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Vol. 84, Issue 1, 222-228, January 1998
Division of Pulmonary Diseases, University of Miami School of Medicine, Mount Sinai Medical Center, Miami Beach, Florida 33140
Martinez-Salas, José, Richard Mendelssohn, William M. Abraham, Bernard Hsiao, and Tahir Ahmed. Inhibition of allergic airway responses by inhaled low-molecular-weight heparins:
molecular-weight dependence. J. Appl.
Physiol. 84(1): 222-228, 1998.
Inhaled heparin prevents antigen-induced bronchoconstriction and inhibits
anti-immunoglobulin E-mediated mast cell degranulation. We hypothesized
that the antiallergic action of heparin may be molecular weight
dependent. Therefore, we studied the effects of three different
low-molecular-weight fractions of heparin [medium-, low-, and
ultralow-molecular-weight heparin (MMWH, LMWH, ULMWH,
respectively)] on the antigen-induced acute bronchoconstrictor
response (ABR) and airway hyperresponsiveness (AHR) in allergic sheep.
Specific lung resistance was measured in 22 sheep before and after
airway challenge with Ascaris
suum antigen, without and after
pretreatment with inhaled fractionated heparins at doses of
0.31-5.0 mg/kg. Airway responsiveness was estimated before and 2 h
postantigen as the cumulative provocating dose of carbachol in breath
units that increased specific lung resistance by 400%. All
fractionated heparins caused a dose-dependent inhibition of ABR and
AHR. ULMWH was the most effective fraction, with the inhibitory dose
causing 50% protection (ID50)
against ABR of 0.5 mg/kg, whereas
ID50 values of LMWH and MMWH were
1.25 and 1.8 mg/kg, respectively. ULMWH was also the most effective fraction in attenuating AHR; the
ID50 values for ULMWH, LMWH, and
MMWH were 0.5, 2.5, and 4.7 mg/kg, respectively. These data suggest
that 1) fractionated
low-molecular-weight heparins attenuate antigen-induced ABR and AHR;
2) there is an inverse relationship between the antiallergic activity of heparin fractions and molecular weight; and 3) ULMWH is the most
effective fraction preventing allergic bronchoconstriction and airway
hyperresponsiveness.
airway hyperresponsiveness; mast cells
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