Impaired Iron Homeostasis and Haematopoiesis Impacts Inflammation in the Ageing Process in Down Syndrome Dementia

Down syndrome (DS) subjects are more likely to develop the clinical features of Alzheimer’s disease (AD) very early in the disease process due to the additional impact of neuroinflammation and because of activation of innate immunity. Many factors involved in the neuropathology of AD in DS, includin...

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Autores principales: Raha-Chowdhury, Ruma, Raha, Animesh Alexander, Henderson, James, Ghaffari, Seyedeh Deniz, Grigorova, Monika, Beresford-Webb, Jessica, Allinson, Kieren, Chakraborty, Subhojit, Holland, Anthony, Zaman, Shahid H.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8268765/
https://www.ncbi.nlm.nih.gov/pubmed/34209847
http://dx.doi.org/10.3390/jcm10132909
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author Raha-Chowdhury, Ruma
Raha, Animesh Alexander
Henderson, James
Ghaffari, Seyedeh Deniz
Grigorova, Monika
Beresford-Webb, Jessica
Allinson, Kieren
Chakraborty, Subhojit
Holland, Anthony
Zaman, Shahid H.
author_facet Raha-Chowdhury, Ruma
Raha, Animesh Alexander
Henderson, James
Ghaffari, Seyedeh Deniz
Grigorova, Monika
Beresford-Webb, Jessica
Allinson, Kieren
Chakraborty, Subhojit
Holland, Anthony
Zaman, Shahid H.
author_sort Raha-Chowdhury, Ruma
collection PubMed
description Down syndrome (DS) subjects are more likely to develop the clinical features of Alzheimer’s disease (AD) very early in the disease process due to the additional impact of neuroinflammation and because of activation of innate immunity. Many factors involved in the neuropathology of AD in DS, including epigenetic factors, innate immunity and impaired haematopoiesis, contribute significantly towards the pathophysiology and the enhanced ageing processes seen in DS and as a consequence of the triplication of genes RUNX1, S100β and OLIG2, together with the influence of proteins that collectively protect from cellular defects and inflammation, which include hepcidin, ferritin, IL-6 and TREM2. This study is aimed at determining whether genetic variants and inflammatory proteins are involved in haematopoiesis and cellular processes in DS compared with age-matched control participants, particularly with respect to neuroinflammation and accelerated ageing. Serum protein levels from DS, AD and control participants were measured by enzyme-linked immunosorbent assay (ELISA). Blood smears and post-mortem brain samples from AD and DS subjects were analysed by immunohistochemistry. RUNX1 mRNA expression was analysed by RT-PCR and in situ hybridisation in mouse tissues. Our results suggest that hepcidin, S100β and TREM2 play a critical role in survival and proliferation of glial cells through a common shared pathway. Blood smear analysis showed the presence of RUNX1 in megakaryocytes and platelets, implying participation in myeloid cell development. In contrast, hepcidin was expressed in erythrocytes and in platelets, suggesting a means of possible entry into the brain parenchyma via the choroid plexus (CP). The gene product of RUNX1 and hepcidin both play a critical role in haematopoiesis in DS. We propose that soluble TREM2, S100β and hepcidin can migrate from the periphery via the CP, modulate the blood–brain immune axis in DS and could form an important and hitherto neglected avenue for possible therapeutic interventions to reduce plaque formation.
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spelling pubmed-82687652021-07-10 Impaired Iron Homeostasis and Haematopoiesis Impacts Inflammation in the Ageing Process in Down Syndrome Dementia Raha-Chowdhury, Ruma Raha, Animesh Alexander Henderson, James Ghaffari, Seyedeh Deniz Grigorova, Monika Beresford-Webb, Jessica Allinson, Kieren Chakraborty, Subhojit Holland, Anthony Zaman, Shahid H. J Clin Med Article Down syndrome (DS) subjects are more likely to develop the clinical features of Alzheimer’s disease (AD) very early in the disease process due to the additional impact of neuroinflammation and because of activation of innate immunity. Many factors involved in the neuropathology of AD in DS, including epigenetic factors, innate immunity and impaired haematopoiesis, contribute significantly towards the pathophysiology and the enhanced ageing processes seen in DS and as a consequence of the triplication of genes RUNX1, S100β and OLIG2, together with the influence of proteins that collectively protect from cellular defects and inflammation, which include hepcidin, ferritin, IL-6 and TREM2. This study is aimed at determining whether genetic variants and inflammatory proteins are involved in haematopoiesis and cellular processes in DS compared with age-matched control participants, particularly with respect to neuroinflammation and accelerated ageing. Serum protein levels from DS, AD and control participants were measured by enzyme-linked immunosorbent assay (ELISA). Blood smears and post-mortem brain samples from AD and DS subjects were analysed by immunohistochemistry. RUNX1 mRNA expression was analysed by RT-PCR and in situ hybridisation in mouse tissues. Our results suggest that hepcidin, S100β and TREM2 play a critical role in survival and proliferation of glial cells through a common shared pathway. Blood smear analysis showed the presence of RUNX1 in megakaryocytes and platelets, implying participation in myeloid cell development. In contrast, hepcidin was expressed in erythrocytes and in platelets, suggesting a means of possible entry into the brain parenchyma via the choroid plexus (CP). The gene product of RUNX1 and hepcidin both play a critical role in haematopoiesis in DS. We propose that soluble TREM2, S100β and hepcidin can migrate from the periphery via the CP, modulate the blood–brain immune axis in DS and could form an important and hitherto neglected avenue for possible therapeutic interventions to reduce plaque formation. MDPI 2021-06-29 /pmc/articles/PMC8268765/ /pubmed/34209847 http://dx.doi.org/10.3390/jcm10132909 Text en © 2021 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
Raha-Chowdhury, Ruma
Raha, Animesh Alexander
Henderson, James
Ghaffari, Seyedeh Deniz
Grigorova, Monika
Beresford-Webb, Jessica
Allinson, Kieren
Chakraborty, Subhojit
Holland, Anthony
Zaman, Shahid H.
Impaired Iron Homeostasis and Haematopoiesis Impacts Inflammation in the Ageing Process in Down Syndrome Dementia
title Impaired Iron Homeostasis and Haematopoiesis Impacts Inflammation in the Ageing Process in Down Syndrome Dementia
title_full Impaired Iron Homeostasis and Haematopoiesis Impacts Inflammation in the Ageing Process in Down Syndrome Dementia
title_fullStr Impaired Iron Homeostasis and Haematopoiesis Impacts Inflammation in the Ageing Process in Down Syndrome Dementia
title_full_unstemmed Impaired Iron Homeostasis and Haematopoiesis Impacts Inflammation in the Ageing Process in Down Syndrome Dementia
title_short Impaired Iron Homeostasis and Haematopoiesis Impacts Inflammation in the Ageing Process in Down Syndrome Dementia
title_sort impaired iron homeostasis and haematopoiesis impacts inflammation in the ageing process in down syndrome dementia
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8268765/
https://www.ncbi.nlm.nih.gov/pubmed/34209847
http://dx.doi.org/10.3390/jcm10132909
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