Maternal Intake of Either Fructose or the Artificial Sweetener Acesulfame-K Results in Differential and Sex-Specific Alterations in Markers of Skin Inflammation and Wound Healing Responsiveness in Mouse Offspring: A Pilot Study

Author:

Bridge-Comer Pania E.1,Vickers Mark H.1ORCID,Ferraro Sandra23,Pagnon Aurélie4,Reynolds Clare M.5,Sigaudo-Roussel Dominique23

Affiliation:

1. Liggins Institute, University of Auckland, Auckland 1023, New Zealand

2. Laboratory of Tissue Biology and Therapeutic Engineering (LBTI), UMR 5305 National Center for Scientific Research (CNRS), 7 Passage du Vercors, CEDEX 7, 69367 Lyon, France

3. UFR Biosciences, University of Claude Bernard Lyon 1, 69622 Villeurbanne CEDEX, France

4. NOVOTEC, ZAC du Chene_Europarc, 11 Rue Edison, 69500 Bron, France

5. School of Public Health, Physiotherapy and Sports Science, Conway Institute, Institute of Food and Health, University College Dublin, 4 Dublin, Ireland

Abstract

Growing evidence has demonstrated that maternal artificial sweetener (AS) consumption may not be a beneficial alternative when compared to sugar-sweetened beverages and potentially leads to metabolic dysfunction in adult offspring. Compromised skin integrity and wound healing associated with type 2 diabetes can lead to complications such as diabetic pressure injury (PI). In this context, the skin plays an important role in the maintenance of metabolic homeostasis, yet there is limited information on the influence of sugar- or AS-sweetened beverages during pregnancy on developmental programming and offspring skin homeostasis. This study examined the impact of maternal fructose or acesulfame-k consumption on offspring wound healing. Female C57Bl/6 mice received a chow diet ad libitum with either water (CD), fructose (FR; 34.7 mM fructose), or AS (AS; 12.5 mM Acesulfame-K) throughout pregnancy and lactation. PIs were induced in offspring at 9 weeks of age (n = 6/sex/diet). PIs and healthy skin biopsies were collected for later analysis. Maternal AS intake increased skin inflammatory markers in healthy biopsies while an FR diet increased Tgfb expression, and both diets induced subtle changes in inflammatory markers post-wound inducement in a sex-specific manner. Furthermore, a maternal FR diet had a significant effect on pressure wound severity and early wound healing delay, while AS maternal diet had a sex-specific effect on the course of the healing process. This study demonstrates the need for a better understanding of developmental programming as a mediator of later-life skin integrity and wound responsiveness.

Funder

Faculty Research Development Fund

University of Auckland Foundation

University of Lyon

Health Research Council of New Zealand

Royal Society of New Zealand

University College Dublin

Publisher

MDPI AG

Subject

Food Science,Nutrition and Dietetics

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