Oxylipin secretion by human CD3+ T lymphocytes in vitro is modified by the exogenous essential fatty acid ratio and life stage

Johanna von Gerichten; Annette L West; Nicola A Irvine; Elizabeth A Miles; Philip C Calder; Karen A Lillycrop; Graham C Burdge; Barbara A Fielding

doi:10.3389/fimmu.2023.1206733

Oxylipin secretion by human CD3⁺ T lymphocytes in vitro is modified by the exogenous essential fatty acid ratio and life stage

Front Immunol. 2023 Jun 14:14:1206733. doi: 10.3389/fimmu.2023.1206733. eCollection 2023.

Authors

Johanna von Gerichten¹, Annette L West², Nicola A Irvine², Elizabeth A Miles², Philip C Calder^{2

3}, Karen A Lillycrop⁴, Graham C Burdge^{2

3}, Barbara A Fielding⁵

Affiliations

¹ School of Chemistry and Chemical Engineering, Faculty of Engineering and Physical Sciences, University of Surrey, Guildford, Surrey, United Kingdom.
² School of Human Development and Health, Faculty of Medicine, University of Southampton, Southampton, Hampshire, United Kingdom.
³ NIHR Southampton Biomedical Research Centre, University Hospital Southampton NHS Foundation Trust and University of Southampton, Southampton, Hampshire, United Kingdom.
⁴ Centre for Biological Sciences, Faculty of Natural and Environmental Sciences, University of Southampton, Southampton, Hampshire, United Kingdom.
⁵ Department of Nutritional Sciences, Faculty of Health and Medical Sciences, University of Surrey, Guildford, Surrey, United Kingdom.

Abstract

Immune function changes across the life stages; for example, senior adults exhibit a tendency towards a weaker cell-mediated immune response and a stronger inflammatory response than younger adults. This might be partly mediated by changes in oxylipin synthesis across the life course. Oxylipins are oxidation products of polyunsaturated fatty acids (PUFAs) that modulate immune function and inflammation. A number of PUFAs are precursors to oxylipins, including the essential fatty acids (EFAs) linoleic acid (LA) and α-linolenic acid (ALA). LA and ALA are also substrates for synthesis of longer chain PUFAs. Studies with stable isotopes have shown that the relative amounts of LA and ALA can influence their partitioning by T lymphocytes between conversion to longer chain PUFAs and to oxylipins. It is not known whether the relative availability of EFA substrates influences the overall pattern of oxylipin secretion by human T cells or if this changes across the life stages. To address this, the oxylipin profile was determined in supernatants from resting and mitogen activated human CD3⁺ T cell cultures incubated in medium containing an EFA ratio of either 5:1 or 8:1 (LA : ALA). Furthermore, oxylipin profiles in supernatants of T cells from three life stages, namely fetal (derived from umbilical cord blood), adults and seniors, treated with the 5:1 EFA ratio were determined. The extracellular oxylipin profiles were affected more by the EFA ratio than mitogen stimulation such that n-3 PUFA-derived oxylipin concentrations were higher with the 5:1 EFA ratio than the 8:1 ratio, possibly due to PUFA precursor competition for lipoxygenases. 47 oxylipin species were measured in all cell culture supernatants. Extracellular oxylipin concentrations were generally higher for fetal T cells than for T cells from adult and senior donors, although the composition of oxylipins was similar across the life stages. The contribution of oxylipins towards an immunological phenotype might be due to the capacity of T cells to synthesize oxylipins rather than the nature of the oxylipins produced.

Keywords: T lymphocytes; eicosanoid; immunosenescence; lipid metabolism; oxylipin.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adult
Fatty Acids, Essential
Fatty Acids, Omega-3*
Humans
Linoleic Acid
Mitogens
Oxylipins*
T-Lymphocytes

Substances

Oxylipins
Mitogens
Fatty Acids, Essential
Fatty Acids, Omega-3
Linoleic Acid

Grants and funding

This research was supported by grants from the Biological Sciences and Biotechnology Research Council (grant numbers BB/S00548X/1, BB/S005358/1 and BB/R00028X/1). GB and PC are supported by the National Institute for Health and Care Research through the NIHR Southampton Biomedical Research Centre. The funder was not involved in the study design, collection, analysis, interpretation of data, the writing of this article, or the decision to submit it for publication. Publication costs were paid by the University of Surrey.