Abstract

- With improved survival of the premature infant, immaturity of the stratum corneum (SC) with an incompetent cutaneous barrier has become a major source of morbidity. The investigator has recently shown that ligands of several receptors in the nuclear receptor superfamily (for example, glucocorticoids, thyroid hormone) are important regulators of fetal SC development. However, because SC development proceeds normally in fetal skin organ cultures in the absence of hormones and in vivo in the face of glucocorticoid or thyroid hormone deficiency the applicants hypothesized that fetal SC development may also be activated by locally generated ligands of nuclear hormone receptors. Recently, they have shown that activators of PPARalpha (activator-fatty acids) or FXR (activator-farnesol, an isoprenoid derived from intermediates in the cholesterol biosynthetic pathway) accelerate fetal epidermal and SC development. Fetal epidermis is a very active site of both fatty acid and cholesterol synthesis, and therefore both of these nuclear hormone receptor ligands/activators are produced locally and thereby could modulate SC development. Both PPARalpha and FXR are members of the RXR subgroup of nuclear hormones receptors which also includes RXR, RAR, and Vitamin D receptor. Given the important regulatory role of nuclear receptors in the skin it is likely that both PPARalpha and FXR will also have crucial roles in epidermal physiology. Hypothesis: Formation of the SC and a competent barrier during fetal development requires both the generation of extracellular lipid-enriched lamellar membranes and the cornified envelope, both of which are regulated by activation of PPARalpha and/or FXR nuclear receptors.
Specific Aims : 1) To determine if PPARalpha and FXR activators accelerate SC development in utero and following premature birth. 2) To elucidate the basis for the acceleration of SC ontogenesis the investigators will determine if PPARalpha and/or FXR activators increase the expression and/or activity of key enzymes and structural proteins required for SC formation. 3) To determine if PPARalpha and/or FXR are the crucial signaling proteins that regulate the timetable of development of the SC/permeability barrier.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Project (R01)
Project #
5R01HD029706-07
Application #
6182218
Study Section
General Medicine A Subcommittee 2 (GMA)
Program Officer
Catz, Charlotte S
Project Start
1994-05-15
Project End
2003-04-30
Budget Start
2000-05-01
Budget End
2001-04-30
Support Year
7
Fiscal Year
2000
Total Cost
$231,812
Indirect Cost

  Institution

Name
Northern California Institute Research & Education
Department
Type
DUNS #
City
San Francisco
State
CA
Country
United States
Zip Code
94121

  Publications

Feingold, Kenneth R; Moser, Arthur; Shigenaga, Judy K et al. (2014) Inflammation stimulates niacin receptor (GPR109A/HCA2) expression in adipose tissue and macrophages. J Lipid Res 55:2501-8
Feingold, Kenneth R; Shigenaga, Judy K; Kazemi, Mahmood R et al. (2012) Mechanisms of triglyceride accumulation in activated macrophages. J Leukoc Biol 92:829-39
Feingold, Kenneth R; Grunfeld, Carl; Heuer, Josef G et al. (2012) FGF21 is increased by inflammatory stimuli and protects leptin-deficient ob/ob mice from the toxicity of sepsis. Endocrinology 153:2689-700
Feingold, Kenneth R; Shigenaga, Judy K; Cross, Andrew S et al. (2012) Angiopoietin like protein 4 expression is decreased in activated macrophages. Biochem Biophys Res Commun 421:612-5
Feingold, Kenneth R; Moser, Arthur; Shigenaga, Judy K et al. (2011) Inflammation inhibits GPR81 expression in adipose tissue. Inflamm Res 60:991-5
Feingold, Kenneth R; Shigenaga, Judy K; Patzek, Sophie M et al. (2011) Endotoxin, zymosan, and cytokines decrease the expression of the transcription factor, carbohydrate response element binding protein, and its target genes. Innate Immun 17:174-82
Hachem, Jean-Pierre; Roelandt, Truus; Schürer, Nanna et al. (2010) Acute acidification of stratum corneum membrane domains using polyhydroxyl acids improves lipid processing and inhibits degradation of corneodesmosomes. J Invest Dermatol 130:500-10
Lu, Biao; Moser, Arthur; Shigenaga, Judy K et al. (2010) The acute phase response stimulates the expression of angiopoietin like protein 4. Biochem Biophys Res Commun 391:1737-41
Feingold, Kenneth R; Kazemi, Mahmood R; Magra, Amy L et al. (2010) ADRP/ADFP and Mal1 expression are increased in macrophages treated with TLR agonists. Atherosclerosis 209:81-8
Fluhr, Joachim W; Elias, Peter M; Man, Mao-Qiang et al. (2010) Is the filaggrin-histidine-urocanic acid pathway essential for stratum corneum acidification? J Invest Dermatol 130:2141-4

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