Literature DB >> 10973493

Portosystemic shunting and persistent fetal vascular structures in aryl hydrocarbon receptor-deficient mice.

G P Lahvis1, S L Lindell, R S Thomas, R S McCuskey, C Murphy, E Glover, M Bentz, J Southard, C A Bradfield.   

Abstract

A physiological examination of mice harboring a null allele at the aryl hydrocarbon (Ah) locus revealed that the encoded aryl hydrocarbon receptor plays a role in the resolution of fetal vascular structures during development. Although the aryl hydrocarbon receptor is more commonly studied for its role in regulating xenobiotic metabolism and dioxin toxicity, a developmental role of this protein is supported by the observation that Ah null mice display smaller livers, reduced fecundity, and decreased body weights. Upon investigating the liver phenotype, we found that the decrease in liver size is directly related to a reduction in hepatocyte size. We also found that smaller hepatocyte size is the result of massive portosystemic shunting in null animals. Colloidal carbon uptake and microsphere perfusion studies indicated that 56% of portal blood flow bypasses the liver sinusoids. Latex corrosion casts and angiography demonstrated that shunting is consistent with the existence of a patent ductus venosus in adult animals. Importantly, fetal vascular structures were also observed at other sites. Intravital microscopy demonstrated an immature sinusoidal architecture in the liver and persistent hyaloid arteries in the eyes of adult Ah null mice, whereas corrosion casting experiments described aberrations in kidney vascular patterns.

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Year:  2000        PMID: 10973493      PMCID: PMC27043          DOI: 10.1073/pnas.190256997

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  44 in total

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Journal:  Proc Natl Acad Sci U S A       Date:  1993-09-15       Impact factor: 11.205

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Authors:  H Reyes; S Reisz-Porszasz; O Hankinson
Journal:  Science       Date:  1992-05-22       Impact factor: 47.728

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Journal:  Am J Physiol       Date:  1981-05

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Journal:  J Pediatr Ophthalmol Strabismus       Date:  1985 Sep-Oct       Impact factor: 1.402

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  106 in total

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Review 3.  Dioxins: diagnostic and prognostic challenges arising from complex mechanisms.

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Journal:  Biochem Pharmacol       Date:  2010-03-30       Impact factor: 5.858

5.  Aryl hydrocarbon receptor-dependent liver development and hepatotoxicity are mediated by different cell types.

Authors:  Jacqueline A Walisser; Edward Glover; Kalyan Pande; Adam L Liss; Christopher A Bradfield
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6.  Endothelial cell-specific aryl hydrocarbon receptor knockout mice exhibit hypotension mediated, in part, by an attenuated angiotensin II responsiveness.

Authors:  Larry N Agbor; Khalid M Elased; Mary K Walker
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7.  A hypomorphic allele of aryl hydrocarbon receptor-associated protein-9 produces a phenocopy of the AHR-null mouse.

Authors:  Bernice C Lin; Linh P Nguyen; Jacqueline A Walisser; Christopher A Bradfield
Journal:  Mol Pharmacol       Date:  2008-07-31       Impact factor: 4.436

8.  Nonadditive effects of PAHs on Early Vertebrate Development: mechanisms and implications for risk assessment.

Authors:  Sonya M Billiard; Joel N Meyer; Deena M Wassenberg; Peter V Hodson; Richard T Di Giulio
Journal:  Toxicol Sci       Date:  2007-12-20       Impact factor: 4.849

9.  Genomewide analysis of aryl hydrocarbon receptor binding targets reveals an extensive array of gene clusters that control morphogenetic and developmental programs.

Authors:  Maureen A Sartor; Michael Schnekenburger; Jennifer L Marlowe; John F Reichard; Ying Wang; Yunxia Fan; Ci Ma; Saikumar Karyala; Danielle Halbleib; Xiangdong Liu; Mario Medvedovic; Alvaro Puga
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10.  Dioxin-dependent and dioxin-independent gene batteries: comparison of liver and kidney in AHR-null mice.

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