AcSDKP is down-regulated in anaemia induced by Trypanosoma brucei infection in mice

BACKGROUND: Anaemia commonly results from destruction of erythrocytes in the peripheral blood and failure of the bone marrow haematopoietic cells to replenish the erythrocytes. The mechanisms involved in trypanosoma-induced anaemia, including the role of the bone marrow haematopoietic cells are inco...

Descripción completa

Detalles Bibliográficos
Autores principales: Musaya, Janelisa, Matovu, Enock, Senga, Edward, Nyirenda, Moffat, Chisi, John
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Medical Association Of Malawi 2017
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5811999/
https://www.ncbi.nlm.nih.gov/pubmed/29872517
http://dx.doi.org/10.4314/mmj.v29i3.6
_version_ 1783299958366011392
author Musaya, Janelisa
Matovu, Enock
Senga, Edward
Nyirenda, Moffat
Chisi, John
author_facet Musaya, Janelisa
Matovu, Enock
Senga, Edward
Nyirenda, Moffat
Chisi, John
author_sort Musaya, Janelisa
collection PubMed
description BACKGROUND: Anaemia commonly results from destruction of erythrocytes in the peripheral blood and failure of the bone marrow haematopoietic cells to replenish the erythrocytes. The mechanisms involved in trypanosoma-induced anaemia, including the role of the bone marrow haematopoietic cells are incompletely understood. We studied the responses of a tetrapeptide, AcSDKP, and IL-10, and their association with bone marrow nucleated cells in a Trypanosoma brucei brucei GVR35 experimental infection model. METHODS: Mouse infection was done intraperitoneally with 1 × 10(3) trypanosomes/mL. Mice were either infected or left uninfected (N = 100). At days 0, 9, 16, 23, 30, 37, and 44 post-infection, mice were euthanised and blood was collected by cardiac puncture to examine for parasitaemia and packed cell volume (PCV) and then centrifuged for plasma, which was used for cytokine ELISA. The mice's femurs were also dissected and bone marrow was collected for femur cellularity. RESULTS: PCV dropped from 39.6% to 27% in infected animals by day 9 and remained low (relative to uninfected mice) for the duration of the experiment. AcSDKP levels decreased from day 0 (11.5 × 104 pg/mL) to day 16 (10 × 104), and increased by day 30 (12.6 × 104). There was a significant difference at day 16 (P = 0.023) between the infected and uninfected groups. By contrast, expression of IL-10 markedly increased between day 0 (18.6 pg/mL) and day 16 (145 pg/mL) and decreased by day 30 (42.8 pg/mL). There was also a significant difference in IL-10 expression between infected and uninfected mice at day 16 (P < 0.001). Bone marrow nucleated cells were significantly reduced during periods of low plasma AcSDKP and high plasma IL-10 concentrations (5.4 × 106 infected vs 6.2 × 106 on day 0 and 4.9 × 106 infected vs 10 × 106 uninfected on day 16). CONCLUSIONS: These data unravel a possible negative feedback interaction between AcSDKP and IL-10 in trypanosome infection. More importantly, this study implicates an IL-10/AcSDKP cytokine network in the regulation of bone marrow nucleated cells and provides a new potential mechanism in the pathogenesis of trypanosoma-induced anaemia. Further mechanistic blocking experiments on AcSDKP and IL-10 are recommended to further clarify understanding of the interaction.
format Online
Article
Text
id pubmed-5811999
institution National Center for Biotechnology Information
language English
publishDate 2017
publisher The Medical Association Of Malawi
record_format MEDLINE/PubMed
spelling pubmed-58119992018-06-05 AcSDKP is down-regulated in anaemia induced by Trypanosoma brucei infection in mice Musaya, Janelisa Matovu, Enock Senga, Edward Nyirenda, Moffat Chisi, John Malawi Med J Original Research BACKGROUND: Anaemia commonly results from destruction of erythrocytes in the peripheral blood and failure of the bone marrow haematopoietic cells to replenish the erythrocytes. The mechanisms involved in trypanosoma-induced anaemia, including the role of the bone marrow haematopoietic cells are incompletely understood. We studied the responses of a tetrapeptide, AcSDKP, and IL-10, and their association with bone marrow nucleated cells in a Trypanosoma brucei brucei GVR35 experimental infection model. METHODS: Mouse infection was done intraperitoneally with 1 × 10(3) trypanosomes/mL. Mice were either infected or left uninfected (N = 100). At days 0, 9, 16, 23, 30, 37, and 44 post-infection, mice were euthanised and blood was collected by cardiac puncture to examine for parasitaemia and packed cell volume (PCV) and then centrifuged for plasma, which was used for cytokine ELISA. The mice's femurs were also dissected and bone marrow was collected for femur cellularity. RESULTS: PCV dropped from 39.6% to 27% in infected animals by day 9 and remained low (relative to uninfected mice) for the duration of the experiment. AcSDKP levels decreased from day 0 (11.5 × 104 pg/mL) to day 16 (10 × 104), and increased by day 30 (12.6 × 104). There was a significant difference at day 16 (P = 0.023) between the infected and uninfected groups. By contrast, expression of IL-10 markedly increased between day 0 (18.6 pg/mL) and day 16 (145 pg/mL) and decreased by day 30 (42.8 pg/mL). There was also a significant difference in IL-10 expression between infected and uninfected mice at day 16 (P < 0.001). Bone marrow nucleated cells were significantly reduced during periods of low plasma AcSDKP and high plasma IL-10 concentrations (5.4 × 106 infected vs 6.2 × 106 on day 0 and 4.9 × 106 infected vs 10 × 106 uninfected on day 16). CONCLUSIONS: These data unravel a possible negative feedback interaction between AcSDKP and IL-10 in trypanosome infection. More importantly, this study implicates an IL-10/AcSDKP cytokine network in the regulation of bone marrow nucleated cells and provides a new potential mechanism in the pathogenesis of trypanosoma-induced anaemia. Further mechanistic blocking experiments on AcSDKP and IL-10 are recommended to further clarify understanding of the interaction. The Medical Association Of Malawi 2017-09 /pmc/articles/PMC5811999/ /pubmed/29872517 http://dx.doi.org/10.4314/mmj.v29i3.6 Text en 2017 The College of Medicine and the Medical Association of Malawi © 2017 The College of Medicine and the Medical Association of Malawi. This work is licensed under the Creative Commons Attribution 4.0 International License. This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/)
spellingShingle Original Research
Musaya, Janelisa
Matovu, Enock
Senga, Edward
Nyirenda, Moffat
Chisi, John
AcSDKP is down-regulated in anaemia induced by Trypanosoma brucei infection in mice
title AcSDKP is down-regulated in anaemia induced by Trypanosoma brucei infection in mice
title_full AcSDKP is down-regulated in anaemia induced by Trypanosoma brucei infection in mice
title_fullStr AcSDKP is down-regulated in anaemia induced by Trypanosoma brucei infection in mice
title_full_unstemmed AcSDKP is down-regulated in anaemia induced by Trypanosoma brucei infection in mice
title_short AcSDKP is down-regulated in anaemia induced by Trypanosoma brucei infection in mice
title_sort acsdkp is down-regulated in anaemia induced by trypanosoma brucei infection in mice
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5811999/
https://www.ncbi.nlm.nih.gov/pubmed/29872517
http://dx.doi.org/10.4314/mmj.v29i3.6
work_keys_str_mv AT musayajanelisa acsdkpisdownregulatedinanaemiainducedbytrypanosomabruceiinfectioninmice
AT matovuenock acsdkpisdownregulatedinanaemiainducedbytrypanosomabruceiinfectioninmice
AT sengaedward acsdkpisdownregulatedinanaemiainducedbytrypanosomabruceiinfectioninmice
AT nyirendamoffat acsdkpisdownregulatedinanaemiainducedbytrypanosomabruceiinfectioninmice
AT chisijohn acsdkpisdownregulatedinanaemiainducedbytrypanosomabruceiinfectioninmice

Ejemplares similares