Auditory Brainstem Response in Term and Preterm Infants with Neonatal Complications: The Importance of the Sequential Evaluation

Silva, Daniela da; Lopez, Priscila; Mantovani, Jair Cortez

doi:10.1055/s-0034-1378137

Abstract

Introduction

Literature data are not conclusive as to the influence of neonatal complications in the maturational process of the auditory system observed by auditory brainstem response (ABR) in infants at term and preterm.

Objectives

Check the real influence of the neonatal complications in infants by the sequential auditory evaluation.

Methods

Historical cohort study in a tertiary referral center. A total of 114 neonates met inclusion criteria: treatment at the Universal Neonatal Hearing Screening Program of the local hospital; at least one risk indicator for hearing loss; presence in both evaluations (the first one after hospital discharge from the neonatal unit and the second one at 6 months old); all latencies in ABR and transient otoacoustic emissions present in both ears.

Results

The complications that most influenced the ABR findings were Apgar scores less than 6 at 5 minutes, gestational age, intensive care unit stay, peri-intraventricular hemorrhage, and mechanical ventilation.

Conclusion

Sequential auditory evaluation is necessary in premature and term newborns with risk indicators for hearing loss to correctly identify injuries in the auditory pathway.

neonatology; evoked potentials; auditory brainstem

Introduction

Neonatal hearing screening in newborns with complications should be performed using the evoked otoacoustic emissions (OAE) and auditory brainstem response (ABR) because they are complementary tools and together provide a complete evaluation of the auditory system.¹1 Joint Committee on Infant Hearing. Year 2000 position statement: principles and guidelines for early hearing detection and intervention programs. Am J Audiol 2000;9(1):9-29 ²2 Stephens D, Hétu R. Impairment, disability and handicap in audiology: towards a consensus. Audiology 1991;30(4):185-200 The ABR test is a noninvasive neurophysiologic assessment of brainstem maturation in babies and could be a useful electrophysiologic test to verify neuronal myelination in preterm infants.³3 Roopakala MS, Dayananda G, Manjula P, et al. A comparative study of brainstem auditory evoked potentials in preterm and full-term infants. Indian J Physiol Pharmacol 2011;55(1):44-52

Furthermore, the ABR has shown fewer false-positives and lower referral rates compared with OAE, is less sensitive to noise and middle ear disorders even in very premature infants, and is an essential tool in the diagnosis of hearing loss in the pediatric population.⁴4 Lin HC, Shu MT, Lee KS, Lin HY, Lin G. reducing false positives in newborn hearing screening program: how and why. Otol Neurotol 2007;28(6):788-792 ⁵5 Benito-Orejas JI, Ramírez B, Morais D, Almaraz A, Fernández-Calvo JL. Comparison of two-step transient evoked otoacoustic emissions (TEOAE) and automated auditory brainstem response (AABR) for universal newborn hearing screening programs. Int J Pediatr Otorhinolaryngol 2008;72(8):1193-1201 ⁶6 Granell J, Gavilanes J, Herrero J, Sánchez-Jara JL, Velasco MJ, Martín G. [Is universal newborn hearing screening more efficient with auditory evoked potentials compared to otoacoustic emissions?] Acta Otorrinolaringol Esp 2008;59(4):170-175 ⁷7 Pedersen L, Møller TR, Wetke R, Ovesen T. [Neonatal hearing screening. A comparison of automatic auditory brainstem audiometry and otoacoustic emissions]. Ugeskr Laeger 2008;170(8): 642-646

The ABR in neonates may have a high variability of response. The frequently observed prolonged latencies can be considered normal due to the characteristics of the maturation process of the auditory system, explained by the hypothesis that the structures that generate the ABR core components take more time to completely mature.⁸8 Morgan DE, Zimmerman MC, Dubno JR. Auditory brain stem evoked response characteristics in the full-term newborn infant. Ann Otol Rhinol Laryngol 1987;96(2 Pt 1):142-151 ⁹9 Zimmerman MC, Morgan DE, Dubno JR. Auditory brain stem evoked response characteristics in developing infants. Ann Otol Rhinol Laryngol 1987;96(3 Pt 1):291-299 ¹⁰10 Ponton CW, Moore JK, Eggermont JJ. Auditory brain stem response generation by parallel pathways: differential maturation of axonal conduction time and synaptic transmission. Ear Hear 1996;17(5): 402-410 Therefore, the literature remains unclear whether these changes in the ABR responses would be permanent, thus indicating hearing loss, or whether they could be normalized with increasing age.¹¹11 Jiang ZD, Xiu X, Brosi DM, Shao XM, Wilkinson AR. Sub-optimal function of the auditory brainstem in term infants with transient low Apgar scores. Clin Neurophysiol 2007;118(5):1088-1096 ¹²12 Jiang ZD, Wilkinson AR. Brainstem auditory evoked response at term in preterm infants after perinatal hypoxia-ischaemia. Acta Paediatr 2006;95(11):1400-1404 ¹³13 Wilkinson AR, Brosi DM, Jiang ZD. Functional impairment of the brainstem in infants with bronchopulmonary dysplasia. Pediatrics 2007;120(2):362-371 ¹⁴14 Jiang ZD, Yin R, Wilkinson AR. Brainstem auditory evoked responses in very low birthweight infants with chronic lung disease. Eur J Paediatr Neurol 2007;11(3):153-159

According to Kohelet et al,¹⁵15 Kohelet D, Arbel E, Goldberg M, Arlazoroff A. Brainstem auditory evoked response in newborns and infants. J Child Neurol 2000; 15(1):33-35 the ABR response in full-term and preterm newborns of the same chronological age was similar, regardless of gestational age. Nevertheless, Sleifer et al observed that absolute and interpeak latencies were statistically different between 4-month-olds and 12-month-olds.¹⁶16 Sleifer P, da Costa SS, Cóser PL, Goldani MZ, Dornelles C, Weiss K. Auditory brainstem response in premature and full-term children. Int J Pediatr Otorhinolaryngol 2007;71(9):1449-1456 At 20 months, only wave I was similar. The authors concluded that the maturation of the auditory pathway occurs in a different way between full-term and preterm newborns, and that gestational age must be considered in the ABR analysis, mainly in infants younger than 20 months. In a recent study, Roopakala et al compared the ABR results in 25 preterm and 25 full-term infants and observed a significant increased latency of ABR waveform V in preterm infants.³3 Roopakala MS, Dayananda G, Manjula P, et al. A comparative study of brainstem auditory evoked potentials in preterm and full-term infants. Indian J Physiol Pharmacol 2011;55(1):44-52

However, the ABR response in full-term and preterm newborns may be impacted by neonatal complications that are considered of risk for hearing loss and, consequently, may delay the maturation process.¹⁷17 Jiang ZD, Brosi DM, Li ZH, Chen C, Wilkinson AR. Brainstem auditory function at term in preterm babies with and without perinatal complications. Pediatr Res 2005;58(6):1164-1169 Most of the studies show the influence of neonatal complications that are considered of risk for hearing loss in the ABR results. Some authors reported that neonates with transient low Apgar scores had a significant increase in I to V interval at very high click rates in the first 3 days of life.¹¹11 Jiang ZD, Xiu X, Brosi DM, Shao XM, Wilkinson AR. Sub-optimal function of the auditory brainstem in term infants with transient low Apgar scores. Clin Neurophysiol 2007;118(5):1088-1096 In another study, very low-birth-weight infants had prolonged interpeak III to V.¹²12 Jiang ZD, Wilkinson AR. Brainstem auditory evoked response at term in preterm infants after perinatal hypoxia-ischaemia. Acta Paediatr 2006;95(11):1400-1404 The ABR in extremely preterm infants with bronchopulmonary dysplasia showed a significant increase in wave V and interpeak intervals I to V and particularly III to V.¹³13 Wilkinson AR, Brosi DM, Jiang ZD. Functional impairment of the brainstem in infants with bronchopulmonary dysplasia. Pediatrics 2007;120(2):362-371 Extremely low birth weight and mechanical ventilation may, as well, cause abnormal ABR.¹⁴14 Jiang ZD, Yin R, Wilkinson AR. Brainstem auditory evoked responses in very low birthweight infants with chronic lung disease. Eur J Paediatr Neurol 2007;11(3):153-159

The question is whether these ABR findings will be recovered with increasing age or neurodevelopment. The objective of this study was to understand the real influence of neonatal complications considered of risk for hearing loss, in infants, using the sequential ABR evaluation.

Methods

Study Population

This historical cohort study was conducted in a tertiary referral center from October 2008 to October 2010. The inclusion criteria were: treatment at the Universal Neonatal Hearing Screening Program of the local hospital; at least one risk indicator for hearing loss according to the Joint Committee on Infant Hearing¹⁸18 American Academy of Pediatrics, Joint Committee on Infant Hearing. Year 2007 position statement: principles and guidelines for early hearing detection and intervention programs. Pediatrics 2007;120(4):898-921; presence in both evaluations (the first upon neonatal unit discharge, and the second at 6 months of age); all the ABR latencies; transient otoacoustic emissions confirmed in both ears; consent form signed by the newborn's parents or guardians.

For comparison, gestational age was divided into three categories: term ≥ 37 weeks, premature between 31 and 36 weeks, and extremely premature < 31 weeks.

Audiological Assessment

For the ABR analysis, the rarefaction click stimulus was presented by the 3Ω insertion phone, with intensity of 80-dB nHL (normal Hearing Level) and a presentation rate of 20.1 c/s (clicks/seconds) with a bandpass filter of 100 and 3,000 Hz and average of 1,024 stimuli on Interacoustics EP15 Eclipse (Interacoustics A/S, Assens, Denmark). Duplicate recordings were made in response to each stimulus condition to examine reproducibility. The ABR was captured through electrocardiogram disposable electrodes (Neuroline, Ambu A/S, Baltorpbakken, Denmark), after cleaning the skin with electrocardiogram/electroencephalograph abrasive gel (NUPREP, Weaver and Company, Aurora, USA). The impedance level was kept between 1 and 3 kΩ for the electrodes; the active electrode was positioned in F_z, the reference electrode in M₁ and M₂, and the ground electrode in F_pz. No sedatives were used.

Variable and Statistical Analyses

Predictor variables included gender, gestational age, birth weight < 1,500 g, low Apgar score, infection, intensive care unit (ICU) stay, hyperbilirubinemia, peri-intraventricular hemorrhage, use of mechanical ventilation and ototoxic medication. Outcome variables included absolute latencies (I, III, and V) and interpeak latencies (I to III, III to V, and I to V) of the ABR in both ears.

ABR change (in percentage) at 6 months of age (moment 2) was calculated in relation to the ABR performed upon hospital discharge (moment 1) using the following expression: ABR at 6 months of age − ABR postdischarge / ABR postdischarge 0.100% .

The relation between risk indicator for hearing loss and variation of ABR were analyzed using Mann-Whitney and Kruskal-Wallis test, followed by Dunn for multiple comparisons of the gestational age. Statistical analysis was performed with SPSS v15 and Graph Pad Prism v5 software (SPSS Inc., Chicago, IL, USA). A pvalue of < 0.05 was accepted as statistically significant.

Ethics

This study was approved by the Research Ethics Committee, process no. 402/08.

Results

A total of 114 newborns, 51 (45% ) girls and 63 (55) boys, met the inclusion criteria. Other sample data are shown in Table 1.

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Table 1
Description of the 114 newborn according to gestational age and risk indicators for hearing loss

Table 2 shows that Apgar score lower than 6 in the first minute, gestational age, and ICU stay best correlated with the variation of the absolute ABR latencies (p < 0.05).

Thumbnail

Table 2
The p values of the relation between the variation of ABR absolute latencies and gestational age as well as risk indicators for hearing loss

Table 3 shows that ICU stay, peri-intraventricular hemorrhage, mechanical ventilation, and gestational age showed the best relationship to the interpeak variation (p < 0.05).

Thumbnail

Table 3
The p values of the relation between the variation of ABR interpeaks and gestational age as well as risk indicators for hearing loss

Discussion

The objective of our cohort study was to verify the real influence of the neonatal complications considered of risk for hearing loss, by analyzing the variation of the ABR parameters between two moments: at hospital discharge and at 6 months of age. This second evaluation moment was chosen based on the need of an early diagnosis of hearing loss and intervention by 6 months of age. Obviously, children with a history of hearing risk indicators are more likely to have hearing impairment and then require periodic evaluation even if they had an initial normal auditory assessment.¹⁸18 American Academy of Pediatrics, Joint Committee on Infant Hearing. Year 2007 position statement: principles and guidelines for early hearing detection and intervention programs. Pediatrics 2007;120(4):898-921 ¹⁹19 Lewis DR, Marone SAM, Mendes BCA, Cruz OLM, de Nóbrega M. Comitê Multiprofissional em Saúde Auditiva COMUSA. Braz J Otorhinolaryngol 2010;76:121-128

Newborns with risk indicators for hearing loss have some coexistent neonatal complications. However, such complications are not considered by most of the studies, which compare only one risk indicator in healthy babies in only one moment or in the first days of life.

This study intended to show the real influence of risk indicators coexisting with prematurity or not and yet clarify whether the findings in the first evaluation remain abnormal in the second one even with increasing age, considering the present risks. Therefore, in this study, an ABR follow-up was performed in two moments, the first at hospital discharge and the second at 6 months of age, to assess whether these possible alterations are transient or permanent.

Results show that ABR latencies and interpeaks were higher in extremely preterm infants than in full-term newborns, confirming other published results.³3 Roopakala MS, Dayananda G, Manjula P, et al. A comparative study of brainstem auditory evoked potentials in preterm and full-term infants. Indian J Physiol Pharmacol 2011;55(1):44-52 ¹⁶16 Sleifer P, da Costa SS, Cóser PL, Goldani MZ, Dornelles C, Weiss K. Auditory brainstem response in premature and full-term children. Int J Pediatr Otorhinolaryngol 2007;71(9):1449-1456 ¹⁷17 Jiang ZD, Brosi DM, Li ZH, Chen C, Wilkinson AR. Brainstem auditory function at term in preterm babies with and without perinatal complications. Pediatr Res 2005;58(6):1164-1169 Apparently, this difference decreases with increasing age, possibly due to the maturational process.¹⁶16 Sleifer P, da Costa SS, Cóser PL, Goldani MZ, Dornelles C, Weiss K. Auditory brainstem response in premature and full-term children. Int J Pediatr Otorhinolaryngol 2007;71(9):1449-1456 Sleifer et al reported differences between these children, with very similar results at 24 months of age.¹⁶16 Sleifer P, da Costa SS, Cóser PL, Goldani MZ, Dornelles C, Weiss K. Auditory brainstem response in premature and full-term children. Int J Pediatr Otorhinolaryngol 2007;71(9):1449-1456Furthermore, Turchetta et al observed an improvement over time of the estimated hearing threshold in ABR follow-up in preterm and full-term newborns.²⁰20 Turchetta R, Orlando MP, Cammeresi MG, et al. Modifications of auditory brainstem responses (ABR): observations in full-term and pre-term newborns. J Matern Fetal Neonatal Med 2012;25(8): 1342-1347

In the second assessment, when we analyzed the percentage of changes between these two moments, extremely premature infants showed greater reduction in the absolute latency of wave I in both ears. Despite the statistical significance, this finding has no clinical relevance, because the values are similar to those in older children and healthy adults.¹⁰10 Ponton CW, Moore JK, Eggermont JJ. Auditory brain stem response generation by parallel pathways: differential maturation of axonal conduction time and synaptic transmission. Ear Hear 1996;17(5): 402-410 ¹⁷17 Jiang ZD, Brosi DM, Li ZH, Chen C, Wilkinson AR. Brainstem auditory function at term in preterm babies with and without perinatal complications. Pediatr Res 2005;58(6):1164-1169 This result shows that the peripheral transmission matures faster as compared with subsequent waveforms and the same reasoning cannot be applied to reductions of interpeaks I to III, III to V, and I to V between the two assessments due to improper myelination of auditory pathway and improper efficacy of higher-order neurons in infant population.²¹21 Chalak S, Kale A, Deshpande VK, Biswas DA. Establishment of normative data for monoaural recordings of auditory brainstem response and its application in screening patients with hearing loss: a cohort study. J Clin Diagn Res 2013;7(12):2677-2679

The percentage of change in interpeak latencies I to III and III to V was higher in preterm infants than in full-term infants, giving the impression that auditory maturation occurs more rapidly in preterm infants. Both showed change in the ABR values between the assessments, characterized by reduced latencies due to the maturation process. But in the second assessment, preterm infants had higher values, showing that the improvement might be related to the maturation of the auditory pathways that was not complete at birth and changed according to gestational age.²⁰20 Turchetta R, Orlando MP, Cammeresi MG, et al. Modifications of auditory brainstem responses (ABR): observations in full-term and pre-term newborns. J Matern Fetal Neonatal Med 2012;25(8): 1342-1347 ²²22 Casali RL, Santos MFC. Auditory brainstem evoked response: response patterns of full-term and premature infants. Braz J Otorhinolaryngol 2010;76(6):729-738

On the other hand, not only gestational age may cause ABR alterations, but other neonatal complications may as well contribute to auditory maturation impairment. Despite being frequently studied, both aspects are not considered concurrently.

These studies evaluated healthy babies, without risk indicators for hearing loss, although it is very common that preterm neonates have many associated risk factors, hence the need for a detailed analysis of the factors to which preterm infants may have been exposed and that may have contributed to these remaining differences after the end of maturation.

In this study, newborns whose Apgar score was less than 4 at 1 minute after birth and normal after 5 minutes showed no significant increase in the ABR latencies, but those infants who had a low Apgar score at 5 minutes after birth had significant differences in the absolute latency of wave III in both ears.

According to these findings, the low Apgar score at 5 minutes caused worse damages in the auditory pathway, despite increasing age. Jiang et al observed an increase in interpeak I to V only within the first 3 days of life, as well as normal results within 1 month of life for the newborns who had a low Apgar score but had good recovery after 5 minutes.¹⁴14 Jiang ZD, Yin R, Wilkinson AR. Brainstem auditory evoked responses in very low birthweight infants with chronic lung disease. Eur J Paediatr Neurol 2007;11(3):153-159 The authors highlighted that the ABR changes observed within the first 3 days of life are of little significance because they normalized with the development of the maturation process. Therefore, a low Apgar score at 1 minute poses low risk for auditory changes, and a persistently low score may affect the auditory pathways.

An interesting finding in this study that has not been reported in the literature is that the infants who had a longer ICU stay, without considering the primary status of such admission, presented clear alterations between the first and second ABR assessments. Reductions in the absolute latency of wave III in the right ear, interpeak I to III in both ears, and in interpeak III to V in the left ear were statistically significant between the first and second assessments.

Other conditions contribute to the ABR differences, such as peri-intraventricular hemorrhage, maternal infection, chorioamnionitis, and neonatal infection or sepsis. These conditions have been associated with the development of neonatal brain damage and adverse neurodevelopmental outcomes.²³23 Baumert M, Brozek G, Paprotny M, et al. Epidemiology of peri/ intraventricular haemorrhage in newborns at term. J Physiol Pharmacol 2008;59(Suppl 4):67-75 ²⁴24 Yanowitz TD, Jordan JA, Gilmour CH, et al. Hemodynamic disturbances in premature infants born after chorioamnionitis: association with cord blood cytokine concentrations. Pediatr Res 2002; 51(3):310-316 ²⁵25 De Dooy J, Colpaert C, Schuerwegh A, et al. Relationship between histologic chorioamnionitis and early inflammatory variables in blood, tracheal aspirates, and endotracheal colonization in pre-term infants. Pediatr Res 2003;54(1):113-119 ²⁶26 Dammann O, Leviton A. Maternal intrauterine infection, cytokines, and brain damage in the preterm newborn. Pediatr Res 1997; 42(1):1-8 In this study, alterations in the ABR components were observed in these infants, showing that the occurrence of this injury deserves special attention as its association with hearing loss is rarely reported in literature.

Likewise, the use of mechanical ventilation, regardless of the primary disease, changes the ABR recordings and is, therefore, a confounding factor along with other hearing risk indicators.¹⁴14 Jiang ZD, Yin R, Wilkinson AR. Brainstem auditory evoked responses in very low birthweight infants with chronic lung disease. Eur J Paediatr Neurol 2007;11(3):153-159 ²⁷27 Hille ET, van Straaten HI, Verkerk PH; Dutch NICU Neonatal Hearing Screening Working Group. Prevalence and independent risk factors for hearing loss in NICU infants. Acta Paediatr 2007; 96(8):1155-1158 This was observed in this study when newborns using mechanical ventilation showed reduced interpeak I to III for the right ear and reduced interpeak latency I to V for the left ear.

Nevertheless, other conditions frequently associated with hearing loss, such as low birth weight, infections, hyperbilirubinemia with serum level requiring transfusion, and use of ototoxic drugs, showed no significance in the ABR parameters with increasing age.

Results showed that the waveform I is less sensitive to the injuries that occurred during pregnancy and/or neonatal complications. However, waves III and V, which characterize the maturation of axons and synaptic mechanisms in the brainstem level, are more likely to be affected by the risk analyzed in this study.²⁸28 Amorim RB, Agostinho-Pesse RS, Alvarenga KdeF. The maturational process of the auditory system in the first year of life characterized by brainstem auditory evoked potentials. J Appl Oral Sci 2009; 17(Suppl):57-62 Therefore, the differences in the ABR responses between full-term and preterm newborns and with some risk indicators for hearing loss cannot only be due to nervous maturation, but might as well be caused by injuries occurred during pregnancy and/or neonatal complications.¹⁷17 Jiang ZD, Brosi DM, Li ZH, Chen C, Wilkinson AR. Brainstem auditory function at term in preterm babies with and without perinatal complications. Pediatr Res 2005;58(6):1164-1169

We believe that these findings bring an important contribution to clinical practice. Neonates with complications deserve more attention paid to auditory evaluation, because prematurity and neonatal complications may interfere in the ABR findings. The interpretation and/or standardization of the results may be uncertain if only one assessment is performed.

Conclusion

The complications that most impacted the ABR findings were: Apgar scores less than 6 at 5 minutes of birth, gestational age, ICU stay, peri-intraventricular hemorrhage, and mechanical ventilation.

The sequential auditory evaluation is necessary in preterm and full-term newborns with risk indicators for hearing loss to correctly identify injuries in the auditory pathway.

References

¹
Joint Committee on Infant Hearing. Year 2000 position statement: principles and guidelines for early hearing detection and intervention programs. Am J Audiol 2000;9(1):9-29
²
Stephens D, Hétu R. Impairment, disability and handicap in audiology: towards a consensus. Audiology 1991;30(4):185-200
³
Roopakala MS, Dayananda G, Manjula P, et al. A comparative study of brainstem auditory evoked potentials in preterm and full-term infants. Indian J Physiol Pharmacol 2011;55(1):44-52
⁴
Lin HC, Shu MT, Lee KS, Lin HY, Lin G. reducing false positives in newborn hearing screening program: how and why. Otol Neurotol 2007;28(6):788-792
⁵
Benito-Orejas JI, Ramírez B, Morais D, Almaraz A, Fernández-Calvo JL. Comparison of two-step transient evoked otoacoustic emissions (TEOAE) and automated auditory brainstem response (AABR) for universal newborn hearing screening programs. Int J Pediatr Otorhinolaryngol 2008;72(8):1193-1201
⁶
Granell J, Gavilanes J, Herrero J, Sánchez-Jara JL, Velasco MJ, Martín G. [Is universal newborn hearing screening more efficient with auditory evoked potentials compared to otoacoustic emissions?] Acta Otorrinolaringol Esp 2008;59(4):170-175
⁷
Pedersen L, Møller TR, Wetke R, Ovesen T. [Neonatal hearing screening. A comparison of automatic auditory brainstem audiometry and otoacoustic emissions]. Ugeskr Laeger 2008;170(8): 642-646
⁸
Morgan DE, Zimmerman MC, Dubno JR. Auditory brain stem evoked response characteristics in the full-term newborn infant. Ann Otol Rhinol Laryngol 1987;96(2 Pt 1):142-151
⁹
Zimmerman MC, Morgan DE, Dubno JR. Auditory brain stem evoked response characteristics in developing infants. Ann Otol Rhinol Laryngol 1987;96(3 Pt 1):291-299
¹⁰
Ponton CW, Moore JK, Eggermont JJ. Auditory brain stem response generation by parallel pathways: differential maturation of axonal conduction time and synaptic transmission. Ear Hear 1996;17(5): 402-410
¹¹
Jiang ZD, Xiu X, Brosi DM, Shao XM, Wilkinson AR. Sub-optimal function of the auditory brainstem in term infants with transient low Apgar scores. Clin Neurophysiol 2007;118(5):1088-1096
¹²
Jiang ZD, Wilkinson AR. Brainstem auditory evoked response at term in preterm infants after perinatal hypoxia-ischaemia. Acta Paediatr 2006;95(11):1400-1404
¹³
Wilkinson AR, Brosi DM, Jiang ZD. Functional impairment of the brainstem in infants with bronchopulmonary dysplasia. Pediatrics 2007;120(2):362-371
¹⁴
Jiang ZD, Yin R, Wilkinson AR. Brainstem auditory evoked responses in very low birthweight infants with chronic lung disease. Eur J Paediatr Neurol 2007;11(3):153-159
¹⁵
Kohelet D, Arbel E, Goldberg M, Arlazoroff A. Brainstem auditory evoked response in newborns and infants. J Child Neurol 2000; 15(1):33-35
¹⁶
Sleifer P, da Costa SS, Cóser PL, Goldani MZ, Dornelles C, Weiss K. Auditory brainstem response in premature and full-term children. Int J Pediatr Otorhinolaryngol 2007;71(9):1449-1456
¹⁷
Jiang ZD, Brosi DM, Li ZH, Chen C, Wilkinson AR. Brainstem auditory function at term in preterm babies with and without perinatal complications. Pediatr Res 2005;58(6):1164-1169
¹⁸
American Academy of Pediatrics, Joint Committee on Infant Hearing. Year 2007 position statement: principles and guidelines for early hearing detection and intervention programs. Pediatrics 2007;120(4):898-921
¹⁹
Lewis DR, Marone SAM, Mendes BCA, Cruz OLM, de Nóbrega M. Comitê Multiprofissional em Saúde Auditiva COMUSA. Braz J Otorhinolaryngol 2010;76:121-128
²⁰
Turchetta R, Orlando MP, Cammeresi MG, et al. Modifications of auditory brainstem responses (ABR): observations in full-term and pre-term newborns. J Matern Fetal Neonatal Med 2012;25(8): 1342-1347
²¹
Chalak S, Kale A, Deshpande VK, Biswas DA. Establishment of normative data for monoaural recordings of auditory brainstem response and its application in screening patients with hearing loss: a cohort study. J Clin Diagn Res 2013;7(12):2677-2679
²²
Casali RL, Santos MFC. Auditory brainstem evoked response: response patterns of full-term and premature infants. Braz J Otorhinolaryngol 2010;76(6):729-738
²³
Baumert M, Brozek G, Paprotny M, et al. Epidemiology of peri/ intraventricular haemorrhage in newborns at term. J Physiol Pharmacol 2008;59(Suppl 4):67-75
²⁴
Yanowitz TD, Jordan JA, Gilmour CH, et al. Hemodynamic disturbances in premature infants born after chorioamnionitis: association with cord blood cytokine concentrations. Pediatr Res 2002; 51(3):310-316
²⁵
De Dooy J, Colpaert C, Schuerwegh A, et al. Relationship between histologic chorioamnionitis and early inflammatory variables in blood, tracheal aspirates, and endotracheal colonization in pre-term infants. Pediatr Res 2003;54(1):113-119
²⁶
Dammann O, Leviton A. Maternal intrauterine infection, cytokines, and brain damage in the preterm newborn. Pediatr Res 1997; 42(1):1-8
²⁷
Hille ET, van Straaten HI, Verkerk PH; Dutch NICU Neonatal Hearing Screening Working Group. Prevalence and independent risk factors for hearing loss in NICU infants. Acta Paediatr 2007; 96(8):1155-1158
²⁸
Amorim RB, Agostinho-Pesse RS, Alvarenga KdeF. The maturational process of the auditory system in the first year of life characterized by brainstem auditory evoked potentials. J Appl Oral Sci 2009; 17(Suppl):57-62

Publication Dates

Publication in this collection
Apr-Jun 2015

History

Received
25 Feb 2014
Accepted
26 Apr 2014

This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License, which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.

[1] ¹
Joint Committee on Infant Hearing. Year 2000 position statement: principles and guidelines for early hearing detection and intervention programs. Am J Audiol 2000;9(1):9-29

[2] ²
Stephens D, Hétu R. Impairment, disability and handicap in audiology: towards a consensus. Audiology 1991;30(4):185-200

[3] ³
Roopakala MS, Dayananda G, Manjula P, et al. A comparative study of brainstem auditory evoked potentials in preterm and full-term infants. Indian J Physiol Pharmacol 2011;55(1):44-52

[4] ⁴
Lin HC, Shu MT, Lee KS, Lin HY, Lin G. reducing false positives in newborn hearing screening program: how and why. Otol Neurotol 2007;28(6):788-792

[5] ⁵
Benito-Orejas JI, Ramírez B, Morais D, Almaraz A, Fernández-Calvo JL. Comparison of two-step transient evoked otoacoustic emissions (TEOAE) and automated auditory brainstem response (AABR) for universal newborn hearing screening programs. Int J Pediatr Otorhinolaryngol 2008;72(8):1193-1201

[6] ⁶
Granell J, Gavilanes J, Herrero J, Sánchez-Jara JL, Velasco MJ, Martín G. [Is universal newborn hearing screening more efficient with auditory evoked potentials compared to otoacoustic emissions?] Acta Otorrinolaringol Esp 2008;59(4):170-175

[7] ⁷
Pedersen L, Møller TR, Wetke R, Ovesen T. [Neonatal hearing screening. A comparison of automatic auditory brainstem audiometry and otoacoustic emissions]. Ugeskr Laeger 2008;170(8): 642-646

[8] ⁸
Morgan DE, Zimmerman MC, Dubno JR. Auditory brain stem evoked response characteristics in the full-term newborn infant. Ann Otol Rhinol Laryngol 1987;96(2 Pt 1):142-151

[9] ⁹
Zimmerman MC, Morgan DE, Dubno JR. Auditory brain stem evoked response characteristics in developing infants. Ann Otol Rhinol Laryngol 1987;96(3 Pt 1):291-299

[10] ¹⁰
Ponton CW, Moore JK, Eggermont JJ. Auditory brain stem response generation by parallel pathways: differential maturation of axonal conduction time and synaptic transmission. Ear Hear 1996;17(5): 402-410

[11] ¹¹
Jiang ZD, Xiu X, Brosi DM, Shao XM, Wilkinson AR. Sub-optimal function of the auditory brainstem in term infants with transient low Apgar scores. Clin Neurophysiol 2007;118(5):1088-1096

[12] ¹²
Jiang ZD, Wilkinson AR. Brainstem auditory evoked response at term in preterm infants after perinatal hypoxia-ischaemia. Acta Paediatr 2006;95(11):1400-1404

[13] ¹³
Wilkinson AR, Brosi DM, Jiang ZD. Functional impairment of the brainstem in infants with bronchopulmonary dysplasia. Pediatrics 2007;120(2):362-371

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Variables	n (% )
Gestational age < 31 wk	29 (25% )
Gestational age 32–36 wk	49 (43% )
Gestational age ≥37 wk	36 (32% )
Birth weight <1,500 g: no	79 (69% )
Birth weight <1,500 g: yes	35 (31% )
Apgar < 4 (1 min): no	59 (52% )
Apgar < 4 (1 min): yes	55 (48% )
Apgar < 6 (5 min): no	94 (82% )
Apgar < 6 (5 min): yes	20 (18% )
Infection: no	71 (62% )
Infection: yes	43 (38% )
Intensive care units: no	38 (33% )
Intensive care units: yes	76 (67% )
Hyperbilirubinemia: no	109 (96% )
Hyperbilirubinemia: yes	05 (4% )
Peri-intraventricular hemorrhage: no	101 (89% )
Peri-intraventricular hemorrhage: yes	13 (11% )
Mechanical ventilation: no	53 (46% )
Mechanical ventilation: yes	61 (54% )
Ototoxic drugs: no	74 (65% )
Ototoxic drugs: yes	40 (35% )

Characteristics	Right ear			Left ear
Characteristics	I	III	V	I	III	V
Apgar < 6 (5 min): no (n = 94) × yes (n = 20)	0.433	0.016	0.164	0.032	0.006	0.026
GA: <31 wk (n = 29) × 32–36 wk (n = 49) × ≥ 37 wk (n = 36)	0.018^a < 31 ≠ ≥ 37 (Dunn test for multiple comparisons).	0.683	0.217	0.043	0.278	0.258
ICU: no (n = 38) × yes (n= 76)	0.320	0.025	0.815	0.134	0.157	0.907
BW < 1,500 g: no (n = 79) × yes (n = 35)	0.110	0.636	0.606	0.054	0.654	0.958
Apgar < 4 (1 min): no (n = 59) × yes (n = 55)	0.814	0.195	0.107	0.187	0.171	0.053
Infection: no (n = 71) × yes (n = 43)	0.255	0.338	0.309	0.684	0.312	0.205
Hyperbilirubinemia: no (n = 109) × yes (n = 5)	0.841	0.668	0.447	0.140	0.175	0.533
PIVH: no (n = 101) × yes (n = 13)	0.107	0.206	0.380	0.083	0.820	0.199
MV: no (n = 53) × yes (n= 61)	0.084	0.154	0.360	0.201	0.666	0.189
Ototoxic drugs: no (n = 74) × yes (n = 40)	0.764	0.960	0.204	0.667	0.838	0.268
Sex: F (n = 51) × M (n = 63)	0.468	0.346	0.174	0.934	0.401	0.130

Characteristics	Right ear			Left ear
Characteristics	I–III	III–V	I–V	I–III	III–V	I–V
ICU: no (n = 38) × yes (n= 76)	0.003	0.004	0.907	0.022	0.117	0.514
PIVH: no (n = 101) × yes (n = 13)	0.459	0.077	0.070	0.297	0.028	0.026
MV: no (n = 53) × yes (n= 61)	0.006	0.558	0.079	0.162	0.282	0.041
GA: <31 (n = 29) × 32–36 (n = 49) × ≥ 37 (n = 36)	0.066	0.006^a < 31 ≠ 32–36; <31 ≠ ≥ 37 (Dunn test for multiple comparisons).	0.984	0.434	0.307	0.767
BW < 1,500 g: no (n = 79) × yes (n = 35)	0.252	0.324	0.842	0.468	0.580	0.144
Apgar < 4 (1 min): no (n = 59) × yes (n = 55)	0.220	0.203	0.065	0.527	0.226	0.276
Apgar < 6 (5 min): no (n = 94) × yes (n = 20)	0.159	0.890	0.200	0.994	0.127	0.329
Infection: no (n = 71) × yes (n = 43)	0.944	0.309	0.781	0.617	0.420	0.276
Hyperbilirubinemia: no (n = 109) × yes (n = 5)	0.410	0.609	0.171	0.934	0.678	0.552
Ototoxic drugs: no (n = 74) × Yes (n = 40)	0.891	0.059	0.311	0.854	0.152	0.381
Sex: F (n = 51) × M (n = 63)	0.180	0.514	0.067	0.268	0.227	0.065

Brasil

Brasil

Auditory Brainstem Response in Term and Preterm Infants with Neonatal Complications: The Importance of the Sequential Evaluation

Abstract

Introduction

Objectives

Methods

Results

Conclusion

Introduction

Methods

Study Population

Audiological Assessment

Variable and Statistical Analyses

Ethics

Results

Discussion

Conclusion

References

Publication Dates

History