Cryptococcus neoformans induces IL-8 secretion and CXCL1 expression by human bronchial epithelial cells

A Odom; B Schmeck; BC Fries; CN Still; DL Goldman; DL Goldman; E Hoffmann; FL Wormley Jr.; FM Barbosa; FM Barbosa; G Diamond; GB Huffnagle; GJ Merkel; HA Torres; J Rivera; JR Perfect; K Kawakami; K Kawakami; KL Wozniak; L Guillot; L Guillot; L Li; M Del Poeta; P Amstad; P Zhang; Q Sha; R Bals; R Ganendren; S Agarwal; S Hippenstiel; SM Levitz; T Matsusaka; TG Mitchell; TN Cassel; V Lakshminarayanan; W Chaka; X Lin; X Shao; Y Ishikawa; YC Chang; Z Zhang

Cryptococcus neoformans induces IL-8 secretion and CXCL1 expression by human bronchial epithelial cells

Authors: A Odom
B Schmeck
BC Fries
CN Still
DL Goldman
DL Goldman
E Hoffmann
FL Wormley Jr.
FM Barbosa
FM Barbosa
G Diamond
GB Huffnagle
GJ Merkel
HA Torres
J Rivera
JR Perfect
K Kawakami
K Kawakami
KL Wozniak
L Guillot
L Guillot
L Li
M Del Poeta
P Amstad
P Zhang
Q Sha
R Bals
R Ganendren
S Agarwal
S Hippenstiel
SM Levitz
T Matsusaka
TG Mitchell
TN Cassel
V Lakshminarayanan
W Chaka
X Lin
X Shao
Y Ishikawa
YC Chang
Z Zhang
Publication date: 1 January 2008
Publisher: BioMed Central
Doi

Abstract

Abstract Background <it>Cryptococcus neoformans </it>(<it>C. neoformans</it>) is a globally distributed fungal pathogen with the potential to cause serious disease, particularly among immune compromised hosts. Exposure to this organism is believed to occur by inhalation and may result in pneumonia and/or disseminated infection of the brain as well as other organs. Little is known about the role of airway epithelial cells in cryptococcal recognition or their ability to induce an inflammatory response. Methods Immortalized BEAS-2B bronchial epithelial cells and primary normal human bronchial epithelium (NHBE) were stimulated <it>in vitro </it>with encapsulated or acapsular <it>C. neoformans </it>cultivated at room temperature or 37°C. Activation of bronchial epithelial cells was characterized by analysis of inflammatory cytokine and chemokine expression, transcription factor activation, fungal-host cell association, and host cell damage. Results Viable <it>C. neoformans </it>is a strong activator of BEAS-2B cells, resulting in the production of the neutrophil chemokine Interleukin (IL)-8 in a time- and dose-dependent manner. IL-8 production was observed only in response to acapsular <it>C. neoformans </it>that was grown at 37°C. <it>C. neoformans </it>was also able to induce the expression of the chemokine CXCL1 and the transcription factor CAAT/enhancer-binding protein beta (CEBP/β) in BEAS-2B cells. NHBE was highly responsive to stimulation with <it>C. neoformans</it>; in addition to transcriptional up regulation of CXCL1, these primary cells exhibited the greatest IL-8 secretion and cell damage in response to stimulation with an acapsular strain of <it>C. neoformans</it>. Conclusion This study demonstrates that human bronchial epithelial cells mediate an acute inflammatory response to <it>C. neoformans </it>and are susceptible to damage by this fungal pathogen. The presence of capsular polysaccharide and <it>in vitro </it>fungal culture conditions modulate the host inflammatory response to <it>C. neoformans</it>. Human bronchial epithelial cells are likely to contribute to the initial stages of pulmonary host defense <it>in vivo</it>.</p