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Protein Extract of a Probiotic Strain of Hafnia alvei and Bacterial ClpB Protein Improve Glucose Tolerance in Mice

A commercial strain of Hafnia alvei (H. alvei) 4597 bacteria was shown to reduce food intake and promote weight loss, effects possibly induced by the bacterial protein ClpB, an antigen-mimetic of the anorexigenic α-melanocyte-stimulating hormone. A decrease in the basal plasma glucose levels was als...

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Autores principales: Zolotarev, Vasiliy A., Murovets, Vladimir O., Sepp, Anastasiya L., Sozontov, Egor A., Lukina, Ekaterina A., Khropycheva, Raisa P., Pestereva, Nina S., Ivleva, Irina S., El Mehdi, Mouna, Lahaye, Emilie, Chartrel, Nicolas, Fetissov, Sergueï O.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10341392/
https://www.ncbi.nlm.nih.gov/pubmed/37445766
http://dx.doi.org/10.3390/ijms241310590
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author Zolotarev, Vasiliy A.
Murovets, Vladimir O.
Sepp, Anastasiya L.
Sozontov, Egor A.
Lukina, Ekaterina A.
Khropycheva, Raisa P.
Pestereva, Nina S.
Ivleva, Irina S.
El Mehdi, Mouna
Lahaye, Emilie
Chartrel, Nicolas
Fetissov, Sergueï O.
author_facet Zolotarev, Vasiliy A.
Murovets, Vladimir O.
Sepp, Anastasiya L.
Sozontov, Egor A.
Lukina, Ekaterina A.
Khropycheva, Raisa P.
Pestereva, Nina S.
Ivleva, Irina S.
El Mehdi, Mouna
Lahaye, Emilie
Chartrel, Nicolas
Fetissov, Sergueï O.
author_sort Zolotarev, Vasiliy A.
collection PubMed
description A commercial strain of Hafnia alvei (H. alvei) 4597 bacteria was shown to reduce food intake and promote weight loss, effects possibly induced by the bacterial protein ClpB, an antigen-mimetic of the anorexigenic α-melanocyte-stimulating hormone. A decrease in the basal plasma glucose levels was also observed in overweight fasted humans and mice receiving H. alvei. However, it is not known whether H. alvei influences sweet taste preference and whether its protein extract or ClpB are sufficient to increase glucose tolerance; these are the objectives tested in the present study. C57BL/6J male mice were kept under standard diet and were gavaged daily for 17 days with a suspension of H. alvei (4.5 × 10(7) CFU/animal) or with H. alvei total protein extract (5 μg/animal) or saline as a control. Sweet taste preference was analyzed via a brief-access licking test with sucrose solution. Glucose tolerance tests (GTT) were performed after the intraperitoneal (IP) or intragastric (IG) glucose administration at the 9th and 15th days of gavage, respectively. The expression of regulatory peptides’ mRNA levels was assayed in the hypothalamus. In another experiment performed in non-treated C57BL/6J male mice, effects of acute IP administration of recombinant ClpB protein on glucose tolerance were studied by both IP- and IG-GTT. Mice treated with the H. alvei protein extract showed an improved glucose tolerance in IP-GTT but not in IG-GTT. Both groups treated with H. alvei bacteria or protein extract showed a reduction of pancreatic tissue weight but without significant changes to basal plasma insulin. No significant effects of H. alvei bacteria or its total protein extract administration were observed on the sweet taste preference, insulin tolerance and expression of regulatory peptides’ mRNA in the hypothalamus. Acute administration of ClpB in non-treated mice increased glucose tolerance during the IP-GTT but not the IG-GTT, and reduced basal plasma glucose levels. We conclude that both the H. alvei protein extract introduced orally and the ClpB protein administered via IP improve glucose tolerance probably by acting at the glucose postabsorptive level. Moreover, H. alvei probiotic does not seem to influence the sweet taste preference. These results justify future testing of both the H. alvei protein extract and ClpB protein in animal models of diabetes.
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spelling pubmed-103413922023-07-14 Protein Extract of a Probiotic Strain of Hafnia alvei and Bacterial ClpB Protein Improve Glucose Tolerance in Mice Zolotarev, Vasiliy A. Murovets, Vladimir O. Sepp, Anastasiya L. Sozontov, Egor A. Lukina, Ekaterina A. Khropycheva, Raisa P. Pestereva, Nina S. Ivleva, Irina S. El Mehdi, Mouna Lahaye, Emilie Chartrel, Nicolas Fetissov, Sergueï O. Int J Mol Sci Article A commercial strain of Hafnia alvei (H. alvei) 4597 bacteria was shown to reduce food intake and promote weight loss, effects possibly induced by the bacterial protein ClpB, an antigen-mimetic of the anorexigenic α-melanocyte-stimulating hormone. A decrease in the basal plasma glucose levels was also observed in overweight fasted humans and mice receiving H. alvei. However, it is not known whether H. alvei influences sweet taste preference and whether its protein extract or ClpB are sufficient to increase glucose tolerance; these are the objectives tested in the present study. C57BL/6J male mice were kept under standard diet and were gavaged daily for 17 days with a suspension of H. alvei (4.5 × 10(7) CFU/animal) or with H. alvei total protein extract (5 μg/animal) or saline as a control. Sweet taste preference was analyzed via a brief-access licking test with sucrose solution. Glucose tolerance tests (GTT) were performed after the intraperitoneal (IP) or intragastric (IG) glucose administration at the 9th and 15th days of gavage, respectively. The expression of regulatory peptides’ mRNA levels was assayed in the hypothalamus. In another experiment performed in non-treated C57BL/6J male mice, effects of acute IP administration of recombinant ClpB protein on glucose tolerance were studied by both IP- and IG-GTT. Mice treated with the H. alvei protein extract showed an improved glucose tolerance in IP-GTT but not in IG-GTT. Both groups treated with H. alvei bacteria or protein extract showed a reduction of pancreatic tissue weight but without significant changes to basal plasma insulin. No significant effects of H. alvei bacteria or its total protein extract administration were observed on the sweet taste preference, insulin tolerance and expression of regulatory peptides’ mRNA in the hypothalamus. Acute administration of ClpB in non-treated mice increased glucose tolerance during the IP-GTT but not the IG-GTT, and reduced basal plasma glucose levels. We conclude that both the H. alvei protein extract introduced orally and the ClpB protein administered via IP improve glucose tolerance probably by acting at the glucose postabsorptive level. Moreover, H. alvei probiotic does not seem to influence the sweet taste preference. These results justify future testing of both the H. alvei protein extract and ClpB protein in animal models of diabetes. MDPI 2023-06-24 /pmc/articles/PMC10341392/ /pubmed/37445766 http://dx.doi.org/10.3390/ijms241310590 Text en © 2023 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Zolotarev, Vasiliy A.
Murovets, Vladimir O.
Sepp, Anastasiya L.
Sozontov, Egor A.
Lukina, Ekaterina A.
Khropycheva, Raisa P.
Pestereva, Nina S.
Ivleva, Irina S.
El Mehdi, Mouna
Lahaye, Emilie
Chartrel, Nicolas
Fetissov, Sergueï O.
Protein Extract of a Probiotic Strain of Hafnia alvei and Bacterial ClpB Protein Improve Glucose Tolerance in Mice
title Protein Extract of a Probiotic Strain of Hafnia alvei and Bacterial ClpB Protein Improve Glucose Tolerance in Mice
title_full Protein Extract of a Probiotic Strain of Hafnia alvei and Bacterial ClpB Protein Improve Glucose Tolerance in Mice
title_fullStr Protein Extract of a Probiotic Strain of Hafnia alvei and Bacterial ClpB Protein Improve Glucose Tolerance in Mice
title_full_unstemmed Protein Extract of a Probiotic Strain of Hafnia alvei and Bacterial ClpB Protein Improve Glucose Tolerance in Mice
title_short Protein Extract of a Probiotic Strain of Hafnia alvei and Bacterial ClpB Protein Improve Glucose Tolerance in Mice
title_sort protein extract of a probiotic strain of hafnia alvei and bacterial clpb protein improve glucose tolerance in mice
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10341392/
https://www.ncbi.nlm.nih.gov/pubmed/37445766
http://dx.doi.org/10.3390/ijms241310590
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