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Inhaled Corticosteroids in Wheezy Infants

We thank Drs. Merkus and de Jongste for their letter discussing our study (1). We reassert that the functional response of infants with asthma to inhaled corticosteroids (ICS) has not yet been fully addressed. The discussants claim that we did not consider the five published studies using lung function as endpoint. We would like to address this point. Of the five, curiously, the first cited is ours. The second (2) did not find any functional difference (by body plethysmography) between infants who received a short-time dose of beclomethasone + albuterol and others that received only albuterol. The third (3) evaluated patients with bronchial obstruction after bronchiolitis; the objective of our study, on the other hand, was to evaluate the response to ICS in infants with risk factors to develop asthma. The fourth (4) we considered in the discussion section, where we proposed reasons for the difference in the results. Finally, the study by Hofhuis and coworkers (5) was published after our manuscript was submitted and thus was not timely to our article. The authors of this last article did not find significant changes in pulmonary function (max_FRC) after 13 wk of treatment with fluticasone propionate (FP) 200 µg/d. However, the graphic that illustrates the change in pulmonary function shows that many of the infants treated with ICS who have the lowest max_FRC, as measured by Z score, improved their airway caliber compared with the placebo infants, who changed very little. We believe that these findings could be similar to our results if only children with airflow obstruction were included and patients were treated during a longer period.

Drs. Merkus and de Jongste also commented that the studies that show clinical benefits of ICS in young children were performed for the most part in preschool children, whereas no study done in infants and children younger than 2 yr old showed a difference in symptoms when compared with placebo. However, they neglected to mention our previously published study of the clinical efficacy and safety of a 6-mo treatment with FP in children less than 2 yr of age (6). Also, Hofhuis and coworkers (5) found significant changes regarding the symptoms of cough, wheeze, and dyspnea using FP, compared with both baseline and placebo.

We fully agree with Drs. Merkus and de Jongste that our population was cautiously selected with regard to inclusion criteria. We purposely chose infants with risk factors to develop asthma. In addition, to find out whether use of ICS improves lung function, we chose only the subgroup of children that had a low airway caliber, having a Z score max_FRC less than 0 (7).

At the 2005 ATS International Conference, results were presented from an NIH-sponsored study named "Preventing Early Asthma in Kids (PEAK)." In this study, clinical and functional improvements were achieved in slightly older children with asthma receiving ICS. We agree that there is no simple and precise method to identify those children who will benefit from ICS treatment. Nevertheless, the group of infants who have major and/or minor risk factors to develop asthma (8) do have a clinical benefit from use of ICS treatment and, as we found, a functional benefit also. Future studies will have to evaluate if early intervention in this particular kind of patient could prevent the development of irreversible changes in the airways.

Alejandro M. Teper, Carlos D. Kofman and Santiago M. Vidaurreta

Ricardo Gutierrez Children's Hospital, Buenos Aires, Argentina

FOOTNOTES

Conflict of Interest Statement: None of the authors have a financial relationship with a commercial entity that has an interest in the subject of this manuscript.

REFERENCES

1. Teper AM, Kofman CD, Szulman GA, Vidaurreta SM, Maffey AF. Fluticasone improves pulmonary function in children under 2 years old with risk factors for asthma. Am J Respir Crit Care Med 2005;171:587–590.[Abstract/Free Full Text]
2. Kraemer R, Graf Bigler U, Casaulta Aebischer C, Weder M, Birrer P. Clinical and physiological improvement after inhalation of low-dose beclomethasone dipropionate and salbutamol in wheezy infants. Respiration (Herrlisheim) 1997;64:342–349.
3. Maayan C, Itzhaki T, Bar-Yishay E, Gross S, Tal A, Godfrey S. The functional response of infants with persistent wheezing to nebulized beclomethasone dipropionate. Pediatr Pulmonol 1986;2:9–14.[Medline]
4. Stick SM, Burton PR, Clough JB, Cox M, LeSouef PN, Sly PD. The effects of inhaled beclomethasone dipropionate on lung function and histamine responsiveness in recurrently wheezy infants. Arch Dis Child 1995;73:327–332.[Abstract]
5. Hofhuis W, van der Wiel EC, Nieuwhof EM, Hop WC, Affourtit MJ, Smit FJ, Vaessen-Verberne AA, Versteegh FG, de Jongste JC, Merkus PJ. Efficacy of fluticasone propionate on lung function and symptoms in wheezy infants. Am J Respir Crit Care Med 2005;171:328–333.[Abstract/Free Full Text]
6. Teper AM, Colom AJ, Kofman CD, Maffey AF, Vidaurreta SM, Bergada I. Effects of inhaled fluticasone propionate in children less than 2 years old with recurrent wheezing. Pediatr Pulmonol 2004;37:111–115.[CrossRef][Medline]
7. Hoo AF, Dezateux C, Hanrahan JP, Cole TJ, Tepper RS, Stocks J. Sexspecific prediction equations for max_FRC in infancy: a multicenter collaborative study. Am J Respir Crit Care Med 2002;165:1084–1092.[Abstract/Free Full Text]
8. Castro-Rodriguez JA, Holberg CJ, Wright AL, Martinez FD. A clinical index to define risk of asthma in young children with recurrent wheezing. Am J Respir Crit Care Med 2000;162:1403–1406.[Abstract/Free Full Text]

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