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Authordc.contributor.authorNanthakumar, Nanda 
Authordc.contributor.authorMeng, Di es_CL
Authordc.contributor.authorGoldstein, Allan M. es_CL
Authordc.contributor.authorZhu, Weishu es_CL
Authordc.contributor.authorLu, Lei es_CL
Authordc.contributor.authorUauy Dagach-Imbarack, Ricardo es_CL
Authordc.contributor.authorLlanos, Adolfo es_CL
Authordc.contributor.authorClaud, Erika C. es_CL
Authordc.contributor.authorWalker, W. Allan es_CL
Admission datedc.date.accessioned2011-11-28T16:25:00Z
Available datedc.date.available2011-11-28T16:25:00Z
Publication datedc.date.issued2011-03-21
Cita de ítemdc.identifier.citationPLOS ONE Volume: 6 Issue: 3 Article Number: e17776 Published: MAR 21 2011es_CL
Identifierdc.identifier.issn1932-6203
Identifierdc.identifier.otherDOI: 10.1371/journal.pone.0017776
Identifierdc.identifier.urihttps://repositorio.uchile.cl/handle/2250/123990
General notedc.descriptionArtículo de publicación ISIes_CL
Abstractdc.description.abstractNecrotizing enterocolitis (NEC) is a devastating neonatal intestinal inflammatory disease, occurring primarily in premature infants, causing significant morbidity and mortality. The pathogenesis of NEC is associated with an excessive inflammatory IL-8 response. In this study, we hypothesized that this excessive inflammatory response is related to an immature expression of innate immune response genes. To address this hypothesis, intestinal RNA expression analysis of innate immune response genes was performed after laser capture microdissection of resected ileal epithelium from fetuses, NEC patients and children and confirmed in ex vivo human intestinal xenografts. Changes in mRNA levels of toll-like receptors (TLR)-2 and -4, their signaling molecules and transcription factors (MyD88, TRAF-6 and NF kappa B1) and negative regulators (SIGIRR, IRAK-M, A-20 and TOLLIP) and the effector IL-8 were characterized by qRT-PCR. The expression of TLR2, TLR4, MyD88, TRAF-6, NFkB1 and IL-8 mRNA was increased while SIGIRR, IRAK-M, A-20 and TOLLIP mRNA were decreased in fetal vs. mature human enterocytes and further altered in NEC enterocytes. Similar changes in mRNA expression were observed in immature, but not mature, human intestinal xenografts. Confirmation of gene expression was also validated with selective protein measurements and with suggested evidence that immature TRL4 enterocyte surface expression was internalized in mature enterocytes. Cortisone, an intestinal maturation factor, treatment corrected the mRNA differences only in the immature intestinal xenograft. Using specific siRNA to attenuate expression of primary fetal enterocyte cultures, both TOLLIP and A-20 were confirmed to be important when knocked down by exhibiting the same excessive inflammatory response seen in the NEC intestine. We conclude that the excessive inflammatory response of the immature intestine, a hallmark of NEC, is due to a developmental immaturity in innate immune response genes.es_CL
Patrocinadordc.description.sponsorshipNational Institutes of Health (NIH) R01 HD059126 R01-HD012437 R01 DK070260 P01 DK033506 P30 DK040561 R01 DK080914 R01 HD059123 R21 HD055237 R21 AT004044es_CL
Lenguagedc.language.isoenes_CL
Publisherdc.publisherPUBLIC LIBRARY SCIENCEes_CL
Keywordsdc.subjectEPITHELIAL-CELLSes_CL
Títulodc.titleThe Mechanism of Excessive Intestinal Inflammation in Necrotizing Enterocolitis: An Immature Innate Immune Responsees_CL
Document typedc.typeArtículo de revista


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