Tanshinone IIA and Neural Stem Cell Combination Therapy Decreases Gut Inflammation and Maintains Gut Integrity in a Translational Pig Ischemic Stroke Model

OBJECTIVES: Impaired gut homeostasis has been found in stroke, leading to leaky gut syndrome, increased levels of gut, brain, and systemic inflammation that further exacerbating brain damage. Tanshinone IIA (Tan IIA) and induced pluripotent stem cell derived neural stem cells (iNSCs) have been shown...

Descripción completa

Detalles Bibliográficos
Autores principales: Jeon, Julie, Kaiser, Erin, Waters, Elizabeth, Yang, Xueyuan, Lourenco, Jeferson, Scheulin, Kelly, Sneed, Sydney, Shin, Soo, Kinder, Holly, Kumar, Anil, Platt, Simon, Ahn, Jeongyoun, Rothrock Jr., Michael, Callaway, Todd, Xie, Jin, West, Franklin, Park, Hea Jin
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2022
Materias:
Neuroscience/Nutrition and the Brain
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9194273/
http://dx.doi.org/10.1093/cdn/nzac064.014
_version_ 1784726684305457152
author Jeon, Julie
Kaiser, Erin
Waters, Elizabeth
Yang, Xueyuan
Lourenco, Jeferson
Scheulin, Kelly
Sneed, Sydney
Shin, Soo
Kinder, Holly
Kumar, Anil
Platt, Simon
Ahn, Jeongyoun
Rothrock Jr., Michael
Callaway, Todd
Xie, Jin
West, Franklin
Park, Hea Jin
author_facet Jeon, Julie
Kaiser, Erin
Waters, Elizabeth
Yang, Xueyuan
Lourenco, Jeferson
Scheulin, Kelly
Sneed, Sydney
Shin, Soo
Kinder, Holly
Kumar, Anil
Platt, Simon
Ahn, Jeongyoun
Rothrock Jr., Michael
Callaway, Todd
Xie, Jin
West, Franklin
Park, Hea Jin
author_sort Jeon, Julie
collection PubMed
description OBJECTIVES: Impaired gut homeostasis has been found in stroke, leading to leaky gut syndrome, increased levels of gut, brain, and systemic inflammation that further exacerbating brain damage. Tanshinone IIA (Tan IIA) and induced pluripotent stem cell derived neural stem cells (iNSCs) have been shown to decrease inflammation in the brain post-stroke resulting in reduced lesion volume and improved recovery response in rodent models. However, no group has evaluated the effect of Tan IIA and iNSCs brain treatments on intestinal changes. We evaluate the effects of Tan IIA and iNSCs delivered to the brain post-stroke on gut homeostasis in an ischemic stroke pig model. METHODS: Yucatan pigs (n = 12) underwent middle cerebral artery occlusion surgery and received either PBS (CON) or Tan IIA loaded PLGA nanoparticle (Tan IIA-NPs) and iNSCs treatment (TRT). PBS or Tan IIA-NPs were administered intracisternally at 1 hour post-stroke and PBS or iNSCs were transplanted into the perilesional region at 5 days post-stroke. Changes in fecal total SCFAs level were analyzed up to 12 weeks (wk) post-treatment (PT) and jejunum scrapings were collected at 12 wk PT for analysis. RESULTS: TRT had higher levels of total SCFAs than CON throughout the study period. Protein levels of jejunal TNF-α, TNFR1, and phosphorylation of Ikbα at 12 wk PT were lower in TRT compared to CON, suggesting that the treatment in brain decreased gut inflammation. The expression of jejunal Occludin, Claudin1, and ZO-1 was higher in TRT compared to CON. Moreover, protein levels of TNF-α and phosphorylation of Ikbα were negatively correlated with fecal total SCFAs levels at early stages of treatment (1–4 wk PT). Interestingly, total SCFA level at early treatment stages (up to 4 wk PT) was inversely related to hemorrhage volume measured by magnetic resonance imaging 1 day post-stroke, indicating a potential link between stroke severity and gut homeostasis. CONCLUSIONS: The findings of the study indicate that local post-stroke brain treatment with Tan IIA and iNSCs decreases inflammation and membrane permeability through dynamic interplay with SCFAs in the gut. This study suggests further research on inflammation and SCFAs as key regulatory components and potential therapeutic targets that can modulate the gut brain axis to enhance stroke recovery in patients. FUNDING SOURCES: This work was supported by the National Institutes of Health.
format Online
Article
Text
id pubmed-9194273
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher Oxford University Press
record_format MEDLINE/PubMed
spelling pubmed-91942732022-06-14 Tanshinone IIA and Neural Stem Cell Combination Therapy Decreases Gut Inflammation and Maintains Gut Integrity in a Translational Pig Ischemic Stroke Model Jeon, Julie Kaiser, Erin Waters, Elizabeth Yang, Xueyuan Lourenco, Jeferson Scheulin, Kelly Sneed, Sydney Shin, Soo Kinder, Holly Kumar, Anil Platt, Simon Ahn, Jeongyoun Rothrock Jr., Michael Callaway, Todd Xie, Jin West, Franklin Park, Hea Jin Curr Dev Nutr Neuroscience/Nutrition and the Brain OBJECTIVES: Impaired gut homeostasis has been found in stroke, leading to leaky gut syndrome, increased levels of gut, brain, and systemic inflammation that further exacerbating brain damage. Tanshinone IIA (Tan IIA) and induced pluripotent stem cell derived neural stem cells (iNSCs) have been shown to decrease inflammation in the brain post-stroke resulting in reduced lesion volume and improved recovery response in rodent models. However, no group has evaluated the effect of Tan IIA and iNSCs brain treatments on intestinal changes. We evaluate the effects of Tan IIA and iNSCs delivered to the brain post-stroke on gut homeostasis in an ischemic stroke pig model. METHODS: Yucatan pigs (n = 12) underwent middle cerebral artery occlusion surgery and received either PBS (CON) or Tan IIA loaded PLGA nanoparticle (Tan IIA-NPs) and iNSCs treatment (TRT). PBS or Tan IIA-NPs were administered intracisternally at 1 hour post-stroke and PBS or iNSCs were transplanted into the perilesional region at 5 days post-stroke. Changes in fecal total SCFAs level were analyzed up to 12 weeks (wk) post-treatment (PT) and jejunum scrapings were collected at 12 wk PT for analysis. RESULTS: TRT had higher levels of total SCFAs than CON throughout the study period. Protein levels of jejunal TNF-α, TNFR1, and phosphorylation of Ikbα at 12 wk PT were lower in TRT compared to CON, suggesting that the treatment in brain decreased gut inflammation. The expression of jejunal Occludin, Claudin1, and ZO-1 was higher in TRT compared to CON. Moreover, protein levels of TNF-α and phosphorylation of Ikbα were negatively correlated with fecal total SCFAs levels at early stages of treatment (1–4 wk PT). Interestingly, total SCFA level at early treatment stages (up to 4 wk PT) was inversely related to hemorrhage volume measured by magnetic resonance imaging 1 day post-stroke, indicating a potential link between stroke severity and gut homeostasis. CONCLUSIONS: The findings of the study indicate that local post-stroke brain treatment with Tan IIA and iNSCs decreases inflammation and membrane permeability through dynamic interplay with SCFAs in the gut. This study suggests further research on inflammation and SCFAs as key regulatory components and potential therapeutic targets that can modulate the gut brain axis to enhance stroke recovery in patients. FUNDING SOURCES: This work was supported by the National Institutes of Health. Oxford University Press 2022-06-14 /pmc/articles/PMC9194273/ http://dx.doi.org/10.1093/cdn/nzac064.014 Text en © The Author 2022. Published by Oxford University Press on behalf of The International Society for Human and Animal Mycology. https://creativecommons.org/licenses/by-nc/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (https://creativecommons.org/licenses/by-nc/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Neuroscience/Nutrition and the Brain
Jeon, Julie
Kaiser, Erin
Waters, Elizabeth
Yang, Xueyuan
Lourenco, Jeferson
Scheulin, Kelly
Sneed, Sydney
Shin, Soo
Kinder, Holly
Kumar, Anil
Platt, Simon
Ahn, Jeongyoun
Rothrock Jr., Michael
Callaway, Todd
Xie, Jin
West, Franklin
Park, Hea Jin
Tanshinone IIA and Neural Stem Cell Combination Therapy Decreases Gut Inflammation and Maintains Gut Integrity in a Translational Pig Ischemic Stroke Model
title Tanshinone IIA and Neural Stem Cell Combination Therapy Decreases Gut Inflammation and Maintains Gut Integrity in a Translational Pig Ischemic Stroke Model
title_full Tanshinone IIA and Neural Stem Cell Combination Therapy Decreases Gut Inflammation and Maintains Gut Integrity in a Translational Pig Ischemic Stroke Model
title_fullStr Tanshinone IIA and Neural Stem Cell Combination Therapy Decreases Gut Inflammation and Maintains Gut Integrity in a Translational Pig Ischemic Stroke Model
title_full_unstemmed Tanshinone IIA and Neural Stem Cell Combination Therapy Decreases Gut Inflammation and Maintains Gut Integrity in a Translational Pig Ischemic Stroke Model
title_short Tanshinone IIA and Neural Stem Cell Combination Therapy Decreases Gut Inflammation and Maintains Gut Integrity in a Translational Pig Ischemic Stroke Model
title_sort tanshinone iia and neural stem cell combination therapy decreases gut inflammation and maintains gut integrity in a translational pig ischemic stroke model
topic Neuroscience/Nutrition and the Brain
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9194273/
http://dx.doi.org/10.1093/cdn/nzac064.014
work_keys_str_mv AT jeonjulie tanshinoneiiaandneuralstemcellcombinationtherapydecreasesgutinflammationandmaintainsgutintegrityinatranslationalpigischemicstrokemodel
AT kaisererin tanshinoneiiaandneuralstemcellcombinationtherapydecreasesgutinflammationandmaintainsgutintegrityinatranslationalpigischemicstrokemodel
AT waterselizabeth tanshinoneiiaandneuralstemcellcombinationtherapydecreasesgutinflammationandmaintainsgutintegrityinatranslationalpigischemicstrokemodel
AT yangxueyuan tanshinoneiiaandneuralstemcellcombinationtherapydecreasesgutinflammationandmaintainsgutintegrityinatranslationalpigischemicstrokemodel
AT lourencojeferson tanshinoneiiaandneuralstemcellcombinationtherapydecreasesgutinflammationandmaintainsgutintegrityinatranslationalpigischemicstrokemodel
AT scheulinkelly tanshinoneiiaandneuralstemcellcombinationtherapydecreasesgutinflammationandmaintainsgutintegrityinatranslationalpigischemicstrokemodel
AT sneedsydney tanshinoneiiaandneuralstemcellcombinationtherapydecreasesgutinflammationandmaintainsgutintegrityinatranslationalpigischemicstrokemodel
AT shinsoo tanshinoneiiaandneuralstemcellcombinationtherapydecreasesgutinflammationandmaintainsgutintegrityinatranslationalpigischemicstrokemodel
AT kinderholly tanshinoneiiaandneuralstemcellcombinationtherapydecreasesgutinflammationandmaintainsgutintegrityinatranslationalpigischemicstrokemodel
AT kumaranil tanshinoneiiaandneuralstemcellcombinationtherapydecreasesgutinflammationandmaintainsgutintegrityinatranslationalpigischemicstrokemodel
AT plattsimon tanshinoneiiaandneuralstemcellcombinationtherapydecreasesgutinflammationandmaintainsgutintegrityinatranslationalpigischemicstrokemodel
AT ahnjeongyoun tanshinoneiiaandneuralstemcellcombinationtherapydecreasesgutinflammationandmaintainsgutintegrityinatranslationalpigischemicstrokemodel
AT rothrockjrmichael tanshinoneiiaandneuralstemcellcombinationtherapydecreasesgutinflammationandmaintainsgutintegrityinatranslationalpigischemicstrokemodel
AT callawaytodd tanshinoneiiaandneuralstemcellcombinationtherapydecreasesgutinflammationandmaintainsgutintegrityinatranslationalpigischemicstrokemodel
AT xiejin tanshinoneiiaandneuralstemcellcombinationtherapydecreasesgutinflammationandmaintainsgutintegrityinatranslationalpigischemicstrokemodel
AT westfranklin tanshinoneiiaandneuralstemcellcombinationtherapydecreasesgutinflammationandmaintainsgutintegrityinatranslationalpigischemicstrokemodel
AT parkheajin tanshinoneiiaandneuralstemcellcombinationtherapydecreasesgutinflammationandmaintainsgutintegrityinatranslationalpigischemicstrokemodel

Ejemplares similares