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p300 Serine 89: A Critical Signaling Integrator and Its Effects on Intestinal Homeostasis and Repair

SIMPLE SUMMARY: Given their high degree of identity and even greater similarity at the amino acid level, Kat3 coactivators, CBP (Kat3A) and p300 (Kat3B), have long been considered redundant. We describe the generation of novel p300 S89A knock-in mice carrying a single site directed amino acid mutati...

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Autores principales: Lai, Keane K. Y., Hu, Xiaohui, Chosa, Keisuke, Nguyen, Cu, Lin, David P., Lai, Keith K., Kato, Nobuo, Higuchi, Yusuke, Highlander, Sarah K., Melendez, Elizabeth, Eriguchi, Yoshihiro, Fueger, Patrick T., Ouellette, Andre J., Chimge, Nyam-Osor, Ono, Masaya, Kahn, Michael
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7999107/
https://www.ncbi.nlm.nih.gov/pubmed/33799418
http://dx.doi.org/10.3390/cancers13061288
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author Lai, Keane K. Y.
Hu, Xiaohui
Chosa, Keisuke
Nguyen, Cu
Lin, David P.
Lai, Keith K.
Kato, Nobuo
Higuchi, Yusuke
Highlander, Sarah K.
Melendez, Elizabeth
Eriguchi, Yoshihiro
Fueger, Patrick T.
Ouellette, Andre J.
Chimge, Nyam-Osor
Ono, Masaya
Kahn, Michael
author_facet Lai, Keane K. Y.
Hu, Xiaohui
Chosa, Keisuke
Nguyen, Cu
Lin, David P.
Lai, Keith K.
Kato, Nobuo
Higuchi, Yusuke
Highlander, Sarah K.
Melendez, Elizabeth
Eriguchi, Yoshihiro
Fueger, Patrick T.
Ouellette, Andre J.
Chimge, Nyam-Osor
Ono, Masaya
Kahn, Michael
author_sort Lai, Keane K. Y.
collection PubMed
description SIMPLE SUMMARY: Given their high degree of identity and even greater similarity at the amino acid level, Kat3 coactivators, CBP (Kat3A) and p300 (Kat3B), have long been considered redundant. We describe the generation of novel p300 S89A knock-in mice carrying a single site directed amino acid mutation in p300, changing the highly evolutionarily conserved serine 89 to alanine, thus enhancing Wnt/CBP/catenin signaling (at the expense of Wnt/p300/catenin signaling). p300 S89A knock-in mice exhibit multiple organ system, immunologic and metabolic differences, compared with their wild type counterparts. In particular, these p300 S89A knock-in mice are highly sensitive to intestinal injury resulting in colitis which is known to significantly predispose to colorectal cancer. Our results highlight the critical role of this region in p300 as a signaling nexus and provide further evidence that p300 and CBP are non-redundant, playing definite and distinctive roles in development and disease. ABSTRACT: Differential usage of Kat3 coactivators, CBP and p300, by β-catenin is a fundamental regulatory mechanism in stem cell maintenance and initiation of differentiation and repair. Based upon our earlier pharmacologic studies, p300 serine 89 (S89) is critical for controlling differential coactivator usage by β-catenin via post-translational phosphorylation in stem/progenitor populations, and appears to be a target for a number of kinase cascades. To further investigate mechanisms of signal integration effected by this domain, we generated p300 S89A knock-in mice. We show that S89A mice are extremely sensitive to intestinal insult resulting in colitis, which is known to significantly increase the risk of developing colorectal cancer. We demonstrate cell intrinsic differences, and microbiome compositional differences and differential immune responses, in intestine of S89A versus wild type mice. Genomic and proteomic analyses reveal pathway differences, including lipid metabolism, oxidative stress response, mitochondrial function and oxidative phosphorylation. The diverse effects on fundamental processes including epithelial differentiation, metabolism, immune response and microbiome colonization, all brought about by a single amino acid modification S89A, highlights the critical role of this region in p300 as a signaling nexus and the rationale for conservation of this residue and surrounding region for hundreds of million years of vertebrate evolution.
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spelling pubmed-79991072021-03-28 p300 Serine 89: A Critical Signaling Integrator and Its Effects on Intestinal Homeostasis and Repair Lai, Keane K. Y. Hu, Xiaohui Chosa, Keisuke Nguyen, Cu Lin, David P. Lai, Keith K. Kato, Nobuo Higuchi, Yusuke Highlander, Sarah K. Melendez, Elizabeth Eriguchi, Yoshihiro Fueger, Patrick T. Ouellette, Andre J. Chimge, Nyam-Osor Ono, Masaya Kahn, Michael Cancers (Basel) Article SIMPLE SUMMARY: Given their high degree of identity and even greater similarity at the amino acid level, Kat3 coactivators, CBP (Kat3A) and p300 (Kat3B), have long been considered redundant. We describe the generation of novel p300 S89A knock-in mice carrying a single site directed amino acid mutation in p300, changing the highly evolutionarily conserved serine 89 to alanine, thus enhancing Wnt/CBP/catenin signaling (at the expense of Wnt/p300/catenin signaling). p300 S89A knock-in mice exhibit multiple organ system, immunologic and metabolic differences, compared with their wild type counterparts. In particular, these p300 S89A knock-in mice are highly sensitive to intestinal injury resulting in colitis which is known to significantly predispose to colorectal cancer. Our results highlight the critical role of this region in p300 as a signaling nexus and provide further evidence that p300 and CBP are non-redundant, playing definite and distinctive roles in development and disease. ABSTRACT: Differential usage of Kat3 coactivators, CBP and p300, by β-catenin is a fundamental regulatory mechanism in stem cell maintenance and initiation of differentiation and repair. Based upon our earlier pharmacologic studies, p300 serine 89 (S89) is critical for controlling differential coactivator usage by β-catenin via post-translational phosphorylation in stem/progenitor populations, and appears to be a target for a number of kinase cascades. To further investigate mechanisms of signal integration effected by this domain, we generated p300 S89A knock-in mice. We show that S89A mice are extremely sensitive to intestinal insult resulting in colitis, which is known to significantly increase the risk of developing colorectal cancer. We demonstrate cell intrinsic differences, and microbiome compositional differences and differential immune responses, in intestine of S89A versus wild type mice. Genomic and proteomic analyses reveal pathway differences, including lipid metabolism, oxidative stress response, mitochondrial function and oxidative phosphorylation. The diverse effects on fundamental processes including epithelial differentiation, metabolism, immune response and microbiome colonization, all brought about by a single amino acid modification S89A, highlights the critical role of this region in p300 as a signaling nexus and the rationale for conservation of this residue and surrounding region for hundreds of million years of vertebrate evolution. MDPI 2021-03-14 /pmc/articles/PMC7999107/ /pubmed/33799418 http://dx.doi.org/10.3390/cancers13061288 Text en © 2021 by the authors. 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 (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Lai, Keane K. Y.
Hu, Xiaohui
Chosa, Keisuke
Nguyen, Cu
Lin, David P.
Lai, Keith K.
Kato, Nobuo
Higuchi, Yusuke
Highlander, Sarah K.
Melendez, Elizabeth
Eriguchi, Yoshihiro
Fueger, Patrick T.
Ouellette, Andre J.
Chimge, Nyam-Osor
Ono, Masaya
Kahn, Michael
p300 Serine 89: A Critical Signaling Integrator and Its Effects on Intestinal Homeostasis and Repair
title p300 Serine 89: A Critical Signaling Integrator and Its Effects on Intestinal Homeostasis and Repair
title_full p300 Serine 89: A Critical Signaling Integrator and Its Effects on Intestinal Homeostasis and Repair
title_fullStr p300 Serine 89: A Critical Signaling Integrator and Its Effects on Intestinal Homeostasis and Repair
title_full_unstemmed p300 Serine 89: A Critical Signaling Integrator and Its Effects on Intestinal Homeostasis and Repair
title_short p300 Serine 89: A Critical Signaling Integrator and Its Effects on Intestinal Homeostasis and Repair
title_sort p300 serine 89: a critical signaling integrator and its effects on intestinal homeostasis and repair
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7999107/
https://www.ncbi.nlm.nih.gov/pubmed/33799418
http://dx.doi.org/10.3390/cancers13061288
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