Dietary intake of micronized avian eggshell membrane in aged mice reduces circulating inflammatory markers, increases microbiota diversity, and attenuates skeletal muscle aging

Sissel Beate Rønning; Harald Carlsen; Sérgio Domingos Cardoso Rocha; Ida Rud; Nina Solberg; Vibeke Høst; Eva Veiseth-Kent; Henriette Arnesen; Silje Bergum; Bente Kirkhus; Ulrike Böcker; Nada Abedali; Amanda Rundblad; Pia Bålsrud; Ingrid Måge; Kirsten Bjørklund Holven; Stine Marie Ulven; Mona Elisabeth Pedersen

doi:10.3389/fnut.2023.1336477

Dietary intake of micronized avian eggshell membrane in aged mice reduces circulating inflammatory markers, increases microbiota diversity, and attenuates skeletal muscle aging

Front Nutr. 2024 Jan 15:10:1336477. doi: 10.3389/fnut.2023.1336477. eCollection 2023.

Authors

Sissel Beate Rønning¹, Harald Carlsen², Sérgio Domingos Cardoso Rocha³, Ida Rud¹, Nina Solberg¹, Vibeke Høst¹, Eva Veiseth-Kent¹, Henriette Arnesen⁴, Silje Bergum¹, Bente Kirkhus¹, Ulrike Böcker¹, Nada Abedali⁵, Amanda Rundblad⁵, Pia Bålsrud⁵, Ingrid Måge¹, Kirsten Bjørklund Holven^{5

6}, Stine Marie Ulven⁵, Mona Elisabeth Pedersen¹

Affiliations

¹ Nofima AS, Food Division, Ås, Norway.
² Faculty of Chemistry, Biotechnology and Food Science, Norwegian University of Life Sciences, Ås, Norway.
³ Faculty of Biosciences, Norwegian University of Life Sciences, Ås, Norway.
⁴ Faculty of Veterinary Medicine, Norwegian University of Life Sciences, Ås, Norway.
⁵ Department of Nutrition, Institute of Basic Medical Sciences, University of Oslo, Oslo, Norway.
⁶ National Advisory Unit on Familial Hypercholesterolemia, Department of Endocrinology, Morbid Obesity and Preventive Medicine, Oslo University Hospital, Oslo, Norway.

Abstract

Introduction: Avian eggshell membrane (ESM) is a complex extracellular matrix comprising collagens, glycoproteins, proteoglycans, and hyaluronic acid. We have previously demonstrated that ESM possesses anti-inflammatory properties in vitro and regulates wound healing processes in vivo. The present study aimed to investigate if oral intake of micronized ESM could attenuate skeletal muscle aging associated with beneficial alterations in gut microbiota profile and reduced inflammation.

Methods: Elderly male C57BL/6 mice were fed an AIN93G diet supplemented with 0, 0.1, 1, or 8% ESM. Young mice were used as reference. The digestibility of ESM was investigated using the static in vitro digestion model INFOGEST for older people and adults, and the gut microbiota profile was analyzed in mice. In addition, we performed a small-scale pre-clinical human study with healthy home-dwelling elderly (>70 years) who received capsules with a placebo or 500 mg ESM every day for 4 weeks and studied the effect on circulating inflammatory markers.

Results and discussion: Intake of ESM in elderly mice impacted and attenuated several well-known hallmarks of aging, such as a reduction in the number of skeletal muscle fibers, the appearance of centronucleated fibers, a decrease in type IIa/IIx fiber type proportion, reduced gene expression of satellite cell markers Sdc3 and Pax7 and increased gene expression of the muscle atrophy marker Fbxo32. Similarly, a transition toward the phenotypic characteristics of young mice was observed for several proteins involved in cellular processes and metabolism. The digestibility of ESM was poor, especially for the elderly condition. Furthermore, our experiments showed that mice fed with 8% ESM had increased gut microbiota diversity and altered microbiota composition compared with the other groups. ESM in the diet also lowered the expression of the inflammation marker TNFA in mice and in vitro in THP-1 macrophages. In the human study, intake of ESM capsules significantly reduced the inflammatory marker CRP. Altogether, our results suggest that ESM, a natural extracellular biomaterial, may be attractive as a nutraceutical candidate with a possible effect on skeletal muscle aging possibly through its immunomodulating effect or gut microbiota.

Keywords: eggshell membrane; inflammatory responses; microbiota; protein digestibility; skeletal muscle aging.

Grants and funding

The author(s) declare financial support was received for the research, authorship, and/or publication of this article. This work was supported by a grant from the Research Council of Norway (NFR 282247) and the Norwegian Fund for Research Fees for Agricultural Products (FFL) for supporting the study through the project “SusHealth” (project number 314599) and “Precision” (project number 314111).