Epithelial cells in fetal intestine produce chemerin to recruit macrophages

doi:10.1152/ajpgi.90730.2008

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Am J Physiol Gastrointest Liver Physiol 297: G1-G10, 2009. First published May 14, 2009; doi:10.1152/ajpgi.90730.2008
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MUCOSAL BIOLOGY

Epithelial cells in fetal intestine produce chemerin to recruit macrophages

Akhil Maheshwari,¹^,2^,3^,4 Ashish R. Kurundkar,¹ Sadiq S. Shaik,¹ David R. Kelly,³ Yolanda Hartman,¹ Wei Zhang,¹ Reed Dimmitt,¹^,5 Shehzad Saeed,¹ David A. Randolph,¹ Charles Aprahamian,⁵ Geeta Datta,⁶ and Robin K. Ohls⁷

Departments of ¹Pediatrics, ²Cell Biology, ³Pathology, ⁵Surgery, and ⁶Internal Medicine, University of Alabama at Birmingham (UAB), Birmingham, Alabama; ⁴Translational Research in Normal and Disordered Development (TReNDD) Program, UAB Department of Pediatrics; and ⁷Department of Pediatrics, University of New Mexico, Albuquerque, New Mexico

Submitted 29 December 2008 ; accepted in final form 10 May 2009

Macrophages are first seen in the fetal intestine at 11–12wk and rapidly increase in number during the 12- to 22-wk periodof gestation. The development of macrophage populations in thefetal intestine precedes the appearance of lymphocytes and neutrophilsand does not require the presence of dietary or microbial antigens.In this study, we investigated the role of chemerin, a recentlydiscovered, relatively selective chemoattractant for macrophages,in the recruitment of macrophage precursors to the fetal intestine.Chemerin mRNA/protein expression was measured in jejunoilealtissue from 10- to 24-wk human fetuses, neonates operated forintestinal obstruction, and adults undergoing bariatric surgery.The expression of chemerin in intestinal epithelial cells (IECs)was confirmed by using cultured primary IECs and IEC-like celllines in vitro. The regulatory mechanisms involved in chemerinexpression were investigated by in silico and immunolocalizationtechniques. IECs in the fetal, but not mature, intestine expresschemerin. Chemerin expression peaked in the fetal intestineat 20–24 wk and then decreased to original low levelsby full term. During the 10- to 24-wk period, chemerin accountedfor most of the macrophage chemotactic activity of culturedfetal IECs. The maturational changes in chemerin expressioncorrelated with the expression of retinoic acid receptor-βin the intestine. Chemerin is an important mediator of epithelial-macrophagecross talk in the fetal/premature, but not in the mature, intestine.Understanding the regulation of the gut macrophage pool is animportant step in development of novel strategies to boost mucosalimmunity in premature infants and other patient populationsat risk of microbial translocation.

intestine; chemotaxis; enterocyte; cytokine; development

Address for reprint requests and other correspondence: A. Maheshwari, Pediatrics/Neonatology, Univ. of Alabama at Birmingham, VH648C, 1670 Univ. Blvd., Birmingham, AL 35294 (e-mail: akhil{at}peds.uab.edu)