Saturday, May 4
5:15pm – 7:15pm, Exhibit Hall F & G
4413
Late Breaker Poster Session
LB3 Poster
Board 473
Elevated Creatinine Clearance and Altered Renal
Prostaglandin Balance in Pre-Type I and Early After Onset
of Type I Diabetes Mellitus
Vikas R. Dharnidharka, Gisette Seferina,
Yancy van Patten, Rui-Hua Peng, Michael Clare-Salzler. Departments
of Pediatrics and Pathology, University of Florida College
of Medicine, Gainesville FL.
BACKGROUND: Diabetes mellitus (DM)
nephropathy is influenced by multiple risk factors,
including genetic predispositions. We have previously
reported the aberrant expression of cyclooxygenase-2
(COX-2) in monocytes of subjects at-risk for and with Type
I DM vs. healthy subjects (Litherland et al, JCI 1999).
OBJECTIVE: We hypothesized that altered
prostaglandins (PGs) production through COX-2 mediated
mechanisms may also affect renal hemodynamics and
contribute to nephropathy.
METHODS: Our study groups were
pediatric age subjects that a) were at-risk for Type I DM,
siblings with islet cell autoantibodies + (pre-Type I); b)
had established Type I DM < 1 year; or c) were normal
age-matched controls. We analyzed peripheral blood and
24-hr urinary collections for creatinine clearance (CrCl,
ml/min/1.73sq.m.), CD14+ monocyte COX-2 +ve (flow
cytometry) and urinary metabolites of the main renal PGs:
PGE2, PGI2 and TXA2 (PGE2, 6-ketoPGF1a
and TXB2, respectively) by enzyme immunoassay (expressed
as ng/mg/Cr or as ratios, mean + SE).
RESULTS: In this pilot study, pre-Type
I DM subjects and patients with Type I DM had elevated
24-hr CrCl (Table), despite normal urinary 24-hr albumin
excretions in all. Pre-Type I and Type I DM subjects had
elevated percentages of CD14+ blood monocytes positive for
COX-2. The mean urinary PGE2/TXB2 ratio was depressed in
pre-Type I DM and early Type I DM but not in early
pediatric age Type II DM, in comparison to healthy age
matched controls.
|
Group |
n |
Age |
24-hr CrCl |
UPGE2/TXB2 |
%CD14 COX-2+ |
|
Pre-Type I DM |
13 |
13.1 + 0.9 |
151 + 5.9 |
2.474 + 0.5 |
10.24 + 4.09 |
|
Early Type I DM |
19 |
12.0 + 1.0 |
155 + 7.6 |
2.621 + 0.3 |
28.78 + 5.43 |
|
Controls |
10 |
9.8 + 1.0 |
132 + 10.3 |
4.284 + 1.4 |
3.136 + 2.91 |
CONCLUSIONS: Renal hyperfiltration
begins before the onset of overt diabetes and may be
mediated by a shift in renal prostaglandin balance in
autoimmune diabetes.
LB4 Poster
Board 474
Early vs Delayed Tube Placement for Persistent
Middle-Ear Effusion in the First 3 Years of Life: Effects
on Cognition, Language, and Speech Sound Production at Age
4 Years
J. L. Paradise, H. M. Feldman, C. A.
Dollaghan, T. F. Campbell, D.K. Colborn, D. L. Pitcairn,
H.E. Rockette, J. E. Janosky, M. Kurs-Lasky, D. L. Sabo,
B. S. Bernard, C. G. Smith.
Departments of Pediatrics, Children’s Hosp. of
Pittsburgh and U. of Pittsburgh School of Medicine,
Pittsburgh, PA.
BACKGROUND: To examine possible
developmental effects of persistent early-life MEE and of
tympanostomy-tube placement (TTP), we randomly assigned
children with persistent MEE in the first three years of
life to undergo TTP either promptly or after an extended
period if MEE persisted. TTP markedly reduced subsequent
MEE occurrence, but we found no differences between the
two groups in measures of cognition, language, and speech
sound production at age 3 yr (NEJM 2001;344:1179).
OBJECTIVE: To determine whether
differences not present at age 3 yr were present at age 4
yr.
DESIGN/METHODS: We enrolled 6350
healthy infants aged < 2 mo and monitored them closely
for MEE. 429 who reached specified thresholds for
persistent MEE during the first 3 years of life were
randomly assigned to undergo TTP either promptly or 6
months later if bilateral MEE persisted or 9 months later
if unilateral MEE persisted. At ages 3, 4, and 6 yr we
administered a battery of tests to the children; 397
(92.5%) were tested at age 4. Measures were: for
cognition, McCarthy Scales of Children's Abilities,
comprising General Cognitive Index (GCI) and Verbal,
Perceptual Performance, and Quantitative subscales; for
receptive language, Peabody Picture Vocabulary
Test-Revised (PPVT-R); for expressive language, Number of
Different Words (NDW) and Mean Length of Utterance in
Morphemes (MLUm); and for speech, Percentage of Consonants
Correct-Revised (PCC-R).
RESULTS: Mean (SD) values were as follows. None of the
differences were statistically significant.
|
Group (n) |
McGCI |
Verbal |
P Perf |
Quant |
PPVT |
NDW |
MLUm |
PCC |
|
Early TTP (204) |
97 (14) |
48 (8) |
49 (9) |
49 (9) |
90 (15) |
150 (34) |
3.4 (0.8) |
92 (5) |
|
Delayed TTP (193) |
98 (14) |
49 (9) |
49 (9) |
51 (9) |
92 (16) |
150 (31) |
3.4 (0.7) |
93 (5) |
CONCLUSIONS: These results suggest that
early TTP for persistent MEE in the first three years of
life does not favorably affect cognition, receptive
language, expressive language, or speech sound production
at age 4 years. Funded by NICHD, AHRQ, GlaxoSmithKline,
and Pfizer.
LB5 Poster
Board 475
Implications of Recent Changes in the
Global Landscape of Circulating Influenza A and B Viruses
Kanta Subbarao, Michael W. Shaw,
Catherine B. Smith, Xiyan Xu, Henrietta Hall, Alexander
Klimov, and Nancy J. Cox.
Influenza Branch, Centers for Disease Control, Atlanta, GA
Background: Influenza A H1N1 and H3N2
viruses have co-circulated with influenza B viruses since
1977. Two antigenically and genetically distinct lineages
of influenza B viruses, represented by the reference
strains B/Victoria/2/87 and B/Yamagata/16/88 have
co-circulated in humans since at least 1983. Between 1992
and 2000, Victoria lineage viruses were only detected in
eastern Asia; young children outside Asia have had no
exposure to these viruses. Influenza A H1N1 and B virus
infections are seen more commonly in children than adults
and can be associated with outbreaks among school age
children.
OBJECTIVE: The goal of global influenza
surveillance is to monitor the circulation of antigenic
variants of influenza and the appearance of novel subtypes
of influenza A.
RESULTSs: In the 2001-2002 influenza
season we identified two significant changes among
circulating influenza viruses. Influenza A viruses with an
H1 hemagglutinin (HA) that derived the remaining gene
segments from the circulating influenza A (H3N2) virus
were identified in the US, Canada, Singapore, Malaysia,
India, Oman and Egypt. This is the first instance of
widespread circulation of such reassortants. In the same
season, influenza B viruses of the Victoria lineage
reappeared in several countries including Canada, USA,
Philippines, India and Oman and have been associated with
outbreaks on every continent except South America and
Australia.
CONCLUSIONS: The H1N2 viruses likely
arose by genetic reassortment between the 2 subtypes of
circulating influenza A viruses. Although interesting as a
virologic phenomenon, this event has not prompted concerns
about vaccine composition because the recommended vaccine
contains A/New Caledonia/20/99 (H1N1) and A/Panama/2007/99
(H3N2) viruses, with H1 and N2 antigens similar to those
of the recent H1N2 viruses. In contrast, the majority of
the B/Victoria-like isolates have poor cross reactivity to
B/Sichuan/379/99-like viruses in current vaccines.
Therefore, the reemergence of B/Victoria-like viruses has
resulted in a World Health Organization recommendation for
the inclusion of a B/Victoria-like strain in vaccines for
the 2002-2003 season for the northern hemisphere.
LB6 Poster
Board 476
Respiratory Burst Activity in Bronchopulmonary
Dysplasia and Changes with Dexamethasone
Praveen Ballabh, M. Simm, C. Califano,
Z. Aghai, C. Sison, A. N. Krauss, S. Cunningham-Rundles.
Pediatrics, New York Presbyterian Hospital, Weill Medical
College of Cornell University, New York; Division of New
Born Medicine, Westchester Medical Center, Valhalla, New
York.
BACKGROUND: Since development of
Bronchopulmonary dysplasia (BPD) has been linked with
increased oxidative stress and oxygen free radicals may
play a significant role in pathogenesis of BPD, we
hypothesized that respiratory burst activity is increased
in the premature neonates who develop BPD.
OBJECTIVES: To evaluate longitudinal
change in the respiratory burst activity (RBA) in
neutrophils and monocytes in VLBW infants with respiratory
distress syndrome (RDS) and to examine differences between
non-BPD and BPD neonates, and also to investigate the
effects of dexamethasone on RBA.
DESIGN AND METHODS: We measured RBA on
neutrophils and monocytes in heparinized blood in response
to E.Coli, fMLP (N-formyl-met-leu-phe) and PMA (phorbol 12
myristate) stimulation by flow-cytometry on days 3, 7, 14
and 21 of life, before and 2-3 days after initiating a
6-day course of dexamethasone treatment. Infants were
followed until discharge and were classified as non-BPD
(n=12, GA 28.7 ± 1.2 weeks, weight 1118 ± 137 grams) and
either 1) BPD d28 reflecting their oxygen requirement at
day of life 28 (n=16, GA 26.1± 1.2 weeks, weight 856 ±
112 grams), or 2) BPD 36 weeks reflecting oxygen
dependence at 36 weeks’ corrected gestational age (n=11,
GA 24.8 ± 0.9 weeks, weight 692 ± 105 grams). The
diagnosis of BPD was supported by radiological changes of
BPD.
RESULTS: The percentage of activated
neutrophils producing a respiratory burst increased in all
premature infants with increasing postnatal days during
the first 21 days of life, when the physiological
stimulus, E Coli was used as an activator (p < 0.02).
There was no significant difference in the RBA
measured either as percent activation or as mean
fluorescence intensity between non–BPD and BPD infants
after adjusting for the difference in weight and
gestational age between the groups. The treatment with
dexamethasone did cause decreased percent activation of
neutrophils (p < 0.005) when E. Coli was used as a
stimulus.
CONCLUSION: A significant increase in
neutrophil respiratory burst activity occurs during the
first month of life in VLBW infants. Greater pulmonary
damage in BPD cannot be attributed to increased burst
activity in either neutrophils or monocytes. Decreased
neutrophilic burst activity on dexamethasone treatment may
be a mechanism of corticosteroid to reduce lung
inflammation in BPD.
Funded by NIH Grant # 06020
LB7 Poster
Board 477
Discovery
of A Previously Unreported Apparently Pervasive Error in
Clinical Pulseoximetry
Dale R. Gerstmann.
Utah Valley Regional Medical Center, Provo, UT; Office of
Research and Education, Pediatrix Medical Group, Sunrise,
FL.
BACKGROUND: Based on an NICU index case in which we were
unable to reconcile disparate values between simultaneous
pulseoximeter (SpO2) and oximeter (sO2) functional
saturations, we hypothesized a possible systematic error
in our clinical use of pulseoximetry or in blood gas
oximetry.
OBJECTIVE: To identify the source of error in SpO2 or sO2
measurement.
METHODS: Critical observation by supervisors and industry
scientists/engineers of device setup, sensor use practice,
and blood gas timing and analysis; and, analysis of
simultaneous SpO2 and arterial sO2 from a) 7 yr historical
NICU data (N=30,918); b) prospective NICU data (N=632); c)
verification data using 2 oximeters (N=50); d) adult
critical care data (N=383); and e) NICU data from 2 remote
centers (N=95, N=168). The error function (SpO2-sO2) was
plotted and regressed against sO2, the measured standard.
RESULTS: No systematic technical or procedural errors were
identified during intensive observation. Sensors and
monitors functioned normally. A significant negative
correlation between the error function and sO2 was found
for each of the 4 local and 2 outside data sets. Plotted
is the NICU historical data, which are typical of the
other data sets (p<0.001). Error functions were similar
for devices from Datex-Ohmeda, Nellcor, Massimo, Space
Labs, Hewlett-Packard, and DataScope.
CONCLUSIONS: These data suggest pulseoximetry
significantly overestimates true saturation as values
decrease. If the error is also device independent,
industry standard signal processing algorithms may need to
be recalibrated for parameters thought to be patient or
disease invariant.
(Dr. B. Yoder, Santa Rosa Children’s
Hosp, San Antonio, and L. Greenway, PhD, LDS Hosp, Salt
Lake City, kindly contributed their data. Scientific
support provided by Datex-Ohmeda and Nellcor.)
LB8 Poster
Board 478
A Novel
Method of Reflectance Pulse Oximetry from Core Body in
Neonates
Amir Kugelman, Yoram Wasserman,
David Bader. Department of
Neonatology, Bnai Zion Medical Center, B Rappaport Faculty
of Medicine, Technion-IIT, Haifa, Israel.
BACKGROUND: Reflectance pulse oximetry (RPO) is a
potential alternative to the traditional transmission
oximetry. A novel RPO capable of measuring from the core
body of neonates is presented. Its major advantage would
be in infants in cardiovascular collapse, poor perfusion,
or during motion artifacts when the transmission pulse
oximetry signal is poor. The advantage of the reflectance
method is demonstrated in a case of a premature infant
with hypovolemic shock, where blood gas or transmission
pulse oximetry could not be obtained because of
cardiovascular collapse.
OBJECTIVE: The aim of our study was to compare pulse
oximetry data measured by the reflectance and transmission
methods in neonates.
METHODS: We monitored 16 infants (birth weight 1484+830
gr., study weight 1852+843 gr., gestational age 31+4
weeks) by the two methods simultaneously, and data were
collected on a computer placed at the bedside. The
transmission oximetry (N395-Nellcor, Puritan Bennett,
Inc.,CA, USA), was measured from the finger of the infant
on the hand or the foot, while the reflectance oximetry
(PRO2, Imagyn Medical Technologies, CA, USA) was measured
on the upper back. Data were measured for 2-4 hours from
each infant. We compared data obtained from the 2 methods.
Informed consent was obtained from all parents whose
infants participated in the study.
RESULTS: Mean oxygen saturation obtained from the
reflectance method was 96.6+7.3 % and that measured
by the transmission methods was 97.2+3.0 %. The
mean difference between the methods was 0.55 %, and the
standard deviation of the absolute errors was 6 %. No side
effects were seen during the study.
CONCLUSIONS: The reflectance pulse oximetry method is
comparable to the transmission methods in its accuracy and
is safe to use in neonates. We speculate that the
reflectance method might be advantageous in cases of poor
peripheral perfusion in neonates.
This work was funded by Cybro Medical Ltd., Haifa, Israel.
LB9 Poster
Board 479
Variation
in Clinical Presentation of Pharyngitis Syndrome and
Streptococcal Pharyngitis. A Multinational Study
Anne W. Rimoin; Antonio L.A.
da Cunha; Rashmi Kumar; Mark C. Steinhoff. The
International Group A Streptococcal Pharyngitis (GRASP)
Study. Department of
International Health, Pediatrics, Johns Hopkins Medical
Institutions, MD.
BACKGROUND: Data on the clinical presentation of
pharyngitis syndrome and group A beta hemolytic
streptococcal (GABHS) pharyngitis derives largely from
studies in high income countries. In low-income countries
there are few prospective studies that provide data on
pharyngitis syndrome and GABHS pharyngitis.
OBJECTIVES: To compare presenting signs and symptoms of
pharyngitis syndrome and their association with GAHBS
pharyngitis in children in 2 countries.
DESIGN/METHODS: Prospective, descriptive study to compare
signs and symptoms associated with a) acute pharyngitis
syndrome and b) throat culture. Participants were children
age 2 – 12 years seeking care in pediatric outpatient
clinics in Rio de Janeiro, Brazil (N=152) and Lucknow,
India (N=206). Data on patient demographics and signs and
symptoms were collected using a standard format. Data were
recorded for each patient and compared with culture using χ2
and student t-tests.
RESULTS: Mean age of patients was 8 vs. 5 years (India vs.
Brazil for all comparisons). Patients were mostly male: 66
vs. 51%. GABHS culture positivity was: 9% vs.21%, p= .018.
There were differences in pharyngitis syndrome
presentation with cough (86% vs. 76%, p=.036), complaint
of sore throat (38% vs. 60%, p=.000), tonsillar erythema
(91% vs. 80%, p=.018), and tonsillar exudate (2% vs.15%,
p=.000). There were no differences between countries for
signs of hoarseness and nares excoriation or symptoms of
fever, runny nose, disturbed sleep. Signs associated with
GABHS in each country: tonsillar exudate (p=.05, Brazil)
and enlarged cervical lymph nodes (p < .01 for
both).
CONCLUSION: There appear to be substantial differences in
clinical presentation of pharyngitis syndrome between
these 2 countries. These differences may be due to
etiologic spectrum, cultural, socio-economic, or other
factors. Selected specific signs for GABHS were more
similar. These data suggest that GABHS pharyngitis is a
biological entity that is roughly similar in all humans,
whereas presentation of pharyngitis syndrome varies among
populations.
Funded by USAID.
LB10 Poster
Board 480
Daily
Physical Exercise Stimulates Growth in Premature Infants:
A Randomized Controlled Trial
Sahar M. Hassanein, Mohamed F.
Moustafa, and Hanna A. Amer. Ain
Shams University, Cairo, Egypt
BACKGROUND: Premature infants have limited accretion of
bone mass in utero. Limited physical activity
during hospitalization increases bone resorption and
demineralization. Mechanical loading on bone and joints
increases activity of osteoblasts and stimulates bone
formation and growth.
OBJECTIVE: To test the hypothesis that daily physical
exercise (PE) can enhance the growth of the premature
infant and shorten the length of hospital stay.
DESIGN/METHODS: A prospective randomized trial was
conducted on 34 Preterm infants. Healthy premature infants
who were on full enteral feeds and whom postconceptual age
were <36 weeks were included in this study. Infants
with congenital anomalies, sepsis, neurological and
metabolic problems were not included. Infants were
randomly assigned to one of two groups: Group I (n=16)
subject to PE program, and Group II (n = 18) control. PE
consisted of daily passive flexion and extensions of each
joint of upper and lower extremities repeated 5 times
each. Vital signs and oxygen saturation were recorded for
an hour around the daily PE. Anthropometric measurements
were done weekly until discharge. Serum minerals (Ca, P,
Mg) and alkaline phosphatase enzyme levels were monitored.
Trial continues until infants’ weight reaches 1700 g.
RESULTS: Mean gestational age (week) in Group I (31.4±
1.13), did not differ from Group II (32.5±
1.73); p>0.05. At enrolment, weight (kg), length (cm),
head circumference (cm) and forearm length (cm) were
comparable in Group I (1.46 ±
0.13, 39± 2.39, 29.1±
2.93 and 10.6± 1.1) vs. Group
II (1.47± 0.15, 38.3±
2.11, 28.4± 2.01 and 10.3±
1.12) respectively; p>0.05. Average daily caloric
intake in Group I (137.6± 19.2
cal/kg) was not different than Group II (132.3±
29.4); p=0.12. At the end of the trial period, Group I
infants were significantly longer than Group II (42.3±
2.22 vs. 39.9± 2.28);
p<0.001. However, there was no difference between
groups in head circumference or in forearm length: Group I
(30.5± 2.87 and 11.6±
0.93) and Group II (28.4± 2.01
and 11.0± 1.11) respectively;
p=>0.05. Mean hospital stay was significantly shorter
for Group I (12.1± 2.25 days)
than Group II (20.1± 4.65
days); p<0.01.
CONCLUSION: Daily physical exercise can enhance the growth
of the premature infant.
Sunday, May 5
8:00am – 10:00am, Ballroom IV
5049
Clinical Trials: Perinatal and Neonatal I Platform Session
LB1 Presentation
Time 8:00am
A Randomized, Multicenter Masked
Comparison Trial of Curosurf and Survanta in the Treatment
of Established Neonatal Respiratory Distress Syndrome (RDS)
in Preterm Infants
Rangasamy Ramanathan, Maynard R.
Rasmussen, Dale Gerstmann, Neil Finer, Krishnamurthy Sekar
and The North American Study Group.
Department of Pediatrics, Division of Neonatology, Women’s
and Children’s Hospital, University of Southern
California, Los Angeles, CA.
OBJECTIVES: To compare the onset of
clinical response and overall clinical outcome using three
different initial surfactant doses in preterm infants
weighing 750 – 1750 g at birth.
METHODS: Preterm infants with
established RDS were randomized to receive an initial dose
of 100 or 200 mg/kg of Curosurf or 100 mg/kg of Survanta.
All repeat dosing was given at 100 mg/kg of Curosurf or
Survanta. The onset of clinical response was studied by
comparing the changes in the fraction of inspired oxygen
between 0 and 6 hours (FiO2 AUC0-6)
after the first dose. In addition, the overall clinical
outcomes at 28 days and at 36 weeks postconceptional age
were evaluated.
RESULTS: Three hundred and one infants
were enrolled in this trial. Of those, 293 infants had
post-treatment assessment for FiO2 AUC0-6.
Ninety-six infants received 100 mg/kg of Curosurf, 99
infants received 200 mg/kg of Curosurf, and 98 infants
received 100 mg/kg of Survanta as the initial dose. Mean
birthweight, gestational age, gender, race, and age at
randomization were similar between the 3 groups. The mean
FiO2 AUC0-6 for 100 and 200 mg/kg
Curosurf groups were significantly lower than that for
Survanta (p <0.003). There was no significant
difference between the mean FiO2 AUC0-6 in
infants treated with 100 or 200 mg/kg of Curosurf. The
incidence of air leaks, patent ductus arteriosus,
necrotizing enterocolitis, pulmonary hemorrhage, rescue
high frequency ventilation, ³
grade III intraventricular hemorrhage, duration of
mechanical ventilation, oxygen requirement at 28 days or
at 36 weeks postconceptional age was not different between
the groups. Neonatal mortality was 3% in the 200 mg/kg
Curosurf group as compared to 6% and 8% in the 100 mg/kg
Curosurf and Survanta groups respectively.
CONCLUSIONS: Treatment with Curosurf
100 or 200 mg/kg is associated with faster weaning of
supplemental oxygen compared to Survanta. Our data
indicate that infants treated with an initial dose of 200
mg/kg, followed by 100 mg/kg of Curosurf have a modest
benefit in the acute phase of RDS.
Supported by Dey, L.P.
LB2 Presentation
Time 8:45am
Morphine Infusions Do Not Alter
Neurologic Outcomes in Ventilated Preterm Neonates:
Primary Outcomes from the NEOPAIN Multicenter Trial
NEOPAIN Multicenter Trial Group.
Department of Pediatrics, University of Arkansas for
Medical Sciences, Little Rock, AR; Maryland Medical
Research Institute, Baltimore, MD.
BACKGROUND: Effects of opioid analgesia
on the survival and neurologic outcomes of ventilated
preterm neonates remains unknown, although large numbers
of neonates are exposed to repetitive pain/stress and
opioid analgesics.
OBJECTIVE: To investigate whether
pre-emptive morphine analgesia decreases the incidence of
death, intraventricular hemorrhage (IVH, Grade III or IV),
or periventricular leukomalacia (PVL) in ventilated
preterm neonates.
DESIGN/METHODS: Ventilated preterm
neonates from 16 NICUs received blinded placebo (N=414) or
low-dose morphine (N=406) therapy. Randomization and
morphine infusion rates were stratified by GA (23-26 wk @
10mcg/kg/hr; 27-29 wk @ 20mcg/kg/hr; 30-32 wk @
30mcg/kg/hr). Early and late cranial ultrasonograms were
assessed centrally for IVH and PVL by two radiologists.
RESULTS: The commonest reason for
exclusion was "not ventilated" (66%) and for
non-enrollment was "parent refused consent"
(36%). Enrolled babies were significantly smaller
(1079±388 vs. 1169±441 g, P<0.001) and younger
(27.6±2.4 vs. 28.2±2.6 wk, P<0.001) than the
non-enrolled infants. The randomized groups were similar
with regard to maternal variables (antenatal/perinatal),
severity of illness (Apgar / CRIB scores, diagnoses),
demographic factors (gestation, birth weight, sex),
therapeutic interventions (ventilation, feeds, drugs), and
other clinical factors. No differences occurred in the
incidence of mortality (10.9% vs. 13.1%), severe IVH
(10.8% vs. 12.1%), or PVL (10.2% vs. 8.3%) in the placebo
vs. morphine groups. In 27-29 wk neonates, composite of
death, IVH, or PVL seemed to occur more frequently in the
morphine group (16.7% vs. 26.4%, p=0.06). No differences
occurred in the secondary outcomes between the two
randomized groups.
CONCLUSIONS: Low-dose morphine
analgesia does not increase the vulnerability to poor
neurologic outcomes in preterm neonates. Higher morphine
doses in the 27-29 wk neonates may promote the occurrence
of early neurologic injury.
Funded by NICHD (HD36484, HD36270)
Tuesday, May
7
8:00am –
10:00am, Ballroom IV
7062
Late Breaker Platform Session
LB11
Presentation
Time 8:00am
PKHD1,
the Polycystic Kidney and Hepatic Disease 1 Gene Encodes a
Novel Large Protein Containing Multiple IPT Domains and
PbH1 Repeats
Luiz F. Onuchic, Laszlo Furu,
Yasuyuki Nagasawa, Xiaoying Hou, Thomas Eggermann, Zhiyong
Ren, Carsten Bergmann, Jan Senderek, Ernie Esquivel, Raoul
Zeltner, Sabine Rudnik-Schöneborn, Michael Mrug, William
Sweeney, Ellis D. Avner, Klaus Zerres, Lisa M.
Guay-Woodford, Stefan Somlo, Gregory G. Germino.
Depts Med. and Genet., Johns Hopkins Univ., Baltimore MD;
Dept Med., Univ. Sao Paulo, Sao Paulo, Brazil; Dept Med.
and Genet., Yale University School of Medicine, New Haven
CT; Dept of Med. and Pediatr., UAB, Birmingham, AL; Instit.
Human Genet., Technical Univ. Aachen, Germany; Dept.
Pediatr., Case Western Reserve Univ., Cleveland OH.
Autosomal recessive polycystic kidney disease (ARPKD) is a
severe form of polycystic kidney disease with an estimated
incidence of 1:20,000. The typical onset occurs in
neonates and infants and is characterized by cystic
dilatation of the renal collecting ducts and congenital
hepatic fibrosis. Although disease expression is variable,
all phenotypes have been linked to a single locus, PKHD1,
on chromosome 6p21.1-p12. Using a positional cloning
strategy, we have identified the PKHD1 gene. The
genomic sequence extends over 469 kb and includes at least
86 exons that are variably assembled into a number of
alternatively spliced transcripts. The gene is primarily
expressed in fetal and adult kidney. The longest
continuous open reading frame encodes a 4074 amino acid
protein, polyductin, that is predicted to have a single
transmembrane spanning domain (TM) near its carboxyl
terminus and IPT (Ig-like, Plexin, Transcription
factor) domains and PbH1 (parallel beta-helix)
repeats in its amino terminus. Several transcripts encode
truncated products that lack the TM and may be secreted if
translated. The PKHD1 gene products are members of
a novel protein class that share structural features with
hepatocyte growth factor receptor and plexins and belong
to a superfamily of proteins involved in regulation of
cellular adhesion and repulsion and of cell proliferation.
LB12 Presentation
Time 8:15am
Correction
of Krabbe Disease with Neonatal Hematopoietic Stem Cell
Transplantation
Joanne Kurtzberg, Karen Richards,
David Wenger, James Provenzale, Maria L. Escolar, Donna
Wall, Martin A. Champagne, William Krivit.
Duke University Medical Center, Durham, NC; San Antonio
Military Pediatric Center, San Antonio, TX; Jefferson
Medical College, Philadelphia, PA; Texas Transplant
Institute, San Antonio, TX; Universite de Montreal by
Hopital Sainte-Justine, Montreal, ON, Canada; University
of Minnesota, Minneapolis, MN.
Globoid cell leukodystrophy is caused by a deficiency of
galactocerebrosidase resulting in accumulation of
psychosine which is toxic to the brain. When this occurs
in the infantile form (Krabbe disease, KD), loss of
central nervous system function is rapid and death occurs
before 2 years of age. We now report outcomes of 7 infants
with KD transplanted (6 with unrelated umbilical cord
blood [UCB] and 1 with matched sibling bone marrow) after
preparation with high dose chemotherapy in the neonatal
period. All patients had a previous sibling who had died
from KD leading to early diagnosis and treatment. In the 6
patients lacking a related donor, unrelated UCB donors
were selected.
All babies survived the transplant and engrafted
neutrophils within 4 weeks and platelets within 8 weeks of
transplant. All achieved 100% donor chimerism before 100
days post transplant. The 6/7 recipients of unrelated UCB
remain full donor chimeras from 2 months – 4.5 years
post transplant. The 1 patient who received HLA-matched
sibling bone marrow is a mixed chimera (75% donor, 25%
host) 5 years post transplant. With a median follow-up of
>3 years, all patients have survived well beyond their
affected siblings and all have experienced remarkably
positive clinical courses, gaining normal milestones,
development and growth post transplant. In all cases, MRI
demonstrated increased myelination and nerve conduction
velocities improved over time.
We conclude that neonatal transplantation for KD produces
excellent results. The use of UCB donors for patients
lacking related donors facilitates transplantation therapy
shortly after birth. In contrast, the use of stem cell
transplantation in patients without a family history who
were symptomatic at >3 months after birth, fails to
produce positive results. Planning is now underway for
identifying non-familial cases by neonatal screening as
well as for selection of UCB donors with high levels of
endogenous enzyme.
LB13 Presentation
Time 8:30am
Mutations
in the IRF6 Gene Cause Van der Woude and Popliteal
Pterygium Syndromes
Brian C. Schutte, Shinji Kondo,
Bryan C. Bjork, Yoriko Watanabe, Michael J. Dixon, Jeffrey
C. Murray. Department of
Pediatrics and Genetics PhD Program, The University of
Iowa, Iowa City, IA; School of Biological Sciences, The
University of Manchester, UK
BACKGROUND AND OBJECTIVE: Non-syndromic orofacial clefts
are a common birth defect with complex etiology, involving
multiple genetic and environmental factors. In order to
identify genetic factors that cause clefts, we study
disorders that exhibit Mendelian inheritance.
DESIGN: We used a positional cloning approach to identify
the gene responsible for Van der Woude syndrome (VWS). VWS
is an autosomal dominant clefting disorder. It is
significant because it is fairly common, accounting for 2%
of all clefts; and it has a remarkably similar phenotype
to non-syndromic clefts, distinguished only by pits in the
lower lip.
RESULTS: We mapped the VWS locus to a 350 kb region at
chromosome 1q32-q41 that contains at least 11 genes,
including the IRF6 gene. We screened these genes
for mutations by direct DNA sequence analysis and
identified a stop codon in the IRF6 gene in the
affected sib of a monozygotic twin pair discordant for VWS.
The unaffected sib and parents did not carry this
mutation. DNA sequence analysis of 121 unrelated
individuals with VWS identified 30 additional mutations in
this gene. The IRF6 gene belongs to a family of
nine transcription factor genes that are best known for
regulating interferon expression following viral
infection. We discovered nonsense and frameshift mutations
throughout the coding region and found missense mutations
clustered in the DNA binding domain and the protein
binding domain. We also identified a distinct set of
mutations in 11 individuals affected with Poplyteal
Pterygium syndrome, a similar orofacial clefting disorder
that includes webbing of the lower limbs.
CONCLUSIONS: We conclude that the IRF6 gene is
essential for craniofacial development and is involved in
limb development. The distribution of nonsense and
frameshift mutations in the VWS population confirms that
is caused by haploinsufficiency, and the cluster of
missense mutations predicts the protein domains important
for function. The distinctive mutations and more extensive
phenotype in the PPS population suggest a dominant
negative effect by mutations that cause PPS.
LB14 Presentation
Time 8:45am
Possible
Innate Variation in Biological Susceptibility to
Inhalational Anthrax
Anne W. Rimoin, Derek A.
Cummings, Donald S. Burke, Mark C. Steinhoff.
Department of International Health, Johns Hopkins
Bloomberg School of Public Health, Baltimore, MD.
BACKGROUND: Inhalational anthrax (IA) is a rare
disease, but exceptionally unusual in children.
OBJECTIVE: To evaluate the hypothesis that children
have reduced innate biological susceptibility to IA,
compared to older subjects using existing data.
DESIGN/METHODS: Retrospective analysis of age distribution
and latency period in outbreaks of IA in Sverdlovsk, USSR,
1979 and United States, 2001.
RESULTS: In Sverdlovsk, USSR, approximately 7000 people
were exposed in an accidental aerosol release of anthrax.
All 77 reported cases were adults (24 – 72 years).
Assuming no differential reporting of disease or deaths
between adults and children, it appears that no children
within the estimated aerosol spore isopleths became ill,
hence may have been less susceptible to an exposure in
which at least 2% (10/450) of exposed adults became ill.
Among the reported adults with IA, there is an inverse
association between age and length of the latent period
(range: 2 – 43 days). (R2 = -.435, p=.001).
The mean latent period for those less than the median age
of 44 years was 23 vs. 15 days for cases > 45
years (Wilcoxon rank-sum, p=.015). In the USA outbreak of
2001, 22 cases of anthrax have been reported; 11 confirmed
as IA, and 11 (7 confirmed, 4 suspected) cutaneous. Median
ages for cutaneous and inhalational groups are 35 (range:
7 months – 51 years) vs. 56 years (range 47 – 94
years). (Wilcoxon rank-sum, p= .000). The oldest reported
case of IA in the US outbreak at 94 years was probably
exposed to a very low dose by cross-contamination of mail.
This suggests that a much lower dose will cause IA in
older subjects, a reflection of possible increased
susceptibility.
CONCLUSION: The relative lack of clinical reports of IA in
children and infants compared to adults may be due to 1)
absence of occupational aerosol exposure of younger
children, 2) lack of recognition of the disease in
children, or 3) decreased susceptibility after exposure of
children. In Sverdlovsk, assumption of approximately equal
exposure by age group suggests that there may be an
age-associated susceptibility to IA. In the USA outbreak
there is a significant difference in age distribution of
anthrax clinical syndromes. These data suggest that there
may be a difference in the biology of IA in younger vs.
older populations, similar to other infectious diseases.
LB15
Presentation
Time 9:00am
Reported
Fatal and Serious Adverse Events Associated with
Palivizumab
Thomas J. Moore, Sheila R. Weiss,
Carol J. Blaisdell. Center for
Health Services Research and Policy, George Washington
Univ., Washington, DC; Schools of Pharmacy and Medicine,
and Pediatric Pulmonology, Univ. of Maryland, Baltimore,
MD.
BACKGROUND: Monthly injections of palivizumab, a humanized
monoclonal antibody, reduced hospitalizations for RSV in a
randomized clinical trial prior to approval. Adverse
events reported to the FDA provide safety data from a much
larger and more diverse patient population.
OBJECTIVE: To compare reported fatal and serious
adverse events associated with palivizumab during its
first 2 full years of marketing with other medications
used in children under 2 years age.
DESIGN/METHODS: From data abstracts of all adverse event
reports received by the FDA in 1999-2000, we extracted
reports for infants and children under 2 years age. The
study included only adverse events resulting in death or
hospitalization, or events that were life threatening or
required intervention to prevent permanent harm. Only
drugs identified as a principal suspect were considered.
RESULTS: Among 341 different drugs named as suspect in
2239 reports, palivizumab accounted for 36% of all fatal
and serious adverse event reports, more than the combined
total of the 40 next most frequently implicated
medications. In the 2-year period, palivizumab was
associated with 117 deaths, and 623 other serious adverse
events in infants and children under 2 years. In reports
with a death outcome, 53% had adverse event terms
referring to the respiratory organ system, 27% to
infections, 26% to cardiac functions and 67% referred to 1
or more of the preceding.
CONCLUSIONS: These data provide a warning signal that
palivizumab may be associated with serious or fatal
adverse events that are not revealed in the literature, on
the product label, or in the FDA evaluation prior to
approval. The data abstracts from the reports in this
study were not detailed enough to permit a medically
specific characterization of the adverse events. The
reporting rate for serious and fatal adverse events in
infants is unknown, with estimates that among all
individuals about 10% are reported, with some studies
showing 1% or less. The volume of voluntary reports can be
influenced by company contacts with consumers, the
severity of underlying illness, the number of infants
exposed, and other factors unrelated to the safety of
palivizumab.
Dr. Blaisdell has been a consultant to the manufacturer,
MedImmune
LB16 Presentation
Time 9:15am
Early vs
Delayed Tube Placement for Persistent Middle-Ear Effusion
in the First 3 Years of Life: Effects on Intelligence,
Receptive Language, and Auditory Processing at Age 6 Years
H. M. Feldman, J. L. Paradise, C.
A. Dollaghan, T. F. Campbell, D.K. Colborn, D. L.
Pitcairn, H.E. Rockette, J. E. Janosky, M. Kurs-Lasky, D.
L. Sabo, B. S. Bernard, C. G. Smith.
Departments of Pediatrics, Children’s Hosp. of
Pittsburgh and U. of Pittsburgh School of Medicine,
Pittsburgh, PA
BACKGROUND: Tympanostomy-tube placement (TTP) is often
undertaken out of concern about adverse developmental
effects of persistent middle-ear effusion (MEE). We
randomly assigned children with persistent MEE in the
first 3 years of life to undergo TTP either promptly or
after an extended period if MEE persisted. Thereafter the
early-TTP group had substantially less MEE than the
delayed-TTP group. Nonetheless we found no differences
between the two groups in measures of speech, language,
cognition, and psychosocial development at age 3 yr (NEJM
2001;344:1179-87).
OBJECTIVE: To determine whether differences are present at
age 6 yr between the early-TTP group and the delayed-TTP
group in measures of intelligence, receptive language, and
auditory processing.
DESIGN/METHODS: We enrolled 6350 healthy infants aged <
2 mo and monitored them closely for MEE. 429 who reached
specified thresholds for persistent MEE during the first 3
years of life were randomly assigned to undergo TTP either
promptly or 6 months later if bilateral MEE persisted or 9
months later if unilateral MEE persisted. At ages 3, 4,
and 6 yr we administered a battery of tests to the
children; 395 (92%) were tested at age 6. We administered
the Weschler Intelligence Scale for Children-III
(full-scale IQ[FS IQ], verbal IQ [VIQ], and performance IQ
[PIQ]), the Peabody Picture Vocabulary Test-Revised (PPVT-R),
and the SCAN, a test of auditory processing abilities.
RESULTS: Mean (SD) values were as follows. None of the
differences were statistically significant.
|
Group |
FS IQ |
V IQ |
P IQ |
PPVT |
SCAN |
|
Early TTP (n=193-201) |
97.8 (13.2) |
97.8 (12.9) |
98.3 (13.7) |
93.6 (13.8) |
93.9 (15.0) |
|
Delayed TTP (n=187-193) |
98.2 (14.4) |
98.0 (14.0) |
98.7 (14.9) |
93.9 (20.2) |
95.7 (14.3) |
CONCLUSIONS: Results suggest that early
TTP for persistent MEE in the first three years of life
does not benefit intelligence, receptive vocabulary, or
auditory processing abilities at age 6 years.
Funded by NICHD, AHRQ, GlaxoSmithKline, and Pfizer.
LB17 Presentation
Time 9:45am
A
Comparison of the Efficacy and Safety of Atorvastatin
Versus Placebo in the Treatment of Children and
Adolescents with Familial or Severe Hypercholesterolemia
Brian W. McCrindle, Leiv Ose, and
David Marais. Hospital for Sick
Children, Toronto, Canada; Rikshospitalet, Oslo, Norway;
University of Cape Town Medical School, Cape Town, South
Africa.
BACKGROUND: Drug treatment of elevated lipid levels in
children ≥ 10 years old is recommended if their
plasma low-density lipoprotein cholesterol (LDL-C) level
is ≥ 190 mg/dL (4.91 mmol/L), or if LDL-C is ≥
160 mg/dL (4.14 mmol/L) and there is either a positive
family history of premature cardiovascular disease (CVD),
or the presence of at least 2 risk factors for CVD.
OBJECTIVES: To evaluate the efficacy and safety of
lipid-lowering therapy with atorvastatin, versus placebo,
in decreasing elevated lipid levels in pediatric subjects,
aged 10-17 years, who have familial hypercholesterolemia (FH)
or severe hypercholesterolemia (SH).
DESIGN/METHOD: This was a 1-year, randomized,
double-blind, placebo-controlled, multicenter study. After
a 4-week placebo run-in period, subjects were randomized
to receive either placebo (n=47), or atorvastatin 10
mg/day (titrated to 20 mg/day at Week 4 if LDL-C > 130
mg/dL)(n=140), for 6 months. The double-blind phase was
followed by a 6-month atorvastatin 10 mg/day open-label
extension. The primary efficacy parameter was the percent
change in LDL-C from baseline to Week 26. Secondary
parameters included the percent change in total
cholesterol (TC), triglycerides (TG), high-density
lipoprotein cholesterol (HDL-C), and apo B, from baseline
to Week 26.
RESULTS: Atorvastatin treatment resulted in a significant
reduction in LDL-C from baseline to Week 26, compared with
placebo (-40% vs. -0.4%; P < 0.001). By Week 26,
60% of subjects in the atorvastatin group, compared with
0% in the placebo group, achieved the LDL-C target of <
130 mg/dL. Mean % changes, from baseline to Week 26, were
also significantly in favor of atorvastatin for TC (-32.3%
vs. -2.0%; P < 0.001), TG (-12.0% vs. +1.0%; P
=0.029), HDL-C (-2.4% vs. -8.0%; P =0.022), and
apo B (-32.8% vs. +2.2%; P < 0.001). The
incidence of treatment-related adverse events was low, and
similar for the atorvastatin and placebo treatment groups
(7.1% vs. 4.3%).
CONCLUSION: Lipid-lowering therapy with atorvastatin 10 or
20 mg/day for 6 months is effective and safe for pediatric
subjects with known FH or SH. Administration of
atorvastatin 10 mg/day for a further 6 months was also
shown to be effective and safe.
The study was funded by Pfizer Inc.
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