Adult mice are unresponsive to AAV8-Gremlin1 gene therapy targeting the liver

OBJECTIVE: Gremlin 1 (GREM1) is a secreted BMP2/4 inhibitor which regulates commitment and differentiation of human adipose precursor cells and prevents the browning effect of BMP4. GREM1 is an insulin antagonist and serum levels are high in type 2 diabetes (T2D). We here examined in vivo effects of...

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Autores principales: Khatib Shahidi, Roxana, M. Hoffmann, Jenny, Hedjazifar, Shahram, Bonnet, Laurianne, K. Baboota, Ritesh, Heasman, Stephanie, Church, Christopher, Elias, Ivet, Bosch, Fatima, Boucher, Jeremie, Hammarstedt, Ann, Smith, Ulf
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2021
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7895349/
https://www.ncbi.nlm.nih.gov/pubmed/33606810
http://dx.doi.org/10.1371/journal.pone.0247300
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author Khatib Shahidi, Roxana
M. Hoffmann, Jenny
Hedjazifar, Shahram
Bonnet, Laurianne
K. Baboota, Ritesh
Heasman, Stephanie
Church, Christopher
Elias, Ivet
Bosch, Fatima
Boucher, Jeremie
Hammarstedt, Ann
Smith, Ulf
author_facet Khatib Shahidi, Roxana
M. Hoffmann, Jenny
Hedjazifar, Shahram
Bonnet, Laurianne
K. Baboota, Ritesh
Heasman, Stephanie
Church, Christopher
Elias, Ivet
Bosch, Fatima
Boucher, Jeremie
Hammarstedt, Ann
Smith, Ulf
author_sort Khatib Shahidi, Roxana
collection PubMed
description OBJECTIVE: Gremlin 1 (GREM1) is a secreted BMP2/4 inhibitor which regulates commitment and differentiation of human adipose precursor cells and prevents the browning effect of BMP4. GREM1 is an insulin antagonist and serum levels are high in type 2 diabetes (T2D). We here examined in vivo effects of AAV8 (Adeno-Associated Viral vectors of serotype eight) GREM 1 targeting the liver in mature mice to increase its systemic secretion and also, in a separate study, injected recombinant GREM 1 intraperitoneally. The objective was to characterize systemic effects of GREM 1 on insulin sensitivity, glucose tolerance, body weight, adipose cell browning and other local tissue effects. METHODS: Adult mice were injected with AAV8 vectors expressing GREM1 in the liver or receiving regular intra-peritoneal injections of recombinant GREM1 protein. The mice were fed with a low fat or high fat diet (HFD) and followed over time. RESULTS: Liver-targeted AAV8-GREM1 did not alter body weight, whole-body glucose and insulin tolerance, or adipose tissue gene expression. Although GREM1 protein accumulated in liver cells, GREM1 serum levels were not increased suggesting that it may not have been normally processed for secretion. Hepatic lipid accumulation, inflammation and fibrosis were also not changed. Repeated intraperitoneal rec-GREM1 injections for 5 weeks were also without effects on body weight and insulin sensitivity. UCP1 was slightly but significantly reduced in both white and brown adipose tissue but this was not of sufficient magnitude to alter body weight. We validated that recombinant GREM1 inhibited BMP4-induced pSMAD1/5/9 in murine cells in vitro, but saw no direct inhibitory effect on insulin signalling and pAkt (ser 473 and thr 308) activation. CONCLUSION: GREM1 accumulates intracellularly when overexpressed in the liver cells of mature mice and is apparently not normally processed/secreted. However, also repeated intraperitoneal injections were without effects on body weight and insulin sensitivity and adipose tissue UCP1 levels were only marginally reduced. These results suggest that mature mice do not readily respond to GREMLIN 1 but treatment of murine cells with GREMLIN 1 protein in vitro validated its inhibitory effect on BMP4 signalling while insulin signalling was not altered.
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spelling pubmed-78953492021-03-01 Adult mice are unresponsive to AAV8-Gremlin1 gene therapy targeting the liver Khatib Shahidi, Roxana M. Hoffmann, Jenny Hedjazifar, Shahram Bonnet, Laurianne K. Baboota, Ritesh Heasman, Stephanie Church, Christopher Elias, Ivet Bosch, Fatima Boucher, Jeremie Hammarstedt, Ann Smith, Ulf PLoS One Research Article OBJECTIVE: Gremlin 1 (GREM1) is a secreted BMP2/4 inhibitor which regulates commitment and differentiation of human adipose precursor cells and prevents the browning effect of BMP4. GREM1 is an insulin antagonist and serum levels are high in type 2 diabetes (T2D). We here examined in vivo effects of AAV8 (Adeno-Associated Viral vectors of serotype eight) GREM 1 targeting the liver in mature mice to increase its systemic secretion and also, in a separate study, injected recombinant GREM 1 intraperitoneally. The objective was to characterize systemic effects of GREM 1 on insulin sensitivity, glucose tolerance, body weight, adipose cell browning and other local tissue effects. METHODS: Adult mice were injected with AAV8 vectors expressing GREM1 in the liver or receiving regular intra-peritoneal injections of recombinant GREM1 protein. The mice were fed with a low fat or high fat diet (HFD) and followed over time. RESULTS: Liver-targeted AAV8-GREM1 did not alter body weight, whole-body glucose and insulin tolerance, or adipose tissue gene expression. Although GREM1 protein accumulated in liver cells, GREM1 serum levels were not increased suggesting that it may not have been normally processed for secretion. Hepatic lipid accumulation, inflammation and fibrosis were also not changed. Repeated intraperitoneal rec-GREM1 injections for 5 weeks were also without effects on body weight and insulin sensitivity. UCP1 was slightly but significantly reduced in both white and brown adipose tissue but this was not of sufficient magnitude to alter body weight. We validated that recombinant GREM1 inhibited BMP4-induced pSMAD1/5/9 in murine cells in vitro, but saw no direct inhibitory effect on insulin signalling and pAkt (ser 473 and thr 308) activation. CONCLUSION: GREM1 accumulates intracellularly when overexpressed in the liver cells of mature mice and is apparently not normally processed/secreted. However, also repeated intraperitoneal injections were without effects on body weight and insulin sensitivity and adipose tissue UCP1 levels were only marginally reduced. These results suggest that mature mice do not readily respond to GREMLIN 1 but treatment of murine cells with GREMLIN 1 protein in vitro validated its inhibitory effect on BMP4 signalling while insulin signalling was not altered. Public Library of Science 2021-02-19 /pmc/articles/PMC7895349/ /pubmed/33606810 http://dx.doi.org/10.1371/journal.pone.0247300 Text en © 2021 Khatib Shahidi et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Khatib Shahidi, Roxana
M. Hoffmann, Jenny
Hedjazifar, Shahram
Bonnet, Laurianne
K. Baboota, Ritesh
Heasman, Stephanie
Church, Christopher
Elias, Ivet
Bosch, Fatima
Boucher, Jeremie
Hammarstedt, Ann
Smith, Ulf
Adult mice are unresponsive to AAV8-Gremlin1 gene therapy targeting the liver
title Adult mice are unresponsive to AAV8-Gremlin1 gene therapy targeting the liver
title_full Adult mice are unresponsive to AAV8-Gremlin1 gene therapy targeting the liver
title_fullStr Adult mice are unresponsive to AAV8-Gremlin1 gene therapy targeting the liver
title_full_unstemmed Adult mice are unresponsive to AAV8-Gremlin1 gene therapy targeting the liver
title_short Adult mice are unresponsive to AAV8-Gremlin1 gene therapy targeting the liver
title_sort adult mice are unresponsive to aav8-gremlin1 gene therapy targeting the liver
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7895349/
https://www.ncbi.nlm.nih.gov/pubmed/33606810
http://dx.doi.org/10.1371/journal.pone.0247300
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