Changes to insulin sensitivity in glucose clearance systems and redox following dietary supplementation with a novel cysteine-rich protein: A pilot randomized controlled trial in humans with type-2 diabetes

We recently developed a novel keratin-derived protein (KDP) rich in cysteine, glycine, and arginine, with the potential to alter tissue redox status and insulin sensitivity. The KDP was tested in 35 human adults with type-2 diabetes mellitus (T2DM) in a 14-wk randomised controlled pilot trial compri...

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Autores principales: Peeters, W.M., Gram, M., Dias, G.J., Vissers, M.C.M., Hampton, M.B., Dickerhof, N., Bekhit, A.E., Black, M.J., Oxbøll, J., Bayer, S., Dickens, M., Vitzel, K., Sheard, P.W., Danielson, K.M., Hodges, L.D., Brønd, J.C., Bond, J., Perry, B.G., Stoner, L., Cornwall, J., Rowlands, D.S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2023
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10570009/
https://www.ncbi.nlm.nih.gov/pubmed/37812879
http://dx.doi.org/10.1016/j.redox.2023.102918
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author Peeters, W.M.
Gram, M.
Dias, G.J.
Vissers, M.C.M.
Hampton, M.B.
Dickerhof, N.
Bekhit, A.E.
Black, M.J.
Oxbøll, J.
Bayer, S.
Dickens, M.
Vitzel, K.
Sheard, P.W.
Danielson, K.M.
Hodges, L.D.
Brønd, J.C.
Bond, J.
Perry, B.G.
Stoner, L.
Cornwall, J.
Rowlands, D.S.
author_facet Peeters, W.M.
Gram, M.
Dias, G.J.
Vissers, M.C.M.
Hampton, M.B.
Dickerhof, N.
Bekhit, A.E.
Black, M.J.
Oxbøll, J.
Bayer, S.
Dickens, M.
Vitzel, K.
Sheard, P.W.
Danielson, K.M.
Hodges, L.D.
Brønd, J.C.
Bond, J.
Perry, B.G.
Stoner, L.
Cornwall, J.
Rowlands, D.S.
author_sort Peeters, W.M.
collection PubMed
description We recently developed a novel keratin-derived protein (KDP) rich in cysteine, glycine, and arginine, with the potential to alter tissue redox status and insulin sensitivity. The KDP was tested in 35 human adults with type-2 diabetes mellitus (T2DM) in a 14-wk randomised controlled pilot trial comprising three 2×20 g supplemental protein/day arms: KDP-whey (KDPWHE), whey (WHEY), non-protein isocaloric control (CON), with standardised exercise. Outcomes were measured morning fasted and following insulin-stimulation (80 mU/m(2)/min hyperinsulinaemic-isoglycaemic clamp). With KDPWHE supplementation there was good and very-good evidence for moderate-sized increases in insulin-stimulated glucose clearance rate (GCR; 26%; 90% confidence limits, CL 2%, 49%) and skeletal-muscle microvascular blood flow (46%; 16%, 83%), respectively, and good evidence for increased insulin-stimulated sarcoplasmic GLUT4 translocation (18%; 0%, 39%) vs CON. In contrast, WHEY did not effect GCR (-2%; -25%, 21%) and attenuated HbA1c lowering (14%; 5%, 24%) vs CON. KDPWHE effects on basal glutathione in erythrocytes and skeletal muscle were unclear, but in muscle there was very-good evidence for large increases in oxidised peroxiredoxin isoform 2 (oxiPRX2) (19%; 2.2%, 35%) and good evidence for lower GPx1 concentrations (-40%; -4.3%, -63%) vs CON; insulin stimulation, however, attenuated the basal oxiPRX2 response (4%; -16%, 24%), and increased GPx1 (39%; -5%, 101%) and SOD1 (26%; -3%, 60%) protein expression. Effects of KDPWHE on oxiPRX3 and NRF2 content, phosphorylation of capillary eNOS and insulin-signalling proteins upstream of GLUT4 translocation Akt(Ser437) and AS160(Thr642) were inconclusive, but there was good evidence for increased IRS(Ser312) (41%; 3%, 95%), insulin-stimulated NFκB-DNA binding (46%; 3.4%, 105%), and basal PAK-1(Thr423)/2(Thr402) phosphorylation (143%; 66%, 257%) vs WHEY. Our findings provide good evidence to suggest that dietary supplementation with a novel edible keratin protein in humans with T2DM may increase glucose clearance and modify skeletal-muscle tissue redox and insulin sensitivity within systems involving peroxiredoxins, antioxidant expression, and glucose uptake.
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spelling pubmed-105700092023-10-14 Changes to insulin sensitivity in glucose clearance systems and redox following dietary supplementation with a novel cysteine-rich protein: A pilot randomized controlled trial in humans with type-2 diabetes Peeters, W.M. Gram, M. Dias, G.J. Vissers, M.C.M. Hampton, M.B. Dickerhof, N. Bekhit, A.E. Black, M.J. Oxbøll, J. Bayer, S. Dickens, M. Vitzel, K. Sheard, P.W. Danielson, K.M. Hodges, L.D. Brønd, J.C. Bond, J. Perry, B.G. Stoner, L. Cornwall, J. Rowlands, D.S. Redox Biol Research Paper We recently developed a novel keratin-derived protein (KDP) rich in cysteine, glycine, and arginine, with the potential to alter tissue redox status and insulin sensitivity. The KDP was tested in 35 human adults with type-2 diabetes mellitus (T2DM) in a 14-wk randomised controlled pilot trial comprising three 2×20 g supplemental protein/day arms: KDP-whey (KDPWHE), whey (WHEY), non-protein isocaloric control (CON), with standardised exercise. Outcomes were measured morning fasted and following insulin-stimulation (80 mU/m(2)/min hyperinsulinaemic-isoglycaemic clamp). With KDPWHE supplementation there was good and very-good evidence for moderate-sized increases in insulin-stimulated glucose clearance rate (GCR; 26%; 90% confidence limits, CL 2%, 49%) and skeletal-muscle microvascular blood flow (46%; 16%, 83%), respectively, and good evidence for increased insulin-stimulated sarcoplasmic GLUT4 translocation (18%; 0%, 39%) vs CON. In contrast, WHEY did not effect GCR (-2%; -25%, 21%) and attenuated HbA1c lowering (14%; 5%, 24%) vs CON. KDPWHE effects on basal glutathione in erythrocytes and skeletal muscle were unclear, but in muscle there was very-good evidence for large increases in oxidised peroxiredoxin isoform 2 (oxiPRX2) (19%; 2.2%, 35%) and good evidence for lower GPx1 concentrations (-40%; -4.3%, -63%) vs CON; insulin stimulation, however, attenuated the basal oxiPRX2 response (4%; -16%, 24%), and increased GPx1 (39%; -5%, 101%) and SOD1 (26%; -3%, 60%) protein expression. Effects of KDPWHE on oxiPRX3 and NRF2 content, phosphorylation of capillary eNOS and insulin-signalling proteins upstream of GLUT4 translocation Akt(Ser437) and AS160(Thr642) were inconclusive, but there was good evidence for increased IRS(Ser312) (41%; 3%, 95%), insulin-stimulated NFκB-DNA binding (46%; 3.4%, 105%), and basal PAK-1(Thr423)/2(Thr402) phosphorylation (143%; 66%, 257%) vs WHEY. Our findings provide good evidence to suggest that dietary supplementation with a novel edible keratin protein in humans with T2DM may increase glucose clearance and modify skeletal-muscle tissue redox and insulin sensitivity within systems involving peroxiredoxins, antioxidant expression, and glucose uptake. Elsevier 2023-10-05 /pmc/articles/PMC10570009/ /pubmed/37812879 http://dx.doi.org/10.1016/j.redox.2023.102918 Text en © 2023 The Authors https://creativecommons.org/licenses/by/4.0/This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Research Paper
Peeters, W.M.
Gram, M.
Dias, G.J.
Vissers, M.C.M.
Hampton, M.B.
Dickerhof, N.
Bekhit, A.E.
Black, M.J.
Oxbøll, J.
Bayer, S.
Dickens, M.
Vitzel, K.
Sheard, P.W.
Danielson, K.M.
Hodges, L.D.
Brønd, J.C.
Bond, J.
Perry, B.G.
Stoner, L.
Cornwall, J.
Rowlands, D.S.
Changes to insulin sensitivity in glucose clearance systems and redox following dietary supplementation with a novel cysteine-rich protein: A pilot randomized controlled trial in humans with type-2 diabetes
title Changes to insulin sensitivity in glucose clearance systems and redox following dietary supplementation with a novel cysteine-rich protein: A pilot randomized controlled trial in humans with type-2 diabetes
title_full Changes to insulin sensitivity in glucose clearance systems and redox following dietary supplementation with a novel cysteine-rich protein: A pilot randomized controlled trial in humans with type-2 diabetes
title_fullStr Changes to insulin sensitivity in glucose clearance systems and redox following dietary supplementation with a novel cysteine-rich protein: A pilot randomized controlled trial in humans with type-2 diabetes
title_full_unstemmed Changes to insulin sensitivity in glucose clearance systems and redox following dietary supplementation with a novel cysteine-rich protein: A pilot randomized controlled trial in humans with type-2 diabetes
title_short Changes to insulin sensitivity in glucose clearance systems and redox following dietary supplementation with a novel cysteine-rich protein: A pilot randomized controlled trial in humans with type-2 diabetes
title_sort changes to insulin sensitivity in glucose clearance systems and redox following dietary supplementation with a novel cysteine-rich protein: a pilot randomized controlled trial in humans with type-2 diabetes
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10570009/
https://www.ncbi.nlm.nih.gov/pubmed/37812879
http://dx.doi.org/10.1016/j.redox.2023.102918
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