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RhoA targeting by probiotics as strategy to interfere the critical link to major hallmarks of Alzheimer disease / Muhammad Zaki Ramli

Alzheimer’s disease (AD) is the commonest form of dementia characterised by aggregation of amyloid beta (Aβ) plaque. RhoA, which is being increasingly recognised for its role in AD pathogenesis through the amyloidogenic pathway, may serve as a potential therapeutic target. Preliminary screening of M...

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Main Author: Ramli, Muhammad Zaki
Format: Thesis
Language:English
Published: 2019
Online Access:https://ir.uitm.edu.my/id/eprint/84010/1/84010.pdf
https://ir.uitm.edu.my/id/eprint/84010/
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spelling my.uitm.ir.840102023-11-29T09:22:06Z https://ir.uitm.edu.my/id/eprint/84010/ RhoA targeting by probiotics as strategy to interfere the critical link to major hallmarks of Alzheimer disease / Muhammad Zaki Ramli Ramli, Muhammad Zaki Alzheimer’s disease (AD) is the commonest form of dementia characterised by aggregation of amyloid beta (Aβ) plaque. RhoA, which is being increasingly recognised for its role in AD pathogenesis through the amyloidogenic pathway, may serve as a potential therapeutic target. Preliminary screening of MRS broth fermented with lactic acid bacteria (LAB) yielded strain-dependent inhibition of RhoA activation in vitro. LAB also significantly inhibited Aβ produced by SK-N-SH transfected with amyloid precursor protein (APP) gene. A strong correlation was found between inhibition of RhoA and Aβ. LAB-derived supernatant were also presented with increased organic acids which included lactic acid (>100%), acetic acid (>15.3%), butyric acid (>34.5%) and propionic acid (>29.1%). The findings were validated using lipopolysaccharide (LPS)-challenged rats with neuroinflammation that mimic AD. Sprague Dawley rats (male, 3 months) were divided (n=6/group) into wild-type, control, vehicle controls and treatment groups [109 CFU/ mL LAB6/ Pediococus pentasaceus or LAB12/ Lactobacillus plantarum and 10 mg/kg ibuprofen (positive control) for 31 days]. Except for wild-type, all rats were injected (i.p.) with 0.25 mg/kg LPS for 4 days starting from day 28. The rodents were then subjected to the Morris Water Maze Test. Brains were harvested and subjected to Western Blot, immunohistostaining and biochemical analyses. LAB-fed LPS-challenged rats exhibited significantly (p<0.05) reduced escape latency and escape distance. They remained longer in the platform quadrant (>9.8±0.5 sec) when compared to control (<5.1±1.9 sec). The improved memory was accompanied by significantly (p<0.05) decreased Aβ (<31.4%) and RhoA activity (<22.5%), augmented BDNF (>15.4%) and ACh (>32.3%), reduced AChE (<40.1%) and NO (<30.3%) levels. LAB-fed rats also showed increased IL-10 (>32.1%) and decreased IL-1β (<39.5%). The LAB was then investigated using Aβ-induced rats that mimic Aβ plaque aggregation in AD. Sprague Dawley rats (male, 3 months) were divided (n=7/group) into wild-type, sham, control, vehicle controls and treatment groups. Except for wild type and sham, all rats were subjected to intracranial injection with 5 μg/μL Aβ 1-42 peptide. Treatment groups (day 4) were administered with either 109 CFU/mL LAB6, LAB12 or 10 mg/kg ibuprofen for 30 days. The Aβ-induced rats were assessed for parameters similar to those of LPS-challenged rats. LAB-fed rats exhibited significantly (p<0.05) reduced escape latency, escape distance and remained longer in platform quadrant. The improved memory was accompanied by reduced Aβ (<31.4%) and RhoA activity (<35.7%), increased BDNF (>18.3%) and ACh (>30.3%), reduced AChE (<28.8%) and NO (<33.6%). LAB-fed rats also exhibited up-regulation of IL-10 (>33.3%) and down-regulation of IL-1β (<41.6%). The present findings indicated that LAB-induced neuroprotection could be mediated via inhibition of RhoA-Aβ generated neuroinflammation and accompanied by increased production of organic acid metabolites, restored BDNF, reduced degradation of acetylcholine and down-regulation of pro-inflammatory as well as up-regulation of anti-inflammatory cytokines. 2019 Thesis NonPeerReviewed text en https://ir.uitm.edu.my/id/eprint/84010/1/84010.pdf RhoA targeting by probiotics as strategy to interfere the critical link to major hallmarks of Alzheimer disease / Muhammad Zaki Ramli. (2019) PhD thesis, thesis, Universiti Teknologi MARA (UiTM).
institution Universiti Teknologi Mara
building Tun Abdul Razak Library
collection Institutional Repository
continent Asia
country Malaysia
content_provider Universiti Teknologi Mara
content_source UiTM Institutional Repository
url_provider http://ir.uitm.edu.my/
language English
description Alzheimer’s disease (AD) is the commonest form of dementia characterised by aggregation of amyloid beta (Aβ) plaque. RhoA, which is being increasingly recognised for its role in AD pathogenesis through the amyloidogenic pathway, may serve as a potential therapeutic target. Preliminary screening of MRS broth fermented with lactic acid bacteria (LAB) yielded strain-dependent inhibition of RhoA activation in vitro. LAB also significantly inhibited Aβ produced by SK-N-SH transfected with amyloid precursor protein (APP) gene. A strong correlation was found between inhibition of RhoA and Aβ. LAB-derived supernatant were also presented with increased organic acids which included lactic acid (>100%), acetic acid (>15.3%), butyric acid (>34.5%) and propionic acid (>29.1%). The findings were validated using lipopolysaccharide (LPS)-challenged rats with neuroinflammation that mimic AD. Sprague Dawley rats (male, 3 months) were divided (n=6/group) into wild-type, control, vehicle controls and treatment groups [109 CFU/ mL LAB6/ Pediococus pentasaceus or LAB12/ Lactobacillus plantarum and 10 mg/kg ibuprofen (positive control) for 31 days]. Except for wild-type, all rats were injected (i.p.) with 0.25 mg/kg LPS for 4 days starting from day 28. The rodents were then subjected to the Morris Water Maze Test. Brains were harvested and subjected to Western Blot, immunohistostaining and biochemical analyses. LAB-fed LPS-challenged rats exhibited significantly (p<0.05) reduced escape latency and escape distance. They remained longer in the platform quadrant (>9.8±0.5 sec) when compared to control (<5.1±1.9 sec). The improved memory was accompanied by significantly (p<0.05) decreased Aβ (<31.4%) and RhoA activity (<22.5%), augmented BDNF (>15.4%) and ACh (>32.3%), reduced AChE (<40.1%) and NO (<30.3%) levels. LAB-fed rats also showed increased IL-10 (>32.1%) and decreased IL-1β (<39.5%). The LAB was then investigated using Aβ-induced rats that mimic Aβ plaque aggregation in AD. Sprague Dawley rats (male, 3 months) were divided (n=7/group) into wild-type, sham, control, vehicle controls and treatment groups. Except for wild type and sham, all rats were subjected to intracranial injection with 5 μg/μL Aβ 1-42 peptide. Treatment groups (day 4) were administered with either 109 CFU/mL LAB6, LAB12 or 10 mg/kg ibuprofen for 30 days. The Aβ-induced rats were assessed for parameters similar to those of LPS-challenged rats. LAB-fed rats exhibited significantly (p<0.05) reduced escape latency, escape distance and remained longer in platform quadrant. The improved memory was accompanied by reduced Aβ (<31.4%) and RhoA activity (<35.7%), increased BDNF (>18.3%) and ACh (>30.3%), reduced AChE (<28.8%) and NO (<33.6%). LAB-fed rats also exhibited up-regulation of IL-10 (>33.3%) and down-regulation of IL-1β (<41.6%). The present findings indicated that LAB-induced neuroprotection could be mediated via inhibition of RhoA-Aβ generated neuroinflammation and accompanied by increased production of organic acid metabolites, restored BDNF, reduced degradation of acetylcholine and down-regulation of pro-inflammatory as well as up-regulation of anti-inflammatory cytokines.
format Thesis
author Ramli, Muhammad Zaki
spellingShingle Ramli, Muhammad Zaki
RhoA targeting by probiotics as strategy to interfere the critical link to major hallmarks of Alzheimer disease / Muhammad Zaki Ramli
author_facet Ramli, Muhammad Zaki
author_sort Ramli, Muhammad Zaki
title RhoA targeting by probiotics as strategy to interfere the critical link to major hallmarks of Alzheimer disease / Muhammad Zaki Ramli
title_short RhoA targeting by probiotics as strategy to interfere the critical link to major hallmarks of Alzheimer disease / Muhammad Zaki Ramli
title_full RhoA targeting by probiotics as strategy to interfere the critical link to major hallmarks of Alzheimer disease / Muhammad Zaki Ramli
title_fullStr RhoA targeting by probiotics as strategy to interfere the critical link to major hallmarks of Alzheimer disease / Muhammad Zaki Ramli
title_full_unstemmed RhoA targeting by probiotics as strategy to interfere the critical link to major hallmarks of Alzheimer disease / Muhammad Zaki Ramli
title_sort rhoa targeting by probiotics as strategy to interfere the critical link to major hallmarks of alzheimer disease / muhammad zaki ramli
publishDate 2019
url https://ir.uitm.edu.my/id/eprint/84010/1/84010.pdf
https://ir.uitm.edu.my/id/eprint/84010/
_version_ 1783950436097589248
score 13.214268

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