J ALLERGY CLIN IMMUNOL
VOLUME 127, NUMBER 2
Abstracts AB87
SUNDAY
323 Effect of Budesonide/Formoterol Pressurized Metered-DoseInhaler (BUD/FM pMDI) on Proportion of the Mean PeakForced Expiratory Volume in 1 Second (FEV1) Over Time inPatients With Chronic Obstructive Pulmonary Disease orPersistent Asthma
F. Ahmad, J. G. Zangrilli, U. J. Martin; AstraZeneca LP, Wilmington, DE.
RATIONALE: The spirometric response to an inhaled medication over
time provides insight into the peak effects characteristic of bronchodila-
tors. We assessed lung function as a proportion of maximal FEV1 over
time (ie, greatest change from baseline or peak FEV1) to evaluate BUD/
FM pMDI response at the beginning of the dosing interval.
METHODS: Analysis of 12-hour serial spirometry data (day of random-
ization and 2 subsequent visits) from 2 double-blind studies of patients >_40
years with moderate to severe chronic obstructive pulmonary disease
(COPD; I [12-month]: NCT00206167 [Drugs. 2008;69:549]) or >_12 years
with moderate to severe persistent asthma (II [12-week]: NCT00652002
[Drugs. 2006;66:2235]) who were randomized to twice-daily BUD/FM
pMDI 320/9 mg was conducted. The mean percentage change from base-
line FEV1 at each spirometry time point as a proportion of peak FEV1
(eg, change from baseline FEV1 peak) was assessed.
RESULTS: Study I (COPD, n5121): The peak percentage change from
baseline FEV1 occurred at 2 hours postdose for all 3 visits and ranged
from 27-29% across visits. Clinically significant bronchodilation (>_15%
change from baseline in predose FEV1) occurred within 5 minutes, repre-
senting 64-81% of mean peak FEV1. Study II (asthma, n5124): The peak
percentage change from baseline FEV1 occurred 1-3 hours postdose and
ranged from 19-21% across visits. Clinically significant bronchodilation
was achieved within 15minutes, representing 78-87% of mean peak FEV1.
CONCLUSIONS: Patients with COPD and asthma achieved a high pro-
portion of peak FEV1 rapidly (within 5 and 15 minutes, respectively), as
measured after the morning dose of BUD/FM pMDI 320/9 mg.
324 Inhibitory Effect of Constituents Isolated from Ganodermalucidum on LPS-stimulated Macrophages TNF-a Production
Y. Chuang, C. Liu, N. Yang, Y. Song, B. Liang, X. Li; Pediatric Allergy &
Immunology, The Mount Sinai School of Medicine, New York, NY.
RATIONALE: TNF-a is a pro-inflammatory cytokine that had been im-
plicated in many aspects of asthmatic airway pathophysiology. ASHMI
(Antiasthma Simplified Herbal Medicine Intervention) was shown to
have therapeutic effects in an animal model of asthma and in a controlled
clinical trial. Ganoderma lucidum (Ling-Zhi) one of the three herbs in
ASHMI, has an inhibitory effect on TNF-a production similar that of
ASHMI. We performed activity-guide isolation to identify the bio-active
compounds in Ling-Zhi that inhibit TNF-a production.
METHODS: Liquid-liquid extraction, silica gel column chromatography,
sephadex LH-20 column chromatography and preparative HPLC were
used to obtain pure compounds from Ling-Zhi. The effect of these isolated
compounds on TNF-a production by RAW 264.7 macrophages was exam-
ined. Cell viability was measured by MTT assay.
RESULTS: 16 pure compounds (1-16) were isolated from Ling-Zhi.
Inhibitory activity of these compounds on macrophages TNF-a production
was tested at different doses. Comp.8 and Comp.11 significantly inhibit
TNF-a production at 40mg/mL (48.4% and 47.7%, respectively, P
<0.0001 vs untreated cells). A synergistic effect was obtained when
Comp.8 (20mg/mL) and Comp.11 (20mg/mL) were combined (55.7% inhi-
bition). No compounds were cytotoxic at concentrations up to 40mg/mL.
CONCLUSIONS: Individual constituents (Comp.8, Comp.11) and the
combination (Comp.8 and Comp.11) isolated from Ling-Zhi inhibit
TNF-a production in vitro and may have potential for treating allergic in-
flammatory conditions.
325 Successful Treatment of Acute HemorrhagicLeukoencephalitis, a Novel Phenotype for ComplementFactor I Deficiency
L. Broderick, C. Gandhi, J. L. Mueller, C. D. Putnam, K. Shayan, K. S.
Peterson, S. S. Aceves, R. M. Sheets, B. M. Peterson, R. O. Newbury,
H. M. Hoffman, J. F. Bastian; University of California, San Diego, San
Diego, CA.
RATIONALE: Acute Hemorrhagic Leukoencephalitis (AHLE) is a rare,
acute onset demyelination disorder, causing rapid neurologic deterioration
and mortality. It is most often described as a post-infectious complication
of an upper respiratory illness, although its precise pathophysiology re-
mains unclear. We describe two pediatric patients with AHLE with com-
plement factor I (CFI) deficiency whose successful treatment included
the interleukin-1 (IL-1) receptor antagonist, anakinra, implicating a role
for CFI and IL-1 in demyelinating neurodegenerative disorders.
METHODS: Extensive clinical evaluation of two patients presenting with
AHLE revealed complement abnormalities, specifically related to the alter-
native pathway and its regulator, CFI. Gene sequencing of the CFI coding
regions of the patients and their immediate families was performed on
peripheral blood samples. Immunohistochemical analysis of fixed brain
biopsy tissue was used to investigate the complement pathway and the
mechanism behind the successful use of anakinra.
RESULTS: Both patients received aggressive management with steroids
and immunoglobulin. Treatment with anakinra ultimately led to improve-
ment of clinical status and return to neurologic baseline in both patients.
Two novel mutations in CFI were identified in our patients, which were
not identified in controls. Additionally, immunohistochemical evaluation
of brain biopsy tissue demonstrates increased C3, membrane attack com-
plex (MAC) and IL-1 positivity compared to normal control tissue.
CONCLUSIONS:AHLE is a novel phenotype for CFI deficiency. The up-
regulation of C3 andMACwith subsequent demyelination observed in our
patients supports a role for uncontrolled complement in AHLE, and sug-
gest modulation of innate immunity by anakinra as an important therapy
for neurodegenerative disorders on the demyelination disease spectrum.
326 Complement C6 Null Mutations in Extreme PrematurityT. P. Atkinson1, N. Ambalavanan1, R. A. Kaslow1, M. Peralta-
Carcelen1, S. S. Cosby1, V. A. Phillips1, C. Li2, Y. Dai1; 1University of
Alabama at Birmingham, Birmingham, AL, 2State Perinatal Program,
Alabama Dept of Public Health, Montgomery, AL.
RATIONALE: Since the prevalence of Complement C6 null alleles is in-
creased among African-Americans and the incidence of premature birth is
likewise higher among African-American mothers, we conducted a study
to assess a possible association of complement C6 null alleles in
African-American mothers of extremely low birth weight infants
(ELBW) and ELBWAfrican-American infants.
METHODS:We screened 78 ELBW infants and 55 mothers of ELBW in-
fants for three loss-of-function C6 mutations using PCR and heteroduplex
analysis.
RESULTS: Three infants (3.9%) were found to be heterozygous for a C6
null mutation, a prevalence similar to that in our historical control group
(4.9%). Five mothers were heterozygous for a C6 null allele, and one
was a compound heterozygote indicating complete deficiency; this preva-
lence was significantly higher than in our historical control group (p 50.029). Interestingly, six sets of twins and one set of triplets were born to
cohort mothers, and three of the mothers who had given birth to twins
were heterozygous for C6 null alleles (p5 0.022). Five of the six mothers
bearing C6 null alleles compared with 11 of the other 29 evaluable mothers
had histological chorioamnionitis (p 5 0.073).
CONCLUSIONS: These data suggest that partial C6 deficiency and, by
implication, partial deficiency of other terminal complement components
represent a risk factor for extreme prematurity, and part of this risk may
be related to an increased prevalence in multiple births in mothers bearing
C6 null alleles.
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