Pakistan Medical Association, 52, 143147.Google ScholarPubMed
Shinwell, E. S. (2002). Neonatal and long-term outcomes of very low birth weight infants from single and multiple pregnancies. Seminars in Neonatalogy, 7 (3), 203209.Google Scholar
Suri, K., Bhandari, V., Lerer, T., Rosenkrantz, T. S., & Hussain, N. (2001). Morbidity and mortality of preterm twins and higher-order multiple births. Journal of Perinatology, 21, 293299.Google Scholar
Sutcliffe, A. G., & Derom, C. (2006). Follow-up of twins: Health, behaviour, speech, language outcomes and implications for parents. Early Human Development, 82, 379386.CrossRefGoogle ScholarPubMed
Tamaru, S., Kikuchi, A., Takagi, K., Wakamatsu, M., Ono, K., Horikoshi, T., Kihara, H., & Nakamura, T. (2011). Neurodevelopmental outcomes of very low birth weight and extremely low birth weight infants at 18 months of corrected age associated with prenatal risk factors. Early Human Development, 87, 5559.Google Scholar
The ESHRE Capri Workshop Group. (2000). Multiple gestation pregnancy. Human Reproduction, 15, 18561864.Google Scholar
Wadhawan, R., Oh, W., Perritt, R. L., McDonald, S. A., Das, A., Poole, W. K., Vohr, B. R., . . .Higgins, R. D. (2009). Twin gestation and neurodevelopmental outcome in extremely low birth weight infants. Pediatrics, 123, 220227.Google Scholar
Wadhawan, R., Oh, W., Vohr, B. R., Wrage, L., Das, A., Bell, E. F., . . . Eunice Kennedy Shriver National Institute of Child Health & Human Development Neonatal Research Network. (2011). Neurodevelopmental outcomes of triplets or high-order extremely low birth weight infants. Pediatrics, 127, 654–60.Google Scholar
Wilson-Castello, D., Friedman, H., Minich, N., Fanaroff, A. A., & Hack, M. (2005). Improved survival rates with increased neurodevelopmental disability for extremely low birth weight infants in the 1990s. Pediatrics, 115, 9971003.Google Scholar
Figure 0

FIGURE 1 Flowchart of the study population.

Figure 1

TABLE 1 Perinatal Characteristics of Infants

Figure 2

TABLE 2 Long-Term Outcomes of Study Infants at 12–18 Months Corrected Age