A novel long chain polyunsaturated fatty acid, β-oxa 21:3n-3, inhibits T lymphocyte proliferation, cytokine production, delayed-type hypersensitivity, and carrageenan-induced paw reaction and selectively targets intracellular signals

被引：21

作者：

Costabile, M

Hii, CST

Robinson, BS

Rathjen, DA

Pitt, M

Easton, C

Miller, RC

Poulos, A

Murray, AW

Ferrante, A

机构：

[1] Univ Adelaide, Womens & Childrens Hosp, Dept Immunopathol, Adelaide, SA 5006, Australia

[2] Univ Adelaide, Womens & Childrens Hosp, Dept Paediat, Adelaide, SA 5006, Australia

[3] Univ S Australia, Sch Pharmaceut Mol & Biomed Sci, Adelaide, SA 5001, Australia

[4] Australian Natl Univ, Res Sch Chem, Canberra, ACT, Australia

[5] Flinders Univ S Australia, Sch Biol Sci, Adelaide, SA 5001, Australia

[6] Peptech Ltd, N Ryde, NSW, Australia

来源：

JOURNAL OF IMMUNOLOGY | 2001年 / 167卷 / 07期

关键词：

D O I：

10.4049/jimmunol.167.7.3980

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

A novel polyunsaturated fatty acid (PUFA), beta -oxa 21:3n-3, containing an oxygen atom in the beta position, was chemically synthesized, and found to have more selective biological activity than the n-3 PUFA, docosahexaenoic acid (22:6n-3) on cells of the immune system. Although beta -oxa 21:3n-3 was very poor compared with 22:6n-3 at stimulating oxygen radical production in neutrophils, it was more effective at inhibiting human T lymphocyte proliferation (IC50 of 1.9 vs 5.2 muM, respectively). beta -Oxa 21:3n-3 also inhibited the production of TNF-beta, IFN-gamma, and IL-2 by purified human T lymphocytes stimulated with PHA plus PMA, anti-CD3 plus anti-CD28 mAbs, or PMA plus A23187. Metabolism of beta -oxa 21:3n-3 via the cyclooxygenase and lipoxygenase pathways was not required for its inhibitory effects. Consistent with its ability to suppress T lymphocyte function, beta -oxa 21:3n-3 significantly inhibited the delayed-type hypersensitivity response and carrageenan-induced paw edema in mice. In T lymphocytes, beta -oxa 21:3n-3 inhibited the agonist-stimulated translocation of protein kinase C-betaI and -epsilon, but not -alpha, -beta II, or -theta to a particulate fraction, and also inhibited the activation of the extracellular signal-regulated protein kinase, but not c-Jun NH2 terminal kinase and p38. In contrast, 22:6n-3 had no effects on these protein kinase C isozymes. The increase in antiinflammatory activity and loss of unwanted bioaction through the generation of a novel synthetic 22:6n-3 analogue provides evidence for a novel strategy in the development of anti-inflammatory agents by chemically engineering PUFA.

引用

页码：3980 / 3987

页数：8

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