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Arch Dis Child Fetal Neonatal Ed. Author manuscript; available in PMC 2018 September
01.
Published in final edited form as:
Arch Dis Child Fetal Neonatal Ed. 2017 September ; 102(5): F428–F433. doi:10.1136/
archdischild-2016-312279.
Cry presence and amplitude do not reflect cortical processing of
painful stimuli in newborns with distinct responses to touch or
cold
Author Manuscript
Nathalie L Maitre1,2, Ann R Stark3, Carrie C McCoy Menser4, Olena D Chorna1, Daniel J
France4,5, Alexandra F Key2,6, Ken Wilkens7, Melissa Moore-Clingenpeel8,9, Don M
Wilkes10, and Stephen Bruehl4
1Center
for Perinatal Research, Nationwide Children's Hospital, Columbus, Ohio, USA
2Department
of Hearing and Speech Sciences, Vanderbilt University Medical Center, Nashville,
Tennessee, USA
3Department
of Pediatrics, Vanderbilt University School of Medicine, Nashville, Texas, USA
4Department
of Anesthesiology, Vanderbilt University Medical Center, Nashville, Tennessee, USA
5Center
for Research & Innovation in Systems Safety, Vanderbilt University, Nashville, Tennessee,
USA
6Vanderbilt
7Institute
Kennedy Center, Vanderbilt University, Nashville, Tennessee, USA
of Imaging Science Vanderbilt University, Vanderbilt University, Nashville, Tennessee,
Author Manuscript
USA
8Biostatistics
Core at The Research Institute, Nationwide Children's Hospital, Columbus, Ohio,
USA
9Division
of Pediatric Critical Care Medicine, Nationwide Children's Hospital, Columbus, Ohio,
USA
10Electrical
Engineering & Computer Science, Vanderbilt University, Nashville, Tennessee, USA
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To request permissions go to: http://group.bmj.com/group/rights-licensing/permissions
Address Correspondence to: Dr Nathalie L Maitre, 700 Children’s Drive, WB6225, Columbus, OH, 43205, USA;
nathalie.maitre@nationwidechildrens.org.
Contributors NLM: designed the study in its final form, participated in data collection, carried out preliminary analyses, wrote,
reviewed and revised all drafts the manuscript and approved the final manuscript as submitted. ARS: contributed to study
interpretation, reviewed and revised all drafts of the manuscript and approved the final manuscript as submitted. CCMM: participated
in the study design and in data collection, drafted the initial manuscript, and approved the final manuscript as submitted. ODC:
participated in data collection, reviewed and revised all drafts of the manuscript and approved the final manuscript as submitted. DJF:
designed the study in its final form, carried out preliminary analyses, reviewed and revised all drafts of the manuscript and approved
the final manuscript as submitted. AFK: participated in data collection, reviewed and revised all drafts of the manuscript and approved
the final manuscript as submitted. KW: designed the touch apparatus, carried out preliminary analyses, reviewed and revised all drafts
of the manuscript and approved the final manuscript as submitted. MMC: designed and performed the final statistical analyses and
approved the final manuscript as submitted. DMW: carried out preliminary analyses, reviewed and revised all drafts of the manuscript
and approved the final manuscript as submitted. SB: designed the study in its final form, carried out preliminary analyses, reviewed
and revised all drafts of the manuscript and approved the final manuscript as submitted.
Competing interests None declared.
Ethics approval Vanderbilt University Institutional Review Board.
Provenance and peer review Not commissioned; externally peer reviewed.
�Maitre et al.
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Abstract
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Objective—Newborns requiring hospitalisation frequently undergo painful procedures.
Prevention of pain in infants is of prime concern because of adverse associations with
physiological and neurological development. However, pain mitigation is currently guided by
behavioural observation assessments that have not been validated against direct evidence of pain
processing in the brain. The aim of this study was to determine whether cry presence or amplitude
is a valid indicator of pain processing in newborns.
Design—Prospective observational cohort.
Setting—Newborn nursery.
Patients—Healthy infants born at >37 weeks and <42 weeks gestation.
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Interventions—We prospectively studied newborn cortical responses to light touch, cold and
heel stick, and the amplitude of associated infant vocalisations using our previously published
paradigms of time-locked electroencephalogram (EEG) with simultaneous audio recordings.
Results—Latencies of cortical peak responses to each of the three stimuli type were significantly
different from each other. Of 54 infants, 13 (24%), 19 (35%) and 35 (65%) had cries in response to
light touch, cold and heel stick, respectively. Cry in response to non-painful stimuli did not predict
cry in response to heel stick. All infants with EEG data had measurable pain responses to heel
stick, whether they cried or not. There was no association between presence or amplitude of cries
and cortical nociceptive amplitudes.
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Conclusions—In newborns with distinct brain responses to light touch, cold and pain, cry
presence or amplitude characteristics do not provide adequate behavioural markers of pain
signalling in the brain. New bedside assessments of newborn pain may need to be developed using
brain-based methodologies as benchmarks in order to provide optimal pain mitigation.
INTRODUCTION
Prevention of pain in newborns is essential because repeated painful exposures have shortterm and long-term adverse effects on physiological and neurological development.1
Because the development of somatosensory processing after birth is dependent on early
sensory experience, atypical exposures can have grave consequences for long-term sensory
processing and pain perception.23 Procedures such as heel sticks, venipunctures or
intubations are associated with lower cognitive and motor scores in early childhood and with
later alterations in visual-perceptual ability and somatosensory sensitivity.45
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Optimal neonatal pain management requires valid non-verbal pain assessment, yet clinical
methodology to assess neonatal pain is rudimentary. Semiquantitative scales of behavioural
observations are widely used, however their validation rarely involves comparison to nonpainful stimuli. Similarly, cry acoustic measures are sometimes associated with behavioural
scales but not with nociceptive (pain) processing6 in the brain.5 Amplitude of cortical
nociceptive-evoked potentials accurately reflects the intensity of pain perception.78
Furthermore, functional MRI (fMRI) evidence in both adults and infants demonstrates
activation of the anterior cingulate cortex (emotional processing) in response to painful
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stimuli, indicating that infants process pain even if they do not exhibit adult behavioural
expressions of pain.78 Therefore, brain-based methodologies can objectively and
quantitatively detect cortical responses to somatosensory stimuli, including pain, even in
infants and preverbal children.9–13
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Assessment of infant cries is a potential approach to quantitative bedside evaluation of pain,
logistically less challenging than brain-based techniques. However, the association between
presence or loudness of a cry (amplitude) and cortical intensity of nociceptive signals is not
known; nor is the specificity of the cry response to a painful stimulus compared with other
somatosensory inputs, such as pressure due to light touch or changes in temperature. We
therefore performed a prospective study using time-locked EEG methodologies to test the
hypothesis that presence of cry and acoustic amplitudes of cries during painful procedures in
infants are associated with amplitude of the brain nociceptive responses, and are distinct
from responses to light touch and cold.
METHODS
We included healthy term infants born at >37 weeks and <42 weeks gestation, between 24
hours and 72 hours of age, before blood sampling for their state-mandated metabolic screen.
Infants had been examined by board-certified paediatricians and diagnosed as healthy term
newborns with no major congenital abnormalities or illnesses since birth. We excluded
infants with signs of neonatal abstinence syndrome, with mothers having a history of
substance abuse, and who had skin punctures or circumcisions prior to data collection. We
recorded demographic information, time of breast feeding or bottle feeding preceding the
testing and total bilirubin level if indicated at testing time.
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We recorded EEG using a previously described event-related potential (ERP) system.1415
Infants were tested in a quiet room in an examiner’s lap, in drowsy or quiet alert states. No
infants were tested in skin-to-skin holds. No sucrose or other oral solutions were used during
the procedure, as per standard practice in the Newborn Nursery. A 128-channel EEG softsponge net (Geodesic Sensor Net, EGI, Eugene, Oregon, USA) soaked in warm saline was
applied to the infant’s head. As per published protocols, the midline Cz electrode was used
as the reference14 (figure 1), sampling was every 1 ms with filters set at 0.1–400 Hz,
continuously recorded using Net Station V.4.3; (EGI, Eugene, Oregon, USA). We recorded
vocalisations using a portable high-quality field recorder (TASCAM DR-100) with a
unidirectional external microphone located 25 cm from the subject’s mouth. Cry samples
were digitised using a 32-bit analogue to digital converter at 44.1 kHz sampling rate.
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The system14–16 delivered tactile stimuli supplied from a standard medical air outlet reduced
by a regulator to a steady 5 pounds per square inch (psi) at the skin. Two valves produced
either a stimulus at the foot or a sham (air puff directed away from foot), with 50 air puffs
and 50 shams (20 ms duration) delivered at randomly varying intervals between 2000 ms
and 2500 ms. E-prime software V. 2.0 (PST, Pittsburgh, Pennsylvania, USA) triggered the
puffs. The apparatus included custom inputs that detected trigger releases on the cold spray
and heel stick, converting them to distinct markings in the EEG, using an interface modified
from Slater and colleagues.10 A single administration of a medical cold spray (Medi-First
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Topical Skin Cold Spray) generated a temperature of 4°C at the skin when triggered for 0.5 s
at 10 cm from the foot. Due to spray diffusion, the stimulus generated <1 psi at the skin. A 2
min wait followed to rewarm the heel with a pad. Heel stick sampling required for routine
state-mandated laboratory testing provided the pain stimulus. Heel sticks were performed by
two physicians who underwent manualised training for heel stick collection (including
written and standardised video material). A Newborn Nursery nurse trainer required 100%
compliance with the protocol from both physicians. Because every heel stick was preceded
by heel warming, no manual squeezing was necessary to obtain the initial data recordings or
drops of blood for the newborn screen. When squeezing did occur, it was after >2 min, well
beyond the EEG and audio recording times.
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The sequence of recording events was standardised and maintained across all subjects as
follows: ERP net placement (5 min), tactile paradigm (6 min), cold puff (2 min), rewarming
(2 min), heel stick (1 min).
Preprocessing of audio recording performed using Adobe Audition CS6 removed identifying
information and extraneous noise. The acoustic analysis approach was based on the sourcefilter model of speech production.17 Mean values were subtracted to compensate for
variability during recording and remaining signals were divided into 25 ms frames
comprising periods of voiced waveform for the signals to appear quasistationary and to
contain at least one cycle of the desired frequency.18
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ERP data were filtered using a 0.3–40 Hz bandpass filter and segmented.1920 Segments
contaminated by motor or ocular artefacts were excluded using standard algorithms included
in NetStation and verified by manual review. Four scalp regions of interest were defined
using clusters of electrodes identified in published studies of somatosensory stimuli (figure
1). Time windows after stimulus onset were 250–350 ms for air puff and 350–700 ms for
heel stick.21 For cold, mean amplitudes were calculated across 100 ms intervals centred on
the maximal amplitude of the grand averaged response (320–420 ms) as this stimulus was
not previously described in infants. Latency to peak maxima were determined for each
stimulus.
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Sample Power: we initially powered the study to distinguish cry acoustics during painful
versus non-painful stimuli. The effect size for the difference (Cohen’s d=0.81) was based on
fundamental frequency (F0) values between infants with rated pain scores.22 Assuming a
correlation between conditions of r=0.30 and a two-tailed p < 0.05, 26 subjects would allow
a power of 0.90. Allowing for 15% data loss due to unanalysable recordings, we proposed a
sample of n = 30 infants. We continued enrolment until obtaining the planned sample of
subjects with cries.
Statistical analyses were performed using SAS V.9.3 (SAS Institute, Cary, North Carolina,
USA), with two-sided p-values <0.05 considered statistically significant. Normality
assumption was confirmed for all models and Kenward-Roger adjustment accounted for
unequal variances across groups.23 Paired-test comparisons studied latency differences to
response maximum in individual subjects for each pair (puff-stick, puff-cold, cold-stick) and
compared cry amplitude characteristics between stick versus cold, among infants who cried
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after both stimuli. Z-tests for differences in paired proportions determined whether infants
who cried to puff, cold, or both puff and cold were more likely to also cry to pain. Repeated
measures analysis of variance with scalp location as a within-subject repeated factor
compared ERP amplitudes between subjects with cry versus none, and quantified
associations between cry characteristics and ERP mean amplitudes among infants who cried.
Where significant interactions indicated that estimated effects of stimulus, cry status or cry
amplitude differed by scalp region, we assessed comparisons within each region, while
taking the covariance structure of the repeated factors into account. When no significant
interactions were noted, we computed marginal means and associations, averaged over scalp
regions. The Bonferroni-Holm procedure adjusted for multiple comparisons.24 When
analysing cry versus ERP amplitudes, we excluded those infants who had a grimace but no
audible cry.
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RESULTS
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Infants with and without audible cries
We studied 54 full-term infants (table 1). Data for one participant were excluded due to an
insufficient number of artefact-free ERP trials in all conditions. Of the remaining 53
subjects, all had measurable, artefact-free cortical responses for light touch, 32 for cold and
33 for heel stick response.
All infants with motion-artefact-free waveforms displayed measurable responses to heel
stick and cold. Grand averaged waveforms are shown in figure 1. Latencies of cortical peak
responses to each stimulus type were significantly different from each other (table 2). Mean
ERP amplitudes to all stimuli were normally distributed (table 3). Responses to puff were
significantly different from sham at all locations and in all subjects (p < 0.001).
Of 54 infants, 13 (24%), 19 (35%) and 35 (65%) had cries in response to puff, cold and heel
stick, respectively. There were no associations at group or individual levels between crying
in response to the first two conditions and crying to heel stick. Specifically, the risk that an
infant would cry after a heel stick was not associated with the risk of the same infant
previously crying from an air puff with a paired proportion of 0.488 CI (0.348 to 0.641) nocry-to-puff versus 0.615 CI (0.351 to 0.880) for cry-to-puff (p=0.422). Similarly, the risk
that an infant would cry after a heel stick was not associated with the risk of the same infant
previously crying from cold stimulus (0.486 CI (0.325 to 0.647) for no-cry-to-cold versus
0.588 CI (0.354 to 0.822) for cry-to-cold (p=0.487)). Similar results were found in infants
who cried neither to cold nor puff (0.4706 CI (0.3028 to 0.6384) vs 0.6 CI (0.3853 to
0.8147), (p=0.358)).
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Infants with ERP data
Thirty-two infants with cortical responses to light touch had analysable data after cold
stimulation. Of these, 4 had an audible cry, 4 had a grimace but no cry and 26 had no audible
cry or grimace. ERP amplitudes to cold stimulation at any location were not statistically
different between infants who cried and those who did not (all p > 0.5).
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Of 33 infants with cortical responses to both light touch and heel stick, 16 had an audible
cry, 3 had a grimace but no cry and 14 had no audible cry or grimace. There was no
statistically significant interaction between cry status and scalp location (p = 0.212).
Marginal mean ERP pain responses for infants who did or did not cry were not statistically
different (5.51 vs 0.91 µV, p = 0.193) (table 4).
The proportion of variance in ERP amplitude attributed to cry status was only 3%. Marginal
means and 95% CIs for ERP amplitude among infants who cried versus didn’t cry showed
considerable overlap, suggesting that even with a larger sample size there would be no
significant difference.
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Among infants who cried in response to pain, we found no significant association between
ERP amplitude and cry amplitude characteristics (table 5) even in individual scalp locations
(see online supplementary figure). We found no significant associations between time of
breast/bottle feeding before testing or bilirubin levels with either cry presence or cry
amplitude.
Estimated effect is interpreted as a 1 unit increase in cry amplitude characteristic
corresponds to an increase/decrease in ERP amplitude.
DISCUSSION
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In contrast to our hypothesis, we found that cortical responses to pain following a heel stick
are often not associated with either presence or amplitude of cries in term infants who have
intact processing of light touch and cold. Nearly half of infants with measurable cortical
responses to pain had no audible cry or grimace, behaviours traditionally associated with
infants’ expression of physical pain and often used clinically to identify pain in infants.
Infants cried to both painful and non-painful stimuli, and more infants overall cried in
response to pain than to light touch or cold stimuli. However, in individual infants, we found
no association between crying in response to one type of stimulus versus another.
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The three types of somatosensory stimuli elicited signal processes in the brain that were
distinct from each other, consistent with published literature on pain and touch. No other
study has reported the cold response in infants. In adults, light touch, a non-nociceptive
stimulus, activates low-pressure mechanoreceptors, resulting in neural signals conducted
through Aβ myelinated fibres through the dorsal column-medial lemniscal system to the
thalamus and eventually the somatosensory cortex.25 Cold activates thermosensitive
excitatory transient receptors, Aδ and pain activates polymodal receptors; both are
conducted through the anterolateral system.26 Polymodal nociceptors use slow conducting
unmyelinated C-fibres and displayed a late response on ERP, as in previous infant work.610
Our ERP results are also consistent with published findings for touch and pain,2728
indicating that our selected measures were appropriate and sensitive, even in newborns.
Furthermore, the three stimulus types (touch, cold and pain) generated distinct neural
responses, demonstrating that the infants we studied process noxious and benign
somatosensory stimuli differently. Distinct cortical responses to pain in combination with a
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lack of stimulus-related differences in crying, further supports the contention that crying
may not be an informative marker of pain experience in newborns.
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In those infants who cried, we measured cry amplitude as a possible behavioural marker of
pain response. While infant cry is presumed to be a common, possibly automatic, response
to distress,29 a large proportion of infants in our study did not generate vocalisations in
response to heel stick even though they processed the stimulation appropriately. Newborns’
cries are usually innate vocal reactions dependent on limbic vocal pathways rather than more
complex laryngeal cortical pathways30 and it is possible that the connectivity necessary for
these pathways remains immature at birth. In addition, laryngeal structures and control in
response to stress are still immature in newborn infants.31 The use of cries for vocal
communication, beyond brainstem-controlled cries, has also been demonstrated to involve
motor learning.32 Because our study population was 48–72 hours old, systems responsible
for vocal production may be too immature to deliver an audible cry reliably and in close
temporal proximity to a painful stimulus. The current findings are consistent with reports
suggesting that processing of pain responses, including associated behavioural
manifestations, continues to develop several months after term birth.910
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Our initial sample size was estimated to be representative of the term infant population.
However, only 60% of the infants with cortical response to light touch had useable data for
cold and pain stimuli. This discrepancy was due to the limitation of administering only one
trial of cold and pain conditions, stimuli that could elicit motion artefact through reflex
withdrawal. Although single-trial time-locked EEG studies are not optimal to study
mechanistic processes, seminal studies on infant pain processing have resulted from this
approach610 and used similar population sizes. Furthermore, while infant ERP data in our
study were normally distributed and most likely representative of term newborns, we used a
limited behavioural data set (cry and grimace). In addition, cry amplitude is only one
acoustic property, and onset time, power in specific frequencies, and duration may be more
informative.
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Although brain-based measures appear more sensitive to pain than infant cries, it is not
feasible to monitor brain activity during each painful experience in the clinical setting,
especially for infants with prolonged hospitalisations. Human and animal evidence suggests
that long-term outcomes may be related to changes in neural connections established
between the thalamus and sensory cortex after exposure to painful stimuli in critical
windows of development,23334 often coincident with hospitalisations for ill or preterm
newborns. Thus, continued examination of brain-behaviour connections for potentially
accurate behavioural markers of pain remains critical to improving the outcomes of high-risk
infants. Because maturation contributes to brain and behavioural responses, future studies
should account for developmental differences in response to pain between full-term and
preterm infants and changes in sensitivity or overt reactions to noxious stimuli over time.
CONCLUSION
In term newborns with distinct cortical responses to light touch, cold and pain, presence of
cry or cry amplitude characteristics do not provide adequate behavioural markers of pain
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signals in the brain. These findings have important implications for clinical care, procedural
support and pain assessment methods in newborns. Clinicians should be aware that
newborns experience pain in response to skin-breaking procedures whether or not overt
behavioural manifestations are present.
Supplementary Material
Refer to Web version on PubMed Central for supplementary material.
Acknowledgments
Funding This work was supported by the Hobbs Discovery Grant from the Vanderbilt Kennedy Center, NICHD
grants [P30HD015052], [U54HD083211], [K23H-D074736(01A1], [1R01HD081120(01A1], NCATS/NIH [UL1
TR000445].
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References
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Author Manuscript
1. Keels E, Sethna N, Watterberg KL, et al. Committee on fetus and newborn and section on
anesthesiology and pain medicine. Prevention and management of procedural pain in the neonate:
an update. Pediatrics. 2016; 137:e20154271. [PubMed: 26810788]
2. Walker SM, Beggs S, Baccei ML. Persistent changes in peripheral and spinal nociceptive processing
after early tissue injury. Exp Neurol. 2016; 275:253–60. [PubMed: 26103453]
3. Schmelzle-Lubiecki BM, Campbell KA, Howard RH, et al. Long-term consequences of early infant
injury and trauma upon somatosensory processing. Eur J Pain. 2007; 11:799–809. [PubMed:
17320438]
4. Grunau RE, Whitfield MF, Petrie-Thomas J, et al. Neonatal pain, parenting stress and interaction, in
relation to cognitive and motor development at 8 and 18 months in preterm infants. Pain. 2009;
143:138–46. [PubMed: 19307058]
5. Fuller B. Meanings of discomfort and fussy-irritable in infant pain assessment. J Pediatr Health
Care. 1996; 10:255–63. [PubMed: 9052116]
6. Fabrizi L, Slater R, Worley A, et al. A shift in sensory processing that enables the developing human
brain to discriminate touch from pain. Curr Biol. 2011; 21:1552–8. [PubMed: 21906948]
7. Lee MC, Mouraux A, Iannetti GD. Characterizing the cortical activity through which pain emerges
from nociception. J Neurosci. 2009; 29:7909–16. [PubMed: 19535602]
8. Roberts K, Papadaki A, Gonçalves C, et al. Contact heat evoked potentials using simultaneous EEG
and fMRI and their correlation with evoked pain. BMC Anesthesiol. 2008; 8:8. [PubMed:
19091117]
9. Slater R, Cantarella A, Franck L, et al. How well do clinical pain assessment tools reflect pain in
infants? PLoS Med. 2008; 5:e129. [PubMed: 18578562]
10. Slater R, Worley A, Fabrizi L, et al. Evoked potentials generated by noxious stimulation in the
human infant brain. Eur J Pain. 2010; 14:321–6. [PubMed: 19481484]
11. Williams G, Fabrizi L, Meek J, et al. Functional magnetic resonance imaging can be used to
explore tactile and nociceptive processing in the infant brain. Acta Paediatr. 2015; 104:158–66.
[PubMed: 25358870]
12. Khoshnejad M, Piché M, Saleh S, et al. Serial processing in primary and secondary somatosensory
cortex: a DCM analysis of human fMRI data in response to innocuous and noxious electrical
stimulation. Neurosci Lett. 2014; 577:83–8. [PubMed: 24933536]
13. Schweizer R, Voit D, Frahm J. Finger representations in human primary somatosensory cortex as
revealed by high-resolution functional MRI of tactile stimulation. Neuroimage. 2008; 42:28–35.
[PubMed: 18550386]
14. Maitre NL, Barnett ZP, Key AP, Apf K. Novel assessment of cortical response to somatosensory
stimuli in children with hemiparetic cerebral palsy. J Child Neurol. 2012; 27:1276–83. [PubMed:
22378658]
Arch Dis Child Fetal Neonatal Ed. Author manuscript; available in PMC 2018 September 01.
�Maitre et al.
Page 9
Author Manuscript
Author Manuscript
Author Manuscript
15. Maitre NL, Key AP. Quantitative assessment of cortical auditory-tactile processing in children with
disabilities. J Vis Exp. 2014:e51054–4.
16. Maitre NL, Henderson G, Gogliotti S, et al. Feasibility of event-related potential methodology to
evaluate changes in cortical processing after rehabilitation in children with cerebral palsy: a pilot
study. J Clin Exp Neuropsychol. 2014; 36:669–79. [PubMed: 24953907]
17. Kent, RD., Kim, Y., et al. Acoustic analysis of speech. In: Ball, MJ.Perkins, MR.Mller, N., Sara,
H., editors. The handbook of clinical linguistics. Oxford, UK: Blackwell Publishing Ltd; 2008. p.
360-80.
18. France DJ, Shiavi RG, Silverman S, et al. Acoustical properties of speech as indicators of
depression and suicidal risk. IEEE Trans Biomed Eng. 2000; 47:829–37. [PubMed: 10916253]
19. Michail G, Dresel C, Witkovský V, et al. Neuronal oscillations in various frequency bands differ
between pain and touch. Front Hum Neurosci. 2016; 10:300. [PubMed: 27445745]
20. Schulz E, Tiemann L, Schuster T, et al. Neurophysiological coding of traits and states in the
perception of pain. Cereb Cortex. 2011; 21:2408–14. [PubMed: 21378113]
21. Worley A, Fabrizi L, Boyd S, et al. Multi-modal pain measurements in infants. J Neurosci
Methods. 2012; 205:252–7. [PubMed: 22285660]
22. Bellieni CV, Sisto R, Cordelli DM, et al. Cry features reflect pain intensity in term newborns: an
alarm threshold. Pediatr Res. 2004; 55:142–6. [PubMed: 14605260]
23. Kenward MG, Roger JH. Small sample inference for fixed effects from restricted maximum
likelihood. Biometrics. 1997; 53:983–97. [PubMed: 9333350]
24. Holm S. A simple sequentially rejective multiple test procedure. Scand J Stat. 1979; 6:65–70.
25. Abraira VE, Ginty DD. The sensory neurons of touch. Neuron. 2013; 79:618–39. [PubMed:
23972592]
26. Björnsdotter M, Löken L, Olausson H, et al. Somatotopic organization of gentle touch processing
in the posterior insular cortex. J Neurosci. 2009; 29:9314–20. [PubMed: 19625521]
27. Slater R, Cornelissen L, Fabrizi L, et al. Oral sucrose as an analgesic drug for procedural pain in
newborn infants: a randomised controlled trial. Lancet. 2010; 376:1225–32. [PubMed: 20817247]
28. Verriotis M, Fabrizi L, Lee A, et al. Cortical activity evoked by inoculation needle prick in infants
up to one-year old. Pain. 2015; 156:222–30. [PubMed: 25599443]
29. Ahola Kohut S, Pillai Riddell R, Flora DB, Kohut SA, Riddell RP, et al. A longitudinal analysis of
the development of infant facial expressions in response to acute pain: immediate and regulatory
expressions. Pain. 2012; 153:2458–65. [PubMed: 23103435]
30. Simonyan K, Horwitz B. Laryngeal motor cortex and control of speech in humans. Neuroscientist.
2011; 17:197–208. [PubMed: 21362688]
31. Silva M, Mijovic B, Van den Bergh BR, et al. Decoupling between fundamental frequency and
energy envelope of neonate cries. Early Hum Dev. 2010; 86:35–40. [PubMed: 20096511]
32. Schneider DM, Mooney R. Motor-related signals in the auditory system for listening and learning.
Curr Opin Neurobiol. 2015; 33:78–84. [PubMed: 25827273]
33. Ranger M, Grunau RE. Early repetitive pain in preterm infants in relation to the developing brain.
Pain Manag. 2014; 4:57–67. [PubMed: 24641344]
34. Grunau RE. Neonatal pain in very preterm infants: long-term effects on brain, neurodevelopment
and pain reactivity. Rambam Maimonides Med J. 2013; 4:e0025. [PubMed: 24228168]
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What is already known on this topic?
►
Due to potential short-term and long-term developmental consequences,
mitigation of procedural pain in newborns is a priority.
►
It is unclear at this time whether behavioural assessment of pain using
newborn crying reflects actual pain experience.
What this study adds?
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►
Newborns have distinct brain responses to light touch, cold and pain.
►
However, crying is not specific to pain nor does it reflect pain experience in
the brain.
►
Cry amplitude characteristics also do not provide adequate behavioural
markers of pain signalling in the brain.
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Figure 1.
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(A) Distribution of electrodes and scalp locations of interest. Scalp locations for analysis and
grand averaged waveform were as follows: F3, frontal left; F4, frontal right; C3, central left,
C4, central right. (B) Cold, air puff and heel stick response amplitude across time.
Comparison of cortical responses to air puff, cold, and heel stick stimulus. All tracings
represent grand averaged waveforms of all patients with available data across all valid trials.
Stimulus occurs at time 0 ms.
Arch Dis Child Fetal Neonatal Ed. Author manuscript; available in PMC 2018 September 01.
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Table 1
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Demographics
n=54
%
EGA in weeks, median (IQR)
39 (38, 40)
Male sex
25
46.2
Caucasian
43
79.6
African-American
8
14.8
Race
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*
Other
3
5.5
Hispanic ethnicity
4
7.4
Hours between feeding and heel stick, median (IQR)
1.8 (0.8, 3.1)
Bilirubin drawn at time of heel stick
8
Total bilirubin level (median, IQR)*
8.7 (7.8, 10.1)
14.8
One subject’s total bilirubin level drawn again 75 min later was 17.9 mg/dL, phototherapy followed.
IQR: 25th, 75th.
EGA, estimated gestational age at birth.
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Table 2
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Latency to maximal stimulus response at selected electrode clusters
Electrode
location
Stimulus type
n
ms to maximum response (SD)
p value
C3
Light touch versus pain
33
301 (40.8) vs 569 (122.2)
<0.001
Pain versus cold
22
570 (120.9) vs 382 (42.5)
<0.001
Cold versus light touch
31
394 (42.4) vs 297 (43.3)
<0.001
Light touch versus pain
33
308 (39.8) vs 523 (132.3)
<0.001
Pain versus cold
22
522 (134.3) vs 379 (46.6)
<0.001
C4
F3
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F4
Cold versus light touch
31
382 (41.9) vs 301 (37.5)
<0.001
Light touch versus pain
33
292 (40.1) vs 532 (124.7)
<0.001
Pain versus cold
22
512 (130.8) vs 387 (34.8)
<0.001
Cold versus light touch
31
384 (37.0) vs 293 (41.6)
<0.001
Light touch versus pain
33
292 (38.2) vs 506 (118.3)
<0.001
Pain versus cold
22
494 (120.5) vs 390 (43.4)
<0.001
Cold versus light touch
31
376 (45.3) vs 293 (41.1)
<0.001
F3, frontal left; F4, frontal right; C3, central left, C4, central right; ms, milliseconds.
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Table 3
Arch Dis Child Fetal Neonatal Ed. Author manuscript; available in PMC 2018 September 01.
Location
Stimulus
Mean
SE
Lower
95% CL
Upper
95% CL
F3
Cold
10.95
3.37
4.08
17.83
F3
Pain
1.20
2.91
−4.71
7.12
F3
Puff
1.43
0.28
0.87
1.99
F3
Sham
0.54
0.31
−0.08
1.16
F4
Cold
9.79
3.10
3.46
16.12
F4
Pain
0.97
2.46
−4.04
5.97
F4
Puff
0.79
0.26
0.27
1.31
F4
Sham
0.15
0.28
−0.42
0.72
C3
Cold
−0.50
2.30
−5.18
4.18
C3
Pain
4.18
2.24
−0.38
8.75
C3
Puff
−0.41
0.25
−0.92
0.10
C3
Sham
−0.18
0.19
−0.56
0.19
C4
Cold
−0.55
3.29
−7.27
6.16
C4
Pain
5.50
3.87
−2.37
13.37
C4
Puff
−0.90
0.23
−1.36
−0.44
C4
Sham
−0.56
0.26
−1.08
−0.04
Maitre et al.
Estimated mean stimulus response at selected electrode clusters in stimulus-associated time windows (all results in microvolts)
F3, frontal left; F4, frontal right; C3, central left, C4: central right.
CL, confidence level.
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Table 4
Arch Dis Child Fetal Neonatal Ed. Author manuscript; available in PMC 2018 September 01.
Group
LS-mean
SE
Lower
95% CL
Upper
95% CL
No cry
0.91
1.95
−3.07
4.88
Cry
5.51
2.33
0.76
10.26
p Vvalue
Maitre et al.
Comparison of cortical responses to heel stick for infants with and without audible cries—estimated mean amplitudes in 500–700 ms time window
0.1398
CL, confidence level; LS-mean, marginal mean.
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Table 5
Arch Dis Child Fetal Neonatal Ed. Author manuscript; available in PMC 2018 September 01.
Cry
amplitude
variable
Estimated
effect
SE
Lower
95% CL
Upper
95% CL
p Value
Mean
−51.97
43.53
−144.49
40.55
0.25
Minimum
−45.20
26.60
−101.72
11.33
0.11
Maximum
3.98
2.71
−1.81
9.78
0.16
Range
4.16
2.56
−1.32
9.64
0.13
Maitre et al.
Lack of associations between cry amplitude characteristics and amplitudes of ERP responses
CL, confidence level. ERP, event-related potential.
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Alexandra Key