Chitooligosaccharides Improve the Efficacy of Checkpoint Inhibitors in a Mouse Model of Lung Cancer

YKL-40 (also named chitinase 3 like-1 protein [CHI3L1]) is a secreted chitinase-like protein which is upregulated in cancers and suggested to have pro-tumorigenic activity. YKL-40 lacks enzymatic function, but it can bind carbohydrates such as chitin. Chitooligosaccharides (COS) derived from deacety...

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Autores principales: Johansen, Astrid Zedlitz, Carretta, Marco, Thorseth, Marie-Louise, Khan, Shawez, Fjæstad, Klaire Yixin, Brøchner, Christian Beltoft, Linder, Hannes, Ankjærgaard, Christina, Donia, Marco, Chen, Inna, Nielsen, Dorte Lisbet, Behrens, Claus Preibisch, Madsen, Daniel Hargbøl
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9147765/
https://www.ncbi.nlm.nih.gov/pubmed/35631632
http://dx.doi.org/10.3390/pharmaceutics14051046
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author Johansen, Astrid Zedlitz
Carretta, Marco
Thorseth, Marie-Louise
Khan, Shawez
Fjæstad, Klaire Yixin
Brøchner, Christian Beltoft
Linder, Hannes
Ankjærgaard, Christina
Donia, Marco
Chen, Inna
Nielsen, Dorte Lisbet
Behrens, Claus Preibisch
Madsen, Daniel Hargbøl
author_facet Johansen, Astrid Zedlitz
Carretta, Marco
Thorseth, Marie-Louise
Khan, Shawez
Fjæstad, Klaire Yixin
Brøchner, Christian Beltoft
Linder, Hannes
Ankjærgaard, Christina
Donia, Marco
Chen, Inna
Nielsen, Dorte Lisbet
Behrens, Claus Preibisch
Madsen, Daniel Hargbøl
author_sort Johansen, Astrid Zedlitz
collection PubMed
description YKL-40 (also named chitinase 3 like-1 protein [CHI3L1]) is a secreted chitinase-like protein which is upregulated in cancers and suggested to have pro-tumorigenic activity. YKL-40 lacks enzymatic function, but it can bind carbohydrates such as chitin. Chitooligosaccharides (COS) derived from deacetylation and hydrolysis of chitin might be used for the blockade of YKL-40 function. Here, public single-cell RNA sequencing datasets were used to elucidate the cellular source of YKL-40 gene expression in human tumors. Fibroblasts and myeloid cells were the primary sources of YKL-40. Screening of YKL-40 gene expression in syngeneic mouse cancer models showed the highest expression in the Lewis lung carcinoma (LL2) model. LL2 was used to investigate COS monotherapy and combinations with immune checkpoint inhibitors (anti-PD-L1 and anti-CTLA-4) (ICIs) and radiotherapy (8 Gy × 3) (RT). COS tended to reduce plasma YKL-40 levels, but it did not affect tumor growth. LL2 showed minimal responses to ICIs, or to RT alone. Interestingly, ICIs combined with COS led to delayed tumor growth. RT also enhanced the efficacy of ICIs; however, the addition of COS did not further delay the tumor growth. COS may exert their anti-tumorigenic effects through the inhibition of YKL-40, but additional functions of COS should be investigated.
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spelling pubmed-91477652022-05-29 Chitooligosaccharides Improve the Efficacy of Checkpoint Inhibitors in a Mouse Model of Lung Cancer Johansen, Astrid Zedlitz Carretta, Marco Thorseth, Marie-Louise Khan, Shawez Fjæstad, Klaire Yixin Brøchner, Christian Beltoft Linder, Hannes Ankjærgaard, Christina Donia, Marco Chen, Inna Nielsen, Dorte Lisbet Behrens, Claus Preibisch Madsen, Daniel Hargbøl Pharmaceutics Article YKL-40 (also named chitinase 3 like-1 protein [CHI3L1]) is a secreted chitinase-like protein which is upregulated in cancers and suggested to have pro-tumorigenic activity. YKL-40 lacks enzymatic function, but it can bind carbohydrates such as chitin. Chitooligosaccharides (COS) derived from deacetylation and hydrolysis of chitin might be used for the blockade of YKL-40 function. Here, public single-cell RNA sequencing datasets were used to elucidate the cellular source of YKL-40 gene expression in human tumors. Fibroblasts and myeloid cells were the primary sources of YKL-40. Screening of YKL-40 gene expression in syngeneic mouse cancer models showed the highest expression in the Lewis lung carcinoma (LL2) model. LL2 was used to investigate COS monotherapy and combinations with immune checkpoint inhibitors (anti-PD-L1 and anti-CTLA-4) (ICIs) and radiotherapy (8 Gy × 3) (RT). COS tended to reduce plasma YKL-40 levels, but it did not affect tumor growth. LL2 showed minimal responses to ICIs, or to RT alone. Interestingly, ICIs combined with COS led to delayed tumor growth. RT also enhanced the efficacy of ICIs; however, the addition of COS did not further delay the tumor growth. COS may exert their anti-tumorigenic effects through the inhibition of YKL-40, but additional functions of COS should be investigated. MDPI 2022-05-12 /pmc/articles/PMC9147765/ /pubmed/35631632 http://dx.doi.org/10.3390/pharmaceutics14051046 Text en © 2022 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
Johansen, Astrid Zedlitz
Carretta, Marco
Thorseth, Marie-Louise
Khan, Shawez
Fjæstad, Klaire Yixin
Brøchner, Christian Beltoft
Linder, Hannes
Ankjærgaard, Christina
Donia, Marco
Chen, Inna
Nielsen, Dorte Lisbet
Behrens, Claus Preibisch
Madsen, Daniel Hargbøl
Chitooligosaccharides Improve the Efficacy of Checkpoint Inhibitors in a Mouse Model of Lung Cancer
title Chitooligosaccharides Improve the Efficacy of Checkpoint Inhibitors in a Mouse Model of Lung Cancer
title_full Chitooligosaccharides Improve the Efficacy of Checkpoint Inhibitors in a Mouse Model of Lung Cancer
title_fullStr Chitooligosaccharides Improve the Efficacy of Checkpoint Inhibitors in a Mouse Model of Lung Cancer
title_full_unstemmed Chitooligosaccharides Improve the Efficacy of Checkpoint Inhibitors in a Mouse Model of Lung Cancer
title_short Chitooligosaccharides Improve the Efficacy of Checkpoint Inhibitors in a Mouse Model of Lung Cancer
title_sort chitooligosaccharides improve the efficacy of checkpoint inhibitors in a mouse model of lung cancer
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9147765/
https://www.ncbi.nlm.nih.gov/pubmed/35631632
http://dx.doi.org/10.3390/pharmaceutics14051046
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