Genome-wide gene expression analysis implicates the immune response and lymphangiogenesis in the pathogenesis of fetal chylothorax.
Fetal chylothorax (FC) is a rare condition characterized by lymphocyte-rich pleural effusion. Although its pathogenesis remains elusive, it may involve inflammation, since there are increased concentrations of proinflammatory mediators in pleural fluids. Only a few hereditary lymphedema-associated g...
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2012-01-01
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doaj-ebcd4dce1ea547cca3904f0e525d1a072020-11-25T02:26:58ZengPublic Library of Science (PLoS)PLoS ONE1932-62032012-01-0174e3490110.1371/journal.pone.0034901Genome-wide gene expression analysis implicates the immune response and lymphangiogenesis in the pathogenesis of fetal chylothorax.Chen-Hsiang YeangGwo-Chin MaJin-Chung ShihYu-Shih YangChih-Ping ChenShun-Ping ChangSheng-Hai WuChin-San LiuShou-Jen KuoHung-Chieh ChouWuh-Liang HwuAlan D CameronNorman A GinsbergYi-Shing LinMing ChenFetal chylothorax (FC) is a rare condition characterized by lymphocyte-rich pleural effusion. Although its pathogenesis remains elusive, it may involve inflammation, since there are increased concentrations of proinflammatory mediators in pleural fluids. Only a few hereditary lymphedema-associated gene loci, e.g. VEGFR3, ITGA9 and PTPN11, were detected in human fetuses with this condition; these cases had a poorer prognosis, due to defective lymphangiogenesis. In the present study, genome-wide gene expression analysis was conducted, comparing pleural and ascitic fluids in three hydropic fetuses, one with and two without the ITGA9 mutation. One fetus (the index case), from a dizygotic pregnancy (the cotwin was unaffected), received antenatal OK-432 pleurodesis and survived beyond the neonatal stage, despite having the ITGA9 mutation. Genes and pathways involved in the immune response were universally up-regulated in fetal pleural fluids compared to those in ascitic fluids. Furthermore, genes involved in the lymphangiogenesis pathway were down-regulated in fetal pleural fluids (compared to ascitic fluid), but following OK-432 pleurodesis, they were up-regulated. Expression of ITGA9 was concordant with overall trends of lymphangiogenesis. In conclusion, we inferred that both the immune response and lymphangiogenesis were implicated in the pathogenesis of fetal chylothorax. Furthermore, genome-wide gene expression microarray analysis may facilitate personalized medicine by selecting the most appropriate treatment, according to the specific circumstances of the patient, for this rare, but heterogeneous disease.http://europepmc.org/articles/PMC3329545?pdf=render |
| collection |
DOAJ |
| language |
English |
| format |
Article |
| sources |
DOAJ |
| author |
Chen-Hsiang Yeang Gwo-Chin Ma Jin-Chung Shih Yu-Shih Yang Chih-Ping Chen Shun-Ping Chang Sheng-Hai Wu Chin-San Liu Shou-Jen Kuo Hung-Chieh Chou Wuh-Liang Hwu Alan D Cameron Norman A Ginsberg Yi-Shing Lin Ming Chen |
| spellingShingle |
Chen-Hsiang Yeang Gwo-Chin Ma Jin-Chung Shih Yu-Shih Yang Chih-Ping Chen Shun-Ping Chang Sheng-Hai Wu Chin-San Liu Shou-Jen Kuo Hung-Chieh Chou Wuh-Liang Hwu Alan D Cameron Norman A Ginsberg Yi-Shing Lin Ming Chen Genome-wide gene expression analysis implicates the immune response and lymphangiogenesis in the pathogenesis of fetal chylothorax. PLoS ONE |
| author_facet |
Chen-Hsiang Yeang Gwo-Chin Ma Jin-Chung Shih Yu-Shih Yang Chih-Ping Chen Shun-Ping Chang Sheng-Hai Wu Chin-San Liu Shou-Jen Kuo Hung-Chieh Chou Wuh-Liang Hwu Alan D Cameron Norman A Ginsberg Yi-Shing Lin Ming Chen |
| author_sort |
Chen-Hsiang Yeang |
| title |
Genome-wide gene expression analysis implicates the immune response and lymphangiogenesis in the pathogenesis of fetal chylothorax. |
| title_short |
Genome-wide gene expression analysis implicates the immune response and lymphangiogenesis in the pathogenesis of fetal chylothorax. |
| title_full |
Genome-wide gene expression analysis implicates the immune response and lymphangiogenesis in the pathogenesis of fetal chylothorax. |
| title_fullStr |
Genome-wide gene expression analysis implicates the immune response and lymphangiogenesis in the pathogenesis of fetal chylothorax. |
| title_full_unstemmed |
Genome-wide gene expression analysis implicates the immune response and lymphangiogenesis in the pathogenesis of fetal chylothorax. |
| title_sort |
genome-wide gene expression analysis implicates the immune response and lymphangiogenesis in the pathogenesis of fetal chylothorax. |
| publisher |
Public Library of Science (PLoS) |
| series |
PLoS ONE |
| issn |
1932-6203 |
| publishDate |
2012-01-01 |
| description |
Fetal chylothorax (FC) is a rare condition characterized by lymphocyte-rich pleural effusion. Although its pathogenesis remains elusive, it may involve inflammation, since there are increased concentrations of proinflammatory mediators in pleural fluids. Only a few hereditary lymphedema-associated gene loci, e.g. VEGFR3, ITGA9 and PTPN11, were detected in human fetuses with this condition; these cases had a poorer prognosis, due to defective lymphangiogenesis. In the present study, genome-wide gene expression analysis was conducted, comparing pleural and ascitic fluids in three hydropic fetuses, one with and two without the ITGA9 mutation. One fetus (the index case), from a dizygotic pregnancy (the cotwin was unaffected), received antenatal OK-432 pleurodesis and survived beyond the neonatal stage, despite having the ITGA9 mutation. Genes and pathways involved in the immune response were universally up-regulated in fetal pleural fluids compared to those in ascitic fluids. Furthermore, genes involved in the lymphangiogenesis pathway were down-regulated in fetal pleural fluids (compared to ascitic fluid), but following OK-432 pleurodesis, they were up-regulated. Expression of ITGA9 was concordant with overall trends of lymphangiogenesis. In conclusion, we inferred that both the immune response and lymphangiogenesis were implicated in the pathogenesis of fetal chylothorax. Furthermore, genome-wide gene expression microarray analysis may facilitate personalized medicine by selecting the most appropriate treatment, according to the specific circumstances of the patient, for this rare, but heterogeneous disease. |
| url |
http://europepmc.org/articles/PMC3329545?pdf=render |
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