1998
DOI: 10.1016/s0091-6749(98)70332-x
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Improved bronchodilation with levalbuterol compared with racemic albuterol in patients with asthma☆☆☆★★★

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Cited by 180 publications
(110 citation statements)
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References 29 publications
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“…9 Nelson ve arkadaşlarının yaptığı çalışmada da genç hastaların 2,5 mg salbutamol kullanımı sonrasında kalp hızının arttığı bildirilmiştir. 10 Yüksek doz beta-2 mimetik tedavisi alan hastaların kan salbutamol düzeyi de yüksek bulunmuş ve bu hastalarda SVT riskinin arttığı saptanmıştır. 11,12 Hastamı-za uygulanmış olan salbutamol dozu 0,15 mg/kg/doz idi.…”
Section: Discussionunclassified
“…9 Nelson ve arkadaşlarının yaptığı çalışmada da genç hastaların 2,5 mg salbutamol kullanımı sonrasında kalp hızının arttığı bildirilmiştir. 10 Yüksek doz beta-2 mimetik tedavisi alan hastaların kan salbutamol düzeyi de yüksek bulunmuş ve bu hastalarda SVT riskinin arttığı saptanmıştır. 11,12 Hastamı-za uygulanmış olan salbutamol dozu 0,15 mg/kg/doz idi.…”
Section: Discussionunclassified
“…For regular administration in chronic stable asthma, the evidence from randomised double-blind studies is mixed, with one study supporting [61] and one not supporting [62] a therapeutic advantage for levalbuterol. There do not appear to have been any double-blind studies comparing levalbuterol and racemic albuterol in the management of asthma exacerbations in adults, and several recent double-blind studies in acute asthma in children have failed to find a therapeutic advantage for levalbuterol [63][64][65].…”
Section: -Agonists In the Management Of Exacerbationsmentioning
confidence: 99%
“…There do not appear to have been any double-blind studies comparing levalbuterol and racemic albuterol in the management of asthma exacerbations in adults, and several recent double-blind studies in acute asthma in children have failed to find a therapeutic advantage for levalbuterol [63][64][65]. The observed development of bronchodilator tolerance with regular administration of SABA [66] is obviously of concern in the context of increasing b 2 -agonist usage during asthma exacerbations, but the initial suggestion that such tachyphylaxis may be due to (S)-albuterol [61] appears not to be supported by evidence [67,68].…”
Section: -Agonists In the Management Of Exacerbationsmentioning
confidence: 99%
“…The possibility that these effects are due to the distomers of b 2 -agonists has been addressed in a recent clinical study by NELSON et al [17]. In a placebo-controlled parallel group study, these investigators compared equivalent doses of R-and R,S-salbutamol given regularly by nebulizer over a four week period, and found evidence of a detrimental effect on the forced expiratory volume in one second (FEV1) with the racemate, which they attributed to the presence of the distomer.…”
mentioning
confidence: 99%
“…The validity of their findings and their clinical relevance has been debated [18]. More germane to the current question is the suggestion that the reason for any toxic effects attributable to b 2 -agonists is the longer half-life of the distomers, allowing them to exert negative effects in the absence of the mitigating actions of the bronchodilating eutomers [8,17]. Unfortunately, this argument is weakened by the fact that salbutamol is unique among the b 2 -agonists in undergoing more rapid enantioselective first pass metabolism of the eutomer.…”
mentioning
confidence: 99%