Author: Lin, Beryl; Kennedy, Brendan; McBride, Jamie; Dallaâ€Pozza, Luciano; Trahair, Toby; McCowage, Geoffrey; Coward, Emma; Plush, Leanne; Robinson, Paul D.; Hardaker, Kate; Widger, John; Ng, Anthea; Jaffe, Adam; Selvadurai, Hiran
Title: Longâ€term morbidity of respiratory viral infections during chemotherapy in children with leukaemia Cord-id: o1xic89x Document date: 2019_8_8
ID: o1xic89x
Snippet: BACKGROUND: Respiratory viruses are a common cause of infection in immunosuppressed children undergoing cancer therapy. Pulmonary sequelae have been documented following respiratory viral infections (RVIs) in hematopoietic stem cell transplant (HSCT) recipients; however potential late effects in children undergoing nonmyeloablative chemotherapy have not been investigated. AIM: To evaluate the longâ€term pulmonary morbidity of respiratory viral infections during chemotherapy in children with acu
Document: BACKGROUND: Respiratory viruses are a common cause of infection in immunosuppressed children undergoing cancer therapy. Pulmonary sequelae have been documented following respiratory viral infections (RVIs) in hematopoietic stem cell transplant (HSCT) recipients; however potential late effects in children undergoing nonmyeloablative chemotherapy have not been investigated. AIM: To evaluate the longâ€term pulmonary morbidity of respiratory viral infections during chemotherapy in children with acute lymphoblastic leukemia (ALL). METHODS: Childhood ALL survivors, aged 7 to 18 years, greater than 6 months posttreatment were recruited. Exclusion criteria included HSCT or proven bacterial/fungal respiratory infection during treatment. Subjects were classified into “viral†or “control†groups according to retrospective medical records that documented the presence of laboratoryâ€proven RVIs during chemotherapy. Symptom questionnaires (Liverpool, ISAAC) and lung function testing (spirometry, plethysmography, diffusing capacity, forced oscillation technique to ATS/ERS standards) were then performed crossâ€sectionally at the time of recruitment. RESULTS: Fiftyâ€four patients (31 viral, 23 control) were recruited: median (range) age 11.2 (7.2â€18.1) years, and at 4.9 (0.5â€13) years posttherapy. Abnormalities were detected in 17 (31%) individuals (8 viral, 9 control), with the most common being DLCO impairment (3 viral, 4 control) and reduced respiratory reactance at 5 Hz (5 viral, 6 control). Children with RVIs during chemotherapy reported more current respiratory symptoms, particularly wheeze (odds ratio [OR], 3.0; 95% confidence interval [CI]: 0.9â€10.0; P = .09) and cough (OR, 2.7; 95% CI: 0.8â€9.5; P = .11). No differences in lung function tests were observed between the two groups. CONCLUSIONS: Our study found children with RVIs during chemotherapy developed more longâ€term respiratory symptoms than controls; however, differences did not reach statistical significance. No differences in static lung function were found between the two groups. Overall, pulmonary abnormalities and/or significant ongoing respiratory symptoms were detected in nearly a third of ALL survivors treated without HSCT. Larger, prospective studies are warranted to evaluate the etiology and clinical significance of these findings.
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