Author: CHIEN, Jungâ€Yien; HSUEH, Poâ€Ren; CHENG, Wernâ€Cherng; YU, Chongâ€Jen; YANG, Panâ€Chyr
Title: Temporal changes in cytokine/chemokine profiles and pulmonary involvement in severe acute respiratory syndrome Cord-id: o27rp468 Document date: 2006_10_16
ID: o27rp468
Snippet: Objective and background: Pathological changes in severe acute respiratory syndrome (SARS) suggest that SARS sequelae are associated with dysregulation of cytokine and chemokine production. To improve understanding of the immunoâ€pathological processes involved in lung injury associated with SARS, the temporal changes in cytokine/chemokine profiles in the sera of SARS patients were compared with those of patients with communityâ€acquired pneumonia (CAP), according to the degree of lung involve
Document: Objective and background: Pathological changes in severe acute respiratory syndrome (SARS) suggest that SARS sequelae are associated with dysregulation of cytokine and chemokine production. To improve understanding of the immunoâ€pathological processes involved in lung injury associated with SARS, the temporal changes in cytokine/chemokine profiles in the sera of SARS patients were compared with those of patients with communityâ€acquired pneumonia (CAP), according to the degree of lung involvement. Methods: Serum levels of 11 cytokines and chemokines, in 14 patients with SARS and 24 patients with CAP, were serially checked using a beadâ€based multiassay system. Sera from 12 healthy subjects were used as normal controls. Results: The serum levels of interferonâ€Î³â€inducible proteinâ€10 (IPâ€10), ILâ€2 and ILâ€6 were significantly elevated during SARS infection. In patients with CAP, but not in those with SARS, the levels of interferonâ€Î³, ILâ€10, ILâ€8 and monokine induced by interferonâ€Î³ (MIG) were significantly elevated compared with the levels in healthy controls. Among the chemokines/cytokines, ILâ€6 levels correlated most strongly with radiographic scores (r = 0.62). The elevation of IPâ€10 and ILâ€2 antedated the development of chest involvement and reached peak levels earlier than the radiographic scores. In contrast, the dynamic changes in ILâ€6, Câ€reactive protein and neutrophils occurred synchronously with the changes in radiographic scores. The mean ratio of ILâ€6 to ILâ€10 in SARS patients (4.84; range 0.41–21) was significantly higher than that in CAP patients (2.95; range 0.02–10.57) (P = 0.04). Conclusions: The early induction of IPâ€10 and ILâ€2, as well as the subsequent overâ€production of ILâ€6 and lack of ILâ€10 production, probably contribute to the main immunoâ€pathological processes involved in lung injury in SARS. These changes in cytokine/chemokine profile are remarkably different from those observed in CAP patients.
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